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Differential effects of norUDCA and UDCA in obstructive cholestasis in mice

BACKGROUND & AIMS: The quest for effective drugs to treat cholangiopathies led to the development of norUDCA previously shown to have potent choleretic effects and to heal cholangiopathy in Abcb4 knockout (Abcb4(−/−)) mice. Its mother compound UDCA had detrimental effects in common bile duct lig...

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Autores principales: Fickert, Peter, Pollheimer, Marion J., Silbert, Dagmar, Moustafa, Tarek, Halilbasic, Emina, Krones, Elisabeth, Durchschein, Franziska, Thüringer, Andrea, Zollner, Gernot, Denk, Helmut, Trauner, Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3650580/
https://www.ncbi.nlm.nih.gov/pubmed/23369794
http://dx.doi.org/10.1016/j.jhep.2013.01.026
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author Fickert, Peter
Pollheimer, Marion J.
Silbert, Dagmar
Moustafa, Tarek
Halilbasic, Emina
Krones, Elisabeth
Durchschein, Franziska
Thüringer, Andrea
Zollner, Gernot
Denk, Helmut
Trauner, Michael
author_facet Fickert, Peter
Pollheimer, Marion J.
Silbert, Dagmar
Moustafa, Tarek
Halilbasic, Emina
Krones, Elisabeth
Durchschein, Franziska
Thüringer, Andrea
Zollner, Gernot
Denk, Helmut
Trauner, Michael
author_sort Fickert, Peter
collection PubMed
description BACKGROUND & AIMS: The quest for effective drugs to treat cholangiopathies led to the development of norUDCA previously shown to have potent choleretic effects and to heal cholangiopathy in Abcb4 knockout (Abcb4(−/−)) mice. Its mother compound UDCA had detrimental effects in common bile duct ligated (CBDL) mice, presumably related to its choleretic effects. norUDCA choleretic effects may therefore raise safety concerns when used in cholangiopathies with biliary obstruction. We therefore aimed at comparing the effects of UDCA and norUDCA in clear-cut obstructive cholestasis. METHODS: 0.5% UDCA- or norUDCA-fed wild type and Abcb4(−/−) mice were subjected to CBDL or selective bile duct ligation (SBDL) and compared to controls with regard to liver injury. Bile flow, bile composition, and biliary manometry were compared in UDCA-fed, norUDCA-fed and control mice. Toxicity of UDCA and norUDCA was compared in vitro. RESULTS: Compared to UDCA, liver injury in CBDL mice was significantly lower in almost all norUDCA groups. In SBDL mice, only UDCA induced bile infarcts in the ligated lobes, whereas norUDCA even ameliorated liver injury. In vitro, UDCA induced cellular ATP depletion and was significantly more toxic than norUDCA in HepG2 cells, mouse bile duct epithelial cells, and primary human hepatocytes. CONCLUSIONS: Compared to norUDCA, UDCA is significantly more toxic in CBDL mice. norUDCA, in contrast to UDCA, significantly ameliorates liver injury in SBDL mice. Our findings uncover profound differences in metabolism and therapeutic mechanisms of both bile acids with important clinical consequences.
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spelling pubmed-36505802013-06-01 Differential effects of norUDCA and UDCA in obstructive cholestasis in mice Fickert, Peter Pollheimer, Marion J. Silbert, Dagmar Moustafa, Tarek Halilbasic, Emina Krones, Elisabeth Durchschein, Franziska Thüringer, Andrea Zollner, Gernot Denk, Helmut Trauner, Michael J Hepatol Research Article BACKGROUND & AIMS: The quest for effective drugs to treat cholangiopathies led to the development of norUDCA previously shown to have potent choleretic effects and to heal cholangiopathy in Abcb4 knockout (Abcb4(−/−)) mice. Its mother compound UDCA had detrimental effects in common bile duct ligated (CBDL) mice, presumably related to its choleretic effects. norUDCA choleretic effects may therefore raise safety concerns when used in cholangiopathies with biliary obstruction. We therefore aimed at comparing the effects of UDCA and norUDCA in clear-cut obstructive cholestasis. METHODS: 0.5% UDCA- or norUDCA-fed wild type and Abcb4(−/−) mice were subjected to CBDL or selective bile duct ligation (SBDL) and compared to controls with regard to liver injury. Bile flow, bile composition, and biliary manometry were compared in UDCA-fed, norUDCA-fed and control mice. Toxicity of UDCA and norUDCA was compared in vitro. RESULTS: Compared to UDCA, liver injury in CBDL mice was significantly lower in almost all norUDCA groups. In SBDL mice, only UDCA induced bile infarcts in the ligated lobes, whereas norUDCA even ameliorated liver injury. In vitro, UDCA induced cellular ATP depletion and was significantly more toxic than norUDCA in HepG2 cells, mouse bile duct epithelial cells, and primary human hepatocytes. CONCLUSIONS: Compared to norUDCA, UDCA is significantly more toxic in CBDL mice. norUDCA, in contrast to UDCA, significantly ameliorates liver injury in SBDL mice. Our findings uncover profound differences in metabolism and therapeutic mechanisms of both bile acids with important clinical consequences. Elsevier 2013-06 /pmc/articles/PMC3650580/ /pubmed/23369794 http://dx.doi.org/10.1016/j.jhep.2013.01.026 Text en © 2013 Elsevier B.V. This document may be redistributed and reused, subject to certain conditions (http://www.elsevier.com/wps/find/authorsview.authors/supplementalterms1.0) .
spellingShingle Research Article
Fickert, Peter
Pollheimer, Marion J.
Silbert, Dagmar
Moustafa, Tarek
Halilbasic, Emina
Krones, Elisabeth
Durchschein, Franziska
Thüringer, Andrea
Zollner, Gernot
Denk, Helmut
Trauner, Michael
Differential effects of norUDCA and UDCA in obstructive cholestasis in mice
title Differential effects of norUDCA and UDCA in obstructive cholestasis in mice
title_full Differential effects of norUDCA and UDCA in obstructive cholestasis in mice
title_fullStr Differential effects of norUDCA and UDCA in obstructive cholestasis in mice
title_full_unstemmed Differential effects of norUDCA and UDCA in obstructive cholestasis in mice
title_short Differential effects of norUDCA and UDCA in obstructive cholestasis in mice
title_sort differential effects of norudca and udca in obstructive cholestasis in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3650580/
https://www.ncbi.nlm.nih.gov/pubmed/23369794
http://dx.doi.org/10.1016/j.jhep.2013.01.026
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