Your search keyword '"Matsuo, Seiichi"' showing total 60 results

1. Health-related Quality of Life in 10 years Long-term Survivors of Chronic Kidney Disease: A From-J Study

Author

Okubo, Reiko, Kondo, Masahide, Imasawa, Toshiyuki, Saito, Chie, Kai, Hirayasu, Tsunoda, Ryoya, Hoshino, Junichi, Watanabe, Tsuyoshi, Narita, Ichiei, Matsuo, Seiichi, Makino, Hirofumi, Hishida, Akira, and Yamagata, Kunihiro

Abstract

The Chronic Kidney Disease (CKD) practice facilitation program in the Frontier of Renal Outcome Modifications in Japan study reduced cardiovascular disease (CVD) events in patients with CKD. 10-year long-term survivors with CKD lived with serious complications, including end-stage kidney disease and CVD. This study aimed to measure health-related quality of life in 10-year long-term CKD survivors and examine the predictors and determinants of clinical indices for measured quality of life (QOL) scores.

Published

2024

2. Therapeutic neovascularization using cord blood-derived endothelial progenitor cells for diabetic neuropathy

Author

Naruse, Keiko, Hamada, Yoji, Nakashima, Eitaro, Kato, Koichi, Mizubayashi, Ryuichi, Kamiya, Hideki, Yuzawa, Yukio, Matsuo, Seiichi, Murohara, Toyoaki, Matsubara, Tatsuaki, Oiso, Yutaka, and Nakamura, Jiro

Subjects

Neovascularization -- Usage, Diabetes -- Complications and side effects -- Care and treatment, Fetal blood -- Usage, Peripheral nerve diseases -- Care and treatment -- Complications and side effects, Diabetic neuropathies -- Care and treatment -- Complications and side effects, Health

Abstract

Diabetic neuropathy is based on the impairment of nerve blood flow and the metabolic disorder. Although the vasodilating agents and anticoagulants improve nerve function and symptoms in diabetic neuropathy, more effective treatments are needed. Because endothelial progenitor cells (EPCs) have been identified in adult human peripheral blood, many studies have shown that transplantation of EPCs improves circulation to ischemic tissues. In this study, we have demonstrated that therapeutic neovascularization using human umbilical cord blood-derived EPCs reversed diabetic neuropathy. EPCs were isolated and expanded on day 7 of culture from cord blood mononuclear cells. Unilateral intramuscular injection of EPCs into hindlimb skeletal muscles significantly ameliorated impaired sciatic motor nerve conduction velocity and sciatic nerve blood flow in the EPC-injected side of streptozotocin-induced diabetic nude rats compared with the saline-injected side of diabetic nude rats. Histological study revealed an increased number of microvessels in hindlimb skeletal muscles in the EPC-injected side of diabetic rats. These findings suggest that transplantation of EPCs from cord blood may be a useful treatment for diabetic neuropathy., Diabetic neuropathy, which is the most frequent and earliest diabetes complication, decreases the quality of life and increases the morbidity of diabetic patients (1) and occurs because of the impairment [...]

Published

2005

3. Febuxostat Therapy for Patients With Stage 3 CKD and Asymptomatic Hyperuricemia: A Randomized Trial

Author

Kimura, Kenjiro, Hosoya, Tatsuo, Uchida, Shunya, Inaba, Masaaki, Makino, Hirofumi, Maruyama, Shoichi, Ito, Sadayoshi, Yamamoto, Tetsuya, Tomino, Yasuhiko, Ohno, Iwao, Shibagaki, Yugo, Iimuro, Satoshi, Imai, Naohiko, Kuwabara, Masanari, Hayakawa, Hiroshi, Ohtsu, Hiroshi, Ohashi, Yasuo, Kimura, Kenjiro, Hosoya, Tatsuo, Ito, Sadayoshi, Inaba, Masaaki, Tomino, Yasuhiko, Uchida, Shunya, Makino, Hirofumi, Matsuo, Seiichi, Yamanaka, Hisashi, Yamamoto, Tetsuya, Ohno, Iwao, Shibagaki, Yugo, Iimuro, Satoshi, Imai, Naohiko, Kuwabara, Masanari, Hayakawa, Hiroshi, Akizawa, Tadao, Teramoto, Tamio, Kasanuki, Hiroshi, Yoshimura, Kenichi, Kimura, Kenjiro, Hosoya, Tatsuo, Shibagaki, Yugo, Ohno, Iwao, Sato, Hiroshi, Uchida, Shunya, Horikoshi, Satoshi, Maruyama, Syoichi, Inaba, Masahiko, Moriwaki, Yuji, Uchida, Haruhito, Kaneshiro, Nagayuki, Imai, Naohiko, Moriya, Hidekazu, Komatsu, Yasuhiro, Kaname, Shinya, Hanaoka, Kazunari, Ogura, Makoto, Ikeda, Masato, Kasai, Kenji, Sugiura, Akira, Takahashi, Kazushi, Kojima, Kenichiro, Nitta, Kosaku, Tamai, Hirofumi, Nagaya, Hiroshi, Okuno, Senji, Kakiya, Ryusuke, Takeoka, Hiroya, Hirata, Kyouji, Asano, Kenichiro, Fukaya, Yasuo, Iwaida, Yasushi, Tsuneda, Yasuo, Nishimura, Shigeaki, Hiramatsu, Takeyuki, Isaka, Yoshitaka, Ito, Takafumi, Yuzawa, Yukio, Yamagata, Kunihiro, Sofue, Tadashi, Jinguji, Yoshimi, Hirano, Keita, Matsuyama, Kazuhiro, Mizumoto, Teruhiko, Shibuya, Yuko, Sugawara, Masahiro, Kadomura, Moritoshi, Teshima, Yasuaki, Ohtani, Hiroshi, Kamata, Hiroki, Okawara, Susumu, Fukushima, Masaki, Takemura, Katsumi, Kinugasa, Eriko, Kogure, Masami, and Ehara, Yoichi

Abstract

Epidemiologic and clinical studies have suggested that urate-lowering therapy may slow the progression of chronic kidney disease (CKD). However, definitive evidence is lacking.

Published

2018

4. Association of ETS1polymorphism with granulomatosis with polyangiitis and proteinase 3-anti-neutrophil cytoplasmic antibody positive vasculitis in a Japanese population

Author

Kawasaki, Aya, Yamashita, Keita, Hirano, Fumio, Sada, Ken-ei, Tsukui, Daisuke, Kondo, Yuya, Kimura, Yoshitaka, Asako, Kurumi, Kobayashi, Shigeto, Yamada, Hidehiro, Furukawa, Hiroshi, Nagasaka, Kenji, Sugihara, Takahiko, Yamagata, Kunihiro, Sumida, Takayuki, Tohma, Shigeto, Kono, Hajime, Ozaki, Shoichi, Matsuo, Seiichi, Hashimoto, Hiroshi, Makino, Hirofumi, Arimura, Yoshihiro, Harigai, Masayoshi, and Tsuchiya, Naoyuki

Abstract

ETS proto-oncogene 1, transcription factor (ETS1) is involved in various immune responses. Genome-wide association studies on systemic lupus erythematosus in Chinese populations identified the association of ETS1polymorphism in 3′ untranslated region, rs1128334A, which was associated with lower ETS1expression. In view of substantial sharing of susceptibility genes across multiple autoimmune diseases, we examined whether ETS1is associated with a rare autoimmune rheumatic disease, anti-neutrophil cytoplasmic antibody (ANCA)-associated vasculitis (AAV). Association of rs1128334 was tested in 466 Japanese patients with AAV and 1099 healthy controls by logistic regression analysis under the additive model. AAV patients were classified into 285 microscopic polyangiitis (MPA), 92 granulomatosis with polyangiitis (GPA), 56 eosinophilic GPA, and 33 unclassifiable AAV, according to the European Medicines Agency (EMEA) algorithm. Among the patients, 376 were positive for MPO–ANCA and 62 for PR3–ANCA. When the patients were classified according to the EMEA classification, rs1128334A allele was significantly increased in GPA (P= 0.0060, Pc= 0.030, odds ratio (OR), 1.54; 95% confidence interval (CI), 1.13–2.10). With respect to the ANCA specificity, significant association was observed in PR3–ANCA positive AAV (P= 0.0042, Pc= 0.021, OR, 1.72; 95% CI, 1.19–2.49). In conclusion, ETS1polymorphism was suggested to be associated with GPA and PR3–ANCA positive AAV in a Japanese population.

Published

2018

5. Prediction of response to remission induction therapy by gene expression profiling of peripheral blood in Japanese patients with microscopic polyangiitis

Author

Ishizu, Akihiro, Tomaru, Utano, Masuda, Sakiko, Sada, Ken-ei, Amano, Koichi, Harigai, Masayoshi, Kawaguchi, Yasushi, Arimura, Yoshihiro, Yamagata, Kunihiro, Ozaki, Shoichi, Dobashi, Hiroaki, Homma, Sakae, Okada, Yasunori, Sugiyama, Hitoshi, Usui, Joichi, Tsuboi, Naotake, Matsuo, Seiichi, and Makino, Hirofumi

Abstract

Microscopic polyangiitis (MPA), which is classified as an anti-neutrophil cytoplasmic antibody (ANCA)-associated small vessel vasculitis, is one of the most frequent primary vasculitides in Japan. We earlier nominated 16 genes (IRF7, IFIT1, IFIT5, OASL, CLC, GBP-1, PSMB9, HERC5, CCR1, CD36, MS4A4A, BIRC4BP, PLSCR1, DEFA1/DEFA3, DEFA4, and COL9A2) as predictors of response to remission induction therapy against MPA. The aim of this study is to determine the accuracy of prediction using these 16 predictors. Thirty-nine MPA patients were selected randomly and retrospectively from the Japanese nationwide RemIT-JAV-RPGN cohort and enrolled in this study. Remission induction therapy was conducted according to the Guidelines of Treatment for ANCA-Associated Vasculitis published by the Ministry of Health, Labour, and Welfare of Japan. Response to remission induction therapy was predicted by profiling the altered expressions of the 16 predictors between the period before and 1 week after the beginning of treatment. Remission is defined as the absence of clinical manifestations of active vasculitis (Birmingham Vasculitis Activity Score 2003: 0 or 1 point). Persistent remission for 18 months is regarded as a “good response,” whereas no remission or relapse after remission is regarded as a “poor response.” “Poor” and “good” responses were predicted in 7 and 32 patients, respectively. Five out of 7 patients with “poor” prediction and 1 out of 32 patients with “good” prediction experienced relapse after remission. One out of 7 patients with “poor” prediction was not conducted to remission. Accordingly, the sensitivity and specificity to predict poor response was 85.7% (6/7) and 96.9% (31/32), respectively. Response to remission induction therapy can be predicted by monitoring the altered expressions of the 16 predictors in the peripheral blood at an early point of treatment in MPA patients.

