Updated on 2024/11/14

写真a

 
HIRASAWA Akira
 
Organization
Faculty of Medicine, Dentistry and Pharmaceutical Sciences Professor
Position
Professor
External link

Degree

  • M.D,Ph.D. ( 2004.3   Keio University )

Research Areas

  • Life Science / System genome science

  • Life Science / Tumor diagnostics and therapeutics

  • Life Science / Tumor biology

Education

  • 慶應義塾大学大学院   医学研究科博士課程  

    - 2004.3

      More details

  • Keio University   医学部  

    1989.4 - 1995.3

      More details

Research History

  • Department of Clinical Genomic Medicine. Graduate School of Medicine, Dentistry and Pharmaceutical Sciences, Okayama University   Professor

    2018.6

      More details

  • 慶應義塾大学医学部産婦人科 専任講師

    2015.4

      More details

  • 日本学術振興会二国間交流事業オープンパートナーシップ共同研究 日本側研究代表者, Institute for Molecular Medicine Finland, Senior Researcher (フィンランドアカデミー)

    2014.7

      More details

  • 慶應義塾大学医学部産婦人科 特任講師

    2013.1

      More details

  • 日本学術振興会 特定国派遣研究者事業 平成24年度特定国派遣研究者 Institute for Molecular Medicine Finland, visiting researcher

    2012.4

      More details

  • 日本学術振興会 組織的な若手研究者等海外派遣プログラムInstitute for Molecular Medicine Finland, 日本学術振興会 組織的な若手研究者等海外派遣プログラム Institute for Molecular Medicine Finland, visiting researcher

    2011.10

      More details

  • 慶應義塾大学医学部臨床遺伝学センター センター員(併任)

    2011.8

      More details

  • 慶應義塾大学医学部産婦人科学助教(助手)・診療医長(婦人科)

    2005.9

      More details

  • 独立行政法人国立病院機構東京医療センター(産婦人科)

    2004.4 - 2005.8

      More details

  • 栃木県立がんセンター研究所(研修医)

    2002.7

      More details

  • 東京医科歯科大学難治疾患研究所遺伝疾患研究部門 (分子細胞遺伝)共同研究者

    2000.6

      More details

  • 慶應義塾大学医学部助手(専修医)

    1999.11 - 2004.3

      More details

  • 芳賀赤十字病院(産婦人科)

    1999.9 - 1999.10

      More details

  • 慶應義塾大学医学部助手(専修医)(産婦人科学)

    1998.6 - 1999.8

      More details

  • 大田原赤十字病院(産婦人科)

    1997.6 - 1998.5

      More details

  • 国立埼玉病院(産婦人科)

    1996.6 - 1997.5

      More details

  • 慶應義塾大学医学部研修医(産婦人科)

    1995.5 - 1996.5

      More details

▼display all

Professional Memberships

▼display all

Committee Memberships

  • 日本臨床薬理学会   保険委員会 委員  

    2023.1   

      More details

    Committee type:Academic society

    researchmap

  • 厚生労働省   がんゲノム医療中核拠点病院等の指定に関する検討会 委員  

    2022.12 - 2024.3   

      More details

    Committee type:Government

    researchmap

  • 一般社団法人日本遺伝性乳癌卵巣癌総合診療制度機構   ガイドライン作成統括委員(遺伝領域)  

    2022.11 - 2025.10   

      More details

    Committee type:Other

    researchmap

  • 日本婦人科腫瘍学会   子宮体がん治療ガイドライン2023 評価委員  

    2022.8 - 2023.3   

      More details

    Committee type:Academic society

    researchmap

  • 日本遺伝性腫瘍学会   理事、学術・教育委員会委員長  

    2022.6   

      More details

    Committee type:Academic society

    researchmap

  • 岡山県臨床細胞学会   学術委員会 委員  

    2022.4   

      More details

    Committee type:Academic society

    researchmap

  • 一般社団法人 日本臨床検査医学会 医療政策委員会   遺伝子関連検査に関する小委員会 委員  

    2022.4   

      More details

    Committee type:Academic society

    researchmap

  • 臨床検査振興協議会   遺伝子関連検査に関する小委員会 委員  

    2022.4   

      More details

  • 厚生労働省   がんゲノム医療中核拠点病院等の指定要件に関するワーキンググループ 構成員  

    2021.12   

      More details

    Committee type:Government

    researchmap

  • 日本学術会議   連携会員  

    2020.10   

      More details

  • 一般社団法人日本遺伝性乳癌卵巣癌総合診療制度機構   理事・広報部会長  

    2020.6   

      More details

  • 日本婦人科腫瘍学会   がんゲノム医療、HBOC診療の適正化に関するWG委員  

    2020.6   

      More details

  • HBOC診療ガイドライン作成委員   遺伝診断・遺伝カウンセリング 領域リーダー  

    2020.3   

      More details

  • 日本癌学会   評議員  

    2020.1   

      More details

  • 日本産科婦人科学会   PGT-Mに関する倫理審議会 委員  

    2019.12   

      More details

  • 日本産科婦人科遺伝診療学会   理事  

    2019.12   

      More details

  • 日本人類遺伝学会   理事  

    2019.10   

      More details

  • 日本婦人科腫瘍学会   卵巣がん治療ガイドライン2020年版評価委員  

    2019.5   

      More details

  • 日本遺伝カウンセリング学会   倫理問題検討委員会 委員  

    2019.4   

      More details

  • 成人・小児進行固形がんにおける臓器横断的ゲノム診療のガイドライン   作成委員  

    2019.4   

      More details

  • 日本遺伝カウンセリング学会   遺伝学的検査委員会 委員  

    2019.4   

      More details

  • クリニカルバイオバンク学会   理事  

    2019.3   

      More details

  • 日本臨床薬理学会   指導医  

    2018.10   

      More details

  • 全国遺伝子医療部門連絡会議   理事  

    2018.10   

      More details

  • 日本家族性腫瘍学会 (現 日本遺伝性腫瘍学会)   学術・教育委員会 委員長  

    2018.6   

      More details

  • 厚生労働科学研究費補助金(がん対策推進総合研究事業) 「希少癌診療ガイドラインの作成を通した医療提供体制の質向上」「進行固形腫瘍患者におけるDNAミスマッチ修復機能欠損検査ガイドライン作成プロジェクト」   プロジェクトメンバー  

    2018.1   

      More details

  • 日本家族性腫瘍学会(現 日本遺伝性腫瘍学会)   家族性腫瘍指導医(現 遺伝性腫瘍指導医)  

    2017.10   

      More details

  • 日本婦人科腫瘍学会   修練カリキュラム・教育プログラム改訂委員  

    2017.9   

      More details

  • 日本婦人科腫瘍学会   PARP阻害薬使用における遺伝学的検査の実施体制等に関する検討委員会  

    2017.9   

      More details

  • 日本産科婦人科遺伝診療学会   認定制度ワーキンググループ  

    2017.4   

      More details

  • 日本家族性腫瘍学会   学術・教育委員会委員  

    2017.4   

      More details

  • Ovarian Cancer Association Consortium (OCAC)   委員  

    2017.1   

      More details

  • 日本婦人科腫瘍学会   査読委員  

    2016.8   

      More details

  • 日本家族性腫瘍学会   編集委員会委員  

    2016.6   

      More details

  • 遺伝性乳癌卵巣癌症候群診療の手引き(厚生労働科研 がん対策推進総合研究事業「わが国における遺伝性乳癌卵巣癌の臨床遺伝学的特徴の解明と遺伝子情報を用いた生命予後の改善に関する研究」研究班)   作製委員  

    2016.6   

      More details

  • 日本遺伝性腫瘍学会   評議員  

    2016.6   

      More details

  • ホルモン補充療法ガイドライン2017年度版   作成委員  

    2016.4   

      More details

  • Taiwan Precision Medicine Society   Honor board member  

    2015.12   

      More details

  • 日本女性医学学会   代議員  

    2015.11   

      More details

  • 日本人類遺伝学会   評議員  

    2015.10   

      More details

  • 遺伝性大腸癌診療ガイドライン   作成委員  

    2015.9   

      More details

  • 日本産科婦人科遺伝診療学会   幹事  

    2015.7   

      More details

  • Evidence-based Network for the Interpretation of Germline Mutant Alleles (ENIGMA)   委員  

    2015.7   

      More details

  • 日本産科婦人科学会 婦人科腫瘍委員会 遺伝性乳癌卵巣癌(HBOC)の啓発および取り扱い小委員会   委員  

    2015.4   

      More details

  • 東京産科婦人科学会   評議員  

    2015.4   

      More details

  • 日本産科婦人科学会ガイドライン婦人科外来編 ガイドライン   作成員  

    2014.11   

      More details

  • 日本HBOCコンソーシアム   評議員  

    2013.1   

      More details

  • 日本婦人科腫瘍学会 婦人科腫瘍   専門医  

    2013.1   

      More details

  • 日本女性医学学会   認定医  

    2011.10   

      More details

    Committee type:Academic society

    researchmap

  • 日本がん治療認定医機構   がん治療認定医  

    2009.3   

      More details

    Committee type:Other

    researchmap

  • 日本がん治療認定医機構   暫定教育医  

    2007.8   

      More details

    Committee type:Other

    researchmap

  • 日本臨床細胞学会   評議員  

    2007.4   

      More details

    Committee type:Academic society

    researchmap

  • 日本産科婦人科学会東京地方部会   編集幹事  

    2006.4 - 2011.8   

      More details

    Committee type:Academic society

    researchmap

  • 日本婦人科腫瘍学会   評議員  

    2006.4   

      More details

    Committee type:Academic society

    researchmap

  • 日本人類遺伝学会   臨床遺伝専門医制度専門医  

    2004.12   

      More details

    Committee type:Academic society

    researchmap

  • 日本臨床細胞学会   細胞診専門医  

    2003.12   

      More details

    Committee type:Academic society

    researchmap

  • 日本産科婦人科学会   専門医  

    2000.10   

      More details

    Committee type:Academic society

    researchmap

▼display all

 

Papers

  • Nationwide survey of the secondary findings in cancer genomic profiling: survey including liquid biopsy. International journal

    Saki Shimada, Takahiro Yamada, Akari Minamoto, Manami Matsukawa, Ichiro Yabe, Hiroshi Tada, Katsutoshi Oda, Arisa Ueki, Satomi Higashigawa, Maki Morikawa, Yuki Sato, Akira Hirasawa, Masanobu Ogawa, Tomohiro Kondo, Masahiro Yoshioka, Masashi Kanai, Manabu Muto, Shinji Kosugi

    Journal of human genetics   2024.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    We surveyed the status of the secondary finding (SF) disclosure in comprehensive genome profiling (CGP) in 2020. The situation has changed: increase in the number of hospitals that provide CGP, an update to the Comprehensive Tumor Genomic Profiling: Materials for Review of Secondary Findings (CTGPMRSF), and the addition of a liquid biopsy test, FoundationOne® Liquid CDx (F1L). Moreover, the actual situation was unclear because the 2020 survey did not include all designated and cooperative hospitals. Herein, we conducted a questionnaire survey of all designated-core, designated, and cooperative hospitals to identify the current status and challenges concerning SF in the CGP in 2022. A total of 82.1% of the hospitals responded and 77.7% of the response was from cooperative hospitals. Approximately 80% of the hospitals used CTGPMRSF. SF disclosure, confirmatory test implementation, and SF confirmation rates were 12.4%, 31.6%, and 46.6% for FoundationOne® CDx (F1CDx), respectively, and 6.8%, 31.8%, and 70.7% for F1L, respectively. The implementation rate of the confirmatory test was substantially higher in hospitals with genetic experts and in hospitals that could conduct confirmatory tests on the same day. Our survey provides insight into how SF is handled in Japan. The percentage of cases leading to confirmatory tests has gradually increased, although challenges such as insurance coverage limitations and varied understanding of SF among patients and healthcare providers persist. With the increasing use of whole-genome analysis, our findings will provide valuable insights into establishing an effective SF disclosure system.

    DOI: 10.1038/s10038-024-01294-x

    PubMed

    researchmap

  • [Diagnosis of Hereditary Tumors Using Multi Gene Panel Testing(MGPT)-Current Status and Issues in Japan or Worldwide].

    Akira Hirasawa

    Gan to kagaku ryoho. Cancer & chemotherapy   51 ( 7 )   677 - 680   2024.7

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    Pathogenic variant carriers of hereditary tumors have the risk of developing cancer in multiple organs, and genetic testing can be used as an opportunity to conduct surveillance for early detection of cancer and to prevent the development of new cancers and it becomes possible to develop individualized preventive strategies including risk-reductive surgery. Multi gene panel testing(MGPT), which simultaneously measures several dozen to more than 100 genes, has been widely used to diagnose of hereditary tumors in worldwide since around 2014. Although, MGPTs has not been approved under the Pharmaceutical and Medical Devices Act in Japan. MGPTs for hereditary tumors can be expected to become the mainstream of diagnosis for hereditary tumors in near future.

    PubMed

    researchmap

  • 神経線維腫症1型を中心とした遺伝性骨・軟部腫瘍に対する専門外来の有用性

    中田 英二, 二川 摩周, 平沢 晃, 山本 英喜, 国定 俊之, 板野 拓人, 藤原 智洋, 尾崎 敏文

    日本整形外科学会雑誌   98 ( 6 )   S1614 - S1614   2024.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • 多職種から見た骨・軟部腫瘍治療の現状と課題 肉腫発生ハイリスク患者に対する遺伝性骨・軟部腫瘍外来の取り組み

    二川 摩周, 中田 英二, 山本 英喜, 深野 智華, 加藤 芙美乃, 大住 理沙, 藤原 智洋, 国定 俊之, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   98 ( 6 )   S1579 - S1579   2024.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • 加速する骨・軟部腫瘍に対するゲノム医療: 現状と課題 肉腫におけるゲノム医療の現状と課題

    中田 英二, 遠西 大輔, 二宮 貴一朗, 山本 英喜, 冨田 秀太, 藤原 智洋, 国定 俊之, 平沢 晃, 豊岡 伸一, 尾崎 敏文

    日本整形外科学会雑誌   98 ( 6 )   S1457 - S1457   2024.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • Assessing the efficacy of target adaptive sampling long-read sequencing through hereditary cancer patient genomes. International journal

    Wataru Nakamura, Makoto Hirata, Satoyo Oda, Kenichi Chiba, Ai Okada, Raúl Nicolás Mateos, Masahiro Sugawa, Naoko Iida, Mineko Ushiama, Noriko Tanabe, Hiromi Sakamoto, Shigeki Sekine, Akira Hirasawa, Yosuke Kawai, Katsushi Tokunaga, Shin-Ichi Tsujimoto, Norio Shiba, Shuichi Ito, Teruhiko Yoshida, Yuichi Shiraishi

    NPJ genomic medicine   9 ( 1 )   11 - 11   2024.2

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Innovations in sequencing technology have led to the discovery of novel mutations that cause inherited diseases. However, many patients with suspected genetic diseases remain undiagnosed. Long-read sequencing technologies are expected to significantly improve the diagnostic rate by overcoming the limitations of short-read sequencing. In addition, Oxford Nanopore Technologies (ONT) offers adaptive sampling and computationally driven target enrichment technology. This enables more affordable intensive analysis of target gene regions compared to standard non-selective long-read sequencing. In this study, we developed an efficient computational workflow for target adaptive sampling long-read sequencing (TAS-LRS) and evaluated it through application to 33 genomes collected from suspected hereditary cancer patients. Our workflow can identify single nucleotide variants with nearly the same accuracy as the short-read platform and elucidate complex forms of structural variations. We also newly identified several SINE-R/VNTR/Alu (SVA) elements affecting the APC gene in two patients with familial adenomatous polyposis, as well as their sites of origin. In addition, we demonstrated that off-target reads from adaptive sampling, which is typically discarded, can be effectively used to accurately genotype common single-nucleotide polymorphisms (SNPs) across the entire genome, enabling the calculation of a polygenic risk score. Furthermore, we identified allele-specific MLH1 promoter hypermethylation in a Lynch syndrome patient. In summary, our workflow with TAS-LRS can simultaneously capture monogenic risk variants including complex structural variations, polygenic background as well as epigenetic alterations, and will be an efficient platform for genetic disease research and diagnosis.

    DOI: 10.1038/s41525-024-00394-z

    PubMed

    researchmap

  • 神経線維腫症1型患者由来ヒトiPS細胞株の樹立

    大澤 太郎, 中田 英二, 岡本 真幸, 山田 大祐, 二川 摩周, 高尾 知佳, 平沢 晃, 尾崎 敏文, 宝田 剛志

    日本レックリングハウゼン病学会学術大会プログラム・抄録集   15回   24 - 24   2024.2

     More details

    Language:Japanese   Publisher:日本レックリングハウゼン病学会  

    researchmap

  • Patient survey on cancer genomic medicine in Japan under the national health insurance system. International journal

    Hidenori Kage, Nana Akiyama, Hyangri Chang, Aya Shinozaki-Ushiku, Mirei Ka, Junichi Kawata, Manabu Muto, Yusuke Okuma, Natsuko Okita, Katsuya Tsuchihara, Junko Kikuchi, Hidekazu Shirota, Hideyuki Hayashi, Toshio Kokuryo, Shinichi Yachida, Akira Hirasawa, Makoto Kubo, Hirotsugu Kenmotsu, Masahiko Tanabe, Tetsuo Ushiku, Kaori Muto, Yasuyuki Seto, Katsutoshi Oda

    Cancer science   115 ( 3 )   954 - 962   2024.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    In Japan, comprehensive genomic profiling (CGP) tests have been reimbursed under the national health care system for solid cancer patients who have finished standard treatment. More than 50,000 patients have taken the test since June 2019. We performed a nation-wide questionnaire survey between March 2021 and July 2022. Questionnaires were sent to 80 designated Cancer Genomic Medicine Hospitals. Of the 933 responses received, 370 (39.7%) were web based and 563 (60.3%) were paper based. Most patients (784, 84%) first learned about CGP tests from healthcare professionals, and 775 (83.1%) gave informed consent to their treating physician. At the time of informed consent, they were most worried about test results not leading to novel treatment (536, 57.4%). On a scale of 0-10, 702 respondents (75.2%) felt that the explanations of the test result were easy to understand (7 or higher). Ninety-one patients (9.8%) started their recommended treatment. Many patients could not receive recommended treatment because no approved drugs or clinical trials were available (102/177, 57.6%). Ninety-eight patients (10.5%) did not wish their findings to be disclosed. Overall satisfaction with the CGP test process was high, with 602 respondents (64.5%) giving a score of 7-10. The major reason for choosing 0-6 was that the CGP test result did not lead to new treatment (217/277, 78.3%). In conclusion, satisfaction with the CGP test process was high. Patients and family members need better access to information. More patients need to be treated with genomically matched therapy.

    DOI: 10.1111/cas.16065

    PubMed

    researchmap

  • Ligneous periodontitis exacerbated by Behçet's disease in a patient with plasminogen deficiency and a stop-gained variant PLG c.1468C > T: a case report. International journal

    Yuki Shinoda-Ito, Anna Hirai, Kazuhiro Omori, Hidetaka Ideguchi, Hideki Yamamoto, Fumino Kato, Kyoichi Obata, Tatsuo Ogawa, Keisuke Nakano, Takato Nakadoi, Eri Katsuyama, Soichiro Ibaragi, Tadashi Yamamoto, Hitoshi Nagatsuka, Akira Hirasawa, Shogo Takashiba

    BMC oral health   23 ( 1 )   843 - 843   2023.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: Plasminogen serves as the precursor to plasmin, an essential element in the fibrinolytic process, and is synthesized primarily in the liver. Plasminogen activation occurs through the action of plasminogen activator, converting it into plasmin. This conversion greatly enhances the fibrinolytic system within tissues and blood vessels, facilitating the dissolution of fibrin clots. Consequently, congenital deficiency of plasminogen results in impaired fibrin degradation. Patients with plasminogen deficiency typically exhibit fibrin deposits in various mucosal sites throughout the body, including the oral cavity, eyes, vagina, and digestive organs. Behcet's disease is a chronic recurrent systemic inflammatory disease with four main symptoms: aphthous ulcers of the oral mucosa, vulvar ulcers, skin symptoms, and eye symptoms, and has been reported worldwide. This disease is highly prevalent around the Silk Road from the Mediterranean to East Asia. We report a case of periodontitis in a patient with these two rare diseases that worsened quickly, leading to alveolar bone destruction. Genetic testing revealed a novel variant characterized by a stop-gain mutation, which may be a previously unidentified etiologic gene associated with decreased plasminogen activity. CASE PRESENTATION: This case report depicts a patient diagnosed with ligneous gingivitis during childhood, originating from plasminogen deficiency and progressing to periodontitis. Genetic testing revealed a suspected association with the PLG c.1468C > T (p.Arg490*) stop-gain mutation. The patient's periodontal condition remained stable with brief intervals of supportive periodontal therapy. However, the emergence of Behçet's disease induced acute systemic inflammation, necessitating hospitalization and treatment with steroids. During hospitalization, the dental approach focused on maintaining oral hygiene and alleviating contact-related pain. The patient's overall health improved with inpatient care and the periodontal tissues deteriorated. CONCLUSIONS: Collaborative efforts between medical and dental professionals are paramount in comprehensively evaluating and treating patients with intricate complications from rare diseases. Furthermore, the PLG c.1468C > T (p.Arg490*) stop-gain mutation could contribute to the association between plasminogen deficiency and related conditions.

    DOI: 10.1186/s12903-023-03586-8

    PubMed

    researchmap

  • 多遺伝子パネル検査を用いて治療方針を決定した若年の非浸潤性乳管癌患者の一例

    鈴木 陽子, 岩谷 胤生, 仁科 卓也, 吉本 皓一, 宇野 摩耶, 中本 翔伍, 高橋 侑子, 突沖 貴宏, 岩本 高行, 伊波 茂道, 平沢 晃, 枝園 忠彦

    日本臨床外科学会雑誌   84 ( 11 )   1830 - 1830   2023.11

     More details

    Language:Japanese   Publisher:日本臨床外科学会  

    J-GLOBAL

    researchmap

  • 多遺伝子パネル検査を用いて治療方針を決定した若年の非浸潤性乳管癌患者の一例

    鈴木 陽子, 岩谷 胤生, 仁科 卓也, 吉本 皓一, 宇野 摩耶, 中本 翔伍, 高橋 侑子, 突沖 貴宏, 岩本 高行, 伊波 茂道, 平沢 晃, 枝園 忠彦

    日本臨床外科学会雑誌   84 ( 11 )   1830 - 1830   2023.11

     More details

    Language:Japanese   Publisher:日本臨床外科学会  

    researchmap

  • ベーチェット病を併発したプラスミノーゲン低下症に伴うLigneous歯周炎患者の臨床的・遺伝学的考察

    平井 杏奈, 伊東 有希, 井手口 英隆, 大森 一弘, 加藤 芙美乃, 山本 英喜, 平沢 晃, 山本 直史, 高柴 正悟

    日本歯周病学会会誌   65 ( 秋季特別 )   178 - 178   2023.10

     More details

    Language:Japanese   Publisher:(NPO)日本歯周病学会  

    researchmap

  • がんゲノムプロファイリング検査のための超音波内視鏡下採取膵癌組織でのMOSEの取組み

    永谷 たみ, 小倉 千尋, 下舞 裕美, 廣尾 嘉樹, 春名 勝也, 木村 祥佳, 堀田 真智子, 伏見 聡一郎, 井上 博文, 平沢 晃, 和仁 洋治

    日本臨床細胞学会雑誌   62 ( Suppl.2 )   536 - 536   2023.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • ベーチェット病を併発したプラスミノーゲン低下症に伴うLigneous歯周炎患者の臨床的・遺伝学的考察

    平井 杏奈, 伊東 有希, 井手口 英隆, 大森 一弘, 加藤 芙美乃, 山本 英喜, 平沢 晃, 山本 直史, 高柴 正悟

    日本歯周病学会会誌   65 ( 秋季特別 )   178 - 178   2023.10

     More details

    Language:Japanese   Publisher:(NPO)日本歯周病学会  

    researchmap

  • When and how to enlighten citizens on genetics and hereditary cancer: a web survey of online video viewers. International journal

    Reimi Sogawa, Takahito Wada, Noriyuki Yamashita, Mariko Kochi, Mashu Futagawa, Fumino Kato, Yusaku Urakawa, Yayoi Tanimura, Hideki Yamamoto, Shuta Tomida, Shinji Kosugi, Akira Hirasawa

    Journal of community genetics   14 ( 6 )   575 - 581   2023.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    With the rapid expansion of genomic medicine, more citizens are compelled to think about genetics in their daily lives. This study aims to explore appropriate types of educational media and methods to enlighten activities for genetics and hereditary cancer. We presented an 18-min YouTube video on genetics and hereditary cancer to participants at a scientific event, Science Agora 2020, and administered a web questionnaire to investigate their opinions about when and how citizens should start learning about genetics and hereditary cancer. We recruited 133 participants who watched the video, and 26.3% (35/133) responded to the questionnaire. Most of them were evaluated to understand and appreciate the contents of the video. They identified websites, or videos as suitable learning media, irrespective of their sex, age, or profession. They highlighted upper elementary school or junior high school as appropriate educational stages to start learning about genetics and hereditary cancer to facilitate collecting their own genetic information by themselves. Our findings show that educational institutions should provide opportunities to learn about genetics and hereditary cancers, especially for upper elementary school and junior high school students, using learning media, such as videos, depending on their level or demand.

    DOI: 10.1007/s12687-023-00663-x

    PubMed

    researchmap

  • Comprehensive genomic profiling of Japanese patients with thoracic malignancies: A single-center retrospective study. International journal

    Tetsu Hirakawa, Mihoko Doi, Kosuke Hamai, Ryo Katsura, Shinya Miyake, Suguru Fujita, Sayaka Ueno, Ken Masuda, Takuya Tanimoto, Takashi Nishisaka, Takao Hinoi, Akira Hirasawa, Nobuhisa Ishikawa

    Respiratory investigation   61 ( 6 )   746 - 754   2023.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: Few studies have been conducted on comprehensive genomic profiling (CGP) panels in Japanese patients with thoracic malignancies after completing standard treatment. Consequently, its value in clinical practice remains unclear. METHODS: We conducted a retrospective study of Japanese patients with thoracic malignancies who underwent CGP between June 2019 and November 2022 at our hospital. We evaluated the detection rate of actionable genetic alterations and percentage of patients who received genomically-matched therapy. Furthermore, we examined the value of the CGP panel in patients who underwent multiplex gene-panel testing prior to their initial treatment. This study was performed in accordance with the principles of the Declaration of Helsinki. RESULTS: The study included 56 patients, of whom 47 (83.9%) had actionable genetic alterations and 8 (14.3%) received genomically-matched therapy. Of these, four patients were treated with approved drugs and three patients were treated with investigational agents. In addition, one patient was treated with approved drugs using the patient-directed care system. Of the 17 patients who had multiplex gene-panel testing performed at the start of their initial therapy, two (11.8%) were newly identified by the CGP panel and subsequently received genomically-matched therapy. EGFR L718Q and MET amplification were observed in two of the seven patients with epidermal growth factor receptor-tyrosine kinase inhibitor resistance. CONCLUSIONS: The CGP panel could identify genetic alterations, thereby facilitating genomically-matched therapy, even in patients with thoracic malignancies who could not be identified using multiplex gene-panel testing.

    DOI: 10.1016/j.resinv.2023.08.005

    PubMed

    researchmap

  • Proposal for combined macroscopic and microscopic on-site evaluation (cMOSES) of fresh tissue from liver tumor biopsies for histopathological diagnosis and comprehensive genomic panel testing. International journal

    Tami Nagatani, Yoji Wani, Soichiro Fushimi, Yu Matsuo, Shiho Murakami, Toshifumi Tada, Shinichiro Nakamura, Hirofumi Inoue, Maki Tanioka, Hiroyuki Okada, Akira Hirasawa

    Pathology international   73 ( 12 )   612 - 614   2023.9

     More details

    Language:English  

    DOI: 10.1111/pin.13377

    PubMed

    researchmap

  • 網羅的がんゲノム医療時代の遺伝性腫瘍診療と遺伝カウンセリング 遺伝性腫瘍のリスク評価・診断のための多遺伝子パネル検査受検例の施設横断的な検討(Hereditary tumor syndromes and genetic counseling in the era of cancer genomic medicine Cross-institutional case review of multi-gene panel testing for risk assessments and diagnosis of hereditary tumors)

    山本 英喜, 藤田 裕子, 田村 和朗, 浦川 優作, 二川 摩周, 十川 麗美, 加藤 芙美乃, 植野 さやか, 重安 邦俊, 原賀 順子, 小川 千加子, 河内 麻里子, 深野 智華, 甲斐 恭平, 塩崎 滋弘, 平沢 晃

    日本癌学会総会記事   82回   821 - 821   2023.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • Japanese Society of Medical Oncology/Japan Society of Clinical Oncology/Japanese Society of Pediatric Hematology/Oncology-led clinical recommendations on the diagnosis and use of immunotherapy in patients with DNA mismatch repair deficient (dMMR) tumors, third edition.

    Saori Mishima, Yoichi Naito, Kiwamu Akagi, Naomi Hayashi, Akira Hirasawa, Tomoro Hishiki, Ataru Igarashi, Masafumi Ikeda, Shigenori Kadowaki, Hiroaki Kajiyama, Motohiro Kato, Hirotsugu Kenmotsu, Yasuhiro Kodera, Keigo Komine, Takafumi Koyama, Osamu Maeda, Mitsuru Miyachi, Hiroshi Nishihara, Hiroyuki Nishiyama, Shouichi Ohga, Wataru Okamoto, Eiji Oki, Shigeru Ono, Masashi Sanada, Ikuo Sekine, Tadao Takano, Kayoko Tao, Keita Terashima, Katsuya Tsuchihara, Yasushi Yatabe, Takayuki Yoshino, Eishi Baba

    International journal of clinical oncology   28 ( 10 )   1237 - 1258   2023.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: Clinical trials have reported the efficacy of immune checkpoint inhibitors in the treatment of mismatch repair-deficient (dMMR) advanced solid tumors. The accumulated evidence of tumor agnostic agent has been made since PD-1 inhibitor was approved and used in clinical practice. Therefore, we have revised the guideline "Japan Society of Clinical Oncology provisional clinical opinion for the diagnosis and use of immunotherapy in patients with deficient DNA mismatch repair tumors, cooperated by Japanese Society of Medical Oncology, First Edition". METHODS: Clinical questions regarding medical care were formulated for patients with dMMR advanced solid tumors. Relevant publications were searched by PubMed and Cochrane Database. Critical publications and conference reports were added manually. Systematic reviews were performed for each clinical question for the purpose of developing clinical recommendations. The committee members identified by Japan Society of Clinical Oncology (JSCO), Japanese Society of Medical Oncology (JSMO), and Japanese society of pediatric hematology/oncology (JSPHO) voted to determine the level of each recommendation considering the strength of evidence, expected risks and benefits to patients, and other related factors. Thereafter, a peer review by experts nominated from JSCO, JSMO, and JSPHO and the public comments among all societies' members were done. RESULTS: The current guideline describes two clinical questions and eight recommendations for whom, when, and how MMR status should be tested. CONCLUSION: In this guideline, the committee proposed eight recommendations for performing MMR testing properly to select patients who are likely to benefit from immunotherapy.

    DOI: 10.1007/s10147-023-02397-9

    PubMed

    researchmap

  • Japanese Society of Medical Oncology/Japan Society of Clinical Oncology/Japanese Society of Pediatric Hematology/Oncology-led clinical recommendations on the diagnosis and use of immunotherapy in patients with high tumor mutational burden tumors.

    Saori Mishima, Yoichi Naito, Kiwamu Akagi, Naomi Hayashi, Akira Hirasawa, Tomoro Hishiki, Ataru Igarashi, Masafumi Ikeda, Shigenori Kadowaki, Hiroaki Kajiyama, Motohiro Kato, Hirotsugu Kenmotsu, Yasuhiro Kodera, Keigo Komine, Takafumi Koyama, Osamu Maeda, Mitsuru Miyachi, Hiroshi Nishihara, Hiroyuki Nishiyama, Shouichi Ohga, Wataru Okamoto, Eiji Oki, Shigeru Ono, Masashi Sanada, Ikuo Sekine, Tadao Takano, Kayoko Tao, Keita Terashima, Katsuya Tsuchihara, Yasushi Yatabe, Takayuki Yoshino, Eishi Baba

    International journal of clinical oncology   28 ( 8 )   941 - 955   2023.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    The development of novel antitumor agents and accompanying biomarkers has improved survival across several tumor types. Previously, we developed recommendations for tumor-agnostic treatments in patients with solid tumors with DNA mismatch repair deficient or neurotrophic receptor tyrosine kinase fusions. Recently, immune checkpoint inhibitors have shown efficacy in patient with tumor mutation burden-high (TMB-H) solid tumors and have been established as a third tumor-agnostic agent, making it necessary to develop the guideline prioritized for these patients. Clinical questions regarding medical care were formulated for patients with TMB-H advanced solid tumors. Relevant publications were searched by PubMed and Cochrane Database. Critical publications and conference reports were added manually. Systematic reviews were performed for each clinical question for the purpose of developing clinical recommendations. The committee members identified by Japan Society of Clinical Oncology (JSCO), Japanese Society of Medical Oncology (JSMO), and Japanese society of pediatric hematology/oncology (JSPHO) voted to determine the level of each recommendation considering the strength of evidence, expected risks and benefits to patients, and other related factors. Thereafter, a peer review by experts nominated from JSCO, JSMO, and JSPHO, and the public comments among all societies' members was done. The current guideline describes three clinical questions and seven recommendations for whom, when, and how TMB should be tested, and what is recommended for patients with TMB-H advanced solid tumors. In this guideline, the committee proposed seven recommendations for performing TMB testing properly to select patients who are likely to benefit from immunotherapy.

    DOI: 10.1007/s10147-023-02360-8

    PubMed

    researchmap

  • 肉腫診療におけるがん遺伝子パネルの有用性

    中田 英二, 藤原 智洋, 国定 俊之, 遠西 大輔, 山本 英喜, 二宮 貴一朗, 冨田 秀太, 二川 摩周, 平沢 晃, 豊岡 伸一, 尾崎 敏文

    日本整形外科学会雑誌   97 ( 8 )   S1894 - S1894   2023.8

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • A case of ovarian carcinosarcoma with a germline pathogenic variant of BRCA2 involving a perforated appendix with an abscess. International journal

    Ayaka Saito, Eiko Yamashita, Urara Sakurai, Akira Hirasawa, Maki Tanioka, Kazuya Tamura, Satoshi Umezawa

    The journal of obstetrics and gynaecology research   49 ( 10 )   2553 - 2557   2023.7

     More details

    Language:English  

    We report a case of rare and aggressive ovarian carcinosarcoma with a germline pathogenic BRCA2 variant. A patient with a history of breast cancer who developed an inflammatory ovarian tumor with peritonitis carcinomatosis involving the appendix suffered from cachexia. Following three cycles of weekly paclitaxel and carboplatin chemotherapy, emergency surgery was required owing to sepsis. Bilateral salpingo-oophorectomy, total hysterectomy, appendectomy, and small intestine adhesiolysis were performed. Histologically, the tumor comprised an admixture of carcinomatous and sarcomatous components, with involvement of the appendix, which had caused perforation and abscess formation. The final diagnosis was ovarian carcinosarcoma with a germline pathogenic BRCA2 variant, c.658_659del (p.Val220fs). The patient responded completely to adjuvant chemotherapy. A combination of chemotherapy and surgery might be beneficial to patients with ovarian carcinosarcoma and germline pathogenic BRCA2 variants with a poor general condition. This is the first report of ovarian carcinosarcoma with a germline pathogenic BRCA2 variant that responded favorably to chemotherapy.

    DOI: 10.1111/jog.15736

    PubMed

    researchmap

  • Japanese Society of Medical Oncology/Japan Society of Clinical Oncology/Japanese Society of Pediatric Hematology/Oncology-led clinical recommendations on the diagnosis and use of tropomyosin receptor kinase inhibitors in adult and pediatric patients with neurotrophic receptor tyrosine kinase fusion-positive advanced solid tumors.

    Yoichi Naito, Saori Mishima, Kiwamu Akagi, Naomi Hayashi, Akira Hirasawa, Tomoro Hishiki, Ataru Igarashi, Masafumi Ikeda, Shigenori Kadowaki, Hiroaki Kajiyama, Motohiro Kato, Hirotsugu Kenmotsu, Yasuhiro Kodera, Keigo Komine, Takafumi Koyama, Osamu Maeda, Mitsuru Miyachi, Hiroshi Nishihara, Hiroyuki Nishiyama, Shouichi Ohga, Wataru Okamoto, Eiji Oki, Shigeru Ono, Masashi Sanada, Ikuo Sekine, Tadao Takano, Kayoko Tao, Keita Terashima, Katsuya Tsuchihara, Yasushi Yatabe, Takayuki Yoshino, Eishi Baba

    International journal of clinical oncology   28 ( 7 )   827 - 840   2023.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: Clinical trials have reported the efficacy of tropomyosin receptor kinase (TRK) inhibitors against neurotrophic receptor tyrosine kinase (NTRK) fusion gene-positive advanced solid tumors. The accumulated evidence of tumor-agnostic agent has made since TRK inhibitors were approved and used in clinical practice. Therefore, we have revised the 'Japan Society of Clinical Oncology (JSCO)/Japanese Society of Medical Oncology (JSMO)-led clinical recommendations on the diagnosis and use of tropomyosin receptor kinase inhibitors in adult and pediatric patients with neurotrophic receptor tyrosine kinase fusion-positive advanced solid tumors, cooperated by the Japanese Society of Pediatric Hematology/Oncology (JSPHO)'. METHODS: Clinical questions regarding medical care were formulated for patients with NTRK fusion-positive advanced solid tumors. Relevant publications were searched by PubMed and Cochrane Database. Critical publications and conference reports were added manually. Systematic reviews were performed for each clinical question for the purpose of developing clinical recommendations. The committee members identified by JSCO, JSMO, and JSPHO voted to determine the level of each recommendation considering the strength of evidence, expected risks and benefits to patients, and other related factors. Thereafter, a peer review by experts nominated from JSCO, JSMO, and JSPHO, and the public comments among all societies' members was done. RESULTS: The current guideline describes 3 clinical questions and 14 recommendations for whom, when, and how NTRK fusion should be tested, and what is recommended for patients with NTRK fusion-positive advanced solid tumors. CONCLUSION: The committee proposed 14 recommendations for performing NTRK testing properly to select patients who are likely to benefit from TRK inhibitors.

    DOI: 10.1007/s10147-023-02345-7

    PubMed

    researchmap

  • 婦人科遺伝性腫瘍とデータシェアリング Invited

    平沢 晃

    HORMONE FRONTIER IN GYNECOLOGY   30 ( 2 )   45 - 52   2023.6

     More details

    Authorship:Lead author   Language:Japanese  

    J-GLOBAL

    researchmap

  • Survey of the Current Status of the Secondary Findings Disclosure Process for Tumor Genomic Profiling: A Multicenter Questionnaire Survey

    島田咲, 島田咲, 山田崇弘, 山田崇弘, 山田崇弘, 源明理, 松川愛未, 松川愛未, 矢部一郎, 青木洋子, 織田克利, 植木有紗, 東川智美, 森川真紀, 佐藤友紀, 平沢晃, 小川昌宣, 小川昌宣, 近藤知大, 吉岡正博, 金井雅史, 武藤学, 小杉眞司, 松川愛未, 矢部一郎, 青木洋子, 織田克利, 植木有紗, 東川智美, 森川真紀, 佐藤友紀, 平沢晃, 小川昌宣, 近藤知大, 吉岡正博, 金井雅史, 小杉眞司

    日本遺伝カウンセリング学会誌   44 ( 2 )   92 - 92   2023.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Human resources for administrative work to carry out a comprehensive genomic profiling test in Japan. International journal

    Hidenori Kage, Katsutoshi Oda, Manabu Muto, Katsuya Tsuchihara, Natsuko Okita, Yusuke Okuma, Junko Kikuchi, Hidekazu Shirota, Hideyuki Hayashi, Toshio Kokuryo, Daisuke Sakai, Akira Hirasawa, Makoto Kubo, Hirotsugu Kenmotsu, Nana Akiyama, Aya Shinozaki-Ushiku, Masahiko Tanabe, Tetsuo Ushiku, Kiyoshi Miyagawa, Yasuyuki Seto

    Cancer science   114 ( 7 )   3041 - 3049   2023.5

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Comprehensive genomic profiling (CGP) tests have been nationally reimbursed in Japan since June 2019 under strict restrictions, and over 46,000 patients have taken the test. Core Hospitals and Designated Hospitals host molecular tumor boards, which is more time-consuming than simply participating in them. We sent a questionnaire to government-designated Cancer Genomic Medicine Hospitals, including all 12 Core Hospitals, all 33 Designated Hospitals, and 117 of 188 Cooperative Hospitals. The questionnaire asked how much time physicians and nonphysicians spent on administrative work for cancer genomic medicine. For every CGP test, 7.6 h of administrative work was needed. Physicians spent 2.7 h/patient, while nonphysicians spent 4.9 h/patient. Time spent preparing for molecular tumor boards, called Expert Panels, was the longest, followed by time spent participating in Expert Panels. Assuming an hourly wage of \24,000/h for physicians and \2800/h for nonphysicians, mean labor cost was \78,071/patient. On a monthly basis, more time was spent on administrative work at Core Hospitals compared with Designated Hospitals and Cooperative Hospitals (385 vs. 166 vs. 51 h/month, respectively, p < 0.001). Consequently, labor cost per month was higher at Core Hospitals than at Designated Hospitals and Cooperative Hospitals (\3,951,854 vs. \1,687,167 vs. \487,279/month, respectively, p < 0.001). Completing a CGP test for a cancer patient in Japan is associated with significant labor at each hospital, especially at Core Hospitals. Streamlining the exchange of information and simplifying Expert Panels will likely alleviate this burden.

    DOI: 10.1111/cas.15833

    PubMed

    researchmap

  • 今,再考するROSEの意義 EUS-FNA検体のゲノム医療における有用性と限界

    井上 博文, 松岡 博美, 實平 悦子, 松岡 昌志, 安村 早優美, 田中 健大, 寺澤 裕之, 松本 和幸, 加藤 博也, 平沢 晃

    日本臨床細胞学会雑誌   62 ( Suppl.1 )   187 - 187   2023.5

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 今,再考するROSEの意義 EUS-FNA検体のゲノム医療における有用性と限界

    井上 博文, 松岡 博美, 實平 悦子, 松岡 昌志, 安村 早優美, 田中 健大, 寺澤 裕之, 松本 和幸, 加藤 博也, 平沢 晃

    日本臨床細胞学会雑誌   62 ( Suppl.1 )   187 - 187   2023.5

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • マイクロアレイ染色体検査にてCharcot-Marie-Tooth病責任領域の重複が認められたMiller-Dieker症候群の遺伝カウンセリング

    十川 麗美, 秋山 倫之, 衛藤 英理子, 二川 摩周, 加藤 芙美乃, 山本 英喜, 平沢 晃, 大守 伊織, 小林 勝弘

    脳と発達   55 ( Suppl. )   S302 - S302   2023.5

     More details

    Language:Japanese   Publisher:(一社)日本小児神経学会  

    researchmap

  • The DNA integrity number and concentration are useful parameters for successful comprehensive genomic profiling test for cancer using formalin-fixed paraffin embedded tissue. International journal

    Emmy Yanagita, Hiroshi Yamada, Tetsuro Kobayashi, Eriko Aimono, Kohei Nakamura, Akira Hirasawa, Hiroshi Nishihara

    Pathology international   73 ( 5 )   198 - 206   2023.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    The acquisition of high-quality biospecimens and the appropriate handling of these materials are indispensable for successful clinical sequencing. We developed a cancer clinical sequencing system targeting 160 cancer genes: PleSSision-Rapid. Through the PleSSision-Rapid system, we have analyzed DNA quality evaluated by DIN (DNA integrity number) with 1329 formalin-fixed paraffin embedded (FFPE) samples including 477 prospectively collected tissues for genomic test (P) and 852 archival samples after routine pathological diagnosis (A1/A2). As a result, the samples with more than DIN 2.1 was 92.0% (439/477) in prospectively collected sample (P), while it was 85.6% (332/388) and 76.7% (356/464) in two types of archival samples (A1/A2). We performed the PleSSision-Rapid sequence using the samples with over DIN 2.1 and DNA concentration >10 ng/μL with which we were able to construct a DNA library, and the probability of sequence success was almost equivalent during all types of specimen processing, at 90.7% (398/439) in (P), 92.5% (307/332) in (A1) and 90.2% (321/356) in (A2), respectively. Our result indicated the clinical benefit to prepare the prospective collection of FFPE materials for indisputable clinical sequence, and that DIN ≥ 2.1 would be a solid parameter for sample preparation of comprehensive genomic profiling tests.

    DOI: 10.1111/pin.13318

    PubMed

    researchmap

  • [Ⅲ. The Role of Comprehensive Genomic Profiling in Sarcoma].

    Eiji Nakata, Tomohiro Fujiwara, Toshiyuki Kunisada, Toshifumi Ozaki, Shinichi Toyooka, Daisuke Ennishi, Hideki Yamamoto, Kiichiro Ninomiya, Shuta Tomida, Akira Hirasawa, Mashu Futagawa, Masahiro Tabata

    Gan to kagaku ryoho. Cancer & chemotherapy   50 ( 3 )   314 - 320   2023.3

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    PubMed

    researchmap

  • CCNE1 and survival of patients with tubo-ovarian high-grade serous carcinoma: An Ovarian Tumor Tissue Analysis consortium study. International journal

    Eun-Young Kang, Ashley Weir, Nicola S Meagher, Kyo Farrington, Gregg S Nelson, Prafull Ghatage, Cheng-Han Lee, Marjorie J Riggan, Adelyn Bolithon, Gordana Popovic, Betty Leung, Katrina Tang, Neil Lambie, Joshua Millstein, Jennifer Alsop, Michael S Anglesio, Beyhan Ataseven, Ellen Barlow, Matthias W Beckmann, Jessica Berger, Christiani Bisinotto, Hans Bösmüller, Jessica Boros, Alison H Brand, Angela Brooks-Wilson, Sara Y Brucker, Michael E Carney, Yovanni Casablanca, Alicia Cazorla-Jiménez, Paul A Cohen, Thomas P Conrads, Linda S Cook, Penny Coulson, Madeleine Courtney-Brooks, Daniel W Cramer, Philip Crowe, Julie M Cunningham, Cezary Cybulski, Kathleen M Darcy, Mona A El-Bahrawy, Esther Elishaev, Ramona Erber, Rhonda Farrell, Sian Fereday, Anna Fischer, María J García, Simon A Gayther, Aleksandra Gentry-Maharaj, C Blake Gilks, Marcel Grube, Paul R Harnett, Shariska Petersen Harrington, Philipp Harter, Arndt Hartmann, Jonathan L Hecht, Sebastian Heikaus, Alexander Hein, Florian Heitz, Joy Hendley, Brenda Y Hernandez, Susanna Hernando Polo, Sabine Heublein, Akira Hirasawa, Estrid Høgdall, Claus K Høgdall, Hugo M Horlings, David G Huntsman, Tomasz Huzarski, Andrea Jewell, Mercedes Jimenez-Linan, Michael E Jones, Scott H Kaufmann, Catherine J Kennedy, Dineo Khabele, Felix K F Kommoss, Roy F P M Kruitwagen, Diether Lambrechts, Nhu D Le, Marcin Lener, Jenny Lester, Yee Leung, Anna Linder, Liselore Loverix, Jan Lubiński, Rashna Madan, G Larry Maxwell, Francesmary Modugno, Susan L Neuhausen, Alexander Olawaiye, Siel Olbrecht, Sandra Orsulic, José Palacios, Celeste Leigh Pearce, Malcolm C Pike, Carmel M Quinn, Ganendra Raj Mohan, Cristina Rodríguez-Antona, Matthias Ruebner, Andy Ryan, Stuart G Salfinger, Naoko Sasamoto, Joellen M Schildkraut, Minouk J Schoemaker, Mitul Shah, Raghwa Sharma, Yurii B Shvetsov, Naveena Singh, Gabe S Sonke, Linda Steele, Colin J R Stewart, Karin Sundfeldt, Anthony J Swerdlow, Aline Talhouk, Adeline Tan, Sarah E Taylor, Kathryn L Terry, Aleksandra Tołoczko, Nadia Traficante, Koen K Van de Vijver, Maaike A van der Aa, Toon Van Gorp, Els Van Nieuwenhuysen, Lilian van-Wagensveld, Ignace Vergote, Robert A Vierkant, Chen Wang, Lynne R Wilkens, Stacey J Winham, Anna H Wu, Javier Benitez, Andrew Berchuck, Francisco J Candido Dos Reis, Anna DeFazio, Peter A Fasching, Ellen L Goode, Marc T Goodman, Jacek Gronwald, Beth Y Karlan, Stefan Kommoss, Usha Menon, Hans-Peter Sinn, Annette Staebler, James D Brenton, David D Bowtell, Paul D P Pharoah, Susan J Ramus, Martin Köbel

    Cancer   129 ( 5 )   697 - 713   2022.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: Cyclin E1 (CCNE1) is a potential predictive marker and therapeutic target in tubo-ovarian high-grade serous carcinoma (HGSC). Smaller studies have revealed unfavorable associations for CCNE1 amplification and CCNE1 overexpression with survival, but to date no large-scale, histotype-specific validation has been performed. The hypothesis was that high-level amplification of CCNE1 and CCNE1 overexpression, as well as a combination of the two, are linked to shorter overall survival in HGSC. METHODS: Within the Ovarian Tumor Tissue Analysis consortium, amplification status and protein level in 3029 HGSC cases and mRNA expression in 2419 samples were investigated. RESULTS: High-level amplification (>8 copies by chromogenic in situ hybridization) was found in 8.6% of HGSC and overexpression (>60% with at least 5% demonstrating strong intensity by immunohistochemistry) was found in 22.4%. CCNE1 high-level amplification and overexpression both were linked to shorter overall survival in multivariate survival analysis adjusted for age and stage, with hazard stratification by study (hazard ratio [HR], 1.26; 95% CI, 1.08-1.47, p = .034, and HR, 1.18; 95% CI, 1.05-1.32, p = .015, respectively). This was also true for cases with combined high-level amplification/overexpression (HR, 1.26; 95% CI, 1.09-1.47, p = .033). CCNE1 mRNA expression was not associated with overall survival (HR, 1.00 per 1-SD increase; 95% CI, 0.94-1.06; p = .58). CCNE1 high-level amplification is mutually exclusive with the presence of germline BRCA1/2 pathogenic variants and shows an inverse association to RB1 loss. CONCLUSION: This study provides large-scale validation that CCNE1 high-level amplification is associated with shorter survival, supporting its utility as a prognostic biomarker in HGSC.

    DOI: 10.1002/cncr.34582

    PubMed

    researchmap

  • Drug response profiles in patient-derived cancer cells across histological subtypes of ovarian cancer: real-time therapy tailoring for a patient with low-grade serous carcinoma. International journal

    Astrid Murumägi, Daniela Ungureanu, Suleiman Khan, Mariliina Arjama, Katja Välimäki, Aleksandr Ianevski, Philipp Ianevski, Rebecka Bergström, Alice Dini, Anna Kanerva, Riitta Koivisto-Korander, Johanna Tapper, Heini Lassus, Mikko Loukovaara, Andrus Mägi, Akira Hirasawa, Daisuke Aoki, Vilja Pietiäinen, Teijo Pellinen, Ralf Bützow, Tero Aittokallio, Olli Kallioniemi

    British journal of cancer   128 ( 4 )   678 - 690   2022.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Many efforts are underway to develop novel therapies against the aggressive high-grade serous ovarian cancers (HGSOCs), while our understanding of treatment options for low-grade (LGSOC) or mucinous (MUCOC) of ovarian malignancies is not developing as well. We describe here a functional precision oncology (fPO) strategy in epithelial ovarian cancers (EOC), which involves high-throughput drug testing of patient-derived ovarian cancer cells (PDCs) with a library of 526 oncology drugs, combined with genomic and transcriptomic profiling. HGSOC, LGSOC and MUCOC PDCs had statistically different overall drug response profiles, with LGSOCs responding better to targeted inhibitors than HGSOCs. We identified several subtype-specific drug responses, such as LGSOC PDCs showing high sensitivity to MDM2, ERBB2/EGFR inhibitors, MUCOC PDCs to MEK inhibitors, whereas HGSOCs showed strongest effects with CHK1 inhibitors and SMAC mimetics. We also explored several drug combinations and found that the dual inhibition of MEK and SHP2 was synergistic in MAPK-driven EOCs. We describe a clinical case study, where real-time fPO analysis of samples from a patient with metastatic, chemorefractory LGSOC with a CLU-NRG1 fusion guided clinical therapy selection. fPO-tailored therapy with afatinib, followed by trastuzumab and pertuzumab, successfully reduced tumour burden and blocked disease progression over a five-year period. In summary, fPO is a powerful approach for the identification of systematic drug response differences across EOC subtypes, as well as to highlight patient-specific drug regimens that could help to optimise therapies to individual patients in the future.

    DOI: 10.1038/s41416-022-02067-z

    PubMed

    researchmap

  • Handling of Germline Findings in Clinical Comprehensive Cancer Genomic Profiling.

    Mika Okazawa-Sakai, Yasuko Yamamoto, Mashu Futagawa, Miki Okamura, Satoko Miyawaki, Tomohiro Nishina, Kazuhiro Takehara, Toshiyuki Kozuki, Shuta Tomida, Ichinosuke Hyodo, Shozo Ohsumi, Akira Hirasawa

    Acta medica Okayama   76 ( 6 )   673 - 678   2022.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Patients found to have presumed germline pathogenic variants (PGPVs) during comprehensive genomic profiling (CGP) require genetic counseling (GC) referrals. We retrospectively investigated the outcomes of patients with PGPVs. Among 159 patients who underwent CGP, we recommended GC for the 16 patients with PGPVs (3 with [FG group] and 13 without [G Group] a family/personal history of hereditary cancer) as well as for the 8 patients with no PGPVs, but a history (F group); 2 (67%), 5 (38%), and 3 (38%) patients received GC in the FG, G, and F groups, respectively. Germline testing results were positive in 1 and 2 patients of the FG and G groups, respectively. Among the patients recommended for GC, 58% did not receive GC due to lack of interest, poor performance status, or death. CGP contributes to the identification of germline variants in patients without a history of hereditary cancer. However, the proportion of patients who undergo GC should be improved.

    DOI: 10.18926/AMO/64117

    PubMed

    researchmap

  • がんゲノムプロファイリング検査による大腸癌でのBRAF阻害薬の適応判断

    山本 英喜, 重安 邦俊, 河内 麻里子, 座間味 義人, 平沢 晃

    日本臨床薬理学会学術総会抄録集   43回   1 - 6   2022.12

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    J-GLOBAL

    researchmap

  • RAS/BRAF解析においてPCR-rSSO法とNGS法の併用による補完性が示された大腸癌の二例

    山本 英喜, 重安 邦俊, 柳井 広之, 井上 博文, 松岡 博美, 青江 伯規, 東影 明人, 藤井 敬子, 大塚 文男, 草野 展周, 平沢 晃

    日本臨床検査医学会誌   70 ( 補冊 )   258 - 258   2022.10

     More details

    Language:Japanese   Publisher:(一社)日本臨床検査医学会  

    J-GLOBAL

    researchmap

  • [The Cooperation with Medical Staff, Medical Staff and Patients, and Patients and Their Families in Cancer Precision Medicine].

    Akira Hirasawa

    Gan to kagaku ryoho. Cancer & chemotherapy   49 ( 9 )   1000 - 1001   2022.9

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    The cooperation among medical staff, medical staff and patients, and patients and their families is important in cancer precision medicine. Cancer prevention based on genomic information should lead national cancer death as defined of cancer precision medicine in Japan.

    PubMed

    J-GLOBAL

    researchmap

  • がんゲノム医療における「連携」 主に患者、家族・血縁者との連携にかかる課題について 全国がんプロ協議会・ゲノム医療部会報告

    平沢 晃

    癌と化学療法   49 ( 9 )   1000 - 1001   2022.9

     More details

    Language:Japanese   Publisher:(株)癌と化学療法社  

    医療者間の連携、医療者と患者の連携および患者と家族間の連携はがん診療全般でも必要事項ではあり、がんゲノム医療のもつ特性を考えた連携を構築することが望ましい。わが国のがんゲノム医療の定義で提唱されているとおり、がん未発症者を含むがん発症予防が可能になって初めて国民の確実ながん死低減が可能になる。(著者抄録)

    researchmap

  • 骨・軟部肉腫に対するがんゲノムプロファイリング検査から検出されるpresumed germline pathogenic variantsの意義

    二川 摩周, 中田 英二, 十川 麗美, 加藤 芙美乃, 浦川 優作, 河内 麻里子, 山本 英喜, 藤原 智洋, 国定 俊之, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 8 )   S1770 - S1770   2022.9

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • [Panel Discussion - Problems in the Cancer Genomic Medicine].

    Chikashi Ishioka, Manabu Muto, Shinichi Yachida, Hidekazu Shirota, Akira Hirasawa, Kiyoshi Miyagawa, Kazuto Ashizawa, Ichiro Kinoshita, Hiroshi Nishihara, Nariaki Matsuura, Akihiro Sakurai

    Gan to kagaku ryoho. Cancer & chemotherapy   49 ( 9 )   1014 - 1017   2022.9

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    About 4 and a half years have passed since"Cancer Genome Medicine"was first mentioned in the Third Phase of the Basic Plan to Promote Cancer Control Programs that started in October 2017. Currently, cancer genomic medicine is being carried out by the cancer gene panel test, which is covered by public insurance, mainly at the 12 Cancer Genome Medicine Core Center Hospital designated nationwide by the Ministry of Health, Labor, and Welfare in Japan. Cancer genomic medicine has come to be positioned as a standard medical treatment. However, there are various challenges in operating an expert panel that professionally examines the results of the gene panel tests and reports treatment recommendations and secondary findings that suggest hereditary tumors. In addition, there is an urgent need to disseminate and educate healthcare professionals and patients about cancer genomic medicine. In this panel discussion on January 14, 2022, 10 panelists discussed how to solve these issues and the prospects for the future.

    PubMed

    researchmap

  • 骨・軟部腫瘍の基礎科学のトピックス クリニカルシークエンスによる肉腫のゲノム医療

    中田 英二, 藤原 智洋, 国定 俊之, 二川 摩周, 遠西 大輔, 久保 寿夫, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 8 )   S1533 - S1533   2022.9

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • Liquid Biopsy Revealed HBOC Pedigree and Led to Medical Management Among the Relatives.

    Chikako Ogawa, Akira Hirasawa, Reimi Sogawa, Kayoko Hasuoka, Shuta Tomida, Mashu Futagawa, Yusaku Urakawa, Mariko Kochi, Hideki Yamamoto, Keiichiro Nakamura, Hisashi Masuyama

    Acta medica Okayama   76 ( 4 )   479 - 483   2022.8

     More details

    Language:English  

    A hereditary breast and ovarian cancer (HBOC) pedigree was detected via liquid biopsy, and cancer prevention was initiated for the patient's daughter, after receiving a definitive result from BRCA genetic testing. A 48-yearold woman with ovarian cancer was administered precision medicine, which used cell-free DNA from plasma. The results revealed a pathogenic variant of BRCA1 as a presumed germline pathogenic mutation. We confirmed the germline pathological variant BRCA1 c.81-1G> A and suggested treatment with a PARP inhibitor. One of her three children had the variant, was diagnosed as an unaffected pathogenic variant carrier, and was advised to initiate surveillance.

    DOI: 10.18926/AMO/63908

    PubMed

    researchmap

  • Alteration in peritoneal cells with the chemokine CX3CL1 reverses age-associated impairment of recognition memory. International journal

    Yoshinori Takei, Yoko Amagase, Keiko Iida, Tomohiro Sagawa, Ai Goto, Ryuichi Kambayashi, Hiroko Izumi-Nakaseko, Akio Matsumoto, Shinichi Kawai, Atsushi Sugiyama, Tatsuyuki Takada, Akira Hirasawa

    GeroScience   44 ( 4 )   2305 - 2318   2022.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Cognitive function progressively declines with advancing age. The aging process can be promoted by obesity and attenuated by exercise. Both conditions affect levels of the chemokine CX3CL1 in peripheral tissues; however, its role in cognitive aging is unknown. In the current study, we administered CX3CL1 into the peritoneal cavity of aged mice to investigate its impact on the aging process. In the peritoneal cavity, CX3CL1 not only reversed the age-associated accumulation of cells expressing the senescence marker p16INK4a but also increased peritoneal phagocytic activity, indicating that CX3CL1 affected the phenotypes of peritoneal cells. In the hippocampus of aged mice, intraperitoneal administration of CX3CL1 increased the number of Type-2 neural stem cells and promoted brain-derived neurotrophic factor (BDNF) expression. This treatment, furthermore, improved novel object recognition memory impaired with advancing age. Intraperitoneal transplantation of peritoneal cells from CX3CL1-treated aged mice improved novel object recognition memory in recipient aged mice. It indicates that peritoneal cells have a critical role in the CX3CL1-induced improvement of recognition memory in aged mice. Vagotomy inhibited the CX3CL1-induced increase in BDNF expression, demonstrating that the vagus nerve is involved in the hippocampal BDNF expression induced by intraperitoneal administration of CX3CL1. Thus, our results demonstrate that a novel connection among the peritoneal cells, the vagus nerve, and the hippocampus can reverse the age-associated decline in recognition memory.

    DOI: 10.1007/s11357-022-00579-3

    PubMed

    researchmap

  • がん遺伝子パネル検査の現状と課題 がんゲノム医療overview 国民のがん死低減をめざして

    平沢 晃

    日本婦人科腫瘍学会雑誌   40 ( 3 )   120 - 124   2022.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    がんゲノム医療は「がん患者の腫瘍部および正常部のゲノム情報を用いて治療の最適化・予後予測・発症予防をおこなう医療(未発症者も対象とすることがある。またゲノム以外のマルチオミックス情報も含める)」と定義される(がんゲノム医療推進コンソーシアム懇談会報告書〜国民参加型がんゲノム医療の構築に向けて〜厚生労働省HP平成29年6月27日)。「治療の最適化」についてはがん医療へコンパニオン診断の導入から、2019年6月のがん遺伝子パネル検査の保険収載を契機に、個別化治療に到達する道筋が整備されてきている。一方でがんゲノム医療は定義にあるように「がん未発症者」を含む「がん発症予防」を含む概念である。がん発症高リスクのがん未発症者に対する介入が可能になってはじめて、国民の確実ながん死低減が可能になるといえる。婦人科診療を窓口に個々のゲノム情報に応じて未発症者も既発症者の区別なく対応していき、「治療の最適化・予後予測・発症予防」によって最終的に国民のがん死低減に寄与することが可能になる。(著者抄録)

    J-GLOBAL

    researchmap

  • Cancer precision medicine and germline findings.

    植野さやか, 平沢晃

    月刊糖尿病・内分泌代謝科   55 ( 1 )   126 - 135   2022.7

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Surveillance for tumorous lesions in neurofibromatosis type 1

    二川摩周, 二川摩周, 中田英二, 十川麗美, 加藤芙美乃, 浦川優作, 河内麻里子, 山本英喜, 山本英喜, 藤原智洋, 国定俊之, 尾崎敏文, 平沢晃, 平沢晃

    日本遺伝カウンセリング学会誌   43 ( 2 )   92 - 92   2022.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Genetic counseling for parents who wish a prenatal diagnosis for their second child although the previous child’s chromosomal abnormality was occurred in de novo

    衛藤英理子, 三苫智裕, 横畑理美, 三島桜子, 大平安希子, 桐野智江, 谷和祐, 牧尉太, 早田桂, 増山寿, 秋山倫之, 大守伊織, 十川麗美, 河内麻里子, 平沢晃

    日本遺伝カウンセリング学会誌   43 ( 2 )   95 - 95   2022.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Development and evaluation of a teaching material to improve general literacy for cancer precision medicine

    十川麗美, 十川麗美, 和田敬仁, 榎朗兆, 岩本結香子, 黒飛恵子, 金井雅史, 近藤知大, 近藤知大, 本田明夏, 山田崇弘, 平沢晃, 武藤学, 小杉眞司

    日本遺伝カウンセリング学会誌   43 ( 1 )   15 - 27   2022.5

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 成人になって診断のついたHajdu-Cheney症候群の一例

    二川 奈都子, 長谷川 高誠, 西田 圭一郎, 平沢 晃, 河内 麻里子

    日本内分泌学会雑誌   98 ( 1 )   377 - 377   2022.4

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • Current status and issues related to secondary findings in the first public insurance covered tumor genomic profiling in Japan: multi-site questionnaire survey. International journal

    Akari Minamoto, Takahiro Yamada, Saki Shimada, Ichiro Kinoshita, Yoko Aoki, Katsutoshi Oda, Arisa Ueki, Satomi Higashigawa, Maki Morikawa, Yuki Sato, Akira Hirasawa, Masanobu Ogawa, Tomohiro Kondo, Masahiro Yoshioka, Masashi Kanai, Manabu Muto, Shinji Kosugi

    Journal of human genetics   67 ( 10 )   557 - 563   2022.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    In June 2019, the Japanese National Health Insurance (NHI) system introduced coverage for two types of tumor genomic profiling (TGP): FoundationOneⓇ CDx (F1) and OncoGuide™ NCC OncoPanel System (NCCOP). TGP sometimes reveals germline variants that are potentially pathogenic as secondary findings (SFs). We conducted a questionnaire-based survey to find out the operational statuses of F1 and NCCOP at institutions where TGP was performed to elucidate issues related to SFs. Responses were received from 97 of 112 institutions (86.6%). As of May 31, 2020, 88 (90.7%) and 78 (80.4%) institutions started performing F1 and NCCOP, respectively. Since F1 only examines tumor samples, germline confirmatory testing is necessary to determine whether they are actually germline pathogenic variants (GPVs). When physicians are obtaining informed consent all but 2.3% of the patients requested SF disclosure. Conversely, when presumed germline pathogenic variants (PGPVs) were detected, 46.2% were not willing to receive confirmatory tests as they wanted to prioritize cancer treatment over SFs investigation, while only 23.3% underwent confirmatory tests. Problems in cancer genomic medicine reported by clinical genetics departments included short-staffing (n = 10), insufficient interdepartmental cooperation (n = 9), inconsistent understanding of genetics among healthcare professionals (n = 8), and low utilization rate of SFs due to lack of insurance coverage for confirmatory tests and post-test health checkups (n = 8). Solutions include; determining the appropriate timing to confirm patient intent on SF disclosure, covering confirmatory tests for PGPVs by the NHI, and establishing cooperation between the oncology and clinical genetics departments.

    DOI: 10.1038/s10038-022-01028-x

    PubMed

    researchmap

  • TP53 variants in p53 signatures and the clonality of STICs in RRSO samples. International journal

    Tomoko Akahane, Kenta Masuda, Akira Hirasawa, Yusuke Kobayashi, Arisa Ueki, Miho Kawaida, Kumiko Misu, Kohei Nakamura, Shimpei Nagai, Tatsuyuki Chiyoda, Wataru Yamagami, Shigenori Hayashi, Fumio Kataoka, Kouji Banno, Kokichi Sugano, Hajime Okita, Kenjiro Kosaki, Hiroshi Nishihara, Daisuke Aoki

    Journal of gynecologic oncology   33 ( 4 )   e50   2022.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    OBJECTIVE: Precursor lesions may be identified in fallopian tube tissue after risk-reducing salpingo-oophorectomy (RRSO) in patients with pathogenic variants of BRCA1/2. Serous tubal intraepithelial carcinoma (STIC) is considered a precursor of high-grade serous carcinoma, whereas the significance of the p53 signature remains unclear. In this study, we investigated the relationship between the p53 signature and the risk of ovarian cancer. METHODS: We analyzed the clinicopathological findings and conducted DNA sequencing for TP53 variants of p53 signatures and STIC lesions isolated using laser capture microdissection in 13 patients with pathogenic variants of BRCA1/2 who underwent RRSO and 17 control patients with the benign gynecologic disease. RESULTS: TP53 pathogenic variants were detected significantly higher in RRSO group than control (p<0.001). No difference in the frequency of p53 signatures were observed between groups (53.8% vs 29.4%; p=0.17). TP53 sequencing and next-generation sequencing analysis in a patient with STIC and occult cancer revealed 2 TP53 mutations causing different p53 staining for STICs and another TP53 mutation shared between STIC and occult cancer. CONCLUSION: The sequence analysis for TP53 revealed 2 types of p53 signatures, one with a risk of progression to STIC and ovarian cancer with pathological variants in TP53 and the other with a low risk of progression without pathological variants in TP53 as seen in control.

    DOI: 10.3802/jgo.2022.33.e50

    PubMed

    researchmap

  • Hemothorax and Bloody Ascites Caused by Vascular Ehlers-Danlos Syndrome. International journal

    Shuichi Tanaka, Hiroyuki Honda, Kou Hasegawa, Koji Tomita, Reimi Sogawa, Hideki Yamamoto, Takao Hiraki, Akira Hirasawa, Fumio Otsuka

    The American journal of medicine   135 ( 7 )   e210-e211   2022.3

     More details

  • がんゲノム中核拠点病院における、がん遺伝子パネルで同定されたGermline Findingsに対する診療システムの構築

    中田 英二, 二川 摩周, 国定 俊之, 藤原 智洋, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 2 )   S439 - S439   2022.3

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • Hereditary gynecologic tumors and precision cancer medicine. International journal

    Chikako Ogawa, Akira Hirasawa, Naoyuki Ida, Keiichiro Nakamura, Hisashi Masuyama

    The journal of obstetrics and gynaecology research   48 ( 5 )   1076 - 1090   2022.2

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Gynecologic cancers are more often caused by genetic factors than other cancers. Genetic testing has become a promising avenue for the prevention, prognosis, and treatment of cancers. This review describes molecular features of gynecologic tumors linked to hereditary syndromes, gives an overview of the current state of clinical management, and clarifies the role of gynecology in the treatment of hereditary tumors. Typical hereditary gynecologic tumors include hereditary breast and ovarian cancer, Lynch syndrome, Peutz-Jeghers syndrome, and Cowden syndrome. Multigene panel testing, which analyzes a preselected subset of genes for genetic variants, has recently become the first-choice test because it can provide more accurate risk assessment than a single test. Furthermore, comprehensive genomic cancer profiling enables personalized cancer treatment and aids in germline findings.

    DOI: 10.1111/jog.15197

    PubMed

    researchmap

  • ATM: Functions of ATM Kinase and Its Relevance to Hereditary Tumors. International journal

    Sayaka Ueno, Tamotsu Sudo, Akira Hirasawa

    International journal of molecular sciences   23 ( 1 )   2022.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Ataxia-telangiectasia mutated (ATM) functions as a key initiator and coordinator of DNA damage and cellular stress responses. ATM signaling pathways contain many downstream targets that regulate multiple important cellular processes, including DNA damage repair, apoptosis, cell cycle arrest, oxidative sensing, and proliferation. Over the past few decades, associations between germline ATM pathogenic variants and cancer risk have been reported, particularly for breast and pancreatic cancers. In addition, given that ATM plays a critical role in repairing double-strand breaks, inhibiting other DNA repair pathways could be a synthetic lethal approach. Based on this rationale, several DNA damage response inhibitors are currently being tested in ATM-deficient cancers. In this review, we discuss the current knowledge related to the structure of the ATM gene, function of ATM kinase, clinical significance of ATM germline pathogenic variants in patients with hereditary cancers, and ongoing efforts to target ATM for the benefit of cancer patients.

    DOI: 10.3390/ijms23010523

    PubMed

    researchmap

  • Homologous Recombination Deficiencies and Hereditary Tumors. International journal

    Hideki Yamamoto, Akira Hirasawa

    International journal of molecular sciences   23 ( 1 )   2021.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Homologous recombination (HR) is a vital process for repairing DNA double-strand breaks. Germline variants in the HR pathway, comprising at least 10 genes, such as BRCA1, BRCA2, ATM, BARD1, BRIP1, CHEK2, NBS1(NBN), PALB2, RAD51C, and RAD51D, lead to inherited susceptibility to specific types of cancers, including those of the breast, ovaries, prostate, and pancreas. The penetrance of germline pathogenic variants of each gene varies, whereas all their associated protein products are indispensable for maintaining a high-fidelity DNA repair system by HR. The present review summarizes the basic molecular mechanisms and components that collectively play a role in maintaining genomic integrity against DNA double-strand damage and their clinical implications on each type of hereditary tumor.

    DOI: 10.3390/ijms23010348

    PubMed

    researchmap

  • Familial pancreatic cancer with PALB2 and NBN pathogenic variants: a case report

    Kodai Abe, Arisa Ueki, Yusaku Urakawa, Minoru Kitago, Tomoko Yoshihama, Yoshiko Nanki, Yuko Kitagawa, Daisuke Aoki, Kenjiro Kosaki, Akira Hirasawa

    Hereditary Cancer in Clinical Practice   19 ( 1 )   2021.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BioMed Central Ltd  

    Background: Family history is one of the risk factors for pancreatic cancer. It is suggested that patients with pancreatic cancer who have a familial history harbor germline pathogenic variants of BRCA1 and/or BRCA2 (BRCA1/2), PALB2, or ATM. Recently, some germline variants of familial pancreatic cancers (FPCs), including PALB2, have been detected. Several countries, including Japan, perform screening workups and genetic analysis for pancreatic cancers. We have been carrying out active surveillance for FPC through epidemiological surveys, imaging analyses, and genetic analysis. Case presentation: Here, we present the case of a female patient harboring pathogenic variants of PALB2 and NBN, with a family history of multiple pancreatic cancer in her younger brother, her aunt, and her father. Moreover, her father harbored a PALB2 pathogenic variant and her daughter harbored the same NBN pathogenic variant. Given the PALB2 and NBN variants, we designed surveillance strategies for the pancreas, breast, and ovary. Conclusions: Further studies are required to develop strategies for managing FPCs to facilitate prompt diagnosis before their progression.

    DOI: 10.1186/s13053-020-00160-z

    Scopus

    researchmap

  • Retroperitoneal leiomyosarcoma in a female patient with a germline splicing variant RAD51D c.904-2A > T: a case report. International journal

    Mashu Futagawa, Hideki Yamamoto, Mariko Kochi, Yusaku Urakawa, Reimi Sogawa, Fumino Kato, Mika Okazawa-Sakai, Daisuke Ennishi, Katsunori Shinozaki, Hirofumi Inoue, Hiroyuki Yanai, Akira Hirasawa

    Hereditary cancer in clinical practice   19 ( 1 )   48 - 48   2021.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: RAD51D (RAD51 paralog D) is an intermediate cancer susceptibility gene for primary ovarian cancer, including fallopian tube and peritoneal carcinomas and breast cancer. Although gynecological non-epithelial tumors such as uterine sarcomas are associated with genomic instability, including BRCA impairment, there is no clear evidence of the relationship between RAD51D variants and the risk of sarcoma development. CASE PRESENTATION: A Japanese woman in her 50s underwent multiple surgical resections and several regimens of chemotherapy for tumors that originated in the retroperitoneum and recurred in the peritoneum over a clinical course of approximately 4 years. The peritoneal tumor was histologically diagnosed as a leiomyosarcoma and was genetically identified to show a splice variant of RAD51D c.904-2A > T [NM_002878] through tumor profiling performed as a part of cancer precision medicine. The confirmatory genetic test performed after genetic counseling revealed that the RAD51D splicing variant detected in her tumor was of germline origin. In silico analyses supported the possible pathogenicity of the detected splice variant of RAD51D with a predicted attenuation in mRNA transcription and truncated protein production due to frameshifting, which was attributed to a single-nucleotide alteration in the splicing acceptor site at the 3'-end of intron 9 of RAD51D. Considering her unfavorable clinical outcome, which showed a highly aggressive phenotype of leiomyosarcoma with altered RAD51D, this case provided novel evidence for the relationship of a RAD51D splicing variant with malignant tumor development or progression. We report the findings of this rare case with possible involvement of the germline variant of RAD51D c.904-2A > T as a potential predisposing factor for malignant tumors, including leiomyosarcoma. CONCLUSIONS: We present the findings of a case of leiomyosarcoma in the peritoneum of a female patient with a novel germline splicing variant of RAD51D as potential evidence for the pathogenicity of the variant and its involvement in the risk of sarcoma etiology and/or development. To the best of our knowledge, this is the first case report describing a leiomyosarcoma carrying a germline RAD51D splicing variant and elucidating its pathogenicity on the basis of computational prediction of the impairment of normal transcription and the presumed loss of functional protein production.

    DOI: 10.1186/s13053-021-00205-x

    PubMed

    researchmap

  • MCM3 is a novel proliferation marker associated with longer survival for patients with tubo-ovarian high-grade serous carcinoma. International journal

    Eun Young Kang, Joshua Millstein, Gordana Popovic, Nicola S Meagher, Adelyn Bolithon, Aline Talhouk, Derek S Chiu, Michael S Anglesio, Betty Leung, Katrina Tang, Neil Lambie, Marina Pavanello, Annalyn Da-Anoy, Diether Lambrechts, Liselore Loverix, Siel Olbrecht, Christiani Bisinotto, Jesus Garcia-Donas, Sergio Ruiz-Llorente, Monica Yagüe-Fernandez, Robert P Edwards, Esther Elishaev, Alexander Olawaiye, Sarah Taylor, Beyhan Ataseven, Andreas du Bois, Philipp Harter, Jenny Lester, Claus K Høgdall, Sebastian M Armasu, Yajue Huang, Robert A Vierkant, Chen Wang, Stacey J Winham, Sabine Heublein, Felix K F Kommoss, Daniel W Cramer, Naoko Sasamoto, Lilian van-Wagensveld, Maria Lycke, Constantina Mateoiu, Janine Joseph, Malcolm C Pike, Kunle Odunsi, Chiu-Chen Tseng, Celeste L Pearce, Sanela Bilic, Thomas P Conrads, Arndt Hartmann, Alexander Hein, Michael E Jones, Yee Leung, Matthias W Beckmann, Matthias Ruebner, Minouk J Schoemaker, Kathryn L Terry, Mona A El-Bahrawy, Penny Coulson, John L Etter, Katherine LaVigne-Mager, Juergen Andress, Marcel Grube, Anna Fischer, Nina Neudeck, Greg Robertson, Rhonda Farrell, Ellen Barlow, Carmel Quinn, Anusha Hettiaratchi, Yovanni Casablanca, Ramona Erber, Colin J R Stewart, Adeline Tan, Yu Yu, Jessica Boros, Alison H Brand, Paul R Harnett, Catherine J Kennedy, Nikilyn Nevins, Terry Morgan, Peter A Fasching, Ignace Vergote, Anthony J Swerdlow, Francisco J Candido Dos Reis, G Larry Maxwell, Susan L Neuhausen, Arantzazu Barquin-Garcia, Francesmary Modugno, Kirsten B Moysich, Philip J Crowe, Akira Hirasawa, Florian Heitz, Beth Y Karlan, Ellen L Goode, Peter Sinn, Hugo M Horlings, Estrid Høgdall, Karin Sundfeldt, Stefan Kommoss, Annette Staebler, Anna H Wu, Paul A Cohen, Anna DeFazio, Cheng-Han Lee, Helen Steed, Nhu D Le, Simon A Gayther, Kate Lawrenson, Paul D P Pharoah, Gottfried Konecny, Linda S Cook, Susan J Ramus, Linda E Kelemen, Martin Köbel

    Virchows Archiv : an international journal of pathology   480 ( 4 )   855 - 871   2021.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Tubo-ovarian high-grade serous carcinomas (HGSC) are highly proliferative neoplasms that generally respond well to platinum/taxane chemotherapy. We recently identified minichromosome maintenance complex component 3 (MCM3), which is involved in the initiation of DNA replication and proliferation, as a favorable prognostic marker in HGSC. Our objective was to further validate whether MCM3 mRNA expression and possibly MCM3 protein levels are associated with survival in patients with HGSC. MCM3 mRNA expression was measured using NanoString expression profiling on formalin-fixed and paraffin-embedded tissue (N = 2355 HGSC) and MCM3 protein expression was assessed by immunohistochemistry (N = 522 HGSC) and compared with Ki-67. Kaplan-Meier curves and the Cox proportional hazards model were used to estimate associations with survival. Among chemotherapy-naïve HGSC, higher MCM3 mRNA expression (one standard deviation increase in the score) was associated with longer overall survival (HR = 0.87, 95% CI 0.81-0.92, p < 0.0001, N = 1840) in multivariable analysis. MCM3 mRNA expression was highest in the HGSC C5.PRO molecular subtype, although no interaction was observed between MCM3, survival and molecular subtypes. MCM3 and Ki-67 protein levels were significantly lower after exposure to neoadjuvant chemotherapy compared to chemotherapy-naïve tumors: 37.0% versus 46.4% and 22.9% versus 34.2%, respectively. Among chemotherapy-naïve HGSC, high MCM3 protein levels were also associated with significantly longer disease-specific survival (HR = 0.52, 95% CI 0.36-0.74, p = 0.0003, N = 392) compared to cases with low MCM3 protein levels in multivariable analysis. MCM3 immunohistochemistry is a promising surrogate marker of proliferation in HGSC.

    DOI: 10.1007/s00428-021-03232-0

    PubMed

    researchmap

  • Prospective feasibility study of neoadjuvant dose-dense paclitaxel plus carboplatin with bevacizumab therapy followed by interval debulking surgery for advanced ovarian, fallopian tube, and primary peritoneal cancer patients.

    Naomi Iwasa-Inoue, Hiroyuki Nomura, Fumio Kataoka, Tatsuyuki Chiyoda, Tomoko Yoshihama, Yoshiko Nanki, Kensuke Sakai, Yusuke Kobayashi, Wataru Yamagami, Tohru Morisada, Akira Hirasawa, Daisuke Aoki

    International journal of clinical oncology   27 ( 2 )   441 - 447   2021.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: This study aimed to investigate the clinical benefit of dose-dense paclitaxel plus carboplatin (TC) with bevacizumab therapy for advanced ovarian, fallopian tube, and primary peritoneal cancer patients in the neoadjuvant setting. METHODS: Ovarian, fallopian tube or primary peritoneal cancer patients with stage III-IV disease received neoadjuvant chemotherapy (NAC) every 3 weeks consisting of paclitaxel (80 mg/m2) on days 1, 8, and 15; carboplatin (AUC 6.0 mg/mL × min.) on day 1; and bevacizumab (15 mg/kg) on day 1. Interval debulking surgery (IDS) was performed after 3 cycles of dose-dense TC-bevacizumab therapy. The primary endpoint was the rate of complete resection by IDS. Secondary endpoints were treatment completion rate, treatment exposure, response rate to NAC, adverse events, and perioperative complications. RESULTS: Twenty-four patients were included in this study. The median age was 55.5 years (37-80 years), and most patients had high-grade serous carcinoma accounted (n = 18). IDS was performed in all patients with complete resection achieved in 75% (95% confidence interval: 57.7-92.3%). The lower limit exceeded the preset threshold rate of 55%. The response rate to NAC was 79%, and serum CA125 levels were in the normal range after NAC in 57% of patients. Grade 4 hematological toxicities and grade 3/4 non-hematological toxicities occurred in 29% and 17% of patients during NAC, respectively. Grade 3/4 perioperative complications were seen in 29% of patients, but no gastrointestinal perforations or treatment-related deaths occurred. CONCLUSIONS: Neoadjuvant dose-dense TC-bevacizumab therapy was well tolerated, and a satisfactory rate of complete resection by IDS was achieved.

    DOI: 10.1007/s10147-021-02050-3

    PubMed

    researchmap

  • 参照配列の違いからゲノム解析結果が異なる解釈に至った遺伝学的検査の一例

    山本 英喜, 加藤 芙美乃, 浦川 優作, 河内 麻里子, 二川 摩周, 十川 麗美, 植野 さやか, 平沢 晃

    日本臨床検査医学会誌   69 ( 補冊 )   183 - 183   2021.10

     More details

    Language:Japanese   Publisher:(一社)日本臨床検査医学会  

    researchmap

  • Medium-chain triglycerides inhibit long-chain triglyceride-induced GIP secretion through GPR120-dependent inhibition of CCK. International journal

    Yuki Murata, Norio Harada, Shigenobu Kishino, Kanako Iwasaki, Eri Ikeguchi-Ogura, Shunsuke Yamane, Tomoko Kato, Yoshinori Kanemaru, Akiko Sankoda, Tomonobu Hatoko, Sakura Kiyobayashi, Jun Ogawa, Akira Hirasawa, Nobuya Inagaki

    iScience   24 ( 9 )   102963 - 102963   2021.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Long-chain triglycerides (LCTs) intake strongly stimulates GIP secretion from enteroendocrine K cells and induces obesity and insulin resistance partly due to GIP hypersecretion. In this study, we found that medium-chain triglycerides (MCTs) inhibit GIP secretion after single LCT ingestion and clarified the mechanism underlying MCT-induced inhibition of GIP secretion. MCTs reduced the CCK effect after single LCT ingestion in wild-type (WT) mice, and a CCK agonist completely reversed MCT-induced inhibition of GIP secretion. In vitro studies showed that medium-chain fatty acids (MCFAs) inhibit long-chain fatty acid (LCFA)-stimulated CCK secretion and increase in intracellular Ca2+ concentrations through inhibition of GPR120 signaling. Long-term administration of MCTs reduced obesity and insulin resistance in high-LCT diet-fed WT mice, but not in high-LCT diet-fed GIP-knockout mice. Thus, MCT-induced inhibition of GIP hypersecretion reduces obesity and insulin resistance under high-LCT diet feeding condition.

    DOI: 10.1016/j.isci.2021.102963

    PubMed

    researchmap

  • Hereditary pancreatic cancer.

    Kodai Abe, Minoru Kitago, Yuko Kitagawa, Akira Hirasawa

    International journal of clinical oncology   26 ( 10 )   1784 - 1792   2021.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Pancreatic cancer is associated with both family and hereditary cancer syndromes. Multigene panel testing for pancreatic cancer detected the germline variants BRCA1/2, PALB2, ATM, TP53, MLH1, STK11/LKB1, APC, CDKN2A, and SPINK1/PRSS1 as high-risk genes. A latest genome-wide association study revealed the common, but low-risk germline variants in pancreatic cancer patients. Active pancreatic surveillance using magnetic resonance imaging and endoscopic ultrasound is recommended for high-risk individuals who have a family history of pancreatic cancer or harbor these germline pathogenic variants to improve the detection rate and prognosis of pancreatic cancer. Since poly-ADP-ribose polymerase (PARP) inhibitor has been shown to be effective in improving the prognosis of BRCA-positive pancreatic cancer as well as hereditary breast and ovarian cancer syndrome, PARP inhibitor therapy is currently being applied as precision medicine to pancreatic cancer patients harboring the BRCA1/2 germline variant. This review highlights the importance of surveillance for germline pathogenic variants in pancreatic cancer and is expected to lead to improvements in the diagnosis and prevention of pancreatic cancer as well as facilitate the development of effective therapeutic strategies and precision medicine.

    DOI: 10.1007/s10147-021-02015-6

    PubMed

    researchmap

  • Incidence of germline variants in Lynch syndrome-related genes among Japanese endometrial cancer patients aged 40 years or younger.

    Takeshi Makabe, Wataru Yamagami, Akira Hirasawa, Izumi Miyabe, Tomokazu Wakatsuki, Mari Kikuchi, Akemi Takahashi, Junko Noda, Go Yamamoto, Daisuke Aoki, Kiwamu Akagi

    International journal of clinical oncology   26 ( 9 )   1767 - 1774   2021.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    [Objective] Lynch syndrome (LS) is an autosomal dominant inherited disorder caused by a germline pathogenic variant in DNA mismatch repair (MMR) genes. Endometrial cancer frequently precedes another LS-associated tumor. This study aimed to clarify the incidence and features of LS in young Japanese endometrial cancer patients.[Methods] Sixty-five patients aged 40 years or younger, who were diagnosed with endometrial cancer, were enrolled in this study. Targeted sequencing of a hereditary colorectal cancer-related gene panel including the MMR genes MLH1, MSH2, MSH6, and PMS2 was conducted on DNA samples extracted from blood cells.[Results] Overall, 6 missense variants (2 in MSH2, 2 in MSH6, and 2 in PMS2), 1 inframe deletion variant in MSH2, 1 splice variant in MSH2, and 1 two-base substitution in the 3' untranslated region in MLH1 were detected in 9 (13.8%) patients. Among these, the splice variant c.1276G > T (p.Ile411_Gly426del16) in MSH2 was annotated as pathogenic, while other variants were of uncertain significance. The patient with the pathogenic variant had a family history of endometrial and colorectal cancer and was diagnosed with endometrial cancer at age 35.[Conclusion] The incidence of LS among Japanese endometrial cancer patients of reproductive age (≤ 40 years) in this study was at least 1.5%; however, 12.3% of patients had variants of uncertain significance in MMR genes.

    DOI: 10.1007/s10147-021-01953-5

    PubMed

    researchmap

  • Secretory carcinoma of the skin with lymph node metastases and recurrence in both lungs: A case report. International journal

    Kohei Taniguchi, Hiroyuki Yanai, Tatsuya Kaji, Toshio Kubo, Daisuke Ennishi, Akira Hirasawa, Tadashi Yoshino

    Journal of cutaneous pathology   48 ( 8 )   1069 - 1074   2021.8

     More details

    Language:English  

    Secretory carcinoma of the skin is an extremely rare adnexal tumor, histopathologically identical to homologous lesions in the salivary glands and breast tissue. Although this tumor was previously reported as indolent, we report a case of secretory carcinoma of the skin with metastases and recurrence. The patient, a 31-year-old women, had a subcutaneous mass in the right axilla. The resected specimen contained a circumscribed mass, with proliferating tumor cells that exhibited prominent nucleoli. They exhibited glandular and papillary growth patterns and there were amphophilic secretions in the glands. Immunohistochemically, the tumor cells were positive for mammaglobin and S100. The tumor was surrounded by sweat glands and there was no mammary glandular tissue, suggesting that it was derived from axillary sweat glands. Accordingly, we made a diagnosis of secretory carcinoma of the skin. Four years after the operation, there were metastases in both lungs. The resected specimen revealed a tumor identical to that of the original skin tumor. Next-generation sequencing-based multiplex gene assay performed on the metastatic tissue revealed an ETV6-NTRK3 fusion gene. This is a rare case report of secretory carcinoma of the skin with lymph node metastases and recurrence in both lungs.

    DOI: 10.1111/cup.14028

    PubMed

    researchmap

  • Japanese Society for Cancer of the Colon and Rectum (JSCCR) guidelines 2020 for the Clinical Practice of Hereditary Colorectal Cancer.

    Naohiro Tomita, Hideyuki Ishida, Kohji Tanakaya, Tatsuro Yamaguchi, Kensuke Kumamoto, Toshiaki Tanaka, Takao Hinoi, Yasuyuki Miyakura, Hirotoshi Hasegawa, Tetsuji Takayama, Hideki Ishikawa, Takeshi Nakajima, Akiko Chino, Hideki Shimodaira, Akira Hirasawa, Yoshiko Nakayama, Shigeki Sekine, Kazuo Tamura, Kiwamu Akagi, Yuko Kawasaki, Hirotoshi Kobayashi, Masami Arai, Michio Itabashi, Yojiro Hashiguchi, Kenichi Sugihara

    International journal of clinical oncology   26 ( 8 )   1353 - 1419   2021.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Hereditary colorectal cancer (HCRC) accounts for < 5% of all colorectal cancer cases. Some of the unique characteristics commonly encountered in HCRC cases include early age of onset, synchronous/metachronous cancer occurrence, and multiple cancers in other organs. These characteristics necessitate different management approaches, including diagnosis, treatment or surveillance, from sporadic colorectal cancer management. There are two representative HCRC, named familial adenomatous polyposis and Lynch syndrome. Other than these two HCRC syndromes, related disorders have also been reported. Several guidelines for hereditary disorders have already been published worldwide. In Japan, the first guideline for HCRC was prepared by the Japanese Society for Cancer of the Colon and Rectum (JSCCR), published in 2012 and revised in 2016. This revised version of the guideline was immediately translated into English and published in 2017. Since then, several new findings and novel disease concepts related to HCRC have been discovered. The currently diagnosed HCRC rate in daily clinical practice is relatively low; however, this is predicted to increase in the era of cancer genomic medicine, with the advancement of cancer multi-gene panel testing or whole genome testing, among others. Under these circumstances, the JSCCR guidelines 2020 for HCRC were prepared by consensus among members of the JSCCR HCRC Guideline Committee, based on a careful review of the evidence retrieved from literature searches, and considering the medical health insurance system and actual clinical practice settings in Japan. Herein, we present the English version of the JSCCR guidelines 2020 for HCRC.

    DOI: 10.1007/s10147-021-01881-4

    PubMed

    researchmap

  • Germline Whole-Gene Deletion of FH Diagnosed from Tumor Profiling. International journal

    Arisa Ueki, Kokichi Sugano, Kumiko Misu, Eriko Aimono, Kohei Nakamura, Shigeki Tanishima, Nobuyuki Tanaka, Shuji Mikami, Akira Hirasawa, Miho Ando, Teruhiko Yoshida, Mototsugu Oya, Hiroshi Nishihara, Kenjiro Kosaki

    International journal of molecular sciences   22 ( 15 )   2021.7

     More details

    Language:English  

    Hereditary leiomyomatosis and renal cell carcinoma (HL (RCC)) entails cutaneous and uterine leiomyomatosis with aggressive type 2 papillary RCC-like histology. HLRCC is caused by pathogenic variants in the FH gene, which encodes fumarate hydratase (FH). Here, we describe an episode of young-onset RCC caused by a genomic FH deletion that was diagnosed via clinical sequencing. A 35-year-old woman was diagnosed with RCC and multiple metastases: histopathological analyses supported a diagnosis of FH-deficient RCC. Although the patient had neither skin tumors nor a family history of HLRCC, an aggressive clinical course at her age and pathological diagnosis of FH-deficient RCC suggested a germline FH variant. After counseling, the patient provided written informed consent for germline genetic testing. She was simultaneously subjected to paired tumor profiling tests targeting the exome to identify a therapeutic target. Although conventional germline sequencing did not detect FH variants, exome sequencing revealed a heterozygous germline FH deletion. As such, paired tumor profiling, not conventional sequencing, was required to identify this genetic deletion. RCC caused by a germline FH deletion has hitherto not been described in Japan, and the FH deletion detected in this patient was presumed to be of maternal European origin. Although the genotype-phenotype correlation in HLRCC-related tumors is unclear, the patient's family was advised to undergo genetic counseling to consider additional RCC screening.

    DOI: 10.3390/ijms22157962

    PubMed

    researchmap

  • Preclinical diagnosis and identification of the chimeric CYP11B1/CYP11B2 gene in two pediatric cases of a Japanese family with glucocorticoid-remediable aldosteronism. International journal

    Yasuhiro Nakano, Nahoko Iwata, Kanako Ogura-Ochi, Kosei Hasegawa, Akira Hirasawa, Fumio Otsuka

    Hypertension research : official journal of the Japanese Society of Hypertension   44 ( 7 )   891 - 893   2021.7

     More details

  • CYP11B1/B2キメラ遺伝子を確認した家族性アルドステロン症小児例

    中野 靖浩, 岩田 菜穂子, 長谷川 高誠, 越智 可奈子, 山本 紘一郎, 高瀬 了輔, 長谷川 功, 堀口 繁, 山本 英喜, 平沢 晃, 大塚 文男

    日本内分泌学会雑誌   97 ( Suppl.Update )   71 - 73   2021.7

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    約20年前にCYP11B1/B2キメラ遺伝子を確認しグルココルチコイド反応性アルドステロン症(GRA)と診断された日本人1家系3例(発端者、母、妹)のうち、発端者が出産した5歳と3歳の男児に対し遺伝子検査を行った。その結果、男児2人ともキメラ遺伝子を検出しGRA保因者であることが明らかとなった。また、キメラ遺伝子の交叉部位について検討した結果、2児と発端者は同一のシークエンスで、交叉部位はエクソン3とイントロン5間であった。2児とも高血圧を認めないが低レニン・高アルドステロン症を伴っており、今後、成人期までの慎重な経過観察が必要である。

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2021&ichushi_jid=J01160&link_issn=&doc_id=20210811280023&doc_link_id=10.1507%2Fendocrine.97.S.Update_71&url=https%3A%2F%2Fdoi.org%2F10.1507%2Fendocrine.97.S.Update_71&type=J-STAGE&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00007_3.gif

  • SMAD4 Germline Pathogenic Variant-Related Gastric Juvenile Polyposis with Adenocarcinoma Treated with Laparoscopic Total Gastrectomy: A Case Report. International journal

    Yuya Sakurai, Satoru Kikuchi, Kunitoshi Shigeyasu, Yoshihiko Kakiuchi, Takehiro Tanaka, Hibiki Umeda, Masaki Sakamoto, Sho Takeda, Shuya Yano, Mashu Futagawa, Fumino Kato, Reimi Sogawa, Hideki Yamamoto, Shinji Kuroda, Yoshitaka Kondo, Fuminori Teraishi, Hiroyuki Kishimoto, Masahiko Nishizaki, Shunsuke Kagawa, Akira Hirasawa, Toshiyoshi Fujiwara

    The American journal of case reports   22   e932241   2021.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND Juvenile polyposis syndrome is an uncommon, autosomal-dominant hereditary disease that is distinguished by multiple polyps in the stomach or intestinal tract. It is associated with a high risk of malignancy. Pathogenic variants in SMAD4 or BMPR1A account for 40% of all cases. CASE REPORT A 49-year-old woman underwent esophagogastroduodenoscopy because of exacerbation of anemia. She had numerous erythematous polyps in most parts of her stomach. Based on biopsy findings, juvenile polyposis syndrome (JPS) was suspected morphologically, but there was no evidence of malignancy. Colonoscopy showed stemmed hyperplastic polyps and an adenoma; video capsule endoscopy revealed no lesions in the small intestine. After preoperative surveillance, laparoscopic total gastrectomy with D1 lymph node dissection was performed to prevent malignant transformation. The pathological diagnosis was juvenile polyp-like polyposis with adenocarcinoma. In addition, a germline pathogenic variant in the SMAD4 gene was detected with genetic testing. CONCLUSIONS JPS can be diagnosed with endoscopy and genetic testing. Further, appropriate surgical management may prevent cancer-related death in patients with this condition.

    DOI: 10.12659/AJCR.932241

    PubMed

    researchmap

  • Best practices for the extraction of genomic DNA from formalin-fixed paraffin-embedded tumor tissue for cancer genomic profiling tests. International journal

    Hirofumi Inoue, Shuta Tomida, Shigeru Horiguchi, Hironari Kato, Hiromi Matsuoka, Etsuko Sanehira, Masashi Matsuoka, Hiroyuki Yanai, Akira Hirasawa, Shinichi Toyooka

    Pathology international   71 ( 5 )   360 - 364   2021.5

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Recently, two cancer genomic profiling tests have been approved in Japan and implemented in routine clinical practice: the FDA-approved FoundationOne CDx test, and the OncoGuide NCC Oncopanel test. The quality and quantity of DNA significantly affects the sequencing results; therefore, preparing a sufficient amount of high-quality DNA for clinical cancer genomic profiling tests is important. We examined the best practices for the extraction of cancer genomic DNA from formalin-fixed paraffin-embedded (FFPE) tumor tissues of pancreatic, lung and colon cancer specimens. We found that the quality of cancer genomic DNA extracted from 10-μm-thick FFPE samples improved significantly, compared with that from 4-μm-thick FFPE samples, suggesting that 10-μm-thick FFPE samples are preferable for clinical cancer genomic profiling tests. For convenience, we created a quick reference table for calculating the required number of FFPE slides.

    DOI: 10.1111/pin.13086

    PubMed

    researchmap

  • SUCCESSFUL MANAGEMENT OF BONE METASTASES FROM HEREDITARY LEIOMYOMATOSIS AND RENAL CELL CARCINOMA (HLRCC)-ASSOCIATED RENAL CELL CARCINOMA (HLRCC-RCC) BY USING COMBINED IMMUNOTHERAPY COMPRISING IPILIMUMAB PLUS NIVOLUMAB: A CASE REPORT

    渡部智文, 榮枝一磨, 津川昌也, 関戸崇了, 富永悠介, 高本篤, 定平卓也, 小林泰之, 荒木元朗, 渡邉豊彦, 小田和歌子, 黒田直人, 十川麗美, 山本英喜, 平沢晃, 那須保友

    西日本泌尿器科(Web)   83 ( 1 )   31 - 36   2021.4

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • RRSO検体におけるp53 signatureとSTICの特性に関する検討

    赤羽 智子, 増田 健太, 平沢 晃, 小林 佑介, 永井 晋平, 千代田 達幸, 林 茂徳, 片岡 史夫, 冨永 英一郎, 阪埜 浩司, 田中 守, 青木 大輔

    日本産科婦人科学会雑誌   73 ( 臨増 )   S - 570   2021.3

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • Germline multigene panel testing revealed a BRCA2 pathogenic variant in a patient with suspected Lynch syndrome International journal

    Tomoko Yoshihama, Akira Hirasawa, Kokichi Sugano, Teruhiko Yoshida, Mineko Ushiama, Arisa Ueki, Tomoko Akahane, Yoshiko Nanki, Kensuke Sakai, Takeshi Makabe, Wataru Yamagami, Nobuyuki Susumu, Kaori Kameyama, Kenjiro Kosaki, Daisuke Aoki

    International Cancer Conference Journal   10 ( 1 )   6 - 10   2021.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:Springer Science and Business Media LLC  

    <title>Abstract</title>There has been a rapid advance in germline multigene panel testing by next-generation sequencing, and it is being widely used in clinical settings. A 56-year-old woman suspected of having Lynch syndrome was identified as a <italic>BRCA2</italic> pathogenic variant carrier by multigene panel testing. The patient was diagnosed with endometrial cancer at the age of 39 years, and total laparoscopic hysterectomy and bilateral salpingectomy were performed at the age of 49 years; however, bilateral oophorectomy was not performed at that time. As she had a family history of colorectal cancer and a history of endometrial cancer, Lynch syndrome was suspected. However, germline multigene panel testing revealed a pathogenic <italic>BRCA2</italic> variant rather than pathogenic variants in mismatch repair genes. In this case, with conventional genetic risk assessment, we were unable to determine whether the patient had a high risk of hereditary breast and ovarian cancer; thus, germline multigene panel testing may provide valuable information to improve disease management strategies for patients in clinical settings. Particularly, germline multigene panel testing may be useful for detecting hereditary tumor syndromes if a patient does not present with a typical family history of cancer.

    DOI: 10.1007/s13691-020-00449-9

    Web of Science

    PubMed

    researchmap

    Other Link: http://link.springer.com/article/10.1007/s13691-020-00449-9/fulltext.html

  • 最新産婦人科遺伝診療ABC 10.婦人科腫瘍領域における遺伝診療総論

    坂井美佳, 坂井美佳, 竹原和宏, 平沢晃

    産科と婦人科   88 ( 1 )   65 - 72   2021

     More details

    Authorship:Corresponding author   Language:Japanese   Publisher:(株)診断と治療社  

    遺伝性乳がん卵巣がん症候群(HBOC)やLynch症候群を代表とする遺伝性腫瘍は婦人科腫瘍とのかかわりが深い。特にごく最近では2019年のBRCA1/2遺伝学的検査のコンパニオン診断とがんゲノム医療の保険診療化、そして2020年4月のHBOC診療の一部保険診療化に伴い、産婦人科医にとって遺伝性腫瘍の知識は不可欠なものとなっている。個々の遺伝情報を知ることは、がん治療および予防の観点から有用性が高い。(著者抄録)

    J-GLOBAL

    researchmap

    Other Link: https://search-tp.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2021&ichushi_jid=J00525&link_issn=&doc_id=20201221170010&doc_link_id=%2Fae4sanke%2F2021%2F008801%2F011%2F0065-0072%26dl%3D0&url=https%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Fae4sanke%2F2021%2F008801%2F011%2F0065-0072%26dl%3D0&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_2.gif

  • Molecular Features and Clinical Management of Hereditary Gynecological Cancers. International journal

    Arisa Ueki, Akira Hirasawa

    International journal of molecular sciences   21 ( 24 )   2020.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Hereditary gynecological cancers are caused by several inherited genes. Tumors that arise in the female reproductive system, such as ovaries and the uterus, overlap with hereditary cancers. Several hereditary cancer-related genes are important because they might lead to therapeutic targets. Treatment of hereditary cancers should be updated in line with the advent of various new methods of evaluation. Next-generation sequencing has led to rapid, economical genetic analyses that have prompted a concomitant and significant paradigm shift with respect to hereditary cancers. Molecular tumor profiling is an epochal method for determining therapeutic targets. Clinical treatment strategies are now being designed based on biomarkers based on tumor profiling. Furthermore, the National Comprehensive Cancer Network (NCCN) guidelines significantly changed the genetic testing process in 2020 to initially consider multi-gene panel (MGP) evaluation. Here, we reviewed the molecular features and clinical management of hereditary gynecological malignancies, such as hereditary breast and ovarian cancer (HBOC), and Lynch, Li-Fraumeni, Cowden, and Peutz-Jeghers syndromes. We also reviewed cancer-susceptible genes revealed by MGP tests.

    DOI: 10.3390/ijms21249504

    PubMed

    researchmap

  • Attitudes toward and current status of disclosure of secondary findings from next-generation sequencing: a nation-wide survey of clinical genetics professionals in Japan International journal

    Mio Tsuchiya, Takahiro Yamada, Rina Akaishi, Haruka Hamanoue, Akira Hirasawa, Maki Hyodo, Issei Imoto, Tomoki Kosho, Kenji Kurosawa, Hiromi Murakami, Kaname Nakatani, Fumio Nomura, Aiko Sasaki, Kenji Shimizu, Mariko Tamai, Hiroshi Umemura, Atsushi Watanabe, Akiko Yoshida, Hiroshi Yoshihashi, Junko Yotsumoto, Shinji Kosugi

    JOURNAL OF HUMAN GENETICS   65 ( 12 )   1045 - 1053   2020.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPRINGERNATURE  

    The management of secondary findings (SFs), which are beyond the intended purpose of the analysis, from clinical comprehensive genomic analysis using next generation sequencing (NGS) presents challenges. Policy statements regarding their clinical management have been announced in Japan and other countries. In Japan, however, the current status of and attitudes of clinical genetics professionals toward reporting them are unclear. We conducted a questionnaire survey of clinical genetics professionals at two time points (2013 and 2019) to determine the enforcement of the SF management policy in cases of comprehensive genetic analysis of intractable diseases and clinical cancer genome profiling testing. According to the survey findings, 40% and 70% of the respondents stated in the 2013 and 2019 surveys, respectively, that they had an SF policy in the field of intractable diseases, indicating that SF policy awareness in Japan has changed significantly in recent years. Furthermore, a total of 80% of respondents stated that their facility had established a policy for clinical cancer genome profiling testing in the 2019 survey. In both surveys, the policies included the selection criteria for genes to be disclosed and the procedure to return SFs, followed by recommendations and proposals regarding SFs in Japan and other countries. To create a better list of the genes to be disclosed, further examination is needed considering the characteristics of each analysis.

    DOI: 10.1038/s10038-020-0802-2

    Web of Science

    PubMed

    researchmap

  • Retrospective evaluation of risk-reducing salpingo-oophorectomy for BRCA1/2 pathogenic variant carriers among a cohort study in a single institution. International journal

    Yusuke Kobayashi, Akira Hirasawa, Tatsuyuki Chiyoda, Arisa Ueki, Kenta Masuda, Kumiko Misu, Miho Kawaida, Shigenori Hayashi, Fumio Kataoka, Kouji Banno, Kenjiro Kosaki, Daisuke Aoki

    Japanese journal of clinical oncology   51 ( 2 )   213 - 217   2020.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: Risk-reducing salpingo-oophorectomy is performed for the primary prevention of ovarian cancer in patients with hereditary breast-ovarian cancer syndrome. We performed risk-reducing salpingo-oophorectomy for the first time in Japan in 2008, and we experienced 20 cases of risk-reducing salpingo-oophorectomy through 2019. In the past, the use of risk-reducing salpingo-oophorectomy in Japan was restricted because it was not covered by a Japanese National Health Insurance. Since April 2020, risk-reducing salpingo-oophorectomy has been covered by insurance for patients with breast-ovarian cancer syndrome and pre-existing breast cancer, and this surgery is expected to become more widely implemented in Japan. METHODS: To contribute to the widespread use of risk-reducing salpingo-oophorectomy in the future, we retrospectively reviewed 20 cases of risk-reducing salpingo-oophorectomy at our hospital cohort study to clarify the issues in its implementation. RESULTS: The variant genes for which risk-reducing salpingo-oophorectomy was indicated were BRCA1 and BRCA2 in 13 (65%) and 7 patients (35%), respectively. The median age at which risk-reducing salpingo-oophorectomy was performed was 49 years (range, 38-58), 13 patients (65%) had gone through menopause, and 16 patients (80%) had a history of breast cancer. Of the five patients (25%) with vasomotor symptoms, four received Chinese medicine, and only one received hormone replacement therapy. Occult cancer was detected in the removed ovaries in two patients (10%), although no postoperative peritoneal carcinogenesis has been observed to date. CONCLUSIONS: Women who paid for risk-reducing salpingo-oophorectomy out of pocket were older than the recommended age at which the procedure should be performed, and this may explain the higher rate of occult cancers than previously reported. We need to perform risk-reducing salpingo-oophorectomy at the recommended age to ensure that the procedure is effective for primary prevention.

    DOI: 10.1093/jjco/hyaa173

    PubMed

    researchmap

  • Patient-derived ovarian cancer organoids capture the genomic profiles of primary tumours applicable for drug sensitivity and resistance testing. International journal

    Yoshiko Nanki, Tatsuyuki Chiyoda, Akira Hirasawa, Aki Ookubo, Manabu Itoh, Masaru Ueno, Tomoko Akahane, Kaori Kameyama, Wataru Yamagami, Fumio Kataoka, Daisuke Aoki

    Scientific reports   10 ( 1 )   12581 - 12581   2020.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    The use of primary patient-derived organoids for drug sensitivity and resistance testing could play an important role in precision cancer medicine. We developed expandable ovarian cancer organoids in < 3 weeks; these organoids captured the characteristics of histological cancer subtypes and replicated the mutational landscape of the primary tumours. Seven pairs of organoids (3 high-grade serous, 1 clear cell, 3 endometrioid) and original tumours shared 59.5% (36.1-73.1%) of the variants identified. Copy number variations were also similar among organoids and primary tumours. The organoid that harboured the BRCA1 pathogenic variant (p.L63*) showed a higher sensitivity to PARP inhibitor, olaparib, as well as to platinum drugs compared to the other organoids, whereas an organoid derived from clear cell ovarian cancer was resistant to conventional drugs for ovarian cancer, namely platinum drugs, paclitaxel, and olaparib. The overall success rate of primary organoid culture, including those of various histological subtypes, was 80% (28/35). Our data show that patient-derived organoids are suitable physiological ex vivo cancer models that can be used to screen effective personalised ovarian cancer drugs.

    DOI: 10.1038/s41598-020-69488-9

    PubMed

    researchmap

  • Japan society of clinical oncology/Japanese society of medical oncology-led clinical recommendations on the diagnosis and use of tropomyosin receptor kinase inhibitors in adult and pediatric patients with neurotrophic receptor tyrosine kinase fusion-positive advanced solid tumors, cooperated by the Japanese society of pediatric hematology/oncology.

    Yoichi Naito, Saori Mishima, Kiwamu Akagi, Ataru Igarashi, Masafumi Ikeda, Susumu Okano, Shunsuke Kato, Tadao Takano, Katsuya Tsuchihara, Keita Terashima, Hiroshi Nishihara, Hiroyki Nishiyama, Eiso Hiyama, Akira Hirasawa, Hajime Hosoi, Osamu Maeda, Yasushi Yatabe, Wataru Okamoto, Shigeru Ono, Hiroaki Kajiyama, Fumio Nagashima, Yutaka Hatanaka, Mitsuru Miyachi, Yasuhiro Kodera, Takayuki Yoshino, Hiroya Taniguchi

    International journal of clinical oncology   25 ( 3 )   403 - 417   2020.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: The development of novel antitumor agents and accompanying biomarkers has improved survival across several tumor types. Previously, we published provisional clinical opinion for the diagnosis and use of immunotherapy in patients with deficient DNA mismatch repair tumors. Recently, efficacy of tropomyosin receptor kinase inhibitors against neurotrophic receptor tyrosine kinase (NTRK) fusion gene-positive advanced solid tumors have been established as the second tumor-agnostic treatment, making it necessary to develop the guideline prioritized for these patients. METHODS: Clinical questions regarding medical care were formulated for patients with NTRK-positive advanced solid tumors. Relevant publications were searched by PubMed and Cochrane Database. Critical publications and conference reports were added manually. Systematic reviews were performed for each clinical question for the purpose of developing clinical recommendations. The committee members identified by Japan Society of Clinical Oncology (JSCO) and Japanese Society of Medical Oncology (JSMO) voted to determine the level of each recommendation considering the strength of evidence, expected risks and benefits to patients, and other related factors. Thereafter, a peer review by experts nominated from JSCO, JSMO, and Japanese Society of Pediatric Hematology/Oncology, and the public comments among all Societies' members was done. RESULTS: The current guideline describes 3 clinical questions and 15 recommendations for whom, when, and how NTRK fusion should be tested, and what is recommended for patients with NTRK fusion-positive advanced solid tumors. CONCLUSION: In the NTRK guideline, the committee proposed 15 recommendations for performing NTRK testing properly to select patients who are likely to benefit from tropomyosin receptor kinase inhibitors.

    DOI: 10.1007/s10147-019-01610-y

    PubMed

    researchmap

  • Japan Society of Clinical Oncology provisional clinical opinion for the diagnosis and use of immunotherapy in patients with deficient DNA mismatch repair tumors, cooperated by Japanese Society of Medical Oncology, First Edition. Reviewed

    Saori Mishima, Hiroya Taniguchi, Kiwamu Akagi, Eishi Baba, Yutaka Fujiwara, Akira Hirasawa, Masafumi Ikeda, Osamu Maeda, Kei Muro, Hiroshi Nishihara, Hiroyki Nishiyama, Tadao Takano, Katsuya Tsuchihara, Yasushi Yatabe, Yasuhiro Kodera, Takayuki Yoshino

    International journal of clinical oncology   25 ( 2 )   217 - 239   2020.2

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    BACKGROUND: Novel therapeutic agents have improved survival outcomes in patients with advanced solid tumors. In parallel, the development of predictive biomarkers to identify patients who are likely to benefit from a certain treatment has also contributed to the improvement of survival. Recently, clinical trials have reported the efficacy of immune checkpoint inhibitors in the treatment of mismatch repair-deficient (dMMR) advanced solid tumors. In Japan, a PD-1 inhibitor for dMMR advanced solid tumors, regardless of the primary tumor site, has been approved. However, there are some issues related to administering immune checkpoint inhibitors in the clinical practice setting, making it necessary to develop the guidelines. METHODS: Clinical questions (CQs) regarding medical care were formulated for patients with dMMR advanced solid tumors, and evidence to the CQs was collected by manual search to prepare recommendations. Then, the committee members voted to determine the level of each recommendation considering the strength of evidence, expected risks and benefits to patients, and other factors. RESULTS: The current guideline, which we consider a provisional clinical opinion at this point, describes the 11 requirements to be considered in terms of patients for whom dMMR testing is recommended, the timing and methods of dMMR testing, and clinical care systems required to perform dMMR testing properly and to administer immune checkpoint inhibitors safely. CONCLUSION: This provisional clinical opinion proposes the requirements for performing dMMR testing properly to select patients who are likely to benefit from immune checkpoint inhibitors and administering them safely.

    DOI: 10.1007/s10147-019-01498-8

    PubMed

    researchmap

  • 多発小腸GISTに対し手術を施行した神経線維腫症1型の1例 Reviewed

    母里 淑子, 重安 邦俊, 吉岡 貴裕, 永坂 岳司, 原賀 順子, 香川 俊輔, 寺石 文則, 豊岡 伸一, 平沢 晃, 藤原 俊義

    家族性腫瘍   19 ( 2 )   77 - 82   2020.2

     More details

    Language:Japanese   Publisher:日本家族性腫瘍学会  

    researchmap

  • Identification of a novel uterine leiomyoma GWAS locus in a Japanese population. International journal

    Kensuke Sakai, Chizu Tanikawa, Akira Hirasawa, Tatsuyuki Chiyoda, Wataru Yamagami, Fumio Kataoka, Nobuyuki Susumu, Chikashi Terao, Yoichiro Kamatani, Atsushi Takahashi, Yukihide Momozawa, Makoto Hirata, Michiaki Kubo, Nobuo Fuse, Takako Takai-Igarashi, Atsushi Shimizu, Akimune Fukushima, Aya Kadota, Kokichi Arisawa, Hiroaki Ikezaki, Kenji Wakai, Taiki Yamaji, Norie Sawada, Motoki Iwasaki, Shoichiro Tsugane, Daisuke Aoki, Koichi Matsuda

    Scientific reports   10 ( 1 )   1197 - 1197   2020.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Uterine leiomyoma is one of the most common gynaecologic benign tumours, but its genetic basis remains largely unknown. Six previous GWAS identified 33 genetic factors in total. Here, we performed a two-staged GWAS using 13,746 cases and 70,316 controls from the Japanese population, followed by a replication analysis using 3,483 cases and 4,795 controls. The analysis identified 9 significant loci, including a novel locus on 12q23.2 (rs17033114, P = 6.12 × 10-25 with an OR of 1.177 (1.141-1.213), LINC00485). Subgroup analysis indicated that 5 loci (3q26.2, 5p15.33, 10q24.33, 11p15.5, 13q14.11) exhibited a statistically significant effect among multiple leiomyomas, and 2 loci (3q26.2, 10q24.33) exhibited a significant effect among submucous leiomyomas. Pleiotropic analysis indicated that all 9 loci were associated with at least one proliferative disease, suggesting the role of these loci in the common neoplastic pathway. Furthermore, the risk T allele of rs2251795 (3q26.2) was associated with longer telomere length in both normal and tumour tissues. Our findings elucidated the significance of genetic factors in the pathogenesis of leiomyoma.

    DOI: 10.1038/s41598-020-58066-8

    PubMed

    researchmap

  • Establishment and characterization of a new malignant peritoneal mesothelioma cell line, KOG-1, from the ascitic fluid of a patient with pemetrexed chemotherapy resistance.

    Tomoko Akahane, Akira Hirasawa, Issei Imoto, Aki Okubo, Manabu Itoh, Yoshiko Nanki, Tomoko Yoshihama, Eichiro Tominaga, Daisuke Aoki

    Human cell   33 ( 1 )   272 - 282   2020.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Malignant peritoneal mesothelioma (MPeM) is a rare and aggressive form of malignant mesothelioma. Sufficient biological tools for studying the functional characteristics of this cancer have not been developed. Therefore, in this study, a novel human cancer cell line, KOG-1, was established from ascites fluids isolated from a 39-year-old Japanese woman with pemetrexed-resistant MPeM. Cells were dendritic or linear immediately after thawing, showed a jigsaw puzzle-like and spindle arrangement during growth, and formed monolayers without contact inhibition in two-dimensional (2D) culture. The population doubling time was 13.7 h. Karyotypic and molecular genetic analyses showed that chromosome numbers ranged from 62 to 142, with a peak of 73 with complicated copy number alterations. No germline BAP1 pathogenic variant was detected. Cells expressed various tumor markers of mesothelioma, such as calretinin, podoplanin, and Wilms tumor 1 (WT-1). Drug sensitivity and resistance testing with a set of 36 drugs using 2D and three-dimensional (3D) culture models demonstrated that KOG-1 cells showed high and low sensitivity to pemetrexed under 2D and 3D culture conditions, respectively, whereas control ovarian cancer cell lines showed low sensitivity to pemetrexed under both culture conditions. This newly established cell line will be a valuable biological resource to expand the feasibility of functional studies as well as drug testing for potential therapeutic purposes in MPeM.

    DOI: 10.1007/s13577-019-00286-w

    PubMed

    researchmap

  • Familial Pancreatic Cancer with PALB2 and NBN Pathogenic Variant: A Case Report Reviewed International journal

    阿部紘大, 植木有紗, 浦川優作, 北郷実, 吉浜智子, 南木佳子, 北川雄光, 青木大輔, 小崎健次郎, 平沢晃

    日本癌学会学術総会抄録集(Web)   79th ( 1 )   5 - 5   2020

     More details

    Authorship:Corresponding author   Language:English   Publishing type:Research paper (scientific journal)   Publisher:Springer Science and Business Media LLC  

    <title>Abstract</title><sec>
    <title>Background</title>
    Family history is one of the risk factors for pancreatic cancer. It is suggested that patients with pancreatic cancer who have a familial history harbor germline pathogenic variants of <italic>BRCA1</italic> and/or <italic>BRCA2</italic> (<italic>BRCA1/2</italic>), <italic>PALB2</italic>, or <italic>ATM</italic>. Recently, some germline variants of familial pancreatic cancers (FPCs), including <italic>PALB2,</italic> have been detected. Several countries, including Japan, perform screening workups and genetic analysis for pancreatic cancers. We have been carrying out active surveillance for FPC through epidemiological surveys, imaging analyses, and genetic analysis.


    </sec><sec>
    <title>Case presentation</title>
    Here, we present the case of a female patient harboring pathogenic variants of <italic>PALB2</italic> and <italic>NBN</italic>, with a family history of multiple pancreatic cancer in her younger brother, her aunt, and her father. Moreover, her father harbored a <italic>PALB2</italic> pathogenic variant and her daughter harbored the same <italic>NBN</italic> pathogenic variant. Given the <italic>PALB2</italic> and <italic>NBN</italic> variants, we designed surveillance strategies for the pancreas, breast, and ovary.


    </sec><sec>
    <title>Conclusions</title>
    Further studies are required to develop strategies for managing FPCs to facilitate prompt diagnosis before their progression.


    </sec>

    DOI: 10.1186/s13053-020-00160-z

    PubMed

    J-GLOBAL

    researchmap

    Other Link: http://link.springer.com/article/10.1186/s13053-020-00160-z/fulltext.html

  • Prevalence of disease-causing genes in Japanese patients with BRCA1/2-wildtype hereditary breast and ovarian cancer syndrome. International journal

    Tomoko Kaneyasu, Seiichi Mori, Hideko Yamauchi, Shozo Ohsumi, Shinji Ohno, Daisuke Aoki, Shinichi Baba, Junko Kawano, Yoshio Miki, Naomichi Matsumoto, Masao Nagasaki, Reiko Yoshida, Sadako Akashi-Tanaka, Takuji Iwase, Dai Kitagawa, Kenta Masuda, Akira Hirasawa, Masami Arai, Junko Takei, Yoshimi Ide, Osamu Gotoh, Noriko Yaguchi, Mitsuyo Nishi, Keika Kaneko, Yumi Matsuyama, Megumi Okawa, Misato Suzuki, Aya Nezu, Shiro Yokoyama, Sayuri Amino, Mayuko Inuzuka, Tetsuo Noda, Seigo Nakamura

    NPJ breast cancer   6   25 - 25   2020

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Panel sequencing of susceptibility genes for hereditary breast and ovarian cancer (HBOC) syndrome has uncovered numerous germline variants; however, their pathogenic relevance and ethnic diversity remain unclear. Here, we examined the prevalence of germline variants among 568 Japanese patients with BRCA1/2-wildtype HBOC syndrome and a strong family history. Pathogenic or likely pathogenic variants were identified on 12 causal genes for 37 cases (6.5%), with recurrence for 4 SNVs/indels and 1 CNV. Comparisons with non-cancer east-Asian populations and European familial breast cancer cohorts revealed significant enrichment of PALB2, BARD1, and BLM mutations. Younger onset was associated with but not predictive of these mutations. Significant somatic loss-of-function alterations were confirmed on the wildtype alleles of genes with germline mutations, including PALB2 additional somatic truncations. This study highlights Japanese-associated germline mutations among patients with BRCA1/2 wildtype HBOC syndrome and a strong family history, and provides evidence for the medical care of this high-risk population.

