Updated on 2024/12/25

写真a

 
TANABE Katsuyuki
 
Organization
Okayama University Hospital Special-Appointment Lecturer
Position
Special-Appointment Lecturer
External link

Degree

  • PhD ( Okayama University )

Research Interests

  • Acute kidney injury

  • Diabetic kidney disease

  • Renal replacement therapy

  • Chronic kidney disease

Research Areas

  • Life Science / Nephrology

Education

  • Okayama University   医歯学総合研究科  

    2002.4 - 2007.6

      More details

  • Tottori University   医学部   医学科

    1996.4 - 2002.3

      More details

Research History

  • Okayama University Hospital   Division of hemodialysis and apheresis   Assistant professor

    2022.4

      More details

    Country:Japan

    researchmap

  • Okayama University Hospital   Division of hemodialysis and apheresis   Assistant Professor

    2012.9 - 2022.3

      More details

  • University of Colorado Denver   Division of renal disease and hypertension   Postdoctral fellow

    2009.9 - 2012.8

      More details

  • Okayama University   Graduate School of Medicine , Dentistry and Pharmaceutical Sciences

    2008.10 - 2009.8

      More details

  • Okayama University   腎臓・糖尿病・内分泌内科

    2007.10 - 2008.9

      More details

Professional Memberships

  • INTERNATIONAL SOCIETY OF NEPHROLOGY

      More details

  • JAPANESE SOCIETY FOR PERITONEAL DIALYSIS

      More details

  • THE JAPANESE SOCIETY FOR DIALYSIS THERAPY

      More details

  • AMERICAN SOCIETY OF NEPHROLOGY

      More details

  • JAPANESE SOCIETY FOR CLINICAL RENAL TRANSPLANTATION

      More details

  • THE JAPANESE SOCIETY OF INTERNAL MEDICINE

      More details

  • THE JAPAN DIABETES SOCIETY

      More details

  • JAPANESE SOCIETY OF NEPHROLOGY

      More details

▼display all

Committee Memberships

  • 日本透析医学会   評議員  

    2024.6   

      More details

  • 日本腎臓学会   評議員  

    2017.5   

      More details

  • 日本内科学会   中国支部評議員  

    2016.5   

      More details

 

Papers

  • 術前栄養状態と骨格筋評価が腎移植レシピエントの腎予後に与える影響

    山野井 友昭, 西村 慎吾, 関戸 崇了, 吉永 香澄, 定平 卓也, 別宮 謙介, 枝村 康平, 小林 知子, 小林 泰之, 大西 康博, 竹内 英実, 田邊 克幸, 森永 裕士, 荒木 元朗

    移植   59 ( 総会臨時 )   323 - 323   2024.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • Late-onset renal variant Fabry disease with R112H mutation and mild increase in plasma globotriaosylsphingosine: a case report. Reviewed International journal

    Keiko Tanaka, Hitoshi Sugiyama, Hiroshi Morinaga, Akifumi Onishi, Katsuyuki Tanabe, Haruhito A Uchida, Hiroki Maruyama, Jun Wada

    Frontiers in medicine   11   1383309   2024.6

     More details

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

    Fabry disease (FD) is an X-linked disorder resulting in a deficiency of α-galactosidase A (GLA) activity. The R112H mutation of GLA is relatively common in Japanese FD patients, characterized by a late-onset phenotype, almost normal to mild lyso-Gb3 elevation, and mild clinical symptoms, despite low GLA activity. This is due to the structural features of the R112H GLA protein. We herein report the case of a 42-year-old male patient with late-onset FD with a R112H mutation. The patient exhibited only renal involvement with no other organ damage and was successfully treated with galactosidase beta and subsequent migalastat for approximately 10 years. Especially, migalastat was clinically effective in normalizing plasma lyso-Gb3 levels and inhibiting the progression of renal damage associated with FD. Therefore, the use of migalastat in the FD patients with R112H mutation is highly recommended based on this case report.

    DOI: 10.3389/fmed.2024.1383309

    PubMed

    researchmap

  • Preventive effects of vasohibin-2-targeting peptide vaccine for diabetic nephropathy. Reviewed International journal

    Yuri Nakashima, Katsuyuki Tanabe, Tomoyo Mifune, Takato Nakadoi, Hiroki Hayashi, Hironori Nakagami, Yasufumi Sato, Jun Wada

    American journal of physiology. Renal physiology   326 ( 6 )   F1054 - F1065   2024.5

     More details

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

    Diabetic nephropathy remains the leading cause of end-stage kidney disease in many countries, and additional therapeutic targets are needed to prevent its development and progression. Some angiogenic factors are involved in the pathogenesis of diabetic nephropathy. Vasohibin-2 (VASH2) is a novel proangiogenic factor, and our previous study showed that glomerular damage is inhibited in diabetic Vash2 homozygous knockout mice. Therefore, we established a VASH2-targeting peptide vaccine as a tool for anti-VASH2 therapy in diabetic nephropathy. In this study, the preventive effects of the VASH2-targeting peptide vaccine against glomerular injury were examined in a streptozotocin (STZ)-induced diabetic mouse model. The mice were subcutaneously injected with the vaccine at two doses 2 weeks apart and then intraperitoneally injected with 50 mg/kg STZ for 5 consecutive days. Glomerular injury was evaluated 20 weeks after the first vaccination. Treatment with the VASH2-targeting peptide vaccine successfully induced circulating anti-VASH2 antibody without inflammation in major organs. Although the vaccination did not affect blood glucose levels, it significantly prevented hyperglycemia-induced increases in urinary albumin excretion and glomerular volume. The vaccination did not affect increased VASH2 expression but significantly inhibited renal angiopoietin-2 (Angpt2) expression in the diabetic mice. Furthermore, it significantly prevented glomerular macrophage infiltration. The preventive effects of vaccination on glomerular injury were also confirmed in db/db mice. Taken together, the results of this study suggest that the VASH2-targeting peptide vaccine may prevent diabetic glomerular injury in mice by inhibiting Angpt2-mediated microinflammation.

    DOI: 10.1152/ajprenal.00341.2023

    PubMed

    researchmap

  • 大学病院と市中病院における透析内シャント設置術の患者背景及び実施術式に関する比較と考察

    藤井 泰宏, 竹内 英実, 加藤 源太郎, 井上 善紀, 倉田 裕次, 黒子 洋介, 田邊 克幸, 岡本 修吾, 小松 弘明, 枝木 大治, 徳田 雄平, 大澤 晋, 浅川 知彦, 山本 修三, 田蒔 基行, 西岡 聡, 田蒔 昌憲, 和田 淳, 田蒔 正治, 笠原 真悟

    日本透析医学会雑誌   57 ( Suppl.1 )   441 - 441   2024.5

     More details

    Language:Japanese   Publisher:(一社)日本透析医学会  

    researchmap

  • Successful treatment for life threatening recurrent non-traumatic rectus sheath hematoma in a case with microscopic polyangiitis with rapidly progressive glomerulonephritis. Reviewed

    Hiroyuki Nakanoh, Hidemi Takeuchi, Morimoto Shiho, Yuya Terajima, Shugo Okamoto, Yasuhiro Onishi, Keiko Tanaka, Takayuki Katsuyama, Kenji Tsuji, Yoshinori Matsumoto, Katsuyuki Tanabe, Hiroshi Morinaga, Mayu Uka, Koji Tomita, Haruhito A Uchida, Takao Hiraki, Jun Wada

    Internal medicine (Tokyo, Japan)   2024.4

     More details

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

    A 68-year-old woman was admitted to our hospital because of a rapid progression of renal dysfunction with positive myeloperoxidase antineutrophil cytoplasmic antibody and was diagnosed with rapidly progressive glomerulonephritis associated with microscopic polyangiitis (MPA). Severe right rectus sheath hematoma (RSH) bleeding from the inferior epigastric artery developed after starting hemodialysis, which required 4 transarterial embolizations due to recurrent bleeding. After additional treatment with methylprednisolone pulse therapy and rituximab, no rebleeding occurred. Although the giant hematoma reached the pelvis, it shrank spontaneously without any intervention. Nontraumatic RSH should therefore be considered when treating patients with multiple risk factors.

    DOI: 10.2169/internalmedicine.3239-23

    PubMed

    researchmap

  • Early transition to avacopan from glucocorticoids applied during induction therapy for microscopic polyangiitis with rapidly progressive glomerulonephritis. Reviewed

    Hiromasa Miyake, Katsuyuki Tanabe, Shuhei Yamaji, Takashi Kihara

    CEN case reports   2023.12

     More details

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

    Antineutrophil cytoplasmic antibody-associated vasculitis (AAV) is a systemic autoimmune disease characterized by necrotizing inflammation of small blood vessels. Glucocorticoids (GC) in combination with rituximab or cyclophosphamide can reduce AAV-related mortality and rescue renal function. However, several side effects associated with these agents, including GC toxicity, are concerning. Avacopan, an inhibitor of the C5a receptor, is now available for AAV treatment and is expected to mitigate GC toxicity. We present a case of myeloperoxidase-antineutrophil cytoplasmic antibody (MPO-ANCA)-positive microscopic polyangiitis (MPA) with rapidly progressive glomerulonephritis treated with an early switch from GC to avacopan in combination with rituximab during induction therapy. Over a 6-month treatment period, clinical remission was achieved and maintained without infection or elevated liver enzyme levels. Efficacy and safety data regarding avacopan for AAV induction therapy remain limited. Therefore, more case reports are required to clarify the role of avacopan in AAV induction and maintenance therapy. Since the MPO-ANCA titer remained elevated despite the clinical remission of AAV in this case, the ANCA titer may not necessarily be a reliable biomarker for predicting AAV relapse when avacopan is applied as an induction therapy for AAV.

    DOI: 10.1007/s13730-023-00841-3

    PubMed

    researchmap

  • 免疫学的ハイリスク腎移植における低用量リツキシマブを用いた脱感作療法とサイトメガロウイルス感染症 5年間の追跡調査

    吉永 香澄, 関戸 崇了, 丸山 雄樹, 山野井 友昭, 西村 慎吾, 大西 康博, 竹内 英実, 田邊 克幸, 森永 裕士, 枝村 康平, 小林 知子, 小林 泰之, 和田 淳, 荒木 元朗

    移植   58 ( 総会臨時 )   307 - 307   2023.9

  • Elderly Brothers With Fabry Disease Exhibiting Cardiac and Renal Manifestations Reviewed

    Keiko Tanaka, Hitoshi Sugiyama, Hiroshi Morinaga, Akifumi Onishi, Yuzuki Kano, Hidemi Takeuchi, Kenji Tsuji, Motoki Kubo, Katsuyuki Tanabe, Haruhito A. Uchida, Kazufumi Nakamura, Jun Wada

    Annals of Internal Medicine: Clinical Cases   2 ( 5 )   e221003   2023.5

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:American College of Physicians  

    DOI: 10.7326/aimcc.2022.1003

    researchmap

  • The Effect of Medical Cooperation in the CKD Patients: 10-Year Multicenter Cohort Study. Reviewed International journal

    Yasuhiro Onishi, Haruhito A Uchida, Yohei Maeshima, Yuka Okuyama, Nozomu Otaka, Haruyo Ujike, Keiko Tanaka, Hidemi Takeuchi, Kenji Tsuji, Masashi Kitagawa, Katsuyuki Tanabe, Hiroshi Morinaga, Masaru Kinomura, Shinji Kitamura, Hitoshi Sugiyama, Kosuke Ota, Keisuke Maruyama, Makoto Hiramatsu, Yoshiyuki Oshiro, Shigeru Morioka, Keiichi Takiue, Kazuyoshi Omori, Masaki Fukushima, Naoyuki Gamou, Hiroshi Hirata, Ryosuke Sato, Hirofumi Makino, Jun Wada

    Journal of personalized medicine   13 ( 4 )   582   2023.3

     More details

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

    INTRODUCTION: While chronic kidney disease (CKD) is one of the most important contributors to mortality from non-communicable diseases, the number of nephrologists is limited worldwide. Medical cooperation is a system of cooperation between primary care physicians and nephrological institutions, consisting of nephrologists and multidisciplinary care teams. Although it has been reported that multidisciplinary care teams contribute to the prevention of worsening renal functions and cardiovascular events, there are few studies on the effect of a medical cooperation system. METHODS: We aimed to evaluate the effect of medical cooperation on all-cause mortality and renal prognosis in patients with CKD. One hundred and sixty-eight patients who visited the one hundred and sixty-three clinics and seven general hospitals of Okayama city were recruited between December 2009 and September 2016, and one hundred twenty-three patients were classified into a medical cooperation group. The outcome was defined as the incidence of all-cause mortality, or renal composite outcome (end-stage renal disease or 50% eGFR decline). We evaluated the effects on renal composite outcome and pre-ESRD mortality while incorporating the competing risk for the alternate outcome into a Fine-Gray subdistribution hazard model. RESULTS: The medical cooperation group had more patients with glomerulonephritis (35.0% vs. 2.2%) and less nephrosclerosis (35.0% vs. 64.5%) than the primary care group. Throughout the follow-up period of 5.59 ± 2.78 years, 23 participants (13.7%) died, 41 participants (24.4%) reached 50% decline in eGFR, and 37 participants (22.0%) developed end-stage renal disease (ESRD). All-cause mortality was significantly reduced by medical cooperation (sHR 0.297, 95% CI 0.105-0.835, p = 0.021). However, there was a significant association between medical cooperation and CKD progression (sHR 3.069, 95% CI 1.225-7.687, p = 0.017). CONCLUSION: We evaluated mortality and ESRD using a CKD cohort with a long-term observation period and concluded that medical cooperation might be expected to influence the quality of medical care in the patients with CKD.

    DOI: 10.3390/jpm13040582

    PubMed

    researchmap

  • Serum sCD40L and IL-31 in Association with Early Phase of IgA Nephropathy. Reviewed International journal

    Keiko Tanaka, Hitoshi Sugiyama, Hiroshi Morinaga, Masashi Kitagawa, Yuzuki Kano, Yasuhiro Onishi, Koki Mise, Katsuyuki Tanabe, Haruhito A Uchida, Jun Wada

    Journal of clinical medicine   12 ( 5 )   2023.3

     More details

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

    BACKGROUND: IgA nephropathy (IgAN) is a major cause of chronic glomerulonephritis worldwide. T cell dysregulation has been reported to contribute to the pathogenesis of IgAN. Methods We measured a broad range of Th1, Th2 and Th17 cytokines in the serum of IgAN patients. We searched for significant cytokines, which were associated with clinical parameters and histological scores in IgAN patients. RESULTS: Among 15 cytokines, the levels of soluble CD40L (sCD40L) and IL-31 were higher in IgAN patients and were significantly associated with a higher estimated glomerular filtration rate (eGFR), a lower urinary protein to creatinine ratio (UPCR), and milder tubulointerstitial lesions (i.e., the early phase of IgAN). Multivariate analysis revealed that serum sCD40L was an independent determinant of a lower UPCR after adjustment for age, eGFR, and mean blood pressure (MBP). CD40, a receptor of sCD40L, has been reported to be upregulated on mesangial cells in IgAN. The sCD40L/CD40 interaction may directly induce inflammation in mesangial areas and may therefore be involved in the development of IgAN. CONCLUSIONS: The present study demonstrated the significance of serum sCD40L and IL-31 in the early phase of IgAN. Serum sCD40L may be a marker of the beginning of inflammation in IgAN.

    DOI: 10.3390/jcm12052023

    PubMed

    researchmap

  • Effect of Low-Density Lipoprotein Apheresis on Quality of Life in Patients with Diabetes, Proteinuria, and Hypercholesterolemia. Reviewed International journal

    Akinori Hara, Takashi Wada, Eri Muso, Shoichi Maruyama, Sawako Kato, Kengo Furuichi, Kenichi Yoshimura, Tadashi Toyama, Norihiko Sakai, Hiroyuki Suzuki, Tatsuo Tsukamoto, Mariko Miyazaki, Eiichi Sato, Masanori Abe, Yugo Shibagaki, Ichiei Narita, Shin Goto, Yuichi Sakamaki, Hitoshi Yokoyama, Noriko Mori, Satoshi Tanaka, Yukio Yuzawa, Midori Hasegawa, Takeshi Matsubara, Jun Wada, Katsuyuki Tanabe, Kosuke Masutani, Yasuhiro Abe, Kazuhiko Tsuruya, Shouichi Fujimoto, Shuji Iwatsubo, Akihiro Tsuda, Hitoshi Suzuki, Kenji Kasuno, Yoshio Terada, Takeshi Nakata, Noriaki Iino, Tadashi Sofue, Hitomi Miyata, Toshiaki Nakano, Takayasu Ohtake, Shuzo Kobayashi

    Blood purification   52 ( 4 )   373 - 381   2022.12

     More details

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

    INTRODUCTION: Treating diabetic nephropathy with low-density lipoprotein (LDL) apheresis reduces proteinuria and improves prognosis. However, its impact on patients' quality of life (QoL) is unclear. This study evaluated the effect of LDL apheresis on QoL in patients with diabetes, proteinuria, and hypercholesterolemia. METHODS: In this nationwide multicenter prospective study, we enrolled 40 patients with diabetes. Inclusion criteria were proteinuria (defined as an albumin/creatinine ratio ≥3 g/g), serum creatinine levels <2 mg/dL, and serum LDL ≥120 mg/dL despite drug treatment. LDL apheresis was performed 6-12 times within 12 weeks. The 36-item Short Form Health Survey (SF-36) was used to analyze QoL. RESULTS: The study enrolled 35 patients (27 men and 8 women; mean age 58.9 ± 11.9 years). A comparison of baseline SF-36 values with those at the end of the course of apheresis found an improvement in the mean physical component summary (37.9 ± 11.4 vs. 40.6 ± 10.5, p = 0.051) and a significant increase in the mean mental component summary (MCS) (49.4 ± 8.4 vs. 52.5 ± 10.9, p = 0.026). A multivariable linear regression analysis revealed a history of coronary heart disease negatively correlated with the MCS increase at the end of the course of apheresis (β coefficient -6.935, 95% confidence interval, 13.313 to-0.556, p = 0.034). CONCLUSION: Our results suggest that LDL apheresis may improve the mental and physical QoL in patients with diabetes, proteinuria, and hypercholesterolemia.

    DOI: 10.1159/000527900

    PubMed

    researchmap

  • Silica-associated systemic lupus erythematosus with lupus nephritis and lupus pneumonitis: A case report and a systematic review of the literature. Reviewed International journal

    Kazuhiko Fukushima, Haruhito A Uchida, Yasuko Fuchimoto, Tomoyo Mifune, Mayu Watanabe, Kenji Tsuji, Katsuyuki Tanabe, Masaru Kinomura, Shinji Kitamura, Yosuke Miyamoto, Sae Wada, Taisaku Koyanagi, Hitoshi Sugiyama, Takumi Kishimoto, Jun Wada

    Medicine   101 ( 7 )   e28872   2022.2

     More details

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

    INTRODUCTION: Several epidemiological studies have shown that silica exposure triggers the onset of systemic lupus erythematosus (SLE); however, the clinical characteristics of silica-associated SLE have not been well studied. PATIENT CONCERNS: A 67-year-old man with silicosis visited a primary hospital because of a fever and cough. His respiratory condition worsened, regardless of antibiotic medication, and he was referred to our hospital. DIAGNOSIS: The patient showed leukopenia, lymphopenia, serum creatinine elevation with proteinuria and hematuria, decreased serum C3 level, and was positive for anti-double stranded DNA antibody, anti-nuclear antibody, and direct Coombs test. He was diagnosed with SLE. Renal biopsy was performed, and the patient was diagnosed with lupus nephritis (class IV-G(A/C) + V defined by the International Society of Nephrology/Renal Pathology Society classification). Computed tomography revealed acute interstitial pneumonitis, bronchoalveolar lavage fluid showed elevation of the lymphocyte fraction, and he was diagnosed with lupus pneumonitis. INTERVENTIONS: Prednisolone (50 mg/day) with intravenous cyclophosphamide (500 mg/body) were initiated. OUTCOMES: The patient showed a favorable response to these therapies. He was discharged from our hospital and received outpatient care with prednisolone slowly tapered off. He had cytomegalovirus and herpes zoster virus infections during treatment, which healed with antiviral therapy. REVIEW: We searched for the literature on sSLE, and selected 11 case reports and 2 population-based studies. The prevalence of SLE manifestations in sSLE patients were comparative to that of general SLE, particularly that of elderly-onset SLE. Our renal biopsy report and previous reports indicate that lupus nephritis of sSLE patients show as various histological patterns as those of general SLE patients. Among the twenty sSLE patients reported in the case articles, three patients developed lupus pneumonitis and two of them died of it. Moreover, two patients died of bacterial pneumonia, one developed aspergillus abscesses, one got pulmonary tuberculosis, and one developed lung cancer. CONCLUSION: Close attention is needed, particularly for respiratory system events and infectious diseases, when treating patients with silica-associated SLE using immunosuppressive therapies.

    DOI: 10.1097/MD.0000000000028872

    PubMed

    researchmap

  • Vasohibin-1 has α-tubulin detyrosinating activity in glomerular podocytes. Reviewed International journal

    Tomoyo Mifune, Katsuyuki Tanabe, Yuri Nakashima, Satoshi Tanimura, Hitoshi Sugiyama, Yasufumi Sato, Jun Wada

    Biochemical and biophysical research communications   599   93 - 99   2022.2

     More details

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

    Podocytes are highly specialized epithelial cells in glomeruli, with a complex morphology composed of a cell body, primary processes, and foot processes, which maintain barrier function in glomerular filtration. The microtubule-based cytoskeleton is necessary for podocyte morphology. Microtubule structure and function can be affected by post-translational modification of tubulin, including detyrosination. Recent studies have shown that vasohibin-1 (VASH1), an antiangiogenic factor, has tubulin carboxypeptidase activity that causes detyrosination of α-tubulin. We aimed to examine the role of VASH1 in regulating α-tubulin detyrosination in podocytes and the potential involvement of VASH1 deficiency in renal morphology. In normal mouse kidneys, detyrosinated α-tubulin was mainly identified in glomeruli, especially in podocytes; meanwhile, in cultured immortalized podocytes, α-tubulin detyrosination was promoted with cell differentiation. Notably, α-tubulin detyrosination in glomeruli was diminished in Vash1 homozygous knockout (Vash1-/-) mice, and knockdown of VASH1 in cultured podocytes prevented α-tubulin detyrosination. Although VASH1 deficiency-induced downregulation of detyrosination caused no remarkable glomerular lesions, urinary albuminuria excretion and glomerular volume were significantly higher in Vash1-/- mice than in wild-type mice. Furthermore, decreased glomerular nephrin expression and narrower slit diaphragms width were observed in Vash1-/- mice. Taken together, we demonstrated that α-tubulin detyrosination in podocytes was mainly regulated by VASH1 and that VASH1 deficiency-mediated decreases in α-tubulin detyrosination led to minor alterations in podocyte morphology and predisposition to albuminuria. VASH1 expression and α-tubulin detyrosination may be novel targets for maintaining glomerular filtration barrier integrity.

    DOI: 10.1016/j.bbrc.2022.02.047

    PubMed

    researchmap

  • Management of corticosteroid-dependent eosinophilic interstitial nephritis: A case report. Reviewed International journal

    Katsuyuki Tanabe, Natsumi Matsuoka-Uchiyama, Tomoyo Mifune, Chieko Kawakita, Hitoshi Sugiyama, Jun Wada

    Medicine   100 ( 50 )   e28252   2021.12

     More details

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

    INTRODUCTION: Drug-induced acute interstitial nephritis (DI-AIN) is an important cause of acute kidney injury. In renal biopsy specimens, tubulitis with eosinophilic infiltration is suggestive of DI-AIN. Although corticosteroid therapy and discontinuation of the offending drug can improve renal dysfunction in most cases of DI-AIN, some patients experience AIN recurrence, leading to corticosteroid dependency. Corticosteroid-dependent eosinophilic interstitial nephritis presents a difficult dilemma in diagnosis and information regarding optimum management is limited. PATIENT CONCERNS: A 25-year-old man, who received treatment with carbamazepine, zonisamide, valproate, and lacosamide for temporal lobe epilepsy, showed an increase in serum creatinine level from 0.98 to 1.29 mg/dL over a period of 6 months. Although he exhibited no symptoms, his serum creatinine level continued to increase to 1.74 mg/dL. DIAGNOSIS: Renal biopsy revealed tubulitis and interstitial inflammatory infiltrates with eosinophils. Immunological and ophthalmological examinations showed no abnormal findings, and thus, his renal dysfunction was presumed to be caused by DI-AIN. Although oral prednisolone (PSL) administration (40 mg/d) and discontinuation of zonisamide immediately improved his renal function, AIN recurred 10 months later. The increase in PSL dose along with discontinuation of valproate and lacosamide improved renal function. However, 10 months later, recurrent AIN with eosinophilic infiltration was confirmed by further biopsy. The patient was therefore diagnosed with corticosteroid-dependent eosinophilic interstitial nephritis. INTERVENTIONS: To prevent life-threatening epilepsy, carbamazepine could not be discontinued; hence, he was treated with an increased dose of PSL (60 mg/d) and 1500 mg/d of mycophenolate mofetil (MMF). OUTCOMES: MMF was well tolerated and PSL was successfully tapered to 5 mg/d; renal function stabilized over a 20-month period. LESSONS: The presence of underdetermined autoimmune processes and difficulties in discontinuing the putative offending drug discontinuation are contributing factors to corticosteroid dependency in patients with eosinophilic interstitial nephritis. MMF may be beneficial in the management of corticosteroid-dependent eosinophilic interstitial nephritis by reducing the adverse effects related to high-dose and long-term corticosteroid use.

    DOI: 10.1097/MD.0000000000028252

    PubMed

    researchmap

  • Presence of decoy cells for 6 months on urine cytology efficiently predicts BK virus nephropathy in renal transplant recipients. Reviewed International journal

    Takanori Sekito, Motoo Araki, Kasumi Yoshinaga, Yuki Maruyama, Takuya Sadahira, Shingo Nishimura, Koichiro Wada, Masami Watanabe, Toyohiko Watanabe, Katsuyuki Tanabe, Hidemi Takeuchi, Hiroshi Morinaga, Masashi Kitagawa, Shinji Kitamura, Hitoshi Sugiyama, Jun Wada, Hiroyuki Yanai, Yasutomo Nasu

    International journal of urology : official journal of the Japanese Urological Association   28 ( 12 )   1240 - 1246   2021.9

     More details

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

    OBJECTIVES: To investigate the association between duration of consecutive presence of decoy cells on urine cytology and BK virus nephropathy after kidney transplantation. METHODS: In total, 121 kidney transplant recipients were retrospectively evaluated. The best duration of consecutive presence of decoy cells that could be used to predict BK virus nephropathy was analyzed using the area under the curve for each duration, and recipients were divided into two groups based on the best predictive performance. The effectiveness of SV40 immunostaining on urinary cytology was also analyzed. RESULTS: In total, 2534 urine specimens as well as SV40 immunostaining in 2241 urine specimens were analyzed. Six consecutive months of decoy cell positivity had the best predictive performance for BK virus nephropathy (area under the curve = 0.832). The incidence of BK virus nephropathy in recipients with positive decoy cells for 6 months or more consecutive months (5/44) was significantly higher than in those who had positive decoy cells for less than 6 months (0/77; P = 0.005). Decoy cell positivity had a sensitivity, specificity, positive predictive value, and negative predictive value for BK virus nephropathy of 100%, 66%, 11%, and 100% respectively. SV40 immunostaining provided slightly better specificity (68%) and positive predictive value (12%). CONCLUSIONS: The detection of decoy cells at 6 months or more on urine cytology had high predictive value for BK virus nephropathy in kidney transplant recipients. SV40 immunostaining on urine cytology added minimal diagnostic accuracy.

    DOI: 10.1111/iju.14679

    PubMed

    researchmap

  • Feasible kidney donation with living marginal donors, including diabetes mellitus. Reviewed International journal

    Kasumi Yoshinaga, Motoo Araki, Koichiro Wada, Takanori Sekito, Shogo Watari, Yuki Maruyama, Yosuke Mitsui, Takuya Sadahira, Risa Kubota, Shingo Nishimura, Kohei Edamura, Yasuyuki Kobayashi, Katsuyuki Tanabe, Hidemi Takeuchi, Masashi Kitagawa, Shinji Kitamura, Jun Wada, Masami Watanabe, Toyohiko Watanabe, Yasutomo Nasu

    Immunity, inflammation and disease   9 ( 3 )   1061 - 1068   2021.6

     More details

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

    OBJECTIVES: To compare the donor outcomes of living donor kidney transplantation between standard donors (SDs) and marginal donors (MDs) including diabetic patients (MD + DM). METHODS: MDs were defined according to Japanese guideline criteria: (a) age >70-years, (b) blood pressure ≤130/80 mmHg on hypertension medicine, (c) body mass index >25 to ≤32 kg/m2 , (d) 24-h creatinine clearance ≥70 to <80 ml/min/1.73 m2 , and (e) hemoglobin A1c > 6.2 or ≤6.5 with oral diabetic medicine. Fifty-three of 114 donors were MDs. We compared donor kidney functions until 60 months postoperatively. RESULTS: No kidney function parameters were different between SDs and MDs. When comparing SD and MD + DM, MD + DM had a lower postoperative eGFR (48 vs. 41 (1 (month), p = .02), 49 vs. 40 (12, p < .01), 48 vs. 42 (24, p = .04), 47 vs. 38 (36, p = .01)) and the percentage of residual eGFR (SD vs. MD + DM: 63 vs. 57 (1 (month), p < .01), 63 vs. 57 (2, p < .01), 64 vs. 56 (12, p < .01), 63 vs. 57 (24, p < .01), 63 vs. 52 (36, p = .02)). However, when MD with a single risk factor of DM was compared to SD, the difference disappeared. Nine out of 12 (75%) MD + DM had ≥2 risk factors. CONCLUSIONS: Although long-term observation of donor kidney function is necessary, careful MD + DM selection had the potential to expand the donor pool.

    DOI: 10.1002/iid3.470

    PubMed

    researchmap

  • Blood concentrations of tacrolimus upon conversion from rabeprazole to vonoprazan in renal transplant recipients: Correlation with cytochrome P450 gene polymorphisms. Reviewed International journal

    Shogo Watari, Motoo Araki, Jun Matsumoto, Kasumi Yoshinaga, Takanori Sekito, Yuki Maruyama, Yosuke Mitsui, Takuya Sadahira, Risa Kubota, Shingo Nishimura, Koichiro Wada, Yasuyuki Kobayashi, Hidemi Takeuchi, Katsuyuki Tanabe, Masashi Kitagawa, Hiroshi Morinaga, Shinji Kitamura, Hitoshi Sugiyama, Noritaka Ariyoshi, Jun Wada, Masami Watanabe, Toyohiko Watanabe, Yasutomo Nasu

    Drug metabolism and pharmacokinetics   40   100407 - 100407   2021.5

     More details

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

    We evaluated the impact of vonoprazan on blood concentrations of tacrolimus via a retrospective analysis of 52 renal transplant recipients who took tacrolimus and converted from rabeprazole to vonoprazan between August 2018 and September 2019. We compared tacrolimus trough levels upon conversion among groups that were classified based on cytochrome P450 (CYP) gene polymorphisms. CYP3A5 groups were heterozygous or homozygous for CYP3A5∗1 and CYP3A5∗3 alleles. CYP2C19 genotypes were classified as extensive (∗1/∗1), intermediate (∗1/∗2 and ∗1/∗3) or poor metabolizers (∗2/∗2, ∗2/∗3 and ∗3/∗3). Tacrolimus trough levels increased only 0.3 ng/mL upon conversion in the CYP3A5∗3/∗3 group: 5.8 [3.4-7.2] vs 6.1 [3.8-7.9]; p = 0.06. No statistically significance changes in tacrolimus levels also occurred in the CYP3A5∗1/∗1 or CYP3A5∗1/∗3 groups. Subgroup analyses of CYP3A5∗3/∗3 demonstrated low changes for all three CYP2C19 subgroups: 5.2 [4.3-6.5] vs 6.2 [4.3-7.9]; p = 0.07, 6.1 [3.4-7.2] vs 6.7 [4.6-7.9]; p = 0.12 and 5.4 [3.6-6.5] vs 4.7 [3.8-6.3]; p = 1.00, respectively. Conversion to vonoprazan thus resulted in little increase of tacrolimus trough levels, even in the group predicted to be most susceptible (CYP3A5∗3/∗3 and 2C19∗1/∗1), thus supporting the safety of concomitant use of vonoprazan with tacrolimus.

