Background: A multifunctional mediator, endothelin (ET)-1 is implicated in the pathophysiology of liver cirrhosis. Carbon tetrachloride (CCl4)-induced cirrhosis in rats resolves upon termination of CCl4 treatment. We determined the hepatic ET-1 system during such reversal and assessed whether ET-1 receptor antagonism enhances this process. Methods: Cirrhosis was induced in rats by CCl4 treatment for 8 weeks. Treatment with an ETA/ETB antagonist TAK-044 (10 mg/kg per day) was then started and determinations were made at 1, 2 and 4 weeks. Results: After termination of CCl4 treatment, accelerated normalization of liver architecture and portal hypertension occurred in TAK-044-treated rats compared with saline-treated rats. The increased hepatic hydroxyproline concentration and collagen I mRNA expression also declined to greater extents in the TAK-044-treated group. Higher collagenase activity in cirrhosis decreased in saline-treated rats, but did not reach basal values. In TAK-044-treated rats, collagenase activity tended to increase at weeks 2 and 4. Increased ET-1 concentration and ETA receptor density declined to normal values in both groups. In contrast, increased ETB receptor density did not change in saline-treated rats, but decreased to control values in TAK-044-treated rats. Conclulsions: Our results emphasize the role of ET-1 in chronic liver disease and strongly indicate the potential for ET-1 receptor antagonists in its treatment. (C) 2002 Blackwell Publishing Asia Pty Ltd.
机构:
Laboratory of Innovative treatment of Liver Diseases (EA 1833), Université René Descartes
Federation of Digestive Diseases, Amiens North Hospital, University of Picardy, place Victor PauchetLaboratory of Innovative treatment of Liver Diseases (EA 1833), Université René Descartes
Jean-Marc Regimbeau
David Fuks
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Federation of Digestive Diseases, Amiens North Hospital, University of Picardy, place Victor PauchetLaboratory of Innovative treatment of Liver Diseases (EA 1833), Université René Descartes
David Fuks
Niaz Kohneh-Shahri
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Laboratory of Innovative treatment of Liver Diseases (EA 1833), Université René DescartesLaboratory of Innovative treatment of Liver Diseases (EA 1833), Université René Descartes
Niaz Kohneh-Shahri
Benot Terris
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Department of Pathology, Hpital Cochin Port RoyalLaboratory of Innovative treatment of Liver Diseases (EA 1833), Université René Descartes
Benot Terris
Olivier Soubrane
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Laboratory of Innovative treatment of Liver Diseases (EA 1833), Université René DescartesLaboratory of Innovative treatment of Liver Diseases (EA 1833), Université René Descartes