    DOI: 10.1038/s41523-020-0163-1

    PubMed

    researchmap

  • Training Medical Staff with Basic Skills for Data Science in Genomic Medicine

    冨田秀太, 森田瑞樹, 山下範之, 平沢晃, 豊岡伸一

    薬学雑誌(Web)   140 ( 5 )   657 - 661   2020

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    The development of specialized training programs for medical personnel, particularly nurses, clinical laboratory technicians, and pharmacists, is considered critical for the promotion of genomic medicine throughout Japan. Specifically, medical personnel skilled at analyzing and understanding high-throughput genomic data are in high demand. In this symposium, we will introduce the basic knowledge and skills necessary for processing genomic data.

    DOI: 10.1248/yakushi.19-00217-2

    PubMed

    J-GLOBAL

    researchmap

  • DV200 Index for Assessing RNA Integrity in Next-Generation Sequencing. International journal

    Takehiro Matsubara, Junichi Soh, Mizuki Morita, Takahiro Uwabo, Shuta Tomida, Toshiyoshi Fujiwara, Susumu Kanazawa, Shinichi Toyooka, Akira Hirasawa

    BioMed research international   2020   9349132 - 9349132   2020

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Poor quality of biological samples will result in an inaccurate analysis of next-generation sequencing (NGS). Therefore, methods to accurately evaluate sample integrity are needed. Among methods for evaluating RNA quality, the RNA integrity number equivalent (RINe) is widely used, whereas the DV200, which evaluates the percentage of fragments of >200 nucleotides, is also used as a quality assessment standard. In this study, we compared the RINe and DV200 RNA quality indexes to determine the most suitable RNA index for the NGS analysis. Seventy-one RNA samples were extracted from formalin-fixed paraffin-embedded tissue samples (n = 30), fresh-frozen samples (n = 25), or cell lines (n = 16). After assessing RNA quality using the RINe and DV200, we prepared two kinds of stranded mRNA sequencing libraries. Finally, we calculated the correlation between each RNA quality index and the amount of library product (1st PCR product per input RNA). The DV200 measure showed stronger correlation with the amount of library product than the RINe (R2 = 0.8208 for the DV200 versus 0.6927 for the RINe). Receiver operating characteristic curve analyses revealed that the DV200 was the better marker for predicting efficient library production than the RINe using a threshold of >10 ng/ng for the amount of the 1st PCR product per input RNA (cutoff value for the RINe and DV200, 2.3 and 66.1%; area under the curve, 0.99 and 0.91; sensitivity, 82% and 92%; and specificity, 93% and 100%, respectively). Our results indicate that NGS libraries prepared using RNA samples with the DV200 value > 66.1% exhibit greater sensitivity and specificity than those prepared with the RINe values > 2.3. These findings suggest that the DV200 is superior to the RINe, especially for low-quality RNA, because it is a more consistent assessment of the amount of the 1st NGS library product per input.

    DOI: 10.1155/2020/9349132

    PubMed

    researchmap

  • がんゲノム医療と実地臨床での課題

    HIRASAWA AKIRA

    日本婦人科腫瘍学会雑誌   37 ( 4 )   666 - 667   2019.10

     More details

    Language:Japanese  

    researchmap

  • BRCA1/2遺伝子バリアントとがん発症・臨床病理学的特徴および発症リスク因子を明らかにするための卵巣がん未発症を対象としたバイオバンク・コホート研究(JGOG3024)

    HIRASAWA AKIRA

    BRCA1/2遺伝子バリアントとがん発症・臨床病理学的特徴および発症リスク因子を明らかにするための卵巣がん未発症を対象としたバイオバンク・コホート研究(JGOG3024)   18th   67 - 69   2019.8

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Genome-wide DNA methylation profile of early-onset endometrial cancer: its correlation with genetic aberrations and comparison with late-onset endometrial cancer. International journal

    Takeshi Makabe, Eri Arai, Takuro Hirano, Nanako Ito, Yukihiro Fukamachi, Yoriko Takahashi, Akira Hirasawa, Wataru Yamagami, Nobuyuki Susumu, Daisuke Aoki, Yae Kanai

    Carcinogenesis   40 ( 5 )   611 - 623   2019.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    The present study was performed to clarify the significance of DNA methylation alterations during endometrial carcinogenesis. Genome-wide DNA methylation analysis and targeted sequencing of tumor-related genes were performed using the Infinium MethylationEPIC BeadChip and the Ion AmpliSeq Cancer Hotspot Panel v2, respectively, for 31 samples of normal control endometrial tissue from patients without endometrial cancer and 81 samples of endometrial cancer tissue. Principal component analysis revealed that tumor samples had a DNA methylation profile distinct from that of control samples. Gene Ontology enrichment analysis revealed significant differences of DNA methylation at 1034 CpG sites between early-onset endometrioid endometrial cancer (EE) tissue (patients aged ≤40 years) and late-onset endometrioid endometrial cancer (LE) tissue, which were accumulated among 'transcriptional factors'. Mutations of the CTNNB1 gene or DNA methylation alterations of genes participating in Wnt signaling were frequent in EEs, whereas genetic and epigenetic alterations of fibroblast growth factor signaling genes were observed in LEs. Unsupervised hierarchical clustering grouped EE samples in Cluster EA (n = 22) and samples in Cluster EB (n = 12). Clinicopathologically less aggressive tumors tended to be accumulated in Cluster EB, and DNA methylation levels of 18 genes including HOXA9, HOXD10 and SOX11 were associated with differences in such aggressiveness between the two clusters. We identified 11 marker CpG sites that discriminated EB samples from EA samples with 100% sensitivity and specificity. These data indicate that genetically and epigenetically different pathways may participate in the development of EEs and LEs, and that DNA methylation profiling may help predict tumors that are less aggressive and amenable to fertility preservation treatment.

    DOI: 10.1093/carcin/bgz046

    PubMed

    researchmap

  • 遺伝子情報を用いた遺伝性乳癌卵巣癌の予防と治療 Reviewed

    HIRASAWA AKIRA

    病理と臨床   37 ( 6 )   522 - 527   2019.6

     More details

    Language:Japanese  

    researchmap

  • 女性がんの化学予防 Reviewed

    HIRASAWA AKIRA

    産科と婦人科 増刊号   86 ( Suppl. )   350 - 353   2019.4

     More details

    Language:Japanese  

    researchmap

  • Guidelines for office gynecology in Japan: Japan Society of Obstetrics and Gynecology (JSOG) and Japan Association of Obstetricians and Gynecologists (JAOG) 2017 edition. International journal

    Ryuji Kawaguchi, Koji Matsumoto, Shigeo Akira, Ken Ishitani, Kazuhiro Iwasaku, Yutaka Ueda, Ryugo Okagaki, Hiroya Okano, Toshimichi Oki, Kaori Koga, Michiko Kido, Takumi Kurabayashi, Yasushi Kuribayashi, Yuichi Sato, Kaori Shiina, Yasushi Takai, Satoshi Tanimura, Osamu Chaki, Masakazu Terauchi, Yukiharu Todo, Yasuyuki Noguchi, Sayaka Nose-Ogura, Tsukasa Baba, Akira Hirasawa, Takuma Fujii, Tsuneo Fujii, Tetsuo Maruyama, Etsuko Miyagi, Kaoru Yanagida, Osamu Yoshino, Mitsutoshi Iwashita, Tsugio Maeda, Takashi Minegishi, Hiroshi Kobayashi

    The journal of obstetrics and gynaecology research   45 ( 4 )   766 - 786   2019.4

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Six years after the first edition of The Guideline for Gynecological Practice, which was jointly edited by The Japan Society of Obstetrics and Gynecology and The Japan Association of Obstetricians and Gynecologists, the third revised edition was published in 2017. The 2017 Guidelines includes 10 additional clinical questions (CQ), which brings the total to 95 CQ (12 on infectious disease, 28 on oncology and benign tumors, 27 on endocrinology and infertility and 28 on healthcare for women). Currently a consensus has been reached on the Guidelines and therefore the objective of this report is to present the general policies regarding diagnostic and treatment methods used in standard gynecological outpatient care that are considered appropriate. At the end of each answer, the corresponding recommendation level (A, B, C) is indicated.

    DOI: 10.1111/jog.13831

    PubMed

    researchmap

  • がんゲノム医療と女性ヘルスケア Reviewed

    HIRASAWA AKIRA

    医学のあゆみ   269 ( 1 )   85 - 88   2019.4

  • 婦人科がんとがんゲノム医療 Reviewed

    HIRASAWA AKIRA

    Pharma Medica   37 ( 2 )   9 - 14   2019.2

  • 婦人科における遺伝性腫瘍 Reviewed

    HIRASAWA AKIRA

    産婦人科の実際   68 ( 2 )   187 - 191   2019.2

  • Sentinel Node Navigation Surgery for Endometrial Cancer

    Susumu Nobuyuki, Yamagami Wataru, Kataoka Fumio, Hirano Takuro, Makabe Takeshi, Sakai Kensuke, Chiyoda Tatsuyuki, Nomura Hiroyuki, Hirasawa Akira, Aoki Daisuke

    SURGERY FOR GYNECOLOGIC CANCER   295 - 312   2019

  • Genome-wide DNA methylation profile of young-onset endometrial cancer

    Makabe Takeshi, Arai Eri, Hirasawa Akira, Yamagami Wataru, Susumu Nobuyuki, Aoki Daisuke, Kanai Yae

    CANCER SCIENCE   109   1304 - 1304   2018.12

     More details

    Language:English  

    researchmap

  • 遺伝性乳癌卵巣癌に対するリスク低減卵管卵巣摘出後のQOLに関する検討 Reviewed

    谷本 慧子, 平沢 晃, 牧田 和也, 岩田 卓, 堀場 裕子, 横田 めぐみ, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 高松 潔, 青木 大輔

    日本女性医学学会雑誌   26 ( 1 )   45 - 47   2018.11

     More details

    Language:Japanese  

    researchmap

  • Synchronous endometrial and ovarian cancer in Lynch syndrome with a MSH2 germline mutation: A case report. Reviewed International journal

    Takashi Takeda, Kouji Banno, Megumi Yanokura, Mayuka Anko, Arata Kobayashi, Asako Sera, Takayuki Takahashi, Masataka Adachi, Yusuke Kobayashi, Shigenori Hayashi, Hiroyuki Nomura, Akira Hirasawa, Eiichiro Tominaga, Daisuke Aoki

    Molecular and clinical oncology   9 ( 5 )   479 - 484   2018.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Synchronous endometrial and ovarian cancer (SEOC) is a rare entity among gynecological cancers, which exhibits endometrioid histology in its early stages and generally has a good prognosis. However, diagnosis is difficult and recent reports have demonstrated that most clinically diagnosed cases of SEOC have clonally related cancers, indicating metastatic cancer. The association of SEOC with Lynch syndrome is also not clearly understood. We herein present the case of a 41-year-old SEOC patient with MSH2 mutation. The endometrial cancer was an endometrioid adenocarcinoma and the ovarian cancer was mainly endometrioid, but also included a clear cell carcinoma with a borderline clear cell adenofibromatous component, indicating primary ovarian cancer. Both tumors exhibited microsatellite instability (MSI) and loss of expression of MSH2 and MSH6. The patient had a family history of colorectal and gastric cancers. Genetic analysis revealed a germline mutation in exon 6 of MSH2 (c.1042C>T, p.Gln348*) and the patient was diagnosed with Lynch syndrome. This MSH2 mutation has only been registered in one case in the InSiGHT variant databases and has not been reported in a gynecological tumor or SEOC to date. This case is a rare example of a patient with genetically diagnosed Lynch syndrome who also developed SEOC. This synchronous cancer is not common, but it may be caused by Lynch syndrome. Testing for MSI and immunohistochemistry for mismatch repair deficiency is necessary in cases with suspected SEOC.

    DOI: 10.3892/mco.2018.1723

    PubMed

    researchmap

  • 遺伝性腫瘍・家族性腫瘍

    HIRASAWA AKIRA

    日本医師会雑誌   147 ( 7 )   1401 - 1406   2018.10

     More details

    Language:Japanese  

    researchmap

  • GENOME-WIDE DNA METHYLATION ANALYSIS IN YOUNG-ONSET ENDOMETRIAL CANCER

    Makabe T, Arai E, Hirasawa A, Yamagami W, Nobuyuki S, Aoki D, Kanai Y

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   28   79 - 79   2018.9

     More details

    Language:English  

    researchmap

  • THE EFFICACY OF REPEATED HORMONAL THERAPY FOR INTRAUTERINE RECURRENCE FOLLOWING FERTILITY PRESERVING HORMONAL THERAPY FOR ENDOMETRIAL CANCER OR ATYPICAL ENDOMETRIAL HYPERPLASIA. Reviewed

    Hirano T, Yamagami W, Susumu N, Makabe T, Sakai K, Ninomiya T, Chiyoda T, Nomura H, Kataoka F, Hirasawa A, Banno K, Aoki D

    INTERNATIONAL JOURNAL OF GYNECOLOGIC CANCER   28 ( S2 )   1092 - 1092   2018.9

     More details

    Language:English   Publishing type:Research paper (conference, symposium, etc.)  

    researchmap

  • UNSUCCESSFUL HIGH-DOSE HORMONAL THERAPY FOR ENDOMETRIAL CANCER OR ATYPICAL ENDOMETRIAL HYPERPLASIA. Reviewed

    Tamagawa M, Yamagami W, Hirano T, Makabe T, Sakai K, Ninomiya T, Chiyoda T, Nomura H, Kataoka F, Hirasawa A, Banno K, Susumu N, Aoki D

    INTERNATIONAL JOURNAL OF GYNECOLOGIC CANCER   28 ( S2 )   1189 - 1189   2018.9

     More details

    Language:English   Publishing type:Research paper (conference, symposium, etc.)  

    researchmap

  • がんゲノム医療とHBOC

    HIRASAWA AKIRA

    日本HBOCコンソーシアムニュースレター   6   2018.9

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 婦人科疾患ゲノム異常の探索と女性ヘルスケアの個別化

    HIRASAWA AKIRA

    101   64 - 67   2018.8

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • GSTP1 rs1695 is associated with both hematological toxicity and prognosis of ovarian cancer treated with paclitaxel plus carboplatin combination chemotherapy: a comprehensive analysis using targeted resequencing of 100 pharmacogenes. Reviewed International journal

    Yoshihama T, Fukunaga K, Hirasawa A, Nomura H, Akahane T, Kataoka F, Yamagami W, Aoki D, Mushiroda T

    Oncotarget   9 ( 51 )   29789 - 29800   2018.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Purpose: To find genetic variants that predicted toxicity and/or efficacy of paclitaxel plus carboplatin combination therapy (TC therapy). Patients and methods: In a retrospective case-control study, we analyzed 320 patients who had received TC therapy for gynecological cancers (ovarian, fallopian tube, peritoneal, uterine, and cervical cancers) and collected their germline DNA. We performed a comprehensive pharmacogenomic analysis using a targeted resequencing panel of 100 pharmacogenes. For 1,013 variants passing QC, case-control association studies and survival analyses were conducted. Results: GSTP1 rs1695 showed the smallest p value for hematotoxicity association, and the 105Ile wild type allele had a significantly higher risk of severe hematotoxicity (neutropenia G4, thrombocytopenia ≥ G3 and anemia ≥ G3) than the 105Val allele (p=0.00034, odds ratio=5.71 (95% confidence interval:1.77-18.44)). Next, we assessed 5-year progression-free survival (PFS) and overall survival (OS) in 56 advanced ovarian cancer patients who received tri-weekly TC as a first-line chemotherapy. Patients with the 105Ile/105Ile genotype showed significantly better PFS (p=0.00070) and OS (p=0.0012) than those with the 105Ile/105Val or 105Val/105Val genotype. Conclusion: Our study indicates that the GSTP1 rs1695 105Ile/105Ile genotype is associated with both severe hematotoxicity and high efficacy of TC therapy, identifying a possible prognostic indicator for patients with TC therapy.

    DOI: 10.18632/oncotarget.25712

    PubMed

    researchmap

  • 有害事象によりベバシズマブ投与を中止した婦人科がん症例の検討 Reviewed

    大野 あゆみ, 千代田 達幸, 野村 弘行, 同前 愛, 早乙女 啓子, 冨永 英一郎, 岩田 卓, 山上 亘, 片岡 史夫, 平沢 晃, 田中 守, 青木 大輔

    東京産科婦人科学会会誌   67 ( 3 )   396 - 400   2018.7

     More details

    Language:Japanese  

    researchmap

  • 遺伝性腫瘍に対するリスク低減卵管卵巣摘出術 -RRSOの臨床試験やその適応、手技の実際と留意すべきポイント-

    AOKI DAISUKE

    産婦人科の実際   67 ( 5 )   549 - 556   2018.5

  • 遺伝性乳がん

    AOKI DAISUKE

    White   6 ( 1 )   15 - 22   2018.5

  • 遺伝性乳癌卵巣癌症候群に対するリスク低減卵管卵巣摘出後の漢方療法に関する検討 Reviewed

    平沢 晃, 牧田 和也, 岩田 卓, 堀場 裕子, 横田 めぐみ, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 青木 大輔

    産婦人科漢方研究のあゆみ   35 ( 35 )   189 - 191   2018.4

     More details

    Language:Japanese  

    researchmap

  • Is repeated high-dose medroxyprogesterone acetate (MPA) therapy permissible for patients with early stage endometrial cancer or atypical endometrial hyperplasia who desire preserving fertility? Reviewed International journal

    Wataru Yamagami, Nobuyuki Susumu, Takeshi Makabe, Kensuke Sakai, Hiroyuki Nomura, Fumio Kataoka, Akira Hirasawa, Kouji Banno, Daisuke Aoki

    JOURNAL OF GYNECOLOGIC ONCOLOGY   29 ( 2 )   e21   2018.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:KOREAN SOC GYNECOLOGY ONCOLOGY & COLPOSCOPY  

    Objective: Reports on the repeated administration of medroxyprogesterone acetate (MPA) for intrauterine recurrence after fertility-preserving therapy for atypical endometrial hyperplasia (AEH) and early grade 1 endometrioid carcinoma (G1) are lacking. We aimed to clarify the outcomes of repeated MPA therapy in cases of intrauterine recurrence after fertility-preserving therapy with MPA against AEH/early G1.Methods: Patients with AEH or stage IA well-differentiated endometrioid carcinoma without myometrial invasion who underwent first-line MPA therapy for primary lesions or intrauterine recurrence were divided into initial treatment and repeated treatment groups (162 and 82 patients, respectively). Oral MPA administration (400-600 mg/day) was continued until pathological tumor disappearance. Data regarding clinicopathological factors, adverse events, and outcomes following the initial and repeated hormonal treatments were extracted from medical records and analyzed.Results: Complete response rates in the initial and repeated treatment groups were 98.5% and 96.4%, respectively, among patients with AEH, and were 90.7% and 98.1%, respectively, among patients with G1. In the initial treatment group, 5-year recurrence-free survival (RFS) rates were 53.7% and 33.2% among patients with AEH and G1, respectively. In the repeated treatment group, RFS rates were 14.0% and 11.2% among patients with AEH and G1, respectively. Among patients with AEH, the pregnancy rate tended to be lower in the repeated treatment group than in the initial treatment group (11.1% vs. 29.2%; p=0.107), while no significant group difference was observed among patients with G1 (20.8% vs. 22.7%).Conclusion: Repeated treatment is sufficiently effective for intrauterine recurrence after hormonal therapy for AEH/early G1.

    DOI: 10.3802/jgo.2018.29.e21

    Web of Science

    Scopus

    PubMed

    researchmap

  • 婦人科疾患ゲノム異常の探索と女性ヘルスケアの個別化 Invited Reviewed

    HIRASAWA AKIRA

    日本女性医学学会雑誌   25 ( 2 )   156 - 158   2018.2

     More details

    Language:Japanese  

    researchmap

  • ADAM9 is over-expressed in human ovarian clear cell carcinomas and suppresses cisplatin-induced cell death Reviewed International journal

    Mari Ueno, Takayuki Shiomi, Satsuki Mochizuki, Miyuki Chijiiwa, Masayuki Shimoda, Yae Kanai, Fumio Kataoka, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki, Yasunori Okada

    CANCER SCIENCE   109 ( 2 )   471 - 482   2018.2

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY  

    ADAMs (a disintegrin and metalloproteinases) are involved in various biological events such as cell adhesion, migration and invasion, membrane protein shedding and proteolysis. However, there have been no systematic studies on the expression of ADAMs in human ovarian carcinomas. We therefore examined mRNA expression of all the proteolytic ADAM species including ADAM8, 9, 10, 12, 15, 17, 19, 20, 21, 28, 30, 33 and ADAMDEC1 in human ovarian carcinomas, and found that prototype membrane-anchored ADAM9m, but not secreted isoform ADAM9s, is significantly over-expressed in carcinomas than in control non-neoplastic ovarian tissue. Among the histological subtypes of serous, endometrioid, mucinous and clear cell carcinomas, ADAM9m expression was highest in clear cell carcinomas. Immunohistochemistry showed that all the clear cell carcinoma samples displayed ADAM9m primarily on the carcinoma cell membrane. By immunoblotting, ADAM9m was detected mainly in an active form in the clear cell carcinoma tissues. When two clear cell carcinoma cell lines (RMG-I and TOV21G cells) with ADAM9m expression were treated with cisplatin, viability was significantly reduced and apoptosis increased in ADAM9m knockdown cells compared with mock transfectants. In addition, treatment of the cells with neutralizing anti-ADAM9m antibody significantly decreased viability compared with non-immune IgG, whereas ADAM9m over-expression significantly increased viability compared with mock transfectants. Our data show, to the best of our knowledge, for the first time, that ADAM9m is over-expressed in an activated form in human ovarian clear cell carcinomas, and suggest that ADAM9m plays a key role in cisplatin resistance.

    DOI: 10.1111/cas.13469

    Web of Science

    PubMed

    researchmap

  • Japanese Society for Cancer of the Colon and Rectum (JSCCR) Guidelines 2016 for the Clinical Practice of Hereditary Colorectal Cancer (Translated Version). Reviewed

    Hideyuki Ishida, Tatsuro Yamaguchi, Kohji Tanakaya, Kiwamu Akagi, Yasuhiro Inoue, Kensuke Kumamoto, Hideki Shimodaira, Shigeki Sekine, Toshiaki Tanaka, Akiko Chino, Naohiro Tomita, Takeshi Nakajima, Hirotoshi Hasegawa, Takao Hinoi, Akira Hirasawa, Yasuyuki Miyakura, Yoshie Murakami, Kei Muro, Yoichi Ajioka, Yojiro Hashiguchi, Yoshinori Ito, Yutaka Saito, Tetsuya Hamaguchi, Megumi Ishiguro, Soichiro Ishihara, Yukihide Kanemitsu, Hiroshi Kawano, Yusuke Kinugasa, Norihiro Kokudo, Keiko Murofushi, Takako Nakajima, Shiro Oka, Yoshiharu Sakai, Akihiko Tsuji, Keisuke Uehara, Hideki Ueno, Kentaro Yamazaki, Masahiro Yoshida, Takayuki Yoshino, Narikazu Boku, Takahiro Fujimori, Michio Itabashi, Nobuo Koinuma, Takayuki Morita, Genichi Nishimura, Yuh Sakata, Yasuhiro Shimada, Keiichi Takahashi, Shinji Tanaka, Osamu Tsuruta, Toshiharu Yamaguchi, Kenichi Sugihara, Toshiaki Watanabe

    Journal of the anus, rectum and colon   2 ( Suppl I )   S1-S51   2018

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Hereditary colorectal cancer accounts for less than 5% of all colorectal cancer cases. Some of the unique characteristics that are commonly encountered in cases of hereditary colorectal cancer include early age at onset, synchronous/metachronous occurrence of the cancer, and association with multiple cancers in other organs, necessitating different management from sporadic colorectal cancer. While the diagnosis of familial adenomatous polyposis might be easy because usually 100 or more adenomas that develop in the colonic mucosa are in this condition, Lynch syndrome, which is the most commonly associated disease with hereditary colorectal cancer, is often missed in daily medical practice because of its relatively poorly defined clinical characteristics. In addition, the disease concept and diagnostic criteria for Lynch syndrome, which was once called hereditary non-polyposis colorectal cancer, have changed over time with continual research, thereby possibly creating confusion in clinical practice. Under these circumstances, the JSCCR Guideline Committee has developed the "JSCCR Guidelines 2016 for the Clinical Practice of Hereditary Colorectal Cancer (HCRC)," to allow delivery of appropriate medical care in daily practice to patients with familial adenomatous polyposis, Lynch syndrome, or other related diseases. The JSCCR Guidelines 2016 for HCRC were prepared by consensus reached among members of the JSCCR Guideline Committee, based on a careful review of the evidence retrieved from literature searches, and considering the medical health insurance system and actual clinical practice settings in Japan. Herein, we present the English version of the JSCCR Guidelines 2016 for HCRC.

    DOI: 10.23922/jarc.2017-028

    PubMed

    researchmap

  • Genetic Testing and Clinical Management Practices for Variants in Non-BRCA1/2 Breast (and Breast/Ovarian) Cancer Susceptibility Genes: An International Survey by the Evidence-Based Network for the Interpretation of Germline Mutant Alleles (ENIGMA) Clinical Working Group. Reviewed International journal

    Sarah M Nielsen, Diana M Eccles, Iris L Romero, Fahd Al-Mulla, Judith Balmaña, Michela Biancolella, Rien Bslok, Maria Adelaide Caligo, Mariarosaria Calvello, Gabriele Lorenzo Capone, Pietro Cavalli, T L Chris Chan, Kathleen B M Claes, Laura Cortesi, Fergus J Couch, Miguel de la Hoya, Simona De Toffol, Orland Diez, Susan M Domchek, Ros Eeles, Anna Efremidis, Florentia Fostira, David Goldgar, Andreas Hadjisavvas, Thomas V O Hansen, Akira Hirasawa, Claude Houdayer, Petra Kleiblova, Sophie Krieger, Conxi Lázaro, Maria Loizidou, Siranoush Manoukian, Arjen R Mensenkamp, Setareh Moghadasi, Alvaro N Monteiro, Luigi Mori, April Morrow, Nadia Naldi, Henriette R Nielsen, Olufunmilayo I Olopade, Nicholas S Pachter, Edenir I Palmero, Inge S Pedersen, Maria Piane, Marianna Puzzo, Mark Robson, Maria Rossing, Maria Christina Sini, Angela Solano, Jana Soukupova, Gianluca Tedaldi, Manuel Teixeira, Mads Thomassen, Maria Grazia Tibiletti, Amanda Toland, Therese Törngren, Erica Vaccari, Liliana Varesco, Ana Vega, Yvonne Wallis, Barbara Wappenschmidt, Jeffrey Weitzel, Amanda B Spurdle, Arcangela De Nicolo, Encarna B Gómez-García

    JCO precision oncology   2   2018

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Purpose: To describe a snapshot of international genetic testing practices, specifically regarding the use of multigene panels, for hereditary breast/ovarian cancers. We conducted a survey through the Evidence-Based Network for the Interpretation of Germline Mutant Alleles (ENIGMA) consortium, covering questions about 16 non-BRCA1/2 genes. Methods: Data were collected via in-person and paper/electronic surveys. ENIGMA members from around the world were invited to participate. Additional information was collected via country networks in the United Kingdom and in Italy. Results: Responses from 61 cancer genetics practices across 20 countries showed that 16 genes were tested by > 50% of the centers, but only six (PALB2, TP53, PTEN, CHEK2, ATM, and BRIP1) were tested regularly. US centers tested the genes most often, whereas United Kingdom and Italian centers with no direct ENIGMA affiliation at the time of the survey were the least likely to regularly test them. Most centers tested the 16 genes through multigene panels; some centers tested TP53, PTEN, and other cancer syndrome-associated genes individually. Most centers reported (likely) pathogenic variants to patients and would test family members for such variants. Gene-specific guidelines for breast and ovarian cancer risk management were limited and differed among countries, especially with regard to starting age and type of imaging and risk-reducing surgery recommendations. Conclusion: Currently, a small number of genes beyond BRCA1/2 are routinely analyzed worldwide, and management guidelines are limited and largely based on expert opinion. To attain clinical implementation of multigene panel testing through evidence-based management practices, it is paramount that clinicians (and patients) participate in international initiatives that share panel testing data, interpret sequence variants, and collect prospective data to underpin risk estimates and evaluate the outcome of risk intervention strategies.

    DOI: 10.1200/PO.18.00091

    PubMed

    researchmap

  • Prevalence of pathogenic germline variants detected by multigene sequencing in unselected Japanese patients with ovarian cancer. Invited Reviewed International journal

    Akira Hirasawa, Issei Imoto, Takuya Naruto, Tomoko Akahane, Wataru Yamagami, Hiroyuki Nomura, Kiyoshi Masuda, Nobuyuki Susumu, Hitoshi Tsuda, Daisuke Aoki

    Oncotarget   8 ( 68 )   112258 - 112267   2017.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:(in press)  

    Pathogenic germline BRCA1, BRCA2 (BRCA1/2), and several other gene variants predispose women to primary ovarian, fallopian tube, and peritoneal carcinoma (OC), although variant frequency and relevance information is scarce in Japanese women with OC. Using targeted panel sequencing, we screened 230 unselected Japanese women with OC from our hospital-based cohort for pathogenic germline variants in 75 or 79 OC-associated genes. Pathogenic variants of 11 genes were identified in 41 (17.8%) women: 19 (8.3%; BRCA1), 8 (3.5%; BRCA2), 6 (2.6%; mismatch repair genes), 3 (1.3%; RAD51D), 2 (0.9%; ATM), 1 (0.4%; MRE11A), 1 (FANCC), and 1 (GABRA6). Carriers of BRCA1/2 or any other tested gene pathogenic variants were more likely to be diagnosed younger, have first or second-degree relatives with OC, and have OC classified as high-grade serous carcinoma (HGSC). After adjustment for these variables, all 3 features were independent predictive factors for pathogenic variants in any tested genes whereas only the latter two remained for variants in BRCA1/2. Our data indicate similar variant prevalence in Japanese patients with OC and other ethnic groups and suggest that HGSC and OC family history may facilitate genetic predisposition prediction in Japanese patients with OC and referring high-risk patients for genetic counseling and testing.

    DOI: 10.18632/oncotarget.22733

    PubMed

    researchmap

  • Efficacy and safety of dose-dense paclitaxel plus carboplatin as neoadjuvant chemotherapy for advanced ovarian, fallopian tube or peritoneal cancer Reviewed International journal

    Tomoko Yoshihama, Hiroyuki Nomura, Naomi Iwasa, Fumio Kataoka, Shiho Hashimoto, Yoshiko Nanki, Takuro Hirano, Takeshi Makabe, Kensuke Sakai, Wataru Yamagami, Akira Hirasawa, Daisuke Aoki

    JAPANESE JOURNAL OF CLINICAL ONCOLOGY   47 ( 11 )   1019 - 1023   2017.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    Interval debulking surgery (IDS) after neoadjuvant chemotherapy (NAC) is currently one of the preferred treatment options for advanced ovarian, fallopian tube or peritoneal cancer. This study was conducted to evaluate the clinical efficacy and safety of dose-dense paclitaxel plus carboplatin therapy (ddTC therapy) as NAC for these cancers.A retrospective study was conducted in 25 patients with Stage III/IV ovarian, fallopian tube or peritoneal cancer who received ddTC therapy as NAC. For ddTC therapy, paclitaxel (80 mg/m(2)) was administered intravenously on Days 1, 8 and 15 and carboplatin (AUC 6.0 mg/ml x min) was administered intravenously on Day 1 every 3 weeks. IDS was performed after three cycles of ddTC therapy, and ddTC therapy was also continued after surgery.With ddTC therapy as NAC, the response rate was 92% and disease progression did not occur in any patient. Grade 4 hematologic toxicity and >= Grade 3 non-hematologic toxicity both occurred in 8% of the patients, but no patient discontinued NAC because of adverse events. When IDS was performed, the complete surgery rate was 64% and the optimal surgery rate was 96%. >= Grade 3 perioperative complications occurred in 16% of the patients, but there were no perioperative deaths. Median overall survival was 35.7 months and median progression-free survival was 17.7 months.This study showed that ddTC therapy was considerably effective and tolerable as NAC. The complete surgery rate was high with IDS, and perioperative complications were acceptable.

    DOI: 10.1093/jjco/hyx118

    Web of Science

    PubMed

    researchmap

  • 治療薬解説 PARP阻害薬

    AOKI DAISUKE

    カレントテラピー   35 ( 9 )   74 - 77   2017.9

     More details

    Language:Japanese  

    researchmap

  • A Comparison of Dye Versus Fluorescence Methods for Sentinel Lymph Node Mapping in Endometrial Cancer Reviewed International journal

    Wataru Yamagami, Nobuyuki Susumu, Fumio Kataoka, Takeshi Makabe, Kensuke Sakai, Tomomi Ninomiya, Michiko Wada, Hiroyuki Nomura, Akira Hirasawa, Kouji Banno, Tadaki Nakahara, Kaori Kameyama, Daisuke Aoki

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   27 ( 7 )   1517 - 1524   2017.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Objective Sentinel nodes (SNs) have been observed in several reports from Japan and overseas in cases with endometrial cancer; however, no consensus has been reached regarding the types of tracers or the method of their injection. A combination of the radioisotope (RI) and dye method is considered to be desirable. We assessed SN mapping using either dye or near-infrared fluorescence imaging to clarify a suitable method in cases of endometrial cancer.Methods Patients were enrolled from 92 patients diagnosed with endometrial cancer and having no extrauterine metastasis by the preoperative imaging between 2009 and 2014 at our institution. To identify the SNs, we performed 3 methods using either dye or fluorescence solutions in conjunction with a RI method. In the dye method, we injected indocyanine green in the uterine subserosa, visually identifying SNs as stained green. In the fluorescence method, a dilute indocyanine green solution (0.5 mg, fluorescence A or 0.25 mg, fluorescence B, each per 10 mL of solvent) was injected and the SN identified by the HyperEye Medical System.Results The SN detection rates were 100%, 100%, and 96% using dye and fluorescence A or B solution, respectively. Pelvic SNs were detected by the 3 methods in 98%, 100%, and 96% of cases and para-aortic SNs in 65%, 88%, and 74%, respectively. Fluorescence A solution was somewhat better than dye in detecting para-aortic SNs, although not significantly so (P = 0.07). The sensitivity and negative predictive values for detecting SNs with metastases with the dye method were 92% and 98% compared with 100% and 100%, respectively, for both fluorescence solutions.Conclusions Although both dye and fluorescence methods performed well, no method perfectly identified para-aortic SNs. The concomitant use of the RI method is required to detect para-aortic SNs.

    DOI: 10.1097/IGC.0000000000000997

    Web of Science

    PubMed

    researchmap

  • 遺伝性卵巣がん

    AOKI DAISUKE

    成人病と生活習慣病   47 ( 7 )   861 - 866   2017.7

  • 医療機器に生じたトラブル

    AOKI DAISUKE

    産婦人科の実際   66 ( 6 )   767 - 771   2017.6

  • Clinical utility of a self-administered questionnaire for assessment of hereditary gynecologic cancer. International journal

    Kenta Masuda, Akira Hirasawa, Haruko Irie-Kunitomi, Tomoko Akahane, Arisa Ueki, Yusuke Kobayashi, Wataru Yamagami, Hiroyuki Nomura, Fumio Kataoka, Eiichiro Tominaga, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    Japanese journal of clinical oncology   47 ( 5 )   401 - 406   2017.5

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Background: A patient's medical history and familial cancer history are important information for assessing the risk of hereditary cancer. We have generated a self-administered questionnaire for patients with gynecologic cancer. This pilot study analyzed the usefulness of this questionnaire and the rates of patients that meet the Society of Gynecologic Oncology criteria in ovarian cancer and endometrial cancer patients. Method: Ovarian or endometrial cancer patients were recruited for this study. After informed consent was obtained, participants completed the questionnaire. Genetic risks were assessed from the data of each patient's questionnaire by Society of Gynecologic Oncology guideline. Clinical and pathological findings were compared between the genetic risk groups. Results: A total of 105 patients were identified with ovarian cancer and 56 patients with endometrial cancer eligible for this study. According to the Society of Gynecologic Oncology guideline, of the 105 ovarian cancer patients, 25 patients (23%) had a 20-25% risk and three patients (2.9%) had a 5-10% risk of hereditary breast and ovarian cancer syndrome. A further 22 patients (21%) had a 5-10% risk of Lynch syndrome. Two patients (1.9%) met the Amsterdam criteria II. Of 56 endometrial cancer patients, 24 patients (42.9%) had a 5-10% risk of Lynch syndrome. The endometrial cancer patients with genetic risk of Lynch syndrome were younger (mean age: 47.79) at diagnosis compared to patients without a genetic risk of Lynch syndrome (mean age: 57.91). Conclusions: In this study, we were able to show that the newly designed questionnaire is a useful tool for evaluating cancer family history along with Society of Gynecologic Oncology criteria or Amsterdam criteria II. When considering the risk of Lynch syndrome for a patient with ovarian cancer, it is important to collect a second and third relative's family history.

    DOI: 10.1093/jjco/hyx019

    PubMed

    researchmap

  • Clinical utility of a self-administered questionnaire for assessment of hereditary gynecologic cancer. Reviewed International journal

    Kenta Masuda, Akira Hirasawa, Haruko Irie-Kunitomi, Tomoko Akahane, Arisa Ueki, Yusuke Kobayashi, Wataru Yamagami, Hiroyuki Nomura, Fumio Kataoka, Eiichiro Tominaga, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    Japanese journal of clinical oncology   47 ( 5 )   473 - 473   2017.5

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    This study shows that the newly designed self-administered questionnaire is a useful tool to assess the risk of hereditary cancer for patients with gynecologic cancer.A patient's medical history and familial cancer history are important information for assessing the risk of hereditary cancer. We have generated a self-administered questionnaire for patients with gynecologic cancer. This pilot study analyzed the usefulness of this questionnaire and the rates of patients that meet the Society of Gynecologic Oncology criteria in ovarian cancer and endometrial cancer patients.
    Ovarian or endometrial cancer patients were recruited for this study. After informed consent was obtained, participants completed the questionnaire. Genetic risks were assessed from the data of each patient's questionnaire by Society of Gynecologic Oncology guideline. Clinical and pathological findings were compared between the genetic risk groups.
    A total of 105 patients were identified with ovarian cancer and 56 patients with endometrial cancer eligible for this study. According to the Society of Gynecologic Oncology guideline, of the 105 ovarian cancer patients, 25 patients (23%) had a 20-25% risk and three patients (2.9%) had a 5-10% risk of hereditary breast and ovarian cancer syndrome. A further 22 patients (21%) had a 5-10% risk of Lynch syndrome. Two patients (1.9%) met the Amsterdam criteria II. Of 56 endometrial cancer patients, 24 patients (42.9%) had a 5-10% risk of Lynch syndrome. The endometrial cancer patients with genetic risk of Lynch syndrome were younger (mean age: 47.79) at diagnosis compared to patients without a genetic risk of Lynch syndrome (mean age: 57.91).
    In this study, we were able to show that the newly designed questionnaire is a useful tool for evaluating cancer family history along with Society of Gynecologic Oncology criteria or Amsterdam criteria II. When considering the risk of Lynch syndrome for a patient with ovarian cancer, it is important to collect a second and third relative's family history.

    DOI: 10.1093/jjco/hyx037

    Web of Science

    PubMed

    researchmap

  • Carcinoma of the lower uterine segment diagnosed with Lynch syndrome based on MSH6 germline mutation: A case report. Reviewed International journal

    Masataka Adachi, Kouji Banno, Kenta Masuda, Megumi Yanokura, Moito Iijima, Takashi Takeda, Haruko Kunitomi, Yusuke Kobayashi, Wataru Yamagami, Akira Hirasawa, Kaori Kameyama, Kokichi Sugano, Daisuke Aoki

    The journal of obstetrics and gynaecology research   43 ( 2 )   416 - 420   2017.2

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY  

    Endometrial cancer in the lower uterine segment (LUS) is associated with Lynch syndrome with MLH1 or MSH2 germline mutation. Here, we report a case of carcinoma of the LUS diagnosed with Lynch syndrome based on MSH6 germline mutation in a 46-year-old woman with abnormal vaginal bleeding. She had had rectal cancer at age 39 with a family history of colon cancer (father, 75 years), pancreatic cancer (paternal grandmother, 74 years), and colon cancer (maternal grandmother, 85 years). Magnetic resonance imaging showed a tumor in the LUS. Endometrial biopsy revealed endometrioid adenocarcinoma G1. As her cancer history met the revised Bethesda criteria, we examined microsatellite instability and the result was negative, but loss of the MSH6 expression was detected by immunohistochemistry. Genetic testing revealed deleterious germline mutation of MSH6, which was compatible with Lynch syndrome. To our knowledge, this is the first case of endometrial carcinoma of the LUS with MSH6 germline mutation.

    DOI: 10.1111/jog.13202

    Web of Science

    PubMed

    researchmap

  • UGT1A1 polymorphism as a prognostic indicator of stage I ovarian clear cell carcinoma patients treated with irinotecan Reviewed International journal

    Tomoko Yoshihama, Akira Hirasawa, Hiroyuki Nomura, Tomoko Akahane, Yoshiko Nanki, Wataru Yamagami, Fumio Kataoka, Eiichiro Tominaga, Nobuyuki Susumu, Taisei Mushiroda, Daisuke Aoki

    JAPANESE JOURNAL OF CLINICAL ONCOLOGY   47 ( 2 )   170 - 174   2017.2

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    We investigated whether UGT1A1 polymorphisms are associated with the prognosis of ovarian cancer patients treated with irinotecan. UGT1A1 genotypes were analyzed in 11 stage I ovarian clear cell carcinoma patients who received irinotecan as first-line therapy. Progression-free survival, overall survival and adverse events were also assessed for each genotype. Three patients harbored UGT1A1*1/*6 while another three harbored UGT1A1*1/*28. Two patients with a wildtype genotype experienced recurrence and one died, whereas no recurrence or death was observed in patients with heterozygous genotypes. Adverse events tended to be more severe in patients with UGT1A1*6 and *28, although progression-free survival and overall survival rates tended to be better than in wild-type; the differences were not significant. We conclude that UGT1A1 polymorphisms have the potential to be a prognostic marker of irinotecan treatment.

    DOI: 10.1093/jjco/hyw163

    Web of Science

    PubMed

    researchmap

  • Carcinoma of the lower uterine segment diagnosed with Lynch syndrome based on MSH6 germline mutation: A case report Reviewed

    Masataka Adachi, Kouji Banno, Kenta Masuda, Megumi Yanokura, Moito Iijima, Takashi Takeda, Haruko Kunitomi, Yusuke Kobayashi, Wataru Yamagami, Akira Hirasawa, Kaori Kameyama, Kokichi Sugano, Daisuke Aoki

    JOURNAL OF OBSTETRICS AND GYNAECOLOGY RESEARCH   43 ( 2 )   416 - 420   2017.2

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY  

    Endometrial cancer in the lower uterine segment (LUS) is associated with Lynch syndrome with MLH1 or MSH2 germline mutation. Here, we report a case of carcinoma of the LUS diagnosed with Lynch syndrome based on MSH6 germline mutation in a 46-year-old woman with abnormal vaginal bleeding. She had had rectal cancer at age 39 with a family history of colon cancer (father, 75 years), pancreatic cancer (paternal grandmother, 74 years), and colon cancer (maternal grandmother, 85 years). Magnetic resonance imaging showed a tumor in the LUS. Endometrial biopsy revealed endometrioid adenocarcinoma G1. As her cancer history met the revised Bethesda criteria, we examined microsatellite instability and the result was negative, but loss of the MSH6 expression was detected by immunohistochemistry. Genetic testing revealed deleterious germline mutation of MSH6, which was compatible with Lynch syndrome. To our knowledge, this is the first case of endometrial carcinoma of the LUS with MSH6 germline mutation.

    DOI: 10.1111/jog.13202

    Web of Science

    researchmap

  • 遺伝性乳癌卵巣癌症候群と女性ヘルスケア Invited

    平沢 晃, 青木大輔

    更年期と加齢のヘルスケア   16 ( 1 )   42 - 45   2017

     More details

    Language:Japanese  

    researchmap

  • 手術前禁忌薬(経口避妊薬,低用量エストロゲン-プロゲスチン配合薬)に関する医療安全対策 Reviewed

    高柳裕子, 冨永英一郎, 小林佑介, 仲村 勝, 片岡史夫, 平沢 晃, 阪埜浩司, 田中 守, 青木大輔

    東京産科婦人科学会会誌   66 ( 3 )   424 - 428   2017

     More details

    Language:Japanese  

    researchmap

  • 一般病院における家族性腫瘍相談外来とハイリスク外来の開設 –一般病院み求められる家族性腫瘍診療の意義についての考察- . Invited Reviewed

    植木有紗, 中田さくら, 安斎純子, 麻薙美香, 嶋田恭輔, 久保内光一, 三須久美子, 平沢 晃, 阪埜浩司, 菅野康吉, 小崎健次郎, 青木大輔

    家族性腫瘍   16 ( 2 )   38 - 43   2017

  • BRCA1またはBRCA2遺伝子変異陽性女性へのHRT Invited

    平沢 晃, 高松 潔, 青木大輔

    産科と婦人科   84 ( 12 )   1468 - 1471   2017

  • Consistency in drug response profiling. Reviewed International journal

    John Patrick Mpindi, Bhagwan Yadav, Päivi Östling, Prson Gautam, Disha Malani, Astrid Murumägi, Akira Hirasawa, Sara Kangaspeska, Krister Wennerberg, Olli Kallioniemi, Tero Aittokallio

    Nature   540 ( 7631 )   E5-E6 - E6   2016.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    DOI: 10.1038/nature20171

    Web of Science

    PubMed

    researchmap

  • Methylation Analysis of DNA Mismatch Repair Genes Using DNA Derived from the Peripheral Blood of Patients with Endometrial Cancer: Epimutation in Endometrial Carcinogenesis. Reviewed International journal

    Takashi Takeda, Kouji Banno, Megumi Yanokura, Masataka Adachi, Moito Iijima, Haruko Kunitomi, Kanako Nakamura, Miho Iida, Yuya Nogami, Kiyoko Umene, Kenta Masuda, Yusuke Kobayashi, Wataru Yamagami, Akira Hirasawa, Eiichiro Tominaga, Nobuyuki Susumu, Daisuke Aoki

    Genes   7 ( 10 )   e86   2016.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:MDPI AG  

    Germline mutation of DNA mismatch repair (MMR) genes is a cause of Lynch syndrome. Methylation of MutL homolog 1 (MLH1) and MutS homolog 2 (MSH2) has been detected in peripheral blood cells of patients with colorectal cancer. This methylation is referred to as epimutation. Methylation of these genes has not been studied in an unselected series of endometrial cancer cases. Therefore, we examined methylation of MLH1, MSH2, and MSH6 promoter regions of peripheral blood cells in 206 patients with endometrial cancer using a methylation-specific polymerase chain reaction (MSP). Germline mutation of MMR genes, microsatellite instability (MSI), and immunohistochemistry (IHC) were also analyzed in each case with epimutation. MLH1 epimutation was detected in a single patient out of a total of 206 (0.49%)-1 out of 58 (1.72%) with an onset age of less than 50 years. The patient with MLH1 epimutation showed high level MSI (MSI-H), loss of MLH1 expression and had developed endometrial cancer at 46 years old, complicated with colorectal cancer. No case had epimutation of MSH2 or MSH6. The MLH1 epimutation detected in a patient with endometrial cancer may be a cause of endometrial carcinogenesis. This result indicates that it is important to check epimutation in patients with endometrial cancer without a germline mutation of MMR genes.

    DOI: 10.3390/genes7100086

    Web of Science

    PubMed

    researchmap

  • 遺伝性腫瘍領域の新たな潮流

    AOKI DAISUKE

    実験医学   34 ( 16 )   2671 - 2674   2016.10

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 婦人科悪性腫瘍に脳梗塞を合併したTrousseau症候群5例の検討

    AOKI DAISUKE

    日本婦人科腫瘍学会雑誌   34 ( 4 )   620 - 625   2016.10

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Symptoms and effects of physical factors in Japanese middle-aged women. International journal

    Megumi Yokota, Kazuya Makita, Akira Hirasawa, Takashi Iwata, Daisuke Aoki

    Menopause (New York, N.Y.)   23 ( 9 )   974 - 83   2016.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:Lippincott Williams and Wilkins  

    OBJECTIVE: The aim of the study was to clarify the prevalence and severity rates of symptoms and investigate whether symptoms varied in relation to body mass index (BMI). METHODS: The study group composed of 1,969 women, aged 40 to 60 years, who presented at our department from 1993 through 2014. The participation rate was 98%. The presence or absence of symptoms was evaluated by having the participants complete the Keio Questionnaire, a self-administered questionnaire. To allow the results to be compared according to ovarian function, serum levels of follicle-stimulating hormone and estradiol were measured. Participants were classified into three groups according to BMI: underweight, normal weight, and overweight. Symptoms were also compared among these subgroups. RESULTS: The most common symptom was general fatigue. Vasomotor symptoms differed significantly between pre- and postmenopause status. When symptoms were analyzed according to BMI, the severity rates of the following symptoms were significantly higher in the overweight group than in the normal weight and underweight groups: hot flushes, sweats, joint pain, numbness, and incontinence. On the contrary, the underweight group had significantly higher severities of cold constitution, nervousness, and wrinkled skin than did the other groups. In addition, an increase in BMI was associated with an increased severity of vasomotor symptoms. CONCLUSIONS: The prevalence and severities of shoulder stiffness, considered a characteristic symptom in Japanese women, were high. Increased BMI was shown to be associated with a higher severity of vasomotor symptoms, joint pain, nervousness, and urinary symptoms.

    DOI: 10.1097/GME.0000000000000660

    Scopus

    PubMed

    researchmap

  • Symptoms and effects of physical factors in Japanese middle-aged women Reviewed

    Megumi Yokota, Kazuya Makita, Akira Hirasawa, Takashi Iwata, Daisuke Aoki

    MENOPAUSE-THE JOURNAL OF THE NORTH AMERICAN MENOPAUSE SOCIETY   23 ( 9 )   974 - 983   2016.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Objective:The aim of the study was to clarify the prevalence and severity rates of symptoms and investigate whether symptoms varied in relation to body mass index (BMI).Methods:The study group composed of 1,969 women, aged 40 to 60 years, who presented at our department from 1993 through 2014. The participation rate was 98%. The presence or absence of symptoms was evaluated by having the participants complete the Keio Questionnaire, a self-administered questionnaire. To allow the results to be compared according to ovarian function, serum levels of follicle-stimulating hormone and estradiol were measured. Participants were classified into three groups according to BMI: underweight, normal weight, and overweight. Symptoms were also compared among these subgroups.Results:The most common symptom was general fatigue. Vasomotor symptoms differed significantly between pre- and postmenopause status. When symptoms were analyzed according to BMI, the severity rates of the following symptoms were significantly higher in the overweight group than in the normal weight and underweight groups: hot flushes, sweats, joint pain, numbness, and incontinence. On the contrary, the underweight group had significantly higher severities of cold constitution, nervousness, and wrinkled skin than did the other groups. In addition, an increase in BMI was associated with an increased severity of vasomotor symptoms.Conclusions:The prevalence and severities of shoulder stiffness, considered a characteristic symptom in Japanese women, were high. Increased BMI was shown to be associated with a higher severity of vasomotor symptoms, joint pain, nervousness, and urinary symptoms.

    DOI: 10.1097/GME.0000000000000660

    Web of Science

    researchmap

  • Retrospective Analysis on the Feasibility and Efficacy of Docetaxel-Cisplatin Therapy for Recurrent Endometrial Cancer. International journal

    Tomomi Ninomiya, Wataru Yamagami, Nobuyuki Susumu, Takeshi Makabe, Kensuke Sakai, Michiko Wada, Aya Takigawa, Tatsuyuki Chiyoda, Hiroyuki Nomura, Fumio Kataoka, Akira Hirasawa, Kouji Banno, Daisuke Aoki

    Anticancer research   36 ( 4 )   1751 - 8   2016.4

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:INT INST ANTICANCER RESEARCH  

    AIM: There is poor evidence regarding effective treatment for recurrent endometrial cancer. We treated patients with recurrent endometrial cancer with docetaxel-cisplatin (DP) therapy as second-line or third-line chemotherapy. We aimed to evaluate the feasibility and efficacy of DP therapy for patients with recurrent endometrial cancer. PATIENT AND METHODS: We included 26 patients diagnosed with recurrent endometrial cancer, who underwent DP chemotherapy at our Institution. Docetaxel at 70 mg/m(2)and cisplatin at 60 mg/m(2)were administered by intravenous injection every 3 weeks. We retrospectively analyzed the clinicopathological factors associated with the response rate (RR) and prognosis. We also analyzed the adverse effects of DP therapy. RESULTS: Median follow-up was 33.8 months and the median number of therapy cycles was six. Grade 3 or 4 adverse effects included leukopenia (66%), neutropenia (81%), anemia (9%), diarrhea (12%), general fatigue (12%), liver dysfunction (4%), peripheral neuropathy (4%), and hyponatremia (4%). RR was 58% and the median progression-free survival (PFS) was 7.5 months. The group with a treatment-free interval of 6 months or more tended to have better PFS than that with less than 6 months (p=0.01). The group with a platinum-free interval of 6 months or more had significantly better PFS than that with less than 6 months (p=0.09). Although the history of taxane usage was not relevant to prognosis, a taxane-free interval of 12 months or more was associated with a tendency for better PFS (p=0.06). CONCLUSION: DP therapy was fully feasible and demonstrated efficacy for patients with recurrent endometrial cancer.

    Web of Science

    PubMed

    researchmap

  • 婦人科疾患における自覚症状としての「冷え」,疾患単位としての「冷え症」の合併頻度についての検討

    WATANABE KENJI

    日本産科婦人科学会雑誌   68 ( 2 )   677 - 677   2016.2

     More details

    Language:Japanese  

    researchmap

  • 遺伝性乳がん卵巣がんに対するリスク低減卵管卵巣摘出術と術後ヘルスケア

    AOKI DAISUKE

    更年期と加齢のヘルスケア   14 ( 2 )   316 - 318   2016.2

     More details

    Language:Japanese  

    researchmap

  • Factors affecting pregnancy outcomes in young women treated with fertility-preserving therapy for well-differentiated endometrial cancer or atypical endometrial hyperplasia. Reviewed International journal

    Osamu Inoue, Toshio Hamatani, Nobuyuki Susumu, Wataru Yamagami, Seiji Ogawa, Takashi Takemoto, Akira Hirasawa, Kouji Banno, Naoaki Kuji, Mamoru Tanaka, Daisuke Aoki

    Reproductive biology and endocrinology : RB&E   14 ( 1 )   2 - 2   2016.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BIOMED CENTRAL LTD  

    BACKGROUND: Patients hoping to preserve their fertility receive conservative treatment with high-dose medroxyprogesterone acetate (MPA) for well-differentiated endometrioid adenocarcinoma (EC) or atypical endometrial hyperplasia (AEH) . Such treatment generally involves frequent intrauterine operations, including dilation and curettage (D&C) and endometrial biopsy (EMB), which could result in endometritis, endometrial thinning, or intrauterine adhesion. In turn, any of these outcomes could adversely affect implantation and pregnancy development. The current study thus aimed to identify factors that might affect pregnancy following conservative treatment by MPA. METHODS: We compared a pregnancy group (45 patients) with a non-pregnancy group (53 patients) of MPA-treated patients to evaluate the factors affecting clinical pregnancy establishment. We undertook a multivariate logistic regression analysis based on factors shown by univariate analysis to be significantly different between the groups. Univariate analysis identified number of D&C, endometrial thickness, duration of MPA administration, age of pregnancy permission (the age at which a patient was first allowed to attempt pregnancy after disappearance of the lesion), period of disappearance of lesions, and recurrence as independent variables. RESULTS: The odds ratios (95 % confidence interval) of multivariate analysis for disease recurrence, endometrial thickness during ovulation, and age of pregnancy permission were 0.283 (0.102-0.785), 1.677 (1.251-2.248), and 0.889 (0.792-0.998), respectively. There was no significant difference in the other independent variables between groups. CONCLUSIONS: We identified three factors considered to affect pregnancy establishment following conservative treatment with MPA: recurrence, endometrial thickness during ovulation, and the age of the pregnancy permission. Introduction of infertility treatment including assisted reproductive technology (ART) soon after achieving tumor disappearance by MPA would therefore be beneficial for patients with disease recurrence, thin endometrium, or a higher age of pregnancy permission.

    DOI: 10.1186/s12958-015-0136-7

    Web of Science

    PubMed

    researchmap

  • バイオリソースを用いた研究基盤整備に関する国内外の動き Invited Reviewed

    平沢 晃, 青木大輔

    産科と婦人科   83 ( 1 )   13 - 19   2016

  • 遺伝性腫瘍 Invited Reviewed

    平沢 晃, 山上 亘, 青木大輔

    産婦人科の実際   65 ( 6 )   653 - 659   2016

  • Characterization of the STK11 splicing variant as a normal splicing isomer in a patient with Peutz-Jeghers syndrome harboring genomic deletion of the STK11 gene. Reviewed International journal

    Kenta Masuda, Yusuke Kobayashi, Tokuhiro Kimura, Kiyoko Umene, Kumiko Misu, Hiroyuki Nomura, Akira Hirasawa, Kouji Banno, Kenjiro Kosaki, Daisuke Aoki, Kokichi Sugano

    Human genome variation   3   16002 - 16002   2016

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    We report a STK11 splicing variant comprising a 131-bp insertion that is derived from intron 1, which has previously been reported to possess potent pathogenicity. The same variant was detected in a Peutz-Jeghers syndrome patient harboring a genomic deletion in the vicinity of exon 1 of the STK11 gene, which indicated that this variant was derived from the wild-type allele. We also found the same variant in other normal subjects. This variant corresponds to the predicted transcript variant of STK11 (XM_011528209), which is derived from the genomic sequence of Chr19 (NT_011295.12). Therefore, we concluded that the splicing variant was not pathogenic.

    DOI: 10.1038/hgv.2016.2

    PubMed

    researchmap

  • Profiling of Epithelial Ovarian Cancer as BRCAness Status with MLPA Method. Reviewed

    Hirasawa A, Akahane T, Masuda K, Ninomiya T, Yamagami W, Nomura H, Kataoka F, Banno K, Susumu N, Aoki D

    Curr Oncol   23 ( 3 )   e305   2016

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • 子宮体部・卵巣同時発生重複癌40症例の臨床病理学的検討. Reviewed

    小笠原 淳, 小林佑介, 野村弘行, 山上 亘, 片岡史夫, 平沢 晃, 冨永英一郎, 鈴木 淳, 阪埜浩司, 進 伸幸, 田中 守, 青木大輔

    東京産科婦人科学会会誌   65 ( 3 )   436 - 439   2016

     More details

    Language:Japanese  

    researchmap

  • 遺伝性乳がん卵巣がん; 遺伝性腫瘍-実地臨床での対応を目指して Invited

    平沢 晃, 青木大輔

    日本医師会雑誌   145 ( 4 )   705 - 709   2016

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 卵巣・卵管の良性腫瘍・類腫瘍 Invited

    日本女性医学学会編

    女性医学ガイドブック 思春期・性成熟期編2016年度版   151 - 154   2016

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 両側卵巣摘出術を施行した婦人科がんサバイバーのQOL向上を目指した疫学因子および遺伝因子の解析. Invited Reviewed

    平沢 晃

    日本女性医学学会雑誌   24 ( 1 )   48 - 52   2016

     More details

    Language:Japanese  

    researchmap

  • [Free fatty acid receptors as therapeutic targets for metabolic disorders].

    Akira Hirasawa, Masato Takeuchi, Ryouhei Shirai, Zao Chen, Shota Ishii, Keiko Iida

    Nihon yakurigaku zasshi. Folia pharmacologica Japonica   146 ( 6 )   296 - 301   2015.12

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    DOI: 10.1254/fpj.146.296

    PubMed

    researchmap

  • EVALUATION OF PRE- OR INTRA-OPERATIVE DIAGNOSTIC METHOD FOR UTERINE CARCINOSARCOMA

    T. Makabe, W. Yamagami, N. Susumu, K. Sakai, T. Yoshihama, N. Iwasa, N. Nakadaira, S. Hashimoto, T. Ninomiya, M. Wada, A. Takigawa, H. Nomura, F. Kataoka, A. Hirasawa, K. Banno, D. Aoki

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   25 ( 9 )   1107 - 1107   2015.10

     More details

    Language:English   Publishing type:Research paper (international conference proceedings)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Web of Science

    researchmap

  • 子宮体がんの予防とヘルスケア

    AOKI DAISUKE

    産婦人科の実際 女性ヘルスケア 集中講義!   61 ( 10月臨時増刊号 )   399 - 408   2015.10

     More details

    Language:Japanese  

    researchmap

  • 若年子宮体癌、および子宮内膜異型増殖症に対して妊孕性温存治療を施行することによる精神的影響

    横田 めぐみ, 山上 亘, 坂井 健良, 真壁 健, 二宮 委美, 和田 美智子, 野村 弘行, 片岡 史夫, 平澤 晃, 牧田 和也, 阪埜 浩司, 進 伸幸, 青木 大輔, 白波瀬 丈一郎

    日本女性医学学会雑誌   23 ( Suppl. )   140 - 140   2015.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • Intratumoral CD8(+) Lymphocyte Infiltration as a Prognostic Factor and Its Relationship With Cyclooxygenase 2 Expression and Microsatellite Instability in Endometrial Cancer Reviewed

    Tomohiro Suemori, Nobuyuki Susumu, Takashi Iwata, Kouji Banno, Wataru Yamagami, Akira Hirasawa, Kokichi Sugano, Eri Matsumoto, Daisuke Aoki

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   25 ( 7 )   1165 - 1172   2015.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Objective Microsatellite instability (MSI) is caused by a defective DNA mismatch repair system. Colorectal cancer in MSI-positive patients is characterized by an increased number of tumor-infiltrating lymphocytes. On the other hand, it has recently been reported that cyclooxygenase 2 (COX-2) suppresses antitumor immunity. The objectives of the present study were to clarify the relationships among MSI status, COX-2 expression, and antitumor immune status and to verify impact of these factors on the prognosis of endometrial cancer.
    Methods The data of 123 patients with endometrial cancer were analyzed. The numbers of tumor-infiltrating CD8(+) T lymphocytes within cancer cell nests (TILs), as a representative of the antitumor immunity, and COX-2 expression levels in the tumor cells were analyzed by immunohistochemical staining. Microsatellite instability was evaluated by polymerase chain reaction analysis for 11 markers. Fisher exact probability test, Kaplan-Meier method, and proportional hazards analysis were used for the statistical analyses.
    Results The MSI-positive tumors showed significantly higher grades (G2 or G3) and significantly larger numbers of TILs than did the MSI-negative tumors. The COX-2-high group showed significantly fewer TILs than did the COX-2-low group. Multivariate analysis identified a low number of TILs (&lt;10), positive lymph node involvement, and high tumor malignancy grade as factors independently associated with poor prognosis. The prognosis was significantly poorer in the patients with MSI-positive tumors with high COX-2 expression than in those with MSI-positive tumors showing low COX-2 expression.
    Conclusions The number of TILs, which was increased by MSI and decreased by COX-2 expression, was associated with a poorer prognosis in patients with endometrial cancer. We also propose that COX-2 may block MSI-activated TILs in the tumor microenvironment.

    DOI: 10.1097/IGC.0000000000000482

    Web of Science

    researchmap

  • High Expression of p62 Protein Is Associated with Poor Prognosis and Aggressive Phenotypes in Endometrial Cancer. International journal

    Reiko Iwadate, Jun Inoue, Hitoshi Tsuda, Masashi Takano, Kenichi Furuya, Akira Hirasawa, Daisuke Aoki, Johji Inazawa

    The American journal of pathology   185 ( 9 )   2523 - 33   2015.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    High expression of SQSTM1/p62 (p62) protein, which functions as a hub of oncogenic signaling pathways, has been detected in several human cancers. However, the clinicopathological and functional contribution of p62 expression is largely unknown in endometrial cancers (ECs). In this study, we assessed the expression status of p62 in primary ECs (n = 194) by immunohistochemistry and analyzed its clinical significance. Although p62 was expressed in the cytoplasm and/or nucleus in primary ECs, we observed that an expression subtype, high expression of cytoplasmic p62 but low expression of nuclear p62 (cytoplasm(High)/nucleus(Low)), significantly correlated with nonendometrioid types (P = 0.002), high grade (P < 0.001), deep myometrial invasion (P = 0.025), vascular invasion (P = 0.012), and poor prognosis (P < 0.001), and may be an independent prognostic marker of ECs (P = 0.011). Furthermore, RNA interference-mediated inhibition of p62 expression in the HEC-1A EC cell line led to the reduction of invasiveness and resistance to oxidative stress in vitro, as well as the suppression of in vivo tumor growth in an orthotopic mouse model of ECs. High expression of cytoplasmic p62 is a novel prognostic biomarker of ECs, and excess p62 expression may functionally contribute to the acquirement of malignant phenotypes in EC cells.

    DOI: 10.1016/j.ajpath.2015.05.008

    PubMed

    researchmap

  • Intratumoral CD8+ Lymphocyte Infiltration as a Prognostic Factor and Its Relationship With Cyclooxygenase 2 Expression and Microsatellite Instability in Endometrial Cancer. International journal

    Tomohiro Suemori, Nobuyuki Susumu, Takashi Iwata, Kouji Banno, Wataru Yamagami, Akira Hirasawa, Kokichi Sugano, Eri Matsumoto, Daisuke Aoki

    International journal of gynecological cancer : official journal of the International Gynecological Cancer Society   25 ( 7 )   1165 - 72   2015.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    OBJECTIVE: Microsatellite instability (MSI) is caused by a defective DNA mismatch repair system. Colorectal cancer in MSI-positive patients is characterized by an increased number of tumor-infiltrating lymphocytes. On the other hand, it has recently been reported that cyclooxygenase 2 (COX-2) suppresses antitumor immunity. The objectives of the present study were to clarify the relationships among MSI status, COX-2 expression, and antitumor immune status and to verify impact of these factors on the prognosis of endometrial cancer. METHODS: The data of 123 patients with endometrial cancer were analyzed. The numbers of tumor-infiltrating CD8 T lymphocytes within cancer cell nests (TILs), as a representative of the antitumor immunity, and COX-2 expression levels in the tumor cells were analyzed by immunohistochemical staining. Microsatellite instability was evaluated by polymerase chain reaction analysis for 11 markers. Fisher exact probability test, Kaplan-Meier method, and proportional hazards analysis were used for the statistical analyses. RESULTS: The MSI-positive tumors showed significantly higher grades (G2 or G3) and significantly larger numbers of TILs than did the MSI-negative tumors. The COX-2-high group showed significantly fewer TILs than did the COX-2-low group. Multivariate analysis identified a low number of TILs (<10), positive lymph node involvement, and high tumor malignancy grade as factors independently associated with poor prognosis. The prognosis was significantly poorer in the patients with MSI-positive tumors with high COX-2 expression than in those with MSI-positive tumors showing low COX-2 expression. CONCLUSIONS: The number of TILs, which was increased by MSI and decreased by COX-2 expression, was associated with a poorer prognosis in patients with endometrial cancer. We also propose that COX-2 may block MSI-activated TILs in the tumor microenvironment.

    DOI: 10.1097/IGC.0000000000000482

    Web of Science

    PubMed

    researchmap

  • Polymorphisms of estrogen metabolism-related genes ESR1, UGT2B17, and UGT1A1 are not associated with osteoporosis in surgically menopausal Japanese women. Reviewed International journal

    Megumi Yokota, Akira Hirasawa, Kazuya Makita, Tomoko Akahane, Kensuke Sakai, Takeshi Makabe, Yuko Horiba, Wataru Yamagami, Mariko Ogawa, Takashi Iwata, Shigehisa Yanamoto, Ryota Deshimaru, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    Przeglad menopauzalny = Menopause review   14 ( 3 )   161 - 7   2015.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:Termedia Publishing House Ltd.  

    INTRODUCTION: Bilateral salpingo-oophorectomy (BSO) is a risk factor for osteoporosis. Previous studies have reported an association between genetic polymorphisms and the risk of developing osteoporosis. However, the relationship between osteoporosis and genetic polymorphisms in Japanese women treated with BSO is not well understood. To improve the quality of life for post-BSO patients, it is important to determine the genetic factors that influence their risk for osteoporosis. The aim of this study was to investigate the association between gene variations of estrogen metabolism-related genes and osteoporosis in surgically menopausal patients, which may improve their quality of life. MATERIAL AND METHODS: This study included 203 menopausal women treated with BSO because of gynecologic disorders. One hundred and twenty-six women with artificial (surgical) menopause, who had undergone BSO in the premenopausal period, were compared with 77 women with natural menopause, who had undergone BSO in the postmenopausal period. The women were tested for bone mineral density to diagnose osteoporosis. Polymorphisms of estrogen receptor 1 (ESR1) and UDP-glucuronosyl transferase (UGT) genes UGT2B17 and UGT1A1 were analyzed, and their association with bone mass and osteoporosis was statistically evaluated. RESULTS: No significant association was found between osteoporosis and polymorphisms in ESR1, UGT2B17, or UGT1A1 in both groups, suggesting that BSO might be a more significant physiological factor in influencing bone mass density compared to genetic variations. CONCLUSIONS: These results suggest that the ESR1, UGT2B17, and UGT1A1 polymorphisms are not genetic factors affecting osteoporosis in postmenopausal Japanese women.

    DOI: 10.5114/pm.2015.54339

    Scopus

    PubMed

    researchmap

  • 一般病院における家族性腫瘍相談外来とハイリスク外来の開設

    植木 有紗, 安齋 純子, 中田 さくら, 麻薙 美香, 嶋田 恭輔, 久保内 光一, 三須 久美子, 平沢 晃, 阪埜 浩司, 菅野 康吉, 小崎 健次郎, 青木 大輔

    家族性腫瘍   15 ( 2 )   A96 - A96   2015.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 当科健康維持外来初診患者に認められた甲状腺機能異常の現状

    AOKI DAISUKE

    日本女性医学学会雑誌   22 ( 2 )   133 - 137   2015.4

     More details

    Language:Japanese  

    researchmap

  • 子宮体がんの予防とへするケア-妊孕性温存と術後のQOL改善を目指して-

    AOKI DAISUKE

    日本女性医学学会雑誌   22 ( 2 )   282 - 104   2015.4

     More details

    Language:Japanese  

    researchmap

  • Risk-reducing surgery in hereditary gynecological cancer: Clinical applications in Lynch syndrome and hereditary breast and ovarian cancer. Reviewed International journal

    Masataka Adachi, Kouji Banno, Megumi Yanokura, Miho Iida, Kanako Nakamura, Yuya Nogami, Kiyoko Umene, Kenta Masuda, Iori Kisu, Arisa Ueki, Akira Hirasawa, Eiichiro Tominaga, Daisuke Aoki

    Molecular and clinical oncology   3 ( 2 )   267 - 273   2015.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Risk-reducing surgery (RRS) is defined as a prophylactic approach with removal of organs at high risk of developing cancer, which is performed in cases without lesions or absence of clinically significant lesions. Hereditary gynecological cancers for which RRS is performed include hereditary breast and ovarian cancer (HBOC) and Lynch syndrome. For HBOC, RRS in the United States (US) is recommended for women with mutations in the breast cancer susceptibility (BRCA)1 and BRCA2 genes and bilateral salpingo-oophorectomy (BSO) is generally performed. This procedure may reduce the risk of breast, ovarian, Fallopian tube and primary peritoneal cancer, although ovarian deficiency symptoms occur postoperatively. For Lynch syndrome, RRS in the US is considered for postmenopausal women or for women who do not desire to bear children and BSO and hysterectomy are usually performed. This approach may reduce the risk of endometrial and ovarian cancer, although ovarian deficiency symptoms also occur. For RRS, there are several issues that must be addressed to reduce the risk of cancer development in patients with HBOC or Lynch syndrome. To the best of our knowledge, this is the first review to discuss RRS with a focus on hereditary gynecological cancer.

    PubMed

    researchmap

  • Clinicopathologic Analysis With Immunohistochemistry for DNA Mismatch Repair Protein Expression in Synchronous Primary Endometrial and Ovarian Cancers Reviewed

    Yusuke Kobayashi, Kanako Nakamura, Hiroyuki Nomura, Kouji Banno, Haruko Irie, Masataka Adachi, Miho Iida, Kiyoko Umene, Yuya Nogami, Kenta Masuda, Iori Kisu, Arisa Ueki, Wataru Yamagami, Fumio Kataoka, Akira Hirasawa, Eiichiro Tominaga, Nobuyuki Susumu, Daisuke Aoki

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   25 ( 3 )   440 - 446   2015.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Objective: Synchronous primary endometrial and ovarian cancers have been an important topic in clinical medicine because it is sometimes difficult to distinguish whether there are 2 primary tumors or a single primary tumor and an associated metastasis. In addition, although these tumors are recommended for either immunohistochemistry for DNA mismatch repair (MMR) proteins or a microsatellite instability test in the Bethesda guidelines as Lynch syndrome-associated cancers, few studies have completed these analyses. In this study, we characterized the clinicopathologic features and the expression pattern of MMR proteins in synchronous primary endometrial and ovarian cancers.
    Methods: Clinicopathologic features and the expression pattern of MMR proteins (MLH1, MSH2, and MSH6) were characterized and analyzed in 32 synchronous primary endometrial and ovarian cancers.
    Results: Most synchronous cancers are endometrioid type (endometrioid/endometrioid) (n = 24, 75%), grade 1 (n = 19, 59.4%), and diagnosed as stage I (n = 15, 46.9%) in both endometrium and ovary. It is worth mentioning that 75% of the patients (n = 24) had endometriosis, which was more common (n = 21, 87.5%) in endometrioid/endometrioid cancers, whereas only 3 cases (37.5%) were of different histology (P = 0.018). Loss of expression of at least 1 MMR protein was observed in 17 (53.1%) of the endometrial tumors and in 10 (31.3%) of ovarian tumors. Only 4 cases (12.5%) that had specific MMR protein loss showed the same type of loss for both endometrial and ovarian tumors, in which 3 of the cases were losses in MLH1. One case showed concordant MSH6 protein loss, although the cases did not meet the Amsterdam criteria II.
    Conclusions: These results suggest that most synchronous primary endometrial ovarian cancers are not hereditary cancers caused by germ line mutations but rather sporadic cancers.

    DOI: 10.1097/IGC.0000000000000377

    Web of Science

    researchmap

  • Clinicopathologic analysis with immunohistochemistry for DNA mismatch repair protein expression in synchronous primary endometrial and ovarian cancers. International journal

    Yusuke Kobayashi, Kanako Nakamura, Hiroyuki Nomura, Kouji Banno, Haruko Irie, Masataka Adachi, Miho Iida, Kiyoko Umene, Yuya Nogami, Kenta Masuda, Iori Kisu, Arisa Ueki, Wataru Yamagami, Fumio Kataoka, Akira Hirasawa, Eiichiro Tominaga, Nobuyuki Susumu, Daisuke Aoki

    International journal of gynecological cancer : official journal of the International Gynecological Cancer Society   25 ( 3 )   440 - 6   2015.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    OBJECTIVE: Synchronous primary endometrial and ovarian cancers have been an important topic in clinical medicine because it is sometimes difficult to distinguish whether there are 2 primary tumors or a single primary tumor and an associated metastasis. In addition, although these tumors are recommended for either immunohistochemistry for DNA mismatch repair (MMR) proteins or a microsatellite instability test in the Bethesda guidelines as Lynch syndrome-associated cancers, few studies have completed these analyses. In this study, we characterized the clinicopathologic features and the expression pattern of MMR proteins in synchronous primary endometrial and ovarian cancers. METHODS: Clinicopathologic features and the expression pattern of MMR proteins (MLH1, MSH2, and MSH6) were characterized and analyzed in 32 synchronous primary endometrial and ovarian cancers. RESULTS: Most synchronous cancers are endometrioid type (endometrioid/endometrioid) (n = 24, 75%), grade 1 (n = 19, 59.4%), and diagnosed as stage I (n = 15, 46.9%) in both endometrium and ovary. It is worth mentioning that 75% of the patients (n = 24) had endometriosis, which was more common (n = 21, 87.5%) in endometrioid/endometrioid cancers, whereas only 3 cases (37.5%) were of different histology (P = 0.018). Loss of expression of at least 1 MMR protein was observed in 17 (53.1%) of the endometrial tumors and in 10 (31.3%) of ovarian tumors. Only 4 cases (12.5%) that had specific MMR protein loss showed the same type of loss for both endometrial and ovarian tumors, in which 3 of the cases were losses in MLH1. One case showed concordant MSH6 protein loss, although the cases did not meet the Amsterdam criteria II. CONCLUSIONS: These results suggest that most synchronous primary endometrial ovarian cancers are not hereditary cancers caused by germ line mutations but rather sporadic cancers.

    DOI: 10.1097/IGC.0000000000000377

    Web of Science

    PubMed

    researchmap

  • 遺伝性乳癌・卵巣癌とLynch症候群のリスク低減手術

    AOKI DAISUKE

    産婦人科の実際   64 ( 3 )   377 - 383   2015.3

     More details

    Language:Japanese  

    researchmap

  • Osteoporosis is less frequent in endometrial cancer survivors with hypertriglyceridemia. International journal

    Akira Hirasawa, Kazuya Makita, Tomoko Akahane, Wataru Yamagami, Takeshi Makabe, Megumi Yokota, Yuko Horiba, Mariko Ogawa, Shigehisa Yanamoto, Rhota Deshimaru, Eiichiro Tominaga, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    Japanese journal of clinical oncology   45 ( 1 )   127 - 31   2015.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    We previously reported an association between dyslipidemia and endometrial cancers. Osteoporosis is also reported to relate with some cancers. A common etiologic event has been proposed between dyslipidemia and osteoporosis. However, the pattern of interrelationships among dyslipidemia, osteoporosis and endometrial cancer is not well understood. To improve the quality of life of endometrial cancer survivors, these relationships should be determined. This study included 179 Japanese menopausal women who underwent bilateral salpingo-oophorectomy, including 114 women with incident endometrial cancer and 65 without endometrial cancer. The women were categorized according to dyslipidemia status. Bone mineral density was measured and compared between groups. Osteoporosis was statistically more frequent in women with hypertriglyceridemia who did not have endometrial cancer. In contrast, osteoporosis was statistically less frequent in women with hypertriglyceridemia who had endometrial cancer. In this cross-sectional study in a Japanese population, osteoporosis was associated with hypertriglyceridemia in post-menopausal women without endometrial cancer, but was less frequent in endometrial cancer survivors with hypertriglyceridemia.

    DOI: 10.1093/jjco/hyu164

    Web of Science

    PubMed

    researchmap

  • Osteoporosis is less frequent in endometrial cancer survivors with hypertriglyceridemia Reviewed

    Akira Hirasawa, Kazuya Makita, Tomoko Akahane, Wataru Yamagami, Takeshi Makabe, Megumi Yokota, Yuko Horiba, Mariko Ogawa, Shigehisa Yanamoto, Rhota Deshimaru, Eiichiro Tominaga, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    JAPANESE JOURNAL OF CLINICAL ONCOLOGY   45 ( 1 )   127 - 131   2015.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    We previously reported an association between dyslipidemia and endometrial cancers. Osteoporosis is also reported to relate with some cancers. A common etiologic event has been proposed between dyslipidemia and osteoporosis. However, the pattern of interrelationships among dyslipidemia, osteoporosis and endometrial cancer is not well understood. To improve the quality of life of endometrial cancer survivors, these relationships should be determined. This study included 179 Japanese menopausal women who underwent bilateral salpingo-oophorectomy, including 114 women with incident endometrial cancer and 65 without endometrial cancer. The women were categorized according to dyslipidemia status. Bone mineral density was measured and compared between groups. Osteoporosis was statistically more frequent in women with hypertriglyceridemia who did not have endometrial cancer. In contrast, osteoporosis was statistically less frequent in women with hypertriglyceridemia who had endometrial cancer. In this cross-sectional study in a Japanese population, osteoporosis was associated with hypertriglyceridemia in post-menopausal women without endometrial cancer, but was less frequent in endometrial cancer survivors with hypertriglyceridemia.

    DOI: 10.1093/jjco/hyu164

    Web of Science

    researchmap

  • Polymorphisms of estrogen metabolism-related genes ESR1, UGT2B17, and UGT1A1 are not associated with osteoporosis in surgically menopausal Japanese women

    Megumi Yokota, Akira Hirasawa, Kazuya Makita, Tomoko Akahane, Kensuke Sakai, Takeshi Makabe, Yuko Horiba, Wataru Yamagami, Mariko Ogawa, Takashi Iwata, Shigehisa Yanamoto, Ryota Deshimaru, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    MENOPAUSE REVIEW-PRZEGLAD MENOPAUZALNY   14 ( 3 )   161 - 167   2015

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:TERMEDIA PUBLISHING HOUSE LTD  

    Introduction: Bilateral salpingo-oophorectomy (BSO) is a risk factor for osteoporosis. Previous studies have reported an association between genetic polymorphisms and the risk of developing osteoporosis. However, the relationship between osteoporosis and genetic polymorphisms in Japanese women treated with BSO is not well understood. To improve the quality of life for post-BSO patients, it is important to determine the genetic factors that influence their risk for osteoporosis. The aim of this study was to investigate the association between gene variations of estrogen metabolism-related genes and osteoporosis in surgically menopausal patients, which may improve their quality of life.Material and methods: This study included 203 menopausal women treated with BSO because of gynecologic disorders. One hundred and twenty-six women with artificial (surgical) menopause, who had undergone BSO in the premenopausal period, were compared with 77 women with natural menopause, who had undergone BSO in the postmenopausal period. The women were tested for bone mineral density to diagnose osteoporosis. Polymorphisms of estrogen receptor 1 (ESR1) and UDP-glucuronosyl transferase (UGT) genes UGT2B17 and UGT1A1 were analyzed, and their association with bone mass and osteoporosis was statistically evaluated.Results: No significant association was found between osteoporosis and polymorphisms in ESR1, UGT2B17, or UGT1A1 in both groups, suggesting that BSO might be a more significant physiological factor in influencing bone mass density compared to genetic variations.Conclusions: These results suggest that the ESR1, UGT2B17, and UGT1A1 polymorphisms are not genetic factors affecting osteoporosis in postmenopausal Japanese women.

    DOI: 10.5114/pm.2015.54339

    Web of Science

    Scopus

    researchmap

  • High Expression of p62 Protein Is Associated with Poor Prognosis and Aggressive Phenotypes in Endometrial Cancer. Reviewed

    Iwadate R, Inoue J, Tsuda H, Takano M, Furuya K, Hirasawa A, Aoki D, Inazawa J

    Am J Pathol   185 ( 9 )   2523 - 2533   2015

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    DOI: 10.1016/j.ajpath.2015.05.008

    researchmap

  • BRCA1/2遺伝子変異保持者に対するリスク低減卵管卵巣摘出術とサーベイランス Invited Reviewed

    平沢 晃, 増田健太, 青木大輔

    産科と婦人科   82 ( 6 )   639 - 643   2015

  • 臓器・領域別家族性腫瘍の臨床 卵巣癌 Invited Reviewed

    植木有紗, 増田健太, 平沢 晃, 中田さくら, 青木大輔

    日本臨床   73 ( 6 )   462 - 466   2015

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 遺伝性乳癌卵巣癌 Invited Reviewed

    平沢 晃, 増田健太, 青木大輔

    臨床画像   31 ( 10 )   220 - 221   2015

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 子宮体癌の予防とヘルスケア Invited Reviewed

    進 伸幸, 平沢 晃, 山上 亘, 青木大輔

    産婦人科の実際   64 ( 1 )   1741 - 1750   2015

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 遺伝性乳癌卵巣癌の遺伝子検査 Reviewed

    平沢 晃, 増田健太, 青木大輔

    産科と婦人科   82 ( Sup )   202 - 205   2015

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Features of ovarian cancer in Lynch syndrome (Review). Reviewed International journal

    Kanako Nakamura, Kouji Banno, Megumi Yanokura, Miho Iida, Masataka Adachi, Kenta Masuda, Arisa Ueki, Yusuke Kobayashi, Hiroyuki Nomura, Akira Hirasawa, Eiichiro Tominaga, Daisuke Aoki

    Molecular and clinical oncology   2 ( 6 )   909 - 916   2014.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Lynch syndrome is a hereditary ovarian cancer with a prevalence of 0.9-2.7%. Lynch syndrome accounts for 10-15% of hereditary ovarian cancers, while hereditary breast and ovarian cancer syndrome accounts for 65-75% of these cancers. The lifetime risk for ovarian cancer in families with Lynch syndrome is ~8%, which is lower than colorectal and endometrial cancers, and ovarian cancer is not listed in the Amsterdam Criteria II. More than half of sporadic ovarian cancers are diagnosed in stage III or IV, but ≥80% of ovarian cancers in Lynch syndrome are diagnosed in stage I or II. Ovarian cancers in Lynch syndrome mostly have non-serous histology and different properties from those of sporadic ovarian cancers. A screening method for ovarian cancers in Lynch syndrome has yet to be established and clinical studies of prophylactic administration of oral contraceptives are not available. However, molecular profiles at the genetic level indicate that ovarian cancer in Lynch syndrome has a more favorable prognosis than sporadic ovarian cancer. Inhibitors of the phosphatidylinositol 3-kinase/mammalian target of the rapamycin pathway and anti-epidermal growth factor antibodies may have efficacy for the disease. To the best of our knowledge, this is the first review focusing on ovarian cancer in Lynch syndrome.

    PubMed

    researchmap

  • Clinicopathological study on para-aortic lymph node metastasis without pelvic lymph node metastasis in endometrial cancer. Reviewed International journal

    Shoko Tomisato, Wataru Yamagami, Nobuyuki Susumu, Michiko Kuwahata, Aya Takigawa, Hiroyuki Nomura, Fumio Kataoka, Akira Hirasawa, Kouji Banno, Daisuke Aoki

    The journal of obstetrics and gynaecology research   40 ( 6 )   1733 - 9   2014.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY-BLACKWELL  

    AIM: One of the important risk factors for recurrence of endometrial cancer is lymph node metastasis. The regional lymph nodes are pelvic lymph nodes (PLN) and para-aortic lymph nodes (PAN). PAN metastasis was often detected in the cases with PLN metastasis. However, PAN metastasis not associated with PLN metastasis was identified in a few cases. We focused on nine cases with PAN metastasis and without PLN metastasis. MATERIAL AND METHODS: The subjects of this study were 260 cases that were diagnosed with endometrial cancer. The initial treatments were surgery, including pelvic and para-aortic lymphadenectomy. Nine of these cases had PAN metastasis but did not have PLN metastasis. We retrospectively analyzed the clinicopathological factors and prognosis in cases with PLN-PAN+ cases. RESULTS: A total of 91 (35%) cases were identified as positive for either PLN or PAN. PAN metastases were detected in 62.6% of the cases that had some regional lymph node metastases and 3.5% of all cases were PLN- and PAN+. In all PLN-PAN+ cases, PAN swelling was not detected by preoperative chest-abdominal computed tomography scan. There were no clear trends among risk factors of regional lymph node metastasis. The 5-year progression-free survival was 87.1% for PLN-PAN- cases, 67.5% for PLN+PAN- cases, 44.4% for PLN-PAN+ cases, and 33.2% for PLN+PAN+ cases. CONCLUSION: During diagnosis and treatment for endometrial cancer, PLN-PAN+ cases should also be considered because the prognosis in PLN-PAN+ cases tended to be lower than that in PLN-PAN- cases and PLN+PAN- cases.

    DOI: 10.1111/jog.12399

    Web of Science

    PubMed

    researchmap

  • Clinicopathological study on para-aortic lymph node metastasis without pelvic lymph node metastasis in endometrial cancer

    Shoko Tomisato, Wataru Yamagami, Nobuyuki Susumu, Michiko Kuwahata, Aya Takigawa, Hiroyuki Nomura, Fumio Kataoka, Akira Hirasawa, Kouji Banno, Daisuke Aoki

    JOURNAL OF OBSTETRICS AND GYNAECOLOGY RESEARCH   40 ( 6 )   1733 - 1739   2014.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY  

    Aim One of the important risk factors for recurrence of endometrial cancer is lymph node metastasis. The regional lymph nodes are pelvic lymph nodes (PLN) and para-aortic lymph nodes (PAN). PAN metastasis was often detected in the cases with PLN metastasis. However, PAN metastasis not associated with PLN metastasis was identified in a few cases. We focused on nine cases with PAN metastasis and without PLN metastasis. Material and Methods The subjects of this study were 260 cases that were diagnosed with endometrial cancer. The initial treatments were surgery, including pelvic and para-aortic lymphadenectomy. Nine of these cases had PAN metastasis but did not have PLN metastasis. We retrospectively analyzed the clinicopathological factors and prognosis in cases with PLN-PAN+ cases. Results A total of 91 (35%) cases were identified as positive for either PLN or PAN. PAN metastases were detected in 62.6% of the cases that had some regional lymph node metastases and 3.5% of all cases were PLN- and PAN+. In all PLN-PAN+ cases, PAN swelling was not detected by preoperative chest-abdominal computed tomography scan. There were no clear trends among risk factors of regional lymph node metastasis. The 5-year progression-free survival was 87.1% for PLN-PAN- cases, 67.5% for PLN+PAN- cases, 44.4% for PLN-PAN+ cases, and 33.2% for PLN+PAN+ cases. Conclusion During diagnosis and treatment for endometrial cancer, PLN-PAN+ cases should also be considered because the prognosis in PLN-PAN+ cases tended to be lower than that in PLN-PAN- cases and PLN+PAN- cases.

    DOI: 10.1111/jog.12399

    Web of Science

    researchmap

  • A tumor of the uterine cervix with a complex histology in a Peutz-Jeghers syndrome patient with genomic deletion of the STK11 exon 1 region

    Yusuke Kobayashi, Kenta Masuda, Tokuhiro Kimura, Hiroyuki Nomura, Akira Hirasawa, Kouji Banno, Nobuyuki Susumu, Kokichi Sugano, Daisuke Aoki

    FUTURE ONCOLOGY   10 ( 2 )   171 - 177   2014.2

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:FUTURE MEDICINE LTD  

    Patients with Peutz-Jeghers syndrome (PJS) have a risk of complicating malignant tumors, including cancer of the uterine cervix. Mutations in the STK11 gene have been identified as being responsible for PJS. However, the genotype-phenotype correlation in PJS is poorly understood, especially with respect to malignant tumors. Here, we report a detailed analysis of a case of a cervical tumor in a PJS patient showing a large genomic deletion in exon 1 of STK11 without human papillomavirus infection. Histological examination revealed a complex histology consisting of three components: lobular endocervical gland hyperplasia (LEGH), minimal deviation adenocarcinoma (MDA) and mucinous adenocarcinoma. Immunohistochemistry for STK11 was positive in the LEGH and MDA components, while that of the mucinous adenocarcinoma stained very faintly. These findings support a close relationship among LEGH, MDA and mucinous adenocarcinoma and imply that inactivation of STK11 may occur during progression from MDA to mucinous adenocarcinoma.

    DOI: 10.2217/FON.13.180

    Web of Science

    researchmap

  • A tumor of the uterine cervix with a complex histology in a Peutz-Jeghers syndrome patient with genomic deletion of the STK11 exon 1 region. Reviewed International journal

    Yusuke Kobayashi, Kenta Masuda, Tokuhiro Kimura, Hiroyuki Nomura, Akira Hirasawa, Kouji Banno, Nobuyuki Susumu, Kokichi Sugano, Daisuke Aoki

    Future oncology (London, England)   10 ( 2 )   171 - 7   2014.2

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:FUTURE MEDICINE LTD  

    Patients with Peutz-Jeghers syndrome (PJS) have a risk of complicating malignant tumors, including cancer of the uterine cervix. Mutations in the STK11 gene have been identified as being responsible for PJS. However, the genotype-phenotype correlation in PJS is poorly understood, especially with respect to malignant tumors. Here, we report a detailed analysis of a case of a cervical tumor in a PJS patient showing a large genomic deletion in exon 1 of STK11 without human papillomavirus infection. Histological examination revealed a complex histology consisting of three components: lobular endocervical gland hyperplasia (LEGH), minimal deviation adenocarcinoma (MDA) and mucinous adenocarcinoma. Immunohistochemistry for STK11 was positive in the LEGH and MDA components, while that of the mucinous adenocarcinoma stained very faintly. These findings support a close relationship among LEGH, MDA and mucinous adenocarcinoma and imply that inactivation of STK11 may occur during progression from MDA to mucinous adenocarcinoma.

    DOI: 10.2217/fon.13.180

    Web of Science

    PubMed

    researchmap

  • Family History and BRCA1/BRCA2 Status Among Japanese Ovarian Cancer Patients and Occult Cancer in a BRCA1 Mutant Case Reviewed

    Akira Hirasawa, Kenta Masuda, Tomoko Akahane, Arisa Ueki, Megumi Yokota, Tomohiko Tsuruta, Hiroyuki Nomura, Fumio Kataoka, Eiichiro Tominaga, Kouji Banno, Kazuya Makita, Nobuyuki Susumu, Kokichi Sugano, Kenjiro Kosaki, Kaori Kameyama, Daisuke Aoki

    JAPANESE JOURNAL OF CLINICAL ONCOLOGY   44 ( 1 )   49 - 56   2014.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    This study aimed to examine family history among Japanese ovarian cancer patients and to investigate the TP53 status of fallopian tube epithelial and ovarian cancer cells in a Japanese BRCA1 mutant case that may be associated with the transformed state in hereditary ovarian cancer.
    One hundred and two primary ovarian cancer patients were retrospectively evaluated in this cross-sectional study. The family history of cancer was determined in probands. In a BRCA1 mutant case, p53 immunostaining and direct sequencing, followed by laser-capture microdissection, were performed for the fallopian tube, considered the origin of ovarian cancer.
    Nine of 102 (8.8) families were regarded as having hereditary breastovarian cancer syndrome, two families (2.0) were diagnosed with Lynch syndrome and six patients harbored BRCA1 or BRCA2 mutations. One case underwent risk-reductive salpingo-oophorectomy as a BRCA1 mutant carrier was retrospectively diagnosed as occult cancer. Common TP53 mutations were detected in cancer and fallopian tube epithelial cells in the case.
    Here, we integrate family cancer history and histology in ovarian cancer cases as well as TP53 status in a BRCA1 mutant case into a discussion regarding carcinogenesis in a Japanese population. The TP53 status for the BRCA1 mutant case examined here supports the recently proposed theory that ovarian cancer develops because of BRCA1 or BRCA2 inactivation and/or TP53 mutations.

    DOI: 10.1093/jjco/hyt171

    Web of Science

    researchmap

  • Family history and BRCA1/BRCA2 status among Japanese ovarian cancer patients and occult cancer in a BRCA1 mutant case. International journal

    Akira Hirasawa, Kenta Masuda, Tomoko Akahane, Arisa Ueki, Megumi Yokota, Tomohiko Tsuruta, Hiroyuki Nomura, Fumio Kataoka, Eiichiro Tominaga, Kouji Banno, Kazuya Makita, Nobuyuki Susumu, Kokichi Sugano, Kenjiro Kosaki, Kaori Kameyama, Daisuke Aoki

    Japanese journal of clinical oncology   44 ( 1 )   49 - 56   2014.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    BACKGROUND: This study aimed to examine family history among Japanese ovarian cancer patients and to investigate the TP53 status of fallopian tube epithelial and ovarian cancer cells in a Japanese BRCA1 mutant case that may be associated with the transformed state in hereditary ovarian cancer. METHODS: One hundred and two primary ovarian cancer patients were retrospectively evaluated in this cross-sectional study. The family history of cancer was determined in probands. In a BRCA1 mutant case, p53 immunostaining and direct sequencing, followed by laser-capture microdissection, were performed for the fallopian tube, considered the origin of ovarian cancer. RESULTS: Nine of 102 (8.8%) families were regarded as having hereditary breast-ovarian cancer syndrome, two families (2.0%) were diagnosed with Lynch syndrome and six patients harbored BRCA1 or BRCA2 mutations. One case underwent risk-reductive salpingo-oophorectomy as a BRCA1 mutant carrier was retrospectively diagnosed as occult cancer. Common TP53 mutations were detected in cancer and fallopian tube epithelial cells in the case. CONCLUSIONS: Here, we integrate family cancer history and histology in ovarian cancer cases as well as TP53 status in a BRCA1 mutant case into a discussion regarding carcinogenesis in a Japanese population. The TP53 status for the BRCA1 mutant case examined here supports the recently proposed theory that ovarian cancer develops because of BRCA1 or BRCA2 inactivation and/or TP53 mutations.

    DOI: 10.1093/jjco/hyt171

    Web of Science

    PubMed

    researchmap

  • 遺伝性乳がん卵巣がん(HBOC)への対応 Reviewed

    増田健太, 阪埜浩司, 植木有紗, 平沢 晃, 青木大輔

    産婦人科の実際   63 ( 7 )   973 - 980   2014

     More details

    Language:Japanese  

    researchmap

  • High Expression of SQSTM1/p62 Protein Is Associated with Poor Prognosis in Epithelial Ovarian Cancer

    Reiko Iwadate, Jun Inoue, Hitoshi Tsuda, Masashi Takano, Kenichi Furuya, Akira Hirasawa, Daisuke Aoki, Johji Inazawa

    ACTA HISTOCHEMICA ET CYTOCHEMICA   47 ( 6 )   295 - 301   2014

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:JAPAN SOC HISTOCHEMISTRY & CYTOCHEMISTRY  

    High expression of SQSTM1/p62 (p62) protein, which functions as a hub for various cellular signaling pathways, has been detected in several human cancers. However, the clinicopathological impact of high p62 expression is largely unknown in epithelial ovarian cancer (EOC). Here, the expression level of p62 in primary EOCs (n=266) was assessed by immunohistochemistry, and its clinical significance was analyzed. Univariate and multivariate analyses were used to determine the impact of p62 expression on overall survival. p62 was expressed in the cytoplasm (Cyto) and/or nucleus (Nuc) in primary E0Cs, and an expression subtype (Cyto(High)/Nuc(Low)), showing high expression in the cytoplasm but low expression in the nucleus, was significantly correlated with serous carcinoma (P&lt;0.001), advanced stage (P=0.005), presence of residual tumor (P&lt;0.001), and low overall survival rate (P=0.013). Furthermore, in serous carcinomas (n=107), the p62 Cyto(High)/Nuc(Low) subtype was significantly correlated with low overall survival rate (P=0.019) as an independent factor (P=0.044). Thus, our findings suggest that high expression of cytoplasmic p62 may be a novel prognostic biomarker in EOC, particularly in serous carcinoma.

    DOI: 10.1267/ahc.14048

    Web of Science

    researchmap

  • Polymorphisms in the UGT1A1 gene predict adverse effects of irinotecan in the treatment of gynecologic cancer in Japanese patients. International journal

    Akira Hirasawa, Takeru Zama, Tomoko Akahane, Hiroyuki Nomura, Fumio Kataoka, Koichiro Saito, Keisuke Okubo, Eiichiro Tominaga, Kazuya Makita, Nobuyuki Susumu, Kenjiro Kosaki, Yusuke Tanigawara, Daisuke Aoki

    Journal of human genetics   58 ( 12 )   794 - 8   2013.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Irinotecan is a key chemotherapeutic drug used to treat many tumors, including cervical and ovarian cancers; however, irinotecan can cause toxicity, particularly in the presence of uridine diphosphate glucuronosyltransferase 1A1 (UGT1A1) gene polymorphisms, which are associated with reduced enzyme activity. Here, we investigated the prevalence of three different variants of UGT1A1 (UGT1A1*6, UGT1A1*27 and UGT1A1*28) and their relationships with irinotecan-induced adverse events in patients with gynecologic cancer, who are treated with lower doses of irinotecan than patients with other types of solid tumors. Fifty-three female patients treated with irinotecan and 362 female patients not treated with irinotecan were screened for UGT1A1*6, UGT1A1*27 and UGT1A1*28. Homozygosity for UGT1A1*6 or heterozygosity for UGT1A1*6/*28 was associated with a high risk of severe absolute neutrophil count decrease or diarrhea (odds ratios: 16.03 and 31.33, respectively). In contrast, serum bilirubin levels were not associated with irinotecan toxicity. Homozygosity for UGT1A1*6/*6 and heterozygosity for UGT1A1*6/*28 were associated with an increased risk of absolute neutrophil count and/or diarrhea in Japanese gynecologic cancer patients, despite the lower doses of irinotecan used in these patients. UGT1A1*6 and UGT1A1*28 are potential predictors of severe absolute neutrophil decrease and diarrhea caused by low-dose irinotecan in gynecologic cancer patients.

    DOI: 10.1038/jhg.2013.105

    Scopus

    PubMed

    researchmap

  • Polymorphisms in the UGT1A1 gene predict adverse effects of irinotecan in the treatment of gynecologic cancer in Japanese patients

    Akira Hirasawa, Takeru Zama, Tomoko Akahane, Hiroyuki Nomura, Fumio Kataoka, Koichiro Saito, Keisuke Okubo, Eiichiro Tominaga, Kazuya Makita, Nobuyuki Susumu, Kenjiro Kosaki, Yusuke Tanigawara, Daisuke Aoki

    Journal of Human Genetics   58 ( 12 )   794 - 798   2013.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Irinotecan is a key chemotherapeutic drug used to treat many tumors, including cervical and ovarian cancers
    however, irinotecan can cause toxicity, particularly in the presence of uridine diphosphate glucuronosyltransferase 1A1 (UGT1A1) gene polymorphisms, which are associated with reduced enzyme activity. Here, we investigated the prevalence of three different variants of UGT1A1 (UGT1A1*6, UGT1A1*27 and UGT1A1*28) and their relationships with irinotecan-induced adverse events in patients with gynecologic cancer, who are treated with lower doses of irinotecan than patients with other types of solid tumors. Fifty-three female patients treated with irinotecan and 362 female patients not treated with irinotecan were screened for UGT1A1*6, UGT1A1*27 and UGT1A1*28. Homozygosity for UGT1A1*6 or heterozygosity for UGT1A1*6/*28 was associated with a high risk of severe absolute neutrophil count decrease or diarrhea (odds ratios: 16.03 and 31.33, respectively). In contrast, serum bilirubin levels were not associated with irinotecan toxicity. Homozygosity for UGT1A1*6/*6 and heterozygosity for UGT1A1*6/*28 were associated with an increased risk of absolute neutrophil count and/or diarrhea in Japanese gynecologic cancer patients, despite the lower doses of irinotecan used in these patients. UGT1A1*6 and UGT1A1*28 are potential predictors of severe absolute neutrophil decrease and diarrhea caused by low-dose irinotecan in gynecologic cancer patients. © 2013 The Japan Society of Human Genetics All rights reserved 1434-5161/13.

    DOI: 10.1038/jhg.2013.105

    Scopus

    PubMed

    researchmap

  • Polymorphisms in the UGT1A1 gene predict adverse effects of irinotecan in the treatment of gynecologic cancer in Japanese patients Reviewed

    Akira Hirasawa, Takeru Zama, Tomoko Akahane, Hiroyuki Nomura, Fumio Kataoka, Koichiro Saito, Keisuke Okubo, Eiichiro Tominaga, Kazuya Makita, Nobuyuki Susumu, Kenjiro Kosaki, Yusuke Tanigawara, Daisuke Aoki

    Journal of Human Genetics   58 ( 12 )   794 - 798   2013.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Irinotecan is a key chemotherapeutic drug used to treat many tumors, including cervical and ovarian cancers
    however, irinotecan can cause toxicity, particularly in the presence of uridine diphosphate glucuronosyltransferase 1A1 (UGT1A1) gene polymorphisms, which are associated with reduced enzyme activity. Here, we investigated the prevalence of three different variants of UGT1A1 (UGT1A1*6, UGT1A1*27 and UGT1A1*28) and their relationships with irinotecan-induced adverse events in patients with gynecologic cancer, who are treated with lower doses of irinotecan than patients with other types of solid tumors. Fifty-three female patients treated with irinotecan and 362 female patients not treated with irinotecan were screened for UGT1A1*6, UGT1A1*27 and UGT1A1*28. Homozygosity for UGT1A1*6 or heterozygosity for UGT1A1*6/*28 was associated with a high risk of severe absolute neutrophil count decrease or diarrhea (odds ratios: 16.03 and 31.33, respectively). In contrast, serum bilirubin levels were not associated with irinotecan toxicity. Homozygosity for UGT1A1*6/*6 and heterozygosity for UGT1A1*6/*28 were associated with an increased risk of absolute neutrophil count and/or diarrhea in Japanese gynecologic cancer patients, despite the lower doses of irinotecan used in these patients. UGT1A1*6 and UGT1A1*28 are potential predictors of severe absolute neutrophil decrease and diarrhea caused by low-dose irinotecan in gynecologic cancer patients. © 2013 The Japan Society of Human Genetics All rights reserved 1434-5161/13.

    DOI: 10.1038/jhg.2013.105

    Scopus

    PubMed

    researchmap

  • Hereditary gynecological tumors associated with Peutz-Jeghers syndrome Reviewed

    Kouji Banno, Iori Kisu, Megumi Yanokura, Kenta Masuda, Arisa Ueki, Yusuke Kobayashi, Akira Hirasawa, Daisuke Aoki

    ONCOLOGY LETTERS   6 ( 5 )   1184 - 1188   2013.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Peutz-Jeghers syndrome (PJS) is an autosomal dominant disease that is characterized by gastrointestinal hamartomatous polyposis and mucocutaneous melanin spots. The tumor suppressor gene, STK11/LKB1, which is located on chromosome 19p13.3, has been reported to be responsible for this condition. PJS is complicated by benign and malignant tumors of various organs and complications from rare diseases, including sex cord tumor with annular tubules (SCTAT) and minimal deviation adenocarcinoma (MDA), which have also recently attracted attention in the field of gynecology. Among the total MDA cases, 10% are complications of PJS, and mutations in the STK11 gene are closely associated with the development and prognosis of MDA. Furthermore, a new type of uterine cervical tumor, lobular endocervical glandular hyperplasia (LEGH), has been identified and has been predicted to be a precancerous lesion of MDA. The first case of LEGH induced by a germline STK11 mutation has also been described. A high risk of endometrial cancer in PJS has also been reported. These developments suggest that PJS is an important syndrome of hereditary gynecological tumors that requires further study.

    DOI: 10.3892/ol.2013.1527

    Web of Science

    researchmap

  • Hereditary gynecological tumors associated with Peutz-Jeghers syndrome (Review). International journal

    Kouji Banno, Iori Kisu, Megumi Yanokura, Kenta Masuda, Arisa Ueki, Yusuke Kobayashi, Akira Hirasawa, Daisuke Aoki

    Oncology letters   6 ( 5 )   1184 - 1188   2013.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Peutz-Jeghers syndrome (PJS) is an autosomal dominant disease that is characterized by gastrointestinal hamartomatous polyposis and mucocutaneous melanin spots. The tumor suppressor gene, STK11/LKB1, which is located on chromosome 19p13.3, has been reported to be responsible for this condition. PJS is complicated by benign and malignant tumors of various organs and complications from rare diseases, including sex cord tumor with annular tubules (SCTAT) and minimal deviation adenocarcinoma (MDA), which have also recently attracted attention in the field of gynecology. Among the total MDA cases, 10% are complications of PJS, and mutations in the STK11 gene are closely associated with the development and prognosis of MDA. Furthermore, a new type of uterine cervical tumor, lobular endocervical glandular hyperplasia (LEGH), has been identified and has been predicted to be a precancerous lesion of MDA. The first case of LEGH induced by a germline STK11 mutation has also been described. A high risk of endometrial cancer in PJS has also been reported. These developments suggest that PJS is an important syndrome of hereditary gynecological tumors that requires further study.

    DOI: 10.3892/ol.2013.1527

    Web of Science

    PubMed

    researchmap

  • Hereditary gynecological tumors associated with Peutz-Jeghers syndrome

    Kouji Banno, Iori Kisu, Megumi Yanokura, Kenta Masuda, Arisa Ueki, Yusuke Kobayashi, Akira Hirasawa, Daisuke Aoki

    ONCOLOGY LETTERS   6 ( 5 )   1184 - 1188   2013.11

     More details

    Language:English   Publisher:SPANDIDOS PUBL LTD  

    Peutz-Jeghers syndrome (PJS) is an autosomal dominant disease that is characterized by gastrointestinal hamartomatous polyposis and mucocutaneous melanin spots. The tumor suppressor gene, STK11/LKB1, which is located on chromosome 19p13.3, has been reported to be responsible for this condition. PJS is complicated by benign and malignant tumors of various organs and complications from rare diseases, including sex cord tumor with annular tubules (SCTAT) and minimal deviation adenocarcinoma (MDA), which have also recently attracted attention in the field of gynecology. Among the total MDA cases, 10% are complications of PJS, and mutations in the STK11 gene are closely associated with the development and prognosis of MDA. Furthermore, a new type of uterine cervical tumor, lobular endocervical glandular hyperplasia (LEGH), has been identified and has been predicted to be a precancerous lesion of MDA. The first case of LEGH induced by a germline STK11 mutation has also been described. A high risk of endometrial cancer in PJS has also been reported. These developments suggest that PJS is an important syndrome of hereditary gynecological tumors that requires further study.

    DOI: 10.3892/ol.2013.1527

    Web of Science

    researchmap

  • Hypertriglyceridemia is frequent in endometrial cancer survivors. Reviewed International journal

    Akira Hirasawa, Kazuya Makita, Tomoko Akahane, Megumi Yokota, Wataru Yamagami, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    Japanese journal of clinical oncology   43 ( 11 )   1087 - 92   2013.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    OBJECTIVE: Previous studies have reported an association between endometrial cancer and the risk of metabolic syndrome; however, the pattern of endometrial cancer-associated dyslipidemia is not well understood. The standard therapy for endometrial cancer is total abdominal hysterectomy and bilateral salpingo-oophorectomy. Premenopausal bilateral salpingo-oophorectomy may cause adverse events, including dyslipidemia. Gynecologists have to care dyslipidemia in endometrial cancer survivors at cancer follow-up clinic. METHODS: This study included 693 patients who had undergone bilateral salpingo-oophorectomy, and included 412 women with incident endometrial cancer and 281 controls. We divided the patients into two categories according to whether they had a premenopausal or postmenopausal bilateral oophorectomy. Serum lipid levels were measured and statistically analyzed. RESULTS: Hypertriglyceridemia was statistically more frequent in patients who had undergone bilateral salpingo-oophorectomy both before and after menopause than in the corresponding non-endometrial cancer controls. High levels of low-density lipoprotein cholesterol and a high low-density lipoprotein cholesterol/high-density lipoprotein cholesterol ratio were statistically more frequent in patients who had undergone bilateral salpingo-oophorectomy before menopause than in non-endometrial cancer controls. CONCLUSIONS: Our report highlights the importance of the relationship between endometrial cancer and lipid metabolism, which may aid in preventing cerebrovascular or cardiovascular diseases due to dyslipidemia and improving the quality of life in endometrial cancer survivors.

    DOI: 10.1093/jjco/hyt125

    Web of Science

    PubMed

    researchmap

  • Hypertriglyceridemia is Frequent in Endometrial Cancer Survivors

    Akira Hirasawa, Kazuya Makita, Tomoko Akahane, Megumi Yokota, Wataru Yamagami, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    JAPANESE JOURNAL OF CLINICAL ONCOLOGY   43 ( 11 )   1087 - 1092   2013.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    Objective: Previous studies have reported an association between endometrial cancer and the risk of metabolic syndrome; however, the pattern of endometrial cancer-associated dyslipidemia is not well understood. The standard therapy for endometrial cancer is total abdominal hysterectomy and bilateral salpingo-oophorectomy. Premenopausal bilateral salpingo-oophorectomy may cause adverse events, including dyslipidemia. Gynecologists have to care dyslipidemia in endometrial cancer survivors at cancer follow-up clinic.
    Methods: This study included 693 patients who had undergone bilateral salpingo-oophorectomy, and included 412 women with incident endometrial cancer and 281 controls. We divided the patients into two categories according to whether they had a premenopausal or postmenopausal bilateral oophorectomy. Serum lipid levels were measured and statistically analyzed.
    Results: Hypertriglyceridemia was statistically more frequent in patients who had undergone bilateral salpingo-oophorectomy both before and after menopause than in the corresponding non-endometrial cancer controls. High levels of low-density lipoprotein cholesterol and a high low-density lipoprotein cholesterol/high-density lipoprotein cholesterol ratio were statistically more frequent in patients who had undergone bilateral salpingo-oophorectomy before menopause than in non-endometrial cancer controls.
    Conclusions: Our report highlights the importance of the relationship between endometrial cancer and lipid metabolism, which may aid in preventing cerebrovascular or cardiovascular diseases due to dyslipidemia and improving the quality of life in endometrial cancer survivors.

    DOI: 10.1093/jjco/hyt125

    Web of Science

    researchmap

  • Hypertriglyceridemia is Frequent in Endometrial Cancer Survivors

    Akira Hirasawa, Kazuya Makita, Tomoko Akahane, Megumi Yokota, Wataru Yamagami, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    JAPANESE JOURNAL OF CLINICAL ONCOLOGY   43 ( 11 )   1087 - 1092   2013.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    Objective: Previous studies have reported an association between endometrial cancer and the risk of metabolic syndrome; however, the pattern of endometrial cancer-associated dyslipidemia is not well understood. The standard therapy for endometrial cancer is total abdominal hysterectomy and bilateral salpingo-oophorectomy. Premenopausal bilateral salpingo-oophorectomy may cause adverse events, including dyslipidemia. Gynecologists have to care dyslipidemia in endometrial cancer survivors at cancer follow-up clinic.
    Methods: This study included 693 patients who had undergone bilateral salpingo-oophorectomy, and included 412 women with incident endometrial cancer and 281 controls. We divided the patients into two categories according to whether they had a premenopausal or postmenopausal bilateral oophorectomy. Serum lipid levels were measured and statistically analyzed.
    Results: Hypertriglyceridemia was statistically more frequent in patients who had undergone bilateral salpingo-oophorectomy both before and after menopause than in the corresponding non-endometrial cancer controls. High levels of low-density lipoprotein cholesterol and a high low-density lipoprotein cholesterol/high-density lipoprotein cholesterol ratio were statistically more frequent in patients who had undergone bilateral salpingo-oophorectomy before menopause than in non-endometrial cancer controls.
    Conclusions: Our report highlights the importance of the relationship between endometrial cancer and lipid metabolism, which may aid in preventing cerebrovascular or cardiovascular diseases due to dyslipidemia and improving the quality of life in endometrial cancer survivors.

    DOI: 10.1093/jjco/hyt125

    Web of Science

    researchmap

  • Distinguishing between lymphangioleiomyomatosis and carcinomatous peritonitis in a patient with ovarian cancer. International journal

    Akira Hirasawa, Takashi Sato, Mari Ueno, Tomoko Akahane, Nobuyuki Susumu, Tomoko Betsuyaku, Daisuke Aoki

    Journal of clinical oncology : official journal of the American Society of Clinical Oncology   31 ( 28 )   e427-9 - E429   2013.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER SOC CLINICAL ONCOLOGY  

    DOI: 10.1200/JCO.2012.45.3019

    Web of Science

    PubMed

    researchmap

  • Distinguishing Between Lymphangioleiomyomatosis and Carcinomatous Peritonitis in a Patient With Ovarian Cancer

    Akira Hirasawa, Takashi Sato, Mari Ueno, Tomoko Akahane, Nobuyuki Susumu, Tomoko Betsuyaku, Daisuke Aoki

    JOURNAL OF CLINICAL ONCOLOGY   31 ( 28 )   E427 - E429   2013.10

     More details

    Language:English   Publisher:AMER SOC CLINICAL ONCOLOGY  

    DOI: 10.1200/JCO.2012.45.3019

    Web of Science

    researchmap

  • Distinguishing Between Lymphangioleiomyomatosis and Carcinomatous Peritonitis in a Patient With Ovarian Cancer Reviewed

    Akira Hirasawa, Takashi Sato, Mari Ueno, Tomoko Akahane, Nobuyuki Susumu, Tomoko Betsuyaku, Daisuke Aoki

    JOURNAL OF CLINICAL ONCOLOGY   31 ( 28 )   E427 - E429   2013.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER SOC CLINICAL ONCOLOGY  

    DOI: 10.1200/JCO.2012.45.3019

    Web of Science

    researchmap

  • MicroRNA-196a Is a Putative Diagnostic Biomarker and Therapeutic Target for Laryngeal Cancer

    Koichiro Saito, Koji Inagaki, Takahiro Kamimoto, Yoko Ito, Toshiaki Sugita, Satoko Nakajo, Akira Hirasawa, Arifumi Iwamaru, Takashi Ishikura, Hideki Hanaoka, Keisuke Okubo, Tokio Onozaki, Takeru Zama

    PLOS ONE   8 ( 8 )   2013.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PUBLIC LIBRARY SCIENCE  

    Background: MicroRNA (miRNA) is an emerging subclass of small non-coding RNAs that regulates gene expression and has a pivotal role for many physiological processes including cancer development. Recent reports revealed the role of miRNAs as ideal biomarkers and therapeutic targets due to their tissue-or disease-specific nature. Head and neck cancer (HNC) is a major cause of cancer-related mortality and morbidity, and laryngeal cancer has the highest incidence in it. However, the molecular mechanisms involved in laryngeal cancer development remain to be known and highly sensitive biomarkers and novel promising therapy is necessary.
    Methodology/Principal Findings: To explore laryngeal cancer-specific miRNAs, RNA from 5 laryngeal surgical specimens including cancer and non-cancer tissues were hybridized to microarray carrying 723 human miRNAs. The resultant differentially expressed miRNAs were further tested by using quantitative real time PCR (qRT-PCR) on 43 laryngeal tissue samples including cancers, noncancerous counterparts, benign diseases and precancerous dysplasias. Significant expressional differences between matched pairs were reproduced in miR-133b, miR-455-5p, and miR-196a, among which miR-196a being the most promising cancer biomarker as validated by qRT-PCR analyses on additional 84 tissue samples. Deep sequencing analysis revealed both quantitative and qualitative deviation of miR-196a isomiR expression in laryngeal cancer. In situ hybridization confirmed laryngeal cancer-specific expression of miR-196a in both cancer and cancer stroma cells. Finally, inhibition of miR-196a counteracted cancer cell proliferation in both laryngeal cancer-derived cells and mouse xenograft model.
    Conclusions/Significance: Our study provided the possibilities that miR-196a might be very useful in diagnosing and treating laryngeal cancer.

    DOI: 10.1371/journal.pone.0071480

    Web of Science

    researchmap

  • MicroRNA-196a Is a Putative Diagnostic Biomarker and Therapeutic Target for Laryngeal Cancer

    Koichiro Saito, Koji Inagaki, Takahiro Kamimoto, Yoko Ito, Toshiaki Sugita, Satoko Nakajo, Akira Hirasawa, Arifumi Iwamaru, Takashi Ishikura, Hideki Hanaoka, Keisuke Okubo, Tokio Onozaki, Takeru Zama

    PLOS ONE   8 ( 8 )   2013.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PUBLIC LIBRARY SCIENCE  

    Background: MicroRNA (miRNA) is an emerging subclass of small non-coding RNAs that regulates gene expression and has a pivotal role for many physiological processes including cancer development. Recent reports revealed the role of miRNAs as ideal biomarkers and therapeutic targets due to their tissue-or disease-specific nature. Head and neck cancer (HNC) is a major cause of cancer-related mortality and morbidity, and laryngeal cancer has the highest incidence in it. However, the molecular mechanisms involved in laryngeal cancer development remain to be known and highly sensitive biomarkers and novel promising therapy is necessary.
    Methodology/Principal Findings: To explore laryngeal cancer-specific miRNAs, RNA from 5 laryngeal surgical specimens including cancer and non-cancer tissues were hybridized to microarray carrying 723 human miRNAs. The resultant differentially expressed miRNAs were further tested by using quantitative real time PCR (qRT-PCR) on 43 laryngeal tissue samples including cancers, noncancerous counterparts, benign diseases and precancerous dysplasias. Significant expressional differences between matched pairs were reproduced in miR-133b, miR-455-5p, and miR-196a, among which miR-196a being the most promising cancer biomarker as validated by qRT-PCR analyses on additional 84 tissue samples. Deep sequencing analysis revealed both quantitative and qualitative deviation of miR-196a isomiR expression in laryngeal cancer. In situ hybridization confirmed laryngeal cancer-specific expression of miR-196a in both cancer and cancer stroma cells. Finally, inhibition of miR-196a counteracted cancer cell proliferation in both laryngeal cancer-derived cells and mouse xenograft model.
    Conclusions/Significance: Our study provided the possibilities that miR-196a might be very useful in diagnosing and treating laryngeal cancer.

    DOI: 10.1371/journal.pone.0071480

    Web of Science

    researchmap

  • beta-Catenin signaling regulates Foxa2 expression during endometrial hyperplasia formation

    M. Villacorte, K. Suzuki, A. Hirasawa, Y. Ohkawa, M. Suyama, T. Maruyama, D. Aoki, Y. Ogino, S. Miyagawa, T. Terabayashi, Y. Tomooka, N. Nakagata, G. Yamada

    ONCOGENE   32 ( 29 )   3477 - 3482   2013.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    The Wnt/beta-catenin signaling is essential for various organogenesis and is often implicated during tumorigenesis. Dysregulated beta-catenin signaling is associated with the formation of endometrial adenocarcinomas (EACs), which is considered as the common form of endometrial cancer in women. In the current study, we investigate the downstream target of Wnt/beta-catenin signaling in the uterine epithelia and the mechanism leading to the formation of endometrial hyperplasia. We report that conditional ablation and activation of beta-catenin in the uterine epithelia lead to aberrant epithelial structures and endometrial hyperplasia formation, respectively. We demonstrate that beta-catenin regulates Foxa2 with its candidate upstream region for the uterine epithelia. Furthermore, knockdown of Foxa2 leads to defects in cell cycle regulation, suggesting a possible function of Foxa2 in the control of cell proliferation. We also observe that beta-catenin and Foxa2 expression levels are augmented in the human specimens of complex atypical endometrial hyperplasia, which is considered to have a greater risk of progression to EACs. Thus, our study indicates that beta-catenin regulates Foxa2 expression, and this interaction is possibly essential to control cell cycle progression during endometrial hyperplasia formation. Altogether, the augmented expression levels of beta-catenin and Foxa2 are essential features during the formation of endometrial hyperplasia.

    DOI: 10.1038/onc.2012.376

    Web of Science

    researchmap

  • beta-Catenin signaling regulates Foxa2 expression during endometrial hyperplasia formation Reviewed

    M. Villacorte, K. Suzuki, A. Hirasawa, Y. Ohkawa, M. Suyama, T. Maruyama, D. Aoki, Y. Ogino, S. Miyagawa, T. Terabayashi, Y. Tomooka, N. Nakagata, G. Yamada

    ONCOGENE   32 ( 29 )   3477 - 3482   2013.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    The Wnt/beta-catenin signaling is essential for various organogenesis and is often implicated during tumorigenesis. Dysregulated beta-catenin signaling is associated with the formation of endometrial adenocarcinomas (EACs), which is considered as the common form of endometrial cancer in women. In the current study, we investigate the downstream target of Wnt/beta-catenin signaling in the uterine epithelia and the mechanism leading to the formation of endometrial hyperplasia. We report that conditional ablation and activation of beta-catenin in the uterine epithelia lead to aberrant epithelial structures and endometrial hyperplasia formation, respectively. We demonstrate that beta-catenin regulates Foxa2 with its candidate upstream region for the uterine epithelia. Furthermore, knockdown of Foxa2 leads to defects in cell cycle regulation, suggesting a possible function of Foxa2 in the control of cell proliferation. We also observe that beta-catenin and Foxa2 expression levels are augmented in the human specimens of complex atypical endometrial hyperplasia, which is considered to have a greater risk of progression to EACs. Thus, our study indicates that beta-catenin regulates Foxa2 expression, and this interaction is possibly essential to control cell cycle progression during endometrial hyperplasia formation. Altogether, the augmented expression levels of beta-catenin and Foxa2 are essential features during the formation of endometrial hyperplasia.

