Use of prostaglandin I2 analog in treatment of massive hepatic necrosis associated with endothelial cell injury and diffuse sinusoidal fibrin deposition |
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Authors: | Dr. Kenji Fujiward MD PhD Satoshi Mochida MD Akihiko Ohno MD Masahiro Arai MD Atsushi Matsui MD Naohiko Masaki MD Keiichi Hirata MD Tomoaki Tomiya MD Miho Yamaoka MD Sumiko Nagoshi MD Yasuhiko Ohta MD Itsuro Ogata MD Antonio Francavilla MD David H. Van Thiel MD Thomas E. Starzl MD PhD |
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Affiliation: | (1) Third Department of Internal Medicine, Saitama Medical School, 38 Morohongo, Moroyama-machi, Iruma-gun, 350-04 Saitama, Japan;(2) the First Department of Internal Medicine, Faculty of Medicine, University of Tokyo, Japan;(3) University of Pittsburgh, Pittsburgh, Pennsylvania |
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Abstract: | Endothelial cell damage causes massive hepatic necrosis as a result of fibrin deposition in the hepatic sinusoids. When a stable analog of prostaglandin I2, beraprost sodium, was administered to rats given either dimethylnitrosamine, carbon tetrachloride, or endotoxin followingCorynebacterium parvum administration, the hepatic necrosis produced in each was attenuated, but to a greater extent in the dimethylnitrosamine and endotoxin/Corynebacterium parvum models, where fibrin deposition in the hepatic sinusoids occurs, as compared to the carbon tetrachloride model, where such fibrin deposition does not occur. Beraprost sodium reduced the expected increase of portal venous pressure in the endotoxin/Corynebacterium parvum model without affecting plasma thrombin-antithrombin III complex levels. Beraprost sodium also significantly reduced cell killing of both isolated rat hepatocytes and hepatic sinusoidal endothelial cells exposed totert-butyl hydroperoxide when compared to controls. Beraprost sodium could prove to be a therapeutic candidate for the treatment of hepatic necrosis, particularly in cases associated with fibrin deposition in the hepatic sinusoids because of its fibrin clot-clearning action. |
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Keywords: | Prostaglandin I2 beraprost sodium hepatic necrosis intravascular coagulation sinusoidal endothelial cells cytoprotection |
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