    DOI: 10.1016/j.dmpk.2021.100407

    PubMed

    researchmap

  • ABO Blood Incompatibility Positively Affects Early Graft Function: Single-Center Retrospective Cohort Study. Reviewed International journal

    Shogo Watari, Motoo Araki, Koichiro Wada, Kasumi Yoshinaga, Yuki Maruyama, Yosuke Mitsui, Takuya Sadahira, Risa Kubota, Shingo Nishimura, Yasuyuki Kobayashi, Hidemi Takeuchi, Katsuyuki Tanabe, Masashi Kitagawa, Hiroshi Morinaga, Shinji Kitamura, Hitoshi Sugiyama, Jun Wada, Masami Watanabe, Toyohiko Watanabe, Yasutomo Nasu

    Transplantation proceedings   53 ( 5 )   1494 - 1500   2021.4

     More details

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

    BACKGROUND: We investigated the association between ABO-incompatible (ABO-I) kidney transplantation and early graft function. METHODS: We retrospectively analyzed 95 patients who underwent living donor kidney transplantation between May 2009 and July 2019. It included 61 ABO-compatible (ABO-C) and 34 ABO-I transplantations. We extracted data on immunologic profile, sex, age, cold ischemic time, type of immunosuppression, and graft function. Two definitions were used for slow graft function (SGF) as follows: postoperative day (POD) 3 serum creatinine level >3 mg/dL and estimated glomerular filtration rate (eGFR) <20 mL/min/1.73 m2. Logistic regression analysis was performed to analyze the effect of ABO-I on the incidence of SGF. RESULTS: The characteristics between the ABO-C and ABO-I were not different. ABO-I received rituximab and plasma exchange. Patients also received tacrolimus and mycophenolate mofetil for 2 weeks and prednisolone for 1 week before transplantation as preconditioning. Of the 95 study patients, 19 (20%) and 21 (22%) were identified with SGF according to POD 3 serum creatinine level or eGFR, respectively. Multivariable analysis revealed that ABO-I significantly reduced the incidence of SGF (odds ratio, 0.15; 95% confidence interval, 0.03-0.7; P = .02), and cold ischemic time >150 min increased the incidence of SGF (odds ratio, 6.5; 95% confidence interval, 1.7-25; P = .006). Similar results were identified in POD 3 eGFR. Inferior graft function in patients with SGF was identified up to 6 months after transplantation. CONCLUSION: ABO-I reduces the incidence of SGF, which is associated with an inferior graft function up to 6 months.

    DOI: 10.1016/j.transproceed.2021.03.043

    PubMed

    researchmap

  • Successful deceased donor kidney transplantation to a recipient with a history of COVID-19 treatment. Reviewed International journal

    Kasumi Yoshinaga, Motoo Araki, Koichiro Wada, Kou Hasegawa, Takanori Sekito, Shuji Miyake, Shogo Watari, Yuki Maruyama, Takuya Sadahira, Shingo Nishimura, Katsuyuki Tanabe, Hidemi Takeuchi, Yuri Nakashima, Masaru Kinomura, Herik Acosta, Yosuke Mitsui, Risa Kubota, Hirochika Nakajima, Kohei Edamura, Yasuyuki Kobayashi, Masami Watanabe, Toyohiko Watanabe, Fumio Otsuka, Jun Wada, Yasutomo Nasu

    Journal of infection and chemotherapy : official journal of the Japan Society of Chemotherapy   27 ( 7 )   1097 - 1101   2021.3

     More details

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

    CASE PRESENTATION: A 49-year-old Asian male, who had undergone hemodialysis for >16 years, complained of a fever, dysgeusia and dysosmia, and was diagnosed with COVID-19 pneumonia based on severe acute respiratory syndrome coronavirus 2 polymerase chain reaction (SARS-CoV-2 PCR) and computed tomography (CT). Treatment was started with oral favipiravir and ciclesonide inhalation. On the 10th day of treatment, the patient had a persistent high fever and a chest CT showed exacerbation of pneumonia, so dexamethasone was intravenously started. He was discharged after confirming two consecutive negative SARS-CoV-2 PCR tests. Three months after COVID-19 treatment, a SARS-CoV-2 PCR test was negative and he underwent a deceased donor kidney transplantation. Basiliximab induction with triple drug immunosuppression consisting of extended-release tacrolimus, mycophenolate mofetil and prednisolone, which is our regular immunosuppression protocol, was used. He was discharged on postoperative day 18 without the need for postoperative hemodialysis or any complications. The serum creatinine level was 1.72 mg/dL 95 days postoperatively and he had a favorable clinical course that was similar to deceased donor kidney recipients without a history of SARS-CoV-2 infection. CONCLUSION: We report the first case of a kidney transplantation after COVID-19 treatment in Japan and the fourth case globally. We would like to provide information about our successful case due to the anticipated increase in similar candidates in the near future.

    DOI: 10.1016/j.jiac.2021.03.018

    PubMed

    researchmap

  • Renal capsular vein thrombosis. Reviewed

    Katsuyuki Tanabe, Jota Maki, Hikari Nakatou

    Clinical and experimental nephrology   25 ( 4 )   439 - 440   2021.1

     More details

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

    A 30-year-old pregnant woman developed postpartum HELLP syndrome. Abdominal computed tomography revealed a high-density vessel structure in contact with the right kidney and connected to the right ovarian vein, suggesting thrombosis in the right inferior renal capsular vein (RCV). RCV thrombosis is a rare thrombotic disorder in postpartum women, and hypercoagulability related to the pregnancy complications may be the predisposing factor. The potential risk for pulmonary embolism in the rare pregnancy-related thrombosis should be recognized.

    DOI: 10.1007/s10157-020-01998-2

    PubMed

    researchmap

  • Vasohibin-2 Aggravates Development of Ascending Aortic Aneurysms But Not Abdominal Aortic Aneurysms Nor Atherosclerosis in ApoE Deficient Mice. Reviewed International journal

    Nozomu Otaka, Haruhito A Uchida, Michihiro Okuyama, Yoshiko Hada, Yasuhiro Onishi, Yuki Kakio, Hidemi Takeuchi, Ryoko Umebayashi, Katsuyuki Tanabe, Venkateswaran Subramanian, Alan Daugherty, Yasufumi Sato, Jun Wada

    American journal of hypertension   34 ( 5 )   467 - 475   2020.11

     More details

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

    BACKGROUND: Vasohibin-2 (VASH2) has been isolated as a homologue of vasohibin-1 (VASH1) that promote angiogenesis counteracting with VASH1. Chronic angiotensin II (AngII) infusion promotes both ascending and abdominal aortic aneurysms (AAs) in mice. The present study aimed to investigate whether exogenous VASH2 influenced AngII-induced vascular pathology in apolipoprotein E deficient (ApoE  -/-) mice. METHODS: Male, ApoE  -/- mice (9 to 14 weeks old) were injected with Ad LacZ or Ad VASH2. After a week, saline or AngII (1,000 ng/kg/min) was infused into the mice subcutaneously via mini-osmotic pumps for 3 weeks. Consequently, all these mice were divided into 4 groups: saline + LacZ (n=5), saline + VASH2 (n=5), AngII + LacZ (n=18), and AngII + VASH2 (n=17). RESULTS: Exogenous VASH2 had no significant effect on ex vivo maximal diameters of abdominal aortas (AngII + LacZ; 1.67±0.17 mm, AngII + VASH2; 1.52±0.16 mm, n.s.) or elastin fragmentation and accumulation of inflammatory cells. Conversely, exogenous VASH2 significantly increased intima areas of aortic arches (AngII + LacZ; 16.6±0.27 mm 2, AngII + VASH2; 18.6±0.64 mm 2, p=0.006). VASH2 effect of AngII-induced ascending AAs was associated with increased cleaved caspase-3 abundance. AngII-induced atherosclerosis was not altered by VASH2. CONCLUSION: The present study demonstrated that augmented VASH2 expression had no effect of AngII-induced abdominal AAs or atherosclerosis, while increasing dilation in the ascending aorta.

    DOI: 10.1093/ajh/hpaa181

    PubMed

    researchmap

  • Acute Kidney Injury Caused by Evans Syndrome with Systemic Lupus Erythematosus and Systemic Sclerosis. Reviewed

    Natsumi Matsuoka, Haruki Watanabe, Naoko Kurooka, Sumari Kato, Chika Higashi, Katsuyuki Tanabe, Masaru Kinomura, Nobuharu Fujii, Ken-Ei Sada, Hitoshi Sugiyama, Jun Wada

    Internal medicine (Tokyo, Japan)   60 ( 7 )   1055 - 1060   2020.10

     More details

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

    A 65-year-old woman with systemic sclerosis and systemic lupus erythematosus developed acute kidney injury (AKI), Coombs-positive autoimmune hemolytic anemia and autoimmune thrombocytopenia; therefore, she was diagnosed with Evans syndrome (ES). Intravascular hemolysis was suggested as the cause of AKI based on the presence of acute tubular injury and trace hemosiderin deposits on the renal biopsy. The renal function, hemolytic anemia and thrombocytopenia were restored by an increased dose of glucocorticoids, hemodialysis, and plasma exchange. Although ES with severe hemolytic anemia is very rare, it is important to detect possible renal dysfunction when encountering patients with severe hemolysis.

    DOI: 10.2169/internalmedicine.5976-20

    PubMed

    researchmap

  • Low-dose rituximab induction therapy is effective in immunological high-risk renal transplantation without increasing cytomegalovirus infection. Reviewed International journal

    Kasumi Yoshinaga, Motoo Araki, Koichiro Wada, Yuki Maruyama, Yosuke Mitsui, Takuya Sadahira, Risa Kubota, Shingo Nishimura, Yasuyuki Kobayashi, Hidemi Takeuchi, Katsuyuki Tanabe, Masashi Kitagawa, Hiroshi Morinaga, Haruhito Adam Uchida, Shinji Kitamura, Hitoshi Sugiyama, Jun Wada, Masami Watanabe, Toyohiko Watanabe, Yasutomo Nasu

    International journal of urology : official journal of the Japanese Urological Association   27 ( 12 )   1136 - 1142   2020.10

     More details

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

    OBJECTIVES: To analyze the effect and impact of low-dose rituximab induction therapy on cytomegalovirus infection in living-donor renal transplantation. METHODS: A total of 92 recipients undergoing living-donor renal transplantation at Okayama University Hospital from May 2009 to August 2018 were evaluated retrospectively. Indications for preoperative rituximab (200 mg/body) were the following: (i) ABO major mismatch; (ii) ABO minor mismatch; (iii) donor-specific anti-human leukocyte antigen antibody-positive; and (iv) focal segmental glomerulosclerosis. We excluded four recipients who were followed <3 months, five who received >200 mg/body rituximab and seven who received prophylactic therapy for cytomegalovirus. RESULTS: There were 59 patients in the rituximab group and 17 in the non-rituximab group. Groups differed significantly in age (median age 53 vs 37 years, respectively; P = 0.04), but not in sex (male 64% vs 65%, P = 1.00), focal segmental glomerulosclerosis (3% vs 0%, P = 1.00) or percentage of cytomegalovirus-seronegative recipients of renal allografts from cytomegalovirus-seropositive donors (12% vs 18%, P = 0.68). The estimated glomerular filtration rate did not differ significantly between groups until 24 months after transplantation. Cytomegalovirus clinical symptoms (10% vs 24%, P = 0.22), including fever ≥38°C (5% vs 12%, P = 0.31) and gastrointestinal symptoms (5% vs 12%, P = 0.31), and the 5-year survival rates of death-censored graft loss (90% vs 83%, P = 0.43) did not differ significantly between groups. CONCLUSIONS: Low-dose rituximab induction therapy is effective in immunological high-risk recipients without increasing cytomegalovirus infection in the absence of valganciclovir prophylaxis.

    DOI: 10.1111/iju.14382

    PubMed

    researchmap

  • Effects of LDL apheresis on proteinuria in patients with diabetes mellitus, severe proteinuria, and dyslipidemia. Reviewed

    Takashi Wada, Akinori Hara, Eri Muso, Shoichi Maruyama, Sawako Kato, Kengo Furuichi, Kenichi Yoshimura, Tadashi Toyama, Norihiko Sakai, Hiroyuki Suzuki, Tatsuo Tsukamoto, Mariko Miyazaki, Eiichi Sato, Masanori Abe, Yugo Shibagaki, Ichiei Narita, Shin Goto, Yuichi Sakamaki, Hitoshi Yokoyama, Noriko Mori, Satoshi Tanaka, Yukio Yuzawa, Midori Hasegawa, Takeshi Matsubara, Jun Wada, Katsuyuki Tanabe, Kosuke Masutani, Yasuhiro Abe, Kazuhiko Tsuruya, Shouichi Fujimoto, Shuji Iwatsubo, Akihiro Tsuda, Hitoshi Suzuki, Kenji Kasuno, Yoshio Terada, Takeshi Nakata, Noriaki Iino, Tadashi Sofue, Hitomi Miyata, Toshiaki Nakano, Takayasu Ohtake, Shuzo Kobayashi

    Clinical and experimental nephrology   25 ( 1 )   1 - 8   2020.8

     More details

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

    BACKGROUND: Patients with diabetes mellitus and severe proteinuria present with poor renal prognoses, despite improvements in diabetes and kidney disease therapies. In this study, we designed a low-density lipoprotein (LDL)-cholesterol apheresis treatment for patients with diabetic nephropathy (DN)/diabetic kidney disease and severe proteinuria. This was a multicenter prospective LICENSE study to confirm the impact of LDL apheresis on proteinuria that exhibited hyporesponsiveness to treatment. In addition, we sought to determine the efficacy and safety of LDL apheresis by comparing the outcomes to those of historical controls in patients with diabetes, refractory hypercholesterolemia, and severe proteinuria. METHODS: This was a prospective, multicenter study, including 40 patients with diabetes, severe proteinuria, and dyslipidemia. LDL apheresis was performed 6-12 times over a 12-week period. The primary endpoint was the proportion of patients with a decrease in proteinuria excretion of at least 30% in the 6 months after starting therapy. The secondary endpoints included serum creatinine levels and laboratory variables, which were evaluated 4, 6, 12, 18, and 24 months after therapy initiation. RESULTS: LDL apheresis was performed on 40 registered patients with diabetes. The proportion of cases in which proteinuria decreased by 30% or more after 6 months of LDL apheresis was 25%, which was similar to that of historical controls. The overall survival and end-stage kidney disease-free survival rates were significantly higher in the LICENSE group compared to those in historical controls. CONCLUSION: Our results suggest that LDL apheresis may be effective and safe for patients with diabetes, proteinuria, and dyslipidemia. TRIAL REGISTRATION: Trial registration number: jRCTs042180076.

    DOI: 10.1007/s10157-020-01959-9

    PubMed

    researchmap

  • Genetic Deletion of Vasohibin-2 Exacerbates Ischemia-Reperfusion-Induced Acute Kidney Injury. Reviewed International journal

    Hiromasa Miyake, Katsuyuki Tanabe, Satoshi Tanimura, Yuri Nakashima, Tomoyo Morioka, Kana Masuda, Hitoshi Sugiyama, Yasufumi Sato, Jun Wada

    International journal of molecular sciences   21 ( 12 )   4545   2020.6

     More details

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

    Acute kidney injury (AKI) has been increasingly recognized as a risk factor for transition to chronic kidney disease. Recent evidence suggests that endothelial damage in peritubular capillaries can accelerate the progression of renal injury. Vasohibin-2 (VASH2) is a novel proangiogenic factor that promotes tumor angiogenesis. However, the pathophysiological roles of VASH2 in kidney diseases remain unknown. In the present study, we examined the effects of VASH2 deficiency on the progression of ischemia-reperfusion (I/R) injury-induced AKI. I/R injury was induced by bilaterally clamping renal pedicles for 25 min in male wild-type (WT) and Vash2 homozygous knockout mice. Twenty-four hours later, I/R injury-induced renal dysfunction and tubular damage were more severe in VASH2-deficient mice than in WT mice, with more prominent neutrophil infiltration and peritubular capillary loss. After induction of I/R injury, VASH2 expression was markedly increased in injured renal tubules. These results suggest that VASH2 expression in renal tubular epithelial cells might be essential for alleviating I/R injury-induced AKI, probably through protecting peritubular capillaries and preventing inflammatory infiltration.

    DOI: 10.3390/ijms21124545

    PubMed

    researchmap

  • Nivolumab-induced IgA nephropathy in a patient with advanced gastric cancer: A case report. Reviewed International journal

    Katsuyuki Tanabe, Hiromitsu Kanzaki, Takahira Wada, Yuri Nakashima, Hitoshi Sugiyama, Hiroyuki Okada, Jun Wada

    Medicine   99 ( 21 )   e20464   2020.5

     More details

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

    INTRODUCTION: Immune checkpoint inhibitors including nivolumab, an antibody against programmed death-1, have been increasingly introduced in various cancer treatment regimens, and are reported to be associated with immune-related adverse events. Nivolumab-induced renal injury is generally caused by acute interstitial nephritis and is managed by drug discontinuation and steroid therapy. Although this agent can infrequently induce glomerulonephritis, the pathogenesis and therapeutic strategy remain undetermined. PATIENT CONCERNS: A 78-year-old man was diagnosed with advanced gastric cancer with portal thrombosis. First- and second-line chemotherapies were ineffective; thus, nivolumab monotherapy was initiated. Although it effectively prevented tumor growth, proteinuria and microhematuria appeared 2 months later. Despite drug discontinuation, serum creatinine progressively increased from 0.72 to 1.45 mg/dL. Renal biopsy revealed mesangial IgA and C3 deposition in immunofluorescence analysis and mesangial proliferation with crescent formation in light microscopy. DIAGNOSIS: The patient was diagnosed with IgA nephropathy. Based on the temporal relationship between the nivolumab therapy and abnormal urinalysis, IgA nephropathy was considered to have been induced by nivolumab. INTERVENTIONS: A moderate dose (0.6 mg/kg/day) of prednisolone was orally administrated, with tapering biweekly. OUTCOMES: Steroid therapy stabilized his serum creatinine levels and markedly reduced proteinuria. However, bacterial pneumonia substantially impaired his performance status; thus, nivolumab could not be restarted despite tumor regrowth. LESSONS: IgA nephropathy should be recognized as an uncommon renal adverse event during nivolumab therapy. After drug discontinuation, nivolumab-induced IgA nephropathy is likely to respond to moderate doses of steroid therapy with early tapering. However, more evidence is needed to determine whether nivolumab can be safely restarted during or after steroid therapy.

    DOI: 10.1097/MD.0000000000020464

    PubMed

    researchmap

  • Targeting angiogenesis and lymphangiogenesis in kidney disease. Reviewed International journal

    Katsuyuki Tanabe, Jun Wada, Yasufumi Sato

    Nature reviews. Nephrology   16 ( 5 )   289 - 303   2020.3

     More details

    Authorship:Lead author   Language:English   Publishing type:Research paper (scientific journal)  

    The kidney is permeated by a highly complex vascular system with glomerular and peritubular capillary networks that are essential for maintaining the normal functions of glomerular and tubular epithelial cells. The integrity of the renal vascular network depends on a balance of proangiogenic and antiangiogenic factors, and disruption of this balance has been identified in various kidney diseases. Decreased levels of the predominant proangiogenic factor, vascular endothelial growth factor A (VEGFA), can result in glomerular microangiopathy and contribute to the onset of preeclampsia, whereas upregulation of VEGFA has roles in diabetic kidney disease (DKD) and polycystic kidney disease (PKD). Other factors that regulate angiogenesis, such as angiopoietin 1 and vasohibin 1, have been shown to be protective in animal models of DKD and renal fibrosis. The renal lymphatic system is important for fluid homeostasis in the kidney, as well as the transport of immune cells and antigens. Experimental studies suggest that the lymphangiogenic factor VEGFC might have protective effects in PKD, DKD and renal fibrosis. Understanding the physiological and pathological roles of factors that regulate angiogenesis and lymphangiogenesis in the kidney has led to the development of novel therapeutic strategies for kidney diseases.

    DOI: 10.1038/s41581-020-0260-2

    PubMed

    researchmap

  • Quality of Life and Mental Satisfaction Improve Slowly in Preemptive Kidney Transplantation Compared With Nonpreemptive Kidney Transplantation. Reviewed International journal

    Yosuke Mitsui, Motoo Araki, Yuki Maruyama, Kasumi Yoshinaga, Takuya Sadahira, Koichiro Wada, Katsuyuki Tanabe, Masashi Kitagawa, Yasuyuki Kobayashi, Masami Watanabe, Toyohiko Watanabe, Yasutomo Nasu

    Transplantation proceedings   52 ( 3 )   740 - 747   2020.3

     More details

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

    BACKGROUND AND AIMS: Preemptive kidney transplantation (PEKT) is recognized as the best therapy to avoid dialysis. However, it is not clear whether PEKT recipients experience an improvement in quality of life (QoL) after kidney transplantation (KT) that exceeds that of non-PEKT recipients, since PEKT recipients have not experienced the heavy burden of dialysis. The aim of this study was to compare the changes in QoL for PEKT and non-PEKT recipients following transplantation. METHODS: Patients included in this study underwent living donor KT in our hospital. We excluded patients with incomplete SF-36 scores and with factors that could affect QoL, such as complications or rejection. QoL was assessed by the Short Form 36-Item Health Survey version 2.0 preoperatively and 3 and 12 months postoperatively. RESULTS: Eighty-eight patients underwent living donor KT in our hospital. Twelve PEKT and 20 non-PEKT recipients were enrolled in this retrospective study. In the non-PEKT group, both the physical and mental domain scores dramatically improved from baseline at 3 months, and remained at a similar level at 12 months. In contrast, in the PEKT group, only 1 domain of the physical and mental score improved at 3 months, and the social functioning score gradually improved at 12 months. Although the mental component score showed significant improvement in the non-PEKT group, it did not change in the PEKT group. CONCLUSIONS: The improvement of QoL after transplantation is more evident in the non-PEKT group. PEKT recipients have less mental satisfaction than non-PEKT recipients.

    DOI: 10.1016/j.transproceed.2020.01.042

    PubMed

    researchmap

  • Robotic Renal Autotransplantation: A Feasibility Study in a Porcine Model. Reviewed

    Risa Kubota, Motoo Araki, Koichiro Wada, Kasumi Kawamura, Yuki Maruyama, Yosuke Mitsui, Takuya Sadahira, Yuichi Ariyoshi, Takehiro Iwata, Shingo Nishimura, Atsushi Takamoto, Tomoko Sako, Kohei Edamura, Yasuyuki Kobayashi, Yuzuki Kano, Masashi Kitagawa, Katsuyuki Tanabe, Hitoshi Sugiyama, Jun Wada, Masami Watanabe, Toyohiko Watanabe, Yasutomo Nasu

    Acta medica Okayama   74 ( 1 )   53 - 58   2020.2

     More details

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

    We investigated the feasibility of robotic renal autotransplantation (RAT) in a porcine model to reduce invasiveness of RAT. Five pigs underwent robotic RAT using the da Vinci® robotic system. A robotic left nephrectomy was performed in all cases. Robotic RAT was performed on the left side in all but one case. Four ports were used. In 3 cases, the kidney was taken out through the GelPort® and irrigated on ice with Ringer's solution. In 2 cases, a complete intracorporeal robotic RAT was performed. An end-to-side anastomosis was performed between the renal vein and the external iliac vein and between the renal artery and the external iliac artery. Ureteroneocystostomy was also performed in 2 cases. All cases were performed robotically without open conversion. The median (IQR) console time was 3.1 (0.7) h, and the operative time was 3.8 (1.1) h. The estimated blood loss was 30 (0) ml. The warm ischemia time was 4.0 (0.2) min, and the cold ischemia time was 97 (17) min. Intracorporeal transarterial hypothermic renal perfusion was feasible in the 2 complete intracorporeal robotic RAT cases by using a perfusion catheter through a laparoscopic port. Robotic RAT has the potential to be a new minimally invasive substitute for conventional open surgery.

    DOI: 10.18926/AMO/57953

    PubMed

    researchmap

  • Podocyte autophagy is associated with foot process effacement and proteinuria in patients with minimal change nephrotic syndrome. Reviewed International journal

    Ayu Ogawa-Akiyama, Hitoshi Sugiyama, Masashi Kitagawa, Keiko Tanaka, Yuzuki Kano, Koki Mise, Nozomu Otaka, Katsuyuki Tanabe, Hiroshi Morinaga, Masaru Kinomura, Haruhito A Uchida, Jun Wada

    PloS one   15 ( 1 )   e0228337   2020.1

     More details

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

    Autophagy is a cellular mechanism involved in the bulk degradation of proteins and turnover of organelle. Several studies have shown the significance of autophagy of the renal tubular epithelium in rodent models of tubulointerstitial disorder. However, the role of autophagy in the regulation of human glomerular diseases is largely unknown. The current study aimed to demonstrate morphological evidence of autophagy and its association with the ultrastructural changes of podocytes and clinical data in patients with idiopathic nephrotic syndrome, a disease in which patients exhibit podocyte injury. The study population included 95 patients, including patients with glomerular disease (minimal change nephrotic syndrome [MCNS], n = 41; idiopathic membranous nephropathy [IMN], n = 37) and 17 control subjects who underwent percutaneous renal biopsy. The number of autophagic vacuoles and the grade of foot process effacement (FPE) in podocytes were examined by electron microscopy (EM). The relationships among the expression of autophagic vacuoles, the grade of FPE, and the clinical data were determined. Autophagic vacuoles were mainly detected in podocytes by EM. The microtubule-associated protein 1 light chain 3 (LC3)-positive area was co-localized with the Wilms tumor 1 (WT1)-positive area on immunofluorescence microscopy, which suggested that autophagy occurred in the podocytes of patients with MCNS. The number of autophagic vacuoles in the podocytes was significantly correlated with the podocyte FPE score (r = -0.443, p = 0.004), the amount of proteinuria (r = 0.334, p = 0.033), and the level of serum albumin (r = -0.317, p = 0.043) in patients with MCNS. The FPE score was a significant determinant for autophagy after adjusting for the age in a multiple regression analysis in MCNS patients (p = 0.0456). However, such correlations were not observed in patients with IMN or in control subjects. In conclusion, the results indicated that the autophagy of podocytes is associated with FPE and severe proteinuria in patients with MCNS. The mechanisms underlying the activation of autophagy in association with FPE in podocytes should be further investigated in order to elucidate the pathophysiology of MCNS.

    DOI: 10.1371/journal.pone.0228337

    PubMed

    researchmap

  • Urine 5MedC, a Marker of DNA Methylation, in the Progression of Chronic Kidney Disease. Reviewed International journal

    Onishi A, Sugiyama H, Kitagawa M, Yamanari T, Tanaka K, Ogawa-Akiyama A, Kano Y, Mise K, Tanabe K, Morinaga H, Kinomura M, Uchida HA, Wada J

    Disease markers   2019   5432453 - 5432453   2019.7

     More details

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

    Background: Alterations in DNA methylation may be involved in disease progression in patients with chronic kidney disease (CKD). Recent studies have suggested that 5-methyl-2'-deoxycytidine (5MedC) may be a marker of hypermethylation of DNA. Currently, there is no information available regarding the urine levels of 5MedC and its association with the progression of CKD. Method: We examined the urine levels of 5MedC in spot urine samples from 308 patients with CKD (median age: 56 years, male: 53.2%, and glomerulonephritis: 51.0%) using a competitive enzyme-linked immunosorbent assay and investigated the relationships among urine 5MedC, urine albumin, urine α1-microglobulin (α1MG), and the laboratory parameters associated with CKD. The patients were followed for three years to evaluate renal endpoints in a prospective manner. Results: The urine 5MedC level was significantly increased in the later stages of CKD compared to the early to middle stages of CKD. In multiple logistic regression models, urine 5MedC was significantly associated with the prediction of later CKD stages. Urine 5MedC (median value, 65.9 μmol/gCr) was significantly able to predict a 30% decline in the estimated GFR or a development of end-stage renal disease when combined with macroalbuminuria or an increased level of urine α1MG (median value, 5.7 mg/gCr). Conclusion: The present data demonstrate that the urine 5MedC level is associated with a reduced renal function and can serve as a novel and potent biomarker for predicting the renal outcome in CKD patients. Further studies will be necessary to elucidate the role of urine DNA methylation in the progression of CKD.

    DOI: 10.1155/2019/5432453

    PubMed

    researchmap

  • Capnocytophaga canimorsus peritonitis diagnosed by mass spectrometry in a diabetic patient undergoing peritoneal dialysis: a case report. Reviewed International journal

    Tanabe K, Okamoto S, Hiramatsu Asano S, Wada J

    BMC nephrology   20 ( 1 )   219 - 219   2019.6

     More details

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

    BACKGROUND: Bacterial peritonitis is a serious complication of patients undergoing peritoneal dialysis (PD). Although the identification of causative organisms and use of appropriate antibiotics are essential for treatment, rare and fastidious bacteria are sometimes difficult to detect by conventional biochemical assays. Capnocytophaga canimorsus is a fastidious and slow-growing bacterium that forms a part of the normal oral flora of dogs and cats and is extremely rare as a peritonitis-causing organism. This report demonstrates the usefulness of a mass spectrometry-based technique in identifying such a rare organism in PD-related peritonitis and discusses the diagnosis and treatment of C. canimorsus peritonitis. CASE PRESENTATION: A 49-year-old woman with type 2 diabetes mellitus underwent PD for two years. Repeated exit-site infections led to subcutaneous pathway diversion two months ago. She was hospitalized with fever and abdominal pain as well as cloudy dialysis effluent. Laboratory data revealed increased serum C-reactive protein level and white blood cell (WBC) count in the effluent. Her exit site had no sign of infection, leading to the diagnosis of PD-related peritonitis. Initial therapy with intraperitoneal ceftazidime immediately ameliorated her symptoms, and the WBC count in the effluent normalized in five days. Culture test results of the dialysis effluent on admission were negative with no information regarding the infection route. However, mass spectrometry (MALDI Biotyper, Bruker Daltonics) successfully obtained the specific spectral pattern for C. canimorsus. She had four cats in her house and was advised not to allow the cats in the room where the bag exchange took place. CONCLUSIONS: C. canimorsus is a rare cause of peritonitis in PD patients and is usually susceptible to intraperitoneal third-generation cephalosporins. This mass spectrometry-based bacterial identification method could provide more opportunities to identify uncommon causes and promote appropriate antibiotics therapy in PD-related peritonitis.

    DOI: 10.1186/s12882-019-1415-x

    PubMed

    researchmap

  • Contrast-enhanced Computed Tomography-Guided Percutaneous Cryoablation of Renal Cell Carcinoma in a Renal Allograft: First Case in Asia. Reviewed

    Tsuboi I, Araki M, Fujiwara H, Iguchi T, Hiraki T, Arichi N, Kawamura K, Maruyama Y, Mitsui Y, Sadahira T, Kubota R, Nishimura S, Sako T, Takamoto A, Wada K, Kobayashi Y, Watanabe T, Yanai H, Kitagawa M, Tanabe K, Sugiyama H, Wada J, Shiina H, Kanazawa S, Nasu Y

    Acta medica Okayama   73 ( 3 )   269 - 272   2019.6

     More details

    Language:English  

    Nephron-sparing treatment should be offered whenever possible to avoid dialysis in allograph cases. Cryoablation is a new treatment option for treating small-sized renal cell cancer (RCCs). We report a case of RCC arising in a kidney allograft treated by cryoablation. To our knowledge, this is the first case in Asia of RCC in a renal allograft treated using cryoablation. Contrast-enhanced CT-guided percutaneous renal needle biopsy and cryoablation were used to identify the RCC, which could not be identified by other techniques. The postoperative course was uneventful. Contrast-enhanced CT also showed no recurrence or metastases at the 6-month follow-up.

    DOI: 10.18926/AMO/56871

    PubMed

    researchmap

  • Renal tubular injury exacerbated by Vasohibin-1 deficiency in a murine cisplatin-induced acute kidney injury model. Reviewed International journal

    Tanimura S, Tanabe K, Miyake H, Masuda K, Tsushida K, Morioka T, Sugiyama H, Sato Y, Wada J

    American journal of physiology. Renal physiology   317 ( 2 )   F264 - F274   2019.5

     More details

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

    Acute kidney injury (AKI) is frequently encountered in clinical practice, particularly secondarily to cardiovascular surgery and administration of nephrotoxic agents, and is increasingly recognized for initiating a transition to chronic kidney disease. Clarifying the pathogenesis of AKI could facilitate the development of novel preventive strategies, because the occurrence of hospital-acquired AKI is often anticipated. Vasohibin-1 (VASH1) was initially identified as an antiangiogenic factor derived from endothelial cells. VASH1 expression in endothelial cells has subsequently been reported to enhance cellular stress tolerance. Considering the importance of maintaining peritubular capillaries in preventing the progression of AKI, the present study aimed to examine whether VASH1 deletion is involved in the pathogenesis of cisplatin-induced AKI. For this, we injected male C57BL/6J wild-type (WT) and VASH1 heterozygous knockout (VASH1+/-) mice intraperitoneally with either 20 mg/kg cisplatin or vehicle solution. Seventy-two hours after cisplatin injection, increased serum creatinine concentrations and renal tubular injury accompanied by apoptosis and oxidative stress were more prominent in VASH1+/- mice than in WT mice. Cisplatin-induced peritubular capillary loss was also accelerated by VASH1 deficiency. Moreover, the increased expression of ICAM-1 in the peritubular capillaries of cisplatin-treated VASH1+/- mice was associated with a more marked infiltration of macrophages into the kidney. Taken together, VASH1 expression could have protective effects on cisplatin-induced AKI probably by maintaining the number and function of peritubular capillaries.