    DOI: 10.1038/onc.2012.376

    Web of Science

    researchmap

  • beta-Catenin signaling regulates Foxa2 expression during endometrial hyperplasia formation

    M. Villacorte, K. Suzuki, A. Hirasawa, Y. Ohkawa, M. Suyama, T. Maruyama, D. Aoki, Y. Ogino, S. Miyagawa, T. Terabayashi, Y. Tomooka, N. Nakagata, G. Yamada

    ONCOGENE   32 ( 29 )   3477 - 3482   2013.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    The Wnt/beta-catenin signaling is essential for various organogenesis and is often implicated during tumorigenesis. Dysregulated beta-catenin signaling is associated with the formation of endometrial adenocarcinomas (EACs), which is considered as the common form of endometrial cancer in women. In the current study, we investigate the downstream target of Wnt/beta-catenin signaling in the uterine epithelia and the mechanism leading to the formation of endometrial hyperplasia. We report that conditional ablation and activation of beta-catenin in the uterine epithelia lead to aberrant epithelial structures and endometrial hyperplasia formation, respectively. We demonstrate that beta-catenin regulates Foxa2 with its candidate upstream region for the uterine epithelia. Furthermore, knockdown of Foxa2 leads to defects in cell cycle regulation, suggesting a possible function of Foxa2 in the control of cell proliferation. We also observe that beta-catenin and Foxa2 expression levels are augmented in the human specimens of complex atypical endometrial hyperplasia, which is considered to have a greater risk of progression to EACs. Thus, our study indicates that beta-catenin regulates Foxa2 expression, and this interaction is possibly essential to control cell cycle progression during endometrial hyperplasia formation. Altogether, the augmented expression levels of beta-catenin and Foxa2 are essential features during the formation of endometrial hyperplasia.

    DOI: 10.1038/onc.2012.376

    Web of Science

    researchmap

  • Experience of risk-reducing salpingo-oophorectomy for a BRCA1 mutation carrier and establishment of a system performing a preventive surgery for hereditary breast and ovarian cancer syndrome in Japan: our challenges for the future. International journal

    Akira Hirasawa, Kenta Masuda, Tomoko Akahane, Tomohiko Tsuruta, Kouji Banno, Kazuya Makita, Nobuyuki Susumu, Hiromitsu Jinno, Yuko Kitagawa, Kokichi Sugano, Kenjiro Kosaki, Daisuke Aoki

    Japanese journal of clinical oncology   43 ( 5 )   515 - 9   2013.5

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    BACKGROUND: Risk-reducing salpingo-oophorectomy is currently regarded as the most certain primary method for preventing ovarian cancer among BRCA1/2 mutation carriers with hereditary breast and ovarian cancer syndrome. However, risk-reducing salpingo-oophorectomy has rarely been performed in Japan. METHODS: We developed the first system in Japan for performing risk-reducing salpingo-oophorectomy for BRCA1/2 mutation carriers at our university hospital in 2008. RESULTS: The indication for risk-reducing salpingo-oophorectomy for patients with hereditary breast/ovarian cancer syndrome is currently limited in Japan. This situation may be because of the limited number of genetic counseling units, the limited number of facilities that can perform BRCA1/2 genetic testing and the fact that prophylactic surgery is not covered by health insurance in Japan. CONCLUSIONS: Recent treatment guidelines for breast cancer in Japan recommended risk-reducing salpingo-oophorectomy for BRCA1/2 mutation carriers. Risk-reducing salpingo-oophorectomy should be performed in the framework of the standard therapeutic modality for BRCA1/2 mutation carriers in the near future.

    DOI: 10.1093/jjco/hyt036

    Web of Science

    PubMed

    researchmap

  • Experience of Risk-reducing Salpingo-oophorectomy for a BRCA1 Mutation Carrier and Establishment of a System Performing a Preventive Surgery for Hereditary Breast and Ovarian Cancer Syndrome in Japan: Our Challenges for the Future

    Akira Hirasawa, Kenta Masuda, Tomoko Akahane, Tomohiko Tsuruta, Kouji Banno, Kazuya Makita, Nobuyuki Susumu, Hiromitsu Jinno, Yuko Kitagawa, Kokichi Sugano, Kenjiro Kosaki, Daisuke Aoki

    JAPANESE JOURNAL OF CLINICAL ONCOLOGY   43 ( 5 )   515 - 519   2013.5

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    Risk-reducing salpingo-oophorectomy is currently regarded as the most certain primary method for preventing ovarian cancer among BRCA1/2 mutation carriers with hereditary breast and ovarian cancer syndrome. However, risk-reducing salpingo-oophorectomy has rarely been performed in Japan.
    We developed the first system in Japan for performing risk-reducing salpingo-oophorectomy for BRCA1/2 mutation carriers at our university hospital in 2008.
    The indication for risk-reducing salpingo-oophorectomy for patients with hereditary breast/ovarian cancer syndrome is currently limited in Japan. This situation may be because of the limited number of genetic counseling units, the limited number of facilities that can perform BRCA1/2 genetic testing and the fact that prophylactic surgery is not covered by health insurance in Japan.
    Recent treatment guidelines for breast cancer in Japan recommended risk-reducing salpingo-oophorectomy for BRCA1/2 mutation carriers. Risk-reducing salpingo-oophorectomy should be performed in the framework of the standard therapeutic modality for BRCA1/2 mutation carriers in the near future.

    DOI: 10.1093/jjco/hyt036

    Web of Science

    researchmap

  • 高用量黄体ホルモン療法後に妊娠に至った若年性子宮体癌および複雑型子宮内膜異型増殖症43例の妊娠予後と分娩後のサーベイランス Reviewed

    山上 亘, 進 伸幸, 市川 義一, 桑波田 美智子, 野村 弘行, 平沢 晃, 峰岸 一宏, 冨永 英一郎, 宮越 敬, 阪埜 浩司, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   65 ( 2 )   574 - 574   2013.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • The origin of stroma surrounding epithelial ovarian cancer cells. International journal

    Tomoko Akahane, Akira Hirasawa, Hiroshi Tsuda, Fumio Kataoka, Sadako Nishimura, Hideo Tanaka, Eiichiro Tominaga, Hiroyuki Nomura, Tatsuyuki Chiyoda, Yoko Iguchi, Wataru Yamagami, Nobuyuki Susumu, Daisuke Aoki

    International journal of gynecological pathology : official journal of the International Society of Gynecological Pathologists   32 ( 1 )   26 - 30   2013.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Cancer stroma is thought to play an important role in tumor behavior, including invasion or metastasis and response to therapy. Cancer stroma is generally thought either to be non-neoplastic cells, including tissue-marrow or bone-marrow-derived fibroblasts, or to originate in epithelial mesenchymal transition of cancer cells. In this study, we evaluated the status of the p53 gene in both the cancer cells and the cancer stroma in epithelial ovarian cancer (EOC) to elucidate the origin of the stroma. Samples from 16 EOC patients were included in this study. Tumor cells and adjacent nontumor stromal cells were microdissected and DNA was extracted separately. We analyzed p53 sequences (exons 5-8) of both cancer and stromal tissues in all cases. Furthermore, we examined p53 protein expression in all cases. Mutations in p53 were detected in 9 of the 16 EOCs: in 8 of these cases, the mutations were detected only in cancer cells. In 1 case, the same mutation (R248Q) was detected in both cancer and stromal tissues, and p53 protein expression was detected in both the cancer cells and the cancer stroma. Most cancer stroma in EOC is thought to originate from non-neoplastic cells, but some parts of the cancer stroma might originate from cancer cells.

    DOI: 10.1097/PGP.0b013e3182518533

    Web of Science

    PubMed

    researchmap

  • 遺伝性乳癌・卵巣癌に対する婦人科の取り組み Invited

    平沢 晃, 青木大輔

    化療ニュース   22 ( 2 )   13 - 19   2013

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • ホルモンによるがんの化学予防 Invited Reviewed

    平沢 晃, 鶴田智彦, 青木大輔

    産科と婦人科   80 ( Sup )   164 - 168   2013

     More details

    Language:Japanese  

    researchmap

  • 遺伝性乳癌・卵巣癌女性への遺伝カウンセリング Invited Reviewed

    平沢 晃, 青木大輔

    産科と婦人科   80 ( 11 )   1465 - 1472   2013

  • 当科健康維持外来患者からみためまいの現状 Invited

    牧田和也, 橫田めぐみ, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔, 吉村泰典

    日本女性医学学会雑誌   21 ( 1 )   54 - 59   2013

     More details

    Language:Japanese  

    researchmap

  • 子宮峡部癌の臨床病理学的特徴とLynch症候群との関連 Invited Reviewed

    増田健太, 阪埜浩司, 矢野倉恵, 小林佑介, 辻 浩介, 木須伊織, 植木有紗, 野村弘行, 平沢 晃, 進 伸幸, 青木大輔

    家族性腫瘍   13 ( 1 )   1 - 5   2013

  • 子宮体がんとエストロゲン Invited Reviewed

    進 伸幸, 山上 亘, 二宮委美, 桑波田美智子, 片岡史夫, 平沢 晃, 阪埜浩司, 青木大輔

    産婦人科の実際   62 ( 9 )   1181 - 1187   2013

     More details

    Language:Japanese  

    researchmap

  • MicroRNA-196a is a putative diagnostic biomarker and therapeutic target for laryngeal cancer. Reviewed International journal

    Koichiro Saito, Koji Inagaki, Takahiro Kamimoto, Yoko Ito, Toshiaki Sugita, Satoko Nakajo, Akira Hirasawa, Arifumi Iwamaru, Takashi Ishikura, Hideki Hanaoka, Keisuke Okubo, Tokio Onozaki, Takeru Zama

    PloS one   8 ( 8 )   e71480   2013

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PUBLIC LIBRARY SCIENCE  

    BACKGROUND: MicroRNA (miRNA) is an emerging subclass of small non-coding RNAs that regulates gene expression and has a pivotal role for many physiological processes including cancer development. Recent reports revealed the role of miRNAs as ideal biomarkers and therapeutic targets due to their tissue- or disease-specific nature. Head and neck cancer (HNC) is a major cause of cancer-related mortality and morbidity, and laryngeal cancer has the highest incidence in it. However, the molecular mechanisms involved in laryngeal cancer development remain to be known and highly sensitive biomarkers and novel promising therapy is necessary. METHODOLOGY/PRINCIPAL FINDINGS: To explore laryngeal cancer-specific miRNAs, RNA from 5 laryngeal surgical specimens including cancer and non-cancer tissues were hybridized to microarray carrying 723 human miRNAs. The resultant differentially expressed miRNAs were further tested by using quantitative real time PCR (qRT-PCR) on 43 laryngeal tissue samples including cancers, noncancerous counterparts, benign diseases and precancerous dysplasias. Significant expressional differences between matched pairs were reproduced in miR-133b, miR-455-5p, and miR-196a, among which miR-196a being the most promising cancer biomarker as validated by qRT-PCR analyses on additional 84 tissue samples. Deep sequencing analysis revealed both quantitative and qualitative deviation of miR-196a isomiR expression in laryngeal cancer. In situ hybridization confirmed laryngeal cancer-specific expression of miR-196a in both cancer and cancer stroma cells. Finally, inhibition of miR-196a counteracted cancer cell proliferation in both laryngeal cancer-derived cells and mouse xenograft model. CONCLUSIONS/SIGNIFICANCE: Our study provided the possibilities that miR-196a might be very useful in diagnosing and treating laryngeal cancer.

    DOI: 10.1371/journal.pone.0071480

    Web of Science

    PubMed

    researchmap

  • Establishment of a system for performing risk-reducing salpingo-oophorectomy for BRCA1 or BRCA2 mutation carriers in Japan: Our challenges for the future. Reviewed

    Hirasawa A, Masuda K, Akahane T, Tsuruta T, Banno K, Makita K, Susumu N, Sugano K, Kosaki K, Aoki D

    Jpn J Clin Oncol   43 ( 5 )   515-519   2013

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • Lobular endocervical glandular hyperplasia and peritoneal pigmentation associated with Peutz-Jeghers syndrome due to a germline mutation of STK11

    A. Hirasawa, T. Akahane, T. Tsuruta, Y. Kobayashi, K. Masuda, K. Banno, T. Fujii, N. Susumu, T. Itsubo, K. Kameyama, K. Sugano, D. Aoki

    ANNALS OF ONCOLOGY   23 ( 11 )   2990 - 2992   2012.11

     More details

    Language:English   Publisher:OXFORD UNIV PRESS  

    DOI: 10.1093/annonc/mds492

    Web of Science

    researchmap

  • Lobular endocervical glandular hyperplasia and peritoneal pigmentation associated with Peutz-Jeghers syndrome due to a germline mutation of STK11

    A. Hirasawa, T. Akahane, T. Tsuruta, Y. Kobayashi, K. Masuda, K. Banno, T. Fujii, N. Susumu, T. Itsubo, K. Kameyama, K. Sugano, D. Aoki

    ANNALS OF ONCOLOGY   23 ( 11 )   2990 - 2992   2012.11

     More details

    Language:English   Publisher:OXFORD UNIV PRESS  

    DOI: 10.1093/annonc/mds492

    Web of Science

    researchmap

  • Relationship of lower uterine segment cancer with Lynch syndrome: a novel case with an hMLH1 germline mutation. Reviewed International journal

    Kenta Masuda, Kouji Banno, Akira Hirasawa, Megumi Yanokura, Kosuke Tsuji, Yusuke Kobayashi, Iori Kisu, Arisa Ueki, Hiroyuki Nomura, Eiichiro Tominaga, Nobuyuki Susumu, Daisuke Aoki

    Oncology reports   28 ( 5 )   1537 - 43   2012.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Lynch syndrome is a genetic disease that often develops in patients with endometrial cancer and is caused by abnormal DNA mismatch repair (MMR) genes. In the United States, it was recently reported that the prevalence of Lynch syndrome with an hMSH2 mutation in patients with endometrial cancer in the lower uterine segment (LUS) is much greater than that in patients with endometrial cancer, although no such reports have been published in Asia. In this study, we examined the correlation between endometrial cancer in LUS and abnormalities in MMR genes. We examined 625 patients, who were diagnosed with endometrial cancer and underwent a hysterectomy. Nine patients (1.4%) had cancer based on pathological confirmation of a tumor in the lower part of the uterus and no cancer in the upper part. These cases were compared with 27 cases of sporadic endometrial (non-LUS) cancer. The age and BMI of the patients with LUS cancer were significantly lower than those of the patients with non-LUS cancer. No differences were observed in the pathological characteristics. The microsatellite instability (MSI)-positive rates were similar. Immunohistochemistry showed a decreased expression of hMLH1 and hMSH6 in patients with LUS cancer. In contrast with earlier reports from the United States, hMSH2 was expressed in all the cases. Of the 2 patients with LUS cancer who exhibited high MSI, 1 patient showed abnormal methylation of hMLH1, while the other patient was diagnosed with Lynch syndrome with a mutation in the hMLH1 gene. This is the second report on the relationship of LUS cancer and Lynch syndrome, and the first to describe an Asian patient with LUS cancer with Lynch syndrome induced by an hMLH1 mutation.

    DOI: 10.3892/or.2012.2008

    Web of Science

    PubMed

    researchmap

  • Relationship of lower uterine segment cancer with Lynch syndrome: A novel case with an hMLH1 germline mutation

    Kenta Masuda, Kouji Banno, Akira Hirasawa, Megumi Yanokura, Kosuke Tsuji, Yusuke Kobayashi, Iori Kisu, Arisa Ueki, Hiroyuki Nomura, Eiichiro Tominaga, Nobuyuki Susumu, Daisuke Aoki

    ONCOLOGY REPORTS   28 ( 5 )   1537 - 1543   2012.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Lynch syndrome is a genetic disease that often develops in patients with endometrial cancer and is caused by abnormal DNA mismatch repair (MMR) genes. In the United States, it was recently reported that the prevalence of Lynch syndrome with an hMSH2 mutation in patients with endometrial cancer in the lower uterine segment (LUS) is much greater than that in patients with endometrial cancer, although no such reports have been published in Asia. In this study, we examined the correlation between endometrial cancer in LUS and abnormalities in MMR genes. We examined 625 patients, who were diagnosed with endometrial cancer and underwent a hysterectomy. Nine patients (1.4%) :lad cancer based on pathological confirmation of a tumor in the lower part of the uterus and no cancer in the upper part. These cases were compared with 27 cases of sporadic endometrial (non-LUS) cancer. The age and BMI of the patients with LUS cancer were significantly lower than those of the patients with non-LUS cancer. No differences were observed in the pathological characteristics. The microsatellite instability (MSI)-positive rates were similar. Immunohistochemistry showed a decreased expression of hMLH1 and hMSH6 in patients with LUS cancer. In contrast with earlier reports from the United States, hMSH2 was expressed in all the cases. Of the 2 patients with LUS cancer who exhibited high MSI, 1 patient showed abnormal methylation of hMLH1, while the other patient was diagnosed with Lynch syndrome with a mutation in the hMLH1 gene. This is the second report on the relationship of LUS cancer and Lynch syndrome, and the first to describe an Asian patient with LUS cancer with Lynch syndrome induced by an hMLH1 mutation.

    DOI: 10.3892/or.2012.2008

    Web of Science

    researchmap

  • Lobular endocervical glandular hyperplasia and peritoneal pigmentation associated with Peutz-Jeghers syndrome due to a germline mutation of STK11 Reviewed

    A. Hirasawa, T. Akahane, T. Tsuruta, Y. Kobayashi, K. Masuda, K. Banno, T. Fujii, N. Susumu, T. Itsubo, K. Kameyama, K. Sugano, D. Aoki

    ANNALS OF ONCOLOGY   23 ( 11 )   2990 - 2992   2012.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OXFORD UNIV PRESS  

    DOI: 10.1093/annonc/mds492

    Web of Science

    researchmap

  • Blood-direct InvaderPlus® as a new method for genetic testing. International journal

    Akira Hirasawa, Tomoko Akahane, Yusuke Tanigawara, Daisuke Aoki

    Personalized medicine   9 ( 6 )   657 - 663   2012.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:FUTURE MEDICINE LTD  

    AIM: This study compared the efficiency of Blood-direct InvaderPlus® with existing methods for detecting genetic polymorphisms by using clinical samples, and to determine whether this new method can be used for future clinical studies. MATERIALS & METHODS: We developed a new method, called Blood-direct InvaderPlus, for detecting genetic polymorphisms. Whole-blood samples were subjected to genetic analysis with the new method and also the conventional method. RESULTS: The results obtained with the new method were consistent with those of direct sequencing. Blood-direct InvaderPlus was able to detect gene polymorphisms of UGT1A1*6, *27, *28, *60, VKORC1 -1639G>A, VKORC1 1173T>C and CYP2C9 *2 and *3 much faster than the conventional methods. CONCLUSION: Blood-direct InvaderPlus allowed accurate, simple and rapid detection of genetic polymorphisms.

    DOI: 10.2217/pme.12.71

    Web of Science

    PubMed

    researchmap

  • Blood-direct InvaderPlus (R) as a new method for genetic testing Reviewed

    Akira Hirasawa, Tomoko Akahane, Yusuke Tanigawara, Daisuke Aoki

    PERSONALIZED MEDICINE   9 ( 6 )   657 - 663   2012.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:FUTURE MEDICINE LTD  

    Aim: This study compared the efficiency of Blood-direct InvaderPlus (R) with existing methods for detecting genetic polymorphisms by using clinical samples, and to determine whether this new method can be used for future clinical studies. Materials & methods: We developed a new method, called Blood-direct InvaderPlus, for detecting genetic polymorphisms. Whole-blood samples were subjected to genetic analysis with the new method and also the conventional method. Results: The results obtained with the new method were consistent with those of direct sequencing. Blood-direct InvaderPlus was able to detect gene polymorphisms of UGT1A1*6, *2Z *28, *60, VKORC1 -1639G&gt;A, VKORC1 1173T&gt;C and CYP2C9 *2 and *3 much faster than the conventional methods. Conclusion: Blood-direct InvaderPlus allowed accurate, simple and rapid detection of genetic polymorphisms.

    DOI: 10.2217/PME.12.71

    Web of Science

    researchmap

  • Blood-direct InvaderPlus (R) as a new method for genetic testing

    Akira Hirasawa, Tomoko Akahane, Yusuke Tanigawara, Daisuke Aoki

    PERSONALIZED MEDICINE   9 ( 6 )   657 - 663   2012.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:FUTURE MEDICINE LTD  

    Aim: This study compared the efficiency of Blood-direct InvaderPlus (R) with existing methods for detecting genetic polymorphisms by using clinical samples, and to determine whether this new method can be used for future clinical studies. Materials & methods: We developed a new method, called Blood-direct InvaderPlus, for detecting genetic polymorphisms. Whole-blood samples were subjected to genetic analysis with the new method and also the conventional method. Results: The results obtained with the new method were consistent with those of direct sequencing. Blood-direct InvaderPlus was able to detect gene polymorphisms of UGT1A1*6, *2Z *28, *60, VKORC1 -1639G&gt;A, VKORC1 1173T&gt;C and CYP2C9 *2 and *3 much faster than the conventional methods. Conclusion: Blood-direct InvaderPlus allowed accurate, simple and rapid detection of genetic polymorphisms.

    DOI: 10.2217/PME.12.71

    Web of Science

    researchmap

  • 当科健康維持外来受診者における大腿骨近位部骨密度の検討

    AOKI DAISUKE

    Osteoporosis Japan   20 ( 3 )   489 - 491   2012.7

  • 子宮体癌の家族発生と遺伝子診断

    AOKI DAISUKE

    日本臨床 婦人科がん-最新の研究動向-   70 ( 増刊号4 )   292-296 - 296   2012.6

     More details

    Language:Japanese  

    researchmap

  • [Hereditary endometrial cancer and genetic testing].

    Akira Hirasawa, Tomohiko Tsuruta, Kouji Banno, Nobuyuki Susumu, Daisuke Aoki

    Nihon rinsho. Japanese journal of clinical medicine   70 Suppl 4   292 - 6   2012.6

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    PubMed

    researchmap

  • [Hereditary endometrial cancer and genetic testing].

    Hirasawa Akira, Tsuruta Tomohiko, Banno Kouji, Susumu Nobuyuki, Aoki Daisuke

    Nihon rinsho. Japanese journal of clinical medicine   70 Suppl 4   292 - 296   2012.6

     More details

    Language:English  

    researchmap

  • EGRI and FOSB gene expressions in cancer stroma are independent prognostic indicators for epithelial ovarian cancer receiving standard therapy

    Fumio Kataoka, Hiroshi Tsuda, Tokuzo Arao, Sadako Nishimura, Hideo Tanaka, Hiroyuki Nomura, Tatsuyuki Chiyoda, Akira Hirasawa, Tomoko Akahane, Hiroshi Nishio, Kazuto Nishio, Daisuke Aoki

    GENES CHROMOSOMES & CANCER   51 ( 3 )   300 - 312   2012.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY-BLACKWELL  

    Stromal components interact with cancer cells to promote growth and metastasis. The purpose of this study was to identify genes expressed in stroma, which could provide prognostic information in epithelial ovarian cancer (EOC). Seventy-four patients were included. We performed gene expression profiling and confirmed array data using RT-PCR and immunohistochemistry. By microarray analysis, 52 candidate genes associated with progression free survival (PFS) were identified (P &lt; 0.005). Expression of the early growth response 1 (EGR1) and FBJ murine osteosarcoma viral oncogene homolog B (FOSB) genes was further analyzed. Array data were confirmed by RT-PCR and multivariate analysis demonstrated that both EGR1 and FOSB expression in cancer stroma, and EGR1 expression in cancer are independent prognostic factors in EOC. Immunohistochemically, EGR1 protein is localized in cancer cells and a-smooth muscle actin positive stromal fibroblasts. The EGR1 and FOSB expression in stromal cells and EGR1 expression in cancer cells are prognostic indicators in EOC. (c) 2011 Wiley Periodicals, Inc.

    DOI: 10.1002/gcc.21916

    Web of Science

    researchmap

  • EGRI and FOSB gene expressions in cancer stroma are independent prognostic indicators for epithelial ovarian cancer receiving standard therapy Reviewed

    Fumio Kataoka, Hiroshi Tsuda, Tokuzo Arao, Sadako Nishimura, Hideo Tanaka, Hiroyuki Nomura, Tatsuyuki Chiyoda, Akira Hirasawa, Tomoko Akahane, Hiroshi Nishio, Kazuto Nishio, Daisuke Aoki

    GENES CHROMOSOMES & CANCER   51 ( 3 )   300 - 312   2012.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY-BLACKWELL  

    Stromal components interact with cancer cells to promote growth and metastasis. The purpose of this study was to identify genes expressed in stroma, which could provide prognostic information in epithelial ovarian cancer (EOC). Seventy-four patients were included. We performed gene expression profiling and confirmed array data using RT-PCR and immunohistochemistry. By microarray analysis, 52 candidate genes associated with progression free survival (PFS) were identified (P &lt; 0.005). Expression of the early growth response 1 (EGR1) and FBJ murine osteosarcoma viral oncogene homolog B (FOSB) genes was further analyzed. Array data were confirmed by RT-PCR and multivariate analysis demonstrated that both EGR1 and FOSB expression in cancer stroma, and EGR1 expression in cancer are independent prognostic factors in EOC. Immunohistochemically, EGR1 protein is localized in cancer cells and a-smooth muscle actin positive stromal fibroblasts. The EGR1 and FOSB expression in stromal cells and EGR1 expression in cancer cells are prognostic indicators in EOC. (c) 2011 Wiley Periodicals, Inc.

    DOI: 10.1002/gcc.21916

    Web of Science

    researchmap

  • EGRI and FOSB gene expressions in cancer stroma are independent prognostic indicators for epithelial ovarian cancer receiving standard therapy

    Fumio Kataoka, Hiroshi Tsuda, Tokuzo Arao, Sadako Nishimura, Hideo Tanaka, Hiroyuki Nomura, Tatsuyuki Chiyoda, Akira Hirasawa, Tomoko Akahane, Hiroshi Nishio, Kazuto Nishio, Daisuke Aoki

    GENES CHROMOSOMES & CANCER   51 ( 3 )   300 - 312   2012.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY-BLACKWELL  

    Stromal components interact with cancer cells to promote growth and metastasis. The purpose of this study was to identify genes expressed in stroma, which could provide prognostic information in epithelial ovarian cancer (EOC). Seventy-four patients were included. We performed gene expression profiling and confirmed array data using RT-PCR and immunohistochemistry. By microarray analysis, 52 candidate genes associated with progression free survival (PFS) were identified (P &lt; 0.005). Expression of the early growth response 1 (EGR1) and FBJ murine osteosarcoma viral oncogene homolog B (FOSB) genes was further analyzed. Array data were confirmed by RT-PCR and multivariate analysis demonstrated that both EGR1 and FOSB expression in cancer stroma, and EGR1 expression in cancer are independent prognostic factors in EOC. Immunohistochemically, EGR1 protein is localized in cancer cells and a-smooth muscle actin positive stromal fibroblasts. The EGR1 and FOSB expression in stromal cells and EGR1 expression in cancer cells are prognostic indicators in EOC. (c) 2011 Wiley Periodicals, Inc.

    DOI: 10.1002/gcc.21916

    Web of Science

    researchmap

  • 発現解析による子宮体部癌肉腫の生物学的特性の解明.

    千代田達幸, 津田浩史, 片岡史夫, 野村弘行, 田中英雄, 平沢 晃, 進 伸幸, 佐谷秀行, 青木大輔

    日本分子腫瘍マーカー研究会誌   27   23-34 - 24   2012

     More details

    Language:Japanese  

    researchmap

  • Aberrant DNA Methylation in Endometrial Cancer

    Kenta Masuda, Kouji Banno, Megumi Yanokura, Kosuke Tsuji, Iori Kisu, Arisa Ueki, Yusuke Kobayashi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    Epigenetics in Human Disease   471 - 480   2012

     More details

    Language:English   Publishing type:Part of collection (book)   Publisher:Elsevier Inc.  

    DOI: 10.1016/B978-0-12-388415-2.00023-8

    Scopus

    researchmap

  • 遺伝性乳癌卵巣癌 Invited Reviewed

    平沢 晃, 青木大輔

    日本産科婦人科学会雑誌   64 ( 4 )   292 - 296   2012

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 発現解析による子宮体癌再発予測モデルの開発.

    津田浩史, 井口蓉子, 片岡史夫, 野村弘行, 田中英雄, 千代田達幸, 平沢 晃, 進 伸幸, 青木大輔

    日本分子腫瘍マーカー研究会誌   27   45-46 - 46   2012

     More details

    Language:Japanese  

    researchmap

  • 子宮体がんの術後補助療法

    AOKI DAISUKE

    腫瘍内科   8 ( 6 )   563-571 - 571   2011.12

     More details

    Language:Japanese  

    researchmap

  • Immunofluorescence-Detected Infiltration of CD4(+)FOXP3(+) Regulatory T Cells is Relevant to the Prognosis of Patients With Endometrial Cancer Reviewed

    Wataru Yamagami, Nobuyuki Susumu, Hideo Tanaka, Akira Hirasawa, Kouji Banno, Nao Suzuki, Hiroshi Tsuda, Katsumi Tsukazaki, Daisuke Aoki

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   21 ( 9 )   1628 - 1634   2011.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Objective: Host antitumor immune responses are associated with many types of immune cells and soluble components. In particular, CD8(+) cytotoxic T lymphocytes (CTLs) play a central role. Regulatory T cells (Tregs) have been reported to induce tumor immune tolerance in various cancers. In the present study, we evaluated lymphocytic infiltration in endometrial cancer tissue to clarify its relationship with clinicopathological factors and the prognosis of patients.
    Methods: The study included 53 patients whose condition was diagnosed as endometrial cancer between 1994 and 2004 at Keio University hospital. Using formalin-fixed, paraffin-embedded specimens of the uterus, immunohistochemistry was performed with antihuman CD8, antihuman CD4, and antihuman FOXP3 primary antibodies, and the binding sites of the antibodies were visualized using fluorescence-conjugate secondary antibodies. CD4(+) FOXP3(+) cells were identified as Tregs in this study. The numbers of CD8(+) cells, CD4(+) cells, and Tregs as well as the Treg/CD8(+) and Treg/CD4(+) ratios were analyzed to evaluate the relationship between clinicopathological factors and patient prognosis.
    Results: Of the 53 patients studied, 50.9% of them had early-stage disease, 49.1% had advanced stage disease, 47.2% had well-differentiated cancer (grade [G] 1), 24.5% had moderately differentiated cancer (G2), and 28.3% had poorly differentiated cancer (G3). The CD8(+) and CD4(+) cell counts, Treg count, and Treg/CD8(+) and Treg/CD4(+) ratios were significantly higher in the patients with advanced poorly differentiated carcinomas and with positive lymphovascular space invasion than in those with early well-differentiated carcinomas and with negative lymphovascular space invasion. In disease-free survival, the prognosis of the patients with high Treg counts and Treg/CD8(+) ratios was significantly worse than that of the patients with low Treg counts and Treg/CD8(+) ratios (P &lt; 0.05).
    Conclusions: The Treg count and Treg/CD8(+) ratio may be new prognostic factors for endometrial cancer.

    DOI: 10.1097/IGC.0b013e31822c271f

    Web of Science

    researchmap

  • Immunofluorescence-Detected Infiltration of CD4(+)FOXP3(+) Regulatory T Cells is Relevant to the Prognosis of Patients With Endometrial Cancer

    Wataru Yamagami, Nobuyuki Susumu, Hideo Tanaka, Akira Hirasawa, Kouji Banno, Nao Suzuki, Hiroshi Tsuda, Katsumi Tsukazaki, Daisuke Aoki

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   21 ( 9 )   1628 - 1634   2011.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Objective: Host antitumor immune responses are associated with many types of immune cells and soluble components. In particular, CD8(+) cytotoxic T lymphocytes (CTLs) play a central role. Regulatory T cells (Tregs) have been reported to induce tumor immune tolerance in various cancers. In the present study, we evaluated lymphocytic infiltration in endometrial cancer tissue to clarify its relationship with clinicopathological factors and the prognosis of patients.Methods: The study included 53 patients whose condition was diagnosed as endometrial cancer between 1994 and 2004 at Keio University hospital. Using formalin-fixed, paraffin-embedded specimens of the uterus, immunohistochemistry was performed with antihuman CD8, antihuman CD4, and antihuman FOXP3 primary antibodies, and the binding sites of the antibodies were visualized using fluorescence-conjugate secondary antibodies. CD4(+) FOXP3(+) cells were identified as Tregs in this study. The numbers of CD8(+) cells, CD4(+) cells, and Tregs as well as the Treg/CD8(+) and Treg/CD4(+) ratios were analyzed to evaluate the relationship between clinicopathological factors and patient prognosis.Results: Of the 53 patients studied, 50.9% of them had early-stage disease, 49.1% had advanced stage disease, 47.2% had well-differentiated cancer (grade [G] 1), 24.5% had moderately differentiated cancer (G2), and 28.3% had poorly differentiated cancer (G3). The CD8(+) and CD4(+) cell counts, Treg count, and Treg/CD8(+) and Treg/CD4(+) ratios were significantly higher in the patients with advanced poorly differentiated carcinomas and with positive lymphovascular space invasion than in those with early well-differentiated carcinomas and with negative lymphovascular space invasion. In disease-free survival, the prognosis of the patients with high Treg counts and Treg/CD8(+) ratios was significantly worse than that of the patients with low Treg counts and Treg/CD8(+) ratios (P < 0.05).Conclusions: The Treg count and Treg/CD8(+) ratio may be new prognostic factors for endometrial cancer.

    DOI: 10.1097/IGC.0b013e31822c271f

    Web of Science

    researchmap

  • Immunofluorescence-detected infiltration of CD4+FOXP3+ regulatory T cells is relevant to the prognosis of patients with endometrial cancer. International journal

    Wataru Yamagami, Nobuyuki Susumu, Hideo Tanaka, Akira Hirasawa, Kouji Banno, Nao Suzuki, Hiroshi Tsuda, Katsumi Tsukazaki, Daisuke Aoki

    International journal of gynecological cancer : official journal of the International Gynecological Cancer Society   21 ( 9 )   1628 - 34   2011.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    OBJECTIVE: Host antitumor immune responses are associated with many types of immune cells and soluble components. In particular, CD8 cytotoxic T lymphocytes (CTLs) play a central role. Regulatory T cells (Tregs) have been reported to induce tumor immune tolerance in various cancers. In the present study, we evaluated lymphocytic infiltration in endometrial cancer tissue to clarify its relationship with clinicopathological factors and the prognosis of patients. METHODS: The study included 53 patients whose condition was diagnosed as endometrial cancer between 1994 and 2004 at Keio University hospital. Using formalin-fixed, paraffin-embedded specimens of the uterus, immunohistochemistry was performed with antihuman CD8, antihuman CD4, and antihuman FOXP3 primary antibodies, and the binding sites of the antibodies were visualized using fluorescence-conjugate secondary antibodies. CD4FOXP3 cells were identified as Tregs in this study. The numbers of CD8 cells, CD4 cells, and Tregs as well as the Treg/CD8 and Treg/CD4 ratios were analyzed to evaluate the relationship between clinicopathological factors and patient prognosis. RESULTS: Of the 53 patients studied, 50.9% of them had early-stage disease, 49.1% had advanced stage disease, 47.2% had well-differentiated cancer (grade [G] 1), 24.5% had moderately differentiated cancer (G2), and 28.3% had poorly differentiated cancer (G3). The CD8 and CD4 cell counts, Treg count, and Treg/CD8 and Treg/CD4 ratios were significantly higher in the patients with advanced poorly differentiated carcinomas and with positive lymphovascular space invasion than in those with early well-differentiated carcinomas and with negative lymphovascular space invasion. In disease-free survival, the prognosis of the patients with high Treg counts and Treg/CD8 ratios was significantly worse than that of the patients with low Treg counts and Treg/CD8 ratios (P < 0.05). CONCLUSIONS: The Treg count and Treg/CD8 ratio may be new prognostic factors for endometrial cancer.

    DOI: 10.1097/IGC.0b013e31822c271f

    Web of Science

    PubMed

    researchmap

  • Narrow band imaging hysteroscopy: A comparative study using randomized video images Reviewed

    Iori Kisu, Kouji Banno, Yusuke Kobayashi, Asuka Ono, Kenta Masuda, Arisa Ueki, Hiroyuki Nomura, Akira Hirasawa, Takayuki Abe, Keisuke Kouyama, Nobuyuki Susumu, Daisuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   39 ( 5 )   1057 - 1062   2011.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Narrow band imaging (NBI) has been used in the gastrointestinal endoscopy field as a novel endoscopic imaging technique and has contributed to improved qualitative diagnosis and detection of lesions. However, there are only a few studies of use of NBI in the gynecology field. We applied NBI in flexible hysteroscopy at our outpatient clinic and evaluated the utility of NBI hysteroscopy for diagnosis of malignant endometrial lesions by comparison of the sensitivity and specificity between white light alone and white light+NBI using hysteroscopic video images. The subjects were 65 patients with a suspected endometrial lesion in the uterine cavity. These patients underwent flexible hysteroscopy using NBI in addition to conventional white light. Video images from 65 patients were edited into two groups, white light alone (WL group) and white light+NBI (NBI group) (130 images in total). Computerized block randomization of the order was then performed. Four raters independently diagnosed the images without use of other clinical information. Using the pathological diagnosis as the gold standard, we evaluated the sensitivity and specificity of diagnosis of atypical endometrial hyperplasia (AEH) or endometrial carcinoma compared between the WL and NBI groups. The sensitivity of diagnosis of A EH or endometrial carcinoma was numerically higher in the NBI group for all raters, and the average sensitivity was significantly higher in the NBI group compared to the WL group (78.6% vs. 63.7%, P&lt;0.001). The specificity for each rater and the average specificity were comparable between the two groups. Compared to white light hysteroscopy, NBI hysteroscopy had a higher sensitivity for diagnosis of AEH or endometrial carcinoma without loss of specificity. This suggests that NBI hysteroscopy may be more useful than white light hysteroscopy for endoscopic diagnosis of malignant endometrial lesions.

    DOI: 10.3892/ijo.2011.1131

    Web of Science

    researchmap

  • Narrow band imaging hysteroscopy: A comparative study using randomized video images

    Iori Kisu, Kouji Banno, Yusuke Kobayashi, Asuka Ono, Kenta Masuda, Arisa Ueki, Hiroyuki Nomura, Akira Hirasawa, Takayuki Abe, Keisuke Kouyama, Nobuyuki Susumu, Daisuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   39 ( 5 )   1057 - 1062   2011.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Narrow band imaging (NBI) has been used in the gastrointestinal endoscopy field as a novel endoscopic imaging technique and has contributed to improved qualitative diagnosis and detection of lesions. However, there are only a few studies of use of NBI in the gynecology field. We applied NBI in flexible hysteroscopy at our outpatient clinic and evaluated the utility of NBI hysteroscopy for diagnosis of malignant endometrial lesions by comparison of the sensitivity and specificity between white light alone and white light+NBI using hysteroscopic video images. The subjects were 65 patients with a suspected endometrial lesion in the uterine cavity. These patients underwent flexible hysteroscopy using NBI in addition to conventional white light. Video images from 65 patients were edited into two groups, white light alone (WL group) and white light+NBI (NBI group) (130 images in total). Computerized block randomization of the order was then performed. Four raters independently diagnosed the images without use of other clinical information. Using the pathological diagnosis as the gold standard, we evaluated the sensitivity and specificity of diagnosis of atypical endometrial hyperplasia (AEH) or endometrial carcinoma compared between the WL and NBI groups. The sensitivity of diagnosis of A EH or endometrial carcinoma was numerically higher in the NBI group for all raters, and the average sensitivity was significantly higher in the NBI group compared to the WL group (78.6% vs. 63.7%, P&lt;0.001). The specificity for each rater and the average specificity were comparable between the two groups. Compared to white light hysteroscopy, NBI hysteroscopy had a higher sensitivity for diagnosis of AEH or endometrial carcinoma without loss of specificity. This suggests that NBI hysteroscopy may be more useful than white light hysteroscopy for endoscopic diagnosis of malignant endometrial lesions.

    DOI: 10.3892/ijo.2011.1131

    Web of Science

    researchmap

  • Narrow band imaging hysteroscopy: a comparative study using randomized video images. International journal

    Iori Kisu, Kouji Banno, Yusuke Kobayashi, Asuka Ono, Kenta Masuda, Arisa Ueki, Hiroyuki Nomura, Akira Hirasawa, Takayuki Abe, Keisuke Kouyama, Nobuyuki Susumu, Daisuke Aoki

    International journal of oncology   39 ( 5 )   1057 - 62   2011.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Narrow band imaging (NBI) has been used in the gastrointestinal endoscopy field as a novel endoscopic imaging technique and has contributed to improved qualitative diagnosis and detection of lesions. However, there are only a few studies of use of NBI in the gynecology field. We applied NBI in flexible hysteroscopy at our outpatient clinic and evaluated the utility of NBI hysteroscopy for diagnosis of malignant endometrial lesions by comparison of the sensitivity and specificity between white light alone and white light+NBI using hysteroscopic video images. The subjects were 65 patients with a suspected endometrial lesion in the uterine cavity. These patients underwent flexible hysteroscopy using NBI in addition to conventional white light. Video images from 65 patients were edited into two groups, white light alone (WL group) and white light+NBI (NBI group) (130 images in total). Computerized block randomization of the order was then performed. Four raters independently diagnosed the images without use of other clinical information. Using the pathological diagnosis as the gold standard, we evaluated the sensitivity and specificity of diagnosis of atypical endometrial hyperplasia (AEH) or endometrial carcinoma compared between the WL and NBI groups. The sensitivity of diagnosis of AEH or endometrial carcinoma was numerically higher in the NBI group for all raters, and the average sensitivity was significantly higher in the NBI group compared to the WL group (78.6% vs. 63.7%, P<0.001). The specificity for each rater and the average specificity were comparable between the two groups. Compared to white light hysteroscopy, NBI hysteroscopy had a higher sensitivity for diagnosis of AEH or endometrial carcinoma without loss of specificity. This suggests that NBI hysteroscopy may be more useful than white light hysteroscopy for endoscopic diagnosis of malignant endometrial lesions.

    DOI: 10.3892/ijo.2011.1131

    Web of Science

    PubMed

    researchmap

  • miR-152 is a tumor suppressor microRNA that is silenced by DNA hypermethylation in endometrial cancer. International journal

    Tomohiko Tsuruta, Ken-Ichi Kozaki, Atsushi Uesugi, Mayuko Furuta, Akira Hirasawa, Issei Imoto, Nobuyuki Susumu, Daisuke Aoki, Johji Inazawa

    Cancer research   71 ( 20 )   6450 - 62   2011.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    The etiology and development of human cancers that remain little understood might be enlightened by defining tumor suppressor microRNAs (TS-miRNA). In this study, we identified TS-miRNAs silenced by aberrant DNA hypermethylation in endometrial cancer. Functional screening of 327 synthetic miRNAs in an endometrial cancer cell proliferation assay identified 103 miRNAs that inhibited cell growth. We then determined the sequence, DNA methylation status, and expression levels of these miRNAs in endometrial cancer cell lines and primary tumors. These determinations led to the identification of miR-152 as a candidate TS-miRNA gene in endometrial cancer. Epigenetic silencing documented in miR-152 was consistent with its location at 17q21.32 in intron 1 of the COPZ2 gene, which is also silenced often in endometrial cancer by DNA hypermethylation, and also with evidence that miR-152 targets the DNA methyltransferase DNMT1. Notably, restoration of miR-152 expression in endometrial cancer cell lines was sufficient to inhibit tumor cell growth in vitro and in vivo. We identified E2F3, MET, and Rictor as novel candidate targets of miR-152, suggesting how its epigenetic silencing can drive endometrial carcinogenesis. Our findings define a central role for miR-152 in endometrial cancer, and they also suggest its use in new therapeutic strategies to treat this cancer.

    DOI: 10.1158/0008-5472.CAN-11-0364

    Web of Science

    PubMed

    researchmap

  • 妊産婦への向精神薬の投与

    AOKI DAISUKE

    産婦人科治療   103 ( 4 )   417-421 - 421   2011.10

  • Magnifying hysteroscopy with narrow-band imaging for visualization of endometrial lesions

    Kisu I, Banno K, Kobayashi Y, Ono A, Masuda K, Ueki A, Nomura H, Hirasawa A, Abe T, Kouyama K, Susumu N, Aoki D

    Int J Gynaecol Obstet   115 ( 1 )   74-75   2011.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • miR-152 Is a Tumor Suppressor microRNA That Is Silenced by DNA Hypermethylation in Endometrial Cancer Reviewed

    Tomohiko Tsuruta, Ken-ichi Kozaki, Atsushi Uesugi, Mayuko Furuta, Akira Hirasawa, Issei Imoto, Nobuyuki Susumu, Daisuke Aoki, Johji Inazawa

    CANCER RESEARCH   71 ( 20 )   6450 - 6462   2011.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    The etiology and development of human cancers that remain little understood might be enlightened by defining tumor suppressor microRNAs (TS-miRNA). In this study, we identified TS-miRNAs silenced by aberrant DNA hypermethylation in endometrial cancer. Functional screening of 327 synthetic miRNAs in an endometrial cancer cell proliferation assay identified 103 miRNAs that inhibited cell growth. We then determined the sequence, DNA methylation status, and expression levels of these miRNAs in endometrial cancer cell lines and primary tumors. These determinations led to the identification of miR-152 as a candidate TS-miRNA gene in endometrial cancer. Epigenetic silencing documented in miR-152 was consistent with its location at 17q21.32 in intron 1 of the COPZ2 gene, which is also silenced often in endometrial cancer by DNA hypermethylation, and also with evidence that miR-152 targets the DNA methyltransferase DNMT1. Notably, restoration of miR-152 expression in endometrial cancer cell lines was sufficient to inhibit tumor cell growth in vitro and in vivo. We identified E2F3, MET, and Rictor as novel candidate targets of miR-152, suggesting how its epigenetic silencing can drive endometrial carcinogenesis. Our findings define a central role for miR-152 in endometrial cancer, and they also suggest its use in new therapeutic strategies to treat this cancer. Cancer Res; 71(20); 6450-62. (C) 2011 AACR.

    DOI: 10.1158/0008-5472.CAN-11-0364

    Web of Science

    researchmap

  • miR-152 Is a Tumor Suppressor microRNA That Is Silenced by DNA Hypermethylation in Endometrial Cancer

    Tomohiko Tsuruta, Ken-ichi Kozaki, Atsushi Uesugi, Mayuko Furuta, Akira Hirasawa, Issei Imoto, Nobuyuki Susumu, Daisuke Aoki, Johji Inazawa

    CANCER RESEARCH   71 ( 20 )   6450 - 6462   2011.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    The etiology and development of human cancers that remain little understood might be enlightened by defining tumor suppressor microRNAs (TS-miRNA). In this study, we identified TS-miRNAs silenced by aberrant DNA hypermethylation in endometrial cancer. Functional screening of 327 synthetic miRNAs in an endometrial cancer cell proliferation assay identified 103 miRNAs that inhibited cell growth. We then determined the sequence, DNA methylation status, and expression levels of these miRNAs in endometrial cancer cell lines and primary tumors. These determinations led to the identification of miR-152 as a candidate TS-miRNA gene in endometrial cancer. Epigenetic silencing documented in miR-152 was consistent with its location at 17q21.32 in intron 1 of the COPZ2 gene, which is also silenced often in endometrial cancer by DNA hypermethylation, and also with evidence that miR-152 targets the DNA methyltransferase DNMT1. Notably, restoration of miR-152 expression in endometrial cancer cell lines was sufficient to inhibit tumor cell growth in vitro and in vivo. We identified E2F3, MET, and Rictor as novel candidate targets of miR-152, suggesting how its epigenetic silencing can drive endometrial carcinogenesis. Our findings define a central role for miR-152 in endometrial cancer, and they also suggest its use in new therapeutic strategies to treat this cancer. Cancer Res; 71(20); 6450-62. (C) 2011 AACR.

    DOI: 10.1158/0008-5472.CAN-11-0364

    Web of Science

    researchmap

  • 遺伝性乳癌・卵巣がんの取扱いとリスク低減卵管卵巣摘出術

    AOKI DAISUKE

    産科と婦人科   78 ( 9 )   1064-1068 - 1068   2011.9

  • 婦人科疾患と遺伝カウンセリング

    AOKI DAISUKE

    産婦人科の実際   60 ( 9 )   1331-1338 - 1338   2011.9

     More details

    Language:Japanese  

    researchmap

  • 遺伝性腫瘍の基礎知識と遺伝子診断および予防法 ~遺伝性乳がん・卵巣がんに着目して~.

    AOKI DAISUKE

    がん看護   16 ( 6 )   631-635 - 635   2011.9

  • 発現解析による子宮体癌の再発予測モデルの開発

    津田 浩史, 井口 蓉子, 片岡 史夫, 野村 弘行, 田中 英雄, 千代田 達幸, 平沢 晃, 進 伸幸, 青木 大輔

    日本分子腫瘍マーカー研究会プログラム・講演抄録   31回   68 - 69   2011.9

     More details

    Language:Japanese   Publisher:日本分子腫瘍マーカー研究会  

    researchmap

  • 発現解析による子宮体部癌肉腫の生物学的特性の解明

    千代田 達幸, 津田 浩史, 片岡 史夫, 野村 弘行, 田中 英雄, 平沢 晃, 進 伸幸, 佐谷 秀行, 青木 大輔

    日本分子腫瘍マーカー研究会プログラム・講演抄録   31回   46 - 47   2011.9

     More details

    Language:Japanese   Publisher:日本分子腫瘍マーカー研究会  

    researchmap

  • 家系内の遺伝子検査が契機となり早期介入を行ったLynch症候群の1例

    AOKI DAISUKE

    東京産科婦人科学会会誌   60 ( 2 )   293-297 - 297   2011.6

     More details

    Language:Japanese  

    researchmap

  • 産婦人科臨床における遺伝性乳癌卵巣癌の位置づけ

    AOKI DAISUKE

    家族性腫瘍   11 ( 2 )   48-51 - 51   2011.5

  • 老人性腟炎

    AOKI DAISUKE

    臨床婦人科産科   65 ( 4(増大号) )   568-571   2011.4

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • Flexible hysteroscopy with narrow band imaging (NBI) for endoscopic diagnosis of malignant endometrial lesions

    Iori Kisu, Kouji Banno, Yusuke Kobayashi, Asuka Ono, Kenta Masuda, Arisa Ueki, Hiroyuki Nomura, Akira Hirasawa, Takayuki Abe, Keisuke Kouyama, Nobuyuki Susumu, Daisuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   38 ( 3 )   613 - 618   2011.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Narrow band imaging (NBI) for detection of blood vessels and microstructures on the mucosal surface is used in gastrointestinal endoscopy since it can improve qualitative diagnosis and detection of lesion. However, there are no studies on flexible hysteroscopy using NBI. We performed flexible hysteroscopy with NBI for outpatients to investigate the sensitivity and specificity of endoscopic diagnosis of malignant endometrial lesions. Of patients who attended our hospital for suspected lesions in the uterine cavity between April 2009 and May 2010, 104 subjects underwent hysteroscopy with NBI, in addition to white light. Using the pathological diagnosis as the gold-standard, we evaluated the sensitivity and specificity of NBI hysteroscopy for detecting atypical endometrial hyperplasia (AEH) or carcinoma. The results were also compared with historical data (n=209) for conventional hysteroscopy using white light only in 2008. The sensitivities were 97.2% [95% confidence interval (95% CI): 90.3-99.7%] and 82.6% (95% Cl: 74.4-89.0%) for NBI hysteroscopy and conventional hysteroscopy, respectively. The 95% CIs for the two methods did not overlap and the sensitivity of lesion detection was higher with NB! hysteroscopy. Specificities were comparable, 90.6% (95% CI: 75.0-98.0%) and 85.1% (95% CI: 76.3-91.6%) between the methods. NBI hysteroscopy has increased sensitivity for detection of atypical endometrial hyperplasia (AEH) or carcinoma. A comparison with historical data suggested that NBI may be useful for diagnosis of malignant endometrial lesions. As far as we are aware, this is the first evaluation of flexible hysteroscopy with NBI for diagnosis of malignant endometrial lesions.

    DOI: 10.3892/ijo.2011.903

    Web of Science

    researchmap

  • Flexible hysteroscopy with narrow band imaging (NBI) for endoscopic diagnosis of malignant endometrial lesions. International journal

    Iori Kisu, Kouji Banno, Yusuke Kobayashi, Asuka Ono, Kenta Masuda, Arisa Ueki, Hiroyuki Nomura, Akira Hirasawa, Takayuki Abe, Keisuke Kouyama, Nobuyuki Susumu, Daisuke Aoki

    International journal of oncology   38 ( 3 )   613 - 8   2011.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Narrow band imaging (NBI) for detection of blood vessels and microstructures on the mucosal surface is used in gastrointestinal endoscopy since it can improve qualitative diagnosis and detection of lesion. However, there are no studies on flexible hysteroscopy using NBI. We performed flexible hysteroscopy with NBI for outpatients to investigate the sensitivity and specificity of endoscopic diagnosis of malignant endometrial lesions. Of patients who attended our hospital for suspected lesions in the uterine cavity between April 2009 and May 2010, 104 subjects underwent hysteroscopy with NBI, in addition to white light. Using the pathological diagnosis as the gold-standard, we evaluated the sensitivity and specificity of NBI hysteroscopy for detecting atypical endometrial hyperplasia (AEH) or carcinoma. The results were also compared with historical data (n=209) for conventional hysteroscopy using white light only in 2008. The sensitivities were 97.2% [95% confidence interval (95% CI): 90.3-99.7%] and 82.6% (95% CI: 74.4-89.0%) for NBI hysteroscopy and conventional hysteroscopy, respectively. The 95% CIs for the two methods did not overlap and the sensitivity of lesion detection was higher with NBI hysteroscopy. Specificities were comparable, 90.6% (95% CI: 75.0-98.0%) and 85.1% (95% CI: 76.3-91.6%) between the methods. NBI hysteroscopy has increased sensitivity for detection of atypical endometrial hyperplasia (AEH) or carcinoma. A comparison with historical data suggested that NBI may be useful for diagnosis of malignant endometrial lesions. As far as we are aware, this is the first evaluation of flexible hysteroscopy with NBI for diagnosis of malignant endometrial lesions.

    DOI: 10.3892/ijo.2011.903

    Web of Science

    PubMed

    researchmap

  • Carcinoma of the Lower Uterine Segment (LUS): Clinicopathological Characteristics and Association with Lynch Syndrome

    Kenta Masuda, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Iori Kisu, Arisa Ueki, Asuka Ono, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    CURRENT GENOMICS   12 ( 1 )   25 - 29   2011.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BENTHAM SCIENCE PUBL LTD  

    Endometrial cancer arises from the uterine body and fundus in many cases, but can also originate from the lower region of the uterine body through the upper region of the cervix. Such tumors are referred to as carcinoma of the lower uterine segment (LUS) or isthmus, and account for 3-6.3% of all cases of endometrial cancer. This relatively low incidence has permitted performance of only small-scale studies, but the clinical and pathological characteristics of carcinoma of the LUS in all these reports have differed from those of other endometrial cancers. Generally, endometrial cancer is classified into estrogen-dependent endometrioid adenocarcinoma (designated as type I), and non-endometrioid types that are less associated with estrogen and include poorly differentiated adenocarcinoma (type II). In some reports, carcinoma of the LUS has been found to have type II characteristics. Carcinoma of the LUS has also been associated with Lynch syndrome, a hereditary disease with frequent development of colorectal, endometrial, and ovarian cancers. Lynch syndrome is thought to be induced by mismatch repair gene mutation. The frequency of Lynch syndrome in cases of general endometrial cancer is 1-2%. In contrast, the frequency in patients with carcinoma of the LUS is much higher, with up to 29% of cases diagnosable with Lynch syndrome and a high frequency of hMSH2 mutation found in one study. This suggests that further investigation of the clinical and pathological characteristics of carcinoma of the LUS and the association with Lynch syndrome is required through performance of a large-scale survey.

    DOI: 10.2174/138920211794520169

    Web of Science

    researchmap

  • Carcinoma of the Lower Uterine Segment (LUS): Clinicopathological Characteristics and Association with Lynch Syndrome. International journal

    Kenta Masuda, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Iori Kisu, Arisa Ueki, Asuka Ono, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    Current genomics   12 ( 1 )   25 - 9   2011.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BENTHAM SCIENCE PUBL LTD  

    Endometrial cancer arises from the uterine body and fundus in many cases, but can also originate from the lower region of the uterine body through the upper region of the cervix. Such tumors are referred to as carcinoma of the lower uterine segment (LUS) or isthmus, and account for 3-6.3% of all cases of endometrial cancer. This relatively low incidence has permitted performance of only small-scale studies, but the clinical and pathological characteristics of carcinoma of the LUS in all these reports have differed from those of other endometrial cancers. Generally, endometrial cancer is classified into estrogen-dependent endometrioid adenocarcinoma (designated as type I), and non-endometrioid types that are less associated with estrogen and include poorly differentiated adenocarcinoma (type II). In some reports, carcinoma of the LUS has been found to have type II characteristics. Carcinoma of the LUS has also been associated with Lynch syndrome, a hereditary disease with frequent development of colorectal, endometrial, and ovarian cancers. Lynch syndrome is thought to be induced by mismatch repair gene mutation. The frequency of Lynch syndrome in cases of general endometrial cancer is 1-2%. In contrast, the frequency in patients with carcinoma of the LUS is much higher, with up to 29% of cases diagnosable with Lynch syndrome and a high frequency of hMSH2 mutation found in one study. This suggests that further investigation of the clinical and pathological characteristics of carcinoma of the LUS and the association with Lynch syndrome is required through performance of a large-scale survey.

    DOI: 10.2174/138920211794520169

    Web of Science

    PubMed

    researchmap

  • Carcinoma of the Lower Uterine Segment (LUS): Clinicopathological Characteristics and Association with Lynch Syndrome

    Kenta Masuda, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Iori Kisu, Arisa Ueki, Asuka Ono, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    CURRENT GENOMICS   12 ( 1 )   25 - 29   2011.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BENTHAM SCIENCE PUBL LTD  

    Endometrial cancer arises from the uterine body and fundus in many cases, but can also originate from the lower region of the uterine body through the upper region of the cervix. Such tumors are referred to as carcinoma of the lower uterine segment (LUS) or isthmus, and account for 3-6.3% of all cases of endometrial cancer. This relatively low incidence has permitted performance of only small-scale studies, but the clinical and pathological characteristics of carcinoma of the LUS in all these reports have differed from those of other endometrial cancers. Generally, endometrial cancer is classified into estrogen-dependent endometrioid adenocarcinoma (designated as type I), and non-endometrioid types that are less associated with estrogen and include poorly differentiated adenocarcinoma (type II). In some reports, carcinoma of the LUS has been found to have type II characteristics. Carcinoma of the LUS has also been associated with Lynch syndrome, a hereditary disease with frequent development of colorectal, endometrial, and ovarian cancers. Lynch syndrome is thought to be induced by mismatch repair gene mutation. The frequency of Lynch syndrome in cases of general endometrial cancer is 1-2%. In contrast, the frequency in patients with carcinoma of the LUS is much higher, with up to 29% of cases diagnosable with Lynch syndrome and a high frequency of hMSH2 mutation found in one study. This suggests that further investigation of the clinical and pathological characteristics of carcinoma of the LUS and the association with Lynch syndrome is required through performance of a large-scale survey.

    DOI: 10.2174/138920211794520169

    Web of Science

    researchmap

  • 腫瘍間質の遺伝子発現解析を用いた進行上皮性卵巣癌に対する新規バイオマーカーの探索

    AOKI DAISUKE

    日本分子腫瘍マーカー研究会誌   26   32-33 - 33   2011.1

  • ホルモン補充療法が腰椎骨密度に及ぼす長期的な効果の検討 -当科健康維持外来における10年継続投与例からの検証- .

    牧田和也, 松村聡子, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔

    Osteoporosis Japan   18 ( 3 )   83-85 - 539   2011

  • MicroRNA in endometrial cancer Reviewed

    Yanokura M, Banno K, Kisu I, Masuda K, Ueki A, Kobayashi Y, Tsuji K, Yamagami W, Nomura H, Hirasawa A, Susumu N, Aoki D

    Trends in Cancer Research   7   49-55   2011

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • Relationship between DNA Mismatch Repair Deficiency and Endometrial Cancer. Reviewed International journal

    Kenta Masuda, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Iori Kisu, Arisa Ueki, Asuka Ono, Nana Asahara, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    Molecular biology international   2011   256063 - 256063   2011

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Some cases of endometrial cancer are associated with a familial tumor and are referred to as hereditary nonpolyposis colorectal cancer (HNPCC or Lynch syndrome). Lynch syndrome is thought to be induced by germline mutation of the DNA mismatch repair (MMR) gene. An aberration in the MMR gene prevents accurate repair of base mismatches produced during DNA replication. This phenomenon can lead to an increased frequency of errors in target genes involved in carcinogenesis, resulting in cancerization of the cell. On the other hand, aberrant DNA methylation is thought to play a key role in sporadic endometrial carcinogenesis. Hypermethylation of unmethylated CpG islands in the promoter regions of cancer-related genes associated with DNA repair leads to the cell becoming cancerous. Thus, both genetic and epigenetic changes are intricately involved in the process through which cells become cancerous. In this review, we introduce the latest findings on the DNA mismatch repair pathway in endometrial cancer.

    DOI: 10.4061/2011/256063

    PubMed

    researchmap

  • Visual Analogue Scale(VAS)を用いた呉茱萸湯の片頭痛に対する治療効果の検討.

    堀場裕子, 牧田和也, 松村聡子, 平沢 晃, 青木大輔, 吉村泰典

    産婦人科漢方研究のあゆみ   28 ( 28 )   80-83 - 83   2011

     More details

    Language:Japanese  

    researchmap

  • 当科「健康維持外来」におけるホルモン補充療法施行症例についての検証.

    牧田和也, 松村聡子, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔, 吉村泰典

    日本女性医学学会雑誌   19 ( 1 )   18-23 - 24   2011

     More details

    Language:Japanese  

    researchmap

  • 家系内の遺伝子検査が契機となり早期介入に至ったリンチ症候群の1例.

    中村加奈子, 平沢 晃, 赤羽智子, 鶴田智彦, 冨永英一郎, 阪埜浩司, 藤井多久磨, 進 伸幸, 青木大輔, 吉村泰典

    日本産科婦人科学会東京地方部会会誌   60 ( 2 )   293-297   2011

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 大腿骨頸部骨密度測定は腰椎骨骨密度測定の代用となり得るか?—当科健康維持外来受診者からの比較検討—

    牧田和也, 松村聡子, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 青木大輔

    Osteoporosis Japan   19 ( 3 )   481-483 - 483   2011

  • Atypical Polypoid Adenomyoma (APAM) of the Uterine: Relationship with Endometrial Cancer Reviewed

    Kisu I, Banno K, Yanokura M, Kobayashi Y, Ueki A, Ono A, Masuda K, Yamagami W, Nomura H, HIRASAWA AKIRA, Susumu N, Aoki D

    Journal of Cancer Therapy   2 ( 4 )   458-462   2011

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • Gynecological tumors in patients with Peutz-Jeghers syndrome (PJS). Reviewed

    Ueki A, Kisu I, Banno K, Yanokura M, Masuda K, Kobayashi Y, HIRASAWA AKIRA, Aoki D

    Open Journal of Genetics   1 ( 3 )   65-69   2011

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • ASSOCIATION BETWEEN COPY NUMBER VARIATIONS OF ESTROGEN MATABOLISM-RELATED GENE AND BONE MINERAL DENSITY IN POSTMENOPAUSAL WOMEN OF JANANESE Reviewed

    A. Hirasawa, K. Makita, T. Akahane, K. Banno, N. Susumu, D. Aoki

    OSTEOPOROSIS INTERNATIONAL   21 ( 5 )   S722 - S723   2010.12

     More details

    Language:English   Publishing type:Research paper (conference, symposium, etc.)   Publisher:SPRINGER LONDON LTD  

    Web of Science

    researchmap

  • 遺伝性乳癌卵巣癌-婦人科の観点より-

    平沢 晃, 野村 弘行, 青木 大輔

    乳癌の臨床   25 ( 5 )   523-527 - 527   2010.11

     More details

    Language:Japanese   Publisher:篠原出版新社(東京)  

    researchmap

  • MicroRNA and endometrial cancer: Roles of small RNAs in human tumors and clinical applications

    Megumi Yanokura, Kouji Banno, Yusuke Kobayashi, Iori Kisu, Arisa Ueki, Asuka Ono, Kennta Masuda, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    ONCOLOGY LETTERS   1 ( 6 )   935 - 940   2010.11

     More details

    Language:English   Publisher:SPANDIDOS PUBL LTD  

    MicroRNAs (miRNAs) are small non-coding RNAs of approximately 22 base pairs that regulate the expression of genes by targeting messenger RNA with complementarity with the miRNA base sequence. Regulation of gene expression by miRNAs is crucial in cellular development and differentiation, and recent studies suggest a relationship between human diseases and the breakdown of gene silencing mechanisms induced by miRNA abnormalities. In particular, abnormal miRNA expression has been detected in various types of cancer and the target genes have been identified. These results indicate that miRNAs act in a manner equivalent to oncogenes or tumor suppressors. miRNAs may also serve as diagnostic biomarkers and therapeutic targets. In this review, we introduce the latest findings on miRNAs in human endometrial cancer, a common malignancy, and discuss the potential of miRNAs as biomarkers and targets for molecular therapy.

    DOI: 10.3892/ol.2010.173

    Web of Science

    researchmap

  • MicroRNA and endometrial cancer: Roles of small RNAs in human tumors and clinical applications (Review). Reviewed International journal

    Megumi Yanokura, Kouji Banno, Yusuke Kobayashi, Iori Kisu, Arisa Ueki, Asuka Ono, Kennta Masuda, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    Oncology letters   1 ( 6 )   935 - 940   2010.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    MicroRNAs (miRNAs) are small non-coding RNAs of approximately 22 base pairs that regulate the expression of genes by targeting messenger RNA with complementarity with the miRNA base sequence. Regulation of gene expression by miRNAs is crucial in cellular development and differentiation, and recent studies suggest a relationship between human diseases and the breakdown of gene silencing mechanisms induced by miRNA abnormalities. In particular, abnormal miRNA expression has been detected in various types of cancer and the target genes have been identified. These results indicate that miRNAs act in a manner equivalent to oncogenes or tumor suppressors. miRNAs may also serve as diagnostic biomarkers and therapeutic targets. In this review, we introduce the latest findings on miRNAs in human endometrial cancer, a common malignancy, and discuss the potential of miRNAs as biomarkers and targets for molecular therapy.

    DOI: 10.3892/ol.2010.173

    Web of Science

    PubMed

    researchmap

  • MicroRNA and endometrial cancer: Roles of small RNAs in human tumors and clinical applications

    Megumi Yanokura, Kouji Banno, Yusuke Kobayashi, Iori Kisu, Arisa Ueki, Asuka Ono, Kennta Masuda, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    ONCOLOGY LETTERS   1 ( 6 )   935 - 940   2010.11

     More details

    Language:English   Publisher:SPANDIDOS PUBL LTD  

    MicroRNAs (miRNAs) are small non-coding RNAs of approximately 22 base pairs that regulate the expression of genes by targeting messenger RNA with complementarity with the miRNA base sequence. Regulation of gene expression by miRNAs is crucial in cellular development and differentiation, and recent studies suggest a relationship between human diseases and the breakdown of gene silencing mechanisms induced by miRNA abnormalities. In particular, abnormal miRNA expression has been detected in various types of cancer and the target genes have been identified. These results indicate that miRNAs act in a manner equivalent to oncogenes or tumor suppressors. miRNAs may also serve as diagnostic biomarkers and therapeutic targets. In this review, we introduce the latest findings on miRNAs in human endometrial cancer, a common malignancy, and discuss the potential of miRNAs as biomarkers and targets for molecular therapy.

    DOI: 10.3892/ol.2010.173

    Web of Science

    researchmap

  • 腫瘍間質の遺伝子発現解析を用いた進行上皮性卵巣癌に対する新規バイオマーカーの探索

    片岡 史夫, 津田 浩史, 野村 弘行, 千代田 達幸, 平沢 晃, 冨永 英一郎, 鈴木 淳, 進 伸幸, 青木 大輔

    日本分子腫瘍マーカー研究会プログラム・講演抄録   30回   52 - 53   2010.9

     More details

    Language:Japanese   Publisher:日本分子腫瘍マーカー研究会  

    researchmap

  • 女性の片頭痛

    AOKI DAISUKE

    産婦人科治療   101 ( 2 )   135-139 - 139   2010.8

  • Amplification of GNAS may be an independent, qualitative, and reproducible biomarker to predict progression-free survival in epithelial ovarian cancer. International journal

    Ei-ichiro Tominaga, Hiroshi Tsuda, Tokuzo Arao, Sadako Nishimura, Masashi Takano, Fumio Kataoka, Hiroyuki Nomura, Akira Hirasawa, Daisuke Aoki, Kazuto Nishio

    Gynecologic oncology   118 ( 2 )   160 - 6   2010.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ACADEMIC PRESS INC ELSEVIER SCIENCE  

    OBJECTIVES: The purpose of this study was to identify genes that predict progression-free survival (PFS) in advanced epithelial ovarian cancer (aEOC) receiving standard therapy. METHODS: We performed microarray analysis on laser microdissected aEOC cells. All cases received staging laparotomy and adjuvant chemotherapy (carboplatin+paclitaxel) as primary therapy. RESULTS: Microarray analysis identified 50 genes differentially expressed between tumors of patients with no evidence of disease (NED) or evidence of disease (ED) (p<0.001). Six genes (13%) were located at 8q24, and 9 genes (19.6%), at 20q11-13. The ratio of selected gene set/analyzed gene set in chromosomes 8 and 20 are significantly higher than that in other chromosome regions (6/606 vs. 32/13656, p=0.01) and (12/383 vs. 32/13656, p=1.3 x 10(-)(16)). We speculate that the abnormal chromosomal distribution is due to genomic alteration and that these genes may play an important role in aEOC and choose GNAS (GNAS complex locus, NM_000516) on 20q13 based on the p value and fold change. Genomic PCR of aEOC cells also showed that amplification of GNAS was significantly correlated with unfavorable PFS (p=0.011). Real-time quantitative RT-PCR analysis of independent samples revealed that high mRNA expression levels of the GNAS genes, located at chromosome 20q13, was significantly unfavorable indicators of progression-free survival (PFS). Finally, GNAS amplification was an independent prognostic factor for PFS. CONCLUSIONS: Our results suggest that GNAS gene amplification may be an independent, qualitative, and reproducible biomarker of PFS in aEOC.

    DOI: 10.1016/j.ygyno.2010.03.010

    Web of Science

    PubMed

    researchmap

  • 無結紮手術(BiClamp,Ligasure,ハーモニック)-広汎子宮全摘出術におけるBiClamp使用の実際

    AOKI DAISUKE

    産婦人科の実際   59 ( 8 )   1195-1200 - 1200   2010.8

     More details

    Language:Japanese  

    researchmap

  • A genome-wide association study identifies genetic variants in the CDKN2BAS locus associated with endometriosis in Japanese. Reviewed International journal

    Satoko Uno, Hitoshi Zembutsu, Akira Hirasawa, Atsushi Takahashi, Michiaki Kubo, Tomoko Akahane, Daisuke Aoki, Naoyuki Kamatani, Koichi Hirata, Yusuke Nakamura

    Nature genetics   42 ( 8 )   707 - 10   2010.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    Although the pathogenesis of endometriosis is not well understood, genetic factors have been considered to have critical roles in its etiology. Through a genome-wide association study and a replication study using a total of 1,907 Japanese individuals with endometriosis (cases) and 5,292 controls, we identified a significant association of endometriosis with rs10965235 (P = 5.57 x 10(-12), odds ratio = 1.44), which is located in CDKN2BAS on chromosome 9p21, encoding the cyclin-dependent kinase inhibitor 2B antisense RNA. By fine mapping, the SNP showing the strongest association was located in intron 16 of CDKN2BAS and was implicated in regulating the expression of p15, p16 and p14. A SNP, rs16826658, in the LD block including WNT4 on chromosome 1p36, which is considered to play an important role in the development of the female genital tract, revealed a possible association with endometriosis (P = 1.66 x 10(-6), odds ratio = 1.20). Our findings suggest that these regions are new susceptibility loci for endometriosis.

    DOI: 10.1038/ng.612

    Web of Science

    PubMed

    researchmap

  • A genome-wide association study identifies genetic variants in the CDKN2BAS locus associated with endometriosis in Japanese

    Satoko Uno, Hitoshi Zembutsu, Akira Hirasawa, Atsushi Takahashi, Michiaki Kubo, Tomoko Akahane, Daisuke Aoki, Naoyuki Kamatani, Koichi Hirata, Yusuke Nakamura

    NATURE GENETICS   42 ( 8 )   707 - U88   2010.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    Although the pathogenesis of endometriosis is not well understood, genetic factors have been considered to have critical roles in its etiology. Through a genome-wide association study and a replication study using a total of 1,907 Japanese individuals with endometriosis (cases) and 5,292 controls, we identified a significant association of endometriosis with rs10965235 (P = 5.57 x 10(-12), odds ratio = 1.44), which is located in CDKN2BAS on chromosome 9p21, encoding the cyclin-dependent kinase inhibitor 2B antisense RNA. By fine mapping, the SNP showing the strongest association was located in intron 16 of CDKN2BAS and was implicated in regulating the expression of p15, p16 and p14. A SNP, rs16826658, in the LD block including WNT4 on chromosome 1p36, which is considered to play an important role in the development of the female genital tract, revealed a possible association with endometriosis (P = 1.66 x 10(-6), odds ratio = 1.20). Our findings suggest that these regions are new susceptibility loci for endometriosis.

    DOI: 10.1038/ng.612

    Web of Science

    researchmap

  • A genome-wide association study identifies genetic variants in the CDKN2BAS locus associated with endometriosis in Japanese

    Satoko Uno, Hitoshi Zembutsu, Akira Hirasawa, Atsushi Takahashi, Michiaki Kubo, Tomoko Akahane, Daisuke Aoki, Naoyuki Kamatani, Koichi Hirata, Yusuke Nakamura

    NATURE GENETICS   42 ( 8 )   707 - U88   2010.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    Although the pathogenesis of endometriosis is not well understood, genetic factors have been considered to have critical roles in its etiology. Through a genome-wide association study and a replication study using a total of 1,907 Japanese individuals with endometriosis (cases) and 5,292 controls, we identified a significant association of endometriosis with rs10965235 (P = 5.57 x 10(-12), odds ratio = 1.44), which is located in CDKN2BAS on chromosome 9p21, encoding the cyclin-dependent kinase inhibitor 2B antisense RNA. By fine mapping, the SNP showing the strongest association was located in intron 16 of CDKN2BAS and was implicated in regulating the expression of p15, p16 and p14. A SNP, rs16826658, in the LD block including WNT4 on chromosome 1p36, which is considered to play an important role in the development of the female genital tract, revealed a possible association with endometriosis (P = 1.66 x 10(-6), odds ratio = 1.20). Our findings suggest that these regions are new susceptibility loci for endometriosis.

    DOI: 10.1038/ng.612

    Web of Science

    researchmap

  • Amplification of GNAS may be an independent, qualitative, and reproducible biomarker to predict progression-free survival in epithelial ovarian cancer Reviewed

    Ei-ichiro Tominaga, Hiroshi Tsuda, Tokuzo Arao, Sadako Nishimura, Masashi Takano, Fumio Kataoka, Hiroyuki Nomura, Akira Hirasawa, Daisuke Aoki, Kazuto Nishio

    GYNECOLOGIC ONCOLOGY   118 ( 2 )   160 - 166   2010.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ACADEMIC PRESS INC ELSEVIER SCIENCE  

    Objectives. The purpose of this study was to identify genes that predict progression-free survival (PFS) in advanced epithelial ovarian cancer (aEOC) receiving standard therapy.Methods. We performed microarray analysis on laser microdissected aEOC cells. All cases received staging laparotomy and adjuvant chemotherapy (carboplatin + paclitaxel) as primary therapy.Results. Microarray analysis identified 50 genes differentially expressed between tumors of patients with no evidence of disease (NED) or evidence of disease (ED) (p<0.001). Six genes (13%) were located at 8q24, and 9 genes (19.6%), at 20q11-13. The ratio of selected gene set/analyzed gene set in chromosomes 8 and 20 are significantly higher than that in other chromosome regions (6/606 vs. 32/13656, p 0.01) and (12/383 vs. 32/13656, p = 1.3 x 10(-16)). We speculate that the abnormal chromosomal distribution is due to genomic alteration and that these genes may play an important role in aEOC and choose GNAS (GNAS complex locus, NM__000516) on 20q13 based on the p value and fold change. Genomic PCR of aEOC cells also showed that amplification of GNAS was significantly correlated with unfavorable PFS (p = 0.011). Real-time quantitative RT-PCR analysis of independent samples revealed that high mRNA expression levels of the GNAS genes, located at chromosome 20q13, was significantly unfavorable indicators of progression-free survival (PFS). Finally, GNAS amplification was an independent prognostic factor for PFS.Conclusions. Our results suggest that GNAS gene amplification may be an independent, qualitative, and reproducible biomarker of PFS in aEOC. (C) 2010 Elsevier Inc. All rights reserved.

    DOI: 10.1016/j.ygyno.2010.03.010

    Web of Science

    researchmap

  • Amplification of GNAS may be an independent, qualitative, and reproducible biomarker to predict progression-free survival in epithelial ovarian cancer

    Ei-ichiro Tominaga, Hiroshi Tsuda, Tokuzo Arao, Sadako Nishimura, Masashi Takano, Fumio Kataoka, Hiroyuki Nomura, Akira Hirasawa, Daisuke Aoki, Kazuto Nishio

    GYNECOLOGIC ONCOLOGY   118 ( 2 )   160 - 166   2010.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ACADEMIC PRESS INC ELSEVIER SCIENCE  

    Objectives. The purpose of this study was to identify genes that predict progression-free survival (PFS) in advanced epithelial ovarian cancer (aEOC) receiving standard therapy.
    Methods. We performed microarray analysis on laser microdissected aEOC cells. All cases received staging laparotomy and adjuvant chemotherapy (carboplatin + paclitaxel) as primary therapy.
    Results. Microarray analysis identified 50 genes differentially expressed between tumors of patients with no evidence of disease (NED) or evidence of disease (ED) (p&lt;0.001). Six genes (13%) were located at 8q24, and 9 genes (19.6%), at 20q11-13. The ratio of selected gene set/analyzed gene set in chromosomes 8 and 20 are significantly higher than that in other chromosome regions (6/606 vs. 32/13656, p 0.01) and (12/383 vs. 32/13656, p = 1.3 x 10(-16)). We speculate that the abnormal chromosomal distribution is due to genomic alteration and that these genes may play an important role in aEOC and choose GNAS (GNAS complex locus, NM__000516) on 20q13 based on the p value and fold change. Genomic PCR of aEOC cells also showed that amplification of GNAS was significantly correlated with unfavorable PFS (p = 0.011). Real-time quantitative RT-PCR analysis of independent samples revealed that high mRNA expression levels of the GNAS genes, located at chromosome 20q13, was significantly unfavorable indicators of progression-free survival (PFS). Finally, GNAS amplification was an independent prognostic factor for PFS.
    Conclusions. Our results suggest that GNAS gene amplification may be an independent, qualitative, and reproducible biomarker of PFS in aEOC. (C) 2010 Elsevier Inc. All rights reserved.

    DOI: 10.1016/j.ygyno.2010.03.010

    Web of Science

    researchmap

  • Relationship Between ABCF2 Expression and Response to Chemotherapy or Prognosis in Clear Cell Adenocarcinoma of the Ovary Reviewed

    Hiroshi Tsuda, Kiyoshi Ito, Nobuo Yaegashi, Akira Hirasawa, Tamotsu Sudo, Tsunekazu Kita, Yoshito Terai, Junzo Kigawa, Toru Sugiyama, Daisuke Aoki

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   20 ( 5 )   794 - 797   2010.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Objectives: The purpose of this study was to evaluate the association of ABCF2 (adenosine triphosphate-binding cassette superfamily F2) protein expression with response to chemotherapy and prognosis in patients with clear cell adenocarcinoma (CCC) of the ovary.Methods: One hundred sixty-five patients with CCC were studied, and cytoplasmic ABCF2 expression was detected by immunohistochemical staining. All patients underwent platinum-based primary chemotherapy followed by primary surgery.Results: Adenosine triphosphate-binding cassette superfamily F2 expression was detected in 118 (71.5%) of 165 patients and was not related to age or clinical stage. The response rate to chemotherapy in 38 patients with measurable disease was 47.3% (18/38). The response rate tended to be higher in patients without ABCF2 expression than in those with ABCF2 expression; however, this difference was not significant (66.7% vs 34.8%, P = 0.096). There was no significant difference in overall survival between ABCF2-positive and ABCF2-negative cases (median survival time, 1175 vs 1257 days; P = 0.24).Conclusions: Adenosine triphosphate-binding cassette superfamily F2 protein was highly expressed in CCC of the ovary, but expression was not related to age, clinical stage, chemoresponse, or prognosis.

    DOI: 10.1111/IGC.0b013e3181a835fc

    Web of Science

    researchmap

  • Relationship between ABCF2 expression and response to chemotherapy or prognosis in clear cell adenocarcinoma of the ovary. International journal

    Hiroshi Tsuda, Kiyoshi Ito, Nobuo Yaegashi, Akira Hirasawa, Tamotsu Sudo, Tsunekazu Kita, Yoshito Terai, Junzo Kigawa, Toru Sugiyama, Daisuke Aoki

    International journal of gynecological cancer : official journal of the International Gynecological Cancer Society   20 ( 5 )   794 - 7   2010.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    OBJECTIVES: The purpose of this study was to evaluate the association of ABCF2 (adenosine triphosphate-binding cassette superfamily F2) protein expression with response to chemotherapy and prognosis in patients with clear cell adenocarcinoma (CCC) of the ovary. METHODS: One hundred sixty-five patients with CCC were studied, and cytoplasmic ABCF2 expression was detected by immunohistochemical staining. All patients underwent platinum-based primary chemotherapy followed by primary surgery. RESULTS: Adenosine triphosphate-binding cassette superfamily F2 expression was detected in 118 (71.5%) of 165 patients and was not related to age or clinical stage. The response rate to chemotherapy in 38 patients with measurable disease was 47.3% (18/38). The response rate tended to be higher in patients without ABCF2 expression than in those with ABCF2 expression; however, this difference was not significant (66.7% vs 34.8%, P = 0.096). There was no significant difference in overall survival between ABCF2-positive and ABCF2-negative cases (median survival time, 1175 vs 1257 days; P = 0.24). CONCLUSIONS: Adenosine triphosphate-binding cassette superfamily F2 protein was highly expressed in CCC of the ovary, but expression was not related to age, clinical stage, chemoresponse, or prognosis.

    DOI: 10.1111/IGC.0b013e3181a835fc

    Web of Science

    PubMed

    researchmap

  • Relationship Between ABCF2 Expression and Response to Chemotherapy or Prognosis in Clear Cell Adenocarcinoma of the Ovary

    Hiroshi Tsuda, Kiyoshi Ito, Nobuo Yaegashi, Akira Hirasawa, Tamotsu Sudo, Tsunekazu Kita, Yoshito Terai, Junzo Kigawa, Toru Sugiyama, Daisuke Aoki

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   20 ( 5 )   794 - 797   2010.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Objectives: The purpose of this study was to evaluate the association of ABCF2 (adenosine triphosphate-binding cassette superfamily F2) protein expression with response to chemotherapy and prognosis in patients with clear cell adenocarcinoma (CCC) of the ovary.
    Methods: One hundred sixty-five patients with CCC were studied, and cytoplasmic ABCF2 expression was detected by immunohistochemical staining. All patients underwent platinum-based primary chemotherapy followed by primary surgery.
    Results: Adenosine triphosphate-binding cassette superfamily F2 expression was detected in 118 (71.5%) of 165 patients and was not related to age or clinical stage. The response rate to chemotherapy in 38 patients with measurable disease was 47.3% (18/38). The response rate tended to be higher in patients without ABCF2 expression than in those with ABCF2 expression; however, this difference was not significant (66.7% vs 34.8%, P = 0.096). There was no significant difference in overall survival between ABCF2-positive and ABCF2-negative cases (median survival time, 1175 vs 1257 days; P = 0.24).
    Conclusions: Adenosine triphosphate-binding cassette superfamily F2 protein was highly expressed in CCC of the ovary, but expression was not related to age, clinical stage, chemoresponse, or prognosis.

    DOI: 10.1111/IGC.0b013e3181a835fc

    Web of Science

    researchmap

  • 家族性乳癌・遺伝性乳癌の現状と課題 遺伝相談外来を受診したBRCA1/2遺伝子変異を有する遺伝性乳がん卵巣がん家系の臨床遺伝学的特徴

    菅野 康吉, 牧島 恵子, 友田 茉莉, 安藤 二郎, 矢崎 久妙子, 武田 祐子, 平澤 晃, 神野 浩光, 北川 雄光, 和泉 秀子, 古賀 範子, 木下 貴之

    日本乳癌学会総会プログラム抄録集   18回   260 - 260   2010.5

     More details

    Language:Japanese   Publisher:(一社)日本乳癌学会  

    researchmap

  • 月経関連片頭痛に対する呉茱萸湯の周期的投与の試み.

    牧田和也, 堀場裕子, 平沢 晃, 青木大輔, 吉村泰典

    産婦人科漢方研究のあゆみ   27 ( 27 )   73-75 - 75   2010

     More details

    Language:Japanese  

    researchmap

  • ファーマコゲノミクスの臨床応用を目指した簡易迅速な遺伝子多型診断システムの開発.

    平沢 晃

    臨床薬理   41 ( 3 )   109-110 - 110S   2010

     More details

    Language:Japanese  

    DOI: 10.3999/jscpt.41.109S

    researchmap

  • 両側卵巣摘出術施行例における骨代謝関連遺伝子多型の探索-性ホルモン代謝関連酵素遺伝子におけるコピー数多型の検索を中心として-

    平沢 晃, 赤羽智子, 牧田和也, 青木大輔

    Osteoporosis Japan   18 ( 3 )   406-408 - 408   2010

  • 閉経前両側卵巣摘出例における骨密度とFRAXの特徴に関する検討.

    堀場裕子, 平沢 晃, 牧田和也, 松村聡子, 小川真里子, 岩田 卓, 弟子丸亮太, 柳本茂久, 青木大輔

    Osteoporosis Japan   18 ( 3 )   461-465 - 465   2010

  • ゲノム薬理学の最近の親展とUGT1A1遺伝子多型診断について

    AOKI DAISUKE

    産婦人科の実際   58 ( 12 )   2005-2011 - 2011   2009.11

     More details

    Language:Japanese  

    researchmap

  • 私はこうしている:私の主張 週1回のビスフォスフォネート製剤の投与

    AOKI DAISUKE

    産婦人科治療   99 ( 5 )   509-511 - 511   2009.11

  • Analysis of candidate target genes for mononucleotide repeat mutation in microsatellite instability-high (MSI-H) endometrial cancer

    Makiko Kawaguchi, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Arisa Kishimi, Seiji Ogawa, Iori Kisu, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   35 ( 5 )   977 - 982   2009.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Microsatellite instability (MSI) is an indicator of DNA instability and is caused by abnormalities in DNA mismatch repair (MMR) genes such as hMLH1, hMSH2 and hMSH6. MSI occurs frequently in endometrial cancer (in approximately 30% of cases), and accumulation of gene mutations due to MSI may therefore have a major role in the mechanism of malignant transformation. However, a responsible target gene has not been identified in endometrial cancer. In this study, we analyzed mutations in 11 cancer-related genes with mononucleotide repeats susceptible to MST in a coding region [hMSH3 (A8), hMSH6 (C8), TGF-beta RII (A10), MBD4 (A10), BAX (G8), PTEN (A6 in exon 7), HDAC2 (A9), EPHB2 (A9), Caspase-5 (A10), TCF-4 (A9) and Axin2 (G7)] in 22 patients with MSI-H sporadic endometrial cancer. Mutations in hMSH6 (C8) and TGF-beta RII (A10) were found most frequently, at rates of 36.3% (8/22) each. Mutations of BAX (G8) and TCF-4 (A9), which are common in MSI-positive colorectal cancer, occurred at rates of 22.7 and 0%, respectively, which suggests that the MSI target gene may differ between endometrial and colorectal cancers. Mutations in hMSH6 (C8) were correlated with reduced protein expression (p=0.042) and patients with these mutations had significantly more mutations in mononucleotide repeats in other cancer-related genes compared to patients without hMSH6 (C8) mutations (p=0.042). This suggests the possibility of a novel cascade in carcinogenesis of endometrial cancer in which MST mutates hMSH6 (C8), increases gene instability, and leads to accumulation of mutations in other cancer-related genes. To our knowledge, this is the first report to show that hMSH6 (C8) has an important role as an MSI target gene in sporadic endometrial cancer.

    DOI: 10.3892/ijo_00000411

    Web of Science

    researchmap

  • Epigenetic DNA hypermethylation: Clinical applications in endometrial cancer (Review) Reviewed

    Yuriko Muraki, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Makiko Kawaguchi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    ONCOLOGY REPORTS   22 ( 5 )   967 - 972   2009.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Improvements in epigenetics have resulted in identification of a number of genes with aberrant hypermethylation associated with systematic occurrence of cancer. It is now evident that aberrant hypermethylation inactivates cancer-related genes including those associated with cell cycle control, apoptosis, and DNA repair. An epigenetic analysis of DNA hypermethylation in type I endometrial cancer has led to a proposed mechanism for endometrial carcinogenesis. Reduced DNA mismatch repair due to loss of hMLH1expression is thought to have a major role in carcinogenesis and these findings open up approaches to prevention, diagnosis, risk assessment, and treatment of type I endometrial cancer. Aberrant DNA hypermethylation can be detected with high sensitivity for identification of cancer cells in sputum, blood and other biopsy materials, including in endometrial cancer specimens. There have been many attempts to use methylation inhibitors as anticancer agents, and epigenetic abnormalities may be useful as biomarkers of anticancer drug sensitivity and to identify biological characteristics of tumor cells for determination of treatment options based on hypermethylation. For example, aberrant hypermethylation of the CHFR gene is correlated with cellular sensitivity to microtubule inhibitors, and this may be useful in treatment of type I endometrial cancer. An ultimate objective of epigenetics is to identify the type of hereditary methylation responsible for cancer, with the goal of improved diagnosis and treatment based on control of methylation.

    DOI: 10.3892/or_00000523

    Web of Science

    researchmap

  • Analysis of candidate target genes for mononucleotide repeat mutation in microsatellite instability-high (MSI-H) endometrial cancer Reviewed

    Makiko Kawaguchi, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Arisa Kishimi, Seiji Ogawa, Iori Kisu, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   35 ( 5 )   977 - 982   2009.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Microsatellite instability (MSI) is an indicator of DNA instability and is caused by abnormalities in DNA mismatch repair (MMR) genes such as hMLH1, hMSH2 and hMSH6. MSI occurs frequently in endometrial cancer (in approximately 30% of cases), and accumulation of gene mutations due to MSI may therefore have a major role in the mechanism of malignant transformation. However, a responsible target gene has not been identified in endometrial cancer. In this study, we analyzed mutations in 11 cancer-related genes with mononucleotide repeats susceptible to MST in a coding region [hMSH3 (A8), hMSH6 (C8), TGF-beta RII (A10), MBD4 (A10), BAX (G8), PTEN (A6 in exon 7), HDAC2 (A9), EPHB2 (A9), Caspase-5 (A10), TCF-4 (A9) and Axin2 (G7)] in 22 patients with MSI-H sporadic endometrial cancer. Mutations in hMSH6 (C8) and TGF-beta RII (A10) were found most frequently, at rates of 36.3% (8/22) each. Mutations of BAX (G8) and TCF-4 (A9), which are common in MSI-positive colorectal cancer, occurred at rates of 22.7 and 0%, respectively, which suggests that the MSI target gene may differ between endometrial and colorectal cancers. Mutations in hMSH6 (C8) were correlated with reduced protein expression (p=0.042) and patients with these mutations had significantly more mutations in mononucleotide repeats in other cancer-related genes compared to patients without hMSH6 (C8) mutations (p=0.042). This suggests the possibility of a novel cascade in carcinogenesis of endometrial cancer in which MST mutates hMSH6 (C8), increases gene instability, and leads to accumulation of mutations in other cancer-related genes. To our knowledge, this is the first report to show that hMSH6 (C8) has an important role as an MSI target gene in sporadic endometrial cancer.

    DOI: 10.3892/ijo_00000411

    Web of Science

    researchmap

  • Analysis of candidate target genes for mononucleotide repeat mutation in microsatellite instability-high (MSI-H) endometrial cancer. International journal

    Makiko Kawaguchi, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Arisa Kishimi, Seiji Ogawa, Iori Kisu, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    International journal of oncology   35 ( 5 )   977 - 82   2009.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Microsatellite instability (MSI) is an indicator of DNA instability and is caused by abnormalities in DNA mismatch repair (MMR) genes such as hMLH1, hMSH2 and hMSH6. MSI occurs frequently in endometrial cancer (in approximately 30% of cases), and accumulation of gene mutations due to MSI may therefore have a major role in the mechanism of malignant transformation. However, a responsible target gene has not been identified in endometrial cancer. In this study, we analyzed mutations in 11 cancer-related genes with mononucleotide repeats susceptible to MSI in a coding region [hMSH3 (A8), hMSH6 (C8), TGF-beta RII (A10), MBD4 (A10), BAX (G8), PTEN (A6 in exon 7), HDAC2 (A9), EPHB2 (A9), Caspase-5 (A10), TCF-4 (A9) and Axin2 (G7)] in 22 patients with MSI-H sporadic endometrial cancer. Mutations in hMSH6 (C8) and TGF-beta RII (A10) were found most frequently, at rates of 36.3% (8/22) each. Mutations of BAX (G8) and TCF-4 (A9), which are common in MSI-positive colorectal cancer, occurred at rates of 22.7 and 0%, respectively, which suggests that the MSI target gene may differ between endometrial and colorectal cancers. Mutations in hMSH6 (C8) were correlated with reduced protein expression (p=0.042) and patients with these mutations had significantly more mutations in mononucleotide repeats in other cancer-related genes compared to patients without hMSH6 (C8) mutations (p=0.042). This suggests the possibility of a novel cascade in carcinogenesis of endometrial cancer in which MSI mutates hMSH6 (C8), increases gene instability, and leads to accumulation of mutations in other cancer-related genes. To our knowledge, this is the first report to show that hMSH6 (C8) has an important role as an MSI target gene in sporadic endometrial cancer.

    DOI: 10.3892/ijo_00000411

    Web of Science

    PubMed

    researchmap

  • Epigenetic DNA hypermethylation: Clinical applications in endometrial cancer (Review)

    Yuriko Muraki, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Makiko Kawaguchi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    ONCOLOGY REPORTS   22 ( 5 )   967 - 972   2009.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Improvements in epigenetics have resulted in identification of a number of genes with aberrant hypermethylation associated with systematic occurrence of cancer. It is now evident that aberrant hypermethylation inactivates cancer-related genes including those associated with cell cycle control, apoptosis, and DNA repair. An epigenetic analysis of DNA hypermethylation in type I endometrial cancer has led to a proposed mechanism for endometrial carcinogenesis. Reduced DNA mismatch repair due to loss of hMLH1expression is thought to have a major role in carcinogenesis and these findings open up approaches to prevention, diagnosis, risk assessment, and treatment of type I endometrial cancer. Aberrant DNA hypermethylation can be detected with high sensitivity for identification of cancer cells in sputum, blood and other biopsy materials, including in endometrial cancer specimens. There have been many attempts to use methylation inhibitors as anticancer agents, and epigenetic abnormalities may be useful as biomarkers of anticancer drug sensitivity and to identify biological characteristics of tumor cells for determination of treatment options based on hypermethylation. For example, aberrant hypermethylation of the CHFR gene is correlated with cellular sensitivity to microtubule inhibitors, and this may be useful in treatment of type I endometrial cancer. An ultimate objective of epigenetics is to identify the type of hereditary methylation responsible for cancer, with the goal of improved diagnosis and treatment based on control of methylation.

    DOI: 10.3892/or_00000523

    Web of Science

    researchmap

  • Epigenetic DNA hypermethylation: clinical applications in endometrial cancer (Review). International journal

    Yuriko Muraki, Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Makiko Kawaguchi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    Oncology reports   22 ( 5 )   967 - 72   2009.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Improvements in epigenetics have resulted in identification of a number of genes with aberrant hypermethylation associated with systematic occurrence of cancer. It is now evident that aberrant hypermethylation inactivates cancer-related genes including those associated with cell cycle control, apoptosis, and DNA repair. An epigenetic analysis of DNA hypermethylation in type I endometrial cancer has led to a proposed mechanism for endometrial carcinogenesis. Reduced DNA mismatch repair due to loss of hMLH1 expression is thought to have a major role in carcinogenesis and these findings open up approaches to prevention, diagnosis, risk assessment, and treatment of type I endometrial cancer. Aberrant DNA hypermethylation can be detected with high sensitivity for identification of cancer cells in sputum, blood and other biopsy materials, including in endometrial cancer specimens. There have been many attempts to use methylation inhibitors as anticancer agents, and epigenetic abnormalities may be useful as biomarkers of anticancer drug sensitivity and to identify biological characteristics of tumor cells for determination of treatment options based on hypermethylation. For example, aberrant hypermethylation of the CHFR gene is correlated with cellular sensitivity to microtubule inhibitors, and this may be useful in treatment of type I endometrial cancer. An ultimate objective of epigenetics is to identify the type of hereditary methylation responsible for cancer, with the goal of improved diagnosis and treatment based on control of methylation.

    DOI: 10.3892/or_00000523

    Web of Science

    PubMed

    researchmap

  • ファーマコゲノミクスの現状と課題 ファーマコゲノミクスの臨床応用を目指した簡易迅速な遺伝子多型診断システムの開発

    平沢 晃, 松村 聡子, 鶴田 智彦, 赤羽 智子, 野村 弘行, 青木 大輔, 谷川原 祐介, 杉田 哲佳, 緒方 是嗣, 花房 信博

    臨床薬理   40 ( Suppl. )   S138 - S138   2009.11

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • 当科更年期外来受診患者における動脈硬化性疾患の危険因子に関する検討

    柳本 茂久, 牧田 和也, 堀場 裕子, 平沢 晃, 田島 博人, 金田 佳史, 伊藤 仁彦, 高松 潔, 青木 大輔

    日本更年期医学会雑誌   17 ( Suppl. )   113 - 113   2009.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 子宮傍結合織炎

    AOKI DAISUKE

    日本臨床(子宮疾患・子宮内膜症の臨床-基礎・臨床研究のアップデート)   67 ( 増刊号5 )   327-330   2009.8

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • イリノテカン

    AOKI DAISUKE

    小児科   50 ( 7 )   1227-1232   2009.6

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 中高年女性と片頭痛

    AOKI DAISUKE

    産婦人科治療   98 ( 6 )   971-975 - 975   2009.6

  • Analysis of a correlation between the BRAF V600E mutation and abnormal DNA mismatch repair in patients with sporadic endometrial cancer. International journal

    Makiko Kawaguchi, Megumi Yanokura, Kouji Banno, Yusuke Kobayashi, Yoshiko Kuwabara, Maya Kobayashi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    International journal of oncology   34 ( 6 )   1541 - 7   2009.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Point mutations of KRAS and BRAF genes are thought to be important in carcinogenesis of colon cancer. In particular, gene instability caused by decreased expression of the hMLH1 gene, a DNA mismatch repair (MMR) gene, may be linked to the activating BRAF V600E point mutation in sporadic colon cancer. However, a consensus has not been established regarding the correlation between point mutations of KRAS or BRAF and carcinogenesis in patients with endometrial cancer, which is closely related to colon cancer. Therefore, we analyzed aberrant hypermethylation of the hMLH1 gene, microsatellite instability (MSI), and point mutations of KRAS and BRAF in 44 samples of sporadic endo-metrial cancer, with the aim of examining the mechanism of carcinogenesis in patients with endometrial cancer. Aberrant hMLH1 hypermethylation was found in 17 of the 44 cases (38.6%) and showed a significant positive correlation with MSI (p=0.02). This suggests that an abnormal MMR mechanism plays an important role in carcinogenesis of sporadic endometrial cancer. Point mutation of KRAS was found in 6 of the 44 cases (13.6%), but no BRAF V600E mutation was detected. These data suggest that the BRAF V600E mutation is not the target gene for abnormal MMR in carcinogenesis in patients with sporadic endometrial cancer, unlike in colon cancer. This is supported by the relatively few previous reports indicating a correlation between endometrial cancer and the BRAF V600E mutation. Identification of new candidates for the target gene for abnormal MMR in endometrial cancer requires further work.

    DOI: 10.3892/ijo_00000283

    Web of Science

    PubMed

    researchmap

  • Analysis of a correlation between the BRAF V600E mutation and abnormal DNA mismatch repair in patients with sporadic endometrial cancer

    Makiko Kawaguchi, Megumi Yanokura, Kouji Banno, Yusuke Kobayashi, Yoshiko Kuwabara, Maya Kobayashi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Datsuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   34 ( 6 )   1541 - 1547   2009.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Point mutations of KRAS and BRAF genes are thought to be important in carcinogenesis of colon cancer. In particular, gene instability caused by decreased expression of the hMLH1 gene, a DNA mismatch repair (MMR) gene, may be linked to the activating BRAF V600E point mutation in sporadic colon cancer. However, a consensus has not been established regarding the correlation between point mutations of KRAS or BRAF and carcinogenesis in patients with endometrial cancer, which is closely related to colon cancer. Therefore, we analyzed aberrant hypermethylation of the hMLH1 gene, microsatellite instability (MSI), and point mutations of KRAS and BRAF in 44 samples of sporadic endometrial cancer, with the aim of examining the mechanism of carcinogenesis in patients with endometrial cancer. Aberrant hMLH1 hypermethylation was found in 17 of the 44 cases (38.6%) and showed a significant positive correlation with MSI (p=0.02). This suggests that an abnormal MMR mechanism plays an important role in carcinogenesis of sporadic endometrial cancer. Point mutation of KRAS was found in 6 of the 44 cases (13.6%), but no BRAF V600E mutation was detected. These data suggest that the BRAF V600E mutation is not the target gene for abnormal MMR in carcinogenesis in patients with sporadic endometrial cancer, unlike in colon cancer. This is supported by the relatively few previous reports indicating a correlation between endometrial cancer and the BRAF V600E mutation. Identification of new candidates for the target gene for abnormal MMR in endometrial cancer requires further work.

    DOI: 10.3892/ijo_00000283

    Web of Science

    researchmap

  • Analysis of a correlation between the BRAF V600E mutation and abnormal DNA mismatch repair in patients with sporadic endometrial cancer

    Makiko Kawaguchi, Megumi Yanokura, Kouji Banno, Yusuke Kobayashi, Yoshiko Kuwabara, Maya Kobayashi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Datsuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   34 ( 6 )   1541 - 1547   2009.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:SPANDIDOS PUBL LTD  

    Point mutations of KRAS and BRAF genes are thought to be important in carcinogenesis of colon cancer. In particular, gene instability caused by decreased expression of the hMLH1 gene, a DNA mismatch repair (MMR) gene, may be linked to the activating BRAF V600E point mutation in sporadic colon cancer. However, a consensus has not been established regarding the correlation between point mutations of KRAS or BRAF and carcinogenesis in patients with endometrial cancer, which is closely related to colon cancer. Therefore, we analyzed aberrant hypermethylation of the hMLH1 gene, microsatellite instability (MSI), and point mutations of KRAS and BRAF in 44 samples of sporadic endometrial cancer, with the aim of examining the mechanism of carcinogenesis in patients with endometrial cancer. Aberrant hMLH1 hypermethylation was found in 17 of the 44 cases (38.6%) and showed a significant positive correlation with MSI (p=0.02). This suggests that an abnormal MMR mechanism plays an important role in carcinogenesis of sporadic endometrial cancer. Point mutation of KRAS was found in 6 of the 44 cases (13.6%), but no BRAF V600E mutation was detected. These data suggest that the BRAF V600E mutation is not the target gene for abnormal MMR in carcinogenesis in patients with sporadic endometrial cancer, unlike in colon cancer. This is supported by the relatively few previous reports indicating a correlation between endometrial cancer and the BRAF V600E mutation. Identification of new candidates for the target gene for abnormal MMR in endometrial cancer requires further work.

    DOI: 10.3892/ijo_00000283

    Web of Science

    researchmap

  • Endometrial cancer as HNPCC associated tumor

    Kouji Banno, Yusuke Kobayashi, Megumi Yanokura, Arisa Kishimi, Seiji Ogawa, Iori Kisu, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    家族性腫瘍   9 ( 2 )   64-68   2009.5

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • Endometrial Cancer as a Familial Tumor: Pathology and Molecular Carcinogenesis (Review) Reviewed

    Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Makiko Kawaguchi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    CURRENT GENOMICS   10 ( 2 )   127 - 132   2009.4

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BENTHAM SCIENCE PUBL LTD  

    Some cases of endometrial cancer are associated with a familial tumor and are referred to as hereditary nonpolyposis colorectal cancer (HNPCC or Lynch syndrome). Such tumors are thought to be induced by germline mutation of the DNA mismatch repair (MMR) gene, but many aspects of the pathology of familial endometrial cancer are unclear and no effective screening method has been established. However, the pathology of endometrial cancer with familial tumor has been progressively clarified in recent studies. At present, about 0.5% of all cases of endometrial cancers meet the clinical diagnostic criteria for HNPCC. A recent analysis of the three MMR genes (hMLH1, hMSH2 and hMSH6) revealed germline mutations in 18 of 120 cases (15.0%) of endometrial cancer with familial accumulation of cancer or double cancer, with a frameshift mutation of the hMSH6 gene being the most common. Many cases with mutation did not meet the current clinical diagnostic criteria for HNPCC, indicating that familial endometrial cancer is often not diagnosed as HNPCC. The results suggest that the hMSH6 gene mutation may be important in carcinogenesis in endometrial cancer and germline mutations of the MMR gene may be more prevalent in cases associated with familial accumulation of cancer. An international large-scale muticenter study is required to obtain further information about the pathology of endometrial cancer as a familial tumor.

    DOI: 10.2174/138920209787847069

    Web of Science

    researchmap

  • Endometrial Cancer as a Familial Tumor: Pathology and Molecular Carcinogenesis (Review) Reviewed

    Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Makiko Kawaguchi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    CURRENT GENOMICS   10 ( 2 )   127 - 132   2009.4

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BENTHAM SCIENCE PUBL LTD  

    Some cases of endometrial cancer are associated with a familial tumor and are referred to as hereditary nonpolyposis colorectal cancer (HNPCC or Lynch syndrome). Such tumors are thought to be induced by germline mutation of the DNA mismatch repair (MMR) gene, but many aspects of the pathology of familial endometrial cancer are unclear and no effective screening method has been established. However, the pathology of endometrial cancer with familial tumor has been progressively clarified in recent studies. At present, about 0.5% of all cases of endometrial cancers meet the clinical diagnostic criteria for HNPCC. A recent analysis of the three MMR genes (hMLH1, hMSH2 and hMSH6) revealed germline mutations in 18 of 120 cases (15.0%) of endometrial cancer with familial accumulation of cancer or double cancer, with a frameshift mutation of the hMSH6 gene being the most common. Many cases with mutation did not meet the current clinical diagnostic criteria for HNPCC, indicating that familial endometrial cancer is often not diagnosed as HNPCC. The results suggest that the hMSH6 gene mutation may be important in carcinogenesis in endometrial cancer and germline mutations of the MMR gene may be more prevalent in cases associated with familial accumulation of cancer. An international large-scale muticenter study is required to obtain further information about the pathology of endometrial cancer as a familial tumor.

    DOI: 10.2174/138920209787847069

    Web of Science

    researchmap

  • 結合型エストロゲン製剤を用いたホルモン補充療法の腰椎骨密度に対する長期的な効果の検討 ~当科更年期外来における継続投与10年例の結果から~

    AOKI DAISUKE

    Osteoporosis Japan   17 ( 2 )   329-330 - 330   2009.4

     More details

    Language:Japanese  

    researchmap

  • Endometrial cancer as a familial tumor: pathology and molecular carcinogenesis (review). International journal

    Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Makiko Kawaguchi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    Current genomics   10 ( 2 )   127 - 32   2009.4

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Some cases of endometrial cancer are associated with a familial tumor and are referred to as hereditary nonpolyposis colorectal cancer (HNPCC or Lynch syndrome). Such tumors are thought to be induced by germline mutation of the DNA mismatch repair (MMR) gene, but many aspects of the pathology of familial endometrial cancer are unclear and no effective screening method has been established. However, the pathology of endometrial cancer with familial tumor has been progressively clarified in recent studies. At present, about 0.5% of all cases of endometrial cancers meet the clinical diagnostic criteria for HNPCC. A recent analysis of the three MMR genes (hMLH1, hMSH2 and hMSH6) revealed germline mutations in 18 of 120 cases (15.0%) of endometrial cancer with familial accumulation of cancer or double cancer, with a frameshift mutation of the hMSH6 gene being the most common. Many cases with mutation did not meet the current clinical diagnostic criteria for HNPCC, indicating that familial endometrial cancer is often not diagnosed as HNPCC. The results suggest that the hMSH6 gene mutation may be important in carcinogenesis in endometrial cancer and germline mutations of the MMR gene may be more prevalent in cases associated with familial accumulation of cancer. An international large-scale muticenter study is required to obtain further information about the pathology of endometrial cancer as a familial tumor.

    DOI: 10.2174/138920209787847069

    Scopus

    PubMed

    researchmap

  • 当科更年期外来における更年期不定愁訴に対する漢方薬の使用状況について-8年前の調査結果との比較検討-.

    牧田和也, 堀場 裕子, 平沢 晃, 岩田卓, 片岡史夫, 冨永英一郎, 堀口文, 青木大輔, 吉村泰典

    産婦人科漢方研究のあゆみ   26 ( 26 )   44-47 - 47   2009

     More details

    Language:Japanese  

    researchmap

  • 更年期外来受診患者における動脈硬化性疾患の危険因子に関する検討.

    柳本茂久, 牧田和也, 堀場裕子, 平沢 晃, 高松 潔, 堀口 文, 青木大輔

    日本更年期医学会雑誌   17 ( 2 )   171-178 - 178   2009

     More details

    Language:Japanese  

    researchmap

  • Endometrial cancer as a familial tumor: Pathology and molecular carcinogenesis (review)

    Kouji Banno, Megumi Yanokura, Yusuke Kobayashi, Makiko Kawaguchi, Hiroyuki Nomura, Akira Hirasawa, Nobuyuki Susumu, Daisuke Aoki

    Current Genomics   10 ( 2 )   127 - 132   2009

     More details

    Language:English  

    Some cases of endometrial cancer are associated with a familial tumor and are referred to as hereditary nonpolyposis colorectal cancer (HNPCC or Lynch syndrome). Such tumors are thought to be induced by germline mutation of the DNA mismatch repair (MMR) gene, but many aspects of the pathology of familial endometrial cancer are unclear and no effective screening method has been established. However, the pathology of endometrial cancer with familial tumor has been progressively clarified in recent studies. At present, about 0.5% of all cases of endometrial cancers meet the clinical diagnostic criteria for HNPCC. A recent analysis of the three MMR genes (hMLH1, hMSH2 and hMSH6) revealed germline mutations in 18 of 120 cases (15.0%) of endometrial cancer with familial accumulation of cancer or double cancer, with a frameshift mutation of the hMSH6 gene being the most common. Many cases with mutation did not meet the current clinical diagnostic criteria for HNPCC, indicating that familial endometrial cancer is often not diagnosed as HNPCC. The results suggest that the hMSH6 gene mutation may be important in carcinogenesis in endometrial cancer and germline mutations of the MMR gene may be more prevalent in cases associated with familial accumulation of cancer. An international large-scale muticenter study is required to obtain further information about the pathology of endometrial cancer as a familial tumor. © 2009 Bentham Science Publishers Ltd.

    DOI: 10.2174/138920209787847069

    Scopus

    researchmap

  • 閉経後骨粗鬆症に対する予防的治療を行う際の薬剤選択に関する再検証.

    牧田和也, 平沢 晃, 堀場 裕子, 弟子丸亮太, 柳本茂久, 堀口 文, 青木大輔

    Osteoporosis Japan   17 ( 3 )   447-449 - 449   2009

  • 子宮体がん例におけるFRAXを用いた骨折リスク評価.

    平沢 晃, 牧田和也, 堀場 裕子, 弟子丸亮太, 柳本茂久, 阪埜浩司, 進 伸幸, 青木大輔

    Osteoporosis Japan   17 ( 3 )   492-495 - 495   2009

  • 当科更年期外来における塩酸ラロキシフェン治療の現況-子宮体癌術後症例を中心に-.

    牧田和也, 堀場裕子, 岩田 卓, 平沢 晃, 片岡史夫, 富永英一郎, 堀口 文, 青木大輔

    SERM   7   106-107   2009

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • Can ABCF2 protein expression predict the prognosis of uterine cancer? Reviewed

    S. Nishimura, H. Tsuda, Y. Miyagi, A. Hirasawa, A. Suzuki, F. Kataoka, H. Nomura, T. Chiyoda, K. Banno, T. Fujii, N. Susumu, D. Aoki

    BRITISH JOURNAL OF CANCER   99 ( 10 )   1651 - 1655   2008.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    Uterine cervical and endometrial cancers are common malignant solid neoplasms for which there are no useful prognostic markers. In this study, we evaluate the relationship between ATP-binding cassette superfamily F2 (ABCF2) expression and clinical factors including clinical stage, histologic type, grade and prognosis in uterine cervical and endometrial cancer. Two hundred and sixty seven cervical and 103 endometrial cancers were studied. ATP-binding cassette superfamily F2 cytoplasmic expression was detected by immunohistochemical staining and scored as positive or negative. Among cervical cancer cases, 149 (55.8%) expressed ABCF2. The overall survival was longer in ABCF2-negative than ABCF2-positive cases (P=0.0069). Statistically significant prognostic factors for survival were ABCF2 positivity ( risk ratio (rr) = 1.437), old age (rr = 1.550) and advanced stage (rr = 2.577). ATP-binding cassette superfamily F2 positivity was an independent prognostic factor by multivariate proportional hazard test (P=0.0002). Among endometrial cancer cases, 72 (69.9%) were cytoplasmic ABCF2 positive. However, there was no significant relationship between ABCF2 expression and age, clinical stage, histologic type, histologic grade, oestrogen receptor status or prognosis. ATP-binding cassette superfamily F2 expression may be a useful prognostic marker in cervical but not endometrial cancer. The role of ABCF2 protein may differ depending on the type of cancer.

    DOI: 10.1038/sj.bjc.6604734

    Web of Science

    researchmap

  • Can ABCF2 protein expression predict the prognosis of uterine cancer?

    S. Nishimura, H. Tsuda, Y. Miyagi, A. Hirasawa, A. Suzuki, F. Kataoka, H. Nomura, T. Chiyoda, K. Banno, T. Fujii, N. Susumu, D. Aoki

    BRITISH JOURNAL OF CANCER   99 ( 10 )   1651 - 1655   2008.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    Uterine cervical and endometrial cancers are common malignant solid neoplasms for which there are no useful prognostic markers. In this study, we evaluate the relationship between ATP-binding cassette superfamily F2 (ABCF2) expression and clinical factors including clinical stage, histologic type, grade and prognosis in uterine cervical and endometrial cancer. Two hundred and sixty seven cervical and 103 endometrial cancers were studied. ATP-binding cassette superfamily F2 cytoplasmic expression was detected by immunohistochemical staining and scored as positive or negative. Among cervical cancer cases, 149 (55.8%) expressed ABCF2. The overall survival was longer in ABCF2-negative than ABCF2-positive cases (P=0.0069). Statistically significant prognostic factors for survival were ABCF2 positivity ( risk ratio (rr) = 1.437), old age (rr = 1.550) and advanced stage (rr = 2.577). ATP-binding cassette superfamily F2 positivity was an independent prognostic factor by multivariate proportional hazard test (P=0.0002). Among endometrial cancer cases, 72 (69.9%) were cytoplasmic ABCF2 positive. However, there was no significant relationship between ABCF2 expression and age, clinical stage, histologic type, histologic grade, oestrogen receptor status or prognosis. ATP-binding cassette superfamily F2 expression may be a useful prognostic marker in cervical but not endometrial cancer. The role of ABCF2 protein may differ depending on the type of cancer.

    DOI: 10.1038/sj.bjc.6604734

    Web of Science

    researchmap

  • Can ABCF2 protein expression predict the prognosis of uterine cancer?

    S. Nishimura, H. Tsuda, Y. Miyagi, A. Hirasawa, A. Suzuki, F. Kataoka, H. Nomura, T. Chiyoda, K. Banno, T. Fujii, N. Susumu, D. Aoki

    BRITISH JOURNAL OF CANCER   99 ( 10 )   1651 - 1655   2008.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    Uterine cervical and endometrial cancers are common malignant solid neoplasms for which there are no useful prognostic markers. In this study, we evaluate the relationship between ATP-binding cassette superfamily F2 (ABCF2) expression and clinical factors including clinical stage, histologic type, grade and prognosis in uterine cervical and endometrial cancer. Two hundred and sixty seven cervical and 103 endometrial cancers were studied. ATP-binding cassette superfamily F2 cytoplasmic expression was detected by immunohistochemical staining and scored as positive or negative. Among cervical cancer cases, 149 (55.8%) expressed ABCF2. The overall survival was longer in ABCF2-negative than ABCF2-positive cases (P=0.0069). Statistically significant prognostic factors for survival were ABCF2 positivity ( risk ratio (rr) = 1.437), old age (rr = 1.550) and advanced stage (rr = 2.577). ATP-binding cassette superfamily F2 positivity was an independent prognostic factor by multivariate proportional hazard test (P=0.0002). Among endometrial cancer cases, 72 (69.9%) were cytoplasmic ABCF2 positive. However, there was no significant relationship between ABCF2 expression and age, clinical stage, histologic type, histologic grade, oestrogen receptor status or prognosis. ATP-binding cassette superfamily F2 expression may be a useful prognostic marker in cervical but not endometrial cancer. The role of ABCF2 protein may differ depending on the type of cancer.

    DOI: 10.1038/sj.bjc.6604734

    Web of Science

    researchmap

  • 子宮がん患者へのインフォームドコンセント(IC)

    AOKI DAISUKE

    臨床腫瘍プラクティス   4 ( 4 )   313-319 - 319   2008.11

     More details

    Language:Japanese  

    researchmap

  • Cross-sectional analysis of germline BRCA1 and BRCA2 mutations in Japanese patients suspected to have hereditary breast/ovarian cancer. Reviewed International journal

    Kokichi Sugano, Seigo Nakamura, Jiro Ando, Shin Takayama, Hiroyuki Kamata, Isao Sekiguchi, Megumi Ubukata, Tetsuro Kodama, Masami Arai, Fujio Kasumi, Yasuo Hirai, Tadashi Ikeda, Hiromitsu Jinno, Masaki Kitajima, Daisuke Aoki, Akira Hirasawa, Yuko Takeda, Kumiko Yazaki, Takashi Fukutomi, Takayuki Kinoshita, Ryuichiro Tsunematsu, Teruhiko Yoshida, Masako Izumi, Shino Umezawa, Hiroshi Yagata, Hiroko Komatsu, Naoko Arimori, Noriko Matoba, Nobuhisa Gondo, Shiro Yokoyama, Yoshio Miki

    Cancer science   99 ( 10 )   1967 - 76   2008.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY-BLACKWELL  

    The prevalence of BRCA1/2 germline mutations in Japanese patients suspected to have hereditary breast/ovarian cancer was examined by a multi-institutional study, aiming at the clinical application of total sequencing analysis and validation of assay sensitivity in Japanese people using a cross-sectional approach based on genetic factors estimated from personal and family histories. One hundred and thirty-five subjects were referred to the genetic counseling clinics and enrolled in the study. Full sequencing analysis of the BRCA1/2 gene showed 28 types of deleterious mutations in 36 subjects (26.7%), including 13 types of BRCA1 mutations in 17 subjects (12.6%) and 15 types of BRCA2 mutations in 19 subjects (14.1%). Subjects were classified into five groups and 22 subgroups according to their personal and family history of breast and/or ovarian cancer, and the prevalence of deleterious mutations was compared with previously reported data in non-Ashkenazi individuals. Statistical analysis using the Mantel-Haenszel test for groups I through IV revealed that the prevalence of Japanese subjects was significantly higher than that of non-Ashkenazi individuals (P = 0.005, odds ratio 1.87, 95% confidence interval 1.22-2.88). Family history of the probands suffering from breast cancer indicated risk factors for the presence of deleterious mutations of BRCA1/2 as follows: (1) families with breast cancer before age 40 within second degree relatives (P = 0.0265, odds ratio 2.833, 95% confidence interval 1.165-7.136) and (2) families with bilateral breast cancer and/or ovarian cancer within second degree relatives (P = 0.0151, odds ratio 2.88, 95% confidence interval 1.25-6.64).

    DOI: 10.1111/j.1349-7006.2008.00944.x

    Web of Science

    PubMed

    researchmap

  • Cross-sectional analysis of germline BRCA1 and BRCA2 mutations in Japanese patients suspected to have hereditary breast/ovarian cancer

    Kokichi Sugano, Seigo Nakamura, Jiro Ando, Shin Takayama, Hiroyuki Kamata, Isao Sekiguchi, Megumi Ubukata, Tetsuro Kodama, Masami Arai, Fujio Kasumi, Yasuo Hirai, Tadashi Ikeda, Hiromitsu Jinno, Masaki Kitajima, Daisuke Aoki, Akira Hirasawa, Yuko Takeda, Kumiko Yazaki, Takashi Fukutomi, Takayuki Kinoshita, Ryuichiro Tsunematsu, Teruhiko Yoshida, Masako Izumi, Shino Umezawa, Hiroshi Yagata, Hiroko Komatsu, Naoko Arimori, Noriko Matoba, Nobuhisa Gondo, Shiro Yokoyama, Yoshio Miki

    CANCER SCIENCE   99 ( 10 )   1967 - 1976   2008.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:WILEY-BLACKWELL  

    The prevalence of BRCA1/2 germline mutations in Japanese patients suspected to have hereditary breast/ovarian cancer was examined by a multi-institutional study, aiming at the clinical application of total sequencing analysis and validation of assay sensitivity in Japanese people using a cross-sectional approach based on genetic factors estimated from personal and family histories. One hundred and thirty-five subjects were referred to the genetic counseling clinics and enrolled in the study. Full sequencing analysis of the BRCA1/2 gene showed 28 types of deleterious mutations in 36 subjects (26.7%), including 13 types of BRCA1 mutations in 17 subjects (12.6%) and 15 types of BRCA2 mutations in 19 subjects (14.1%). Subjects were classified into five groups and 22 subgroups according to their personal and family history of breast and/or ovarian cancer, and the prevalence of deleterious mutations was compared with previously reported data in non-Ashkenazi individuals. Statistical analysis using the Mantel-Haenszel test for groups I through IV revealed that the prevalence of Japanese subjects was significantly higher than that of non-Ashkenazi individuals (P = 0.005, odds ratio 1.87, 95% confidence interval 1.22-2.88). Family history of the probands suffering from breast cancer indicated risk factors for the presence of deleterious mutations of BRCA1/2 as follows: (1) families with breast cancer before age 40 within second degree relatives (P = 0.0265, odds ratio 2.833, 95% confidence interval 1.165-7.136) and (2) families with bilateral breast cancer and/or ovarian cancer within second degree relatives (P = 0.0151, odds ratio 2.88, 95% confidence interval 1.25-6.64). (Cancer Sci 2008; 99: 1967-1976).

    DOI: 10.1111/j.1349-7006.2008.00944.x

    Web of Science

    researchmap

  • 子宮体がん術後患者における骨密度の特徴に関する検討.

    平沢 晃, 牧田和也, 堀場 裕子, 弟子丸亮太, 柳本茂久, 野村弘行, 片岡史夫, 岩田卓, 冨永英一郎, 阪埜浩司, 進 伸幸, 堀口 文, 青木大輔

    Osteoporosis Japan   16 ( 3 )   429-431   2008

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 子宮体がん術後患者における骨密度の特徴に関する検討

    HIRASAWA AKIRA

    Osteoporosis Japan   16 ( 3 )   429-431 - 431   2008

  • 当科更年期外来にて診断し得た骨粗鬆症/骨量減少症における低エストロゲン血症以外の危険因子の検討

    HIRASAWA AKIRA

    Osteoporosis Japan   16 ( 2 )   308   2008

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 更年期外来でのアンケート調査結果からみた本邦中高年婦人の「night sweats」の実態とホルモン療法の有用性に関する一考察.

