Faculty Profiles - KANAYAMA Naoki

写真a

KANAYAMA Naoki

Organization

Faculty of Interdisciplinary Science and Engineering in Health Systems Associate Professor

Contact information

Homepage

https://sites.google.com/view/molcelleng/

External link

Degree

Ph. D. ( Kyoto University )

Research Interests

リンパ球
B細胞
細胞工学
免疫
抗体
Antibody
Lymphocyte

Research Areas

Life Science / Functional biochemistry
Nanotechnology/Materials / Bio chemistry
Life Science / Immunology
Manufacturing Technology (Mechanical Engineering, Electrical and Electronic Engineering, Chemical Engineering) / Biofunction and bioprocess engineering

Education

京都大学大学院工学研究科合成・生物化学専攻

- 1998

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Country： Japan

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Kyoto University

- 1998

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Kyoto University

- 1992

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Kyoto University 工学部工業化学

- 1992

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Country： Japan

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Research History

Okayama University Graduate School of Interdisciplinary Science and Engineering in Health Systems Associate Professor

2018.4

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岡山大学自然科学研究科機能分子化学専攻

2007.4 - 2018.3

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- Associate Professor,Chemistry and Biochemistry,Graduate School of Natural Science and Technology,Okayama University

2007

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Associate Professor,Chemistry and Biochemistry,Graduate School of Natural Science and Technology,Okayama University

2005 - 2007

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岡山大学自然科学研究科機能分子化学専攻助教授

2005 - 2007

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Senior Assistant Professor,Dept. of Bioscience and Biotechnology,Faculty of Engineering,Okayama University

2002 - 2005

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Okayama University Faculty of Engineering, Department of Bioscience and Biotechnology

2002 - 2005

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Research Associate,Dept. of Bioscience and Biotechnology,Faculty of Engineering,Okayama University

1998 - 2002

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Okayama University Faculty of Engineering, Department of Bioscience and Biotechnology

1998 - 2002

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Postdoctoral Fellowships of Japan Society for the Promotion of Science

1996 - 1998

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Kyoto University Graduate School of Engineering, Department of Synthetic Chemistry and Biological Chemistry

1996 - 1998

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Professional Memberships

Japanese Society of Immunology

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The Japanese Biochemical Society

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The Society of Biotechnoloty, Japan

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The Molecular Biology Society of Japan

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日本農芸化学会

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日本生化学会

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日本分子生物学会

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日本免疫学会

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日本生物工学会

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Papers

The immunoreceptor SLAMF8 promotes the differentiation of follicular dendritic cell-dependent monocytic cells with B cell-activating ability. Reviewed International journal

Masaki Magari, Miku Nishioka, Tomomi Hari, Sayaka Ogawa, Kaho Takahashi, Naoya Hatano, Naoki Kanayama, Junichiro Futami, Hiroshi Tokumitsu

FEBS letters 596 ( 20 ) 2659 - 2667 2022.8

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

Follicular dendritic cells (FDCs) play a crucial role in generating high-affinity antibody-producing B cells during the germinal center (GC) reaction. Herein, we analysed the altered gene expression profile of a mouse FDC line, FL-Y, following lymphotoxin β receptor stimulation, and observed increased Slam-family member 8 (Slamf8) mRNA expression. Forced Slamf8 expression and SLAMF8-Fc addition enhanced the ability of FL-Y cells to induce FDC-induced monocytic cell (FDMC) differentiation. FDMCs accelerated GC-phenotype proliferation in cultured B cells, suggesting that they are capable of promoting GC responses. Furthermore, a pulldown assay showed that SLAMF8-Fc could bind to SLAMF8-His. Overall, the homophilic interaction of SLAMF8 promotes FDMC differentiation and SLAMF8 might act as a novel regulator of GC responses by regulating FDMC differentiation.

DOI： 10.1002/1873-3468.14468

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Substrate recognition by Arg/Pro‐rich insert domain in calcium/calmodulin‐dependent protein kinase kinase for target protein kinases Reviewed

Riku Kaneshige, Satomi Ohtsuka, Yuhei Harada, Issei Kawamata, Masaki Magari, Naoki Kanayama, Naoya Hatano, Hiroyuki Sakagami, Hiroshi Tokumitsu

The FEBS Journal 289 ( Issue19 ) 5971 - 5984 2022.5

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Publishing type：Research paper (scientific journal) Publisher：Wiley

DOI： 10.1111/febs.16467

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Conformation-Dependent Reversible Interaction of Ca²⁺/Calmodulin-Dependent Protein Kinase Kinase with an Inhibitor, TIM-063 Reviewed

Satomi Ohtsuka, Taisei Okumura, Yuna Τabuchi, Tomoyuki Miyagawa, Naoki Kanayama, Masaki Magari, Naoya Hatano, Hiroyuki Sakagami, Futoshi Suizu, Teruhiko Ishikawa, Hiroshi Tokumitsu

Biochemistry 61 ( 7 ) 545 - 553 2022.3

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Publishing type：Research paper (scientific journal) Publisher：American Chemical Society (ACS)

DOI： 10.1021/acs.biochem.1c00796

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Oligomerization of Ca2+/calmodulin-dependent protein kinase kinase Reviewed International journal

Yusei Fukumoto, Yuhei Harada, Satomi Ohtsuka, Naoki Kanayama, Masaki Magari, Naoya Hatano, Hiroyuki Sakagami, Hiroshi Tokumitsu

Biochemical and Biophysical Research Communications 587 160 - 165 2022.1

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

Ca2+/calmodulin-dependent protein kinase kinases (CaMKKα and β) are regulatory kinases for multiple downstream kinases, including CaMKI, CaMKIV, PKB/Akt, and AMP-activated protein kinase (AMPK) through phosphorylation of each activation-loop Thr residue. In this report, we biochemically characterize the oligomeric structure of CaMKK isoforms through a heterologous expression system using COS-7 cells. Oligomerization of CaMKK isoforms was readily observed by treating CaMKK transfected cells with cell membrane permeable crosslinkers. In addition, His-tagged CaMKKα (His-CaMKKα) pulled down with FLAG-tagged CaMKKα (FLAG-CaMKKα) in transfected cells. The oligomerization of CaMKKα was confirmed by the fact that GST-CaMKKα/His-CaMKKα complex from transiently expressed COS-7 cells extracts was purified to near homogeneity by the sequential chromatography using glutathione-sepharose/Ni-sepharose and was observed in a Ca2+/CaM-independent manner by reciprocal pulldown assay, suggesting the direct interaction between monomeric CaMKKα. Furthermore, the His-CaMKKα kinase-dead mutant (D293A) complexed with FLAG-CaMKKα exhibited significant CaMKK activity, indicating the active CaMKKα multimeric complex. Collectively, these results suggest that CaMKKα can self-associate in the cells, constituting a catalytically active oligomer that might be important for the efficient activation of CaMKK-mediated intracellular signaling.

DOI： 10.1016/j.bbrc.2021.11.105

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Regulation of the tubulin polymerization-promoting protein by Ca2+/S100 proteins Reviewed

Seita Doi, Naoki Fujioka, Satomi Ohtsuka, Rina Kondo, Maho Yamamoto, Miwako Denda, Masaki Magari, Naoki Kanayama, Naoya Hatano, Ryo Morishita, Takafumi Hasegawa, Hiroshi Tokumitsu

Cell Calcium 96 102404 - 102404 2021.6

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

DOI： 10.1016/j.ceca.2021.102404

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Identification and Biochemical Characterization of High Mobility Group Protein 20A as a Novel Ca2+/S100A6 Target Reviewed

Maho Yamamoto, Rina Kondo, Haruka Hozumi, Seita Doi, Miwako Denda, Masaki Magari, Naoki Kanayama, Naoya Hatano, Ryo Morishita, Hiroshi Tokumitsu

Biomolecules 11 ( 4 ) 510 - 510 2021.3

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

DOI： 10.3390/biom11040510

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Development and Characterization of Novel Molecular Probes for Ca2+/Calmodulin-Dependent Protein Kinase Kinase, Derived from STO-609. Reviewed International journal

Satomi Ohtsuka, Yui Ozeki, Moeno Fujiwara, Tomoyuki Miyagawa, Naoki Kanayama, Masaki Magari, Naoya Hatano, Futoshi Suizu, Teruhiko Ishikawa, Hiroshi Tokumitsu

Biochemistry 59 ( 17 ) 1701 - 1710 2020.5

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Ca2+/calmodulin-dependent protein kinase kinase (CaMKK) activates particular multifunctional kinases, including CaMKI, CaMKIV, and 5'AMP-activated protein kinase (AMPK), resulting in the regulation of various Ca2+-dependent cellular processes, including neuronal, metabolic, and pathophysiological pathways. We developed and characterized a novel pan-CaMKK inhibitor, TIM-063 (2-hydroxy-3-nitro-7H-benzo[de]benzo[4,5]imidazo[2,1-a]isoquinolin-7-one) derived from STO-609 (7H-benzimidazo[2,1-a]benz[de]isoquinoline-7-one-3-carboxylic acid), and an inactive analogue (TIM-062) as molecular probes for the analysis of CaMKK-mediated cellular responses. Unlike STO-609, TIM-063 had an inhibitory activity against CaMKK isoforms (CaMKKα and CaMKKβ) with a similar potency (Ki = 0.35 μM for CaMKKα, and Ki = 0.2 μM for CaMKKβ) in vitro. Two TIM-063 analogues lacking a nitro group (TIM-062) or a hydroxy group (TIM-064) completely impaired CaMKK inhibitory activities, indicating that both substituents are necessary for the CaMKK inhibitory activity of TIM-063. Enzymatic analysis revealed that TIM-063 is an ATP-competitive inhibitor that directly targets the catalytic domain of CaMKK, similar to STO-609. TIM-063 suppressed the ionomycin-induced phosphorylation of exogenously expressed CaMKI, CaMKIV, and endogenous AMPKα in HeLa cells with an IC50 of ∼0.3 μM, and it suppressed CaMKK isoform-mediated CaMKIV phosphorylation in transfected COS-7 cells. Thus, TIM-063, but not the inactive analogue (TIM-062), displayed cell permeability and the ability to inhibit CaMKK activity in cells. Taken together, these results indicate that TIM-063 could be a useful tool for the precise analysis of CaMKK-mediated signaling pathways and may be a promising lead compound for the development of therapeutic agents for the treatment of CaMKK-related diseases.

DOI： 10.1021/acs.biochem.0c00149

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Phosphorylation and dephosphorylation of Ca2+/calmodulin-dependent protein kinase kinase β at Thr144 in HeLa cells Reviewed International journal

Shota Takabatake, Yusei Fukumoto, Satomi Ohtsuka, Naoki Kanayama, Masaki Magari, Hiroyuki Sakagami, Naoya Hatano, Hiroshi Tokumitsu

Biochemical and Biophysical Research Communications 525 ( 1 ) 251 - 257 2020.4

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

Ca2+/calmodulin-dependent protein kinase kinase β (CaMKKβ) acts as a regulatory kinase that phosphorylates and activates multiple downstream kinases including CaMKI, CaMKIV, 5'AMP-activated protein kinase (AMPK) and protein kinase B (PKB), resulting in regulation of wide variety of Ca2+-dependent physiological responses under normal and pathological conditions. CaMKKβ is regulated by Ca2+/calmodulin-binding, autophosphorylation, and transphosphorylation by multiple protein kinases including cAMP-dependent protein kinase (PKA). In this report, we found that phosphorylation of CaMKKβ is dynamically regulated by protein phosphatase/kinase system in HeLa cells. Global phosphoproteomic analysis revealed the constitutive phosphorylation at 8 Ser residues including Ser128, 132, and 136 in the N-terminal regulatory domain of rat CaMKKβ in unstimulated HeLa cells as well as inducible phosphorylation of Thr144 in the cells treated with a phosphatase inhibitor, okadaic acid (OA). Thr144 phosphorylation in CaMKKβ has shown to be rapidly induced by OA treatment in a time- and dose-dependent manner in transfected HeLa cells, indicating that Thr144 in CaMKKβ is maintained unphosphorylated state by protein phosphatase(s). We confirmed that in vitro dephosphorylation of pThr144 in CaMKKβ by protein phosphatase 2A and 1. We also found that the pharmacological inhibition of protein phosphatase(s) significantly induces CaMKKβ-phosphorylating activity (at Thr144) in HeLa cell lysates as well as in intact cells; however, it was unlikely that this activity was catalyzed by previously identified Thr144-kinases, such as AMPK and PKA. Taken together, these results suggest that the phosphorylation and dephosphorylation of Thr144 in CaMKKβ is dynamically regulated by multiple kinases/phosphatases signaling resulting in fine-tuning of the enzymatic property.

