Identifying olanzapine induced liver injury in the setting of acute hepatitis C: A case report.

The Mental Health Clinician Pub Date : 2022-06-10 eCollection Date: 2022-06-01 DOI:10.9740/mhc.2022.06.210
Andrea Brelje, Bailey Fay, Scott Mariouw, Amy VandenBerg
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引用次数: 2

Abstract

Olanzapine is linked to asymptomatic, transient elevations of liver aminotransferases but is historically thought to rarely cause significant hepatotoxicity. Underlying liver disease is a risk factor for drug-induced liver injury and may complicate the differential diagnosis of acute transaminitis in patients taking medications associated with hepatotoxicity. Ms L presented with 2 months of new psychotic symptoms resulting in hospitalizations. Although psychosis previously improved with haloperidol, she reported symptoms concerning for akathisia. Restlessness improved and psychotic symptoms resolved after initiation of olanzapine. Concurrently, her alanine aminotransferase (ALT) was elevated, prompting further workup and new diagnosis of acute hepatitis C. Over the course of hospitalization, her ALT increased exponentially. Initially attributed solely to acute hepatitis C infection, ALT rapidly decreased after holding olanzapine, implying it was contributing to her liver injury. Subsequently, given her prior response, haloperidol was retrialed with close monitoring for adverse effects. Her subjective restlessness was treated with additional agents, and she was then transitioned to monthly haloperidol decanoate injections to further assist her adherence. Prior to discharge, she had resolution of psychosis and transaminitis. Olanzapine may contribute to hepatotoxicity with concurrent viral hepatitis, and clarity can be obtained by a trial of stopping the suspected medication. Furthermore, olanzapine, when combined with underlying liver disease, may have an additive effect on liver injury, resulting in accelerated elevations in liver aminotransferases.

识别急性丙型肝炎设置奥氮平诱导肝损伤:一个病例报告。
奥氮平与无症状的肝转氨酶短暂升高有关,但历史上认为很少引起显著的肝毒性。潜在的肝脏疾病是药物性肝损伤的危险因素,并且可能使服用与肝毒性相关药物的患者的急性转氨炎的鉴别诊断复杂化。L女士出现2个月的新精神病症状,导致住院治疗。虽然先前使用氟哌啶醇可以改善精神病,但她报告了静坐症的症状。开始使用奥氮平后,躁动改善,精神病症状消失。同时,她的丙氨酸转氨酶(ALT)升高,促使进一步的检查和急性丙型肝炎的新诊断。在住院期间,她的ALT呈指数增长。最初仅归因于急性丙型肝炎感染,服用奥氮平后ALT迅速下降,提示其导致肝损伤。随后,鉴于她先前的反应,在密切监测不良反应的情况下重新使用氟哌啶醇。她的主观躁动症用其他药物治疗,然后转为每月注射癸酸氟哌啶醇以进一步协助她的依从性。出院前,她的精神病和转氨炎已消退。奥氮平可能与并发病毒性肝炎的肝毒性有关,通过停止可疑药物的试验可以获得明确的结果。此外,当奥氮平与潜在的肝脏疾病联合使用时,可能会对肝损伤产生累加效应,导致肝转氨酶加速升高。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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