    DOI: 10.1152/ajprenal.00045.2019

    PubMed

    researchmap

  • Exogenous Vasohibin-2 Exacerbates Angiotensin II-Induced Ascending Aortic Dilation in Mice Reviewed

    Okuyama M, Uchida HA, Hada Y, Kakio Y, Otaka N, Umebayashi R, Tanabe K, Fujii Y, Kasahara S, Subramanian V, Daugherty A, Sato Y, Wada J

    Circulation reports   1 ( 4 )   155 - 161   2019.4

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:Japanese Circulation Society  

    DOI: 10.1253/circrep.cr-19-0008

    researchmap

  • Renal expression of trefoil factor 3 mRNA in association with tubulointerstitial fibrosis in IgA nephropathy. Reviewed International journal

    Tanaka K, Sugiyama H, Yamanari T, Mise K, Morinaga H, Kitagawa M, Onishi A, Ogawa-Akiyama A, Tanabe K, Eguchi J, Ohmoto Y, Shikata K, Wada J

    Nephrology (Carlton, Vic.)   23 ( 9 )   855 - 862   2018.9

     More details

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

    AIM: Trefoil factor 3 (TFF3) is a small peptide that is involved in mucosal protection. TFF3 is widely expressed in multiple tissues including kidney tissue. Previous studies have reported that the levels of urinary TFF3 are significantly increased in patients with chronic kidney disease. The aim of this study is to detect the TFF3 mRNA in kidney and elucidate the relationship between renal TFF3 mRNA and tubulointerstitial fibrosis in IgA nephropathy (IgAN). METHODS: We investigated the renal mRNA expression of TFF3 by real-time PCR analysis in biopsy specimens from patients with IgAN, other glomerulonephritis (OGN) and minor glomerular abnormalities (MGA). We also determined the renal localization of TFF3 and the levels of urinary TFF3 by immunostaining and ELISA, respectively. RESULTS: The renal TFF3 mRNA expression was significantly associated with the urinary TFF3 secretion and the tubulointerstitial fibrosis score in the IgAN group alone. Immunostaining of the renal specimen of IgAN patients revealed that TFF3 is located in the renal tubular epithelial cells. The locations were almost the same as those that showed uromodulin positivity; specifically, the thick ascending limb (TAL) of the loop of Henle and the early portion of the distal tubule. The urinary TFF3 levels were positively correlated with the levels of urinary biomarkers of tubulointerstitial injury in such patients. CONCLUSION: Renal TFF3 mRNA is associated with renal tubulointerstitial fibrosis in IgAN patients. The TFF3 located in the renal tubular epithelial cells may play a role in the progression of tubulointerstitial fibrosis in IgAN patients.

    DOI: 10.1111/nep.13444

    PubMed

    researchmap

  • Endogenous antiangiogenic factors in chronic kidney disease: Potential biomarkers of progression Reviewed

    Katsuyuki Tanabe, Yasufumi Sato, Jun Wada

    International Journal of Molecular Sciences   19 ( 7 )   1859   2018.7

     More details

    Language:English   Publisher:MDPI AG  

    Chronic kidney disease (CKD) is a major global health problem. Unless intensive intervention is initiated, some patients can rapidly progress to end-stage kidney disease. However, it is often difficult to predict renal outcomes using conventional laboratory tests in individuals with CKD. Therefore, many researchers have been searching for novel biomarkers to predict the progression of CKD. Angiogenesis is involved in physiological and pathological processes in the kidney and is regulated by the balance between a proangiogenic factor, vascular endothelial growth factor (VEGF)-A, and various endogenous antiangiogenic factors. In recent reports using genetically engineered mice, the roles of these antiangiogenic factors in the pathogenesis of kidney disease have become increasingly clear. In addition, recent clinical studies have demonstrated associations between circulating levels of antiangiogenic factors and renal dysfunction in CKD patients. In this review, we summarize recent advances in the study of representative endogenous antiangiogenic factors, including soluble fms-related tyrosine kinase 1, soluble endoglin, pigment epithelium-derived factor, VEGF-A165 b, endostatin, and vasohibin-1, in associations with kidney diseases and discuss their predictive potentials as biomarkers of progression of CKD.

    DOI: 10.3390/ijms19071859

    Scopus

    PubMed

    researchmap

  • Anti-MuSK Antibody-positive Myasthenia Gravis Successfully Treated with Outpatient Periodic Weekly Blood Purification Therapy. Reviewed

    Kentaro Deguchi, Kosuke Matsuzono, Yumiko Nakano, Syoichiro Kono, Kota Sato, Shoko Deguchi, Katsuyuki Tanabe, Nozomi Hishikawa, Yasuyuki Ota, Toru Yamashita, Kiyoe Ohta, Masakatsu Motomura, Koji Abe

    Internal medicine (Tokyo, Japan)   57 ( 10 )   1455 - 1458   2018.5

     More details

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

    A 37-year-old man with anti-muscle-specific tyrosine kinase (MuSK) antibody-positive myasthenia gravis (MG) presented with subacute progressive dysphagia and muscle weakness of the neck and bilateral upper extremities. Conventional immune-suppressive treatments and high-dose intravenous immunoglobulin were ineffective. He then displayed repeated exacerbations and remissions over the course of two years, despite two to four sessions of plasma exchange (PE) every two months. The patient was successfully treated with outpatient periodic weekly blood purification therapy with alternative PE and double-filtration plasmapheresis using an internal shunt. This case report suggests the benefits of blood purification therapy with an internal shunt against anti-MuSK antibody-positive MG.

    DOI: 10.2169/internalmedicine.9466-17

    PubMed

    researchmap

  • Estrogen-related receptor α is essential for maintaining mitochondrial integrity in cisplatin-induced acute kidney injury Reviewed

    Keigo Tsushida, Katsuyuki Tanabe, Kana Masuda, Satoshi Tanimura, Hiromasa Miyake, Yuka Arata, Hitoshi Sugiyama, Jun Wada

    Biochemical and Biophysical Research Communications   498 ( 4 )   918 - 924   2018.4

     More details

    Authorship:Corresponding author   Language:English   Publishing type:Research paper (scientific journal)   Publisher:Elsevier B.V.  

    Acute kidney injury (AKI) has been associated with not only higher in-hospital mortality but also the subsequent development of chronic kidney disease (CKD). Recent evidence has suggested the involvement of mitochondrial dysfunction and impaired dynamics in the pathogenesis of AKI. Estrogen-related receptor α (ERRα) is an orphan nuclear receptor that acts as a transcription factor to regulate the transcription of genes required for mitochondrial biogenesis and oxidative phosphorylation. In the present study, we examined the effects of ERRα deficiency on the progression of AKI induced by cisplatin. Male C57BL/6 J wild-type and ERRα−/- mice received a single intraperitoneal injection of 20 mg/kg cisplatin. Seventy-two hours after the injection, kidney function and morphology were evaluated. ERRα expression was observed in renal tubules, and cisplatin inhibited its translocation into nuclei. ERRα deficiency exacerbated cisplatin-induced renal dysfunction and tubular injury, as well as oxidative stress and apoptosis. ERRα−/- mice kidneys revealed lower mitochondrial DNA content and swollen mitochondria with reduced cristae. In addition, these mice had lower expression of the mitochondrial fusion protein mitofusin-2. The cisplatin-induced decrease in mitochondrial DNA and altered mitochondrial structure were more severe in ERRα−/- mice. In cultured mouse proximal tubular epithelial cells, the ERRα inverse agonist XCT-790 significantly inhibited mitofusin-2 expression and induced mitochondrial fragmentation. Taken together, our findings suggest the involvement of ERRα in the progression of cisplatin-induced AKI probably through impaired mitochondrial dynamics.

    DOI: 10.1016/j.bbrc.2018.03.080

    Scopus

    PubMed

    researchmap

  • Deletion of pro-angiogenic factor vasohibin-2 ameliorates glomerular alterations in a mouse diabetic nephropathy model Reviewed

    Kana Masuda, Katsuyuki Tanabe, Haruyo Ujike, Norikazu Hinamoto, Hiromasa Miyake, Satoshi Tanimura, Hitoshi Sugiyama, Yasufumi Sato, Yohei Maeshima, Jun Wada

    PLoS ONE   13 ( 4 )   e0195779   2018.4

     More details

    Authorship:Corresponding author   Language:English   Publishing type:Research paper (scientific journal)   Publisher:Public Library of Science  

    Angiogenesis has been implicated in glomerular alterations in the early stage of diabetic nephropathy. We previously reported the renoprotective effects of vasohibin-1 (VASH1), which is a novel angiogenesis inhibitor derived from endothelial cells, on diabetic nephropathy progression. Vasohibin-2 (VASH2) was originally identified as a VASH1 homolog and possesses pro-angiogenic activity in contrast to VASH1. In addition, VASH2 was recently shown to promote epithelial-to-mesenchymal transition via enhanced transforming growth factor (TGF)-β signaling in cancer cells. Herein, we investigated the pathogenic roles of VASH2 in diabetic nephropathy using VAHS2-deficient mice. The type 1 diabetes model was induced by intraperitoneal injections of streptozoto-cin in VASH2 homozygous knockout (VASH2LacZ/LacZ) or wild-type mice. These mice were euthanized 16 weeks after inducing hyperglycemia. Increased urine albumin excretion and creatinine clearance observed in diabetic wild-type mice were significantly prevented in diabetic VASH2-deficient mice. Accordingly, diabetes-induced increase in glomerular volume and reduction in glomerular slit-diaphragm density were significantly improved in VASH2 knockout mice. Increased glomerular endothelial area was also suppressed in VASH2-deficient mice, in association with inhibition of enhanced vascular endothelial growth factor (VEGF) receptor 2 (VEGFR2), but not VEGF level. Furthermore, glomerular accumulation of mesangial matrix, including type IV collagen, and increased expression of TGF-β were improved in diabetic VASH2 knockout mice compared with diabetic wild-type mice. Based on the immunofluorescence findings, endogenous VASH2 localization in glomeruli was consistent with mesangial cells. Human mesangial cells (HMCs) were cultured under high glucose condition in in vitro experiments. Transfection of VASH2 small interfering RNA (siRNA) into the HMCs resulted in the suppression of type IV collagen production induced by high glucose compared with control siRNA. These results indicate that VASH2 may be involved in diabetes-induced glomerular alterations, particularly impaired filtration barrier and mesangial expansion. Therefore, VASH2 is likely to represent a promising therapeutic target for diabetic nephropathy.

    DOI: 10.1371/journal.pone.0195779

    Scopus

    PubMed

    researchmap

  • Primary peritoneal carcinosarcoma in a dialysis patient Reviewed

    Keiko Tanaka, Katsuyuki Tanabe, Naoko Nishii, Kana Masuda, Yuka Arata, Akifumi Ohnishi, Masaru Kinomura, Hitoshi Sugiyama, Jun Wada

    NEPHROLOGY   22 ( 11 )   925 - 925   2017.11

     More details

    Authorship:Corresponding author   Language:English   Publisher:WILEY  

    DOI: 10.1111/nep.12973

    Web of Science

    PubMed

    researchmap

  • Immunohistochemistry of Vasohibin-2 in Human Kidney Disease: Implications in Impaired Glucose Tolerance and Reduced Renal Function Reviewed

    Yuka Arata, Katsuyuki Tanabe, Norikazu Hinamoto, Hiroko Yamasaki, Hitoshi Sugiyama, Yohei Maeshima, Naoki Kanomata, Yasufumi Sato, Jun Wada

    ACTA MEDICA OKAYAMA   71 ( 5 )   369 - 380   2017.10

     More details

    Authorship:Corresponding author   Language:English   Publishing type:Research paper (scientific journal)   Publisher:OKAYAMA UNIV MED SCHOOL  

    Several angiogenesis-related factors are known to play important roles in the pathogenesis of kidney disease. Vasohibin-2 (VASH-2) was recently reported as a novel proangiogenic factor. Although VASH-2 was demonstrated to accelerate tumor angiogenesis, its roles in non-tumor processes including renal disease have not been well elucidated yet. Here, we performed a retrospective study including an immunohistochemical analysis of human kidney biopsy specimens from 82 Japanese patients with a variety of kidney diseases, and we evaluated the correlations between the immunoreactivity of VASH-2 and the patients' clinicopathological parameters. VASH-2 immunoreactivity was detected in varying degrees in renal tubules as well as in peritubular capillaries and vasa recta. The cortical and medullary tubule VASH-2(+) scores were correlated with the presence of hypertension, and the medullary tubule VASH-2(+) score was significantly correlated with the blood glucose (p=0.029, r=0.35) and hemoglobin A1c levels (p=0.0066, r=0.39). Moreover, decreased VASH-2(+) scores in the vasa recta were associated with reduced renal function (p=0.0003). These results suggest that VASH-2 could play an important role in the pathogenesis of renal diseases, and that VASH-2 is closely associated with hypertension and impaired glucose tolerance.

    DOI: 10.18926/AMO/55434

    Web of Science

    PubMed

    researchmap

  • An angiotensin II type 1 receptor binding molecule has a critical role in hypertension in a chronic kidney disease model Reviewed

    Ryu Kobayashi, Hiromichi Wakui, Kengo Azushima, Kazushi Uneda, Sona Haku, Kohji Ohki, Kotaro Haruhara, Sho Kinguchi, Miyuki Matsuda, Masato Ohsawa, Yoshiyuki Toya, Akira Nishiyama, Akio Yamashita, Katsuyuki Tanabe, Yohei Maeshima, Satoshi Umemura, Kouichi Tamura

    KIDNEY INTERNATIONAL   91 ( 5 )   1115 - 1125   2017.5

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ELSEVIER SCIENCE INC  

    Angiotensin II type 1 receptor-associated protein (ATRAP) promotes AT1R internalization along with suppression of hyperactivation of tissue AT1R signaling. Here, we provide evidence that renal ATRAP plays a critical role in suppressing hypertension in a mouse remnant kidney model of chronic kidney disease. The effect of 5/6 nephrectomy on endogenous ATRAP expression was examined in the kidney of C57BL/6 and 129/Sv mice. While 129/Sv mice with a remnant kidney showed decreased renal ATRAP expression and developed hypertension, C57BL/6 mice exhibited increased renal ATRAP expression and resistance to progressive hypertension. Consequently, we hypothesized that downregulation of renal ATRAP expression is involved in pathogenesis of hypertension in the remnant kidney model of chronic kidney disease. Interestingly, 5/6 nephrectomy in ATRAP-knockout mice on the hypertension resistant C57BL/6 background caused hypertension with increased plasma volume. Moreover, in knockout compared to wild-type C57BL/6 mice after 5/6 nephrectomy, renal expression of the epithelial sodium channel cc-subunit and tumor necrosis factor-alpha was significantly enhanced, concomitant with increased plasma membrane angiotensin II type 1 receptor in the kidneys. Thus, renal ATRAP downregulation is involved in the onset and progression of blood pressure elevation caused by renal mass reduction, and implicates ATRAP as a therapeutic target for hypertension in chronic kidney disease.

    DOI: 10.1016/j.kint.2016.10.035

    Web of Science

    PubMed

    researchmap

  • Antiangiogenic Therapy for Diabetic Nephropathy Reviewed

    Katsuyuki Tanabe, Yohei Maeshima, Yasufumi Sato, Jun Wada

    BIOMED RESEARCH INTERNATIONAL   2017   5724069   2017

     More details

    Authorship:Lead author, Corresponding author   Language:English   Publisher:HINDAWI LTD  

    Angiogenesis has been shown to be a potential therapeutic target for early stages of diabetic nephropathy in a number of animal experiments. Vascular endothelial growth factor (VEGF) is the main mediator for abnormal angiogenesis in diabetic glomeruli. Although beneficial effects of anti-VEGF antibodies have previously been demonstrated in diabetic animal experiments, recent basic and clinical evidence has revealed that the blockade of VEGF signaling resulted in proteinuria and renal thrombotic microangiopathy, suggesting the importance of maintaining normal levels of VEGF in the kidneys. Therefore, antiangiogenic therapy for diabetic nephropathy should eliminate excessive glomerular angiogenic response without accelerating endothelial injury. Some endogenous antiangiogenic factors such as endostatin and tumstatin inhibit overactivation of endothelial cells but do not specifically block VEGF signaling. In addition, the novel endothelium-derived antiangiogenic factor vasohibin-1 enhances stress tolerance and survival of the endothelial cells, while inhibiting excess angiogenesis. These factors have been demonstrated to suppress albuminuria and glomerular alterations in a diabetic mouse model. Thus, antiangiogenic therapy with promising candidates will possibly improve renal prognosis in patients with early stages of diabetic nephropathy.

    DOI: 10.1155/2017/5724069

    Web of Science

    PubMed

    researchmap

  • Sustained Tubulointerstitial Inflammation in Kidney with Severe Leptospirosis Reviewed

    Keiko Tanaka, Katsuyuki Tanabe, Naoko Nishii, Keiichi Takiue, Hitoshi Sugiyama, Jun Wada

    INTERNAL MEDICINE   56 ( 10 )   1179 - 1184   2017

     More details

    Authorship:Corresponding author   Language:English   Publishing type:Research paper (scientific journal)   Publisher:JAPAN SOC INTERNAL MEDICINE  

    Leptospirosis is frequently associated with acute kidney injury. Some survivors are known to progress to chronic kidney disease due to sustained tubulointerstitial inflammation. We present a case of severe leptospirosis with acute renal failure. Although antibiotic therapy resolved the infection, moderate renal dysfunction remained. A renal biopsy demonstrated marked inflammatory infiltration in the tubules and interstitium. Many of the inflammatory cells were CD68-positive monocytes/macrophages, predominantly M1 phenotype. An intermediate dose of oral corticosteroids normalized the patient's serum creatinine levels. We suggest that corticosteroid therapy may be a therapeutic option for some patients with sustained tubulointerstitial nephritis who survive severe leptospirosis.

    DOI: 10.2169/internalmedicine.56.8084

    Web of Science

    PubMed

    researchmap

  • The Efficacy of Rituximab in High-risk Renal Transplant Recipients Reviewed

    Motoo Araki, Koichiro Wada, Yosuke Mitsui, Risa Kubota, Takashi Yoshioka, Yuichi Ariyoshi, Yasuyuki Kobayashi, Masashi Kitagawa, Katsuyuki Tanabe, Hiroshi Sugiyama, Jun Wada, Masami Watanabe, Toyohiko Watanabe, Katsuyuki Hotta, Yasutomo Nasu

    ACTA MEDICA OKAYAMA   70 ( 4 )   295 - 297   2016.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OKAYAMA UNIV MED SCHOOL  

    Although graft survival following renal transplantation (RTx) has improved, outcomes following highrisk RTx are variable. Preexisting antibodies, including donor-specific antibodies (DSA), play an important role in graft dysfunction and survival. We have designed a study to investigate the safety and efficacy of anti-CD20 monoclonal antibodies (rituximab) in high-risk RTx recipients. Major eligibility criteria include: 1) major and minor ABO blood group mismatch, 2) positive DSA. Thirty-five patients will receive 200 mg/body of rituximab. The primary endpoint is the incidence of B cell depletion. This study will clarify whether rituximab is efficacious in improving graft survival in high-risk RTx recipients.

    DOI: 10.18926/AMO/54507

    Web of Science

    PubMed

    researchmap

  • 長期透析患者に対する腎移植症例の検討 Reviewed

    有吉勇一, 荒木元朗, 光井洋介, 吉岡貴史, 和田耕一郎, 小林泰之, 江原伸, 渡邉豊彦, 那須保友, 山下里美, 北川正史, 田邊克幸, 森永裕士, 杉山斉, 和田淳

    日本臨床腎移植学会雑誌   4 ( 1 )   113 - 117   2016.7

     More details

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

    researchmap

  • The urinary levels of prostanoid metabolites predict acute kidney injury in heterogeneous adult Japanese ICU patients: a prospective observational study Reviewed

    Haruyo Ujike-Omori, Yohei Maeshima, Masaru Kinomura, Katsuyuki Tanabe, Kiyoshi Mori, Hiroyuki Watatani, Norikazu Hinamoto, Hitoshi Sugiyama, Yoshiki Sakai, Hiroshi Morimatsu, Hirofumi Makino

    CLINICAL AND EXPERIMENTAL NEPHROLOGY   19 ( 6 )   1024 - 1036   2015.12

     More details

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

    Background Acute kidney injury (AKI) is frequently observed in critically ill patients in the intensive care unit (ICU) and is associated with increased mortality. Prostanoids regulate numerous biological functions, including hemodynamics and renal tubular transport. We herein investigated the ability of urinary prostanoid metabolites to predict the onset of AKI in critically ill adult patients.
    Methods The current study was conducted as a prospective observational study. Urine of patients admitted to the ICU at Okayama University Hospital was collected and the urinary levels of prostaglandin E-2 (PGE(2)), PGI(2) metabolite (2,3-dinor-6-OXO-PGF(1 alpha)), thromboxane A(2) (TXA(2)) metabolite (11-dehydro-TXB2) were determined.
    Results Of the 93 patients, 24 developed AKI (AKIN criteria). Surgical intervention (93, 75 %) was the leading cause of ICU admission. Overall, the ratio of the level of serum Cr on Day 1 after ICU admission to that observed at baseline positively correlated with the urinary 2,3-dinor-6-OXO-PGF(1 alpha)/Cr (r = 0.57, p &lt; 0.0001) and 11-dehydro-TXB2/Cr (r = 0.47, p &lt; 0.0001) ratios. In 16 cases of de novo AKI, the urinary 2,3-dinor-6-OXO-PGF(1 alpha)/Cr and 11-dehydro-TXB2/Cr values were significantly elevated compared with that observed in the non-AKI group, whereas the urinary PGE(2)/Cr values were not. The urinary 2,3-dinor-6-OXO-PGF(1 alpha)/Cr ratio exhibited the best diagnostic and predictive performance among the prostanoid metabolites according to the receiver operating characteristic (ROC) analysis [ROC-area under the curve (AUC): 0.75].
    Conclusions Taken together, these results demonstrate that the urinary 2,3-dinor-6-OXO-PGF(1 alpha)/Cr and 11-dehydro-TXB2/Cr ratios are associated with the subsequent onset of AKI and poor outcomes in adult heterogeneous ICU patients.

    DOI: 10.1007/s10157-015-1092-4

    Web of Science

    PubMed

    researchmap

  • ONO-1301, a Sustained-Release Prostacyclin Analog, Ameliorates the Renal Alterations in a Mouse Type 2 Diabetes Model Possibly Through Its Protective Effects on Mesangial Cells Reviewed

    Hiroyuki Watatani, Hiroko Yamasaki, Yohei Maeshima, Tatsuyo Nasu, Norikazu Hinamoto, Haruyo Ujike, Hitoshi Sugiyama, Yoshiki Sakai, Katsuyuki Tanabe, Hirofumi Makino

    ACTA MEDICA OKAYAMA   69 ( 1 )   1 - 15   2015.2

     More details

    Authorship:Corresponding author   Language:English   Publishing type:Research paper (scientific journal)   Publisher:OKAYAMA UNIV MED SCHOOL  

    Diabetic nephropathy is the most common pathological disorder predisposing patients to end-stage renal disease. Considering the increasing prevalence of type 2 diabetes mellitus worldwide, novel therapeutic approaches are urgently needed. ONO-1301 is a novel sustained-release prostacyclin analog that inhibits thromboxane A(2) synthase. Here we examined the therapeutic effects of the intermittent administration of slow-release ONO-1301 (SR-ONO) on diabetic nephropathy in obese type 2 diabetes mice, as well as its direct effects on mesangial cells. The subcutaneous injection of SR-ONO (3mg/kg) every 3 wks did not affect the obesity or hyperglycemia in the db/db obese mice used as a model of type 2 diabetes, but it significantly ameliorated their albuminuria, glomerular hypertrophy, glomerular accumulation of type IV collagen, and monocyte/macrophage infiltration, and also the increase of TGF-beta 1, a-smooth muscle actin (alpha-SMA) and MCP-1 compared to vehicle treatment. In cultured mouse mesangial cells, ONO-1301 concentration-dependently suppressed the increases in TGF-beta, type IV collagen, alpha-SMA, MCP-1 and fibronectin induced by high ambient glucose, at least partly through prostacyclin (PGI(2)) receptor-mediated signaling. Taken together, these results suggest the potential therapeutic efficacy of the intermittent administration of SR-ONO against type 2 diabetic nephropathy, possibly through protective effects on mesangial cells.

    DOI: 10.18926/AMO/53117

    Web of Science

    PubMed

    researchmap

  • Endogenous Fructose Production and Fructokinase Activation Mediate Renal Injury in Diabetic Nephropathy Reviewed

    Miguel A. Lanaspa, Takuji Ishimoto, Christina Cicerchi, Yoshifuru Tamura, Carlos A. Roncal-Jimenez, Wei Chen, Katsuyuki Tanabe, Ana Andres-Hernando, David J. Orlicky, Esteban Finol, Shinichiro Inaba, Nanxing Li, Christopher J. Rivard, Tomoki Kosugi, Laura G. Sanchez-Lozada, J. Mark Petrash, Yuri Y. Sautin, A. Ahsan Ejaz, Wataru Kitagawa, Gabriela E. Garcia, David T. Bonthron, Aruna Asipu, Christine P. Diggle, Bernardo Rodriguez-Iturbe, Takahiko Nakagawa, Richard J. Johnson

    JOURNAL OF THE AMERICAN SOCIETY OF NEPHROLOGY   25 ( 11 )   2526 - 2538   2014.11

     More details

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

    Diabetes is associated with activation of the polyol pathway, in which glucose is converted to sorbitol by aldose reductase. Previous studies focused on the role of sorbitol in mediating diabetic complications. However, in the proximal tubule, sorbitol can be converted to fructose, which is then metabolized largely by fructokinase, also known as ketohexokinase, leading to ATP depletion, proinflammatory cytokine expression, and oxidative stress. We and others recently identified a potential deleterious role of dietary fructose in the generation of tubulointerstitial injury and the acceleration of CKD. In this study, we investigated the potential role of endogenous fructose production, as opposed to dietary fructose, and its metabolism through fructokinase in the development of diabetic nephropathy. Wild-type mice with streptozotocin-induced diabetes developed proteinuria, reduced GFR, and renal glomerular and proximal tubular injury. Increased renal expression of aldose reductase; elevated levels of renal sorbitol, fructose, and uric acid; and low levels of ATP confirmed activation of the fructokinase pathway. Furthermore, renal expression of inflammatory cytokines with macrophage infiltration was prominent. In contrast, diabetic fructokinase-deficient mice demonstrated significantly less proteinuria, renal dysfunction, renal injury, and inflammation. These studies identify fructokinase as a novel mediator of diabetic nephropathy and document a novel role for endogenous fructose production, or fructoneogenesis, in driving renal disease.

    DOI: 10.1681/ASN.2013080901

    Web of Science

    PubMed

    researchmap

  • Exacerbation of Diabetic Renal Alterations in Mice Lacking Vasohibin-1 Reviewed

    Norikazu Hinamoto, Yohei Maeshima, Hiroko Yamasaki, Tatsuyo Nasu, Daisuke Saito, Hiroyuki Watatani, Haruyo Ujike, Katsuyuki Tanabe, Kana Masuda, Yuka Arata, Hitoshi Sugiyama, Yasufumi Sato, Hirofumi Makino

    PLOS ONE   9 ( 9 )   e107934   2014.9

     More details

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

    Vasohibin-1 (VASH1) is a unique endogenous inhibitor of angiogenesis that is induced in endothelial cells by pro-angiogenic factors. We previously reported renoprotective effect of adenoviral delivery of VASH1 in diabetic nephropathy model, and herein investigated the potential protective role of endogenous VASH1 by using VASH1-deficient mice. Streptozotocininduced type 1 diabetic VASH1 heterozygous knockout mice (VASH1(+/-)) or wild-type diabetic mice were sacrificed 16 weeks after inducing diabetes. In the diabetic VASH1(+/-) mice, albuminuria were significantly exacerbated compared with the diabetic wild-type littermates, in association with the dysregulated distribution of glomerular slit diaphragm related proteins, nephrin and ZO-1, glomerular basement membrane thickning and reduction of slit diaphragm density. Glomerular monocyte/macrophage infiltration and glomerular nuclear translocation of phosphorylated NF-kappa B p65 were significantly exacerbated in the diabetic VASH1(+/-) mice compared with the diabetic wild-type littermates, accompanied by the augmentation of VEGF-A, M1 macrophage-derived MCP-1 and phosphorylation of I kappa B alpha, and the decrease of angiopoietin-1/2 ratio and M2 macrophage-derived Arginase-1. The glomerular CD31(+) endothelial area was also increased in the diabetic VASH1(+/-) mice compared with the diabetic-wild type littermates. Furthermore, the renal and glomerular hypertrophy, glomerular accumulation of mesangial matrix and type IV collagen and activation of renal TGF-beta(1)/Smad3 signaling, a key mediator of renal fibrosis, were exacerbated in the diabetic VASH1(+/-) mice compared with the diabetic wild-type littermates. In conditionally immortalized mouse podocytes cultured under high glucose condition, transfection of VASH1 small interfering RNA (siRNA) resulted in the reduction of nephrin, angiopoietin-1 and ZO-1, and the augmentation of VEGF-A compared with control siRNA. These results suggest that endogenous VASH1 may regulate the development of diabetic renal alterations, partly via direct effects on podocytes, and thus, a strategy to recover VASH1 might potentially lead to the development of a novel therapeutic approach for diabetic nephropathy.

    DOI: 10.1371/journal.pone.0107934

    Web of Science

    PubMed

    researchmap

  • Uric acid-dependent inhibition of AMP kinase induces hepatic glucose production in diabetes and starvation: evolutionary implications of the uricase loss in hominids Reviewed

    Christina Cicerchi, Nanxing Li, James Kratzer, Gabriela Garcia, Carlos A. Roncal-Jimenez, Katsuyuki Tanabe, Brandi Hunter, Christopher J. Rivard, Yuri Y. Sautin, Eric A. Gaucher, Richard J. Johnson, Miguel A. Lanaspa

    FASEB JOURNAL   28 ( 8 )   3339 - 3350   2014.8

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:FEDERATION AMER SOC EXP BIOL  

    Reduced AMP kinase (AMPK) activity has been shown to play a key deleterious role in increased hepatic gluconeogenesis in diabetes, but the mechanism whereby this occurs remains unclear. In this article, we document that another AMP-dependent enzyme, AMP deaminase (AMPD) is activated in the liver of diabetic mice, which parallels with a significant reduction in AMPK activity and a significant increase in intracellular glucose accumulation in human HepG2 cells. AMPD activation is induced by a reduction in intracellular phosphate levels, which is characteristic of insulin resistance and diabetic states. Increased gluconeogenesis is mediated by reduced TORC2 phosphorylation at Ser171 by AMPK in these cells, as well as by the up-regulation of the rate-limiting enzymes PEPCK and G6Pc. The mechanism whereby AMPD controls AMPK activation depends on the production of a specific AMP downstream metabolite through AMPD, uric acid. In this regard, humans have higher uric acid levels than most mammals due to a mutation in uricase, the enzyme involved in uric acid degradation in most mammals, that developed during a period of famine in Europe 1.5 x 10(7) yr ago. Here, working with resurrected ancestral uricases obtained from early hominids, we show that their expression on HepG2 cells is enough to blunt gluconeogenesis in parallel with an up-regulation of AMPK activity. These studies identify a key role AMPD and uric acid in mediating hepatic gluconeogenesis in the diabetic state, via a mechanism involving AMPK down-regulation and overexpression of PEPCK and G6Pc. The uricase mutation in the Miocene likely provided a survival advantage to help maintain glucose levels under condi-tions of near starvation, but today likely has a role in the pathogenesis of diabetes.

    DOI: 10.1096/fj.13-243634

    Web of Science

    PubMed

    researchmap

  • Urinary and Plasma Levels of Vasohibin-1 Can Predict Renal Functional Deterioration in Patients with Renal Disorders Reviewed

    Norikazu Hinamoto, Yohei Maeshima, Daisuke Saito, Hiroko Yamasaki, Katsuyuki Tanabe, Tatsuyo Nasu, Hiroyuki Watatani, Haruyo Ujike, Masaru Kinomura, Hitoshi Sugiyama, Hikaru Sonoda, Yasufumi Sato, Hirofumi Makino

    PLOS ONE   9 ( 6 )   e96932   2014.6

     More details

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

    Vasohibin-1 (VASH-1) is a negative feedback regulator of angiogenesis, and a small vasohibin-binding protein (SVBP) serves as its secretory chaperone and contributes to its antiangiogenic effects. In the present study, we aimed to define the clinical significance of VASH-1 and SVBP in patients with chronic kidney disease (CKD). We recruited 67 Japanese hospitalized patients with renal disorders with (n = 45) or without (n = 22) renal biopsy samples and 10 Japanese healthy controls. We evaluated the correlations between the plasma and urinary levels of VASH-1/VASH-1-SVBP complex/SVBP and the clinicopathological parameters. The plasma levels of VASH-1 were inversely correlated with age and systolic and diastolic blood pressure and positively correlated with crescent formation. Increased plasma and urinary levels of VASH-1 and VASH-1-SVBP complex were significantly correlated with worse renal outcomes. These results demonstrate an association between elevated urinary and plasma levels of VASH-1 and progressive decline of the renal function, thus suggesting a potential role for VASH-1 in predicting a worse renal prognosis in patients with renal disease, including CKD.