DOI： 10.1016/j.bbrc.2020.02.056

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SRSF1-3, a splicing and somatic hypermutation regulator, controls transcription of IgV genes via chromatin regulators SATB2, UBN1 and histone variant H3.3. Reviewed International coauthorship International journal

Amit Kumar Singh, Anubhav Tamrakar, Ankit Jaiswal, Naoki Kanayama, Prashant Kodgire

Molecular immunology 119 69 - 82 2020.1

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SRSF1, a member of the SR protein family, is an important splicing factor and regulator of splicing. Multiple splicing isoforms have been reported for this gene. SRSF1-3, a splicing isoform of SRSF1, is necessary for AID-dependent SHM of IgV genes. However, its precise role in SHM remains enigmatic. Transcriptomic analysis of SRSF1-3 reconstituted cells shows upregulation of transcription factor SATB2 and chromatin regulator UBN1. The increased SATB2 and UBN1 are strikingly enriched in the MAR and promoter regions of the IgL gene, respectively. Furthermore, UBN1 enrichment at the promoter region was coupled with a hundred-fold enhanced occupancy of the histone variant H3.3 at the IgL promoter, that is a hallmark of efficient SHM. The enhanced occupancy of SATB2 at the MAR, UBN1 and histone variant H3.3 at the IgL promoter leads to an increase in IgL transcription, revealing a role of SRSF1-3 in SHM. Thus, SRSF1-3 is likely involved in the regulation of SHM, via upregulation of a crucial transcription factor SATB2, as well as, by overexpression of a chromatin modulator of Ig genes, UBN1, which further assists in the recruitment of the histone variant H3.3. Furthermore, the splicing isoform SRSF1-3 regulates alternate splicing pattern of splicing isoforms for various crucial genes. The present study provides the first evidence that a splicing isoform of an SR protein can regulate the post-transcriptional processing of RNA in vivo.

DOI： 10.1016/j.molimm.2020.01.005

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Splicing regulator SRSF1-3 that controls somatic hypermutation of IgV genes interacts with topoisomerase 1 and AID Reviewed International coauthorship International journal

Kumar Singh, A., Tamrakar, A., Jaiswal, A., Kanayama, N., Agarwal, A., Tripathi, P., Kodgire, P.

Molecular Immunology 116 63 - 72 2019.10

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DOI： 10.1016/j.molimm.2019.10.002

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Regulation of Ca²⁺/calmodulin-dependent protein kinase kinase β by cAMP signaling. Reviewed International journal

Takabatake S, Ohtsuka S, Sugawara T, Hatano N, Kanayama N, Magari M, Sakagami H, Tokumitsu H

Biochimica et biophysica acta. General subjects 1863 ( 4 ) 672 - 680 2019.1

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BACKGROUND: Ca2+/calmodulin-dependent protein kinase kinase (CaMKK) is a pivotal activator of CaMKI, CaMKIV and 5'-AMP-activated protein kinase (AMPK), controlling Ca2+-dependent intracellular signaling including various neuronal, metabolic and pathophysiological responses. Recently, we demonstrated that CaMKKβ is feedback phosphorylated at Thr144 by the downstream AMPK, resulting in the conversion of CaMKKβ into Ca2+/CaM-dependent enzyme. However, the regulatory phosphorylation of CaMKKβ at Thr144 in intact cells and in vivo remains unclear. METHODS: Anti-phosphoThr144 antibody was used to characterize the site-specific phosphorylation of CaMKKβ in immunoprecipitated samples from mouse cerebellum and in transfected mammalian cells that were treated with various agonists and protein kinase inhibitors. CaMKK activity assay and LC-MS/MS analysis were used for biochemical characterization of phosphorylated CaMKKβ. RESULTS: Our data suggest that the phosphorylation of Thr144 in CaMKKβ is rapidly induced by cAMP/cAMP-dependent protein kinase (PKA) signaling in CaMKKβ-transfected HeLa cells, that is physiologically relevant in mouse cerebellum. We confirmed that the catalytic subunit of PKA was capable of directly phosphorylating CaMKKβ at Thr144 in vitro and in transfected cells. In addition, the basal phosphorylation of CaMKKβ at Thr144 in transfected HeLa cells was suppressed by AMPK inhibitor (compound C). PKA-catalyzed phosphorylation reduced the autonomous activity of CaMKKβ in vitro without significant effect on the Ca2+/CaM-dependent activity, resulting in the conversion of CaMKKβ into Ca2+/CaM-dependent enzyme. CONCLUSION: cAMP/PKA signaling may confer Ca2+-dependency to the CaMKKβ-mediated signaling pathway through direct phosphorylation of Thr144 in intact cells. GENERAL SIGNIFICANCE: Our results suggest a novel cross-talk between cAMP/PKA and Ca2+/CaM/CaMKKβ signaling through regulatory phosphorylation.

DOI： 10.1016/j.bbagen.2018.12.012

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Interleukin 34 (IL-34) cell-surface localization regulated by the molecular chaperone 78-kDa glucose-regulated protein facilitates the differentiation of monocytic cells Reviewed

Ogawa, S., Matsuoka, Y., Takada, M., Matsui, K., Yamane, F., Kubota, E., Yasuhara, S., Hieda, K., Kanayama, N., Hatano, N., Tokumitsu, H., Magari, M.

The Journal of biological chemistry 294 ( 7 ) 2386 - 2396 2019

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DOI： 10.1074/jbc.RA118.006226

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Interaction of S100A6 with target proteins in vitro and in living cells Reviewed

Sakane, K., Yamaguchi, F., Tsuchiya, M., Kondo, R., Kanayama, N., Magari, M., Hatano, N., Kobayashi, R., Tokumitsu, H.

Methods in Molecular Biology 1929 367 - 377 2019

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Language：English Publishing type：Research paper (scientific journal) Publisher：Methods in Molecular Biology

DOI： 10.1007/978-1-4939-9030-6_23

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ヘルスシステムの理解とその応用濾胞樹状細胞による抗体の親和性成熟の制御機構の解明(Interdisciplinary Science and Engineering in Health Systems Immunological functions of follicular dendritic cells on affinity maturation of antibody)

Magari Masaki, Ogawa Sayaka, Matsuoka Yukiko, Takada Miho, Kanayama Naoki, Tokumitsu Hiroshi

生物物理 58 ( Suppl.1-2 ) S197 - S197 2018.8

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Language：English Publisher：(一社)日本生物物理学会

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AMP-activated protein kinase-mediated feedback phosphorylation controls the Ca2+/calmodulin (CaM) dependence of Ca2+/CaM-dependent protein kinase kinase Reviewed

Akihiro Nakanishi, Naoya Hatano, Yuya Fujiwara, Arian Sha'ri, Shota Takabatake, Hiroki Akano, Naoki Kanayama, Masaki Magari, Naohito Nozaki, Hiroshi Tokumitsu

JOURNAL OF BIOLOGICAL CHEMISTRY 292 ( 48 ) 19804 - 19813 2017.12

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DOI： 10.1074/jbc.M117.805085

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Identification and characterization of a centrosomal protein, FOR20 as a novel S100A6 target Reviewed

Kyohei Sakane, Miyu Nishiguchi, Miwako Denda, Fuminori Yamagchi, Masaki Magari, Naoki Kanayama, Ryo Morishita, Hiroshi Tokumitsu

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS 491 ( 4 ) 980 - 985 2017.9

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

DOI： 10.1016/j.bbrc.2017.07.161

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SRSF1-3 contributes to diversification of the immunoglobulin variable region gene by promoting accumulation of AID in the nucleus Reviewed

Yuka Kawaguchi, Hiroaki Nariki, Naoko Kawamoto, Yuichi Kanehiro, Satoshi Miyazaki, Mari Suzuki, Masaki Magari, Hiroshi Tokumitsu, Naoki Kanayama

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS 485 ( 2 ) 261 - 266 2017.4

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Authorship：Last author,　Corresponding author Language：English Publishing type：Research paper (scientific journal)

DOI： 10.1016/j.bbrc.2017.02.097

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SRSF1-3 has a role in nuclear localization of AID by regulating its nuclear export Reviewed

N. Kanayama, Y. Kawaguchi, N. Kawamoto, H. Nariki, S. Miyazaki, K. Yokoyama, M. Magari, H. Ohmori, H. Tokumitsu

EUROPEAN JOURNAL OF IMMUNOLOGY 46 1142 - 1142 2016.8

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Authorship：Lead author,　Corresponding author Language：English Publishing type：Research paper (international conference proceedings)

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IL-34-dependent differentiation of monocytic cell with B cell stimulating activity Reviewed

M. Magari, S. Ogawa, Y. Toya, K. Hieda, F. Yamane, N. Kanayama, H. Tokumitsu, H. Ohmori

EUROPEAN JOURNAL OF IMMUNOLOGY 46 1139 - 1139 2016.8

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Language：English Publishing type：Research paper (international conference proceedings)

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Analysis of a role for SRSF1-3 in a transcription-coupled process during IgV hypermutation Reviewed

Y. Kawaguchi, K. Yokoyama, N. Kawamoto, H. Nariki, Y. Matsuyama, Y. Kanehiro, T. Hikasa, M. Magari, H. Ohmori, H. Tokumitsu, N. Kanayama

EUROPEAN JOURNAL OF IMMUNOLOGY 46 1267 - 1268 2016.8

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Identification of striated muscle activator of Rho signaling (STARS) as a novel calmodulin target by a newly developed genome-wide screen Reviewed

Yusui Furuya, Miwako Denda, Kyohei Sakane, Tomoko Ogusu, Sumio Takahashi, Masaki Magari, Naoki Kanayama, Ryo Morishita, Hiroshi Tokumitsu

CELL CALCIUM 60 ( 1 ) 32 - 40 2016.7

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DOI： 10.1016/j.ceca.2016.04.004

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Differential AMP-activated Protein Kinase (AMPK) Recognition Mechanism of Ca2+/Calmodulin-dependent Protein Kinase Kinase Isoforms Reviewed

Yuya Fujiwara, Yoshinori Kawaguchi, Tomohito Fujimoto, Naoki Kanayama, Masaki Magari, Hiroshi Tokumitsu

JOURNAL OF BIOLOGICAL CHEMISTRY 291 ( 26 ) 13802 - 13808 2016.6

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DOI： 10.1074/jbc.M116.727867

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Analysis of Distinct Roles of CaMKK Isoforms Using STO-609-Resistant Mutants in Living Cells Reviewed

Yuya Fujiwara, Yuri Hiraoka, Tomohito Fujimoto, Naoki Kanayama, Masaki Magari, Hiroshi Tokumitsu

BIOCHEMISTRY 54 ( 25 ) 3969 - 3977 2015.6

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DOI： 10.1021/acs.biochem.5b00149

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CSF-1 receptor-mediated differentiation of a new type of monocytic cell with B cell-stimulating activity: its selective dependence on IL-34 Reviewed

Fumihiro Yamane, Yumiko Nishikawa, Kazue Matsui, Miki Asakura, Eriko Iwasaki, Koji Watanabe, Hikaru Tanimoto, Hiroki Sano, Yuki Fujiwara, E. Richard Stanley, Naoki Kanayama, Neil A. Mabbott, Masaki Magari, Hitoshi Ohmori

JOURNAL OF LEUKOCYTE BIOLOGY 95 ( 1 ) 19 - 31 2014.1

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DOI： 10.1189/jlb.0613311

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In vitro substrate phosphorylation by Ca2+/calmodulin-dependent protein kinase kinase using guanosine-5 '-triphosphate as a phosphate donor Reviewed

Saki Yurimoto, Tomohito Fujimoto, Masaki Magari, Naoki Kanayama, Ryoji Kobayashi, Hiroshi Tokumitsu

BMC BIOCHEMISTRY 13 27 2012.12

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DOI： 10.1186/1471-2091-13-27

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Activation-induced cytidine deaminase (AID)-dependent somatic hypermutation requires a splice isoform of the serine/arginine-rich (SR) protein SRSF1 Reviewed

Yuichi Kanehiro, Kagefumi Todo, Misaki Negishi, Junji Fukuoka, Wenjian Gan, Takuya Hikasa, Yoshiaki Kaga, Masayuki Takemoto, Masaki Magari, Xialu Li, James L. Manley, Hitoshi Ohmori, Naoki Kanayama

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 109 ( 4 ) 1216 - 1221 2012.1

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Authorship：Last author,　Corresponding author Language：English Publishing type：Research paper (scientific journal)

DOI： 10.1073/pnas.1120368109

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Flow cytometry-"follow previous" to count the order side by side

Kanayama, N.