    牧田和也, 柳本茂久, 張簡珮怡, 平沢 晃, 冨永英一郎, 高松 潔, 堀口 文, 青木大輔

    日本更年期医学会雑誌   16 ( 2 )   246-251 - 251   2008

     More details

    Language:Japanese  

    researchmap

  • 季節による漢方製剤の切り替えが片頭痛発作の軽減に有効であった1例

    HIRASAWA AKIRA

    産婦人科漢方研究のあゆみ   25   115-118   2008

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 季節による漢方製剤の切り替えが片頭痛発作の軽減に有効であった1例.

    牧田和也, 平沢 晃, 冨永英一郎, 堀口 文, 青木大輔, 吉村泰典

    産婦人科漢方研究のあゆみ   25 ( 25 )   115-118 - 118   2008

     More details

    Language:Japanese  

    researchmap

  • 当科更年期外来にて診断し得た骨粗鬆症/骨量減少症における低エストロゲン血症以外の危険因子の検討.

    牧田和也, 冨永英一郎, 平沢 晃, 堀口 文, 青木大輔

    Osteoporosis Japan   16 ( 2 )   308 - 308   2008

     More details

    Language:Japanese  

    researchmap

  • 当科更年期外来受診者におけるアレンドロネート製剤のweekly投与への切り替えの現状.

    牧田和也, 平沢 晃, 冨永英一郎, 堀口 文, 青木大輔

    Osteoporosis Japan   16 ( 3 )   268-269 - 469   2008

     More details

    Language:Japanese  

    researchmap

  • Epigenetic inactivation of the CHFR gene in cervical cancer contributes to sensitivity to taxanes

    Kouji Banno, Megumi Yanokura, Makiko Kawaguchi, Yoshiko Kuwabara, Jyunko Akiyoshi, Yusuke Kobayashi, Takashi Iwata, Akira Hirasawa, Takuma Fujii, Nobuyuki Susumu, Kastumi Tsukazaki, Daisuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   31 ( 4 )   713 - 720   2007.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    A relationship between inactivation of mitotic checkpoint genes and sensitivity of cancer cells to anticancer agents has been reported. We investigated the effect of epigenetic inactivation by aberrant hypermethylation of the mitotic checkpoint gene CHFR (checkpoint with forkhead and ring finger) on the sensitivity of cervical cancer cells to taxanes. Methylation-specific PCR (MSP) of cervical smears showed aberrant methylation of CHFR in 12.3% (2/14) of adenocarcinoma specimens. In contrast, aberrant DNA methylation was not detected in normal cervical cells or squamous cell carcinoma cells. Aberrant methylation of CHFR was also analyzed in 6 human cervical carcinoma-derived cell lines and was observed in SKG-IIIb and HeLa cells. These cell lines showed high sensitivity to taxanes, but became taxane-resistant upon treatment with 5-azacytidine. Furthermore, suppression of CHFR expression in siRNA-transfected SKG-IIIa cells caused increased sensitivity to taxanes. In conclusion, aberrant methylation of the CHFR gene may be useful as a molecular marker for selection of therapy for patients with cervical adenocarcinoma with a poor prognosis, and may also suggest a new therapeutic strategy of targeting CHFR in cervical cancer. To our knowledge, this study is the first to examine epigenetic inactivation by aberrant hypermethylation of CHFR in cervical cancer.

    Web of Science

    researchmap

  • Epigenetic inactivation of the CHFR gene in cervical cancer contributes to sensitivity to taxanes Reviewed

    Kouji Banno, Megumi Yanokura, Makiko Kawaguchi, Yoshiko Kuwabara, Jyunko Akiyoshi, Yusuke Kobayashi, Takashi Iwata, Akira Hirasawa, Takuma Fujii, Nobuyuki Susumu, Kastumi Tsukazaki, Daisuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   31 ( 4 )   713 - 720   2007.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    A relationship between inactivation of mitotic checkpoint genes and sensitivity of cancer cells to anticancer agents has been reported. We investigated the effect of epigenetic inactivation by aberrant hypermethylation of the mitotic checkpoint gene CHFR (checkpoint with forkhead and ring finger) on the sensitivity of cervical cancer cells to taxanes. Methylation-specific PCR (MSP) of cervical smears showed aberrant methylation of CHFR in 12.3% (2/14) of adenocarcinoma specimens. In contrast, aberrant DNA methylation was not detected in normal cervical cells or squamous cell carcinoma cells. Aberrant methylation of CHFR was also analyzed in 6 human cervical carcinoma-derived cell lines and was observed in SKG-IIIb and HeLa cells. These cell lines showed high sensitivity to taxanes, but became taxane-resistant upon treatment with 5-azacytidine. Furthermore, suppression of CHFR expression in siRNA-transfected SKG-IIIa cells caused increased sensitivity to taxanes. In conclusion, aberrant methylation of the CHFR gene may be useful as a molecular marker for selection of therapy for patients with cervical adenocarcinoma with a poor prognosis, and may also suggest a new therapeutic strategy of targeting CHFR in cervical cancer. To our knowledge, this study is the first to examine epigenetic inactivation by aberrant hypermethylation of CHFR in cervical cancer.

    Web of Science

    researchmap

  • Epigenetic inactivation of the CHFR gene in cervical cancer contributes to sensitivity to taxanes Reviewed

    Kouji Banno, Megumi Yanokura, Makiko Kawaguchi, Yoshiko Kuwabara, Jyunko Akiyoshi, Yusuke Kobayashi, Takashi Iwata, Akira Hirasawa, Takuma Fujii, Nobuyuki Susumu, Kastumi Tsukazaki, Daisuke Aoki

    INTERNATIONAL JOURNAL OF ONCOLOGY   31 ( 4 )   713 - 720   2007.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    A relationship between inactivation of mitotic checkpoint genes and sensitivity of cancer cells to anticancer agents has been reported. We investigated the effect of epigenetic inactivation by aberrant hypermethylation of the mitotic checkpoint gene CHFR (checkpoint with forkhead and ring finger) on the sensitivity of cervical cancer cells to taxanes. Methylation-specific PCR (MSP) of cervical smears showed aberrant methylation of CHFR in 12.3% (2/14) of adenocarcinoma specimens. In contrast, aberrant DNA methylation was not detected in normal cervical cells or squamous cell carcinoma cells. Aberrant methylation of CHFR was also analyzed in 6 human cervical carcinoma-derived cell lines and was observed in SKG-IIIb and HeLa cells. These cell lines showed high sensitivity to taxanes, but became taxane-resistant upon treatment with 5-azacytidine. Furthermore, suppression of CHFR expression in siRNA-transfected SKG-IIIa cells caused increased sensitivity to taxanes. In conclusion, aberrant methylation of the CHFR gene may be useful as a molecular marker for selection of therapy for patients with cervical adenocarcinoma with a poor prognosis, and may also suggest a new therapeutic strategy of targeting CHFR in cervical cancer. To our knowledge, this study is the first to examine epigenetic inactivation by aberrant hypermethylation of CHFR in cervical cancer.

    Web of Science

    researchmap

  • Epigenetic inactivation of the CHFR gene in cervical cancer contributes to sensitivity to taxanes. International journal

    Kouji Banno, Megumi Yanokura, Makiko Kawaguchi, Yoshiko Kuwabara, Jyunko Akiyoshi, Yusuke Kobayashi, Takashi Iwata, Akira Hirasawa, Takuma Fujii, Nobuyuki Susumu, Kastumi Tsukazaki, Daisuke Aoki

    International journal of oncology   31 ( 4 )   713 - 20   2007.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    A relationship between inactivation of mitotic checkpoint genes and sensitivity of cancer cells to anticancer agents has been reported. We investigated the effect of epigenetic inactivation by aberrant hypermethylation of the mitotic checkpoint gene CHFR (checkpoint with forkhead and ring finger) on the sensitivity of cervical cancer cells to taxanes. Methylation-specific PCR (MSP) of cervical smears showed aberrant methylation of CHFR in 12.3% (2/14) of adenocarcinoma specimens. In contrast, aberrant DNA methylation was not detected in normal cervical cells or squamous cell carcinoma cells. Aberrant methylation of CHFR was also analyzed in 6 human cervical carcinoma-derived cell lines and was observed in SKG-IIIb and HeLa cells. These cell lines showed high sensitivity to taxanes, but became taxane-resistant upon treatment with 5-azacytidine. Furthermore, suppression of CHFR expression in siRNA-transfected SKG-IIIa cells caused increased sensitivity to taxanes. In conclusion, aberrant methylation of the CHFR gene may be useful as a molecular marker for selection of therapy for patients with cervical adenocarcinoma with a poor prognosis, and may also suggest a new therapeutic strategy of targeting CHFR in cervical cancer. To our knowledge, this study is the first to examine epigenetic inactivation by aberrant hypermethylation of CHFR in cervical cancer.

    Web of Science

    PubMed

    researchmap

  • 進行子宮体癌の再発・予後因子としてのCOX-2とCD8陽性リンパ球についての検討

    末盛 友浩, 進 伸幸, 鶴田 智彦, 市川 義一, 野村 弘行, 片岡 史夫, 平澤 晃, 冨永 英一郎, 阪埜 浩司, 鈴木 淳, 青木 大輔

    日本癌治療学会誌   42 ( 2 )   508 - 508   2007.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • ヒトモノクローナル抗体HMMC-1の子宮体癌細胞に対する増殖抑制効果の検討

    笈川 文子, 鈴木 淳, 冨永 英一郎, 末盛 友浩, 市川 義一, 野村 弘行, 片岡 史夫, 平澤 晃, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   46 ( Suppl.2 )   448 - 448   2007.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 卵巣明細胞腺癌におけるシアリダーゼ発現の多寡が腹膜播種形成に及ぼす影響の検討

    AOKI DAISUKE

    日本分子腫瘍マーカー研究会誌   22   39429 - 13   2007.4

  • 卵巣癌の各組織型特異的バイオマーカーに基づく診断用マイクロアレイDNAチップ作成

    鈴木 淳, 杉田 哲佳, 東口 敦史, 末盛 友浩, 市川 義一, 野村 弘行, 平澤 晃, 玉田 裕, 進 伸幸, 佐藤 孝明, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   59 ( 2 )   409 - 409   2007.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • Relationship of aberrant DNA hypermethylation of CHFR with sensitivity to taxanes in endometrial cancer Reviewed

    Megumi Yanokura, Kouji Banno, Makiko Kawaguchi, Nobumaru Hirao, Akira Hirasawa, Nobuyuki Susumu, Katsumi Tsukazaki, Daisuke Aoki

    ONCOLOGY REPORTS   17 ( 1 )   41 - 48   2007.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    The relationship of aberrant DNA hypermethylation of cell cycle checkpoint genes with the sensitivity of cancer cells to anticancer drugs is a question of current interest. In this study, we investigated the relationship between aberrant hypermethylation of the CHFR (checkpoint with forkhead-associated and ring finger) mitotic checkpoint gene and sensitivity to taxanes in endometrial cancer. Methylation-specific PCR (MSP) indicated aberrant hypermethylation of CHFR in 12.0% (6/50) of endometrial cancer specimens, and suggested that aberrant hypermethylation is significantly more frequent in poorly differentiated adenocarcinoma (G3) (p &lt; 0.05). Of six culture cell lines, SNG-II and HEC108 cells showed aberrant hypermethylation and reduced expression of CHFR. These cells had high sensitivity to taxanes but became resistant after demethylation. Cancer specimens with aberrant hypermethylation of CHFR also exhibited high sensitivity to taxanes. To our knowledge, this study is the first to examine aberrant hypermethylation of CHFR in endometrial cancer, and our results suggest that the methylation status of CHFR may be a new molecular index that will allow design of personalized treatment in endometrial cancer. This may be particularly important in poorly differentiated adenocarcinoma (G3), which is known to have a poor prognosis.

    Web of Science

    researchmap

  • Relationship of aberrant DNA hypermethylation of CHFR with sensitivity to taxanes in endometrial cancer

    Megumi Yanokura, Kouji Banno, Makiko Kawaguchi, Nobumaru Hirao, Akira Hirasawa, Nobuyuki Susumu, Katsumi Tsukazaki, Daisuke Aoki

    ONCOLOGY REPORTS   17 ( 1 )   41 - 48   2007.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    The relationship of aberrant DNA hypermethylation of cell cycle checkpoint genes with the sensitivity of cancer cells to anticancer drugs is a question of current interest. In this study, we investigated the relationship between aberrant hypermethylation of the CHFR (checkpoint with forkhead-associated and ring finger) mitotic checkpoint gene and sensitivity to taxanes in endometrial cancer. Methylation-specific PCR (MSP) indicated aberrant hypermethylation of CHFR in 12.0% (6/50) of endometrial cancer specimens, and suggested that aberrant hypermethylation is significantly more frequent in poorly differentiated adenocarcinoma (G3) (p < 0.05). Of six culture cell lines, SNG-II and HEC108 cells showed aberrant hypermethylation and reduced expression of CHFR. These cells had high sensitivity to taxanes but became resistant after demethylation. Cancer specimens with aberrant hypermethylation of CHFR also exhibited high sensitivity to taxanes. To our knowledge, this study is the first to examine aberrant hypermethylation of CHFR in endometrial cancer, and our results suggest that the methylation status of CHFR may be a new molecular index that will allow design of personalized treatment in endometrial cancer. This may be particularly important in poorly differentiated adenocarcinoma (G3), which is known to have a poor prognosis.

    Web of Science

    researchmap

  • Relationship of aberrant DNA hypermethylation of CHFR with sensitivity to taxanes in endometrial cancer. International journal

    Megumi Yanokura, Kouji Banno, Makiko Kawaguchi, Nobumaru Hirao, Akira Hirasawa, Nobuyuki Susumu, Katsumi Tsukazaki, Daisuke Aoki

    Oncology reports   17 ( 1 )   41 - 8   2007.1

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    The relationship of aberrant DNA hypermethylation of cell cycle checkpoint genes with the sensitivity of cancer cells to anticancer drugs is a question of current interest. In this study, we investigated the relationship between aberrant hypermethylation of the CHFR (checkpoint with forkhead-associated and ring finger) mitotic checkpoint gene and sensitivity to taxanes in endometrial cancer. Methylation-specific PCR (MSP) indicated aberrant hypermethylation of CHFR in 12.0% (6/50) of endometrial cancer specimens, and suggested that aberrant hypermethylation is significantly more frequent in poorly differentiated adenocarcinoma (G3) (p<0.05). Of six culture cell lines, SNG-II and HEC108 cells showed aberrant hypermethylation and reduced expression of CHFR. These cells had high sensitivity to taxanes but became resistant after demethylation. Cancer specimens with aberrant hypermethylation of CHFR also exhibited high sensitivity to taxanes. To our knowledge, this study is the first to examine aberrant hypermethylation of CHFR in endometrial cancer, and our results suggest that the methylation status of CHFR may be a new molecular index that will allow design of personalized treatment in endometrial cancer. This may be particularly important in poorly differentiated adenocarcinoma (G3), which is known to have a poor prognosis.

    Web of Science

    PubMed

    researchmap

  • 家族内癌集積性を有する子宮体癌症例におけるMMR遺伝子の生殖細胞変異解析

    HIRASAWA AKIRA

    家族性腫瘍   7 ( 1 )   15-18 - 18   2007

  • 妊娠に伴い増悪した片頭痛に対して呉茱萸湯が著効した1例―妊娠期間中の片頭痛治療に関する考察も含めて―

    HIRASAWA AKIRA

    産婦人科漢方研究のあゆみ   24 ( 24 )   98-101 - 101   2007

     More details

    Language:Japanese  

    researchmap

  • 当院更年期外来にて診断された閉経後骨粗鬆症/骨量減少症における血清脂質動態の検討

    HIRASAWA AKIRA

    Osteoporosis Japan   15 ( 2 )   158   2007

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 骨粗鬆症治療薬の服薬コンプライアンス向上に必要な要因の検討

    HIRASAWA AKIRA

    Osteoporosis Japan   15 ( 3 )   142-144 - 486   2007

  • 明細胞腺癌

    AOKI DAISUKE

    産婦人科の実際   55 ( 13 )   2185-2193   2006.12

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • Relationship of the aberrant DNA hypermethylation of cancer-related genes with carcinogenesis of endometrial cancer

    Kouji Banno, Megumi Yanokura, Nobuyuki Susumu, Makiko Kawaguchi, Nobumaru Hirao, Akira Hirasawa, Katsumi Tsukazaki, Daisuke Aoki

    ONCOLOGY REPORTS   16 ( 6 )   1189 - 1196   2006.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    Epigenetic abnormalities including the aberrant DNA hypermethylation of the promoter CpG islands play a key role in the mechanism of gene inactivation in cell carcinogenesis. To identify the genes associated with aberrant DNA hypermethylation in endometrial carcinogenesis, we studied the. hypermethylation of the promoter regions of five genes: hMLH1, APC, E-cadherin, RAR-beta and p16. The frequencies of aberrant hypermethylation were 40.4% (21/52) in hMLH1, 22% (11/50) in APC, 14% (7/50) in E-cadherin, and 2.3% (1/44) in RAR-beta in endometrial cancer specimens. No aberrant DNA methylation was found in p16. In atypical endometrial hyperplasia, the frequencies of aberrant methylation were 14.3% (2/14) in hMLH1 and 7.3% (1/14) in APC, whereas normal endometrial cells showed no aberrant hypermethylation of any of the five genes. The high frequencies of the aberrant DNA hypermethylation of hMLH1, APC and E-cadherin suggest that the methylation of the DNA mismatch repair and Wnt signal-related genes may be associated with endometrial carcinogenesis.

    Web of Science

    researchmap

  • Relationship of the aberrant DNA hypermethylation of cancer-related genes with carcinogenesis of endometrial cancer

    Kouji Banno, Megumi Yanokura, Nobuyuki Susumu, Makiko Kawaguchi, Nobumaru Hirao, Akira Hirasawa, Katsumi Tsukazaki, Daisuke Aoki

    ONCOLOGY REPORTS   16 ( 6 )   1189 - 1196   2006.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    Epigenetic abnormalities including the aberrant DNA hypermethylation of the promoter CpG islands play a key role in the mechanism of gene inactivation in cell carcinogenesis. To identify the genes associated with aberrant DNA hypermethylation in endometrial carcinogenesis, we studied the. hypermethylation of the promoter regions of five genes: hMLH1, APC, E-cadherin, RAR-beta and p16. The frequencies of aberrant hypermethylation were 40.4% (21/52) in hMLH1, 22% (11/50) in APC, 14% (7/50) in E-cadherin, and 2.3% (1/44) in RAR-beta in endometrial cancer specimens. No aberrant DNA methylation was found in p16. In atypical endometrial hyperplasia, the frequencies of aberrant methylation were 14.3% (2/14) in hMLH1 and 7.3% (1/14) in APC, whereas normal endometrial cells showed no aberrant hypermethylation of any of the five genes. The high frequencies of the aberrant DNA hypermethylation of hMLH1, APC and E-cadherin suggest that the methylation of the DNA mismatch repair and Wnt signal-related genes may be associated with endometrial carcinogenesis.

    Web of Science

    researchmap

  • Relationship of the aberrant DNA hypermethylation of cancer-related genes with carcinogenesis of endometrial cancer Reviewed

    Kouji Banno, Megumi Yanokura, Nobuyuki Susumu, Makiko Kawaguchi, Nobumaru Hirao, Akira Hirasawa, Katsumi Tsukazaki, Daisuke Aoki

    ONCOLOGY REPORTS   16 ( 6 )   1189 - 1196   2006.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    Epigenetic abnormalities including the aberrant DNA hypermethylation of the promoter CpG islands play a key role in the mechanism of gene inactivation in cell carcinogenesis. To identify the genes associated with aberrant DNA hypermethylation in endometrial carcinogenesis, we studied the. hypermethylation of the promoter regions of five genes: hMLH1, APC, E-cadherin, RAR-beta and p16. The frequencies of aberrant hypermethylation were 40.4% (21/52) in hMLH1, 22% (11/50) in APC, 14% (7/50) in E-cadherin, and 2.3% (1/44) in RAR-beta in endometrial cancer specimens. No aberrant DNA methylation was found in p16. In atypical endometrial hyperplasia, the frequencies of aberrant methylation were 14.3% (2/14) in hMLH1 and 7.3% (1/14) in APC, whereas normal endometrial cells showed no aberrant hypermethylation of any of the five genes. The high frequencies of the aberrant DNA hypermethylation of hMLH1, APC and E-cadherin suggest that the methylation of the DNA mismatch repair and Wnt signal-related genes may be associated with endometrial carcinogenesis.

    Web of Science

    researchmap

  • Relationship of the aberrant DNA hypermethylation of cancer-related genes with carcinogenesis of endometrial cancer. Reviewed International journal

    Kouji Banno, Megumi Yanokura, Nobuyuki Susumu, Makiko Kawaguchi, Nobumaru Hirao, Akira Hirasawa, Katsumi Tsukazaki, Daisuke Aoki

    Oncology reports   16 ( 6 )   1189 - 96   2006.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:PROFESSOR D A SPANDIDOS  

    Epigenetic abnormalities including the aberrant DNA hypermethylation of the promoter CpG islands play a key role in the mechanism of gene inactivation in cell carcinogenesis. To identify the genes associated with aberrant DNA hypermethylation in endometrial carcinogenesis, we studied the hypermethylation of the promoter regions of five genes: hMLH1, APC, E-cadherin, RAR-beta and p16. The frequencies of aberrant hypermethylation were 40.4% (21/52) in hMLH1, 22% (11/50) in APC, 14% (7/50) in E-cadherin, and 2.3% (1/44) in RAR-beta in endometrial cancer specimens. No aberrant DNA methylation was found in p16. In atypical endometrial hyperplasia, the frequencies of aberrant methylation were 14.3% (2/14) in hMLH1 and 7.3% (1/14) in APC, whereas normal endometrial cells showed no aberrant hypermethylation of any of the five genes. The high frequencies of the aberrant DNA hypermethylation of hMLH1, APC and E-cadherin suggest that the methylation of the DNA mismatch repair and Wnt signal-related genes may be associated with endometrial carcinogenesis.

    Web of Science

    PubMed

    researchmap

  • 卵巣明細胞腺癌におけるシアリダーゼ発現の多寡が腹膜播種形成に及ぼす影響の検討

    野村 弘行, 玉田 裕, 鈴木 淳, 平沢 晃, 進 伸幸, 宮城 妙子, 入村 達郎, 青木 大輔

    日本分子腫瘍マーカー研究会プログラム・講演抄録   26回   28 - 29   2006.9

     More details

    Language:Japanese   Publisher:日本分子腫瘍マーカー研究会  

    researchmap

  • 子宮体癌における腫瘍マーカーの意義

    AOKI DAISUKE

    産婦人科の実際   55 ( 5 )   753-762 - 762   2006.5

     More details

    Language:Japanese  

    researchmap

  • コルポスコピー、コルポ下狙い生検

    AOKI DAISUKE

    臨床婦人科産科   60 ( 4 )   369-375 - 375   2006.4

  • Clinicopathologic manifestations of early-onset endometrial cancer in Japanese women with a familial predisposition to cancer. International journal

    Wataru Yamagami, Nobuyuki Susumu, Kouji Banno, Takeshi Hirao, Fumio Kataoka, Akira Hirasawa, Nao Suzuki, Daisuke Aoki, Shiro Nozawa

    The journal of obstetrics and gynaecology research   31 ( 5 )   444 - 51   2005.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BLACKWELL PUBLISHING  

    AIM: The number of patients under 40 years of age with early-onset endometrial cancer is on the rise in Japan. Preservation of fertility in younger patients is a critical issue. In order to examine the clinical and pathological characteristics of these patients, cases of early-onset endometrial cancer at a single hospital were analyzed. METHODS: Seventy-four patients were diagnosed with endometrial cancer before age 40 and included in this study after obtaining informed consent. RESULTS: The clinical characteristics included a significantly higher prevalence of complications such as nulligravidity and nulliparity (P < 0.001). Pathologically, well-differentiated endometrial carcinoma was significantly more frequent (P = 0.011). The 5-year survival rate was high (98.7%). In regards to the relationship between clinicopathological features and grade of differentiation, the prevalence of G2 and G3 carcinoma was not significantly lower (P = 0.24) in patients with obesity. Although the frequency of G2 and G3 carcinoma was significantly higher in patients with a family history of cancer (P = 0.02), their 5-year survival rate was not significantly lower (100%). CONCLUSION: This study found that these two types of early-onset endometrial cancer are clinicopathologically different. In patients with a family history of cancer, their body mass index was lower, and the frequency of G2 and G3 carcinoma was significantly higher, but their 5-year disease-free survival rate was not significantly lower.

    DOI: 10.1111/j.1447-0756.2005.00318.x

    Web of Science

    PubMed

    researchmap

  • 実地臨床応用が期待される新たな腫瘍マーカー−バイオマーカーとしてのゲノム変化を中心に−

    AOKI DAISUKE

    臨床婦人科産科   59 ( 10 )   1383-1387 - 1387   2005.10

  • [Diagnostic significance of tumor markers for gynecologic malignancies].

    Daisuke Aoki, Akira Hirasawa, Nobuyuki Susumu

    Gan to kagaku ryoho. Cancer & chemotherapy   32 ( 3 )   411 - 6   2005.3

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    Gynecologic malignancies include ovarian cancer, uterine cervical cancer, endometrial cancer, and trophoblastic neoplasms. With ovarian tumors, due to their location within the abdominal cavity, it is difficult to make a preoperative pathological diagnosis of cancer without laparotomy. From this point of view, the use of tumor markers that consist of carbohydrate antigens, such as CA 125, in addition to diagnostic imaging are useful in the diagnosis of ovarian cancer. SCC antigen, a marker for squamous cell carcinoma, is clinically useful in the management of advanced cervical cancer. At present, there are no useful tumor markers for endometrial cancer that exhibit both high sensitivity and specificity, although CA 125 is often used in clinical practice. Finally, human chorionic gonadotropin (hCG) serves as an ideal tumor marker for trophoblastic disease; however, the incidence of trophoblastic neoplasms has decreased dramatically with the incorporation of strict clinical management of post-molar disease as well as with the overall decrease in the number of pregnancies.

    PubMed

    researchmap

  • 婦人科腫瘍

    AOKI DAISUKE

    癌と化学療法   32 ( 33 )   411-416   2005.3

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • Diagnostic significance of tumor markers for gynecologic malignancies

    Aoki Daisuke, Hirasawa Akira, Susumu Nobuyuki

    Gan to kagaku ryoho. Cancer & chemotherapy   32 ( 3 )   411 - 416   2005.3

     More details

    Language:English  

    &lt;p&gt;Gynecologic malignancies include ovarian cancer, uterine cervical cancer, endometrial cancer, and trophoblastic neoplasms. With ovarian tumors, due to their location within the abdominal cavity, it is difficult to make a preoperative pathological diagnosis of cancer without laparotomy. From this point of view, the use of tumor markers that consist of carbohydrate antigens, such as CA 125, in addition to diagnostic imaging are useful in the diagnosis of ovarian cancer. SCC antigen, a marker for squamous cell carcinoma, is clinically useful in the management of advanced cervical cancer. At present, there are no useful tumor markers for endometrial cancer that exhibit both high sensitivity and specificity, although CA 125 is often used in clinical practice. Finally, human chorionic gonadotropin (hCG) serves as an ideal tumor marker for trophoblastic disease; however, the incidence of trophoblastic neoplasms has decreased dramatically with the incorporation of strict clinical management of post-molar disease as well as with the overall decrease in the number of pregnancies.&lt;/p&gt;

    researchmap

  • 子宮体癌手術症例における傍大動脈リンパ節廓清の検討.

    HIRASAWA AKIRA

    日本産科婦人科学会東京地方部会会誌   54 ( 2 )   219-222 - 222   2005

     More details

    Language:Japanese  

    researchmap

  • Clinicopathologic manifestations of early-onset endometrial cancer in Japanese women with a familial predisposition to cancer

    W Yamagami, N Susumu, K Banno, T Hirao, F Kataoka, A Hirasawa, N Suzuki, D Aoki, S Nozawa

    JOURNAL OF OBSTETRICS AND GYNAECOLOGY RESEARCH   31 ( 5 )   444 - 451   2005

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BLACKWELL PUBLISHING  

    Aim: The number of patients under 40 years of age with early-onset endometrial cancer is on the rise in Japan. Preservation of fertility in younger patients is a critical issue. In order to examine the clinical and pathological characteristics of these patients, cases of early-onset endometrial cancer at a single hospital were analyzed.
    Methods: Seventy-four patients were diagnosed with endometrial cancer before age 40 and included in this study after obtaining informed consent.
    Results: The clinical characteristics included a significantly higher prevalence of complications such as nulligravidity and nulliparity (P &lt; 0.001). Pathologically, well-differentiated endometrial carcinoma was significantly more frequent (P = 0.011). The 5-year survival rate was high (98.7%). In regards to the relationship between clinicopathological features and grade of differentiation, the prevalence of G2 and G3 carcinoma was not significantly lower (P = 0.24) in patients with obesity. Although the frequency of G2 and G3 carcinoma was significantly higher in patients with a family history of cancer (P = 0.02), their 5-year survival rate was not significantly lower (100%).
    Conclusion: This study found that these two types of early-onset endometrial cancer are clinicopathologically different. In patients with a family history of cancer, their body mass index was lower, and the frequency of G2 and G3 carcinoma was significantly higher, but their 5-year disease-free survival rate was not significantly lower.

    DOI: 10.1111/j.1447-0756.2005.00318.x

    Web of Science

    researchmap

  • Clinicopathologic manifestations of early-onset endometrial cancer in Japanese women with a familial predisposition to cancer Reviewed

    W Yamagami, N Susumu, K Banno, T Hirao, F Kataoka, A Hirasawa, N Suzuki, D Aoki, S Nozawa

    JOURNAL OF OBSTETRICS AND GYNAECOLOGY RESEARCH   31 ( 5 )   444 - 451   2005

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BLACKWELL PUBLISHING  

    Aim: The number of patients under 40 years of age with early-onset endometrial cancer is on the rise in Japan. Preservation of fertility in younger patients is a critical issue. In order to examine the clinical and pathological characteristics of these patients, cases of early-onset endometrial cancer at a single hospital were analyzed.
    Methods: Seventy-four patients were diagnosed with endometrial cancer before age 40 and included in this study after obtaining informed consent.
    Results: The clinical characteristics included a significantly higher prevalence of complications such as nulligravidity and nulliparity (P &lt; 0.001). Pathologically, well-differentiated endometrial carcinoma was significantly more frequent (P = 0.011). The 5-year survival rate was high (98.7%). In regards to the relationship between clinicopathological features and grade of differentiation, the prevalence of G2 and G3 carcinoma was not significantly lower (P = 0.24) in patients with obesity. Although the frequency of G2 and G3 carcinoma was significantly higher in patients with a family history of cancer (P = 0.02), their 5-year survival rate was not significantly lower (100%).
    Conclusion: This study found that these two types of early-onset endometrial cancer are clinicopathologically different. In patients with a family history of cancer, their body mass index was lower, and the frequency of G2 and G3 carcinoma was significantly higher, but their 5-year disease-free survival rate was not significantly lower.

    DOI: 10.1111/j.1447-0756.2005.00318.x

    Web of Science

    researchmap

  • Involvement of overexpressed wild-type BRAF in the growth of malignant melanoma cell lines. Reviewed International journal

    Hideaki Tanami, Issei Imoto, Akira Hirasawa, Yasuhiro Yuki, Itaru Sonoda, Jun Inoue, Kohichiro Yasui, Akiko Misawa-Furihata, Yutaka Kawakami, Johji Inazawa

    Oncogene   23 ( 54 )   8796 - 804   2004.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    Comparative genomic hybridization (CGH) using 40 cell lines derived from malignant melanomas (MMs) revealed frequent amplification at 7q33-q34 containing BRAF gene, which often is mutated in MM. We found this gene to be amplified to a remarkable degree in the MM cell lines that exhibited high-level gains at 7q33-q34 in CGH. Among 40 cell lines, the eight lines that revealed neither BRAF nor NRAS mutations showed even higher levels of BRAF mRNA expression than the 32 mutated lines, although DNA amplification at 7q33-q34 was not detected in every lines overexpressing BRAF. MM cells that carried wild-type BRAF and NRAS showed constitutive overexpression of B-Raf protein and phosphorylation of extracellular signal-regulated kinase 1/2 (ERK1/2), even after serum starvation. Not only downregulation of the endogenously overexpressed wild-type B-Raf by antisense oligonucleotide but also a treatment with an inhibitor of mitogen-activated protein kinase kinase (MAPKK, MEK) reduced phosphorylated ERK1/2 and cell growth, whereas the exogenously expressed wild-type B-Raf promoted cell growth in MM cells. Our results provide the evidence that overexpression of wild-type B-Raf, in part but not always as a result of gene amplification, is one of the mechanisms underlying constitutive activation of the MAPK pathway that stimulates growth of MM cells.

    DOI: 10.1038/sj.onc.1208152

    Web of Science

    PubMed

    researchmap

  • Involvement of overexpressed wild-type BRAF in the growth of malignant melanoma cell lines

    H Tanami, Imoto, I, A Hirasawa, Y Yuki, Sonoda, I, J Inoue, K Yasui, A Misawa-Furihata, Y Kawakami, J Inazawa

    ONCOGENE   23 ( 54 )   8796 - 8804   2004.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    Comparative genomic hybridization (CGH) using 40 cell lines derived from malignant melanomas (MMs) revealed frequent amplification at 7q33-q34 containing BRAF gene, which often is mutated in MM. We found this gene to be amplified to a remarkable degree in the MM cell lines that exhibited high-level gains at 7q33-q34 in CGH. Among 40 cell lines, the eight lines that revealed neither BRAF nor NRAS mutations showed even higher levels of BRAF mRNA expression than the 32 mutated lines, although DNA amplification at 7q33-q34 was not detected in every lines overexpressing BRAF. MM cells that carried wild-type BRAF and NRAS showed constitutive overexpression of B-Raf protein and phosphorylation of extracellular signal-regulated kinase 1/2 (ERK1/2), even after serum starvation. Not only downregulation of the endogenously overexpressed wild-type B-Raf by antisense oligonucleotide but also a treatment with an inhibitor of mitogen-activated protein kinase kinase (MAPKK, MEK) reduced phosphorylated ERK1/2 and cell growth, whereas the exogenously expressed wild-type B-Raf promoted cell growth in MM cells. Our results provide the evidence that overexpression of wild-type B-Raf, in part but not always as a result of gene amplification, is one of the mechanisms underlying constitutive activation of the MAPK pathway that stimulates growth of MM cells.

    DOI: 10.1038/sj.onc.1208152

    Web of Science

    researchmap

  • Involvement of overexpressed wild-type BRAF in the growth of malignant melanoma cell lines

    H Tanami, Imoto, I, A Hirasawa, Y Yuki, Sonoda, I, J Inoue, K Yasui, A Misawa-Furihata, Y Kawakami, J Inazawa

    ONCOGENE   23 ( 54 )   8796 - 8804   2004.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:NATURE PUBLISHING GROUP  

    Comparative genomic hybridization (CGH) using 40 cell lines derived from malignant melanomas (MMs) revealed frequent amplification at 7q33-q34 containing BRAF gene, which often is mutated in MM. We found this gene to be amplified to a remarkable degree in the MM cell lines that exhibited high-level gains at 7q33-q34 in CGH. Among 40 cell lines, the eight lines that revealed neither BRAF nor NRAS mutations showed even higher levels of BRAF mRNA expression than the 32 mutated lines, although DNA amplification at 7q33-q34 was not detected in every lines overexpressing BRAF. MM cells that carried wild-type BRAF and NRAS showed constitutive overexpression of B-Raf protein and phosphorylation of extracellular signal-regulated kinase 1/2 (ERK1/2), even after serum starvation. Not only downregulation of the endogenously overexpressed wild-type B-Raf by antisense oligonucleotide but also a treatment with an inhibitor of mitogen-activated protein kinase kinase (MAPKK, MEK) reduced phosphorylated ERK1/2 and cell growth, whereas the exogenously expressed wild-type B-Raf promoted cell growth in MM cells. Our results provide the evidence that overexpression of wild-type B-Raf, in part but not always as a result of gene amplification, is one of the mechanisms underlying constitutive activation of the MAPK pathway that stimulates growth of MM cells.

    DOI: 10.1038/sj.onc.1208152

    Web of Science

    researchmap

  • [Outline of treatment for endometrial cancer].

    Daisuke Aoki, Akira Hirasawa, Nobuyuki Susumu, Shiro Nozawa

    Nihon rinsho. Japanese journal of clinical medicine   62 Suppl 10   324 - 8   2004.10

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    PubMed

    researchmap

  • 子宮体癌の治療 治療概論

    青木大輔, 平沢 晃, 進 伸幸, 野澤志朗

    日本臨床   62 ( 増刊 )   324-328 - 328   2004.10

     More details

    Language:Japanese  

    researchmap

  • Two Japanese kindreds occurring endometrial cancer meeting new clinical criteria for hereditary non-polyposis colorectal cancer (HNPCC), Amsterdam Criteria II Reviewed

    K Banno, N Susumu, T Hirao, M Yanokura, A Hirasawa, D Aoki, Y Udagawa, K Sugano, S Nozawa

    JOURNAL OF OBSTETRICS AND GYNAECOLOGY RESEARCH   30 ( 4 )   287 - 292   2004.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BLACKWELL PUBLISHING ASIA  

    Hereditary non-polyposis colorectal cancer (HNPCC), also called Lynch syndrome, is an autosomal dominantly inherited disorder of cancer susceptibility. Patients with HNPCC exhibit an increased risk for HNPCC-associated extracolonic tumors such as cancer of the endometrium. HNPCC is associated with germline mutations in DNA mismatch repair (MMR) genes: hMLH1, hMSH2 and hMSH6.
    Here, we describe two Japanese kindreds (0.5%) who met the new clinical criteria for HNPCC, Amsterdam criteria II, from among 375 endometrial cancer patients treated at Keio University Hospital from 1990 to 2002. From these results, it was found that female HNPCC patients comprised approximately 0.5% of all endometrial cancer patients. Decreased expression of two MMR gene protein products (hMLH1 and hMSH6) was confirmed immunohistochemically in these two endometrial tumors in HNPCC kindreds. This case report provides important information on Japanese HNPCC patients occurring endometrial cancer.

    DOI: 10.1111/j.1447-0756.2004.00195.x

    Web of Science

    researchmap

  • Association of HNPCC and endometrial cancers.

    Kouji Banno, Nobuyuki Susumu, Megumi Yanokura, Takeshi Hirao, Takashi Iwata, Akira Hirasawa, Daisuke Aoki, Kokichi Sugano, Shiro Nozawa

    International journal of clinical oncology   9 ( 4 )   262 - 9   2004.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Hereditary nonpolyposis colorectal cancer (HNPCC) is among the representative familial cancers that are autosomally dominant inherited disorders. Because endometrial cancers develop at high rates in women with HNPCC, it is suggested that some endometrial cancers are familial cancers that are induced by mutations of the DNA mismatch repair (MMR) genes, as in HNPCC. To understand the clinical pathology of familial endometrial cancers that are associated with HNPCC, we surveyed the family histories of 385 patients with endometrial cancer and found that 0.5% of endometrial cancers met the new diagnostic criteria of HNPCC. From molecular and biological analyses, we found microsatellite instability in 30.8% of endometrial cancers and germline mutations of MMR genes in 8.3%. These results suggest a close relationship of MMR gene mutations to the development of endometrial cancers. For a better understanding of the clinical pathology of HNPCC-associated familial endometrial cancers, it is critical for gynecologists to perform a large multicenter study, including detailed family histories.

    DOI: 10.1007/s10147-004-0402-8

    Scopus

    PubMed

    researchmap

  • Association of HNPCC and endometrial cancers

    Kouji Banno, Nobuyuld Susumu, Megumi Yanokura, Takeshi Hirao, Takashi Iwata, Akira Hirasawa, Daisuke Aoki, Kokichi Sugano, Shiro Nozawa

    International Journal of Clinical Oncology   9 ( 4 )   262 - 269   2004.8

     More details

    Language:English  

    Hereditary nonpolyposis colorectal cancer (HNPCC) is among the representative familial cancers that are autosomally dominant inherited disorders. Because endometrial cancers develop at high rates in women with HNPCC, it is suggested that some endometrial cancers are familial cancers that are induced by mutations of the DNA mismatch repair (MMR) genes, as in HNPCC. To understand the clinical pathology of familial endometrial cancers that are associated with HNPCC, we surveyed the family histories of 385 patients with endometrial cancer and found that 0.5% of endometrial cancers met the new diagnostic criteria of HNPCC. From molecular and biological analyses, we found microsatellite instability in 30.8% of endometrial cancers and germline mutations of MMR genes in 8.3%. These results suggest a close relationship of MMR gene mutations to the development of endometrial cancers. For a better understanding of the clinical pathology of HNPCC-associated familial endometrial cancers, it is critical for gynecologists to perform a large multicenter study, including detailed family histories.

    DOI: 10.1007/s10147-004-0402-8

    Scopus

    PubMed

    researchmap

  • Two Japanese kindreds occurring endometrial cancer meeting new clinical criteria for hereditary non-polyposis colorectal cancer (HNPCC), Amsterdam Criteria II. International journal

    Kouji Banno, Nobuyuki Susumu, Takeshi Hirao, Megumi Yanokura, Akira Hirasawa, Daisuke Aoki, Yasuhiro Udagawa, Kokichi Sugano, Shiro Nozawa

    The journal of obstetrics and gynaecology research   30 ( 4 )   287 - 92   2004.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BLACKWELL PUBLISHING ASIA  

    Hereditary non-polyposis colorectal cancer (HNPCC), also called Lynch syndrome, is an autosomal dominantly inherited disorder of cancer susceptibility. Patients with HNPCC exhibit an increased risk for HNPCC-associated extracolonic tumors such as cancer of the endometrium. HNPCC is associated with germline mutations in DNA mismatch repair (MMR) genes: hMLH1, hMSH2 and hMSH6. Here, we describe two Japanese kindreds (0.5%) who met the new clinical criteria for HNPCC, Amsterdam criteria II, from among 375 endometrial cancer patients treated at Keio University Hospital from 1990 to 2002. From these results, it was found that female HNPCC patients comprised approximately 0.5% of all endometrial cancer patients. Decreased expression of two MMR gene protein products (hMLH1 and hMSH6) was confirmed immunohistochemically in these two endometrial tumors in HNPCC kindreds. This case report provides important information on Japanese HNPCC patients occurring endometrial cancer.

    DOI: 10.1111/j.1447-0756.2004.00195.x

    Web of Science

    PubMed

    researchmap

  • Two Japanese kindreds occurring endometrial cancer meeting new clinical criteria for hereditary non-polyposis colorectal cancer (HNPCC), Amsterdam Criteria II

    K Banno, N Susumu, T Hirao, M Yanokura, A Hirasawa, D Aoki, Y Udagawa, K Sugano, S Nozawa

    JOURNAL OF OBSTETRICS AND GYNAECOLOGY RESEARCH   30 ( 4 )   287 - 292   2004.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BLACKWELL PUBLISHING ASIA  

    Hereditary non-polyposis colorectal cancer (HNPCC), also called Lynch syndrome, is an autosomal dominantly inherited disorder of cancer susceptibility. Patients with HNPCC exhibit an increased risk for HNPCC-associated extracolonic tumors such as cancer of the endometrium. HNPCC is associated with germline mutations in DNA mismatch repair (MMR) genes: hMLH1, hMSH2 and hMSH6.
    Here, we describe two Japanese kindreds (0.5%) who met the new clinical criteria for HNPCC, Amsterdam criteria II, from among 375 endometrial cancer patients treated at Keio University Hospital from 1990 to 2002. From these results, it was found that female HNPCC patients comprised approximately 0.5% of all endometrial cancer patients. Decreased expression of two MMR gene protein products (hMLH1 and hMSH6) was confirmed immunohistochemically in these two endometrial tumors in HNPCC kindreds. This case report provides important information on Japanese HNPCC patients occurring endometrial cancer.

    DOI: 10.1111/j.1447-0756.2004.00195.x

    Web of Science

    researchmap

  • Association of HNPCC and endometrial cancers Reviewed

    Kouji Banno, Nobuyuld Susumu, Megumi Yanokura, Takeshi Hirao, Takashi Iwata, Akira Hirasawa, Daisuke Aoki, Kokichi Sugano, Shiro Nozawa

    International Journal of Clinical Oncology   9 ( 4 )   262 - 269   2004.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    Hereditary nonpolyposis colorectal cancer (HNPCC) is among the representative familial cancers that are autosomally dominant inherited disorders. Because endometrial cancers develop at high rates in women with HNPCC, it is suggested that some endometrial cancers are familial cancers that are induced by mutations of the DNA mismatch repair (MMR) genes, as in HNPCC. To understand the clinical pathology of familial endometrial cancers that are associated with HNPCC, we surveyed the family histories of 385 patients with endometrial cancer and found that 0.5% of endometrial cancers met the new diagnostic criteria of HNPCC. From molecular and biological analyses, we found microsatellite instability in 30.8% of endometrial cancers and germline mutations of MMR genes in 8.3%. These results suggest a close relationship of MMR gene mutations to the development of endometrial cancers. For a better understanding of the clinical pathology of HNPCC-associated familial endometrial cancers, it is critical for gynecologists to perform a large multicenter study, including detailed family histories.

    DOI: 10.1007/s10147-004-0402-8

    Scopus

    PubMed

    researchmap

  • Overexpression of PDZK1 within the 1q12-q22 amplicon is likely to be associated with drug resistance phenotype in multiple myeloma

    J Inoue, T Otsuki, A Hirasawa, Imoto, I, Y Matsuo, S Shimizu, M Taniwaki, J Inazawa

    AMERICAN JOURNAL OF PATHOLOGY   165 ( 1 )   71 - 81   2004.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER SOC INVESTIGATIVE PATHOLOGY, INC  

    We investigated DNA copy number aberrations in 37 cell lines derived from multiple myelomas (MMs) using comparative genomic hybridization, and 11 (29.7%) showed high-level gain indicative of gene amplification at 1q12-q22. A corresponding transcriptional mapping using oligonucleotide arrays extracted three up-regulated genes (IRTA2, PDZK1, and S100A6) within the smallest region of overlapping in amplifications. Among them PDZK1 showed amplification and consequent overexpression in the MM cell lines. Amplification of PDZK1 was observed in primary cases of MM as well. MM cell lines with amplification of PDZK1 exhibited the resistance to melphalan-, cis-platin-, and vincristin-induced cell death compared with MM cell lines without its amplifications. Furthermore, down-regulation of PDZK1 with an anti-sense oligonucleotide sensitized a cell line KMS-11 to melphalan, cis-platin, and vincristin. Taken together, our results indicate that PDZK1 is likely to be one of targets for 1q12-q22 amplification in MM and may be associated with the malignant phenotype, including drug resistance, in this type of tumor.

    Web of Science

    researchmap

  • Overexpression of PDZK1 within the 1q12-q22 amplicon is likely to be associated with drug resistance phenotype in multiple myeloma

    J Inoue, T Otsuki, A Hirasawa, Imoto, I, Y Matsuo, S Shimizu, M Taniwaki, J Inazawa

    AMERICAN JOURNAL OF PATHOLOGY   165 ( 1 )   71 - 81   2004.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER SOC INVESTIGATIVE PATHOLOGY, INC  

    We investigated DNA copy number aberrations in 37 cell lines derived from multiple myelomas (MMs) using comparative genomic hybridization, and 11 (29.7%) showed high-level gain indicative of gene amplification at 1q12-q22. A corresponding transcriptional mapping using oligonucleotide arrays extracted three up-regulated genes (IRTA2, PDZK1, and S100A6) within the smallest region of overlapping in amplifications. Among them PDZK1 showed amplification and consequent overexpression in the MM cell lines. Amplification of PDZK1 was observed in primary cases of MM as well. MM cell lines with amplification of PDZK1 exhibited the resistance to melphalan-, cis-platin-, and vincristin-induced cell death compared with MM cell lines without its amplifications. Furthermore, down-regulation of PDZK1 with an anti-sense oligonucleotide sensitized a cell line KMS-11 to melphalan, cis-platin, and vincristin. Taken together, our results indicate that PDZK1 is likely to be one of targets for 1q12-q22 amplification in MM and may be associated with the malignant phenotype, including drug resistance, in this type of tumor.

    Web of Science

    researchmap

  • Overexpression of PDZK1 within the 1q12-q22 amplicon is likely to be associated with drug-resistance phenotype in multiple myeloma. Reviewed International journal

    Jun Inoue, Takemi Otsuki, Akira Hirasawa, Issei Imoto, Yoshinobu Matsuo, Shiroh Shimizu, Masafumi Taniwaki, Johji Inazawa

    The American journal of pathology   165 ( 1 )   71 - 81   2004.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER SOC INVESTIGATIVE PATHOLOGY, INC  

    We investigated DNA copy number aberrations in 37 cell lines derived from multiple myelomas (MMs) using comparative genomic hybridization, and 11 (29.7%) showed high-level gain indicative of gene amplification at 1q12-q22. A corresponding transcriptional mapping using oligonucleotide arrays extracted three up-regulated genes (IRTA2, PDZK1, and S100A6) within the smallest region of overlapping in amplifications. Among them PDZK1 showed amplification and consequent overexpression in the MM cell lines. Amplification of PDZK1 was observed in primary cases of MM as well. MM cell lines with amplification of PDZK1 exhibited the resistance to melphalan-, cis-platin-, and vincristin-induced cell death compared with MM cell lines without its amplifications. Furthermore, down-regulation of PDZK1 with an anti-sense oligonucleotide sensitized a cell line KMS-11 to melphalan, cis-platin, and vincristin. Taken together, our results indicate that PDZK1 is likely to be one of targets for 1q12-q22 amplification in MM and may be associated with the malignant phenotype, including drug resistance, in this type of tumor.

    Web of Science

    PubMed

    researchmap

  • 子宮体癌に対する新たな治療戦略

    平沢 晃, 青木大輔, 野澤志朗

    産科と婦人科   71 ( 2 )   201-207 - 207   2004.2

     More details

    Language:Japanese  

    researchmap

  • 術前細胞診にて癌腫成分のみを示した子宮体部異所性癌肉腫の一例

    HIRASAWA AKIRA

    日本婦人科腫瘍学会雑誌   22 ( 4 )   393-398   2004

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • Outline of treatment for endometrial cancer

    Aoki Daisuke, Hirasawa Akira, Susumu Nobuyuki, Nozawa Shiro

    Nippon rinsho. Japanese journal of clinical medicine   62 Suppl 10   324 - 328   2004

     More details

    Language:English  

    researchmap

  • 腹腔内出血を繰り返した卵巣顆粒細胞腫晩期再発の一例.

    HIRASAWA AKIRA

    日本産科婦人科学会東京地方部会会誌   53 ( 3 )   362-366 - 366   2004

     More details

    Language:Japanese  

    researchmap

  • Unfavorable prognostic factors associated with high frequency of microsatellite instability and comparative genomic hybridization analysis in endometrial cancer. International journal

    Akira Hirasawa, Daisuke Aoki, Jun Inoue, Issei Imoto, Nobuyuki Susumu, Kokichi Sugano, Shiro Nozawa, Johji Inazawa

    Clinical cancer research : an official journal of the American Association for Cancer Research   9 ( 15 )   5675 - 82   2003.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    PURPOSE: Although many articles have been published regarding chromosomal instability (CI) and microsatellite instability (MI) in endometrial adenocarcinoma, the relationship between prognostic factors and the biological mechanisms accounting for genetic instability in these tumors has not yet been precisely defined. To do that, it will be necessary to clarify the molecular mechanisms involved in endometrial carcinogenesis. EXPERIMENTAL DESIGN: Tissue samples from 43 human primary endometrioid endometrial adenocarcinomas (EACs) were analyzed for CI and MI status using comparative genomic hybridization and 11 microsatellite loci, respectively. Methylation status of the promoter of MLH1 was also determined. We analyzed all three of these parameters in relation to each other and to clinicopathological factors. RESULTS: Sixty-five percent of the EACs we examined had detectable CI. Frequent copy number gains were seen at 1q25-41 (23%), 8q11.1-q21.1 (23%), 8q21.3-qter (21%); 28% of these tumors exhibited high-frequency MI (MSI-H); Methylation of the MLH1 promoter was observed in 92% of EACs with MSI-H. Southern blotting showed amplification of MYCN in one tumor, which has been documented for the first time in a primary human EAC. CONCLUSIONS: MSI-H was correlated with histological grade, International Federation of Gynecologists and Obstetricians (FIGO) stage, myometrial invasion, and lymphonode metastasis. Our comparative genomic hybridization results demonstrated that the number of chromosomes involved in genomic alterations in EACs was distinctively fewer than those in other types of tumor. The carcinogenetic process leading to EAC appears to be highly complex; for example, MI and CI may act synergistically, whereas CI and/or MI are likely to be linked with tumor heterogeneity.

    Web of Science

    PubMed

    researchmap

  • Unfavorable prognostic factors associated with high frequency of microsatellite instability and comparative genomic hybridization analysis in endometrial cancer Reviewed

    A Hirasawa, D Aoki, J Inoue, Imoto, I, N Susumu, K Sugano, S Nozawa, J Inazawa

    CLINICAL CANCER RESEARCH   9 ( 15 )   5675 - 5682   2003.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    Purpose: Although many articles have been published regarding chromosomal instability (CI) and microsatellite instability (MI) in endometrial adenocarcinoma, the relationship between prognostic factors and the biological mechanisms accounting for genetic instability in these tumors has not yet been precisely defined. To do that, it will be necessary to clarify the molecular mechanisms involved in endometrial carcinogenesis.
    Experimental Design: Tissue samples from 43 human primary endometrioid endometrial adenocarcinomas (EACs) were analyzed for CI and MI status using comparative genomic hybridization And It microsatellite loci, respectively. Methylation status of the promoter of MLH1 was also determined. We analyzed all three of these parameters in relation to each other and to clinicopathological factors.
    Results: Sixty-five percent of the EACs we examined had detectable CI. Frequent copy number gains were seen at 1q25-41 (23%), 8q11.1-q21.1 (23%), 8q21.3-qter (21%); 28% of these tumors exhibited high-frequency MI (MSI-H); Methylation of the MLH1 promoter was observed in 92% of EACs with MSI-H. Southern blotting showed amplification of MYCN in one tumor, which has been documented for the first time in a primary human EAC.
    Conclusions: MSI-H was correlated with histological grade, International Federation of Gynecologists and Obstetricians (FIGO) stage, myometrial invasion, and lymphonode metastasis. Our comparative genomic hybridization results demonstrated that the number of chromosomes involved in genomic alterations in EACs was distinctively fewer than those in other types of tumor. The carcinogenetic process leading to EAC appears to be highly complex; for example, MI and CI may act synergistically, whereas CI and/or MI are likely to be linked with tumor heterogeneity.

    Web of Science

    researchmap

  • Unfavorable prognostic factors associated with high frequency of microsatellite instability and comparative genomic hybridization analysis in endometrial cancer

    A Hirasawa, D Aoki, J Inoue, Imoto, I, N Susumu, K Sugano, S Nozawa, J Inazawa

    CLINICAL CANCER RESEARCH   9 ( 15 )   5675 - 5682   2003.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    Purpose: Although many articles have been published regarding chromosomal instability (CI) and microsatellite instability (MI) in endometrial adenocarcinoma, the relationship between prognostic factors and the biological mechanisms accounting for genetic instability in these tumors has not yet been precisely defined. To do that, it will be necessary to clarify the molecular mechanisms involved in endometrial carcinogenesis.
    Experimental Design: Tissue samples from 43 human primary endometrioid endometrial adenocarcinomas (EACs) were analyzed for CI and MI status using comparative genomic hybridization And It microsatellite loci, respectively. Methylation status of the promoter of MLH1 was also determined. We analyzed all three of these parameters in relation to each other and to clinicopathological factors.
    Results: Sixty-five percent of the EACs we examined had detectable CI. Frequent copy number gains were seen at 1q25-41 (23%), 8q11.1-q21.1 (23%), 8q21.3-qter (21%); 28% of these tumors exhibited high-frequency MI (MSI-H); Methylation of the MLH1 promoter was observed in 92% of EACs with MSI-H. Southern blotting showed amplification of MYCN in one tumor, which has been documented for the first time in a primary human EAC.
    Conclusions: MSI-H was correlated with histological grade, International Federation of Gynecologists and Obstetricians (FIGO) stage, myometrial invasion, and lymphonode metastasis. Our comparative genomic hybridization results demonstrated that the number of chromosomes involved in genomic alterations in EACs was distinctively fewer than those in other types of tumor. The carcinogenetic process leading to EAC appears to be highly complex; for example, MI and CI may act synergistically, whereas CI and/or MI are likely to be linked with tumor heterogeneity.

    Web of Science

    researchmap

  • Unfavorable prognostic factors associated with high frequency of microsatellite instability and comparative genomic hybridization analysis in endometrial cancer Reviewed

    A Hirasawa, D Aoki, J Inoue, Imoto, I, N Susumu, K Sugano, S Nozawa, J Inazawa

    CLINICAL CANCER RESEARCH   9 ( 15 )   5675 - 5682   2003.11

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    Purpose: Although many articles have been published regarding chromosomal instability (CI) and microsatellite instability (MI) in endometrial adenocarcinoma, the relationship between prognostic factors and the biological mechanisms accounting for genetic instability in these tumors has not yet been precisely defined. To do that, it will be necessary to clarify the molecular mechanisms involved in endometrial carcinogenesis.
    Experimental Design: Tissue samples from 43 human primary endometrioid endometrial adenocarcinomas (EACs) were analyzed for CI and MI status using comparative genomic hybridization And It microsatellite loci, respectively. Methylation status of the promoter of MLH1 was also determined. We analyzed all three of these parameters in relation to each other and to clinicopathological factors.
    Results: Sixty-five percent of the EACs we examined had detectable CI. Frequent copy number gains were seen at 1q25-41 (23%), 8q11.1-q21.1 (23%), 8q21.3-qter (21%); 28% of these tumors exhibited high-frequency MI (MSI-H); Methylation of the MLH1 promoter was observed in 92% of EACs with MSI-H. Southern blotting showed amplification of MYCN in one tumor, which has been documented for the first time in a primary human EAC.
    Conclusions: MSI-H was correlated with histological grade, International Federation of Gynecologists and Obstetricians (FIGO) stage, myometrial invasion, and lymphonode metastasis. Our comparative genomic hybridization results demonstrated that the number of chromosomes involved in genomic alterations in EACs was distinctively fewer than those in other types of tumor. The carcinogenetic process leading to EAC appears to be highly complex; for example, MI and CI may act synergistically, whereas CI and/or MI are likely to be linked with tumor heterogeneity.

    Web of Science

    researchmap

  • Identification of germline MSH2 gene mutations in endometrial cancer not fulfilling the new clinical criteria for hereditary nonpolyposis colorectal cancer. Reviewed International journal

    Kouji Banno, Nobuyuki Susumu, Takeshi Hirao, Megumi Yanokura, Akira Hirasawa, Daisuke Aoki, Yasuhiro Udagawa, Kokichi Sugano, Shiro Nozawa

    Cancer genetics and cytogenetics   146 ( 1 )   58 - 65   2003.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ELSEVIER SCIENCE INC  

    Endometrial cancer is the second most common malignancy in patients with hereditary nonpolyposis colorectal cancer (HNPCC). This cancer is caused by germline mutations in one of the DNA mismatch repair (MMR) genes. The present study was undertaken to analyze the relation between microsatellite instability (MSI) and germline mutations of MMR genes. We analyzed MSI in 38 cases of endometrial cancer. MSI was present in one or more (out of 5 examined) regions in 11 (29%) cases. Furthermore, alterations in MLH1 and MSH2, two culprit genes representative of HNPCC, were examined in the 11 MSI-positive patients using polymerase chain reaction-single-strand conformation polymorphism and sequencing. Germline mutations, namely, 1) a missense mutation at codon 688 (ATG-->ATA, Met-->Ile) and 2) a missense mutation at codon 390 (CTT-->TTT, Leu-->Phe) of the MSH2 gene, were found in 2 of the 11 patients (18%). Although these two cases do not fulfill the new Amsterdam criteria, they had strong family histories of colorectal and endometrial carcinoma. Our results show that genetic testing is important in cases of endometrial cancer with a history suggestive of HNPCC even if the new Amsterdam criteria are not fulfilled.

    DOI: 10.1016/S0165-4608(03)00157-2

    Web of Science

    PubMed

    researchmap

  • Identification of germline MSH2 gene mutations in endometrial cancer not fulfilling the new clinical criteria for hereditary nonpolyposis colorectal cancer

    K Banno, N Susumu, T Hirao, M Yanokura, A Hirasawa, D Aoki, Y Udagawa, K Sugano, S Nozawa

    CANCER GENETICS AND CYTOGENETICS   146 ( 1 )   58 - 65   2003.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ELSEVIER SCIENCE INC  

    Endometrial cancer is the second most common malignancy in patients with hereditary nonpolyposis colorectal cancer (HNPCC). This cancer is caused by germline mutations in one of the DNA mismatch repair (MMR) genes. The present study was undertaken to analyze the relation between microsatellite instability (MSI) and germline mutations of MMR genes. We analyzed MSI in 38 cases of endometrial cancer. MSI was present in one or more (out of 5 examined) regions in 11 (29%) cases. Furthermore, alterations in MLH1 and MSH2, two culprit genes representative of HNPCC, were examined in the 11 MSI-positive patients using polymerase chain reaction-single-strand conformation polymorphism and sequencing. Germline mutations, namely, 1) a missense mutation at codon 688 (ATG--&gt;ATA, Met--&gt;Ile) and 2) a missense mutation at codon 390 (CTT--&gt;TTT, Leu--&gt;Phe) of the MSH2 gene, were found in 2 of the 11 patients (18%). Although these two cases do not fulfill the new Amsterdam criteria, they had strong family histories of colorectal and endometrial carcinoma. Our results show that genetic testing is important in cases of endometrial cancer with a history suggestive of HNPCC even if the new Amsterdam criteria are not fulfilled. (C) 2003 Elsevier Inc. All rights reserved.

    DOI: 10.1016/S0165-4608(03)00157-2

    Web of Science

    researchmap

  • Identification of germline MSH2 gene mutations in endometrial cancer not fulfilling the new clinical criteria for hereditary nonpolyposis colorectal cancer

    K Banno, N Susumu, T Hirao, M Yanokura, A Hirasawa, D Aoki, Y Udagawa, K Sugano, S Nozawa

    CANCER GENETICS AND CYTOGENETICS   146 ( 1 )   58 - 65   2003.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ELSEVIER SCIENCE INC  

    Endometrial cancer is the second most common malignancy in patients with hereditary nonpolyposis colorectal cancer (HNPCC). This cancer is caused by germline mutations in one of the DNA mismatch repair (MMR) genes. The present study was undertaken to analyze the relation between microsatellite instability (MSI) and germline mutations of MMR genes. We analyzed MSI in 38 cases of endometrial cancer. MSI was present in one or more (out of 5 examined) regions in 11 (29%) cases. Furthermore, alterations in MLH1 and MSH2, two culprit genes representative of HNPCC, were examined in the 11 MSI-positive patients using polymerase chain reaction-single-strand conformation polymorphism and sequencing. Germline mutations, namely, 1) a missense mutation at codon 688 (ATG--&gt;ATA, Met--&gt;Ile) and 2) a missense mutation at codon 390 (CTT--&gt;TTT, Leu--&gt;Phe) of the MSH2 gene, were found in 2 of the 11 patients (18%). Although these two cases do not fulfill the new Amsterdam criteria, they had strong family histories of colorectal and endometrial carcinoma. Our results show that genetic testing is important in cases of endometrial cancer with a history suggestive of HNPCC even if the new Amsterdam criteria are not fulfilled. (C) 2003 Elsevier Inc. All rights reserved.

    DOI: 10.1016/S0165-4608(03)00157-2

    Web of Science

    researchmap

  • Identification of germline MSH2 gene mutations in endometrial cancer not fulfilling the new clinical criteria for hereditary nonpolyposis colorectal cancer

    K Banno, N Susumu, T Hirao, M Yanokura, A Hirasawa, D Aoki, Y Udagawa, K Sugano, S Nozawa

    CANCER GENETICS AND CYTOGENETICS   146 ( 1 )   58 - 65   2003.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ELSEVIER SCIENCE INC  

    Endometrial cancer is the second most common malignancy in patients with hereditary nonpolyposis colorectal cancer (HNPCC). This cancer is caused by germline mutations in one of the DNA mismatch repair (MMR) genes. The present study was undertaken to analyze the relation between microsatellite instability (MSI) and germline mutations of MMR genes. We analyzed MSI in 38 cases of endometrial cancer. MSI was present in one or more (out of 5 examined) regions in 11 (29%) cases. Furthermore, alterations in MLH1 and MSH2, two culprit genes representative of HNPCC, were examined in the 11 MSI-positive patients using polymerase chain reaction-single-strand conformation polymorphism and sequencing. Germline mutations, namely, 1) a missense mutation at codon 688 (ATG--&gt;ATA, Met--&gt;Ile) and 2) a missense mutation at codon 390 (CTT--&gt;TTT, Leu--&gt;Phe) of the MSH2 gene, were found in 2 of the 11 patients (18%). Although these two cases do not fulfill the new Amsterdam criteria, they had strong family histories of colorectal and endometrial carcinoma. Our results show that genetic testing is important in cases of endometrial cancer with a history suggestive of HNPCC even if the new Amsterdam criteria are not fulfilled. (C) 2003 Elsevier Inc. All rights reserved.

    DOI: 10.1016/S0165-4608(03)00157-2

    Web of Science

    researchmap

  • 遺伝性子宮内膜癌とは −特にDNAミスマッチ修復遺伝子について

    阪埜浩司, 進 伸幸, 矢野倉恵, 平尾 健, 岩田 卓, 平沢 晃, 青木大輔, 野澤志朗

    産婦人科の世界   55 ( 8 )   863-870 - 870   2003.8

     More details

    Language:Japanese  

    researchmap

  • Association of 17q21-q24 gain in ovarian clear cell adenocarcinomas with poor prognosis and identification of PPM1D and APPBP2 as likely amplification targets

    A Hirasawa, F Saito-Ohara, J Inoue, D Aoki, N Susumu, T Yokoyama, S Nozawa, J Inazawa, Imoto, I

    CLINICAL CANCER RESEARCH   9 ( 6 )   1995 - 2004   2003.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    Purpose: Although tumor stage is considered a prognostic feature for ovarian clear cell adenocarcinomas (OC- CAs), it is not likely to fully account for the clinical and biological variability characteristic of the disease. The aim of this study was to investigate aberrations of DNA copy number in OCCA tumors and identify genetic markers that would increase our understanding of the pathogenesis of OCCA and assist in more accurately predicting the outcome for an individual patient with this disease.
    Experimental Design: We determined copy number aberrations among 20 primary OCCA tumors by means of comparative genomic hybridization and investigated their relationship to clinicopathological data. We also measured expression levels of candidate target genes within critical regions by quantitative real-time reverse transcription-PCRs and compared those data with copy number status and patient outcomes.
    Results: We identified several nonrandom chromosomal aberrations among the 20 primary OCCA tumors examined. Among them, gain of DNA at 17q21-q24 showed significantly negative correlation with disease-free and overall survival (P = 0.0012 and 0.0039, respectively, log-rank test). This correlation held even for patients with stage I tumors. Among 15 candidate genes within the 17q21-q24 region, we found significantly elevated expression of PPM1D and APPBP2, and their heightened expression correlated negatively with disease-free survival (P = 0.0090, log-rank test adjusted for multiple comparisons).
    Conclusions: Information gained from our relatively large panel of OCCA tumors suggested that 17q21-q24 gain and consequent overexpression of two potential targets, PPM1D and APPBP2, are associated with malignant phenotypes of this tumor and may be useful predictors for prognosis.

    Web of Science

    researchmap

  • Association of 17q21-q24 gain in ovarian clear cell adenocarcinomas with poor prognosis and identification of PPM1D and APPBP2 as likely amplification targets

    A Hirasawa, F Saito-Ohara, J Inoue, D Aoki, N Susumu, T Yokoyama, S Nozawa, J Inazawa, Imoto, I

    CLINICAL CANCER RESEARCH   9 ( 6 )   1995 - 2004   2003.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    Purpose: Although tumor stage is considered a prognostic feature for ovarian clear cell adenocarcinomas (OC- CAs), it is not likely to fully account for the clinical and biological variability characteristic of the disease. The aim of this study was to investigate aberrations of DNA copy number in OCCA tumors and identify genetic markers that would increase our understanding of the pathogenesis of OCCA and assist in more accurately predicting the outcome for an individual patient with this disease.
    Experimental Design: We determined copy number aberrations among 20 primary OCCA tumors by means of comparative genomic hybridization and investigated their relationship to clinicopathological data. We also measured expression levels of candidate target genes within critical regions by quantitative real-time reverse transcription-PCRs and compared those data with copy number status and patient outcomes.
    Results: We identified several nonrandom chromosomal aberrations among the 20 primary OCCA tumors examined. Among them, gain of DNA at 17q21-q24 showed significantly negative correlation with disease-free and overall survival (P = 0.0012 and 0.0039, respectively, log-rank test). This correlation held even for patients with stage I tumors. Among 15 candidate genes within the 17q21-q24 region, we found significantly elevated expression of PPM1D and APPBP2, and their heightened expression correlated negatively with disease-free survival (P = 0.0090, log-rank test adjusted for multiple comparisons).
    Conclusions: Information gained from our relatively large panel of OCCA tumors suggested that 17q21-q24 gain and consequent overexpression of two potential targets, PPM1D and APPBP2, are associated with malignant phenotypes of this tumor and may be useful predictors for prognosis.

    Web of Science

    researchmap

  • Association of 17q21-q24 gain in ovarian clear cell adenocarcinomas with poor prognosis and identification of PPM1D and APPBP2 as likely amplification targets Reviewed

    A Hirasawa, F Saito-Ohara, J Inoue, D Aoki, N Susumu, T Yokoyama, S Nozawa, J Inazawa, Imoto, I

    CLINICAL CANCER RESEARCH   9 ( 6 )   1995 - 2004   2003.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    Purpose: Although tumor stage is considered a prognostic feature for ovarian clear cell adenocarcinomas (OC- CAs), it is not likely to fully account for the clinical and biological variability characteristic of the disease. The aim of this study was to investigate aberrations of DNA copy number in OCCA tumors and identify genetic markers that would increase our understanding of the pathogenesis of OCCA and assist in more accurately predicting the outcome for an individual patient with this disease.
    Experimental Design: We determined copy number aberrations among 20 primary OCCA tumors by means of comparative genomic hybridization and investigated their relationship to clinicopathological data. We also measured expression levels of candidate target genes within critical regions by quantitative real-time reverse transcription-PCRs and compared those data with copy number status and patient outcomes.
    Results: We identified several nonrandom chromosomal aberrations among the 20 primary OCCA tumors examined. Among them, gain of DNA at 17q21-q24 showed significantly negative correlation with disease-free and overall survival (P = 0.0012 and 0.0039, respectively, log-rank test). This correlation held even for patients with stage I tumors. Among 15 candidate genes within the 17q21-q24 region, we found significantly elevated expression of PPM1D and APPBP2, and their heightened expression correlated negatively with disease-free survival (P = 0.0090, log-rank test adjusted for multiple comparisons).
    Conclusions: Information gained from our relatively large panel of OCCA tumors suggested that 17q21-q24 gain and consequent overexpression of two potential targets, PPM1D and APPBP2, are associated with malignant phenotypes of this tumor and may be useful predictors for prognosis.

    Web of Science

    researchmap

  • Association of 17q21-q24 gain in ovarian clear cell adenocarcinomas with poor prognosis and identification of PPM1D and APPBP2 as likely amplification targets. International journal

    Akira Hirasawa, Fumiko Saito-Ohara, Jun Inoue, Daisuke Aoki, Nobuyuki Susumu, Tetsuji Yokoyama, Shiro Nozawa, Johji Inazawa, Issei Imoto

    Clinical cancer research : an official journal of the American Association for Cancer Research   9 ( 6 )   1995 - 2004   2003.6

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    PURPOSE: Although tumor stage is considered a prognosticfeature for ovarian clear cell adenocarcinomas (OCCAs), it is not likely to fully account for the clinical and biological variability characteristic of the disease. The aim of this study was to investigate aberrations of DNA copy number in OCCA tumors and identify genetic markers that would increase our understanding of the pathogenesis of OCCA and assist in more accurately predicting the outcome for an individual patient with this disease. EXPERIMENTAL DESIGN: We determined copy number aberrations among 20 primary OCCA tumors by means of comparative genomic hybridization and investigated their relationship to clinicopathological data. We also measured expression levels of candidate target genes within critical regions by quantitative real-time reverse transcription-PCRs and compared those data with copy number status and patient outcomes. RESULTS: We identified several nonrandom chromosomal aberrations among the 20 primary OCCA tumors examined. Among them, gain of DNA at 17q21-q24 showed significantly negative correlation with disease-free and overall survival (P = 0.0012 and 0.0039, respectively, log-rank test). This correlation held even for patients with stage I tumors. Among 15 candidate genes within the 17q21-q24 region, we found significantly elevated expression of PPM1D and APPBP2, and their heightened expression correlated negatively with disease-free survival (P = 0.0090, log-rank test adjusted for multiple comparisons). CONCLUSIONS: Information gained from our relatively large panel of OCCA tumors suggested that 17q21-q24 gain and consequent overexpression of two potential targets, PPM1D and APPBP2, are associated with malignant phenotypes of this tumor and may be useful predictors for prognosis.

    Web of Science

    PubMed

    researchmap

  • HNPCCの診療と研究 遺伝性非腺腫症性大腸癌(HNPCC)と子宮内膜癌

    阪埜浩司, 進 伸幸, 平尾 健, 岩田 卓, 平沢 晃, 青木大輔, 野澤志朗

    家族性腫瘍   3 ( 2 )   62-67 - 67   2003.5

  • 子宮体癌におけるMicrosatellite Instability(MSI)の検出に免疫組織化学は有用か?

    進, 伸幸, 青木, 大輔, 阪埜, 浩司, 平尾, 健, 平沢, 晃, 岩田, 卓, 鈴木, 直, 菅野, 康吉, 向井, 万起男, 野澤, 志朗

    日本婦人科腫瘍学会雑誌   21 ( 3 )   208 - 208   2003

     More details

    Language:Japanese  

    researchmap

  • Differentially regulated genes as putative targets of amplifications at 20q in ovarian cancers Reviewed

    Watanabe T, Imoto I, Katahira T, Hirasawa A, Ishiwata I, Emi M, Takayama M, Sato A, Inazawa J

    Jpn J Cancer Res   93 ( 10 )   1114-1122   2003

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • 子宮体癌におけるMicrosatellite Instabilityと薬剤感受性試験によるcisplatin感受性との関連

    進, 伸幸, 青木, 大輔, 阪埜, 浩司, 平尾, 健, 岩田, 卓, 平沢, 晃, 金杉, 優, 鈴木, 直, 菅野, 康吉, 宇田川, 康博, 吉村, 泰典, 野澤, 志朗

    日本産科婦人科学会雑誌   55 ( 2 )   186 - 186   2003

     More details

    Language:Japanese  

    researchmap

  • Differentially regulated genes as putative targets of amplifications at 20q in ovarian cancers.

    Takafumi Watanabe, Issei Imoto, Tomoyuki Katahira, Akira Hirasawa, Isamu Ishiwata, Mitsuru Emi, Masaomi Takayama, Akira Sato, Johji Inazawa

    Japanese journal of cancer research : Gann   93 ( 10 )   1114 - 22   2002.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BUSINESS CENTER ACADEMIC SOCIETIES JAPAN  

    Frequent amplification of DNA at 20q or part of 20q has been demonstrated by comparative genomic hybridization in ovarian cancer (OC), but the genetic target(s) of these amplification events remain unknown. We examined copy-number changes with respect to six candidate genes, E2F1 (20q11.2), TGIF2 (20q11.2), AIB1 (20q12), PTPN1 (20q13.1), ZNF217 (20q13.2), and BTAK (20q13), and then measured transcription levels of each candidate in 18 OC cell lines. Three distinct cores of amplification were identified: 20q11.2, harboring E2F1 and TGIF2 (region I; 1 of 18 cell lines, 5.6%); 20q13.1, harboring PTPN1 (region II; 5 lines, 27.8%); and 20q13.2, harboring ZNF217 and BTAK (region III; 6 lines, 33.3%). Among the six genes examined, expression levels of PTPN1 and ZNF217 were significantly correlated with absolute copy-number, and those of PTPN1 and TGIF2 were significantly correlated with copy-number relative to the centromere of chromosome 20 (20cen). Among 19 primary OCs examined, moreover, we observed amplification of TGIF2, PTPN1 and ZNF217 in five (26.3%), ten (52.6%), and twelve (63.2%) tumors, respectively. Expression levels of PTPN1 and ZNF217 were significantly correlated with their copy-numbers in those primary OCs. Our results suggest that 20q amplifications in OCs can be extensive and complex, probably due to synergistic or non-synergistic amplification of separate regions of 20q, involving multiple, independently amplified targets.

    Web of Science

    PubMed

    researchmap

  • 婦人科癌とDNAミスマッチ修復遺伝子―HNPCCに関する婦人科癌を中心として―

    Aoki Daisuke, Hirasawa Akira, Susumu Nobuyuki, Nozawa Shirou

    産婦人科の実際   51 ( 10 )   1361-1368 - 1368   2002.10

     More details

    Language:Japanese  

    researchmap

  • Differentially regulated genes as putative targets of amplifications at 20q in ovarian cancers

    T Watanabe, Imoto, I, T Katahira, A Hirasawa, Ishiwata, I, M Emi, M Takayama, A Sato, J Inazawa

    JAPANESE JOURNAL OF CANCER RESEARCH   93 ( 10 )   1114 - 1122   2002.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:BUSINESS CENTER ACADEMIC SOCIETIES JAPAN  

    Frequent amplification of DNA at 20q or part of 20q has been demonstrated by comparative genomic hybridization in ovarian cancer (OC), but the genetic target(s) of these amplification events remain unknown. We examined copy-number changes with respect to six candidate genes, E2F1 (20q11.2), TGIF2 (20q11.2), AIB1 (20q12), PTPN1 (20q13.1), ZNF217 (20q13.2), and BTAK (20q13), and then measured transcription levels of each candidate in 18 OC cell lines. Three distinct cores of amplification were identified: 20q11.2, harboring E2F1 and TGIF2 (region I; I of 18 cell lines, 5.6%); 20q13.1, harboring PTPN1 (region H; 5 lines, 27.8%); and 20q13.2, harboring ZNF217 and BTAK (region 111; 6 lines, 33.3%). Among the six genes examined, expression levels of PTPN1 and ZNF217 were significantly correlated with absolute copy-number, and those of PTPN1 and TGIF2 were significantly correlated with copy-number relative to the centromere of chromosome 20 (20cen). Among 19 primary OCs examined, moreover, we observed amplification of TGIF2, PTPN1 and ZNF217 in five (26.3%), ten (52.6%), and twelve (63.2%) tumors, respectively. Expression levels of PTPN1 and ZNF217 were significantly correlated with their copy-numbers in those primary OCs. Our results suggest that 20q amplifications in OCs can be extensive and complex, probably due to synergistic or non-synergistic amplification of separate regions of 20q, involving multiple, independently amplified targets.

    Web of Science

    researchmap

  • Expression of cIAP1, a target for 11q22 amplification, correlates with resistance of cervical cancers to radiotherapy. Reviewed International journal

    Issei Imoto, Hitoshi Tsuda, Akira Hirasawa, Masahiko Miura, Masaru Sakamoto, Setsuo Hirohashi, Johji Inazawa

    Cancer research   62 ( 17 )   4860 - 6   2002.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    Inhibition of, or increased resistance to, apoptosis is a common property of cancer cells. This means that a constitutive activation of antiapoptotic molecules via genetic or epigenetic mechanisms, including gene amplification, may well be involved in carcinogenesis. Recently we reported that cIAP1, an inhibitor of apoptosis, is overexpressed through 11q22 amplification in cell lines derived from esophageal squamous cell carcinomas and is associated with resistance of esophageal squamous cell carcinomas to drug-induced apoptosis (I. Imoto et al. Cancer Res., 61: 6629-6634, 2001). Because amplification of 11q22 has been implicated in other malignancies also, including cervical squamous cell carcinomas (CSCCs), we attempted to correlate amplification and overexpression of cIAP1 with radiation sensitivity in CSCC-derived cell lines and primary CSCC tumors. In the nine cell lines we examined, two showed amplification and consistent overexpression of cIAP1, as well as significant resistance to radiation-induced cell death as compared with lines showing no cIAP1 amplification. Immunohistochemical analysis of 70 primary CSCCs from patients treated only with radiotherapy demonstrated that both overall survival and local recurrence-free survival was significantly poorer among patients with tumors showing high levels of nuclear cIAP1 staining than among patients whose tumors revealed little or no nuclear cIAP1. Multivariate analysis showed nuclear cIAP1 staining to be an independent predictive factor for local recurrence-free survival after radiotherapy among patients with CSCC. These findings demonstrate that cIAP1 may play an important role in the development/progression of this disease and that cIAP1 could be a novel predictive marker for resistance to radiotherapy in individual CSCC patients.

    Web of Science

    PubMed

    researchmap

  • Expression of cIAP1, a target for 11q22 amplification, correlates with resistance of cervical cancers to radiotherapy

    Imoto, I, H Tsuda, A Hirasawa, M Miura, M Sakamoto, S Hirohashi, J Inazawa

    CANCER RESEARCH   62 ( 17 )   4860 - 4866   2002.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    Inhibition of, or increased resistance to, apoptosis is a common property of cancer cells. This means that a constitutive activation of antiapoptotic molecules via genetic or epigenetic mechanisms, including gene amplification, may well be involved in carcinogenesis. Recently we reported that cIAP1, an inhibitor of apoptosis, is overexpressed through 11q22 amplification in cell lines derived from esophageal squamous cell carcinomas and is associated with resistance of esophageal squamous cell carcinomas to drug-induced apoptosis (I. Imoto et al. Cancer Res., 67: 6629-6634, 2001). Because amplification of 11q22 has been implicated in other malignancies also, including cervical squamous cell carcinomas (CSCCs), we attempted to correlate amplification and overexpression of cIAP1 with radiation sensitivity in CSCC-derived cell lines and primary CSCC tumors. In the nine cell lines we examined, two showed amplification and consistent overexpression of cIAP1, as well as significant resistance to radiation-induced cell death as compared with lines showing no cIAP1 amplification. Immunohistochemical analysis of 70 primary CSCCs from patients treated only with radiotherapy demonstrated that both overall survival and local recurrence-free survival was significantly poorer among patients with tumors showing high levels of nuclear cIAP1 staining than among patients whose tumors revealed little or no nuclear cIAP1. Multivariate analysis showed nuclear cIAP1 staining to be an independent predictive factor for local recurrence-free survival after radiotherapy among patients with CSCC. These findings demonstrate that cIAP1 may play an important role in the development/progression of this disease and that cIAP1 could be a novel predictive marker for resistance to radiotherapy in individual CSCC patients.

    Web of Science

    researchmap

  • Expression of cIAP1, a target for 11q22 amplification, correlates with resistance of cervical cancers to radiotherapy

    Imoto, I, H Tsuda, A Hirasawa, M Miura, M Sakamoto, S Hirohashi, J Inazawa

    CANCER RESEARCH   62 ( 17 )   4860 - 4866   2002.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER ASSOC CANCER RESEARCH  

    Inhibition of, or increased resistance to, apoptosis is a common property of cancer cells. This means that a constitutive activation of antiapoptotic molecules via genetic or epigenetic mechanisms, including gene amplification, may well be involved in carcinogenesis. Recently we reported that cIAP1, an inhibitor of apoptosis, is overexpressed through 11q22 amplification in cell lines derived from esophageal squamous cell carcinomas and is associated with resistance of esophageal squamous cell carcinomas to drug-induced apoptosis (I. Imoto et al. Cancer Res., 67: 6629-6634, 2001). Because amplification of 11q22 has been implicated in other malignancies also, including cervical squamous cell carcinomas (CSCCs), we attempted to correlate amplification and overexpression of cIAP1 with radiation sensitivity in CSCC-derived cell lines and primary CSCC tumors. In the nine cell lines we examined, two showed amplification and consistent overexpression of cIAP1, as well as significant resistance to radiation-induced cell death as compared with lines showing no cIAP1 amplification. Immunohistochemical analysis of 70 primary CSCCs from patients treated only with radiotherapy demonstrated that both overall survival and local recurrence-free survival was significantly poorer among patients with tumors showing high levels of nuclear cIAP1 staining than among patients whose tumors revealed little or no nuclear cIAP1. Multivariate analysis showed nuclear cIAP1 staining to be an independent predictive factor for local recurrence-free survival after radiotherapy among patients with CSCC. These findings demonstrate that cIAP1 may play an important role in the development/progression of this disease and that cIAP1 could be a novel predictive marker for resistance to radiotherapy in individual CSCC patients.

    Web of Science

    researchmap

  • 子宮体癌に対する手術療法

    HIRASAWA AKIRA

    日本婦人科腫瘍学会雑誌   20 ( 1 )   26-32 - 32   2002

     More details

    Language:Japanese  

    researchmap

  • 子宮内膜癌におけるマイクロサテライト不安定性とhMLH1蛋白発現低下との関連

    阪埜, 浩司, 進, 伸幸, 平沢, 晃, 金杉, 優, 岩田, 卓, 鈴木, 直, 青木, 大輔, 菅野, 康吉, 吉村, 泰典, 野澤, 志朗

    日本産科婦人科学会雑誌   54 ( 2 )   325 - 325   2002

     More details

    Language:Japanese  

    researchmap

  • 子宮内膜癌におけるマイクロサテライト不安定性とhMLH1蛋白発現低下との関連

    阪埜, 浩司, 進, 伸幸, 平沢, 晃, 金杉, 優, 岩田, 卓, 青木, 大輔, 菅野, 康吉, 野澤, 志朗

    家族性腫瘍   2 ( 2 )   A43 - A43   2002

     More details

    Language:Japanese  

    researchmap

  • 遺伝性非腺腫性大腸癌(HNPCC)と婦人科癌

    Banno Kouji, Nikata Masanobu, Hirasawa Akira, Susumu Nobuyuki, Aoki Daisuke, Udagawa Yasuhiro, Nozawa Shirou

    産婦人科の実際   50 ( 12 )   1819-1826 - 1826   2001.11

     More details

    Language:Japanese  

    researchmap

  • 卵巣明細胞腺癌におけるPAI-1発現の生物学的意義

    Komiyama Shinichi, Aoki Daisuke, Kanasugi Masaru, Hirasawa Akira, Susumu Nobuyuki, Nozawa Shirou

    日本分子腫瘍マーカー研究会誌   16   48-49   2001.9

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 最近当科で経験したadenoma malignumの3例

    HIRASAWA AKIRA

    日本産婦人科学会東京地方部会誌   50   94-98   2001

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • わが教室における腫瘍マーカー検査

    Hirasawa Akira, Aoki Daisuke, Udagawa Yasuhiro, Nozawa Shiro

    産婦人科治療   79 ( 6 )   680-685 - 685   1999.12

     More details

    Language:Japanese  

    researchmap

  • Genetic analysis of chromosome 17 and 1 in cervical cancers using fluorescencein situ hybridization and RFLP-Southern Blot

    Susumu Nobuyuki, Tsuda Hitoshi, Aoki Daisuke, Udagawa Yasuhiro, Hirasawa A, Kanasugi Masaru, Nozawa Shiro

    International Journal of Gynecological Cancer   9 ( Suppl 1 )   101-102   1999.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • The relationship between MSN-1-reactive carbohydrate antigens and α-1,2 fucosyltransferase genes expressed in endometrial adenocarcinoma

    Tominaga Eiichiro, Aoki Daisuke, Hirasawa Akira, Setoh Eri, Susumu Nobuyuki, Udagawa Yasuhiro, Nozawa Shiro

    International Journal of Gynecological Cancer   9 ( Suppl 1 )   68-69   1999.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)  

    researchmap

  • Two soluble forms of beta 1,4-galactosyltransferase released from ovarian cancer cells and from COS-1 cells transfected with its cDNA

    D Aoki, E Saitoh, Y Matsumoto, E Tominaga, A Hirasawa, N Susumu, Y Udagawa, S Nozawa

    ACTA HISTOCHEMICA ET CYTOCHEMICA   32 ( 3 )   209 - 214   1999

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:JAPAN SOC HISTOCHEMISTRY & CYTOCHEMISTRY  

    Employing RMG-1 cells derived from human ovarian adenocarcinoma and COS-1 cells transfected with cDNA for beta 1,4-galactosyltransferase, we first investigated the intracellular localization of this enzyme anal secondly assayed separately the two types of soluble forms of it (designated as normal GalT and GAT) in their culture supernatants. As results, the binding of anti-beta 1,4-galactosyltransferase monoclonal antibody was strongly positive at the Golgi area surrounding nuclei and the staining pattern was the same between RMG-1 cells and COS-1 transformants. These data demonstrated that the cells were producing beta 1,4-galactosyltransferase and had the ability to release it into the culture medium. As for the two soluble farms released from the cells, they were simultaneously detected in the culture medium by Western blotting and enzyme immunoassay using monoclonal antibodies, i.e., Mab8628 reactive to both GAT and normal-GalT and Mab8513 specific for GAT, indicating that both were derived from RMG-1 and from the cDNA introduced into COS-1 cells. Since serum-GAT clinically reflects tumor growth more accurately or specifically than normal GalT does, RMG-1 and COS-1 cells having cDNA for beta 1,4-galactosyltransferase would be promising as sources of these enzymes in order to investigate the differences in the behaviors of normal GalT and GAT associated with ovarian malignant tumors.

    DOI: 10.1267/ahc.32.209

    Web of Science

    researchmap

  • Two soluble forms of beta 1,4-galactosyltransferase released from ovarian cancer cells and from COS-1 cells transfected with its cDNA

    D Aoki, E Saitoh, Y Matsumoto, E Tominaga, A Hirasawa, N Susumu, Y Udagawa, S Nozawa

    ACTA HISTOCHEMICA ET CYTOCHEMICA   32 ( 3 )   209 - 214   1999

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:JAPAN SOC HISTOCHEMISTRY & CYTOCHEMISTRY  

    Employing RMG-1 cells derived from human ovarian adenocarcinoma and COS-1 cells transfected with cDNA for beta 1,4-galactosyltransferase, we first investigated the intracellular localization of this enzyme anal secondly assayed separately the two types of soluble forms of it (designated as normal GalT and GAT) in their culture supernatants. As results, the binding of anti-beta 1,4-galactosyltransferase monoclonal antibody was strongly positive at the Golgi area surrounding nuclei and the staining pattern was the same between RMG-1 cells and COS-1 transformants. These data demonstrated that the cells were producing beta 1,4-galactosyltransferase and had the ability to release it into the culture medium. As for the two soluble farms released from the cells, they were simultaneously detected in the culture medium by Western blotting and enzyme immunoassay using monoclonal antibodies, i.e., Mab8628 reactive to both GAT and normal-GalT and Mab8513 specific for GAT, indicating that both were derived from RMG-1 and from the cDNA introduced into COS-1 cells. Since serum-GAT clinically reflects tumor growth more accurately or specifically than normal GalT does, RMG-1 and COS-1 cells having cDNA for beta 1,4-galactosyltransferase would be promising as sources of these enzymes in order to investigate the differences in the behaviors of normal GalT and GAT associated with ovarian malignant tumors.

    DOI: 10.1267/ahc.32.209

    Web of Science

    researchmap

  • Two soluble forms of beta 1,4-galactosyltransferase released from ovarian cancer cells and from COS-1 cells transfected with its cDNA

    D Aoki, E Saitoh, Y Matsumoto, E Tominaga, A Hirasawa, N Susumu, Y Udagawa, S Nozawa

    ACTA HISTOCHEMICA ET CYTOCHEMICA   32 ( 3 )   209 - 214   1999

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:JAPAN SOC HISTOCHEMISTRY & CYTOCHEMISTRY  

    Employing RMG-1 cells derived from human ovarian adenocarcinoma and COS-1 cells transfected with cDNA for beta 1,4-galactosyltransferase, we first investigated the intracellular localization of this enzyme anal secondly assayed separately the two types of soluble forms of it (designated as normal GalT and GAT) in their culture supernatants. As results, the binding of anti-beta 1,4-galactosyltransferase monoclonal antibody was strongly positive at the Golgi area surrounding nuclei and the staining pattern was the same between RMG-1 cells and COS-1 transformants. These data demonstrated that the cells were producing beta 1,4-galactosyltransferase and had the ability to release it into the culture medium. As for the two soluble farms released from the cells, they were simultaneously detected in the culture medium by Western blotting and enzyme immunoassay using monoclonal antibodies, i.e., Mab8628 reactive to both GAT and normal-GalT and Mab8513 specific for GAT, indicating that both were derived from RMG-1 and from the cDNA introduced into COS-1 cells. Since serum-GAT clinically reflects tumor growth more accurately or specifically than normal GalT does, RMG-1 and COS-1 cells having cDNA for beta 1,4-galactosyltransferase would be promising as sources of these enzymes in order to investigate the differences in the behaviors of normal GalT and GAT associated with ovarian malignant tumors.

    DOI: 10.1267/ahc.32.209

    Web of Science

    researchmap

  • 子宮肉腫の2症例

    HIRASAWA AKIRA

    栃木県産婦人科医報   25 ( 1 )   40-42 - 42   1998

     More details

    Language:Japanese  

    researchmap

  • 診断に苦慮した子宮頸部原発絨毛癌の1例

    HIRASAWA AKIRA

    栃木県産婦人科医報   25 ( 2 )   113-116 - 116   1998

     More details

    Language:Japanese  

    researchmap

  • 子宮体部に発生した癌肉腫の2例

    HIRASAWA AKIRA

    日本産科婦人科学会埼玉地方部会会誌   28   76-80   1998

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

  • 当院における最近6年間の子宮体癌症例の予後因子について

    HIRASAWA AKIRA

    日本産科婦人科学会埼玉地方部会会誌   27   18-22 - 22   1997

     More details

    Language:Japanese  

    researchmap

  • 産褥期MRSAによる敗血症ショックを来した2症例.

    HIRASAWA AKIRA

    日本産科婦人科学会埼玉地方部会会誌   27   42-46   1997

     More details

    Language:Japanese   Publishing type:Research paper (scientific journal)  

    researchmap

▼display all

Books

  • がん遺伝子パネル検査結果の取り扱いと解釈 Germline findingsの取り扱い

    坂井美佳, 竹原和宏, 平沢 晃( Role: Joint author)

    産婦人科の実際  2020.7 

     More details

  • 岡山大学のエキスパートパネル. ゲノム医療におけるエキスパートパネル

    柳井広之, 都地知紘, 谷口恒平, 西田賢司, 井上博文, 松岡博美, 平沢 晃, 河内麻里子, 山本英喜, 冨田秀太, 遠西大輔( Role: Joint author)

    病理と臨床  2020.6 

     More details

  • ゲノム医療におけるデータサイエンティストの役割と育成.

    冨田秀太, 森田瑞樹, 山下範之, 平沢 晃, 豊岡伸一( Role: Joint author)

    YAKUGAKU ZASSHI  2020.5 

     More details

  • 卵巣がんに対するコンパニオン診断の使い方

    平沢 晃( Role: Sole author)

    臨床婦人科産科  2020.4 

     More details

  • がんクリニカルシーケンスと生殖細胞系列バリアントへの対応

    平沢 晃( Role: Sole author)

    日本婦人科腫瘍学会雑誌  2020.2 

     More details

  • HBOC女性における卵巣摘出と乳がんリスク

    平沢 晃

    日本婦人科腫瘍学会・日本産婦人科乳腺医学会・日本女性医学会編  2020.1 

     More details

  • 遺伝性腫瘍とがん予防.

    平沢 晃( Role: Sole author)

    岡山医学会雑誌  2020.1 

     More details

  • がんゲノム医療実用化 岡山大学病院臨床遺伝子診療科の紹介.

    平沢 晃

    岡山医学会雑誌  2020.1 

     More details

  • がんゲノム医療が婦人科実地臨床に本格導入される際の留意点は?

    平沢 晃( Role: Sole author)

    日本医事新報  2020.1 

     More details

  • がんゲノム医療時代の幕開け

    中谷 中, 平沢 晃, 谷田部 恭, 宮地 勇人

    モダンメディア  2020.1 

     More details

  • マイクロサテライト不安定性検査. やさしくわかる産科婦人科検査マスターブック

    平沢 晃( Role: Sole author)

    産科と婦人科  2020 

     More details

  • がんゲノム医療における遺伝子パネル検査と遺伝性腫瘍.

    平沢 晃( Role: Sole author)

    Urology Today  2020 

     More details

  • 受けたい医療2019年度版

    HIRASAWA AKIRA( Role: Joint author ,  特集がんゲノム医療)

    読売新聞社  2019.9 

     More details

  • 臨床雑誌9 内科

    HIRASAWA AKIRA( Role: Joint author ,  第5章産婦人科 1903-1906)

    南江堂  2019.9 

     More details

  • 実験医学

    HIRASAWA AKIRA( Role: Joint author ,  2645-2650)

    羊土社  2019.9 

     More details

  • 性ホルモン低下療法に続発する骨粗鬆症. 産婦人科医のための骨粗鬆症診療実践ハンドブック.

    横田めぐみ, 平沢 晃, 青木大輔( Role: Joint author)

    中外医学社  2018.1 

     More details

  • 乳がんに対する内分泌療法に続発する骨粗鬆症

    横田めぐみ, 平沢 晃, 青木大輔

    2018.1 

     More details

  • 遺伝性乳がん・卵巣がんの基礎と臨床

    鶴田智彦, 平沢 晃, 青木大輔( Role: Joint author ,  142-146)

    東京  2012.6 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 遺伝性乳がん・卵巣がんの基礎と臨床

    鶴田智彦, 平沢 晃, 青木大輔( Role: Joint author ,  137-141)

    東京  2012.6 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • CANCER OF THE UTERINE ENDOMETRIUM - ADVANCES AND CONTROVERSIES

    Susumu N, Nomura H, Yamagami W, Hirasawa A, Banno K, Tsuda H, Sagae S, Aoki D( Role: Joint author ,  167-182)

    Croatia  2012.2  ( ISBN:9789535101420

     More details

    Language:English Book type:Scholarly book

    researchmap

  • 日本臨床

    平沢 晃, 鶴田智彦, 阪埜浩司, 進 伸幸, 青木大輔( Role: Joint author ,  292-296)

    2012 

     More details

    Language:Japanese

    researchmap

  • Germline Findings Through Precision Oncology for Ovarian Cancer

    Mika Okazawa-Sakai, Akira Hirasawa( Role: Joint author)

    Springer Link  2011.11 

     More details

  • Repair and Human Health

    Masuda K, Banno K, Yanokura M, Kisu I, Ueki A, Ono A, Kobayashi Y, Nomura H, Hirasawa A, Susumu N, Aoki D( Role: Joint author ,  485-494)

    Croatia  2011.10 

     More details

    Language:English Book type:Scholarly book

    researchmap

  • 臨床婦人科産科

    牧田和也, 平沢 晃, 青木大輔( Role: Sole author ,  568-571)

    2011 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 腫瘍内科

    山上 亘, 進 伸幸, 津田浩史, 平沢 晃, 阪埜浩司, 青木大輔( Role: Sole author ,  563-571)

    2011 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • がん看護

    平沢 晃, 青木大輔( Role: Sole author ,  631-635)

    2011 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • NCCN腫瘍学臨床診療ガイドライン

    平沢 晃, 青木大輔( Role: Sole translator)

    2011 

     More details

    Language:Japanese

    researchmap

  • 遺伝性婦人科癌 リスク・予防・マネジメント

    平沢 晃( Role: Sole author ,  73-84)

    2011 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科の実際

    平沢 晃, 鶴田智彦, 青木大輔( Role: Sole author ,  1331-1338)

    2011 

     More details

    Language:Japanese

    researchmap

  • 婦人科がん化学療法ハンドブック.

    進 伸幸, 平沢 晃, 阪埜浩司, 青木大輔( Role: Sole author ,  96-99)

    2011 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 家族性腫瘍

    平沢 晃, 鶴田智彦, 阪埜浩司, 進 伸幸, 三須久美子, 矢崎久妙子, 武田祐子, 菅野康吉, 青木大輔( Role: Sole author ,  48-51)

    2011 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • Surgery Frontier

    平沢 晃, 青木大輔( Role: Sole author ,  52-55)

    2011 

     More details

    Language:Japanese

    researchmap

  • 遺伝性婦人科癌 リスク・予防・マネジメント

    青木大輔, 平沢 晃( Role: Sole author ,  1-12)

    2011 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産科と婦人科

    平沢 晃, 青木大輔( Role: Sole author ,  1064-1068)

    2011 

     More details

    Language:Japanese

    researchmap

  • 産婦人科治療

    牧田和也, 平沢 晃, 青木大輔( Role: Sole author ,  417-421)

    2011 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 患者さんとご家族のための子宮頸がん・体がん・卵巣がん治療ガイドラインの解説.

    平沢 晃( Role: Sole author ,  178-182)

    2010 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科治療

    牧田和也, 平沢 晃, 青木大輔( Role: Sole author ,  135-139)

    2010 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 乳癌の臨床

    平沢 晃, 野村弘行, 青木大輔( Role: Sole author ,  523-527)

    2010 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科の実際

    進 伸幸, 片岡史夫, 野村弘行, 平沢 晃, 藤井多久磨, 青木大輔( Role: Sole author ,  1195-1200)

    2010 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科の実際

    平沢 晃, 青木大輔( Role: Sole author ,  2005-2011)

    2009 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科治療

    牧田和也, 平沢 晃, 高松 潔, 青木大輔( Role: Sole author ,  509-511)

    2009 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 小児科

    平沢 晃, 鶴田智彦, 進 伸幸, 青木大輔( Role: Sole author ,  1227-1232)

    2009 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • The Mainichi Medical Journal

    HIRASAWA AKIRA( Role: Sole author ,  104-105)

    2009 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 婦人科がん標準化学療法の実際

    HIRASAWA AKIRA( Role: Sole author ,  90-94)

    2008 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 臨床腫瘍プラクティス

    HIRASAWA AKIRA( Role: Sole author ,  4(4)313-319)

    2008 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 臨床腫瘍プラクティス4(4)

    HIRASAWA AKIRA( Role: Sole author ,  313-319)

    2008 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 内分泌療法

    HIRASAWA AKIRA( Role: Sole author ,  74-79)

    2008 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 組織細胞化学 2008

    HIRASAWA AKIRA( Role: Sole author ,  177-186)

    2008 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 婦人科がん標準化学療法の実際 内分泌療法

    HIRASAWA AKIRA( Role: Sole author ,  74-79)

    2008 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科の世界 2006特別増刊号 産婦人外来診療マニュアル

    HIRASAWA AKIRA( Role: Sole author ,  128-131)

    2006 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 組織細胞化学2006

    HIRASAWA AKIRA( Role: Sole author ,  pp183-193)

    2006 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科の実際 55(5)

    HIRASAWA AKIRA( Role: Sole author ,  753-762)

    2006 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科の実際 55(13)

    HIRASAWA AKIRA( Role: Sole author ,  2185-2193)

    2006 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人外来診療マニュアル

    HIRASAWA AKIRA( Role: Sole author ,  135-137)

    2006 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 女性診療科外来プラクティス(腫瘍外来 腫瘍外来の検査)

    HIRASAWA AKIRA( Role: Sole author)

    2006 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 癌と化学療法 32(3)

    HIRASAWA AKIRA( Role: Sole author ,  411-416)

    2005 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 臨床婦人科産科 59(10)

    HIRASAWA AKIRA( Role: Sole author ,  1383-1387)

    2005 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産科と婦人科 71(2)

    HIRASAWA AKIRA( Role: Sole author ,  201-207)

    2004 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 日本臨床増刊号 62(10)

    HIRASAWA AKIRA( Role: Sole author ,  324-328)

    2004 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 血液・腫瘍科 48(2)

    HIRASAWA AKIRA( Role: Sole author ,  175-181)

    2004 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 家族性腫瘍 3

    HIRASAWA AKIRA( Role: Sole author ,  62-67)

    2003 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科の実際 51(10)

    HIRASAWA AKIRA( Role: Sole author ,  1361-1368)

    2002 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 産婦人科の実際 50(12)

    HIRASAWA AKIRA( Role: Sole author ,  1819-1825)

    2001 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

  • 婦人科悪性腫瘍(監訳).

    HIRASAWA AKIRA( Role: Sole translator ,  49-48)

    2000 

     More details

    Language:English Book type:Scholarly book

    researchmap

  • 産婦人科治療 79(6)

    HIRASAWA AKIRA( Role: Sole author ,  680-685)

    1999 

     More details

    Language:Japanese Book type:Scholarly book

    researchmap

▼display all

MISC

  • 【これでマスター! 最新 産婦人科ホルモン療法】(第2章)D 腫瘍 女性がんの化学予防

    植野 さやか, 平沢 晃

    産科と婦人科   91 ( Suppl. )   359 - 363   2024.3

     More details

    Language:Japanese   Publisher:(株)診断と治療社  

    <文献概要>薬剤選択のポイント ▼遺伝性腫瘍症候群関連遺伝子の病的バリアント保持者はがん発症リスクが高く,がん一次予防としての化学予防が考慮される.▼低用量経口避妊薬(oral contraceptive:OC)には,卵巣がん・子宮体がん予防効果がある一方,乳がん発症リスク増加の可能性があり,リスク・ベネフィットを十分に検討する必要がある.

    researchmap

    Other Link: https://search.jamas.or.jp/default/link?pub_year=2024&ichushi_jid=J00525&link_issn=&doc_id=20240405020062&doc_link_id=10.34433%2Fog.0000000682&url=https%3A%2F%2Fdoi.org%2F10.34433%2Fog.0000000682&type=%E5%8C%BB%E6%9B%B8.jp_%E3%82%AA%E3%83%BC%E3%83%AB%E3%82%A2%E3%82%AF%E3%82%BB%E3%82%B9&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00024_2.gif

  • 神経線維腫症1型患者由来ヒトiPS細胞株の樹立

    大澤 太郎, 中田 英二, 岡本 真幸, 山田 大祐, 二川 摩周, 高尾 知佳, 平沢 晃, 尾崎 敏文, 宝田 剛志

    日本レックリングハウゼン病学会学術大会プログラム・抄録集   15回   24 - 24   2024.2

     More details

    Language:Japanese   Publisher:日本レックリングハウゼン病学会  

    researchmap

  • がんゲノム医療における遺伝性腫瘍の理解とチーム医療のための人材育成の取り組み

    蓮岡 佳代子, 二川 摩周, 加藤 芙美乃, 山下 範之, 遠西 大輔, 冨田 秀太, 平沢 晃

    日本がん看護学会学術集会   38回   262 - 262   2024.2

     More details

    Language:Japanese   Publisher:(一社)日本がん看護学会  

    researchmap

  • 遺伝性骨・軟部腫瘍外来における肉腫発生at-risk者への取り組み

    二川 摩周, 中田 英二, 山本 英喜, 深野 智華, 加藤 芙美乃, 大住 理沙, 藤原 智洋, 国定 俊之, 平沢 晃, 尾崎 敏文

    日本レックリングハウゼン病学会学術大会プログラム・抄録集   15回   25 - 25   2024.2

     More details

    Language:Japanese   Publisher:日本レックリングハウゼン病学会  

    researchmap

  • Genetic counseling for couples with 22q.11.2 deletion syndrome

    大平安希子, 衛藤英理子, 末森彩乃, 中藤光里, 大羽輝, 三苫智裕, 三島桜子, 桐野智江, 樫野千明, 光井崇, 牧尉太, 深野智華, 谷村弥生, 大住理沙, 加藤芙美乃, 二川摩周, 岡崎哲也, 山本英喜, 平沢晃, 増山寿

    日本遺伝カウンセリング学会誌   45 ( 2 )   2024

  • がん遺伝子パネル検査と病理診断 がん遺伝子パネル検査で検出されるgermline findingsの遺伝性腫瘍症候群診断への活用

    山本英喜, 平沢晃

    病理と臨床   42 ( 1 )   0045 - 0054   2024

     More details

    Language:Japanese   Publisher:(株)文光堂  

    J-GLOBAL

    researchmap

  • Necessity of ICT utilization in genome education: an analysis based on a questionnaire survey of university students

    十川麗美, 十川麗美, 十川麗美, 野田夕月奈, 鶴田智彦, 鶴田智彦, 花岡有為子, 花岡有為子, 平沢晃, 平沢晃, 隈元謙介, 隈元謙介, 大守伊織

    日本遺伝カウンセリング学会誌   45 ( 2 )   2024

  • 最先端医療の今 教育学部を中心とした学生教育に対するゲノム医療リテラシー向上の取り組み

    十川 麗美, 野田 夕月奈, 隈元 謙介, 平沢 晃, 大守 伊織

    Medical Science Digest   49 ( 13 )   722 - 723   2023.12

     More details

    Language:Japanese   Publisher:(株)ニュー・サイエンス社  

    急速なゲノム医療拡大に伴い,個人にゲノム情報からもたらされる治療選択肢が個人に提示される機会が増加している。例えば,遺伝性腫瘍では,自らの健康管理に役立てることやがん細胞の遺伝子変異のタイプによる治療薬の選択が可能になっている。そのため,医療従事者のみならず,市民もゲノム情報に対する正しい知識を持つことが急務である。筆者らは,未来の社会を担う子どもを教育する立場となる,教育学部学生を中心に大学における教育でゲノム医療のリテラシー向上を目的とした講義を展開した。本稿では,その取り組みの一部を紹介する。(著者抄録)

    researchmap

  • がんゲノムプロファイリング検査のための超音波内視鏡下採取膵癌組織でのMOSEの取組み

    永谷 たみ, 小倉 千尋, 下舞 裕美, 廣尾 嘉樹, 春名 勝也, 木村 祥佳, 堀田 真智子, 伏見 聡一郎, 井上 博文, 平沢 晃, 和仁 洋治

    日本臨床細胞学会雑誌   62 ( Suppl.2 )   536 - 536   2023.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 【図解 産婦人科医のための臨床遺伝学必修知識II】バイオバンクの機能と国内外の動向

    山本 英喜, 平沢 晃

    産婦人科の実際   72 ( 9 )   915 - 921   2023.9

     More details

    Language:Japanese   Publisher:金原出版(株)  

    <文献概要>個別化医療・個別化予防のゲノム医療を推進するうえでバイオバンクは必須である。バイオバンクの試料・情報を活用した種々のコホート研究から遺伝性腫瘍に関する新たな情報発信がされている。バイオバンクのシステムを活用した家系情報付き出生コホート調査の情報が蓄積されている。国内のバイオバンクでは,試料・情報の利活用推進のための横断検索システム(バイオバンク横断検索システム)が開発され利用可能である。わが国の全ゲノム解析等のゲノム医療政策では,政府方針が定められているが,バイオバンク試料・情報の集積やデータ解析,データ保存は各施設が個別に担っている。海外での全ゲノム解析等のゲノム・オミックス解析情報,健康情報,医療情報の蓄積では,政府主導による新規大規模国家プロジェクトとしてバイオバンクおよびデータ解析などの管理機関が指定される形態(例:英国のGenomics England,UK Biobankや米国のAll of Us)や,既存のバイオバンクを連携させて組織化する形態(例:北欧のデンマークやフィンランドのバイオバンク)がある。国際的なバイオバンク連携によるデータシェアリングからヒト疾患リスク遺伝子アトラスの構築など,バイオバンクは新たな知見創出の基盤となっている。

    J-GLOBAL

    researchmap

  • 網羅的がんゲノム医療時代の遺伝性腫瘍診療と遺伝カウンセリング 遺伝性腫瘍のリスク評価・診断のための多遺伝子パネル検査受検例の施設横断的な検討(Hereditary tumor syndromes and genetic counseling in the era of cancer genomic medicine Cross-institutional case review of multi-gene panel testing for risk assessments and diagnosis of hereditary tumors)

    山本 英喜, 藤田 裕子, 田村 和朗, 浦川 優作, 二川 摩周, 十川 麗美, 加藤 芙美乃, 植野 さやか, 重安 邦俊, 原賀 順子, 小川 千加子, 河内 麻里子, 深野 智華, 甲斐 恭平, 塩崎 滋弘, 平沢 晃

    日本癌学会総会記事   82回   821 - 821   2023.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • がんゲノム医療と遺伝性腫瘍

    平沢 晃

    日本遺伝看護学会学術大会抄録集   21回   np4 - np4   2023.8

     More details

    Language:Japanese   Publisher:日本遺伝看護学会  

    J-GLOBAL

    researchmap

  • 肉腫診療におけるがん遺伝子パネルの有用性

    中田 英二, 藤原 智洋, 国定 俊之, 遠西 大輔, 山本 英喜, 二宮 貴一朗, 冨田 秀太, 二川 摩周, 平沢 晃, 豊岡 伸一, 尾崎 敏文

    日本整形外科学会雑誌   97 ( 8 )   S1894 - S1894   2023.8

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • 当院におけるMSI陽性者の遺伝外来受診に関する現状と課題

    原賀 順子, 小川 千加子, 長尾 昌二, 依田 尚之, 白河 伸介, 入江 恭平, 松岡 敬典, 中村 圭一郎, 平沢 晃, 増山 寿

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   65回   374 - 374   2023.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • がんゲノム医療における遺伝リテラシー向上に向けた取り組み

    十川 麗美, 二川 摩周, 加藤 芙美乃, 山下 範之, 浦川 優作, 植野 さやか, 深野 智華, 山本 英喜, 冨田 秀太, 平沢 晃

    BIO Clinica   38 ( 7 )   635 - 637   2023.7

     More details

    Language:Japanese   Publisher:(株)北隆館  

    近年の遺伝子解析技術の進歩に伴い,個人が自身のゲノムや遺伝情報を入手する機会は急速に増加している。そのため,医療従事者のみならず,市民もゲノム情報に対する正しい知識を持つことが急務である。筆者らは,医療従事者・学生・市民を対象に,遺伝リテラシーの向上を目的とした取り組みを行ってきた。本稿では,その取り組みの一部を紹介する。(著者抄録)

    researchmap

  • がん遺伝子パネル検査の二次的所見開示プロセスに関する現状調査 多施設対象アンケート調査

    島田 咲, 山田 崇弘, 源 明理, 松川 愛未, 矢部 一郎, 青木 洋子, 織田 克利, 植木 有紗, 東川 智美, 森川 真紀, 佐藤 友紀, 平沢 晃, 小川 昌宣, 近藤 知大, 吉岡 正博, 金井 雅史, 武藤 学, 小杉 眞司

    日本遺伝カウンセリング学会誌   44 ( 2 )   92 - 92   2023.6

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    researchmap

  • 【産婦人科における先端情報処理技術の展開】婦人科遺伝性腫瘍とデータシェアリング

    平沢 晃

    HORMONE FRONTIER IN GYNECOLOGY   30 ( 2 )   129 - 136   2023.6

     More details

    Language:Japanese   Publisher:(株)メディカルレビュー社  

    <文献概要>一般にがんの約1割は遺伝性であるが,婦人科がんにおける遺伝性腫瘍の割合はさらに高頻度である。婦人科腫瘍関連の遺伝性腫瘍症候群としては遺伝性乳がん卵巣がん,Lynch症候群,PTEN過誤腫症候群,Peutz-Jeghers症候群などがある。一方で,遺伝性腫瘍関連遺伝子の病的バリアント保持者であっても,バリアントの座位や環境因子などによって表現型や浸透率が異なる。これらの解決のためには,データシェアリングや前向きコホート研究が重要な意義をなす。

    researchmap

    Other Link: https://search.jamas.or.jp/default/link?pub_year=2023&ichushi_jid=J02833&link_issn=&doc_id=20230609260009&doc_link_id=%2Fai1hogye%2F2023%2F003002%2F008%2F0129b0136%26dl%3D3&url=https%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Fai1hogye%2F2023%2F003002%2F008%2F0129b0136%26dl%3D3&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_4.gif

  • 細胞にワクワクするようにプレゼンテーションにもワクワクを

    平沢 晃, 永谷 たみ, 井上 博文, 山下 範之

    日本臨床細胞学会雑誌   62 ( Suppl.1 )   119 - 119   2023.5

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • HBOCの最新の話題 HBOC診療にかかる保険診療上の課題

    平沢 晃

    日本婦人科腫瘍学会雑誌   41 ( 2 )   207 - 209   2023.4

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • HBOCの最新の話題 HBOC診療にかかる保険診療上の課題

    平沢 晃

    日本婦人科腫瘍学会雑誌   41 ( 2 )   207 - 209   2023.4

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • Beyond BRCA,そしてMGPT 幅広い遺伝性腫瘍と未発症者も対象にした遺伝医療のプレシジョン・メディシンをめざして 厚労科研研究班の活動を振り返り,これからを展望する

    櫻井 晃洋, 平沢 晃, 鈴木 美慧, 吉田 玲子, 厚生労働科学研究費補助金(がん対策推進総合研究事業)「ゲノム情報を活用した遺伝性腫瘍の先制的医療提供体制の整備に関する研究」班

    INNERVISION   38 ( 4 )   69 - 75   2023.3

     More details

    Language:Japanese   Publisher:(株)インナービジョン  

    がん診療において,生殖細胞系列(germline)の遺伝情報を基にリスクの高さやがんの表現型を推定し,術式,予防医療,薬剤の選択を行うプレシジョン・メディシンが展開されている。国内では,2020年に遺伝性乳癌卵巣癌症候群(HBOC)診療の一部が保険収載され,BRCA1/2の遺伝学的検査や遺伝カウンセリングが臨床で活用されるようになっている。厚労科研研究「ゲノム情報を活用した遺伝性腫瘍の先制的医療提供体制の整備に関する研究」班(櫻井班)では,HBOCに限らず多くの遺伝性腫瘍を対象に,また,発症者だけでなく未発症者も含めた遺伝医療の提供,診療の標準化をめざして研究に取り組んできた。2023年3月の研究期間終了を前に櫻井班メンバーが集い,遺伝性腫瘍多遺伝子パネル検査(MGPT)をテーマとした第3回厚労科研研究班Webセミナーの内容を振り返りながら研究を総括するとともに,遺伝性腫瘍診療のこれからについて語り合った。(著者抄録)

    researchmap

  • 肉腫におけるがんゲノム医療の現状と未来 がん遺伝子パネル検査から同定されるGermline Findingsへの対応

    二川 摩周, 中田 英二, 藤原 智洋, 国定 俊之, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   97 ( 2 )   S446 - S446   2023.3

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • 遺伝性腫瘍の実地臨床 遺伝性骨・軟部腫瘍を中心に

    平沢 晃

    日本整形外科学会雑誌   97 ( 2 )   S447 - S447   2023.3

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • Musculoskeletal Tumor: III. The Role of Comprehensive Genomic Profiling in Sarcoma

    中田英二, 藤原智洋, 国定俊之, 尾崎敏文, 豊岡伸一, 遠西大輔, 山本英喜, 二宮貴一朗, 冨田秀太, 平沢晃, 二川摩周, 田端雅弘

    癌と化学療法   50 ( 3 )   314 - 320   2023.3

  • 遺伝性腫瘍の実地臨床 遺伝性骨・軟部腫瘍を中心に

    平沢 晃

    日本整形外科学会雑誌   97 ( 2 )   S447 - S447   2023.3

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • Treatment of NF-1 in clinic of hereditary bone and soft tissue tumors

    中田英二, 二川摩周, 藤原智洋, 国定俊之, 山本英喜, 平沢晃, 尾崎敏文

    日本レックリングハウゼン病学会学術大会プログラム・抄録集   14回   33 - 33   2023.2

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Establishment of registry system and routine surveillance in neurofibromatosis type 1

    二川摩周, 中田英二, 十川麗美, 加藤芙美乃, 浦川優作, 山本英喜, 山本英喜, 藤原智洋, 国定俊之, 平沢晃, 平沢晃, 尾崎敏文

    日本レックリングハウゼン病学会学術大会プログラム・抄録集   14回   34 - 34   2023.2

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • DIAGNOSIS OF GENETIC VARIANT CARRIERS IN A PATIENT WITH ASYMPTOMATIC BIRT-HOGG-DUBE SYNDROME: A CASE REPORT

    和田里章悟, 市川孝治, 平沢晃, 白石裕雅, 徳永素, 窪田理沙, 久住倫宏, 津島知靖, 神農陽子, 古屋充子

    日本泌尿器科学会雑誌(Web)   114 ( 2 )   61 - 65   2023

     More details

    Language:Japanese  

    Birt-Hogg-Dubé (BHD) syndrome is an autosomal dominant disorder caused by germline mutations in the folliculin gene (FLCN). It is characterized by skin tumors, multiple lung cysts, and renal tumors. Active genetic testing and appropriate periodic examinations of family lines of patients with BHD syndrome have not been widely performed. In this report, we present our experience regarding the diagnosis of asymptomatic family members with BHD syndrome. The proband was a 65-year-old female with a family history of colorectal cancer and spontaneous pneumothorax that affected her father. Computed tomography revealed an approximately 10 cm-sized tumor protruding from the upper pole of the left kidney, a buried tumor approximately 1.5 cm in length in the right kidney, and multiple pulmonary cysts. The patient underwent laparoscopic radical left nephrectomy. Pathological examination indicated that the resected tumor was a chromophobe renal cell carcinoma. After the surgery, there was no evidence of local recurrence or metastasis. The size of the tumor in the right kidney was monitored, but it did not increase. On FLCN genetic examination, targeted next generation sequencing revealed a partial deletion of exon 14, thus confirming the diagnosis of the patient to be BHD syndrome that caused the previously unreported pathogenic variant. Three years after the surgery, we conducted genetic counseling for the proposita and her three children. Genetic examination, performed at the request of the second daughter, confirmed that she carried the same genetic variant as her mother. This diagnosis prompted the second daughter to begin managing her health via periodic imaging tests.