    DOI: 10.1371/journal.pone.0096932

    Web of Science

    PubMed

    researchmap

  • Renal distribution of Vasohibin-1 in patients with chronic kidney disease Reviewed

    Norikazu Hinamoto, Yohei Maeshima, Daisuke Saito, Hiroko Yamasakr, Katsuyuki Tanabe, Tatsuyo Nasu, Hiroyuki Watatani, Haruyo Ujike, Masaru Kinomura, Hitoshi Sugiyama, Hikaru Sonoda, Naoki Kanomata, Yasufumi Sate, Hirofumi Makino

    Acta Medica Okayama   68 ( 4 )   219 - 233   2014

     More details

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

    Experimental studies have demonstrated the involvement of angiogenesis-related factors in the progression of chronic kidney disease (CKD). There have so far been no reports investigating the distribution and clinical roles of Vasohibin-1 (VASH-1), a negative feedback regulator of angiogenesis, in CKD. We recruited 54 Japanese CKD patients and 6 patients who had normal renal tissues excised due to localized renal cell carcinoma. We evaluated the correlations between the renal expression level of VASH-1 and the clinical/histological parameters. VASH-1 was observed in renal endothelial/mesangial cells, crescentic lesions and interstitial inflammatory cells. Significant positive correlations were observed between 1) crescent formation and the number of VASH-1+ cells in the glomerulus (r=0.48, /&gt
    = 0.001) or cortex (r = 0.64, p&lt
    0.0001), 2) interstitial cell infiltration and the number of VASH-1+ cells in the cortex (r = 0.34, p = 0.02), 3) the glomerular VEGFR-2+ area and the number of VASH 1+ cells in the glomerulus (r = 0.44, p = 0.01) or medulla (r = 0.63, p = 0.01). These results suggest that the renal levels of VASH-1 may be affected by local inflammation, crescentic lesions and VEGFR-2. © 2014 by Okayama University Medical School.

    DOI: 10.18926/AMO/52788

    Scopus

    PubMed

    researchmap

  • Vasohibin-1 deficiency enhances renal fibrosis and inflammation after unilateral ureteral obstruction Reviewed

    Hiroyuki Watatani, Yohei Maeshima, Norikazu Hinamoto, Hiroko Yamasaki, Haruyo Ujike, Katsuyuki Tanabe, Hitoshi Sugiyama, Fumio Otsuka, Yasufumi Sato, Hirofumi Makino

    Physiological Reports   2 ( 6 )   2014

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:American Physiological Society  

    Tubulointerstitial injuries are known to predict the deterioration of renal function in chronic kidney disease (CKD). We recently reported the protective role of Vasohibin-1(VASH-1), a negative feedback regulator of angiogenesis, in diabetic nephropathy, but its impact on tubulointerstitial injuries remains to be elucidated. In the present study, we evaluated the role of endogenous VASH-1 in regulating the tubulointerstitial alterations induced by unilateral ureteral obstruction (UUO), and assessed its role on fibrogenesis and the activation of Smad3 signaling in renal fibroblasts. UUO was induced in female Vasohibin-1 heterozygous knockout mice (VASH-1+/-) or wild-type (WT) (VASH-1+/+) littermates. Mice were sacrificed on Day 7 after left ureter ligation, and the kidney tissue was obtained. Interstitial fibrosis, the accumulation of type I and type III collagen and monocytes/macrophages infiltration in the obstructed kidneys (OBK) were significantly exacerbated in VASH-1+/- mice compared with WT mice (Day 7). The increases in the renal levels of TGF-β1, pSmad3, NF-jB pp65, CCL2 mRNA, and the number of interstitial fibroblast-specific protein-1 (FSP-1)+ fibroblasts in the OBK were significantly aggravated in VASH-1+/- mice. In addition, treatment with VASH-1 siRNA enhanced the TGF-β1-induced phosphorylation of Smad3, the transcriptional activation of the Smad3 pathway and the production of type I/type III collagen in fibroblasts, in vitro. Taken together, our findings demonstrate a protective role for endogenous VASH-1 on tubulointerstitial alterations via its regulation of inflammation and fibrosis and also show the direct anti-fibrotic effects of VASH-1 on renal fibroblasts through its modulation of TGF-β1 signaling.

    DOI: 10.14814/phy2.12054

    Scopus

    PubMed

    researchmap

  • Umami: The Taste That Drives Purine Intake Reviewed

    Richard J. Johnson, Takahiko Nakagawa, L. Gabriela Sanchez-Lozada, Miguel A. Lanaspa, Yoshifuru Tamura, Katsuyuki Tanabe, Takuji Ishimoto, Jeffrey Thomas, Shinichiro Inaba, Wataru Kitagawa, Christopher J. Rivard

    JOURNAL OF RHEUMATOLOGY   40 ( 11 )   1794 - 1796   2013.11

     More details

    Language:English   Publisher:J RHEUMATOL PUBL CO  

    DOI: 10.3899/jrheum.130531

    Web of Science

    PubMed

    researchmap

  • Epicatechin limits renal injury by mitochondrial protection in cisplatin nephropathy Reviewed

    Katsuyuki Tanabe, Yoshifuru Tamura, Miguel A. Lanaspa, Makoto Miyazaki, Norihiko Suzuki, Waichi Sato, Yohei Maeshima, George F. Schreiner, Francisco J. Villarreal, Richard J. Johnson, Takahiko Nakagawa

    American Journal of Physiology - Renal Physiology   303 ( 9 )   F1264 - F1274   2012.11

     More details

    Authorship:Lead author   Language:English   Publishing type:Research paper (scientific journal)  

    Cisplatin nephropathy can be regarded as a mitochondrial disease. Intervention to halt such deleterious injury is under investigation. Recently, the flavanol (-)-epicatechin emerges as a novel compound to protect the cardiovascular system, owing in part to mitochondrial protection. Here, we have hypothesized that epicatechin prevents the progression of cisplatininduced kidney injury by protecting mitochondria. Epicatechin was administered 8 h after cisplatin injury was induced in the mouse kidney. Cisplatin significantly induced renal dysfunction and tubular injury along with an increase in oxidative stress. Mitochondrial damages were also evident as a decrease in loss of mitochondrial mass with a reduction in the oxidative phosphorylation complexes and low levels of MnSOD. The renal damages and mitochondrial injuries were significantly prevented by epicatechin treatment. Consistent with these observations, an in vitro study using cultured mouse proximal tubular cells demonstrated that cisplatin-induced mitochondrial injury, as revealed by a decrease in mitochondrial succinate dehydrogenase activity, an induction of cytochrome c release, mitochondrial fragmentation, and a reduction in complex IV protein, was prevented by epicatechin. Such a protective effect of epicatechin might be attributed to decreased oxidative stress and reduced ERK activity. Finally, we confirmed that epicatechin did not perturb the anticancer effect of cisplatin in HeLa cells. In conclusion, epicatechin exhibits protective effects due in part to its ability to prevent the progression of mitochondrial injury in mouse cisplatin nephropathy. Epicatechin may be a novel option to treat renal disorders associated with mitochondrial dysfunction. © 2012 the American Physiological Society.

    DOI: 10.1152/ajprenal.00227.2012

    Scopus

    PubMed

    researchmap

  • Nicorandil, a K atp channel opener, alleviates chronic renal injury by targeting podocytes and macrophages Reviewed

    Yoshifuru Tamura, Katsuyuki Tanabe, Wataru Kitagawa, Shunya Uchida, George F. Schreiner, Richard J. Johnson, Takahiko Nakagawa

    American Journal of Physiology - Renal Physiology   303 ( 3 )   F339 - F349   2012.8

     More details

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

    Nicorandil exhibits a protective effect in the vascular system, which is thought to be due to vasodilatation from opening ATP-dependent potassium channels and donation of nitric oxide. Recently, nicorandil was shown to be renoprotective in models of acute kidney injury and glomerulone-phritis. However, the specific mechanisms of renoprotection are unclear. We evaluated the effect of nicorandil on the rat remnant kidney model of chronic kidney disease. Blood pressure was unchanged by a 10-wk course of nicorandil, while albuminuria was significantly reduced. Glomerular injury and tubulointerstitial injury were also ameliorated by nicorandil. Oxidative stress, as noted by renal nitrotyrosine level and urine 8-hydroxy-2′-deoxyguanosine, were elevated in this model and was significantly reduced by nic-orandil treatment. Treatment was associated with maintenance of the mitochondrial antioxidant, manganese SOD, in podocytes and with suppression of xanthine oxidase expression in infiltrating macro-phages. Interestingly, these two cell types express sulfonylurea receptor 2 (SUR2), a binding site of nicorandil in the ATP-dependent K channel. Consistently, we found that stimulating SUR2 with nic-orandil prevented angiotensin II-mediated upregulation of xanthine oxidase in the cultured macrophage, while xanthine oxidase expression was rather induced by blocking SUR2 with glibenclamide. In conclusion, nicorandil reduces albuminuria and ameliorates renal injury by blocking oxidative stress in chronic kidney disease. © 2012 the American Physiological Society.

    DOI: 10.1152/ajprenal.00158.2012

    Scopus

    PubMed

    researchmap

  • Sustained-release prostacyclin analog ONO-1301 ameliorates tubulointerstitial alterations in a mouse obstructive nephropathy model Reviewed

    Tatsuyo Nasu, Masaru Kinomura, Katsuyuki Tanabe, Hiroko Yamasaki, Su le Htay, Daisuke Saito, Norikazu Hinamoto, Hiroyuki Watatani, Haruyo Ujike, Yoshinori Suzuki, Takeshi Sugaya, Hitoshi Sugiyama, Yoshiki Sakai, Kunio Matsumoto, Yohei Maeshima, Hirofumi Makino

    American Journal of Physiology - Renal Physiology   302 ( 12 )   F1616 - F1629   2012.6

     More details

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

    Tubulointerstitial injuries are crucial histological alterations that predict the deterioration of renal function in chronic kidney disease. ONO-1301, a novel sustained-release prostacyclin analog, accompanied by thromboxane synthase activity, exerts therapeutic effects on experimental pulmonary hypertension, lung fibrosis, cardiomyopathy, and myocardial ischemia, partly associated with the induction of hepatocyte growth factor (HGF). In the present study, we examined the therapeutic efficacies of ONO-1301 on tubulointerstitial alterations induced by unilateral ureteral obstruction (UUO). After inducing unilateral ureteral obstruction in C57/BL6J mice, a single injection of sustained-release ONO-1301 polymerized with poly (D,L-lactic-co-glycolic acid) sustained-release ONO-1301 (SR-ONO) significantly suppressed interstitial fibrosis, accumulation of types I and III collagen, increase in the number of interstitial fibroblast-specific protein-1 (FSP-1)+ cells, and interstitial infiltration of monocytes/macrophages (F4/80+) in the obstructed kidneys (OBK
    day 7). Treatment with SR-ONO significantly suppressed the increase of the renal levels of profibrotic factor TGF-β and phosphorylation of Smad2/3, and elevated the renal levels of HGF in the OBK. In cultured mouse proximal tubular epithelial cells (mProx24), ONO-1301 significantly ameliorated the expression of fibroblast-specific protein-1 and α-smooth muscle actin as well as phosphorylation of Smad3 and increased the expression of zonula occludens-1 and E-cadherin in the presence of TGF-β1 as detected by immunoblot and immunocytochemistry, partly dependent on PGI2 receptor-mediated signaling. Administration of rabbit anti-HGF antibodies, but not the control IgG, partly reversed the suppressive effects of SR-ONO on tubulointerstitial injuries in the OBK. Taken together, our findings suggest the potential therapeutic efficacies of ONO-1301 in suppressing tubulointerstitial alterations partly mediated via inducing HGF, an antifibrotic factor counteracting TGF-β. © 2012 the American Physiological Society.

    DOI: 10.1152/ajprenal.00538.2011

    Scopus

    PubMed

    researchmap

  • Nicorandil as a novel therapy for advanced diabetic nephropathy in the eNOS-deficient mouse Reviewed

    Katsuyuki Tanabe, Miguel A. Lanaspa, Wataru Kitagawa, Christopher J. Rivard, Makoto Miyazaki, Jelena Klawitter, George F. Schreiner, Moin A. Saleem, Peter W. Mathieson, Hirofumi Makino, Richard J. Johnson, Takahiko Nakagawa

    American Journal of Physiology - Renal Physiology   302 ( 9 )   F1151 - F1161   2012.5

     More details

    Authorship:Lead author   Language:English   Publishing type:Research paper (scientific journal)  

    Nicorandil is an orally available drug that can act as a nitric oxide donor, an antioxidant, and an ATP-dependent K channel activator. We hypothesized that it may have a beneficial role in treating diabetic nephropathy. We administered nicorandil to a model of advanced diabetic nephropathy (the streptozotocin-induced diabetes in mice lacking endothelial nitric oxide synthase, eNOSKO)
    controls included diabetic eNOS KO mice without nicorandil and nondiabetic eNOS KO mice treated with either nicorandil or vehicle. Mice were treated for 8 wk. Histology, blood pressure, and renal function were determined. Additional studies involved examining the effects of nicorandil on cultured human podocytes. Here, we found that nicorandil did not affect blood glucose levels, blood pressure, or systemic endothelial function, but significantly reduced proteinuria and glomerular injury (mesangiolysis and glomerulosclerosis). Nicorandil protected against podocyte loss and podocyte oxidative stress. Studies in cultured podocytes showed that nicorandil likely protects against glucose-mediated oxidant stress via the ATP-dependent K channel as opposed to its NO-stimulating effects. In conclusion, nicorandil may be beneficial in diabetic nephropathy by preserving podocyte function. We recommend clinical trials to determine whether nicorandil may benefit diabetic nephropathy or other conditions associated with podocyte dysfunction. © 2012 the American Physiological Society.

    DOI: 10.1152/ajprenal.00596.2011

    Scopus

    PubMed

    researchmap

  • Sucrose induces fatty liver and pancreatic inflammation in male breeder rats independent of excess energy intake Reviewed

    Carlos A. Roncal-Jimenez, Miguel A. Lanaspa, Christopher J. Rivard, Takahiko Nakagawa, L. Gabriela Sanchez-Lozada, Diana Jalal, Ana Andres-Hernando, Katsuyuki Tanabe, Magdalena Madero, Nanxing Li, Christina Cicerchi, Kim Mc Fann, Yuri Y. Sautin, Richard J. Johnson

    METABOLISM-CLINICAL AND EXPERIMENTAL   60 ( 9 )   1259 - 1270   2011.9

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:W B SAUNDERS CO-ELSEVIER INC  

    Fructose induces metabolic syndrome in rats; but studies have been criticized for using high concentrations of fructose that are not physiologic, for using only pure fructose, and for not controlling for energy intake. We tested the hypothesis that a 40% sucrose diet (containing 20% fructose) might induce features of metabolic syndrome in male breeder rats independent of excess energy intake. Male Sprague-Dawley breeder rats were pair fed 40% sucrose or isocaloric starch diet for 4 months and evaluated for metabolic syndrome and diabetes. In vitro studies were performed in rat insulinoma cells (RIN-m5F) exposed to uric acid, and markers of inflammation were assessed. Rats fed a 40% sucrose diet developed accelerated features of metabolic syndrome with up-regulation of fructose-dependent transporter Glut5 and fructokinase. Fatty liver and low-grade pancreatic inflammation also occurred. Uric acid was found to stimulate inflammatory mediators and oxidative stress in islet cells in vitro. Sucrose, at concentrations ingested by a subset of Americans, can accelerate metabolic syndrome, fatty liver, and type 2 diabetes mellitus in male breeder rats; and the effects are independent of excess energy intake. (C) 2011 Elsevier Inc. All rights reserved.

    DOI: 10.1016/j.metabol.2011.01.008

    Web of Science

    PubMed

    researchmap

  • Selective Stimulation of VEGFR2 Accelerates Progressive Renal Disease Reviewed

    Waichi Sato, Katsuyuki Tanabe, Tomoki Kosugi, Kelly Hudkins, Miguel A. Lanaspa, Li Zhang, Martha Campbell-Thompson, Qiuhong Li, David A. Long, Charles E. Alpers, Takahiko Nakagawa

    AMERICAN JOURNAL OF PATHOLOGY   179 ( 1 )   155 - 166   2011.7

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ELSEVIER SCIENCE INC  

    Vascular endothelial growth factor A (VEGF-A) can play both beneficial and deleterious roles in renal diseases, where its specific function might be determined by nitric oxide bioavailability. The complexity of VEGF-A in renal disease could in part be accounted for by the distinct roles of its two receptors; VEGFR1 is involved in the inflammatory responses, whereas VEGFR2 predominantly mediates angiogenesis. Because nondiabetic chronic renal disease is associated with capillary loss, we hypothesized that selective stimulation of VEGFR2 could be beneficial in this setting. However, VEGFR2 activation may be deleterious in the presence of nitric oxide deficiency. We systematically overexpressed a mutant form of VEGF-A binding only VEGFR2 (Flk-sel) using an adeno-associated virus-1 vector in wild-type and eNOS knockout mice and then induced renal injury by uninephrectomy. Flksel treatment increased angiogenesis and lowered blood pressure in both mouse types. Flk-set overexpression caused mesangial injury with increased proliferation associated with elevated expression of PDGF, PDGF-beta receptor, and VEGFR2; this effect was greater in eNOS knockout than in wild-type mice. Flk-sel also induced tubulointerstitial injury, with some tubular epithelial cells expressing alpha-smooth muscle actin, indicating a phenotypic evolution toward myofibroblasts. In conclusion, prestimulation of VEGFR2 can potentiate subsequent renal injury in mice, an effect enhanced in the setting of nitric oxide deficiency. Pathol 2011, 179: 155-166. DOI: 10.1016/j.ajpath.2011.03.024)

    DOI: 10.1016/j.ajpath.2011.03.024

    Web of Science

    PubMed

    researchmap

  • Unexpected occurrence of adrenal Cushing&apos;s syndrome in a patient with systemic lupus erythematosus Reviewed

    Akihiro Katayama, Fumio Otsuka, Katsuyuki Tanabe, Naoko Tsukamoto, Ryutaro Yamanaka, Yoshinori Matsumoto, Yasutomo Nasu, Hirofumi Makino

    HYPERTENSION RESEARCH   34 ( 5 )   662 - 663   2011.5

     More details

    Language:English   Publisher:NATURE PUBLISHING GROUP  

    DOI: 10.1038/hr.2011.13

    Web of Science

    PubMed

    researchmap

  • Amelioration of renal alterations in obese type 2 diabetic mice by vasohibin-1, a negative feedback regulator of angiogenesis Reviewed

    Daisuke Saito, Yohei Maeshima, Tatsuyo Nasu, Hiroko Yamasaki, Katsuyuki Tanabe, Hitoshi Sugiyama, Hikaru Sonoda, Yasufumi Sato, Hirofumi Makino

    AMERICAN JOURNAL OF PHYSIOLOGY-RENAL PHYSIOLOGY   300 ( 4 )   F873 - F886   2011.4

     More details

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

    Saito D, Maeshima Y, Nasu T, Yamasaki H, Tanabe K, Sugiyama H, Sonoda H, Sato Y, Makino H. Amelioration of renal alterations in obese type 2 diabetic mice by vasohibin-1, a negative feedback regulator of angiogenesis. Am J Physiol Renal Physiol 300: F873-F886, 2011. First published January 12, 2011; doi:10.1152/ajprenal.00503.2010.-The involvement of VEGF-A as well as the therapeutic efficacy of angiogenesis inhibitors in diabetic nephropathy have been reported. We recently reported the therapeutic effects of vasohibin-1 (VASH-1), an endogenous angiogenesis inhibitor, in a type 1 diabetic nephropathy model (Nasu T, Maeshima Y, Kinomura M, Hirokoshi-Kawahara K, Tanabe K, Sugiyama H, Sonoda H, Sato Y, Makino H. Diabetes 58: 2365-2375, 2009). In this study, we investigated the therapeutic efficacy of VASH-1 on renal alterations in obese mice with type 2 diabetes. Diabetic db/db mice received intravenous injections of adenoviral vectors encoding human VASH-1 (AdhVASH-1) and were euthanized 8 wk later. AdhVASH-1 treatment resulted in significant suppression of glomerular hypertrophy, glomerular hyperfiltration, albuminuria, increase in the CD31(+) glomerular endothelial area, F4/80(+) monocyte/macrophage infiltration, the accumulation of type IV collagen, and mesangial matrix. An increase in the renal levels of VEGF-A, VEGFR-2, transforming growth factor (TGF)-beta 1, and monocyte chemoattractant protein-1 in diabetic animals was significantly suppressed by AdhVASH-1 (immunoblotting). AdhVASH-1 treatment significantly recovered the loss and altered the distribution patterns of nephrin and zonula occludens (ZO)-1 and suppressed the increase in the number of fibroblast-specific protein-1 (FSP-1(+)) and desmin(+) podocytes in diabetic mice. In vitro, recombinant human VASH-1 (rhVASH-1) dose dependently suppressed the upregulation of VEGF induced by high ambient glucose (25 mM) in cultured mouse podocytes. In addition, rhVASH-1 significantly recovered the mRNA levels of nephrin and the protein levels of ZO-1 and P-cadherin and suppressed the increase in protein levels of desmin, FSP-1, Snail, and Slug in podocytes under high-glucose condition. Taken together, these results suggest the potential use of VASH-1 as a novel therapeutic agent in type 2 diabetic nephropathy mediated via antiangiogenic effects and maintenance of podocyte phenotype in association with antiproteinuric effects.

    DOI: 10.1152/ajprenal.00503.2010

    Web of Science

    PubMed

    researchmap

  • Effects of eplerenone on nephrotic syndrome in a patient with renovascular hypertension Reviewed

    Jiro Suzuki, Fumio Otsuka, Kenichi Inagaki, Katsuyuki Tanabe, Naoko Tsukamoto, Tomoko Miyoshi, Eri Nakamura, Toshio Ogura, Isao Kumagai, Hirofumi Makino

    HYPERTENSION RESEARCH   34 ( 3 )   404 - 406   2011.3

     More details

    Language:English   Publisher:NATURE PUBLISHING GROUP  

    DOI: 10.1038/hr.2010.249

    Web of Science

    PubMed

    researchmap

  • Intermittent administration of a sustained-release prostacyclin analog ONO-1301 ameliorates renal alterations in a rat type 1 diabetes model Reviewed

    H. Yamasaki, Y. Maeshima, T. Nasu, D. Saito, K. Tanabe, K. Hirokoshi-Kawahara, H. Sugiyama, Y. Sakai, H. Makino

    PROSTAGLANDINS LEUKOTRIENES AND ESSENTIAL FATTY ACIDS   84 ( 3-4 )   99 - 107   2011.3

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:ELSEVIER SCI LTD  

    Diabetic nephropathy is the most common pathological disorder predisposing end-stage renal disease. ONO-1301 is a novel sustained-release prostacyclin analog possessing thromboxane (T)() synthase inhibitory activity. Here, we aimed to investigate the therapeutic efficacies of ONO-1301 in a rat type 1 diabetic nephropathy model. Streptozotocin (STZ)-induced diabetic rats received injections of slow-release form of ONO-1301 (SR-ONO) every 3 weeks. Animals were sacrificed at Week 14. SR-ONO significantly suppressed albuminuria, glomerular hypertrophy, mesangial matrix accumulation, glomerular accumulation of monocyte/macrophage, increase in glomerular levels of pro-fibrotic factor transforming growth factor (TGF)-beta1 and the number of glomerular alpha-smooth muscle actin (SMA). cells in diabetic animals. The glomerular levels of hepatocyte growth factor (HGF) were significantly increased in SR-ONO-treated diabetic animals. Taken together, these results suggest the potential therapeutic efficacy of intermittent administration of SR-ONO in treating diabetic nephropathy potentially via inducing HGF, thus counteracting the pro-fibrotic effects of TGF-beta1. (C) 2010 Elsevier Ltd. All rights reserved.

    DOI: 10.1016/j.plefa.2010.11.005

    Web of Science

    researchmap

  • Endothelial dysfunction as a potential contributor in diabetic nephropathy Reviewed

    Takahiko Nakagawa, Katsuyuki Tanabe, Byron P. Croker, Richard J. Johnson, Maria B. Grant, Tomoki Kosugi, Qiuhong Li

    NATURE REVIEWS NEPHROLOGY   7 ( 1 )   36 - 44   2011.1

     More details

    Language:English   Publisher:NATURE PUBLISHING GROUP  

    The mechanisms that drive the development of diabetic nephropathy remain undetermined. Only 30-40% of patients with diabetes mellitus develop overt nephropathy, which suggests that other contributing factors besides the diabetic state are required for the progression of diabetic nephropathy. Endothelial dysfunction is associated with human diabetic nephropathy and retinopathy, and advanced diabetic glomerulopathy often exhibits thrombotic microangiopathy, including glomerular capillary microaneurysms and mesangiolysis, which are typical manifestations of endothelial dysfunction in the glomerulus. Likewise, diabetic mice with severe endothelial dysfunction owing to deficiency of endothelial nitric oxide synthase develop progressive nephropathy and retinopathy similar to the advanced lesions observed in humans with diabetes mellitus. Additionally, inhibitors of the renin-angiotensin system fail to be renoprotective in some individuals with diabetic nephropathy (due in part to aldosterone breakthrough) and in some mouse models of the disease. In this Review, we discuss the clinical and experimental evidence that supports a role for endothelial nitric oxide deficiency and subsequent endothelial dysfunction in the progression of diabetic nephropathy and retinopathy. If endothelial dysfunction is the key factor required for diabetic nephropathy, then agents that improve endothelial function or raise intraglomerular nitric oxide level could be beneficial in the treatment of diabetic nephropathy.

    DOI: 10.1038/nrneph.2010.152

    Web of Science

    PubMed

    researchmap

  • Inflammatory Cytokine-induced Expression of Vasohibin-1 by Rheumatoid Synovial Fibroblasts Reviewed

    Kohei Miyake, Keiichiro Nishida, Yasutaka Kadota, Hiroko Yamasaki, Tatsuyo Nasu, Daisuke Saitou, Katsuyuki Tanabe, Hikaru Sonoda, Yasufumi Sato, Yohei Maeshima, Hirofumi Makino

    ACTA MEDICA OKAYAMA   63 ( 6 )   349 - 358   2009.12

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:OKAYAMA UNIV MED SCHOOL  

    Angriogenesis is an essential event in the development of synovial inflammation in rheumatoid arthritis (RA). The aim of the current study was to investigate the expression of vasohibin-1, a novel endothelium-derived vascular endothelial growth factor (VEGF)-inducible angiogenesis inhibitor, in the RA synovium, and to test the effect of inflammatory cytokines on the expression of vasohibin-1 by RA synovial fibroblasts (RASFs). Synovial tissue samples were obtained at surgery from patients with osteoarthritis (OA) and RA, and subjected to immunohistochemistry to investigate the expression and distribution of vasohibin-1 relevant to the degree of synovial inflammation. In an in vitro analysis, RASFs were used to examine the expression of vasohibin-1 and VEGF mRNA by real-time PCR after stimulation with VEGF or inflammatory cytokines under normoxic or hypoxic conditions. The immunohistochemical results showed that vasohibin-1 was expressed in synovial lining cells, endothelial cells, and synovial fibroblasts. In synovial tissue, there was a significant correlation between the expression of vasohibin-1 and histological inflammation score (p = 0.002, r = 0.842). In vitro, stimulation with VEGF induced the expression of vasohibin-1 mRNA in RASFs under normoxic conditions, and stimulation with cytokines induced vasohibin-1 mRNA expression under a hypoxic condition. These results suggest that vasohibin-1 was expressed in RA synovial tissue and might be regulated by inflammatory cytokines.

    DOI: 10.18926/AMO/31820

    Web of Science

    PubMed

    researchmap

  • Vasohibin-1, a Negative Feedback Regulator of Angiogenesis, Ameliorates Renal Alterations in a Mouse Model of Diabetic Nephropathy Reviewed

    Tatsuyo Nasu, Yohei Maeshima, Masaru Kinomura, Kumiko Hirokoshi-Kawahara, Katsuyuki Tanabe, Hitoshi Sugiyama, Hikaru Sonoda, Yasufumi Sato, Hirofumi Makino

    DIABETES   58 ( 10 )   2365 - 2375   2009.10

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:AMER DIABETES ASSOC  

    OBJECTIVE-The involvement of proangiogenic factors such as vascular endothelial growth factor as well as the therapeutic efficacy of angiogenesis inhibitors in early diabetic nephropathy has been reported. Vasohibin-1 (VASH-1) is a unique endogenous angiogenesis inhibitor that is induced in endothelial cells by proangiogenic factors. We investigated the therapeutic efficacy of VASH-1 in an early diabetic nephropathy model.
    RESEARCH DESIGN AND METHODS-Streptozotocin-induced type 1 diabetic mice received intravenous injections of adenoviral vectors encoding VASH-1 (AdhVASH-1) or beta-gal (AdLacZ) every other week and were killed after 28 days.
    RESULTS-Treatment with AdhVASH-1 resulted in sustained increase in the protein levels of VASH-1 in the liver and sera, in the absence of any inflammatory alterations. AdhVASH-1 treatment significantly suppressed renal hypertrophy, glomerular hypertrophy, glomerular hyperfiltration, albuminuria, increase of the CD31(+) glomerular endothelial area, F4/80(+) monocyte/macrophage infiltration, the accumulation of type IV collagen, and mesangial matrix compared with AdLacZ-treated diabetic mice. Increase in the renal levels of transforming growth factor-beta 1, monocyte chemoattractant protein-1, and receptor for advanced glycation end products in diabetic animals was significantly suppressed by AdhVASH-1 (real-time PCR and immunoblot). VASH-1 significantly suppressed the increase of transforming growth factor-beta, monocyte chemoattractant protein-1, and receptor for advanced glycation end products, induced by high ambient glucose in cultured mouse mesangial cells. Increased phosphorylation of VEGFR2 was suppressed in AdVASH-1-treated diabetic animals and in cultured glomerular endothelial cells. Endogenous mouse VASH-1 was localized to the mesangial and endothelial area in glomeruli of diabetic mice.
    CONCLUSIONS-These results suggest the potential therapeutic efficacy of VASH-1 in treating early diabetic nephropathy potentially mediated via glomerular endothelial and mesangial cells. Diabetes 58:2365-2375, 2009

    DOI: 10.2337/db08-1790

    Web of Science

    PubMed

    researchmap

  • Amelioration of cisplatin-induced acute renal injury by renal progenitor-like cells derived from the adult rat kidney Reviewed

    Masaru Kinomura, Shinji Kitamura, Katsuyuki Tanabe, Kunihiro Ichinose, Kumiko Hirokoshi, Yuki Takazawa, Hiroyuki Kitayama, Tatsuyo Nasu, Hitoshi Sugiyama, Yasushi Yamasaki, Takeshi Sugaya, Yohei Maeshima, Hirofumi Makino

    CELL TRANSPLANTATION   17 ( 1-2 )   143 - 158   2008

     More details

    Language:English   Publishing type:Research paper (scientific journal)   Publisher:COGNIZANT COMMUNICATION CORP  

    The replacement of a necrotic tubular epithelium with functional tubular epithelial cells is required for recovery from acute renal failure (ARF). A rat renal progenitor-like (rKS56) cell line was recently established derived from the S3 segment of renal proximal tubules. The therapeutic efficacy of rKS56 cells was examined in a rat model of cisplatin-induced ARE rKS56-lacZ cells expressing P-galactosidase were injected into SD rats either at the subcapsule of the left kidney (rKS-SC) or via the left renal artery (rKS-IA) 2 days after the injection of cisplatin. Bluo-gal(+) rKS56-lacZ cells were observed in the subcapsule in the rKS-SC group on day 5, and were further increased in number on day 9, accompanied by partial distribution in the corticomedullary junction, but not in the rKS-IA group. A portion of Bluo-gal(+) cells coexpressed Ki-67, aquaporin-1, hepatocyte growth factor (HGF), and c-Met. rKS-SC treatment significantly improved the tubular injury scores, ameliorated tubular cell apoptosis, and induced cell proliferation. The renal function also significantly improved in the rKS-SC group on day 5. These results demonstrate that locally implanted rKS56 cells could differentiate into tubular epithelial cells, thereby accelerating the recovery from tubular injury, most likely by producing tubular trophic factors. These results suggest the therapeutic potential of this novel approach for patients with end-stage renal failure.