Seibutsu-kogaku Kaishi 90 ( 12 ) 2012

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IL-21-Dependent B Cell Death Driven by Prostaglandin E-2, a Product Secreted from Follicular Dendritic Cells Reviewed

Masaki Magari, Yumiko Nishikawa, Yasumasa Fujii, Yumi Nishio, Koji Watanabe, Michiya Fujiwara, Naoki Kanayama, Hitoshi Ohmori

JOURNAL OF IMMUNOLOGY 187 ( 8 ) 4210 - 4218 2011.10

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DOI： 10.4049/jimmunol.1100934

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Efficient affinity maturation of antibodies in an engineered chicken B cell line DT40-SW by increasing point mutation Reviewed

Masamichi Kajita, Takahiro Okazawa, Mika Ikeda, Kagefumi Todo, Masaki Magari, Naoki Kanayama, Hitoshi Ohmori

JOURNAL OF BIOSCIENCE AND BIOENGINEERING 110 ( 3 ) 351 - 358 2010.9

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DOI： 10.1016/j.jbiosc.2010.03.006

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Enhancement of hypermutation frequency in the chicken B cell line DT40 for efficient diversification of the antibody repertoire Reviewed

Masaki Magari, Yuichi Kanehiro, Kagefumi Todo, Mika Ikeda, Naoki Kanayama, Hitoshi Ohmori

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS 396 ( 2 ) 353 - 358 2010.5

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DOI： 10.1016/j.bbrc.2010.04.096

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Conditional transformation of immunoglobulin mutation pattern from gene conversion into point mutation by controlling XRCC3 expression in the DT40 B cell line Reviewed

Masamichi Kajita, Masaki Magari, Kagefumi Todo, Naoki Kanayama, Hitoshi Ohmori

JOURNAL OF BIOSCIENCE AND BIOENGINEERING 109 ( 4 ) 407 - 410 2010.4

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DOI： 10.1016/j.jbiosc.2009.09.050

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Enhancement of antibody production from a chicken B cell line DT40 by reducing Pax5 expression Reviewed

Masaki Magari, Takahiro Aya, Mika Ikeda, Kagefumi Todo, Naoki Kanayama, Hitoshi Ohmori

JOURNAL OF BIOSCIENCE AND BIOENGINEERING 107 ( 2 ) 206 - 209 2009.2

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DOI： 10.1016/j.jbiosc.2008.09.014

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Creation of Valuable Antibodies by an In Vitro Antibody Generation System Using a Hypermutating B Cell Line Reviewed

Naoki Kanayama, Kagefumi Todo, Masaki Magari, Hitoshi Ohmori

YAKUGAKU ZASSHI-JOURNAL OF THE PHARMACEUTICAL SOCIETY OF JAPAN 129 ( 1 ) 11 - 17 2009.1

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Language：Japanese

DOI： 10.1248/yakushi.129.11

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Basic Research and Development on Generation Mechanism of High Affinity Antibodies Invited Reviewed

Naoki Kanayama

Seibutsu-Kougaku Kaishi 87 ( 3 ) 116 - 122 2009

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Analysis of B cell selection in the germinal center reaction during a T-dependent antibody response at a single cell level Reviewed

Takahiro Okazawa, Masaki Magari, Takafumi Kimoto, Emi Kouyama, Hitoshi Ohmori, Naoki Kanayama

IMMUNOLOGY LETTERS 117 ( 1 ) 96 - 105 2008.4

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Analysis of antigen-stimulated B cell migration into germinal centers during the early stage of a T-dependent immune response Reviewed

Emi Kouyama, Yumiko Nishikawa, Takahiro Okazawa, Masaki Magari, Hitoshi Ohmori, Naoki Kanayama

IMMUNOLOGY LETTERS 109 ( 1 ) 28 - 35 2007.3

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DOI： 10.1016/j.imlet.2006.12.011

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Novel in vitro screening system for monoclonal antibodies using hypermutating chicken B cell library Reviewed

Kagefumi Todo, Kenji Miyake, Masaki Magari, Naoki Kanayama, Hitoshi Ohmori

JOURNAL OF BIOSCIENCE AND BIOENGINEERING 102 ( 5 ) 478 - 481 2006.11

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DOI： 10.1263/jbb.102.478

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Establishment of lymphotoxin beta receptor signaling-dependent cell lines with follicular dendritic cell phenotypes from mouse lymph nodes Reviewed

Yumiko Nishikawa, Masaki Hikida, Masaki Magari, Naoki Kanayama, Masaharu Mori, Hiroshi Kitamura, Tomohiro Kurosaki, Hitoshi Ohmori

JOURNAL OF IMMUNOLOGY 177 ( 8 ) 5204 - 5214 2006.10

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Suppressive effects of mometasone furoate on an antigen-specific IgE antibody response and production of IL-4 in mice Reviewed

Masaki Magari, Mika Ikeda, Miki Asakura, Naoki Kanayama, Masami Ogawa, Hitoshi Ohmori

IMMUNOPHARMACOLOGY AND IMMUNOTOXICOLOGY 28 ( 3 ) 491 - 500 2006.7

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DOI： 10.1080/08923970600928155

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Genetic manipulation of an exogenous non-immunoglobulin protein by gene conversion machinery in a chicken B cell line Reviewed

N Kanayama, K Todo, S Takahashi, M Magari, H Ohmori

NUCLEIC ACIDS RESEARCH 34 ( 2 ) 2006

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DOI： 10.1093/nar/gnj013

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Immunogenicity of an inflammation-associated product, tyrosine nitrated self-proteins Reviewed

H Ohmori, N Kanayama

AUTOIMMUNITY REVIEWS 4 ( 4 ) 224 - 229 2005.4

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DOI： 10.1016/j.autrev.2004.11.011

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Analysis of marginal zone B cell development in the mouse with limited B cell diversity: Role of the antigen receptor signals in the recruitment of B cells to the marginal zone Reviewed

N Kanayama, M Cascalho, H Ohmori

JOURNAL OF IMMUNOLOGY 174 ( 3 ) 1438 - 1445 2005.2

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Reversible switching of immunoglobulin hypermutation machinery in a chicken B cell line Reviewed

N Kanayama, K Todo, M Reth, H Ohmori

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS 327 ( 1 ) 70 - 75 2005.2

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DOI： 10.1016/j.bbrc.2004.11.143

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Immunogenicity of autologous IgG bearing the inflammation-associated marker 3-nitrotyrosine Reviewed

H Ohmori, M Oka, Y Nishikawa, H Shigemitsu, M Takeuchi, M Magari, N Kanayama

IMMUNOLOGY LETTERS 96 ( 1 ) 47 - 54 2005.1

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DOI： 10.1016/j.imlet.2004.07.004

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Generation of IgM and IgG1 monoclonal antibodies with identical variable regions: comparison of avidity

Naoki Kanayama, Kimi Yamakoshi, Masaaki Kiyomi, Masaki Magari, Hitoshi Ohmori

Memoirs of the Faculty of Engineering Okayama University 38 91 - 96 2004

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Up-regulation of the peroxisomal beta-oxidation system occurs in butyrate-grown Candida tropicalis following disruption of the gene encoding peroxisomal 3-ketoacyl-CoA thiolase Reviewed

M Ueda, N Kanayama, N Kamasawa, M Osumi, A Tanaka

BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR AND CELL BIOLOGY OF LIPIDS 1631 ( 2 ) 160 - 168 2003.3

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DOI： 10.1016/S1388-1981(03)00002-7

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Mechanisms leading to autoantibody production: Link between inflamation and antoimmunity

Hitoshi Ohmori, Naoki Kanayama

Current Drug Targets-Inflamation & Allergy 2 232 - 241 2003

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B cell selection and affinity maturation during an antibody response in the mouse with limited B cell diversity Reviewed

N Kanayama, T Kimoto, K Todo, Y Nishikawa, M Hikida, M Magari, M Cascalho, H Ohmori

JOURNAL OF IMMUNOLOGY 169 ( 12 ) 6865 - 6874 2002.12

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Role for complement receptors (CD21/CD35) in the regulation of recombination activating gene expression in murine peripheral B cells Reviewed

H Ohmori, M Magari, Y Nakayama, N Kanayama, M Hikida

IMMUNOLOGY LETTERS 83 ( 2 ) 95 - 99 2002.9

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DOI： 10.1016/S0165-2478(02)00083-4

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Contribution of light chain rearrangement in peripheral B cells to the generation of high-affinity antibodies Reviewed

M Magari, T Sawatari, Y Kawano, M Cascalho, M Wabl, N Kanayama, M Hikida, H Ohmori

EUROPEAN JOURNAL OF IMMUNOLOGY 32 ( 4 ) 957 - 966 2002.4

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Regulatory role for complement receptors (CD21/CD35) in the recombination activating gene expression in mouse peripheral B cells

Masaki Hikida, Masaki Magari, Yasunori Nakayama, Naoki Kanayama, Hitoshi Ohmori

Memoirs of the Faculty of Engineering Okayama Univiersity 36 ( 2 ) 51 - 60 2002.3

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Use of secondarily revised VH genes in IgE antibodies produced in mice infected with the nematode Nippostrongylus brasiliensis Reviewed

N Kanayama, C Hukue, M Magari, K Ohtani, M Hikida, M Yamada, S Matsuda, H Ohmori

IMMUNOLOGY LETTERS 77 ( 3 ) 181 - 186 2001.7

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DOI： 10.1016/S0165-2478(01)00216-4

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Restoration of immunocyte functions by thymosin alpha 1 in cyclophosphamide induced immunodeficient mice Reviewed

H Ohmori, M Kamo, K Yamakoshi, MHM Nitta, M Hikida, N Kanayama

IMMUNOPHARMACOLOGY AND IMMUNOTOXICOLOGY 23 ( 1 ) 75 - 82 2001

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DOI： 10.1081/IPH-100102569

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Prevention of collagen-induced arthritis in DBA/1 mice by oral administration of AZ-9, a bacterial polysaccharide from Klebsiella oxytoca Reviewed

R Sugihara, M Yoshimura, M Mori, N Kanayama, M Hikida, H Ohmori

IMMUNOPHARMACOLOGY 49 ( 3 ) 325 - 333 2000.9

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DOI： 10.1016/S0162-3109(00)00247-2

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An n-alkane-responsive promoter element found in the gene encoding the peroxisomal protein of Candida tropicalis does not contain a C-6 zinc cluster DNA-binding motif Reviewed

T Kanai, A Hara, N Kanayama, M Ueda, A Tanaka

JOURNAL OF BACTERIOLOGY 182 ( 9 ) 2492 - 2497 2000.5

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DOI： 10.1128/JB.182.9.2492-2497.2000

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Selective augmenting effects of nitric oxide on antigen-specific IgE response in mice Reviewed

H Ohmori, H Egusa, N Ueura, Y Matsumoto, N Kanayama, M Hikida

IMMUNOPHARMACOLOGY 46 ( 1 ) 55 - 63 2000.1

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DOI： 10.1016/S0162-3109(99)00158-7

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Genetic Evaluation of Peroxisomal and Cytosolic Acetoacetyl-CoA Thiolase Isozymes in n-Alkane-Assimilating Diploid Yeast, Candida tropicalis Reviewed

Mitsuyoshi Ueda, Naoki Kanayama, Atsuo Tanaka

Cell Biochemistry and Biophysics 32 285 - 290 2000

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DOI： 10.1385/CBB:32:1-3:285

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Construction of an autonomously replicating plasmid in n-alkane-assimilating yeast, Candida tropicalis Reviewed

A Hara, M Ueda, T Matsui, K Furuhashi, N Kanayama, A Tanaka

JOURNAL OF BIOSCIENCE AND BIOENGINEERING 87 ( 6 ) 717 - 720 1999.6

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DOI： 10.1016/S1389-1723(99)80143-1

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Genetic evaluation of physiological functions of thiolase isozymes in the n-alkane-assimilating yeast Candida tropicalis Reviewed

N Kanayama, M Ueda, H Atomi, A Tanaka

JOURNAL OF BACTERIOLOGY 180 ( 3 ) 690 - 698 1998.2

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Expression of acetoacetyl-CoA thiolase isozyme genes of n-alkane-assimilating yeast, Candida tropicalis: Isozymes in two intracellular compartments are derived from the same genes Reviewed

N Kanayama, Y Himeda, H Atomi, M Ueda, A Tanaka

JOURNAL OF BIOCHEMISTRY 122 ( 3 ) 616 - 621 1997.9

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Derepression of gene expression mediated by the 5' upstream region of the isocitrate lyase gene of Candida tropicalis is controlled by two distinct regulatory pathways in Saccharomyces cerevisiae Reviewed

