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Title: Deleterious effect of oltipraz on extrahepatic cholestasis in bile duct-ligated mice
Authors: Jittima Weerachayaphorn
Yuhuan Luo
Albert Mennone
Carol J. Soroka
Kathy Harry
James L. Boyer
Yale University
Mahidol University
Keywords: Medicine
Issue Date: 1-Jan-2014
Citation: Journal of Hepatology. Vol.60, No.1 (2014), 160-166
Abstract: Background & Aims Oltipraz (4-methyl-5(pyrazinyl-2)-1-2-dithiole-3- thione), a promising cancer preventive agent, has an antioxidative activity and ability to enhance glutathione biosynthesis, phase II detoxification enzymes and multidrug resistance-associated protein-mediated efflux transporters. Oltipraz can protect against hepatotoxicity caused by carbon tetrachloride, acetaminophen and alpha-naphthylisothiocyanate. Whether oltipraz has hepato-protective effects on obstructive cholestasis is unknown. Methods We administered oltipraz to mice for 5 days prior to bile duct ligation (BDL) for 3 days. Liver histology, liver function markers, bile flow rates and hepatic expression of profibrogenic genes were evaluated. Results Mice pretreated with oltipraz prior to BDL demonstrated higher levels of serum aminotransferases and more severe liver damage than in control mice. Higher bile flow and glutathione secretion rates were observed in unoperated mice treated with oltipraz than in control mice, suggesting that liver necrosis in oltipraz-treated BDL mice may be related partially to increased bile-acid independent flow and biliary pressure. Oltipraz treatment in BDL mice enhanced α-smooth muscle actin expression, consistent with activation of hepatic stellate cells and portal fibroblasts. Matrix metalloproteinases (Mmp) 9 and 13 and tissue inhibitors of metalloproteinases (Timp) 1 and 2 levels were increased in the oltipraz-treated BDL group, suggesting that the secondary phase of liver injury induced by oltipraz might be due to excessive Mmp and Timp secretions, which induce remodeling of the extracellular matrix. Conclusions Oltipraz treatment exacerbates the severity of liver injury following BDL and should be avoided as therapy for extrahepatic cholestatic disorders due to bile duct obstruction. © 2013 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.
ISSN: 01688278
Appears in Collections:Scopus 2011-2015

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