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酮康唑相关的肝损伤:已发表证据综述

Liver injury associated with ketoconazole: review of the published evidence.

作者信息

Greenblatt H Karl, Greenblatt David J

机构信息

Program in Pharmacology and Experimental Therapeutics, Tufts University School of Medicine and Tufts Medical Center, Boston, MA, USA.

出版信息

J Clin Pharmacol. 2014 Dec;54(12):1321-9. doi: 10.1002/jcph.400. Epub 2014 Oct 1.

Abstract

The azole antifungal agent ketoconazole has been available since 1981 for the treatment of fungal infections. In 2013, the American Food and Drug Administration and the European Medicines Agency issued warnings or prohibitions against the clinical use of oral ketoconazole due to the risk of liver injury which may lead to liver transplantation or death. From the available published evidence it is difficult to determine the actual incidence or prevalence of liver injury during clinical use of ketoconazole as an antifungal. Hepatic injury, when it occurs, is generally evident as asymptomatic and reversible abnormalities of liver function tests. However, serious liver injury has been reported. Alternatives to ketoconazole (such as itraconazole, fluconazole, voriconazole, and terbinafine) are available, but improved safety with respect to liver injury risk is not clearly established. We are not aware of published reports of significant ketoconazole-associated liver injury in volunteer study participants when ketoconazole has been used as a CYP3A inhibitor in the context of clinical research on drug metabolism. Possible alternatives to ketoconazole as prototype CYP3A inhibitors include ritonavir and potentially itraconazole, but not clarithromycin.

摘要

唑类抗真菌药酮康唑自1981年起就可用于治疗真菌感染。2013年,美国食品药品监督管理局和欧洲药品管理局因肝损伤风险(可能导致肝移植或死亡)发布了关于口服酮康唑临床使用的警告或禁令。从现有的已发表证据来看,很难确定酮康唑作为抗真菌药临床使用期间肝损伤的实际发病率或患病率。肝损伤发生时,通常表现为肝功能检查无症状且可逆的异常。然而,也有严重肝损伤的报道。有酮康唑的替代药物(如伊曲康唑、氟康唑、伏立康唑和特比萘芬),但肝损伤风险方面的安全性改善并未明确确立。在药物代谢的临床研究中,当酮康唑用作CYP3A抑制剂时,我们未发现有关志愿者研究参与者中酮康唑相关严重肝损伤的已发表报告。作为原型CYP3A抑制剂,酮康唑的可能替代药物包括利托那韦以及可能的伊曲康唑,但不包括克拉霉素。

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