Altered intestinal bile salt biotransformation in a cystic fibrosis ( Cftr−/− ) mouse model with hepato-biliary pathology

Abstract Background Cftr −/− tm1Unc mice develop progressive hepato-biliary pathology. We hypothesize that this liver pathology is related to alterations in biliary bile hydrophobicity and bile salt metabolism in Cftr −/− tm1Unc mice. Methods We determined bile production, biliary and fecal bile sal...

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Veröffentlicht in:Journal of cystic fibrosis 2015-07, Vol.14 (4), p.440-446
Hauptverfasser: Bodewes, Frank A.J.A, van der Wulp, Mariëtte Y.M, Beharry, Satti, Doktorova, Marcela, Havinga, Rick, Boverhof, Renze, James Phillips, M, Durie, Peter R, Verkade, Henkjan J
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Sprache:eng
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Zusammenfassung:Abstract Background Cftr −/− tm1Unc mice develop progressive hepato-biliary pathology. We hypothesize that this liver pathology is related to alterations in biliary bile hydrophobicity and bile salt metabolism in Cftr −/− tm1Unc mice. Methods We determined bile production, biliary and fecal bile salt- and lipid compositions and fecal bacterial composition of C57BL/6 J Cftr −/− tm1Unc and control mice. Results We found no differences between the total biliary bile salt or lipid concentrations of Cftr−/− and controls. Compared to controls, Cftr−/− mice had a ~ 30% higher bile production and a low bile hydrophobicity, related to a ~ 7 fold higher concentration of the choleretic and hydrophilic bile salt ursocholate. These findings coexisted with a significantly smaller quantity of fecal Bacteroides bacteria. Conclusions Liver pathology in Cftr −/− tm1Unc is not related to increased bile hydrophobicity. Cftr−/− mice do however display a biliary phenotype characterized by increased bile production and decreased biliary hydrophobicity. Our findings suggest Cftr dependent, alterations in intestinal bacterial biotransformation of bile salts.
ISSN:1569-1993
1873-5010
DOI:10.1016/j.jcf.2014.12.010