K Umemura, H Atomi, T Kanai, S Takeshita, N Kanayama, M Ueda, A Tanaka

EUROPEAN JOURNAL OF BIOCHEMISTRY 243 ( 3 ) 748 - 752 1997.2

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DOI： 10.1111/j.1432-1033.1997.00748.x

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3-KETOACYL COA THIOLASES OF A YEAST, CANDIDA-TROPICALIS - PROPERTIES AND FUNCTIONS Reviewed

A TANAKA, T KURIHARA, N KANAYAMA, H ATOMI, M UEDA

ENZYME ENGINEERING XII 750 39 - 43 1995

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DOI： 10.1111/j.1749-6632.1995.tb19922.x

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COMPARISON OF MOLECULAR-STRUCTURES AND REGULATION OF BIOSYNTHESIS OF UNIQUE THIOLASE ISOZYMES LOCALIZED ONLY IN PEROXISOMES OF N-ALKANE-UTILIZABLE YEAST, CANDIDA-TROPICALIS Reviewed

N KANAYAMA, M UEDA, H ATOMI, T KURIHARA, J KONDO, Y TERANISHI, A TANAKA

JOURNAL OF FERMENTATION AND BIOENGINEERING 78 ( 4 ) 273 - 278 1994

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DOI： 10.1016/0922-338X(94)90356-5

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MOLECULAR EVOLUTION OF YEAST THIOLASE ISOZYMES Reviewed

N KANAYAMA, M UEDA, H ATOMI, T KURIHARA, A TANAKA

JOURNAL OF FERMENTATION AND BIOENGINEERING 78 ( 4 ) 279 - 282 1994

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DOI： 10.1016/0922-338X(94)90357-3

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Molecular cloning of the peroxisomal bifunctional enzyme gene from n-alkane-utilizable yeast, Candida tropicalis pK233(共著)

Wei DZ, Kanayama N, Ueda M, Tanaka A

The Annual Reports of ICBiotech(International Center of Cooperative Research in Biotechnology, Faculty of Engineering, Osaka University, Japan) 16 215 - 222 1993

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PEROXISOMAL ACETOACETYL-COA THIOLASE OF AN N-ALKANE-UTILIZING YEAST, CANDIDA-TROPICALIS Reviewed

T KURIHARA, M UEDA, N KANAYAMA, J KONDO, Y TERANISHI, A TANAKA

EUROPEAN JOURNAL OF BIOCHEMISTRY 210 ( 3 ) 999 - 1005 1992.12

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DOI： 10.1111/j.1432-1033.1992.tb17505.x

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バイオ実験を安全に行うために

(株)化学同人 2018 （ ISBN:9784759819212 ）

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ラボ必携フローサイトメトリーQ&A〜正しいデータを出すための100箇条 (実験医学別冊)

戸村道夫

羊土社 2017.11 （ ISBN:4758122350 ）

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ASIN

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生物工学よもやま話ー実験の基本原理から応用までー

有限会社学進出版 2013 （ ISBN:9784907773052 ）

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ひらく、ひらく「バイオの世界」

化学同人 2012 （ ISBN:9784759815382 ）

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次世代抗体医薬開発に向けた抗体工学の最前線

シーエムシー出版 2012 （ ISBN:9784781306735 ）

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改訂細胞工学

講談社 2010 （ ISBN:9784061398306 ）

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未来をつくるバイオ酒造りから再生医療まで60話社団法人日本生物工学会編 Part 5 生体素子とバイオテクノロジー

学進出版 2008

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生物工学実験書

培風館（東京） 2002

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CaMKKの基質認識機構の解明と特異的阻害分子開発への応用

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日本生化学会大会(Web) 95th 2022

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CaMKK阻害剤(TIM-063)を用いた阻害剤プロテオミクス解析

大塚里美, 波多野直哉, 奥村太晟, 澤直樹, 田邊史子, 傳田美和子, 金山直樹, 曲正樹, 森下了, 石川彰彦, 徳光浩

日本生化学会大会(Web) 94th 2021

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インターラクトーム解析法を用いたヒトS100A6標的分子の探索

坂根恭平, 西口みゆ, 古谷雄穂, 傳田美和子, 山口文徳, 曲正樹, 金山直樹, 森下了, 徳光浩

日本生化学会大会(Web) 88th 1P0204 (WEB ONLY) - [1P0204] 2015.12

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2P-070 High-affinity antibody generation by regulating BCR signal dependent apoptosis in the chicken B cell line

Kanayama Naoki, Koga Mai, Ikeda Mika, Kojima Hiroyuki, Magari Masaki, Tokumitsu Hiroshi, Ohmori Hitoshi

67 192 - 192 2015

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2P-071 Enhanced production of humanized antibody in the chicken B cell line DT40

Nakatani Koji, Danjo Satoshi, Magari Masaki, Tokumitsu Hiroshi, Kanayama Naoki

67 192 - 192 2015

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Ca²⁺/Calmodulin結合型転写因子の網羅的同定

太尾田泰成, 大西和貴, 古谷雄穂, 傳田美和子, 金山直樹, 曲正樹, 森下了, 徳光浩

日本生化学会大会(Web) 88th 3P0185 (WEB ONLY) - [3P0185] 2015

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ヒトCalmodulin標的分子の網羅的同定

古谷雄穂, 西口みゆ, 傳田美和子, 曲正樹, 金山直樹, 森下了, 徳光浩

日本生化学会大会(Web) 87th 4T14A-01(3P-324) (WEB ONLY) - 01] 2014.10

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Role for serine/arginine-rich protein splicing factor (SRSF) in somatic hypermutation of immunoglobulin gene

61 ( 5 ) 489 - 495 2014

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AIDによる免疫グロブリンの体細胞高頻度突然変異誘導と関連分子

臨床免疫・アレルギー科 61 ( 5 ) 467 - 471 2014

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Role for follicular dendritic cells in the negative selection of germinal center B cells

58 ( 3 ) 259 - 265 2012

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in vitro System for Generating and Improving Monoclonal Antibodies by Manipulating Functions of The Hypermutating Chicken B Cell Line

31 ( 10 ) 1159 - 1165 2012

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フローサイトメトリー〜「前にならえ」並べて順に数えます〜

金山直樹

日本生物工学会誌 90 ( 11 ) 785 - 789 2012

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DT40細胞株を用いたin vitro抗体作製システムにおける,抗原レセプターの刺激に依存した生存による抗原特異的抗体産生細胞の選択法の開発

渡邊康二, 藤堂景史, 福岡純司, 曲正樹, 大森齊, 金山直樹

日本分子生物学会年会プログラム・要旨集(Web) 35th 2012

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4Ep15 Affinity maturation of monoclonal antibodies in the hypermutating chicken B cell line DT40-SW

Sai En, Kojima Satoshi, Fujii Shinobu, Kitamura Kouichi, Kamoshita Kayoko, Ikeda Mika, Magari Masaki, Ohmori Hitoshi, Kanayama Naoki

64 212 - 212 2012

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4Ep14 Development of a novel protein display system using a hypermutating B cell line DT40

Hikasa Takuya, Matsuda Shuichi, Uetsuki Hidetomo, Magari Masaki, Ohmori Hitoshi, Kanayama Naoki

64 212 - 212 2012

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4Ep16 Generation of antigen-specific antibodies using a chicken B cell line DT40 that expresses a human antibody

Kawakami Kanae, Inoue Kazue, Okayama Nobuhisa, Kanehiro Yuichi, Ikeda Mika, Magari Masaki, Omori Hitoshi, Kanayama Naoki

64 212 - 212 2012

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B細胞免疫記憶 AIDに依存したIgV変異には、SRタンパク質SRSF1のスプライスアイソフォームが必要である(AID-dependent IgV hypermutation requires a splice isoform of the SR protein SRSF1)

金山直樹, 金広優一, 藤堂景史, 根岸美咲, 福岡純司, 曲正樹, Li Xialu, Manley James L, 大森斉

日本免疫学会総会・学術集会記録 40 172 - 172 2011.11

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AIDに依存した体細胞突然変異には、SRタンパク質SRSF1のスプライスアイソフォームが必要である

金山直樹, 金広優一, 藤堂景史, 根岸美咲, 福岡純司, 曲正樹, Li Xialu, Manley James L, 大森斉

日本生化学会大会プログラム・講演要旨集 84回 3T15a - 15 2011.9

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Germinal center B cell differentiation and follicular dendritic cells

Clinical immunology & allergology 56 ( 2 ) 116 - 122 2011

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3La04 Establishment of efficient methods for screening high-affinity antibodies from antibody library generated by using chicken B cell line DT40-SW

Ikeda Mika, Kojima Hiroyuki, Okazawa Takahiro, Magari Masaki, Ohmori Hitoshi, Kanayama Naoki

63 234 - 234 2011

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1S1p05 In vitro generation and affinity maturation of monoclonal antibodies using the hypermutating B cell line DT40

Kanayama Naoki, Magari Masaki, Ohmori Hitoshi

63 9 - 9 2011

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変異能力を有するニワトリB細胞株DT40-SWを用いたマウスモノクローナル抗体の親和性成熟

鴨下佳代子, 小島聡史, 藤井忍, 北村幸一, 井上和恵, 岡山展久, 松田修一, 小嶋宏侑, 池田美香, 金広優一, 藤堂景史, 曲正樹, 大森齊, 金山直樹

日本生化学会大会・日本分子生物学会年会合同大会講演要旨集 83回・33回 ( Vol.1 ) 2T6 - 10 2010.12

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抗体遺伝子への体細胞突然変異におけるsplicing factor ASF/SF2の寄与

金広優一, 藤堂景史, 根岸美咲, 福岡純司, 曲正樹, 大森齊, 金山直樹

日本生化学会大会・日本分子生物学会年会合同大会講演要旨集 83回・33回 2P - 0478 2010.12

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Efficient in vitro antibody generation system using an engineered chicken B cell line, DT40-SW

Hitoshi Ohmori, Masaki Magari, Naoki Kanayama, Shuichi Matsuda, Yuichi Kanehiro

JOURNAL OF BIOTECHNOLOGY 150 S440 - S441 2010.11

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DOI： 10.1016/j.jbiotec.2010.09.628

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変異能力を有するニワトリB細胞株DT40-SWを用いたマウスモノクローナル抗体の親和性成熟

金山直樹, 小島聡史, 藤井忍, 北村幸一, 井上知恵, 岡山展久, 松田修一, 鴨下佳代子, 藤堂景史, 池田美香, 曲正樹, 大森齊

日本生物工学会大会講演要旨集平成22年度 ( Vol.1 ) 81 - 81 2010.9

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変異能力を有するニワトリB細胞株を用いた抗体の親和性成熟:外来の抗体可変部遺伝子のDT40-SWにおける発現・改良系の構築

小島聡史, 藤井忍, 北村幸一, 井上知恵, 岡山展久, 松田修一, 藤堂景史, 曲正樹, 金山直樹, 大森斉

日本分子生物学会年会講演要旨集 32nd ( Vol.1 ) 2009

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変異能力を有するニワトリB細胞株を用いた抗体の親和性成熟:変異様式の変換による親和性成熟の効率化

梶田真道, 曲正樹, 池田美香, 藤堂景史, 金山直樹, 大森斉

日本分子生物学会年会講演要旨集 32nd ( Vol.1 ) 2009

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2Ep17 In vitro antibody screening system using a chicken B cell line ,DT40-SW : application of converting mutation pattern for high affinity antibodies

KAJITA Masamichi, MAGARI Masaki, TODO Kagefumi, KANAYAMA Naoki, OHMORI Hitoshi

21 65 - 65 2009

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2Ep16 A novel antibody screening system using a chicken B cell line, DT40-SW : switching system of gene conversion and point mutation

MAGARI Masaki, KAJITA Masamichi, KANAYAMA Naoki, OHMORI Hitoshi

21 65 - 65 2009

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2Ep15 Analysis of regulatory mechanism for AID-dependent Ig gene mutation in a chicken B cell line

NEGISHI Misaki, UNE Yukiko, KANEHIRO Yuichi, MAGARI Masaki, KANAYAMA Naoki, OHMORI Hitoshi

21 64 - 64 2009

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変異導入能力を有する培養B細胞株を用いたin vitro抗体作製システムの高機能化

金山直樹, 曲正樹, 梶田真道, 金広優一, 藤堂景史, 大森斉

日本生化学会大会・日本分子生物学会年会合同大会講演要旨集 81回・31回 1T9 - 7 2008.11

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ニワトリB細胞株を用いたin vitro抗体作製システムの高機能化変異様式の転換の高性能抗体作製への応用

梶田真道, 藤堂景史, 曲正樹, 金山直樹, 大森斉

日本生物工学会大会講演要旨集平成20年度 109 - 109 2008.7

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ニワトリB細胞株DT40-SWを用いたin vitro抗体作製システムの高機能化抗体遺伝子への変異導入効率の増強

金広優一, 曲正樹, 藤堂景史, 金山直樹, 大森斉

日本生物工学会大会講演要旨集平成20年度 109 - 109 2008.7

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抗体医薬が切り拓く先端医療培養B細胞株を用いるin vitro抗体作製システムによる有用抗体の創製

金山直樹, 藤堂景史, 曲正樹, 大森齊

日本薬学会年会要旨集 128年会 ( 1 ) 134 - 134 2008.3

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効率的in vitro抗体作製システムの開発

大森斉, 金山直樹

BIO Clinica 23 ( 8 ) 82 - 87 2008

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3Ca13 Selective activation of antigen-specific B cells in vitro by FDC-like line; FL-Y.