Published

2017

6. Sodium chloride promotes tissue inflammation via osmotic stimuli in subtotal-nephrectomized mice

Author

Sakata, Fumiko, Ito, Yasuhiko, Mizuno, Masashi, Sawai, Akiho, Suzuki, Yasuhiro, Tomita, Takako, Tawada, Mitsuhiro, Tanaka, Akio, Hirayama, Akiyoshi, Sagara, Akihiro, Wada, Takashi, Maruyama, Shoichi, Soga, Tomoyoshi, Matsuo, Seiichi, Imai, Enyu, and Takei, Yoshifumi

Abstract

Chronic inflammation, which is often associated with high all-cause and cardiovascular mortality, is prevalent in patients with renal failure; however, the precise mechanisms remain unclear. High-salt intake was reported to induce lymphangiogenesis and autoimmune diseases via osmotic stimuli with accumulation of sodium or chloride. In addition, sodium was recently reported to be stored in the extremities of dialysis patients. We studied the effects and mechanisms of high salt loading on tissue and systemic inflammation in subtotal-nephrectomized mice (5/6Nx) and in cultured cells. Macrophage infiltration in the peritoneal wall (P<0.001), heart (P<0.05) and para-aortic tissues (P<0.001) was significantly higher in 5/6Nx with salt loading (5/6Nx/NaCl) than in 5/6Nx without salt loading (5/6Nx/Water); however, there were no significant differences in blood pressure and renal function between the groups. Tissue interleukin-6, monocyte chemotactic protein-1 (MCP-1), serum- and glucocorticoid-inducible kinase 1 (Sgk1) and tonicity-responsive enhancer binding protein (TonEBP) mRNA were significantly elevated in the peritoneal wall and heart with 5/6Nx/NaCl when compared with 5/6Nx/Water. Sodium was stored in the abdominal wall, exerting high-osmotic conditions. Reversal of salt loading reduced macrophage infiltration associated with decreased TonEBP in 5/6Nx/NaCl. Macrophage infiltration associated with fibrosis induced by salt loading was decreased in the 5/6Nx/NaCl/CC chemokine receptor 2 (CCR2, receptor of MCP-1)-deficient mice when compared with 5/6Nx/NaCl/Wild mice, suggesting that CCR2 is required for macrophage infiltration in 5/6Nx with NaCl loading. In cultured mesothelial cells and cardiomyocytes, culture media with high NaCl concentration induced MCP-1, Sgk1 and TonEBP mRNA, all of which were suppressed by TonEBP siRNA, indicating that both MCP-1 and Sgk1 are downstream of TonEBP. Our study indicates that high NaCl intake induces MCP-1 expression leading to macrophage infiltration via the TonEBP-MCP-1 pathway in 5/6Nx/NaCl mice, and that TonEBP has a central role in inflammation in patients with renal failure taking high salt.

Published

2017

7. Cardiovascular events and death in Japanese patients with chronic kidney disease

Author

Tanaka, Kenichi, Watanabe, Tsuyoshi, Takeuchi, Ayano, Ohashi, Yasuo, Nitta, Kosaku, Akizawa, Tadao, Matsuo, Seiichi, Imai, Enyu, Makino, Hirofumi, and Hishida, Akira

Abstract

The incidence of cardiovascular disease (CVD) is higher in patients with chronic kidney disease (CKD) than in the general population, and the risk of CVD increases with reductions in renal function. However, the incidence of CVD in Japanese patients with CKD has not been sufficiently investigated. To measure this we conducted the Chronic Kidney Disease Japan Cohort (CKD-JAC) Study over four years in 2,966 Japanese patients with CKD to examine the incidence of CVD and all-cause death. These patients had an estimated glomerular filtration rate (eGFR) of 10–59 ml/min/1.73 m2, were under nephrologist care, and pooled from 17 medical institutions in Japan. At the median follow-up of 3.9 years, 69 patients had died, 217 had cardiovascular events, and 514 started maintenance dialysis therapy. The incidences of cardiovascular events were 11.9, 19.1, 25.0, and 39.4 per 1,000 person-years at eGFRs of 45–59, 30–44, 15–29, and under 15 ml/min/1.73 m2, respectively. The adjusted Cox proportional hazards models showed that the risk of cardiovascular events increased as the eGFR decreased, with a significant difference only between CKD stage G5 (eGFR: under 15 ml/min/1.73 m2) and CKD stage G3a (eGFR: 45–59 ml/min/1.73 m2) (hazard ratio 3.16, 95% confidence interval 1.28 to 7.76). Thus, the risk of CVD and all-cause death was related to the decrease in eGFR, but not necessarily elevated in proportion to progression of the CKD stage in Japanese patients with predialysis CKD under a nephrologist’s care.

Published

2017

8. Transfusion of CD206+M2 Macrophages Ameliorates Antibody-Mediated Glomerulonephritis in Mice

Author

Du, Qiuna, Tsuboi, Naotake, Shi, Yiqin, Ito, Sachiko, Sugiyama, Yutaka, Furuhashi, Kazuhiro, Endo, Nobuhide, Kim, Hangsoo, Katsuno, Takayuki, Akiyama, Shin'ichi, Matsuo, Seiichi, Isobe, Ken-Ichi, and Maruyama, Shoichi

Abstract

Macrophages are multifunctional immune cells that may either drive or modulate disease pathogenesis, depending on the activated phenotype. In this study, we investigated the protective effects of CD206+M2 macrophages against nephrotoxic serum nephritis in mice. We found that these immunosuppressive macrophages, derived from bone marrow and stimulated with IL-4/IL-13 [CD206+M2 bone marrow–derived macrophages (M2BMMs)], protected against renal injury, decreased proteinuria, and diminished the infiltration of CD68+macrophages, neutrophils, and T cells into glomerular tissue. Comparable therapeutic results were obtained with CD206+M2 cells derived from induced pluripotent stem cells. Notably, CD206+M2BMMs, which retained an M2 signature, could elicit a switch of M1 to M2 phenotype in co-cultured macrophages. Moreover, these cells were found to induce the production of regulatory T cells in the spleen and renal draining lymph node. Accordingly, mRNA expression of the T helper 1 cytokines tumor necrosis factor-α, interferon-β, interferon-γ, and IL-12 was significantly reduced in kidneys from mice treated with CD206+M2BMMs. Taken together, the data suggest that CD206+M2 may have therapeutic potential against antibody-mediated glomerular injury and presents its therapeutic value for the treatment of crescentic nephritis in humans.

Published

2016

9. Low disease activity of microscopic polyangiitis in patients with anti-myosin light chain 6 antibody that disrupts actin rearrangement necessary for neutrophil extracellular trap formation

Author

Yoshinari, Miku, Nishibata, Yuka, Masuda, Sakiko, Nakazawa, Daigo, Tomaru, Utano, Arimura, Yoshihiro, Amano, Koichi, Yuzawa, Yukio, Sada, Ken-Ei, Atsumi, Tatsuya, Dobashi, Hiroaki, Hasegawa, Hitoshi, Harigai, Masayoshi, Matsuo, Seiichi, Makino, Hirofumi, and Ishizu, Akihiro

Abstract

Background: Neutrophil extracellular traps (NETs) are critically involved in microscopic polyangiitis (MPA) pathogenesis, and some patients with MPA possess anti-NET antibody (ANETA). Anti-myosin light chain 6 (MYL6) antibody is an ANETA that affects NETs. This study aimed to determine the significance of anti-MYL6 antibody in MPA. Methods: The influence of anti-MYL6 antibody on NET formation and actin rearrangement necessary for NET formation was assessed by fluorescent staining. An enzyme-linked immunosorbent assay was established to detect serum anti-MYL6 antibody, and the prevalence of this antibody in MPA was determined. Furthermore, the disease activity and response to remission-induction therapy of MPA were compared between anti-MYL6 antibody-positive and anti-MYL6 antibody-negative MPA patients. Results: Anti-MYL6 antibody disrupted G-actin polymerization into F-actin, suppressing phorbol 12-myristate 13-acetate-induced NET formation. Serum anti-MYL6 antibody was detected in 7 of 59 patients with MPA. The Birmingham vasculitis activity score (BVAS) of anti-MYL6 antibody-positive MPA patients was significantly lower than anti-MYL6 antibody-negative MPA patients. Among the nine BVAS evaluation items, the cutaneous, cardiovascular, and nervous system scores of anti-MYL6 antibody-positive MPA patients were significantly lower than anti-MYL6 antibody-negative MPA patients, although other items, including the renal and chest scores, were equivalent between the two groups. The proportion of patients with remission 6 months after initiation of remission-induction therapy in anti-MYL6 antibody-positive MPA patients was significantly higher than in anti-MYL6 antibody-negative MPA patients. Conclusions: Collective findings suggested that anti-MYL6 antibody disrupted actin rearrangement necessary for NET formation and could reduce the disease activity of MPA.

Published

2022

10. The efficacy of tolvaptan as a diuretic for chronic kidney disease patients

Author

Tanaka, Akihito, Katsuno, Takayuki, Ozaki, Takenori, Sakata, Fumiko, Kato, Noritoshi, Suzuki, Yasuhiro, Kosugi, Tomoki, Kato, Sawako, Tsuboi, Naotake, Sato, Waichi, Yasuda, Yoshinari, Mizuno, Masashi, Ito, Yasuhiko, Matsuo, Seiichi, and Maruyama, Shoichi

Abstract

BackgroundTolvaptan selectively binds to the vasopressin V2 receptor and inhibits reabsorption of free water. Although its effi cacy for heart failure has been proven, its effi cacy for chronic kidney disease (CKD) patients has not been assessed in detail.MethodsWe examined 20 CKD patients (13 men and 7 women) who presented with volume overload and who were administered tolvaptan. We assessed urine volume (UV) and blood biochemistry before administration (d0), 1 day after administration (d1), and 7 to 14 days after administration (d7-14).ResultsThe mean age was 74.0) 13.1 years. Besides CKD, there were 9, 8, and 5 patients with heart failure, liver failure or liver cirrhosis, and severe oedema, respectively. UV signifi cantly increased from 959.0 ) 503.8 mL/day at d0 to 1605.4 ) 964.0 mL/day at d7-14 (P <0.01). Serum creatinine levels were not exacerbated (3.89) 3.43 mg/dL at d0 and 3.66) 3.02 mg/dL at d7-14). Serum albumin (ALB) levels and urinary protein creatinine ratio (uPCR) did not correlate with UV change. Estimated glomerular fi ltration rate (eGFR) correlated with UV change from d0 to d1 (r = 0.6619, P< 0.01). Serum sodiume levation correlated with increased UV (r = 0.4951, P< 0.05).ConclusionTolvaptan is useful to reduce volume overload without exacerbation of the renal function; its eff ect does not depend on ALB or uPCR. The eGFR correlated with the effi cacy of tolvaptan. If UV increases drastically after tolvaptan administration, serum Na levels should be carefully monitored.