    DOI: 10.3727/000000008783907008

    Web of Science

    PubMed

    researchmap

  • Endostatin peptide, an inhibitor of angiogenesis, prevents the progression of peritoneal sclerosis in a mouse experimental model Reviewed

    Katsuyuki Tanabe, Yohei Maeshima, Kunihiro Ichinose, Hiroyuki Kitayama, Yuki Takazawa, Kumiko Hirokoshi, Masaru Kinomura, Hitoshi Sugiyama, Hirofumi Makino

    KIDNEY INTERNATIONAL   71 ( 3 )   227 - 238   2007.2

     More details

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

    Peritoneal sclerosis is a major and serious complication in patients on long-term continuous ambulatory peritoneal dialysis ( PD). The involvement of angiogenesis and proangiogenic factors such as vascular endothelial growth factor ( VEGF)-A in progressing peritoneal sclerosis has been reported. We previously reported the therapeutic efficacy of endostatin peptide, a potent inhibitor of angiogenesis derived from type XVIII collagen, in a mouse diabetic nephropathy model. Here, we examined the therapeutic effect of endostatin peptide in preventing progression in a mouse peritoneal sclerosis model. Male ICR mice received intraperitoneal injections of chlorhexidine gluconate ( CG) every other day to induce peritoneal sclerosis. Endostatin peptide ( 1 or 4mg/kg/day) was administered via subcutaneously implanted osmotic minipumps. Peritoneal sclerosis ( day 24) was significantly suppressed by endostatin peptide in a dose-dependent manner. Peritoneal accumulation of type III collagen was significantly suppressed by endostatin peptide. Increase in the number of CD31( +) blood vessels, F4/80( +) monocyte/macrophage accumulation, and 5-bromodeoxyuridine(+) proliferating cells was significantly inhibited by endostatin peptide. Increase in peritoneal expression of VEGF-A, profibrotic transforming growth factor-beta 1, and alpha-smooth muscle actin was suppressed by endostatin peptide. Immunoreactivity for endogenous endostatin ( whole molecule) and endostatin receptor alpha 5 beta 1-integrin was increased and colocalized to CD31( +) blood vessels in the thickened peritonea of CG-injected mice. These results demonstrate the potential use of antiangiogenic endostatin peptide as a novel therapeutic agent in preventing peritoneal sclerosis, a severe complication in patients undergoing long-term PD.

    DOI: 10.1038/sj.ki.5002040

    Web of Science

    PubMed

    researchmap

▼display all

Books

  • 腎疾患・透析最新の治療 2023-2025

    山縣邦弘, 南学正臣( Role: Contributor ,  糖尿病透析患者の管理)

    南江堂  2023.1 

     More details

  • 腎臓内科 Vol.16 No.5 ライフステージとCKD

    中司敦子( Role: Contributor ,  腎臓専門医のための模擬テスト35)

    科学評論社  2022.11 

     More details

  • 再生誘導剤(セルフリーな再生医療)の展望 月刊BIOINDUSTRY 2020年8月号

    酒井芳紀( Role: Contributor ,  YS-1402による慢性腎臓病の治療効果)

    シーエムシー出版  2020.8 

     More details

  • New専門医を目指すケース・メソッド・アプローチ 腎臓疾患<第3版>

    柏原直樹( Role: Contributor ,  CASE14 皮膚硬化を伴い高度な急性腎障害を呈した50歳女性)

    日本医事新報社  2017.12 

     More details

  • Diabetes Frontier Vol.19 No.5 わが国における最近の糖尿病メガスタディ

    Diabetes Frontier 編集委員会( Role: Contributor ,  血管新生抑制因子Vasohibin-1による糖尿病腎症進展抑制効果の検討)

    メディカルレビュー社  2008.10 

     More details

  • 腎臓 Vol.29 No.2 わが国の慢性腎臓病(CKD)対策の最前線

    腎臓 編集委員( Role: Contributor ,  CKDの定義と分類)

    日本腎臓財団  2006.10 

     More details

▼display all

MISC

  • 平滑筋肉腫の両側腎臓への転移に対して両腎摘出術を契機に血液透析導入とした一例

    浅川知彦, 竹内英実, 岡本修吾, 大西康博, 田中景子, 辻憲二, 田邊克幸, 森永裕士, 内田治仁, 和田淳

    中国腎不全研究会誌   32   2024

  • 当院における非外傷性腹直筋血腫5症例の報告

    中納弘幸, 竹内英実, 森本志帆, 寺嶋悠也, 岡本修吾, 大西康博, 田中景子, 勝山隆行, 辻憲二, 田邊克幸, 森永裕士, 宇賀麻由, 冨田晃司, 平木隆夫, 内田治仁, 和田淳

    中国腎不全研究会誌   32   2024

  • 当院における腎移植後悪性腫瘍の検討

    山野井友昭, 西村慎吾, 関戸崇了, 吉永香澄, 丸山雄樹, 定平卓也, 枝村康平, 小林知子, 小林泰之, 大西康博, 竹内英実, 田邊克幸, 森永裕士, 和田淳, 荒木元朗

    日本移植学会総会プログラム抄録集   59th (Web)   2023

  • テキストマイニングによる腎移植に関する症例報告論文の考察

    関戸 崇了, 荒木 元朗, 吉永 香澄, 丸山 雄樹, 山野井 友昭, 定平 卓也, 片山 聡, 岩田 健宏, 西村 慎吾, 佐古 智子, 枝村 康平, 小林 泰之, 渡部 昌実, 渡邉 豊彦, 田邊 克幸, 竹内 英実, 喜多村 真治, 杉山 斉, 和田 淳, 那須 保友

    日本臨床腎移植学会プログラム・抄録集   55回   227 - 227   2022.2

     More details

    Language:Japanese   Publisher:(一社)日本臨床腎移植学会  

    J-GLOBAL

    researchmap

  • 尿細胞診によるBKウイルス腎症の発症予測は尿沈渣で代替可能か

    関戸崇了, 荒木元朗, 吉永香澄, 山野井友昭, 丸山雄樹, 定平卓也, 西村慎吾, 枝村康平, 小林泰之, 田邊克幸, 竹内英実, 森永裕士, 和田淳, 柳井広之

    日本移植学会総会プログラム抄録集   58th (Web)   2022

  • COVID-19維持透析患者の治療経験と透析室での感染対策

    木野村賢, 田邊克幸, 藤原千尋, 笠原由美子, 長谷川功, 萩谷英大, 大塚文男, 和田淳

    中国腎不全研究会誌   30   2022

  • 中四国地域におけるCKDおよびCVDの関連に関するコホート研究;Kakusyo3C Studyのイベント解析

    大高望, 内田治仁, 竹内英実, 辻憲二, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    日本腎臓学会誌(Web)   63 ( 4 )   2021

  • 腎移植後の尿細胞診で6ヶ月以上持続するDecoy細胞陽性所見はBKウイルス腎症の発症予測に有効である

    関戸崇了, 荒木元朗, 吉永香澄, 丸山雄樹, 定平卓也, 西村慎吾, 和田耕一郎, 渡部昌実, 渡邉豊彦, 田邊克幸, 竹内英実, 和田淳, 柳井広之, 那須保友

    日本移植学会総会プログラム抄録集   57th (Web)   2021

  • 腎移植患者のタクロリムス血中濃度にボノプラザンが与える薬物相互作用の検討

    和田里章悟, 荒木元朗, 松本准, 関戸崇了, 吉永香澄, 丸山雄樹, 定平卓也, 西村慎吾, 和田耕一郎, 小林泰之, 渡邉豊彦, 竹内英実, 田邊克幸, 那須保友

    日本移植学会総会プログラム抄録集   57th (Web)   2021

  • 岡山市CKDネットワーク(OCKD-NET)におけるCKD病診連携10年後の追跡調査

    大西康博, 内田治仁, 大高望, 竹内英実, 辻憲二, 田邊克幸, 森永裕士, 木野村賢, 喜多村真治, 前島洋平, 杉山斉, 太田康介, 丸山啓輔, 大城義之, 森岡茂, 瀧上慶一, 蒲生直幸, 和田淳

    日本腎臓学会誌(Web)   63 ( 4 )   2021

  • 慢性腎臓病における貧血管理~Kakusyo3C Studyからの検討

    奥山由加, 内田治仁, 大高望, 竹内英実, 辻憲二, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    日本腎臓学会誌(Web)   63 ( 4 )   2021

  • 腎不全療法選択説明が緊急透析導入と療法選択に与える影響

    森永裕士, 笠原由美子, 井本紀子, 角川紫野, 矢田光子, 大高望, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 喜多村真治, 内田治仁, 杉山斉, 和田淳

    日本透析医学会雑誌   53 ( Supplement 1 )   2020

  • 慢性腎臓病における貧血管理~Kakusyo3C Studyからの検討

    内山奈津実, 内田治仁, 西脇麻里子, 大高望, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    日本腎臓学会誌(Web)   62 ( 4 )   2020

  • 中四国地域におけるCKDおよびCVDの関連に関するコホート研究Kakusyo3C Study:登録3年後のCKD管理状況

    西脇麻里子, 内田治仁, 大高望, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    日本腎臓学会誌(Web)   62 ( 4 )   2020

  • 中四国地域におけるCKDおよびCVDの関連に関する前向きコホート研究;Kakusyo3C Study:登録3年後の中間解析

    大高望, 内田治仁, 西脇麻里子, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    日本腎臓学会誌(Web)   62 ( 4 )   2020

  • 岡山市CKDネットワーク(OCKD-NET)におけるCKD病診連携9年後の追跡調査

    大西康博, 内田治仁, 大高望, 辻憲二, 田邊克幸, 森永裕士, 木野村賢, 喜多村真治, 前島洋平, 杉山斉, 太田康介, 丸山啓輔, 大城義之, 森岡茂, 大森一慶, 瀧上慶一, 蒲生直幸, 和田淳

    日本腎臓学会誌(Web)   62 ( 4 )   2020

  • 腎移植後に発生し治療により完治したリンパ嚢腫の2例

    窪田 理沙, 荒木 元朗, 和田 耕一郎, 河村 香澄, 丸山 雄樹, 光井 洋介, 西村 慎吾, 山下 里美, 小林 泰之, 渡邉 豊彦, 那須 保友, 加納 弓月, 北川 正史, 田邊 克幸, 和田 淳

    移植   54 ( 総会臨時 )   278 - 278   2019.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 腎虚血再灌流障害における好中球動態の2光子励起顕微鏡を用いた解析

    丸山 雄樹, 荒木 元朗, 城所 研吾, 和田 耕一郎, 河村 香澄, 光井 洋介, 定平 卓也, 窪田 理沙, 西村 慎吾, 渡部 昌実, 渡邉 豊彦, 田邊 克幸, 和田 淳, 柏原 直樹, 那須 保友

    移植   54 ( 総会臨時 )   241 - 241   2019.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 腎移植後に発生し治療により完治したリンパ嚢腫の2例

    窪田 理沙, 荒木 元朗, 和田 耕一郎, 河村 香澄, 丸山 雄樹, 光井 洋介, 西村 慎吾, 山下 里美, 小林 泰之, 渡邉 豊彦, 那須 保友, 加納 弓月, 北川 正史, 田邊 克幸, 和田 淳

    移植   54 ( 総会臨時 )   278 - 278   2019.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 生体腎移植におけるドナー・レシピエントのQoL変化の相違の検討

    光井 洋介, 荒木 元朗, 山下 里美, 丸山 雄樹, 河村 香澄, 窪田 理沙, 西村 慎吾, 和田 耕一郎, 小林 泰之, 渡邉 豊彦, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳, 那須 保友

    移植   54 ( 総会臨時 )   253 - 253   2019.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 生体腎移植におけるドナー・レシピエントのQoL変化の相違の検討

    光井 洋介, 荒木 元朗, 山下 里美, 丸山 雄樹, 河村 香澄, 窪田 理沙, 西村 慎吾, 和田 耕一郎, 小林 泰之, 渡邉 豊彦, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳, 那須 保友

    移植   54 ( 総会臨時 )   253 - 253   2019.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 生体腎移植8年後に回腸末端に発生したPTLDの一例

    和田里 章悟, 荒木 元朗, 河村 香澄, 丸山 雄樹, 光井 洋介, 窪田 理沙, 定平 卓也, 西村 慎吾, 和田 耕一郎, 枝村 康平, 小林 泰之, 渡邉 豊彦, 北川 正史, 田邊 克幸, 那須 保友

    移植   54 ( 総会臨時 )   278 - 278   2019.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 生体腎移植8年後に回腸末端に発生したPTLDの一例

    和田里 章悟, 荒木 元朗, 河村 香澄, 丸山 雄樹, 光井 洋介, 窪田 理沙, 定平 卓也, 西村 慎吾, 和田 耕一郎, 枝村 康平, 小林 泰之, 渡邉 豊彦, 北川 正史, 田邊 克幸, 那須 保友

    移植   54 ( 総会臨時 )   278 - 278   2019.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    J-GLOBAL

    researchmap

  • Exogenous Vasohibin-2 Influences Development of Angiotensin II-induced Ascending Aortic Aneurysms but Not Abdominal Aortic Aneurysms in Either Normolipidemic or Apolipoprotein E-Deficient Mice

    Nozomu Otaka, Haruhito A. Uchida, MIchihiro Okuyama, Yuki Kakio, Yoshiko Hada, Hidemi Takeuchi, Ryoko Umebayashi, Katsuyuki Tanabe, Yasufumi Sato, Jun Wada

    ARTERIOSCLEROSIS THROMBOSIS AND VASCULAR BIOLOGY   39   2019.5

     More details

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

    Web of Science

    researchmap

  • 腹腔鏡下開窓術を施行した腎移植後リンパ嚢腫の1例

    窪田 理沙, 荒木 元朗, 和田 耕一郎, 河村 香澄, 丸山 雄樹, 光井 洋介, 西村 慎吾, 山下 里美, 小林 泰之, 渡邉 豊彦, 那須 保友, 北川 正史, 田邊 克幸, 和田 淳

    日本臨床腎移植学会プログラム・抄録集   52回   226 - 226   2019.2

     More details

    Language:Japanese   Publisher:(一社)日本臨床腎移植学会  

    researchmap

  • 当院で施行した先行的腎移植の検討

    坪井一朗, 荒木元朗, 河村香澄, 丸山雄樹, 窪田理沙, 定平卓也, 西村慎吾, 和田耕一郎, 小林泰之, 渡邉豊彦, 北川正史, 田邊克幸, 杉山斉, 和田淳, 那須保友

    日本臨床腎移植学会プログラム・抄録集   52nd   142 - 142   2019.2

     More details

    Language:Japanese   Publisher:(一社)日本臨床腎移植学会  

    J-GLOBAL

    researchmap

  • 腹腔鏡下開窓術を施行した腎移植後リンパ嚢腫の1例

    窪田 理沙, 荒木 元朗, 和田 耕一郎, 河村 香澄, 丸山 雄樹, 光井 洋介, 西村 慎吾, 山下 里美, 小林 泰之, 渡邉 豊彦, 那須 保友, 北川 正史, 田邊 克幸, 和田 淳

    日本臨床腎移植学会プログラム・抄録集   52回   226 - 226   2019.2

     More details

    Language:Japanese   Publisher:(一社)日本臨床腎移植学会  

    researchmap

  • 当院で施行した先行的腎移植の検討

    坪井 一朗, 荒木 元朗, 河村 香澄, 丸山 雄樹, 窪田 理沙, 定平 卓也, 西村 慎吾, 和田 耕一郎, 小林 泰之, 渡邉 豊彦, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳, 那須 保友

    日本臨床腎移植学会プログラム・抄録集   52回   142 - 142   2019.2

     More details

    Language:Japanese   Publisher:(一社)日本臨床腎移植学会  

    J-GLOBAL

    researchmap

  • Fetuin-Aの糖尿病腎症進展における役割

    三瀬広記, 中司敦子, 山口哲志, 勅使川原早苗, 田邊克幸, 江口潤, 和田淳

    糖尿病(Web)   62 ( Suppl )   2019

  • 生体腎移植レシピエントにおけるCT値を用いた骨密度の変化に関する検討

    丸山 雄樹, 荒木 元朗, 和田 耕一郎, 坪井 一朗, 河村 香澄, 光井 洋介, 窪田 理沙, 西村 慎吾, 小林 泰之, 渡邊 豊彦, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳, 那須 保友

    移植   53 ( 総会臨時 )   490 - 490   2018.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 鰓耳腎症候群の小児に対する生体腎移植の1例

    窪田 理沙, 荒木 元朗, 和田 耕一郎, 河村 香澄, 丸山 雄樹, 光井 洋介, 西村 慎吾, 小林 泰之, 渡邉 豊彦, 那須 保友, 宮井 貴之, 北川 正史, 田邊 克幸, 和田 淳

    移植   53 ( 総会臨時 )   434 - 434   2018.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 鰓耳腎症候群の小児に対する生体腎移植の1例

    窪田 理沙, 荒木 元朗, 和田 耕一郎, 河村 香澄, 丸山 雄樹, 光井 洋介, 西村 慎吾, 小林 泰之, 渡邉 豊彦, 那須 保友, 宮井 貴之, 北川 正史, 田邊 克幸, 和田 淳

    移植   53 ( 総会臨時 )   434 - 434   2018.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 生体腎移植におけるリツキシマブ投与の効果と有害事象

    河村 香澄, 荒木 元朗, 丸山 雄樹, 坪井 一朗, 光井 洋介, 窪田 理沙, 西村 真吾, 和田 耕一郎, 小林 泰之, 渡邉 豊彦, 那須 保友, 山下 里美, 北川 正史, 田邉 克幸, 杉山 斉, 和田 淳

    移植   53 ( 総会臨時 )   481 - 481   2018.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    J-GLOBAL

    researchmap

  • 生体腎移植におけるリツキシマブ投与の効果と有害事象

    河村 香澄, 荒木 元朗, 丸山 雄樹, 坪井 一朗, 光井 洋介, 窪田 理沙, 西村 真吾, 和田 耕一郎, 小林 泰之, 渡邉 豊彦, 那須 保友, 山下 里美, 北川 正史, 田邉 克幸, 杉山 斉, 和田 淳

    移植   53 ( 総会臨時 )   481 - 481   2018.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    J-GLOBAL

    researchmap

  • 生体腎移植レシピエントにおけるCT値を用いた骨密度の変化に関する検討

    丸山 雄樹, 荒木 元朗, 和田 耕一郎, 坪井 一朗, 河村 香澄, 光井 洋介, 窪田 理沙, 西村 慎吾, 小林 泰之, 渡邊 豊彦, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳, 那須 保友

    移植   53 ( 総会臨時 )   490 - 490   2018.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • Exogenous Vasohibin-2 Does Not Influence Angiotensin II-induced Abdominal Aortic Aneurysms Formation in Either Normolipidemic or Apolipoprotein E-Deficient Mice

    Nozomu Otaka, Haruhito A. Uchida, Yoshiko Hada, Hidemi Takeuchi, Yuki Kakio, MIchihiro Okuyama, Ryoko Umebayashi, Katsuyuki Tanabe, Yasufumi Sato, Jun Wada

    ARTERIOSCLEROSIS THROMBOSIS AND VASCULAR BIOLOGY   38   2018.5

     More details

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

    DOI: 10.1161/atvb.38.suppl_1.110

    Web of Science

    researchmap

  • 肝腎同時移植における腎保護

    荒木元朗, 和田耕一郎, 山下里美, 丸山雄樹, 光井洋介, 定平卓也, 西村慎吾, 甲斐誠二, 高本篤, 谷本竜太, 杉本盛人, 小林泰之, 渡邉豊彦, 那須保友, 北川正史, 田邊克幸, 和田淳, 楳田祐三, 藤原俊義, 八木孝仁

    日本臨床腎移植学会プログラム・抄録集   51st   97   2018

     More details

    Language:Japanese  

    J-GLOBAL

    researchmap

  • 珪肺に続発したループス腎炎の1例

    福島和彦, 内田治仁, 御舩朋代, 渊本康子, 和田大広, 大西章史, 北川正史, 田邊克幸, 木野村賢, 喜多村真治, 小崎晋司, 杉山斉, 金廣有彦, 岸本卓巳, 和田淳

    日本腎臓学会誌   60 ( 6 )   2018

  • Vasohibin-2は大動脈瘤モデルマウスにおいてVEGFとは独立して胸部大動脈瘤を増悪させる

    奥山 倫弘, 内田 治仁, 垣尾 勇樹, 梅林 亮子, 田邊 克幸, 藤井 泰宏, 大澤 晋, 佐藤 靖史, 和田 淳

    脈管学   57 ( Suppl. )   S128 - S128   2017.10

     More details

    Language:Japanese   Publisher:(一社)日本脈管学会  

    researchmap

  • 抗血管内皮細胞増殖因子(VEGF)薬硝子体内注射による腎障害が示唆された糖尿病性腎症の1例

    大高 望, 川北 智英子, 木野村 賢, 北川 正史, 田邊 克幸, 江口 潤, 内田 治仁, 杉山 斉, 和田 淳, 清水 章

    日本腎臓学会誌   59 ( 6 )   731 - 731   2017.9

     More details

    Language:Japanese   Publisher:(一社)日本腎臓学会  

    researchmap

  • 腎移植レシピエントにおける術前皮下脂肪・内臓脂肪体積の術後腎機能への影響

    光井 洋介, 荒木 元朗, 河村 香澄, 丸山 雄樹, 西村 慎吾, 和田 耕一郎, 小林 泰之, 渡辺 豊彦, 北川 正史, 田邊 克幸, 那須 保友

    移植   52 ( 総会臨時 )   354 - 354   2017.8

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 生体腎移植レシピエントにおける予防的抗菌薬と周術期感染症に関する後ろ向き調査

    和田 耕一郎, 荒木 元朗, 西村 慎吾, 山下 里美, 河村 香澄, 光井 洋介, 吉岡 貴史, 有吉 勇一, 小林 泰之, 渡邉 豊彦, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳, 那須 保友

    移植   52 ( 総会臨時 )   467 - 467   2017.8

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 術前代謝拮抗剤による関節リウマチ増悪を来すもエベロリムスへの変更によって腎移植可能であった一例

    丸山 雄樹, 荒木 元朗, 光井 洋介, 西村 慎吾, 杉本 盛人, 山下 里美, 和田 耕一郎, 小林 泰之, 渡邉 豊彦, 那須 保友, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳

    移植   52 ( 総会臨時 )   502 - 502   2017.8

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • Overexpression of Vasohibin-2 Exacerbates Development of Angiotensin II-Induced Thoracic Aortic Aneurysms Independent of VeEGF

    Michihiro Okuyama, Haruhito A. Uchida, Ryoko Umebayashi, Yuki Kakio, Hidemi Takeuchi, Katsuyuki Tanabe, Yasufumi Sato, Jun Wada

    ARTERIOSCLEROSIS THROMBOSIS AND VASCULAR BIOLOGY   37   2017.5

     More details

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

    Web of Science

    researchmap

  • 当院における透析導入患者の潜在性結核感染症スクリーニング状況の検討

    加藤 綾子, 大西 章史, 杉山 斉, 森下 美智子, 宮脇 義亜, 荒田 夕佳, 益田 加奈, 秋山 愛由, 梅林 亮子, 山成 俊夫, 森永 裕士, 田邊 克幸, 木野村 賢, 和田 淳

    中国腎不全研究会誌   25   67 - 68   2017.3

     More details

    Language:Japanese   Publisher:中国腎不全研究会  

    researchmap

  • 抗てんかん薬の長期内服中に緩徐進行性の腎機能低下を呈した1例

    御舩朋代, 田邊克幸, 川北智英子, 山成俊夫, 北川正史, 木野村賢, 内田治仁, 喜多村真治, 杉山斉, 和田淳

    日本腎臓学会誌   59 ( 6 )   2017

  • 急性腎障害における血管新生促進因子Vasohibin-2の発現意義についての検討

    三宅広将, 田邊克幸, 益田加奈, 津志田圭吾, 杉山斉, 佐藤靖史, 和田淳

    日本腎臓学会誌   59 ( 3 )   2017

  • 当院における高齢者の生体腎移植レシピエントの検討

    光井 洋介, 荒木 元朗, 山下 里美, 吉岡 貴史, 有吉 勇一, 和田 耕一郎, 小林 泰之, 江原 伸, 渡辺 豊彦, 那須 保友, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳

    移植   51 ( 6 )   509 - 509   2016.12

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 生体腎移植レシピエントにおける周術期感染に関する後ろ向き調査

    和田 耕一郎, 荒木 元朗, 山下 里美, 光井 洋介, 吉岡 貴史, 有吉 勇一, 西村 慎吾, 小林 泰之, 渡辺 豊彦, 北川 正史, 田邊 克幸, 森永 裕士, 杉山 斉, 和田 淳, 那須 保友

    移植   51 ( 総会臨時 )   414 - 414   2016.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 岡山大学病院における生体腎移植レシピエントの術前ワクチン接種の現状

    光井 洋介, 荒木 元朗, 山下 里美, 吉岡 貴史, 有吉 勇一, 西村 慎吾, 和田 耕一郎, 小林 泰之, 渡辺 豊彦, 那須 保友, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳

    移植   51 ( 総会臨時 )   266 - 266   2016.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 岡山大学病院における腹腔鏡下ドナー腎採取術の検討

    西村 慎吾, 荒木 元朗, 小林 泰之, 有森 千聖, 山下 里美, 光井 洋介, 窪田 理沙, 吉岡 貴史, 有吉 勇一, 和田 耕一郎, 渡辺 豊彦, 北川 正史, 田邊 克幸, 和田 淳, 那須 保友

    移植   51 ( 総会臨時 )   331 - 331   2016.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 生体腎移植レシピエントにおける周術期感染症に関する検討

    和田 耕一郎, 定平 卓也, 山本 満寿美, 石井 亜矢乃, 渡辺 豊彦, 那須 保友, 荒木 元朗, 山下 里美, 吉岡 貴史, 有吉 勇一, 光畑 律子, 山成 俊夫, 北川 正史, 田邊 克幸, 森永 裕士, 杉山 斉, 和田 淳

    日本化学療法学会雑誌   64 ( Suppl.A )   177 - 177   2016.5

     More details

    Language:Japanese   Publisher:(公社)日本化学療法学会  

    researchmap

  • 維持血液透析を要したFontan術後成人先天性心疾患(ACHD)の1症例と透析管理の特徴

    木野村 賢, 森下 美智子, 宮脇 義亜, 益田 加奈, 荒田 夕佳, 秋山 愛由, 大西 章史, 山成 俊夫, 田邊 克幸, 杉山 斉, 赤木 禎治, 和田 淳

    日本透析医学会雑誌   49 ( Suppl.1 )   715 - 715   2016.5

     More details

    Language:Japanese   Publisher:(一社)日本透析医学会  

    researchmap

  • 当院における透析導入患者の潜在性結核感染症スクリーニング状況の検討

    大西 章史, 杉山 斉, 森下 美智子, 宮脇 義亜, 荒田 夕佳, 益田 加奈, 秋山 愛由, 梅林 亮子, 山成 俊夫, 森永 裕士, 田邊 克幸, 木野村 賢, 和田 淳

    日本透析医学会雑誌   49 ( Suppl.1 )   807 - 807   2016.5

     More details

    Language:Japanese   Publisher:(一社)日本透析医学会  

    researchmap

  • 不明熱の原因として非結核性抗酸菌(NTM)症が考えられた血液透析患者の1例.

    益田 加奈, 木野村 賢, 竹内 英実, 森下 美智子, 荒田 夕佳, 秋山 愛由, 大西 章史, 田邊 克幸, 佐田 憲映, 谷口 暁彦, 杉山 斉, 和田 淳

    中国腎不全研究会誌   24   183 - 184   2016

     More details

  • 生体腎移植後に移植尿管結石、一時的尿管狭窄を生じた症例

    光井 洋介, 荒木 元朗, 山下 里美, 吉岡 貴史, 有吉 勇一, 和田 耕一郎, 小林 泰之, 江原 伸, 渡邉 豊彦, 那須 保友, 北川 正史, 田辺 克幸, 杉山 斉

    西日本泌尿器科   77 ( 増刊 )   127 - 127   2015.10

     More details

    Language:Japanese   Publisher:西日本泌尿器科学会  

    researchmap

  • 生体腎移植レシピエントにおける周術期感染症に関する検討

    和田 耕一郎, 荒木 元朗, 山下 里美, 吉岡 貴史, 有吉 勇一, 小林 泰之, 江原 伸, 渡辺 豊彦, 山成 俊夫, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳, 那須 保友

    移植   50 ( 総会臨時 )   299 - 299   2015.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 生体腎移植におけるリツキシマブの効果と有害事象の検討

    荒木 元朗, 和田 耕一郎, 宗石 理沙, 吉岡 貴史, 有吉 勇一, 山下 里美, 小林 泰之, 江原 伸, 渡辺 豊彦, 那須 保友, 田邊 克幸, 北川 正史, 杉山 斉, 和田 淳

    移植   50 ( 総会臨時 )   475 - 475   2015.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 当院で施行した先行的腎移植(preemptive renal transplantation:PRT)の検討

    光井 洋介, 荒木 元朗, 山下 里美, 吉岡 貴史, 有吉 勇一, 和田 耕一郎, 小林 泰之, 江原 伸, 渡辺 豊彦, 那須 保友, 北川 正史, 田邊 克幸, 杉山 斉, 和田 淳

    移植   50 ( 総会臨時 )   316 - 316   2015.9

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 多発性嚢胞腎における指定難病重症度分類の評価に関する検討

    大西章史, 杉山斉, 田中景子, 山成俊夫, 秋山愛由, 北川正史, 森永裕士, 井上達之, 菊本陽子, 田邊克幸, 木野村賢, 花山宣久, 内田治仁, 喜多村真治, 和田淳

    日本腎臓学会誌   57 ( 3 )   2015

  • 腎炎所見が紫斑に先行したIgA血管炎(IgAV)の1例

    澁藤宣行, 木野村賢, 北川正史, 田邊克幸, 喜多村真治, 杉山斉, 和田淳

    日本腎臓学会誌   57 ( 6 )   2015

  • 当科で施行した生体腎移植レシピエント、ドナーのQOL評価

    有吉 勇一, 荒木 元朗, 宗石 理沙, 吉岡 貴史, 和田 耕一郎, 小林 泰之, 佐々木 克己, 江原 伸, 渡辺 豊彦, 那須 保友, 公文 裕巳, 有森 千聖, 北川 正史, 田邊 克幸, 森永 裕士, 菊本 陽子, 内田 治仁, 喜多村 真治, 前島 洋平, 杉山 斉, 槇野 博史

    移植   49 ( 4-5 )   377 - 377   2014.11

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • 腎線維化におけるAT1受容体結合因子ATRAPの発現調節についての検討

    大友 優太, 涌井 広道, 田村 功一, 大澤 正人, 小豆島 健護, 畝田 一司, 小林 竜, 大城 光二, 戸谷 義幸, 山下 暁朗, 田邊 克幸, 前島 洋平, 槇野 博史, 梅村 敏

    日本高血圧学会総会プログラム・抄録集   37回   337 - 337   2014.10

     More details

    Language:Japanese   Publisher:(NPO)日本高血圧学会  

    researchmap

  • マウス慢性腎臓病病態モデルにおけるAT1受容体結合因子ATRAP発現調節についての検討

    小林 竜, 田村 功一, 涌井 広道, 大澤 正人, 小豆島 健護, 畝田 一司, 大城 光二, 出島 徹, 前田 晃延, 戸谷 義幸, 山下 暁朗, 田邉 克幸, 前島 洋平, 槇野 博史, 梅村 敏

    日本高血圧学会総会プログラム・抄録集   37回   401 - 401   2014.10

     More details

    Language:Japanese   Publisher:(NPO)日本高血圧学会  

    researchmap

  • 岡山大学泌尿器科におけるpreemptive腎移植症例の検討

    有吉 勇一, 荒木 元朗, 宗石 理沙, 吉岡 貴史, 和田 耕一郎, 小林 泰之, 佐々木 克己, 江原 伸, 渡辺 豊彦, 那須 保友, 公文 裕巳, 清水 千聖, 赤木 滋, 森永 裕士, 田邊 克幸, 北川 正史, 杉山 斉, 和田 淳, 槇野 博史

    移植   49 ( 1 )   167 - 167   2014.5

     More details

    Language:Japanese   Publisher:(一社)日本移植学会  

    researchmap

  • LACK OF VASOHIBIN-1 EXACERBATES RENAL ALTERATIONS INDUCED BY INFUSION OF ANGIOTENSIN-II

    Hinamoto Norikazu, Maeshima Yohei, Yamasaki Hiroko, Watatani Hiroyuki, Ujike Haruyo, Tanabe Katsuyuki, Masuda Kana, Sugiyama Hitoshi, Sato Yasufumi, Makino Hirofumi

    NEPHROLOGY   19   106 - 106   2014.5

     More details

    Language:English   Publishing type:Research paper, summary (international conference)   Publisher:WILEY-BLACKWELL  

    Web of Science

    researchmap

  • REDUCTION OF PROTEINURIA IN THE STREPTOZOTOCIN-INDUCED DIABETIC MICE LACKING ENDOGENOUS VASOHIBIN-2

    Ujike Haruyo, Maeshima Yohei, Hinamoto Norikazu, Watatani Hiroyuki, Tanabe Katsuyuki, Masuda Kana, Sugiyama Hitoshi, Sato Yasufumi, Makino Hirofumi

    NEPHROLOGY   19   43 - 44   2014.5

     More details

    Language:English   Publishing type:Research paper, summary (international conference)   Publisher:WILEY-BLACKWELL  

    Web of Science

    researchmap

  • ORAL ADMINISTRATION OF A PROSTACYCLIN ANALOG ONO-1301 AMELIORATES VASCULAR CALCIFICATION IN A RAT MODEL OF ADENINE-INDUCED CHRONIC KIDNEY DISEASE

    Watatani Hiroyuki, Maeshima Yohei, Hinamoto Norikazu, Ujike Haruyo, Tanabe Katsuyuki, Masuda Kana, Sugiyama Hitoshi, Sakai Yoshiki, Makino Hirofumi

    NEPHROLOGY   19   172 - 172   2014.5

     More details

    Language:English   Publishing type:Research paper, summary (international conference)   Publisher:WILEY-BLACKWELL  

    Web of Science

    researchmap

  • ファブリー病およびファブリー腎症に対する酵素補充療法の長期効果

    菊本陽子, 杉山斉, 大西章史, 山成俊夫, 小川愛由, 北川正史, 森永裕士, 田邊克幸, 喜多村真治, 前島洋平, 槇野博史

    日本腎臓学会誌   56 ( 3 )   2014

  • 当科で施行した生体腎移植レシピエント,ドナーのQOL評価

    有吉勇一, 荒木元朗, 宗石理沙, 吉岡貴史, 和田耕一郎, 小林泰之, 佐々木克己, 江原伸, 渡辺豊彦, 那須保友, 公文裕巳, 有森千聖, 北川正史, 田邊克幸, 森永裕士, 菊本陽子, 内田治仁, 喜多村真治, 前島洋平, 杉山斉, 槇野博史

    移植(Web)   49 ( 4-5 )   2014

  • ファブリー腎症による腎不全に対して酵素補充療法と共に腹膜透析を継続中の1例

    山成俊夫, 杉山斉, 森永裕士, 菊本陽子, 大西章史, 北川正史, 小川愛由, 田邊克幸, 喜多村真治, 前島洋平, 槇野博史

    日本透析医学会雑誌   47 ( Supplement 1 )   2014

  • 慢性腎臓病の経過において尿中Trefoil Factor 3の変化率はアルブミン尿の変化率と有意相関する

    山成俊夫, 杉山斉, 森永裕士, 大西章史, 小川愛由, 北川正史, 菊本陽子, 田邊克幸, 喜多村真治, 前島洋平, 小川大輔, 四方賢一, 大本安一, 槇野博史

    日本腎臓学会誌   56 ( 3 )   2014

  • 慢性腎臓病におけるエピジェネティクスと酸化ストレスの関連に関する検討

    大西章史, 杉山斉, 山成俊夫, 小川愛由, 北川正史, 森永裕士, 菊本陽子, 田邊克幸, 内田治仁, 喜多村真治, 前島洋平, 槇野博史

    日本腎臓学会誌   56 ( 3 )   2014

  • 降圧療法により改善をみた悪性高血圧に伴う腎障害を来した2例

    荒田夕佳, 北川正史, 垣尾勇樹, 加藤綾子, 山成俊夫, 田邊克幸, 森永裕士, 内田治仁, 喜多村真治, 前島洋平, 杉山斉, 和田淳

    日本腎臓学会誌   56 ( 6 )   2014

  • 尿酸代謝におけるUp-to-Date(第8回) 尿酸とフルクトース

    仲川 孝彦, 中山 隆弘, 小杉 智規, 田村 好古, 北川 渡, 田邊 克幸, 佐藤 和一, Johnson Richard J.