MAGARI Masaki, NISHIKAWA Yumiko, SANO Hiroki, FUJII Yasumasa, KANAYAMA Naoki, OHMORI Hitoshi

20 109 - 109 2008

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ニワトリB細胞株DT40-SWを用いるin vitro抗体作製システムの開発変異導入の促進による迅速な抗体ライブラリーの構築

金広優一, 曲正樹, 藤堂景史, 金山直樹, 大森斉

日本生物工学会大会講演要旨集平成19年度 148 - 148 2007.8

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ニワトリB細胞株DT40-SWを用いるin vitro抗体作製システムの開発 Pax5発現抑制による抗体産生の増強

曲正樹, 綾高宏, 藤堂景史, 金山直樹, 大森斉

日本生物工学会大会講演要旨集平成19年度 149 - 149 2007.8

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ニワトリB細胞株DT40-SWを用いるin vitro抗体作製システムの開発抗原特異的クローンのセルソーターによる効率的単離

岡澤貴裕, 藤堂景史, 梶田真道, 曲正樹, 金山直樹, 大森斉

日本生物工学会大会講演要旨集平成19年度 149 - 149 2007.8

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変異機能のON/OFF制御可能なB細胞株を用いた抗体および変異タンパク質の作製システム

大森斉, 藤堂景史, 金山直樹

実験医学 124 (9), pp. 1331-1335 ( 9 ) 1331 - 1335 2006

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1K16-2 Construction of an antibody library from a chicken B cell line, DT40 by controlling point mutation and gene conversion

KAJITA Masamichi, TODO Kagefumi, MAGARI Masaki, KANAYAMA Naoki, OHMORI Hitoshi

18 197 - 197 2006

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1K16-1 Generation of monoclonal antibodies by a novel antibody screening system using a hypermutating B cell line

TODO Kagefumi, MIYAKE Kenji, FUJITA Risako, OKAZAWA Takahiro, IKEDA Mika, MAGARI Masaki, KANAYAMA Naoki, OHMORI Hitoshi

18 197 - 197 2006

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抗体遺伝子変換機構を利用した非抗体タンパクのDNAシャッフリングによる機能改変

藤堂景史, 高橋佐都子, 片岡大輔, 曲正樹, 金山直樹, 大森斉

日本免疫学会総会・学術集会記録 35 80 - 80 2005.11

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培養B細胞株の変異機能を利用する新規なin vitro抗体作製システム

三宅健司, 藤堂景史, 曲正樹, 金山直樹, 大森斉

日本生物工学会大会講演要旨集平成17年度 118 - 118 2005.9

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抗体の多様化メカニズムの不思議

金山直樹

日本生物工学会誌 83 (1), 33 ( 1 ) 33 - 33 2005

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B細胞の遺伝子変換機構を利用する非抗体タンパクの機能改変

藤堂景史, 高橋佐都子, 片岡大輔, 曲正樹, 金山直樹, 大森斉

日本生物工学会大会講演要旨集 2005 2005

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高頻度変異機能のON/OFF制御可能なB細胞株を用いるin vitro抗体作製システム

金山直樹, 藤堂景史, 三宅健司, 曲正樹, 大森斉

日本分子生物学会年会講演要旨集 28th 2005

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B細胞株の遺伝子改変能を利用したタンパク分子改変システムの構築

藤堂景史, 高橋佐都子, 曲正樹, 金山直樹, 大森斉

日本免疫学会総会・学術集会記録 34 263 - 263 2004.11

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B細胞レパトアの限定されたマウスにおけるB細胞選択と親和性成熟の解析

金山直樹, 木本崇文, 藤堂景史, 曲正樹, 大森齊

生化学 76 ( 3 ) 306 - 306 2004.3

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ニワトリB細胞株を用いたタンパク分子改変系の構築:変異導入機能のON/OFF制御

藤堂景史, 曲正樹, 金山直樹, 大森斉

日本生物工学会大会講演要旨集 2004 2004

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ニワトリB細胞株を用いたタンパク分子改変系の構築:外来遺伝子の遺伝子変換

高橋佐都子, 藤堂景史, 曲正樹, 金山直樹, 大森斉

日本生物工学会大会講演要旨集 2004 2004

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2H15-3 Analysis of antibody affinity maturation by single cell PCR

KANAYAMA Naoki, OKAZAWA Takahiro, KOYAMA Emi, MAGARI Masaki, OHMORI Hitoshi

16 215 - 215 2004

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辺縁帯B細胞の特性

金山直樹, 大森斉

臨床免疫 40, 450-453 2003

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B細胞レセプターを介するシグナルとB細胞応答

曲正樹, 金山直樹, 大森斉

臨床免疫 40, 454-457 2003

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平成13年度両備てい園記念財団研究助成金による研究報告 Qmasimonoclonal マウスにおける抗体親和性成熟

金山直樹

生物学に関する試験研究論叢 18, 57-67 2003

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Conversion and expression of foreign genes in the chicken B cell line

Todo Kagefumi, Takahashi Satoko, Magari Masaki, Kanayama Naoki, Ohmori Hitoshi

15 87 - 87 2003

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Analysis of affinity maturation by single-cell PCR

Okazawa Takahiro, Magari Masaki, Kimoto Takafumi, Kouyama Emi, Kanayama Naoki, Ohmori Hitoshi

15 187 - 187 2003

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B細胞多様性の限定されたマウスにおけるクローン選択と親和性成熟の解析

木本崇文, 藤堂景史, 疋田正喜, 曲正樹, 金山直樹, 大森斉

日本免疫学会総会・学術集会記録 32 271 - 271 2002.10

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B細胞多様性の限定されたマウスにおける抗体の親和性成熟機構の解析

藤堂景史, 木本崇文, 曲正樹, 金山直樹, 大森斉

日本生物工学会大会講演要旨集平成14年度 206 - 206 2002.9

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B細胞レパトアの限定されたマウスを用いるB細胞選択と親和性成熟の解析

木本崇文, 松浦正明, 藤堂景史, 曲正樹, 疋田正喜, 金山直樹, 大森齊

生化学 74 ( 8 ) 949 - 949 2002.8

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1130 Detection of RAG expressed cells by a new fluorescence-labeling mothod

Miki Takao, Nishikawa Emiko, Magari Masaki, Hikida Masaki, Kanayama Naoki, Ohmori Hitoshi

14 206 - 206 2002

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末梢でのV(D)J遺伝子再構成の親和性成熟への寄与

疋田正喜, 金山直樹, 大森斉

臨床免疫 36, 54-59 2001

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Analysis of affinity maturation in quasi monoclonal mouse

Kimoto Takafumi, Matsuura Masaaki, Magari Masaki, Kanayama Naoki, Hikida Masaki, Ohmori Hitoshi

13 341 - 341 2001

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末梢リンパ組織における抗体遺伝子の再構成。抗体遺伝子の構造はどこまで柔軟か？

大森斉, 疋田正喜, 金山直樹

細胞工学 19, 482-487 ( 3 ) 482 - 487 2000

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胚中心Ｂ細胞におけるレセプターeditingとその意義。

大森斉, 疋田正喜, 金山直樹

Molecular Midicne 「免疫1999-2000」 36, 20-28 ( 1999 ) 20 - 28 1999

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Analysis of affinity maturation of antibody using Ig-transgenic mice.

Magari Masaki, Sawatari Takashi, Kanayama Naoki, Hikida Masaki, Ohmori Hitoshi

11 139 - 139 1999

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Src family kinase阻害剤感受性因子による抗体遺伝子高頻度突然変異の制御

道廣志龍, 大森晴斗, 秋山美咲, 尾畑早紀, 千原一泰, 定清直, 金山直樹

第47回日本分子生物学会年会 2024.11.29

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抗原刺激強度依存的な遺伝子発現におけるBCRシグナル経路の役割

小野和奏, 安福希, 伊藤雄太, 山西涼矢, 金山直樹

第47回日本分子生物学会年会 2024.11.29

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抗体遺伝子高頻度突然変異に関わるSRSF1のRSドメインの機能

市川千紗, 在間郁冶, 石橋朋之, 金山直樹

第47回日本分子生物学会年会 2024.11.29

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抗原刺激強度に応じて異なる BCR シグナル経路を用いて発現する遺伝子の探索

小野和奏, 安福希, 山西涼矢, 伊藤雄大, 黒崎夏未, 金山直樹

第76回日本生物工学会大会 2024.9.10

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Event date： 2024.9.8 - 2024.9.10

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1Kp16 抗原レセプターシグナル依存的に発現するオーファンレ学セプター NR4A1 の B 細胞における発現制御機構の解明

長門直希, 伊藤雄大, 野田凌太郎, 金山直樹

第75回日本生物工学会大会 2023.9.3

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Event date： 2023.9.3 - 2023.9.5

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1Kp15 抗原刺激強度依存的な遺伝子発現における BCR シグナル経路の役割

小野和奏, 安福希, 伊藤雄大, 金山直樹

第75回日本生物工学会大会 2023.9.3

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[3P-470]B細胞抗原レセプターシグナル誘導性分子の発現に必要なシグナル伝達経路

安福希, 伊藤雄大, 小野和奏, 大塚里美, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第45回日本分子生物学会年会 2022.12.2 日本分子生物学会

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Event date： 2022.11.30 - 2022.12.2

Language：Japanese Presentation type：Poster presentation

Venue：千葉
[3P-470]B細胞抗原レセプターシグナル誘導性分子の発現に必要なシグナル伝達経路

安福希, 伊藤雄大, 小野和奏, 大塚里美, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第45回日本分子生物学会年会 2022.12.2

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[2P-500]抗原レセプターシグナル依存的に発現するオーファンレセプターNR4A1のB細胞における発現制御機構の解明

伊藤雄大, 野田凌太郎, 長門直希, 安福希, 大塚里美, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第45回日本分子生物学会年会 2022.12.1 日本分子生物学会

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Venue：千葉
[2P-815]Src family kinase阻害剤感受性因子によるAID発現制御機構の解明

大森晴斗, 秋山美咲, 道廣志龍, 大塚里美, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第45回日本分子生物学会年会 2022.12.1

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[2P-500]抗原レセプターシグナル依存的に発現するオーファンレセプターNR4A1のB細胞における発現制御機構の解明

伊藤雄大, 野田凌太郎, 長門直希, 安福希, 大塚里美, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第45回日本分子生物学会年会 2022.12.1

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[2P-814]抗体遺伝子高頻度突然変異におけるスプライシング因子SRSF1の機能部位

在間郁冶, 石橋朋之, 成木弘明, 川口佑加, 河本奈緒子, 横山和輝, 市川千紗, 大塚里美, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第45回日本分子生物学会年会 2022.12.1

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[2P-628]単球系細胞が発現するUrokinase-type plasminogen activatorによるB細胞活性化機構の解明

羽里知美, 高田美帆, 西岡美玖, 波多野直哉, 金山直樹, 徳光浩, 曲正樹

第45回日本分子生物学会年会 2022.12.1

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[2P-629]濾胞樹状細胞が活性化に伴い発現するB細胞調節因子の同定

高橋佳歩, 西岡美玖, 金山直樹, 徳光浩, 曲正樹

第45回日本分子生物学会年会 2022.12.1

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[2P-815]Src family kinase阻害剤感受性因子によるAID発現制御機構の解明

大森晴斗, 秋山美咲, 道廣志龍, 大塚里美, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第45回日本分子生物学会年会 2022.12.1 日本分子生物学会

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Venue：千葉
[2P-814]抗体遺伝子高頻度突然変異におけるスプライシング因子SRSF1の機能部位

在間郁冶, 石橋朋之, 成木弘明, 川口佑加, 河本奈緒子, 横山和輝, 市川千紗, 大塚里美, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第45回日本分子生物学会年会 2022.12.1 日本分子生物学会

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Event date： 2022.11.30 - 2022.12.2