Published

2015

11. Increase of Antimyeloperoxidase Antineutrophil Cytoplasmic Antibody (ANCA) in Patients with Renal ANCA-associated Vasculitis: Association with Risk to Relapse

Author

Yamaguchi, Makoto, Ando, Masahiko, Kato, Sawako, Katsuno, Takayuki, Kato, Noritoshi, Kosugi, Tomoki, Sato, Waichi, Tsuboi, Naotake, Yasuda, Yoshinari, Mizuno, Masashi, Ito, Yasuhiko, Matsuo, Seiichi, and Maruyama, Shoichi

Abstract

Objective.The diagnostic values of antiproteinase 3 and antimyeloperoxidase tests using antineutrophil cytoplasmic antibodies (ANCA) are well established. Our study determined whether an increase in ANCA level was a predictor of disease flareup.Methods.Our study included 126 patients with ANCA-associated renal vasculitis treated at 9 nephrology centers in Japan. The relationship between increased ANCA levels and relapse was assessed using time-dependent multivariate Cox regression models adjusted for clinically relevant factors. The outcome of interest was the time from remission to first relapse.Results.During the observation period [median 41 mos, interquartile range (IQR) 23–66 mos], 118 patients (95.8%) achieved remission at least once. After achieving remission, 34 patients relapsed (21.7%). Time-dependent multivariate Cox regression models revealed that lung involvement (adjusted HR 2.29, 95% CI 1.13–4.65, p = 0.022) and increased ANCA levels (adjusted HR 17.4, 95% CI 8.42–36.0, p < 0.001) were significantly associated with relapse. The median time from ANCA level increase to relapse was 0.6 months (IQR 0–2.1 mos).Conclusion.In our study, an increase in ANCA level during remission was associated with a risk of disease relapse. A rise in ANCA level may be useful for guiding treatment decisions in appropriate subsets of patients with ANCA-associated vasculitis.

Published

2015

12. Comparison of Phenotype and Outcome in Microscopic Polyangiitis Between Europe and Japan

Author

Furuta, Shunsuke, Chaudhry, Afzal N., Hamano, Yoshitomo, Fujimoto, Shouichi, Nagafuchi, Hiroko, Makino, Hirofumi, Matsuo, Seiichi, Ozaki, Shoichi, Endo, Tomomi, Muso, Eri, Ito, Chiharu, Kusano, Eiji, Yamagata, Mieko, Ikeda, Kei, Kashiwakuma, Daisuke, Iwamoto, Itsuo, Westman, Kerstin, and Jayne, David

Abstract

Objective.There are differences between Europe and Japan in the incidence and antineutrophil cytoplasmic antibody (ANCA) serotype of patients with microscopic polyangiitis (MPA). However, differences in phenotype or outcome have not been explored. We aimed to identify differences in phenotype and outcome of MPA between Europe and Japan.Methods.Sequential cohorts of patients with MPA and renal limited vasculitis were collected from European and Japanese centers (n = 147 and n = 312, respectively). Trial databases from the European Vasculitis Society and the Japanese patients with Myeloperoxidase (MPO)-ANCA-Associated Vasculitis (JMAAV) trial were studied (n = 254 and n = 48, respectively). We evaluated baseline characteristics including ANCA status and organ involvement, treatment, survival, and renal survival. Differences in survival and renal survival were studied using multivariate analysis.Results.The non-trial cohorts showed patients with MPA in Japan had a higher age at onset, more frequent MPO-ANCA positivity, lower serum creatinine, and more frequent interstitial pneumonitis than those in Europe (all p < 0.01). Comparisons between the trial databases demonstrated similar results. Cumulative patient survival and renal survival rates were not different between Europe and Japan (p = 0.71 and p = 0.38, respectively). Multivariate analysis identified age at onset, serum creatinine, gastrointestinal, and respiratory involvement as factors with higher risk of death. For endstage renal failure, serum creatinine and use of plasma exchange were identified as factors with higher risk, and immunosuppressant use as lower risk factors.Conclusion.Phenotypes in patients with MPA were different between Europe and Japan. However, the outcomes of patient survival and renal survival were similar.

Published

2014

13. Anti-C5a complementary peptide ameliorates acute peritoneal injury induced by neutralization of Crry and CD59

Author

Mizuno, Tomohiro, Mizuno, Masashi, Imai, Masaki, Suzuki, Yasuhiro, Kushida, Mayu, Noda, Yukihiro, Maruyama, Shoichi, Okada, Hidechika, Okada, Noriko, Matsuo, Seiichi, and Ito, Yasuhiko

Abstract

In peritoneal dialysis (PD) therapy, physical stresses such as exposure to peritoneal dialysate, catheter trauma, and peritonitis may induce peritoneal injury that can prevent continued long-term PD therapy. Therefore, protection of the peritoneum is an important target to enable long-term PD therapy in patients with end-stage renal disease. We previously showed that neutralization of the membrane complement regulators (CRegs) Crry and CD59 in rat peritoneum provokes development of acute peritoneal injury due to uncontrolled complement activation. C5a is a key effecter molecule of the complement system released during acute inflammation. Control of C5a has been proposed as a strategy to suppress inflammatory reactions and, because peritoneal injury is accompanied by inflammation, we hypothesized that C5a targeted therapy might be an effective way to suppress peritoneal injury. In the present study we used an established acute peritonitis model induced by neutralization of CRegs to investigate the effects on acute peritoneal injury of inhibiting C5a. Intravenous administration of an anti-C5a complementary peptide (AcPepA) up to 4 h after induction of injury significantly and dose-dependently prevented accumulation of inflammatory cells and reduced tissue damage in the model, accompanied by decreased C3b deposition. We show that C5a contributed to the development of peritoneal injury. Our results suggest that C5a is a target for preventing or treating peritoneal injury in patients undergoing prolonged PD therapy or with infectious complications.

Published

2013

14. Low Serum Cultured Adipose Tissue-Derived Stromal Cells Ameliorate Acute Kidney Injury in Rats

Author

Katsuno, Takayuki, Ozaki, Takenori, Saka, Yosuke, Furuhashi, Kazuhiro, Kim, Hangsoo, Yasuda, Kaoru, Yamamoto, Tokunori, Sato, Waichi, Tsuboi, Naotake, Mizuno, Masashi, Ito, Yasuhiko, Imai, Enyu, Matsuo, Seiichi, and Maruyama, Shoichi

Abstract

Current studies suggest that mesenchymal stromal cells (MSCs) improve acute kidney injury (AKI) via paracrine/ endocrine effects. We established human adipose tissue-derived stromal cells (hASCs) cultured in low (2%) serum (hLASCs), which have great potential of tissue regeneration. The present study was performed to investigate the therapeutic effects of hLASCs on AKI and to clarify the mechanisms involved. In low serum, hASCs proliferated well, while human bone marrow-derived stromal cells (hBMSCs) did not. hLASCs secreted higher levels of hepatocyte growth factor (HGF) and vascular endothelial growth factor (VEGF) than did hASCs cultured in high (20%) serum (hHASCs) or hBMSCs cultured in high serum (hHBMSCs). AKI was induced in nude rats by folic acid, and hLASCs, hHASCs or control medium were administered into the renal subcapsules. hLASCs significantly attenuated acute renal damage, while hHASCs showed far less effect. Furthermore, interstitial fibrosis observed on day 14 was less pronounced in the hLASCs group. Cell tracking experiment showed no evidence of transdifferentiation. Intravenous injection of hLASCs or hHBMSCs or subcapsular injection of hHBMSCs did not ameliorate AKI. Concerning the mechanisms, our in vivo experiments showed that HGF knockdown by siRNA impaired the ability of hLASCs to protect the kidney from acute injury whereas VEGF knockdown did not. In conclusion, hLASCs, but not hHASCs or hHBMSCs, ameliorated AKI via paracrine effects, and HGF is one of the key mediators.

Published

2013

15. Deficiency of Growth Factor Midkine Exacerbates Necrotizing Glomerular Injuries in Progressive Glomerulonephritis

Author

Kojima, Hiroshi, Kosugi, Tomoki, Sato, Waichi, Sato, Yuka, Maeda, Kayaho, Kato, Noritoshi, Kato, Kiyonari, Inaba, Shinichiro, Ishimoto, Takuji, Tsuboi, Naotake, Matsuo, Seiichi, Maruyama, Shoichi, Yuzawa, Yukio, and Kadomatsu, Kenji

Abstract

Inflammatory cell infiltration and fibrin deposition play important roles in the development of crescentic glomerulonephritis (GN). In particular, activation of coagulation is an indispensable factor in crescent formation. However, the mechanisms underlying the pathogenesis of crescent formation have not been completely elucidated. We identified the growth factor midkine (MK) as a novel key molecule in the progression of crescentic GN induced by anti–glomerular basement membrane antibody. Despite the lack of significant differences in autologous and heterologous reactions, MK-deficient (Mdk−/−) mice unexpectedly showed a greater number of necrotizing glomerular injuries than wild-type (Mdk+/+) mice. Likewise, more tubulointerstitial damage was observed in Mdk−/−mice, and this damage positively correlated with glomerular injury. Plasminogen activator inhibitor (PAI)-1 was strongly induced in the injured glomerulus of Mdk−/−mice, particularly in crescents and endothelial cells. This enhanced PAI-1 production was associated with an increase in inflammatory cell infiltration and matrix deposition in the glomerulus and the interstitium of Mdk−/−mice. In line with these in vivodata, primary cultured endothelial cells derived from Mdk−/−mice exhibited higher PAI-1 mRNA expression on fibrin challenge and less fibrinolysis than Mdk+/+mice. In contrast, the expression of plasminogen activators was not affected. Our combined data suggest that MK leads to a blockade of PAI-1, which is closely associated with the suppression of crescentic GN.

