Abstract

In bipolar disorder (BPD), long-term psychotropic drug treatment is often necessary to prevent relapse or recurrence. Nevertheless, adverse drug effects including disturbances in hepatic metabolism are observed and still poorly understood. Here, the association between hepatic gene expression and histopathological changes of the liver was investigated. By the use of microarrays (Affymetrix U133 plus2.0), a genome-wide expression study was performed on BPD patients with psychotropic drug treatment (n = 29) compared to unaffected controls (n = 20) and validated by quantitative real-time PCR. WebGestalt was used to identify over-represented functional pathways of the Reactome database. Association analyses between histopathological changes and differentially expressed genes comprised in the over-represented functional pathways were performed using regression analyses, from which feature-expression heatmaps were drawn. The majority of identified genes were underexpressed and involved in energy supply, metabolism of lipids and proteins, and the innate immune system. Positive associations were found for genes involved in all pathways and degenerative changes. The strongest negative association was observed between genes involved in energy supply and hepatic activity, as well as inflammation. In summary, we found a possible association between gene expression involved in various biological pathways and histopathological changes of the liver in BPD. Further, we found support for the probable primary toxic effect of psychotropic drugs on hepatic injury in BPD. Even if the safety of psychotropic drugs improves, adverse effects especially on hepatic function should not be underestimated.

Highlights

  • Bipolar disorder (BPD) is a severe mental illness characterized by recurrent and chronic fluctuations of manic and depressive episodes

  • Subject characteristics Liver tissue of deceased subjects with the clinical diagnosis of BPD and controls with no known history of psychiatric disorder was included in the study

  • In this study, a gene expression approach was used to investigate effects of psychotropic drugs on liver tissue in BPD subjects compared to controls

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Summary

Introduction

Bipolar disorder (BPD) is a severe mental illness characterized by recurrent and chronic fluctuations of manic and depressive episodes. To prevent relapse or recurrence in patients suffering from BPD, long-term drug treatment is often necessary[2,3]. Psychotropic drugs encompass antipsychotics, antidepressants and mood stabilizers including anticonvulsant drugs and lithium. The treatment aims to improve or resolve mood symptoms and prevent future relapses, adverse effects during the long-term drug treatment in BPD have been observed and reviewed[4,5]. Like renal, thyroid and parathyroid malfunction[6], weight gain[7], and hepatoxicity[8] were described. An induction of hepatoxicity by elevated liver enzymes due to psychotropic drug treatment was reported for antidepressants, antipsychotics, mood stabilizers, and anxiolytic agents[9]

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