    DOI: 10.5980/jpnjurol.114.61

    PubMed

    J-GLOBAL

    researchmap

  • Hereditary breast and ovarian cancer and the national health insurance in Japan

    平沢晃

    遺伝性腫瘍(Web)   23 ( 1 )   2 - 5   2023

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Genetic approaches for hereditary tumors through comprehensive cancer genome profiling testing

    藤田裕子, 甲斐恭平, 田村和朗, 田村和朗, 田村和朗, 山本英喜, 山本英喜, 山根美代子, 伊藤絢子, 井上豊子, 永谷たみ, 平沢晃, 平沢晃

    日本臨床腫瘍学会学術集会(CD-ROM)   20th   2023

  • Two cases of early diagnosis of medullary thyroid carcinoma by genetic risk management for RET pathogenic germline variants

    加藤芙美乃, 山本英喜, 山本英喜, 十川麗美, 二川摩周, 浦川優作, 植野さやか, 稲垣兼一, 柳井広之, 平沢晃, 平沢晃

    日本遺伝カウンセリング学会誌   44 ( 2 )   123 - 123   2023

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 神経線維腫症1型に対するwhole body MRIによるサーベイランス

    二川摩周, 二川摩周, 中田英二, 十川麗美, 加藤芙美乃, 浦川優作, 山本英喜, 山本英喜, 藤原智洋, 国定俊之, 平沢晃, 平沢晃, 尾崎敏文

    日本整形外科学会雑誌   97 ( 6 )   S1463 - S1463   2023

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • Cancer precision medicine and genetic disease

    平沢晃

    日本臨床腫瘍学会学術集会(CD-ROM)   20th   2023

  • EUS-FNA検体のゲノム医療における有用性と限界

    井上博文, 松岡博美, 實平悦子, 松岡昌志, 安村早優美, 田中健大, 寺澤裕之, 松本和幸, 加藤博也, 平沢晃

    日本臨床細胞学会雑誌(Web)   62   2023

  • ゲノム情報を有効に活用するための診療体制の構築

    中田英二, 藤原智洋, 国定俊之, 遠西大輔, 二宮貴一朗, 冨田秀太, 二川摩周, 山本英喜, 平沢晃, 田端雅弘, 豊岡伸一, 尾崎敏文

    日本整形外科学会雑誌   97 ( 6 )   S1305 - S1305   2023

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • 岡大バイオバンク:研究支援を加速するためのDXの推進

    松原岳大, 江見裕美, 石田紀子, 岩木麻希子, 窪田弥生, 柴倉美砂子, 那須遥, 福田俊, 室崎眞奈, 山本英喜, 冨田秀太, 遠西大輔, 平沢晃, 森田瑞樹, 豊岡伸一, 山本英喜, 冨田秀太, 遠西大輔, 平沢晃, 森田瑞樹, 豊岡伸一, 山本英喜, 冨田秀太, 平沢晃, 森田瑞樹, 豊岡伸一

    日本遺伝子診療学会大会プログラム・抄録集   30th   2023

  • Multilayered Regional Collaboration in personalized cancer medicine

    十川麗美, 十川麗美, 二川摩周, 加藤芙美乃, 山下範之, 山下範之, 浦川優作, 植野さやか, 深野智華, 山本英喜, 山本英喜, 山本英喜, 冨田秀太, 平沢晃, 平沢晃, 平沢晃

    Bio Clinica   38 ( 7 )   635 - 637   2023

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 多職種連携によるがん遺伝子パネル検査-翌日出検の試み

    永谷たみ, 永谷たみ, 永谷たみ, 和仁洋治, 和仁洋治, 春名勝也, 井上豊子, 藤田裕子, 山根美代子, 甲斐恭平, 山本英喜, 山本英喜, 平沢晃, 平沢晃

    日本遺伝子診療学会大会プログラム・抄録集   30th   2023

  • 「日本医学会 医療における遺伝学的検査・診断に関するガイドライン」改定から1年が経過して

    平沢晃

    日本遺伝子診療学会大会プログラム・抄録集   30th   2023

  • BRCAの遺伝情報を最大限に生かすために

    吉田玲子, 平沢晃, 渡邊尚文, 田辺真彦, 高津美月, 金子景香, 藤田裕子, 藤田裕子

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • Cross-institutional case review of multi-gene panel testing for risk assessments and diagnosis of hereditary tumors

    山本英喜, 山本英喜, 山本英喜, 山本英喜, 山本英喜, 藤田裕子, 藤田裕子, 藤田裕子, 藤田裕子, 田村和朗, 田村和朗, 田村和朗, 浦川優作, 浦川優作, 浦川優作, 二川摩周, 二川摩周, 二川摩周, 二川摩周, 十川麗美, 十川麗美, 加藤芙美乃, 加藤芙美乃, 植野さやか, 植野さやか, 植野さやか, 重安邦俊, 重安邦俊, 重安邦俊, 原賀順子, 原賀順子, 原賀順子, 小川千加子, 小川千加子, 小川千加子, 河内麻里子, 河内麻里子, 河内麻里子, 深野智華, 深野智華, 深野智華, 甲斐恭平, 甲斐恭平, 甲斐恭平, 塩崎滋弘, 塩崎滋弘, 塩崎滋弘, 平沢晃, 平沢晃, 平沢晃, 平沢晃, 平沢晃

    日本癌学会学術総会抄録集(Web)   82nd   2023

  • 遺伝性骨・軟部腫瘍

    中田英二, 二川摩周, 加藤芙美乃, 浦川優作, 山本英喜, 藤原智洋, 国定俊之, 平沢晃, 尾崎敏文

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • ベーチェット病を併発したプラスミノーゲン低下症に伴うLigneous歯周炎患者の臨床的・遺伝学的考察

    平井杏奈, 伊東有希, 井手口英隆, 大森一弘, 加藤芙美乃, 山本英喜, 平沢晃, 山本直史, 高柴正悟

    日本歯周病学会会誌(Web)   65   2023

  • がんゲノム医療における多遺伝子パネル検査(MGPT)の導入にむけた現状と課題

    平沢晃, 山本英喜

    日本臨床検査医学会誌   71 ( 補冊 )   087 - 087   2023

     More details

    Language:Japanese   Publisher:(一社)日本臨床検査医学会  

    J-GLOBAL

    researchmap

  • がんゲノムプロファイリング検査のための超音波内視鏡下採取膵癌組織でのMOSEの取組み

    永谷たみ, 永谷たみ, 永谷たみ, 小倉千尋, 下舞裕美, 廣尾嘉樹, 春名勝也, 木村祥佳, 堀田真智子, 伏見聡一郎, 井上博文, 平沢晃, 平沢晃, 和仁洋治

    日本臨床細胞学会雑誌(Web)   62   2023

  • 当院における遺伝性乳癌卵巣癌診療の取り組みと現況

    齋藤文香, 齋藤文香, 高野みずき, 塚本可奈子, 小林織恵, 渡邉尚文, 渡邉尚文, 谷岡真樹, 平沢晃, 平沢晃, 田村和也, 梅澤聡

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • 遺伝性腫瘍診断における多遺伝子パネル検査の臨床的有用性と精度管理

    山本英喜, 平沢晃

    日本臨床検査医学会誌   71 ( 補冊 )   184 - 184   2023

     More details

    Language:Japanese   Publisher:(一社)日本臨床検査医学会  

    J-GLOBAL

    researchmap

  • リンチ症候群を含む遺伝性腫瘍症候群の遺伝診療拡充に向けて

    吉田玲子, 平沢晃, 隈元謙介, 加藤芙美乃, 高津美月

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • 岡山大学病院における小児がんゲノム診療の実際と今後の課題

    石田悠志, 塩飽孝宏, 為房宏輔, 藤原かおり, 鷲尾佳奈, 遠西大輔, 冨田秀太, 平沢晃, 豊岡伸一, 塚原宏一

    中国四国小児科学会プログラム・抄録集   75th (Web)   2023

  • 婦人科がんとprecision medicine

    平沢晃

    日本癌治療学会学術集会(Web)   61st   OSP10 - 4   2023

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • リンチ症候群診療の現状と課題-遺伝子医療部門の現場から-

    平沢晃

    日本癌治療学会学術集会(Web)   61st   CCSP4 - 4   2023

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • 神経線維腫症1型による叢状神経線維腫に対するセルメチニブの有効性

    中田英二, 藤原智洋, 国定俊之, 二川摩周, 山本英喜, 十川麗美, 加藤芙美乃, 片山晴喜, 板野拓人, 近藤彩奈, 平沢晃, 尾崎敏文

    中国・四国整形外科学会雑誌   35 ( 3 )   428 - 428   2023

     More details

    Language:Japanese   Publisher:中国・四国整形外科学会  

    J-GLOBAL

    researchmap

  • ゲノム情報を活用した遺伝性腫瘍の先制的医療提供体制の整備に関する研究

    平沢晃

    ゲノム情報を活用した遺伝性腫瘍の先制的医療提供体制の整備に関する研究 令和4年度 総括研究報告書(Web)   2023

  • 岡山大学消化器外科の大腸がん診療におけるがんゲノムプロファイリング検査の活用

    重安邦俊, 香川俊輔, 寺石文則, 楳田祐三, 岡田尚大, 半澤俊哉, 橋本将志, 垣内慶彦, 松三雄騎, 菊地覚次, 黒田新士, 近藤喜太, 二宮貴一朗, 遠西大輔, 平沢晃, 藤原俊義

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • リンチ症候群の医学的管理とユニバーサルスクリーニングに向けた諸課題の整理~当院でのリンチ症候群に関する診療科横断的会議から~

    山本英喜, 山本英喜, 柳井広之, 柳井広之, 重安邦俊, 重安邦俊, 原賀順子, 原賀順子, 小川千加子, 小川千加子, 片山聡, 片山聡, 山崎泰史, 山崎泰史, 大里俊樹, 大里俊樹, 井上博文, 井上博文, 二川摩周, 二川摩周, 加藤芙美乃, 十川麗美, 植野さやか, 植野さやか, 浦川優作, 浦川優作, 浦川優作, 藤原俊義, 藤原俊義, 増山寿, 増山寿, 荒木元朗, 荒木元朗, 大塚基之, 大塚基之, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • 機械学習を活用した遺伝性乳癌卵巣癌のがん発症リスク予測モデルの開発

    二川摩周, 二川摩周, 谷岡真樹, 永家聖, 浦川優作, 浦川優作, 山本英喜, 山本英喜, 荻島創一, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • 健康管理支援ツールを用いた当事者への長期支援の試み~認定遺伝カウンセラーの立場から

    藤田裕子, 藤田裕子, 田村和朗, 田村和朗, 田村和朗, 平沢晃, 平沢晃, 伊藤絢子, 山本英喜, 山本英喜, 山根美代子, 井上豊子, 甲斐恭平

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • 小児発症悪性葉状腫瘍の一例から考えるLi-Fraumeni症候群 サーベイランス運用への課題

    住吉みわ, 山本英喜, 山本英喜, 藤原由樹, 前田礼奈, 金敬徳, 梶原友紀子, 伊藤充矢, 二川摩周, 二川摩周, 岩谷胤生, 岩谷胤生, 枝園忠彦, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • 褐色細胞腫を発端に診断された,多発内分泌腫瘍症2型(MEN2)の1家系

    吉浜圭祐, 船越信介, 塚田ひとみ, 武井眞, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • cis double heterozygoteとしてBRCA2生殖細胞系列病的バリアントを認めた再発乳癌の一例

    梶原友紀子, 河内麻里子, 藤原由樹, 坂井裕樹, 前田礼奈, 築澤良亮, 金敬徳, 森川恵司, 住吉みわ, 植田麻衣子, 依光正枝, 伊藤充矢, 二川摩周, 山本英喜, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • オンライン遺伝診療の実施状況と課題に対する意識調査

    植野さやか, 植野さやか, 浦川優作, 浦川優作, 植木有紗, 吉田玲子, 赤木究, 田村和朗, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • 血縁関係における二人の卵巣癌患者に異なる病的バリアントが検出された症例

    藤原有基, 浦川優作, 浦川優作, 浦川優作, 矢野友梨, 矢野友梨, 早田裕, 堀口育代, 米澤優, 河田健吾, 和唐正樹, 高田雅代, 高田雅代, 高田雅代, 永坂久子, 永坂久子, 中西美恵, 中西美恵, 小笠原豊, 小笠原豊, 小笠原豊, 平沢晃, 平沢晃, 平沢晃, 川上公宏, 川上公宏, 川上公宏

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • 未発症者の来談から確定診断と多施設連携による健康管理につながった網膜芽細胞腫の一家系

    藤田裕子, 甲斐恭平, 中田英二, 山本英喜, 佐藤友紀, 田村和朗, 田村和朗, 田村和朗, 伊藤絢子, 平野雅幸, 柄川剛, 中川卓, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   29th   2023

  • がんゲノム医療総論

    平沢 晃

    専門医通信   ( 65 )   1 - 4   2022.12

     More details

    Language:Japanese   Publisher:日本気管食道科学会  

    researchmap

  • がんゲノムプロファイリング検査による大腸癌でのBRAF阻害薬の適応判断

    山本 英喜, 重安 邦俊, 河内 麻里子, 座間味 義人, 平沢 晃

    日本臨床薬理学会学術総会抄録集   43回   1 - 6   2022.12

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    J-GLOBAL

    researchmap

  • 軟部肉腫に対する薬物療法 がん遺伝子パネルに基づく肉腫診療

    中田 英二, 藤原 智洋, 国定 俊之, 平沢 晃, 遠西 大輔, 尾崎 敏文

    中部日本整形外科災害外科学会雑誌   65 ( 秋季学会 )   77 - 77   2022.10

     More details

    Language:Japanese   Publisher:(一社)中部日本整形外科災害外科学会  

    J-GLOBAL

    researchmap

  • RAS/BRAF解析においてPCR-rSSO法とNGS法の併用による補完性が示された大腸癌の二例

    山本 英喜, 重安 邦俊, 柳井 広之, 井上 博文, 松岡 博美, 青江 伯規, 東影 明人, 藤井 敬子, 大塚 文男, 草野 展周, 平沢 晃

    日本臨床検査医学会誌   70 ( 補冊 )   258 - 258   2022.10

     More details

    Language:Japanese   Publisher:(一社)日本臨床検査医学会  

    J-GLOBAL

    researchmap

  • 遺伝子パネルでがん医療はどう変わるか? がんゲノム医療における生殖細胞系列遺伝情報に対する対応

    平沢 晃

    日本癌治療学会学術集会抄録集   60回   SSY7 - 3   2022.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    researchmap

  • がん遺伝子パネルに基づく肉腫診療

    中田 英二, 藤原 智洋, 平沢 晃, 二川 摩周, 遠西 大輔, 山本 英喜, 冨田 秀太, 久保 寿夫, 田端 雅弘, 国定 俊之, 豊岡 伸一, 尾崎 敏文

    日本癌治療学会学術集会抄録集   60回   O49 - 4   2022.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • がん遺伝子パネルに基づく肉腫診療

    中田 英二, 藤原 智洋, 平沢 晃, 二川 摩周, 遠西 大輔, 山本 英喜, 冨田 秀太, 久保 寿夫, 田端 雅弘, 国定 俊之, 豊岡 伸一, 尾崎 敏文

    日本癌治療学会学術集会抄録集   60回   O49 - 4   2022.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    researchmap

  • 遺伝子パネルでがん医療はどう変わるか? がんゲノム医療における生殖細胞系列遺伝情報に対する対応

    平沢 晃

    日本癌治療学会学術集会抄録集   60回   SSY7 - 3   2022.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • がんゲノム医療における「連携」 主に患者、家族・血縁者との連携にかかる課題について 全国がんプロ協議会・ゲノム医療部会報告

    平沢 晃

    癌と化学療法   49 ( 9 )   1000 - 1001   2022.9

     More details

    Language:Japanese   Publisher:(株)癌と化学療法社  

    医療者間の連携、医療者と患者の連携および患者と家族間の連携はがん診療全般でも必要事項ではあり、がんゲノム医療のもつ特性を考えた連携を構築することが望ましい。わが国のがんゲノム医療の定義で提唱されているとおり、がん未発症者を含むがん発症予防が可能になって初めて国民の確実ながん死低減が可能になる。(著者抄録)

    researchmap

    Other Link: https://search-tp.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2022&ichushi_jid=J00296&link_issn=&doc_id=20220920380020&doc_link_id=%2Fab8gtkrc%2F2022%2F004909%2F023%2F1000b1001%26dl%3D3&url=https%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Fab8gtkrc%2F2022%2F004909%2F023%2F1000b1001%26dl%3D3&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_4.gif

  • 遺伝性腫瘍診断における多遺伝子パネル検査の臨床的有用性と将来展望(Clinical utility of multi-gene panel testing on hereditary tumor diagnosis and its future perspectives)

    山本 英喜, 加藤 芙美乃, 二川 摩周, 十川 麗美, 浦川 優作, 植野 さやか, 平沢 晃

    日本癌学会総会記事   81回   MS4 - 1   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • がんゲノム医療において遺伝性骨・軟部肉腫を同定する臨床的意義(Clinical significance of identifying hereditary bone and soft tissue sarcomas in precision medicine)

    二川 摩周, 中田 英二, 十川 麗美, 加藤 芙美乃, 浦川 優作, 植野 さやか, 山本 英喜, 藤原 智洋, 国定 俊之, 尾崎 敏文, 平沢 晃

    日本癌学会総会記事   81回   P - 3121   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • 多遺伝子パネル検査によって検出されたMSH2とATMのダブルヘテロ接合体保因者(Double heterozygous mutation carrier with MSH2 and ATM detected by multi-gene panel testing.)

    藤原 有基, 浦川 優作, 平沢 晃

    日本癌学会総会記事   81回   P - 3120   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • 脳腫瘍におけるゲノム医療の展開

    市川 智継, 露口 悠太, 平田 雄一, 高橋 悠, 西廣 真吾, 藏本 智士, 合田 雄二, 小野 恭祐, 川上 公宏, 藤原 有基, 平沢 晃

    香川県医師会誌   75 ( 特別 )   84 - 84   2022.9

     More details

    Language:Japanese   Publisher:(一社)香川県医師会  

    researchmap

  • HBOCにおけるRRSOは何歳まで考慮すべきか.(Rethinking the optimal age to consider RRSO in HBOC.)

    浦川 優作, 二川 摩周, 植野 さやか, 加藤 芙美乃, 十川 麗美, 山本 英喜, 平沢 晃

    日本癌学会総会記事   81回   P - 3122   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • STK11生殖細胞系列バリアントが検出されたPeutz-Jeghers症候群の表現型をもつ乳癌女性の一例(A case of breast cancer woman who is suspected of Peutz-Jeghers syndrome with a novel STK11 germline variant)

    加藤 芙美乃, 山本 英喜, 十川 麗美, 二川 摩周, 浦川 優作, 藤原 有基, 川上 公宏, 牛尼 美年子, 後藤 政広, 田辺 記子, 平田 真, 吉田 輝彦, 菅野 康吉, 平沢 晃

    日本癌学会総会記事   81回   P - 3117   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • 多遺伝子パネル検査によって検出されたMSH2とATMのダブルヘテロ接合体保因者(Double heterozygous mutation carrier with MSH2 and ATM detected by multi-gene panel testing.)

    藤原 有基, 浦川 優作, 平沢 晃

    日本癌学会総会記事   81回   P - 3120   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • がんゲノム医療において遺伝性骨・軟部肉腫を同定する臨床的意義(Clinical significance of identifying hereditary bone and soft tissue sarcomas in precision medicine)

    二川 摩周, 中田 英二, 十川 麗美, 加藤 芙美乃, 浦川 優作, 植野 さやか, 山本 英喜, 藤原 智洋, 国定 俊之, 尾崎 敏文, 平沢 晃

    日本癌学会総会記事   81回   P - 3121   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • HBOCにおけるRRSOは何歳まで考慮すべきか.(Rethinking the optimal age to consider RRSO in HBOC.)

    浦川 優作, 二川 摩周, 植野 さやか, 加藤 芙美乃, 十川 麗美, 山本 英喜, 平沢 晃

    日本癌学会総会記事   81回   P - 3122   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 脳腫瘍におけるゲノム医療の展開

    市川 智継, 露口 悠太, 平田 雄一, 高橋 悠, 西廣 真吾, 藏本 智士, 合田 雄二, 小野 恭祐, 川上 公宏, 藤原 有基, 平沢 晃

    香川県医師会誌   75 ( 特別 )   84 - 84   2022.9

     More details

    Language:Japanese   Publisher:(一社)香川県医師会  

    J-GLOBAL

    researchmap

  • 遺伝性腫瘍診断における多遺伝子パネル検査の臨床的有用性と将来展望(Clinical utility of multi-gene panel testing on hereditary tumor diagnosis and its future perspectives)

    山本 英喜, 加藤 芙美乃, 二川 摩周, 十川 麗美, 浦川 優作, 植野 さやか, 平沢 晃

    日本癌学会総会記事   81回   MS4 - 1   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • STK11生殖細胞系列バリアントが検出されたPeutz-Jeghers症候群の表現型をもつ乳癌女性の一例(A case of breast cancer woman who is suspected of Peutz-Jeghers syndrome with a novel STK11 germline variant)

    加藤 芙美乃, 山本 英喜, 十川 麗美, 二川 摩周, 浦川 優作, 藤原 有基, 川上 公宏, 牛尼 美年子, 後藤 政広, 田辺 記子, 平田 真, 吉田 輝彦, 菅野 康吉, 平沢 晃

    日本癌学会総会記事   81回   P - 3117   2022.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 骨・軟部肉腫に対するがんゲノムプロファイリング検査から検出されるpresumed germline pathogenic variantsの意義

    二川 摩周, 中田 英二, 十川 麗美, 加藤 芙美乃, 浦川 優作, 河内 麻里子, 山本 英喜, 藤原 智洋, 国定 俊之, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 8 )   S1770 - S1770   2022.9

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • 骨・軟部腫瘍の基礎科学のトピックス クリニカルシークエンスによる肉腫のゲノム医療

    中田 英二, 藤原 智洋, 国定 俊之, 二川 摩周, 遠西 大輔, 久保 寿夫, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 8 )   S1533 - S1533   2022.9

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • Biobank and residual sample use for medical research

    山本英喜, 平沢晃

    岡山医学会雑誌   134 ( 2 )   119 - 122   2022.8

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • バイオバンクと残余検体使用の考え方

    山本 英喜, 平沢 晃

    岡山医学会雑誌   134 ( 2 )   119 - 122   2022.8

  • 当院で施行した婦人科癌のがんゲノム医療の現況と課題

    依田 尚之, 小川 千加子, 入江 恭平, 岡本 和浩, 松岡 敬典, 久保 光太郎, 中村 圭一郎, 長尾 昌二, 増山 寿, 平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   64回   205 - 205   2022.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • がんゲノム医療と生殖細胞系列の遺伝情報

    植野 さやか, 平沢 晃

    糖尿病・内分泌代謝科   55 ( 1 )   126 - 135   2022.7

     More details

    Language:Japanese   Publisher:(有)科学評論社  

    researchmap

  • HBOCの最近の話題 HBOC診療にかかる保険診療上の課題

    平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   64回   134 - 134   2022.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 遺伝性腫瘍の管理 遺伝性腫瘍と細胞診断学

    平沢 晃

    日本臨床細胞学会中国四国連合会会報   ( 36 )   27 - 27   2022.7

     More details

    Language:Japanese   Publisher:日本臨床細胞学会-中国四国連合会  

    J-GLOBAL

    researchmap

  • HBOCの最近の話題 HBOC診療にかかる保険診療上の課題

    平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   64回 ( 2 )   134 - 134   2022.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 遺伝性腫瘍の管理 遺伝性腫瘍と細胞診断学

    平沢 晃

    日本臨床細胞学会中国四国連合会会報   ( 36 )   27 - 27   2022.7

     More details

    Language:Japanese   Publisher:日本臨床細胞学会-中国四国連合会  

    researchmap

  • 当院で施行した婦人科癌のがんゲノム医療の現況と課題

    依田 尚之, 小川 千加子, 入江 恭平, 岡本 和浩, 松岡 敬典, 久保 光太郎, 中村 圭一郎, 長尾 昌二, 増山 寿, 平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   64回   205 - 205   2022.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • Germline multigene panel testing in gynecological cancer

    Sayaka Ueno, Akira Hirasawa

    EUROPEAN JOURNAL OF GYNAECOLOGICAL ONCOLOGY   43 ( 3 )   25 - 35   2022.6

     More details

    Language:English   Publishing type:Book review, literature introduction, etc.   Publisher:MRE PRESS  

    Multi-gene panel testing (MGPT) has become widely used in clinical practice. MGPT allows a set of genes to be tested simultaneously, making it a powerful, time- and cost-effective tool for detecting genetic variants. The purposes of identifying germline pathogenic variants is threefold: diagnosis, prevention, and treatment. Germline variants in certain genes cause hereditary tumor syndromes. Diagnosing hereditary tumors enable to predict the types of cancer that may develop in the future. The blood relatives of those diagnosed may also suffer from the same hereditary tumor syndrome. For such individuals, medical intervention tailored to their condition can reduce the incidence of cancer or help in cancer detection in the early stages. Diagnosis of hereditary tumors may also change the cancer treatment strategy for the diagnosed patient. To date, more than 100 genes have been found to have a predisposition to cancer. The type of cancer one develops, the risk of developing it, and the possible preventive strategy differs among genes. The association of some genes with cancer predisposition has not yet been fully confirmed. Nowadays, various types of MGPTs are available, and the genes included differ among the tests. In addition, no consensus has been reached on which genes to be included in MGPT. This review is aimed to summarize the advantages and limitations of MGPT along with some practical considerations while performing MGPT and the gynecological tumors associated with genes commonly included in MGPT.

    DOI: 10.22514/ejgo.2022.008

    Web of Science

    researchmap

  • 遺伝性骨・軟部腫瘍外来の取り組み

    中田 英二, 藤原 智洋, 国定 俊之, 二川 摩周, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 6 )   S1315 - S1315   2022.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • 遺伝性骨・軟部腫瘍に対する遺伝学的検査の臨床的意義

    二川 摩周, 中田 英二, 十川 麗美, 加藤 芙美乃, 浦川 優作, 河内 麻里子, 山本 英喜, 藤原 智洋, 国定 俊之, 尾崎 敏文, 平沢 晃

    日本整形外科学会雑誌   96 ( 6 )   S1301 - S1301   2022.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • ゲノム医療時代の骨・軟部腫瘍医 骨・軟部腫瘍診療におけるがん遺伝子パネルの意義

    中田 英二, 藤原 智洋, 国定 俊之, 二川 摩周, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 6 )   S1286 - S1286   2022.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • National Health Insurance among Clinical Cancer Genetics

    平沢晃

    日本遺伝カウンセリング学会誌   43 ( 2 )   72 - 72   2022.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Characterization of PGPV detected in cancer genomic profiling test and methods of intervention in the department of clinical genetics and genomic medicine

    十川麗美, 山本英喜, 山本英喜, 河内麻里子, 二川摩周, 加藤芙美乃, 蓮岡佳代子, 遠西大輔, 冨田秀太, 平沢晃, 平沢晃

    日本遺伝カウンセリング学会誌   43 ( 2 )   77 - 77   2022.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Examination of the usefulness of multigene panel test for cases in which multiple hereditary tumor syndromes are differentially diagnosed

    藤原有基, 浦川優作, 浦川優作, 浦川優作, 松尾聡子, 坂田周治郎, 堀口育代, 矢野友梨, 米澤優, 河田健吾, 和唐正樹, 中西美恵, 高田雅代, 永坂久子, 小笠原豊, 平沢晃, 川上公宏, 高田雅代, 永坂久子, 小笠原豊, 平沢晃, 川上公宏

    日本遺伝カウンセリング学会誌   43 ( 2 )   149 - 149   2022.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Examination of the usefulness of multigene panel test for cases in which multiple hereditary tumor syndromes are differentially diagnosed

    藤原有基, 浦川優作, 浦川優作, 浦川優作, 松尾聡子, 坂田周治郎, 堀口育代, 矢野友梨, 米澤優, 河田健吾, 和唐正樹, 中西美恵, 高田雅代, 永坂久子, 小笠原豊, 平沢晃, 川上公宏, 高田雅代, 永坂久子, 小笠原豊, 平沢晃, 川上公宏

    日本遺伝カウンセリング学会誌   43 ( 2 )   149 - 149   2022.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 前児染色体異常症がde novo発生と判明しながらも次子に出生前診断を希望する両親への遺伝カウンセリング

    衛藤 英理子, 三苫 智裕, 横畑 理美, 三島 桜子, 大平 安希子, 桐野 智江, 谷 和祐, 牧 尉太, 早田 桂, 増山 寿, 秋山 倫之, 大守 伊織, 十川 麗美, 河内 麻里子, 平沢 晃

    日本遺伝カウンセリング学会誌   43 ( 2 )   95 - 95   2022.6

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    researchmap

  • 神経線維腫症1型に合併する腫瘍性病変に対するサーベイランス

    二川 摩周, 中田 英二, 十川 麗美, 加藤 芙美乃, 浦川 優作, 河内 麻里子, 山本 英喜, 藤原 智洋, 国定 俊之, 尾崎 敏文, 平沢 晃

    日本遺伝カウンセリング学会誌   43 ( 2 )   92 - 92   2022.6

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    researchmap

  • がん遺伝子パネル検査で検出されたPGPVの特性および遺伝子医療部門への介入方法の検討

    十川 麗美, 山本 英喜, 河内 麻里子, 二川 摩周, 加藤 芙美乃, 蓮岡 佳代子, 遠西 大輔, 冨田 秀太, 平沢 晃

    日本遺伝カウンセリング学会誌   43 ( 2 )   77 - 77   2022.6

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    researchmap

  • National Health Insurance among Clinical Cancer Genetics

    平沢晃

    日本遺伝カウンセリング学会誌   43 ( 2 )   72 - 72   2022.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 遺伝性骨・軟部腫瘍外来の取り組み

    中田 英二, 藤原 智洋, 国定 俊之, 二川 摩周, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 6 )   S1315 - S1315   2022.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • 遺伝性骨・軟部腫瘍に対する遺伝学的検査の臨床的意義

    二川 摩周, 中田 英二, 十川 麗美, 加藤 芙美乃, 浦川 優作, 河内 麻里子, 山本 英喜, 藤原 智洋, 国定 俊之, 尾崎 敏文, 平沢 晃

    日本整形外科学会雑誌   96 ( 6 )   S1301 - S1301   2022.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • ゲノム医療時代の骨・軟部腫瘍医 骨・軟部腫瘍診療におけるがん遺伝子パネルの意義

    中田 英二, 藤原 智洋, 国定 俊之, 二川 摩周, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 6 )   S1286 - S1286   2022.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • 婦人科腫瘍領域における遺伝診療の現状と課題

    平沢 晃

    関東連合産科婦人科学会誌   59 ( 2 )   160 - 160   2022.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • がんゲノム医療に対する一般市民のリテラシー向上を目的とした教材の開発と評価

    十川 麗美, 和田 敬仁, 榎 朗兆, 岩本 結香子, 黒飛 恵子, 金井 雅史, 近藤 知大, 本田 明夏, 山田 崇弘, 平沢 晃, 武藤 学, 小杉 眞司

    日本遺伝カウンセリング学会誌   43 ( 1 )   15 - 27   2022.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    がんゲノム医療の重要性が加速する今日、一般市民が遺伝医療に対するリテラシーを持つことが急務である。本研究では、一般市民のがんゲノム医療啓発を目的として、「遺伝子とがん」をテーマにしたまんが教材を開発した。そして、教材の有用性を評価するため、高校生124名を対象に、教材介入前後の質問紙調査を行った。開発した教材に対し理解のしやすさや有用性の項目で約9割が肯定的回答を示し、がんの原因や遺伝性のがんに関する知識向上が確認された。教材介入による不安感は遺伝性のがんの割合の質問正答率と関連が見られ、正確な知識を持つことが不安感の軽減に繋がると示唆された。遺伝カウンセラーの認知や理解に対しても肯定的評価を得た。本調査から、高校生が遺伝やがんの早期教育の重要性を認識し、知識習得の機会を期待していたことも明らかとなった。教材の開発がリテラシー向上に有用であり、個々の健康管理に繋がることが期待される。(著者抄録)

    researchmap

  • 婦人科腫瘍領域における遺伝診療の現状と課題

    平沢 晃

    関東連合産科婦人科学会誌   59 ( 2 )   160 - 160   2022.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 【がん遺伝子検査に基づく婦人科がん治療-最前線のレジメン選択法を理解する】遺伝子診断 BRCA病的バリアントが検出された際の対応

    植野 さやか, 平沢 晃

    臨床婦人科産科   76 ( 3 )   324 - 331   2022.4

     More details

    Language:Japanese   Publisher:(株)医学書院  

    <文献概要>●遺伝性乳がん卵巣がん(HBOC)の診断は家系診断であり,がん治療方針の決定だけでなく,家系全体のがん予防においても有益な情報となる.●BRCA1/2遺伝子の病的バリアントはHBOC診断を目的とした検査以外でも検出されるため,それぞれの検査の特性と検出されるバリアントについての理解が必要である.●HBOCは長期にわたって,遺伝カウンセリングを含めた医学的介入を要する.また,バリアント保持者個々の状況に合わせたがん予防・治療戦略が重要である.

    J-GLOBAL

    researchmap

  • 経過中に難治性高血圧症を合併した血管型Ehlers-Danlos症候群の1例

    長谷川 功, 田中 秀一, 山本 紘一郎, 中野 靖浩, 本多 寛之, 萩谷 英大, 冨田 晃司, 戸田 洋伸, 内田 治仁, 平沢 晃, 大塚 文男

    日本内分泌学会雑誌   98 ( 1 )   322 - 322   2022.4

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    researchmap

  • 【がんゲノム医療時代の分子腫瘍学】(第4部)遺伝子パネル検査 遺伝性腫瘍に対する多遺伝子パネル検査

    山本 英喜, 平沢 晃

    病理と臨床   40 ( 臨増 )   390 - 398   2022.4

     More details

    Language:Japanese   Publisher:(株)文光堂  

    J-GLOBAL

    researchmap

  • 経過中に難治性高血圧症を合併した血管型Ehlers-Danlos症候群の1例

    長谷川 功, 田中 秀一, 山本 紘一郎, 中野 靖浩, 本多 寛之, 萩谷 英大, 冨田 晃司, 戸田 洋伸, 内田 治仁, 平沢 晃, 大塚 文男

    日本内分泌学会雑誌   98 ( 1 )   322 - 322   2022.4

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • 骨軟部腫瘍患者におけるがん遺伝子パネル検査によるgermline findingの同定

    中田 英二, 藤原 智洋, 国定 俊之, 二川 摩周, 平沢 晃, 尾崎 敏文

    中部日本整形外科災害外科学会雑誌   65 ( 春季学会 )   125 - 125   2022.4

     More details

    Language:Japanese   Publisher:(一社)中部日本整形外科災害外科学会  

    J-GLOBAL

    researchmap

  • 成人になって診断のついたHajdu-Cheney症候群の一例

    二川 奈都子, 長谷川 高誠, 西田 圭一郎, 平沢 晃, 河内 麻里子

    日本内分泌学会雑誌   98 ( 1 )   377 - 377   2022.4

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • 遺伝性腫瘍の浸透率決定因子の同定と発癌予測モデルの開発

    平沢 晃

    大和証券ヘルス財団研究業績集   ( 45 )   84 - 88   2022.3

     More details

    Language:Japanese   Publisher:(公財)大和証券ヘルス財団  

    遺伝性腫瘍の長期前向きコホート研究を構築し、遺伝性腫瘍に関する基礎データを集積することで浸透率決定因子を同定し、発癌予測モデルを開発し、リスク低減手法を確立するために多施設共同研究を立ち上げた。10年間で5000家系の登録を予定しており、リスク評価、リスク監視、リスク低減に関するデータを集積してゲノム情報に応じた癌予防法の構築を目指している。

    researchmap

  • 遺伝性腫瘍領域における劇的な変化への対応 遺伝性腫瘍にかかるコンパニオン診断

    平沢 晃

    日本遺伝カウンセリング学会誌   42 ( 4 )   385 - 389   2022.3

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    遺伝性腫瘍の診療は、血縁者における遺伝性腫瘍発症歴をはじめとした表現型からリスク評価を得て遺伝学的検査を行うことを契機に、遺伝性腫瘍家系の同定に至るというケースが多かった。一方で近年は治療薬選択を目的としたコンパニオン診断によって遺伝性腫瘍家系が検出されてきている。さらにがん遺伝子パネル検査にもコンパニオン診断機能があり、遺伝性腫瘍家系の推定につながることがある。わが国では、がんゲノム医療は「がん患者の腫瘍部および正常部のゲノム情報を用いて治療の最適化・予後予測・発症予防を行う医療(未発症者も対象とすることがある。またゲノム以外のマルチオミックス情報も含める)」と定義される。しかしながら、がん未発症ハイリスク者に対する介入は端緒についたばかりである。がんゲノム医療実用化が開始した今こそ、様々なアプローチをもとに遺伝性腫瘍家系同定から予防介入に至るアプローチをもとに国民のがん死低減を目指す必要がある。(著者抄録)

    researchmap

  • 肉腫におけるがん遺伝子パネルの有用性

    中田 英二, 国定 俊之, 藤原 智洋, 二川 摩周, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 3 )   S626 - S626   2022.3

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • 遺伝性腫瘍の浸透率決定因子の同定と発癌予測モデルの開発

    平沢 晃

    大和証券ヘルス財団研究業績集   45 ( 45 )   84 - 88   2022.3

     More details

    Language:Japanese   Publisher:(公財)大和証券ヘルス財団  

    遺伝性腫瘍の長期前向きコホート研究を構築し、遺伝性腫瘍に関する基礎データを集積することで浸透率決定因子を同定し、発癌予測モデルを開発し、リスク低減手法を確立するために多施設共同研究を立ち上げた。10年間で5000家系の登録を予定しており、リスク評価、リスク監視、リスク低減に関するデータを集積してゲノム情報に応じた癌予防法の構築を目指している。

    J-GLOBAL

    researchmap

  • 遺伝性腫瘍領域における劇的な変化への対応 遺伝性腫瘍にかかるコンパニオン診断

    平沢 晃

    日本遺伝カウンセリング学会誌   42 ( 4 )   385 - 389   2022.3

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    遺伝性腫瘍の診療は、血縁者における遺伝性腫瘍発症歴をはじめとした表現型からリスク評価を得て遺伝学的検査を行うことを契機に、遺伝性腫瘍家系の同定に至るというケースが多かった。一方で近年は治療薬選択を目的としたコンパニオン診断によって遺伝性腫瘍家系が検出されてきている。さらにがん遺伝子パネル検査にもコンパニオン診断機能があり、遺伝性腫瘍家系の推定につながることがある。わが国では、がんゲノム医療は「がん患者の腫瘍部および正常部のゲノム情報を用いて治療の最適化・予後予測・発症予防を行う医療(未発症者も対象とすることがある。またゲノム以外のマルチオミックス情報も含める)」と定義される。しかしながら、がん未発症ハイリスク者に対する介入は端緒についたばかりである。がんゲノム医療実用化が開始した今こそ、様々なアプローチをもとに遺伝性腫瘍家系同定から予防介入に至るアプローチをもとに国民のがん死低減を目指す必要がある。(著者抄録)

    researchmap

  • がんゲノム中核拠点病院における、がん遺伝子パネルで同定されたGermline Findingsに対する診療システムの構築

    中田 英二, 二川 摩周, 国定 俊之, 藤原 智洋, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 2 )   S439 - S439   2022.3

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • 肉腫におけるがん遺伝子パネルの有用性

    中田 英二, 国定 俊之, 藤原 智洋, 二川 摩周, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   96 ( 3 )   S626 - S626   2022.3

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • 【産婦人科診療に必要な遺伝カウンセリングの基本知識と実際】がんゲノム医療 検査前遺伝カウンセリング

    小川 千加子, 依田 尚之, 増山 寿, 平沢 晃

    産婦人科の実際   71 ( 2 )   155 - 160   2022.2

     More details

    Language:Japanese   Publisher:金原出版(株)  

    <文献概要>・がんゲノム医療とは,狭義の意味ではがん遺伝子パネル検査を指すこと多いが,本質的は未発症者のがん予防も含めた医療であり,薬剤選択に加え,予測される予後や他のがんのリスクを個別に評価し管理することも含んでいる。・がんゲノム医療における遺伝カウンセリングでは,疾患への遺伝医学的な理解を促し,クライエントを全人的に捉え心理面や社会経済面での問題にも対応することで,がん予防やQOLに貢献する。・婦人科領域ではgermline findingsが比較的高率に検出される。特に遺伝性乳癌卵巣癌(HBOC)とLynch症候群が同定される頻度が高い。

    J-GLOBAL

    researchmap

  • A病院におけるがんゲノム医療に対する認識度調査

    蓮岡 佳代子, 西本 仁美, 平沢 晃, 川崎 優子

    日本がん看護学会学術集会   36回   149 - 149   2022.2

     More details

    Language:Japanese   Publisher:(一社)日本がん看護学会  

    researchmap

  • 当科におけるがん遺伝子パネル検査の実際

    関 典子, 平沢 晃, 西田 康平, 大前 彩乃, 相本 法慧, 平田 智子, 西條 昌之, 西田 友美, 河合 清日, 中山 朋子, 小高 晃嗣, 水谷 靖司

    日本産科婦人科学会雑誌   74 ( 臨増 )   S - 337   2022.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    J-GLOBAL

    researchmap

  • 【産婦人科診療に必要な遺伝カウンセリングの基本知識と実際】がんゲノム医療 検査前遺伝カウンセリング

    小川 千加子, 依田 尚之, 増山 寿, 平沢 晃

    産婦人科の実際   71 ( 2 )   155 - 160   2022.2

     More details

    Language:Japanese   Publisher:金原出版(株)  

    <文献概要>・がんゲノム医療とは,狭義の意味ではがん遺伝子パネル検査を指すこと多いが,本質的は未発症者のがん予防も含めた医療であり,薬剤選択に加え,予測される予後や他のがんのリスクを個別に評価し管理することも含んでいる。・がんゲノム医療における遺伝カウンセリングでは,疾患への遺伝医学的な理解を促し,クライエントを全人的に捉え心理面や社会経済面での問題にも対応することで,がん予防やQOLに貢献する。・婦人科領域ではgermline findingsが比較的高率に検出される。特に遺伝性乳癌卵巣癌(HBOC)とLynch症候群が同定される頻度が高い。

    researchmap

  • 当科におけるがん遺伝子パネル検査の実際

    関 典子, 平沢 晃, 西田 康平, 大前 彩乃, 相本 法慧, 平田 智子, 西條 昌之, 西田 友美, 河合 清日, 中山 朋子, 小高 晃嗣, 水谷 靖司

    日本産科婦人科学会雑誌   74 ( 臨増 )   S - 337   2022.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 合併増大号 今月の臨床 産婦人科医が知っておきたい臨床遺伝学のすべて 扉

    澤井 英明, 平沢 晃

    臨床婦人科産科   76 ( 1 )   5 - 5   2022.1

     More details

    Publisher:株式会社医学書院  

    DOI: 10.11477/mf.1409210554

    researchmap

  • 【遺伝性腫瘍学入門 遺伝性腫瘍の基礎知識】疾患各論 HBOC 遺伝性乳癌卵巣癌(Hereditary breast and ovarian cancer:HBOC)

    平沢 晃, 浦川 優作

    遺伝子医学   別冊 ( 遺伝性腫瘍の基礎知識 )   92 - 98   2022.1

     More details

    Language:Japanese   Publisher:(株)メディカルドゥ  

    researchmap

  • 【遺伝性腫瘍学入門 遺伝性腫瘍の基礎知識】疾患各論 HBOC 遺伝性乳癌卵巣癌(Hereditary breast and ovarian cancer:HBOC)

    平沢 晃, 浦川 優作

    遺伝子医学   別冊 ( 遺伝性腫瘍の基礎知識 )   92 - 98   2022.1

     More details

    Language:Japanese   Publisher:(株)メディカルドゥ  

    遺伝性乳癌卵巣癌(hereditary breast and ovarian cancer:HBOC)はBRCA1/2生殖細胞系列病的バリアントに起因する遺伝性疾患で,乳癌,卵巣癌,膵癌,前立腺癌などの腫瘍発症リスクが高い。HBOC家系に対してはBRCA1/2遺伝学的検査を行い,がん予防,予後予測,個別化がん治療選択を通して,がん死低減に結びつけることが可能となる。本稿ではHBOC総論として,BRCA1/2遺伝子とBRCA1/2タンパクの特性,わが国におけるHBOC診療の歴史,および医療システムとしての現状と課題を概説する。(著者抄録)

    researchmap

  • 参照配列の違いによりがん遺伝子パネル検査と生殖細胞系列遺伝学的検査の結果解釈が異なった一例

    加藤芙美乃, 山本英喜, 山本英喜, 河内麻里子, 浦川優作, 十川麗美, 二川摩周, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • 家族性大腸腺腫症における2チームでの経肛門的直腸間膜切除術(Trans anal Total Mesorectal Excision:TaTME)を用いた大腸全摘

    重安邦俊, 武田正, 近藤喜太, 寺石文則, 二川摩周, 加藤芙美乃, 十川麗美, 堀口繁, 香川俊輔, 平沢晃, 藤原俊義

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • 医療圏横断的な遺伝性腫瘍前向きコホート研究の立ちあげ(中央西日本遺伝性腫瘍コホート研究)

    平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • HBOC診療~保険診療における次の一歩~

    平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • 婦人科腫瘍領域における遺伝診療の現状と課題

    平沢晃

    関東連合産科婦人科学会誌(Web)   59 ( 2 )   2022

  • がんゲノムプロファイリング検査から見出される生殖細胞系列病的バリアントに対する手順書作成と課題

    二川摩周, 二川摩周, 浦川優作, 植野さやか, 十川麗美, 加藤芙美乃, 河内麻里子, 山本英喜, 山本英喜, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • わが国の卵巣がん未発症HBOC女性を対象としたバイオバンク・コホート研究(JGOG3024/KGOG3055)

    平沢晃, 平沢晃, 竹原和宏, 竹原和宏, 上浦祥司, 上浦祥司, 小川千加子, 小川千加子, 青木大輔, 青木大輔, 中村和人, 中村和人, 河村京子, 河村京子, 安達将隆, 安達将隆, 二川摩周, 二川摩周, 津田均, 津田均, 関根正幸, 関根正幸, 梶山広明, 梶山広明, 島田宗昭, 島田宗昭, 岡本愛光, 岡本愛光

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • 産婦人科医が知っておきたい臨床遺伝学のすべて 腫瘍 がんゲノム医療とgermline findingsの取り扱い

    小川千加子, 増山寿, 平沢晃

    臨床婦人科産科   76 ( 1 )   111 - 118   2022

     More details

    Language:Japanese   Publisher:(株)医学書院  

    <文献概要>●がんに関連する生殖細胞系列の遺伝情報は,本人の治療だけでなく,本人の次なるがんへの対策や,未発症を含む血縁者のがん予防につながる重要な情報である.●婦人科領域では他がん種に比べ,germline findingsが比較的高率に検出される.遺伝性乳がん卵巣がんとLynch症候群が多いが,それ以外の遺伝性腫瘍もある.●がんゲノムプロファイリング検査で開示すべきgermline findingsが見出されなかったとしても,遺伝性疾患が除外できたわけではないことに留意する.

    J-GLOBAL

    researchmap

  • Research and development of data definitions and tools for data standardization of hereditary tumor family trees

    山下範之, 浦川優作, 加藤芙美乃, 河内麻里子, 平沢晃

    情報処理学会全国大会講演論文集   84th ( 1 )   2022

  • Genomic medicine and new treatment strategies based on biomarkers for soft tissue sarcoma

    中田英二, 藤原智洋, 国定俊之, 尾崎敏文, 平沢晃, 二川摩周, 遠西大輔, 冨田秀太, 久保寿夫, 宮本理史

    整形・災害外科   65 ( 3 )   247 - 262   2022

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 遺伝性骨・軟部腫瘍外来

    中田英二, 二川摩周, 藤原智洋, 国定俊之, 平沢晃, 尾崎敏文

    中国・四国整形外科学会雑誌   34 ( 3 )   393 - 393   2022

     More details

    Language:Japanese   Publisher:中国・四国整形外科学会  

    J-GLOBAL

    researchmap

  • A new subtype of colorectal cancer based of RAS/RAF, micro-satellite status, and mesenchymal type for far-advanced CRC

    矢野修也, 矢野修也, 重安邦俊, 谷岡洋亮, 山崎泰史, 河内麻里子, 平沢晃, 武田正, 香川俊輔, 藤原俊義, 永坂岳司

    日本臨床腫瘍学会学術集会(CD-ROM)   19th   2022

  • 子宮体がんup to date リンチ症候群と子宮体癌

    植野さやか, 植野さやか, 平沢晃

    産婦人科の実際   71 ( 11 )   1317 - 1327   2022

     More details

    Language:Japanese   Publisher:金原出版(株)  

    <文献概要>リンチ症候群女性では,75歳までに約3人に1人が子宮体癌を発症すると予測される。子宮体癌患者の5%程度はリンチ症候群と見込まれるため,子宮体癌患者の診療にあたっては常にリンチ症候群の可能性を念頭に置いておく必要がある。リンチ症候群では,積極的なサーベイランスによって,がんの予防効果が期待される。また,卵巣癌もリンチ症候群関連腫瘍の1つである。リンチ症候群は常染色体顕性(優性)遺伝形式を示すため,診断された本人のみでなく,家系全体に対しての遺伝カウンセリングや医学的介入が必要となる。

    J-GLOBAL

    researchmap

  • がん遺伝子パネル検査のpresumed germline pathogenic variant(PGPV)を契機に遺伝性乳癌卵巣癌(HBOC)診断に至ったHBOC非関連癌の2症例の報告

    鈴木陽子, 河内麻里子, 河内麻里子, 加藤芙美乃, 十川麗美, 二川摩周, 間森智加, 宇野摩耶, 中本翔伍, 山下範之, 山本英喜, 山本英喜, 枝園忠彦, 富田秀太, 遠西大輔, 平成人, 平沢晃, 平沢晃, 土井原博義

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • 医学生を対象としたオンラインツールを用いた遺伝カウンセリングロールプレイ

    十川麗美, 山本英喜, 山本英喜, 河内麻里子, 河内麻里子, 山下範之, 二川摩周, 加藤芙美乃, 浦川優作, 植野さやか, 小川千加子, 片岡祐子, 重安邦俊, 菅谷明子, 長尾昌二, 早田桂, 吉本順子, 阿部彰子, 植木有紗, 岡崎哲也, 木村香里, 隈元謙介, 杉本健樹, 鶴田智彦, 難波栄二, 花岡有為子, 増田健太, 三浦清徳, 山口昌俊, 吉田玲子, 平沢晃, 平沢晃

    日本人類遺伝学会大会プログラム・抄録集   67th (CD-ROM)   2022

  • 多遺伝子パネル検査にてATMとMSH2のdouble heterozygotesを認めた例

    藤原有基, 浦川優作, 浦川優作, 浦川優作, 坂田周治郎, 堀口育代, 矢野友梨, 米澤優, 河田健吾, 和唐正樹, 高田雅代, 高田雅代, 永坂久子, 永坂久子, 谷本竜太, 中村聡子, 中西美恵, 小笠原豊, 小笠原豊, 平沢晃, 平沢晃, 川上公宏, 川上公宏

    日本人類遺伝学会大会プログラム・抄録集   67th (CD-ROM)   2022

  • A woman with Hajdu-Cheney syndrome diagnosed in adulthood

    二川奈都子, 吾郷祐子, 長谷川高誠, 西田圭一郎, 河内麻里子, 平沢晃

    日本小児内分泌学会学術集会プログラム・抄録集   55th   2022

  • 既存のempirical modelを用いたBRCA1/2病的バリアントのリスク評価の有用性と限界

    二川摩周, 二川摩周, 谷岡真樹, 浦川優作, 浦川優作, 十川麗美, 加藤芙美乃, 山本英喜, 山本英喜, 平沢晃, 平沢晃

    日本人類遺伝学会大会プログラム・抄録集   67th (CD-ROM)   2022

  • がん遺伝子パネル検査後に行ったMGPTでリンチ症候群と診断された副腎皮質癌の症例

    藤田裕子, 甲斐恭平, 平沢晃, 平沢晃, 山本英喜, 山本英喜, 原口貴裕, 和仁洋治, 永谷たみ, 谷口真紀, 伊藤絢子, 山根美代子, 井上豊子, 田村和朗, 田村和朗, 田村和朗

    日本人類遺伝学会大会プログラム・抄録集   67th (CD-ROM)   2022

  • がん遺伝医療における保険診療の道のりと課題

    平沢晃

    日本人類遺伝学会大会プログラム・抄録集   67th (CD-ROM)   2022

  • がん遺伝子パネル検査でPositive Biomarkerとして検出されたRAD51Dのバリアントが生殖細胞系列でVUSと判定された一例

    加藤芙美乃, 山本英喜, 山本英喜, 河内麻里子, 河内麻里子, 浦川優作, 浦川優作, 植野さやか, 十川麗美, 二川摩周, 平沢晃, 平沢晃

    日本人類遺伝学会大会プログラム・抄録集   67th (CD-ROM)   2022

  • ゲノム情報を活用した遺伝性腫瘍の先制的医療提供体制の整備に関する研究 未発症者を含む遺伝性腫瘍診療の標準化,均てん化に向けた課題と提言

    平沢晃

    ゲノム情報を活用した遺伝性腫瘍の先制的医療提供体制の整備に関する研究 令和3年度 総括研究報告書(Web)   2022

  • JGOG3024:BRCA1/2遺伝子バリアントとがん発症・臨床病理学的特徴および発症リスク因子を明らかにするための卵巣がん未発症を対象としたバイオバンク・コホート研究

    平沢晃

    婦人科悪性腫瘍研究機構年次会議(総会)記録集   20th   2022

  • 当科におけるHBOCの乳癌患者の治療選択の現状

    間森智加, 河内麻里子, 河内麻里子, 加藤芙美乃, 十川麗美, 二川摩周, 大谷悠介, 吉岡遼, 藤原みわ, 中本翔伍, 鈴木陽子, 宇野摩耶, 安部優子, 鳩野みなみ, 高橋侑子, 岩本高行, 山本英喜, 枝園忠彦, 平成人, 平沢晃, 土井原博義

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • Birt-Hogg-Dube症候群の遺伝学的検査から家系員への介入が可能になった一例

    和田里章悟, 市川孝治, 平沢晃, 白石裕雅, 佐久間貴文, 窪田理沙, 久住倫宏, 津島知靖, 古屋充子

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • 遺伝性骨・軟部腫瘍外来新設に関する取り組みと今後の展望

    二川摩周, 二川摩周, 中田英二, 十川麗美, 加藤芙美乃, 浦川優作, 河内麻里子, 山本英喜, 山本英喜, 藤原智洋, 国定俊之, 平沢晃, 平沢晃, 尾崎敏文

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • 遺伝性腫瘍において遺伝情報が血縁者間で共有される事の検討 医学的管理のメリットと課題について

    藤原有基, 浦川優作, 浦川優作, 坂田周治郎, 堀口育代, 矢野友梨, 米澤優, 河田健吾, 和唐正樹, 谷本竜太, 佐々木克己, 中西美恵, 高田雅代, 永坂久子, 小笠原豊, 平沢晃, 高田雅代, 永坂久子, 小笠原豊, 平沢晃, 川上公宏

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   28th   2022

  • ペムブロリズマブ使用中に下垂体機能低下症と間質性肺炎を発症したが診療科横断的に加療できた高頻度マイクロサテライト不安定性大腸癌の1例

    重安邦俊, 矢野修也, 武田正, 山崎泰史, 河内麻里子, 平沢晃, 香川俊輔, 藤原俊義

    日本臨床腫瘍学会学術集会(CD-ROM)   19th   2022

  • 日本医学会 医療における遺伝学的検査・診断に関するガイドライン」を読み解く

    平沢晃

    日本遺伝子診療学会大会プログラム・抄録集   29th   2022

  • もう知らないとは言わせないHBOC 卵巣癌におけるHBOCの現況と課題 泌尿器科との交差点

    平沢 晃

    日本泌尿器科学会総会   109回   WS8 - 3   2021.12

     More details

    Language:Japanese   Publisher:(一社)日本泌尿器科学会総会事務局  

    J-GLOBAL

    researchmap

  • MEN1疑いの家族歴と上縦隔に進展する副甲状腺癌を認めた1例

    大塚 勇輝, 長谷川 功, 原田 洸, 西村 義人, 岡 浩介, 小野 早和子, 枝園 忠彦, 平沢 晃, 大塚 文男

    日本内分泌学会雑誌   97 ( 4 )   946 - 946   2021.12

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    researchmap

  • がんゲノム医療における生殖細胞系列の遺伝情報

    平沢 晃

    日本臨床薬理学会学術総会抄録集   42回   3 - 2   2021.12

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • がんゲノム医療における保険収載にかかる課題

    平沢 晃

    日本臨床薬理学会学術総会抄録集   42回   2 - 4   2021.12

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • がんゲノム医療における生殖細胞系列の遺伝情報

    平沢 晃

    日本臨床薬理学会学術総会抄録集   42回   3 - 2   2021.12

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • がんゲノム医療における保険収載にかかる課題

    平沢 晃

    日本臨床薬理学会学術総会抄録集   42回   2 - 4   2021.12

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • もう知らないとは言わせないHBOC 卵巣癌におけるHBOCの現況と課題 泌尿器科との交差点

    平沢 晃

    日本泌尿器科学会総会   109回   WS8 - 3   2021.12

     More details

    Language:Japanese   Publisher:(一社)日本泌尿器科学会総会事務局  

    J-GLOBAL

    researchmap

  • MEN1疑いの家族歴と上縦隔に進展する副甲状腺癌を認めた1例

    大塚 勇輝, 長谷川 功, 原田 洸, 西村 義人, 岡 浩介, 小野 早和子, 枝園 忠彦, 平沢 晃, 大塚 文男

    日本内分泌学会雑誌   97 ( 4 )   946 - 946   2021.12

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • 【変わる婦人科がん薬物治療-免疫チェックポイント阻害薬・PARP阻害薬を中心に-】婦人科がん治療におけるバイオマーカーと遺伝子パネル検査

    坂井 美佳, 竹原 和宏, 平沢 晃

    産科と婦人科   88 ( 11 )   1343 - 1349   2021.11

     More details

    Language:Japanese   Publisher:(株)診断と治療社  

    2019年6月の保険収載以降、がん遺伝子パネル検査は日常臨床で実施されている。婦人科がん治療では分子標的治療の導入が進み、がん遺伝子パネル検査やコンパニオン診断薬を含むがんゲノム医療はすでに診療の大きな柱である。今後、全ゲノム解析の日常診療への導入が予想され、がん以外の領域でもゲノム医療の広がりが予想される。ゲノム医療では体細胞あるいは生殖細胞系列バリアントの情報が得られる。ゲノム医療時代の到来を前に、検査結果を適切に解釈し、対応するための知識が求められる。(著者抄録)

    J-GLOBAL

    researchmap

  • Efficacy of using multi gene panel testing for hereditary cancer syndrome diagnosis

    吉田玲子, 平沢晃, 山内英子, 中村清吾, 櫻井晃洋

    日本遺伝カウンセリング学会誌   42 ( 3 )   241 - 248   2021.11

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 【変わる婦人科がん薬物治療-免疫チェックポイント阻害薬・PARP阻害薬を中心に-】婦人科がん治療におけるバイオマーカーと遺伝子パネル検査

    坂井 美佳, 竹原 和宏, 平沢 晃

    産科と婦人科   88 ( 11 )   1343 - 1349   2021.11

     More details

    Language:Japanese   Publisher:(株)診断と治療社  

    2019年6月の保険収載以降、がん遺伝子パネル検査は日常臨床で実施されている。婦人科がん治療では分子標的治療の導入が進み、がん遺伝子パネル検査やコンパニオン診断薬を含むがんゲノム医療はすでに診療の大きな柱である。今後、全ゲノム解析の日常診療への導入が予想され、がん以外の領域でもゲノム医療の広がりが予想される。ゲノム医療では体細胞あるいは生殖細胞系列バリアントの情報が得られる。ゲノム医療時代の到来を前に、検査結果を適切に解釈し、対応するための知識が求められる。(著者抄録)

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2021&ichushi_jid=J00525&link_issn=&doc_id=20211025050012&doc_link_id=%2Fae4sanke%2F2021%2F008811%2F013%2F1343b1349%26dl%3D3&url=https%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Fae4sanke%2F2021%2F008811%2F013%2F1343b1349%26dl%3D3&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_4.gif

  • 包括的ゲノムプロファイリングを用いた神経内分泌癌の治療探索と生殖細胞系列の推定

    山本 英喜, 河内 麻里子, 堀口 繁, 榮 浩行, 久保 寿夫, 二宮 貴一朗, 西森 久和, 高本 篤, 遠西 大輔, 冨田 秀太, 宮本 理史, 田端 雅弘, 柳井 広之, 豊岡 伸一, 平沢 晃

    日本癌治療学会学術集会抄録集   59回   O73 - 3   2021.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • 参照配列の違いからゲノム解析結果が異なる解釈に至った遺伝学的検査の一例

    山本 英喜, 加藤 芙美乃, 浦川 優作, 河内 麻里子, 二川 摩周, 十川 麗美, 植野 さやか, 平沢 晃

    日本臨床検査医学会誌   69 ( 補冊 )   183 - 183   2021.10

     More details

    Language:Japanese   Publisher:(一社)日本臨床検査医学会  

    J-GLOBAL

    researchmap

  • 遺伝性腫瘍

    平沢 晃

    日本臨床細胞学会雑誌   60 ( Suppl.2 )   379 - 379   2021.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 消化器領域細胞診への細胞検査士の挑戦 胆・膵癌におけるがん遺伝子パネル検査の課題 細胞診にできること

    井上 博文, 松岡 博美, 實平 悦子, 松岡 昌志, 冨田 秀太, 松本 和幸, 堀口 繁, 加藤 博也, 山本 英喜, 柳井 広之, 平沢 晃

    日本臨床細胞学会雑誌   60 ( Suppl.2 )   470 - 470   2021.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 包括的ゲノムプロファイリングを用いた神経内分泌癌の治療探索と生殖細胞系列の推定

    山本 英喜, 河内 麻里子, 堀口 繁, 榮 浩行, 久保 寿夫, 二宮 貴一朗, 西森 久和, 高本 篤, 遠西 大輔, 冨田 秀太, 宮本 理史, 田端 雅弘, 柳井 広之, 豊岡 伸一, 平沢 晃

    日本癌治療学会学術集会抄録集   59回   O73 - 3   2021.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • 婦人科がんゲノム医療

    平沢 晃

    現代産婦人科   69 ( Suppl. )   S28 - S28   2021.9

     More details

    Language:Japanese   Publisher:中国四国産科婦人科学会  

    J-GLOBAL

    researchmap

  • 遺伝性がん 遺伝情報の診療録の取り扱いに関する課題

    浦川 優作, 二川 摩周, 十川 麗美, 加藤 芙美乃, 植野 さやか, 河内 麻里子, 山本 英喜, 平沢 晃

    日本癌学会総会記事   80回   [SST6 - 5]   2021.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 認定遺伝カウンセラーからみた遺伝性腫瘍を有する患者・家族へのサポート体制

    二川 摩周, 浦川 優作, 十川 麗美, 河内 麻里子, 山本 英喜, 平沢 晃

    日本癌学会総会記事   80回   [SP1 - 4]   2021.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • がんゲノム医療で見つかるPGPVsの特徴

    十川 麗美, 山本 英喜, 河内 麻里子, 二川 摩周, 浦川 優作, 遠西 大輔, 冨田 秀太, 平沢 晃

    日本癌学会総会記事   80回   [P7 - 7]   2021.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • 家族性膵癌のサーベイランス:現状と課題 当院の家族性および遺伝性膵がんに対する取り組み

    阿部 紘大, 北郷 実, 八木 洋, 阿部 雄太, 長谷川 康, 堀 周太郎, 田中 真之, 中野 容, 小崎 健次郎, 平沢 晃, 北川 雄光

    膵臓   36 ( 3 )   A173 - A173   2021.8

     More details

    Language:Japanese   Publisher:(一社)日本膵臓学会  

    researchmap

  • 遺伝学的検査とがん予防の新たな展望(HBOC Practice Guideline for Collaborative Shared Decision Making)

    山内 英子, 北野 敦子, 有賀 智之, 岡本 愛光, 平沢 晃, 新井 正美, 櫻井 晃洋, 青木 大輔, 中村 清吾

    日本乳癌学会総会プログラム抄録集   29回   19 - 19   2021.7

     More details

    Language:English   Publisher:(一社)日本乳癌学会  

    J-GLOBAL

    researchmap

  • 【ポストコロナ時代の産婦人科医療】遺伝医療

    平沢 晃

    産婦人科の実際   70 ( 7 )   741 - 744   2021.7

     More details

    Language:Japanese   Publisher:金原出版(株)  

    <文献概要>新型コロナウイルス感染症の拡大は医療システムを大きく変化させた。「受診したいけど受診できない患者・クライエント」と,「受診してもらいたいのに受診してもらえない医療者」が双方で模索して歩み寄ることになった。ポストコロナ時代の産婦人科遺伝診療は「変えていくべきもの」と「変えてはいけないもの」のバランスに配慮し,最新の遺伝子解析技術やオンライン診療などを導入するとともに,遺伝リテラシーの向上を通して,遺伝情報,ゲノム情報を当事者のために有効に活用することが求められる。

    researchmap

  • 【ポストコロナ時代の産婦人科医療】遺伝医療

    平沢 晃

    産婦人科の実際   70 ( 7 )   741 - 744   2021.7

     More details

    Language:Japanese   Publisher:金原出版(株)  

    <文献概要>新型コロナウイルス感染症の拡大は医療システムを大きく変化させた。「受診したいけど受診できない患者・クライエント」と,「受診してもらいたいのに受診してもらえない医療者」が双方で模索して歩み寄ることになった。ポストコロナ時代の産婦人科遺伝診療は「変えていくべきもの」と「変えてはいけないもの」のバランスに配慮し,最新の遺伝子解析技術やオンライン診療などを導入するとともに,遺伝リテラシーの向上を通して,遺伝情報,ゲノム情報を当事者のために有効に活用することが求められる。

    J-GLOBAL

    researchmap

  • 遺伝学的検査とがん予防の新たな展望 協力的なShared Decision MakingのためのHBOC診療ガイドライン(HBOC Practice Guideline for Collaborative Shared Decision Making)

    山内 英子, 北野 敦子, 有賀 智之, 岡本 愛光, 平沢 晃, 新井 正美, 櫻井 晃洋, 青木 大輔, 中村 清吾

    日本乳癌学会総会プログラム抄録集   29回   19 - 19   2021.7

     More details

    Language:English   Publisher:(一社)日本乳癌学会  

    researchmap

  • CYP11B1/B2キメラ遺伝子を確認した家族性アルドステロン症小児例

    中野 靖浩, 岩田 菜穂子, 長谷川 高誠, 越智 可奈子, 山本 紘一郎, 高瀬 了輔, 長谷川 功, 堀口 繁, 山本 英喜, 平沢 晃, 大塚 文男

    日本内分泌学会雑誌   97 ( Suppl.Update )   71 - 73   2021.7

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    約20年前にCYP11B1/B2キメラ遺伝子を確認しグルココルチコイド反応性アルドステロン症(GRA)と診断された日本人1家系3例(発端者、母、妹)のうち、発端者が出産した5歳と3歳の男児に対し遺伝子検査を行った。その結果、男児2人ともキメラ遺伝子を検出しGRA保因者であることが明らかとなった。また、キメラ遺伝子の交叉部位について検討した結果、2児と発端者は同一のシークエンスで、交叉部位はエクソン3とイントロン5間であった。2児とも高血圧を認めないが低レニン・高アルドステロン症を伴っており、今後、成人期までの慎重な経過観察が必要である。

    J-GLOBAL

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2021&ichushi_jid=J01160&link_issn=&doc_id=20210811280023&doc_link_id=10.1507%2Fendocrine.97.S.Update_71&url=https%3A%2F%2Fdoi.org%2F10.1507%2Fendocrine.97.S.Update_71&type=J-STAGE&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00007_3.gif

  • コンパニオン診断

    平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   99 - 100   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 卵巣癌易罹患性に関する遺伝学的背景を持つ卵巣子宮内膜症性嚢胞から癌化をきたした2症例

    小川 千加子, 依田 尚之, 松岡 敬典, 入江 恭平, 岡本 和浩, 春間 朋子, 中村 圭一郎, 平沢 晃, 増山 寿

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   245 - 245   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 婦人科がん治療医の遺伝性乳癌卵巣癌症候群(HBOC)診療に関する実態調査から見えてきたこと

    小林 佑介, 高橋 孝幸, 増田 健太, 平沢 晃, 竹原 和宏, 津田 均, 渡部 洋, 織田 克利, 永瀬 智, 万代 昌紀, 岡本 愛光, 八重樫 伸生, 三上 幹男, 榎本 隆之, 青木 大輔

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   219 - 219   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 当科における子宮頸癌に対するがんパネル検査の現況

    松岡 敬典, 小川 千加子, 岡本 和浩, 依田 尚之, 久保 光太郎, 春間 朋子, 中村 圭一郎, 平沢 晃, 増山 寿

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   337 - 337   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • がん遺伝子パネル検査の現状と課題 がんゲノム医療overview 国民のがん死低減を目指して

    平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   109 - 109   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 当院における子宮体がんの遺伝子パネル検査の検討

    岡本 和浩, 小川 千加子, 松岡 敬典, 依田 尚之, 久保 光太郎, 春間 朋子, 中村 圭一郎, 平沢 晃, 増山 寿

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   214 - 214   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 当院で施行した卵巣がんのがんゲノム医療の現況

    依田 尚之, 小川 千加子, 岡本 和浩, 松岡 敬典, 久保 光太郎, 春間 朋子, 中村 圭一郎, 増山 寿, 平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   209 - 209   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 当院における子宮体がんの遺伝子パネル検査の検討

    岡本 和浩, 小川 千加子, 松岡 敬典, 依田 尚之, 久保 光太郎, 春間 朋子, 中村 圭一郎, 平沢 晃, 増山 寿

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   214 - 214   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 婦人科がん治療医の遺伝性乳癌卵巣癌症候群(HBOC)診療に関する実態調査から見えてきたこと

    小林 佑介, 高橋 孝幸, 増田 健太, 平沢 晃, 竹原 和宏, 津田 均, 渡部 洋, 織田 克利, 永瀬 智, 万代 昌紀, 岡本 愛光, 八重樫 伸生, 三上 幹男, 榎本 隆之, 青木 大輔

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   219 - 219   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 当院で施行した卵巣がんのがんゲノム医療の現況

    依田 尚之, 小川 千加子, 岡本 和浩, 松岡 敬典, 久保 光太郎, 春間 朋子, 中村 圭一郎, 増山 寿, 平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   209 - 209   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 卵巣癌易罹患性に関する遺伝学的背景を持つ卵巣子宮内膜症性嚢胞から癌化をきたした2症例

    小川 千加子, 依田 尚之, 松岡 敬典, 入江 恭平, 岡本 和浩, 春間 朋子, 中村 圭一郎, 平沢 晃, 増山 寿

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   245 - 245   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 当科における子宮頸癌に対するがんパネル検査の現況

    松岡 敬典, 小川 千加子, 岡本 和浩, 依田 尚之, 久保 光太郎, 春間 朋子, 中村 圭一郎, 平沢 晃, 増山 寿

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   337 - 337   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • がん遺伝子パネル検査の現状と課題 がんゲノム医療overview 国民のがん死低減を目指して

    平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   109 - 109   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • コンパニオン診断

    平沢 晃

    日本婦人科腫瘍学会学術講演会プログラム・抄録集   63回   99 - 100   2021.7

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 婦人科におけるHBOC診療の現状と課題

    平沢 晃

    東北連合産科婦人科学会総会・学術講演会プログラム・抄録集   149回   31 - 31   2021.6

     More details

    Language:Japanese   Publisher:東北連合産科婦人科学会・北日本産科婦人科学会  

    J-GLOBAL

    researchmap

  • 骨・軟部腫瘍のgermline findingsに対する遺伝子医療部門の取り組み

    二川 摩周, 中田 英二, 十川 麗美, 加藤 芙美乃, 浦川 優作, 河内 麻里子, 山本 英喜, 国定 俊之, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   95 ( 6 )   S1251 - S1251   2021.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • 遺伝性平滑筋腫症-腎細胞癌症候群関連腎細胞癌の術後骨転移に対してイピリムマブ・ニボルマブ併用療法が有効であった1例

    渡部 智文, 榮枝 一磨, 津川 昌也, 関戸 崇了, 富永 悠介, 高本 篤, 定平 卓也, 小林 泰之, 荒木 元朗, 渡邉 豊彦, 小田 和歌子, 黒田 直人, 十川 麗美, 山本 英喜, 平沢 晃, 那須 保友

    西日本泌尿器科   83 ( 1 )   9 - 9   2021.6

     More details

    Language:Japanese   Publisher:西日本泌尿器科学会  

    researchmap

  • がんゲノム医療におけるCRCの取り組みと役割

    宮本 理史, 奥田 浩人, 武田 達明, 難波 志穂子, 黒田 智, 平沢 晃, 千堂 年昭, 四方 賢一

    薬理と治療   49 ( 6 )   826 - 829   2021.6

     More details

    Language:Japanese   Publisher:ライフサイエンス出版(株)  

    J-GLOBAL

    researchmap

  • Clinical issues of companion diagnostics and hereditary tumors

    平沢晃

    日本遺伝カウンセリング学会誌   42 ( 2 )   37 - 37   2021.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Current status and issues regarding the operation of cancer genome profiling tests: A multi-institutional questionnaire survey-Focusing on addressing secondary findings-

    源明理, 山田崇弘, 山田崇弘, 吉岡正博, 吉岡正博, 近藤知大, 金井雅史, 春山瑳依子, 佐々木佑菜, 島田咲, 川崎秀徳, 川崎秀徳, 和田敬仁, 和田敬仁, 武藤学, 平沢晃, 小杉眞司, 小杉眞司

    日本遺伝カウンセリング学会誌   42 ( 2 )   70 - 70   2021.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Practice and report of genetic education using videos

    十川麗美, 山下範之, 河内麻里子, 二川摩周, 加藤芙美乃, 浦川優作, 山本英喜, 山本英喜, 冨田秀太, 平沢晃, 平沢晃

    日本遺伝カウンセリング学会誌   42 ( 2 )   119 - 119   2021.6

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • がんゲノム医療と緩和医療

    平沢 晃

    Palliative Care Research   16 ( Suppl. )   S22 - S22   2021.6

     More details

    Language:Japanese   Publisher:(NPO)日本緩和医療学会  

    J-GLOBAL

    researchmap

  • 遺伝性平滑筋腫症-腎細胞癌症候群関連腎細胞癌の術後骨転移に対してイピリムマブ・ニボルマブ併用療法が有効であった1例

    渡部 智文, 榮枝 一磨, 津川 昌也, 関戸 崇了, 富永 悠介, 高本 篤, 定平 卓也, 小林 泰之, 荒木 元朗, 渡邉 豊彦, 小田 和歌子, 黒田 直人, 十川 麗美, 山本 英喜, 平沢 晃, 那須 保友

    西日本泌尿器科   83 ( 1 )   9 - 9   2021.6

     More details

    Language:Japanese   Publisher:(一社)西日本泌尿器科学会  

    researchmap

  • 骨・軟部腫瘍のgermline findingsに対する遺伝子医療部門の取り組み

    二川 摩周, 中田 英二, 十川 麗美, 加藤 芙美乃, 浦川 優作, 河内 麻里子, 山本 英喜, 国定 俊之, 平沢 晃, 尾崎 敏文

    日本整形外科学会雑誌   95 ( 6 )   S1251 - S1251   2021.6

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    researchmap

  • 【卵巣癌におけるHRDとPARP阻害薬の効果】遺伝性乳癌卵巣癌症候群の診療

    坂井 美佳, 竹原 和宏, 平沢 晃

    産婦人科の実際   70 ( 5 )   501 - 508   2021.5

     More details

    Language:Japanese   Publisher:金原出版(株)  

    <文献概要>遺伝性乳癌卵巣癌症候群(HBOC)はBRCA1/2生殖細胞系列病的バリアントに起因する遺伝性腫瘍で,乳癌,卵巣癌,膵癌,前立腺癌の発症リスクが高い。HBOCの診断は,がん既発症者では二次がんの対策につながり,がん未発症者においても関連がんの予防やサーベイランスの実施につながる。卵巣癌におけるHBOCの割合は約15%と高頻度であり,発症年齢や家族歴にかかわらず全例にBRCA1/2遺伝学的検査が推奨されている。わが国では,卵巣癌あるいは乳癌既発症のHBOC症例に対する遺伝カウンセリング,遺伝学的検査,サーベイランス,リスク低減手術は保険診療となっている。HBOCは「診断・予防・治療」で一貫した医療介入が可能であり,その診療には産婦人科と遺伝医療のシームレスな連携が求められる。

    J-GLOBAL

    researchmap

  • 婦人科領域の遺伝性(家族性)腫瘍と細胞診の役割について

    進 伸幸, 山上 亘, 平沢 晃

    日本臨床細胞学会雑誌   60 ( Suppl.1 )   90 - 90   2021.5

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 婦人科領域の遺伝性(家族性)腫瘍と細胞診の役割について

    進 伸幸, 山上 亘, 平沢 晃

    日本臨床細胞学会雑誌   60 ( Suppl.1 )   90 - 90   2021.5

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 著明なALP高値を契機に発見された若年発症の副甲状腺癌の1例

    長谷川 功, 大塚 勇輝, 原田 洸, 中野 靖浩, 安田 美帆, 萩谷 英大, 三好 智子, 小川 弘子, 小野 早和子, 枝園 忠彦, 平沢 晃, 柳井 広之, 大塚 文男

    日本内分泌学会雑誌   97 ( 1 )   277 - 277   2021.4

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • Germline variants for precision oncology and companion diagnosis in gynecologic tumors

    平沢晃

    日本産科婦人科学会雑誌   73 ( 4 )   559 - 565   2021.4

     More details

    Authorship:Lead author   Language:Japanese  

    J-GLOBAL

    researchmap

  • 治療法の再整理とアップデートのために 専門家による私の治療 遺伝性乳癌卵巣癌症候群

    平沢 晃

    日本医事新報   ( 5058 )   40 - 41   2021.4

     More details

    Language:Japanese   Publisher:(株)日本医事新報社  

    researchmap

  • 【産婦人科患者説明ガイド-納得・満足を引き出すために】悪性腫瘍 がん遺伝子パネル検査を行うにあたっての患者説明

    坂井 美佳, 竹原 和宏, 平沢 晃

    臨床婦人科産科   75 ( 4 )   354 - 361   2021.4

     More details

    Language:Japanese   Publisher:(株)医学書院  

    J-GLOBAL

    researchmap

  • 【産婦人科患者説明ガイド-納得・満足を引き出すために】悪性腫瘍 コンパニオン診断を行うにあたっての患者説明

    坂井 美佳, 竹原 和宏, 平沢 晃

    臨床婦人科産科   75 ( 4 )   362 - 369   2021.4

     More details

    Language:Japanese   Publisher:(株)医学書院  

    J-GLOBAL

    researchmap

  • 遺伝性平滑筋腫症-腎細胞癌症候群関連腎細胞癌の術後骨転移に対してイピリムマブ・ニボルマブ併用療法が有効であった1例

    渡部 智文, 榮枝 一磨, 津川 昌也, 関戸 崇了, 富永 悠介, 高本 篤, 定平 卓也, 小林 泰之, 荒木 元朗, 渡邉 豊彦, 小田 和歌子, 黒田 直人, 十川 麗美, 山本 英喜, 平沢 晃, 那須 保友

    西日本泌尿器科   83 ( 1 )   31 - 36   2021.4

     More details

    Language:Japanese   Publisher:西日本泌尿器科学会  

    researchmap

  • 遺伝性腫瘍に対する包括的な取り組みと問題点 家族性膵がんおよび遺伝性膵がんに対する当院の包括的な取り組み

    阿部 紘大, 北郷 実, 林田 哲, 八木 洋, 阿部 雄太, 長谷川 康, 堀 周太郎, 田中 真之, 中野 容, 植木 有紗, 平沢 晃, 小崎 健次郎, 北川 雄光

    日本外科学会定期学術集会抄録集   121回   NES - 1   2021.4

     More details

    Language:Japanese   Publisher:(一社)日本外科学会  

    J-GLOBAL

    researchmap

  • 遺伝性腫瘍に対する包括的な取り組みと問題点 消化器系遺伝性腫瘍のスクリーニングとサーベイランスのための早期介入プログラムの構築

    重安 邦俊, 武田 正, 矢野 修也, 二川 摩周, 山本 英喜, 近藤 喜太, 寺石 文則, 香川 俊輔, 平沢 晃, 藤原 俊義

    日本外科学会定期学術集会抄録集   121回   NES - 4   2021.4

     More details

    Language:Japanese   Publisher:(一社)日本外科学会  

    J-GLOBAL

    researchmap

  • Genome medicine in sarcoma

    中田英二, 藤原智洋, 国定俊之, 尾崎敏文, 遠西大輔, 冨田秀太, 平沢晃, 二川摩周, 武田達明

    別冊整形外科   ( 79 )   75 - 83   2021.4

  • 遺伝性腫瘍に対する包括的な取り組みと問題点 消化器系遺伝性腫瘍のスクリーニングとサーベイランスのための早期介入プログラムの構築

    重安 邦俊, 武田 正, 矢野 修也, 二川 摩周, 山本 英喜, 近藤 喜太, 寺石 文則, 香川 俊輔, 平沢 晃, 藤原 俊義

    日本外科学会定期学術集会抄録集   121回   NES - 4   2021.4

     More details

    Language:Japanese   Publisher:(一社)日本外科学会  

    researchmap

  • 遺伝性腫瘍に対する包括的な取り組みと問題点 家族性膵がんおよび遺伝性膵がんに対する当院の包括的な取り組み

    阿部 紘大, 北郷 実, 林田 哲, 八木 洋, 阿部 雄太, 長谷川 康, 堀 周太郎, 田中 真之, 中野 容, 植木 有紗, 平沢 晃, 小崎 健次郎, 北川 雄光

    日本外科学会定期学術集会抄録集   121回   NES - 1   2021.4

     More details

    Language:Japanese   Publisher:(一社)日本外科学会  

    researchmap

  • RRSO検体におけるp53 signatureとSTICの特性に関する検討

    赤羽 智子, 増田 健太, 平沢 晃, 小林 佑介, 永井 晋平, 千代田 達幸, 林 茂徳, 片岡 史夫, 冨永 英一郎, 阪埜 浩司, 田中 守, 青木 大輔

    日本産科婦人科学会雑誌   73 ( 臨増 )   S - 570   2021.3

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    J-GLOBAL

    researchmap

  • ウイメンズヘルス HBOC~婦人科の立場から

    坂井 美佳, 平沢 晃

    CANCER BOARD of the BREAST   6 ( 2 )   53 - 57   2021.2

     More details

  • ウイメンズヘルス HBOC 婦人科の立場から

    坂井 美佳, 平沢 晃

    Cancer Board of the Breast   6 ( 2 )   125 - 129   2021.2

  • 【最新産婦人科遺伝診療ABC】婦人科腫瘍領域における遺伝診療総論

    坂井 美佳, 竹原 和宏, 平沢 晃

    産科と婦人科   88 ( 1 )   65 - 72   2021.1

     More details

    Language:Japanese   Publisher:(株)診断と治療社  

    遺伝性乳がん卵巣がん症候群(HBOC)やLynch症候群を代表とする遺伝性腫瘍は婦人科腫瘍とのかかわりが深い。特にごく最近では2019年のBRCA1/2遺伝学的検査のコンパニオン診断とがんゲノム医療の保険診療化、そして2020年4月のHBOC診療の一部保険診療化に伴い、産婦人科医にとって遺伝性腫瘍の知識は不可欠なものとなっている。個々の遺伝情報を知ることは、がん治療および予防の観点から有用性が高い。(著者抄録)

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2021&ichushi_jid=J00525&link_issn=&doc_id=20201221170010&doc_link_id=%2Fae4sanke%2F2021%2F008801%2F011%2F0065b0072%26dl%3D3&url=https%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Fae4sanke%2F2021%2F008801%2F011%2F0065b0072%26dl%3D3&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_4.gif

  • Precision oncology and germline findings.

    平沢晃

    月刊腫瘍内科   27 ( 1 )   43 - 46   2021.1

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 閉経前の子宮頸癌患者における同時化学放射線療法が骨密度に及ぼす影響とホルモン補充療法の効果

    谷本 慧子, 横田 めぐみ, 田中 恒成, 陳 冠良, 加藤 侑希, 西尾 浩, 仲村 勝, 山上 亘, 森定 徹, 片岡 史夫, 冨永 英一郎, 平沢 晃, 弟子丸 亮太, 岩田 卓, 阪埜 浩司, 青木 大輔

    日本婦人科腫瘍学会雑誌   39 ( 1 )   341 - 341   2021.1

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 初代卵巣癌組織を用いた3次元オルガノイド培養法の確立

    南木 佳子, 千代田 達幸, 平沢 晃, 大久保 亜紀, 伊藤 学, 赤羽 智子, 早乙女 啓子, 同前 愛, 平野 卓朗, 黒田 由香, 吉村 拓馬, 山上 亘, 片岡 史夫, 青木 大輔

    日本婦人科腫瘍学会雑誌   39 ( 1 )   392 - 392   2021.1

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 遺伝性乳癌卵巣癌(HBOC)の婦人科実地診療における課題

    坂井 美佳, 岡村 弥妃, 松山 裕美, 高畑 敬之, 横山 貴紀, 友野 勝幸, 藤本 悦子, 山本 弥寿子, 大亀 真一, 大住 省三, 平沢 晃, 竹原 和宏

    日本婦人科腫瘍学会雑誌   39 ( 1 )   431 - 431   2021.1

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • グルココルチコイド反応性アルドステロン症の1家系に発症前診断しえた2例

    中野 靖浩, 岩田 菜穂子, 長谷川 高誠, 越智 可奈子, 山本 紘一郎, 高瀬 了輔, 長谷川 功, 堀口 繁, 山本 英喜, 平沢 晃, 大塚 文男

    日本内分泌学会雑誌   96 ( 3 )   782 - 782   2021.1

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • Current practices for reporting germline findings on multi-gene tumor testing

    坂井美佳, 坂井美佳, 二川摩周, 加藤芙美乃, 十川麗美, 浦川優作, 河内麻里子, 河内麻里子, 山本英喜, 山本英喜, 平沢晃, 平沢晃

    日本臨床腫瘍学会学術集会(CD-ROM)   18th   2021

  • 遺伝情報の診療録における取り扱いに関するアンケート調査から見えた課題

    浦川優作, 浦川優作, 二川摩周, 二川摩周, 十川麗美, 加藤芙美乃, 植野さやか, 植野さやか, 河内麻里子, 山本英喜, 山本英喜, 平沢晃, 平沢晃

    日本人類遺伝学会大会プログラム・抄録集   66th (CD-ROM)   2021

  • 診療科横断的な遺伝性大腸癌診療体制の構築

    重安邦俊, 武田正, 矢野修也, 二川摩周, 加藤芙美乃, 十川麗美, 山本英喜, 香川俊輔, 平沢晃, 藤原俊義

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   27th   2021

  • 認定遺伝カウンセラーからみた遺伝性腫瘍を有する患者・家族へのサポート体制

    二川 摩周, 浦川 優作, 十川 麗美, 河内 麻里子, 山本 英喜, 平沢 晃

    日本癌学会総会記事   80th   [SP1 - 4]   2021

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • 遺伝性がん 遺伝情報の診療録の取り扱いに関する課題

    浦川 優作, 二川 摩周, 十川 麗美, 加藤 芙美乃, 植野 さやか, 河内 麻里子, 山本 英喜, 平沢 晃

    日本癌学会総会記事   80th   [SST6 - 5]   2021

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • がんゲノム医療で見つかるPGPVsの特徴

    十川 麗美, 山本 英喜, 河内 麻里子, 二川 摩周, 浦川 優作, 遠西 大輔, 冨田 秀太, 平沢 晃

    日本癌学会総会記事   80th   [P7 - 7]   2021

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • Precision cancer medicine through collaboration

    平沢晃

    日本がん転移学会学術集会・総会プログラム抄録集   30th   2021

  • 子宮体癌と乳癌を合併したCowden症候群の1例

    間森智加, 河内麻里子, 加藤芙美乃, 二川摩周, 前田礼奈, 鳩野みなみ, 笹原麻子, 土井原博義, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   27th   2021

  • BRCA1およびSMAD4に病的バリアントを認めた一家系

    加藤芙美乃, 山本英喜, 山本英喜, 坂井美佳, 坂井美佳, 河内麻里子, 河内麻里子, 二川摩周, 十川麗美, 間森智加, 笹原麻子, 重安邦俊, 香川俊輔, 藤原俊義, 土井原博義, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   27th   2021

  • 婦人科領域の遺伝性(家族性)腫瘍と細胞診の役割について

    進伸幸, 山上亘, 平沢晃

    日本臨床細胞学会雑誌(Web)   60   2021

  • 私の治療 遺伝性乳癌卵巣癌症候群

    平沢晃

    週刊日本医事新報   ( 5058 )   2021

  • 当院の家族性および遺伝性膵がんに対する取り組み

    阿部紘大, 北郷実, 八木洋, 阿部雄太, 長谷川康, 堀周太郎, 田中真之, 中野容, 小崎健次郎, 平沢晃, 北川雄光

    膵臓(Web)   36 ( 3 )   2021

  • がんゲノム医療におけるPGPVに対する遺伝子医療部門の取り組み

    十川麗美, 河内麻里子, 二川摩周, 加藤芙美乃, 蓮岡佳代子, 浦川優作, 坂井美佳, 坂井美佳, 山本英喜, 山本英喜, 遠西大輔, 冨田秀太, 平沢晃, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   27th   2021

  • 遺伝性腫瘍教育により防ぎえた症例から学ぶ親世代のHBOC

    小川千加子, 十川麗美, 二川摩周, 加藤芙美乃, 河内麻里子, 依田尚之, 松岡敬典, 岡本和浩, 中村圭一郎, 平沢晃, 平沢晃, 増山寿

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   27th   2021

  • 乳癌診療におけるHBOC診療一部保険収載後の現状と取り組み

    河内麻里子, 河内麻里子, 山本英喜, 山本英喜, 加藤芙美乃, 十川麗美, 二川摩周, 間森智加, 鳩野みなみ, 笹原麻子, 露無祐子, 浦川優作, 浦川優作, 岩本高行, 枝園忠彦, 平成人, 土井原博義, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   27th   2021

  • BRCA1/2遺伝学的検査陰性でがん遺伝子プロファイル検査からBRCA1病的バリアントを認めた卵巣癌の1例

    二川摩周, 松岡敬典, 加藤芙美乃, 十川麗美, 浦川優作, 山本英喜, 山本英喜, 河内麻里子, 依田尚之, 小川千加子, 中村圭一郎, 増山寿, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   27th   2021

  • Treatment for colorectal liver metastasis: evolving paradigms and future perspectives

    楳田祐三, 田澤大, 矢野修也, 重安邦俊, 神崎洋光, 寺石文則, 黒田新士, 香川俊輔, 八木孝仁, 平沢晃, 岡田裕之, 藤原俊義

    日本がん転移学会学術集会・総会プログラム抄録集   30th   2021

  • 遺伝性腫瘍

    平沢晃

    日本臨床細胞学会雑誌(Web)   60   2021

  • 胆・膵癌におけるがん遺伝子パネル検査の課題-細胞診にできること-

    井上博文, 井上博文, 井上博文, 松岡博美, 實平悦子, 松岡昌志, 冨田秀太, 松本和幸, 堀口繁, 加藤博也, 山本英喜, 山本英喜, 柳井広之, 平沢晃

    日本臨床細胞学会雑誌(Web)   60   2021

  • がん遺伝子パネル検査でATMのPresumed Germline Pathogenic Variant(PGPV)が検出された3例

    加藤芙美乃, 山本英喜, 山本英喜, 十川麗美, 二川摩周, 浦川優作, 植野さやか, 河内麻里子, 遠西大輔, 冨田秀太, 平沢晃, 平沢晃

    日本人類遺伝学会大会プログラム・抄録集   66th (CD-ROM)   2021

  • OncoGuide NCCオンコパネルシステムの改定に伴う二次的所見開示推奨度に関するアンケート調査

    小杉眞司, 小杉眞司, 小杉眞司, 平沢晃, 平沢晃, 矢部一郎, 矢部一郎, 多田寛, 多田寛, 桑田健, 桑田健, 植木有紗, 植木有紗, 植木有紗, 織田克利, 織田克利, 平田真, 平田真, 東川智美, 東川智美, 久島周, 久島周, 金井雅史, 金井雅史, 佐藤友紀, 佐藤友紀, 加藤芙美乃, 加藤芙美乃, 小川昌宣, 小川昌宣, 福田博政, 福田博政

    日本人類遺伝学会大会プログラム・抄録集   66th (CD-ROM)   2021

  • 本邦の遺伝性乳癌卵巣癌症候群(HBOC)診療の課題点~婦人科がん治療医の実態調査から見えてきたこと~

    小林佑介, 増田健太, 増田健太, 平沢晃, 竹原和宏, 津田均, 渡部洋, 織田克利, 永瀬智, 万代昌紀, 岡本愛光, 八重樫伸生, 三上幹男, 榎本隆之, 青木大輔, 青木大輔

    日本人類遺伝学会大会プログラム・抄録集   66th (CD-ROM)   2021

  • 令和4年度診療報酬改定に向けた課題と取組み(悪性腫瘍領域)

    平沢晃

    日本人類遺伝学会大会プログラム・抄録集   66th (CD-ROM)   2021

  • Double heterozygoteとしてBRCA1/2のgermline pathogenic variants(GPV)を認めた卵巣癌の1例

    二川摩周, 二川摩周, 河内麻里子, 十川麗美, 加藤芙美乃, 浦川優作, 山本英喜, 山本英喜, 平沢晃, 平沢晃

    日本人類遺伝学会大会プログラム・抄録集   66th (CD-ROM)   2021

  • 婦人科がんにおけるゲノム医療 がんゲノム医療と遺伝性腫瘍

    平沢 晃

    日本産科婦人科学会雑誌   72 ( 12 )   1710 - 1712   2020.12

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 内側半月板後根断裂に対して経脛骨pull out修復術を施行した3例

    林 伸晃, 向山 俊輔, 相庭 温臣, 門田 領, 弓手 惇史, 平沢 累, 土岐 恭範, 具志堅 翔, 下山 勝仁

    静岡整形外科医学雑誌   13 ( 1-2 )   73 - 76   2020.12

     More details

    Language:Japanese   Publisher:静岡県整形外科医会  

    内側半月板後根断裂(MMPRT:medial meniscus posterior root tear)は内側半月板逸脱をきたし、膝関節軟骨の接触圧を増加させる疾患である。軽微な外傷で受傷し、受傷時に膝後内側部痛とpop音を聴取することが特徴であり、MRI検査でgiraffe neck sign等の特徴的な所見を認める。短期間での変形性膝関節症の進行や特発性膝関節骨壊死の発生が危惧されるため、早期診断と適切な治療が必要とされる。今回我々は従来のmulti-useガイドより骨孔作成を容易にするMMPRTガイドを用いて脛骨骨孔を作成し、経脛骨pull out修復術を施行した3例3膝の短期成績を評価した。内側逸脱量の進行を認めた症例で骨孔の作成位置が本来の骨孔位置に対して前方で作成されていた。変形性膝関節症の進行抑制につながる内側半月板逸脱の改善には骨孔を適切な位置に作成することが重要と考えられた。(著者抄録)

    researchmap

  • 最新版!ゲノム診断における細胞診【春秋シリーズ】がんゲノム医療に順応する細胞診検査体制 Rapid on-site evaluation:ROSEへの対応

    井上 博文, 松岡 博美, 實平 悦子, 松岡 昌志, 冨田 秀太, 平沢 晃, 柳井 広之

    日本臨床細胞学会雑誌   59 ( Suppl.2 )   480 - 480   2020.11

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • PALB2およびNBNの病的バリアントを認めた家族生膵癌家系の一例

    阿部 紘大, 植木 有紗, 浦川 優作, 北郷 実, 吉浜 智子, 南木 佳子, 北川 雄光, 青木 大輔, 小崎 健次郎, 平沢 晃

    日本癌学会総会記事   79回   OE7 - 4   2020.10

     More details

    Language:English   Publisher:日本癌学会  

    researchmap

  • がんゲノム医療の実地診療における課題

    平沢 晃

    臨床薬理   51 ( Suppl. )   S113 - S113   2020.10

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • 卵巣癌オルガノイドは元腫瘍組織の遺伝学的特徴を有する

    南木 佳子, 千代田 達幸, 平沢 晃, 大久保 亜希, 伊藤 学, 吉村 拓馬, 赤羽 智子, 山上 亘, 青木 大輔

    日本癌学会総会記事   79回   OE14 - 2   2020.10

     More details

    Language:English   Publisher:(一社)日本癌学会  

    J-GLOBAL

    researchmap

  • がん遺伝子パネル検査によって検出された正常多型が推定されるMUTYHスプライシングバリアント

    山本 利枝, 西阪 隆, 服部 結, 土井 美帆子, 篠崎 勝則, 石川 暢久, 山本 英喜, 平沢 晃, 原 鐵晃, 板本 敏行

    日本癌学会総会記事   79回   PJ7 - 8   2020.10

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 遺伝性腫瘍-最新情報と今後の方向性 がん遺伝子パネル検査によるがん個別化医療と遺伝性腫瘍への実効果

    山本 英喜, 久保 寿夫, 冨田 秀太, 遠西 大輔, 豊岡 伸一, 平沢 晃

    日本癌学会総会記事   79回   S21 - 5   2020.10

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 婦人科がんにおけるクリニカルシークエンス 婦人科がんゲノム医療と生殖細胞系列遺伝子バリアント

    平沢 晃

    日本癌治療学会学術集会抄録集   58回   SY27 - 4   2020.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • 生殖細胞系列BRCA1/2変異陽性者の乳癌の特徴

    永山 愛子, 林田 哲, 高橋 麻衣子, 関 朋子, 菅野 康吉, 平沢 晃, 北川 雄光

    日本癌治療学会学術集会抄録集   58回   O9 - 4   2020.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • がん遺伝子パネル検査におけるgermline findingsの頻度と遺伝学的診療への導入

    植木 有紗, 三須 久美子, 中村 康平, 永妻 晶子, 四十物 絵理子, 今井 光穂, 林 秀幸, 持田 かおり, 藤倉 知花, 中川 智貴, 毛利 凉, 谷嶋 成樹, 平沢 晃, 菅野 康吉, 西原 広史

    日本癌治療学会学術集会抄録集   58回   O62 - 4   2020.10

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • ALP高値から上縦隔に発見されたMEN1疑い副甲状腺機能亢進症の1例

    大塚 勇輝, 西村 義人, 原田 洸, 岡 浩介, 長谷川 功, 小川 弘子, 三好 智子, 花山 宜久, 枝園 忠彦, 平沢 晃, 大塚 文男

    日本内分泌学会雑誌   96 ( 2 )   549 - 549   2020.10

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • CYP11B1/B2キメラ遺伝子を確認した家族性アルドステロン症小児例

    中野 靖浩, 岩田 菜穂子, 長谷川 高誠, 越智 可奈子, 山本 紘一郎, 高瀬 了輔, 長谷川 功, 堀口 繁, 山本 英喜, 平沢 晃, 大塚 文男

    日本内分泌学会雑誌   96 ( 2 )   535 - 535   2020.10

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • 耳鼻咽喉科の新規医療 がんゲノム医療

    平沢 晃

    日本耳鼻咽喉科学会会報   123 ( 4 )   934 - 934   2020.9

     More details

    Language:Japanese   Publisher:(一社)日本耳鼻咽喉科学会  

    J-GLOBAL

    researchmap

  • 遺伝診療のアップデート 遺伝性乳がん卵巣がん診療の最新動向

    平沢 晃

    関東連合産科婦人科学会誌   57 ( 2 )   176 - 176   2020.6

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 遺伝診療のアップデート 遺伝性乳がん卵巣がん診療の最新動向

    平沢 晃

    関東連合産科婦人科学会誌   57 ( 2 )   176 - 176   2020.6

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • チームアプローチで実現するゲノム医療と薬剤師の役割 ゲノム医療におけるデータサイエンティストの役割と育成

    冨田 秀太, 森田 瑞樹, 山下 範之, 平沢 晃, 豊岡 伸一

    薬学雑誌   140 ( 5 )   657 - 661   2020.5

     More details

    Language:Japanese   Publisher:(公社)日本薬学会  

    次世代シークエンサーを用いた遺伝子パネル検査とそのデータ解析はゲノム医療の根幹であるにもかかわらず、その担い手であるデータサイエンティストが極端に不足している。基本的なデータ解析の流れを理解し、解析結果の解釈ができる人材育成が喫緊の課題である。遺伝子パネル検査の流れを概説するとともに、遺伝子変異量(TMB)の概念と遺伝子パネル検査におけるTMBの算出方法について解説した。

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2020&ichushi_jid=J01459&link_issn=&doc_id=20200528480008&doc_link_id=%2Fcs7yakug%2F2020%2F014005%2F010%2F0657-0661%26dl%3D0&url=http%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Fcs7yakug%2F2020%2F014005%2F010%2F0657-0661%26dl%3D0&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_2.gif

  • 悪性腹膜中皮腫細胞株KOG-1の3次元立体培養と2次元平面培養によるPEM薬剤感受性の比較

    赤羽 智子, 平沢 晃, 冨永 英一郎, 井本 逸勢, 大久保 亜希, 伊藤 学, 南木 佳子, 吉浜 智子, 増田 健太, 千代田 達幸, 山上 亘, 片岡 史夫, 青木 大輔

    日本臨床細胞学会雑誌   59 ( Suppl.1 )   187 - 187   2020.5

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • チームアプローチで実現するゲノム医療と薬剤師の役割 ゲノム医療におけるデータサイエンティストの役割と育成

    冨田 秀太, 森田 瑞樹, 山下 範之, 平沢 晃, 豊岡 伸一

    薬学雑誌   140 ( 5 )   657 - 661   2020.5

     More details

    Language:Japanese   Publisher:(公社)日本薬学会  

    次世代シークエンサーを用いた遺伝子パネル検査とそのデータ解析はゲノム医療の根幹であるにもかかわらず、その担い手であるデータサイエンティストが極端に不足している。基本的なデータ解析の流れを理解し、解析結果の解釈ができる人材育成が喫緊の課題である。遺伝子パネル検査の流れを概説するとともに、遺伝子変異量(TMB)の概念と遺伝子パネル検査におけるTMBの算出方法について解説した。

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2020&ichushi_jid=J01459&link_issn=&doc_id=20200528480008&doc_link_id=%2Fcs7yakug%2F2020%2F014005%2F010%2F0657-0661%26dl%3D0&url=http%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Fcs7yakug%2F2020%2F014005%2F010%2F0657-0661%26dl%3D0&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_2.gif

  • Precision medicineクリニカルシークエンスの現状と課題 がんクリニカルシークエンスと生殖細胞系列バリアントへの対応

    平沢 晃

    日本婦人科腫瘍学会雑誌   38 ( 2 )   101 - 105   2020.4

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • がんゲノム医療が婦人科実地臨床に本格導入される際の留意点は? 保険適用の条件等、多岐にわたる

    平沢 晃, 佐々木 愛子

    日本医事新報   ( 5008 )   58 - 59   2020.4

     More details

    Language:Japanese   Publisher:(株)日本医事新報社  

    researchmap

  • 【徹底解説!卵巣がんの最新治療-複雑化する治療を整理する】新規治療薬の作用機序と使いどころ《コンパニオン診断》 卵巣がんに対するコンパニオン診断の使い方

    平沢 晃

    臨床婦人科産科   74 ( 3 )   317 - 323   2020.4

     More details

    Language:Japanese   Publisher:(株)医学書院  

    <文献概要>●マイクロサテライト不安定性(MSI)検査は,免疫チェックポイント阻害薬ペムブロリズマブの選択を目的としたコンパニオン診断に用いられる.●BRCA1/2遺伝学的検査は,BRCA1/2陽性の卵巣がんに対する初回化学療法後の維持療法にPARP阻害薬オラパリブを使用するためのコンパニオン診断に用いられる.●卵巣がんのコンパニオン診断を契機として,Lynch症候群や遺伝性乳がん卵巣がん(Hereditary breast and ovarian cancer: HBOC)などの遺伝性腫瘍が判明することがある.知ることのメリットを活かす対応が重要である.

    J-GLOBAL

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2020&ichushi_jid=J01564&link_issn=&doc_id=20200414050003&doc_link_id=10.11477%2Fmf.1409209936&url=https%3A%2F%2Fdoi.org%2F10.11477%2Fmf.1409209936&type=%88%E3%8F%91.jp_%83I%81%5B%83%8B%83A%83N%83Z%83X&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00024_2.gif

  • 【やさしくわかる 産科婦人科検査マスターブック】(第2章)婦人科腫瘍分野 マイクロサテライト不安定性検査

    平沢 晃

    産科と婦人科   87 ( Suppl. )   118 - 120   2020.3

     More details

    Language:Japanese   Publisher:(株)診断と治療社  

    J-GLOBAL

    researchmap

  • がんゲノム医療における遺伝子パネル検査と遺伝性腫瘍

    平沢 晃

    Urology Today   27 ( 1 )   8 - 12   2020.3

     More details

    Language:Japanese   Publisher:アステラス製薬(株)  

    researchmap

  • 多発小腸GISTに対し手術を施行した神経線維腫症1型の1例

    母里 淑子, 重安 邦俊, 吉岡 貴裕, 永坂 岳司, 原賀 順子, 香川 俊輔, 寺石 文則, 豊岡 伸一, 平沢 晃, 藤原 俊義

    家族性腫瘍   19 ( 2 )   77 - 82   2020.2

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    症例は54歳男性.大量出血を伴う小腸多発GIST(Gastrointestinal stromal tumor)を認めて緊急入院となった.姉が神経線維腫症1型(neurofibromatosis type 1:NF1)と診断されており,患者にもおよそ20個の神経線維腫を疑う腫瘤とcafe au lait斑を6個以上認めたためNF1と診断した.出血コントロール目的に開腹手術を行ったが,GISTはおよそ20個多発しており,大量小腸切除を避けるために10mm以上の腫瘍のみ外科的切除を行い,多発微小腫瘍は経過観察とした不完全切除を選択した.切除標本の病理検査では紡錘形核と好酸性胞体を有する紡錘形細胞が密に錯綜する腫瘍を認め,免疫染色でKIT陽性.核分裂数は5以下/50HPFsであり低悪性度GISTと診断した.NF1に伴うGISTは比較的予後が良いとの報告もあるが,このような多発微小病変については明らかな治療指針がない.今後さらなる症例の集積と検討を要する.(著者抄録)

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2020&ichushi_jid=J03931&link_issn=&doc_id=20200310200005&doc_link_id=10.18976%2Fjsft.19.2_77&url=https%3A%2F%2Fdoi.org%2F10.18976%2Fjsft.19.2_77&type=J-STAGE&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00007_3.gif

  • がんゲノム医療時代の幕開け

    中谷 中, 平沢 晃, 谷田部 恭, 宮地 勇人

    Modern Media   66 ( 1 )   1 - 23   2020.1

     More details

    Language:Japanese   Publisher:栄研化学(株)  

    researchmap

  • がん遺伝子パネル検査実施に伴う看護体制の構築

    蓮岡佳代子, 西本仁美, 平沢晃

    日本がん看護学会学術集会(Web)   34th   [O13 - 059]   2020

     More details

    Language:Japanese   Publisher:(一社)日本がん看護学会  

    J-GLOBAL

    researchmap

  • 肉腫診療における認定遺伝カウンセラーの役割

    二川摩周, 中田英二, 十川麗美, 浦川優作, 河内麻里子, 山本英喜, 遠西大輔, 西森久和, 国定俊之, 尾崎敏文, 平沢晃, 平沢晃

    日本整形外科学会雑誌   94 ( 6 )   S1381 - S1381   2020

     More details

    Language:Japanese   Publisher:(公社)日本整形外科学会  

    J-GLOBAL

    researchmap

  • ゲノム医療におけるエキスパートパネル【がんゲノム医療中核拠点病院でのエキスパートパネル】岡山大学のエキスパートパネル

    柳井広之, 都地友紘, 谷口恒平, 西田賢司, 井上博文, 井上博文, 松岡博美, 平沢晃, 平沢晃, 河内麻里子, 河内麻里子, 山本英喜, 山本英喜, 冨田秀太, 冨田秀太, 遠西大輔

    病理と臨床   38 ( 6 )   527 - 530   2020

     More details

    Language:Japanese   Publisher:(株)文光堂  

    J-GLOBAL

    researchmap

  • フィンランドにおけるゲノム情報・医療情報の利活用のための基盤整備

    中田はる佳, 中田はる佳, 平沢晃

    遺伝子医学   10 ( 3 )   151 - 157   2020

     More details

    Language:Japanese   Publisher:(株)メディカルドゥ  

    日本では,次世代医療基盤法の施行や,医療分野のデータベース整備など医療情報の二次利用促進が期待される。これらの運用に際して,海外の先進的な取り組みが参考になる。フィンランドでは,個人の情報は電子化され,これらを二次利用する法整備が進んでいる。一つはゲノム法案で,公的ゲノム情報データベースの構築が予定されている。もう一つは社会健康情報の二次利用に関する法律で,本人の再同意なく各データベースの情報を連結して二次利用できる。日本でも,市民・患者の理解を得ながら医療情報の二次利用と同意のあり方を検討していく必要がある。(著者抄録)

    J-GLOBAL

    researchmap

  • 婦人科医が知っておくべきがん遺伝子パネル検査の基礎知識 III.がん遺伝子パネル検査結果の取り扱いと解釈 Germline findingsの取り扱い

    坂井美佳, 坂井美佳, 竹原和宏, 平沢晃

    産婦人科の実際   69 ( 7 )   721 - 727   2020

     More details

    Language:Japanese   Publisher:金原出版(株)  

    <文献概要>がん遺伝子パネル検査では,腫瘍の体細胞病的バリアントを検出すると同時に生殖細胞系列バリアント(germline variants)が同定されることがある(germline findings)。生殖細胞系列バリアントから得られる遺伝情報は,患者本人の治療法選択および二次がんの予防へつながり,さらに血縁者のがん予防・健康管理につなげることが可能な場合がある。生殖細胞系列バリアントは生涯変化せず,血縁者間で一部共有される情報である。また,血縁者における将来のがん発症予測が可能な場合がある。卵巣癌などの婦人科がんは他がん種と比較してgermline findingsが比較的高頻度に検出されることが知られている。生殖細胞系列バリアントの適切な取り扱いは,がん診療にかかわるすべての産婦人科医が身につけておくべき知識である。

    J-GLOBAL

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2020&ichushi_jid=J00535&link_issn=&doc_id=20200731060008&doc_link_id=10.18888%2Fsp.0000001328&url=https%3A%2F%2Fdoi.org%2F10.18888%2Fsp.0000001328&type=%88%E3%8F%91.jp_%83I%81%5B%83%8B%83A%83N%83Z%83X&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00024_2.gif

  • The present status and attitudes for reporting secondary findings in genomic analysis using a next-generation sequencer: A nation-wide questionnaire survey of clinical genetic professionals in Japan

    土屋実央, 山田崇弘, 赤石理奈, 井本逸勢, 梅村啓史, 清水健司, 浜之上はるか, 平沢晃, 吉田晶子, 吉橋博史, 四元淳子, 渡邉淳, 小杉眞司

    日本遺伝カウンセリング学会誌   41 ( 2 )   141 - 141   2020

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 閉経前の子宮頸癌患者における同時化学放射線療法が骨密度に及ぼす影響とホルモン補充療法の効果

    谷本慧子, 横田めぐみ, 西尾浩, 仲村勝, 森定徹, 弟子丸亮太, 平沢晃, 岩田卓, 田中守, 青木大輔

    日本産科婦人科学会雑誌   72 ( 臨増 )   S - 432   2020

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    J-GLOBAL

    researchmap

  • Cancer Precision Medicine and Germline Findings

    平沢晃

    日本産科婦人科学会雑誌   72 ( 12 )   S - 74   2020

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • がんゲノム医療の実地診療における課題

    平沢晃

    臨床薬理   51 ( Supplement )   S113 - S113   2020

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    J-GLOBAL

    researchmap

  • Cancer Precision Medicine and Germline Findings

    平沢晃

    日本産科婦人科学会雑誌   72 ( 12 )   1710 - 1712   2020

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • ALP高値から上縦隔に発見されたMEN1疑い副甲状腺機能亢進症の1例

    大塚勇輝, 西村義人, 原田洸, 岡浩介, 長谷川功, 小川弘子, 三好智子, 花山宜久, 枝園忠彦, 平沢晃, 大塚文男

    日本内分泌学会雑誌   96 ( 2 )   549 - 549   2020

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • ゲノム情報を活用した遺伝性乳癌卵巣癌診療の標準化と先制医療実装にむけたエビデンス構築に関する研究 HBOCに関する市民の認識の向上に関する研究

    平沢晃, 櫻井晃洋

    ゲノム情報を活用した遺伝性乳癌卵巣癌診療の標準化と先制医療実装にむけたエビデンス構築に関する研究 令和元年度 総括研究報告書(Web)   2020

  • 耳鼻咽喉科の新規医療 がんゲノム医療

    平沢晃

    日本耳鼻咽喉科学会会報   123 ( 4 )   934 - 934   2020

     More details

    Language:Japanese   Publisher:(一社)日本耳鼻咽喉科学会  

    J-GLOBAL

    researchmap

  • 希少MSI-H大腸癌患者由来組織片を用いたマウスモデル(PDX)による擬似クローン化の試み

    矢野修也, 矢野修也, 重安邦俊, 三村直毅, 岸本浩行, 母里淑子, 黒田新士, 近藤喜太, 寺石文則, 香川俊輔, 平沢晃, 藤原俊義

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • ゲノム情報を活用した遺伝性乳癌卵巣癌診療の標準化と先制医療実装にむけたエビデンス構築に関する研究

    青木大輔, 平沢晃

    ゲノム情報を活用した遺伝性乳癌卵巣癌診療の標準化と先制医療実装にむけたエビデンス構築に関する研究 令和元年度 総括研究報告書(Web)   2020

  • Practical impacts of multi-gene cancer profiling on cancer precision medicine and hereditary tumor

    山本英喜, 山本英喜, 久保寿夫, 冨田秀太, 遠西大輔, 豊岡伸一, 豊岡伸一, 平沢晃

    日本癌学会学術総会抄録集(Web)   79th   S21 - 5   2020

     More details

    Language:English   Publisher:日本癌学会  

    J-GLOBAL

    researchmap

  • CYP11B1/B2キメラ遺伝子を確認した家族性アルドステロン症小児例

    中野靖浩, 岩田菜穂子, 長谷川高誠, 越智可奈子, 山本紘一郎, 高瀬了輔, 長谷川功, 堀口繁, 山本英喜, 平沢晃, 大塚文男

    日本内分泌学会雑誌   96 ( 2 )   535 - 535   2020

     More details

    Language:Japanese   Publisher:(一社)日本内分泌学会  

    J-GLOBAL

    researchmap

  • Ovarian cancer organoids recapitulate genomic alterations of the parental tumors.

    南木佳子, 千代田達幸, 平沢晃, 大久保亜希, 伊藤学, 吉村拓馬, 赤羽智子, 山上亘, 青木大輔

    日本癌学会学術総会抄録集(Web)   79th   OE14 - 2   2020

     More details

    Language:English   Publisher:日本癌学会  

    J-GLOBAL

    researchmap

  • A plausible normal polymorphism of MUTYH splicing variant detected through multi-gene cancer panel testing

    山本利枝, 山本利枝, 西阪隆, 西阪隆, 西阪隆, 服部結, 服部結, 土井美帆子, 篠崎勝則, 篠崎勝則, 石川暢久, 石川暢久, 山本英喜, 山本英喜, 平沢晃, 原鐵晃, 原鐵晃, 板本敏行, 板本敏行

    日本癌学会学術総会抄録集(Web)   79th   PJ7 - 8   2020

     More details

    Language:English   Publisher:日本癌学会  

    J-GLOBAL

    researchmap

  • BRCA1VUS保持卵巣癌例おけるバリアントの病的意義に関する検討

    赤羽智子, 赤羽智子, 西原広史, 平沢晃, 平沢晃, 平沢晃, 井本逸勢, 井本逸勢, 増田健太, 坂本一平, 野原祥夫, 谷嶋成樹, 青木大輔

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • 遺伝性乳がん卵巣がん診療の課題

    坂井美佳, 坂井美佳, 坂井美佳, 岡村弥妃, 松山裕美, 横山貴紀, 藤本悦子, 山本弥寿子, 大亀真一, 大亀真一, 小林成行, 小林成行, 堀伸一郎, 堀伸一郎, 大住省三, 大住省三, 平沢晃, 竹原和宏, 竹原和宏

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • がんゲノムプロファイリング検査によって同定または疑われた生殖細胞系列バリアントに対するGermline boardの取り組み

    二川摩周, 十川麗美, 浦川優作, 坂井美佳, 山本英喜, 河内麻里子, 河内麻里子, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • ペムブロリズマブ使用中に下垂体機能低下症を来たしステロイド投与が著効した高頻度マイクロサテライト不安定性大腸癌の1例

    重安邦俊, 岸本浩行, 母里淑子, 武田正, 矢野修也, 黒田新士, 近藤喜太, 寺石文則, 香川俊輔, 平沢晃, 藤原俊義

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • 遺伝性乳がん卵巣がん診療の最新動向

    平沢晃

    関東連合産科婦人科学会誌(Web)   57 ( 2 )   2020

  • がんゲノム医療に順応する細胞診検査体制~Rapid on-site evaluation:ROSEへの対応~

    井上博文, 井上博文, 松岡博美, 實平悦子, 松岡昌志, 冨田秀太, 平沢晃, 柳井広之

    日本臨床細胞学会雑誌(Web)   59   2020

  • がん医療から遺伝医療へつなげるために-がんゲノム医療外来に携わる看護師の立場から看護連携の必要性について-

    蓮岡佳代子, 西本仁美, 十川麗美, 二川摩周, 河内麻里子, 山本英喜, 遠西大輔, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • がん遺伝子パネル検査受検を契機にHBOCが判明し本人および血縁者介入につながった一例

    十川麗美, 小川千加子, 蓮岡佳代子, 冨田秀太, 井上博文, 松原岳大, 二川摩周, 浦川優作, 河内麻里子, 河内麻里子, 山本英喜, 増山寿, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • がん遺伝子パネル検査を施行した乳癌症例のGermline findingsに関する検討

    河内麻里子, 河内麻里子, 山本英喜, 坂井美佳, 梶原友紀子, 笹原麻子, 十川麗美, 二川摩周, 浦川優作, 岩本高行, 枝園忠彦, 平成人, 土井原博義, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • AYA世代発症の肉腫・希少がんに対するがん遺伝子プロファイリング検査の意義

    山本英喜, 河内麻里子, 十川麗美, 二川摩周, 浦川優作, 井上博文, 井上博文, 遠西大輔, 久保寿夫, 中田英二, 田端雅弘, 亀田雅博, 黒住和彦, 柳井広之, 嶋田明, 平沢晃, 平沢晃

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • 家族歴と血縁者のMSI-High大腸癌からLynch症候群を疑いMLH1がVUSであった大腸癌・乳癌の重複癌の1例

    梶原友紀子, 枝園忠彦, 藤原みわ, 鈴木陽子, 鳩野みなみ, 笹原麻子, 十川麗美, 二川摩周, 浦川優作, 河内麻里子, 河内麻里子, 山本英喜, 岩本高行, 平成人, 平沢晃, 土井原博義

    日本遺伝性腫瘍学会学術集会プログラム・抄録集   26th   2020

  • 厚生労働科学研究成果報告書 第3回 がんゲノム医療推進を目指した医療情報の利活用にかかる国内外の法的基盤の運用と課題に関する調査研究

    中田はる佳, 平沢晃, 田代志門, 丸祐一

    医療情報学   40 ( 1 )   2020

  • がんゲノム医療外来で遺伝性腫瘍が疑われた症例に関する詳細と当院の取り組み

    十川麗美, 河内麻里子, 二川摩周, 加藤芙美乃, 蓮岡佳代子, 浦川優作, 坂井美佳, 山本英喜, 山本英喜, 遠西大輔, 冨田秀太, 平沢晃, 平沢晃, 十川麗美

    日本人類遺伝学会大会プログラム・抄録集   65th (CD-ROM)   2020

  • 遺伝性腫瘍診療の診療における多遺伝子パネル検査の役割

    菅野康吉, 菅野康吉, 菅野康吉, 青木幸恵, 竹前大, 田辺記子, 渡辺智子, 牛尼美年子, 平田真, 吉田輝彦, 三須久美子, 植木有紗, 小崎健次郎, 平沢晃, 菅野康吉, 菅野康吉, 菅野康吉

    日本人類遺伝学会大会プログラム・抄録集   65th (CD-ROM)   2020

  • がん遺伝子パネル検査から判明したFH完全欠失の1例

    植木有紗, 植木有紗, 菅野康吉, 菅野康吉, 三須久美子, 中村康平, 谷嶋成樹, 田中伸之, 三上修司, 平沢晃, 平沢晃, 大家基嗣, 西原広史, 小崎健次郎, 植木有紗, 植木有紗

    日本人類遺伝学会大会プログラム・抄録集   65th (CD-ROM)   2020

  • 保険収載されたがん遺伝子パネル検査における実施状況と,生殖細胞系列バリアントへの対応状況に関する現状調査と課題提起

    小林明理, 山田崇弘, 山田崇弘, 吉岡正博, 吉岡正博, 近藤知大, 近藤知大, 金井雅史, 金井雅史, 木下一郎, 青木洋子, 青木洋子, 織田克利, 織田克利, 植木有紗, 植木有紗, 森川真紀, 森川真紀, 佐藤友紀, 佐藤友紀, 小川昌宣, 小川昌宣, 東川智美, 武藤学, 平沢晃, 平沢晃, 小杉眞司, 小杉眞司, 小杉眞司, 小林明理

    日本人類遺伝学会大会プログラム・抄録集   65th (CD-ROM)   2020

  • FoundationOne CDxから病的意義不明として検出されるバリアントに対する病的意義の再検討

    二川摩周, 浦川優作, 十川麗美, 加藤芙美乃, 坂井美佳, 河内麻里子, 山本英喜, 山本英喜, 冨田秀太, 平沢晃, 平沢晃, 二川摩周

    日本人類遺伝学会大会プログラム・抄録集   65th (CD-ROM)   2020

  • 国内バイオバンクに関する利活用ハンドブックの作成を通じたゲノム研究開発活性化の試み

    甲畑(照井)宏子, 長神風二, 武藤香織, 飯田香織, 秦健一郎, 田中敏博, 丸山英二, 平沢晃, 信國宇洋, 相澤弥生, 相澤弥生, 長谷川冬雪, 宮原麗子, 竹本暁, 川澄みゆり, 木村恵子, 吉田雅幸, 吉田雅幸

    日本人類遺伝学会大会プログラム・抄録集   65th (CD-ROM)   2020

  • がんゲノム医療におけるCRCの取り組みと役割

    宮本理史, 奥田浩人, 奥田浩人, 武田達明, 難波志穂子, 黒田智, 黒田智, 平沢晃, 千堂年昭, 四方賢一

    CRCと臨床試験のあり方を考える会議プログラム・抄録集   20th ( 6 )   826 - 829   2020

  • 悪性腹膜中皮腫細胞株KOG-1の3次元立体培養と2次元平面培養によるPEM薬剤感受性の比較

    赤羽智子, 赤羽智子, 平沢晃, 平沢晃, 冨永英一郎, 井本逸勢, 井本逸勢, 大久保亜希, 伊藤学, 南木佳子, 吉浜智子, 増田健太, 千代田達幸, 山上亘, 片岡史夫, 青木大輔

    日本臨床細胞学会雑誌(Web)   59   2020

  • がんゲノム医療実用化 岡山大学病院臨床遺伝子診療科の紹介.