Published

2013

16. Association of Cardiac Valvular Calcifications and C-Reactive Protein With Cardiovascular Mortality in Incident Hemodialysis Patients: A Japanese Cohort Study

Author

Takahashi, Hiroshi, Ishii, Hideki, Aoyama, Toru, Kamoi, Daisuke, Kasuga, Hirotake, Ito, Yasuhiko, Yasuda, Kaoru, Tanaka, Miho, Yoshikawa, Daiji, Maruyama, Shoichi, Matsuo, Seiichi, Murohara, Toyoaki, and Yuzawa, Yukio

Abstract

Cardiac valve calcification is seen frequently in patients undergoing dialysis. Serum C-reactive protein (CRP) level also is reported to predict future cardiovascular events. We investigated the association among valve calcification, CRP level, and mortality in patients with end-stage renal disease who were just beginning hemodialysis (HD) therapy.

Published

2013

17. GFR Estimation Using Standardized Serum Cystatin C in Japan

Author

Horio, Masaru, Imai, Enyu, Yasuda, Yoshinari, Watanabe, Tsuyoshi, and Matsuo, Seiichi

Abstract

Recently, the Chronic Kidney Disease Epidemiology Collaboration (CKD-EPI) developed glomerular filtration rate (GFR)-estimating equations based on standardized serum cystatin C (CKD-EPIcys) and standardized serum creatinine plus standardized serum cystatin C (CKD-EPIcr-cys). We developed new GFR-estimating equations based on standardized cystatin C for a Japanese population and compared their accuracy with the CKD-EPI equations.

Published

2013

18. Membrane complement regulators protect against fibrin exudation increases in a severe peritoneal inflammation model in rats

Author

Mizuno, Masashi, Ito, Yasuhiko, Mizuno, Tomohiro, Harris, Claire L., Suzuki, Yasuhiro, Okada, Noriko, Matsuo, Seiichi, and Morgan, B. Paul

Abstract

Peritonitis and the rare sequela of encapsulating peritoneal sclerosis (EPS) are serious problems in patients on peritoneal dialysis therapy. Chronic and persistent peritoneal injuries may be a risk factor of EPS. We previously reported that a chronic, proliferative peritonitis developed when zymosan was administered intraperitoneally following scraping injury of rat peritoneum (Mizuno M, Ito Y, Hepburn N, Mizuno T, Noda Y, Yuzawa Y, Harris CL, Morgan BP, Matsuo S. J Immunol183: 1403–1412, 2009). Peritoneal membrane complement regulators (CRegs), especially Crry and CD59, protected from injury by inhibiting local complement activation, suggesting that CRegs play important roles in maintaining homeostasis in rat peritoneum. Here, we investigated roles of complement in the development of EPS by neutralizing CReg function with monoclonal antibodies (MAbs). Proliferative peritonitis was induced by scraping the peritoneum, followed by daily intraperitoneal administration of zymosan. When either Crry or CD59 alone was neutralized by MAb, the tissue injuries were not significantly changed compared with rats without neutralizing MAb. When both Crry and CD59 were neutralized in this model, severe fibrin exudation was observed on the peritoneal surface on day 5, accompanied by inflammatory cell infiltration, resembling the early stages of development of EPS. Dense peritoneal deposition of C3 fragments and membrane attack complex were observed, along with the fibrin exudates. Intravenous administration of cobra venom factor, which profoundly activates complement, further enhanced these pathological changes. Our results show that complement activation in injured peritoneum drives peritoneal inflammation, and that enhancement of complement activation by inhibiting CReg and/or enhancing systemic activation contributes to the initiation of EPS; therefore, anti-complement agents might be of therapeutic value in humans for the treatment of EPS.

Published

2012

19. Basigin/CD147 Promotes Renal Fibrosis after Unilateral Ureteral Obstruction

Author

Kato, Noritoshi, Kosugi, Tomoki, Sato, Waichi, Ishimoto, Takuji, Kojima, Hiroshi, Sato, Yuka, Sakamoto, Kazuma, Maruyama, Shoichi, Yuzawa, Yukio, Matsuo, Seiichi, and Kadomatsu, Kenji

Abstract

Regardless of their primary causes, progressive renal fibrosis and tubular atrophy are the main predictors of progression to end-stage renal disease. Basigin/CD147 is a multifunctional molecule–it induces matrix metalloproteinases and hyaluronan, for example–and has been implicated in organ fibrosis. However, the relationship between basigin and organ fibrosis has been poorly studied. We investigated basigin's role in renal fibrosis using a unilateral ureteral obstruction model. Basigin-deficient mice (Bsg−/−) demonstrated significantly less fibrosis after surgery than Bsg+/+mice. Fewer macrophages had infiltrated in Bsg−/−kidneys. Consistent with these in vivodata, primary cultured tubular epithelial cells from Bsg−/−mice produced less matrix metalloproteinase and exhibited less motility on stimulation with transforming growth factor β. Furthermore, Bsg−/−embryonic fibro blasts produced less hyaluronan and α-smooth muscle actin after transforming growth factor β stimulation. Together, these results demonstrate for the first time that basigin is a key regulator of renal fibrosis. Basigin could be a candidate target molecule for the prevention of organ fibrosis.

Published

2011

20. Expression patterns of connective tissue growth factor and of TGF-β isoforms during glomerular injury recapitulate glomerulogenesis

Author

Ito, Yasuhiko, Goldschmeding, Roel, Kasuga, Hirotake, Claessen, Nike, Nakayama, Masahiro, Yuzawa, Yukio, Sawai, Akiho, Matsuo, Seiichi, Weening, Jan J., and Aten, Jan

Abstract

Transforming growth factor (TGF)-β1, -β2, and -β3are involved in control of wound repair and development of fibrosis. Connective tissue growth factor (CTGF) expression is stimulated by all TGF-β isoforms and is abundant in glomerulosclerosis and other fibrotic disorders. CTGF is hypothesized to mediate profibrotic effects of TGF-β1or to facilitate interaction of TGF-β1with its receptor, but its interactions with TGF-β isoforms in nonpathological conditions are unexplored so far. Tissue repair and remodeling may recapitulate gene transcription at play in organogenesis. To further delineate the relationship between CTGF and TGF-β, we compared expression patterns of CTGF and TGF-β isoforms in rat and human glomerulogenesis and in various human glomerulopathies. CTGF mRNA was present in the immediate precursors of glomerular visceral and parietal epithelial cells in the comma- and S-shaped stages, but not in earlier stages of nephron development. During the capillary loop and maturing glomerular stages and simultaneous with the presence of TGF-β1, -β2, and -β3protein, CTGF mRNA expression was maximal and present only in differentiating glomerular epithelial cells. CTGF protein was also present on precursors of mesangium and glomerular endothelium, suggesting possible paracrine interaction. Concomitant with the presence of TGF-β2and -β3protein, and in the absence of TGF-β1, CTGF mRNA and protein expression was restricted to podocytes in normal adult glomeruli. However, TGF-β1and CTGF were again coexpressed, often with TGF-β2and -β3, in particular in podocytes in proliferative glomerulonephritis and also in mesangial cells in diabetic nephropathy and IgA nephropathy (IgA NP). Coordinated expression of TGF-β isoforms and of CTGF may be involved in normal glomerulogenesis and possibly in maintenance of glomerular structure and function at adult age. Prolonged overexpression of TGF-β1and CTGF is associated with development of severe glomerulonephritis and glomerulosclerosis.

Published

2010

21. Connective tissue growth factor (CTGF/CCN2) is increased in peritoneal dialysis patients with high peritoneal solute transport rate

Author

Mizutani, Makoto, Ito, Yasuhiko, Mizuno, Masashi, Nishimura, Hayato, Suzuki, Yasuhiro, Hattori, Ryohei, Matsukawa, Yoshihisa, Imai, Masaki, Oliver, Noelynn, Goldschmeding, Roel, Aten, Jan, Krediet, Raymond T., Yuzawa, Yukio, and Matsuo, Seiichi

Abstract

Peritoneal fibrosis (PF) is an important complication of peritoneal dialysis (PD) therapy that often occurs in association with peritoneal high transport rate and ultrafiltration failure (UFF). To study the possible pathogenic role of connective tissue growth factor (CTGF) in the relationship of PF and UFF, dialysate CTGF contents (n= 178) and tissue CTGF expression (n= 61) were investigated by ELISA, real-time PCR, immunohistochemistry, and in situ hybridization. CTGF production with and without TGF-β1stimulation in human peritoneal mesothelial cells (HPMC) from the spent patients' peritoneal dialysate (n= 32) was studied in vitro. The dialysate-to-plasma ratio for creatinine (D/P Cr) was positively correlated to dialysate CTGF concentration and estimated local peritoneal production of CTGF. CTGF mRNA expression was 11.4-fold higher in peritoneal membranes with UFF than in pre-PD renal failure peritoneum and was correlated with thickness of the peritoneum. CTGF protein and mRNA were detected in mesothelium and in fibroblast-like cells. In cultured HPMC, TGF-β1-induced expression of CTGF mRNA was increased at 12 and 24 h and was correlated with D/P Cr. In contrast, bone morphogenic protein-4 mRNA expression was inversely correlated with D/P Cr. Our results suggest that high peritoneal transport state is associated with fibrosis and increased peritoneal CTGF expression and production by mesothelial cells, which can be stimulated by TGF-β1. Dialysate CTGF concentration could be a biomarker for both peritoneal fibrosis and membrane function. Functional alteration of mesothelial cells may be involved in progression of peritoneal fibrosis in high transport state.

Published

2010

22. eNOS Knockout Mice with Advanced Diabetic Nephropathy Have Less Benefit from Renin-Angiotensin Blockade than from Aldosterone Receptor Antagonists

Author

Kosugi, Tomoki, Heinig, Marcelo, Nakayama, Takahiro, Matsuo, Seiichi, and Nakagawa, Takahiko

Abstract

While blockade of the renin angiotensin system (RAS) is beneficial in treating many patients with diabetic nephropathy, some patients show a poor response. We hypothesized that the poor response of RAS blockade is attributed to inability to stimulate endothelial nitric oxide. Recently, we reported that diabetic eNOS knockout (KO) mice develop advanced diabetic nephropathy similar to human disease. Here, we tested the hypothesis that blockade of the RAS would be less beneficial in this model than in diabetic wild-type mice. Both enalapril and telmisartan were less effective at reducing renal injury in diabetic eNOSKO mice compared with diabetic wild-type mice. Blood pressure was only transiently reduced by these treatments in diabetic eNOSKO mice and later returned to levels similar to that of untreated diabetic eNOSKO mice. Serum aldosterone tended to be paradoxically higher with enalapril or telmisartan in diabetic eNOSKO mice, whereas these treatments tended to lower aldosterone in diabetic wild-type mice. The pathogenic role of aldosterone was demonstrated by the evidence that spironolactone significantly reduced blood pressure and prevented renal injury. In addition, a higher dose of enalapril also failed to prevent hypertension and renal injury in diabetic eNOSKO mice. In conclusion, an impaired endothelial NO response could lessen the benefit of RAS inhibition in diabetic renal disease. Aldosterone blockade may provide superior protection in this setting.