    医薬の門   53 ( 2 )   68 - 73   2013.5

     More details

    Language:Japanese   Publisher:鳥居薬品(株)  

    臨床検討にて、近年のフルクトース消費増加とメタボリックシンドローム発症の間に相関を認める。また動物モデルにおいても、フルクトースにより、初期には高尿酸血症を伴う高血圧、高中性脂肪血症、インスリン抵抗性、腎臓尿細管障害を認め、晩期にはインスリン分泌低下や脂肪肝の発症を認める。しかしながら、高尿酸血症治療により初期のメタボリックシンドローム様症状は軽減されうる。最近のわれわれの実験結果を中心に、メタボリックシンドロームにおけるフルクトースと尿酸の役割を紹介したい。(著者抄録)

    researchmap

  • 急性腎不全で発症し透析を離脱し得たSLEの1例

    大西章史, 森永裕士, 赤木滋, 北川正史, 井上章子, 寺見直人, 山成俊夫, 辻憲二, 氏家はる代, 小川愛由, 中山和典, 綿谷博雪, 井上淳子, 田邊克幸, 杉山斉, 槇野博史

    日本腎臓学会誌   55 ( 6 )   2013

  • AN69膜と酢酸フリー透析剤は炎症を抑制し血管内皮機能を改善させる

    中本成美, 喜多村真治, 白花哲也, 齋藤和輝, 田村尚三, 家木裕司, 田邊克幸, 長尾俊彦

    日本透析医学会雑誌   46 ( Supplement 1 )   2013

  • 患者の訴えに傾聴し重複腫瘍を発見し治療しえた透析患者の一例

    釜地智子, 喜多村真治, 中川拓也, 細川香, 田邊克幸, 長尾俊彦

    日本透析医学会雑誌   46 ( Supplement 1 )   2013

  • 統合失調症の妻と二人暮らしの透析患者への支援の試み

    細川香, 喜多村真治, 中川拓也, 釜地智子, 田邊克幸, 長尾俊彦

    日本透析医学会雑誌   46 ( Supplement 1 )   2013

  • The 2009 Okayama Medical Association Awards: Vasohibin-1, a negative feedback regulator of angiogenesis, ameliorates renal alterations in a mouse model of diabetic nephropathy

    那須 達世, 前島 洋平, 木野村 賢, 川原(広越, 久美子, 田邊 克幸, 杉山 斉, 園田 光, 佐藤 靖史, 槇野 博史

    Journal of Okayama Medical Association   123 ( 1 )   19 - 25   2011.4

     More details

    Language:Japanese   Publisher:岡山医学会  

    DOI: 10.4044/joma.123.19

    CiNii Article

    CiNii Books

    researchmap

  • 血管新生関連因子の遺伝子導入アプローチを用いた腹膜線維化進展機序の解明と新規治療法開発の基礎的検討.

    前島洋平, 田邉克幸, 杉山 斉, 槇野博史

    腎と透析   69   142 - 145   2010

     More details

  • PREVEND IT Prevention of Renal and Vascular Endstage Disease Intervention Trial.

    田邉克幸, 前島洋平, 槇野博史

    DATA UPDATE 循環系 第4版   344 - 345   2009

     More details

  • ONO-1301による上皮間葉系移行(EMT)制御を介する尿細管間質病変抑制効果の検討

    那須達世, 前島洋平, 斎藤大輔, 田邊克幸, 三宅剛平, 山崎浩子, ス レティ, 喜多村真治, 杉山斉, 酒井芳紀, 槇野博史

    日本腎臓学会誌   51 ( 3 )   2009

  • ONO-1301による1型糖尿病性腎症治療効果の検討

    山崎浩子, 前島洋平, 那須達世, 斎藤大輔, 田邊克幸, 三宅剛平, ス レテイ, 喜多村真治, 杉山斉, 酒井芳紀, 槇野博史

    日本腎臓学会誌   51 ( 3 )   2009

  • Vasohibin-1による糸球体足細胞形質維持作用を介する糖尿病性腎症進展抑制機序の検討

    斎藤大輔, 前島洋平, 那須達世, 山崎浩子, 田邊克幸, 三宅剛平, ス レティ, 喜多村真治, 杉山斉, 園田光, 佐藤靖史, 槇野博史

    日本腎臓学会誌   51 ( 3 )   2009

  • 腹膜再生プログラムの進歩 血管新生抑制因子vasohibinによる腹膜硬化症抑制効果の検討

    田邊 克幸, 前島 洋平, 那須 達世, 高沢 有紀, 木野村 賢, 広越 久美子, 井上 達之, 斉藤 大輔, 杉山 斉, 園田 光, 佐藤 靖史, 槇野 博史

    腎と透析   65 ( 別冊 腹膜透析2008 )   84 - 87   2008.8

     More details

    Language:Japanese   Publisher:(株)東京医学社  

    腹膜硬化症モデルマウスを用いてvasohibinの効果を組織学的、免疫組織化学的に検討した。結果、vasohibinは抗血管新生作用、抗炎症作用、抗線維化作用を介して腹膜硬化症の進展を抑制することが示唆された。

    researchmap

  • IgA腎症に対する扁桃摘出術・ステロイドパルス療法非寛解症例の検討

    井上達之, 杉山斉, 瀧上慶一, 森永裕士, 田邊克幸, 喜多村真治, 赤木滋, 佐田憲映, 前島洋平, 槇野博史

    日本腎臓学会誌   50 ( 6 )   2008

  • 多彩な自己抗体を有し膜性腎症と半月体形成性糸球体腎炎を合併した1症例

    田邊克幸, 佐田憲映, 井上達之, 木野村賢, 喜多村真治, 前島洋平, 杉山斉, 槇野博史

    日本腎臓学会誌   50 ( 6 )   2008

  • 診療controversy medical decision makingのために ループス腎炎に対する免疫抑制療法 慎重な立場から

    田邊 克幸, 佐田 憲映, 槇野 博史

    内科   99 ( 4 )   697 - 700   2007.4

     More details

    Language:Japanese   Publisher:(株)南江堂  

    researchmap

  • シスプラチン誘導急性腎不全モデルにおけるラット腎幹/前駆細胞(rKS56)治療効果の検討

    木野村賢, 喜多村真治, 田邊克幸, 一瀬邦弘, 広越久美子, 高沢有紀, 来山浩之, 那須達世, 杉山斉, 山崎康司, 菅谷健, 前島洋平, 槇野博史

    Organ Biology   14 ( 3 )   2007

  • わが国の慢性腎臓病(CKD)対策の最前線 CKDの定義と分類

    田邊 克幸, 前島 洋平, 槇野 博史

    腎臓   29 ( 2 )   78 - 81   2006.10

     More details

    Language:Japanese   Publisher:(公財)日本腎臓財団  

    researchmap

  • NM-3による糖尿病腎症進展抑制機序の検討

    一瀬邦弘, 前島洋平, 山本佳彦, 縣直樹, 來山浩之, 高沢有紀, 木野村賢, 広越久美子, 田邊克幸, 杉山斉, 山崎康司, 槙野博史

    日本腎臓学会誌   48 ( 3 )   2006

  • アデノウイルスを用いたangiopoietin-1遺伝子治療による尿細管間質病変制御効果の検討

    高沢有紀, 前島洋平, 一瀬邦弘, 田邊克幸, 来山浩之, 広越久美子, 木野村賢, 山本佳彦, 杉山斉, 伊藤克礼, 滝正樹, 藤原俊義, 濱田洋文, 槇野博史

    日本腎臓学会誌   48 ( 3 )   2006

  • 血管新生抑制因子endostatin peptideによる腹膜硬化症抑制効果の検討

    田邊克幸, 前島洋平, 一瀬邦弘, 高沢有紀, 來山浩之, 広越久美子, 木野村賢, 杉山斉, 槇野博史

    日本腎臓学会誌   48 ( 3 )   2006

  • シスプラチン誘導急性腎不全モデルにおけるラット腎幹/前駆細胞(rKS56)治療効果の検討

    木野村賢, 前島洋平, 喜多村真治, 一瀬邦弘, 高沢有紀, 來山浩之, 広越久美子, 田邉克幸, 菅谷健, 山崎康司, 杉山斉, 槇野博史

    日本腎臓学会誌   48 ( 3 )   2006

  • 悪性腎硬化症を呈した2型糖尿病の1例

    中尾 一志, 市川 晴夫, 田邊 克幸, 矢野 愛, 来山 浩之, 清田 綾, 和田 淳, 四方 賢一, 槇野 博史

    糖尿病   46 ( 3 )   289 - 289   2003.3

     More details

    Language:Japanese   Publisher:(一社)日本糖尿病学会  

    researchmap

▼display all

Presentations

  • SMAP法における出口部作成時カテーテル閉塞に関する検討

    竹内英実, 浅川知彦, 岡本修吾, 西村慎吾, 田邊克幸, 森永裕士, 内田治仁, 荒木元朗, 和田淳

    第30回日本腹膜透析医学会  2024.11.16 

     More details

    Event date: 2024.11.16 - 2024.11.17

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Temporal and Apparent Decrease of Creatinine-Derived eGFR in the Patients with Cancer Treated with Poly ADP-Ribose Polymerase Inhibitors

    Shiho Morimoto, Yasuhiro Onishi, Saori Ariki, Hiroshi Morinaga, Katsuyuki Tanabe, Haruhito A Uchida, Yoshito Zamami, Hisashi Masuyama, Motoo Araki, Jun Wada

    American Society of Nephrology Kidney Week 2024  2024.10.25 

     More details

    Event date: 2024.10.23 - 2024.10.27

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 原発性アルドステロン症を呈する2型糖尿病を合併した慢性腎臓病患者に対してフィネレノンを投与した1例

    浅川知彦, 大西康博, 寺坂友博, 櫻武敬真, 片山勝喜, 岡本修吾, 内山奈津美, 竹内英実, 梅林亮子, 田邊克幸, 森永裕士, 内田治仁, 和田淳

    第46回日本高血圧学会  2024.10.14 

     More details

    Event date: 2024.10.12 - 2024.10.14

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 膜性増殖性糸球体腎炎様の病理像を呈しGd-IgA1抗体染色が診断に有用であったIgA腎症の一例

    金澤実由, 辻憲二, 三宅広将, 森本志帆, 久保田菜月, 青木亮弥, 須江美裕, 中納弘幸, 田邊克幸, 和田淳

    第54回日本腎臓学会西部学術大会  2024.10.6 

     More details

    Event date: 2024.10.5 - 2024.10.6

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 不全型Behcet病にみられた好中球浸潤を伴う急性尿細管間質性腎炎の一例

    内田成彦, 田中景子, 三宅広将, 久保田菜月, 森本志帆, 志田原健太, 勝山隆行, 田邊克幸, 和田淳

    第54回日本腎臓学会西部学術大会  2024.10.5 

     More details

    Event date: 2024.10.5 - 2024.10.6

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Preventive strategy with vasohibin-2-targeting peptide vaccine against diabetic kidney disease

    Yuri Nakashima, Katsuyuki Tanabe, Takato Nakadoi, Tomoyo Mifune, Hironori Nakagami, Yasufumi Sato, Jun Wada

    Kidney Health in Aging and Aged Societies: JSN/ERA Symposium  2024.9.15 

     More details

    Event date: 2024.9.14 - 2024.9.15

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 岡山市CKDネットワーク(OCKD-NET) 2の登録2年後のデータ解析

    田中景子, 内田治仁, 大西康博, 岡本修吾, 竹内英実, 辻憲二, 田邊克幸, 森永裕士, 太田康介, 丸山啓輔, 大城義之, 森岡茂, 瀧上慶一, 蒲生直幸, 杉山斉, 和田淳

    第67回日本腎臓学会  2024.6.30 

     More details

    Event date: 2024.6.28 - 2024.6.30

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 医学生教育における腎生検シミュレーターを用いた腎生検実習の意義

    辻憲二, 大西康博, 岡本修吾, 田中景子, 竹内英実, 田邊克幸, 森永裕士, 内田治仁, 和田淳

    第67回日本腎臓学会  2024.6.29 

     More details

    Event date: 2024.6.28 - 2024.6.30

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • CDK4/6阻害薬による血清クレアチニン値上昇に関する後方視的検討

    有木沙織, 大西康博, 森本志帆, 田邊克幸, 森永裕士, 内田治仁, 座間味義人, 枝園忠彦, 豊岡伸一, 和田淳

    第67回日本腎臓学会  2024.6.29 

     More details

    Event date: 2024.6.28 - 2024.6.30

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 糖尿病性腎症の進行におけるVasohibin-2発現増加の意義の検討

    中土井崇人, 田邊克幸, 中島有理, 佐藤靖史, 和田淳

    第67回日本腎臓学会  2024.6.29 

     More details

    Event date: 2024.6.28 - 2024.6.30

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 腎病理所見におけるChronicity scoreに関する検証

    大西康博, 杉山斉, 三瀬広記, 田邊克幸, 森永裕士, 内田治仁, 和田淳

    第67回日本腎臓学会  2024.6.28 

     More details

    Event date: 2024.6.28 - 2024.6.30

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 私の透析ー透析患者の血糖管理ー

    和田淳, 田原稔久, 大西康博, 野島一郎, 森永裕士, 田邊克幸, 小林直哉, 御舩朋代, 大西学

    第69回日本透析医学会  2024.6.9 

     More details

    Event date: 2024.6.7 - 2024.6.9

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • Fetuin-Aの糖尿病腎症進展及びバイオマーカーとしての意義

    三瀬広記, 中司敦子, 田邊克幸, 和田淳

    第69回日本透析医学会  2024.6.9 

     More details

    Event date: 2024.6.7 - 2024.6.9

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 大学病院と市中病院における透析内シャント設置術の患者背景及び実施術式に関する比較と考察

    藤井泰宏, 竹内英実, 岡本修吾, 浅川知彦, 和田淳, 加藤源太郎, 井上善紀, 倉田裕次, 黒子洋介, 小松弘明, 枝木大治, 徳田雄平, 山本修三, 田蒔基行, 西岡聡, 田蒔昌憲, 田蒔正治, 田邊克幸, 大澤晋, 笠原真吾

    第69回日本透析医学会  2024.6.7 

     More details

    Event date: 2024.6.7 - 2024.6.9

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 当院における生体腎移植ドナーの術後フォローアップ状況

    山野井友昭, 西村慎吾, 関戸崇了, 吉永香澄, 丸山雄樹, 定平卓也, 別宮謙介, 枝村康平, 小林知子, 小林泰之, 大西康博, 竹内英実, 田邊克幸, 森永裕士, 荒木元朗

    第57回日本臨床腎移植学会  2024.2.16 

     More details

    Event date: 2024.2.14 - 2024.2.16

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 当院における先行的生体腎移植の検討

    吉永香澄, 関戸崇了, 丸山雄樹, 山野井友昭, 西村慎吾, 富永悠介, 定平卓也, 片山聡, 岩田健宏, 大西康博, 竹内英実, 田邊克幸, 森永裕士, 和田淳, 枝村康平, 小林知子, 小林泰之, 荒木元朗

    第57回日本臨床腎移植学会  2024.2.16 

     More details

    Event date: 2024.2.14 - 2024.2.16

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 家族性高コレステロール血症の妊婦に対してLDLアフェレーシスを妊娠中も安全に継続できた1例

    櫻武敬真, 内田治仁, 奥山由加, 浅川知彦, 岡本修吾, 大西康博, 内山奈津美, 藤原千尋, 田中景子, 竹内英実, 梅林亮子, 田邊克幸, 森永裕士, 和田淳

    第32回中国腎不全研究会  2023.12.3 

     More details

    Event date: 2023.12.3

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • ANCA関連血管炎による急速進行性腎炎症候群を呈し血液透析開始後に非外傷性腹直筋血腫を発症した1例

    中納弘幸, 竹内英実, 森本志帆, 寺嶋悠也, 岡本修吾, 大西康博, 田中景子, 勝山隆行, 辻憲二, 田邊克幸, 森永裕士, 宇賀麻由, 冨田晃司, 平木隆夫, 内田治仁, 和田淳

    第32回中国腎不全研究会  2023.12.3 

     More details

    Event date: 2023.12.3

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 血液透析患者において持続血糖モニタリング(CGM)により血糖改善が得られた2症例

    田原稔久, 大西康博, 御舩朋代, 大西学, 小林直哉, 櫻武敬真, 森本志帆, 岡田梨乃, 杉谷宗一郎, 野島一郎, 森永裕士, 田邊克幸, 内田治仁, 中司敦子, 江口潤, 和田淳

    第32回中国腎不全研究会  2023.12.3 

     More details

    Event date: 2023.12.3

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 平滑筋肉腫の両側腎臓への転移に対して両腎摘出術を契機に血液透析導入とした一例

    浅川知彦, 竹内英実, 岡本修吾, 大西康博, 田中景子, 辻憲二, 田邊克幸, 森永裕士, 内田治仁, 和田淳

    第32回中国腎不全研究会  2023.12.3 

     More details

    Event date: 2023.12.3

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Greater Variability in eGFR Is Associated with CKD Progression: A Retrospective Japanese Nationwide Database Study CKD

    Yasuhiro Onishi, Hajime Nagasu, Kenji Tsuji, Katsuyuki Tanabe, Hiroshi Morinaga, Haruhito A. Uchida, Yuichiro Yano, Naoki Kashihara, Jun Wada

    American Society of Nephrology Kidney Week 2023  2023.11.3 

     More details

    Event date: 2023.11.2 - 2023.11.5

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 腎糸球体ポドサイトにおける細胞骨格ダイナミクスの解明

    竹居孝二, 阿部匡史, 竹田哲也, 田邊克幸, 山田浩司

    第96回日本生化学会  2023.11.1 

     More details

    Event date: 2023.10.31 - 2023.11.2

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Bechet病の経過中にIgA腎症を合併し、ステロイド療法とコルヒチン併用により蛋白尿の大幅な改善を認めた一例

    浅川知彦, 内田治仁, 片山祐, 田中景子, 竹内英実, 辻憲二, 梅林亮子, 田邊克幸, 森永裕士, 和田淳

    第53回日本腎臓学会西部学術大会  2023.10.7 

     More details

    Event date: 2023.10.7 - 2023.10.8

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 糖尿病性腎症へのLDLアフェレシスを考える

    田邊克幸, 宮田仁美

    第53回日本腎臓学会西部学術大会  2023.10.7 

     More details

    Event date: 2023.10.7 - 2023.10.8

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • PARP阻害薬による血清クレアチニン値上昇に関する後方視的検討

    森本志帆, 大西康博, 有木沙織, 田邊克幸, 森永裕士, 内田治仁, 座間味義人, 増山寿, 豊岡伸一, 荒木元朗, 大塚基之, 和田淳

    第53回日本腎臓学会西部学術大会  2023.10.7 

     More details

    Event date: 2023.10.7 - 2023.10.8

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Cronkhite-Canada症候群に膜性腎症を合併した1例

    中納弘幸, 森本志帆, 辻憲二, 田邊克幸, 内田治仁, 和田淳

    第53回日本腎臓学会西部学術大会  2023.10.7 

     More details

    Event date: 2023.10.7 - 2023.10.8

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 腹膜透析導入後に横隔膜交通症と診断され胸腔鏡下横隔膜縫縮術を施行し、腹膜透析が可能となった一例

    中納弘幸, 森本志帆, 辻憲二, 森永裕士, 田邊克幸, 和田淳

    第29回日本腹膜透析医学会  2023.10.1 

     More details

    Event date: 2023.9.30 - 2023.10.1

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 免疫学的ハイリスク腎移植における低用量リツキシマブを用いた脱感作療法とサイトメガロウイルス感染症:5年間の追跡調査

    吉永香澄, 関戸崇了, 丸山雄樹, 山野井友昭, 西村慎吾, 大西康博, 竹内英実, 田邊克幸, 森永裕士, 枝村康平, 小林知子, 小林泰之, 和田淳, 荒木元朗

    第59回日本移植学会  2023.9.23 

     More details

    Event date: 2023.9.21 - 2023.9.23

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 当院における腎移植後悪性腫瘍の検討

    山野井友昭, 西村慎吾, 関戸崇了, 吉永香澄, 丸山雄樹, 定平卓也, 枝村康平, 小林知子, 小林泰之, 大西康博, 竹内英実, 田邊克幸, 森永裕士, 和田淳, 荒木元朗

    第59回日本移植学会  2023.9.22 

     More details

    Event date: 2023.9.21 - 2023.9.23

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 小児期からLDLアフェレシスを継続中の家族性高コレステロール血症(ホモ接合体)患者で、妊娠中も安全にアフェレシスを継続できた1例

    内田治仁, 奥山由加, 藤原千尋, 竹内英実, 梅林亮子, 田邊克幸, 和田淳

    第55回日本動脈硬化学会  2023.7.9 

     More details

    Event date: 2023.7.8 - 2023.7.9

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • SDM-Q-9を用いた療法選択の質の評価と維持透析期QOLに関する検討

    大西康博, 森永裕士, 田邊克幸, 内田治仁, 和田淳, 小林直哉, 西田千夏, 石原裕之, 横山智久, 小橋雄一, 杉山斉, 池田美世, 笠原由美子, 齋藤信也

    第68回日本透析医学会  2023.6.18 

     More details

    Event date: 2023.6.16 - 2023.6.18

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 岡山市CKDネットワーク(OCKD-NET)におけるCKD病診連携12年後の追跡調査

    大西康博, 内田治仁, 田中景子, 岡本修吾, 竹内英実, 辻憲二, 田邊克幸, 森永裕士, 喜多村真治, 前島洋平, 太田康介, 丸山啓輔, 大城義之, 森岡茂, 瀧上慶一, 蒲生直幸, 杉山斉, 和田淳

    第66回日本腎臓学会  2023.6.11 

     More details

    Event date: 2023.6.9 - 2023.6.11

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 岡山市CKDネットワーク(OCKD-NET)2の登録時データ解析~OCKD-NET1との比較

    田中景子, 内田治仁, 大西康博, 岡本修吾, 竹内英実, 辻憲二, 田邊克幸, 森永裕士, 太田康介, 丸山啓輔, 大城義之, 森岡茂, 瀧上慶一, 蒲生直幸, 杉山斉, 和田淳

    第66回日本腎臓学会  2023.6.10 

     More details

    Event date: 2023.6.9 - 2023.6.11

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 医学生に対する腎セミナー開催についての検討

    辻憲二, 岡本修吾, 大西康博, 田中景子, 竹内英実, 田邊克幸, 森永裕士, 内田治仁, 喜多村真治, 和田淳

    第66回日本腎臓学会  2023.6.10 

     More details

    Event date: 2023.6.9 - 2023.6.11

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • オラパリブ投与開始後に⾎清クレアチニン値の上昇を認めたBRCA遺伝⼦変異陽性膵癌の⼀例

    山崎珠里亜, 大⻄康博, 田邊克幸, 森本志帆, 中納弘幸, 有木沙織, 森永裕士, 内田治仁, 加藤博也, 和田淳

    第128回日本内科学会中国地方会  2023.5.21 

     More details

    Event date: 2023.5.21

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 当院におけるCOVID-19感染症の検討

    吉永香澄, 丸山雄樹, 山野井友昭, 西村慎吾, 大西康博, 竹内英美, 田邊克幸, 森永裕士, 枝村康平, 小林知子, 小林泰之, 渡辺豊彦, 荒木元朗

    第56会日本臨床腎移植学会  2023.2.11 

     More details

    Event date: 2023.2.11 - 2023.2.12

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 糖尿病性腎症における血管新生関連因子の治療標的としての役割 Invited

    田邊克幸, 佐藤靖史, 中神啓徳, 和田淳

    第33回日本糖尿病性腎症研究会  2022.12.3 

     More details

    Event date: 2022.12.3 - 2022.12.4

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • Vasohibin-2を標的とした糖尿病性腎症に対する新規治療の開発

    田邊克幸

    第45回日本分子生物学会  2022.12.1 

     More details

    Event date: 2022.11.30 - 2022.12.2

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    researchmap

  • 腎不全療法選択説明と腹膜透析選択率・緊急導入の検討

    大西康博, 森永裕士, 杉山斉, 岡本修吾, 竹内英実, 田邊克幸, 内田治仁, 笠原由美子, 池田美世, 和田淳

    第28回日本腹膜透析医学会  2022.11.26 

     More details

    Event date: 2022.11.26 - 2022.11.27

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • SDM-Q-9を用いた療法選択の質の評価と腹膜透析選択率の検討

    大西康博, 森永裕士, 小林直哉, 田邊克幸, 内田治仁, 笠原由美子, 池田美世, 片山智恵, 齋藤信也, 和田淳

    第28回日本腹膜透析医学会  2022.11.26 

     More details

    Event date: 2022.11.26 - 2022.11.27

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 尿細胞診によるBKウイルス腎症の発症予測は尿沈渣で代替可能か

    関戸崇了, 荒木元朗, 吉永香澄, 山野井友昭, 丸山雄樹, 定平卓也, 西村慎吾, 枝村康平, 小林泰之, 田邊克幸, 竹内英実, 森永裕士, 和田淳, 柳井広之

    第58回日本移植学会  2022.10.15 

     More details

    Event date: 2022.10.13 - 2022.10.15

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 当院における腎移植後コロナウイルス感染症の臨床経過

    吉永香澄, 関戸崇了, 丸山雄樹, 山野井友昭, 西村慎吾, 竹内英実, 田邉克幸, 森永裕士, 内田治仁, 和田淳, 枝村康平, 小林知子, 小林泰之, 荒木元朗

    第58回日本移植学会  2022.10.14 

     More details

    Event date: 2022.10.13 - 2022.10.15

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • ゆで卵を用いた模擬腎生検:コロンブスの卵

    辻憲二, 田中景子, 竹内英実, 田邊克幸, 森永裕士, 木野村賢, 内田治仁, 喜多村真治, 杉山斉, 和田淳

    第65回日本腎臓学会  2022.6.11 

     More details

    Event date: 2022.6.10 - 2022.6.12

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 早期糖尿病性腎症に対するVasohibin-2を標的としたペプチドワクチン療法の有効性

    中島有理, 田邊克幸, 御舩朋代, 林宏樹, 中神啓徳, 杉山斉, 佐藤靖史, 和田淳

    第65回日本腎臓学会  2022.6.11 

     More details

    Event date: 2022.6.10 - 2022.6.12

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 岡山市CKDネットワーク(OCKD-NET)におけるCKD病診連携11年後の追跡調査

    大西康博, 内田 治仁, 竹内英実, 田中景子, 辻憲二, 田邊克幸, 森永裕士, 木野村賢, 喜多村真治, 前島洋平, 杉山斉, 太田康介, 丸山啓輔, 大城義之, 森岡茂, 瀧上慶一, 蒲生直幸, 和田淳

    第65回日本腎臓学会  2022.6.11 

     More details

    Event date: 2022.6.10 - 2022.6.12

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • テキストマイニングによる腎移植に関する症例報告論文の考察

    関戸崇了, 荒木元朗, 吉永香澄, 丸山雄樹, 山野井友昭, 定平卓也, 片山聡, 岩田健宏, 西村慎吾, 佐古智子, 枝村康平, 小林泰之, 渡部昌実, 渡邉豊彦, 田邊克幸, 竹内英実, 喜多村真治, 杉山斉, 和田淳, 那須保友

    第55回日本臨床腎移植学会  2022.2.24 

     More details

    Event date: 2022.2.23 - 2022.2.25

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 妊娠中に加温式リサキュレーション法を施行した家族性高コレステロール血症(ホモ接合体)の1例

    奥山由加, 内田治仁, 竹内英美, 高橋健作, 藤原千尋, 田邊克幸, 木野村賢, 和田淳

    第66回日本透析医学会  2021.6.5 

     More details

    Event date: 2021.6.4 - 2021.6.5

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Vasohibin-1及び2を標的とした糖尿病性腎症の治療戦略

    田邊克幸

    第15回Vasohibin研究会  2021.2.27 

     More details

    Event date: 2021.2.27

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 高血圧・糖尿病に焦点を当てたマージナルドナーからの生体腎移植

    吉永香澄, 荒木元朗, 関戸崇了, 和田里章悟, 丸山茂樹, 定平卓也, 窪田理沙, 西村慎吾, 佐古智子, 和田耕一郎, 枝村康平, 小林泰之, 竹内英実, 田邊克幸, 森永裕士, 杉山斉, 和田淳, 渡部昌実, 渡邉豊彦, 那須保友

    第54回日本臨床腎移植学会  2021.2.18 

     More details

    Event date: 2021.2.17 - 2021.2.19

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 血液透析を導入したチアノーゼ性成人先天性心疾患(ACHD)合併腎不全の2例

    木野村賢, 高橋謙作, 森岡朋代, 加納弓月, 川北智英子, 谷村智史, 田邊克幸, 和田淳

    第65回日本透析医学会  2020.11.2 

     More details

    Event date: 2020.11.2 - 2020.11.3

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 腎不全療法選択説明が緊急透析導入と療法選択に与える影響