Language：Japanese Presentation type：Poster presentation

Venue：千葉
[2P-629]濾胞樹状細胞が活性化に伴い発現するB細胞調節因子の同定

高橋佳歩, 西岡美玖, 金山直樹, 徳光浩, 曲正樹

第45回日本分子生物学会年会 2022.12.1 日本分子生物学会

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Event date： 2022.11.30 - 2022.12.2

Language：Japanese Presentation type：Poster presentation

Venue：千葉
[2P-628]単球系細胞が発現するUrokinase-type plasminogen activatorによるB細胞活性化機構の解明

羽里知美, 高田美帆, 西岡美玖, 波多野直哉, 金山直樹, 徳光浩, 曲正樹

第45回日本分子生物学会年会 2022.12.1 日本分子生物学会

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Event date： 2022.11.30 - 2022.12.2

Language：Japanese Presentation type：Poster presentation

Venue：千葉
[2P-343] B細胞活性化能力を有する単球系細胞の分化におけるIL-34の糖鎖修飾による制御

曲正樹, 岡本千怜, 小川紗也香, 金山直樹, 波多野直哉, 徳光浩

第95回日本生化学会大会 2022.11.10 日本生化学会

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Event date： 2022.11.9 - 2022.11.11

Language：Japanese Presentation type：Poster presentation

Venue：名古屋
[2P-343] B細胞活性化能力を有する単球系細胞の分化におけるIL-34の糖鎖修飾による制御

曲正樹, 岡本千怜, 小川紗也香, 金山直樹, 波多野直哉, 徳光浩

第95回日本生化学会大会 2022.11.10

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Event date： 2022.11.9 - 2022.11.11

Language：Japanese Presentation type：Poster presentation

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[3P-380（1T18e-06）] キナーゼ阻害剤プロテオミクス法を用いた薬効再評価法の開発

大塚里美, 吉田朱里, 波多野直哉, 奥村太晟, 澤直樹, 金山直樹, 曲正樹, 石川彰彦, 徳光浩

第95回日本生化学会大会 2022.11.10 日本生化学会

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Event date： 2022.11.9 - 2022.11.11

Language：Japanese Presentation type：Oral presentation (general)

Venue：名古屋
[3P-203（1T12a-07）] CaMKKの基質認識機構の解明と特異的阻害分子開発への応用

川俣一晟, 美馬光志, 山内陽生, 北前勝哉, 山内香奈, 大塚里美, 曲正樹, 金山直樹, 徳光浩

第95回日本生化学会大会 2022.11.10 日本生化学会

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Event date： 2022.11.9 - 2022.11.11

Language：Japanese Presentation type：Oral presentation (general)

Venue：名古屋
[3P-203（1T12a-07）] CaMKKの基質認識機構の解明と特異的阻害分子開発への応用

川俣一晟, 美馬光志, 山内陽生, 北前勝哉, 山内香奈, 大塚里美, 曲正樹, 金山直樹, 徳光浩

第95回日本生化学会大会 2022.11.10

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Event date： 2022.11.9 - 2022.11.10

Language：Japanese Presentation type：Oral presentation (general)

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[3P-380（1T18e-06）] キナーゼ阻害剤プロテオミクス法を用いた薬効再評価法の開発

大塚里美, 吉田朱里, 波多野直哉, 奥村太晟, 澤直樹, 金山直樹, 曲正樹, 石川彰彦, 徳光浩

第95回日本生化学会大会 2022.11.10

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Event date： 2022.11.9 - 2022.11.10

Language：Japanese Presentation type：Oral presentation (general)

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B細胞活性化能力を有する単球系細胞の分化におけるIL-34作用機構の解明

岡本千怜, 小川紗也香, 松岡由希子, 金山直樹, 波多野直哉, 徳光浩, 曲正樹

第44回日本分子生物学会年会 2021.12.2

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Event date： 2021.12.1 - 2021.12.3

Language：Japanese Presentation type：Poster presentation

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濾胞樹状細胞の発現するSLAM-family memberによる抗体応答の制御

西岡美玖, 西岡美穂, 小川紗也香, 金山直樹, 波多野直哉, 徳光浩, 曲正樹

第44回日本分子生物学会年会 2021.12.2

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Event date： 2021.12.1 - 2021.12.3

Language：Japanese Presentation type：Poster presentation

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シグナル伝達因子LynによるAID発現制御機構の解明

秋山美咲, 大森晴斗, 梶浦雄也, 石橋朋之, 久原亜弓, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第44回日本分子生物学会年会 2021.12.2

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Event date： 2021.12.1 - 2021.12.3

Language：Japanese Presentation type：Poster presentation

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濾胞樹状細胞依存的に発生する単球系細胞が発現するB細胞活性化因子の同定

羽里知美, 高田美帆, 波多野直哉, 金山直樹, 徳光浩, 曲正樹

第44回日本分子生物学会年会 2021.12.2

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Event date： 2021.12.1 - 2021.12.3

Language：Japanese Presentation type：Poster presentation

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B細胞抗原レセプターシグナル強度に依存して誘導される分子の探索

安福希, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第44回日本分子生物学会年会 2021.12.1

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Event date： 2021.12.1 - 2021.12.3

Language：Japanese Presentation type：Poster presentation

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CaMKK阻害剤(TIM-063)を用いた阻害剤プロテオミクス解析

大塚里美, 波多野直哉, 奥村太晟, 澤直樹, 田邊史子, 傳田美和子, 金山直樹, 曲正樹, 森下了, 石川彰彦, 徳光浩

日本生化学会大会(Web) 94th 2021 日本生化学会

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Event date： 2021

Language：Japanese Presentation type：Poster presentation
CaMKK阻害剤(TIM-063)を用いた阻害剤プロテオミクス解析

大塚里美, 波多野直哉, 奥村太晟, 澤直樹, 田邊史子, 傳田美和子, 金山直樹, 曲正樹, 森下了, 石川彰彦, 徳光浩

日本生化学会大会(Web) 94th 2021

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Event date： 2021

Language：Japanese Presentation type：Poster presentation

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濾胞樹状細胞の発現する SLAM-family member による胚中心反応の制御

西岡美玖, 西岡美穂, 小川紗也香, 波多野直哉, 金山直樹, 徳光浩, 曲正樹

第 43 回日本分子生物学会年会

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Event date： 2020.12.2 - 2020.12.4

Language：Japanese Presentation type：Poster presentation

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191 濾胞樹状細胞依存的に分化する B 細胞活性化能力を有した単球系細胞の分化機構の解析

曲正樹, 小川紗也香, 岡本千怜, 西岡美玖, 金山直樹, 波多野直哉, 徳光浩

第43 回日本分子生物学会年会

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Event date： 2020.12.2 - 2020.12.4

Language：Japanese Presentation type：Poster presentation

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分子プローブとしてのCa2+/Calmodulin-dependent pro- tein kinase kinase 新規阻害剤と不活性類縁体の開発

大塚里美, 尾関唯, 藤原萌乃, 宮川知之, 金山直樹, 曲正樹, 石川彰彦, 徳光浩

第 61 回日本生化学会中国・四国大会 2020.5.23

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Event date： 2020.5.23 - 2020.5.24

Language：Japanese Presentation type：Oral presentation (general)

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新規S100A6標的分子(HMG20A)の同定と相互作用解析

山本真穂, 近藤里奈, 傳田美和子, 土居青太, 金山直樹, 曲正樹, 森下了, 徳光浩

日本生化学会大会プログラム・講演要旨集 2019.9 (公社)日本生化学会

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Event date： 2019.9

Language：Japanese

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scFv型抗体を発現するニワトリB細胞株DT40の樹立と利用

岡知里, 野田凌太郎, 曲正樹, 徳光浩, 金山直樹

日本生物工学会大会講演要旨集 2019.8 (公社)日本生物工学会

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Event date： 2019.8

Language：Japanese

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ニワトリB細胞株DT40におけるscFv型抗体の発現効率の改善

野田凌太郎, 岡知里, 曲正樹, 徳光浩, 金山直樹

日本生物工学会大会講演要旨集 2019.8 (公社)日本生物工学会

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Event date： 2019.8

Language：Japanese

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BCRシグナル伝達を介したAID発現制御の解析

石橋朋之, 梶浦雄也, 久原亜弓, 大柳翔, 秋山美咲, 曲正樹, 徳光浩, 金山直樹

日本分子生物学会年会プログラム・要旨集(Web) 2019

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Event date： 2019

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CaMKKβのリン酸化/脱リン酸化による動的制御機構の解明

高畠翔太, 福本侑世, 金山直樹, 曲正樹, 波多野直哉, 徳光浩

日本分子生物学会年会プログラム・要旨集(Web) 2019

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Event date： 2019

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筋肉特異的Calmodulin結合分子,Striated Muscle Activator of Rho Signaling(STARS)の分子間相互作用解析

赤木魁, 田中啓之, 金山直樹, 曲正樹, 波多野直哉, 徳光浩

日本分子生物学会年会プログラム・要旨集(Web) 2019

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Event date： 2019

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STO-609をリード化合物とした新規CaMKK阻害薬の創製

大塚里美, 尾関唯, 藤井つかさ, 金山直樹, 曲正樹, 石川彰彦, 徳光浩

日本生化学会大会(Web) 2019

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Event date： 2019

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濾胞樹状細胞の活性化に伴い高発現する分子の探索とその機能解析

西岡美玖, 西岡美穂, 小川紗也香, 波多野直哉, 金山直樹, 徳光浩, 曲正樹

日本分子生物学会年会プログラム・要旨集(Web) 2019

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Event date： 2019

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濾胞樹状細胞表面に発現するIL-34がB細胞活性化能力を有する単球系細胞の分化に関与する

曲正樹, 小川紗也香, 松岡由希子, 高田美帆, 金山直樹, 波多野直哉, 徳光浩

日本分子生物学会年会プログラム・要旨集(Web) 2019

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Event date： 2019

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CaMKKβシグナル伝達のAMPKおよびPKAによるリン酸化制御機構の解明

大塚里美, 高畠翔太, 金山直樹, 曲正樹, 徳光浩

日本生化学会大会プログラム・講演要旨集 2018.9 (公社)日本生化学会

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Event date： 2018.9

Language：Japanese

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スプライシング因子の過剰発現及び標的遺伝子配列の操作によるニワトリB細胞株における遺伝子変異の増強

金山直樹, 太田愛美, 西山由美子, 岡知里, 曲正樹, 徳光浩

日本生物工学会大会講演要旨集 2018.8 (公社)日本生物工学会

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Event date： 2018.8

Language：Japanese

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GRP78により発現制御される濾胞樹状細胞表面のIL-34が単球系細胞の分化に関与する

小川紗也香, 松岡由希子, 高田美帆, 松井一恵, 山根文寛, 安原詩織, 金山直樹, 波多野直哉, 徳光浩, 曲正樹

日本分子生物学会年会プログラム・要旨集(Web) 2018

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Event date： 2018

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AID発現とSHM誘導におけるBCRシグナルの役割

梶浦雄也, 金廣優一, 曲正樹, 徳光浩, 金山直樹

生命科学系学会合同年次大会 2017.12 生命科学系学会合同年次大会運営事務局

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Event date： 2017.12

Language：Japanese

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スプライシング因子の過剰発現及び標的遺伝子配列の操作によるニワトリB細胞株における遺伝子変異の増強

太田愛美, 西山由美子, 曲正樹, 徳光浩, 金山直樹

生命科学系学会合同年次大会 2017.12 生命科学系学会合同年次大会運営事務局

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Event date： 2017.12

Language：Japanese

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抗体遺伝子変異の転写関連過程におけるSRSF1-3の役割の解析

金山直樹, 川口祐加, 横山和輝, 石橋朋之, 曲正樹, 徳光浩

生命科学系学会合同年次大会 2017.12 生命科学系学会合同年次大会運営事務局

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Event date： 2017.12

Language：Japanese

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濾胞樹状細胞の発現するCSF-1の単球系細胞分化への関与の解析

安原詩織, 松岡由希子, 小川紗也香, 金山直樹, 徳光浩, 曲正樹

生命科学系学会合同年次大会 2017.12 生命科学系学会合同年次大会運営事務局

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Event date： 2017.12

Language：Japanese

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抗体遺伝子変異能力を操作できるニワトリB細胞を用いた動物細胞ディスプレイ

金山直樹, 太田愛美, 中谷元紀, 中谷耕治, 植月英智, 西山由美子, 仲尾祐輝, 曲正樹, 徳光浩

日本生物工学会大会講演要旨集 2017.8 (公社)日本生物工学会

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Event date： 2017.8

Language：Japanese

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インターラクトーム解析法を用いたヒトS100A6標的分子の探索