Published

2010

23. Tissue-type plasminogen activator deficiency attenuates peritoneal fibrosis in mice

Author

Kurata, Kei, Maruyama, Shoichi, Kato, Sawako, Sato, Waichi, Yamamoto, Jun-ichiro, Ozaki, Takenori, Nitta, Atsumi, Nabeshima, Toshitaka, Morita, Yoshiki, Mizuno, Masashi, Ito, Yasuhiko, Yuzawa, Yukio, and Matsuo, Seiichi

Abstract

Peritoneal fibrosis (PF) is an important complication of peritoneal dialysis therapy. The present study was performed to examine the mechanisms of PF in view of the plasminogen activator (PA)/plasmin/matrix metalloproteinase (MMP) cascade. PF was induced in tissue-type PA (tPA) deficient mice and wild-type mice by intraperitoneal injection of chlorhexidine gluconate. Mice were killed on day 21, and tissue samples were taken. Histopathological studies were performed. Plasmin activity, gelatinases activity, and the levels of tPA, transforming growth factor-β1 (TGF-β1), and MMP-2 mRNA were determined. Protein levels of MMP-3, tissue inhibitor of metalloproteinases (TIMP)-1, -2, and -3, phospho-Smad3, membrane-type 1 (MT1)-MMP, and MT3-MMP were also studied. On day 21, tPA +/+ mice showed severe PF, whereas tPA −/− mice showed milder change. Submesothelial basement membranes were dissolved in tPA +/+ mice while they were relatively preserved in tPA −/− mice. The levels of macrophage infiltration, staining for α-smooth muscle actin (α-SMA) and collagen type III, and vascular density were all significantly lower in tPA −/− mice than in tPA +/+ mice. The levels of plasmin activity, pro- and active MMP-2, mRNA expression of tPA and TGF-β1, and phospho-Smad3 protein were also lower in tPA −/− mice. No difference was observed between the two groups concerning the protein levels of MMP-3, TIMP-1, TIMP-2, TIMP-3, MT1-MMP, or MT3-MMP. These results indicate that the presence of tPA enhances inflammation, angiogenesis, and fibrogenesis in the peritoneum of the PF model mice. Activation of the PA/plasmin/MMP cascade may play a pivotal role in the pathogenesis of PF.

Published

2009

24. Prognostic Values of C-Reactive Protein Levels on Clinical Outcome After Implantation of Sirolimus-Eluting Stents in Patients on Hemodialysis

Author

Ishii, Hideki, Toriyama, Takanobu, Aoyama, Toru, Takahashi, Hiroshi, Amano, Tetsuya, Hayashi, Mutsuharu, Tanaka, Miho, Kawamura, Yoshihiro, Yasuda, Yoshinari, Yuzawa, Yukio, Maruyama, Shoichi, Matsuo, Seiichi, Matsubara, Tatsuaki, and Murohara, Toyoaki

Abstract

Percutaneous coronary intervention (PCI) using drug-eluting stents significantly reduces the risk of restenosis in the general population. However, in patients on hemodialysis, adverse cardiac events are frequently seen even if treated with drug-eluting stents. Recent studies suggest that C-reactive protein (CRP) reflects vascular wall inflammation and can predict adverse cardiac events. We evaluated possible prognostic values of CRP on outcomes in patients on hemodialysis undergoing PCI with drug-eluting stents.

Published

2009

25. Prevalence of Pancreatic Cystic Lesions Including Intraductal Papillary Mucinous Neoplasms in Patients With End-Stage Renal Disease on Hemodialysis

Author

Ishikawa, Takuya, Takeda, Kinichi, Itoh, Masatsugu, Imaizumi, Tadashi, Oguri, Kenji, Takahashi, Hiroshi, Kasuga, Hirotake, Toriyama, Takanobu, Matsuo, Seiichi, Hirooka, Yoshiki, Itoh, Akihiro, Kawashima, Hiroki, Kasugai, Toshifumi, Ohno, Eizaburo, Miyahara, Ryoji, Ishigami, Masatoshi, Katano, Yoshiaki, Ohmiya, Naoki, Niwa, Yasumasa, and Goto, Hidemi

Abstract

Pancreatic cystic (PC) lesions are not necessarily rare, and it is important to diagnose whether PC lesions are neoplastic such as intraductal papillary mucinous neoplasm (IPMN) because of its malignant potential. Reports on PC lesions in hemodialysis (HD) patients are remarkably limited. The aim of this study was to clarify the prevalence and characteristics of PC lesions in HD patients.

Published

2009

26. Lipid Droplet-Associated Proteins Protect Renal Tubular Cells from Fatty Acid-Induced Apoptosis

Author

Urahama, Yoshimichi, Ohsaki, Yuki, Fujita, Yutaka, Maruyama, Shoichi, Yuzawa, Yukio, Matsuo, Seiichi, and Fujimoto, Toyoshi

Abstract

Proteinuria is a major cause of tubulointerstitial kidney damage, and free fatty acids bound to albumin are thought to play an important role in its pathogenesis. However, the mechanism whereby proteinuria causes tubulointerstitial damage to the kidney is unclear. Using primary human renal proximal tubular cells, we observed that albumin replete with fatty acids (rBSA) and defatted albumin (dBSA) complexed with linoleic acid (LA) induced significantly more apoptosis than did defatted albumin alone. Oxidative stress was partially involved in apoptotic induction by LA/dBSA but not by rBSA. Administration of fatty acid-bound BSA increased the number of lipid droplets (LDs) and the LD-associated proteins, adipocyte differentiation-related protein and TIP47. LDs are organelles that store esterified fatty acids, and the LD-associated proteins are presumed to facilitate LD formation. Knockdown of adipocyte differentiation-related protein or TIP47 by RNA interference enhanced induction of apoptosis by both rBSA and LA/dBSA. Apoptotic induction was observed similarly when either rBSA or LA/dBSA was applied to only the apical surfaces of polarized LLC-PK1 cells. The present results suggest that LDs and LD-associated proteins have protective effects against apoptosis induced by fatty acid-bound albumin by sequestering free fatty acids. Therapeutic manipulation of these LD-associated proteins could aid in the amelioration of nephritic diseases.

Published

2008

27. Mineralocorticoid receptor blockade ameliorates peritoneal fibrosis in new rat peritonitis model

Author

Nishimura, Hayato, Ito, Yasuhiko, Mizuno, Masashi, Tanaka, Akio, Morita, Yoshiki, Maruyama, Shoichi, Yuzawa, Yukio, and Matsuo, Seiichi

Abstract

Peritoneal fibrosis (PF) is an important complication of long-term peritoneal dialysis. Although mineralocorticoid and mineralocorticoid receptor (MR) have attracted increasing attention in the field of vascular injury, including the heart, kidney, and vessels, little is known about the role of mineralocorticoid in PF. This work was designed to explore the effects of MR blockade on PF. We developed a new model of PF in rats based on mechanical scraping of the peritoneum. This model is characterized by acute-phase inflammation (neutrophil and macrophage infiltration on days 0–3) and late-phase PF (α-smooth muscle actin-positive fibroblast infiltration, type III collagen accumulation, and neoangiogenesis on days 7–14). Peritoneal thickening peaked on day 14. MR was expressed in rat peritoneum and a rat fibroblast cell line. Expression of its effector kinase [serum- and glucocorticoid-induced kinase-1 (Sgk1)], transforming growth factor-β (TGF-β), plasminogen activator inhibitor-1 (PAI-1), and CD31-positive vessels increased during the course of PF. Rats were treated with spironolactone, angiotensin receptor blockade (ARB), or angiotensin-converting enzyme inhibitor (ACEI)-ARB-spironolactone starting at 6 h after peritoneal scraping. All parameters, including peritoneal thickening, number of macrophages and CD31-positive vessels, and expression of monocyte chemoattractant protein-1, TGF-β, PAI-1, and Sgk1, were significantly suppressed by spironolactone (10 mg·kg−1·day−1). The effects of spironolactone (10 and 20 mg·kg−1·day−1) were very similar to those of triple blockade. ARB, but not ACEI, significantly reduced peritoneal thickening. Furthermore, peritoneal function assessed by peritoneal equilibration test was significantly improved by spironolactone. Our results suggest that MR is a potential target to prevent inflammation-induced PF in patients on peritoneal dialysis.

Published

2008

28. High Mobility Group Box Chromosomal Protein 1 in Patients with Renal Diseases

Author

Sato, Fumihiko, Maruyama, Shoichi, Hayashi, Hiroki, Sakamoto, Izumi, Yamada, Shingo, Uchimura, Tomonori, Morita, Yoshiki, Ito, Yasuhiko, Yuzawa, Yukio, Maruyama, Ikuro, and Matsuo, Seiichi

Abstract

AbstractBackground/Aim:The high mobility group box chromosomal protein 1 (HMGB1), a nuclear DNA-binding protein, has recently been recognized as a new proinflammatory cytokine. The purpose of this study was to examine the significance of HMGB1 in patients with renal diseases. Methods:HMGB1 concentrations in sera were measured by enzyme-linked immunosorbent assay, and antibodies against HMGB1 were examined by Western blotting in patients who underwent renal biopsies and in healthy controls. Immunohistochemistry for HMGB1 was also performed. Results:Serum HMGB1 was more likely to be positive in patients who underwent renal biopsies as compared with the controls. Patients with anti-neutrophil cytoplasmic antibody-related glomerulonephritis (ANCA-GN) and those with Henoch-Schönlein purpura nephritis showed a significantly higher tendency to be HMGB1 positive. The presence of anti-HMGB1 antibody was not associated with the presence of serum HMGB1. Immunohistochemistry revealed that HMGB1 was expressed in mononuclear cells in the interstitium or in the glomeruli of some patients with ANCA-GN or IgA nephropathy (IgAN). Subanalysis demonstrated that among patients with IgAN, those who had crescent formation showed a higher tendency to be HMGB1 positive than those who did not. Conclusions:HMGB1 was expressed in the sera of patients with renal diseases who underwent renal biopsies, especially among those who had vasculitis including ANCA-GN, Henoch-Schönlein purpura nephritis, and IgAN with glomerular crescents.Copyright © 2008 S. Karger AG, Basel

