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女性性别作为药物性肝损伤的一个易感性因素。

Female gender as a susceptibility factor for drug-induced liver injury.

作者信息

Amacher David E

机构信息

Toxadvisor Toxicology Consulting, USA.

出版信息

Hum Exp Toxicol. 2014 Sep;33(9):928-39. doi: 10.1177/0960327113512860. Epub 2013 Dec 3.

Abstract

Adverse drug reactions (ADRs) can involve all tissues and organs, but liver injuries are considered among the most serious. A number of prospective, multicenter studies have confirmed a higher risk of ADRs in general among female subjects compared to a male cohort. Although drug-induced liver injury (DILI) is infrequently encountered, the preponderance of evidence suggests that women appear to be more susceptible than men to fulminate hepatic/acute liver failure especially in response to some anti-infective drugs and to autoimmune-like hepatitis following exposure to certain other therapeutic drugs. A number of hypotheses have been proposed to explain this sex difference in susceptibility to DILI. Collectively, these hypotheses suggest three basic sex-dependent mechanisms that include differences in various aspects of drug pharmacokinetics (PK) or pharmacodynamics following the administration of certain drugs; specific hormonal effects or interactions with immunomodulating agents or signaling molecules; and differences in the adverse response of the immune system to some drugs, reactive drug metabolites, or drug-protein adducts. At the preclinical drug safety stage, there is a need for more research on hormonal effects on drug PK and for additional research on gender differences in aberrant immune responses that may lead to idiosyncratic DILI in some female patients. Because the detection of rare but serious hepatic ADRs requires the exposure of very large patient populations, pharmacovigilance networks will continue to play a key role in the postmarketing surveillance for their detection and reporting.

摘要

药物不良反应(ADR)可累及所有组织和器官,但肝损伤被认为是最严重的不良反应之一。多项前瞻性多中心研究证实,与男性队列相比,女性受试者总体上发生药物不良反应的风险更高。尽管药物性肝损伤(DILI)并不常见,但大量证据表明,女性似乎比男性更容易发生暴发性肝衰竭/急性肝衰竭,尤其是在使用某些抗感染药物以及接触某些其他治疗药物后发生自身免疫样肝炎时。人们提出了许多假说来解释这种对DILI易感性的性别差异。总体而言,这些假说提出了三种基本的性别依赖性机制,包括在使用某些药物后药物药代动力学(PK)或药效学各方面的差异;特定的激素效应或与免疫调节因子或信号分子的相互作用;以及免疫系统对某些药物、反应性药物代谢产物或药物-蛋白质加合物不良反应的差异。在临床前药物安全阶段,需要更多关于激素对药物PK影响的研究,以及关于异常免疫反应性别差异的更多研究,这些差异可能导致一些女性患者发生特异质性DILI。由于罕见但严重的肝脏ADR的检测需要大量患者群体的暴露,药物警戒网络将继续在上市后监测中发挥关键作用,以检测和报告这些不良反应。

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