    平沢 晃

    岡山医学会雑誌   132   25 - 28   2020

     More details

  • 北部方面衛生隊検閲野外病院集約型の成果について

    佐藤 晃, 沼田 秀樹, 三代川 和彦, 六渡 正則, 田中 淳一, 坂路 和弘, 平沢 宏太, 蝶野 元希

    防衛衛生   67 ( 別冊 )   106 - 106   2019.12

     More details

    Language:Japanese   Publisher:(一社)日本防衛衛生学会  

    researchmap

  • 遺伝子医療と女性ヘルスケア

    平沢 晃

    徳島産婦人科医報   ( 52 )   30 - 30   2019.10

     More details

    Language:Japanese   Publisher:徳島産科婦人科学会・徳島県産婦人科医会  

    researchmap

  • バイオバンクでの長期保存生体試料の品質管理標準化のための予備的検討

    山本 英喜, 松原 岳大, 森田 瑞樹, 冨田 秀太, 豊岡 伸一, 平沢 晃

    臨床病理   67 ( 補冊 )   283 - 283   2019.10

     More details

    Language:Japanese   Publisher:(一社)日本臨床検査医学会  

    J-GLOBAL

    researchmap

  • がんゲノム医療外来における看護連携に関する取り組み

    蓮岡 佳代子, 西本 仁美, 河内 麻里子, 平沢 晃

    日本癌治療学会学術集会抄録集   57回   O28 - 1   2019.10

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 遺伝性腫瘍

    平沢 晃

    日本臨床細胞学会雑誌   58 ( Suppl.2 )   493 - 493   2019.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 【がん免疫療法の個別化を支える 新・腫瘍免疫学】第II部 がん免疫療法の臨床開発における課題と対応 (第4章)臨床開発における重要ポイントと課題 がんゲノム医療・遺伝性腫瘍の課題

    平沢 晃

    実験医学   37 ( 15 )   2645 - 2650   2019.9

     More details

    Language:Japanese   Publisher:(株)羊土社  

    がん免疫療法を選択するうえでMSIやミスマッチ修復遺伝子の機能不全を検出する必要がある。このことはがん患者本人がリンチ症候群の原因となるミスマッチ修復遺伝子の病的バリアント保持者である可能性があるのみならず、その家系員が同じ遺伝子バリアントを保持している可能性を示すものである。医療者のなかにも、MSIやミスマッチ修復遺伝子の検査によってリンチ症候群が「わかってしまった、知ってしまった」という認識をもち、発言する人がいるが、この考えは不適切であるといえる。遺伝性腫瘍の生殖細胞系列バリアント保持者に対しては、がん発症者、未発症者ともにがん治療や予防対策を講じることが可能となるため、遺伝情報を知ることのメリットを認識すべきである。(著者抄録)

    researchmap

  • 【内科医に求められる他科の知識-専門家が伝えるDo/Don't】(第5章)産婦人科 卵巣がん・子宮体がんと遺伝

    平沢 晃

    内科   124 ( 3 )   1903 - 1906   2019.9

  • 我が国にゲノム医療を適切に展開するため備えるべき3つのこと

    平沢 晃

    日本歯科麻酔学会雑誌   47 ( 抄録号 )   94 - 94   2019.9

     More details

    Language:Japanese   Publisher:(一社)日本歯科麻酔学会  

    researchmap

  • 子宮体癌の術前子宮鏡検査と腹腔細胞診

    平野 卓朗, 山上 亘, 真壁 健, 坂井 健良, 二宮 委美, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   58 ( 5 )   196 - 201   2019.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    目的:子宮体癌の腹腔細胞診陽性の背景因子を明らかにし、子宮鏡検査が腹腔細胞診陽性に与える影響を検討することを目的とした。方法:当院にて子宮鏡検査を施行した後に、開腹もしくは腹腔鏡下に手術療法を施行した414例に関して、腹腔細胞診の結果と臨床病理学的因子との関連を後方視的に検討した。成績:414例中13例(3%)で腹腔細胞診陽性であった。腹腔細胞診陽性の有意なリスク因子として、単変量解析では類内膜癌Grade 3+特殊組織型、付属器転移、大網転移、腹膜播種が挙げられ(p<0.001)、多変量解析では類内膜癌Grade 3+特殊組織型(p=0.01)と大網転移が挙げられた(p<0.001)。またリスク因子別では大網転移陽性例で腹腔細胞診陽性例が最も多かった(7/10例、70%)。12例で腹腔細胞診陽性のリスク因子である類内膜癌Grade 3+特殊組織型もしくは大網転移を認めた。1例のみリスク因子を有さず腹腔細胞診が陽性となった症例を認め、多発子宮筋腫や子宮腺筋症によって、子宮鏡の検査時間や還流圧を通常より要したことが原因と推定されたが、術後再発を認めず経過している。結論:術前に子宮鏡検査を施行したにもかかわらず腹腔細胞診陽性となった例は少なく、そのほとんどが腹腔細胞診陽性のリスク因子を有する症例であったため、術前子宮鏡検査による腹腔細胞診への影響は軽微であろうと考えられた。(著者抄録)

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2019&ichushi_jid=J01209&link_issn=&doc_id=20191028260002&doc_link_id=%2Few5saibo%2F2019%2F005805%2F003%2F0196-0201%26dl%3D0&url=http%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Few5saibo%2F2019%2F005805%2F003%2F0196-0201%26dl%3D0&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_2.gif

  • ゲノム医療実用化と臨床実地での対応

    平沢 晃

    岡山医学会雑誌   131 ( 2 )   121 - 121   2019.8

     More details

    Language:Japanese   Publisher:岡山医学会  

    researchmap

  • Hereditary tumors and cancer prevention

    平沢晃

    岡山医学会雑誌   131 ( 2 )   83 - 87   2019.8

  • 病理コンパニオン診断と細胞診 がん遺伝子パネル検査の実地臨床での課題

    山本 英喜, 河内 麻里子, 井上 博文, 柳井 広之, 平沢 晃

    日本臨床細胞学会中国四国連合会会報   ( 34 )   13 - 13   2019.7

     More details

    Language:Japanese   Publisher:日本臨床細胞学会-中国四国連合会  

    researchmap

  • 病理コンパニオン診断と細胞診 がんゲノム医療を考慮した病理検体取扱いについて

    井上 博文, 冨田 秀太, 山本 英喜, 柳井 広之, 平沢 晃

    日本臨床細胞学会中国四国連合会会報   ( 34 )   15 - 15   2019.7

     More details

    Language:Japanese   Publisher:日本臨床細胞学会-中国四国連合会  

    researchmap

  • Precision medicineクリニカルシークエンスの現状と課題 がんクリニカルシークエンスと生殖細胞系列バリアントへの対応

    平沢 晃

    日本婦人科腫瘍学会雑誌   37 ( 3 )   323 - 323   2019.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 生殖細胞系列の遺伝子パネル検査をうけた、家族性の乳癌、卵巣癌が疑われた27例の検討

    千代田 達幸, 吉浜 智子, 早乙女 啓子, 同前 愛, 南木 佳子, 平野 卓朗, 小林 佑介, 山上 亘, 野村 弘行, 片岡 史夫, 植木 有紗, 平沢 晃, 青木 大輔

    日本婦人科腫瘍学会雑誌   37 ( 3 )   581 - 581   2019.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 若年性子宮体がん症例における妊孕性温存治療適応診断マーカーの開発

    平野 卓朗, 新井 恵吏, 真壁 健, 平沢 晃, 山上 亘, 進 伸幸, 青木 大輔, 金井 弥栄

    日本病理学会会誌   108 ( 1 )   412 - 412   2019.4

     More details

    Language:Japanese   Publisher:(一社)日本病理学会  

    J-GLOBAL

    researchmap

  • ADAM9のヒト卵巣明細胞癌での発現とシスプラチン誘導性癌細胞死抑制作用

    上野 万里, 潮見 隆之, 望月 早月, 下田 将之, 金井 弥栄, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔, 岡田 保典

    日本病理学会会誌   108 ( 1 )   307 - 307   2019.4

     More details

    Language:Japanese   Publisher:(一社)日本病理学会  

    J-GLOBAL

    researchmap

  • 岡山大学病院における大腸癌エキスパートパネル診療

    母里 淑子, 矢野 修也, 遠西 大輔, 田端 雅弘, 柳井 広之, 豊岡 伸一, 平沢 晃, 藤原 俊義

    日本外科学会定期学術集会抄録集   119回   PS - 1   2019.4

     More details

    Language:Japanese   Publisher:(一社)日本外科学会  

    researchmap

  • チームアプローチで実現するゲノム医療と薬剤師の役割 ゲノム医療におけるデータサイエンティストの役割と育成

    冨田 秀太, 森田 瑞樹, 山下 範之, 平沢 晃, 豊岡 伸一

    日本薬学会年会要旨集   139年会 ( 1 )   264 - 264   2019.3

     More details

    Language:Japanese   Publisher:(公社)日本薬学会  

    researchmap

  • がんゲノム医療の現状と課題〜その人らしさを支えるための個別化医療〜 がんゲノム医療を導入する際の課題 安心できるゲノム医療を展開するために

    平沢 晃

    日本がん看護学会誌   33 ( Suppl. )   115 - 115   2019.1

     More details

    Language:Japanese   Publisher:(一社)日本がん看護学会  

    researchmap

  • Release manga teaching materials for improving citizen’s literacy on cancer precision medicine

    十川麗美, 十川麗美, 和田敬仁, 金井雅史, 近藤知大, 近藤知大, 本田明夏, 永田美保, 馬場遥香, 山田崇弘, 平沢晃, 武藤学, 小杉眞司

    日本遺伝子診療学会大会プログラム・抄録集   26th ( 2 )   76 - 76   2019

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Development and practice for new way to expert knowledge and information to convey genome medicine

    小林朋子, 安田有理, 平沢晃, 吉田晶子, 加納圭, 飯野均, 川上雅弘, 長神風二

    日本遺伝子診療学会大会プログラム・抄録集   26th ( 2 )   77 - 77   2019

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • Multiple gastrointestinal stromal tumors of the small intestine in a patient with neurofibromatosis type 1: a case report

    母里淑子, 重安邦俊, 吉岡貴裕, 永坂岳司, 原賀順子, 香川俊輔, 寺石文則, 豊岡伸一, 平沢晃, 藤原俊義

    家族性腫瘍(Web)   19 ( 2 )   2019

  • 遺伝性腫瘍

    平沢晃

    日本臨床細胞学会雑誌(Web)   58   2019

  • がんゲノム医療連携病院で行う遺伝勉強会の意義と展望

    二川摩周, 大谷彰一郎, 川崎賢祐, 十川麗美, 江見裕美, 浦川優作, 山下範之, 東平翔子, 藤原奈央子, 山本英喜, 河内麻里子, 河内麻里子, 平沢晃, 平沢晃

    日本人類遺伝学会大会プログラム・抄録集   64th   2019

  • リキッドバイオプシーでBRCA1の生殖細胞系列病的バリアントが示唆され遺伝カウンセリングを通じて確定診断に至った一例

    十川麗美, 小川千加子, 蓮岡佳代子, 冨田秀太, 井上博文, 松原岳大, 二川摩周, 江見裕美, 浦川優作, 河内麻里子, 河内麻里子, 増山寿, 平沢晃, 平沢晃

    日本人類遺伝学会大会プログラム・抄録集   64th   2019

  • 新時代のホルモン療法マニュアル 第2章 D 腫瘍 8 女性がんの化学予防

    平沢晃

    産科と婦人科   86   2019

  • Clinical experience of PARPi and limitation in BRCAnalysis CDx

    星野舞, 星野舞, 星野舞, 植木有紗, 植木有紗, 青木優, 青木優, 武井眞, 酒井元, 酒井元, 酒井元, 中澤敦, 佐藤隆宣, 平沢晃, 平沢晃, 船越信介, 船越信介, 船越信介

    日本人類遺伝学会大会プログラム・抄録集   64th   2019

  • Lynch症候群 診断のピットフォール

    菅野康吉, 菅野康吉, 菅野康吉, 菅野康吉, 斎藤伸哉, 高井響子, 高井響子, 青木幸恵, 高橋雅博, 安東美穂, 吉田輝彦, 牛尼美年子, 田辺記子, 関根茂樹, 阪埜浩司, 平沢晃, 平沢晃, 三須久美子, 小崎健次郎

    日本家族性腫瘍学会学術集会プログラム・抄録集   25th   2019

  • 日赤和歌山医療センターにおけるHBOC診療の取り組み~家系情報は変化する~患者の気持ちも変化する~

    秋丸憲子, 中木村朋美, 林雪, 岩谷里恵, 亀田由紀, 豊福彩, 平沢晃, 芳林浩史

    日本家族性腫瘍学会学術集会プログラム・抄録集   25th   2019

  • 婦人科がん治療戦略としての個別化医療の展開〜基礎から臨床へ〜 婦人科遺伝性腫瘍およびがんゲノム異常の解析とゲノム医療実用化に向けた取り組み

    平沢 晃

    日本産科婦人科学会雑誌   70 ( 12 )   2521 - 2529   2018.12

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • フィンランドにおけるゲノム医療関連政策の動向

    中田 はる佳, 高島 響子, 吉田 幸恵, 永井 亜貴子, 平沢 晃

    家族性腫瘍   18 ( 2 )   42 - 47   2018.12

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    日本の状況に合わせた遺伝情報を含めた医療情報の利活用を支える法的・社会的基盤を整備するためには、まず医療情報の利活用先進国における、それらに関連する政策動向を明らかにすることが重要である。本研究では、がんゲノム医療との関連を見据えつつ、医療情報の利活用が進むフィンランドを参考として、日本で検討すべき課題を抽出し、今後の方針を検討することを目的として現地調査を行った。中でも、ゲノム法や社会健康情報の二次利用に関する法制定準備、FinnGenプロジェクトなどが注目すべき事項であった。日本への示唆として、既存の研究基盤の再活用、医療情報の二次利用を適正化するためのバイオバンク同意の積極的な活用と法的裏付けの検討、医療と研究の試料・情報を結び付けるID制度の仕組みなどが挙げられた。今後、がんゲノム医療の実装が進められている米国の状況なども調査し、日本のがんゲノム医療に資する法的・社会的基盤を検討していく必要がある。(著者抄録)

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2018&ichushi_jid=J03931&link_issn=&doc_id=20190121370005&doc_link_id=%2Fcg3kazok%2F2018%2F001802%2F006%2F0042-0047%26dl%3D0&url=https%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Fcg3kazok%2F2018%2F001802%2F006%2F0042-0047%26dl%3D0&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_2.gif

  • 北部方面衛生隊における職種隊付教育成果について

    佐藤 晃, 塩谷 昂祐, 能味 耕介, 中嶋 緑, 堀 真吾, 黒澤 祐典, 後藤 綾美, 小野寺 めぐみ, 坂路 和弘, 平沢 宏太

    防衛衛生   66 ( 別冊 )   93 - 93   2018.12

     More details

    Language:Japanese   Publisher:(一社)日本防衛衛生学会  

    researchmap

  • 【臨床応用に向けた疾患シーケンス解析】(第5章)がん 遺伝性腫瘍に対するクリニカルシーケンス

    平沢 晃

    遺伝子医学MOOK   ( 34 )   130 - 134   2018.11

     More details

    Language:Japanese   Publisher:(株)メディカルドゥ  

    従来より遺伝性腫瘍に対する遺伝学的検査は、十分な遺伝カウンセリングの実施と、リスク評価に基づいて遺伝子バリアントを保持している可能性が高い遺伝子の検査から施行するというアプローチが主流であった。しかしながら、近年のがんクリニカルシーケンスやPARP阻害薬を用いるためのコンパニオン診断を行う機会に、遺伝性腫瘍に関連した生殖細胞系列病的バリアントが同定される機会が増えてきている。遺伝性腫瘍の生殖細胞系列病的バリアント保持者に対しては、適切ながん予防策を講じることで、がん死を低減することが可能となることがあるため、がんゲノム医療実用化時代においてこそ遺伝性腫瘍に関する知識が重要である。(著者抄録)

    researchmap

  • ゲノム医療における情報伝達プロセスに関する提言 がん遺伝子パネル検査と生殖細胞系列全ゲノム 全エクソーム解析について【初版】

    小杉 眞司, 金井 雅史, 川目 裕, 後藤 雄一, 櫻井 晃洋, 武藤 学, 宮本 恵宏, 三宅 秀彦, 孫 徹, 和田 敬仁, 山田 崇弘, 平沢 晃, 松本 繁巳, 高 忠之, 西垣 昌和, 佐藤 智佳, 赤羽 智子, 清水 玲子, 宮崎 幸子, 本田 明夏, 稲葉 慧, 松川 愛未, AMED「医療現場でのゲノム情報の適切な開示のための体制整備に関する研究」班

    臨床病理レビュー   ( 160 )   23 - 34   2018.11

     More details

    Language:Japanese   Publisher:臨床病理刊行会  

    researchmap

  • 子宮体癌および子宮内膜異型増殖症に対するMPA療法の治療予後予測因子の検討

    坂井 健良, 山上 亘, 平野 卓朗, 真壁 健, 二宮 委美, 千代田 達幸, 野村 弘行, 片岡 史夫, 平沢 晃, 阪埜 浩司, 進 伸幸, 青木 大輔

    日本癌治療学会学術集会抄録集   56回   O37 - 3   2018.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    researchmap

  • がん遺伝子パネル検査由来の二次的所見とバリアント保持者のマネージメント

    早乙女 啓子, 平沢 晃, 西原 広史, 野村 弘行, 赤羽 智子, 植木 有紗, 谷嶋 成樹, 高石 官均, 青木 大輔

    日本癌治療学会学術集会抄録集   56回   O35 - 3   2018.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    researchmap

  • 【がんゲノム医療】がんゲノム医療における生殖細胞系列バリアントに対する対応

    平沢 晃

    細胞   50 ( 11 )   576 - 579   2018.10

     More details

    Language:Japanese   Publisher:(株)ニュー・サイエンス社  

    がんゲノム医療実用化の流れと並行して、生殖細胞系列のバリアントを扱う遺伝(子)医療の領域は大きな潮流の中にある。がんクリニカルシーケンスを行うことにより、疾患関連遺伝子の生殖細胞系列病的バリアント(病的変異)が同定される事がある。がんゲノム医療においては、がん罹患者本人のがん治療が最も重要であるが、遺伝カウンセリングと遺伝学的検査を施行して、遺伝性腫瘍の原因遺伝子の生殖細胞系列病的バリアント保持の有無を明らかにすることは、本人の二次癌に対する対応や、未発症家系員に対するがん予防の観点から重要になってくる。(著者抄録)

    researchmap

  • 子宮体癌および子宮内膜異型増殖症に対するMPA療法の治療予後予測因子の検討

    坂井 健良, 山上 亘, 平野 卓朗, 真壁 健, 二宮 委美, 千代田 達幸, 野村 弘行, 片岡 史夫, 平沢 晃, 阪埜 浩司, 進 伸幸, 青木 大輔

    日本癌治療学会学術集会抄録集   56回   O37 - 3   2018.10

     More details

    Language:English   Publisher:(一社)日本癌治療学会  

    researchmap

  • プレシジョンメディシンの将来展望 細胞診の果たす役割 細胞からのプレシジョンメディシン

    平沢 晃

    日本臨床細胞学会雑誌   57 ( Suppl.2 )   545 - 545   2018.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 産後ケア病床の立ち上げの経験(第2報)

    弟子丸 亮太, 河西 明代, 小野寺 成実, 西山 紘子, 大熊 優子, 横田 めぐみ, 堀場 裕子, 平沢 晃, 岩田 卓, 牧田 和也, 青木 大輔, 岸 郁子

    日本女性医学学会雑誌   26 ( Suppl. )   221 - 221   2018.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 若年性子宮体がんのゲノム網羅的DNAメチル化プロファイル(Genome-wide DNA methylation profile of young-onset endometrial cancer)

    真壁 健, 新井 恵吏, 平沢 晃, 山上 亘, 進 伸幸, 青木 大輔, 金井 弥栄

    日本癌学会総会記事   77回   2305 - 2305   2018.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 頸管浸潤を伴う子宮体癌が疑われたが子宮鏡下手術にて子宮温存可能と診断された異型ポリープ状腺筋腫の3例

    早乙女 啓子, 山上 亘, 同前 愛, 平野 卓朗, 千代田 達幸, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   34 ( Suppl.I )   393 - 393   2018.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • 頸管浸潤を伴う子宮体癌が疑われたが子宮鏡下手術にて子宮温存可能と診断された異型ポリープ状腺筋腫の3例

    早乙女 啓子, 山上 亘, 同前 愛, 平野 卓朗, 千代田 達幸, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   34 ( Suppl.I )   393 - 393   2018.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • 術後診断が漿液粘液性境界悪性腫瘍であった卵巣腫瘍の臨床的背景の検討

    千代田 達幸, 早乙女 啓子, 同前 愛, 南木 佳子, 吉浜 智子, 平野 卓郎, 真壁 健, 坂井 健良, 山上 亘, 野村 弘行, 片岡 史夫, 平沢 晃, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   34 ( Suppl.I )   274 - 274   2018.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • HBOCの現状と展望 HBOCサーベイランスとRRSOについて

    平沢 晃, 植木 有紗, 千代田 達幸, 小林 佑介, 林 茂徳, 野村 弘行, 片岡 史夫, 青木 大輔

    日本婦人科腫瘍学会雑誌   36 ( 3 )   474 - 474   2018.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 子宮体癌妊孕性温存療法における筋層浸潤の評価に子宮鏡下手術が有用であった2例

    同前 愛, 山上 亘, 平野 卓朗, 真壁 健, 坂井 健良, 千代田 達幸, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔

    産婦人科手術   ( 29 )   179 - 179   2018.6

     More details

    Language:Japanese   Publisher:(株)メジカルビュー社  

    researchmap

  • 異型ポリープ状腺筋腫に対し高用量黄体ホルモン療法を行った22例の検討

    清河 駿樹, 千代田 達幸, 山上 亘, 平野 卓朗, 真壁 健, 坂井 健良, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 田中 守, 青木 大輔

    関東連合産科婦人科学会誌   55 ( 2 )   283 - 283   2018.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 卵巣癌化学療法の個別化を目指した腫瘍組織および腹水中細胞の初代3次元培養法確立

    南木 佳子, 平沢 晃, 野村 弘行, 赤羽 智子, 千代田 達幸, 片岡 史夫, 冨永 英一郎, 青木 大輔

    日本臨床細胞学会雑誌   57 ( Suppl.1 )   372 - 372   2018.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 当院における分葉状頸管腺過形成(LEGH)の臨床的検討

    安康 真由香, 冨永 英一郎, 高橋 孝幸, 辻 浩介, 小林 佑介, 平沢 晃, 阪埜 浩司, 照井 仁美, 亀山 香織, 青木 大輔

    日本臨床細胞学会雑誌   57 ( Suppl.1 )   213 - 213   2018.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 卵巣癌化学療法の個別化を目指した腫瘍組織および腹水中細胞の初代3次元培養法確立

    南木 佳子, 平沢 晃, 野村 弘行, 赤羽 智子, 千代田 達幸, 片岡 史夫, 冨永 英一郎, 青木 大輔

    日本臨床細胞学会雑誌   57 ( Suppl.1 )   372 - 372   2018.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 卵巣腫瘍 婦人科腫瘍専門医からみた卵巣腫瘍の超音波診断の意義と問題点

    野村 弘行, 岩佐 尚美, 早乙女 啓子, 同前 愛, 千代田 達幸, 片岡 史夫, 平沢 晃, 青木 大輔

    超音波医学   45 ( Suppl. )   S349 - S349   2018.4

     More details

    Language:Japanese   Publisher:(公社)日本超音波医学会  

    researchmap

  • 子宮体癌/子宮内膜異型増殖症でのMPA療法の効果判定における子宮内膜細胞診の有用性

    坂井 健良, 山上 亘, 平野 卓朗, 真壁 健, 野村 弘行, 片岡 史夫, 平沢 晃, 阪埜 浩司, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   57 ( Suppl.1 )   219 - 219   2018.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 卵巣癌術前化学療法(NAC)奏効不良例の体腔液細胞診所見と臨床的背景の検討

    早乙女 啓子, 野村 弘行, 片岡 史夫, 岩佐 尚美, 同前 愛, 南木 佳子, 吉浜 智子, 山上 亘, 平沢 晃, 青木 大輔

    日本臨床細胞学会雑誌   57 ( Suppl.1 )   223 - 223   2018.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 婦人科がん治療戦略としての個別化医療の展開〜基礎から臨床へ〜 婦人科遺伝性腫瘍およびがんゲノム異常の解析とゲノム医療実用化に向けた取り組み

    平沢 晃

    日本産科婦人科学会雑誌   70 ( 2 )   351 - 354   2018.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • ゲノム医療実用化と遺伝性腫瘍に対する対応

    平沢晃, 青木大輔

    日本臨床腫瘍学会学術集会(CD-ROM)   16th   2018

  • 当院で経験したIlizarov創外固定器の症例

    平沢累, 紺野健太, 奥山晃平, 服部史弥, 北崎等

    千葉医学   94 ( 4 )   2018

  • BRCA1/2変異卵巣癌の血縁者における乳癌および卵巣癌の罹患に関する検討

    岩佐 尚美, 平沢 晃, 野村 弘行, 赤羽 智子, 千代田 達幸, 山上 亘, 片岡 史夫, 井本 逸勢, 青木 大輔

    日本乳癌検診学会誌   26 ( 3 )   353 - 353   2017.10

     More details

    Language:Japanese   Publisher:(NPO)日本乳癌検診学会  

    J-GLOBAL

    researchmap

  • Prevention and therapeutic strategies for hereditary ovarian cancer

    Akira Hirasawa, Daisuke Aoki

    ANNALS OF ONCOLOGY   28   2017.10

     More details

    Language:English   Publishing type:Research paper, summary (international conference)   Publisher:OXFORD UNIV PRESS  

    Web of Science

    researchmap

  • 婦人科疾患ゲノム異常の探索と女性ヘルスケアの個別化

    平沢 晃

    日本女性医学学会雑誌   25 ( Suppl. )   103 - 103   2017.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 卵巣癌ステージング手術における腹膜生検の意義についての検討

    高橋 美央, 千代田 達幸, 早乙女 啓子, 同前 愛, 南木 佳子, 吉浜 智子, 山上 亘, 野村 弘行, 片岡 史夫, 平沢 晃, 田中 守, 青木 大輔

    関東連合産科婦人科学会誌   54 ( 3 )   350 - 350   2017.10

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • ベバシズマブを投与した卵巣癌症例における有害事象の発現時期および治療効果との関連

    千代田 達幸, 野村 弘行, 片岡 史夫, 岩佐 尚美, 南木 佳子, 吉浜 智子, 山上 亘, 平沢 晃, 青木 大輔

    日本癌治療学会学術集会抄録集   55回   P59 - 2   2017.10

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 肥満を合併した若年子宮体癌患者に対する妊孕性温存ホルモン療法の検討

    山上 亘, 進 伸幸, 平野 卓朗, 真壁 健, 坂井 健良, 二宮 委美, 小林 佑介, 野村 弘行, 片岡 史夫, 平沢 晃, 阪埜 浩司, 青木 大輔

    日本癌治療学会学術集会抄録集   55回   O12 - 5   2017.10

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 「それぞれの癌」遺伝性腫瘍の実臨床 理想と現実 遺伝性腫瘍の婦人科領域における最近の展開

    平沢 晃, 青木 大輔

    日本癌治療学会学術集会抄録集   55回   SY11 - 5   2017.10

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    J-GLOBAL

    researchmap

  • 産後ケア病床の立ち上げの経験

    弟子丸 亮太, 河西 明代, 小野寺 成実, 西山 紘子, 大熊 優子, 平沢 晃, 岩田 卓, 牧田 和也, 青木 大輔, 岸 郁子

    日本女性医学学会雑誌   25 ( Suppl. )   224 - 224   2017.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    J-GLOBAL

    researchmap

  • 【乳癌ゲノム医療最前線-臨床応用はどこまで進んだか】治療薬解説 PARP阻害薬

    平沢 晃, 青木 大輔

    カレントテラピー   35 ( 9 )   888 - 891   2017.9

     More details

    Language:Japanese   Publisher:(株)ライフメディコム  

    J-GLOBAL

    researchmap

  • 腹腔鏡下骨盤リンパ節郭清後の有害事象の検討

    早乙女 啓子, 山上 亘, 平野 卓朗, 南木 佳子, 坂井 健良, 真壁 健, 吉浜 智子, 二宮 委美, 千代田 達幸, 林 茂徳, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   33 ( Suppl.I )   1375 - 1375   2017.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • 腹腔鏡下骨盤リンパ節郭清後の有害事象の検討

    早乙女 啓子, 山上 亘, 平野 卓朗, 南木 佳子, 坂井 健良, 真壁 健, 吉浜 智子, 二宮 委美, 千代田 達幸, 林 茂徳, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   33 ( Suppl.I )   1375 - 1375   2017.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • BMIが腹腔鏡下子宮体癌手術に及ぼす影響の検討

    平野 卓朗, 片岡 史夫, 南木 佳子, 真壁 健, 坂井 健良, 吉浜 智子, 山上 亘, 林 茂徳, 野村 弘行, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   33 ( Suppl.I )   411 - 411   2017.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • 当院で施行した卵巣癌腫瘍減量拡大術式に関する検討

    吉浜 智子, 野村 弘行, 片岡 史夫, 岩佐 尚美, 南木 佳子, 中平 直希, 山上 亘, 平沢 晃, 冨永 英一郎, 青木 大輔

    日本婦人科腫瘍学会雑誌   35 ( 3 )   630 - 630   2017.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体癌I、II期の再発リスクを有する群に対するCAP療法の至適サイクル数の検討

    平野 卓朗, 山上 亘, 南木 佳子, 真壁 健, 坂井 健良, 二宮 委美, 小林 佑介, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   35 ( 3 )   623 - 623   2017.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体癌における頸部間質浸潤の深度に関する検討

    真壁 健, 山上 亘, 平野 卓朗, 坂井 健良, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   35 ( 3 )   593 - 593   2017.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 婦人科悪性腫瘍患者におけるD-dimer値による深部静脈血栓症/肺血栓塞栓症スクリーニングの検討

    吉村 拓馬, 山上 亘, 平野 卓朗, 坂井 健良, 真壁 健, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   35 ( 3 )   561 - 561   2017.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • ゲノムワイド関連解析による新規子宮筋腫関連遺伝子の同定

    坂井 健良, 平沢 晃, 山上 亘, 進 伸幸, 青木 大輔, 平田 真, 谷川 千津, 鎌谷 洋一郎, 久保 充明, 松田 浩一

    日本婦人科腫瘍学会雑誌   35 ( 3 )   528 - 528   2017.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 遺伝性婦人科がんにおける遺伝子検査・リスク低減手術の選択 ゲノム異常と女性医学から考えるリスク低減手術

    平沢 晃, 青木 大輔

    日本婦人科腫瘍学会雑誌   35 ( 3 )   457 - 457   2017.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    J-GLOBAL

    researchmap

  • 10年以上に亘るホルモン補充療法が女性の健康維持に及ぼす効果についての検証(第2報)

    牧田 和也, 堀場 裕子, 平沢 晃, 岩田 卓, 高松 潔, 青木 大輔

    日本抗加齢医学会総会プログラム・抄録集   17回   182 - 182   2017.6

     More details

    Language:Japanese   Publisher:(一社)日本抗加齢医学会  

    researchmap

  • BRCA1/2遺伝学的検査受検後のリスク低減卵管卵巣摘出術選択に影響する要因の検討

    三須 久美子, 武田 祐子, 平沢 晃, 植木 有紗, 増田 健太, 阪埜 浩司, 青木 大輔, 菅野 康吉, 小崎 健次郎

    日本遺伝カウンセリング学会誌   38 ( 2 )   104 - 104   2017.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    researchmap

  • 卵巣癌術前化学療法における腹水細胞診の有用性とピットフォール 当院における穿刺腹腔細胞診所見に基づく卵巣癌術前化学療法適用の実際

    野村 弘行, 岩佐 尚美, 片岡 史夫, 南木 佳子, 吉浜 智子, 山上 亘, 平沢 晃, 冨永 英一郎, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   56 ( Suppl.1 )   180 - 180   2017.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 腹水卵巣癌細胞のCD44各アイソフォーム発現量と化学療法の効果との関連性の検討

    蔦 幸児, 冨永 英一郎, 戸澤 晃子, 赤羽 智子, 大原 樹, 小林 佑介, 平沢 晃, 阪埜 浩司, 鈴木 直, 青木 大輔

    日本臨床細胞学会雑誌   56 ( Suppl.1 )   369 - 369   2017.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 子宮体癌の術前子宮鏡検査と腹水細胞診

    平野 卓朗, 山上 亘, 真壁 健, 坂井 健良, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   56 ( Suppl.1 )   301 - 301   2017.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 子宮体癌および子宮内膜異型増殖症に対するMPA療法後の長期予後についての検討

    平野 卓朗, 山上 亘, 進 信幸, 坂井 健良, 真壁 健, 二宮 委美, 野村 弘行, 片岡 史夫, 平沢 晃, 阪埜 浩司, 田中 守, 青木 大輔

    日本産科婦人科学会雑誌   69 ( 2 )   661 - 661   2017.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • BRCA1またはBRCA2遺伝子変異保持者に対するリスク低減卵管卵巣摘出術(RRSO)の効果は? Invited

    平沢 晃, 青木大輔, 百枝幹雄編

    女性内分泌クリニカルクエスチョン.   なし   199 - 200   2017

     More details

    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)   Publisher:診断と治療社  

    researchmap

  • 乳癌のホルモン療法の使い分けは? Invited

    平沢 晃, 青木大輔, 百枝幹雄編

    女性内分泌クリニカルクエスチョン.   193 - 195   2017

     More details

    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)   Publisher:診断と治療社  

    researchmap

  • 乳癌ゲノム医療最前線—臨床応用はどこまで進んだか,PARP阻害薬. Invited

    平沢 晃, 青木大輔

    カレントテラピー   74 ( 77 )   1751 - 1758   2017

     More details

    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)   Publisher:ライフメディコム  

    researchmap

  • タモキシフェンの子宮内膜に対する副作用とその対策は? Invited

    平沢 晃, 青木大輔, 百枝幹雄編

    女性内分泌クリニカルクエスチョン.   なし   196 - 198   2017

     More details

    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)   Publisher:診断と治療社  

    researchmap

  • 腹水卵巣癌細胞のCD44各アイソフォーム発現量と化学療法の効果との関連性の検討

    蔦幸児, 冨永英一郎, 戸澤晃子, 赤羽智子, 大原樹, 小林佑介, 平沢晃, 阪埜浩司, 鈴木直, 青木大輔

    日本臨床細胞学会雑誌(Web)   56   2017

  • 乳癌ゲノム医療最前線 臨床応用はどこまで進んだか,PARP阻害薬

    平沢 晃

    カレントテラピー. ライフメディコム   35(9)   74 - 77   2017

     More details

  • DIAGNOSTIC ACCURACY OF INTRA-OPERATIVE TOUCH IMPRINTING CYTOLOGY OF SENTINEL LYMPH NODES IN ENDOMETRIAL CANCER

    N. Susumu, F. Kataoka, W. Yamagami, T. Makabe, K. Sakai, T. Ninomiya, H. Nomura, A. Hirasawa, K. Banno, K. Tanaka, T. Nakahara, K. Kameyama, D. Aoki

    INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER   26 ( 10. Suppl 3 )   1083 - 1083   2016.10

     More details

    Language:English   Publishing type:Research paper, summary (international conference)   Publisher:LIPPINCOTT WILLIAMS & WILKINS  

    Web of Science

    researchmap

  • 内膜細胞診の有用性 臨床医の観点から

    進 伸幸, 山上 亘, 片岡 史夫, 平沢 晃, 亀山 香織, 阪埜 浩司, 青木 大輔

    日本臨床細胞学会雑誌   55 ( Suppl.2 )   448 - 448   2016.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 内膜病変UP-TO-DATE リンチ症候群 その遺伝子型と表現型

    平沢 晃, 山上 亘, 阪埜 浩司, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   55 ( Suppl.2 )   410 - 410   2016.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • BRCA遺伝子変異陽性卵巣がんとPARP阻害薬 本邦における承認前の課題 卵巣癌ゲノム異常と臨床薬理学への展開

    平沢 晃, 青木 大輔

    臨床薬理   47 ( Suppl. )   S129 - S129   2016.10

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • 【ゲノムデータをどう扱えば、医学と医療は変わるのか 遺伝統計学の力と創薬・個別化医療】遺伝性腫瘍領域の新たな潮流

    平沢 晃, 青木 大輔

    実験医学   34 ( 16 )   2671 - 2674   2016.10

     More details

    Language:Japanese   Publisher:(株)羊土社  

    researchmap

  • 伝性乳癌卵巣癌に対するリスク低減卵管卵巣摘出後のQOLに関する検討

    谷本 慧子, 平沢 晃, 牧田 和也, 岩田 卓, 堀場 裕子, 横田 めぐみ, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 高松 潔, 青木 大輔

    日本女性医学学会雑誌   24 ( Suppl. )   137 - 137   2016.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • ゲノムワイド関連解析による新規子宮筋腫感受性遺伝子の同定

    坂井 健良, 平田 真, 谷川 千津, 鎌谷 洋一郎, 久保 充明, 平沢 晃, 松田 浩一

    日本癌学会総会記事   75回   P - 3366   2016.10

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 腹水細胞中からの樹立したヒト悪性腹膜中皮腫由来細胞株の特性に関する検討

    赤羽 智子, 冨永 英一郎, 平沢 晃, 青木 大輔

    日本臨床細胞学会雑誌   55 ( Suppl.2 )   635 - 635   2016.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 遺伝性乳がん卵巣がんと女性ヘルスケア

    平沢 晃, 青木 大輔

    更年期と加齢のヘルスケア学会・日本サプリメント学会学術集会プログラム・抄録集   15回・4回   18 - 18   2016.9

     More details

    Language:Japanese   Publisher:更年期と加齢のヘルスケア学会((NPO)更年期と加齢のヘルスケア)  

    researchmap

  • 当院における腹腔鏡下手術の腸管損傷に関する検討

    真壁 健, 山上 亘, 坂井 健良, 吉浜 智子, 中平 直希, 西尾 浩, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 進 伸幸, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   32 ( Suppl.I )   168 - 168   2016.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    J-GLOBAL

    researchmap

  • 当院における婦人科疾患に合併した深部静脈血栓症/肺塞栓症の検討

    吉村 拓馬, 山上 亘, 平野 卓朗, 南木 佳子, 坂井 健良, 真壁 健, 野村 宏行, 片岡 史夫, 平沢 晃, 阪埜 浩司, 田中 守, 青木 大輔

    関東連合産科婦人科学会誌   53 ( 3 )   397 - 397   2016.8

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 婦人科遺伝性腫瘍の実地臨床

    平沢 晃, 青木 大輔

    関東連合産科婦人科学会誌   53 ( 3 )   360 - 360   2016.8

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 腹腔鏡下手術によって卵巣癌と診断され妊孕性温存の可否を検討した早期子宮体癌/子宮内膜異型増殖症の3症例

    平野 卓朗, 山上 亘, 南木 佳子, 坂井 健良, 真壁 健, 吉浜 智子, 二宮 委美, 野村 弘行, 片岡 史夫, 平沢 晃, 進 信幸, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   32 ( Suppl.I )   296 - 296   2016.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • 当院における腹腔鏡下骨盤リンパ節郭清に関連した周術期合併症の検討

    片岡 史夫, 進 伸幸, 野村 弘行, 吉浜 智子, 中平 直希, 南木 佳子, 坂井 健良, 真壁 健, 平沢 晃, 山上 亘, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   32 ( Suppl.I )   255 - 255   2016.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • 婦人科遺伝性腫瘍取扱いの実際と今後の展望 HBOCに関する最近の動向

    平沢 晃, 青木 大輔

    日本婦人科腫瘍学会雑誌   34 ( 3 )   384 - 384   2016.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 10年以上に亘るホルモン補充療法が女性の健康維持に及ぼす効果についての検証

    牧田 和也, 横田 めぐみ, 堀場 裕子, 岩田 卓, 平沢 晃, 青木 大輔

    日本抗加齢医学会総会プログラム・抄録集   16回   169 - 169   2016.6

     More details

    Language:Japanese   Publisher:(一社)日本抗加齢医学会  

    researchmap

  • 卵巣癌初回手術における手術完遂度の予測モデルの構築

    岩佐 尚美, 野村 弘行, 片岡 史夫, 南木 佳子, 吉浜 智子, 中平 直希, 山上 亘, 平沢 晃, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   34 ( 3 )   441 - 441   2016.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体癌のセンチネルリンパ節(SN)内転移巣の局在・大きさとnon-SNへの転移との関連

    進 伸幸, 片岡 史夫, 山上 亘, 坂井 健良, 真壁 健, 二宮 委美, 和田 美智子, 野村 弘行, 平沢 晃, 田中 京子, 阪埜 浩司, 亀山 香織, 中原 理紀, 青木 大輔

    日本婦人科腫瘍学会雑誌   34 ( 3 )   412 - 412   2016.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 婦人科遺伝性腫瘍取扱いの実際と今後の展望 婦人科遺伝性腫瘍における遺伝カウンセリングと、地域がん診療連携拠点病院における家族性腫瘍相談外来の課題

    植木 有紗, 中田 さくら, 平沢 晃, 阪埜 浩司, 青木 大輔

    日本婦人科腫瘍学会雑誌   34 ( 3 )   386 - 386   2016.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 遺伝性乳がん卵巣がんの現状と本邦での取り組み

    平沢 晃, 青木 大輔

    日本臨床細胞学会雑誌   55 ( Suppl.1 )   98 - 98   2016.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 卵巣腫瘍 判別分析法によるTC療法中の好中球減少と相関する一塩基多型(SNP)の抽出

    岩佐 尚美, 野村 弘行, 片岡 史夫, 南木 佳子, 吉浜 智子, 中平 直希, 山上 亘, 平沢 晃, 進 伸幸, 田中 守, 青木 大輔

    日本産科婦人科学会雑誌   68 ( 2 )   615 - 615   2016.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌術後患者における卵巣欠落症状とQOLに及ぼす影響に関する検討

    横田 めぐみ, 牧田 和也, 平沢 晃, 堀場 裕子, 岩田 卓, 小川 真里子, 柳本 茂久, 弟子丸 亮太, 田中 守, 青木 大輔

    日本産科婦人科学会雑誌   68 ( 2 )   669 - 669   2016.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体がん Invited

    平沢 晃, 青木大輔, 太田博明編

    女性医学のすべて   64 - 67   2016

     More details

    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)   Publisher:メディカルレビュー社  

    &lt;p&gt;OBJECTIVE:: The aim of the study was to clarify the prevalence and severity rates of symptoms and investigate whether symptoms varied in relation to body mass index (BMI). METHODS:: The study group composed of 1,969 women, aged 40 to 60 years, who presented at our department from 1993 through 2014. The participation rate was 98%. The presence or absence of symptoms was evaluated by having the participants complete the Keio Questionnaire, a self-administered questionnaire. To allow the results to be compared according to ovarian function, serum levels of follicle-stimulating hormone and estradiol were measured. Participants were classified into three groups according to BMI: underweight, normal weight, and overweight. Symptoms were also compared among these subgroups. RESULTS:: The most common symptom was general fatigue. Vasomotor symptoms differed significantly between pre- and postmenopause status. When symptoms were analyzed according to BMI, the severity rates of the following symptoms were significantly higher in the overweight group than in the normal weight and underweight groups: hot flushes, sweats, joint pain, numbness, and incontinence. On the contrary, the underweigh

    researchmap

  • 遺伝性乳がん卵巣がん症候群-婦人科医の立場から Invited

    平沢 晃, 増田健太, 青木大輔

    遺伝子医学MOOK 最新遺伝性腫瘍・家族性腫瘍研究と遺伝カウンセリング   別冊 ( 最新遺伝性腫瘍・家族性腫瘍研究と遺伝カウンセリング )   117 - 123   2016

     More details

    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)   Publisher:メディカル・ドゥ  

    researchmap

  • 遺伝性乳がん卵巣がん Invited

    平沢 晃, 青木大輔, 太田博明編

    女性医学のすべて   64 - 67   2016

     More details

    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)   Publisher:メディカルレビュー社  

    &lt;p&gt;OBJECTIVE:: The aim of the study was to clarify the prevalence and severity rates of symptoms and investigate whether symptoms varied in relation to body mass index (BMI). METHODS:: The study group composed of 1,969 women, aged 40 to 60 years, who presented at our department from 1993 through 2014. The participation rate was 98%. The presence or absence of symptoms was evaluated by having the participants complete the Keio Questionnaire, a self-administered questionnaire. To allow the results to be compared according to ovarian function, serum levels of follicle-stimulating hormone and estradiol were measured. Participants were classified into three groups according to BMI: underweight, normal weight, and overweight. Symptoms were also compared among these subgroups. RESULTS:: The most common symptom was general fatigue. Vasomotor symptoms differed significantly between pre- and postmenopause status. When symptoms were analyzed according to BMI, the severity rates of the following symptoms were significantly higher in the overweight group than in the normal weight and underweight groups: hot flushes, sweats, joint pain, numbness, and incontinence. On the contrary, the underweigh

    researchmap

  • 当院における婦人科疾患に合併した深部静脈血栓症/肺塞栓症の検討

    吉村拓馬, 山上亘, 平野卓朗, 南木佳子, 坂井健良, 真壁健, 野村宏行, 片岡史夫, 平沢晃, 阪埜浩司, 田中守, 青木大輔

    関東連合産科婦人科学会誌(Web)   53 ( 3 )   2016

  • ISP-7-4 Mutation of any DNA mismatch repair gene can cause lower uterine segment cancer with Lynch syndrome(Group 7 Endometrial Cancer 2,International Session Poster) :

    Iijima Moito, Banno Kouji, Masuda Kenta, Yanokura Megumi, Adachi Masataka, Nogami Yuya, Yamagami Wataru, Tominaga Eiichiro, Hirasawa Akira, Susumu Nobuyuki, Tanaka Mamoru, Aoki Daisuke

    68 ( 2 )   497 - 497   2016

  • ISP-12-8 BRCAness status of ovarian cancer with somatic large genomic rearrangements(Group 12 Ovarian Cancer 1,International Session Poster) :

    Ninomiya Tomomi, Hirasawa Akira, Akahane Tomoko, Masuda Kenta, Yamagami Wataru, Nomura Hiroyuki, Kataoka Fumio, Banno Kouji, Susumu Nobuyuki, Tanaka Mamoru, Aoki Daisuke

    68 ( 2 )   511 - 511   2016

  • ISP-39-12 A prospective study on the safety on chemotherapy combined with bevacizumab in Japanese patients with recurrent ovarian cancer(Group 39 Oncology,International Session Poster) :

    Nanki Yoshiko, Nomura Hiroyuki, Kataoka Fumio, Iwasa Naomi, Yoshihama Tomoko, Nakadaira Naoki, Ninomiya Tomomi, Yamagami Wataru, Hirasawa Akira, Susumu Nobuyuki, Tanaka Mamoru, Aoki Daisuke

    68 ( 2 )   591 - 591   2016

  • IS-AC-2-3 An analysis of short-term recurrent cases following medroxyprogesterone acetate (MPA) therapy for endometrial cancer and atypical endometrial hyperplasia(Group 2 Oncology 2,International Session Award Candidate) :

    Yamagami Wataru, Susumu Nobuyuki, Sakai Kensuke, Makabe Takeshi, Ninomiya Tomomi, Nomura Hiroyuki, Kataoka Fumio, Hirasawa Akira, Banno Kouji, Tanaka Mamoru, Aoki Daisuke

    68 ( 2 )   457 - 457   2016

  • ISP-12-9 TAS-117, a novel allosteric AKT inhibitor, shows potent antitumor activity on ovarian clear cell adenocarcinoma cells from fresh surgical samples in 3-dimentional culture(Group 12 Ovarian Cancer 1,International Session Poster) :

    Tsuta Kohji, Tominaga Eiichiro, Tozawa Akiko, Akahane Tomoko, Uekawa Atsushi, Ohara Tatsuru, Nomura Hiroyuki, Kataoka Fumio, Hirasawa Akira, Banno Kouji, Suzuki Nao, Aoki Daisuke

    68 ( 2 )   512 - 512   2016

  • 当院におけるBRCA1/2遺伝子変異保持者に対する腹腔鏡下でのリスク低減卵管卵巣摘出術の実施経験

    吉浜 智子, 片岡 史夫, 野村 弘行, 平沢 晃, 増田 健太, 岩佐 尚美, 中平 直希, 南木 佳子, 二宮 委美, 西尾 浩, 山上 亘, 阪埜 浩司, 進 伸幸, 青木 大輔

    日本内視鏡外科学会雑誌   20 ( 7 )   OS67 - 2   2015.12

     More details

    Language:Japanese   Publisher:(一社)日本内視鏡外科学会  

    researchmap

  • 腹腔鏡補助下子宮筋腫核出術(LAM)における術式定型化の工夫

    南木 佳子, 野村 弘行, 片岡 史夫, 岩佐 尚美, 吉浜 智子, 中平 直希, 二宮 委美, 西尾 浩, 山上 亘, 平沢 晃, 進 伸幸, 青木 大輔

    日本内視鏡外科学会雑誌   20 ( 7 )   OS214 - 4   2015.12

     More details

    Language:Japanese   Publisher:(一社)日本内視鏡外科学会  

    J-GLOBAL

    researchmap

  • 子宮体部漿液性腺癌の早期診断に子宮内膜細胞診が有用であった2例の検討

    坂井 健良, 進 伸幸, 山上 亘, 真壁 健, 二宮 委美, 南木 佳子, 吉浜 智子, 岩佐 尚美, 中平 直希, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 青木 大輔

    日本臨床細胞学会雑誌   54 ( Suppl.2 )   659 - 659   2015.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • BRCA1/2遺伝子変異保持者に対するリスク低減卵管卵巣摘出後のQOLに関する検討

    平沢 晃, 牧田 和也, 横田 めぐみ, 堀場 裕子, 岩田 卓, 小川 真里子, 柳本 茂久, 弟子丸 亮太, 高松 潔, 青木 大輔

    日本女性医学学会雑誌   23 ( Suppl. )   131 - 131   2015.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 本格的な施行開始後3年目を迎えた子宮体癌術後患者の卵巣欠落症状に対するエストロゲン療法(ET)の現状

    牧田 和也, 横田 めぐみ, 堀場 ゆうこ, 山上 亘, 平沢 晃, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 阪埜 浩司, 進 伸幸, 高松 潔, 青木 大輔

    日本女性医学学会雑誌   23 ( Suppl. )   127 - 127   2015.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 前立腺 前立腺がんのリスク予測 メバロン酸合成経路を標的とした卵巣癌新規治療戦略の検討

    小林 佑介, 阪埜 浩司, 増田 健太, 野村 弘行, 片岡 史夫, 冨永 英一郎, 平沢 晃, 進 伸幸, Wang Tian-Li, Shih Ie-Ming, 青木 大輔

    日本癌治療学会誌   50 ( 3 )   133 - 133   2015.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 子宮 子宮体がん治療の個別化を目指して 40歳以上の子宮体癌に対する高用量MPA療法は有用か

    山上 亘, 進 伸幸, 坂井 健良, 真壁 健, 二宮 委美, 和田 美智子, 野村 弘行, 片岡 史夫, 平沢 晃, 阪埜 浩司, 青木 大輔

    日本癌治療学会誌   50 ( 3 )   1093 - 1093   2015.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 卵巣 卵巣がんに対する新規治療法の開発 再発卵巣癌に対するベバシズマブ併用化学療法の安全性に関する前方視的検討

    岩佐 尚美, 野村 弘行, 片岡 史夫, 吉浜 智子, 中平 直希, 二宮 委美, 山上 亘, 平沢 晃, 進 伸幸, 青木 大輔

    日本癌治療学会誌   50 ( 3 )   398 - 398   2015.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 卵巣 卵巣がん治療の個別化に向けて 進行卵巣癌に対する術前化学療法におけるdose-dense TC療法の臨床効果に関する検討

    吉浜 智子, 片岡 史夫, 野村 弘行, 橋本 志歩, 岩佐 尚美, 中平 直希, 二宮 委美, 山上 亘, 平沢 晃, 進 伸幸, 青木 大輔

    日本癌治療学会誌   50 ( 3 )   179 - 179   2015.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 腹腔鏡下骨盤リンパ節郭清後に絞扼性イレウスを発症した1例

    真壁 健, 山上 亘, 坂井 健良, 二宮 委美, 中平 直希, 岩佐 尚美, 吉浜 智子, 野村 弘之, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   31 ( Suppl.I )   145 - 145   2015.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • I期、II期の子宮体部類内膜癌における再発リスク因子の検討

    小塙 理人, 山上 亘, 二宮 委美, 坂井 健良, 真壁 健, 野村 弘行, 片岡 史夫, 平沢 晃, 阪埜 浩司, 進 伸幸, 田中 守, 青木 大輔

    関東連合産科婦人科学会誌   52 ( 3 )   453 - 453   2015.8

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 腹腔鏡下子宮体癌根治術における、開腹移行症例の検討

    坂井 健良, 片岡 史夫, 真壁 健, 二宮 委美, 吉浜 智子, 岩佐 尚美, 中平 直希, 山上 亘, 野村 弘行, 平沢 晃, 田中 京子, 進 伸幸, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   31 ( Suppl.I )   266 - 266   2015.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • 当院産婦人科における緊急腹腔鏡下手術の後方視的検討

    二宮 委美, 片岡 史夫, 坂井 健良, 真壁 健, 吉浜 智子, 岩佐 尚美, 中平 直希, 佐藤 卓, 山上 亘, 野村 弘行, 升田 博隆, 佐藤 健二, 平沢 晃, 進 伸幸, 青木 大輔

    日本産科婦人科内視鏡学会雑誌   31 ( Suppl.I )   191 - 191   2015.8

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • HBOC BRCA1/2遺伝子検査と産婦人科臨床

    平沢 晃, 青木 大輔

    日本婦人科腫瘍学会雑誌   33 ( 3 )   473 - 473   2015.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 当院における子宮体癌術後再発低リスク群における再発症例の検討

    坂井 健良, 山上 亘, 進 伸幸, 真壁 健, 二宮 委美, 岩佐 尚美, 中平 直希, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 青木 大輔

    日本婦人科腫瘍学会雑誌   33 ( 3 )   603 - 603   2015.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • HBOC高リスク群に対するBRCA1/2遺伝子検査の陽性率についての検討

    増田 健太, 梅根 紀代子, 植木 有紗, 安達 将隆, 中村 加奈子, 飯田 美穂, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 三須 久美子, 武田 祐子, 小崎 健次郎, 青木 大輔, 菅野 康吉, 清水 千佳子

    家族性腫瘍   15 ( 2 )   A85 - A85   2015.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 産婦人科医が関わる遺伝カウンセリングの現状と今後の課題 地域がん診療連携拠点病院における家族性腫瘍相談外来の開設と、婦人科遺伝性腫瘍における遺伝カウンセリング

    植木 有紗, 中田 さくら, 安齋 純子, 麻薙 美香, 三須 久美子, 平沢 晃, 増田 健太, 阪埜 浩司, 菅野 康吉, 小崎 健次郎, 青木 大輔

    日本遺伝カウンセリング学会誌   36 ( 2 )   36 - 36   2015.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    J-GLOBAL

    researchmap

  • 細胞診標本中に出現する微量細胞からの遺伝子解析

    赤羽 智子, 平沢 晃, 冨永 英一郎, 青木 大輔

    日本臨床細胞学会雑誌   54 ( Suppl.1 )   210 - 210   2015.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 【産婦人科医必読!臨床遺伝学の最新知識】 腫瘍と遺伝 遺伝性乳癌・卵巣癌とLynch症候群のリスク低減手術(解説/特集) Invited

    安達将隆, 阪埜浩司, 増田健太, 植木有紗, 平沢晃, 冨永英一郎, 青木大輔

    産婦人科の実際   64 ( 3 )   189 - 193   2015.3

     More details

    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (trade magazine, newspaper, online media)  

    CiNii Article

    J-GLOBAL

    researchmap

  • 卵巣がん 新規治療法の探索 新規アロステリック型AKT阻害剤TAS-117は卵巣癌患者腹水中の癌細胞に対して有効性を示す

    蔦 幸児, 冨永 英一郎, 戸澤 晃子, 赤羽 智子, 大原 樹, 野村 弘行, 片岡 史夫, 平沢 晃, 阪埜 浩司, 鈴木 直, 青木 大輔

    日本産科婦人科学会雑誌   67 ( 2 )   500 - 500   2015.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    J-GLOBAL

    researchmap

  • 卵巣がん high-grade漿液性腺癌/HBOC BRCA1/2遺伝子生殖細胞変異例における良性卵管上皮細胞のp53蛋白発現とTP53遺伝子変異の意義

    赤羽 智子, 平沢 晃, 増田 健太, 片岡 史夫, 冨永 英一郎, 阪埜 浩司, 進 伸幸, 田中 守, 青木 大輔

    日本産科婦人科学会雑誌   67 ( 2 )   501 - 501   2015.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    J-GLOBAL

    researchmap

  • 女性ヘルスケア集中講義!-次世代の女性医学の可能性を求めて-】 外来でできる婦人科がんの予防とヘルスケア指導 子宮体がんの予防とヘルスケア

    進 伸幸, 平沢 晃, 山上 亘, 青木 大輔

    産婦人科の実際   64 ( 11 )   1741 - 1750   2015

     More details

    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (trade magazine, newspaper, online media)  

    researchmap

  • ISP-1-6 Is repeated fertility-preserving hormonal therapy using medroxyprogesterone acetate acceptable for young patients with recurrent endometrial cancer or atypical hyperplasia?(Group 1 Oncology 1,IS Poster,International Session) :

    Sakai Kensuke, Kataoka Fumio, Hirasawa Akira, Banno Kouji, Tanaka Mamoru, Aoki Daisuke

    67 ( 2 )   1004 - 1004   2015

  • 遺伝性乳癌卵巣癌の診療におけるVUSへの対応

    増田健太, 増田健太, 梅根紀代子, 植木有紗, 植木有紗, 入江晴子, 安達将隆, 中村加奈子, 飯田美穂, 平沢晃, 平沢晃, 冨永英一郎, 阪埜浩司, 三須久美子, 三須久美子, 武田祐子, 武田祐子, 小崎健次郎, 青木大輔, 菅野康吉, 菅野康吉

    日本人類遺伝学会大会プログラム・抄録集   60th   2015

  • 当科における子宮体癌術後患者の卵巣欠落症状に対するエストロゲン療法(ET)の試み

    牧田 和也, 横田 めぐみ, 堀場 裕子, 山上 亘, 平沢 晃, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 阪埜 浩司, 進 伸幸, 高松 潔, 青木 大輔

    日本女性医学学会雑誌   22 ( Suppl. )   143 - 143   2014.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • p62/SQSTM1タンパク質の高発現は子宮体癌の悪性形質および不良な予後と相関する(High expression level of p62/SQSTM1 protein correlate with aggressive phenotype and poor prognosis in endometrial cancer)

    岩舘 怜子, 井上 純, 津田 均, 平沢 晃, 青木 大輔, 稲澤 譲治

    日本癌学会総会記事   73回   J - 1004   2014.9

     More details

    Language:English   Publisher:日本癌学会  

    researchmap

  • CLINOPATHOLOGIC FEATURES AND DNA MISMATCH REPAIR PROTEIN EXPRESSION IN 32 CASES OF SYNCHRONOUS PRIMARY ENDOMETRIAL CANCER AND OVARIAN CANCER.

    Nakamura K, Kobayashi Y, Banno K, Nomura H, Adachi M, Iida M, Masuda K, Kisu I, Ueki A, Yamagami W, Kataoka F, Hirasawa A, Tominaga E, Susumu N, Aoki D

    International Journal of Gynecological Cancer   24 ( 9 Suppl.4 )   1451 - 1452   2014.9

     More details

    Language:English   Publishing type:Research paper, summary (international conference)  

    researchmap

  • SUCCESSFUL PREGNANCIES IN 54 PATIENTS FOLLOWING FERTILITY-PRESERVING HORMONAL THERAPY FOR ENDOMETRIAL CANCER.

    Ninomiya T, Wada M, Yokota M, Ichikawa Y, Susumu N, Yamagami W, Nomura H, Kataoka F, Hirasawa A, Suzuki A, Tominaga E, Banno K, Aoki D

    International Journal of Gynecological Cancer   24 ( 9 Suppl.4 )   1497 - 1497   2014.9

     More details

    Language:English   Publishing type:Research paper, summary (international conference)  

    researchmap

  • HBOC症例およびBRCA1/2遺伝子変異保持者における卵管上皮細胞のP53特性とBRCA1遺伝子の欠損(P53 status and LOH of BRCA1 in HBOC and BRCA1/2 mutant carrier)

    赤羽 智子, 平沢 晃, 片岡 史夫, 増田 健太, 野村 弘行, 阪埜 浩司, 冨永 英一郎, 進 伸幸, 青木 大輔

    日本癌学会総会記事   73回   J - 2013   2014.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • DNAミスマッチ修復タンパクの免疫組織化学による子宮体部・卵巣同時発生重複癌の検討

    中村 加奈子, 阪埜 浩司, 小林 佑介, 野村 弘行, 矢野倉 恵, 飯田 美穂, 安達 政隆, 野上 侑哉, 梅根 紀代子, 増田 健太, 植木 有紗, 山上 亘, 平沢 晃, 冨永 英一郎, 進 伸幸, 青木 大輔

    日本組織細胞化学会総会・学術集会講演プログラム・予稿集   55回   79 - 79   2014.9

     More details

    Language:Japanese   Publisher:日本組織細胞化学会  

    researchmap

  • 婦人科更年期外来受診者の腰椎骨密度値の時代による変化

    杉本 到, 牧田 和也, 平沢 晃, 高松 潔, 青木 大輔

    Osteoporosis Japan   22 ( Suppl.1 )   363 - 363   2014.9

     More details

    Language:Japanese   Publisher:ライフサイエンス出版(株)  

    researchmap

  • BRCA1/2遺伝子変異保持者の卵管上皮細胞におけるp53とMDM2の発現の検討

    赤羽 智子, 平沢 晃, 片岡 史夫, 増田 健太, 冨永 英一郎, 阪埜 浩司, 進 伸幸, 亀山 香織, 青木 大輔

    日本組織細胞化学会総会・学術集会講演プログラム・予稿集   55回   80 - 80   2014.9

     More details

    Language:Japanese   Publisher:日本組織細胞化学会  

    J-GLOBAL

    researchmap

  • 子宮体部・卵巣同時発生重複癌におけるDNAミスマッチ修復タンパクの免疫組織化学染色による解析

    中村 加奈子, 阪埜 浩司, 小林 佑介, 野村 弘行, 矢野倉 恵, 飯田 美穂, 安達 将隆, 野上 侑哉, 梅根 紀代子, 増田 健太, 植木 有紗, 山上 亘, 平沢 晃, 進 伸幸, 青木 大輔

    家族性腫瘍   14 ( 2 )   A41 - A41   2014.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    J-GLOBAL

    researchmap

  • Peutz-Jeghers syndrome(PJS)患者に認められたSTK11遺伝子スプライシング異常の病的意義についての検討

    増田 健太, 小林 佑介, 植木 有紗, 野村 弘行, 平沢 晃, 阪埜 浩司, 青木 大輔, 三須 久美子, 小崎 健次郎, 牛尼 美年子, 吉田 輝彦, 斎藤 伸哉, 菅野 康吉

    家族性腫瘍   14 ( 2 )   A49 - A49   2014.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • ホルモン治療と内膜細胞診 良性疾患から内膜癌治療後まで 若年子宮体癌に対する妊孕性温存療法後の子宮内再発の診断とその予防

    山上 亘, 進 伸幸, 二宮 委美, 和田 美智子, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 青木 大輔

    日本臨床細胞学会雑誌   53 ( Suppl.1 )   111 - 111   2014.4

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 婦人科悪性腫瘍・最近の話題 BRCA1/2遺伝子変異例における卵管上皮細胞のP53の特性に関する検討

    赤羽 智子, 冨永 英一郎, 平沢 晃, 片岡 史夫, 野村 弘行, 増田 健太, 阪埜 浩司, 進 伸幸, 吉村 泰典, 青木 大輔

    日本産科婦人科学会雑誌   66 ( 2 )   441 - 441   2014.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    J-GLOBAL

    researchmap

  • BRCA1/2遺伝子変異保持者における卵管上皮細胞のp53 statusとその意義

    赤羽 智子, 冨永 英一郎, 平沢 晃, 片岡 史夫, 増田 健太, 植木 有紗, 阪埜 浩司, 進 伸幸, 亀山 香織, 青木 大輔

    日本臨床細胞学会雑誌   52 ( Suppl.2 )   740 - 740   2013.10

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • ゲノムワイド関連解析による卵巣がん感受性遺伝子の同定(GWASs identify different susceptibility loci for various subtypes of epithelial ovarian cancer in Japanese population)

    前佛 均, チャ・ペイチェン, 平沢 晃, 高橋 篤, 赤羽 智子, ロウ・シューキー, 青木 大輔, 久保 充明, 中村 祐輔

    日本癌学会総会記事   72回   118 - 118   2013.10

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • BRCA陽性患者における卵管上皮のp53ステータス(TP53 status of fallopian tubes in BRCA1 or BRCA2 mutant patients)

    赤羽 智子, 平沢 晃, 増田 健太, 鶴田 智彦, 野村 弘行, 片岡 史夫, 冨永 英一郎, 阪埜 浩司, 進 伸幸, 亀山 香織, 青木 大樹

    日本癌学会総会記事   72回   283 - 283   2013.10

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 若年子宮体癌に対する妊孕性温存療法後の子宮内再発診断における子宮内膜細胞診の有用性

    山上 亘, 進 伸幸, 桑波田 美智子, 滝川 彩, 横田 めぐみ, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 塚崎 克己, 青木 大輔

    日本婦人科腫瘍学会雑誌   31 ( 3 )   430 - 430   2013.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 家族性乳癌・婦人科腫瘍 遺伝性婦人科腫瘍に対する診療

    増田 健太, 阪埜 浩司, 平沢 晃, 植木 有紗, 小崎 健次郎, 菅野 康吉, 青木 大輔

    家族性腫瘍   13 ( 2 )   A33 - A33   2013.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 子宮体癌ホルモン療法の効果判定、効果予測 子宮体癌における妊孕性温存黄体ホルモン療法後の再発予後因子の検討

    進 伸幸, 山上 亘, 市川 義一, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 鈴木 淳, 阪埜 浩司, 塚崎 克己, 青木 大輔

    日本臨床細胞学会雑誌   52 ( Suppl.1 )   114 - 114   2013.5

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 細胞診検体からの遺伝子診断を志向した微量細胞からの遺伝子解析の試み

    赤羽 智子, 冨永 英一郎, 山上 亘, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   52 ( Suppl.1 )   286 - 286   2013.5

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 日本人卵巣癌における血縁腫瘍歴の頻度およびBRCA1/2遺伝子変異保持者卵管細胞のp53変異に関する検討

    赤羽智子, 平沢晃, 平沢晃, 増田健太, 冨永英一郎, 片岡史夫, 野村弘行, 鶴田智彦, 植木有紗, 阪埜浩司, 進伸幸, 菅野康吉, 小崎健次郎, 亀山香織, 青木大輔

    日本人類遺伝学会大会プログラム・抄録集   58th   2013

  • 家族性腫瘍における婦人科癌診療の実際

    植木有紗, 阪埜浩司, 平沢晃, 平沢晃, 増田健太, 小崎健次郎, 菅野康吉, 青木大輔

    日本臨床腫瘍学会学術集会(CD-ROM)   11th   2013

  • 子宮体癌の再発を予測できる間質遺伝子の発現に基づいた卵巣癌症例のグループ化(Classification of ovarian cancer based on the stromal gene expression related with recurrence of endometrial cancer)

    津田 浩史, 伊藤 陽一, 片岡 央夫, 田中 英雄, 野村 弘行, 千代田 達幸, 井口 蓉子, 平沢 晃, 冨永 英一郎, 山上 亘, 進 伸幸, 青木 大輔

    日本癌学会総会記事   71回   433 - 433   2012.8

     More details

    Language:English   Publisher:日本癌学会  

    researchmap

  • 婦人科悪性腫瘍に対するセンチネルノードナビゲーションサージャリー(SNNS) 早期子宮体癌症例に対するセンチネルリンパ節ナビゲーションシステム(SNNS)の確立に向けて

    進 伸幸, 片岡 史夫, 山上 亘, 井口 蓉子, 千代田 達幸, 野村 弘行, 平沢 晃, 田中 京子, 鈴木 淳, 阪埜 浩司, 津田 浩史, 青木 大輔, 亀山 香織, 中原 理紀, 竹内 裕也

    日本婦人科腫瘍学会雑誌   30 ( 3 )   324 - 325   2012.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体癌手術における大網切除の臨床病理学的検討

    坂井 健良, 山上 亘, 進 伸幸, 井口 蓉子, 千代田 達幸, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 津田 浩史, 青木 大輔

    日本婦人科腫瘍学会雑誌   30 ( 3 )   389 - 389   2012.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体癌における化学療法 子宮体癌の化学療法 本邦における臨床試験を中心に

    山上 亘, 進 伸幸, 野村 弘行, 平沢 晃, 阪埜 浩司, 津田 浩史, 青木 大輔

    日本婦人科腫瘍学会雑誌   30 ( 3 )   329 - 330   2012.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • hMLH1遺伝子のepimutationと子宮内膜癌 末梢血DNAを用いたメチル化解析

    辻 浩介, 阪埜 浩司, 矢野倉 恵, 増田 健太, 植木 有紗, 木須 伊織, 小林 佑介, 山上 亘, 平沢 晃, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   30 ( 3 )   396 - 396   2012.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 若年子宮体がんに対する治療戦略 若年の子宮内膜異型増殖症と類内膜腺癌に対する妊孕性温存の挑戦

    進 伸幸, 山上 亘, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 青木 大輔, 市川 義一

    日本婦人科腫瘍学会雑誌   30 ( 3 )   341 - 342   2012.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 2010年度日本乳癌学会班研究課題最終報告「我が国における遺伝性乳癌・卵巣癌(BRCA陽性患者)及び未発症陽性者のデータベース構築及び対策に関する研究」

    中村清吾, 高橋將人, 戸崎光宏, 中山貴寛, 野水整, 三木義男, 村上茂, 村上好恵, 青木大輔, 新井正美, 有賀智之, 岩瀬拓士, 大住省三, 繁永礼奈, 清水忠夫, 西村誠一郎, 馬場信一, 阪埜浩司, 平沢晃, 藤森実, 森美樹, 山内英子, 四元淳子

    日本乳癌学会学術総会プログラム・抄録集   20th   232 - 232   2012.5

     More details

    Language:Japanese   Publisher:(一社)日本乳癌学会  

    J-GLOBAL

    researchmap

  • 日本人の遺伝性乳がん卵巣がん(HBOC)症例に対するBRCA1/2遺伝子検査 遺伝子検査費用の軽減と高リスク群同定に関する研究

    菅野 康吉, 牧島 恵子, 羽田 恵梨, 青木 幸恵, 小杉 眞司, 平沢 晃, 青木 大輔, 赤木 究, 櫻井 晃洋, 野水 整, 田中屋 宏爾, 増田 春菜, 大住 省三, 吉田 輝彦, 和泉 秀子, 清水 千佳子

    家族性腫瘍   12 ( 2 )   A49 - A49   2012.5

     More details

    Language:Japanese   Publisher:日本家族性腫瘍学会  

    researchmap

  • Lynch症候群、基礎から臨床まで(より深い理解のために) 若年子宮体癌患者末梢血を用いたDNAミスマッチ修復遺伝子のepimutation解析

    阪埜 浩司, 辻 浩介, 矢野倉 恵, 増田 健太, 植木 有紗, 木須 伊織, 山上 亘, 平沢 晃, 富永 英一郎, 進 伸幸, 青木 大輔

    家族性腫瘍   12 ( 2 )   A21 - A21   2012.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 子宮体癌手術例における傍大動脈リンパ節のみへの単独転移例の病理学的検討

    富里 祥子, 山上 亘, 進 伸幸, 小林 佑介, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 津田 浩史, 青木 大輔, 吉村 泰典

    関東連合産科婦人科学会誌   49 ( 2 )   285 - 285   2012.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 【遺伝性婦人科悪性腫瘍】遺伝性乳癌・卵巣癌

    平沢 晃, 青木 大輔

    日本産科婦人科学会雑誌   64 ( 4 )   1315 - 1320   2012.4

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 卵巣明細胞腺癌細胞におけるHNF1β蛋白発現解析

    赤羽 智子, 冨永 英一郎, 平沢 晃, 青木 大輔

    日本臨床細胞学会雑誌   51 ( Suppl.1 )   380 - 380   2012.3

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 子宮体部癌肉腫の癌部ではTGF-β-Smad2/3経路が活性化し上皮間葉転換(EMT)をきたしている

    千代田 達幸, 津田 浩史, 片岡 史夫, 野村 弘行, 井口 蓉子, 冨永 英一郎, 平沢 晃, 山上 亘, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   64 ( 2 )   401 - 401   2012.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌の再発を予測できる間質遺伝子の発現に基づいた卵巣癌症例のグループ化

    井口 蓉子, 津田 浩史, 片岡 史夫, 野村 弘行, 千代田 達幸, 平沢 晃, 冨永 英一郎, 山上 亘, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   64 ( 2 )   417 - 417   2012.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌においてDNA過剰メチル化により発現抑制される癌抑制遺伝子型microRNA miR-152の同定

    鶴田 智彦, 平沢 晃, 進 伸幸, 岩舘 怜子, 高橋 峰夫, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   64 ( 2 )   408 - 408   2012.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 若年体癌症例155例に対する子宮温存目的酢酸メドロキシプロゲステロン(MPA)療法の非成功例の検討 子宮摘出に至った37例を中心に

    進 伸幸, 山上 亘, 市川 義一, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 鈴木 淳, 阪埜 浩司, 津田 浩史, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   64 ( 2 )   409 - 409   2012.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌における制御性T細胞と予後との関連性の検討

    山上 亘, 進 伸幸, 野村 弘行, 片岡 史夫, 平沢 晃, 岩田 卓, 冨永 英一郎, 阪埜 浩司, 津田 浩史, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   64 ( 2 )   416 - 416   2012.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • Preface

    JOURNAL OF FAMILIAL TUMORS   12 ( 2 )   31   2012

     More details

    Language:Japanese   Publisher:The Japanese Society for Hereditary Tumors  

    DOI: 10.18976/jsft.12.2_31

    CiNii Article

    researchmap

  • 当科健康維持外来受診患者からみた「めまい」の現状

    牧田 和也, 横田 めぐみ, 堀場 裕子, 平沢 晃, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 高松 潔, 青木 大輔, 吉村 泰典

    日本女性医学学会雑誌   19 ( Suppl. )   103 - 103   2011.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 当科健康維持外来受診患者における潜在性甲状腺機能低下症に関する検討

    横田 めぐみ, 牧田 和也, 堀場 裕子, 平沢 晃, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 高松 潔, 青木 大輔, 吉村 泰典

    日本女性医学学会雑誌   19 ( Suppl. )   104 - 104   2011.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 婦人科がんにおける基礎から臨床への研究 発現解析に基づいた低中リスク子宮体癌の術後再発予測モデル(A gene expression profile as a predictor of recurrence in low and intermediate-risk endometrial cancer)

    津田 浩史, 伊藤 陽一, 田中 英雄, 高野 政志, 西村 貞子, 片岡 史夫, 野村 弘行, 千代田 達幸, 平沢 晃, 進 伸幸, 青木 大輔

    日本癌学会総会記事   70回   419 - 419   2011.9

     More details

    Language:English   Publisher:日本癌学会  

    researchmap

  • 卵巣 上皮性卵巣癌における初回化学療法のprognostic markerとしての血液毒性

    野村 弘行, 津田 浩史, 片岡 史夫, 田中 京子, 千代田 達幸, 山上 亘, 平沢 晃, 冨永 英一郎, 進 伸幸, 青木 大輔

    日本癌治療学会誌   46 ( 2 )   454 - 454   2011.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 子宮体癌における血漿中遊離DNA量の測定の意義(The significance of measurement of cell free DNA in the endometrial cancer)

    田中 英雄, 津田 浩史, 野村 弘行, 片岡 史夫, 平沢 晃, 千代田 達幸, 進 伸幸, 青木 大輔

    日本癌学会総会記事   70回   318 - 318   2011.9

     More details

    Language:English   Publisher:日本癌学会  

    researchmap

  • エピジェネティックに制御されるmiR-34bは子宮体癌細胞に対して癌抑制効果を示す(Epigenetically controlled miR-34b has antitumor activity against endometrial cancer cells)

    阪埜 浩司, 矢野倉 恵, 小林 佑介, 木須 伊織, 植木 有紗, 増田 健太, 野村 弘行, 平沢 晃, 進 伸幸, 青木 大輔

    日本癌学会総会記事   70回   316 - 316   2011.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • STK11遺伝子陽性を示し子宮頸部分葉状頸管過形成を合併したPeutz-Jeghers症候群の1例

    赤羽 智子, 平沢 晃, 小林 佑介, 鶴田 智彦, 阪埜 浩司, 藤井 多久磨, 進 伸幸, 菅野 康吉, 青木 大輔

    日本臨床細胞学会雑誌   50 ( Suppl.2 )   596 - 596   2011.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 子宮肉腫に対するifosfamide、doxorubicin、cisplatin療法(IAP療法)の後方視的検討

    山上 亘, 進 伸幸, 津田 浩史, 増田 健太, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 青木 大輔

    日本癌治療学会誌   46 ( 2 )   733 - 733   2011.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 骨・ミネラル代謝研究の進歩 他領域研究との融合 卵巣摘出術を施行した婦人科がんサーバイバーのQOL向上を目的とした環境因子および遺伝因子に関する検討

    平沢 晃, 牧田 和也, 赤羽 智子, 青木 大輔

    日本骨代謝学会学術集会プログラム抄録集   29回   129 - 129   2011.7

     More details

    Language:Japanese   Publisher:(一社)日本骨代謝学会  

    researchmap

  • 抗癌剤耐性 子宮頸癌におけるウェルナー(WRN)遺伝子のエピジェネティックな発現抑制と抗癌剤感受性

    増田 健太, 阪埜 浩司, 矢野倉 恵, 小林 佑介, 木須 伊織, 植木 有紗, 小野 あすか, 平沢 晃, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   29 ( 3 )   497 - 497   2011.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 若年子宮体癌の妊孕性温存MPA療法はいつまで継続してよいか G1腺癌88例の長期予後解析より

    進 伸幸, 山上 亘, 市川 義一, 小林 佑介, 鶴田 智彦, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 鈴木 淳, 阪埜 浩司, 津田 浩史, 塚崎 克己, 青木 大輔

    日本婦人科腫瘍学会雑誌   29 ( 3 )   515 - 515   2011.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • What's New in SURGERY FRONTIER(第69回) SNP解析に基づくオーダーメイド医療 イリノテカンと遺伝子多型

    平沢 晃, 青木 大輔

    Surgery Frontier   18 ( 2 )   164 - 167   2011.6

     More details

    Language:Japanese   Publisher:(株)メディカルレビュー社  

    researchmap

  • 子宮体部漿液性腺癌術前診断の問題点

    山上 亘, 進 伸幸, 小林 佑介, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 津田 浩史, 青木 大輔, 吉村 泰典

    関東連合産科婦人科学会誌   48 ( 2 )   178 - 178   2011.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • Lower uterine segment(LUS)から発生する子宮体癌とLynch症候群との関連

    増田 健太, 阪埜 浩司, 矢野倉 恵, 小林 佑介, 植木 有紗, 木須 伊織, 野村 弘行, 平沢 晃, 進 伸幸, 青木 大輔

    家族性腫瘍   11 ( 2 )   A63 - A63   2011.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • Lower uterine segment(LUS)から発生する子宮体癌とLynch症候群との関連

    増田 健太, 阪埜 浩司, 矢野倉 恵, 小林 佑介, 植木 有紗, 木須 伊織, 野村 弘行, 平沢 晃, 進 伸幸, 青木 大輔

    日本遺伝カウンセリング学会誌   32 ( 2 )   63 - 63   2011.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝カウンセリング学会  

    researchmap

  • 【婦人科内分泌療法 病態の理解と正しい診断に基づく対処・治療のポイント】更年期・老年期 老人性腟炎

    牧田 和也, 平沢 晃, 青木 大輔

    臨床婦人科産科   65 ( 4 )   568 - 571   2011.4

  • P2-14-25 エピゲノム異常により発現抑制され細胞増殖抑制活性を有する子宮体がん関連microRNA及びその標的分子の同定(Group98 子宮体部悪性腫瘍・基礎2,一般演題,第63回日本産科婦人科学会学術講演会)

    鶴田 智彦, 平沢 晃, 阪埜 浩司, 進 伸幸, 小崎 健一, 稲澤 譲治, 青木 大輔, 吉村 泰典

    日本産科婦人科學會雜誌   63 ( 2 )   787 - 787   2011.2

     More details

    Language:Japanese   Publisher:社団法人日本産科婦人科学会  

    CiNii Article

    researchmap

  • シアリダーゼ発現の低下は卵巣癌腹膜播種形成を抑制する

    野村 弘行, 津田 浩史, 玉田 裕, 片岡 史夫, 千代田 達幸, 平沢 晃, 冨永 英一郎, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   63 ( 2 )   838 - 838   2011.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 卵巣癌間質の遺伝子発現解析を用いた新規バイオマーカーの探索 癌間質のEGR-1発現は上皮性卵巣癌の予後予測因子である

    片岡 史夫, 津田 浩史, 野村 弘行, 千代田 達幸, 赤羽 智子, 平沢 晃, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   63 ( 2 )   704 - 704   2011.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体部癌肉腫の遺伝子発現パターンに基づいた治療戦略の考察

    千代田 達幸, 津田 浩史, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   63 ( 2 )   816 - 816   2011.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 若年子宮体癌132例に対する妊孕性温存療法の長期予後解析結果 分娩後再発を中心に

    市川 義一, 進 伸幸, 鶴田 智彦, 平沢 晃, 冨永 英一郎, 鈴木 淳, 阪埜 浩司, 津田 浩史, 塚崎 克己, 服部 政博, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   63 ( 2 )   447 - 447   2011.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • Lower uterine segment(LUS)から発生する子宮体癌とLynch症候群との関連

    増田 健太, 阪埜 浩司, 矢野倉 恵, 小林 佑介, 植木 有紗, 木須 伊織, 小野 あすか, 野村 弘行, 平沢 晃, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   63 ( 2 )   806 - 806   2011.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮内膜病変の診断におけるNBI(Narrow Band Imaging)システムを用いた軟性子宮鏡の有用性の検討 録画画像を用いた無作為化比較試験による解析

    木須 伊織, 阪埜 浩司, 小林 佑介, 植木 有紗, 増田 健太, 小野 あすか, 野村 弘行, 平沢 晃, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   63 ( 2 )   792 - 792   2011.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 更年期外来における漢方診療の対象例および使用薬剤の特徴に関する検討

    堀場 裕子, 牧田 和也, 平沢 晃, 松村 聡子, 小川 真里子, 岩田 卓, 弟子丸 亮太, 柳本 茂久, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   63 ( 2 )   471 - 471   2011.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 1 研究概要 1.1 施設研究 1.1.2 日本人における遺伝性非ポリポーシス大腸癌(HNPCC)の臨床像の解明

    菅野康吉, 笠原優一, 斉藤聡, 石川秀樹, 石川秀樹, 冨田尚裕, 小杉眞司, 長谷川博俊, 武田祐子, 進伸幸, 平澤晃, 藤田伸, 赤須孝之, 山本聖一郎, 森谷宜皓, 牛尾恭輔, 那須淳一郎, 岩間毅夫, 福嶋義光, 櫻井晃洋, 固武健二郎, 松井孝至, 野水整

    栃木県立がんセンター年報   ( 23 )   2011

  • 閉経後の片頭痛患者の特徴に関する実態調査(第1報)

    牧田 和也, 平沢 晃, 柴田 護, 清水 利彦, 青木 大輔, 鈴木 則宏

    日本頭痛学会誌   37 ( 2 )   238 - 238   2010.11

     More details

    Language:Japanese   Publisher:(一社)日本頭痛学会  

    researchmap

  • 抗がん剤のPK/PDとPGx 個別化投薬へ向けて がん臨床現場におけるファーマコゲノミクスの導入

    平沢 晃, 赤羽 智子, 鶴田 智彦, 野村 弘行, 進 伸幸, 小崎 健次郎, 谷川原 祐介, 青木 大輔

    臨床薬理   41 ( Suppl. )   S149 - S149   2010.11

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • 子宮体癌両側卵巣摘出例における骨密度とESR1およびUGT2B17遺伝子コピー数多型との関連についての検討

    平沢 晃, 牧田 和也, 赤羽 智子, 池ノ上 学, 松村 聡子, 堀場 裕子, 岩田 卓, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 吉村 泰典, 青木 大輔

    日本更年期医学会雑誌   18 ( Suppl. )   154 - 154   2010.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 当科健康維持外来における更年期女性に対する漢方製剤の使用状況について

    堀場 裕子, 牧田 和也, 平沢 晃, 岩田 卓, 小川 真理子, 弟子丸 亮太, 柳本 茂久, 青木 大輔

    日本更年期医学会雑誌   18 ( Suppl. )   132 - 132   2010.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 当科健康維持外来受診患者が初診時に訴える諸症状に関する検討

    松村 聡子, 牧田 和也, 堀場 裕子, 平沢 晃, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 高松 潔, 青木 大輔

    日本更年期医学会雑誌   18 ( Suppl. )   132 - 132   2010.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 再発卵巣がん治療 最先端を覗く プラチナ耐性再発卵巣癌に対する薬物療法の選択 CPT-11およびPLD投与例の比較から

    野村 弘行, 津田 浩史, 片岡 史夫, 千代田 達幸, 平沢 晃, 冨永 英一郎, 進 伸幸, 青木 大輔

    日本癌治療学会誌   45 ( 2 )   456 - 456   2010.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 卵巣明細胞腺癌におけるHNF1βの発現特異性と臨床病理学的因子との関連に関する検討

    赤羽 智子, 冨永 英一郎, 平沢 晃, 進 伸幸, 青木 大輔

    日本組織細胞化学会総会・学術集会講演プログラム・予稿集   51回   78 - 78   2010.9

     More details

    Language:Japanese   Publisher:日本組織細胞化学会  

    researchmap

  • 分子診断に焦点を合わせた内膜病変の診断法、検査法 子宮内膜細胞診検体を用いたエピジェネティックなDNA異常メチル化とその診断への応用

    阪埜 浩司, 小林 佑介, 植木 有紗, 木須 伊織, 増田 健太, 小野 あすか, 野村 弘行, 平沢 晃, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   49 ( Suppl.2 )   498 - 498   2010.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 当科『健康維持外来』におけるラロキシフェン発売以来今日までの使用状況についての検討

    牧田 和也, 平沢 晃, 松村 聡子, 堀場 裕子, 岩田 卓, 青木 大輔

    SERM: Selective Estrogen Receptor Modulator   ( 8 )   76 - 77   2010.9

     More details

    Language:Japanese   Publisher:(株)メディカルレビュー社  

    researchmap

  • 子宮体癌の子宮鏡検査と細胞診

    照井 仁美, 進 伸幸, 荒井 ゆり子, 長島 義男, 木須 伊織, 平沢 晃, 阪埜 浩司, 塚崎 克己, 青木 大輔

    日本臨床細胞学会雑誌   49 ( Suppl.2 )   554 - 554   2010.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 卵巣癌におけるHNF1βの発現特異性と臨床病理学的因子との関連

    赤羽 智子, 冨永 英一郎, 平沢 晃, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   49 ( Suppl.2 )   654 - 654   2010.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 間質におけるVimentin陽性となる紡錘形細胞のEGR-1発現は、上皮性卵巣癌の予後規定因子である(EGR-1 expression of vimentin-positive spindle-shaped cells in stroma is a prognostic indicator of ovarian cancer)

    片岡 史夫, 津田 浩史, 荒尾 徳三, 田中 英雄, 西村 貞子, 野村 弘行, 千代田 達幸, 平沢 晃, 鈴木 淳, 進 伸幸, 西尾 和人, 青木 大輔

    日本癌学会総会記事   69回   261 - 261   2010.8

     More details

    Language:English   Publisher:日本癌学会  

    researchmap

  • シアリダーゼ発現の低下は卵巣癌腹膜播種形成を抑制しうる(Decrease in sialidase expression may lead to suppressed development of peritoneal metastasis in ovarian cancer)

    野村 弘行, 津田 浩史, 片岡 史夫, 千代田 達幸, 平沢 晃, 冨永 英一郎, 進 伸幸, 青木 大輔

    日本癌学会総会記事   69回   467 - 467   2010.8

     More details

    Language:English   Publisher:日本癌学会  

    researchmap

  • 子宮体癌細胞株の機能的スクリーニングを用いたエピゲノム異常により発現抑制される癌抑制遺伝子型microRNAの同定(Functional screening of tumor-suppressive microRNA silenced by DNA hypermethylation in endometrial cancer)

    鶴田 智彦, 小崎 健一, 平沢 晃, 阪埜 浩司, 進 伸幸, 井本 逸勢, 青木 大輔, 稲澤 譲治

    日本癌学会総会記事   69回   404 - 404   2010.8

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 子宮体癌培養細胞株を用いたエピジェネティックに制御され癌抑制遺伝子として機能するmicroRNAの検索(A microRNA that is epigenetically regulated and functions as a tumor suppressor in endometrial cancer)

    阪埜 浩司, 矢野倉 恵, 小林 佑介, 植木 有紗, 木須 伊織, 野村 弘行, 平沢 晃, 進 伸幸, 青木 大輔

    日本癌学会総会記事   69回   173 - 174   2010.8

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 喉頭癌および子宮体癌における癌特異的miRNAsならびにDNAメチル化異常(Comparative analysis of cancer-specific miRNAs and aberrant DNA methylation in laryngeal cancer or endometrial cancer)

    木村 美和子, 平沢 晃, 神本 高宏, 矢部 はる奈, 小川 郁, 齋藤 康一郎, 座間 猛

    日本癌学会総会記事   69回   223 - 223   2010.8

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 腫瘍間質のVimentin陽性細胞のEGR-1発現は上皮性卵巣癌の予後と相関する

    片岡 史夫, 津田 浩史, 西村 貞子, 冨永 英一郎, 野村 弘行, 千代田 達幸, 平沢 晃, 鈴木 淳, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   28 ( 3 )   303 - 303   2010.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 進行期I期上皮性卵巣癌における予後因子の解析

    野村 弘行, 津田 浩史, 片岡 史夫, 千代田 達幸, 鈴木 淳, 平沢 晃, 冨永 英一郎, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   28 ( 3 )   302 - 302   2010.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 進行子宮体癌の集学的治療 リンパ節郭清範囲と化学療法内容は進行子宮体癌の予後へ影響を与えるか?

    進 伸幸, 野村 弘行, 平沢 晃, 阪埜 浩司, 津田 浩史, 青木 大輔

    日本婦人科腫瘍学会雑誌   28 ( 3 )   256 - 256   2010.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体癌肺転移症例の解析による胸部X線検査の有用性

    小林 佑介, 阪埜 浩司, 木須 伊織, 岸見 有紗, 松村 聡子, 野村 弘行, 平沢 晃, 進 伸幸, 塚崎 克己, 青木 大輔

    日本婦人科腫瘍学会雑誌   28 ( 3 )   339 - 339   2010.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 若年子宮体癌G2類内膜癌4例に対する妊孕性温存黄体ホルモン療法の経験 G2例に適応してよいか?

    進 伸幸, 木須 伊織, 植木 有紗, 小林 佑介, 秋好 順子, 鶴田 智彦, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 鈴木 淳, 阪埜 浩司, 津田 浩史, 青木 大輔

    日本婦人科腫瘍学会雑誌   28 ( 3 )   337 - 337   2010.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • NBI(Narrow Band Imaging)システムを用いた子宮鏡検査の有用性

    木須 伊織, 阪埜 浩司, 小林 佑介, 岸見 有紗, 野村 弘行, 平沢 晃, 進 伸幸, 塚崎 克己, 青木 大輔

    日本婦人科腫瘍学会雑誌   28 ( 3 )   335 - 335   2010.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 癌と遺伝カウンセリング BRCA1/2の外来における遺伝子診断 産婦人科臨床の立場から

    平沢 晃, 菅野 康吉, 鶴田 智彦, 阪埜 浩司, 進 伸幸, 三須 久美子, 矢崎 久妙子, 武田 祐子, 青木 大輔

    家族性腫瘍   10 ( 2 )   A26 - A26   2010.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • Peutz-Jegher症候群に対する遺伝相談外来受診を契機として発見された子宮頸部分葉状頸管腺過形成の1例

    平沢 晃, 鶴田 智彦, 小林 祐介, 阪埜 浩司, 進 伸幸, 矢崎 久妙子, 武田 祐子, 菅野 康吉, 青木 大輔

    家族性腫瘍   10 ( 2 )   A50 - A50   2010.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 本領域の分子生物学的特性 頭頸部腫瘍とmiRNA 網羅的解析による喉頭腫瘍のmiRNAプロファイリング

    齋藤 康一郎, 長西 秀樹, 稲垣 康治, 平沢 晃, 大久保 啓介, 小川 郁, 座間 猛

    日本気管食道科学会会報   61 ( 2 )   221 - 222   2010.4

     More details

    Language:Japanese   Publisher:(NPO)日本気管食道科学会  

    researchmap

  • 本領域の分子生物学的特性 頭頸部腫瘍とmiRNA 喉頭癌の血中マーカー・治療標的としてのmiR-196a

    齋藤 康一郎, 矢部 はる奈, 稲垣 康治, 長西 秀樹, 平沢 晃, 伊藤 葉子, 杉田 紀明, 佐竹 恵美子, 中條 聖子, 大久保 啓介, 小川 郁, 座間 猛

    日本気管食道科学会会報   61 ( 2 )   222 - 222   2010.4

     More details

    Language:Japanese   Publisher:(NPO)日本気管食道科学会  

    researchmap

  • 本領域の分子生物学的特性 頭頸部腫瘍とmiRNA 喉頭癌におけるバイオマーカーとしてのmiRNAs

    宇野 光祐, 齋藤 康一郎, 伊藤 葉子, 椙田 紀明, 中條 聖子, 平沢 晃, 森 有子, 長西 秀樹, 稲垣 康治, 大久保 啓介, 小川 郁, 座間 猛

    日本気管食道科学会会報   61 ( 2 )   222 - 222   2010.4

     More details

    Language:Japanese   Publisher:(NPO)日本気管食道科学会  

    researchmap

  • 腫瘍間質の遺伝子発現解析による進行上皮性卵巣癌の予後規定因子の同定

    片岡 史夫, 津田 浩史, 西村 貞子, 野村 弘行, 千代田 達幸, 平沢 晃, 冨永 英一郎, 鈴木 淳, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   62 ( 2 )   421 - 421   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • GNAS遺伝子の増幅は標準治療を施行した上皮性卵巣癌の独立した予後因子である

    冨永 英一郎, 津田 浩史, 西村 貞子, 千代田 達幸, 野村 弘行, 片岡 史夫, 鈴木 淳, 平沢 晃, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   62 ( 2 )   419 - 419   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • sentinel navigation system(SNS)を用いて微小転移リンパ節を確認し得た子宮体癌4症例

    進 伸幸, 片岡 史夫, 野村 弘行, 平沢 晃, 阪埜 浩司, 中原 理紀, 竹内 裕也, 亀山 香織, 津田 浩史, 栗林 幸夫, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   62 ( 2 )   340 - 340   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • NBI(Narrow Band Imaging)システムを用いた軟性子宮鏡による子宮内膜病変の診断への応用

    木須 伊織, 阪埜 浩司, 小林 佑介, 小川 誠司, 岸見 有紗, 松村 聡子, 山上 亘, 平沢 晃, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   62 ( 2 )   687 - 687   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 加味逍遙散投与、ホルモン補充療法の更年期障害に対する効果の比較 精神神経症状評価スケール、症状推移からみた比較

    樋口 毅, 片桐 清一, 真鍋 麻美, 斎藤 勝, 橋本 哲司, 松本 貴, 前田 由子, 蓮尾 豊, 松尾 健志, 藤盛 嘉章, 小川 克弘, 小野 大志, 野呂 秀逸, 坂本 知巳, 高橋 秀身, 冨浦 一行, 丹藤 伴江, 高松 潔, 櫻木 範明, 蝦名 康彦, 大場 洋子, 武田 真人, 八重樫 稔, 田中 信一, 吉村 泰典, 青木 大輔, 牧田 和也, 平沢 晃, 冨永 英一郎, 高橋 峰夫, 深谷 孝夫, 池上 信夫, 和氣 徳夫, 加藤 聖子, 野崎 雅裕, 若槻 明彦, 神谷 直樹, 水沼 英樹, 谷口 綾亮, 柞木田 礼子, 阿部 和弘, 飯野 香理

    日本産科婦人科学会雑誌   62 ( 2 )   631 - 631   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌術後例における血清脂質値の特徴

    松村 聡子, 平沢 晃, 牧田 和也, 堀場 裕子, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 阪埜 浩司, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   62 ( 2 )   629 - 629   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮癌肉腫と子宮内膜癌の臨床的相違に関する検討

    岸見 有紗, 阪埜 浩司, 小林 佑介, 木須 伊織, 小川 誠司, 堀場 裕子, 野村 弘行, 平沢 晃, 進 伸幸, 塚崎 克己, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   62 ( 2 )   548 - 548   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 再発子宮体癌症例に対するPlatinum free intervalに基づいた治療戦略の検証

    小林 佑介, 阪埜 浩司, 野村 弘行, 岸見 有紗, 小川 誠司, 木須 伊織, 市川 義一, 平沢 晃, 進 伸幸, 塚崎 克己, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   62 ( 2 )   532 - 532   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌培養細胞株を用いたエピジェネティックに制御され癌抑制遺伝子として機能するmicroRNAの検索

    阪埜 浩司, 矢野倉 恵, 小林 佑介, 岸見 有紗, 木須 伊織, 小川 誠司, 野村 弘行, 平沢 晃, 進 伸幸, 塚崎 克己, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   62 ( 2 )   409 - 409   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 機能的スクリーニングを用いたDNA過剰メチル化により発現抑制される子宮体癌新規癌抑制型microRNAの探索

    鶴田 智彦, 平沢 晃, 阪埜 浩司, 進 伸幸, 小崎 健一, 井本 逸勢, 稲澤 譲治, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   62 ( 2 )   409 - 409   2010.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 日本人における遺伝性非ポリポーシス大腸癌(HNPCC)の臨床像の解明

    菅野康吉, 笠原優一, 斉藤聡, 石川秀樹, 石川秀樹, 冨田尚裕, 小杉眞司, 長谷川博俊, 武田祐子, 進伸幸, 平澤晃, 藤田伸, 赤須孝之, 山本聖一郎, 森谷宜皓, 牛尾恭輔, 那須淳一郎, 岩間毅夫, 福嶋義光, 櫻井晃洋, 固武健二郎, 松井孝至, 野水整

    栃木県立がんセンター年報   ( 22 )   2010

  • 閉経後の片頭痛患者の特徴に関する実態調査(第1報)

    牧田和也, 平沢晃, 柴田護, 清水利彦, 青木大輔, 鈴木則宏

    日本頭痛学会誌   37 ( 2 )   2010

  • 当科「健康維持外来」におけるホルモン補充療法施行症例についての多角的検討

    牧田 和也, 松村 聡子, 堀場 裕子, 平沢 晃, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 高松 潔, 青木 大輔

    日本更年期医学会雑誌   17 ( Suppl. )   84 - 84   2009.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 当科「健康維持外来」における子宮体癌術後症例に認められる不定愁訴の検討

    松村 聡子, 牧田 和也, 堀場 裕子, 平沢 晃, 小川 真里子, 弟子丸 亮太, 柳本 茂久, 高松 潔, 青木 大輔

    日本更年期医学会雑誌   17 ( Suppl. )   120 - 120   2009.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 遺伝性乳がん卵巣がんに対する予防的卵巣摘出術施行に伴う課題の検討

    平沢 晃, 牧田 和也, 堀場 裕子, 松村 聡子, 鶴田 智彦, 小川 真里子, 柳本 茂久, 弟子丸 亮太, 菅野 康吉, 青木 大輔

    日本更年期医学会雑誌   17 ( Suppl. )   120 - 120   2009.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 閉経前両側卵巣摘出例の骨密度とFRAXを用いた骨折リスクの検討・評価とその有用性についての検討

    堀場 裕子, 平沢 晃, 牧田 和也, 松村 聡子, 小川 真里子, 岩田 卓, 弟子丸 亮太, 柳本 茂久, 青木 大輔

    日本更年期医学会雑誌   17 ( Suppl. )   101 - 101   2009.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 老人性腟炎に対するエストリオール製剤の効果における年齢別の検討

    弟子丸 亮太, 牧田 和也, 箕輪 昌子, 渡辺 英明, 堀場 裕子, 松村 聡子, 三上 佳子, 小川 真里子, 柳本 茂久, 平沢 晃, 高橋 峰夫, 青木 大輔

    日本更年期医学会雑誌   17 ( Suppl. )   85 - 85   2009.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 上皮性卵巣癌における後腹膜リンパ節郭清の意義についての検討

    野村 弘行, 津田 浩史, 片岡 史夫, 千代田 達幸, 平沢 晃, 冨永 英一郎, 鈴木 淳, 進 伸幸, 青木 大輔

    日本癌治療学会誌   44 ( 2 )   628 - 628   2009.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 子宮内膜細胞診疑陽性検体におけるhMLH1異常メチル化は内膜癌の存在を示唆するか

    木須 伊織, 阪埜 浩司, 小林 佑介, 岸見 有紗, 小川 誠司, 平沢 晃, 進 伸幸, 塚崎 克己, 長谷川 寿彦, 青木 大輔

    日本臨床細胞学会雑誌   48 ( Suppl.2 )   491 - 491   2009.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 子宮体癌治療後腟再発症例の解析による腟細胞診検査の有用性についての検討

    小林 佑介, 阪埜 浩司, 野村 弘行, 小川 誠司, 岸見 有紗, 木須 伊織, 堀場 裕子, 平沢 晃, 津田 浩史, 進 伸幸, 塚崎 克己, 青木 大輔

    日本癌治療学会誌   44 ( 2 )   618 - 618   2009.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 子宮体癌における腹腔細胞診の臨床的意義と新規診断マーカーの検索

    冨永 英一郎, 進 伸幸, 赤羽 智子, 山上 亘, 東口 敦司, 平沢 晃, 青木 大輔

    日本組織細胞化学会総会・学術集会講演プログラム・予稿集   50回   96 - 96   2009.9

     More details

    Language:Japanese   Publisher:日本組織細胞化学会  

    researchmap

  • 子宮体癌におけるTリンパ球浸潤と臨床病理学的因子の検討

    山上 亘, 進 伸幸, 田中 英雄, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 津田 浩史, 吉村 泰典, 青木 大輔

    日本組織細胞化学会総会・学術集会講演プログラム・予稿集   50回   95 - 95   2009.9

     More details

    Language:Japanese   Publisher:日本組織細胞化学会  

    researchmap

  • 子宮体部癌肉腫12例の細胞学的検討

    荒井 ゆり子, 照井 仁美, 長島 義男, 野村 弘行, 平沢 晃, 阪埜 浩司, 藤井 多久磨, 進 伸幸, 塚崎 克己, 青木 大輔

    日本臨床細胞学会雑誌   48 ( Suppl.2 )   596 - 596   2009.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • FRAXの子宮体癌例への応用についての課題

    平沢 晃, 牧田 和也, 堀場 裕子, 岩田 卓, 小川 真理子, 弟子丸 亮太, 柳本 茂久, 阪埜 浩司, 進 伸幸, 青木 大輔

    Osteoporosis Japan   17 ( Suppl.1 )   226 - 226   2009.9

     More details

    Language:Japanese   Publisher:ライフサイエンス出版(株)  

    researchmap

  • 当科更年期外来における塩酸ラロキシフェン使用の現状 子宮体癌術後症例を中心に

    牧田 和也, 堀場 裕子, 岩田 卓, 平沢 晃, 片岡 史夫, 富永 英一郎, 堀口 文, 青木 大輔

    SERM: Selective Estrogen Receptor Modulator   ( 7 )   74 - 75   2009.8

     More details

    Language:Japanese   Publisher:(株)メディカルレビュー社  

    researchmap

  • 【子宮疾患・子宮内膜症の臨床 基礎・臨床研究のアップデート】感染症・炎症性疾患 子宮傍結合織炎

    進 伸幸, 平沢 晃, 青木 大輔

    日本臨床   67 ( 増刊5 子宮疾患・子宮内膜症の臨床 )   327 - 330   2009.8

  • Aurora-A siRNAはin vivoにおける子宮体がん細胞に対するタキサン製剤の抗腫瘍効果を増強する(Aurora-A siRNA enhances the antitumor effect of taxanes for endometrial cancer in vivo)

    阪埜 浩司, 矢野倉 恵, 小林 佑介, 小川 誠司, 岸見 有紗, 野村 弘行, 平沢 晃, 進 伸幸, 青木 大輔

    日本癌学会総会記事   68回   330 - 331   2009.8

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 子宮体癌細胞株の機能的スクリーニングを用いたエピゲノム異常により発現抑制される癌抑制遺伝子型microRNAの探索(Functional screening of tumor-suppressive microRNAs silenced by DNA hypermethylation in endometrial cancer)

    鶴田 智彦, 小崎 健一, 平沢 晃, 阪埜 浩司, 進 伸幸, 井本 逸勢, 青木 大輔, 稲澤 譲治

    日本癌学会総会記事   68回   258 - 258   2009.8

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 頭頸部癌におけるマイクロRNA(Distinct Roles of microRNAs in Head and Neck Squamous Cell Carcinoma)

    宇野 光祐, 齋藤 康一郎, 稲垣 康治, 平沢 晃, 椙田 紀明, 伊藤 葉子, 大久保 啓介, 座間 猛

    日本癌学会総会記事   68回   146 - 146   2009.8

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 卵巣癌3rd line化学療法の効果予測因子の検討

    千代田 達幸, 津田 浩史, 野村 弘行, 片岡 史夫, 冨永 英一郎, 鈴木 淳, 平沢 晃, 山上 亘, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   27 ( 3 )   294 - 294   2009.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 腫瘍-間質相互作用に着目した上皮性卵巣癌標準治療の効果予測システムの構築

    片岡 史夫, 津田 浩史, 冨永 英一郎, 西村 貞子, 平沢 晃, 野村 弘行, 千代田 達幸, 鈴木 淳, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   27 ( 3 )   296 - 296   2009.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 【小児疾患における臨床遺伝学の進歩】遺伝子診断がもたらす治療の進歩 イリノテカン

    平沢 晃, 鶴田 智彦, 進 伸幸, 青木 大輔

    小児科   50 ( 7 )   1227 - 1232   2009.6

     More details

    Language:Japanese   Publisher:金原出版(株)  

    researchmap

  • 子宮体がんにおけるマイクロRNAの発現プロファイリング

    平沢 晃, 齋藤 康一郎, 赤羽 智子, 伊藤 葉子, 椙田 紀明, 中條 聖子, 進 伸幸, 青木 大輔, 座間 猛

    日本婦人科腫瘍学会雑誌   27 ( 3 )   281 - 281   2009.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 産婦人科受診者を対象としたBRCA1およびBRCA2遺伝子解析とサーベイランスに関する検討

    堀場 裕子, 平沢 晃, 小林 佑介, 鶴田 智彦, 阪埜 浩司, 武田 祐子, 進 伸幸, 菅野 泰吉, 青木 大輔

    日本婦人科腫瘍学会雑誌   27 ( 3 )   292 - 292   2009.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体癌治療後腟再発症例の解析による腟壁部分切除の意義についての検討

    小林 佑介, 阪埜 浩司, 野村 弘行, 堀場 裕子, 平沢 晃, 進 伸幸, 塚崎 克己, 青木 大輔

    日本婦人科腫瘍学会雑誌   27 ( 3 )   283 - 283   2009.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体部・卵巣同時性重複癌31症例に対する臨床病理学的検討

    小林 佑介, 阪埜 浩司, 野村 弘行, 平沢 晃, 津田 浩史, 進 伸幸, 塚崎 克己, 青木 大輔

    家族性腫瘍   9 ( 2 )   A42 - A42   2009.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 新アムステルダムクライテリアを満たす子宮体癌の頻度と臨床的特徴

    阪埜 浩司, 小林 佑介, 平沢 晃, 進 伸幸, 長谷川 清志, 宇田川 康博, 大和田 倫孝, 平井 康夫, 青木 大輔

    家族性腫瘍   9 ( 2 )   A42 - A42   2009.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 遺伝性乳がん卵巣がんをとりまく課題 卵巣がんサーベイランスにおける予防的卵巣摘出術に関する課題

    平沢 晃, 菅野 康吉, 鶴田 智彦, 小林 佑介, 阪埜 浩司, 進 伸幸, 矢崎 久妙子, 武田 祐子, 青木 大輔

    家族性腫瘍   9 ( 2 )   A22 - A22   2009.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 喉頭癌におけるマイクロRNA(4) バイオマーカーとしての血液循環マイクロRNA

    長西 秀樹, 齋藤 康一郎, 伊藤 葉子, 椙田 紀明, 佐竹 恵美子, 中條 聖子, 大久保 啓介, 稲垣 康治, 矢部 はる奈, 平沢 晃, 座間 猛

    頭頸部癌   35 ( 2 )   142 - 142   2009.5

     More details

    Language:Japanese   Publisher:(一社)日本頭頸部癌学会  

    researchmap

  • 遺伝性乳がん・卵巣がんの遺伝カウンセリング広報活動報告

    矢崎 久妙子, 武田 祐子, 平沢 晃, 菅野 康吉

    家族性腫瘍   9 ( 2 )   A48 - A48   2009.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 喉頭癌におけるマイクロRNA(1) 網羅的解析による発現プロファイリング

    齋藤 康一郎, 伊藤 葉子, 椙田 紀明, 中條 聖子, 長西 秀樹, 大久保 啓介, 稲垣 康治, 平沢 晃, 座間 猛

    頭頸部癌   35 ( 2 )   141 - 141   2009.5

     More details

    Language:Japanese   Publisher:(一社)日本頭頸部癌学会  

    researchmap

  • 喉頭癌におけるマイクロRNA(3) 新たな治療標的としてのマイクロRNA

    稲垣 康治, 齋藤 康一郎, 長西 秀樹, 大久保 啓介, 赤羽 智子, 平沢 晃, 座間 猛

    頭頸部癌   35 ( 2 )   142 - 142   2009.5

     More details

    Language:Japanese   Publisher:(一社)日本頭頸部癌学会  

    researchmap

  • 喉頭癌におけるマイクロRNA(2) 喉頭癌におけるバイオマーカーとしてのマイクロRNAs

    宇野 光祐, 齋藤 康一郎, 伊藤 葉子, 椙田 紀明, 中條 聖子, 長西 秀樹, 大久保 啓介, 稲垣 康治, 平沢 晃, 座間 猛

    頭頸部癌   35 ( 2 )   142 - 142   2009.5

     More details

    Language:Japanese   Publisher:(一社)日本頭頸部癌学会  

    researchmap

  • 当科健康維持外来患者におけるWHO骨折リスク評価ツール(FRAX)の有用性に関する検討

    堀場 裕子, 平沢 晃, 牧田 和也, 弟子丸 亮太, 柳本 茂久, 野村 弘行, 片岡 史夫, 岩田 卓, 冨永 英一郎, 堀口 文, 青木 大輔, 吉村 泰典

    日本産科婦人科学会関東連合地方部会誌   46 ( 2 )   210 - 210   2009.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 子宮体癌腹腔洗浄細胞診の今日的話題 子宮体癌腹腔細胞診の臨床的意義

    冨永 英一郎, 進 伸幸, 平沢 晃, 赤羽 智子, 長島 義男, 照井 仁美, 青木 大輔

    日本臨床細胞学会雑誌   48 ( Suppl.1 )   108 - 108   2009.3

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 子宮体癌治療後経過観察における腟細胞診検査の有用性についての検討

    小林 佑介, 阪埜 浩司, 野村 弘行, 三上 佳子, 山上 亘, 平沢 晃, 津田 浩史, 進 伸幸, 塚崎 克己, 青木 大輔

    日本臨床細胞学会雑誌   48 ( Suppl.1 )   221 - 221   2009.3

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • サイトメトリーによる細胞解析と臨床応用(日本サイトメトリー学会合同ワークショップ) アレイCGHによる子宮体癌関連遺伝子および薬剤感受性遺伝子の探索

    鶴田 智彦, 平沢 晃, 赤羽 智子, 山上 亘, 阪埜 浩司, 井本 逸勢, 稲澤 譲治, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   48 ( Suppl.1 )   137 - 137   2009.3

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • サイトメトリーによる細胞解析と臨床応用(日本サイトメトリー学会合同ワークショップ) FISH法の子宮体癌への臨床応用 癌診断と治療効果推定

    進 伸幸, 平沢 晃, 阪埜 浩司, 青木 大輔

    日本臨床細胞学会雑誌   48 ( Suppl.1 )   137 - 137   2009.3

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 標準治療を受けた表層上皮性卵巣癌の再発リスクを規程する遺伝子の探索

    冨永 英一郎, 津田 浩史, 西村 貞子, 千代田 達幸, 野村 弘行, 片岡 史夫, 鈴木 淳, 平沢 晃, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   61 ( 2 )   658 - 658   2009.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • FRAXを用いた産婦人科諸疾患における骨折リスク評価の検討

    堀場 裕子, 平沢 晃, 牧田 和也, 弟子丸 亮太, 柳本 茂久, 野村 弘行, 片岡 史夫, 岩田 卓, 冨永 英一郎, 堀口 文, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   61 ( 2 )   641 - 641   2009.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮頸癌細胞におけるWRN遺伝子異常メチル化と抗癌剤感受性との関連

    阪埜 浩司, 矢野倉 恵, 小林 佑介, 三上 佳子, 平沢 晃, 進 伸幸, 塚崎 克己, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   61 ( 2 )   674 - 674   2009.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • Aurora-A siRNAはin vivoにおける子宮体癌細胞に対するタキサン製剤の抗腫瘍効果を増強する

    矢野倉 恵, 阪埜 浩司, 小林 佑介, 三上 佳子, 平沢 晃, 進 伸幸, 塚崎 克己, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   61 ( 2 )   538 - 538   2009.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌手術における傍大動脈リンパ節郭清は省略可能か?