Published

2008

29. A Protein Toxin from the Sea Anemone Phyllodiscus semoniTargets the Kidney and Causes a Severe Renal Injury with Predominant Glomerular Endothelial Damage

Author

Mizuno, Masashi, Nozaki, Masatoshi, Morine, Nobuya, Suzuki, Norihiko, Nishikawa, Kazuhiro, Morgan, B. Paul, and Matsuo, Seiichi

Abstract

Envenomation by the sea anemone Phyllodiscus semonicauses fulminant dermatitis and, rarely, acute renal failure in humans. Here, we investigated whether the venom extracted from the nematocysts (PsTX-T) was nephrotoxic when administered intravenously in rats and whether PsTX-T induced activation of the complement system. Although small dose of PsTX-T induced acute tubular necrosis in rats resembling pathology seen in patients, kidneys displayed glomerular injury with glomerular endothelial damage, thrombus formation, mesangiolysis, and partial rupture of glomerular basement membrane, accompanied by severe tubular necrosis at 24 hours after administration of 0.03 mg of PsTX-T per animal, similar to the glomerular findings typical of severe hemolytic uremic syndrome. The early stage injury was accompanied by specific PsTX-T binding, massive complement C3b, and membrane attack complex deposition in glomeruli in the regions of injury and decreased glomerular expression of complement regulators. A pathogenic role for complement was confirmed by demonstrating that systemic complement inhibition reduced renal injury. The isolated nephrotoxic component, a 115-kd protein toxin (PsTX-115), was shown to cause identical renal pathology. The demonstration that PsTX-T and PsTX-115 were highly nephrotoxic acting via induction of complement activation suggests that inhibition of complement might be used to prevent acute renal damage following envenomation by P. semoni.

Published

2007

30. Growth Factor Midkine Is Involved in the Pathogenesis of Diabetic Nephropathy

Author

Kosugi, Tomoki, Yuzawa, Yukio, Sato, Waichi, Kawai, Hanayo, Matsuo, Seiichi, Takei, Yoshifumi, Muramatsu, Takashi, and Kadomatsu, Kenji

Abstract

Diabetic nephropathy is a life-threatening disease associated with diabetes mellitus. Longstanding hyperglycemia induces pathological reactions of glomerular mesangial cells, such as overproduction of extracellular matrix, which finally lead to nephropathy. However, the mechanisms underlying its pathogenesis have not been completely elucidated. Using the Streptozotocin-induced model of diabetes, we report that mice deficient in the growth factor midkine (Mdk−/−) exhibited strikingly milder nephropathy than Mdk+/+ mice, even though both mice showed similar extents of hyperglycemia after Streptozotocin injection. Midkine expression was induced in the glomerular mesangium of Mdk+/+ mice with diabetic nephropathy and in primary cultured mesangial cells exposed to high glucose. Mdk−/− mesangial cells exhibited reduced phosphorylation of protein kinase C and extracellular signal-regulated kinase as well as reduced production of transforming growth factor-β1on high glucose loading. Addition of exogenous midkine restored extracellular signal-regulated kinase phosphorylation in Mdk−/− cells under high glucose conditions, whereas a midkine antisense oligodeoxynucleotide suppressed midkine in Mdk+/+ cells. Therefore, this study identifies midkine as a key molecule in diabetic nephropathy and suggests that midkine accelerates the intracellular signaling network evoked by hyperglycemia in nephropathy.

Published

2006

31. Shiga Toxin 1 Causes Direct Renal Injury in Rats

Author

Yamamoto, Elise T., Mizuno, Masashi, Nishikawa, Kiyotaka, Miyazawa, Shinobu, Zhang, Lianshan, Matsuo, Seiichi, and Natori, Yasuhiro

Abstract

Infection with Shiga toxin (Stx)-producing Escherichia coli has been implicated to cause hemolytic uremic syndrome, which is characterized by histological abnormalities such as microvascular thrombi and tubular cell damage in the kidney. Although Stx is known to be the major virulence factor of the pathogen, it is still unclear whether Stx directly impairs renal cells in vivo to cause such histological changes and deterioration of renal function. To assess the consequence of the direct action of Stx on renal cells, left kidneys of rats were perfused with Stx1 from the renal artery through the renal vein and then revascularized. Kidneys of control animals were perfused with the vehicle alone. On day 1, apoptosis and induction of tumor necrosis factor alpha gene expression were noticed to occur in the medulla of the Stx1-perfused kidneys. On day 3, extensive tubular injuries were observed by light microscopy: aggregated platelets and monocytic infiltrates in both glomeruli and the medullary interstitium were detected by immunostaining. Tubular changes were more extensive on day 9, with areas of infarction seen in the cortex and medulla. These changes were not found to occur in the sham-operated kidneys. No obvious glomerular changes were detected by light microscopy at any time point. When nonperfused right kidneys were removed after the Stx1 perfusion of the left kidneys, the serum creatinine and blood urea nitrogen levels were increased from day 2, and acute renal failure followed on day 3. These results indicate that Stx1 caused glomerular platelet aggregation, tubular damage, and acute deterioration of renal function by acting directly on renal cells.

Published

2005

32. Expression of CD46 in Developing Rat Spermatozoa: Ultrastructural Localization and Utility as a Marker of the Various Stages of the Seminiferous Tubuli1

Author

Mizuno, Masashi, Harris, Claire L., Suzuki, Norihiko, Matsuo, Seiichi, and Morgan, B. Paul

Abstract

Identification of the various stages of the seminal tubule epithelium that are important in spermatogenesis in humans and rodents requires considerable expertise for analysis of ultrastructural appearance under light microscopy. Few good stage-specific markers have been reported to facilitate the process. We recently described characterization of the expression of CD46 (membrane cofactor protein) in the rat using a novel monoclonal antibody. Expression of CD46 was restricted to spermatozoa and their immediate precursors in the testis. In the present study, we used a combination of morphological analyses, known acrosome markers, actin staining, direct nuclear staining, and staining for CD46 to delineate precisely the subcellular location of CD46. Staining of CD46 colocalized with known acrosome markers in late spermatids and mature spermatozoa and was confirmed by electron microscopy to be acrosome-restricted. Expression was first detected in step 7 spermatids, whereas known markers were not expressed until step 9. The CD46 staining pattern differed through spermatid development, and distinct patterns of staining could be identified that, when combined with 4′-6-diamino-2-phenylindole-2HCl nuclear staining, enabled the accurate staging of the seminiferous tubule epithelium in different profiles. This detailed description of the spatiotemporal expression patterns of CD46 provides a valuable tool for analysis of spermatogenesis in the rat. Furthermore, this information will aid ongoing studies regarding the roles of CD46 in acrosome-related spermatozoal functions.

Published

2005

33. Lack of the Growth Factor Midkine Enhances Survival against Cisplatin-Induced Renal Damage

Author

Kawai, Hanayo, Sato, Waichi, Yuzawa, Yukio, Kosugi, Tomoki, Matsuo, Seiichi, Takei, Yoshifumi, Kadomatsu, Kenji, and Muramatsu, Takashi

Abstract

Although cisplatin acts directly on proximal tubule epithelial cells and causes cell death, little is known regarding the biological significance of its secondary effects, such as inflammation. The growth factor midkine is highly expressed in the proximal tubule and exerts ambivalent activities as to cisplatin nephrotoxicity, ie, anti-apoptotic and chemotactic ones. Here we report that midkine-deficient mice show a significantly higher survival rate than wild-type mice. The levels of blood urea nitrogen and tubular degeneration and apoptosis were higher in wild-type mice despite the anti-apoptotic activity of midkine. We found that recruitment of neutrophils was more enhanced in wild-type mice, this being consistent with the chemotactic activity of midkine. Midkine expression in wild-type mice persisted for 24 hours, and then dramatically decreased. Preadministration of midkine anti-sense oligodeoxyribonucleotide to wild-type mice suppressed midkine expression, and consequently neutrophil infiltration. It is of note that neutrophil infiltration, apoptosis, and elevation of blood urea nitrogen became conspicuous sequentially, namely 1, 2, and 3 days after cisplatin administration, respectively. These findings suggest that early molecular events involving midkine induce inflammatory response and their circuits eventually enhance the death of the proximal tubule epithelial cells. The results indicate the crucial role of inflammation in cisplatin-induced renal damage, and provide a candidate molecular target for its prevention.

Published

2004

34. Non-dipping is a potent predictor of cardiovascular mortality and is associated with autonomic dysfunction in haemodialysis patients.

Author

Liu, Manchang, Takahashi, Hiroshi, Morita, Yoshiki, Maruyama, Shoichi, Mizuno, Masashi, Yuzawa, Yukio, Watanabe, Midoriko, Toriyama, Takanobu, Kawahara, Hirohisa, and Matsuo, Seiichi

Abstract

Lack of nocturnal blood pressure (BP) fall (non-dipping) is common among haemodialysis (HD) patients, but much less is known regarding its association with cardiovascular (CV) disease morbidity and mortality.

Published

2003

35. Risk Factors for IgA Nephropathy: A Case-Control Study with Incident Cases in Japan

Author

Wakai, Kenji, Nakai, Shigeru, Matsuo, Seiichi, Kawamura, Takashi, Hotta, Nigishi, Maeda, Kenji, and Ohno, Yoshiyuki

Abstract

Background/Aim:Our previous study with prevalent cases suggested that some genetic, immunological and lifestyle-related factors increased the risk of immunoglobulin A nephropathy (IgAN). To confirm this hypothesis, we conducted another case-control study. Methods:The study included 116 incident cases and 276 sex-, age- and residence-matched controls in central Japan. Information on family and individual history and on lifestyle was collected using a self-administered questionnaire. The strength of association between IgAN and a potential risk factor was assessed by calculating an odds ratio. Results:A family history of chronic glomerulonephritis, susceptibility to the common cold, episodes of tonsillitis in the preceding year, preference for salty foods and a high intake of rice and n–6 polyunsaturated fatty acids (PUFA) were associated with an increased risk of IgAN. Coffee consumption and dietary calcium intake were somewhat negatively related to the risk. A significance of alcohol drinking, use of vitamin supplements, consumption of raw eggs and intake of nutrients other than n–6 PUFA and calcium, though previously suggested, was not shown in the present study. Conclusion:Our findings imply that some genetic factors, immune response to infections in the upper respiratory tract and nutritional imbalance would promote the development of IgAN.