坂根恭平, 西口みゆ, 古谷雄穂, 傳田美和子, 山口文徳, 曲正樹, 金山直樹, 森下了, 徳光浩

日本生化学会大会(Web) 2015.12 (公社)日本生化学会

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Event date： 2015.12

Language：Japanese

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Ca²⁺/Calmodulin結合型転写因子の網羅的同定

太尾田泰成, 大西和貴, 古谷雄穂, 傳田美和子, 金山直樹, 曲正樹, 森下了, 徳光浩

日本生化学会大会(Web) 2015

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Event date： 2015

Language：Japanese

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3P-032 Engineering of antibodies using the hypermutating B cell line

Kanayama Naoki, Watanabe Koji, Koga Mai, Kawakami Kanae, Uetsuki Hidetomo, Tokumitsu Hiroshi, Magari Masaki, Ohmori Hitoshi

2014

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Event date： 2014

Language：Japanese

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Other Link： http://search.jamas.or.jp/link/ui/2016046032
3P-003 Protein evolution in a protein display system using the hypermutating B cell line DT40-SW

Watanabe Koji, Hikasa Takuya, Uetsuki Hidetomo, Tokumitsu Hiroshi, Magari Masaki, Ohmori Hitoshi, Kanayama Naoki

2013

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Event date： 2013

Language：Japanese

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Other Link： http://search.jamas.or.jp/link/ui/2014247582
3P-002 High-affinity antibody generation using the chicken B cell line DT40-SW by regulating B cell receptor-mediated apoptosis

Koga Mai, Ikeda Mika, Kojima Hiroyuki, Kawakami Kanae, Watanabe Koji, Tokumitsu Hiroshi, Magari Masaki, Ohmori Hitoshi, Kanayama Naoki

2013

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Event date： 2013

Language：Japanese

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Other Link： http://search.jamas.or.jp/link/ui/2014247581
4Ep16 Generation of antigen-specific antibodies using a chicken B cell line DT40 that expresses a human antibody

Kawakami Kanae, Inoue Kazue, Okayama Nobuhisa, Kanehiro Yuichi, Ikeda Mika, Magari Masaki, Omori Hitoshi, Kanayama Naoki

2012

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Event date： 2012

Language：Japanese

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4Ep14 Development of a novel protein display system using a hypermutating B cell line DT40

Hikasa Takuya, Matsuda Shuichi, Uetsuki Hidetomo, Magari Masaki, Ohmori Hitoshi, Kanayama Naoki

2012

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Event date： 2012

Language：Japanese

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Other Link： http://search.jamas.or.jp/link/ui/2013125690
4Ep15 Affinity maturation of monoclonal antibodies in the hypermutating chicken B cell line DT40-SW

Sai En, Kojima Satoshi, Fujii Shinobu, Kitamura Kouichi, Kamoshita Kayoko, Ikeda Mika, Magari Masaki, Ohmori Hitoshi, Kanayama Naoki

2012

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Event date： 2012

Language：Japanese

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Other Link： http://search.jamas.or.jp/link/ui/2013125691
DT40細胞株を用いたin vitro抗体作製システムにおける,抗原レセプターの刺激に依存した生存による抗原特異的抗体産生細胞の選択法の開発

渡邊康二, 藤堂景史, 福岡純司, 曲正樹, 大森齊, 金山直樹

日本分子生物学会年会プログラム・要旨集(Web) 2012

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B細胞免疫記憶 AIDに依存したIgV変異には、SRタンパク質SRSF1のスプライスアイソフォームが必要である(AID-dependent IgV hypermutation requires a splice isoform of the SR protein SRSF1)

金山直樹, 金広優一, 藤堂景史, 根岸美咲, 福岡純司, 曲正樹, Li Xialu, Manley James L, 大森斉

日本免疫学会総会・学術集会記録 2011.11 (NPO)日本免疫学会

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Event date： 2011.11

Language：English

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B細胞免疫反応と免疫記憶超変異ニワトリB細胞株を用いたin vitro抗原生産システム(In vitro antibody generation system using a hypermutating chicken B cell line)

Kanayama Naoki, Todo Kagefumi, Okazawa Takahiro, Ikeda Mika, Fujita Risako, Magari Masaki, Ohmori Hitoshi

日本免疫学会総会・学術集会記録 2006.11 (NPO)日本免疫学会

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Event date： 2006.11

Language：English

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Conversion and expression of foreign genes in the chicken B cell line

Todo Kagefumi, Takahashi Satoko, Magari Masaki, Kanayama Naoki, Ohmori Hitoshi

2003

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Event date： 2003

Language：Japanese

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B細胞多様性の限定されたマウスにおける抗体の親和性成熟機構の解析

藤堂景史, 木本崇文, 曲正樹, 金山直樹, 大森斉

日本生物工学会大会講演要旨集 2002.9 (公社)日本生物工学会

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Event date： 2002.9

Language：Japanese

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胚中心B細胞におけるRAGと並行するλ5,VpreBの再発現とその調節

金山直樹, 疋田正喜, 烏山一, 大森斉

日本免疫学会総会・学術集会記録 1999

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Event date： 1999

Language：Japanese

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Affinity Maturation of Antibodies Using Hypermutating B Cell Line Invited

Naoki Kanayama

International Symposium of Innovative R&D on Health Systems: Universiti Malaysia Pahang and Okayama University 2021.9.28

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Language：English Presentation type：Oral presentation (invited, special)

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転写および翻訳段階におけるAID発現調節機構の解析

大森晴斗, 秋山美咲, 梶浦雄也, 石橋朋之, 久原亜弓, 大柳昇, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第62回日本生化学会中国・四国支部例会 2021年9月10日 2021.9.11

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新規 CaMKK 阻害剤結合担体を用いた酵素・阻害剤相互作用解析

大塚里美, 波多野直哉, 奥村太晟, 澤直樹, 金山直樹, 曲正樹, 石川彰彦, 徳光浩

第62回日本生化学会中国・四国支部例会 2021.9.11

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抗原レセプターシグナル依存的に発現するオーファンレセプターNR4A1の B 細胞における発現制御機構の解明

伊藤雄大, 野田凌太郎, 長門直希, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第62回日本生化学会中国・四国支部例会 2021.9.11

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抗体遺伝子高頻度突然変異におけるSRSF1-3の機能部位の特定

在間郁冶, 石橋朋之, 成木弘明, 川口祐加, 曲正樹, 波多野直哉, 徳光浩, 金山直樹

第62回日本生化学会中国・四国支部例会 2021.9.11

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Ca2+/calmodulin-dependent protein kinase kinase (CaMKK)の多量体形成

福本侑世, 原田裕平, 波多野直哉, 曲正樹, 金山直樹, 徳光浩

第62回日本生化学会中国・四国支部例会 2021.9.10

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抗原レセプターシグナル依存的に発現するオーファンレセプターNR4A1 のB 細胞における発現制御機構の解明

野田凌太郎, 曲正樹, 徳光浩, 金山直樹

第 39 回岡山免疫懇話会 2021.3.3

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抗原レセプターシグナル依存的に発現するオーファンレセプターNR4A1のB細胞における発現制御機構の解明

野田凌太郎, 曲正樹, 徳光浩, 金山直樹

日本生物工学会西日本支部大会2020 2020.11.14

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Industrial property rights

ヒト型抗体を産生するＢ細胞の作製方法

金山直樹, 大森齊

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Applicant：国立大学法人岡山大学

Application no：特願2012-544298 Date applied：2011.11.17

Patent/Registration no：特許第5904468号 Date issued：2016.3.25

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ヒト型抗体を産生するB細胞の作製方法

金山直樹, 大森齊

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Applicant：国立大学法人岡山大学

Application no：JP2011076533 Date applied：2011.11.17

Announcement no：WO2012-067188 Date announced：2012.5.24

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所望のポリペプチドを産生する抗体産生細胞の製造方法

大森齊, 金山直樹, 藤井忍

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Applicant：株式会社免疫工学研究所

Application no：特願2012-523755 Date applied：2010.11.18

Announcement no：特表2013-511258 Date announced：2013.4.4

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B細胞の抗体遺伝子変異様式の転換方法

大森齊, 金山直樹, 曲正樹

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Applicant：国立大学法人岡山大学

Application no：特願2007-231741 Date applied：2007.9.6

Announcement no：特開2009-060850 Date announced：2009.3.26

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抗体産生細胞の特異的選択方法

大森齊, 金山直樹

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Application no：特願2005-247074 Date applied：2005.8.29

Announcement no：特開2007-060907 Date announced：2007.3.15

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抗体産生細胞の特異的選択方法

大森齊, 金山直樹

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Application no：特願2005-247074 Date applied：2005.8.29

Announcement no：特開2007-060907 Date announced：2007.3.15

Patent/Registration no：特許第4482693号 Date issued：2010.4.2

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細胞の遺伝子変異機能の制御による変異タンパク質の作製方法

大森齊, 金山直樹

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Applicant：国立大学法人岡山大学

Application no：特願2004-298072 Date applied：2004.10.12

Announcement no：特開2006-109711 Date announced：2006.4.27

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細胞の遺伝子変異機能の制御による変異タンパク質の作製方法

大森齊, 金山直樹

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Application no：特願2004-298072 Date applied：2004.10.12

Announcement no：特開2006-109711 Date announced：2006.4.27

Patent/Registration no：特許第4487068号 Date issued：2010.4.9

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Awards

内山勇三科学技術賞

2013 岡山工学振興会

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Country：Japan

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岡山工学振興会科学技術賞

2009 岡山工学振興会

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第44回生物工学奨励賞（斉藤賞）

2008 日本生物工学会

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岡山工学振興会科学技術賞

2004 岡山工学振興会

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Research Projects

B細胞抗原レセプターによる抗原親和性の認識機構の解明と高親和性抗体選択への応用

Grant number：24K08172 2024.04 - 2028.03

日本学術振興会科学研究費助成事業基盤研究(C)

金山直樹

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Grant amount：\4680000 （ Direct expense: \3600000 、 Indirect expense：\1080000 ）

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スプライシング因子によるDNA編集酵素の活性調節機構の解明

2023.05 - 2024.09

公益財団法人日本応用酵素協会 2023年度酵素研究助成

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Authorship：Principal investigator Grant type：Competitive

Grant amount：\50 （ Direct expense: \50 ）

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スプライシング因子によるDNA 編集酵素の活性調節機構の解明

2022.05 - 2023.09

公益財団法人日本応用酵素協会 2022年度酵素研究助成

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Authorship：Principal investigator Grant type：Competitive

Grant amount：\100 （ Direct expense: \100 ）

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Antigen affinity-dependent regulation of B cell antigen receptor signaling

Grant number：20K05231 2020.04 - 2024.03

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)

金山直樹

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Grant amount：\4420000 （ Direct expense: \3400000 、 Indirect expense：\1020000 ）

本研究では、抗原レセプターと抗原との親和性に依存したシグナル調節機構を明らかにして、生体内の抗体産生系の新規な細胞選択機構を見し、これを応用して抗原レセプターシグナルの強度を細胞生存シグナルの強度に変換し、生体内での高親和性抗体の高効率な選択機構を模倣する技術を開発する。本研究では、DT40細胞を用いて抗原への親和性に依存した抗原レセプターシグナル調節機構を解明し、この知見を利用した有用な目的抗体の高効率選択技術を開発する。
抗原レセプター刺激に依存して誘導されるNR4A1 (nuclear receptor 4A1)の転写に必要なシグナル経路ついて、前年度明らかにしたCa2+イオンをセカンドメッセンジャーとするシグナル伝達経路の下流シグナル経路について各種阻害剤を用いて詳細に解析した。DT40細胞のNR4A1発現は、カルシウムシグナルのうち、CaMK経路には依存せず、カルシーニューリンとPKCの経路に依存していることが明らかになった。最終的な遺伝子の発現調節領域の同定とシグナル経路の関与も解析を進めている。
抗原レセプター刺激に依存して発現される遺伝子について、公的データベース上のDT40細胞を用いた関連研究のトランスクリプトーム解析データから絞り込んだ遺伝子群を、本研究の実験系においても検証したところ発現誘導される候補遺伝子のこれらの多くは、Ca2+イオンをセカンドメッセンジャーとするシグナル伝達経路に依存し、その下流経路は遺伝子によって異なっていることを見出した。これらがBCRの刺激強度と発現量の時間的変化にどのように関与しているかにについて現在、解析を進めている。

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Regulation of somatic hypermutation on the immunoglobulin gene by novel functions of an RNA splicing factor

Grant number：16K14783 2016.04 - 2018.03

Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Challenging Exploratory Research Grant-in-Aid for Challenging Exploratory Research

KANAYAMA Naoki

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Grant amount：\3770000 （ Direct expense: \2900000 、 Indirect expense：\870000 ）

The affinity of antibodies is improved by somatic hypermutation on the immunoglobulin variable region gene. Although it has been shown that AID is essential for somatic hypermutation, it remains unclear how the AID-dependent mutation machinery works. In this study, functions of SRSF1-3, which is an isoform of the RNA splicing factor SRSF1 and essential for somatic hypermutation, were analyzed using a hypermutating B cell line. Results revealed that SRSF1-3 forms a protein complex with AID, and promotes somatic hypermutation through a mechanism linked to the C-terminal region of AID.