    藤本 俊郎, 片桐 清一, 真鍋 麻美, 齋藤 勝, 橋本 哲司, 松本 貴, 前田 由子, 蓮尾 豊, 松尾 健志, 藤盛 嘉章, 小川 克弘, 小野 大志, 野呂 秀逸, 坂本 知巳, 高橋 秀身, 冨浦 一行, 丹藤 伴江, 高松 潔, 櫻木 範明, 蝦名 康彦, 大場 洋子, 武田 真人, 八重樫 稔, 田中 信一, 吉村 泰典, 青木 大輔, 牧田 和也, 平沢 晃, 冨永 英一郎, 高橋 峰夫, 深谷 孝夫, 池上 信夫, 和氣 徳夫, 加藤 聖子, 野崎 雅裕, 若槻 明彦, 神谷 直樹, 水沼 英樹, 樋口 毅, 谷口 綾亮, 柞木田 礼子

    日本産科婦人科学会雑誌   61 ( 2 )   455 - 455   2009.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • UGT1A1遺伝子多型とイリノテカンの有害事象およびグルクロン酸抱合能に関するゲノム薬理学的検討

    平沢 晃, 赤羽 智子, 野村 弘行, 阪埜 浩司, 津田 浩史, 齋藤 康一郎, 座間 猛, 後田 奈緒美, 谷川原 祐介, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   61 ( 2 )   444 - 444   2009.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 若年体癌症例に対する子宮温存目的酢酸メドロキシプロゲステロン(MPA)療法のpitfall 子宮摘出に至った21症例における子宮外病変の検討より

    進 伸幸, 平沢 晃, 鶴田 智彦, 市川 義一, 末盛 友浩, 山上 亘, 片岡 史夫, 鈴木 淳, 阪埜 浩司, 津田 浩史, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   61 ( 2 )   659 - 659   2009.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 日本人における遺伝性非ポリポーシス大腸癌(HNPCC)の臨床像の解明-Muir-Torre症候群とHNPCC-

    菅野康吉, 小山尚樹, 斉藤聡, 石川秀樹, 石川秀樹, 冨田尚裕, 小杉眞司, 長谷川博俊, 武田祐子, 進伸幸, 平澤晃, 藤田伸, 赤須孝之, 山本聖一郎, 森谷宜皓, 牛尾恭輔, 那須淳一郎, 岩間毅夫, 福嶋義光, 櫻井晃洋, 固武健二郎, 松井孝至, 野水整

    栃木県立がんセンター年報   ( 21 )   2009

  • 傍卵巣嚢腫から発生した腫瘍の二例

    秋田大宇, 奥田茂男, 秋田あやの, 陣崎雅弘, 谷本伸弘, 藤井多久磨, 平沢晃, 浅田弘法, 青木大輔, 栗林幸夫

    Abstracts. Annual Symposium. Japanese Society for the Advancement of Women’s Imaging   10th (Web)   2009

  • UGT1A1遺伝子多型と血清ビリルビン値の関連および婦人科イリノテカン療法副作用への関与に関する検討

    平沢 晃, 赤羽 智子, 長西 秀樹, 大久保 啓介, 齋藤 康一郎, 座間 猛, 野村 弘行, 津田 浩史, 進 伸幸, 後田 奈緒美, 谷川原 祐介, 青木 大輔

    臨床薬理   39 ( Suppl. )   S286 - S286   2008.11

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • 再発子宮体癌治療における白金製剤反復投与の意義とplatinum free intervalに関する検討

    市川 義一, 進 伸幸, 末盛 友浩, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 津田 浩史, 阪埜 浩司, 青木 大輔

    日本癌治療学会誌   43 ( 2 )   412 - 412   2008.10

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 再発卵巣癌に対する治療戦略 再発卵巣癌に対する治療戦略 卵巣癌初回治療後のサーベイランスの観点から

    野村 弘行, 津田 浩史, 片岡 史夫, 山上 亘, 平沢 晃, 冨永 英一郎, 鈴木 淳, 進 伸幸, 青木 大輔

    日本癌治療学会誌   43 ( 2 )   375 - 375   2008.10

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 当科更年期外来におけるラロキシフェンの使用状況について

    牧田 和也, 堀場 裕子, 岩田 卓, 平沢 晃, 片岡 史夫, 富永 英一郎, 堀口 文, 青木 大介

    SERM: Selective Estrogen Receptor Modulator   ( 6 )   60 - 61   2008.10

     More details

    Language:Japanese   Publisher:(株)メディカルレビュー社  

    researchmap

  • 当科健康維持外来受診者におけるFRAXによる骨折リスク評価の検討

    堀場 裕子, 牧田 和也, 平沢 晃, 弟子丸 亮太, 柳本 茂久, 堀口 文, 青木 大輔

    日本更年期医学会雑誌   16 ( Suppl. )   85 - 85   2008.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 当科「健康維持外来」の現状 更年期外来から女性のトータルヘルスケア外来への転換

    牧田 和也, 堀場 裕子, 平沢 晃, 弟子丸 亮太, 柳本 茂久, 高松 潔, 堀口 文, 青木 大輔

    日本更年期医学会雑誌   16 ( Suppl. )   98 - 98   2008.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 標準治療を施行した進行上皮性卵巣癌の予後因子の網羅的探索(Expression profile of epithelial ovarian cancer patients receiving standard therapy)

    冨永 英一郎, 荒尾 徳三, 津田 浩史, 山上 亘, 野村 弘行, 平沢 晃, 鈴木 淳, 進 伸幸, 西村 貞子, 青木 大輔, 西尾 和人

    日本癌学会総会記事   67回   487 - 487   2008.9

     More details

    Language:English   Publisher:日本癌学会  

    researchmap

  • 卵巣境界悪性腫瘍における腹腔細胞診疑陽性症例の検討

    片岡 史夫, 津田 浩史, 千代田 達幸, 山上 亘, 野村 弘行, 平沢 晃, 冨永 英一郎, 鈴木 淳, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   47 ( Suppl.2 )   472 - 472   2008.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • エピジェネティック異常により発現抑制される子宮体がん関連癌抑制遺伝子のMPA療法における役割(Role of epigenetically silenced tumor suppressor genes in medroxyprogesterone acetate therapy for endometrial cancer)

    鶴田 智彦, 井本 逸勢, 平沢 晃, 小崎 健一, 阪埜 浩司, 進 伸幸, 青木 大輔, 稲澤 譲治

    日本癌学会総会記事   67回   109 - 109   2008.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • Pharmacogenomicsの進歩と展望 塩酸イリノテカンによるがん個別化治療を目指したUGT1A1遺伝子多型と血清ビリルビン値に関する検討(Recent Progress and Perspective of Pharmacogenomics Analysis of UGT1A1 polymorphisms and serum bilirubin levels for individualized cancer therapy using irinotecan)

    平沢 晃, 赤羽 智子, 山上 亘, 野村 弘行, 阪埜 浩司, 津田 浩司, 津田 浩史, 長西 秀樹, 大久保 啓介, 齋藤 康一郎, 座間 猛, 谷川原 祐介, 進 伸幸, 青木 大輔

    日本癌学会総会記事   67回   286 - 286   2008.9

     More details

    Language:English   Publisher:(一社)日本癌学会  

    researchmap

  • 子宮体癌術後例における血清脂質値と骨密度の特徴に関する検討

    堀場 裕子, 平沢 晃, 牧田 和也, 岩田 卓, 弟子丸 亮太, 柳本 茂久, 阪埜 浩司, 進 伸幸, 堀口 文, 青木 大輔, 吉村 泰典

    日本産科婦人科学会関東連合地方部会誌   45 ( 3 )   243 - 243   2008.8

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 病理診断 子宮内膜病変診断法としての2色FISH法の治療への応用 若年子宮体癌に対する妊孕性温存療法治療終了時期判定

    進 伸幸, 片岡 史夫, 平沢 晃, 阪埜 浩司, 青木 大輔

    組織細胞化学   2008   177 - 186   2008.7

     More details

    Language:Japanese   Publisher:日本組織細胞化学会  

    researchmap

  • カウンセリングを必要とした閉経期女性の態度および行動

    堀口 文, 牧田 和也, 平沢 晃, 冨永 英一郎, 堀場 裕子, 青木 大輔

    心身医学   48 ( 6 )   525 - 525   2008.6

  • ヒトモノクローナル抗体HMMC-1認識抗原が卵巣癌細胞の後腹膜リンパ節転移に与える影響

    冨永 英一郎, 鈴木 淳, 鶴田 智彦, 山上 亘, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   26 ( 3 )   329 - 329   2008.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 婦人科手術後に発症した疼痛性障害(pain disorder)の1例

    牧田 和也, 堀場 裕子, 平沢 晃, 堀口 文, 高松 潔, 青木 大輔

    女性心身医学   13 ( 1-2 )   59 - 59   2008.6

  • 卵巣癌初回治療後サーベイランスに関する検討

    野村 弘行, 鶴田 智彦, 山上 亘, 片岡 史夫, 平沢 晃, 冨永 英一郎, 鈴木 淳, 津田 浩史, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   26 ( 3 )   267 - 267   2008.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体部・卵巣同時発生重複癌27症例の臨床病理学的検討

    小林 佑介, 野村 弘行, 秋好 順子, 平沢 晃, 冨永 英一郎, 鈴木 淳, 津田 浩史, 阪埜 浩司, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   26 ( 3 )   272 - 272   2008.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • M期チェックポイントCHFR遺伝子siRNAによる子宮癌細胞株の抗癌剤感受性の変化

    阪埜 浩司, 矢野倉 恵, 小林 佑介, 秋好 順子, 桑原 佳子, 平沢 晃, 進 伸幸, 塚崎 克己, 青木 大輔

    日本婦人科腫瘍学会雑誌   26 ( 3 )   328 - 328   2008.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 乳がん 遺伝子診断・2次予防・カウンセリング 遺伝性乳がん・卵巣がんの遺伝子検査実施後の状況と遺伝相談外来の役割

    武田 祐子, 矢崎 久妙子, 平沢 晃, 青木 大輔, 池田 正, 神野 浩光, 菅野 康吉

    家族性腫瘍   8 ( 2 )   A50 - A50   2008.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 若年子宮体癌類内膜癌G2症例4例の妊孕性温存黄体ホルモン療法

    秋好 順子, 進 伸幸, 小林 佑介, 市川 義一, 末盛 友浩, 野村 弘行, 片岡 史夫, 平沢 晃, 鈴木 淳, 阪埜 浩司, 青木 大輔, 吉村 泰典

    日本産科婦人科学会関東連合地方部会誌   45 ( 2 )   176 - 176   2008.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • がん遺伝カウンセリング体制の基礎づくり 遺伝相談外来の役割を考える 遺伝相談外来の受診がHNPCC患者とその同胞のがん予防を促すきっかけとなった一事例

    矢崎 久妙子, 武田 祐子, 平沢 晃, 菅野 康吉

    家族性腫瘍   8 ( 2 )   A39 - A39   2008.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 腹腔内細胞診 子宮体癌における腹腔細胞診の意義

    冨永 英一郎, 進 伸幸, 長島 義男, 照井 仁美, 平沢 晃, 阪埜 浩司, 青木 大輔

    日本臨床細胞学会雑誌   47 ( Suppl.1 )   76 - 76   2008.3

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 塩酸イリノテカンの副作用軽減を目指したUGT1A1遺伝子多型解析

    平沢 晃, 鶴田 智彦, 市川 義一, 末盛 友浩, 東口 敦司, 冨永 英一郎, 阪埜 浩司, 進 伸幸, 後田 奈緒美, 谷川原 祐介, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   60 ( 2 )   782 - 782   2008.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌高転移細胞株の細胞表面糖鎖および分子発現解析

    鈴木 淳, 山上 亘, 冨永 英一郎, 末盛 友浩, 野村 弘行, 片岡 史夫, 平沢 晃, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   60 ( 2 )   540 - 540   2008.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 遺伝性乳癌卵巣癌の可能性がある受診者を対象としたBRCA1およびBRCA2遺伝子解析

    堀場 裕子, 平沢 晃, 小林 佑介, 鶴田 智彦, 野村 弘行, 片岡 史夫, 阪埜 浩司, 鈴木 淳, 進 伸幸, 菅野 康吉, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   60 ( 2 )   690 - 690   2008.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 若年子宮体癌の高容量黄体ホルモン療法の治療終了時期判定に有用な2色FISH法

    進 伸幸, 市川 義一, 末盛 友浩, 山上 亘, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 鈴木 淳, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   60 ( 2 )   817 - 817   2008.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • Lipid metabolism in patients with endometrial caner

    Akira Hirasawa, Yuko Horiba, Eiichiro Tominaga, Kouji Banno, Kazuya Makita, Nobuyuki Susumu, Fumi Horiguchi, Daisuke Aoki

    INTERNATIONAL JOURNAL OF CARDIOLOGY   122   115 - 115   2007.12

     More details

    Language:English   Publishing type:Research paper, summary (international conference)   Publisher:ELSEVIER IRELAND LTD  

    Web of Science

    researchmap

  • 更年期に認められる女性ホルモンの低下が片頭痛患者に及ぼす影響についての検討

    牧田 和也, 平沢 晃, 青木 大輔

    日本頭痛学会誌   34 ( 1 )   123 - 123   2007.11

     More details

    Language:Japanese   Publisher:(一社)日本頭痛学会  

    researchmap

  • UGT1A1遺伝子多型解析およびハプロタイプの血清総ビリルビン値への関与

    平沢 晃, 鶴田 智彦, 東口 敦司, 進 伸幸, 後田 奈緒美, 谷川原 祐介, 青木 大輔

    臨床薬理   38 ( Suppl. )   S191 - S191   2007.11

     More details

    Language:Japanese   Publisher:(一社)日本臨床薬理学会  

    researchmap

  • 子宮体癌症例における脂質代謝動態に関する検討

    平沢 晃, 牧田 和也, 堀場 裕子, 市川 義一, 末盛 友浩, 冨永 英一郎, 阪埜 浩司, 進 伸幸, 堀口 文, 青木 大輔

    日本更年期医学会雑誌   15 ( Suppl. )   117 - 117   2007.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 当科更年期外来受診者における動脈硬化性疾患の危険因子に関する検討

    堀場 裕子, 牧田 和也, 平沢 晃, 冨永 英一郎, 高松 潔, 堀口 文, 青木 大輔

    日本更年期医学会雑誌   15 ( Suppl. )   97 - 97   2007.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • ホルモン療法をいつまで行い、どういう形で終わらせるのがベターか? 当科更年期外来での実例からの一考察

    牧田 和也, 堀場 裕子, 平沢 晃, 冨永 英一郎, 高松 潔, 堀口 文, 青木 大輔

    日本更年期医学会雑誌   15 ( Suppl. )   109 - 109   2007.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 子宮体癌における高用量MPA療法の効果と再発危険因子の解析

    市川 義一, 進 伸幸, 鶴田 智彦, 末盛 友浩, 野村 弘行, 片岡 史夫, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 鈴木 淳, 青木 大輔

    日本癌治療学会誌   42 ( 2 )   506 - 506   2007.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 血管運動神経症状がSERM療法を選択する際に及ぼす影響についての基礎的検討(第3報) 閉経後骨量減少例のさらなる検証

    牧田 和也, 平沢 晃, 富永 英一郎, 堀口 文, 青木 大輔

    SERM: Selective Estrogen Receptor Modulator   ( 5 )   106 - 107   2007.8

     More details

    Language:Japanese   Publisher:(株)メディカルレビュー社  

    骨量減少と診断した症例を更に腰椎骨密度で細分類し、それぞれの血管運動神経症状による影響を比較検討した。10年間に、DXA法による腰椎骨密度値から骨量減少と診断され、かつ初診時に不定愁訴に関する調査を行った183例を対象とした。YMA 75%以上を骨量減少の軽度群、それ以下を高度群とした。もう一つの分類は、YMA 70%以上72%未満を骨粗鬆症予備軍、72%以上78%未満を真の骨量減少群、78%以上80%未満を正常近傍群とした。Hot flush、発汗ともに、重症率は骨量減少軽度群が高度群に比べて有意に高く、3群での検討では、骨粗鬆症予備軍が他の2群に比べて有意に低値であった。正常近傍群における重症率は、3群の中でも最も高値であった。

    researchmap

  • 再発子宮体癌に対するDP(docetaxel、cisplatin)療法の認容性および治療効果に関する検討

    市川 義一, 進 伸幸, 末盛 友浩, 野村 弘行, 平沢 晃, 玉田 裕, 冨永 英一郎, 阪埜 浩司, 鈴木 淳, 青木 大輔

    日本婦人科腫瘍学会雑誌   25 ( 3 )   236 - 236   2007.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 卵巣明細胞腺癌の基礎と臨床 HNF1B(hepatocyte nuclear factor-1β)の明細胞腺癌診断マーカーおよび予後関連因子としての有用性

    東口 敦司, 平沢 晃, 羽根 直美, 山上 亘, 野村 弘行, 冨永 英一郎, 鈴木 淳, 藤井 多久磨, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   25 ( 3 )   198 - 198   2007.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体癌の予後因子 再発子宮体癌における腫瘍マーカー測定の意義に関する検討

    鶴田 智彦, 進 伸幸, 市川 義一, 野村 弘行, 平沢 晃, 玉田 裕, 冨永 英一郎, 阪埜 浩司, 鈴木 淳, 青木 大輔

    日本婦人科腫瘍学会雑誌   25 ( 3 )   208 - 208   2007.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 卵巣癌細胞に発現するHMMC-1認識抗原がリンパ節転移能へ与える影響についての検討

    冨永 英一郎, 鈴木 淳, 鶴田 智彦, 末盛 友浩, 山上 亘, 東口 敦司, 野村 弘行, 平沢 晃, 進 伸幸, 青木 大輔

    日本婦人科腫瘍学会雑誌   25 ( 3 )   232 - 232   2007.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 日本人におけるBRCA1およびBRCA2遺伝子の全塩基配列直接解析法による基礎データ収集と、家族性乳がん、卵巣がんを対象とした易罹患性検査としての有用性に関する研究

    菅野 康吉, 安藤 二郎, 鎌田 裕之, 関口 勲, 生方 恵, 児玉 哲郎, 三木 義男, 新井 正美, 霞 富士雄, 平井 康雄, 池田 正, 神野 浩光, 北島 政樹, 青木 大輔, 平澤 晃, 野澤 志朗, 武田 祐子, 矢崎 久妙子, 福富 隆志, 吉田 輝彦, 恒松 隆一郎, 和泉 雅子, 梅澤 志乃, 中村 清吾, 矢形 寛, 小松 浩子, 有森 直子, 射場 典子, 権藤 延久, 横山 士郎, BRCA, 多施設共同研究グループ

    家族性腫瘍   7 ( 2 )   A42 - A42   2007.5

     More details

    Language:Japanese   Publisher:日本家族性腫瘍学会  

    researchmap

  • 癌診療における家族性腫瘍の位置付け 家族性腫瘍としての子宮体癌 その病態と臨床的特徴について

    阪埜 浩司, 進 伸幸, 平沢 晃, 山上 亘, 矢野倉 恵, 菅野 康吉, 三木 義男, 青木 大輔

    家族性腫瘍   7 ( 2 )   A28 - A28   2007.5

     More details

    Language:Japanese   Publisher:日本家族性腫瘍学会  

    researchmap

  • 子宮体癌における術前腫瘍マーカー測定の意義

    鶴田 智彦, 進 伸幸, 市川 義一, 末盛 友浩, 野村 弘行, 平沢 晃, 玉田 裕, 冨永 英一郎, 阪埜 浩司, 鈴木 淳, 青木 大輔, 吉村 泰典

    日本産科婦人科学会関東連合地方部会会報   44 ( 2 )   159 - 159   2007.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 研究参加によるBRCA1/2遺伝子検査を契機に家系内の受診・治療へとつなげられた一事例

    矢崎 久妙子, 武田 祐子, 菅野 康吉, 平沢 晃, 神野 浩光, 青木 大輔

    家族性腫瘍   7 ( 2 )   A39 - A39   2007.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 婦人科外来受診者を対象としたBRCA1/2遺伝子変異陽性例に関する検討

    平沢 晃, 菅野 康吉, 矢崎 久妙子, 武田 祐子, 鶴田 智彦, 阪埜 浩司, 進 伸幸, 青木 大輔

    家族性腫瘍   7 ( 2 )   A41 - A41   2007.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 当科更年期外来にて診断された閉経後骨粗鬆症/骨量減少例における血清脂質動態の検討

    牧田 和也, 富永 英一郎, 平沢 晃, 堀口 文, 青木 大輔

    Osteoporosis Japan   15 ( 2 )   288 - 288   2007.4

     More details

    Language:Japanese   Publisher:ライフサイエンス出版(株)  

    researchmap

  • 筋層浸潤の判定にTCRが有用であった子宮体癌の1例

    進 伸幸, 野村 弘行, 平沢 晃, 冨永 英一郎, 阪埜 浩司, 鈴木 淳, 福地 剛, 藤井 多久麿, 青木 大輔, 吉村 泰典

    日本産科婦人科内視鏡学会雑誌   22 ( 2 )   329 - 329   2007.3

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • 子宮体癌の大網転移に影響する臨床病理学的因子の検討

    市川 義一, 進 伸幸, 鶴田 智彦, 末盛 友浩, 東口 敦司, 野村 弘行, 平沢 晃, 玉田 裕, 阪埜 浩司, 鈴木 淳, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   59 ( 2 )   427 - 427   2007.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌における妊孕性温存高用量MPA療法の予後解析

    進 伸幸, 市川 義一, 末盛 友浩, 東口 敦司, 野村 弘行, 平沢 晃, 玉田 裕, 阪埜 浩司, 鈴木 淳, 塚崎 克己, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   59 ( 2 )   349 - 349   2007.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮頸癌におけるM期チェックポイント遺伝子CHFR異常メチル化の分子指標としての可能性

    矢野倉 恵, 阪埜 浩司, 進 伸幸, 桑原 佳子, 平尾 薫丸, 平沢 晃, 藤井 多久磨, 塚崎 克己, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   59 ( 2 )   363 - 363   2007.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • マイクロサテライト不安定性(MSI)陽性子宮体癌におけるフレームシフト変異標的遺伝子の解析

    阪埜 浩司, 矢野倉 恵, 進 伸幸, 桑原 佳子, 平沢 晃, 塚崎 克己, 菅野 康吉, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   59 ( 2 )   383 - 383   2007.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • COX-2発現量およびCD8陽性リンパ球数が進行期子宮体癌の予後に与える影響

    末盛 友浩, 進 伸幸, 矢野倉 恵, 市川 義一, 野村 弘行, 平沢 晃, 玉田 裕, 阪埜 浩司, 鈴木 淳, 塚崎 克己, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   59 ( 2 )   392 - 392   2007.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • ゲノム大領域遺伝子再構成検出ツールMLPA法を用いた卵巣癌における増幅遺伝子プロファイル検出の試み

    平沢 晃, 東口 敦司, 鶴田 智彦, 末盛 友浩, 市川 義一, 野村 弘行, 玉田 裕, 阪埜 浩司, 鈴木 淳, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   59 ( 2 )   393 - 393   2007.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 婦人科悪性腫瘍におけるHNF1B(hepatocyte nuclear factor-1β)の発現とその意義に関する検討

    東口 敦司, 平沢 晃, 鈴木 淳, 野村 弘行, 玉田 裕, 羽根 直美, 末盛 友浩, 市川 義一, 藤井 多久麿, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   59 ( 2 )   414 - 414   2007.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌における傍大動脈リンパ節転移に関わる危険因子および術中迅速病理診断の有用性に関する検討

    野村 弘行, 進 伸幸, 鶴田 智彦, 末盛 友浩, 市川 義一, 東口 敦司, 平沢 晃, 玉田 裕, 阪埜 浩司, 鈴木 淳, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   59 ( 2 )   426 - 426   2007.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 更年期に認められる女性ホルモンの低下が片頭痛患者に及ぼす影響についての検討

    牧田和也, 平沢晃, 青木大輔

    日本頭痛学会誌   34 ( 1 )   2007

  • 【卵巣癌の新しい予後因子とバイオマーカー】CGH法を用いた新しい予後因子やバイオマーカー探索 明細胞腺癌

    平沢 晃, 進 伸幸, 青木 大輔

    産婦人科の実際   55 ( 13 )   2185 - 2193   2006.12

     More details

    Language:Japanese   Publisher:金原出版(株)  

    researchmap

  • 当科更年期外来受診者に認められる慢性頭痛の頻度と機能性頭痛との関連に関する検討

    牧田 和也, 張簡 珮怡, 平沢 晃, 高松 潔, 堀口 文, 青木 大輔

    日本更年期医学会雑誌   14 ( Suppl. )   81 - 81   2006.10

     More details

    Language:Japanese   Publisher:(一社)日本女性医学学会  

    researchmap

  • 子宮頸癌におけるM期チェックポイント遺伝子CHFRの異常メチル化とタキサン製剤感受性との関連

    矢野倉 恵, 阪埜 浩司, 進 伸幸, 桑原 佳子, 平尾 薫丸, 平沢 晃, 藤井 多久磨, 塚崎 克己, 青木 大輔

    日本癌学会総会記事   65回   199 - 199   2006.9

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • 子宮体癌細胞株を用いた癌性腹膜炎モデルの確立と腹水産生亜株の樹立

    玉田 裕, 野村 弘行, 平沢 晃, 鈴木 淳, 進 伸幸, 青木 大輔

    日本癌学会総会記事   65回   312 - 312   2006.9

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • 血管運動神経症状がSERM療法を選択する際に及ぼす影響についての基礎的検討(第2報)

    牧田 和也, 平沢 晃, 堀口 文, 青木 大輔

    Osteoporosis Japan   14 ( Suppl.1 )   151 - 151   2006.9

     More details

    Language:Japanese   Publisher:ライフサイエンス出版(株)  

    researchmap

  • 子宮体癌の大網転移に影響する臨床病理学的因子の検討

    市川 義一, 進 伸幸, 末盛 友浩, 川口 牧子, 富田 明代, 平沢 晃, 玉田 裕, 阪埜 浩司, 鈴木 淳, 向井 萬起男, 青木 大輔

    日本癌治療学会誌   41 ( 2 )   400 - 400   2006.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 卵巣明細胞腺癌の細胞診用診断マーカーとしてのHNF1Bの有用性に関する検討

    東口 敦司, 鈴木 淳, 平沢 晃, 玉田 裕, 野村 弘行, 進 伸幸, 青木 大輔

    日本臨床細胞学会雑誌   45 ( Suppl.2 )   442 - 442   2006.9

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 子宮内膜病変の治療選択における2色FISH法の応用(VI.病理診断・治療への応用)

    進 伸幸, 野田 朋美, 平尾 健, 野村 弘行, 平沢 晃, 阪埜 浩司, 鈴木 淳, 青木 大輔

    組織細胞化学   2006   183 - 193   2006.7

     More details

    Language:Japanese   Publisher:日本組織細胞化学会  

    CiNii Article

    CiNii Books

    researchmap

  • 異型ポリープ状腺筋腫内に発生した類内膜腺癌6症例の診断・治療におけるTCRの有用性

    進 伸幸, 川口 牧子, 市川 義一, 末盛 友浩, 平沢 晃, 玉田 裕, 阪埜 浩司, 鈴木 淳, 青木 大輔, 吉村 泰典

    日本産科婦人科内視鏡学会雑誌   22 ( 1 )   147 - 147   2006.7

     More details

    Language:Japanese   Publisher:(一社)日本産科婦人科内視鏡学会  

    researchmap

  • 子宮癌における新たな予後因子 子宮体癌の予後因子としてのCOX-2発現および腫瘍内CD8陽性リンパ球数の意義

    末盛 友浩, 進 伸幸, 野田 朋美, 矢野倉 恵, 市川 義一, 平沢 晃, 玉田 裕, 阪埜 浩司, 鈴木 淳, 青木 大輔

    日本婦人科腫瘍学会雑誌   24 ( 3 )   231 - 231   2006.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 子宮体癌における妊孕性温存療法 子宮体癌における妊孕性温存高用量MPA(酢酸メドロキシプロゲステロン)療法の適応と安全性

    進 伸幸, 市川 義一, 末盛 友浩, 冨田 明代, 平沢 晃, 玉田 裕, 阪埜 浩, 鈴木 淳, 塚崎 克己, 青木 大輔

    日本婦人科腫瘍学会雑誌   24 ( 3 )   218 - 218   2006.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 卵巣癌化学療法におけるtaxane導入の効果に対する後方視的検討

    富田 明代, 鈴木 淳, 市川 義一, 末盛 友浩, 平沢 晃, 玉田 裕, 進 伸幸, 青木 大輔, 吉村 泰典

    日本産科婦人科学会関東連合地方部会会報   43 ( 2 )   171 - 171   2006.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 進行・再発子宮体癌に対するAP療法の完遂率および有害事象に関する検討

    市川 義一, 進 伸幸, 川口 牧子, 末盛 友浩, 富田 明代, 平沢 晃, 玉田 裕, 阪埜 浩司, 鈴木 淳, 青木 大輔, 吉村 泰典

    日本産科婦人科学会関東連合地方部会会報   43 ( 2 )   162 - 162   2006.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • P-102 アフィニティナノビーズによる抗癌剤結合蛋白質の同定・解析とその臨床応用への可能性(その他 3,一般演題・示説,第47回日本臨床細胞学会総会(春期大会))

    櫻井 信行, 鈴木 貴, 平沢 晃, 進 伸幸, 玉田 裕, 鈴木 淳, 塚崎 克己, 笹野 公伸, 半田 宏, 青木 大輔

    日本臨床細胞学会雑誌   45 ( 1 )   261 - 261   2006.3

     More details

    Language:Japanese   Publisher:特定非営利活動法人日本臨床細胞学会  

    CiNii Article

    researchmap

  • 臨床細胞学のNew Challenge Molecular Cytopathology 子宮体癌における癌関連遺伝子の異常メチル化とその分子指標としての可能性

    阪埜 浩司, 進 伸幸, 平尾 薫丸, 桑原 佳子, 川口 牧子, 平沢 晃, 塚崎 克己, 青木 大輔

    日本臨床細胞学会雑誌   45 ( Suppl.1 )   91 - 91   2006.3

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • NEU3(形質膜シアリダーゼ)発現は卵巣明細胞腺癌における腹膜播種形成に影響を与える

    野村 弘行, 玉田 裕, 平沢 晃, 鈴木 淳, 進 伸幸, 白石 悟, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   58 ( 2 )   622 - 622   2006.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 【産婦人科外来診療マニュアル】外陰白斑症,外陰癌

    平沢 晃, 青木 大輔

    産婦人科の世界   58 ( 特別増刊 )   135 - 137   2006.2

     More details

    Language:Japanese   Publisher:(有)医学の世界社  

    researchmap

  • 【産婦人科外来診療マニュアル】腫瘍マーカーによる卵巣腫瘍の診断

    平沢 晃, 青木 大輔

    産婦人科の世界   58 ( 特別増刊 )   128 - 131   2006.2

     More details

    Language:Japanese   Publisher:(有)医学の世界社  

    researchmap

  • CD151を介した細胞表面でのproMMP-7の活性化機構と子宮体癌の浸潤の検討

    片岡 史夫, 進 伸幸, 鈴木 淳, 玉田 裕, 平沢 晃, 岡田 保典, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   58 ( 2 )   401 - 401   2006.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 進行子宮体癌における新たな予後因子 CD8陽性cytotoxic lymphocyteとマイクロサテライト不安定性(MSI)

    進 伸幸, 平尾 健, 川口 牧子, 東口 敦司, 片岡 史夫, 平沢 晃, 玉田 裕, 阪埜 浩司, 鈴木 淳, 塚崎 克己, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   58 ( 2 )   463 - 463   2006.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 卵巣明細胞腺癌の予後関連バイオマーカーの網羅的探索

    平沢 晃, 進 伸幸, 東口 敦司, 片岡 史夫, 鈴木 淳, 井本 逸勢, 稲澤 譲治, 青木 大輔, 吉村 泰典

    日本産科婦人科学会雑誌   58 ( 2 )   621 - 621   2006.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 卵巣癌における組織型別予後因子の検討

    加藤 有美, 平沢 晃, 木村 奈央, 山本 阿紀子, 上野 和典, 石谷 健, 山下 博, 田中 淳, 新井 宏治

    日本癌治療学会誌   40 ( 2 )   537 - 537   2005.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 卵巣明細胞腺癌の臨床病理学的因子に関する検討

    加藤 有美, 平沢 晃, 木村 奈央, 山本 阿紀子, 上野 和典, 石谷 健, 山下 博, 田中 淳, 新井 宏治

    日本産科婦人科学会関東連合地方部会会報   42 ( 3 )   373 - 373   2005.8

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 臨床検査,診断に用いる腫瘍マーカー 婦人科腫瘍

    青木 大輔, 平沢 晃, 進 伸幸, 野澤 志朗

    癌と化学療法   32 ( 3 )   411 - 416   2005.3

     More details

    Language:Japanese   Publisher:(株)癌と化学療法社  

    産婦人科領域の悪性腫瘍には主なものとして卵巣癌,子宮頸癌,子宮体癌,絨毛癌などがある.卵巣癌は腹腔内に位置することから,治療前に厳密な意味での病理組織学的確定診断がほとんどの場合不可能であるために腫瘍マーカーのもつ意義は大きく,CA125をはじめ糖鎖抗原を中心とした多数の腫瘍マーカーが用いられている.婦人科癌のなかで最も多い子宮頸癌の約半数は早期癌の状態で発見されるものの,ある程度進行したものについては扁平上皮癌の腫瘍マーカーであるSCC抗原の測定が効果的である.また,子宮体癌については,特異性が高くしかも高陽性率を示す腫瘍マーカーは存在しないのが現状である.一方で,絨毛癌については妊娠数の減少や,胞状可胎が寛解に至るまでの厳重な一次管理が行われていることによりその数は激減したが,ヒト絨毛性ゴナドトロピン(human chorionic gonadotropin:hCG)というほぼ理想的な腫瘍マーカーが存在する(著者抄録)

    researchmap

    Other Link: https://search.jamas.or.jp/index.php?module=Default&action=Link&pub_year=2005&ichushi_jid=J00296&link_issn=&doc_id=20050317170021&doc_link_id=%2Fab8gtkrc%2F2005%2F003203%2F021%2F0411-0416%26dl%3D0&url=https%3A%2F%2Fwww.medicalonline.jp%2Fjamas.php%3FGoodsID%3D%2Fab8gtkrc%2F2005%2F003203%2F021%2F0411-0416%26dl%3D0&type=MedicalOnline&icon=https%3A%2F%2Fjk04.jamas.or.jp%2Ficon%2F00004_2.gif

  • GnRH agonist療法施行時のrisedronate併用投与における服薬コンプライアンスに関する検討

    石谷 健, 山本 阿紀子, 上野 和典, 平沢 晃, 山下 博, 田中 淳, 新井 宏治

    日本産科婦人科学会雑誌   57 ( 2 )   780 - 780   2005.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮内膜癌におけるp16INK4aメチル化異常の解析

    矢野倉 恵, 阪埜 浩司, 平尾 健, 平尾 薫丸, 平沢 晃, 進 伸幸, 青木 大輔, 野澤 志朗

    日本癌学会総会記事   63回   177 - 177   2004.9

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • 子宮内膜発癌過程における癌抑制遺伝子メチル化異常の関与

    阪埜 浩司, 矢野倉 恵, 平尾 健, 平尾 薫丸, 平沢 晃, 進 伸幸, 青木 大輔, 野澤 志朗

    日本癌治療学会誌   39 ( 2 )   734 - 734   2004.9

     More details

    Language:Japanese   Publisher:(一社)日本癌治療学会  

    researchmap

  • 家系内癌集積傾向を示す子宮体癌症例におけるMMR遺伝子生殖細胞変異の解析

    阪埜 浩司, 矢野倉 恵, 平尾 健, 平沢 晃, 進 伸幸, 青木 大輔, 武田 祐子, 菅野 康吉, 三木 義男, 野澤 志朗

    家族性腫瘍   4 ( 2 )   A29 - A29   2004.5

     More details

    Language:Japanese   Publisher:日本家族性腫瘍学会  

    researchmap

  • 【がんゲノム学】がんゲノム増幅領域と原因遺伝子

    平沢 晃, 稲澤 譲治

    血液・腫瘍科   48 ( 2 )   175 - 181   2004.2

     More details

    Language:Japanese   Publisher:(有)科学評論社  

    researchmap

  • 悪性黒色腫細胞株におけるWild-Type BRAF高発現の意義

    田波 秀朗, 井本 逸勢, 平沢 晃, 柚木 泰広, 園田 格, 井上 純, 安居 幸一郎, 河上 裕, 稲澤 譲治

    日本癌学会総会記事   62回   194 - 194   2003.8

     More details

    Language:Japanese   Publisher:日本癌学会  

    researchmap

  • 遺伝性腫瘍としての子宮内膜癌の頻度と病態に関する解析

    阪埜 浩司, 進 伸幸, 平尾 健, 岩田 卓, 平沢 晃, 青木 大輔, 菅野 康吉, 野澤 志朗

    日本癌学会総会記事   62回   351 - 351   2003.8

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • hMSH6にmissense変異(R300P)を認めたatypical HNPCC家系の1例

    権田 憲士, 山内 絵里, 市川 明, 深山 紀子, 平沢 晃, 松井 孝至, 固武 健二郎, 小山 靖夫, 野水 整, 竹之下 誠一, 菅野 康吉

    日本癌学会総会記事   62回   193 - 193   2003.8

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • 子宮体癌におけるhMLH1遺伝子プロモーター領域のメチル化プロファイルの検討

    平沢 晃, 菅野 康吉, 宮倉 安幸, 阪埜 浩司, 進 伸幸, 青木 大輔, 野澤 志朗, 坂本 優, 五十嵐 誠治

    日本癌学会総会記事   62回   282 - 282   2003.8

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • 17q増幅標的遺伝子PPM1Dの発現と卵巣明細胞癌

    斎藤 深美子[小原], 平沢 晃, 津田 均, 井本 逸勢, 青木 大輔, 進 伸幸, 野澤 志朗, 稲澤 譲治

    日本癌学会総会記事   62回   350 - 350   2003.8

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • CGH法を用いた卵巣明細胞腺癌ゲノム異常の網羅的解析と標的遺伝子の探索

    平沢 晃, 青木 大輔, 進 伸幸, 井本 逸勢, 稲澤 譲治, 野澤 志朗

    日本婦人科腫瘍学会雑誌   21 ( 3 )   189 - 189   2003.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • hMSH6にmissense変異(R300P)を認めたatypical HNPCC家系の1例

    権田 憲士, 山内 絵里, 市川 明, 深山 紀子, 平沢 晃, 松井 孝至, 固武 健二郎, 小山 靖夫, 野水 整, 竹之下 誠一, 菅野 康吉

    家族性腫瘍   3 ( 2 )   A33 - A33   2003.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 遺伝性腫瘍としての子宮内膜癌の頻度と病態に関する解析

    阪埜 浩司, 進 伸幸, 平尾 健, 岩田 卓, 平沢 晃, 青木 大輔, 菅野 康吉, 野澤 志朗

    家族性腫瘍   3 ( 2 )   A31 - A31   2003.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 子宮体癌におけるマイクロサテライト不安定性とhMLH1プロモーター領域のメチル化に関する検討

    平沢 晃, 菅野 康吉, 宮倉 安幸, 山内 絵里, 市川 明, 阪埜 浩司, 進 伸幸, 青木 大輔, 野澤 志朗, 小屋松 安子, 坂本 優, 関口 勲, 鎌田 裕之, 五十嵐 誠治

    家族性腫瘍   3 ( 2 )   A31 - A31   2003.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 遺伝子子宮内膜癌の病態に関する分子疫学的検討

    阪埜 浩司, 進 伸幸, 平尾 健, 鈴木 直, 平沢 晃, 岩田 卓, 青木 大輔, 菅野 康吉, 宇田川 康博, 吉村 泰典, 野澤 志朗

    日本産科婦人科学会雑誌   55 ( 2 )   186 - 186   2003.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 悪性黒色腫細胞株のCGH解析による新規癌関連遺伝子の同定

    田波 秀朗, 平沢 晃, 井本 逸勢, 園田 格, 柚木 泰広, 井上 純, 岩井 武尚, 杉原 健一, 河上 裕, 稲澤 譲治

    日本癌学会総会記事   61回   293 - 293   2002.10

     More details

    Language:Japanese   Publisher:日本癌学会  

    researchmap

  • 卵巣明細胞腺癌の悪性形質獲得にかかわるゲノムコピー数異常とその標的遺伝子の探索

    平沢 晃, 井本 逸勢, 斎藤 深美子[小原], 青木 大輔, 進 伸幸, 野澤 士朗, 稲澤 譲治

    日本癌学会総会記事   61回   293 - 293   2002.10

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • 11q22増幅標的遺伝子cIAP1発現の子宮頸部扁平上皮癌の放射線感受性に及ぼす意義

    井本 逸勢, 津田 均, 平沢 晃, 三浦 雅彦, 坂本 優, 広橋 説雄, 稲澤 譲治

    日本癌学会総会記事   61回   99 - 99   2002.10

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • 高用量黄体ホルモン療法中の体癌症例における染色体変化 2色FISH法による核異型度判定の試み

    進 伸幸, 金杉 優, 瀬藤 江里, 内藤 恵美, 東口 敦司, 片岡 史夫, 平沢 晃, 鈴木 直, 青木 大輔, 野澤 志朗

    日本婦人科腫瘍学会雑誌   20 ( 3 )   364 - 364   2002.6

     More details

    Language:Japanese   Publisher:(公社)日本婦人科腫瘍学会  

    researchmap

  • 若年体癌83例における家族内癌集積性と臨床病理学的特徴の関連

    進 伸幸, 山上 亘, 青木 大輔, 平沢 晃, 金杉 優, 瀬藤 江里, 阪埜 浩司, 吉村 泰典, 野澤 志朗

    日本産科婦人科学会雑誌   54 ( 2 )   400 - 400   2002.2

  • 子宮体癌におけるゲノム不安定性と臨床病理学的因子との関連性についての検討

    平沢 晃, 青木 大輔, 進 伸幸, 阪埜 浩司, 井本 逸勢, 稲澤 譲治, 吉村 泰典, 野澤 志朗

    日本産科婦人科学会雑誌   54 ( 2 )   326 - 326   2002.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 子宮体癌組織における染色体不安定性及びマイクロサテライト不安定性の検討

    平沢 晃, 井本 逸勢, 青木 大輔, 進 伸幸, 野澤 志朗, 稲澤 譲治

    日本癌学会総会記事   60回   403 - 403   2001.9

     More details

    Language:Japanese   Publisher:(一社)日本癌学会  

    researchmap

  • 当院における若年性体癌83例の臨床病理学的検討

    山上 亘, 進 伸幸, 青木 大輔, 阪埜 浩二, 金杉 優, 平沢 晃, 瀬藤 江里, 片岡 史夫, 鈴木 直, 吉村 泰典

    日本産科婦人科学会関東連合地方部会会報   38 ( 3 )   318 - 318   2001.8

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 子宮体部腫瘍外来で発見された家族内癌集積を示す3症例の解析

    阪埜 浩司, 二河田 雅信, 平沢 晃, 金杉 優, 進 伸幸, 青木 大輔, 宇田川 康博, 菅野 康吉, 野澤 志朗

    家族性腫瘍   1 ( 2 )   A40 - A40   2001.5

     More details

    Language:Japanese   Publisher:(一社)日本遺伝性腫瘍学会  

    researchmap

  • 子宮体癌における抗癌剤感受性試験に関する検討

    金杉 優, 青木 大輔, 平沢 晃, 瀬藤 江里, 中田 さくら, 鈴木 直, 進 伸幸, 野澤 志朗

    日本臨床細胞学会雑誌   40 ( Suppl.1 )   170 - 170   2001.3

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 91 TGFβ1によって誘導されるPAI-1と卵巣明細胞腺癌の生物学的特性との関連

    小宮山 慎一, 青木 大輔, 平沢 晃, 片岡 史夫, 進 伸幸, 三上 幹男, 吉村 [ヤス]典, 野澤 志朗

    日本産科婦人科學會雜誌   53 ( 2 )   255 - 255   2001.2

     More details

    Language:Japanese   Publisher:社団法人日本産科婦人科学会  

    CiNii Article

    researchmap

  • 子宮体癌における第1,第17染色体の数的,構造的異常の検索 2色FISH法,モノレイヤー標本作製法(ThinPrep法)を用いて

    進 伸幸, 青木 大輔, 金杉 優, 瀬藤 江里, 平沢 晃, 片岡 史夫, 鈴木 直, 吉村 泰典, 野澤 志朗, 津田 均

    日本産科婦人科学会雑誌   53 ( 2 )   477 - 477   2001.2

  • 表層上皮性卵巣癌I期におけるTGFβレセプターII型発現の特徴

    冨永 英一郎, 青木 大輔, 小宮山 慎一, 平沢 晃, 金杉 優, 進 伸幸, 野澤 志朗

    日本臨床電子顕微鏡学会誌   33 ( 増刊 )   S97 - S97   2000.8

     More details

    Language:Japanese   Publisher:日本臨床分子形態学会  

    researchmap

  • 卵巣癌症例の後腹膜リンパ節転移の検討 組織型と分化度との関連を中心に

    平沢 晃, 進 伸幸, 青木 大輔, 小宮山 慎一, 金杉 優, 冨永 英一郎, 吉村 泰典, 野澤 志朗

    日本産科婦人科学会関東連合地方部会会報   37 ( 2 )   180 - 180   2000.5

     More details

    Language:Japanese   Publisher:(一社)関東連合産科婦人科学会  

    researchmap

  • 82 卵巣癌I期症例における腹水細胞診の判定と予後に関する検討

    平沢 晃, 青木 大輔, 小宮山 慎一, 玉田 裕, 冨永 英一郎, 進 伸幸, 野澤 志朗

    日本臨床細胞学会雑誌   39 ( 1 )   122 - 122   2000.3

     More details

    Language:Japanese   Publisher:特定非営利活動法人日本臨床細胞学会  

    CiNii Article

    researchmap

  • P-71 卵巣癌における第1および第17染色体の数的構造的異常 : 2色FISH法を用いた検索

    進 伸幸, 津田 均, 青木 大輔, 小宮山 慎一, 冨永 英一郎, 平澤 晃, 宇田川 康博, 吉村 泰典, 野澤 志朗

    日本産科婦人科學會雜誌   52 ( 2 )   "396(S - 320)"   2000.2

     More details

    Language:Japanese   Publisher:社団法人日本産科婦人科学会  

    CiNii Article

    CiNii Books

    researchmap

  • 270 卵巣明細胞腺癌におけるTGF-β1およびTGF-β1レセプターII型に関する免疫組織化学的検討

    平沢 晃, 青木 大輔, 小宮山 慎一, 冨永 英一郎, 進 伸幸, 宇田川 康博, 野澤 志朗

    日本臨床細胞学会雑誌   38 ( 1 )   222 - 222   1999.3

     More details

    Language:Japanese   Publisher:特定非営利活動法人日本臨床細胞学会  

    CiNii Article

    researchmap

  • P-136 卵巣明細胞腺癌におけるTGFβレセプター発現の動向 : 子宮内膜症との相互作用に関連して

    小宮山 慎一, 青木 大輔, 平沢 晃, 進 伸幸, 飯田 俊彦, 宇田川 康博, 吉村 泰典, 野澤 志朗

    日本産科婦人科學會雜誌   51 ( 0 )   "S - 427"   1999.2

     More details

    Language:Japanese   Publisher:社団法人日本産科婦人科学会  

    CiNii Article

    researchmap

  • 子宮体癌に特異的に出現する糖鎖の発現機構におけるフコース転移酵素の関与について

    冨永 英一郎, 青木 大輔, 平沢 晃, 瀬藤 江里, 進 伸幸, 宇田川 康博, 吉村 泰典, 野澤 志朗

    日本産科婦人科学会雑誌   51 ( 臨増 )   S367 - S367   1999.2

     More details

    Language:Japanese   Publisher:(公社)日本産科婦人科学会  

    researchmap

  • 264 子宮頸部に発生した絨毛癌の1例

    佐々木 宏輔, 北岡 芳久, 平沢 晃, 大谷 美雄, 杉江 和明

    日本臨床細胞学会雑誌   37 ( 1 )   221 - 221   1998.3

     More details

    Language:Japanese   Publisher:特定非営利活動法人日本臨床細胞学会  

    CiNii Article

    CiNii Books

    researchmap

  • 当院における最近6年間の子宮体癌症例の予後因子について

    平沢 晃, 進 伸幸, 古宮 京子, 堺 正長, 新井 宏治

    埼玉県医学会雑誌   32 ( 8 )   1130 - 1130   1998.3

     More details

    Language:Japanese   Publisher:埼玉県医学会  

    researchmap

  • 細胞診で横紋構造を呈する腫瘍細胞を認めた子宮体部異所性癌肉腫の1例

    平沢 晃

    日本臨床細胞学会雑誌   37 ( 補冊1 )   283 - 283   1998.3

     More details

    Language:Japanese   Publisher:(公社)日本臨床細胞学会  

    researchmap

  • 当科における十代の妊娠・分娩に関する検討

    平沢 晃

    日赤医学   49 ( 1 )   87 - 87   1997.10

     More details

    Language:Japanese   Publisher:日本赤十字社医学会  

    researchmap

▼display all

Presentations

  • がんゲノム医療における生殖細胞系列の遺伝情報 がんゲノム医療と臨床薬理学.

    平沢 晃

    第42回日本臨床薬理学会学術総会 

     More details

    Event date: 2021.12.9 - 2021.12.11

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • がんゲノム医療における保険収載にかかる課題 がんゲノム診療に関わる諸問題:遺伝子検査から遺伝子診療へ

    平沢 晃

    第42回日本臨床薬理学会学術総会 

     More details

    Event date: 2021.12.9 - 2021.12.11

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • 遺伝性腫瘍

    平沢 晃

    第60回日本臨床細胞学会秋期大会 

     More details

    Event date: 2021.11.20 - 2021.11.21

    Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • OncoGuide NCCオンコパネルシステムの改定に伴う二次的所見開示推奨度に関するアンケート調査

    小杉 眞司, 平沢 晃, 矢部 一郎, 多田 寛, 桑田 健, 植木 有紗, 織田 克利, 平田 真, 東川 智美, 久島 周, 金井 雅史, 佐藤 友紀, 加藤 芙美乃, 小川 昌宣, 福田 博政

    日本人類遺伝学会第66回大会・第28回日本遺伝子診療学会大会 

     More details

    Event date: 2021.10.13 - 2021.10.16

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • 本邦の遺伝性乳癌卵巣癌症候群(HBOC)診療の課題点 ~婦人科がん治療医の実態調査から見えてきたこと~

    小林 佑介, 増田 健太, 平沢 晃, 竹原 和宏, 津田 均, 渡部 洋, 織田 克利, 永瀬 智, 万代 昌紀, 岡本 愛光, 八重樫 伸生, 三上 幹男, 榎本 隆之, 青木 大輔

    日本人類遺伝学会第66回大会・第28回日本遺伝子診療学会大会(シンポジウム) 

     More details

    Event date: 2021.10.13 - 2021.10.16

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • 遺伝情報の診療録における取り扱いに関するアンケート調査から見えた課題

    浦川 優作, 二川 摩周, 十川 麗美, 加藤 芙美乃, 植野 さやか, 河内 麻里子, 山本 英喜, 平沢 晃

    日本人類遺伝学会第66回大会・第28回日本遺伝子診療学会大会 

     More details

    Event date: 2021.10.13 - 2021.10.16

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • がん遺伝子パネル検査でATMのPresumed Germline Pathogenic Variant(PGPV) が検出された3例.

    加藤 芙美乃, 山本 英喜, 十川 麗美, 二川 摩周, 浦川 優作, 植野 さやか, 河内 麻里子, 遠西 大輔, 冨田 秀太, 平沢 晃

    日本人類遺伝学会第66回大会・第28回日本遺伝子診療学会大会 

     More details

    Event date: 2021.10.13 - 2021.10.16

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • 令和4年度診療報酬改定に向けた課題と取組み(悪性腫瘍領域)

    平沢 晃

    日本人類遺伝学会第66回大会・第28回日本遺伝子診療学会大会 

     More details

    Event date: 2021.10.13 - 2021.10.16

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • Double heterozygoteとしてBRCA1/2 のgermline pathogenic variants(GPV)を認めた卵巣癌の1例

    二川 摩周, 河内 麻里子, 十川 麗美, 加藤 芙美乃, 浦川 優作, 山本 英喜, 平沢 晃

    日本人類遺伝学会第66回大会・第28回日本遺伝子診療学会大会 

     More details

    Event date: 2021.10.13 - 2021.10.16

    Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • がんゲノム医療で見つかるPGPVsの特徴.

    十川麗美, 山本英喜, 河内 麻里子, 二川摩周, 浦川優作, 遠西大輔, 冨田秀太, 平沢 晃

    第80回日本癌学会学術総会 

     More details

    Event date: 2021.9.30 - 2021.10.2

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 遺伝情報の診療録の取り扱いに関する課題

    浦川優作, 二川摩周, 十川麗美, 加藤 芙美乃, 植野 さやか, 河内 麻里子, 山本 英喜, 平沢 晃

    第80回日本癌学会学術総会 

     More details

    Event date: 2021.9.30 - 2021.10.2

    Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • 認定遺伝カウンセラーからみた遺伝性腫瘍を有する患者・家族へのサポート体制 Invited

    二川摩周, 浦川優作, 十川麗美, 河内 麻里子, 山本英喜, 平沢 晃

    第80回日本癌学会学術総会 

     More details

    Event date: 2021.9.30 - 2021.10.2

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • Predisposing germline variants in ovarian cancer. Invited

    Hirasawa A

    International Society of Precision Cancer Medicine (ISPCM) 2021 

     More details

    Event date: 2021.9.25 - 2021.9.26

    Language:English   Presentation type:Oral presentation (invited, special)  

    researchmap

  • 婦人科がんゲノム医療

    平沢 晃

    第73回中国四国産科婦人科学会  2021.9.18 

     More details

    Event date: 2021.9.18 - 2021.9.19

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    researchmap

  • 遺伝性腫瘍に関わるコンパニオン診断の現状と今後の課題

    平沢 晃

    第45回日本遺伝カウンセリング学会学術集会 2021.7.2-4(web) 

     More details

    Event date: 2021.7.2 - 2021.7.4

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • 婦人科におけるHBOC診療の現状と課題. Invited

    平沢 晃

    第149回東北連合産科婦人科学会学術講演会(教育セミナー) 

     More details

    Event date: 2021.6.12 - 2021.6.13

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    researchmap

  • Prospective Cohort Study and Biobanking with Japanese BRCA1/2 Pathogenic Variant Carriers by the Japanese Gynecologic Oncology Group (JGOG) (JGOG3024)

    Hirasawa A, Futagawa M, Ogawa C, Aoki D, Imoto I, Matsuo K, Tsuda H, Minegishi N, Shimada M, Enomoto T

     More details

    Event date: 2021.5.4 - 2021.5.7

    Language:English  

    researchmap

  • がんゲノム医療に順応する細胞診検査態勢 〜Rapid on-site evaluation:ROSEへの対応〜

    井上博文, 松岡博美, 實平悦子, 松岡昌志, 冨田秀太, 平沢 晃, 柳井広之

    第59回日本臨床細胞学会秋期大会 

     More details

    Event date: 2020.11.21 - 2020.11.22

    researchmap

  • がんゲノム医療外来で遺伝性腫瘍が疑われた症例に関する課題と検討.

    十川麗美, 河内麻里子, 二川摩周, 加藤芙美乃, 蓮岡佳代子, 浦川優作, 坂井美佳, 山本英喜, 遠西大輔, 冨田秀太, 平沢晃

    日本人類遺伝学会第65回大会 

     More details

    Event date: 2020.11.18 - 2020.11.21

    researchmap

  • 保険収載されたがん遺伝子パネル検査における実施状況と, 生殖細胞系列バリアントへの対応状況に関する現状調査と課題提起

    小林明理, 山田崇弘, 吉岡正博, 近藤知大, 金井雅史, 木下一郎, 青木洋子, 織田克利, 植木有紗, 森川真紀, 佐藤友紀, 小川昌宣, 東川智美, 武藤学, 平沢晃, 小杉眞司

    日本人類遺伝学会第65回大会 

     More details

    Event date: 2020.11.18 - 2020.11.21

    researchmap

  • BRCA1/2, PALB2, ATM病的バリアント保持者における膵病変とそのサーベイランス.

    阿部紘大, 植木有紗, 浦川優作, 北郷実, 吉浜智子, 南木佳子, 北川雄光, 青木大輔, 小崎健次郎, 平沢晃

    日本人類遺伝学会第65回大会 

     More details

    Event date: 2020.11.18 - 2020.11.21

    researchmap

  • 国内バイオバンクに関する利活用ハンドブックの作成を通じたゲノム研究開発活性化の試み.

    甲畑宏子, 長神風二, 武藤香織, 飯田香緒里, 秦 健一郎, 田中敏博, 丸山英二, 平沢 晃, 信國宇洋, 相澤弥生, 長谷川冬雪, 宮原麗子, 竹本 暁, 川澄みゆり, 木村恵子, 吉田雅幸

    日本人類遺伝学会第65回大会 

     More details

    Event date: 2020.11.18 - 2020.11.21

    researchmap

  • FoundationOne CDxから病的意義不明として検出されるバリアントに対する病的意義の再検討

    二川摩周, 浦川優作, 十川麗美, 加藤芙美乃, 坂井美佳, 河内麻里子, 山本英喜, 冨田秀太, 平沢晃

    日本人類遺伝学会第65回大会 

     More details

    Event date: 2020.11.18 - 2020.11.21

    researchmap

  • 血清ALP異常高値から発見されたMEN1異所性副甲状腺機能亢進症の1例

    大塚勇輝, 西村義人, 原田洸, 岡浩介, 長谷川功, 小川弘子, 三好智子, 花山宜久, 枝園忠彦, 平沢 晃, 大塚文男

    第30回臨床内分泌代謝Update 

     More details

    Event date: 2020.11.13 - 2020.11.14

    researchmap

  • Cancer precision medicine and germline variants in gynecologic tumors. Invited

    2020.10.24 

     More details

    Event date: 2020.10.24

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    researchmap

  • がん遺伝子パネル検査におけるgermline findingsの頻度と遺伝学的診療への導入. Invited

    植木有紗, 三須久美子, 中村康平, 長妻晶子, 四十物絵理子, 今井美穂, 林 秀行, 持田かおり, 藤倉知花, 谷嶋成樹, 平沢 晃, 菅野康吉, 西原広史

    第58回日本癌治療学会学術集会 

     More details

    Event date: 2020.10.22 - 2020.10.24

    Language:Japanese  

    researchmap

  • がんゲノム医療におけるCRCの取り組みと役割.

    宮本理史, 奥田浩人, 武田達明, 難波志穂子, 黒田 智, 平沢 晃, 千堂年昭, 四方賢一

    第20回CRCと臨床試験のあり方を考える会議 

     More details

    Event date: 2020.10.3 - 2020.10.4

    researchmap

  • がん遺伝子パネル検査を施行した乳癌症例のGermline findingsに関する検討.

    河内麻里子, 山本英喜, 坂井美佳, 梶原友記子, 笹原麻子, 十川麗美, 二川摩周, 浦川 優作, 岩本高行, 枝園忠彦, 平 成人, 土井原 博義, 平沢 晃

    第26回日本遺伝性腫瘍学会学術集会 

     More details

    Event date: 2020.8.21 - 2020.8.31

    researchmap

  • 遺伝性乳がん卵巣がん診療の課題.

    坂井美佳, 岡村弥妃, 松山裕美, 横山貴紀, 藤本悦子, 山本弥寿子, 大亀真一, 小林成行, 堀 伸一郎, 大住省三, 平沢 晃, 竹原和宏

    第26回日本遺伝性腫瘍学会学術集会 

     More details

    Event date: 2020.8.21 - 2020.8.31

    researchmap

  • 家族歴と血縁者のMSI-High大腸癌からLynch症候群を疑いMLH1がVUSであった大腸癌・乳癌の重複癌の1例.

    梶原友紀子, 枝園忠彦, 藤原みわ, 鈴木陽子, 鳩野みなみ, 笹原麻子, 十川麗美, 二川摩周, 浦川優作, 河内麻里子, 山本英喜, 岩本高行, 平成人, 平沢晃, 土井原博義

    第26回日本遺伝性腫瘍学会学術集会 

     More details

    Event date: 2020.8.21 - 2020.8.31

    researchmap

  • AYA世代発症の肉腫・希少がんに対するがん遺伝子プロファイリング検査の意義.

    山本英喜, 河内麻里子, 十川麗美, 二川摩周, 浦川優作, 井上博文, 遠西大輔, 久保寿夫, 中田英二, 田端雅弘, 亀田雅博, 黒住和彦, 柳井広之, 嶋田 明, 平沢 晃

    第26回日本遺伝性腫瘍学会学術集会 

     More details

    Event date: 2020.8.21 - 2020.8.31

    researchmap

  • ゲノム医療における二次的所見の取り扱いに関する実態調査 –遺伝医療専門家を対象とした質問票調査より倫理問題検討委員会報告–

    土屋実央, 山田崇弘, 赤石理奈, 井本逸勢, 梅村啓史, 清水健司, 浜之上はるか, 平沢晃, 吉田晶子, 吉橋博史, 四元淳子, 渡辺淳, 小杉眞司

    第44回日本遺伝カウンセリング学会学術集会 2020 

     More details

    Event date: 2020.7.3 - 2020.7.5

    researchmap

  • がんゲノム医療と遺伝性腫瘍.

    平沢 晃

    第72回日本産科婦人科学会学術講演会(生涯教育セミナー) 

     More details

    Event date: 2020.4.23 - 2020.4.28

    Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • Primary tissue ovarian cancer organoids capturing histological and genetical features of the original tumor and applications in drug resistance and sensitivity testing

    Nanki Y, Chiyoda T, Hirasawa A, Akahane T, Yamagami W, Kataoka F, Tanaka M, Aoki D

    第72回日本産科婦人科学会学術講演会 

     More details

    Event date: 2020.4.22 - 2020.4.28

    researchmap

  • Genome-Based Medicine: Hereditary tumors. Invited

    The 26th Asia and Oceania Federation of Obstetrics and Gynecology (AOFOG) Congress.  2019.11.14 

     More details

    Event date: 2019.11.10 - 2019.11.14

    Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • Utility of plasma circulating tumor DNA in ovarian cancer monitoring.

    The 6th Biennial Meeting of Asian Society of Gynecologic Oncology 

     More details

    Event date: 2019.10.10 - 2019.10.12

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • 生殖細胞系列の遺伝子パネル検査をうけた,家族性の乳癌,卵巣癌が疑われた27例の検討.

    千代田達幸, 吉浜智子, 早乙女啓子, 同前 愛, 南木佳子, 平野卓朗, 小林佑介, 山上 亘, 野村弘行, 片岡史夫, 植木有紗, 平沢 晃, 青木大輔

    第61回日本婦人科腫瘍学会学術講演会 

     More details

    Event date: 2019.7.4 - 2019.7.6

    researchmap

  • がんクリニカルシークエンスと生殖細胞系列バリアントへの対応.

    平沢 晃

    第61回日本婦人科腫瘍学会学術講演会(シンポジウム) 

     More details

    Event date: 2019.7.4 - 2019.7.6

    Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • Germline pathogenic variants of cancer susceptibility genes among Japanese ovarian cancer patients.

    Hirasawa A, Imoto I, Naruto T, Akahane T, Yamagami W, Nomura H, Masuda K, Susumu N, Tsuda H, Aoki D

    European Human Genetics Conference 2019 

     More details

    Event date: 2019.6.15 - 2019.6.18

    Presentation type:Poster presentation  

    researchmap

  • Plasma circulating tumor DNA as a genomic biomarker for ovarian cancer.

    Nanki Y, George A, Chen Y, Brueffer C, Chiyoda T, Akahane T, Hirasawa A, Aoki D, Saal L

    European Human Genetics Conference 2019 

     More details

    Event date: 2019.6.15 - 2019.6.18

    Presentation type:Poster presentation  

    researchmap

  • 遺伝性腫瘍の実地診療における課題.

    平沢 晃

    第25回日本家族性腫瘍学会学術集会 

     More details

    Event date: 2019.6.14 - 2019.6.15

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • ADAM9のヒト卵巣明細胞癌での発現とシスプラチン誘導性癌細胞死抑制作用.

    上野万里, 潮見隆之, 望月早月, 下田将之, 金井弥栄, 片岡史夫, 平沢 晃, 進 伸幸, 青木大輔, 岡田 保典

    第108回日本病理学会総会 

     More details

    Event date: 2019.5.9 - 2019.5.11

    researchmap

  • 若年性子宮体がん症例における妊孕性温存治療適応診断マーカーの開発.

    平野卓朗, 新井恵吏, 真壁 健, 平沢 晃, 山上 亘, 進 伸幸, 青木大輔, 金井弥栄

    第108回日本病理学会総会 

     More details

    Event date: 2019.5.9 - 2019.5.11

    researchmap

  • Circulating tumor DNA as a novel biomarker for ovarian cancer monitoring.

    Nanki Y, Hirasawa A, Chen Y, George AM, Akahane T, Chiyoda T, Nomura H, Saal LH, Tanaka M, Aoki D

    第71回日本産科婦人科学会学術講演会 

     More details

    Event date: 2019.4.11 - 2019.4.14

    researchmap

  • Clinical implementation of precision systems oncology in the treatment of ovarian cancer based on ex-vivo drug testing and molecular profiling.

    Murumägi A, Ungureanu D, Khan S, Hirasawa A, Arjama1 M, Välineva1 K, Mikkonen P, Niininen W, Kumar A, Pellinen T, Pietiäinen1 V, Mägi A, Koivisto-Korander R, Tapper J, Loukovaara M, Aittokallio T, Bützow R, Kallioniemi O

    AACR annual meeting 2019 

     More details

    Event date: 2019.3.29 - 2019.4.3

    Presentation type:Poster presentation  

    researchmap

  • Genetic variants of hereditary tumors with ovarian cancer patients in Japanese. Invited

    Hirasawa A

    3rd meeting of ineternatnational society for precision Cancer Medicine 

     More details

    Event date: 2019.3.12 - 2019.3.15

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • 「細胞」からのプレシジョンメディシン. Invited

    平沢 晃, 青木大輔

    第57回日本臨床細胞学会秋期大会 

     More details

    Event date: 2018.11.17 - 2018.11.18

    Presentation type:Oral presentation (keynote)  

    researchmap

  • がんゲノム医療と遺伝子医療部門.

    平沢 晃

    第16回全国遺伝子医療部門連絡会議 

     More details

    Event date: 2018.11.13 - 2018.11.14

    Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • がん遺伝子パネル検査由来の二次的所見とバリアント保持者のマネージメント.

    早乙女啓子, 平沢 晃, 西原広史, 野村弘行, 赤羽智子, 植木有紗, 谷嶋成樹, 高石官均, 青木大輔

    第56回日本癌治療学会学術集会 

     More details

    Event date: 2018.10.20

    Presentation type:Oral presentation (general)  

    researchmap

  • 子宮体癌および子宮内膜異型増殖症に対するMPA療法の治療予後予測因子の検討.

    坂井健良, 山上 亘, 平野卓朗, 真壁 健, 二宮委美, 千代田達幸, 野村弘行, 片岡史夫, 平沢 晃, 阪埜浩司, 進 伸幸, 青木大輔

    第56回日本癌治療学会学術集会 

     More details

    Event date: 2018.10.18 - 2018.10.20

    Presentation type:Oral presentation (general)  

    researchmap

  • Clinical sequencing in cancers and hereditary tumors. Invited

    平沢 晃

    日本人類遺伝学会第63回大会 

     More details

    Event date: 2018.10.10 - 2018.10.13

    Language:English   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • 乳癌既往歴があり耳下腺癌を発症したBRCA1 germline pathogenic variant 保持者の1例.

    赤羽智子, 平沢 晃, 片岡史夫, 野村弘行, 山下年成, 羽田恵梨, 亀山香織, 小崎健次郎, 青木大輔

    日本人類遺伝学会第63回大会 

     More details

    Event date: 2018.10.10 - 2018.10.13

    Presentation type:Poster presentation  

    researchmap

  • 子宮体癌に対するセンチネルリンパ節(SN)マッピングの結果を踏まえた当院のSNナビゲーション手術戦略. Invited

    真壁 健, 山上 亘, 片岡史夫, 平野卓朗, 坂井健良, 二宮委美, 平沢 晃, 阪埜浩司, 進 伸幸, 青木大輔

    第20回SNNS研究会学術集会 

     More details

    Event date: 2018.10.10 - 2018.10.11

    Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • Recent topics of clinical trials on endometrial cancer in Japan. Invited

    Nomura H, Yamagami W, Hirasawa A, Aoki D

    第60回日本婦人科腫瘍学会学術講演会 

     More details

    Event date: 2018.9.14 - 2018.9.16

    Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • 頸管浸潤を伴う子宮体癌が疑われたが子宮鏡下手術にて子宮温存可能と診断された異型ポリープ状腺筋腫の3例.

    早乙女啓子, 山上 亘, 同前 愛, 平野卓朗, 千代田達幸, 野村弘行, 片岡史夫, 平沢 晃, 進 伸幸, 青木大輔

    第58回日本産科婦人科内視鏡学会学術講演会 

     More details

    Event date: 2018.8.2 - 2018.8.4

    Presentation type:Oral presentation (general)  

    researchmap

  • 術後診断が漿液粘液性境界悪性腫瘍であった卵巣腫瘍の臨床的背景の検討.

    千代田達幸, 早乙女啓子, 同前 愛, 南木佳子, 吉浜智子, 平野卓朗, 真壁 健, 坂井健良, 山上 亘, 野村弘行, 片岡史夫, 平沢 晃, 青木大輔

    第58回日本産科婦人科内視鏡学会学術講演会 

     More details

    Event date: 2018.8.2 - 2018.8.4

    Presentation type:Oral presentation (general)  

    researchmap

  • 婦人科腫瘍専門医からみた卵巣腫瘍の超音波診断の意義と問題点. Invited

    野村弘行, 岩佐尚美, 早乙女啓子, 同前 愛, 千代田達幸, 片岡史夫, 平沢 晃, 青木大輔

    日本超音波医学会第91回学術集会 

     More details

    Event date: 2018.6.8 - 2018.6.10

    Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • MPA療法を施行した若年子宮体癌/子宮内膜異型増殖症患者の腫瘍家族歴と治療予後.

    平野卓朗, 山上 亘, 真壁 健, 坂井健良, 二宮委美, 千代田達幸, 小林佑介, 野村弘行, 片岡史夫, 平沢 晃, 阪埜浩司, 進 伸幸, 青木大輔

    第24回日本家族性腫瘍学会学術集会 2018.6.8-9 (兵庫) 

     More details

    Event date: 2018.6.8 - 2018.6.9

    researchmap

  • 卵巣癌における家族歴を用いたLynch症候群の拾い上げおよび臨床病理学的検討.

    竹田 貴, 阪埜浩司, 矢野倉 恵, 國富晴子, 安達将隆, 小林佑介, 平沢 晃, 冨永英一郎, 青木大輔

    第24回日本家族性腫瘍学会学術集会 

     More details

    Event date: 2018.6.8 - 2018.6.9

    Presentation type:Oral presentation (general)  

    researchmap

  • 子宮体癌/子宮内膜異型増殖症でのMPA療法の効果判定における子宮内膜細胞診の有用性.

    坂井健良, 山上 亘, 平野卓朗, 真壁 健, 野村弘行, 片岡史夫, 平沢 晃, 阪埜浩司, 進 伸幸, 青木大輔

    第59回日本臨床細胞学会総会(春期大会) 

     More details

    Event date: 2018.6.1 - 2018.6.3

    researchmap

  • 当院における分葉状頸管腺過形成(LEGH)の臨床的検討.

    安康真由香, 冨永英一郎, 高橋孝幸, 辻 浩介, 小林佑介, 平沢 晃, 阪埜浩司, 照井仁美, 亀山香織, 青木大輔

    第59回日本臨床細胞学会総会(春期大会) 

     More details

    Event date: 2018.6.1 - 2018.6.3

    researchmap

  • 卵巣癌化学療法の個別化を目指した腫瘍組織および腹水中細胞の初代3次元培養法確立.

    南木佳子, 平沢 晃, 野村弘行, 赤羽智子, 千代田達幸, 片岡史夫, 冨永英一郎, 青木大輔

    第59回日本臨床細胞学会総会(春期大会) 

     More details

    Event date: 2018.6.1 - 2018.6.3

    researchmap

  • 卵巣癌術前化学療法(NAC)奏効不良例の体腔液細胞診所見と臨床的背景の検討.

    早乙女啓子, 野村弘行, 片岡史夫, 岩佐尚美, 同前 愛, 南木佳子, 吉浜智子, 山上 亘, 平沢 晃, 青木大輔

    第59回日本臨床細胞学会総会(春期大会) 

     More details

    Event date: 2018.6.1 - 2018.6.3

    researchmap

  • 婦人科がん診療における多遺伝子パネル検査(MGPT)の導入にむけた現状と課題

    平沢 晃, 山本英喜

    第 9 回日本産科婦人科遺伝診療学会学術講演会 シンポジウム 「HBOC診療のUp to date」  2023.12.15 

     More details

    Language:Japanese  

    researchmap

  • がんゲノム医療における多遺伝子パネル検査(MGPT) の導入にむけた現状と課題

    平沢 晃, 山本英喜

    第70回日本臨床検査医学会学術集会 遺伝子委員会企画 「網羅的遺伝子解析による臨床検査の現在とこれから」  2023.11.17 

     More details

    Language:Japanese  

    researchmap

  • 「遺伝を知ることでがんを予防する」 〜地域医療・家庭医療としてのがん予防 in 島根〜 Invited

    平沢 晃

    2023年島根大学がん医療従事者研修会  2023.11.11 

     More details

    Language:Japanese  

    researchmap

  • Navigating the Genetic and Molecular Realms: Insights from BRCA1/2 Variant Carriers and the Ovarian Cancer Landscape KGOG3055/JGOG3024: Prospective cohort study of variant carriers with BRCA1/2

    HIRASAWA, Akira

    KGOG 2023 Fall Semi-annual meeting  2023.11.4 

     More details

    Language:English   Presentation type:Oral presentation (invited, special)  

    researchmap

  • Precision medicine for gynecologic tumors Invited

    HIRASAWA, Akira

    2023.10.23 

     More details

    Language:English   Presentation type:Oral presentation (invited, special)  

    researchmap

  • リンチ症候群診療の現状と課題 -遺伝子医療部門の現場から-

    平沢 晃

    第61回日本癌治療学会学術集会 領域横断シンポジウム  2023.10.20 

     More details

    Language:English   Presentation type:Oral presentation (invited, special)  

    researchmap

  • がん遺伝子パネル検査における生殖細胞系列バリアントと 遺伝カウンセリングについて ー小児固形癌を中心としてー Invited

    平沢 晃

    JCCGセミナー  2023.9.9 

     More details

    Language:Japanese  

    researchmap

  • BRCA1/2遺伝子バリアントとがん発症・臨床病理学的特徴 および発症リスク因子を明らかにするための 卵巣がん未発症を対象としたバイオバンク・コホート研究 (JGOG3024)

    平沢 晃

    第20回日本婦人科がん会議  2023.9.8 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 「日本医学会 医療における遺伝学的検査・診断に関するガイドライン」改定から1年が経過して

    平沢 晃

    第30回日本遺伝子診療学会大会・ 第8回クリニカルバイオバンク学会シンポジウム 合同学術集会 シンポジウム1 ゲノム医療にかかる法制化や指針の動向と今後の課題  2023.7.28 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    researchmap

  • Prospective cohort study of variant carriers with BRCA1 and BRCA2 (JGOG3024/KGOG3055)

    HIRASAWA, Akira

    2023.5.26 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    researchmap

  • BRCA1/2バリアントとがん発症リスク因子等を明らかにするための前向きコホート研究(JGOG3024)

    平沢 晃, 二川 摩周, 上浦 祥司, 小川 千加子, 竹原 和宏, 青木 大輔, 中村 和人, 安達 将隆, 河村 京子, 金田 倫子, 久慈 志保, 関根 正幸, 梶山 広明, 島田 宗昭, 津田 均, 岡本 愛光

    第3回JOHBOC学術総会  2023.5.20 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 遺伝性腫瘍の実地臨床 ー遺伝性骨軟部腫瘍を中心にー Invited

    平沢 晃

    第96回 日本整形外科学会学術集会 教育研修講演  2023.5.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    researchmap

  • 学会発表マニュアル(スライドおよびポスター作り)

    平沢 晃, 永谷たみ, 井上博文, 山下範之

    第64回日本臨床細胞学会総会(春期大会) 教育講演  2023.5.10 

     More details

    Language:Japanese  

    researchmap

  • Cancer precision medicine and genetic disease

    2023.3.18 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • アカデミアおよび実地診療における課題と取組 Invited

    平沢 晃

    第14回日本臨床試験学会学術集会総会 シンポジウム Patient and Public Involvement ~Beautiful Harmonyを目指して~  2023.2.9 

     More details

    Language:Japanese  

    researchmap

  • 卵巣癌におけるHBOCの現況と課題; 泌尿器科との交差点. もう知らないとは言わせないHBOC. Invited

    平沢 晃

    第109回日本泌尿器科学会総会  2021.12.7 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • いま、医療者に知っておいて欲しい「遺伝性腫瘍の基礎知識」

    平沢 晃

    島根大学がん医療従事者研修会 2021.11.29  2021.11.29 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • 卵巣癌と遺伝子関連検査

    平沢 晃

    第73回日本産科婦人科学会学術講演会  2021.4.23 

     More details

    Language:Japanese  

    researchmap

  • がん遺伝子パネル検査と産科婦人科遺伝診療. Invited

    平沢 晃

    第6回日本産科婦人科遺伝診療学会学術講演会.  2020.12.13 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • Preoperative surveillance is essential for Lynch syndrome patients.

    2020.11.14 

     More details

  • 遺伝性のがん-地域医療としての遺伝医療とがん予防について- Invited

    平沢 晃

    岡山県医師会学術奨励賞受賞講演並びに日本医師会生涯教育講座要望講演  2020.2.8 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • がんゲノム医療の実地臨床における課題. Invited

    平沢 晃

    北信がんプロ第10回オンコロジーセミナー  2020.2.7 

     More details

  • 中央西日本遺伝性腫瘍前向きコホート研究

    浦川優作, 十川麗美, 二川摩周, 河内麻里子, 山本英喜, 平沢 晃

    第1回せとうち臨床遺伝研究会  2020.2.1 

     More details

  • がん遺伝子パネル検査でBRCA1病的バリアントが同定され本人および血縁者の介入につながった一例

    十川麗美, 小川千加子, 蓮岡佳代子, 冨田秀太, 井上博文, 松原岳大, 二川摩周, 浦川優作, 河内麻里子, 山本英喜, 増山 寿, 平沢 晃

    第1回せとうち臨床遺伝研究会  2020.2.1 

     More details

  • がんゲノム医療の最新事情と課題. Invited

    平沢 晃

    令和元年度遺伝子医療技術研修会  2020.1.22 

     More details

    Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • がんゲノム医療の課題と生殖細胞系列バリアントへの対応. Invited

    平沢 晃

    第5回日本産科婦人科遺伝診療学会学術講演会  2019.12.20 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • 卵巣癌発症との関連性が推測されたBRCA1 遺伝子のVUS に関する検討.

    赤羽智子, 西原広史, 平沢 晃, 井本逸勢, 坂本一平, 野原祥男, 谷嶋成樹, 青木大輔

    第5回日本産科婦人科遺伝診療学会学術講演会  2019.12.20 

     More details

  • 卵巣癌オルガノイド培養系の確立と卵巣癌組織とのゲノム解析による比較.

    南木佳子, 千代田達幸, 平沢 晃, 赤羽智子, 早乙女啓子, 同前 愛, 平野卓朗, 黒田由香, 吉村拓馬, 山上 亘, 片岡史夫, 青木大輔

    第5回日本産科婦人科遺伝診療学会学術講演会  2019.12.20 

     More details

  • がんゲノム医療に関する話題 -がんゲノム医療と実地臨床での課題- Invited

    平沢 晃

    第6回日本婦人科腫瘍学会研修会  2019.12.14 

     More details

    Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • がんゲノム医療の動向と実地臨床における課題.

    平沢 晃

    ゲノム医療と大腸癌治療研究会  2019.11.27 

     More details

  • バイオバンクでの長期保存生体試料の品質管理標準化のための予備的検討.

    山本英喜, 松原岳大, 森田瑞樹, 冨田秀太, 豊岡伸一, 平沢 晃

    第65回日本臨床検査医学会学術集会  2019.11.21 

     More details

  • 遺伝性腫瘍 Invited

    平沢 晃

    第58回日本臨床細胞学会秋期大会  2019.11.17 

     More details

  • がんゲノム医療と遺伝医療. Invited

    平沢 晃

    日本人類遺伝学会第64回大会(教育セッション)  2019.11.8 

     More details

    Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • がんゲノム医療実用化と実地臨床での対応. Invited

    平沢 晃

    日本消化器病学会四国支部会例会  2019.11.2 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • 我が国にゲノム医療を適切に展開するため備えるべき3つのこと. Invited

    平沢 晃

    第47回日本歯科麻酔学会総会・学術集会  2019.10.26 

     More details

  • がんゲノム医療でBRCA1/2病的バリアントが同定された人への遺伝カウンセリング. Invited

    平沢 晃

    第2回HBOCアドバンストセミナー  2019.9.29 

     More details

  • がんゲノム医療実用化と産婦人科実地臨床における課題. Invited

    平沢 晃

    第391回東京産科婦人科学会例会  2019.9.29 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • 遺伝性乳がん卵巣がんとリスク低減手術.

    平沢 晃

    第59回日本産科婦人科内視鏡学会学術講演会  2019.9.12 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • ゲノム医療の最新動向と産婦人科領域における対応

    平沢 晃

    岡山県産婦人科専門医会(岡山県医師会産婦人科部会研修会)  2019.7.21 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • がんゲノム医療と実地臨床における対応. Invited

    平沢 晃

    第17回日本臨床腫瘍学会学術集会  2019.7.19 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • がんゲノム医療の実地臨床Q&A.

    平沢 晃

    遺伝カウンセリングアドバンストセミナー 臨床遺伝専門職のためのがんゲノムセミナー  2019.7.18 

     More details

    Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • がんゲノム医療と「細胞」 Invited

    平沢 晃

    第39回 岡山県臨床細胞学会・学術集会  2019.7.13 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • がんゲノム医療中核拠点病院の取り組み. Invited

    平沢 晃

    第66回全国公立大学法人病院検査部会議  2019.6.28 

     More details

  • がんゲノム医療で見つかってきた体細胞および体細胞と生殖細胞系列療法でBRCA1/2病的バリアントのみつかった方への遺伝カウンセリング. Invited

    平沢 晃

    HBOCコンソーシアム 第1回HBOCアドバンストセミナー  2019.5.12 

     More details

    Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • がんゲノム医療を導入する際の課題―安心できるゲノム医療を展開するためにー Invited

    平沢 晃

    第33回日本がん看護学会  2019.2.23 

     More details

  • データシェアリングとバイオバンクの国際動向.

    平沢 晃

    第4回研究倫理を語る会  2019.2.9 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • がん遺伝子パネル検査にてPMS2遺伝子に生殖細胞バリアントが検出された1例.

    赤羽智子, 平沢 晃, 西原広史, 植木有紗, 谷嶋成樹, 千代田達幸, 岸 郁子, 青木大輔

    第4回日本産科婦人科遺伝診療学会学術講演会  2018.12.14 

     More details

  • がんゲノム医療における婦人科腫瘍に対する対応.

    平沢 晃

    第3回日本肉腫学会・日本臨床肉腫学会合同年次総会  2018.12.12 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • 婦人科がんと女性ヘルスケア

    HIRASAWA AKIRA

    婦人科がんヘルスケア研究会  2018.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    researchmap

  • がんゲノム医療実用化と産婦人科診療における課題.

    HIRASAWA AKIRA

    第4回日本産科婦人科遺伝診療学会学術講演会  2018.12 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • Japanese perspectives on HGC.

    HIRASAWA AKIRA

    2018 Korean Society of Gynecologic Oncology Hereditary Gynecologic Cancer Symposium.  2018.11.17 

     More details

    Language:English   Presentation type:Oral presentation (invited, special)  

    researchmap

  • 「細胞」からのプレシジョンメディシン

    平沢 晃, 青木大輔

    第57回日本臨床細胞学会秋季大会  2018.11 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    researchmap

  • 香川県立中央病院におけるがんゲノム医療外来とがん遺伝相談外来について

    HIRASAWA AKIRA

    香川県立中央病院病診連携講習会  2018.11 

     More details

    Language:Japanese  

    researchmap

  • がんクリニカルシーケンスと遺伝性腫瘍

    HIRASAWA AKIRA

    日本人類遺伝学会第63回大会  2018.10 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • ゲノム医療実用化と婦人科がん領域における課題 International conference

    HIRASAWA AKIRA

    JSAWI2018  2018.9.1 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    researchmap

  • ゲノム医療実用化と遺伝性腫瘍に対する対応

    HIRASAWA AKIRA

    Brainstorming 2018 at Carillon House in Setouchi City  2018.9 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Frequency of germline pathogenic variants of cancer susceptibility genes for Japanese ovarian cancer patients. International conference

    Hirasawa A, Imoto I, Naruto T, Akahane T, Yamagami W, Nomura H, Masuda K, Susumu N, Tsuda H, Aoki D

    Third meeting of the European hereditary tumor group  2018.9 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • HBOCサーベイランスとRRSOについて

    平沢 晃, 植木有紗, 千代田達幸, 小林佑介, 青木大輔

    第60回日本婦人科腫瘍学会学術講演会  2018.9 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    researchmap

  • がんゲノム医療の現状と今後の展望 Invited

    平沢 晃

    日本臨床試験学会第7回がん臨床試験セミナー ~考え方から実践まで~  2018.8.4 

     More details

    Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    researchmap

  • がんゲノム医療の現状と今後の展望

    HIRASAWA AKIRA

    第12回広島臨床遺伝セミナー  2018.7.14 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    researchmap

  • 異型ポリープ状腺筋腫に対して高用量黄体ホルモン療法を行った22例の検討.

    清河駿樹, 千代田達幸, 山上 亘, 平野卓朗, 真壁 健, 坂井健良, 野村弘行, 片岡史夫, 平沢 晃, 進 伸幸, 田中 守, 青木大輔

    第135回関東連合産科婦人科学会学術集会  2018.6 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • がんゲノム医療時代における遺伝子情報の読み方

    平沢 晃, 千代田達幸, 植木有紗, 真壁 健

    第135回関東連合産科婦人科学会学術集会  2018.6 

     More details

    Language:Japanese  

    researchmap

  • 遺伝情報の特徴の理解に向けた短編映像の制作:ドラマ「知ること、知らないこと―遺伝子を調べることで生じることとは?―」

    小林朋子, 平沢 晃, 鈴木吉也, 吉田晶子, 安田有理, 多田 寛, 石田孝宣, 長神風二

    第24回日本家族性腫瘍学会学術集会  2018.6 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 婦人科遺伝性腫瘍およびがんゲノム異常の解析とゲノム医療実用化に向けた取り組み.

    HIRASAWA AKIRA

    第70回日本産科婦人科学会学術講演会  2018.5 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • GSTP1 rs1695 is a predictive indicator of both hematological toxicity and prognosis of ovarian cancer treated with paclitaxel plus carboplatin.

    Yoshihama T, Hirasawa A, Nomura H, Akahane T, Kataoka F, Yamagami W, Mushiroda T, Tanaka M, Aoki D

    第70回日本産科婦人科学会学術講演会  2018.5 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    researchmap

  • Gentic and epigenetic characterizataion of young-onset endometrial cancer.

    Makabe T, Arai E, Hirasawa A, Yamagami W, Susumu N, Tanaka M, Aoki D, Kanai Y

    第70回日本産科婦人科学会学術講演会  2018.5 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    researchmap

  • A genome-wide association study identifies 10 new susceptibility loci for uterine leiomyomain Japanese population.

    Sakai K, Hirasawa A, Yamagami W, Susumu N, Tanaka M, Aoki, D.Matsuda K

    第70回日本産科婦人科学会学術講演会  2018.5 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    researchmap

  • Ascites-derived and tissue-derived ovarian cancer cell primary 3D cultures aimed for precision medicine. International conference

    HIRASAWA AKIRA

    Ineternatnational society for precision Cancer Medicine Annual meeting 2018  2018.3 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    researchmap

  • Germline variants of cancer susceptibility genes for ovarian, fallopian tube, and peritoneal cancers in Japanese. International conference

    Hirasawa A, Imoto I, Naruto T, Akahane T, Yamagami W, Nomura H, Masuda K, Susumu N, Tsuda H, Aoki D

    The 57th Annual Congress of Taiwan Association of Obstetrics and Gynecology 2018  2018.3 

     More details

    Language:English   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • がんゲノム医療実用化時代における産婦人科実地臨床の課題.

    HIRASAWA AKIRA

    平成29年度広島県産婦人科研修会  2018.2.4 

     More details

    Presentation type:Oral presentation (invited, special)  

    researchmap

  • 有害事象によりベバシズマブ投与を中止した婦人科がん症例の検討.

    大野あゆみ, 千代田達幸, 野村弘行, 同前 愛, 早乙女啓子, 冨永英一郎, 岩田 卓, 山上 亘, 片岡史夫, 平沢 晃, 田中 守, 青木大輔

    第 385 回 東京産科婦人科学会例会  2018.2 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 産婦人科領域におけるがんと遺伝

    HIRASAWA AKIRA

    第184回秋田県産科婦人科学会学術講演会・秋田県産婦人科医会研修会  2018.1.28 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    researchmap

  • 産婦人科領域におけるがんゲノム医療実用化.

    HIRASAWA AKIRA

    第3回日本産婦人科遺伝診療学会(ワークショップ)  2017.12.15 

     More details

    Language:Japanese  

    Venue:兵庫  

    researchmap

  • 卵巣癌ステージング手術における腹膜生検の意義についての検討.

    高橋美央, 千代田達幸, 早乙女啓子, 同前 愛, 南木佳子, 吉浜智子, 山上 亘, 野村弘行, 片岡史夫, 平沢 晃, 田中 守, 青木大輔

    第134回関東連合産科婦人科学会学術集会  2017.12.9 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:東京  

    researchmap

  • PARP阻害薬が切り拓く卵巣がんの個別化医療.

    HIRASAWA AKIRA

    第7回日本HBOCコンソーシアム教育セミナー  2017.12.3 

     More details

    Language:Japanese  

    researchmap

  • Pathogenic germline variants of ovarian, fallopian tube, and peritoneal cancers in Japanese. International conference

    Hirasawa A, Aoki D

    5th Biennial Meeting of Asian Society of Gynecologic Oncology.  2017.11.30 

     More details

    Language:English   Presentation type:Symposium, workshop panel (nominated)  

    Venue:Tokyo  

    researchmap

  • Genomics innovations from the field of hereditary tumors

    HIRASAWA AKIRA

    日本人類遺伝学会第62回大会(教育講演)  2017.11.15 

     More details

    Language:Japanese  

    Venue:兵庫  

    researchmap

  • BRCA1/2変異卵巣癌の血縁者における乳癌および卵巣癌の罹患に関する検討.

    HIRASAWA AKIRA

    第27回日本乳癌検診学会学術総会  2017.11.10 

     More details

    Language:Japanese  

    Venue:徳島  

    researchmap

  • 産後ケア病床の立ち上げの経験.

    HIRASAWA AKIRA

    第32回日本女性医学学会学術集会  2017.11.4 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • がんゲノム医療実用化時代における女性ヘルスケアの重要性

    HIRASAWA AKIRA

    第32回日本女性医学学会学術集会(ランチョンセミナー)  2017.11.4 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • がんゲノム医療実用化と女性ヘルスケアの個別化,

    HIRASAWA AKIRA

    第32回日本女性医学学会学術集会(学会奨励賞受賞公演)  2017.11.4 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • 遺伝性腫瘍の婦人科領域における最近の展開〜遺伝性腫瘍の実臨床・理想と現実ー

    HIRASAWA AKIRA

    第55回日本癌治療学会学術集会(シンポジウム)  2017.10.20 

     More details

    Language:Japanese  

    Venue:神奈川  

    researchmap

  • Peutz–Jeghers syndrome as a hereditary gynecological tumor. Invited International conference

    HIRASAWA AKIRA, Aoki D

    Shanghai Pudong Cervical Disease Summit Forum & Classes on Research Progress of the Relationship between HPV Molecular Variation and Cervical Disease.  2017.10.14 

     More details

    Language:English   Presentation type:Oral presentation (invited, special)  

    Venue:上海, 中国  

    researchmap

  • Post-pregnancy outcomes of young patients with endometrial cancer or atypical endometrial hyperplasia who received fertility-preserving hormonal therapy using medroxyprogesterone acetate. International conference

    Susumu N, Yamagami W, Hirano T, Makabe T, Sakai K, Chiyoda T, Nomura H, Kataoka F, Saitoh E, HIRASAWA AKIRA, Tominaga E, Banno K, Aoki D

    The 20th international meeting of the European Society of Gynaecological Oncology  2017.10.4 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Vienna,Austria  

    researchmap

  • The contribution of germline pathogenic variants of cancer susceptibility genes for primary ovarian, fallopian tube, and peritoneal cancers in Japanese. International conference

    HIRASAWA AKIRA, Issei I, Naruto T, Akahane T, Yamagami W, Nomura H, Masuda K, Susumu N, Tsuda H, Aoki D

    AACR 2017 Addressing Critical Questions in Ovarian Cancer Research and Treatment.  2017.10.1 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Pittsburgh, PA, USA  

    researchmap

  • Ascites-derived and tissue-derived ovarian cancer cell primary 3D cultures aimed for personalized medicine. International conference

    Nanki Y, HIRASAWA AKIRA, Nomura H, Okubo A, Itoh M, Akahane A, Chiyoda T, Kataoka F, Tominaga E, Aoki D

    AACR 2017 Addressing Critical Questions in Ovarian Cancer Research and Treatment.  2017.10.1 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Pittsburgh, PA, USA  

    researchmap

  • UGT1A1 polymorphism may be a prognostic indicator of stage I ovarian clear cell carcinoma patients treated with irinotecan. International conference

    Yoshihama T, HIRASAWA AKIRA, Nomura H, Akahane T, Nanki Y, Yamagami W, Kataoka F, Tominaga E, Susumu N, Mushiroda T, Aoki D

    15th International Congress of Therapeutic Drug Monitoring and Clinical Toxicology.  2017.9.24 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:Kyoto, Japan  

    researchmap

  • 婦人科実地臨床における遺伝性卵巣癌の診療

    HIRASAWA AKIRA

    Scientific Exchange Meeting in Fukushima  2017.9.8 

     More details

    Language:Japanese  

    Venue:福島  

    researchmap

  • 遺伝性乳癌卵巣癌症候群に対するリスク低減卵管卵巣摘出後の漢方療法に関する検討.

    第37回産婦人科漢方研究会学術集会  2017.8.27 

     More details

    Language:Japanese  

    Venue:北海道  

    researchmap

  • ヒト卵巣癌でのADAM 分子の網羅的発現および機能解析.

    第22回日本病態プロテアーゼ学会学術集会  2017.8.11 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • RRSOと女性QOL.

    HIRASAWA AKIRA

    第23回家族性腫瘍学会学術集会(要望演題)  2017.8.4 

     More details

    Language:Japanese  

    Venue:北海道  

    researchmap

  • ゲノム異常と女性医学から考えるリスク低減手術.

    HIRASAWA AKIRA

    第59回日本婦人科腫瘍学会学術講演会(ワークショップ)  2017.7.27 

     More details

    Language:Japanese  

    Venue:熊本  

    researchmap

  • Prevention and treatment strategy for hereditary ovarian cancer: Present and future sattus of Hereditary Cancer Prophylactic

    HIRASAWA AKIRA

    第15回日本臨床腫瘍学学術集会  2017.7.27 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:兵庫  

    researchmap

  • RARP阻害薬と卵巣癌治療.

    HIRASAWA AKIRA

    第24回日本遺伝子診療学会大会(シンポジウム)  2017.7.13 

     More details

    Language:Japanese  

    Venue:千葉  

    researchmap

  • PARP 阻害剤と卵巣がん治療.

    HIRASAWA AKIRA

    第6回日本HBOCコンソーシアム教育セミナー  2017.6.25 

     More details

    Language:Japanese  

    Venue:東京  

    researchmap

  • BRCA1/2遺伝学的検査受検後のリスク低減卵管卵巣摘出術選択に影響する要因の検討

    2017.6.22 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • 遺伝子診療とHBOC

    HIRASAWA AKIRA

    Scientific Exchange Meeting in Tama  2017.6.19 

     More details

    Language:Japanese  

    Venue:東京  

    researchmap

  • JGOGにおけるTranslational Research

    HIRASAWA AKIRA

    JGOG3024. 第14回日本婦人科がん会議  2017.6.9 

     More details

    Language:Japanese  

    Venue:新潟  

    researchmap

  • 卵巣癌ゲノム国際データシェアリングの現状.

    第45回北陸産科婦人科学会  2017.6.4 

     More details

    Language:Japanese  

    Venue:新潟  

    researchmap

  • 腹水卵巣癌細胞のCD44各アイソフォーム発現量と化学療法の効果との関連性の検討.

    第58回日本臨床細胞学会総会(春期大会)  2017.5.27 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • 当院における穿刺腹腔細胞診所見に基づく卵巣癌術前化学療法適用の実際.

    第58回日本臨床細胞学会総会(春期大会)(ワークショップ)  2017.5.27 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • 子宮体癌の術前子宮鏡検査と腹水細胞診.

    第58回日本臨床細胞学会総会(春期大会)  2017.5.27 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • Clinical trials of the Japanese Gynecologic Oncology Group (JGOG) and JGOG/ToMMo biobank will facilitate precision medicine for gynecologic malignancies. International conference

    HIRASAWA AKIRA, Yoshihara K, Sekine M, Enomoto T, Daisuke A, Sugiyama S

    the 3rd Taiwan-Japan academic research organization workshop.  2017.5.13 

     More details

    Language:English   Presentation type:Oral presentation (invited, special)  

    Venue:Fukuoka, Japan  

    researchmap

  • Polymorphisms of the genes ESR1, UGT2B17, and UGT1A1 associated with estrogen metabolism are not associated with osteoporosis in Japanese women after artificial menopause. International conference

    Yokota M, HIRASAWA AKIRA, Kazuya K, Akahane T, Sakai K, Makabe T, Horiba Y, Yamagami W, Ogawa M, Iwata T, Yanamoto S, Deshimaru R, Banno K, Susumu N, Aoki D

    6th Scientific Meeting of the Asia Pacific Menopause Federation.  2017.4.20 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • The contribution of deleterious germ-line mutations of susceptibility genes to ovarian, fallopian tube, and peritoneal cancers in Japanese. International conference

    Hirasawa A, Imoto I, Naruto T, Akahane T, Yamagami W, Susumu N, Tsuda H, Aoki D

    AACR Annual Meeting 2017  2017.4.1 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Washington, D.C., USA  

    researchmap

  • HBOCの診療 —産婦人科の観点から(遺伝性乳癌卵巣癌)

    HIRASAWA AKIRA

    Scientific Exchange Meeting in Akita -HBOC  2017.3.25 

     More details

    Language:Japanese  

    Venue:秋田  

    researchmap

  • 婦人科における遺伝性卵巣がんの診療(遺伝性乳癌卵巣癌)

    HIRASAWA AKIRA

    Scientific Exchange Meeting in Aomori -HBOC  2017.3.11 

     More details

    Language:Japanese  

    Venue:青森  

    researchmap

  • HBOCにおけるがん予防 —その個別化と女性QOL-

    HIRASAWA AKIRA

    第6回TM遺伝性乳がん卵巣がん研究会  2017.3.2 

     More details

    Language:Japanese  

    Venue:東京  

    researchmap

  • 手術前禁忌薬剤(経口避妊薬)に関する医療安全対策.

    HIRASAWA AKIRA

    第381回東京産科婦人科学会例会  2017.2.25 

     More details

    Language:Japanese  

    Venue:東京  

    researchmap

  • Germ-line mutations of cancer susceptibility genes among Japanese ovarian, fallopian tube, and peritoneal cancer patients. International conference

    Hirasawa A, Aoki D

    4th Meeting of the International Ovarian Cancer Consortium  2017.2.23 

     More details

    Language:English   Presentation type:Oral presentation (invited, special)  

    Venue:Seoul, Korea  

    researchmap

  • 遺伝性乳癌卵巣癌およびBRCA1/2検査に関する最近のトピック.

    HIRASAWA AKIRA

    第20回東北家族性腫瘍研究会  2017.2.18 

     More details

    Language:Japanese  

    Venue:宮城  

    researchmap

  • 北欧バイオバンク事情と遺伝性腫瘍.

    HIRASAWA AKIRA

    北海道大学臨床遺伝子診療部・腫瘍センター共催定期講演会(平成28年度第10回腫瘍センターセミナー)  2017.2.10 

     More details

    Language:Japanese  

    Venue:北海道  

    researchmap

  • がん個別化予防法としてのRRSOと女性QOL.

    平沢 晃, 牧田和也, 岩田 卓, 堀場裕子, 林 茂徳, 野村弘行, 片岡史夫, 冨永英一郎, 青木大輔

    第5回日本HBOCコンソーシアム学術総会  2017.1.21 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:北海道  

    researchmap

  • 子宮体癌206例の末梢血を用いたDNAミスマッチ修復遺伝子のメチル化解析.

    竹田 貴, 阪埜浩司, 矢野倉恵, 安達将隆, 小林佑介, 山上 亘, 平沢 晃, 冨永英一郎, 進 伸幸, 青木大輔

    第2回日本産科婦人科遺伝診療学会学術講演会  2016.12.16 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • 血縁腫瘍歴聴取票を用いた婦人科関連遺伝性腫瘍のスクリーニングに関する検討.

    平野卓朗, 平沢 晃, 真壁 健, 坂井健良, 赤羽智子, 増田健太, 小林佑介, 山上 亘, 野村弘行, 片岡史夫, 冨永英一郎, 阪埜浩司, 進 伸幸, 青木大輔

    第2回日本産科婦人科遺伝診療学会学術講演会  2016.12.16 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • BRCA1/2遺伝子変異保持者に対するリスク低減卵管卵巣摘出術実施例に関する検討.

    吉村拓馬, 平沢 晃, 吉浜智子, 赤羽智子, 平野卓朗, 増田健太, 山上 亘, 林 茂徳, 野村弘行, 片岡史夫, 阪埜浩司, 進 伸幸, 青木大輔

    第2回日本産科婦人科遺伝診療学会学術講演会  2016.12.16 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • がんの予防・治療と遺伝子関連検査.

    平沢 晃

    (株)日立製作所 研究討論会  2016.12.5 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:東京  

    researchmap

  • 卵巣がんの遺伝学的特性および臨床薬理学的特徴.

    平沢 晃, 青木大輔

    第37回日本臨床薬理学会学術集会  2016.12.1 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:鳥取  

    researchmap

  • 腹水細胞中から樹立したヒト悪性腹膜中皮腫由来細胞株の特性に関する検討.

    赤羽智子, 冨永英一郎, 平沢 晃, 青木大輔

    第55回日本臨床細胞学会秋期大会  2016.11.18 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:大分  

    researchmap

  • リンチ症候群-その遺伝子型と表現型-

    平沢 晃, 山上 亘, 阪埜浩司, 進 伸幸, 青木大輔

    第55回日本臨床細胞学会秋期大会  2016.11.18 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:大分  

    researchmap

  • 内膜細胞診の有用性-臨床医の観点から-

    進 伸幸, 山上 亘, 片岡史夫, 平沢 晃, 亀山香織, 阪埜浩司, 青木大輔

    第55回日本臨床細胞学会秋期大会  2016.11.18 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:大分  

    researchmap

  • 遺伝性乳癌卵巣癌に対するリスク低減卵管卵巣摘出後のQOLに関する検討.

    谷本慧子, 平沢 晃, 牧田和也, 岩田 卓, 堀場裕子, 横田めぐみ, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔

    第31回日本女性医学学会学術集会  2016.11.5 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • Hysteroscopic diagnosis of myometrial invasion for the horomonal treatment in cases with endometrial cancer. International conference

    Yamagami W, Susumu N, Hirano T, Nanki Y, Makabe T, Sakai K, Nomura H, Kataoka F, Hirasawa A, Aoki D

    17th APAGE Annual Congress 2016  2016.11.4 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Taipei, Taiwan  

    researchmap

  • Three parients with atypical entometrial hyperplasia/endometrial cancer who underwent laparoscopic surgery in order to be diagnosed as double cancer of ovary. International conference

    Hirano T, Yamagami W, Sakai K, Makabe T, Yoshihama T, Nomura H, Kataoka F, Hirasawa A, Susumu N, Aoki D

    17th APAGE Annual Congress 2016  2016.11.4 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Taipei, Taiwan  

    researchmap

  • A successful case of young patient with endometrial cancer for preserving fertility by trans cervical resection (TCR) for giant intrauterine tumor. International conference

    Susumu N, Yamagami W, Hirano T, Saeki N, Makabe T, Sakai K, Nomura H, Kataoka F, Hirasawa A, Aoki D

    17th APAGE Annual Congress 2016  2016.11.4 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Taipei, Taiwan  

    researchmap

  • 遺伝性乳がん卵巣がんと女性ヘルスケア.

    平沢 晃, 青木大輔

    第15回更年期と加齢のヘルスケア学会  2016.10.22 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:東京  

    researchmap

  • 婦人科遺伝性腫瘍の実地臨床.

    平沢 晃, 青木大輔

    第132回関東連合産科婦人科学会  2016.10.15 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:東京  

    researchmap

  • 当院における婦人科疾患に合併した深部静脈血栓症/肺塞栓症の検討.

    吉村拓馬, 山上 亘, 平野卓朗, 南木佳子, 坂井健良, 真壁 健, 野村弘行, 片岡史夫, 平沢 晃, 阪埜浩司, 田中 守, 青木大輔

    第132回関東連合産科婦人科学会  2016.10.15 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 婦人科癌と女性QOL.

    平沢 晃, 青木大輔

    調布・狛江・府中三産婦人科医会秋季研修会  2016.10.13 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:東京  

    researchmap

  • 婦人科遺伝性腫瘍と予防・治療法の個別化.

    平沢 晃, 青木大輔

    第23回日本遺伝子診療学会大会  2016.10.7 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:東京  

    researchmap

  • A genome-wide association stdy identidies 3 new susceptibility loci for uterine fibrosis in Jananese population.

    Sakai K, Hirata M, Tanikawa C, Kamatani Y, Kubo M, Hirasawa A, Matsuda K

    第75回日本癌学会学術総会  2016.10.6 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:神奈川  

    researchmap

  • 遺伝性腫瘍と患者支援

    平沢 晃

    平成28年度第7回 慶應義塾大学病院がん看護研修  2016.9.20 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:東京  

    researchmap

  • 欧州バイオバンク事情と本邦における課題.

    平沢 晃

    第66回徳島大学糖尿病臨床・研究開発センター講演会.  2016.9.6 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:徳島  

    researchmap

  • 遺伝性卵巣癌〜HBOCを中心に〜

    平沢 晃, 青木大輔

    JSAWI第17回シンポジウム  2016.9.4 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:兵庫  

    researchmap

  • Data driven lead optimization: Computational integration of structural properties, biomarkers, and drug responses. International conference

    Khan SA, Murumägi A, Hirasawa A, Arjama M, Kallioniemi OP, Aittokallio T

    FIMM-Pharma meeting  2016.8.22 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Helsinki, Finland  

    researchmap

  • 産婦人科医に知ってほしい乳がんのリスク因子(家族性腫瘍を含めて)

    平沢 晃, 青木大輔

    第8回関東産婦人科乳腺医学会  2016.7.24 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:東京  

    researchmap

  • 遺伝性卵巣がんの予防と治療.

    平沢 晃, 青木大輔

    第17回臨床腫瘍夏期セミナー  2016.7.22 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:東京  

    researchmap

  • 遺伝性乳がん卵巣がんをめぐる最新事情.

    平沢 晃, 青木大輔

    Scientific exchange meeting in Ehime  2016.7.16 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:愛媛  

    researchmap

  • 遺伝性乳癌卵巣癌とリスク低減手術.

    平沢 晃

    高知大学臨床遺伝診療部セミナー  2016.7.15 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:高知  

    researchmap

  • HBOCに関する最近の動向

    平沢 晃, 青木大輔

    第58回日本婦人科腫瘍学会学術講演会  2016.7.8 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:鳥取  

    researchmap

  • 卵巣摘出術と女性QOLー更年期症状、脂質異常症、骨粗鬆症などの管理についてー

    平沢 晃, 青木大輔

    第131回関東連合産科婦人科学会学術集会  2016.6.18 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:鳥取  

    researchmap

  • Lynch症候群とCowden病 婦人科編

    平沢 晃, 青木大輔

    北野病院遺伝性腫瘍セミナー  2016.6.11 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:大阪  

    researchmap

  • がんプロフェッショナル養成基盤推進プランを通した医療従事者への家族性腫瘍教育の取り組み –HBOCに対するPARP阻害薬承認を見据えて-.

    植木有紗, 平沢 晃, 今村知世, 武田祐子, 守屋利佳, 赤羽智子, 増田健太, 中田さくら, 安齋純子, 三須久美子, 阪埜浩司, 小崎健次郎, 谷川原祐介, 青木大輔

    第22回日本家族性腫瘍学会学術集会  2016.6.3 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:愛媛  

    researchmap

  • 自己記入式がん家族歴聴取票を使用した遺伝高リスク家系の抽出.

    國富晴子, 増田健太, 平沢 晃, 赤羽智子, 小林佑介, 山上 亘, 野村弘行, 片岡史夫, 冨永英一郎, 阪埜浩司, 進 伸幸, 青木大輔

    第22回日本家族性腫瘍学会学術集会  2016.6.3 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:愛媛  

    researchmap

  • MSH6の生殖細胞系列変異によりLynch症候群と診断された体下部発生子宮体癌の1例.

    安達将隆, 阪埜浩司, 植木有紗, 増田健太, 矢野倉恵, 飯島茂異人, 竹田 貴, 小林佑介, 山上 亘, 冨永英一郎, 平沢 晃, 菅野康吉, 青木大輔

    第22回日本家族性腫瘍学会学術集会  2016.6.3 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:愛媛  

    researchmap

  • 遺伝性乳がん卵巣がんの現状と本邦での取り組み

    平沢 晃, 青木大輔

    第57回日本臨床細胞学会総会  2016.5.28 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:神奈川  

    researchmap

  • Profiling of epithelial ovarian cancer as BRCAness status with MLPA method. International conference

    HIRASAWA AKIRA, Akahane T, Masuda K, Ninomiya T, Yamagami W, Nomura H, Kataoka F, Banno k, Susumu N, Aoki D

    The sixth International Symposium on Hereditary Breast and Ovarian Cancer  2016.5.10 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:(Montréal, Canada)  

    researchmap

  • 5年前に調査した当科健康維持外来における塩酸ラロキシフェン誌用症例のその後の服用状況についての検討.

    牧田和也, 橫田めぐみ, 平沢 晃, 岩田 卓, 青木大輔

    第11回SERM学術研究会  2016.5.9 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:東京  

    researchmap

  • 判別分析法によるTC療法中の好中球減少と相関する一塩基多型(SNP)の抽出.

    岩佐尚美, 野村弘行, 片岡史夫, 南木佳子, 吉浜智子, 中平直希, 山上 亘, 平沢 晃, 進 伸幸, 田中 守, 青木大輔

    第68回日本産科婦人科学会学術講演会  2016.4.21 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • A prospective study on the safety of chemotherapy combined with bevacizumab in Japanese patients with recurrent ovarian cancer.

    Nanki Y, Nomura H, Kataoka F, Iwasa N, Yoshihama T, Nakadaira N, Ninomiya T, Yamagami W, Hirasawa A, Susumu N, Tanaka M, Aoki D

    第68回日本産科婦人科学会学術講演会  2016.4.21 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • An analysis of short-term reccurent cases following medroxyprogesterone acetate (MPA) therapy for endometrial cancer and atypical endometrial hyperplasia.

    Yamagami W, Susumu N, Sakai K, Makabe T, Ninomiya T, Nomura H, Kataoka F, Hirasawa A, Bonno K, Tanaka M, Aoki D

    第68回日本産科婦人科学会学術講演会  2016.4.21 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • BRCAness status of ovarian cancer with somatic large genomic rearrangement.

    Ninomiya T, Hirasawa A, Akahane T, Masuda K, Yamagami W, Nomura H, Kataoka F, Susumu N, Bonno K, Tanaka M, Aoki D

    第68回日本産科婦人科学会学術講演会  2016.4.21 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • TAS-117, a novel allosteric AKT inhibitor, shows potent antitumor activity on ovarian clear cell adenocarcinoma cells from fresh surgical samples in 3-dimentional culture.

    Tsuta K, Tominaga E, Tozawa A, Akahane T, Uekawa A, Ohara T, Nomura H, Kataoka F, Hirasawa A, Bonno K, Suzuki N, Aoki D

    第68回日本産科婦人科学会学術講演会  2016.4.21 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • 子宮体癌術後患者における卵巣欠落症状とQOLに及ぼす影響に関する検討.

    橫田めぐみ, 牧田和也, 平沢 晃, 堀場裕子, 岩田 卓, 小川真里子, 柳本茂久, 弟子丸亮太, 田中 守, 青木大輔

    第68回日本産科婦人科学会学術講演会  2016.4.21 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • 婦人科疾患における自覚症状としての「冷え」,疾患単位としての「冷え症」の合併頻度についての検討.

    堀場裕子, 吉野鉄大, 平沢 晃, 牧田和也, 橫田めぐみ, 岩田 卓, 渡辺賢治, 青木大輔

    第68回日本産科婦人科学会学術講演会  2016.4.21 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • Mutation of any DNA mismatch gene can cause lower uterine segment cancer with Lynch syndrome.

    Iijima M, Banno K, Masuda K, Yanokura M, Adachi M, Nogami Y, Yamagami W, Tominaga E, Hirasawa A, Susumu N, Tanaka M, Aoki D

    第68回日本産科婦人科学会学術講演会  2016.4.21 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • 遺伝性乳がん卵巣がん-産婦人科の立場から

    平沢 晃, 青木大輔

    第13回日本乳癌学会九州地方会・市民公開講座  2016.3.6 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:福岡  

    researchmap

  • 子宮体部・卵巣同時発生重複癌症例の臨床病理学的検討

    小笠原純, 小林佑介, 野村弘行, 山上 亘, 片岡史夫, 平沢 晃, 冨永英一郎, 鈴木 淳, 阪埜浩司, 進 伸幸, 田中 守, 青木大輔

    第377回東京産科婦人科学会例会  2016.2.20 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 遺伝性乳癌卵巣癌およびBRCA1/2検査に関する最近のトピック. Invited

    平沢 晃

    第20回東北家族性腫瘍研究会  2016.2.18 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:仙台  

    researchmap

  • Ovarian cancers with BRCA1/2 mutations. International conference

    HIRASAWA AKIRA, Aoki D

    The 31st Nagoya International Cancer Treatment Symposium  2016.2.13 

     More details

    Language:English   Presentation type:Symposium, workshop panel (nominated)  

    Venue:(Aichi, Japan)  

    researchmap

  • Profiling of epithelial ovarian cancer as BRCAness status with MLPA method. International conference

    Susumu N, YamagamiW, Kataoka F, Makabe T, Sakai K, Ninomiya T, HIRASAWA AKIRA, Nakahara T, Kameyama K, Aoki D

    Usefulness of intra-operative touch imprinting cytology of sentinel lymph nodes in endometrial cancer for improving intra-operative diagnostic accuracy.  2016.2.13 

     More details

    Language:English  

    Venue:(Yokohama, Japan)  

    researchmap

  • 北欧におけるバイオバンク事情.

    平沢 晃, 青木大輔

    東京医科歯科大学疾患バイオリソースセンター大学院セミナー  2016.2.12 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:東京  

    researchmap

  • 北欧バイオバンク事情と遺伝性腫瘍. 北海道大学臨床遺伝子診療部・腫瘍センター共催定期講演会 Invited

    平沢 晃

    平成28年度第10回腫瘍センターセミナー  2016.2.10 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:札幌  

    researchmap

  • 発がんリスクの層別化と個別化予防法の確立を目指して.

    平沢 晃, 青木大輔

    第4回日本HBOCコンソーシアム学術総会  2016.1.24 

     More details

    Language:Japanese   Presentation type:Public lecture, seminar, tutorial, course, or other speech  

    Venue:東京  

    researchmap

  • Collaboration and future clinical trial of hereditary gynecologic cancer. Invited International conference

    HIRASAWA AKIRA, Aoki D

    2016 Korean Society of Gynecologic Oncology; Hereditary Gynecologic Cancer Symposium .  2016.1.9 

     More details

    Language:English   Presentation type:Symposium, workshop panel (nominated)  

    Venue:(Souel, Korea)  

    researchmap

  • SNP 解析を用いた卵巣癌化学療法の毒性および効果予測.

    岩佐尚美, 野村弘行, 片岡史夫, 南木佳子, 吉浜智子, 中平直希, 山上 亘, 平沢 晃, 進 伸幸, 青木大輔

    第1回日本産科婦人科遺伝診療学会学術講演会  2015.12.18 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:長崎  

    researchmap

  • 婦人科疾患バイオバンクの現状と家族性腫瘍のスクリーニングに関する検討.

    赤羽智子, 平沢 晃, 増田健太, 真壁 健, 坂井健良, 吉浜智子, 山上 亘, 野村弘行, 片岡史夫, 阪埜浩司, 進 伸幸, 青木大輔

    第1回日本産科婦人科遺伝診療学会学術講演会  2015.12.18 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:長崎  

    researchmap

  • MSH6生殖細胞系列変異によりLynch 症候群と診断された体下部発生子宮体癌の1例.

    安達将隆, 阪埜浩司, 増田健太, 矢野倉恵, 飯島茂異人, 竹田貴, 山上 亘, 冨永英一郎, 平沢 晃, 菅野康吉, 青木大輔

    第1回日本産科婦人科遺伝診療学会学術講演会  2015.12.18 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:長崎  

    researchmap

  • 遺伝性乳癌卵巣癌に対するリスク低減卵管卵巣摘出術後のヘルスケアに関する検討.

    横田めぐみ, 平沢 晃, 牧田 和也, 堀場 裕子, 岩田 卓, 青木大輔, 冨永英一郎

    第1回日本産科婦人科遺伝診療学会学術講演会  2015.12.18 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:長崎  

    researchmap

  • 腹腔鏡補助下子宮筋腫核出術(LAM)における術式定型化の工夫.

    南木佳子, 野村弘行, 片岡史夫, 岩佐尚美, 吉浜智子, 中平直希, 二宮委美, 西尾浩, 山上亘, 平沢 晃, 進 伸幸, 青木大輔

    第28回日本内視鏡外科学会総会  2015.12.10 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • 当院におけるBRCA1/2遺伝子変異保持者に対する腹腔鏡下でのリスク低減卵管卵巣摘出術の実施経験.

    吉浜智子, 片岡史夫, 野村弘行, 平沢 晃, 増田健太, 岩佐尚美, 中平直希, 南木佳子, 二宮委美, 西尾 浩, 山上 亘, 阪埜浩司, 進 伸幸, 青木大輔

    第28回日本内視鏡外科学会総会  2015.12.10 

     More details

    Language:Japanese  

    Venue:大阪  

    researchmap

  • 子宮体部漿液性腺癌の早期診断に子宮内膜細胞診が有用であった 2 例の検討.

    坂井健良, 進 伸幸, 山上 亘, 真壁 健, 二宮委美, 南木佳子, 吉浜智子, 岩佐尚美, 中平直希, 野村弘行, 片岡史夫, 平沢 晃, 冨永英一郎, 阪埜浩司, 青木大輔

    第54回日本臨床細胞学会秋季大会  2015.11.21 

     More details

    Language:Japanese  

    Venue:愛知  

    researchmap

  • Profiling of epithelial ovarian cancer with BRCAness status International conference

    HIRASAWA AKIRA, Masuda K, Akahane T, Ninomiya T, Yamagami W, Nomura H, Kataoka F, Banno K, Susumu N, Aoki D

    The 4th Biennial Meeting of Asian Society of Gynecologic Oncology  2015.11.12 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:(Souel, Korea)  

    researchmap

  • BRCA1/2遺伝子変異保持者に対するリスク低減卵管卵巣摘出後のQOLに関する検討.

    平沢 晃, 牧田和也, 横田めぐみ, 堀場裕子, 岩田卓, 小川真里子, 柳本茂久, 弟子丸亮太, 高松 潔, 青木大輔

    第30回日本女性医学学会学術集会  2015.11.7 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:愛知  

    researchmap

  • 進行卵巣癌に対する術前化学療法におけるdose-dense TC療法の臨床効果に関する検討.

    岩佐尚美, 吉浜智子, 片岡 史夫, 野村 弘行, 橋本 志歩, 岩佐 尚美, 中平 直希, 二宮 委美, 山上 亘, 平沢 晃, 進 伸幸, 青木大輔

    第53回日本癌治療学会学術集会  2015.10.29 

     More details

    Language:Japanese  

    Venue:京都  

    researchmap

  • 40歳以上の子宮体癌に対する高用量MPA療法は有用か.

    山上 亘, 進 伸幸, 坂井健良, 真壁 健, 二宮委美, 和田美智子, 野村弘行, 片岡史夫, 平沢 晃, 阪埜浩司, 青木大輔

    第53回日本癌治療学会学術集会  2015.10.29 

     More details

    Language:Japanese  

    Venue:京都  

    researchmap

  • メバロン酸合成経路を標的とした卵巣癌新規治療戦略の検討.

    小林佑介, 阪埜浩司, 増田健太, 野村弘行, 片岡史夫, 冨永英一郎, 平沢 晃, 進 伸幸, Tian-li Wang, Ie-ming Shih, 青木大輔

    第53回日本癌治療学会学術集会  2015.10.29 

     More details

    Language:Japanese  

    Venue:京都  

    researchmap

  • 再発卵巣癌に対するベバシズマブ併用化学療法の安全性に関する前方視的検討.

    野村弘行, 片岡史夫, 吉浜智子, 中平直希, 二宮委美, 山上 亘, 平沢 晃, 進 伸幸, 青木 大輔

    第53回日本癌治療学会学術集会  2015.10.29 

     More details

    Language:Japanese  

    Venue:京都  

    researchmap

  • I期,II期の子宮体部類内膜癌における再発リスク因子の検討.

    小塙理人, 山上 亘, 二宮委美, 坂井健良, 真壁 健, 野村弘行, 片岡史夫, 平沢 晃, 阪埜浩司, 進 伸幸, 田中 守, 青木大輔

    第130回関東連合産科婦人科学会学術集会  2015.10.24 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:千葉  

    researchmap

  • 北欧におけるバイオバンク事情.

    平沢 晃

    日本人類遺伝学会第60回大会(エキスパートセミナー)  2015.10.14 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:東京  

    researchmap

  • リスク低減卵管卵巣摘出術後の卵巣欠落症状に対する漢方療法に関する検討.

    橫田めぐみ, 平沢 晃, 牧田和也, 堀場裕子, 岩田 卓, 小川真里子, 柳本茂久, 弟子丸亮太, 高松 潔, 青木大輔

    第35回産婦人科漢方研究会学術集会  2015.9.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • BRCA1/2遺伝子検査と産婦人科臨床

    平沢 晃, 青木大輔

    第57回日本婦人科腫瘍学会学術講演会(ワークショップ)  2015.8.7 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:岩手  

    researchmap

  • 一般病院における家族性腫瘍相談外来とハイリスク外来の開設.

    植木有紗, 安斎純子, 中田さくら, 麻薙美香, 嶋田恭輔, 久保内光一, 三須久美子, 平沢 晃, 阪埜浩司, 菅野康吉, 小崎健次郎, 青木大輔

    第21回日本家族性腫瘍学会学術集会  2015.6.5 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:埼玉  

    researchmap

  • Novel therapeutic possibilities for chemorefractory ovarian cancer patients identified by functional ex vivo drug sensitivity testing of primary cells from ascites. International conference

    Murumägi A, HIRASAWA AKIRA, Arjama M, Välimäki K, Bhagwan Y, Tang J, Szwajda A, Turunen L, JP Mpindi, Pellinen T, Wennerberg K, Bützow R, Aittokallio T, Kallioniemi O

    AACR Annual Meeting 2015  2015.4.18 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:(Philadelphia, USA)  

    researchmap

  • BRCA1/2遺伝子生殖細胞変異例における良性卵管上皮細胞のp53蛋白発現とTP53遺伝子変異の意義.

    赤羽智子, 平沢 晃, 増田健太, 片岡史夫, 冨永英一郎, 阪埜浩司, 進 伸幸, 田中 守, 青木大輔

    第67回日本産科婦人科学会学術講演会  2015.4.9 

     More details

    Language:Japanese  

    Venue:神奈川  

    researchmap

  • 婦人科領域における遺伝性腫瘍.

    平沢 晃, 青木大輔

    第67回日本産科婦人科学会学術講演会(ランチョンセミナー)  2015.4.9 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神奈川  

    researchmap

  • 新規アロステリック型AKT阻害剤TAS-117は卵巣癌患者腹水中の癌細胞に対して有効性を示す.

    蔦 幸児, 冨永英一郎, 戸澤晃子, 赤羽智子, 大原 樹, 野村弘行, 片岡史夫, 平沢 晃, 阪埜浩司, 鈴木 直, 青木大輔

    第67回日本産科婦人科学会学術講演会  2015.4.9 

     More details

    Language:Japanese  

    Venue:神奈川  

    researchmap

  • 当科における子宮体癌術後患者の卵巣欠落症状に対するエストロゲン療法(ET)の試み.

    牧田和也, 橫田めぐみ, 堀場裕子, 山上 亘, 平沢 晃, 小川 真里子, 弟子丸亮太, 柳本茂久, 阪埜浩司, 進 伸幸, 高松 潔, 青木大輔

    第29回日本女性医学学会学術集会  2014.11.19 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 遺伝性腫瘍の発症前診断とサーベイランスおよび予防的介入 BRCA1/2遺伝子変異保持者に対するリスク低減卵巣卵管切除術.

    平沢 晃, 増田健太, 赤羽智子, 片岡史夫, 冨永英一郎, 阪埜浩司, 進 伸幸, 菅野康吉, 小崎健次郎, 青木大輔

    第59回日本人類遺伝学会・第21回日本遺伝子診療学会 合同大会 (シンポジウム)  2014.11.19 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    Venue:東京  

    researchmap

  • 当科における子宮体癌術後患者の卵巣欠落症状に対するエストロゲン療法(ET)の試み.

    牧田和也, 橫田めぐみ, 堀場裕子, 山上 亘, 平沢 晃, 小川 真里子, 弟子丸亮太, 柳本茂久, 阪埜浩司, 進 伸幸, 高松 潔, 青木大輔

    第29回日本女性医学学会学術集会  2014.11.1 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • p62/SQSTM1 タンパク質の高発現は子宮体癌の悪性形質および不良な予後と相関する.

    岩舘怜子, 井上 純, 津田 均, 平沢 晃, 青木大輔, 稲澤譲治

    第73回日本癌学会学術総会  2014.9.25 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • High-throughput drug sensitivity and resistance testing of ovarian cancer cell lines provides useful strategy for assessing drug repositioning and therapeutic possibilities of emerging drugs. International conference

    Hirasawa A, Murumägi A, Arjama1 M, Bhagwan Y, JP Mpindi, Arjama M, Wennerberg K, Aittokallio T, Aoki D, Kallioniemi O

    The 10th Biennial Ovarian Cancer Research Symposium  2014.9.8 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Seattle  

    researchmap

  • Peutz-Jeghers syndrome (PJS) 患者に認められたSTK11遺伝子スプライシング異常の病的意義についての検討.

    増田健太, 小林佑介, 植木有紗, 野村弘行, 平沢 晃, 阪埜浩司, 青木大輔, 三須久美子, 小崎健次郎, 牛尼美年子, 吉田輝彦, 齋藤伸哉, 菅野康吉

    第18回日本家族性腫瘍学会学術集会  2014.6.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:福島  

    researchmap

  • 子宮体部・卵巣同時発生重複癌におけるDNAミスマッチ修復タンパクの免疫組織化学的染色による解析.

    中村加奈子, 阪埜浩司, 小林佑介, 野村弘行, 矢野倉恵, 飯田美穂, 安達将隆, 野上侑哉, 梅根紀代子, 増田健太, 植木有紗, 山上 亘, 平沢 晃, 進 伸幸, 青木大輔

    第20回日本家族性腫瘍学会学術集会  2014.6.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:福島  

    researchmap

  • 子宮体部・卵巣同時発生重複癌におけるDNAミスマッチ修復タンパクの免疫組織化学的染色による解析.

    山上 亘, 進 伸幸, 二宮委美, 和田美智子, 野村弘行, 片岡史夫, 平沢 晃, 冨永英一郎, 阪埜浩司, 青木大輔

    第55回日本臨床細胞学会総会  2014.6.5 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神奈川  

    researchmap

  • BRAC1/2遺伝子変異例における卵管上皮細胞のp53の特性に関する検討.

    赤羽智子, 冨永英一郎, 平沢 晃, 片岡史夫, 野村弘行, 増田健太, 阪埜浩司, 進 伸幸, 吉村泰典, 青木大輔

    第66回日本産科婦人科学会学術講演会  2014.4.18 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神奈川  

    researchmap

  • Drug Set Enrichment Analysis (DSEA): A Computational Approach to Identify Functional Drug Sets. International conference

    JP Mpindi, Bychkov D, Bhagwan Y, Malani D, Hirasawa A, Saeed K, Hultsch S, Kangaspeska S, Murumägi A, Heckman CA, Porkka K, Aittokallio T, Wennerberg K, stling, Kallioniemi O

    AACR Annual Meeting 2014  2014.4.5 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:San Diego  

    researchmap

  • Systematic high-throughput drug sensitivity and resistance testing (DSRT) of ovarian cancer cell lines indicates novel therapeutic possibilities with existing and emerging drugs. International conference

    Hirasawa A, Murumägi A, Bhagwan Y, JP Mpindi, Arjama M, Wennerberg K, Aittokallio T, Aoki D, Kallioniemi, O.Aittokallio T, Wennerberg K, stling, Kallioniemi O

    AACR Annual Meeting 2014  2014.4.5 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:San Diego  

    researchmap

  • 子宮体癌手術例における傍大動脈リンパ節のみへの単独転移例の病理学的検討.

    富里祥子, 山上 亘, 進 伸幸, 小林祐介, 野村弘行, 片岡史夫, 平沢 晃, 冨永英一郎, 阪埜浩司, 津田浩史, 青木大輔, 吉村泰典

    第123回関東連合産科婦人科学会総会・学術集会  2012.6.17 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 日本人の遺伝性乳がん卵巣がん(HBOC)症例に対するBRCA1/2遺伝子検査-遺伝子検査費用の軽減と高リスク群同定に関する研究-

    菅野康吉, 牧島恵子, 羽田恵梨, 青木幸恵, 小杉眞司, 平沢 晃, 青木大輔, 赤城 究, 櫻井晃洋, 野水 整, 田中屋宏爾, 増田春菜, 大住省三, 吉田輝彦, 和泉秀子, 清水千佳子

    第18回日本家族性腫瘍学会学術集会  2012.6.15 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:大阪  

    researchmap

  • 卵巣明細胞腺癌細胞におけるHNF1β蛋白発現解析.

    赤羽智子, 冨永英一郎, 平沢 晃, 青木大輔

    第53回日本臨床細胞学会総会  2012.6.1 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:千葉  

    researchmap

  • Risk assessment for BRCA1/2 mutations based on recursive partitioning analysis in Japanese HBOC cohort. Fourth International Symposium on Hereditary Breast and Ovarian Cancer. International conference

    Sugano K, Ando J, Sekiguchi I, Kamata H, Makishima K, Haneda E, Jinno H, Kitagawa Y, Hirasawa A, Aoki D, Shimizu C, Hojyo T, Kasamatsu T, Yoshida T

    Fourth International Symposium on Hereditary Breast and Ovarian Cancer.  2012.4.25 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:Montréal (Canada)  

    researchmap

  • 子宮体癌の再発を予測できる間質遺伝子の発現に基づいた卵巣癌症例のグループ化.

    井口蓉子, 津田浩史, 片岡史夫, 野村弘行, 千代田達幸, 平沢 晃, 冨永英一郎, 山上 亘, 進 伸幸, 青木大輔, 吉村泰典

    第64回日本産科婦人科学会学術講演会  2012.4.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神戸  

    researchmap

  • 子宮体部癌肉腫の癌部ではTGF-β-Smad2/3経路が活性化し上皮間葉転換(EMT)を期待している.

    千代田達幸, 津田浩史, 片岡史夫, 井口蓉子, 冨永英一郎, 平沢 晃, 山上 亘, 進 伸幸, 青木大輔, 吉村泰典

    第64回日本産科婦人科学会学術講演会  2012.4.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神戸  

    researchmap

  • 子宮体癌における抑制型T細胞と予後との関連性の検討.

    山上 亘, 進 伸幸, 野村弘行, 片岡史夫, 平沢 晃, 岩田 卓, 冨永英一郎, 阪埜浩司, 津田浩史, 青木大輔, 吉村泰典

    第64回日本産科婦人科学会学術講演会  2012.4.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神戸  

    researchmap

  • 子宮体癌においてDNA過剰メチル化により発現抑制される癌抑制遺伝子型microRNA miR-152の同定.

    鶴田智彦, 平沢 晃, 進 伸幸, 岩舘怜子, 高橋峰夫, 青木大輔, 吉村泰典

    第64回日本産科婦人科学会学術講演会  2012.4.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神戸  

    researchmap

  • 子宮体癌症例155例に対する子宮温存目的酢酸メドロキシプロゲステロン(MPA)療法の非成功例の検討-子宮摘出に至った37例を中心に-

    進 伸幸, 山上 亘, 市川義一, 野村弘行, 片岡史夫, 平沢 晃, 冨永英一郎, 鈴木 淳, 阪埜浩司, 津田浩史, 青木大輔, 吉村泰典

    第64回日本産科婦人科学会学術講演会  2012.4.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神戸  

    researchmap

  • 当科健康維持外来からみた「めまい」の現状.

    牧田和也, 橫田めぐみ, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔, 吉村泰典

    第26回日本女性医学学会学術集会  2011.11.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神戸  

    researchmap

  • 当科健康維持外来における潜在性甲状腺機能低下症に関する検討.

    橫田めぐみ, 牧田和也, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔, 吉村泰典

    第26回日本女性医学学会学術集会  2011.11.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神戸  

    researchmap

  • 婦人科遺伝性腫瘍の臨床における課題. Invited

    平沢 晃, 鶴田智彦, 青木大輔

    日本人類遺伝学会第56回大会(シンポジウム)  2011.11.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:千葉  

    researchmap

  • 当科健康維持外来受診者における大腿骨近位部骨密度の検討.

    牧田和也, 平沢 晃, 青木大輔

    第22回婦人科骨粗鬆症研究会学術集会  2011.11.10 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 上皮性卵巣癌における初回化学療法のprognostic marker としての血液毒性.

    野村弘行, 津田浩史, 片岡史夫, 田中京子, 千代田達幸, 山上 亘, 平沢 晃, 冨永英一郎, 進 伸幸, 青木大輔

    日本癌治療学会第49回学術集会  2011.10.27 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:名古屋  

    researchmap

  • STK11遺伝子陽性を示し子宮頸部分葉状頸管過形成を合併したPeutz-Jegher症候群の1例.

    赤羽智子, 平沢 晃, 小林佑介, 鶴田智彦, 阪埜浩司, 藤井多久磨, 進 伸幸, 菅野康吉, 青木大輔

    第50回日本臨床細胞学会秋期大会  2011.10.22 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • Lobular endocervical glandular hyperplasia found in a Peutz-Jeghers syndrome patient positive for STK11 mutation. International conference

    Hirasawa A, Akahane T, Tsuruta T, Banno K, Susumu N, Sugano K, Aoki D

    The 12th International Congress of Human Genetics and the American Society of Human Genetics 61st Annual Meeting.  2011.10.11  American Society of Human Genetics International Congress of Human Genetics

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Montreal (Canada)  

    researchmap

  • Kampo treatment for menopausal disorders. International conference

    Horiba Y, Makita K, Hirasawa A, Aoki D, Yoshimura Y

    The XXII Asian and Oceanic Congress of Obstetrics and Gynecology  2011.9.23 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Taipei (Taiwan)  

    researchmap

  • 子宮頸部に転移した尿路上皮癌の1例.

