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Characterization of agomelatine-induced liver injury, incidence and risk factors: A pooled analysis of 7605 treated patients

Published online by Cambridge University Press:  23 March 2020

G. Perlemuter*
Affiliation:
Antoine-Béclère Hospital, Assistance publique–Hôpitaux de Paris, Hepato-gastroenterology, Clamart, France
P. Cacoub
Affiliation:
Groupe hospitalier Pitié-Salpétrière, Internal medicine and clinical immunology, Paris, France
D. Valla
Affiliation:
Hôpital Beaujon, Hepatology, Clichy, France
D. Guyader
Affiliation:
CHU de Rennes, Liver disease unit and National reference center for rare iron overload diseases of genetic origin, Rennes, France
B. Saba
Affiliation:
Institut de Recherches Internationales Servier, Neuropsychiatrie, Suresnes, France
C. Batailler
Affiliation:
Institut de Recherches Internationales Servier, Neuropsychiatrie, Suresnes, France
K. Moore
Affiliation:
Royal Free Campus, University College London, UCL Institute of Liver and Digestive Health, London, United Kingdom
*
*Corresponding author.

Abstract

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Introduction/objective

The hepatic safety of agomelatine was assessed in 49 phase II and III studies. The aim was to analyze the characteristics of patients who developed an increase in transaminases whilst taking agomelatine.

Method

A retrospective pooled analysis of changes in serum transaminase in 7605 patients treated with agomelatine (25 mg or 50 mg/day) from 49 completed studies was undertaken. A significant increase in serum transaminase was defined as > 3-fold the upper limit of normal (> 3 ULN). Final causality was determined in a case-by-case review by five academic experts.

Results

Transaminase increased to > 3 ULN in 1.3% and 2.5% of patients treated with 25 mg and 50 mg of agomelatine respectively, compared to 0.5% for placebo. The onset of increased transaminases occurred at < 12 weeks in 64% of patients. The median time to recovery (to ≤ 2ULN) was 14 days following treatment withdrawal. Liver function tests recovered in 36.1% patients despite the continuation of agomelatine, suggesting the presence of a liver adaptive mechanism. Patients with elevated transaminases at baseline, secondary to obesity and fatty liver disease (NAFLD), had an equally increased risk of developing further elevations of transaminases with agomelatine and placebo. This reflects the widespread fluctuations of serum transaminases in patients with NAFLD.

Conclusions

The overall incidence of abnormal transaminases was low and dose dependent. No specific population was identified regarding potential risk factors. Withdrawal of agomelatine led to rapid recovery, and some patients exhibited an adaptive phenomenon. The liver profile of agomelatine seems safe when serum transaminases are monitored.

Disclosure of interest

The authors have not supplied their declaration of competing interest.

Type
EW448
Copyright
Copyright © European Psychiatric Association 2014
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