Published

2002

36. Membrane complement regulators protect against the development of type II collagen–induced arthritis in rats

Author

Mizuno, Masashi, Nishikawa, Kazuhiro, Spiller, O. Brad, Morgan, B. Paul, Okada, Noriko, Okada, Hidechika, and Matsuo, Seiichi

Abstract

To investigate changes in the distribution patterns of membrane complement regulators (MCRs) during the development of type II collagen–induced arthritis (CIA) and to examine the protective effects of these molecules against the augmentation of CIA in the knee joint. Immunohistochemistry was used to examine the distribution of the MCRs Crry, DAF, and CD59 in the synovium of knee joints before and 2, 4, and 10 weeks after induction of CIA by immunization with type II collagen. In addition, at 2 or 10 weeks after induction of CIA, rats were injected intraarticularly with anti-Crry and/or anti-CD59 as the F(ab')2 fraction of monoclonal antibodies (mAb). Knee joint swelling and histologic changes in the synovium were examined 2 weeks after mAb injection. Synovial expression of Crry, DAF, and CD59 decreased in parallel with increased inflammation. When Crry and CD59 were functionally blocked at 2 weeks after the induction of CIA, swelling of the knee joints was markedly increased. Blocking of either regulator alone had no effect on swelling. Thickening of the synovial surface and proliferation of subsynovial tissue were all increased after blocking Crry and CD59, whereas blocking of either MCR alone had no effect. When both Crry and CD59 were blocked, deposits of membrane attack complex were found in the synovium. Our findings indicate that in rats with CIA and severely inflamed synovium, local expression of MCR is reduced. The MCRs Crry and CD59 appear to suppress the development of CIA.

Published

2001

37. Effects of a new synthetic selectin blocker in an acute rat thrombotic glomerulonephritis

Author

Ito, Isao, Yuzawa, Yukio, Mizuno, Masashi, Nishikawa, Kazuhiro, Tashita, Akira, Jomori, Takahito, Hotta, Nigishi, and Matsuo, Seiichi

Abstract

In an attempt to explore a novel therapeutic approach, a new synthetic sulfatide derivative (SKK60037) was evaluated in an acute rat model of P-selectin and leukocyte-dependent thrombotic glomerulonephritis (TG). In vitro, SKK60037 inhibits the function of P- and L-selectin more effectively than sialyl Lewis X (sLex), a well-established selectin blocker. TG was induced by the intravenous administration of nephrotoxic globulin (NTG) to rats pretreated with a subclinical dose of lipopolysaccharide. In this model, platelet accumulation was remarkable within 10 minutes after induction of disease, followed by the infiltration of leukocytes, mainly neutrophils and macrophages. Thrombus formation and fibrinogen deposition in the glomeruli were observed within 1 hour, and they proceeded until 6 hours. P-selectin was highly expressed in glomeruli, whereas E-selectin and L-selectin ligands were not detected. We tested the effects of SKK60037 in this model in comparison with sLexand antirat P-selectin monoclonal antibody (ARP2-4). SKK60037 blocked platelet accumulation in glomerular capillaries at 10 minutes after NTG injection. At 6 hours, leukocyte infiltration and thrombosis were significantly suppressed. Protective effects of SKK60037 were similar to those of ARP2-4, whereas sLexshowed minimum effect. The superior effects and more favorable characteristics of SKK60037 to sLexsuggest the potential of SKK60037 for clinical application. [copy ] 2001 by the National Kidney Foundation, Inc.

Published

2001

38. Simultaneous Measurement of Anandamide and 2-Arachidonoylglycerol by Polymyxin B-Selective Adsorption and Subsequent High-Performance Liquid Chromatography Analysis: Increase in Endogenous Cannabinoids in the Sera of Patients with Endotoxic Shock

Author

Wang, Yin, Liu, Yan, Ito, Yasuhiko, Hashiguchi, Teruto, Kitajima, Isao, Yamakuchi, Munekazu, Shimizu, Hideaki, Matsuo, Seiichi, Imaizumi, Hitoshi, and Maruyama, Ikuro

Abstract

Anandamide (ANA) and 2-arachidonoylglycerol (2-AG), two endogenous cannabinoids, can be generated by activated macrophages and platelets, respectively, in the context of endotoxic shock, and are proposed to play a crucial role in the induction of the shock-related hypotension. Taking advantage of our recently discovered function of polymyxin B (PMB) binding to ANA and 2-AG, we developed a new method for measuring ANA and 2-AG by applying PMB-immobilized beads to selectively adsorb them in biological fluids, instead of organic solvent extraction. The eluate from beads can be directly fractionated by reverse-phase high-performance liquid chromatography (HPLC), and the fractionations corresponding to authentic ANA and 2-AG are collected and derivatized with fluorogenic reagent and subsequently quantified by HPLC with fluorometric detection. The calibration graphs of ANA and 2-AG were linear over a range of 1 to 500 pmol/ml. The limits of detection for ANA and 2-AG were 20 and 50 fmol, respectively. Intraassay precision was 2.24–4.25 and 3.47–5.44%, and interassay was 4.05–6.14 and 4.92–7.28% for ANA and 2-AG, respectively. Using this method, we first determined a 4-fold and 3-fold higher level of ANA and 2-AG, respectively, in the sera of patients with endotoxic shock than in normal serum. This finding should help in elucidating the role of the endogenous cannabinoids in the hypotension of human endotoxic shock. This method is rapid, sensitive, and reliable for simultaneously quantifying ANA and 2-AG in biological fluids, and has potential for clinical usage. Copyright 2001 Academic Press.

Published

2001

39. Glomerulocystic Kidney Associated With Subacute Necrotizing-Encephalomyelopathy

Author

Yamakawa, Taishi, Yoshida, Futoshi, Kumagai, Toshiyuki, Watanabe, Hirohisa, Takano, Akemi, Mizuno, Masashi, Ikeguchi, Hiroshi, Morita, Yoshiki, Sobue, Gen, and Matsuo, Seiichi

Abstract

A 22-year-old man with subacute necrotizing-encephalomyelopathy (SNE; Leigh's disease) was diagnosed as having progressive renal dysfunction. The clinical diagnosis of Leigh's disease was obtained by the typical central nervous lesions, abnormalities in other organs, and increased lactate concentrations in blood and cerebrospinal fluid. We performed an open biopsy of the right kidney. Light microscopic studies of the renal specimen showed diffuse glomerulocystic kidney (GCK) with tubulointerstitial damage. Electron microscopic examination showed marked swelling and increase in the number of mitochondria of the renal tubular epithelial cells. Therefore, it is suggested that mitochondrial disease seems to play an important role in developing GCK.

Published

2001

40. Acute renal failure after a sea anemone sting

Author

Mizuno, Masashi, Nishikawa, Kazuhiro, Yuzawa, Yukio, Kanie, Tami, Mori, Hijiri, Araki, Yasutetsu, Hotta, Nigishi, and Matsuo, Seiichi

Abstract

A 27-year-old man suffering from severe swelling and pain in his right arm was referred to our hospital. He showed signs of acute renal failure (ARF) with severe dermatitis of his right arm. Three days before being admitted, he accidentally touched some kind of marine organism with his right hand while snorkeling in the Sulu Sea around Cebu Island. Within a few minutes, he was experiencing severe pain in his right hand. Then his right hand gradually became swollen. The marine creature responsible for this injury was thought to have been a sea anemone, which is a type of coelenterate. Histologic findings of a renal biopsy indicated that acute tubular necrosis (ATN) had caused ARF in this patient’s case. Supportive therapies improved renal function of this patient, and steroid pulse therapy attenuated the severe skin discoloration. The ATN was thought to have been caused by the poison from a sea anemone because there were no other conceivable reasons for the patient’s condition. This is the first time that a marine envenomation case has been reported in which the sting of a sea anemone has caused ATN without the failure of any other organs.

Published

2000

41. Molecular Cloning and Partial Characterization of Rat Procarboxypeptidase R and Carboxypeptidase N

Author

Kato, Tomomi, Akatsu, Hiroyasu, Sato, Tomoo, Matsuo, Seiichi, Yamamoto, Takayuki, Campbell, William, Hotta, Nigishi, Okada, Noriko, and Okada, Hidechika

Abstract

Carboxypeptidase R (EC 3.4.17.20) (CPR) and carboxypeptidase N (EC 3.4.17.3) (CPN) cleave carboxy‐terminal arginine or lysine residues from biologically active peptides such as kinins or anaphylatoxins in the circulation thereby regulating their activities. Although CPN is present in a stable active form in plasma, CPR is generated from proCPR, a plasma zymogen, by proteolytic enzymes such as thrombin, thrombin‐thrombomodulin complex and plasmin. We have isolated rat proCPR and CPN cDNA clones which can induce enzymatic activities in culture supernatants of the transfected cells. mRNA of proCPR was detected only in rat liver by Northern hybridization and showed hepatocyte‐specific expression. Expression of proCPR mRNA was enhanced following LPS injection, indicating that proCPR production is increased under inflammatory conditions.

Published

2000

42. Abolition of anti-glomerular basement membrane antibody-mediated glomerulonephritis in FcRγ-deficient mice

Author

Wakayama, Hisashi, Hasegawa, Yoshinori, Kawabe, Tsutomu, Hara, Toru, Matsuo, Seiichi, Mizuno, Masashi, Takai, Toshiyuki, Kikutani, Hitoshi, and Shimokata, Kaoru

Abstract

Several recent studies have demonstrated the central role of Fc receptors (FcR) rather than the complement system in triggering hypersensitivity reactions. We investigated the role of FcR for IgG (FcγR) using a murine model of accelerated anti-glomerular basement membrane (GBM) antibody-mediated glomerulonephritis as a representative of type II hypersensitivity diseases. Intravenous injection of rabbit anti-GBM antibody after preimmunization with normal rabbit IgG induced proteinuria and azotemia in wild-type C57BL / 6 and CD40^+ / – mice but not in FcR γ chain (FcRγ)^– / – mice or CD40^– / – mice. Light microscopic findings revealed marked tissue damage in the glomeruli of wild-type C57BL / 6 and CD40^+ / – mice. However, no tissue damage except polymorphonuclear cell infiltration was observed in the glomeruli of FcRγ^– / – mice. The glomeruli of CD40^– / – mice were almost normal. Immunohistochemistry revealed the binding of rabbit IgG to the GBM in all mice injected with anti-GBM antibody. However, depositions of mouse IgG and complement to the glomeruli were not observed in CD40^– / – mice, and deposition of fibrin was not observed in FcRγ^– / – or CD40^– / – mice. These findings suggest that FcγR may initiate anti-GBM antibody-mediated renal disease. We conclude that FcγR rather than the complement system is critically involved in the development of type II hypersensitivity diseases.

