卡马西平引起的肝毒性和谷胱甘肽在事件中的可能的病理作用。回顾性审查旧数据并呼吁进行新的调查。

Miklós Péter Kalapos
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引用次数: 56

摘要

抗癫痫药物卡马西平被广泛用于治疗不同类型的癫痫发作以及情感和行为障碍。本文介绍了卡马西平引起的肝损伤和死亡的流行病学研究,并描述了其毒性的可能机制。对临床数据的回顾性分析显示,儿童肝性死亡的可能性相对较高,特别是当他们同时接受多个aed药物治疗时,而可逆性肝损伤更可能发生在老年患者中。如本文所述,卡马西平肝毒性的发展是罕见的,以目前的知识水平是不可预测的,但它与谷胱甘肽代谢紊乱有关,尽管这方面的数据不完善。似乎有两种类型的卡马西平引起的特异性肝损伤,过敏和毒素诱导。这是可行的,两者都是由于有毒代谢物的积累,芳烃氧化物可能被认为是卡马西平代谢的有害衍生物。尽管缺乏明确的潜在临床和实验结果,在这些患者中,遗传的药物消除能力的弱点存在,这些条件可能会恶化谷胱甘肽平衡,可能会增加卡马西平治疗期间出现毒性事件的可能性。最后,对卡马西平的治疗提出了一些建议。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Carbamazepine-provoked hepatotoxicity and possible aetiopathological role of glutathione in the events. Retrospective review of old data and call for new investigation.

The antiepileptic drug (AED) carbamazepine is widely used in the treatment of different kinds of seizures as well as affective and behavioural disorders. This paper presents an epidemiological study of carbamazepine-induced hepatic injuries and death, and describes the possible mechanisms of its toxicity. A retrospective analysis of clinical data revealed that the likelihood of hepatic death was comparatively higher in children, particularly when they were receiving medication with multiple AEDs, whereas reversible hepatic injuries were more likely to be seen in elderly patients. As suggested in this paper, the development of carbamazepine hepatotoxicity is rare, and unpredictable with the present state of knowledge, but it is somehow related to disturbance of glutathione metabolism, although data in this regard are imperfect. There appear to be two types of carbamazepine-initiated idiosyncratic liver injury, hypersensitivity and toxin-induced. It is feasible that both are due to the accumulation of toxic metabolite(s), and arene oxides may probably be considered as damaging derivatives of carbamazepine metabolism. Despite the lack of clear-cut underlying clinical and experimental findings in those patients in whom an inherited weakness of drug eliminating capacity is present, those conditions that may deteriorate glutathione balance, may increase the possibility of the emergence of toxic events during carbamazepine therapy. Finally, some recommendations for carbamazepine therapy are presented.

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