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Improvement of an animal cell-displaying technology by using a splicing factor

Grant number：15H04196 2015.04 - 2019.03

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)

Kanayama Naoki

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Grant amount：\16640000 （ Direct expense: \12800000 、 Indirect expense：\3840000 ）

We have been developing an animal cell-displaying technology using the hypermutating B cell line DT40. In this study, we elucidated a function of a splicing factor, SRSF1, which we have previously found that is essential for hypermutation of the immunoglobulin gene, and developed a method to increase hypermutation efficiency by manipulation of SRSF1 expression.

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Analysis of a novel role of an RNA splicing factor in somatic hypermutation of the IgV gene

Grant number：26650126 2014.04 - 2016.03

Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Challenging Exploratory Research Grant-in-Aid for Challenging Exploratory Research

Kanayama Naoki

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Grant amount：\4030000 （ Direct expense: \3100000 、 Indirect expense：\930000 ）

In this study, we analyzed molecular mechanisms for SRSF1-3 to contribute to somatic hypermutation of the IgV gene. It is revealed that although isoforms SRSF1 and SRSF1-3 are different only in the C-terminal region, the C-terminal region of SRSF1-3 is not essential for SHM, suggesting that the conserved region might be involved in SHM. In addition, this study indicated that SRSF1-3 may have a role in regulating the nuclear export of AID during SHM processes.

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Antibody engineering in a hypermutaing B cell line

Grant number：24360343 2012.04 - 2015.03

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)

KANAYAMA NAOKI, MAGARI Masaki

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Grant amount：\12480000 （ Direct expense: \9600000 、 Indirect expense：\2880000 ）

Antibody is being applied for a next generation molecular targeting drug, and modified versions of antibodies, such as single chain antibodies, are also being developed. We have established an in vitro antibody generation system using a hypermutating chicken B cell line, DT40. In this study, we established a novel animal display system, in which any antibody or antibody variant of interest, even though it is derived from the other technology, can be introduced and expressed as a chimeric antibody with the human IgG1 constant region on DT40 cells, and then can be improved in its affinity with the mutation machinery of DT40 cells. This study will be useful for creating antibodies that have valuable activities as antibody drugs.

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Novel functions of ASF/SF2 in somatic hypermutation on the immunoglobulin gene.

Grant number：23657092 2011 - 2012

Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Challenging Exploratory Research Grant-in-Aid for Challenging Exploratory Research

KANAYAMA Naoki

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Grant amount：\3900000 （ Direct expense: \3000000 、 Indirect expense：\900000 ）

The affinity of antibodies for antigens is improved by somatic hypermutation (SHM) occurred on the immunoglobulin (Ig) gene. In this study, using the hypermutating chicken B cell line DT40, we found that an isoform of the alternative-splicing factor ASF/SF2, ASF3 is essential for SHM on the Ig gene. The results also suggest that ASF3 might have a role in the activation and targeting of the mutation machinery through the regulation of post-transcriptional processing on the Ig gene.

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ニワトリB細胞株を利用する抗体の分子進化システムの構築と応用

Grant number：15760589 2003 - 2004

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)

金山直樹

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Grant amount：\3500000 （ Direct expense: \3500000 ）

本研究は、DT40細胞の抗体遺伝子改変能力を利用して、抗体の分子進化システムを構築することを目的としている。昨年度、DT40細胞株において抗体遺伝子への突然変異と遺伝子変換の導入を厳密かつ任意に制御するために、突然変異と遺伝子変換に必須の因子であるAID遺伝子の発現をCre/loxPシステムを用いた遺伝子組み換えによって制御できる細胞株の育種を達成した。この細胞は、導入したCre-ERにより、4-hydroxytamoxyfen(4-OHT)添加時にloxPで挟まれたAIDの発現をON/OFFする。AIDの発現はGFPの発現でモニターし、AID OFFの時はピューロマイシン耐性として選択できる。
本年度、この細胞の変異能力とスイッチ能力について評価した。4-OHTで48時間処理後、48時間追加培養したところ、OFF細胞から平均20%のGFP陽性細胞が出現した。このGFP陽性をセルソーターによって一細胞ずつ分離してAID ON細胞として培養した。2ヶ月間の継続培養後、ほぼすべてがGFP陽性であり、AIDの発現が安定して維持されていることが明らかになった。また、抗体軽鎖遺伝子上に蓄積された変異を解析したところ、解析した24クローン中13クローンで変異が認められ、DT40が本来有している能力に相当するあるいはそれ以上の変異能力を有していた。さらに、ON細胞を4-OHT処理したところ、平均50%のGFP陰性細胞が出現し、ピューロマイシン添加によりOFF細胞のみに純化できた。このOFF細胞から、再度の4-OHT処理でON細胞が出現し、ON細胞の単離、培養、OFF細胞へのスイッチが繰り返し可能であった。すなわち、この細胞を用いて、有用な変異体を取得後、AID OFFにより変異を固定し、再度ONにして抗体遺伝子に二次的変異を導入して改良することが可能になった。

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Analysis and application of the capability of immune system to improve antigen-specificity of antibodies.

Grant number：12450334 2000 - 2002

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)

OHMORI Hitoshi, KANAYAMA Naoki

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Grant amount：\12700000 （ Direct expense: \12700000 ）

Recently, peripheral B cells have been shown to undergo secondary V(D)J rearrangement of Ig genes, but the physiological role of this event has not been fully elucidated. Here, we investigated whether rearrangement of L chain genes in the periphery is involved in the generation of high-affinity Abs. To test this possibility, we used a 17.2.25 rearranged VHDJH gene (VHT)-knockin mouse whose B cell diversity is limited due to the expression of the site-directed transgene. Immunization of the mouse with p-nitrophenylacetyl (pNP)-conjugated chicken γ-globulin (CGG) preferentially led to the production of anti-pNP IgG Abs comprised of non-VHT-encoded H chains and λ chains, which constituted a majority of high-affinity IgG to this hapten. We isolated three independent anti-pNP IgG1 mAbs (two bearing λ1 with high-affinity and one bearing κ with low-affinity), all of which used a common VHDJH containing an identical point mutation, thus suggesting that κ to λ1 replacement contributed to an increase of the Ab affinity. RAG-2 mRNA and the recombination signal sequence break reflecting the λ1 gene rearrangement were detected in the draining lymph node (LN) of immunized mice, but not of non-immunized animals. There was a close correlation between the levels of the λ gene rearrangement and λ^+ high-affinity anti-pNP IgG. Thus, our findings suggest that new rearrangement of λ genes in the periphery contributes to affinity maturation of anti-pNP IgG.

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トランスジェニックマウスの成熟B細胞を用いた代替軽鎖の機能解析系の構築と応用

Grant number：12750704 2000 - 2001

日本学術振興会科学研究費助成事業奨励研究(A) 奨励研究(A)

金山直樹

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Grant amount：\2200000 （ Direct expense: \2200000 ）

本年度は、平成12年度に確立したin vitro代替軽鎖発現系を用いて、トランスジェニックマウスのB細胞での代替軽鎖の発現について検討し、また、発現細胞の由来について野生型マウスを用いて検討して、以下のような成果が得られた。
1.B細胞レパトアが限定されたトランスジェニックマウスの脾臓B細胞を単離し、anti-CD40抗体およびIL-7で刺激したところ、λ5およびRAG2の発現がRT-PCR荷よって確認された。したがって、in vitroでの代替軽鎖はRAG2の発現は、マウスの系統やB細胞レパトアの大きさに関係なく起こる現象であり、トランスジェニックマウスを用いたin vitroの解析系は代替軽鎖およびRAGの機能解析に適していることが示された。
2.脾臓細胞中において代替軽鎖を発現する細胞集団を同定するため、未熟B細胞に発現する抗原を認識する493抗体でB細胞を分画して、代替軽鎖の発現を検討した。単離細胞中に最初から存在する代替軽鎖発現細胞は、多くが未熟B細胞である可能性が示されたが、それらを除去したB細胞においても、in vitro刺激に依存して代替軽鎖の発現が確認されたことから、末梢成熟B細胞において代替軽鎖が発現していることが示唆された。
今後、このトランスジェニックマウスを用いた代替軽鎖解析系を用いて、末梢B細胞における抗体遺伝子再構成の機構について詳細な検討をする予定である。

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Analytical Chemistry （2022academic year） 1st and 2nd semester - 水1～2
Analytical Chemistry （2022academic year） 1st and 2nd semester - 水1～2
Analytical Chemistry 1 （2022academic year） 1st semester - 水1～2
Analytical Chemistry 2 （2022academic year） Second semester - 水1～2
Laboratory Work and Practice on Basic Engineering （2022academic year） 1st and 2nd semester - 火5～8
Laboratory Work and Practice on Basic Engineering （2022academic year） 1st and 2nd semester - 火5～8
Technical Writing and Presentation （2022academic year） Late - その他
Technical Writing and Presentation （2022academic year） Late - その他
Analytical Chemistry in Environmental Fields Ⅱ （2022academic year） Second semester - 水1～2
Analytical Chemistry in Environmental Fields I （2022academic year） 1st semester - 水1～2
Biochemistry 3 （2022academic year） 1st semester - 火3～4,金3～4
Biochemistry 3 （2022academic year） Fourth semester - 月3～4,木1～2
Applied Biology （2022academic year） Fourth semester - 月1～2
Applied Biology （2022academic year） Fourth semester - 月1～2
Cell Technology （2022academic year） Prophase - 不開講
Advanced Cell Technology （2022academic year） Late - その他
SDGs:Life Science （2021academic year） Fourth semester - 木7～8
Technical English for Interdisciplinary Medical Sciences and Engineering （2021academic year） Late - その他
Research Works for Interdisciplinary Medical Sciences and Engineering （2021academic year） Year-round - その他
Advanced Hospital Practice （2021academic year） Prophase - その他
Analytical Chemistry （2021academic year） 1st and 2nd semester - 木3,木4
Analytical Chemistry 1 （2021academic year） 1st semester - 木3,木4
Analytical Chemistry 2 （2021academic year） Second semester - 木3,木4
Laboratory Work and Practice on Basic Engineering （2021academic year） 1st and 2nd semester - 火5,火6,火7,火8
Laboratory Work and Practice on Basic Engineering （2021academic year） 1st and 2nd semester - 火5,火6,火7,火8
Laboratory Work and Practice on Basic Engineering （2021academic year） 1st and 2nd semester - 火5,火6,火7,火8
Technical Writing and Presentation （2021academic year） Late - その他
Technical Writing and Presentation （2021academic year） Late - その他
Radiation Safety Usage Engineering 2 （2021academic year） Second semester - 金5,金6
Radiation Safety Engineering and Experiments （2021academic year） 1st and 2nd semester - 金5,金6
Biochemistry 3 （2021academic year） 1st semester - 火3,火4,金3,金4
Applied Biology （2021academic year） Fourth semester - 月3,月4
Applied Biology （2021academic year） Fourth semester - 月3,月4
Cell Technology （2021academic year） Prophase - 月1～2
Advanced Cell Technology （2021academic year） Late - その他
Internship for Interdisciplinary Medical Sciences and Engineering （2020academic year） Year-round - その他
Technical English for Interdisciplinary Medical Sciences and Engineering （2020academic year） Late - その他
Research Works for Interdisciplinary Medical Sciences and Engineering （2020academic year） Year-round - その他
Analytical Chemistry （2020academic year） 1st and 2nd semester - 水3,水4
Analytical Chemistry 1 （2020academic year） 1st semester - 水3,水4
Analytical Chemistry 2 （2020academic year） Second semester - 水3,水4
Technical Writing and Presentation （2020academic year） Late - その他
Radiation Safety Usage Engineering 2 （2020academic year） Second semester - 金5,金6
Radiation Safety Engineering and Experiments （2020academic year） 1st and 2nd semester - 金5,金6
Biology (Introduction to Biotechnology) （2020academic year） special - その他
Biology (Introduction to Biotechnology) （2020academic year） Fourth semester - 木3,木4
Biochemistry 3 （2020academic year） 1st semester - 火3,火4,金3,金4
Applied Biology （2020academic year） Fourth semester - 月3,月4
Applied Biology （2020academic year） Fourth semester - 月3,月4
Advanced Cell Technology （2020academic year） Late - その他

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