Published

2000

43. Constitutive Activation of MAP Kinase Kinase (MEK1) Is Critical and Sufficient for the Activation of MMP-2

Author

Kurata, Hisashi, Thant, Aye Aye, Matsuo, Seiichi, Senga, Takeshi, Okazaki, Kenji, Hotta, Nigishi, and Hamaguchi, Michinari

Abstract

We investigated the role of MEK1 signaling in MMP-2 activation by use of constitutive active/dominant negative forms of MEK1 and MEK1-specific inhibitor. We found that cell transformation with active forms of MEK1 dramatically increased secretion and proteolytic activation of MMP-2 and subsequently stimulated invasiveness of cells. Contrary, expression of dominant negative form of MEK1 in v-src-transformed cells or in Con A-activated cells resulted in the suppression of the augmented secretion and proteolytic activation of MMP-2. In addition, treatment of v-src-transformed cells with PD98059, a MEK1-specific inhibitor, strongly suppressed the secretion and activation of MMP-2, whereas treatment with wortmannin, a PI3 kinase inhibitor, showed no clear effect on MMP-2 secretion. Taken together, these results strongly suggest that MEK–MAP kinase signaling, but not PI3 kinase signaling, plays a critical role in the activation of MMP-2 secretion and, subsequently, in the invasiveness of v-src-transformed cells.

Published

2000

44. Risk factors for IgA nephropathy: A case-control study in Japan

Author

Wakai, Kenji, Kawamura, Takashi, Matsuo, Seiichi, Hotta, Nigishi, and Ohno, Yoshiyuki

Abstract

To disclose the risk factors for immunoglobulin A nephropathy (IgAN), we conducted a case-control study in the Tokai area of central Japan. The subjects were 94 patients, aged 20 years or older at diagnosis, who had histologically confirmed IgAN. Two sex-, age-, and residence-matched controls were randomly selected for each case from the general population. Information on medical history and lifestyle was collected using a self-administered questionnaire. The strength of association between IgAN and a potential risk factor was assessed by calculating an odds ratio. A family history of chronic nephritis, susceptibility to the common cold, preference for salty foods, frequent consumption of raw eggs, and a high intake of carbohydrates, including rice, were significantly associated with an increased risk for IgAN. Alcohol consumption, use of antioxidant vitamin supplements, and a high intake of protein, fat, monounsaturated fatty acids, and all/n-3 polyunsaturated fatty acids were somewhat protective against IgAN. Episodes of tonsillitis and exposure to organic solvents were found not to be associated with the risk in the present study. Our findings may provide some clues to the cause of IgAN.

Published

1999

45. Complement-mediated renal injury: Mechanisms and role of membrane regulators of complement

Author

Matsuo, Seiichi, Morita, Yoshiki, Mizuno, Masashi, Nishikawa, Kazuhiro, and Yuzawa, Yukio

Abstract

Complement-mediated renal injuries occur not only in immune-mediated diseases, but also in nonimmune conditions. Membrane regulators of complement abundantly expressed in the kidney seem to play important roles in the maintenance of the normal function of the kidney under physiologic and pathologic conditions. We hope these findings have relevance to the development of therapeutic strategies for progressive renal injury.

Published

1998

46. Ultrastructural observation of glomerular lesions in a new mouse strain manifesting high proteinuria and progressive glomerulosclerosis

Author

Yoshida, Futoshi, Fujishima, Hiroshi, Kuno, Naoko, Matsuo, Seiichi, and Tomita, Takeshi

Abstract

Abstract: Renal pathology of the FGS/Nga strain of mice, which has been known to develop proteinuria and progressive glomerulosclerosis, was studied by light and electron microscopy. Sclerotic changes had increased by 6 months and most of the glomeruli were totally obsolescent by 10 months. By electron microscopy, electron dense deposits were seen in the mice by 3 months and thereafter. Splitting or the irregular thickening of the glomerular basement membrane (GBM) was observed, and some mice showed reticulation in the GBM. The fixed negative charges detectable with polyethyleneimine (PEI) were decreased in the mice with massive proteinuria.

Published

1993

47. The Target Antigen of Anti-Tubular Basement Membrane Antibody-Mediated Interstitial Nephritis

Author

Miyazato, Hirofumi, Yoshioka, Kazuo, Hino, Satoshi, Aya, Naobhumi, Matsuo, Seiichi, Suzuki, Norihiko, Suzuki, Yasuyuki, Sinohara, Hyogo, and Maki, Sunao

Abstract

Our previous studies showed that 54 kD and 48 kD tubular basement membrane (TBM) proteins were the major form of the target antigen involved in anti-TBM antibody-mediated tubulo-interstitial nephritis in humans. In those studies, we isolated the 54 kD glycoprotein (named gp54) from collagenase-digested bovine TBM. NH2-terminal amino acid sequencing indicated that gp54 represented a newly defined glycoprotein. In this study, we further characterized the target antigen, using mouse monoclonal antibodies to gp54 and polyclonal anti-gp54 peptide antibody. Two monoclonal antibodies (H79 and H80) were established, and they reacted, by immunofluorescence, predominantly with the proximal TBM of humans, rabbits, and Wistar, Sprague-Dawley, and Brown-Norway rats, but not with that of Lewis rats. They were also fixed by blotting intensely to the 54 kD component and weakly to the 48 kD component of collagenase-digested human TBM. In vivo transfer of H79 to Wistar rats showed extensive linear binding of mouse IgG to the TBM and the basal membrane of the small intestine; however, no pathologic changes were seen by light microscopy. The anti-gp54 peptide antibody reacted with both the 54 kD and 48 kD TBM components of human TBM. mRNA was prepared from rabbit kidneys, and fractionated to enrich mRNA encoding the 54 kD and 48 kD peptides. On in vitro translation experiments with the mRNA fraction, the 54 kD and 48 kD peptides were immunoprecipitated with anti-gp54 antibodies. These findings indicate that the 54 kD and 48 kD components are encoded with different mRNA, but that they share the same antigenic epitope. It is likely that they are structurally related and exist as isoforms.

Published

1994

48. ACUTE RENAL FAILURE AND DEGENERATIVE TUBULAR LESIONS ASSOCIATED WITH IN SITU FORMATION OF ADENOVIRUS IMMUNE COMPLEXES IN A PATIENT WITH ALLOGENEIC BONE MARROW TRANSPLANTATION

Author

YUZAWA, YUKIO, AOI, NAOKI, FUKATSU, ATSUSHI, ICHIDA, SHIZUNORI, YOSHIDA, FUTOSHI, AKATSUKA, YOSHIKI, MINAMI, SABURO, KODERA, YOSHINAO, and MATSUO, SEIICHI

Abstract

We describe the development of acute renal failure and degenerative tubular lesions associated with local immune deposits in a patient with allogeneic bone marrow transplantation. A 21-year-old man with an acute myelocytic leukemia received a bone marrow graft from a cousin mismatched for a single HLA-DR locus antigen. Hemorrhagic cystitis due to adenovirus type 11 infection occurred 26 days after transplantation, and 17 days later the patient developed acute renal failure. A study of renal tissue obtained by needle biopsy showed degenerative and necrotic lesions, especially in the distal part of the nephron. By electron microscopy adenovirus type 11 particles were found in the nuclei of tubular cells and in cellular debris in tubular lumina. By immunofluorescence technique, granular immune deposits containing adenovirus type 11 related antigen(s), immunoglobulins, C3, and membrane attack complex (MAC) C5b-9 of the complement system were detected along the tubular basement membranes but not in glomeruli. The patient's IgG did not bind to normal human kidneys. These findings suggest that adenovirus type 11 directly induced acute tubular damage, and that the tubular immune deposits were formed “in situ” by viral antigens and circulating viral antibody.

Published

1993

49. Glucocorticoid-induced apoptosis of rat mesangial cells in culture

Author

Miyazato, Hirofumi, Takemura, Tsukasa, Hino, Satoshi, Yagi, Kazuro, Fukushima, Kyohji, Matsuo, Seiichi, and Yoshioka, Kazuo

Abstract

Apoptosis of glomerular mesangial cells is shown in experimental and human glumerulonephritis. But it is unclear whether or not glucocorticoids can induce apoptosis in mesangial cells. Rat mesangial cells in culture were incubated with dexamethazone and methylprednisolone. Apoptosis was evaluated by DNA-specific staining with fluorescent dye (H33258), in situ nick end labeling, gel electrophoresis of extracted DNA, and electron microscopy. The proportion of lysed cells and cells positive for nick end labeling increased at a concentration of 0.2 to 5 mmol/L of dexamethazone and methylprednisolone. Chromatin condensation and DNA ladders in those cells were also seen. Actinomycin D, a transcriptional inhibitor, or cycloheximide, a translational inhibitor, partially blocked glucocorticoid-induced apoptosis of rat mesangial cells. Glucocorticoids induced typical apoptosis in rat mesangial cells. These data provide new information on the pharmacologic action of glucocorticoids on mesangial cells.

Published

1998

50. Cost-effectiveness of behavior modification intervention for patients with chronic kidney disease in the FROM-J study

Author

Okubo, Reiko, Kondo, Masahide, Hoshi, Shu-Ling, Okada, Masafumi, Doi, Mariko, Takahashi, Hideto, Kai, Hirayasu, Saito, Chie, Iseki, Kunitoshi, Iseki, Chiho, Watanabe, Tsuyoshi, Narita, Ichiei, Matsuo, Seiichi, Makino, Hirofumi, Hishida, Akira, and Yamagata, Kunihiro

Abstract

Chronic kidney disease (CKD) is a significant public health problem. An advanced, or innovative, CKD care system of clinical practice collaboration among general physicians (GPs), nephrologists, and other healthcare workers achieved behavior modification in patients with Stage 3 CKD in the Frontier of Renal Outcome Modifications in Japan (FROM-J) study. This behavior modification intervention consisted of educational sessions on nutrition and lifestyle, as well as encouragement of patients’ regular visits. The intervention contributed to slowing CKD progression. This study aimed to evaluate the cost-effectiveness of the widespread diffusion of the behavior modification intervention proven effective by the FROM-J study.

Published

2021