Genetic susceptibility to hepatoxicity due to bosentan treatment in pulmonary hypertension

Hans-Jürgen Seyfarth; Nadine Favreau; Carsten Tennert; Claudia Ruffert; Michael Halank; Hubert Wirtz; Joachim Mössner; Jonas Rosendahl; Peter Kovacs; Henning Wittenburg

Annals of Hepatology (Nov 2014)

Genetic susceptibility to hepatoxicity due to bosentan treatment in pulmonary hypertension

Hans-Jürgen Seyfarth,
Nadine Favreau,
Carsten Tennert,
Claudia Ruffert,
Michael Halank,
Hubert Wirtz,
Joachim Mössner,
Jonas Rosendahl,
Peter Kovacs,
Henning Wittenburg

Affiliations

Hans-Jürgen Seyfarth: Division of Respiratory Medicine, University Hospital of Leipzig, Germany; Correspondence and reprint request:
Nadine Favreau: Division of Gastroenterology and Rheumatology, University Hospital of Leipzig, Germany
Carsten Tennert: Institute of Laboratory Medicine, Clinical Chemistry and Molecular Diagnostics, Department of Internal Medicine, Neurology and Dermatology, University Hospital of Leipzig, Germany
Claudia Ruffert: Division of Gastroenterology and Rheumatology, University Hospital of Leipzig, Germany
Michael Halank: Internal Medicine I Carl Gustav Carus University Dresden, Germany
Hubert Wirtz: Division of Respiratory Medicine, University Hospital of Leipzig, Germany
Joachim Mössner: Division of Gastroenterology and Rheumatology, University Hospital of Leipzig, Germany
Jonas Rosendahl: Division of Gastroenterology and Rheumatology, University Hospital of Leipzig, Germany
Peter Kovacs: Integrated Research and Treatment Center Adiposity Diseases, University of Leipzig, Germany
Henning Wittenburg: Division of Gastroenterology and Rheumatology, University Hospital of Leipzig, Germany; HELIOS Hospital Schleswig, Germany

Journal volume & issue: Vol. 13, no. 6
pp. 803 – 809

Abstract

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Background. Hepatotoxicity is a major side effect of treatment with bosentan in patients with pulmonary hypertension (PH). Bosentan is metabolized by the cytochrome CYP2C9 and inhibits the bile salt export pump, which is encoded by ABCB11. This suggests that genetic variants of CYP2C9 and/or ABCB11 may predispose patients to bosentan-induced liver injury.Material and methods. PH patients with (n = 23) or Without (n = 25) an increase of alanine-aminotransferase (ALT) or aspartate-aminotransferase (AST) during bosentan therapy were included in our analysis. Functionally relevant alleles of CYP2C9 and 16 representative variants of ABCB11 were genotyped. Data were analyzed using logistic regression.Results. Variants of ABCB11 were not associated with bosentan-induced liver injury. In contrast, variant alleles of CYP2C9 were more common in patients with elevated transaminases (allele frequency 52%) compared to controls (allele frequency 24%, P = 0.04, odds ratio 3.5, 95% confidence interval 1.01-11.8).Conclusion. Our data indicate hepatotoxicity of bosentan from decreased hepatic metabolism due to common variants of CYP2C9.

Published in Annals of Hepatology

ISSN: 1665-2681 (Print); 2659-5982 (Online)
Publisher: Elsevier
Country of publisher: Spain
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine
Website: https://www.journals.elsevier.com/annals-of-hepatology

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