    冨永英一郎, 赤羽智子, 荒井ゆり子, 長島達男, 照井仁美, 平沢 晃, 進 伸幸, 青木大輔

    第25回日本臨床細胞学会関東連合学術集会  2011.9.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神奈川  

    researchmap

  • 大建中湯の長期内服が深部静脈血栓症発症後の下肢痛に有効であった1例.

    堀場裕子, 牧田和也, 橫田めぐみ, 平沢 晃, 岩田 卓, 青木大輔, 吉村泰典

    第31回産婦人科漢方研究会学術集会  2011.9.4 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:徳島  

    researchmap

  • Lobular endocervical glandular hyperplasia associated with STK11 mutation: report of a case of Peutz-Jeghers syndrome. International conference

    Hirasawa A, Akahane T, Tsuruta T, Banno K, Susumu N, Sugano K, Aoki D

    The 23rd European Congress of Pathology  2011.8.27 

     More details

    Presentation type:Poster presentation  

    Venue:Helsinki (Finland)  

    researchmap

  • 卵巣摘出術を施行した婦人科がんサーバイバーのQOL向上を目的とした環境因子および遺伝因子に関する検討. Invited

    平沢 晃, 牧田和也, 赤羽智子, 青木大輔

    第29回日本骨代謝学会学術集会(シンポジウム)  2011.7.30 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:大阪  

    researchmap

  • 子宮頸癌におけるウェルナー(WRN)遺伝子のエピジェネティックな発現抑制と抗癌剤感受性.

    増田健太, 阪埜浩司, 矢野倉恵, 小林佑介, 木須伊織, 植木有紗, 小野あすか, 平沢 晃, 進 伸幸, 青木大輔

    第50回日本婦人科腫瘍学会学術集会  2011.7.22 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:札幌  

    researchmap

  • 若年子宮体癌の妊孕性温存MPA療法はいつまで継続してよいか -G1腺癌88例の長期予後解析より-

    進 伸幸, 山上 亘, 市川義一, 小林佑介, 鶴田智彦, 野村弘行, 片岡史夫, 平沢 晃, 冨永英一郎, 鈴木 淳, 阪埜浩司, 津田浩史, 塚崎克己, 青木大輔

    第50回日本婦人科腫瘍学会学術集会  2011.7.22 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:札幌  

    researchmap

  • Lower uterine segment(LUS)から発生する子宮体癌とLynch症候群との関連.

    増田健太, 阪埜浩司, 矢野倉恵, 小林佑介, 植木有紗, 木須伊織, 野村弘行, 平沢 晃, 進 伸幸, 青木大輔

    遺伝医学合同学術集会2011  2011.6.16 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • 再帰的分割法による遺伝性乳がん卵巣がんのリスク評価.

    菅野康吉, 牧島恵子, 友田茉莉, 三須久美子, 平沢 晃, 武田祐子, 和泉秀子, 吉田輝彦

    遺伝医学合同学術集会2011  2011.6.16 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • 子宮体部漿液性腺癌術前診断の問題点.

    山上 亘, 進 伸幸, 小林佑介, 野村弘行, 片岡史夫, 平沢 晃, 冨永英一郎, 阪埜浩司, 津田浩史, 青木大輔, 吉村泰典

    第121回関東連合産科婦人科学会総会・学術集会  2011.6.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • Association between UGT1A1 Polymorphism and Adverse Events in Gynecological Patients Treated with Low-dose Irinotecan. International conference

    Hirasawa A, Akahane T, Tsuruta T, Nomura H, Susumu N, Tanigawara Y, Aoki D

    European Human Genetics Conference 2011  2011.5.28 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Amsterdam (Netherlands)  

    researchmap

  • 家系内の遺伝子検査が契機となり早期介入に至ったリンチ症候群の1例.

    中村加奈子, 平沢 晃, 赤羽智子, 鶴田智彦, 冨永英一郎, 阪埜浩司, 藤井多久磨, 進 伸幸, 青木大輔, 吉村泰典

    第357回日本産科婦人科学会東京地方部会例会  2011.2.19 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • Association between copy number variations of estorogen matabolism-related gene and bone mineral density in postmenopausal women of Japanese. International conference

    Hirasawa A, Makita K, Akahane T, Banno K, Susumu N, Aoki D

    1st Asia-Pacific Osteoporosis Meeting  2010.12.10 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Singapore  

    researchmap

  • がん臨床現場におけるファーマコゲノミクスの導入 Invited

    平沢 晃, 赤羽智子, 鶴田智彦, 野村弘行, 進 伸幸, 小崎健次郎, 谷川原祐介, 青木大輔

    第31回日本臨床薬理学会年会(シンポジウム)  2010.12.1 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:京都  

    researchmap

  • 子宮内膜細胞診検体を用いたエピジェネティックなDNA異常メチル化とその診断への応用.

    阪埜浩司, 小林佑介, 植木有紗, 木須伊織, 増田健太, 小野あすか, 野村弘行, 平沢 晃, 進 伸幸, 青木大輔

    第49回日本臨床細胞学会秋期大会  2010.11.21 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:兵庫  

    researchmap

  • 子宮体癌の子宮鏡検査と細胞診.

    照井仁美, 進 伸幸, 荒井ゆり子, 長島義男, 木須伊織, 平沢 晃, 阪埜浩司, 塚崎克己, 青木大輔

    第49回日本臨床細胞学会秋期大会  2010.11.21 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:兵庫  

    researchmap

  • 卵巣癌におけるHNF1β発現の組織特異性と臨床病理学的因子との関連.

    赤羽智子, 冨永英一郎, 平沢 晃, 進 伸幸, 青木大輔

    第49回日本臨床細胞学会秋期大会  2010.11.21 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:兵庫  

    researchmap

  • 閉経後の片頭痛患者の特徴に関する実態調査(第1報).

    牧田和也, 平沢 晃, 柴田 護, 清水利彦, 青木大輔, 鈴木則宏

    第38回日本頭痛学会総会  2010.11.19 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • Alleviation of Migraine Attack by Seasonal Switching of Kampo Drug in One Migraine Patient. International conference

    Horiba Y, Makita K, Hirasawa A, Matsumura S, Ogawa M, Iwata T, Deshimaru R, Yanamoto S, Aoki D

    The 2nd Asian Regional Conference for Headache meeting  2010.11.16 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Seoul (South Korea))  

    researchmap

  • 大腿骨頸部骨密度測定は腰椎骨密度測定の代用となり得るか?—当科健康維持外来受診者からの比較検討—.

    牧田和也, 松村聡子, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔

    第21回婦人科骨粗鬆症研究会  2010.11.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • プラチナ耐性卵巣癌に対する薬物療法の選択 —CPT-11およびPLD投与例の比較から-.

    野村弘行, 津田浩史, 片岡史夫, 千代田達幸, 平沢 晃, 冨永英一郎, 進 伸幸, 青木大輔

    第48回日本癌治療学会学術集会  2010.10.28 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:京都  

    researchmap

  • STK11遺伝子陽性Peutz-Jegher症候群例で発見された子宮頸部分葉状頸管腺過形成の1例.

    平沢 晃, 菅野康吉, 鶴田智彦, 小林佑介, 阪埜浩司, 進 伸幸, 三須久美子, 矢崎久妙子, 武田祐子, 青木大輔

    日本人類遺伝学会第55回大会  2010.10.27 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:埼玉  

    researchmap

  • A genome-wide association study identifies genetic variants in the gene A locus associated with endometriosis in Japanese.

    前佛 均, 宇野智子, 平沢 晃, 高橋篤, 久保充明, 赤羽智子, 青木大輔, 鎌谷直之, 平田公一, 中村祐輔

    日本人類遺伝学会第55回大会  2010.10.27 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:埼玉  

    researchmap

  • 子宮体癌両側卵巣摘出例における骨密度とESR1およびUGT2B17遺伝子コピー数多型との関連についての検討.

    平沢 晃, 牧田和也, 赤羽智子, 池ノ上学, 松村聡子, 堀場裕子, 岩田 卓, 小川真里子, 弟子丸亮太, 柳本茂久, 吉村泰典, 青木大輔

    第25回日本更年期医学会学術集会  2010.10.2 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:鹿児島  

    researchmap

  • 当科健康維持外来受診患者が初診時に訴える諸症状に関する検討.

    松村聡子, 牧田和也, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔

    第25回日本更年期医学会学術集会  2010.10.2 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:鹿児島  

    researchmap

  • 当科健康維持外来における更年期女性に対する漢方製剤の使用状況について.

    堀場裕子, 牧田和也, 平沢 晃, 岩田 卓, 小川真里子, 弟子丸亮太, 柳本茂久, 青木大輔

    第25回日本更年期医学会学術集会  2010.10.2 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:鹿児島  

    researchmap

  • シアリダーゼ発現の低下は卵巣癌腹膜播種形成を抑制しうる.

    野村弘行, 津田浩史, 片岡史夫, 千代田達幸, 平沢 晃, 冨永英一郎, 進 伸幸, 青木大輔

    第69回日本癌学会学術総会  2010.9.22 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:大阪  

    researchmap

  • 子宮体癌細胞株の機能的スクリーニングを用いたエピゲノム異常により発現抑制される癌抑制遺伝子型microRNAの同定.

    鶴田智彦, 小崎健一, 平沢 晃, 阪埜浩司, 進 伸幸, 井本逸勢, 青木大輔, 稲澤譲治

    第69回日本癌学会学術総会  2010.9.22 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:大阪  

    researchmap

  • Visual Analogue Scale(VAS)を用いた呉茱萸湯の片頭痛に対する治療効果の検討.

    堀場裕子, 牧田和也, 松村聡子, 平沢 晃, 青木大輔, 吉村泰典

    第30回産婦人科漢方研究会学術集会  2010.9.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:富山  

    researchmap

  • 卵巣明細胞腺癌におけるHNFβの発現特異性と臨床病理学的因子との関連に関する検討.

    赤羽智子, 冨永英一郎, 平沢 晃, 進 伸幸, 青木大輔

    第51回日本組織細胞化学会総会・学術集会  2010.9.4 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • Association of Genetic Variants of UGT1A1 Gene with Serum Bilirubin Level in the Japanese The 16th World Congress of Basic and Clinical Pharmacology International conference

    Hirasawa A, Akahane T, Tsuruta T, Nomura H, Saito K, Zama T, Tanigawara Y, Susumu N, Aoki D

    The 16th World Congress of Basic and Clinical Pharmacology.  2010.7.17 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Copenhagen (Denmark)  

    researchmap

  • Peutz-Jegher症候群に関する遺伝相談外来受診を契機として発見された子宮頸部分葉状頸管腺過形成の1例.

    平沢 晃, 鶴田智彦, 小林佑介, 阪埜浩司, 進 伸幸, 矢崎久妙子, 武田祐子, 菅野康吉, 青木大輔

    第16回日本家族性腫瘍学会学術集会  2010.7.9 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:新潟  

    researchmap

  • BRCA1/2の外来における遺伝子診断—産婦人科臨床の立場から-. Invited

    平沢 晃, 菅野康吉, 鶴田智彦, 阪埜浩司, 進 伸幸, 三須久美子, 矢崎久妙子, 武田祐子, 青木大輔

    第16回日本家族性腫瘍学会学術集会(シンポジウム)  2010.7.9 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:新潟  

    researchmap

  • リンパ節郭清範囲と化学療法内容は進行子宮体癌の予後へ影響を与えるか?.

    進 伸幸, 野村弘行, 平沢 晃, 阪埜浩司, 津田浩史, 青木大輔

    第48回婦人科腫瘍学会学術講演会  2010.7.8 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:茨城  

    researchmap

  • 腫瘍間質のVimentin陽性細胞のEGR-1発現は上皮性卵巣癌の予後と相関する.

    片岡史夫, 津田浩史, 西村貞子, 冨永英一郎, 野村弘行, 千代田達幸, 平沢 晃, 鈴木 淳, 進 伸幸, 青木大輔

    第48回婦人科腫瘍学会学術講演会  2010.7.8 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:茨城  

    researchmap

  • 若年子宮体癌G2類内膜癌4例に対する妊孕性温存黄体ホルモン療法の経験 — G2例に適応して良いか —.

    進 伸幸, 木須伊織, 植木有紗, 小林佑介, 秋好順子, 鶴田智彦, 野村弘行, 片岡史夫, 平沢 晃, 冨永英一郎, 鈴木 淳, 阪埜浩司, 津田浩史, 青木大輔

    第48回婦人科腫瘍学会学術講演会  2010.7.8 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:茨城  

    researchmap

  • 子宮体癌肺転移症例の解析による胸部X線検査の有用性.

    小林佑介, 阪埜浩司, 木須伊織, 岸見有紗, 松村聡子, 野村弘行, 平沢 晃, 進 伸幸, 塚崎克己, 青木大輔

    第48回婦人科腫瘍学会学術講演会  2010.7.8 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:茨城  

    researchmap

  • 進行期I期上皮性卵巣癌における予後因子の解析.

    野村弘行, 津田浩史, 片岡史夫, 千代田達幸, 鈴木 淳, 平沢 晃, 冨永英一郎, 進 伸幸, 青木大輔

    第48回婦人科腫瘍学会学術講演会  2010.7.8 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:茨城  

    researchmap

  • 遺伝相談外来を受診したBRCA1/2 遺伝子変異を有する遺伝性乳がん卵巣がん家系の臨床遺伝学的特徴.

    菅野康吉, 牧島恵子, 友田茉莉, 安藤二郎, 矢崎久妙子, 武田祐子, 平沢 晃, 神野浩光, 北川雄光, 和泉雅子, 古賀範子, 木下貴之

    第18回日本乳癌学会学術総会  2010.6.24 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:北海道  

    researchmap

  • Association between the UGT1A1 polymorphism, dyslipidemia and endometrial cancer risk. International conference

    Hirasawa A, Akahane T, Matsumura S, Tsuruta T, Banno K, Makita K, Susumu N, Aoki D

    European Human Genetics Conference 2010  2010.6.12 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Gothenburg (Sweden)  

    researchmap

  • 当科「健康維持外来」における塩酸ラロキシフェン発売以来今日までの使用状況についての検討.

    牧田和也, 平沢 晃, 松村聡子, 堀場裕子, 岩田 卓, 青木大輔

    第6回SERM学術研究会  2010.5.22 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 加味逍遥散投与,ホルモン補充療法の更年期障害に対する比較—精神神経症状評価スケール,症状推移からみた比較-

    更年期不定愁訴治療研究会

    第62回日本産科婦人科学会学術講演会  2010.4.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • sentinel navigation system(SNS)を用いて微小転移リンパ節を確認し得た子宮体癌4症例

    進 伸幸, 片岡史夫, 野村弘行, 平沢 晃, 阪埜浩司, 中原理紀, 竹内裕也, 亀山香織, 津田浩史, 栗林幸夫, 青木大輔, 吉村泰典

    第62回日本産科婦人科学会学術講演会  2010.4.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • 子宮体癌術後例における血清脂質値の特徴.

    松村聡子, 平沢 晃, 牧田和也, 堀場裕子, 小川真里子, 弟子丸亮太, 柳本茂久, 阪埜浩司, 進伸幸, 青木大輔, 吉村泰典

    第62回日本産科婦人科学会学術講演会  2010.4.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • 機能的スクリーングを用いたDNA過剰メチル化により発現抑制される子宮体癌新規癌抑制型miRNAの探索.

    鶴田智彦, 平沢 晃, 阪埜浩司, 進 伸幸, 小崎健一, 井本逸勢, 稲澤譲治, 青木大輔, 吉村泰典

    第62回日本産科婦人科学会学術講演会  2010.4.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • 再発子宮体癌症例に対するPlatinum free interval に基づいた治療戦略の検証.

    小林佑介, 阪埜浩司, 野村弘行, 岸見有紗, 小川誠司, 木須伊織, 市川義一, 平沢 晃, 進 伸幸, 塚崎克己, 青木大輔, 吉村泰典

    第62回日本産科婦人科学会学術講演会  2010.4.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • 子宮肉腫と子宮内膜癌の臨床的相違に関する検討.

    岸見有紗, 阪埜浩司, 小林佑介, 木須伊織, 小川誠司, 堀場裕子, 野村弘行, 平沢 晃, 進 伸幸, 塚崎克己, 青木大輔, 吉村泰典

    第62回日本産科婦人科学会学術講演会  2010.4.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • GNAS遺伝子の増幅は標準治療を施行した上皮性卵巣癌の独立した予後因子である.

    冨永英一郎, 津田浩史, 西村貞子, 千代田達幸, 野村弘行, 片岡史夫, 鈴木 淳, 平沢 晃, 進 伸幸, 青木大輔

    第62回日本産科婦人科学会学術講演会  2010.4.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • 腫瘍間質の遺伝子発現解析による進行上皮性卵巣癌の予後規定因子の同定.

    片岡史夫, 津田浩史, 西村貞子, 野村弘行, 千代田達幸, 平沢 晃, 冨永英一郎, 鈴木 淳, 進 伸幸, 青木大輔

    第62回日本産科婦人科学会学術講演会  2010.4.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • NBI(Narrow Band Imaging)システムを用いた軟性子宮鏡による子宮内膜病変の診断への応用.

    木須伊織, 阪埜浩司, 小林佑介, 小川誠司, 岸見有紗, 松村聡子, 山上 亘, 平沢 晃, 進 伸幸, 青木大輔, 吉村泰典

    第62回日本産科婦人科学会学術講演会  2010.4.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • Association between the UGT1A1 polymorphism, bilirubin levels, and dyslipidemia in endometrial cancer. International conference

    Matsumura S, Hirasawa A, Akahane T, Makita K, Tsuruta T, Banno K, Susumu N, Aoki D

    AACR/JCA Joint Conference 2010  2010.2.5 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Hawaii (USA)  

    researchmap

  • Genetic polymorphism involved in estrogen metabolism and endometrial cancer risk. International conference

    Hirasawa A, Akahane T, Matsumura S, Tsuruta T, Makita K, Banno K, Susumu N, Aoki D

    AACR/JCA Joint Conference 2010  2010.2.5 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Hawaii (USA)  

    researchmap

  • Functional screening of tumor-suppressive microRNAs silenced by DNA hypermethylation in endometrial cancer. International conference

    Tsuruta T, Kozaki k, Hirasawa A, Banno K, Susumu N, Imoto I, Aoki D, Inazawa J

    AACR/JCA Joint Conference 2010  2010.2.5 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Hawaii (USA)  

    researchmap

  • ファーマコゲノミクスの臨床応用を目指した新規遺伝子多型診断システムの確立. Invited

    平沢 晃, 松村聡子, 鶴田智彦, 赤羽智子, 野村弘之, 青木大輔, 谷川原祐介, 杉田哲佳, 緒方是嗣, 花房信博

    第30回日本臨床薬理学会年会(シンポジウム)  2009.12.3 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:神奈川  

    researchmap

  • 婦人科諸疾患における閉経前両側卵巣摘出術例の骨密度とFRAXの特徴.

    堀場裕子, 平沢 晃, 牧田和也, 松村聡子, 小川真里子, 岩田卓, 弟子丸亮太, 柳本茂久, 青木大輔

    第20回婦人科骨粗鬆症研究会  2009.11.14 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • ホルモン補充療法が腰椎骨密度に及ぼす長期的な効果の検討—当科健康維持外来における10年継続投与例からの検証—.

    牧田和也, 松村聡子, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔

    第20回婦人科骨粗鬆症研究会  2009.11.14 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 頭頸部腫瘍とmiRNA(1) —網羅的解析による喉頭腫瘍のmiRNAプロファイリング—.

    齋藤康一郎, 長西秀樹, 稲垣康治, 平沢 晃, 大久保啓介, 座間 猛

    第61回日本気管食道科学会学術講演会  2009.11.5 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神奈川  

    researchmap

  • 頭頸部腫瘍とmiRNA(2) —喉頭癌におけるバイオマーカーとしてのmiRNAs—.

    宇野光祐, 齋藤康一郎, 伊藤葉子, 椙田紀明, 中條聖子, 平沢 晃, 森, 長西秀樹, 稲垣康治, 大久保啓介, 座間 猛

    第61回日本気管食道科学会学術講演会  2009.11.5 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神奈川  

    researchmap

  • 頭頸部腫瘍とmiRNA(3) —喉頭癌の血中マーカー・治療標的としてのmiR-196a—.

    齋藤康一郎, 矢部はる奈, 稲垣康治, 長西秀樹, 平沢 晃, 伊藤葉子, 椙田紀明, 佐竹恵美子, 中條聖子, 大久保啓介, 座間 猛

    第61回日本気管食道科学会学術講演会  2009.11.5 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神奈川  

    researchmap

  • 子宮体部癌肉腫12例の細胞学的検討.

    荒井ゆり子, 照井仁美, 長島義男, 野村弘行, 平沢 晃, 阪埜浩司, 藤井多久磨, 進 伸幸, 塚崎克己, 青木大輔

    第48回日本臨床細胞学会秋期大会  2009.10.30 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:福岡  

    researchmap

  • 子宮内膜細胞診擬陽性検体におけるhMLH1異常メチル化は内膜癌の存在を示唆するか.

    木須伊織, 阪埜浩司, 小林佑介, 岸見有紗, 小川誠司, 平沢 晃, 進 伸幸, 塚崎克己, 長谷川寿彦, 青木大輔

    第48回日本臨床細胞学会秋期大会  2009.10.30 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:福岡  

    researchmap

  • Analysis of UGT1A1 *6,*27,*28 and *60polymorphism and serum bilirubin levels for individualized cancer therapy using irinotecan. International conference

    Hirasawa A, Akahane T, Tsuruta T, Kobayashi Y, Nomura H, Banno K, Saito K, Zama T, Tanigawara Y, Susumu N, Aoki D

    The 4th Asian Confernce on Pharmacoepidemiology  2009.10.23 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Tainan (Taiwan)  

    researchmap

  • 子宮体癌治療後腟再発症例の解析による腟細胞診検査の有用性についての検討.

    小林佑介, 阪埜浩司, 野村弘行, 小川誠司, 岸見有紗, 堀場裕子, 平沢 晃, 津田浩史, 進 伸幸, 塚崎克己, 青木大輔

    第46回日本癌治療学会学術総会  2009.10.22 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:神奈川  

    researchmap

  • 上皮性卵巣癌における後腹膜リンパ節郭清の意義についての検討.

    野村弘行, 津田浩史, 片岡史夫, 千代田達幸, 平沢 晃, 冨永英一郎, 鈴木 淳, 進伸幸, 青木大輔

    第46回日本癌治療学会学術総会  2009.10.22 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:神奈川  

    researchmap

  • Effects of UGT1A1 polymorphism on irinotecan-induced drug reaction and serum bilirubin levels. International conference

    Hirasawa A, Akahane T, Tsuruta T, Kobayashi Y, Nomura H, Banno K, Tsuda H, Saito K, Zama T, Tanigawara Y, Susumu N, Aoki D

    The 59th Annual Meeting of The American Society of Human Genetics  2009.10.20 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Hawaii(USA)  

    researchmap

  • FRAXの子宮体癌例への応用についての課題.

    平沢 晃, 牧田和也, 堀場裕子, 岩田 卓, 小川真理子, 弟子丸亮太, 柳本茂久, 阪埜浩司, 進 伸幸, 青木大輔

    第11回日本骨粗鬆症学会  2009.10.14 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:愛知  

    researchmap

  • Pitfalls in fertility-preserving high-dose medroxyprogesterone acetate (MPA) therapy for young patients with endometrial cancer - A retrospective study of 23 patients who subsequently underwent hysterectomy-. International conference

    Susumu N, Hirasawa A, Kobayashi Y, Tsuruta T, Ichikawa Y, Yamagami W, Nomura H, Kataoka F, Suzuki A, Banno K, Tsuda H, Aoki D

    International Meeting of the European Society of Gynaecological Oncology  2009.10.11 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Belgrade (Serbia)  

    researchmap

  • 当科「健康維持外来」における子宮体癌術後症例に認められる不定愁訴の検討.

    松村聡子, 牧田和也, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔

    第24回日本更年期医学会学術集会  2009.10.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:青森  

    researchmap

  • 閉経前両側卵巣摘出例の骨密度とFRAXを用いた骨折リスクの検討・評価とその有用性についての検討.

    堀場裕子, 平沢 晃, 牧田和也, 松村聡子, 小川真里子, 岩田 卓, 弟子丸亮太, 柳本茂久, 青木大輔

    第24回日本更年期医学会学術集会  2009.10.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:青森  

    researchmap

  • 当科「健康維持外来」におけるホルモン補充療法施行症例についての多角的検討.

    牧田和也, 松村聡子, 堀場裕子, 平沢 晃, 小川真里子, 弟子丸亮太, 柳本茂久, 高松 潔, 青木大輔

    第24回日本更年期医学会学術集会  2009.10.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:青森  

    researchmap

  • 遺伝性乳がん卵巣がんに対する予防的卵巣摘出術施行に伴う課題の検討.

    平沢 晃, 牧田和也, 堀場裕子, 松村聡子, 鶴田智彦, 小川真里子, 柳本茂久, 弟子丸亮太, 菅野康吉, 青木大輔

    第24回日本更年期医学会学術集会  2009.10.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:青森  

    researchmap

  • 老人性腟炎に対するエストリール製剤の効果における年齢別検討.

    弟子丸亮太, 牧田和也, 箕輪昌子, 渡辺英明, 堀場裕子, 松村聡子, 三上佳子, 小川真里子, 柳本茂久, 平沢 晃, 高橋峰夫, 青木大輔

    第24回日本更年期医学会学術集会  2009.10.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:青森  

    researchmap

  • 当科更年期外来受診患者における動脈硬化性疾患の危険因子に関する検討.

    柳本茂久, 牧田和也, 堀場 裕子, 平沢 晃, 田島博人, 金田佳史, 伊藤仁彦, 高松潔, 青木大輔

    第24回日本更年期医学会学術集会  2009.10.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:青森  

    researchmap

  • 子宮体癌細胞株の機能的スクリーニングを用いたエピゲノム異常により発現抑制される癌抑制遺伝子型microRNAの探索.

    鶴田智彦, 小崎健一, 平沢 晃, 阪埜浩司, 進 伸幸, 井本逸勢, 青木大輔, 稲澤譲治

    第68回日本癌学会総会  2009.10.1 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神奈川  

    researchmap

  • 子宮体癌における腹腔細胞診の臨床的意義と新規診断マーカーの検索.

    冨永英一郎, 進 伸幸, 赤羽智子, 山上亘, 東口敦司, 平沢 晃, 青木大輔

    第50回日本組織細胞化学会総会  2009.9.26 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:滋賀  

    researchmap

  • 子宮体癌におけるTリンパ球浸潤と臨床病理学的因子の検討.

    山上 亘, 進 伸幸, 田中英雄, 野村弘行, 片岡史夫, 平沢 晃, 冨永英一郎, 阪埜浩司, 津田浩史, 吉村泰典, 青木大輔

    第50回日本組織細胞化学会総会  2009.9.26 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:滋賀  

    researchmap

  • UGT1A1遺伝子多型と血清ビリルビン値およびイリノテカンの有害事象に関するゲノム薬理学的検討.

    平沢 晃, 赤羽智子, 鶴田智彦, 小林佑介, 阪埜浩司, 進 伸幸, 谷川原祐介, 青木大輔

    日本人類遺伝学会第54回大会  2009.9.24 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:東京  

    researchmap

  • 子宮頸癌細胞におけるWRN遺伝子のエピジェネティックな発現低下と抗癌剤感受性との関連.

    阪埜浩司, 矢野倉恵, 小林佑介, 小川誠司, 岸見有紗, 野村弘行, 平沢 晃, 進 伸幸, 塚崎克己, 青木大輔

    第27回日本ヒト細胞学会学術集会  2009.8.22 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 卵巣癌3rd line化学療法の効果予測因子の検討.

    千代田達幸, 津田浩史, 野村弘行, 片岡史夫, 冨永英一郎, 鈴木 淳, 平沢 晃, 山上 亘, 進 伸幸, 青木大輔

    第46回日本婦人科腫瘍学会学術集会  2009.7.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:新潟  

    researchmap

  • 産婦人科受診者を対象としたBRCA1およびBRCA2遺伝子解析とサーべイランスに関する検討.

    堀場裕子, 平沢 晃, 鶴田智彦, 小林佑介, 阪埜浩司, 武田祐子, 進 伸幸, 菅野康吉, 青木大輔

    第46回日本婦人科腫瘍学会学術集会  2009.7.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:新潟  

    researchmap

  • 子宮体癌治療後腟再発症例の解析による腟壁部分切除の意義についての検討.

    小林佑介, 阪埜浩司, 野村弘行, 堀場裕子, 平沢 晃, 進 伸幸, 塚崎克己, 青木大輔

    第46回日本婦人科腫瘍学会学術集会  2009.7.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:新潟  

    researchmap

  • 子宮体がんにおけるマイクロRNAの発現プロファイリング.

    平沢 晃, 齋藤康一郎, 赤羽智子, 伊藤葉子, 椙田紀明, 中條聖子, 進 伸幸, 青木大輔, 座間 猛

    第46回日本婦人科腫瘍学会学術集会  2009.7.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:新潟  

    researchmap

  • 腫瘍-間質相互作用に着目した上皮性卵巣癌標準治療の効果予測システムの構築.

    片岡史夫, 津田浩史, 冨永英一郎, 西村貞子, 平沢 晃, 野村弘行, 千代田達之, 鈴木淳, 進伸幸, 青木大輔

    第46回日本婦人科腫瘍学会学術集会  2009.7.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:新潟  

    researchmap

  • 子宮体癌腹腔細胞診の臨床的意義.

    冨永英一郎, 進 伸幸, 平沢 晃, 赤羽智子, 長島義男, 照井仁美, 青木大輔

    第50回日本臨床細胞学会総会  2009.6.26 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • アレイCGHによる子宮体癌関連遺伝子および薬剤感受性遺伝子の探索.

    鶴田智彦, 平沢 晃, 赤羽智子, 山上 亘, 阪埜浩司, 井本逸勢, 稲澤譲治, 進 伸幸, 青木大輔

    第50回日本臨床細胞学会総会  2009.6.26 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 子宮体癌治療後経過観察における腟細胞診検査の有用性についての検討.

    小林佑介, 阪埜浩司, 野村弘行, 三上佳子, 山上 亘, 平沢 晃, 津田浩史, 進 伸幸, 塚崎克己, 青木大輔

    第50回日本臨床細胞学会総会  2009.6.26 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • FISH法の子宮体癌への臨床応用—癌診断と治療効果判定—.

    進 伸幸, 平沢 晃, 阪埜浩司, 青木大輔

    第50回日本臨床細胞学会総会  2009.6.26 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 当科健康維持外来患者におけるWHO骨折リスク評価ツール(FRAX)の有用性に関する検討.

    堀場裕子, 平沢 晃, 牧田和也, 弟子丸亮太, 柳本茂久, 野村弘行, 片岡史夫, 岩田 卓, 冨永英一郎, 堀口 文, 青木大輔, 吉村泰典

    第117回日本産科婦人科学会関東連合地方部会学術集会  2009.6.14 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 遺伝性乳がん卵巣がんの遺伝カウンセリング広報活動報告.

    矢崎久妙子, 武田祐子, 平沢 晃, 菅野康吉

    第15回日本家族性腫瘍学会学術集会  2009.6.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 新アムステルダムクライテリアを満たす子宮体癌の頻度と臨床的特徴.

    阪埜浩司, 小林佑介, 平沢 晃, 進 伸幸, 長谷川清志, 宇田川康博, 大和田倫孝, 平井康夫, 青木大輔

    第15回日本家族性腫瘍学会学術集会  2009.6.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 子宮体部・卵巣同時性重複癌31例に対する臨床病理学的検討.

    小林佑介, 阪埜浩司, 野村弘行, 平沢 晃, 津田浩史, 進 伸幸, 塚崎克己, 青木大輔

    第15回日本家族性腫瘍学会学術集会  2009.6.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • BRCA1/2陽性例における卵巣がんサーべイランスおよび予防的卵巣摘出術に関する検討. Invited

    平沢 晃, 菅野康吉, 鶴田智彦, 小林佑介, 阪埜浩司, 進 伸幸, 矢崎久妙子, 武田祐子, 青木大輔

    第15回日本家族性腫瘍学会学術集会(シンポジウム)  2009.6.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:東京  

    researchmap

  • 日本人の遺伝性腫瘍に関するエビデンスの構築 -研究から医療への展開—.

    菅野康吉, 牧島恵子, 友田茉莉, 矢崎久妙子, 平沢 晃, 武田祐子, 和泉秀子, 牛尼美年子, 吉田輝彦

    第15回日本家族性腫瘍学会学術集会  2009.6.12 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 喉頭癌におけるマイクロRNA-4.バイオマーカーとしての血液循環マイクロRNA

    長西秀樹, 齋藤康一郎, 伊藤葉子, 椙田紀明, 佐竹恵美子, 中條聖子, 大久保 啓介, 稲垣康治, 矢部はる奈, 平沢 晃, 座間 猛

    第33回日本頭頸部癌学会  2009.6.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:北海道  

    researchmap

  • 喉頭癌におけるマイクロRNA-1.網羅的解析による発現プロファイリング.

    齋藤康一郎, 伊藤葉子, 椙田紀明, 中條聖子, 長西秀樹, 大久保啓介, 稲垣康治, 平沢 晃, 座間 猛

    第33回日本頭頸部癌学会  2009.6.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:北海道  

    researchmap

  • 喉頭癌におけるマイクロRNA-2.喉頭癌におけるバイオマーカーとしてのマイクロRNAs

    宇野光祐, 齋藤康一郎, 伊藤葉子, 椙田紀明, 中條聖子, 長西秀樹, 大久保啓介, 稲垣康治, 平沢 晃, 座間 猛

    第33回日本頭頸部癌学会  2009.6.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:北海道  

    researchmap

  • 喉頭癌におけるマイクロRNA-3.新たな治療標的としてのマイクロRNA.

    稲垣康治, 齋藤康一郎, 長西秀樹, 大久保啓介, 赤羽智子, 平沢 晃, 座間 猛

    第33回日本頭頸部癌学会  2009.6.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:北海道  

    researchmap

  • Pharmacogenomic effects of UDP-glucuronosyltransferase 1A1 on irinotecan-induced drug reaction and serum bilirubin levels. International conference

    Hirasawa A, Akahane T, Tsuruta T, Nomura H, Banno K, Tsuda H, Saito K, Zama T, Tanigawara Y, Susumu N, Aoki D

    2009 European Human Genetics Conference  2009.5.23 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Vienna (Austria)  

    researchmap

  • 成人に発症する遺伝性腫瘍に対する遺伝カウンセリングとがん予防.

    菅野康吉, 牧島恵子, 友田茉莉, 矢崎久妙子, 平沢 晃, 武田祐子, 和泉秀子, 牛尼美年子, 吉田輝彦

    第33回日本遺伝カウンセリング学会学術集会  2009.5.22 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:兵庫  

    researchmap

  • 当科更年期外来における塩酸ラロキシフェン使用の現状—子宮体癌術後症例を中心に-

    牧田和也, 堀場裕子, 岩田 卓, 平沢 晃, 片岡史夫, 冨永英一郎, 堀口 文, 青木大輔

    第5回SERM学術研究会  2009.5.9 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • MicroRNA expression signature reveals putative diagnostic biomarkers for laryngeal cancer. International conference

    Saito K, Okubo K, Naganishi H, Inagaki K, Hirasawa A, Zama T

    The Annual Meeting of the American Association for Cancer Research 100th Annual Meeting  2009.4.18 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Denver (USA)  

    researchmap

  • FRAXを用いた産婦人科諸疾患における骨折リスク評価の検討.

    堀場裕子, 平沢 晃, 牧田和也, 弟子丸亮太, 柳本茂久, 野村弘行, 片岡史夫, 岩田卓, 冨永英一郎, 堀口 文, 青木大輔, 吉村泰典

    第61回日本産科婦人科学会学術講演会  2009.4.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:京都  

    researchmap

  • UGT1A1遺伝子多型とイリノテカンの有害事象およびグルクロン酸抱合能に関するゲノム薬理学的検討.

    平沢 晃, 赤羽智子, 野村弘行, 阪埜浩司, 津田浩史, 齋藤康一郎, 座間 猛, 後田奈緒美, 谷川原祐介, 進 伸幸, 青木大輔, 吉村泰典

    第61回日本産科婦人科学会学術講演会  2009.4.3 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • 若年体癌症例に対する子宮温存目的酢酸メドロキシプロゲステロン(MPA)療法のpitfall —子宮摘出に至った21症例における子宮体病変の検討より-.

    進 伸幸, 平沢 晃, 鶴田智彦, 市川義一, 末盛友浩, 山上 亘, 片岡史夫, 鈴木 淳, 阪埜浩司, 津田浩史, 青木大輔, 吉村泰典

    第61回日本産科婦人科学会学術講演会  2009.4.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:京都  

    researchmap

  • 標準治療を受けた表層上皮性卵巣癌の再発リスクを規定する遺伝子の探索.

    冨永英一郎, 津田浩史, 西村貞子, 千代田達幸, 野村弘行, 片岡史夫, 鈴木 淳, 平沢 晃, 進 伸幸, 青木大輔, 吉村泰典

    第61回日本産科婦人科学会学術講演会  2009.4.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:京都  

    researchmap

  • Aurora-A si-RNAはin vivoにおける子宮体癌細胞に対するタキサン製剤の抗腫瘍効果を増強する.

    矢野倉恵, 阪埜浩司, 小林佑介, 三上佳子, 平沢 晃, 進 伸幸, 塚崎克己, 青木大輔, 吉村泰典

    第61回日本産科婦人科学会学術講演会  2009.4.3 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:京都  

    researchmap

  • 結合型エストロゲン製剤を用いたホルモン補充療法の腰椎骨密度に対する長期的な効果の検討—当科更年期外来における継続投与10年例の結果から−.

    牧田和也, 堀場 裕子, 平沢 晃, 岩田卓, 冨永英一郎, 堀口 文, 青木大輔

    第9回東京骨・カルシウム・ホルモン代謝研究会  2008.12.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • ゲノム薬理学に基づいたがん個別化治療戦略

    HIRASAWA AKIRA

    抗がん剤ゲノム講演会  2008.12.10 

     More details

    Presentation type:Oral presentation (general)  

    Venue:栃木  

    researchmap

  • UGT1A1遺伝子多型と血清ビリルビン値の関連 および婦人科イリノテカン療法副作用への関与に関する検討

    HIRASAWA AKIRA

    第29回日本臨床薬理学会  2008.12.4 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 子宮体癌術後例における血清脂質値と骨密度の特徴に関する検討

    HIRASAWA AKIRA

    第116回日本産科婦人科学会関東連合地方部会  2008.11.29 

     More details

    Presentation type:Oral presentation (general)  

    Venue:宇都宮  

    researchmap

  • 当科「健康維持外来」の現状―更年期外来から女性のトータルヘル スケア外来への転換―

    HIRASAWA AKIRA

    第23回日本更年期医学会学術集会  2008.11.15 

     More details

    Presentation type:Oral presentation (general)  

    Venue:横浜  

    researchmap

  • 当科健康維持外来受診者におけるFRAXによる骨折リスク評価の検討

    HIRASAWA AKIRA

    第23回日本更年期医学会学術集会  2008.11.15 

     More details

    Presentation type:Oral presentation (general)  

    Venue:横浜  

    researchmap

  • 卵巣境界悪性腫瘍における腹腔細胞診疑陽性症例の検討.

    片岡史夫, 津田浩史, 千代田達幸, 山上 亘, 野村弘行, 平沢 晃, 冨永英一郎, 鈴木 淳, 進 伸幸, 青木大輔

    第47回日本臨床細胞学会秋期大会  2008.11.14 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 閉経後骨粗鬆症に対する予防的治療を行う際の薬剤選択に関する再検証

    HIRASAWA AKIRA

    第19回婦人科骨粗鬆症研究会学術集会  2008.11.8 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • FRAXを用いた骨折リスク評価における子宮体癌例の特徴

    HIRASAWA AKIRA

    第19回婦人科骨粗鬆症研究会学術集会(ワークショップ)  2008.11.8 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 再発子宮体癌における白金製剤反復投与の意 義とputinum free intervalに関する検討

    HIRASAWA AKIRA

    第46回日本癌治療学会学術総会(ワーク ショップ)  2008.10.30 

     More details

    Presentation type:Oral presentation (general)  

    Venue:名古屋  

    researchmap

  • 再発卵巣癌に対する治療戦略 ―卵巣癌初回治療後のサーべーランスの 観点から-

    HIRASAWA AKIRA

    第46回日本癌治療学会学術総会(ワーク ショップ)  2008.10.30 

     More details

    Presentation type:Oral presentation (general)  

    Venue:名古屋  

    researchmap

  • エピジェネティック異常により発現抑制される子宮体がん関連癌抑制遺 伝子のMPA療法における役割

    HIRASAWA AKIRA

    第67回日本癌学会学術総会(ワークショップ)  2008.10.28 

     More details

    Presentation type:Oral presentation (general)  

    Venue:名古屋  

    researchmap

  • 標準治療を施行した進行上皮性卵巣癌の予後因子の網羅的解析

    HIRASAWA AKIRA

    第67回日本癌学会学術総会(ワークショップ)  2008.10.28 

     More details

    Presentation type:Oral presentation (general)  

    Venue:名古屋  

    researchmap

  • Analysis of UGT1A1 polymorphism and serum bilirubin levels for individualized cancer therapy using irinotecan. Invited

    Hirasawa A, Akahane T, Yamagami W, Nomura H, Banno K, Tsuda H, Naganishi H, Okubo K, Saito K, Zama T, Tanigawara Y, Susumu N, Aoki D

    67th Annual meeting of the Japanese cancer assosiation  2008.10.28 

     More details

    Language:English   Presentation type:Oral presentation (invited, special)  

    Venue:Nagoya (Japan)  

    researchmap

  • 塩酸イリノテカンによるがん個別化治療を目 指したUGT1A1遺伝子多型と血清ビリルビン値に関する検討

    HIRASAWA AKIRA

    第67回日本癌学会学術総会(シンポジウム)  2008.10.28 

     More details

    Presentation type:Oral presentation (general)  

    Venue:名古屋  

    researchmap

  • 当科更年期外来における更年期不定愁訴に対する漢方製剤の使用状況について —8年前の調査結果との比較検討—

    HIRASAWA AKIRA

    第28回産婦人科漢方研究会学術集会  2008.9.21 

     More details

    Presentation type:Oral presentation (general)  

    Venue:宇都宮  

    researchmap

  • 遺伝性乳がん・卵巣がんの遺伝子検査実施後の状況と遺伝相談外来の役割

    HIRASAWA AKIRA

    第14回日本家族性腫瘍学会学術集会  2008.6.20 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 遺伝相談外来の役割を考える-遺伝相談外来の受診がHNPCC患者とその同胞のがん予防を促すきっかけとなった一事例-

    HIRASAWA AKIRA

    第14回日本家族性腫瘍学会学術集会  2008.6.20 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 若年子宮体癌類内膜癌G2症例4例の妊孕性温存黄体ホルモン療法

    HIRASAWA AKIRA

    第115回日本産科婦人科学会関東連合地方部会・学術集会  2008.6.15 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • カウンセリングを必要とした閉経期女性の態度および行動

    HIRASAWA AKIRA

    第49回日本心身医学会学術講演会  2008.6.12 

     More details

    Presentation type:Oral presentation (general)  

    Venue:札幌  

    researchmap

  • 子宮体癌における腹腔細胞診の意義

    HIRASAWA AKIRA

    第49回日本臨床細胞学会総会学術集会  2008.6.7 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 当科更年期外来における塩酸ラロキシフェンの使用状況について

    HIRASAWA AKIRA

    第4回SERM学術研究会学術集会  2008.5.10 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 塩酸イリノテカン個別化治療の確立を目指したUGT1A1遺伝子多型解析

    HIRASAWA AKIRA

    第60回 日本産科婦人科学会総会・学術講演会  2008.4.12 

     More details

    Presentation type:Oral presentation (general)  

    Venue:横浜  

    researchmap

  • 遺伝性乳癌卵巣癌の可能性がある受診者を対象としたBRCA1およびBRCA2遺伝子解析

    HIRASAWA AKIRA

    第60回 日本産科婦人科学会総会・学術講演会  2008.4.12 

     More details

    Presentation type:Oral presentation (general)  

    Venue:横浜  

    researchmap

  • Association of Genetic Variants of UDP-glucuronosyltransferase 1A1 Gene with Serum Bilirubin Level in the Japanese. International conference

    Hirasawa A, Tsuruta T, Nomura H, Kataoka F, Tominaga E, Banno K, Suzuki A, Tsuda H, Naganishi H, Saito K, Zama T, Tanigawara Y, Susumu N, Aoki D

    2008 International Conference on Pharamagogenomics  2008.4.9 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Busan (Korea)  

    researchmap

  • ゲノム情報に基づいたがん化学療法の個別化治療戦略

    HIRASAWA AKIRA

    Gynecologic Cancer Symposium III  2008.2.2 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 下谷医師会月経に伴う女性の諸症状とその対策

    HIRASAWA AKIRA

    下谷医師会学術講演会  2008.1.23 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • Investigation of serum lipids in patients with postmenopausal osteoporosis and decreased bone mass. International conference

    Horiba Y, Makita K, Hirasawa A, Tominaga E, Horiguchi F, Aoki D

    The 16th Asian Pacific Congress of Cardiology  2007.12.13 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Taipei (Taiwan)  

    researchmap

  • Lipid metabolism in patients with endometrial cancer. The 16th Asian Pacific Congress of Cardiology. International conference

    Hirasawa A, Horiba Y, Tominaga E, Banno K, Makita K, Susumu N, Horiguchi F, Aoki D

    The 16th Asian Pacific Congress of Cardiology  2007.12.13 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Taipei (Taiwan)  

    researchmap

  • 当科更年期外来にて診断し得た骨粗鬆症/骨量減少症における低エストロゲン血症以外の危険因子の検討

    HIRASAWA AKIRA

    第8回東京 骨・カルシウム・ホルモン代謝研究会  2007.12.8 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • ヒトモノクローナル抗体HMMC-1の子宮体癌細胞に対する増殖抑制効果の検討

    HIRASAWA AKIRA

    第46回日本臨床細胞学会秋期大会  2007.11.30 

     More details

    Presentation type:Oral presentation (general)  

    Venue:仙台  

    researchmap

  • UGT1A1遺伝子多型解析およびハプロタイプの血清総ビリルビン値への関与

    HIRASAWA AKIRA

    第28回日本臨床薬理学会年会  2007.11.28 

     More details

    Presentation type:Oral presentation (general)  

    Venue:宇都宮  

    researchmap

  • 当科更年期外来受診者における動脈硬化性疾患の危険因子に関する検討

    HIRASAWA AKIRA

    第22回日本更年期医学会学術集会  2007.11.17 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 子宮体癌症例における脂質代謝動態に関する検討

    HIRASAWA AKIRA

    第22回日本更年期医学会学術集会  2007.11.17 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 「ホルモン療法をいつまで行い、どういう形で終わらせるのがベターか?」—当科更年期外来での実例からの一考察

    HIRASAWA AKIRA

    第22回日本更年期医学会学術集会  2007.11.17 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 子宮体がん術後患者における骨代謝動態に関する検討

    HIRASAWA AKIRA

    第18回婦人科骨粗鬆症研究会学術集会  2007.11.3 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 当科更年期外来受診者によるアレンドロネート製剤のweekly投与への切り替えの状況

    HIRASAWA AKIRA

    第18回婦人科骨粗鬆症研究会学術集会  2007.11.3 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • Analysis of haplotype structures of UGT1A1 gene complex; For individualized cancer therapy using irinotecan hydrochloride.

    Hirasawa A, Tsuruta T, Higashiguchi A, Susumu N, Goda N, Tanigawara Y, Aoki D

    21st Century Center of Exellence (COE) program, Keio University International Symposium 2007  2007.10.27 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:Tokyo (Japan)  

    researchmap

  • 子宮体癌における高用量MPA療法の効果と再発危険因子の解析

    HIRASAWA AKIRA

    第45回日本癌治療学会総会  2007.10.24 

     More details

    Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • 進行子宮体癌の再発・予後因子としてのCOX-2とCD8陽性リンパ球についての検討

    HIRASAWA AKIRA

    第45回日本癌治療学会総会  2007.10.24 

     More details

    Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • 季節による漢方製剤の切り替えが片頭痛発作の軽減に有効であった1例

    HIRASAWA AKIRA

    第27回産婦人科漢方研究会学術集会  2007.9.9 

     More details

    Presentation type:Oral presentation (general)  

    Venue:大阪  

    researchmap

  • 再発子宮体癌における腫瘍マーカー測定の意義に関する検討

    HIRASAWA AKIRA

    第42回日本婦人科腫瘍学会学術集会 ワークショップ  2007.6.28 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • HNF-1b(hepatocyte nuclear factor-1b)の明細胞腺癌診断マーカーおよび予後因子としての有用性

    HIRASAWA AKIRA

    第42回日本婦人科腫瘍学会学術集会 シンポジウム  2007.6.28 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 婦人科外来受診者を対象としたBRCA1/2遺伝子変異陽性例に関する検討

    HIRASAWA AKIRA

    第13回日本家族性腫瘍学会学術集会  2007.6.15 

     More details

    Presentation type:Oral presentation (general)  

    Venue:高知  

    researchmap

  • 日本人におけるBRCA1およびBRCA2遺伝子の全塩基配列直接解析法による基礎データ収集と、家族性乳がん・卵巣がんを対象とした易罹患性検査としての有用性に関する検討

    HIRASAWA AKIRA

    第13回日本家族性腫瘍学会学術集会  2007.6.15 

     More details

    Presentation type:Oral presentation (general)  

    Venue:高知  

    researchmap

  • 家族性腫瘍としての子宮体癌 –その病態と臨床的特徴について-

    HIRASAWA AKIRA

    第13回日本家族性腫瘍学会学術集会  2007.6.15 

     More details

    Presentation type:Oral presentation (general)  

    Venue:高知  

    researchmap

  • ゲノム診断に基づいた婦人科がん個別化医療の確立

    平沢 晃

    研究推進センターによる研究者助成制度 2006年度採択者による研究発表会  2007.6.7 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 子宮体癌における術前腫瘍マーカー測定の意義

    HIRASAWA AKIRA

    第113回日本産科婦人科学会関東連合地方部会総会・学術集会  2007.6.3 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 血管運動症状がSERM療法を選択する際に及ぼす影響についての基礎的検討(第3報)—閉経後骨量減少例の更なる検証-

    HIRASAWA AKIRA

    第3回SERM学術研究会学術集会  2007.5.12 

     More details

    Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • Usefulness of HNF-1b as an immunocytochemical diagnostic marker of ovarian clear cell adenocarcinoma in ascites specimens. International conference

    Higashiguchi A, Suzuki A, Hirasawa A, Tamada Y, Susumu N, Suzuki N, Aoki D, Sakamoto M

    The 7th joint meeting of the Japan Society of histochemistry and cytochemistry and the histochemical society  2006.8.23 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Hawaii (USA)  

    researchmap

  • Safety of long-term GnRH agonist therapy in combination with resedronate: analysis of patient compliance to the combined medication. International conference

    Ishitani K, Ohta H, KATO N, Yamamoto A, Ueno K, Hirasawa A, Yamashita H, Arai H

    The XIXth Asian and Oceanic Congress of Obstetrics & Gynecology  2005.10.1 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:Seoul (South Korea)  

    researchmap

  • Clinical Characteristics of clear cell adenocarcinomas of ovary International conference

    Hirasawa A, Kato N, Yamamoto A, Ueno K, Ishitani K, Yamashita H, Tanaka J, Arai H

    The XIXth Asian and Oceanic Congress of Obstetrics & Gynecology  2005.10.1 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:Seoul (South Korea)  

    researchmap

  • Evaluation of para-aortic lymphadenectomy in endometrial cancer. International conference

    Yamamoto A, Hirasawa A, Tanaka J, Kato N, Ueno K, Ishitani K, Yamashita H, Arai H

    The XIXth Asian and Oceanic Congress of Obstetrics & Gynecology  2005.10.1 

     More details

    Presentation type:Oral presentation (general)  

    Venue:Seoul (South Korea)  

    researchmap

  • Amplification and consequent overexpression of PDZK1 within the 1q12-q22 amplicon is associated with drug-resistance phenotype in multiple myeloma. International conference

    Inazawa J, Otsuki T, Hirasawa A, Imoto I, Yoshinobu M, Shimizu S, Taniwaki M, Inoue J

    The 2004 Annual Meeting of the American Association for Cancer Research  2004.3.27 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Orlando (USA)  

    researchmap

  • Possible involvement of overexpressed wild-type BRAF in the growth of malignant melanoma cell lines. International conference

    Imoto I, Tanami H, Hirasawa A, Yuki Y, Sonoda I, Inoue J, Yasui K, Misawa-Furihata A, Kawakami Y, Inazawa J

    The 2004 Annual Meeting of the American Association for Cancer Research  2004.3.27 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Orlando (USA)  

    researchmap

  • 遺伝性腫瘍としての子宮内膜癌の頻度と病態に関する解析 Invited

    阪埜浩司, 進 伸幸, 平尾 健, 岩田 卓, 平沢 晃, 青木大輔, 菅野康吉, 野澤志朗

    第62回日本癌学会総会  2003.9.25 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:愛知県名古屋市  

    researchmap

  • 子宮体癌におけるhMLH1遺伝子プロモーター領域のメチル化プロファイルの検討 Invited

    平沢 晃, 菅野康吉, 宮倉安幸, 阪埜浩司, 進 伸幸, 青木大輔, 野澤志朗, 坂本 優, 五十嵐誠治

    第62回日本癌学会総会  2003.9.25 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:愛知県名古屋市  

    researchmap

  • 17q増幅標的遺伝子PPM1Dの発現と卵巣明細胞癌 Invited

    斎藤(小原, 深美子, 平沢 晃, 津田 均, 井本逸勢, 青木大輔, 進 伸幸, 野澤志朗, 稲澤譲治

    第62回日本癌学会総会  2003.9.25 

     More details

    Language:Japanese   Presentation type:Oral presentation (invited, special)  

    Venue:愛知県名古屋市  

    researchmap

  • 子宮体癌におけるMicrosatellite Instability(MSI)の検出に免疫組織化学は有用か?

    進 伸幸, 青木大輔, 阪埜浩司, 平尾 健, 平沢 晃, 岩田 卓, 鈴木 直, 菅野康吉, 向井萬起男, 野澤志朗

    第34回日本婦人科腫瘍学会・学術集会  2003.7.10 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:京都  

    researchmap

  • CGH法を用いた卵巣明細胞腺癌ゲノム異常の網羅的解析と標的遺伝子の検索

    平沢 晃, 青木大輔, 進 伸幸, 井本逸勢, 稲澤譲治, 野澤志朗

    第34回日本婦人科腫瘍学会・学術集会  2003.7.10 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:京都  

    researchmap

  • ワークショップ.家族性腫瘍における女性の腫瘍 子宮体癌におけるマイクロサテライト不安定性とhMLH1プロモーター領域のメチル化に関する検討

    平沢 晃, 菅野康吉, 宮倉安幸, 山内絵里, 市川 明, 阪埜 浩司, 進 伸幸, 青木大輔, 野澤志朗, 小屋松安子, 坂本 優, 関口 勲, 鎌田裕之, 五十嵐誠治

    第9回家族性腫瘍研究会学術集会  2003.6.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • ワークショップ.遺伝性腫瘍としての子宮内膜癌の頻度と病態に関する解析

    阪埜浩司, 進 伸幸, 平尾 健, 岩田 卓, 平沢 晃, 青木大輔, 菅野康吉, 野澤志朗

    第9回家族性腫瘍研究会学術集会  2003.6.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:東京  

    researchmap

  • 遺伝性子宮内膜癌の病態に関する分子免疫学的検討

    阪埜浩司, 進 伸幸, 平尾 健, 鈴木 直, 平沢 晃, 岩田 卓, 青木大輔, 菅野康吉, 宇田川康博, 吉村泰典, 野澤志朗

    第55回日本産科婦人科学会総会・学術講演会  2003.4.14 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:福岡  

    researchmap

  • 子宮体癌におけるMicrosatellite Instability と薬剤感受性試験によるcisplatin感受性との関連

    進 伸幸, 青木大輔, 阪埜浩司, 平尾 健, 岩田 卓, 平沢 晃, 金杉 優, 鈴木 直, 菅野康吉, 宇田川康博, 吉村泰典, 野澤志朗

    第55回日本産科婦人科学会総会・学術講演会  2003.4.14 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:福岡  

    researchmap

  • PPM1D and APPBP2 are targets for 17q21-q24 gain and are associated with malignant phenotypes in ovarian clear cell adenocarcinomas. International conference

    Hirasawa A, Imoto I, Saito-Ohara F, Inoue J, Aoki D, Susumu N, Nozawa S, Inazawa J

    AACR 94th Annual meeting  2003.4.5 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Tronto (Canada)  

    researchmap

  • 卵巣明細胞腺癌のCGH解析と増幅領域の標的遺伝子の探索 International conference

    Hirasawa Akira, Imoto IッSei, Saitou(ohara) Fumiko, Aoki Daisuke, Susumu Nobuyuki, Nozawa Shirou, Inazawa Jouji

    第47回日本人類遺伝学会  2002.11 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:未登録  

    researchmap

  • Clinical application of two-color FISH with liquid-based thin-layer cytological preparations for endometrial cancers. International conference

    Susumu N, Aoki D, Kanasugi M, Hirasawa A, Suzuki N, Nozawa S

    9th Biennial meeting of the International Gynecologic Cancer Society  2002.10.20 

     More details

    Presentation type:Oral presentation (general)  

    Venue:Souel, Korea  

    researchmap

  • Relationship between genomic imbalances and clinicopathological features in endometiral cancer. International conference

    Hirasawa A, Aoki D, Susumu N, Imoto I, Inazawa J, Nozawa S

    9th Biennial meeting of the International Gynecologic Cancer Society  2002.10.20 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Seoul (South Korea)  

    researchmap

  • Relation between Microsatellite Instability and Loss of hMLH1 Protein Expression in Endometrial Cancer. International conference

    Banno K, Susumu N, Hirasawa A, Aoki D, Udagawa Y, Sugano K, Nozawa S

    The first APOCP conference  2002.10.6 

     More details

    Presentation type:Oral presentation (general)  

    Venue:Nagoya, Japan  

    researchmap

  • 悪性黒色腫細胞株のCGH解析による新規癌関連遺伝子の同定

    Tanami Hideaki, Hirasawa Akira, Imoto IッSei, Sonoda Itaru, Yuzuki Yasuhiro, Inoue Jun, Iwai Takehisa, Sugihara Kenichi, Kawakami Yutaka, Inesawa Jouji

    第61回日本癌学会  2002.10 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 卵巣明細胞腺癌の悪性形質獲得にかかわるゲノムコピー数異常とその標的遺伝子の検索

    Hirasawa Akira, Imoto IッSei, Saitou Fumiko, Aoki Daisuke, Susumu Nobuyuki, Nozawa Shirou, Inazawa Jouji

    第61回日本癌学会総会  2002.10 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:未登録  

    researchmap

  • Clinical application of two-color FISH with liquid-based thin-layer cytological preparations for endometrial cancers International conference

    Susumu Nobuyuki, Aoki Daisuke, Kanasugi Masaru, Hirasawa Akira, Suzuki Nao, Nozawa Shiro

    Biennial Meeting of the International Gynecologic Cancer Society  2002.10 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:Seoul (South Korea)  

    researchmap

  • Relation between microsatellite instability and loss of hMLH1 protein expression in endometrial cancer International conference

    Banno Koji, Susumu Nobuyuki, Hirasawa Akira, Aoki Daisuke, Udagawa Yasuhiro, Sugano Kokichi, Nozawa Shiro

    Asian Pacific Organization for Cancer Prevention Conference“Inflammation and Cancer”  2002.10 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:Nagoya (Japan)  

    researchmap

  • Relationship between genomic imbalances and clinicopathlogical features in endometrial cancer International conference

    Hirasawa Akira, Aoki Daisuke, Susumu Nobuyuki, Imoto Issei, Inazawa Johji, Nozawa Shiro

    Biennial Meeting of the International Gynecologic Cancer Society  2002.10 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:未登録  

    researchmap

  • 高用量黄体ホルモン療法中の体癌症例における染色体変化-2色FISH法による核異型度判定の試み-

    Susumu Nobuyuki, Kanasugi Masaru, Setou Eri, Naitou Emi, Higashiguchi Atsushi, Kataoka Fumio, Hirasawa Akira, Suzuki Nao, Aoki Daisuke, Nozawa Shirou

    第32回日本婦人科腫瘍学会学術集会  2002.7 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 子宮内膜癌におけるマイクロサテライト不安定性とhMLH1蛋白発現低下との関連

    Banno Kouji, Susumu Nobuyuki, Hirasawa Akira, Kanasugi Masaru, Iwata Takashi, Aoki Daisuke, Sugano Koukichi, Nozawa Shirou

    第8回家族性腫瘍研究会学術集会  2002.6 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:未登録  

    researchmap

  • Genomic instabilities are correlated with clinicopathological variables in endometiral cancer. International conference

    Hirasawa A, Imoto I, Aoki D, Susumu N, Nozawa S, Inazawa J

    AACR 93rd annual meeting  2002.4.6 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:San Francisco (USA)  

    researchmap

  • High expression of cIAP1, a novel target for 11q22 amplification, correlates with poor prognosis in cervical cancer after radiotherapy. International conference

    Imoto I, Tsuda H, Hirasawa A, Hirohashi S, Inazawa J

    AACR 93rd annual meeting  2002.4.6 

     More details

    Language:English   Presentation type:Poster presentation  

    Venue:San Francisco (USA)  

    researchmap

  • 子宮内膜癌におけるマイクロサテライト不安定性とhMLH1蛋白発現低下との関連

    Banno Kouji, Susumu Nobuyuki, Hirasawa Akira, Kanasugi Masaru, Iwata Takashi, Suzuki Nao, Aoki Daisuke, Sugano Koukichi, Yoshimura Yasunori, Nozawa Shirou

    第54回日本産科婦人科学会総会および学術講演会  2002.4 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Genomic instabilities are correlated with clinicopathological variables in endometrial cancer International conference

    Hirasawa Akira, Imoto Issei, Aoki Daisuke, Susumu Nobuyuki, Nozawa Shiro, Inazawa Johji

    Annual Meeting of the American Association for Cancer Research  2002.4 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • High Expression of clAP1,a novel target for 11q22 amplification,correlates with poor prognosis in cervical cancer after radiotherapy International conference

    Imoto Issei, Tsuda Hitoshi, Hirasawa Akira, Hirohashi Setsuo, Inazawa Johji

    Annual Meeting of the American Association for Cancer Research  2002.4 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 子宮体癌におけるゲノム不安定性と臨床病理学的因子との関連性についての検討

    Hirasawa Akira, Aoki Daisuke, Susumu Nobuyuki, Banno Kouji, Imoto IッSei, Inazawa Jouji, Yoshimura Yasunori, Nozawa Shirou

    第54回日本産科婦人科学会総会および学術講演会  2002.4 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:未登録  

    researchmap

  • 若年体癌83例における家族内癌集積性と臨床病理学的特徴の関連

    Susumu Nobuyuki, Yamagami Wataru, Aoki Daisuke, Hirasawa Akira, Kanasugi Masaru, Setou Eri, Banno Kouji, Yoshimura Yasunori, Nozawa Shirou

    第54回日本産科婦人科学会総会および学術講演会  2002.4 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    Venue:未登録  

    researchmap

  • 当院における若年性体癌83例の臨床病理学的検討

    Yamagami Wataru, Susumu Nobuyuki, Aoki Daisuke, Banno Kouji, Kanasugi Masaru, Hirasawa Akira, Setou Eri, Kataoka Fumio, Suzuki Nao, Yoshimura Yasunori, Nozawa Shirou

    第102回日本産科婦人科学会関東連合地方部会総会  2001.10 

     More details

    Language:Japanese  

    researchmap

  • 子宮内膜癌における染色体不安定性とマイクロサテライト不安定性に関する検討

    Hirasawa Akira, Imoto Isei, Aoki Daisuke, Susumu Nobuyuki, Nozawa Shirou, Inasawa Jouji

    第46回日本人類遺伝学会  2001.10 

     More details

    Language:Japanese  

    researchmap

  • 子宮体癌組織における染色体不安定性およびマイクロサテライト不安定性の検討

    Hirasawa Akira, Imoto Isei, Aoki Daisuke, Susumu Nobuyuki, Nozawa Shirou, Inazawa Jouji

    第60回日本癌学会総会  2001.9 

     More details

    Language:Japanese  

    researchmap

  • 子宮体癌における抗癌剤感受性試験に関する検討

    Kanasugi Masaru, Aoki Daisuke, Hirasawa Akira, Setou Eri, Nakada Sakura, Suzuki Nao, Susumu Nobuyuki, Nozawa Shirou

    第42回日本臨床細胞学会総会  2001.6 

     More details

    Language:Japanese  

    researchmap

  • 子宮体部腫瘍外来で発見された家族内癌集積を示す3症例の解析

    Banno Kouji, Nikata Masanobu, Hirasawa Akira, Susumu Nobuyuki, Aoki Daisuke, Udagawa Yasuhiro, Sugano Koukichi, Nozawa Shirou

    第7回家族性腫瘍研究会  2001.6 

     More details

    Language:Japanese  

    researchmap

  • 子宮体癌における第1,第17染色体の数的,構造的異常の検索―2色FISH法,モノレイヤー標本作製法(Thin Prep法)を用いて―

    Susumu Nobuyuki, Aoki Daisuke, Kanasugi Masaru, Setou Eri, Hirasawa Akira, Kataoka Fumio, Suzuki Nao, Yoshimura Yasunori, Nozawa Shirou, Tsuda Hitoshi

    第53回日本産科婦人科学会総会および学術講演会  2001.5 

     More details

    Language:Japanese  

    researchmap

  • TGFβ1によって誘導されるPAI-1と卵巣明細胞腺癌の生物学的特性との関連

    Komiyama Shinichi, Aoki Daisuke, Hirasawa Akira, Kataoka Fumio, Susumu Nobuyuki, Mikami Mikio, Yoshimura Yasunori, Nozawa Shirou

    第53回日本産科婦人科学会総会および学術講演会  2001.5 

     More details

    Language:Japanese  

    researchmap

  • 卵巣癌に対するPaclitaxelを用いたHDRA法の有用性についての検討

    Kanasugi Masaru, Aoki Daisuke, Hirasawa Akira, Kataoka Fumio, Noda Tomomi, Suzuki Nao, Susumu Nobuyuki, Nozawa Shirou, Nakada Sakura, Udagawa Yasuhiro

    制癌剤適応研究会  2001.3 

     More details

    Language:Japanese  

    researchmap

  • 最近当科で経験したadenoma malignumの3例

    Hayashi Shigenori, Fukuchi Takeshi, Kataoka Fumio, Hirasawa Akira, Kubushiro Kaneyuki, Tsukazaki Katsumi, Yoshimura Yasunori, Nozawa Shirou, Mukai Makio

    日本産科婦人科学会東京地方部会例会  2000.12 

     More details

    Language:Japanese  

    researchmap

  • 卵巣明細胞腺癌におけるPAI-1発現の生物学的意義

    Komiyama Shinichi, Aoki Daisuke, Kanasugi Masaru, Hirasawa Akira, Nozawa Shirou

    日本分子腫瘍マーカー研究会  2000.10 

     More details

    Language:Japanese  

    researchmap

  • 表層上皮性卵巣癌I期におけるTGFβレセプターII型発現の特徴

    Tominaga Eiichirou, Aoki Daisuke, Komiyama Shinichi, Hirasawa Akira, Kanasugi Masaru, Susumu Nobuyuki, Nozawa Shirou

    日本臨床電子顕微鏡学会総会  2000.9 

     More details

    Language:Japanese  

    researchmap

  • 卵巣癌症例の後腹膜リンパ節転移の検討―組織型と分化度との関連を中心に―

    Hirasawa Akira, Susumu Nobuyuki, Aoki Daisuke, Komiyama Shinichi, Kanasugi Masaru, Tominaga Eiichirou, Yoshimura Yasunori, Nozawa Shirou

    日本産科婦人科学会関東連合地方部会総会  2000.6 

     More details

    Language:Japanese  

    researchmap

  • 卵巣癌I期症例における腹水細胞診の判定と予後に関する検討

    Hirasawa Akira, Aoki Daisuke, Komiyama Shinichi, Tamada Yutaka, Tominaga Eiichirou, Susumu Nobuyuki, Nozawa Shirou

    日本臨床細胞学会総会  2000.5 

     More details

    Language:Japanese  

    researchmap

  • 卵巣癌における第1および第17染色体の数的構造的異常 ―2色FISH法を用いた検索―

    Susumu Nobuyuki, Tsuda Hitoshi, Aoki Daisuke, Komiyama Shinichi, Tominaga Eiichirou, Hirasawa Akira, Udagawa Yasuhiro, Yoshimura Yasunori, Nozawa Shirou

    日本産科婦人科学会総会・学術講演会  2000.4 

     More details

    Language:Japanese  

    researchmap

  • Genetic analysis of chromosome 17 and 1 in cervical cancers using fluorescence in situ hybridization and RFLP-Southern Blot International conference

    Susumu Nobuyuki, Tsuda Hitoshi, Aoki Daisuke, Udagawa Yasuhiro, Hirasawa Akira, Kanasugi Masaru, Nozawa Shiro

    Biennial Meeting of the International Gynecologic Cancer Society (7th ; 1999 ; Rome)  1999.9 

     More details

    Language:English  

    researchmap

  • The relationship between MSN-1-Reactive carbohydrate antigens and α-1,2 fucosyltransferase genes expressed in endometrial adenocarcinoma International conference

    Tominaga Eiichiro, Aoki Daisuke, Hirasawa Akira, Setoh Eri, Susumu Nobuyuki, Udagawa Yasuhiro, Nozawa Shiro

    Biennial Meeting of the International Gynecologic Cancer Society (7th ; 1999 ; Rome)  1999.9 

     More details

    Language:English  

    researchmap

  • 卵巣明細胞腺癌におけるTGF-β1およびTGF-β1レセプターII型に関する免疫組織化学的検討

    Hirasawa Akira, Aoki Daisuke, Komiyama Shinichi, Tominaga Eiichiro, Susumu Nobuyuki, Udagawa Yasuhiro, Nozawa Shiro

    第40回日本臨床細胞学会総会  1999.6 

     More details

    Language:Japanese  

    researchmap

  • 卵巣明細胞腺癌におけるTGFβレセプター発現の動向 ─子宮内膜症との相互作用に関連して─

    Komiyama Shinichi, Aoki Daisuke, Hirasawa Akira, Susumu Nobuyuki, Iida Toshihiko, Udagawa Yasuhiro, Yoshimura Yasuhiro, Nozaawa Shiro

    第51回日本産科婦人科学会総会・学術講演会  1999.4 

     More details

    Language:Japanese  

    researchmap

  • 子宮体癌に特異的に出現する糖鎖の発現機構におけるフコース転移酵素の関与について

    Tominaga Eiichiro, Aoki Daisuke, Hirasawa Akira, Setoh Eri, Susumu Nobuyuki, Udagawa Yasuhiro, Yoshimura Yasuhiro, Nozaawa Shiro

    第51回日本産科婦人科学会総会・学術講演会  1999.4 

     More details

    Language:Japanese  

    researchmap

  • 臨床進行期I期の卵巣明細胞腺癌と子宮内膜症との関連

    Komiyama Shinichi, Aoki Daisuke, Hirasawa Akira, Susumu Nobuyuki, Udagawa Yasuhiro, Nozawa Shirou

    第20回エンドメトリオシース研究会  1999.1 

     More details

    Language:Japanese  

    researchmap

  • 当院における最近6年間の子宮体癌症例の予後因子について

    Hirasawa Akira, Susumu Nobuyuki, Komiya Kyoko, Sakai Masanaga, Arai Hiroharu, Hayashi Hirotaka

    第50回日本産科婦人科学会埼玉地方部会平成8年度後期学術集会  1996.11 

     More details

    Language:Japanese  

    researchmap

  • Agonist-induced calcium oscillation and cell cycle via α1b-adrenoceptor International conference

    Awaji Takeo, Tsujimoto Gozoh, Hirasawa Akira, Horie Kuniko, Izumi Shunichiro, Nemoto Taiko, Makino Tsunehisa, Yoshimura Yasunori

    第10回 International Congress of Endocrinology (ICE'96)  1996.6 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    Venue:未記入  

    researchmap

▼display all

Industrial property rights

  • 婦人科癌オルガノイドの製造方法、婦人科癌オルガノイド、婦人科癌オルガノイド製造用培地、及び薬効評価方法

    大久保 亜希, 平沢 晃, 青木 大輔, 南木 佳子

     More details

    Applicant:JSR株式会社

    Application no:特願2019-192034  Date applied:2019.10.21

    Announcement no:特開2021-065129  Date announced:2021.4.30

    J-GLOBAL

    researchmap

  • 頭頸部腫瘍増殖抑制剤

    座間 猛, 齋藤 康一郎, 平沢 晃, 稲垣 康治

     More details

    Applicant:学校法人慶應義塾

    Application no:特願2011-509224  Date applied:2010.4.16

    Publication no:WO2010-119698  Date published:20101021

    Patent/Registration no:特許第5567555号  Date registered:2014.6.27 

    J-GLOBAL

    researchmap

  • 頭頸部腫瘍増殖抑制剤

    座間 猛, 齋藤 康一郎, 平沢 晃, 稲垣 康治

     More details

    Applicant:学校法人慶應義塾

    Application no:JP2010002764  Date applied:2010.4.16

    Publication no:WO2010-119698  Date published:20101021

    J-GLOBAL

    researchmap

  • 頭頸部腫瘍増殖抑制剤

    座間 猛, 齋藤 康一郎, 平沢 晃, 稲垣 康治

     More details

    Applicant:学校法人慶應義塾

    Application no:特願2011-509224  Date applied:2010.4.16

    Patent/Registration no:特許第5567555号  Date registered:2014.6.27 

    J-GLOBAL

    researchmap

  • バイオマーカーとしてのマイクロRNAを用いた婦人科がんの診断・治療選択

    座間 猛, 平沢 晃, 齋藤 康一郎, 赤羽 智子

     More details

    Applicant:学校法人慶應義塾

    Application no:特願2009-150986  Date applied:2009.6.25

    Announcement no:特開2010-154843  Date announced:2010.7.15

    J-GLOBAL

    researchmap

  • バイオマーカーとしてのマイクロRNAを用いた頭頸部腫瘍の診断・治療選択

    座間 猛, 齋藤 康一郎, 平沢 晃, 長西 秀樹

     More details

    Applicant:学校法人慶應義塾

    Application no:特願2009-099849  Date applied:2009.4.16

    Announcement no:特開2010-094122  Date announced:2010.4.30

    J-GLOBAL

    researchmap

▼display all

Works

  • 卵巣がんの基礎知識

    HIRASAWA AKIRA

    2011.8.26
    -
    2011.8.28

     More details

  • 婦人科腫瘍の臨床と標準治療法

    HIRASAWA AKIRA

    2010.12.18

     More details

  • ゲノム薬理学に基づいたがん個別化治療戦略

    HIRASAWA AKIRA

    2010.12.10

     More details

  • 婦人科における遺伝性腫瘍

    HIRASAWA AKIRA

    2010.8.6

     More details

  • 第15回臨床研修指導医養成ワークショップ

    HIRASAWA AKIRA

    2010.7.30
    -
    2010.7.31

     More details

  • がん診療に携わる医師に対する緩和ケア研修会

    HIRASAWA AKIRA

    2010.5.8
    -
    2010.5.9

     More details

  • 家族性乳癌・卵巣癌の治療(婦人科編)

    HIRASAWA AKIRA

    2009.8.20
    -
    2009.8.23

     More details

  • 卵巣がん一般の診断・治療総論

    HIRASAWA AKIRA

    2009.1.9
    -
    2010.1.10

     More details

  • 第13回共用試験医学系OSCE評価者認定講習会 修了

    HIRASAWA AKIRA

    2008.10.19

     More details

  • 月経に伴う女性の諸症状とその対策

    2008.1.23

     More details

  • CGH法を用いた婦人科がん ゲノム異常の検索

    HIRASAWA AKIRA

    2007.1.31

     More details

▼display all

Awards

  • Best Presentation Award

    2022.6   Prospective cohort study of germline variant carriers with BRCA1 and BRCA2 (JGOG3024/KGOG3055)

     More details

  • 平成29年度日本女性医学学会学術奨励賞

    2017.11   日本女性医学学会   がんゲノム医療実用化と女性ヘルスケアの個別化

     More details

    Award type:Award from Japanese society, conference, symposium, etc. 

    researchmap

  • 第61回日本産科婦人科学会学術講演会 グッドプレゼンテーション賞

    2009.4   UGT1A1遺伝子多型とイリノテカンの有害事象およびグルクロン酸抱合能に関するゲノム薬理学的検討

    平沢 晃, 赤羽智子, 野村弘行, 阪埜浩司, 津田浩史, 齋藤康一郎, 座間 猛, 後田奈緒美, 谷川原祐介, 進 伸幸, 青木大輔, 吉村泰典

     More details

  • 第60回日本産科婦人科学会学術講演会 グットプレゼンテーション賞

    2008.4   塩酸イリノテカン個別化治療の確立を目指したUGT1A1遺伝子多型解析.

    平沢 晃, 鶴田智彦, 市川義一, 末盛友浩, 東口敦司, 冨永英一郎, 阪埜浩司, 進 伸幸, 後田奈緒美, 谷川原祐介, 青木大輔, 吉村泰典

     More details

Research Projects

  • BRCA病的バリアント保持者女性における卵巣癌危険因子の層別化に向けた多施設共同研究

    Grant number:24K02589  2024.04 - 2029.03

    日本学術振興会  科学研究費助成事業  基盤研究(B)

    平沢 晃

      More details

    Grant amount:\18590000 ( Direct expense: \14300000 、 Indirect expense:\4290000 )

    researchmap

  • Cancer prevention for Lynch syndrome through splicing mechanisms of RNA editing enzyme gene ADAR1

    Grant number:24K13439  2024.04 - 2027.03

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research  Grant-in-Aid for Scientific Research (C)

    山本 英喜, 重安 邦俊, 平沢 晃, 冨田 秀太, 遠西 大輔

      More details

    Grant amount:\4420000 ( Direct expense: \3400000 、 Indirect expense:\1020000 )

    researchmap

  • ゲノム情報に応じたがん予防にかかる指針の策定と遺伝性腫瘍に関する医療・社会体制の整備および国民の理解と参画に関する研究

    Grant number:23EA1037  2023.11 - 2026.03

    厚生労働科学研究費補助金  がん対策推進総合研究事業 

    平沢 晃、吉田玲子、桑田 健、平田 真、岩谷胤生

      More details

    Authorship:Principal investigator 

    researchmap

  • Development and validation of a health promotion application for hereditary tumors

    Grant number:23K10870  2023.04 - 2026.03

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research  Grant-in-Aid for Scientific Research (C)

    山下 範之, 平沢 晃

      More details

    Grant amount:\4680000 ( Direct expense: \3600000 、 Indirect expense:\1080000 )

    researchmap

  • 23がん種14万人を用いた遺伝・環境・生活習慣を統合した各個人の疾患リスクの推定

    2023

    日本医療研究開発機構  革新的がん医療実現化研究事業 

    桃沢 幸秀, 松尾 恵太郎, 平沢 晃

      More details

    Authorship:Coinvestigator(s) 

    researchmap

  • 神経線維腫症1型患者のNF1遺伝子変異に基づく病態解明と個別化医療を目的とした疾患特異的iPS細胞の樹立

    2023

    国立研究開発法人日本医療研究開発機構  再生・細胞医療・遺伝子治療実現加速化プログラム(疾患特異的iPS細胞を用いた病態解明・創薬研究課題) 

    中田英二、宝田剛志、尾﨑敏文、平沢晃、山田大祐

      More details

    Authorship:Coinvestigator(s) 

    researchmap

  • 利活用を目的とした日本疾患バイオバンクの運営・管理

    2023

    日本医療研究開発機構  ゲノム医療実現バイオバンク利活用プログラム(ゲノム研究バイオバンク) 

      More details

  • 卵巣癌予防のためのエビデンス創出を目的とした国際臨床研究

    2022.04 - 2024.03

    日本学術振興会  二国間交流事業共同研究 

    平沢 晃, 榎本隆之, 島田宗昭, 津田 均, 井本逸勢, 松尾 恵太郎, 坂井美佳, 二川摩周

      More details

    Authorship:Principal investigator 

    researchmap

  • 大規模疾患コホート・アカデミア連携を基盤とするオミックス解析・サーベイランス体制の整備による新興感染症重症化リスク因子の探索

    2022

    日本医療研究開発機構  ワクチン開発のための世界トップレベル研究開発拠点の形成事業 

      More details

    Authorship:Coinvestigator(s) 

    researchmap

  • 遺伝性腫瘍に見られるVUSに対する、包括的in vivoスクリーニングとin silico構造解析を融合した高精度機能的アノテーション

    2022

    日本医療研究開発機構  ゲノム創薬基盤推進研究事業 

      More details

    Authorship:Coinvestigator(s) 

    researchmap

  • オンライン遺伝診療:家系単位での遺伝医療を実現する遠隔診療ネットワークの構築

    Grant number:21K19667  2021.07 - 2024.03

    日本学術振興会  科学研究費助成事業 挑戦的研究(萌芽)  挑戦的研究(萌芽)

    植野 さやか, 田村 和朗, 赤木 究, 平沢 晃, 吉田 玲子, 植木 有紗

      More details

    Grant amount:\6370000 ( Direct expense: \4900000 、 Indirect expense:\1470000 )

    本年度は研究代表者が試験的に4件のオンライン診療を実施した。診療から得られた情報を基に、「オンライン遺伝診療に対する意識調査」の準備及び、オンライン遺伝診療に用いるシステム・ツールの選定を主に行った。
    <オンライン遺伝診療に対する意識調査の準備>
    研究代表者が行ったオンライン遺伝診療の実施経験から、遺伝診療のオンライン化には3つのハードルが存在することが浮かび上がった。①受診するクライエント側のハードル、②提供する医療者個人のハードル、③提供する施設のハードルの3点である。当初は、クライエント側のハードルに焦点を当てていたが、提供する側の医療者及び施設のハードルも明らかにすることにより、より一層スムーズなオンライン診療の導入につながるものと考えられた。クライエントに対するアンケート調査に加えて、遺伝医療に携わる医療者側へのアンケート調査も実施することとした。本年度は調査票を作成し、研究実施機関の承認を取得した。2022年度から2023年度にかけて実施予定である。
    <オンライン遺伝診療に用いるシステム・ツールの選定>
    現在、複数のオンライン診療システムがある。遺伝診療では、疾患の発症リスク・遺伝形式の説明など、文書を用いた情報提供が必要な場面が多い。また、診療にはできるだけ家族や血縁者が同席することが望ましく、複数のクライエントとコミュニケーションを取る必要がある。一方で、医療者側も、さまざまな側面からクライエントに対応できるよう、医師のみならず遺伝カウンセラーや看護師など多職種が同席することが多い。このように、遺伝診療に特徴的な状況において、複数人を対象とした双方向性のコミュニケーションを可能にするには、音声や画像の鮮明さや雑音の除去など種々の要因を考慮する必要があることが明らかになった。2022年度以降、さらに検証を進めていく。

    researchmap

  • 遺伝性腫瘍の浸透率決定因子の同定と発癌予測モデルの開発

    2020.09 - 2021.03

    公益財団法人 大和証券ヘルス財団  令和2年度(第47回)調査研究助成 

      More details

    Authorship:Principal investigator 

    researchmap

  • 遺伝性乳癌卵巣癌症候群サバイバーおよびプレバイバーに対する情報提供と意志決定支援を目指した医療圏連携体制の構築

    2020.09 - 2021.03

    公益財団法人がん研究振興財団  令和2年度がんサバイバーシップ研究助成金 

      More details

    Authorship:Principal investigator 

    researchmap

  • 医療圏における遺伝性腫瘍コホートの構築と日本人のがん死低減に向けた基盤データの策定 ―中央西日本遺伝性腫瘍コホート研究―

    2020.09 - 2021.02

    岡山大学  次世代研究拠点形成支援事業 令和2年度岡山大学次世代研究育成グループ 

      More details

    Authorship:Principal investigator 

    researchmap

  • 卵巣癌オルガノイドとドライバージーン解析に基づいた難治性卵巣癌個別化治療法の確立

    Grant number:20K09630  2020.04 - 2024.03

    日本学術振興会  科学研究費助成事業 基盤研究(C)  基盤研究(C)

    片岡 史夫, 赤羽 智子, 平沢 晃

      More details

    Grant amount:\4420000 ( Direct expense: \3400000 、 Indirect expense:\1020000 )

    卵巣癌の初回治療終了後から6カ月以内の再発はプラチナ抵抗性とされる。プラチナ抵抗性の再発卵巣癌に対する治療は選択薬剤が乏しいうえ、完治が難しいという理由から緩和医療やQOLの向上および生存期間の延長を目的とする治療がなされているのが現状である。そこで本研究はプラチナ抵抗性卵巣癌に対するセカンドライン以降の治療薬剤の選択ツールをゲノム解析と薬剤感受性試験(DSRT)から確立することを目的としている。
    本年度は患者腹水検体より樹立した細胞株にてDSRTを行い培養環境条件の違いによる差異について基礎的検討を行った。樹立細胞株由来の腹水は初診時には卵巣癌が疑われていたが病理学的検索から悪性腹膜中皮腫(MPeM)と診断された検体を使用した。腹水採取時の臨床状態はシスプラチン(CDDP)とぺネトレキセド(PEM)併用療法終了後に再発が確認され、PEM単剤にて追加治療中であった。検体の腫瘍細胞含有割合は細胞診標本による顕微鏡下での目視確認にて90%以上を占めていた。樹立細胞株を2次元平面培養用Plateと3次元立体培養用NanoCulture Plateにそれぞれ播種して異なる培養環境を模倣した。各Plateは5%CO2条件下で37℃で培養した後、細胞播種から3日目に薬剤添加、6日目にATP活性を吸光度測定し、数値をグラフ化して基準値と比較しIC50を示す薬剤濃度を評価した。MPeM細胞株の比較対象として卵巣癌由来細胞株OVCAR-3とSKOV-3を使用した。
    その結果、PEMのDSRTはMPeM由来細胞株は2次元平面培養で感受性を示したのに対し、3次元立体培養では細胞増殖抑制傾向は示したが最終的には非感受性であった。比較対象のOVCAR-3とSKOV-3では高濃度のPEMでも非感受性であった。CDDPはすべての細胞で培養条件に関わらず非感受性を示した。
    今回の結果から、MPeM由来樹立細胞株の3次元立体培養による環境条件はPEM抵抗性を示した臨床状態に類似した環境を模倣したと考えられた。

    researchmap

  • 国民が安心してゲノム医療を受けるための社会実現に向けた倫理社会的課題抽出と社会環境整備

    2020.04 - 2023.03

    厚生労働科学研究費補助金  倫理的法的社会的課題研究事業 

      More details

    Authorship:Coinvestigator(s) 

    researchmap

  • ゲノム情報を活用した遺伝性腫瘍の先制的医療提供体制の整備に関する研究

    2020.04 - 2023.03

    厚生労働科学研究費補助金  がん対策推進総合研究事業 

      More details

    Authorship:Coinvestigator(s) 

    researchmap

  • ゲノム情報を活用した遺伝性乳癌卵巣癌診療の標準化と先制医療実装にむけたエビデンス構築に関する研究

    2019.04 - 2020.03

    厚生労働科学研究費補助金  がん対策推進総合研究事業 

      More details

    Authorship:Coinvestigator(s) 

    researchmap

  • 医療圏の連携による遺伝性腫瘍コホートの構築とがん予防の実証的研究

    2019.03 - 2020.03

    公益財団法人がん研究振興財団  平成30年度(第51回)がん研究助成金 

      More details

    Authorship:Principal investigator 

    researchmap

  • Precision medicine for ovarian cancer by DSRT and genomic analysis

    Grant number:18K09298  2018.04 - 2021.03

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)  Grant-in-Aid for Scientific Research (C)

    TOMINAGA Eiichiro

      More details

    Grant amount:\4420000 ( Direct expense: \3400000 、 Indirect expense:\1020000 )

    This study reported a new cell line of malignant peritoneal mesothelioma established from ascites for the purpose of performing DSRT for ovarian cancer.
    The following research results were obtained. The characteristics of the tumor tissue and established cell line were verified to be the same using protein expression analysis of immunohistochemical staining. The established cell line mimicked the difference in environment between two- and three-dimensional culture, which clarified that the difference in culture environment causes the difference response of pemetrexed agents. The results obtained from this research project were reported in a treatise.

    researchmap

  • 卵巣癌precision medicineを目指した血液中遊離DNAの同定

    2018.04 - 2020.03

    日本学術振興会  二国間交流事業 

    HIRASAWA AKIRA

      More details

    Authorship:Principal investigator  Grant type:Competitive

    researchmap

  • Identification of factors related to penetrance and predictive model for ovarian cancer among BRCA1or BRCA2 mutation carriers

    Grant number:17K19611  2017.06 - 2020.03

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Challenging Research (Exploratory)  Grant-in-Aid for Challenging Research (Exploratory)

    Hirasawa Akira

      More details

    Grant amount:\6500000 ( Direct expense: \5000000 、 Indirect expense:\1500000 )

    This multicenter prospective cohort study aim to recruit germline pathogenic variant carrier of the BRCA1 / 2 genes to provides basic data for cancer prevention. Our study aimed to establish an individualized intervention strategy and we started evaluation of related tumor incidence, survival rate, management, QOL evaluation by risk reduction surgery, and genomic epidemiological analysis in pedigree of hereditary breast and ovarian cancer syndrome. Clinicopathological information was confirmed by regular follow-up surveys, human samples of registered HBOC biobank and international data sharing was constructed.

    researchmap

  • 医療現場でのゲノム情報の適切な開示のための体制整備に関する研究

    2017.04 - 2020.03

    国立研究開発法人日本医療研究開発機構  ゲノム創薬基盤推進研究事業 

      More details

    Authorship:Collaborating Investigator(s) (not designated on Grant-in-Aid) 

    researchmap

  • がんゲノム医療推進を目指した医療情報等の利活用にかかる国内外の法的基盤の運用と課題に関する調査研究

    2017.04 - 2019.03

    厚生労働科学研究費 倫理的法的社会的課題研究事業 

    中田はる佳

      More details

    Grant type:Competitive

    Grant amount:\2002000

    researchmap

  • Sensitivities for anti-cancer drugs/hormones for endometrial cancer - from the viewpoint of tumor immunology

    Grant number:16K11156  2016.04 - 2019.03

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)  Grant-in-Aid for Scientific Research (C)

    SUSUMU NOBUYUKI, YAMAGAMI Wataru, HIRASAWA Akira, SAKAI Kensuke, MAKABE Takeshi, HIRANO Takuro, KATAOKA Fumio, BANNO Kouji, AOKI Daisuke

      More details

    Grant amount:\4680000 ( Direct expense: \3600000 、 Indirect expense:\1080000 )

    We performed fertility-preserving MPA therapy for young patients with endometrial cancer (EC) and atypical endometrial hyperplasia (AEH). Tumor disappeared in 98.5% in 131 AEH cases, 91.9% in 160 G1 EC cases, 100% in 6 G2 EC cases. Tumor relapsed in uterine cavity in 55%, 83%, 75%, respectively. Pregnancy was obtained in 87 cases. In total, 138 times pregnancies and 103 live-birth children were obtained, and the pregnancy rate was 45%. The pregnancy rates by age and pathological types were 35 to 75% under 40 years in both AEHC and EC patients, however, EC patients in age 40 or more showed 5% pregnancy rate. Repeated MPA therapy after recurrence showed high tumor disappearance rate and pregnancy rate as well as after initial MPA therapy. The clinicopathological factors such as polycystic ovary, irregular menstrual cycle, low expression of hMLH1 were associated with elevated recurrence rate. The data regarding regulatory T cells and sensitivity for progesterone are now in analysis.

    researchmap

  • 遺伝性腫瘍の遺伝学的検査とバイオバンクに関するELSIの情報共有

    2016.04 - 2018.03

    国立研究開発法人日本医療研究開発機構 研究倫理に関する情報共有と国民理解の推進事業(ゲノム医療実用化に係るELSI分野)委託研究開発費 

      More details

    Grant type:Competitive

    Grant amount:\5000000

    researchmap

  • Molecular profiling of ovarian cancer for improvement of therapeutic management using Olaparib

    2016.04

    アストラゼネカ(株) Externally Sponsored Research プログラム 

      More details

    Grant type:Competitive

    Grant amount:\49200000

    researchmap

  • BRCAness機構の解明に基づいた難治性卵巣癌precision medicineの確立

    2015.04 - 2018.03

    慶應義塾学事振興基金(個人研究) 

      More details

    Grant type:Competitive

    Grant amount:\2500000

    researchmap

  • 卵巣癌細胞の薬剤感受性と遺伝子プロファイルに基づいた治療法の確立

    2015.04 - 2018.03

    日本学術振興会科学研究費補助金 基盤研究(C)  Grant-in-Aid for Scientific Research 

    冨永英一郎

      More details

    Grant type:Competitive

    Grant amount:\700000

    researchmap

  • Towards precision medicine for ovarian cancer using drug sensitivity and resistance testing and genomic analysis

    Grant number:15K10730  2015.04 - 2018.03

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)  Grant-in-Aid for Scientific Research (C)

    Eichirou Tominaga

      More details

    Grant amount:\4810000 ( Direct expense: \3700000 、 Indirect expense:\1110000 )

    The following results were raised within this research project.
    ①We successfully established a new cell line from malignant mesothelioma ascites. This cell line is a valuable biological resource to study the mechanisms underlying carcinogenesis in peritoneal mesothelioma and for drug sensitivity tests (DSRT).②DSRT were conducted in two dimensional and three dimensional cultures using established cell lines. The pemetrexed (PEM) is used for standard therapy of malignant mesothelioma. PEM was drug susceptibility in two dimensional culture by DSRT, but there was no drug effect in three dimensional culture. Those results were consistent with the clinical course and it was possible to conduct a DSRT that mimics the in vivo environment.③Cell cultured from ovarian carcinoma tumor tissue fragments formed spheroids and succeeded in creating a ductal structure similar to the in vivo structure. We succeeded in forming spheroids derived from ovarian cancer tumor tissue.

    researchmap

  • 卵巣癌早期診断を目的とした血液中遊離DNAの同定

    2015.04 - 2017.03

    日本学術振興会二国間交流事業 対応機関との合意に基づく共同研究(スウェーデン) 

      More details

    Grant type:Competitive

    Grant amount:\4900000

    researchmap

  • 難治性卵巣癌におけるdriver mutationの同定と新規治療法の開発

    2014.04 - 2015.03

    日本学術振興会二国間交流事業 オープンパートナーシップ共同研究(フィンランド)  Grant-in-Aid for Scientific Research 

      More details

    Grant type:Competitive

    Grant amount:\5000000

    researchmap

  • 難治性卵巣癌の薬剤感受性とゲノム異常に基づいたドラッグリポジショニングの開発

    2014

    佐川がん研究振興財団 佐川がん研究助成 

      More details

    Grant type:Competitive

    Grant amount:\1000000

    researchmap

  • 脂質および糖代謝動態の探索による子宮体癌分子機構の解明

    2013.04 - 2016.03

    日本学術振興会科学研究費補助金 基盤研究(C)  Grant-in-Aid for Scientific Research 

      More details

    Grant type:Competitive

    Grant amount:\5070000

    researchmap

  • Biological characteristics of endometrial cancer with lifestyle-related diseases.

    Grant number:25462609  2013.04 - 2016.03

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)  Grant-in-Aid for Scientific Research (C)

    Hirasawa Akira

      More details

    Grant amount:\5070000 ( Direct expense: \3900000 、 Indirect expense:\1170000 )

    This study aimed to reveal relationship between environmental factors and genetic factors in endometrial cancer survivors. We recruited clinical informations and samples from menopause clinic, Keio University Hospital, Tokyo, Japan. Our results revealed 1)Hypertriglyceridemia was statistically more frequent in patients who had undergone bilateral salpingo-oophorectomy both before and after menopause than in the corresponding non-endometrial cancer controls, 2) Osteoporosis was associated with hypertriglyceridemia in post-menopausal women without endometrial cancer, but was less frequent in endometrial cancer survivors with hypertriglyceridemia, and 3) No significant association was found between osteoporosis and polymorphisms in ESR1, UGT2B17, or UGT1A1 in both groups, suggesting that BSO might be a more significant physiological factor in influencing bone mass density compared to genetic variations.

    researchmap

  • Alteration of tumor immunity and anti-cancer drug / hormone sensitivity in endometrial cancer with frequent MMR mechanism abnormality

    Grant number:25462612  2013.04 - 2016.03

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)  Grant-in-Aid for Scientific Research (C)

    SUSUMU NOBUYUKI, YAMAGAMI Wataru, NODA Tomomi, SAKAI Kensuke, MAKABE Takesi, NINOMIYA Tomomi, HIRASAWA Akira, KATAOKA Fumio, NOMURA Hiroyuki, BANNO Kouji, AOKI Daisuke

      More details

    Grant amount:\5070000 ( Direct expense: \3900000 、 Indirect expense:\1170000 )

    The MSI-positive tumors showed significantly higher grades and larger numbers of TILs than MSI-negative tumors. The COX-2-high group showed fewer TILs than COX-2-low group. Multivariate analysis identified a low number of TILs, positive lymph node involvement, and high tumor malignancy grade as factors independently associated with poor prognosis. The number of TILs, which was increased by MSI and decreased by COX-2 expression, was associated with a poorer prognosis in patients with endometrial cancer. We also propose that COX-2 may block MSI-activated TILs in the tumor microenvironment. Regarding fertility-preserving hormonal therapy, we performed hormonal therapy for 214 young patients with atypical endometrial hyperplasia or endometrioid adenocarcinoma G1. We succeeded in 83 pregnancies in 62 patients and showed 7.5% as the frequency of double cancer, and also revealed the safety and effectiveness of repeated MPA therapy after recurrence with the low incidence of double cancer.

    researchmap

  • 難治性卵巣癌の生物学的特性の解析に基づいた治療標的分子シーズの探索

    2013

    武田科学振興財団 医学研究奨励(臨床) 

      More details

    Grant type:Competitive

    Grant amount:\2000000

    researchmap

  • フィンランド分子医学研究所におけるがんシステムの統合的解析に基づいた治療抵抗性卵巣癌に対する新規治療法に関する研究

    2013

    スカンジビア・ニッポンササカワ財団助成 

      More details

    Grant type:Competitive

    Grant amount:\300000

    researchmap

  • 卵巣癌ゲノム異常の統合的解析と個別化医療への応用

    2012.04 - 2014.03

    日本学術振興会特定国派遣研究者事業  Grant-in-Aid for Scientific Research 

      More details

    Grant type:Competitive

    researchmap

  • 婦人科癌関連癌抑制型microRNA replacement therapyの有用性の検討

    2012

    東京医科歯科大学 難治疾患共同研究拠点共同研究研究費 

      More details

    Grant type:Competitive

    Grant amount:\200000

    researchmap

  • 更年期女性ための自己健康管理を目的としたICTシステムの構築

    2012

    公益財団法人総合健康推進財団 一般研究奨励助成 

      More details

    Grant type:Competitive

    Grant amount:\900000

    researchmap

  • 難治性卵巣癌に対する新規治療法開発を目指した橋渡し研究

    2011

    日本学術振興会 組織的な若手研究者等海外派遣プログラム 「癌領域における基礎から臨床への翻訳能と国際競争力を有する次世代リーダーの育成」  Grant-in-Aid for Scientific Research 

      More details

    Grant type:Competitive

    researchmap

  • 両側卵巣摘出術施行例の長期的QOL向上を志向した環境因子および遺伝因子の統合的解析

    2011

    日本女性医学学会 JMWH Bayer Grand 

      More details

    Grant type:Competitive

    Grant amount:\1000000

    researchmap

  • ゲノム・エピゲノム解析による新規婦人科癌関連遺伝子の網羅的探求とその分子機構の解明

    2010.04 - 2012.03

    東京医科歯科大学 難治疾患共同研究拠点共同研究研究費 

      More details

    Grant type:Competitive

    Grant amount:\600000

    researchmap

  • 機能的スクリーニング法を用いた子宮体癌関連マイクロRNAの探索と核酸医薬への応用

    2010.04 - 2012.03

    日本学術振興会科学研究費補助金 基盤研究(B)  Grant-in-Aid for Scientific Research 

    青木大輔

      More details

    Grant type:Competitive

    Grant amount:\2700000

    researchmap

  • Exploration of endometrial cancer-associated microRNAs by using a functional screening method and its application to medication

    Grant number:22390313  2010 - 2012

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (B)  Grant-in-Aid for Scientific Research (B)

    AOKI Daisuke, BANNO Kouji, HIRASAWA Akira, NOMURA Hiroyukiu, INAZAWA Johji, KOZAKI Ken-ichi

      More details

    Grant amount:\19110000 ( Direct expense: \14700000 、 Indirect expense:\4410000 )

    The aim of this study is to identify a tumor-suppressor microRNA (miRNA) silenced by aberrant DNA methylation in endometrial cancer. By investigating escalation of expression level of microRNAs after exposure of 5-Aza-CdR in endometrial cancer cells, miR-

    researchmap

  • Exploratory studyof dose adjustmentof oncologic drugs for special populations

    Grant number:22590142  2010 - 2012

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)  Grant-in-Aid for Scientific Research (C)

    IMAMURA Chiyo, TANIGAWARA Yusuke, HIRASAWA Akira

      More details

    Grant amount:\4550000 ( Direct expense: \3500000 、 Indirect expense:\1050000 )

    We studied to explore dose adjustment index of docetaxel for elderly patients with advanced or metastatic Non-Small-Cell Lung Cancer. Although there was a trend that docetaxel CL decreased with increasing patient age, there was great interpatient variabil

    researchmap

  • Alteration of tumor immunity and anti-cancer drug / hormone sensitivity accompanied by MMR mechanism abnormality in endometrial cancer

    Grant number:22591867  2010 - 2012

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)  Grant-in-Aid for Scientific Research (C)

    SUSUMU Nobuyuki, BANNO Kouji, HIRASAWA Akira, YAMAGAMI Wataru

      More details

    Grant amount:\4420000 ( Direct expense: \3400000 、 Indirect expense:\1020000 )

    We detected that those cases with endometrial cancer with many infiltrative regulatory T cells (Treg) were significantly poorly-differentiated or advanced-stage cancer and had poor prognosis, and that those cases with high Treg/CD8 ratio had poor prognosi

    researchmap

  • 遺伝性卵巣がんの一次予防とサーベイランスおよびQOLに関する検討

    2009.04 - 2012.03

    がん研究振興財団 がん研究助成金 

      More details

    Grant type:Competitive

    Grant amount:\9000000

    researchmap

  • 血中メチル化DNAの新規検出方法を利用した喉頭癌・子宮体癌の迅速診断システムの開発

    2009

    独立行政法人新エネルギー・産業技術総合開発機構 産業技術研究助成事業(若手研究グラント) 

    座間 猛

      More details

    Grant type:Competitive

    Grant amount:\5000000

    researchmap

  • 閉経前卵巣摘出施行骨粗鬆症高危険例に対する早期介入および骨粗鬆症個別化治療を目的とした骨代謝・骨粗鬆症治療薬代謝酵素関連遺伝子多型診断ツールの確立

    2009

    第5回リリー研究助成プログラム 

      More details

    Grant type:Competitive

    Grant amount:\800000

    researchmap

  • 全自動遺伝子多型解析システムに向けたゲノム薬理学の臨床応用

    2008.04 - 2010.03

    慶應義塾 外部連携研究創出助成制度 

      More details

    Grant type:Competitive

    Grant amount:\12000000

    researchmap

  • 子宮体癌における統合的ゲノム解析ならびにマイクロRNA解析による分子機構の解明

    2008.04 - 2010.03

    日本学術振興会科学研究費補助金 若手研究(B)  Grant-in-Aid for Scientific Research 

      More details

    Grant type:Competitive

    Grant amount:\3200000

    researchmap

  • Integrative genomic analysis and screening of microRNA expression status in endometrial cancer.

    Grant number:20791165  2008 - 2009

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Young Scientists (B)  Grant-in-Aid for Young Scientists (B)

    HIRASAWA Akira

      More details

    Grant amount:\4160000 ( Direct expense: \3200000 、 Indirect expense:\960000 )

    MicroRNAs (miRNAs) are small non-coding RNAs and negative regulators for their gene targets. Although the tumor-suppressive functions of several miRNAs have been demonstrated, the dysregulation of miRNAs and their molecular mechanisms in endometrial cancer still remain unclear. To identify tumor-suppressive miRNAs (TS-miRs) silenced by DNA hypermethylation during endometrial carcinogenesis, we performed functional screening for TS-miRs in endometrial cancer cell lines. We further analyzed DNA hypermethylation of CpG-islands around mature miRNAs, resulting in identification of some miRNAs as the candidate TS-miRs silencing by CpG island hypermethylation. Our data suggest that these TS-miRs might play an important role in endometrial carcinogenesis.

    researchmap

  • 17q領域に注目した子宮内膜症ならびに卵巣明細胞腺癌発癌メカニズムの解明

    2008

    慶應義塾 学事振興基金 

      More details

    Grant type:Competitive

    Grant amount:\300000

    researchmap

  • スペシャル・ポピュレーションに対する抗がん剤の指摘投与量・用量調節指標の探索

    2007.04 - 2009.03

    日本学術振興会科学研究費補助金 基盤研究(C)  Grant-in-Aid for Scientific Research 

    今村知世

      More details

    Grant type:Competitive

    Grant amount:\200000

    researchmap

  • DVELOPMENT OF HUMAN MONOCLONAL ANTIBODIES WHICH SHOW INHIBITORY EFFECTS TUMOR PROGRESSION.

    Grant number:19390430  2007 - 2009

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (B)  Grant-in-Aid for Scientific Research (B)

    AOKI Daisuke, SUSUMU Nobuyuki, SUZUKI Nao, SUZUKI Atsushi, BANNO Kouji, HIRASAWA Akira, OIKAWA Fumiko

      More details

    Grant amount:\18850000 ( Direct expense: \14500000 、 Indirect expense:\4350000 )

    We have developed a human monoclonal antibody HMMC-1 specific to gynecological cancers and it showed anti tumor activity for gynecological cancers. Mass spectrometry analysis revealed that HMMC-1 antigen was at least CD166. HMMC-1 intereaction with possibly CD166, may have a direct effect on the growth of cells with high metastatic potential. The chlorate treatment demonstrates that sulfation is necessary for HMMC-1 antigen activity.

    researchmap

  • Relation between alteration of DNA mismatch repair/tumor immunologyand sensitivities of anti-cancer drugs and hormone in endometrialcancer

    Grant number:19591943  2007 - 2008

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)  Grant-in-Aid for Scientific Research (C)

    SUSUMU Nobuyuki, BANNO Banno, HIRASAWA Akira, SUGANO Kokichi

      More details

    Grant amount:\4550000 ( Direct expense: \3500000 、 Indirect expense:\1050000 )

    初期子宮体癌113例に対して妊孕性温存療法の高用量黄体ホルモン(MPA)療法を行った。病変消失率はG1腺癌で86.9%、異型増殖症で95.7%と好成績を示したが、再発率はともに約50%と高値であった。再発に影響する因子を多変量解析にて検討すると、遺伝性非ポリポーシス大腸癌関連腫瘍の家系内集積性とhMLH1蛋白発現減弱の2項目が高用量MPA療法後の再発に対する独立予後因子であることが初めて示された。

    researchmap

  • 17q遺伝子増幅に着目した卵巣がん予後関連バイオマーカーの探索

    2007

    慶應義塾 福澤諭吉記念慶應義塾学事振興基金 

      More details

    Grant type:Competitive

    Grant amount:\2820000

    researchmap

  • ゲノム情報に基づいた脂質異常症ならびに骨粗鬆症に関する至適予防法の確立

    2007

    慶應義塾 学事振興基金 

      More details

    Grant type:Competitive

    Grant amount:\200000

    researchmap

  • 17q領域に着目した卵巣明細胞腺癌の悪性形質獲得に関与する遺伝子の探索

    2006.04 - 2008.03

    日本学術振興会科学研究費補助金 若手研究(B)  Grant-in-Aid for Scientific Research 

      More details

    Grant type:Competitive

    Grant amount:\3500000

    researchmap

  • 17q領域に着目した卵巣明細胞腺癌の悪性形質獲得に関与する遺伝子の探索

    Grant number:18791177  2006 - 2007

    日本学術振興会  科学研究費助成事業 若手研究(B)  若手研究(B)

    平沢 晃

      More details

    Grant amount:\3500000 ( Direct expense: \3500000 )

    癌関連遺伝子活性化の分子機構のーつとして特定遺伝子の増幅現象が広く知られている。しかしながら卵巣癌の中でも特に予後不良であるといわれている卵巣明細胞腺癌に特異的な増幅遺伝子については一定の見解が得られていない。申請者らは現在までに卵巣明細胞腺癌における潜在的遺伝子増幅を網羅的に検索する目的で、CGH (Comparative genomic hybridization)法を用い、17q23. 2領域に存在する2遺伝子、APPBP2とPPM1Dが明細胞腺癌の予後関連バイオマーカーになりうることを突き止めた。また同領域に座位するHNF-1βが明細胞腺癌特異的に高発現し、当該遺伝子をターゲットにした分子標的治療の可能性を指摘した。
    さらに、近年開発され、少量のDNA検体で一塩基単位から染色体レベルまで幅広い領域のゲノム変化を多領域同時に効率良く解析可能な遺伝子検査法であるMLPA (Multiplex Llgation-dependent Probe Amplification)法を用いて、従来型のシークエンス等によっても検出困難であった卵巣癌遺伝子大領域欠失や重複の検出を試みた。本法にて遺伝子増幅が知られている72種類の癌関連遺伝子につきゲノムコピー数の多寡を測定した結果、全例で何らかのゲノムコピー数の変化を認めた。さらに本法を用いることにより、卵巣癌における一定の遺伝子増幅プロファイルの作製に成功した。以上の結果よりMLPA法によるゲノム増幅プロファイルの作製は、分子標的医療を含めた個別化治療導入に際して、重要な解析ツールとなりうる可能性を指摘した。

    researchmap

  • 閉経前卵巣摘出後の高脂血症・骨粗鬆症予防を目的とした遺伝子多型診断ツールの開発

    2006

    慶應義塾 総合的研究創出のための研究若手・新人研究者助成 

      More details

    Grant type:Competitive

    Grant amount:\800000

    researchmap

  • 遺伝子多型診断に基づいた塩酸イリノテカン投与によるがん個別化治療の確立

    2006

    慶應義塾 学事振興基金 

      More details

    Grant type:Competitive

    Grant amount:\200000

    researchmap

  • 予後不良卵巣癌に特異的なバイオマーカーの探索と悪性形質獲得機序の解明

    2006

    慶應義塾 福澤諭吉記念慶應義塾学事振興基金 

      More details

    Grant type:Competitive

    Grant amount:\2400000

    researchmap

▼display all

 

Class subject in charge

  • Genomic Medicine (2024academic year) special  - その他

  • Introduction to Medical Genomics (2024academic year) Second semester  - 木7~8

  • Professionalism and Behavior Science 2 (2024academic year) special  - その他

  • Research Presentation in Molecular Medicine (2024academic year) special  - その他

  • Medical AI Seminar (2024academic year) special  - その他

  • Medical AI Introduction (2024academic year) special  - その他

  • Medical AI Advanced Subject I (2024academic year) special  - その他

  • Medical AI Advanced Subject II (2024academic year) special  - その他

  • Medical AI Advanced Subject I (2024academic year) special  - その他

  • Introduction to Clinical Medicine and Dentistry (2024academic year) Concentration  - その他

  • Practicals: Clinical Genomic Medicine (2024academic year) special  - その他

  • Research Projects: Clinical Genomic Medicine (2024academic year) special  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine I (2024academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine I (2024academic year) special  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine II (2024academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine II (2024academic year) special  - その他

  • Genomic Medicine (2023academic year) special  - その他

  • Introduction to Medical Genomics (2023academic year) Second semester  - 木7~8

  • Professionalism and Behavior Science 2 (2023academic year) special  - その他

  • Research Presentation in Molecular Medicine (2023academic year) special  - その他

  • Medical AI Seminar (2023academic year) special  - その他

  • Medical AI Introduction (2023academic year) special  - その他

  • Medical AI Advanced Subject I (2023academic year) special  - その他

  • Medical AI Advanced Subject II (2023academic year) special  - その他

  • Medical AI Advanced Subject I (2023academic year) special  - その他

  • Medical Ethics and Legal and Social Issues (2023academic year) special  - その他

  • Social Medicine and Dentistry (2023academic year) Concentration  - その他

  • Practicals: Clinical Genomic Medicine (2023academic year) special  - その他

  • Research Projects: Clinical Genomic Medicine (2023academic year) special  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine I (2023academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine I (2023academic year) special  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine II (2023academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine II (2023academic year) special  - その他

  • Genomic Medicine (2022academic year) special  - その他

  • Introduction to Medical Genomics (2022academic year) 1st semester  - 火1~2

  • Professionalism and Behavior Science 2 (2022academic year) special  - その他

  • プロフェッショナリズム・行動科学Ⅱ (2022academic year) 特別  - その他

  • Research Presentation in Molecular Medicine (2022academic year) special  - その他

  • Medical AI Seminar (2022academic year) special  - その他

  • Medical AI Introduction (2022academic year) special  - その他

  • Medical AI Advanced Subject I (2022academic year) special  - その他

  • Medical AI Advanced Subject II (2022academic year) special  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine I (2022academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine I (2022academic year) special  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine II (2022academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine II (2022academic year) special  - その他

  • Genomic Medicine (2021academic year) Fourth semester  - その他

  • Professionalism and Behavior Science 2 (2021academic year) Fourth semester  - その他

  • Research Presentation in Molecular Medicine (2021academic year) special  - その他

  • Medical AI Seminar (2021academic year) special  - その他

  • Medical AI Introduction (2021academic year) special  - その他

  • Medical AI Advanced Subject I (2021academic year) special  - その他

  • Medical AI Advanced Subject II (2021academic year) special  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine I (2021academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine I (2021academic year) special  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine II (2021academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine II (2021academic year) special  - その他

  • Genomic Medicine (2020academic year) Fourth semester  - その他

  • Professionalism and Behavior Science 2 (2020academic year) special  - その他

  • Professionalism and Behavior Science 3 (2020academic year) special  - その他

  • Research Presentation in Molecular Medicine (2020academic year) Year-round  - その他

  • Molecular Medicine (2020academic year) Year-round  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine I (2020academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine I (2020academic year) special  - その他

  • Research Projects and Practicals: Clinical Genomic Medicine II (2020academic year) special  - その他

  • Lecture and Research Projects: Clinical Genomic Medicine II (2020academic year) special  - その他

▼display all

 

Social Activities

  • 玉野市×岡山大学イベント市民公開講座 聞いてみられー!来てみられー!遺伝の話

    Role(s):Appearance

    玉野市  玉野市市民公開講座  2024.8.18

     More details

    Type:Science festival

    researchmap

  • 第 10 回リンチ症候群研究会・日本消化器病学会関連研究会第6回がんゲノム医療時代における Lynch 症候群研究会 市民公開フォーラム

    Role(s):Lecturer

    厚生労働科学研究費補助金 がん対策推進総合研究事業 「ゲノム情報に応じたがん予防にかかる指針の策定と遺伝性腫瘍に関する医療・社会体制の整備および国民の理解と参画に関する研究」班  2024.8.11

     More details

    Type:Lecture

    researchmap

  • がん市民公開講座

    Role(s):Appearance

    埼玉県立がんセンター、厚生労働科学研究費補助金 がん対策推進総合研究事業 「ゲノム情報に応じたがん予防にかかる指針の策定と遺伝性腫瘍に関する医療・社会体制の整備および国民の理解と参画に関する研究」班  2024.6.14

     More details

    Type:Lecture

    researchmap

  • 遺伝性腫瘍としての婦人科がん

    Role(s):Appearance

    国際医療福祉大学大学院 多職種協働市民公開シンポジウム  文部科学省事業「次世代のがんプロフェッショナ ル養成プラン」  2023.10.22

     More details

    Type:Lecture

    researchmap

  • がんは遺伝しますか?遺伝子で体質を知り, がんを防ぐ時代へ ~多遺伝子パネル検査の活用による遺伝性がんの予防~

    Role(s):Appearance, Lecturer

    厚生労働科学研究費補助金 がん対策推進総合研究事業 ゲノム情報を活用した遺伝性腫瘍の先制的医療提供体制の整備に関する研究(櫻井班)  2023.3.21

     More details

    Type:Lecture

    researchmap

  • 遺伝を知ることでがんを予防する

    Role(s):Lecturer

    姫路赤十字病院  姫路赤十字病院 ~第50回市民講座 がんについてもっと知ろう~  2023.2.12

     More details

    Type:Lecture

    researchmap

  • 実地診療から考える多遺伝子パネル検査(MGPT)の有用性と課題

    Role(s):Lecturer

    厚生労働科学研究費補助金(がん対策推進総合研究事業)「ゲノム情報を活用した遺伝性腫瘍の先制的医療提供体制の整備に関する研究」班(研究代表:櫻井晃洋)  第3回 厚労科研研究班Webセミナー  2022.11.23

     More details

  • がんゲノム医療と遺伝性腫瘍

    Role(s):Lecturer

    厚生労働省科学研究費補助金がん対策推進総合研究事業(瀬戸班)  市民公開セミナー「がん遺伝子パネル検査のアンケート調査研究」  2022.10.10

     More details

    Type:Internet

    researchmap

  • 卵巣がんは遺伝と関係あるの?

    Role(s):Lecturer

    卵巣癌市民公開講座  2022.5.29

     More details

    Type:Internet

    researchmap

  • 家族でがんを予防する 〜がんと遺伝について〜

    Role(s):Lecturer

    広島市立広島市民病院  第12回がん診療連携拠点病院共催市民講演会  2021.10.15 - 2021.10.30

     More details

    Type:Internet

    researchmap

  • 女性のがんと遺伝

    Role(s):Lecturer

    津山ガン対策協議会  第41回津山地区がん征圧大会  2021.10.9

     More details

    Type:Lecture

    researchmap

  • わが家ってがん家系? 家族で考えるがん予防

    Role(s):Lecturer

    香川県立図書館  香川県立図書館 健やか生活応援講座 おしえて!がんゲノム医療  2021.2.13

     More details

    Type:Citizen’s meeting/Assembly

    researchmap

  • せとうち医療地域を見据えた遺伝性腫瘍への対応.

    Role(s):Lecturer, Planner

    香川県立中央病院  香川県立中央病院 市民公開講座みんなで考えよう!遺伝性乳がん卵巣がん  2020.2.11

     More details

    Type:Citizen’s meeting/Assembly

    researchmap

  • 公開講座 がんと遺伝 ~リスクを知って予防をめざす~

    Role(s):Lecturer, Planner

    岡山健康講座  2019.9.13

     More details

    Type:Citizen’s meeting/Assembly

    researchmap

  • 公開講座 女性のがんと遺伝 リスクをきちんと知ってがん予防につなげる

    Role(s):Lecturer, Planner

    香川県立中央病院  2019.6.2

     More details

    Type:Citizen’s meeting/Assembly

    researchmap

  • 女性のがんと遺伝.

    Role(s):Lecturer, Planner

    岡山臨床遺伝カンファレンス  2019.5.11

     More details

  • 公開講座 がんと遺伝の関係について.

    Role(s):Lecturer, Planner

    香川県立中央病院  2019.3.2

     More details

    Type:Citizen’s meeting/Assembly

    researchmap

  • 世界の医学研究に貢献するバイオバンク

    Role(s):Lecturer

    サイエンスカフェ@ナレッジキャピタル  サイエンスカフェ@ナレッジキャピタル  2018.12.18

     More details

    Type:Science cafe

    researchmap

  • 遺伝性の卵巣がんと遺伝カウンセリング外来

    Role(s):Lecturer, Planner

    厚生労働科学研究費補助金がん対策推進総合研究事業 「ゲノム情報を活用した遺伝性乳癌卵巣癌診療の標準化と先制医療実装にむけたエビデンス構築に関する研究」班 市民公開講座  私のがんは遺伝ですか?家族のがんは遺伝ですか? ~あるある市民公開講座inおかやま~  2018.10.8

     More details

    Type:Citizen’s meeting/Assembly

    researchmap

▼display all

Media Coverage

  • 遺伝の仕組み知って Newspaper, magazine

    山陽新聞  2024.8.21

     More details

  • 遺伝子回生結果を活用した健康づくり Promotional material

    玉野市  広報 たまの No.1284  2024.8

     More details

    Author:Other 

    researchmap

  • 検査で発見 「遺伝性がん」は予防的切除が選択肢に Newspaper, magazine

    文藝春秋  文藝春秋社  pp193-202  2024.5

     More details

  • 遺伝子検査で病気予防 岡山大や玉野市がモデル事業 90疾患発症リスク低減 専門家が保健指導 Newspaper, magazine

    日本経済新聞  中国四国版  2024.5

     More details

  • 遺伝子検査で病気を予防 Newspaper, magazine

    山陽新聞  2024.4

     More details

  • 「市民に無料で遺伝子検査→専門家が将来の病気リスクや対策を説明」健康増進へ玉野市・岡山大・企業が連携 TV or radio program

    KSB  2024.4

     More details

  • 遺伝情報活用で健康増進 岡山大など連携「究極の地域医療に」 Newspaper, magazine

    毎日新聞  2024.4

     More details

  • 遺伝子検査を活用 発症リスク分析 岡山大と玉野市 全国初の事業 Newspaper, magazine

    山陽新聞  2024.4

     More details

  • 文藝春秋 スーパードクターに教わる最新治療 2024 Newspaper, magazine

    文藝春秋  がんゲノム医療  2023.11

     More details

  • 医療ルネサンス 卵巣がん<4>「遺伝性」 予防切除を検討 Newspaper, magazine

    読売新聞  読売新聞  2023.7

     More details

  • がん治療のリアル・遺伝子でわかること Newspaper, magazine

    毎日新聞  2023.5

     More details

  • 遺伝情報の適切な共有探る 患者らの利益に、岡山大 日本医学会も指針改定 Newspaper, magazine

    共同通信  共同通信  47NEWS 52新聞社と共同通信のよんななニュース  2023.3

     More details

  • 一人ひとりの遺伝情報に基づいたがん予防 Newspaper, magazine

    ビサビ  ビサビ  2023.3

     More details

  • どうすれば安全安心:遺伝情報の保護と共有 患者の利益へ「適切」模索

    毎日新聞  全国版夕刊  2023.2.16

     More details

  • 遺伝学的検査から分かるがんのリスク ひとりひとりに合わせたがんの早期発見・早期治療へ Newspaper, magazine

    産経新聞  産経新聞中国版  2023.1.29

     More details

    Author:Myself 

    researchmap

  • 遺伝子情報を知ることでがん予防が可能となることがあります Newspaper, magazine

    産経新聞  2022.10.7

     More details

  • 岡山のグッドトクター 遺伝子の特徴を知ってがんの予防・早期発見を Promotional material

    山陽新聞・OHKの生活情報誌「さりお」  2022.9.23

     More details

  • 遺伝的な特徴を知ることで予防できるがんがある Newspaper, magazine

    産経新聞  2022.6.24

     More details

  • 中国・四国地方の住民と医療機関の協力による遺伝性のがんに対する取り組み Newspaper, magazine

    産経新聞  2021.1.29

     More details

  • 香川の医療最前線 がんゲノム医療 最適な治療法探る Newspaper, magazine

    四国新聞  2019.2.17

     More details

  • 岡山大学病院のがんゲノム医療とは 新設診療科長の平沢教授に聞く Newspaper, magazine

    山陽新聞  2018.9.9

     More details

  • がんゲノム医療へ診療科 岡山大学病院きょう開設 治療、予防法探る Newspaper, magazine

    山陽新聞  2018.9.1

     More details

  • 山陽新聞こども記者 がんゲノム医療 遺伝子解析し薬選ぶ Newspaper, magazine

    山陽新聞  2018.8

     More details

▼display all