    森永祐士, 笠原由美子, 井本紀子, 角川紫野, 矢田光子, 田邊克幸, 木野村賢, 大高望, 辻憲二, 北川正史, 内田治仁, 喜多村真治, 杉山斉, 和田淳

    第65回日本透析医学会  2020.11.2 

     More details

    Event date: 2020.11.2 - 2020.11.3

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 岡山市CKDネットワーク(OCKD-NET)におけるCKD病診連携9年後の追跡調査

    大西康博, 内田治仁, 大高望, 辻憲二, 田邊克幸, 森永裕士, 木野村賢, 喜多村真治, 前島洋平, 杉山斉, 太田康介, 丸山啓輔, 大城義之, 森岡茂, 大森一慶, 瀧上慶一, 蒲生直幸, 和田淳

    第63回日本腎臓学会  2020.8.21 

     More details

    Event date: 2020.8.19 - 2020.8.21

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 中四国地域におけるCKDおよびCVDの関連に関する前向きコホート研究;Kakusyo 3C Study:登録3年後の中間解析

    大高望, 内田治仁, 西脇麻里子, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    第63回日本腎臓学会  2020.8.20 

     More details

    Event date: 2020.8.19 - 2020.8.21

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 中四国地域におけるCKDおよびCVDの関連に関するコホート研究 Kakusyo 3C Study:登録3年後のCKD管理状況

    西脇麻里子, 内田治仁, 大高望, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田 淳

    第63回日本腎臓学会  2020.8.19 

     More details

    Event date: 2020.8.19 - 2020.8.21

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 慢性腎臓病における貧血管理〜Kakusyo 3C Studyからの検討

    内山奈津実, 内田治仁, 西脇麻里子, 大高望, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    第63回日本腎臓学会  2020.8.19 

     More details

    Event date: 2020.8.19 - 2020.8.21

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 生体腎移植後に発症したBKウイルス腎症の2例

    関戸崇了, 荒木元朗, 河村香澄, 和田里章悟, 丸山雄樹, 光井洋介, 窪田理沙, 西村慎吾, 和田耕一郎, 山下里美, 佐古智子, 枝村康平, 小林泰之, 渡邉豊彦, 加納弓月, 北川正史, 田邊克幸, 杉山斉, 和田淳, 那須保友

    第53回日本臨床腎移植学会  2020.2.21 

     More details

    Event date: 2020.2.19 - 2020.2.21

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • CMV初感染の腎移植レシピエントへのリツキシマブ投与の検討

    河村香澄, 荒木元朗, 関戸崇了, 和田里章悟, 丸山雄樹, 光井洋介, 窪田理沙, 西村慎吾, 和田耕一郎, 小林泰之, 渡邉豊彦, 加納弓月, 北川正史, 田邊克幸, 杉山斉, 和田淳, 那須保友

    第53回日本臨床腎移植学会  2020.2.20 

     More details

    Event date: 2020.2.19 - 2020.2.21

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 生体腎移植レシピエントにおけるCT値と骨密度の関係と推移

    丸山雄樹, 荒木元朗, 関戸崇了, 和田里章悟, 河村香澄, 光井洋介, 窪田理沙, 西村慎吾, 枝村康平, 小林泰之, 渡邉豊彦, 北川正史, 田邊克幸, 那須保友

    第53回日本臨床腎移植学会  2020.2.20 

     More details

    Event date: 2020.2.19 - 2020.2.21

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 生体腎移植後slow graft functionのリスク因子の検討

    和田里章悟, 荒木元朗, 河村香澄, 関戸崇了, 丸山雄樹, 光井洋介, 窪田理沙, 西村慎吾, 和田耕一郎, 小林泰之, 渡邉豊彦, 北川正史, 田邊克幸, 杉山斉, 和田淳, 那須保友

    第53回日本臨床腎移植学会  2020.2.20 

     More details

    Event date: 2020.2.19 - 2020.2.21

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 腎虚血再灌流障害における好中球動態の2光子励起顕微鏡を用いた解析

    丸山雄樹, 荒木元朗, 城所研吾, 和田耕一郎, 河村香澄, 光井洋介, 定平卓也, 窪田理沙, 西村慎吾, 渡部昌実, 渡邉豊彦, 田邊克幸, 和田淳, 柏原直樹, 那須保友

    第55回日本移植学会  2019.10.12 

     More details

    Event date: 2019.10.10 - 2019.10.12

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • A Consultation for Decision Making Related to Renal Replacement Therapy May Reduce a Risk for an Urgent Dialysis Initiation

    Yumiko Kasahara, Hiroshi Morinaga, Noriko Imoto, Mitsuko Yata, Katsuyuki Tanabe, Masaru Kinomura, Hitoshi Sugiyama, Jun Wada

    9th Asia Pacific Chapter Meeting of International Society for Peritoneal Dialysis  2019.9.7 

     More details

    Event date: 2019.9.5 - 2019.9.7

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Exogenous Vasohibin-2 Does Not Influence Angiotensin II-induced Abdominal Aortic Aneurysms Formation in Either Normolipidemic or Apolipoprotein E-Deficient Mice

    Nozomu Otaka, Haruhito A. Uchida, Yoshiko Hada, Hidemi Takeuchi, Yuki Kakio, MIchihiro Okuyama, Ryoko Umebayashi, Katsuyuki Tanabe, Yasufumi Sato, Jun Wada

    Arteriosclerosis, Thrombosis, and Vascular Biology 2018  2018.5.10 

     More details

    Event date: 2018.5.10 - 2018.5.12

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 岡山大学泌尿器科における移植医と腎臓内科医との連携体制

    有吉勇一, 山下里美, 荒木元朗, 光井洋介, 吉岡貴史, 北川正史, 田邊克幸

    第49回日本臨床腎移植学会  2016.3.24 

     More details

    Event date: 2016.3.23 - 2016.3.25

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 重炭酸腹膜透析液使用前後における血中重炭酸イオン濃度の経時的変化

    山成俊夫, 杉山斉, 森永裕士, 大西章史, 田邊克幸, 菊本陽子, 木野村賢, 和田淳

    第21回日本腹膜透析医学会  2015.11.28 

     More details

    Event date: 2015.11.28 - 2015.11.29

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 腎炎所見が紫斑に先行したIgA血管炎(IgAV)の1例

    澁藤宣行, 木野村賢, 北川正史, 田邊克幸, 喜多村真治, 杉山斉, 和田淳

    第45回日本腎臓学会西部学術大会  2015.10.23 

     More details

    Event date: 2015.10.23 - 2015.10.24

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 生体腎移植におけるリツキシマブの効果と有害事象の検討

    荒木元朗, 和田耕一郎, 宗石理沙, 吉岡貴史, 有吉勇一, 山下里美, 小林泰之, 江原伸, 渡辺豊彦, 那須保友, 田邊克幸, 北川正史, 杉山斉, 和田淳

    第51回日本移植学会  2015.10.3 

     More details

    Event date: 2015.10.1 - 2015.10.3

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 当院で施行した先行的腎移植(preemptive renal transplantation:PRT)の検討

    光井洋介, 荒木元朗, 山下里美, 吉岡貴史, 有吉勇一, 和田耕一郎, 小林泰之, 江原伸, 渡辺豊彦, 那須保友, 北川正史, 田邊克幸, 杉山斉, 和田淳

    第51回日本移植学会  2015.10.2 

     More details

    Event date: 2015.10.1 - 2015.10.3

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 肺高血圧症を合併する全身性強皮症への血液透析導入例

    田邊克幸, 田中景子, 竹内英実, 澁藤宣行, 大西章史, 益田加奈, 荒田夕佳, 寺見直人, 秋山愛由, 木野村賢, 藤井泰宏, 大澤晋, 杉山斉, 和田淳

    第60回日本透析医学会  2015.6.28 

     More details

    Event date: 2015.6.26 - 2015.6.28

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Assisted PDの現状~アンケート調査と今後の課題~

    森永裕士, 杉山斉, 山成俊夫, 田邊克幸, 木野村賢, 赤木滋, 木原隆司, 森本尚孝, 中尾一志, 丸山啓輔, 浅野健一郎, 太田康介, 山﨑康司, 福島正樹, 西村誠明, 平松信, 和田淳

    第60回日本透析医学会  2015.6.27 

     More details

    Event date: 2015.6.26 - 2015.6.28

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • PDカテーテル挿入術の実態調査~アンケート集計結果より~

    大西章史, 森永裕士, 杉山斉, 山成俊夫, 田邊克幸, 木野村賢, 森本尚孝, 赤木滋, 中尾一志, 丸山啓輔, 関川孝司, 太田康介, 浅野健一郎, 山崎康司, 福島正樹, 西村誠明, 平松信, 和田淳

    第60回日本透析医学会  2015.6.27 

     More details

    Event date: 2015.6.26 - 2015.6.28

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 多発性嚢胞腎における指定難病重症度分類の評価に関する検討

    大西章史, 杉山斉, 田中景子, 山成俊夫, 秋山愛由, 北川正史, 森永祐士, 井上達之, 菊本陽子, 田邊克幸, 木野村賢, 花山宣久, 内田治仁, 喜多村真治, 和田淳

    第58回日本腎臓学会  2015.6.6 

     More details

    Event date: 2015.6.5 - 2015.6.7

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 血管新生促進因子Vasohibin-2欠損が糖尿病性腎症の進展に及ぼす効果に関する検討

    益田加奈, 大森はる代, 田邊克幸, 雛元紀和, 杉山斉, 佐藤靖史, 前島洋平, 和田淳

    第58回日本腎臓学会  2015.6.6 

     More details

    Event date: 2015.6.5 - 2015.6.7

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 膀胱拡大術を先行した生体腎移植の一例

    和田耕一郎, 荒木元朗, 宗石理沙, 吉岡貴史, 有吉勇一, 藤尾圭, 佐々木克己, 小林泰之, 江原伸, 渡邉豊彦, 那須保友, 有森千聖, 野田卓男, 山成俊夫, 北川正史, 田邊克幸, 森永裕士, 杉山斉, 和田淳, 公文裕巳

    第48回日本臨床腎移植学会  2015.2.5 

     More details

    Event date: 2015.2.4 - 2015.2.6

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Renal Tubulointerstitial Distribution of Vasohibin-2 and Its Association with Clinicopathological Parameters in Patients with Renal Disorders

    Arata Y, Watatani H, Omori H, Masuda K, Tanabe K, Wada J, Sugiyama H, Kanomata N, Sato Y, MaeshimaY

    American Society of Nephrology Kidney Week 2014  2014.11.14 

     More details

    Event date: 2014.11.11 - 2014.11.16

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 高度進行性強皮症に対し自家静脈内シャントを行った一症例

    藤井泰宏, 大澤晋, 黒子洋介, 川畑拓也, 増田善逸, 小谷恭弘, 吉積功, 新井禎彦, 笠原真悟, 堀尾直裕, 後藤拓哉, 田邊克幸, 佐野俊二

    第55回日本脈管学会  2014.11.1 

     More details

    Event date: 2014.10.30 - 2014.11.1

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 降圧療法により改善をみた悪性高血圧を伴う腎障害を来した2例

    荒田夕佳, 北川正史, 垣尾勇樹, 加藤綾子, 山成俊夫, 田邊克幸, 森永裕士, 内田治仁, 喜多村真治, 前島洋平, 杉山斉, 和田淳

    第44回日本腎臓学会西部学術大会  2014.10.4 

     More details

    Event date: 2014.10.3 - 2014.10.4

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • ファブリー腎症による腎不全に対して酵素補充療法と腹膜透析を継続中、重度の僧帽弁閉鎖不全症を合併した1例

    山成俊夫, 杉山斉, 森永裕士, 菊本陽子, 大西章史, 北川正史, 秋山愛由, 田邊克幸, 喜多村真治, 前島洋平, 槇野博史

    第20回日本腹膜透析医学会  2014.9.6 

     More details

    Event date: 2014.9.6 - 2014.9.7

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 大網巻絡を伴うCAPDカテーテル位置異常に対し、整復および非吸収糸を用いて骨盤腹膜に固定を行った1例

    大西章史, 森永裕史, 井上章子, 荒木亮一, 山成俊夫, 田邊克幸, 篠浦先, 信岡大輔, 杉山斉, 槇野博史

    第20回日本腹膜透析医学会  2014.9.6 

     More details

    Event date: 2014.9.6 - 2014.9.7

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 岡山市国保特定健診受診者における健診フォローアップ事業結果について

    綿谷博雪, 前島洋平, 雛元紀和, 氏家はる代, 田邊克幸, 益田加奈, 杉山斉, 山本静子, 頼藤貴志, 土居弘幸, 中瀬克己, 槇野博史

    第57回日本腎臓学会  2014.7.6 

     More details

    Event date: 2014.7.4 - 2014.7.6

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 岡山市CKDネットワーク(OCKD-NET)におけるCKD病診連携3年後の追跡調査

    氏家はる代, 前島洋平, 山崎浩子, 田邊克幸, 杉山斉, 太田康介, 平松信, 大城義之, 森岡茂, 福島正樹, 槇野博史

    第57回日本腎臓学会  2014.7.5 

     More details

    Event date: 2014.7.4 - 2014.7.6

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 慢性腎臓病の経過において尿中Trefoil Factor 3の変化率はアルブミン尿の変化率と有意相関する

    山成俊夫, 杉山斉, 森永裕士, 大西章史, 小川愛由, 北川正史, 菊本陽子, 田邊克幸, 喜多村真治, 前島洋平, 小川大輔, 四方賢一, 大本安一, 槇野博史

    第57回日本腎臓学会  2014.7.4 

     More details

    Event date: 2014.7.4 - 2014.7.6

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • ファブリー病およびファブリー腎症に対する酵素補充療法の長期効果

    菊本陽子, 杉山斉, 大西章史, 山成俊夫, 小川愛由, 北川正史, 森永裕士, 田邊克幸, 喜多村真治, 前島洋平, 槇野博史

    第57回日本腎臓学会  2014.7.4 

     More details

    Event date: 2014.7.4 - 2014.7.6

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 慢性腎臓病におけるエピジェネティクスと酸化ストレスの関連に関する検討

    大西章史, 杉山斉, 山成俊夫, 小川愛由, 北川正史, 森永裕士, 菊本陽子, 田邊克幸, 内田治仁, 喜多村真治, 前島洋平, 槇野博史

    第57回日本腎臓学会  2014.7.4 

     More details

    Event date: 2014.7.4 - 2014.7.6

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 内因性血管新生促進因子Vasohibin-2欠損の糖尿病性腎症進展における意義についての検討

    氏家はる代, 前島洋平, 雛元紀和, 綿谷博雪, 田邊克幸, 益田加奈, 杉山斉, 佐藤靖史, 槇野博史

    第57回日本腎臓学会  2014.7.4 

     More details

    Event date: 2014.7.4 - 2014.7.6

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • ファブリー腎症による腎不全に対して酵素補充療法と共に腹膜透析を継続中の1例

    山成俊夫, 杉山斉, 森永裕士, 菊本陽子, 大西章史, 北川正史, 小川愛由, 田邊克幸, 喜多村真治, 前島洋平, 槇野博史

    第59回日本透析医学会  2014.6.15 

     More details

    Event date: 2014.6.13 - 2014.6.15

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 化学療法中に発生した血液透析を要する急性腎不全症例の検討

    田邊克幸, 田中景子, 小松原基, 大西章史, 寺見直人, 中山和典, 綿谷博雪, 益田加奈, 井上淳子, 山成俊夫, 森永裕士, 杉山斉, 槇野博史

    第59回日本透析医学会  2014.6.15 

     More details

    Event date: 2014.6.13 - 2014.6.15

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 激しい運動に伴いCAPDカテーテル位置異常をきたし整復および骨盤腹膜に固定を行った1例

    大西章史, 森永裕士, 井上章子, 荒木亮一, 山成俊夫, 田邊克幸, 篠浦先, 信岡大輔, 杉山斉, 槇野博史

    第59回日本透析医学会  2014.6.14 

     More details

    Event date: 2014.6.13 - 2014.6.15

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 高齢CKD患者の透析導入予後を考慮した保存期管理 Invited

    前島洋平, 田邊克幸, 槇野博史

    第59回日本透析医学会  2014.6.14 

     More details

    Event date: 2014.6.13 - 2014.6.15

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • ONO-1301はアデニン誘発慢性腎不全ラットの血管石灰化を抑制する

    綿谷博雪, 前島洋平, 雛元紀和, 氏家はる代, 田邊克幸, 益田加奈, 杉山斉, 酒井芳紀, 槇野博史

    第59回日本透析医学会  2014.6.14 

     More details

    Event date: 2014.6.13 - 2014.6.15

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 急性腎不全、高度肝障害と血小板減少を呈した重症レプトスピラ症の1例

    田中景子, 田邊克幸, 西井尚子, 瀧上慶一, 大西章史, 寺見直人, 山成俊夫, 中山和典, 綿谷博雪, 井上淳子, 益田加奈, 杉山斉, 槇野博史

    第59回日本透析医学会  2014.6.13 

     More details

    Event date: 2014.6.13 - 2014.6.15

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • PD腹膜炎診療の実態調査~アンケート集計結果の変遷と今後の課題~

    森永裕士, 杉山斉, 田邊克幸, 喜多村真治, 前島洋平, 赤木滋, 木原隆司, 森本尚孝, 秋山賢次, 中尾一志, 丸山啓輔, 木野村賢, 浅野健一郎, 山﨑康司, 福島正樹, 西村誠明, 平松信, 槇野博史

    第59回日本透析医学会  2014.6.13 

     More details

    Event date: 2014.6.13 - 2014.6.15

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Oral administration of a prostacyclin analog ONO-1301 ameliorates vascular calcification in a rat model of adenine-induced chronic kindey disease

    Watatani H, Maeshima Y, Hinamoto N, Ujike H, Tanabe K, Masuda K, Sugiyama H, Sakai Y, Makino H

    The 14th Asian Pacific Congress of Nephrology 2014  2014.5.17 

     More details

    Event date: 2014.5.14 - 2014.5.17

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Lack of vasohibin-1 exacerbates renal alteration induced by infusion of angiotensin-II

    Hinamoto N, Maeshima Y, Yamasaki H, Watatani H, Ujike H, Tanabe K, Masuda K, Sugiyama H, Sato Y, Makino H

    The 14th Asian Pacific Congress of Nephrology 2014  2014.5.15 

     More details

    Event date: 2014.5.14 - 2014.5.17

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 岡山市国保特定健診受診者におけるCKD有病リスク因子の検討と健診フォローアップ事業

    綿谷博雪, 前島洋平, 山崎浩子, 田邊克幸, 雛元紀和, 氏家はる代, 杉山斉, 山本静子, 頼藤貴志, 土居弘幸, 中瀬克己, 槇野博史

    第56回日本腎臓学会  2014.5.11 

     More details

    Event date: 2014.5.10 - 2014.5.12

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 生体腎移植におけるリツキシマブ使用症例の検討

    荒木元朗, 和田耕一郎, 有森千聖, 宗石理沙, 吉岡貴史, 有吉勇一, 小林泰之, 佐々木克己, 江原伸, 上原慎也渡邉豊彦, 那須保友, 公文裕巳, 森永裕士, 田邊克幸, 北川正史, 杉山斉, 和田淳, 槇野博史

    第47回日本臨床腎移植学会  2014.3.14 

     More details

    Event date: 2014.3.12 - 2014.3.14

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 内因性血管新生促進因子Vasohibin-2欠損の糖尿病性腎症進展における意義についての検討

    氏家はる代, 前島洋平, 雛元紀和, 綿谷博雪, 田邊克幸, 益田加奈, 杉山斉, 佐藤靖史, 槇野博史

    第28回日本糖尿病・肥満動物学会  2014.2.14 

     More details

    Event date: 2014.2.14 - 2014.2.15

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Therapeutic Effects of ONO-1301 on Vascular Calcification in a Rat Model of Adenine-Induced Chronic Kidney Disease

    Maeshima Y, Watatani H, Hinamoto N, Tanabe K, Masuda K, Ujike H, Sugiyama H, Sakai Y, Makino H

    American Society of Nephrology Kidney Week 2013  2013.11.8 

     More details

    Event date: 2013.11.5 - 2013.11.10

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Novel Prostacyclin Analog ONO-1301 (SR-ONO) Ameliorates AKI in a Rat Experimental Contrast-Induced Nephropathy Model

    Ujike H, Maeshima Y, Hinamoto N, Watatani H, Masuda K, Tanabe K, Sugiyama H, Sakai Y, Makino H

    American Society of Nephrology Kidney Week 2013  2013.11.7 

     More details

    Event date: 2013.11.5 - 2013.11.10

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Protective Effects of Endogenous Vasohibin-1 on Podocytes in Diabetic Nephropathy

    Hinamoto N, Maeshima Y, Watatani H, Ujike H, Tanabe K, Masuda K, Sugiyama H, Sato Y, Makino H

    American Society of Nephrology Kidney Week 2013  2013.11.7 

     More details

    Event date: 2013.11.5 - 2013.11.10

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 急性腎不全で発症し透析を離脱し得たSLEの1例

    大西章史, 森永裕士, 赤木滋, 北川正史, 井上章子, 寺見直人, 山成俊夫, 辻憲二, 氏家はる代, 小川愛由, 中山和典, 綿谷博雪, 井上淳子, 田邊克幸, 杉山斉, 槇野博史

    第43回日本腎臓学会西部学術大会  2013.10.11 

     More details

    Event date: 2013.10.11 - 2013.10.12

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 末期腎不全患者への治療法選択説明とShared Dicision Makingの認知度

    森永裕士, 杉山斉, 田邊克幸, 喜多村真治, 前島洋平, 赤木滋, 木原隆司, 森本尚孝, 秋山賢次, 開原正展, 橋本昌美, 中尾一志, 丸山啓補, 木野村賢, 浅野健一郎, 山﨑康司, 福島正樹, 西村誠明, 平松信, 槇野博史

    第19回日本腹膜透析医学会  2013.9.28 

     More details

    Event date: 2013.9.28 - 2013.9.29

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 重症心不全に対してイコデキストリン腹膜透析により体液管理を施行した1例

    大西章史, 杉山斉, 赤木滋, 井上章子, 垣尾勇樹, 荒田夕佳, 田邊克幸, 森永裕士, 河野晋久, 槇野博史

    第19回日本腹膜透析医学会  2013.9.28 

     More details

    Event date: 2013.9.28 - 2013.9.29

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • AN69膜と酢酸フリー透析剤は炎症を抑制し血管内皮機能を改善させる

    中本成美, 喜多村真治, 白花哲也, 齋藤和輝, 田村尚三, 家木裕司, 田邊克幸, 長尾俊彦

    第58回日本透析医学会  2013.6.23 

     More details

    Event date: 2013.6.21 - 2013.6.23

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 統合失調症の妻と二人暮らしの透析患者への支援の試み

    細川香, 喜多村真治, 中川拓也, 釜地智子, 田邊克幸, 長尾俊彦

    第58回日本透析医学会  2013.6.23 

     More details

    Event date: 2013.6.21 - 2013.6.23

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 中枢神経系原発悪性リンパ腫と診断された透析患者の一例

    赤木滋, 中山和典, 山成俊夫, 綿谷博雪, 井上淳子, 山崎浩子, 田邊克幸, 森永裕士, 槇野博史, 黒住和彦, 伊達勲

    第58回日本透析医学会  2013.6.21 

     More details

    Event date: 2013.6.21 - 2013.6.23

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • プロスタグランジン代謝産物(6keto-PGF1α)の透析患者における心血管イベント・総死亡の予知因子としての有用性の検討

    綿谷博雪, 前島洋平, 山崎浩子, 田邊克幸, 雛元紀和, 氏家はる代, 杉山斉, 松原龍也, 有元克彦, 真鍋康二, 瀧正史, 福島正樹, 酒井芳紀, 槇野博史

    第58回日本透析医学会  2013.6.21 

     More details

    Event date: 2013.6.21 - 2013.6.23

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 患者の訴えに傾聴し重複腫瘍を発見し治療しえた透析患者の一例

    釜地智子, 喜多村真治, 中川拓也, 細川香, 田邊克幸, 長尾俊彦

    第58回日本透析医学会  2013.6.21 

     More details

    Event date: 2013.6.21 - 2013.6.23

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Analysis on the mechanisms involved in aggravation if renal relterations in diabetic Vasohibin-1 knockout mice

    Maeshima Y, Hinamoto N, Yamasaki H, Watatani H, Ujike H, Tanabe K, Sugiyama H, Sato Y, Makino H

    International Society of Nephrology World Congress of Nephrology 2013  2013.6.1 

     More details

    Event date: 2013.5.31 - 2013.6.4

    Language:English   Presentation type:Poster presentation  

    researchmap

  • アデニン誘発慢性腎不全モデルにおけるONO-1301による血管石灰化抑制効果の検討

    綿谷博雪, 前島洋平, 山崎浩子, 田邊克幸, 雛元紀和, 氏家はる代, 杉山斉, 酒井芳紀, 槇野博史

    第56回日本腎臓学会  2013.5.12 

     More details

    Event date: 2013.5.10 - 2013.5.12

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 造影剤誘発急性腎障害モデルにおけるONO-1301による治療効果の検討

    氏家はる代, 前島洋平, 山崎浩子, 綿谷博雪, 雛元紀和, 田邊克幸, 杉山斉, 酒井芳紀, 槇野博史

    第56回日本腎臓学会  2013.5.11 

     More details

    Event date: 2013.5.10 - 2013.5.12

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 内在性血管新生制御因子Vasohibin-1の糖尿病性腎症進展抑制機序についての検討

    雛元紀和, 前島洋平, 山崎浩子, 綿谷博雪, 氏家はる代, 田邊克幸, 杉山斉, 佐藤靖史, 槇野博史

    第56回日本腎臓学会  2013.5.11 

     More details

    Event date: 2013.5.10 - 2013.5.12

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 虚血再還流モデルにおけるONO-1301による治療効果の検討

    山崎浩子, 前島洋平, 氏家はる代, 綿谷博雪, 雛元紀和, 田邊克幸, 杉山斉, 酒井芳紀

    第56回日本腎臓学会  2013.5.11 

     More details

    Event date: 2013.5.10 - 2013.5.12

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 当院CKD・CVD精査外来受診患者の検討:CVD精査の有用性

    雛元紀和, 前島洋平, 吉田賢司, 山崎浩子, 綿谷博雪, 氏家はる代, 田邊克幸, 杉山斉, 伊藤浩, 槇野博史

    第56回日本腎臓学会  2013.5.10 

     More details

    Event date: 2013.5.10 - 2013.5.12

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 1型糖尿病モデルにおける内因性血管新生抑制因子Vasohibin-1(VASH1)欠損による腎症増悪機序についての検討

    雛元紀和, 前島洋平, 斎藤大輔, 山崎浩子, 綿谷博雪, 氏家はる代, 田邊克幸, 杉山斉, 四方賢一, 佐藤靖史, 槇野博史

    第24回日本糖尿病性腎症研究会  2012.12.1 

     More details

    Event date: 2012.12.1 - 2012.12.2

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Fructose Production and Fructokinase Activation in the Proximal Tubule Mediate Tubular Injury in Ciabetic Nephropathy

    Cicerchi C, Roncal-jimenez CA, Ishimoto T, Tamura Y, Tanabe K, Li N, Nakagawa T, Johnson RJ, Lanaspa MA

    American Society of Nephrology Kidney Week 2012  2012.11.3 

     More details

    Event date: 2012.10.30 - 2012.11.4

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Opening KATP Channels with Nicorandil in the Podocytes and Macrophages Improves Chronic Renal Disease in the Rats

    Tamura Y, Tanabe K, Kitagawa W, Uchida S, Johnson RJ, Nakagawa T

    American Society of Nephrology Kidney Week 2012  2012.11.1 

     More details

    Event date: 2012.10.30 - 2012.11.4

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Nicorandil Ameliorates Podocyte Injury through the Activation of ATP- Dependent K+ Channel in Diabetic Nephropathy

    Tanabe K, Lanaspa MA, Kitagawa W, Rivard CJ, Johnson RJ, Nakagawa T

    American Society of Nephrology Kidney Week 2011  2011.11.12 

     More details

    Event date: 2011.11.8 - 2011.11.13

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Renoprotective Effects of Nicorandil in the Rat Remnant Kidney Model

    Tamura Y, Roncal-Jimenez CA, Rivard CJ, Tanabe K, Kitagawa W, Johnson RJ, Nakagawa T

    American Society of Nephrology Kidney Week 2011  2011.11.11 

     More details

    Event date: 2011.11.8 - 2011.11.13

    Language:English   Presentation type:Poster presentation  

    researchmap

  • ACE Inhibition Attenuates Renal Injury in Mice Lacking Endothelial Nitric Oxide Synthase

    Kitagawa W, Tanabe K, Tamura Y, Klawitter J, Rivard CJ, Johnson RJ, Nakagawa T

    American Society of Nephrology Kidney Week 2011  2011.11.10 

     More details

    Event date: 2011.11.8 - 2011.11.13

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Intermittent Administration of ONO-1301, a Sustained-Release Prostacyclin Analog, Ameliorates Renal Alterations in Obese Type 2 Diabetes Mice

    Yamasaki H, Maeshima Y, Nasu T, Saito D, Tanabe K, Sugiyama H, Makino H

    American Society of Nephrology Kidney Week 2010  2010.11.20 

     More details

    Event date: 2010.11.16 - 2010.11.21

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Prostacyclin Analog ONO-1301 Ameliorates Tubulointerstitial Alterations through Induction of HGF

    Nasu T, Maeshima Y, Saito D, Yamasaki H, Tanabe K, Kinomura M, Sugiyama H, Makino H

    American Society of Nephrology Kidney Week 2010  2010.11.18 

     More details

    Event date: 2010.11.16 - 2010.11.21

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Nicorandil Ameliorates Glomerular and Tubulointerstitial Injury in an Advanced Diabetic Nephropathy Mouse Model

    Tanabe K, Kitagawa W, Rivard CJ, Johnson RJ, Nakagawa T

    American Society of Nephrology Kidney Week 2010  2010.11.18 

     More details

    Event date: 2010.11.16 - 2010.11.21

    Language:English   Presentation type:Poster presentation  

    researchmap

  • ONO-1301による尿細管間質病変抑制効果におけるHGFの関与についての検討

    那須達世, 前島洋平, 斎藤大輔, 田邊克幸, 山崎浩子, 杉山斉, 中山瑞穂, 松本邦夫, 酒井芳紀, 槇野博史

    第53回日本腎臓学会  2010.6.17 

     More details

    Event date: 2010.6.16 - 2010.6.18

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 徐放性ONO-1301による2型糖尿病モデルにおける腎症治療効果の検討

    山崎浩子, 前島洋平, 那須達世, 斎藤大輔, 田邊克幸, 杉山斉, 酒井芳紀, 槇野博史

    第53回日本腎臓学会  2010.6.16 

     More details

    Event date: 2010.6.16 - 2010.6.18

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Prostacycline analog ONO-1301 ameliorates tubulointerstitial alterations via induction of HGF in a mouse UUO model

    Nasu T, Maeshia Y, Saito D, Tanabe K, Yamasaki H, Sugiyama H, Nakayama M, Matsumoto K, Sakai Y, Makino H

    ISN-NEXUS Synpodium 2010  2010.4.16 

     More details

    Event date: 2010.4.15 - 2010.4.18

    Language:English   Presentation type:Poster presentation  

    researchmap

  • ONO-1301 MS, a sustained-release prostacycline analog, ameliorates renal damage in obase type 2 diabetic mice

    Yamasaki H, Maeshima Y, Nasu T, Saito D, Tanabe K, Sugiyama H, Sakai Y, Makino H

    ISN-NEXUS Synpodium 2010  2010.4.16 

     More details

    Event date: 2010.4.15 - 2010.4.18

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Protective effects of anti-angiogenic Vasohibin-1 on podocytes in obese type 2 diabetic mice

    Saito D, Maeshima Y, Yamasaki H, TanabeK, Kitamura S, Sugiyama H, Sonoda H, Sato Y, Makino H

    ISN-NEXUS Synpodium 2010  2010.4.16 

     More details

    Event date: 2010.4.15 - 2010.4.18

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Intermittent Administration of a Sustained-Release Prostacyclin Analog ONO-1301 MS Ameliorates Renal Alterations in a Rat Type 1 Diabetes Model

    Yamasaki H, Maeshima Y, Nasu T, Saito D, Tanabe K, Sugiyama H, Sakai Y, Makino H

    American Society of Nephrology Kidney Week 2009  2009.10.31 

     More details

    Event date: 2009.10.27 - 2009.11.1

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Vasohibin-1 Maintains the Phenotype of Podocytes in Association with Its Therapeutic Effects on Albuminuria in Diabetic Nephropathy

    Saito D, Maeshima Y, Nasu T, Yamasaki H, Tanabe K, Kitamura S, Sugiyama H, Sonoda H, Sato Y, Makino H

    American Society of Nephrology Kidney Week 2009  2009.10.31 

     More details

    Event date: 2009.10.27 - 2009.11.1

    Language:English   Presentation type:Poster presentation  

    researchmap

  • A Sustained-Release Prostacyclin Analog ONO-1301 Ameliorates Tubulointerstitial Alterations Via Regulating Epithelial-to-Mesenchymal Transition (EMT)

