Enoxaparin-Induced Liver Injury: Case Report and Review of the Literature and FDA Adverse Event Reporting System (FAERS).

Katherine J Hahn, Shannon J Morales, James H Lewis
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Abstract

Anticoagulants are a well known cause of drug-induced liver injury (DILI). We recently encountered a 45-year-old male who developed DILI during treatment with enoxaparin, a low-molecular-weight heparin (LMWH), for dural venous thrombosis. The man received enoxaparin 80 mg subcutaneously, twice daily. After 4 days, the patient was asymptomatic but he developed liver aminotransferase elevations: AST 340 U/L and ALT 579 U/L. Investigation revealed an R ratio of 19.9 by day 5 and a Roussel Uclaf Causality Assessment Method score of 10, giving a high probable likelihood that enoxaparin was the cause of hepatic injury. Enoxaparin was discontinued on day 7, and 1 week later AST and ALT had decreased to 61 and 273 U/L, respectively. This case prompted a literature search and a review of the FDA Adverse Event Reporting System (FAERS) database for the range of hepatic adverse events (HAEs) associated with this class. A MEDLINE/PubMed search was conducted using DILI terms and cross-referenced with the anticoagulant classes. A Freedom of Information Act (FOIA) request was also made to identify adverse events (AEs) associated with enoxaparin in FAERS. Case type, severity of outcome, and demographic information were analyzed. Five publications have reported DILI with enoxaparin. Trial data found elevations in ALT >3 times the upper limit of normal (ULN) for unfractionated heparins (UFH) and LMWH in 8 and 4-13 % of subjects, respectively. However, liver injury in all cases was mild, self-limited, and asymptomatic. Our FOIA request yielded 8336 adverse events related to enoxaparin over a 14-year period (Jan 2000-Sept 2014). Specific HAEs were found in 4 % of reports, but all were described with other serious adverse events. The reported outcomes of hospitalization (75 %), death (17 %), and life-threatening medical events (5 %) were likely due to other related serious adverse events such as hemorrhage (28 %) and thrombocytopenia (11 %). We conclude that LMWH-related liver injury is uncommon and reversible. The mechanism of liver injury is not known, although an idiosyncratic effect is postulated. Although the FAERS database lists hepatic injury in 4 % of all enoxaparin-related AEs, it appears that serious outcomes are related to non-hepatic events.

依诺肝素诱发的肝损伤:病例报告、文献综述和 FDA 不良事件报告系统 (FAERS)。
众所周知,抗凝剂是药物性肝损伤(DILI)的诱因之一。我们最近遇到一名 45 岁的男性,他在使用低分子量肝素(LMWH)依诺肝素治疗硬脑膜静脉血栓期间出现了 DILI。该男子皮下注射依诺肝素 80 毫克,每天两次。4 天后,患者无任何症状,但出现肝脏转氨酶升高:AST 340 U/L,ALT 579 U/L。调查显示,到第 5 天,R 比值为 19.9,Roussel Uclaf 因果关系评估法评分为 10 分,极有可能是依诺肝素导致了肝损伤。第 7 天停用了依诺肝素,1 周后,AST 和 ALT 分别降至 61 和 273 U/L。该病例引发了文献检索和对 FDA 不良事件报告系统 (FAERS) 数据库的审查,以了解与该类药物相关的肝脏不良事件 (HAE) 的范围。使用 DILI 术语进行了 MEDLINE/PubMed 搜索,并与抗凝剂类别进行了交叉引用。此外,还申请了《信息自由法案》(FOIA),以确定 FAERS 中与依诺肝素相关的不良事件 (AE)。对病例类型、结果严重程度和人口统计学信息进行了分析。有五篇文献报道了依诺肝素引起的 DILI。试验数据发现,分别有8%和4%-13%的受试者的ALT升高>正常值上限(ULN)的3倍,而非分数肝素(UFH)和LMWH的受试者的ALT升高>正常值上限(ULN)的3倍。然而,所有病例的肝损伤均为轻度、自限性和无症状。我们的 FOIA 申请获得了 8336 例与依诺肝素有关的不良事件,时间跨度长达 14 年(2000 年 1 月至 2014 年 9 月)。在4%的报告中发现了特定的HAE,但所有报告都描述了其他严重不良事件。所报告的住院(75%)、死亡(17%)和危及生命的医疗事件(5%)很可能是由出血(28%)和血小板减少(11%)等其他相关严重不良事件引起的。我们的结论是,与 LMWH 相关的肝损伤并不常见,而且是可逆的。肝损伤的机制尚不清楚,但推测可能是一种特异性效应。虽然 FAERS 数据库列出的肝损伤占所有依诺肝素相关 AE 的 4%,但似乎严重后果与非肝损伤事件有关。
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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