Selective Antagonism of the ET_A Receptor, but Not the ET_B Receptor, Is Protective Against Ischemic Acute Renal Failure in Rats
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概要
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We investigated the effects of ABT-627, a selective ETA-receptor antagonist, and A-192621, a selective ETB-receptor antagonist, on ischemic acute renal failure(ARF)in rats.Ischemic ARF was induced by clamping the left renal artery and vein for 45min, 2 weeks after the contralateral nephrectomy.Renal function in untreated ARF rats markedly decreased at 24h after reperfusion and thereafter tended to recover gradually.ABT-627(1mg/kg, i.v.)administration before ischemia markedly attenuated the renal dysfunction induced by the ischemia/reperfusion, whereas A-192621(3mg/kg, i.v.)pretreatment was without effect.Histopathological examination of the kidney of untreated ARF rats revealed severe renal damage such as tubular necrosis, proteinaceous casts in tubuli and medullary congestion.Histologically evident damage was improved by pretreatment with ABT-627, but not with A-192621.Daily oral administration of ABT-627(10mg/kg per day), but not A-192621(30mg/kg per day), given after the ischemia/reperfusion period also exerted protective effects.These findings clearly indicate that endothelin, acting via the ETA receptor, participates in the pathogenesis of ischemic ARF.Thus, selective ETA-receptor antagonism may be useful in the treatment of human ischemic ARF, whereas selective blockade of the ETB receptor will probably be ineffective.
- 2000-04-01
著者
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Takaoka Masanori
Department Of Internal Medicine Iii Osaka Medical College
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MATSUMURA Yasuo
Department of Pharmacology, Osaka University of Pharmaceutical Sciences
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KOBAYASHI YUTAKA
Department of Pediatrics, Kobe Central Municipal Hospital
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Kobayashi Yutaka
Department Of Environmental Medicine Graduate School Of Medical Sciences Kyushu University
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Kobayashi Masayuki
Hematology Division National Cancer Center Hospital
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Matsumura Yasuo
Laboratory Of Pathological And Molecular Pharmacology Osaka University Of Pharmaceutical Sciences
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Matsumura Yasuo
Department Of Pharmacology Osaka University Of Phiarmaceutical Sciences
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Matsumura Yasuo
Department Of Mechanical Physics Kyoto University
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Takaoka Masanori
Department Of Electrical And Electronic Engineering University Of Miyazaki
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Matsumura Y
Asahi Glass Co. Ltd. Tokyo Jpn
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KURO Toshihiko
Department of Pharmacology, Osaka University of Pharmaceutical Sciences
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Takaoka M
Laboratory Of Pathological And Molecular Pharmacology Osaka University Of Pharmaceutical Sciences
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KOHNOU Kaori
Department of Pharmacology, Osaka University of Pharmaceutical Sciences
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OPGENORTH Terry
Diabetes and Vascular Research Division, Abbott Laboratories
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WESSALE Jerry
Diabetes and Vascular Research Division, Abbott Laboratories
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Kawai Yu
Department Of Pharmacology Osaka University Of Pharmaceutical Sciences
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Kuro T
Department Of Pharmacology Osaka University Of Pharmaceutical Sciences
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Kuro Toshihiko
Department Of Pharmacology Osaka University Of Pharmaceutical Sciences
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Kohnou Kaori
Department Of Pharmacology Osaka University Of Pharmaceutical Sciences
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Wessale Jerry
Diabetes And Vascular Research Division Abbott Laboratories
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Opgenorth Terry
Diabetes And Vascular Research Division Abbott Laboratories
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Kobayashi Yutaka
Department Of Cardiovascular Surgery Iwaki Kyoritsu General Hospital
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Kobayashi Yutaka
Department Of Applied Physics Fukui University
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