    Nasu T, Maeshima Y, Tanabe K, Yamasaki H, Saito D, Kitamura S, Sakai Y, Sugiyama H, Makino H

    American Society of Nephrology Kidney Week 2009  2009.10.30 

     More details

    Event date: 2009.10.27 - 2009.11.1

    Language:English   Presentation type:Poster presentation  

    researchmap

  • A Novel Prostacyclin Analog ONO-1301 Ameliorates Renal Alterations in a Rat Progressive Thy-1 Nephritis Model

    Tanabe K, Maeshima Y, Nasu T, Saito D, Yamasaki H, Sugiyama H, Sakai Y, Makino H

    American Society of Nephrology Kidney Week 2009  2009.10.29 

     More details

    Event date: 2009.10.27 - 2009.11.1

    Language:English   Presentation type:Poster presentation  

    researchmap

  • RS3PE症候群が疑われ少量ステロイドが奏功したCAPD患者の1例

    田邊克幸, 中尾一志, 中村絵里, 赤木滋, 矢野隆介, 杉山斉, 槇野博史

    第54回日本透析医学会  2009.6.5 

     More details

    Event date: 2009.6.5 - 2009.6.7

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Vasohibin-1による糸球体足細胞形質維持作用を介する糖尿病性腎症進展抑制機序の検討

    斎藤大輔, 前島洋平, 那須達世, 山崎浩子, 田邊克幸, 三宅剛平, ス・レティ, 喜多村真治, 杉山斉, 園田光, 佐藤靖史, 槇野博史

    第52回日本腎臓学会  2009.6.4 

     More details

    Event date: 2009.6.3 - 2009.6.5

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • プロスタサイクリンアゴニストONO-1301による進行性腎障害抑制効果の検討

    田邊克幸, 前島洋平, 那須達世, 斎藤大輔, 山崎浩子, 三宅剛平, 杉山斉, 酒井芳紀, 槇野博史

    第52回日本腎臓学会  2009.6.4 

     More details

    Event date: 2009.6.3 - 2009.6.5

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • ONO-1301による上皮間葉系移行(EMT)制御を介する尿細管間質病変抑制効果の検討

    那須達世, 前島洋平, 斎藤大輔, 田邊克幸, 三宅剛平, 山崎浩子, ス・レティ, 喜多村真治, 杉山斉, 酒井芳紀, 槇野博史

    第52回日本腎臓学会  2009.6.4 

     More details

    Event date: 2009.6.3 - 2009.6.5

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • ONO-1301による1型糖尿病性腎症治療効果の検討

    山崎浩子, 前島洋平, 那須達世, 斎藤大輔, 田邊克幸, 三宅剛平, ス・レティ, 喜多村真治, 杉山斉, 酒井芳紀, 槇野博史

    第52回日本腎臓学会  2009.6.3 

     More details

    Event date: 2009.6.3 - 2009.6.5

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • SLE・腎腫瘍・肝腫瘍を伴った副腎性Cushing症候群 の一例

    中村真之, 田邊克幸, 大塚文男, 塚本尚子, 相田哲史, 槇野 博史

    第99回日本内科学会中国地方会  2008.11.8 

     More details

    Event date: 2008.11.8

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • IgA腎症に対する扁桃摘出術・ステロイドパルス療法非寛解症例の検討

    井上達之, 杉山斉, 瀧上慶一, 森永裕士, 田邊克幸, 喜多村真治, 赤木滋, 佐田憲映, 前島洋平, 槇野博史

    第38回日本腎臓学会西部学術大会  2008.9.26 

     More details

    Event date: 2008.9.26 - 2008.9.27

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 多彩な自己抗体を有し膜性腎症と半月体形成性糸球体腎炎を合併した1症例

    田邊克幸, 佐田憲映, 井上達之, 木野村賢, 喜多村真治, 前島洋平, 杉山斉, 槇野博史

    第38回日本腎臓学会西部学術大会  2008.9.26 

     More details

    Event date: 2008.9.26 - 2008.9.27

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Vasohibin-1によるメサンギウム細胞への直接作用を介する糖尿病腎症進展制御メカニズムの検討

    那須達世, 前島洋平, 斉藤大輔, 木野村賢, 広越久美子, 田邊克幸, 三宅剛平, 杉山斉, 佐藤靖史, 園田光, 槇野博史

    第51回日本腎臓学会  2008.6.1 

     More details

    Event date: 2008.5.30 - 2008.6.1

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 徐放性製剤ONO-1301による線維化シグナル制御を介する尿細管間質病変抑制効果の検討

    那須達世, 前島洋平, 斉藤大輔, 田邊克幸, 三宅剛平, 木野村賢, 杉山斉, 酒井芳紀, 槇野博史

    第51回日本腎臓学会  2008.5.31 

     More details

    Event date: 2008.5.30 - 2008.6.1

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 血管新生抑制因子Vasohibin-1による2型糖尿病腎症進展抑制効果の検討

    斎藤大輔, 前島洋平, 那須達世, 木野村賢, 広越久美子, 田邊克幸, 三宅剛平, 杉山斉, 佐藤靖史, 園田光, 槇野博史

    第51回日本腎臓学会  2008.5.30 

     More details

    Event date: 2008.5.30 - 2008.6.1

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Sonic hedgehog遺伝子導入による腹膜硬化症抑制効果の検討

    田邊克幸, 前島洋平, 那須達世, 斎藤大輔, 三宅剛平, 木野村賢, 広越久美子, 杉山斉, 相川竜一, 草野研吾, 槇野博史

    第51回日本腎臓学会  2008.5.30 

     More details

    Event date: 2008.5.30 - 2008.6.1

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 急性腎不全にて発症し血液透析を離脱し得た高齢者の膜性増殖性糸球体腎炎の一例

    森永裕士, 佐田憲映, 瀧上慶一, 井上達之, 那須達世, 田邊克幸, 古城昭一郎, 広越久美子, 斎藤大輔, 木野村賢, 菊本陽子, 中尾一志, 前島洋平, 杉山斉, 槇野博史

    第37回日本腎臓学会西部学術大会  2007.10.19 

     More details

    Event date: 2007.10.19 - 2007.10.20

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 抗リン脂質抗体症候群を合併したサルコイドーシスの1例

    斎藤大輔, 那須達世, 田邊克幸, 井上達之, 森永裕士, 菊本陽子, 木野村賢, 丸山美江, 佐田憲映, 前島洋平, 杉山斉, 槇野博史

    第37回日本腎臓学会西部学術大会  2007.10.19 

     More details

    Event date: 2007.10.19 - 2007.10.20

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 血管新生抑制因子vasohibinによる糖尿病腎症進展抑制効果の検討

    那須達世, 前島洋平, 木野村賢, 広越久美子, 田邊克幸, 杉山斉, 佐藤靖史, 槇野博史

    第50回日本腎臓学会  2007.5.26 

     More details

    Event date: 2007.5.25 - 2007.5.27

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 血管新生抑制因子vasohibinによる腹膜硬化症抑制効果の検討

    田邊克幸, 前島洋平, 那須達世, 高沢有紀, 木野村賢, 広越久美子, 井上達之, 杉山斉, 佐藤靖史, 槇野博史

    第50回日本腎臓学会  2007.5.25 

     More details

    Event date: 2007.5.25 - 2007.5.27

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 新規免疫抑制剤FTY720による腎尿細管間質障害モデルにおける治療効果の検討

    広越久美子, 前島洋平, 田邊克幸, 那須達世, 木野村賢, 杉山斉, 槇野博史

    第50回日本腎臓学会  2007.5.25 

     More details

    Event date: 2007.5.25 - 2007.5.27

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • COVID-19維持透析患者の治療経験と透析室での感染対策 Invited

    木野村賢, 田邊克幸, 藤原千尋, 笠原由美子, 長谷川功, 萩谷英大, 大塚文男, 和田淳

    第30回中国腎不全研究会  2021.12.5 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (nominated)  

    researchmap

  • 腎移植後の尿細胞診で6ヶ月以上持続するDecoy細胞陽性所見はBKウイルス腎症の発症予測に有効である

    関戸崇了, 荒木元朗, 吉永香澄, 丸山雄樹, 定平卓也, 西村慎吾, 和田耕一郎, 渡部昌実, 渡辺豊彦, 田邊克幸, 竹内英実, 和田 淳, 柳井広之, 那須保友

    第57回日本移植学会  2021.9.20 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 腎移植患者のタクロリムス血中濃度にボノプラザンが与える薬物相互作用の検討

    和田里章悟, 荒木元朗, 松本 准, 関戸崇了, 吉永香澄, 丸山雄樹, 定平卓也, 西村慎吾, 和田耕一郎, 小林泰之, 渡辺豊彦, 竹内英実, 田邊克幸, 那須保友

    第57回日本移植学会  2021.9.18 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 岡山市 CKD ネットワーク (OCKD-NET) における CKD 病診連携 10 年後の追跡調査

    大西康博, 内田治仁, 大高望, 竹内英実, 辻憲二, 田邊克幸, 森永裕士, 木野村賢, 喜多村真治, 前島洋平, 杉山斉, 太田康介, 丸山啓輔, 大城義之, 森岡茂, 瀧上慶一, 蒲生直幸, 和田淳

    第64回日本腎臓学会  2021.6.18 

     More details

    Presentation type:Poster presentation  

    researchmap

  • 中四国地域における CKD および CVD の関連に関するコホート研究;Kakusyo 3C Study のイベント解析

    大高望, 内田治仁, 竹内英実, 辻憲二, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田 淳

    第64回日本腎臓学会  2021.6.18 

     More details

    Presentation type:Poster presentation  

    researchmap

  • 慢性腎臓病における貧血管理~Kakusyo 3C Study からの検討

    奥山由加, 内田治仁, 大高望, 竹内英実, 辻憲二, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    第64回日本腎臓学会  2021.6.18 

     More details

    Presentation type:Poster presentation  

    researchmap

  • 両側乳頭浮腫を伴う肥厚性硬膜炎を発症した維持血液透析患者の一例

    内山奈津実, 木野村賢, 高橋謙作, 谷村智史, 森岡朋代, 加納弓月, 川北智英子, 田邊克幸, 内田治仁, 杉山斉, 難波清人, 和田淳

    第29回中国腎不全研究会  2021.3.7 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 腎疾患の進行におけるVasohibinの役割

    田邊克幸

    第43回日本分子生物学会  2020.12.2 

     More details

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    researchmap

  • Vasohibin-1 has α-tubulin detyrosinating activity in podocytes

    Morioka T, Tanabe K, Tanimura S, Sugiyama H, Sato Y, WadaJ

    The 9th Chronic Kidney Disease Frontier Meeting  2020.2.15 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    researchmap

  • Vasohibin-1 is essential for the post-transcriptional modification of α-tubulin on microtubules in podocytes International conference

    Morioka T, Tanabe K, Tanimura S, Sugiyama H, Wada J

    American Society of Nephrology Kidney Week 2019  2019.11.7 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Peritoneal dialysis in patients with polycystic kidney disease is unlikely associated with technical failure International conference

    Onishi Y, Tanabe K, Otaka N, Katagawa M, Morinaga H, Kinomura M, Uchida H, Sugiyama H, Wada J

    9th Asia Pacific Chapter Meeting of International Society for Peritoneal Dialysis  2019.9.6 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 当院で腹膜透析を導入した多発性嚢胞腎患者に関する検討

    大西康博, 田邊克幸, 大高望, 大西章史, 北川正史, 森永裕士, 木野村賢, 内田治仁, 杉山斉, 和田淳

    第64回日本透析医学会  2019.6.30 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 中四国地域におけるCKDおよびCVDの関連に関するコホート研究;Kakusho 3C Study:登録2年後の中間解析

    大高望, 内田治仁, 大西章史, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    第62回日本腎臓学会  2019.6.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 血清尿酸値はドナー腎における腎細動脈硝子化と関連し移植後一年の腎予後に影響を及ぼす

    加納弓月, 北川正史, 田邊克幸, 杉山斉, 西村慎吾, 和田耕一郎, 荒木元朗, 那須保友, 和田淳

    第62回日本腎臓学会  2019.6.23 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 中四国地域におけるCKDおよびCVDの関連に関するコホート研究;Kakusho 3C Study:登録2年後のCKD管理状況

    西脇麻里子, 内田治仁, 大高望, 大西章史, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    第62回日本腎臓学会  2019.6.23 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 慢性腎臓病における貧血管理~Kakusho 3C Studyからの検討

    松岡奈津美, 内田治仁, 大高望, 大西章史, 辻憲二, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    第62回日本腎臓学会  2019.6.22 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 岡山市CKDネットワーク(OCKD-NET)におけるCKD病診連携8年後の追跡調査

    大西康博, 内田治仁, 大高望, 田邊克幸, 森永裕士, 木野村賢, 前島洋平, 杉山斉, 太田康介, 丸山啓補, 平松信, 大城義之, 森岡茂, 福島正樹, 和田淳

    第62回日本腎臓学会  2019.6.22 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • vasohibin-1はポドサイトにおける微小管α-tubulinの脱チロシン化を制御する

    森岡朋代, 田邊克幸, 谷村智史, 杉山斉, 佐藤靖史, 和田淳

    第62回日本腎臓学会  2019.6.21 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 慢性腎臓病の進行における腎Vasohibin発現の関与の解明

    田邊克幸, 森岡朋代, 谷村智史

    第14回Vasohibin研究会  2019.2.17 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 腹腔鏡下開窓術を施行した腎移植後リンパ嚢腫の1例

    窪田理沙, 荒木元朗, 和田耕一郎, 河村香澄, 丸山雄樹, 光井洋介, 西村慎吾, 山下里美, 小林泰之, 渡邉豊彦, 那須保友, 北川正史, 田邊克幸, 和田淳

    第52回日本臨床腎移植学会  2019.2.14 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 当院で施行した先行的腎移植の検討

    坪井一朗, 荒木元朗, 河村香澄, 丸山雄樹, 窪田理沙, 定平卓也, 西村慎吾, 和田耕一郎, 小林泰之, 渡邉豊彦, 北川正史, 田邊克幸, 杉山斉, 和田淳, 那須保友

    第52回日本臨床腎移植学会  2019.2.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 鰓耳腎症候群の小児に対する生体腎移植の1例

    窪田理沙, 荒木元朗, 和田耕一郎, 河村香澄, 丸山雄樹, 光井洋介, 西村慎吾, 小林泰之, 渡邉豊彦, 那須保友, 宮井貴之, 北川正史, 田邊克幸, 和田淳

    第54回日本移植学会  2018.10.4 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 生体腎移植レシピエントにおけるCT値を用いた骨密度の変化に関する検討

    丸山雄樹, 荒木元朗, 和田耕一郎, 坪井一朗, 河村香澄, 光井洋介, 窪田理沙, 西村慎吾, 小林泰之, 渡邊豊彦, 北川正史, 田邊克幸, 杉山斉, 和田淳, 那須保友

    第54回日本移植学会  2018.10.4 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 腎移植患者における24時間蓄尿から見る1日塩分・蛋白摂取量の意義

    光井洋介, 荒木元朗, 丸山雄樹, 坪井一朗, 河村香澄, 窪田理沙, 西村慎吾, 和田耕一郎, 小林泰之, 渡辺豊彦, 北川正史, 田邊克幸, 杉山斉, 和田淳, 那須保友

    第54回日本移植学会  2018.10.4 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 珪肺に続発したループス腎炎の1例

    福島和彦, 内田治仁, 御舩朋代, 渊本康子, 和田大広, 大西章史, 北川正史, 田邊克幸, 木野村賢, 喜多村真治, 小崎晋司, 杉山斉, 金廣有彦, 岸本卓巳, 和田淳

    第48回日本腎臓学会西部学術大会  2018.9.28 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 保存期腎不全の進行に腎臓病教室が与える効果の検討

    延山桂香, 笠原由美子, 尺田峰, 藤原千尋, 難波志穂子, 田邊克幸

    第63回日本透析医学会  2018.7.1 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Estrogen-related receptor α欠損はシスプラチン腎症におけるミトコンドリア障害を促進する

    田邊克幸, 津志田圭吾, 三宅広将, 益田加奈, 谷村智史, 杉山斉, 和田淳

    第61回日本腎臓学会  2018.6.10 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 当院におけるドナー腎の組織学的評価と腎予後の比較

    加納弓月, 北川正史, 田邊克幸, 杉山斉, 西村慎吾, 和田耕一郎, 荒木元朗, 那須保友, 和田淳

    第61回日本腎臓学会  2018.6.9 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 中四国地域における慢性腎臓病(CKD)および心血管疾患(CVD)の関連に関するコホート研究 Kakusyo 3C Study

    大高望, 内田治仁, 北川正史, 田邊克幸, 木野村賢, 吉田賢司, 前島洋平, 杉山斉, 伊藤浩, 和田淳

    第61回日本腎臓学会  2018.6.9 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 岡山市CKDネットワーク(OCKD-NET)におけるCKD病診連携7年後の追跡調査

    大西康博, 内田治仁, 大高望, 奥山由加, 田邊克幸, 森永裕士, 木野村賢, 前島洋平, 杉山斉, 太田康介, 平松信, 大城義之, 森岡茂, 福島正樹, 和田淳

    第61回日本腎臓学会  2018.6.9 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 腎疾患におけるVasohibin-2の役割に関する検討

    田邊克幸, 益田加奈, 谷村智史, 三宅広将, 津志田圭吾

    第13回Vasohibin研究会  2018.2.24 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Estrogen-related receptor-α is necessary for maintaining mitochondrial biogenesis in cisplatin-induced acute kidney injury International conference

    Tsushida K, Tanabe K, Miyake H, Masuda K, Tanimura S, Sugiyama H, Wada J

    International Society of Nephrology Frontiers Meeting 2018  2018.2.23 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Deficiency of proangiogenic factor vasohibin-2 exacerbates acute kidney injury via impaired renal tubular cell survival International conference

    Miyake H, Tanabe K, Masuda K, Tsushida K, Tanimura S, Sugiyama H, Sato Y, Wada J

    International Society of Nephrology Frontiers Meeting 2018  2018.2.23 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 当院での腎移植後低リン血症とPTHレベルとの関連性の検討

    田邊克幸, 北川正史, 荒木元朗, 和田耕一郎, 西村慎吾, 光井洋介, 丸山雄樹, 那須保友, 和田淳

    第51回日本臨床腎移植学会  2018.2.16 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 肝腎同時移植における腎保護 Invited

    荒木元朗, 和田耕一郎, 山下里美, 丸山雄樹, 光井洋介, 定平卓也, 西村慎吾, 甲斐誠二, 高本篤, 谷本竜太, 杉本盛人, 小林泰之, 渡邉豊彦, 那須保友, 北川正史, 田邊克幸, 和田淳, 楳田祐三, 藤原俊義, 八木孝仁

    第51回日本臨床腎移植学会  2018.2.15 

     More details

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

    researchmap

  • 生体腎移植における好中球・リンパ球比変化と術後腎機能の検討

    丸山雄樹, 荒木元朗, 河村香澄, 光井洋介, 山下里美, 西村慎吾, 和田耕一郎, 渡邉豊彦, 北川正史, 田邊克幸, 和田淳, 那須保友

    第51回日本臨床腎移植学会  2018.2.15 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Lack of vasohibin-1, a negative feedback regulator of angiogenesis, exacerbates renal injury in murine cisplatin nephropathy model International conference

    Tanimura S, Tanabe K, Masuda K, Miyake H, Sugiyama H, Wada J

    American Society of Nephrology Kidney Week 2017  2017.11.2 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Genetic Ablation of Vasohibin-2 Prevents the Progression of Diabetic Nephropathy in an Experimental Mouse Model International conference

    Masuda K, Tanabe K, Ujike H, Hinamoto N, Miyake H, Sugiyama H, Maeshima Y, Wada J

    American Society of Nephrology Kidney Week 2017  2017.11.2 

     More details

    Language:English   Presentation type:Oral presentation (general)  

    researchmap

  • Vasohibin-2は大動脈瘤モデルマウスにおいてVEGFとは独立して胸部大動脈瘤を増悪させる

    奥山倫弘, 内田治仁, 垣尾勇樹, 梅林亮子, 田邊克幸, 藤井泰宏, 大澤晋, 佐藤靖史, 和田淳

    第58回日本脈管学会  2017.10.19 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 抗てんかん薬の長期内服中に緩徐進行性の腎機能低下を呈した1例

    御舩朋代, 田邊克幸, 川北智英子, 山成俊夫, 北川正史, 木野村賢, 内田治仁, 喜多村真治, 杉山斉, 和田淳

    第47回日本腎臓学会西部学術大会  2017.10.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 抗血管内皮細胞増殖因子(VEGF)薬硝子体内注射による腎障害が示唆された糖尿病性腎症の1例

    大高望, 川北智英子, 木野村賢, 北川正史, 田邊克幸, 江口潤, 内田治仁, 杉山斉, 和田淳, 清水章

    第47回日本腎臓学会西部学術大会  2017.10.13 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 血管新生抑制因子Vasohibin-1の急性腎障害の発生への関与についての検討

    谷村智史, 田邊克幸, 益田加奈, 三宅広将, 津志田圭吾, 杉山斉, 佐藤靖史, 和田淳

    第60回日本腎臓学会  2017.5.26 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 急性腎障害における血管新生促進因子Vasohibin-2の発現意義についての検討

    三宅広将, 田邊克幸, 益田加奈, 津志田圭吾, 杉山斉, 佐藤靖史, 和田淳

    第60回日本腎臓学会  2017.5.26 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 急性腎障害におけるestrogen-related receptor αの役割に関する検討

    津志田圭吾, 田邊克幸, 三宅広将, 益田加奈, 谷村智史, 杉山斉, 和田淳

    第60回日本腎臓学会  2017.5.26 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • Overexpression of Vasohibin-2 Exacerbates Development of Angiotensin II-induced Thoracic Aortic Aneurysms Independent of VEGF International conference

    Okuyama M, Uchida HA, Umebayashi R, Kakio Y, Takeuchi H, Tanabe K, Sato Y, Wada J

    Arteriosclerosis, Thrombosis and Vascular Biology 2017  2017.5.4 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • Genetic ablation of Vasohibin-2 improves progression of diabetic nephropathy in an experimental mouse model

    益田加奈, 田邊克幸, 氏家はる代, 杉山斉, 佐藤靖史, 前島洋平, 和田淳

    第6回CKD Frontier Meeting  2017.2.25 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 急性腎障害におけるVasohibin-1及び-2の発現意義についての検討

    田邊克幸, 三宅広将, 益田加奈, 谷村智史, 津志田圭吾

    第12回Vasohibin研究会  2017.2.4 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Genetic Deletion of Endogenous Proangiogenic Factor Vasohibin-2 Exacerbates Renal Ischemic Reperfusion Injury International conference

    Tanabe K, Masuda K, Arata Y, Sugiyama H, Wada J

    American Society of Nephrology Kidney Week 2016  2016.11.17 

     More details

    Language:English   Presentation type:Poster presentation  

    researchmap

  • 不明熱の原因として非結核性抗酸菌(NTM)症が考えられた血液透析患者の1例

    益田加奈, 木野村賢, 竹内英実, 森下美智子, 荒田夕佳, 秋山愛由, 大西章史, 田邊克幸, 佐田憲映, 谷口暁彦, 杉山斉, 和田淳

    第25回中国腎不全研究会  2016.10.16 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • Vasohibin-2は大動脈瘤モデルマウスにおいて胸部大動脈瘤を増悪させる

    奥山倫弘, 内田治仁, 梅林亮子, 垣尾勇樹, 田邊克幸, 藤井泰宏, 大澤晋, 佐藤靖史, 佐野俊二, 和田淳

    第57回日本脈管学会  2016.10.14 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 急性腎障害における内因性血管新生促進因子Vasohibin-2の役割に関する検討

    田邊克幸, 益田加奈, 荒田夕佳, 三宅広将, 杉山斉, 佐藤靖史, 和田淳

    第59回日本腎臓学会  2016.6.18 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 成人先天性心疾患(ACHD)経過中に出現した腎障害の検討

    木野村賢, 山成俊夫, 北川正史, 田邊克幸, 菊本陽子, 内田治仁, 杉山斉, 和田淳

    第59回日本腎臓学会  2016.6.18 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

  • 血管新生促進因子Vasohibin-2欠損が糖尿病性腎症の進展に及ぼす効果に関する検討

    益田加奈, 大森はる代, 田邊克幸, 三宅広将, 雛元紀和, 杉山斉, 佐藤靖史, 前島洋平, 和田淳

    第59回日本腎臓学会  2016.6.17 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 岡山市CKDネットワーク(OCKD-NET)におけるCKD病診連携5年後の追跡調査

    奥山由加, 内田治仁, 大森はる代, 田邊克幸, 森永裕士, 木野村賢, 前島洋平, 杉山斉, 太田康介, 平松信, 大城義之, 森岡茂, 福島正樹, 和田淳

    第59回日本腎臓学会  2016.6.17 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 当院における透析導入患者の潜在性結核感染症スクリーニング状況の検討

    大西章史, 杉山斉, 森下美智子, 宮脇義亜, 荒田夕佳, 益田加奈, 秋山愛由, 梅林亮子, 山成俊夫, 森永裕士, 田邊克幸, 木野村賢, 和田淳

    第61回日本透析医学会  2016.6.10 

     More details

    Language:Japanese   Presentation type:Poster presentation  

    researchmap

  • 急性及び慢性の腎障害におけるVasohibin-2の発現意義についての検討

    田邊克幸, 益田加奈, 荒田夕佳, 三宅広将

    第11回Vasohibin研究会  2016.1.23 

     More details

    Language:Japanese   Presentation type:Oral presentation (general)  

    researchmap

▼display all

Industrial property rights

  • バソヒビン含有治療剤

    佐藤 靖史, 前島 洋平, 那須 達世, 田邊 克幸, 槇野 博史

     More details

    Applicant:国立大学法人 岡山大学, 塩野義製薬株式会社

    Application no:JP2008055744  Date applied:2008.3.26

    Announcement no:WO2008-123308  Date announced:2008.10.16

    J-GLOBAL

    researchmap

  • バソヒビン含有治療剤

    佐藤 靖史, 前島 洋平, 那須 達世, 田邊 克幸, 槇野 博史

     More details

    Applicant:国立大学法人 岡山大学, 塩野義製薬株式会社

    Application no:特願2009-509145  Date applied:2008.3.26

    Patent/Registration no:特許第5256192号  Date issued:2013.4.26

    J-GLOBAL

    researchmap

Research Projects

  • 慢性腎臓病克服をめざす糸球体ポドサイトのマルチスケール解析

    2024.06 - 2025.02

    令和6年度岡山県特別電源所在県科学技術振興事業

    山田浩司, 竹居孝二, 田邊克幸, 米澤朋子

      More details

    Authorship:Coinvestigator(s) 

    researchmap

  • CKD患者の病気認知に「腑に落ちる」体験を踏まえた療養行動支援プログラムの構築

    Grant number:24K13778  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)

    梶原 右揮, 森本 美智子, 田邊 克幸

      More details

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

    researchmap

  • 慢性腎臓病克服をめざす糸球体ポドサイトのマルチスケール解析

    2023.06 - 2024.02

    令和5年度岡山県特別電源所在県科学技術振興事業

    竹居孝二, 山田浩司, 田邊克幸

      More details

    Authorship:Coinvestigator(s) 

    researchmap

  • 慢性腎臓病に対するVasohibin-2ペプチドワクチン療法の有効性の検討

    2021.04 - 2024.03

    日本学術振興会  科学研究費助成事業 基盤研究(C) 

    田邊克幸

      More details

    Authorship:Principal investigator 

    researchmap

  • 血管新生促進因子Vasohibin-2を標的とした慢性腎臓病の新規治療法の開発

    2018.04 - 2021.03

    日本学術振興会  科学研究費助成事業 基盤研究(C) 

    田邊 克幸

      More details

    Authorship:Principal investigator  Grant type:Competitive

    researchmap

  • 腎線維化と血管傷害におけるVasohibinの役割と治療的意義の検討

    2017.04 - 2019.03

    東北大学加齢医学研究所  共同研究・共同利用 

    田邊 克幸

      More details

    Authorship:Principal investigator  Grant type:Competitive

    researchmap

  • Novel therapeutic strategy for acute kidney injury targeting lipid accumulation and oxidative stress

    Grant number:17K16088  2017.04 - 2019.03

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research  Grant-in-Aid for Young Scientists (B)

    Masuda Kana, TANABE katsuyuki, TSUSHIDA keigo

      More details

    Grant amount:\4160000 ( Direct expense: \3200000 、 Indirect expense:\960000 )

    In this study, we examined the involvement of estrogen-related receptor-α (ERRα), a regulator of mitochondrial biogenesis, in the progression of acute kidney injury. ERRα-deficient mice showed the exacerbation of cisplatin-induced acute tubular injury, with abnormalities in mitochondrial morphology, compared with wild-type mice. in addition, pharmacological inhibition of ERRα with XCT-790 in cultured proximal tubular cells caused decreased expression of mitochondrial protein and enhanced cinsplatin-induced expression of proapoptotic protein. Taken together, this study suggests that ERRα is essential for maintaining mitochondrial integrity in renal tubular cells and preserved expression of ERRα in renal tubular cells may be a potential therapeutic strategy against acute kidney injury.

    researchmap

  • バゾヒビンによるミトコンドリア障害の制御を介した急性腎障害治療効果の検討

    2015.04 - 2018.03

    日本学術振興会  科学研究費助成事業 基盤研究(C) 

    田邊 克幸

      More details

    Authorship:Principal investigator  Grant type:Competitive

    researchmap

  • 慢性腎臓病におけるVasohibinファミリー分子の病態意義についての検討

    2014.09 - 2016.03

    東北大学加齢医学研究所  共同研究・共同利用 

    田邊 克幸

      More details

    Authorship:Principal investigator  Grant type:Competitive

    researchmap

  • PGC-1α-ERRα経路を標的とした糖尿病性腎症の新規治療法の開発

    2013.04 - 2015.03

    日本学術振興会  科学研究費助成事業 若手研究(B) 

    田邊 克幸

      More details

    Authorship:Principal investigator  Grant type:Competitive

    researchmap

  • ONO-1301 を用いた慢性腎臓病の新規治療法開発の試み

    Grant number:21790812  2009.04 - 2011.03

    日本学術振興会  科学研究費助成事業  若手研究(B)

    田邊 克幸

      More details

    Authorship:Principal investigator  Grant type:Competitive

    慢性腎臓病(CKD)は末期腎不全への進行のみならず、心血管イベント発生のリスクファクターとなる。本邦においてCKDの進展によって末期腎不全から血液透析に至る患者数は増加の一途をたどっており、CKDの進展抑制のための有効な治療法の開発が腎臓内科領域において急務となっている。ONO-1301は構造的に安定な非プロスタノイド骨格の化合物で、長時間作用型のプロスタサイクリン(PGI2)アゴニストとトロンボキサンA2(TXA2)合成酵素阻害作用による強力な抗血小板作用を有する。徐放性製剤ONO-1301MSは皮下もしくは筋肉内投与にて安定した血中濃度を示すが、肺線維症モデルにおける線維化抑制効果、心筋梗塞モデルにおける左室拡張能改善効果、生存率の改善が報告されている。ONO-1301による治療効果の発現機序として、血管平滑筋細胞におけるERKリン酸化抑制、間葉系細胞(線維芽細胞など)からのHGF発現誘導等が検討されている。腎障害が進展する共通のメカニズムである尿細管間質線維化と、糖尿病性腎症における糸球体病変に対してONO-1301が抗線維化作用等を介して進展抑制効果を示す、との仮説のもとに、本研究にて以下の検討を行った。
    1) マウス片側尿管結紮(UUO)モデルにおけるONO-1301投与による尿細管間質線維化抑制効果:ONO-1301徐放性製剤(3mg/kg,単回)投与により第3、7病日における腎間質線維化、間質炎症細胞浸潤、I,III型コラーゲン蓄積が有意に抑制された。
    2) ONO-1301の尿細管間質線維化抑制への作用機序の解析:ONO-1301投与群では腎皮質における線維化促進因子TGF-βの発現増加が抑制され、同因子に拮抗的に作用するHGF発現増加が観察された。
    3) 2型糖尿病モデルマウス(db/dbマウス)における、ONO-1301投与による腎症改善効果:db/dbマウスに8週齢よりONO-1301徐放性製剤(3mg/kg)を3週毎に投与した。16週齢の時点で、アルブミン尿、糸球体メサンギウム基質蓄積の抑制効果が観察された。
    4) ONO-1301の糸球体病変改善効果の機序:培養メサンギウム細胞にて高糖濃度培養条件下におけるTGF-β,α-SMA発現増加、IV型コラーゲン産生増加がONO-1301投与により抑制された。
    以上の結果より、慢性腎臓病治療におけるONO-1301の有用性が示唆され、将来的な臨床応用の可能性が期待される。

    researchmap

▼display all