Douros Antonios, Bronder Elisabeth, Andersohn Frank, Klimpel Andreas, Thomae Michael, Sarganas Giselle, Kreutz Reinhold, Garbe Edeltraut
Department of Clinical Pharmacology and Toxicology, Charité-Universitätsmedizin Berlin, Berlin, Germany.
Leibniz Institute for Prevention Research and Epidemiology - BIPS, Bremen, Germany.
Br J Clin Pharmacol. 2015 Jun;79(6):988-99. doi: 10.1111/bcp.12565.
Drug-induced liver injury (DILI) is often responsible for acute liver failure, drug withdrawal, boxed warnings or drug non-approval. Therefore, we conducted a case-control study to determine the hepatotoxic risk of a wide range of drugs.
The Berlin Case-Control Surveillance Study FAKOS included all 51 Berlin hospitals in a hospital network. Between 2002 and 2011, 198 patients with acute idiopathic hepatitis, 377 inpatient controls and 708 outpatient controls were ascertained. Case patients were thoroughly validated using anamnestic, clinical, laboratory and histological data. Drug exposure was obtained in a face-to-face interview. A possible drug aetiology was assessed in individual patients by applying the updated Council for International Organizations of Medical Sciences (CIOMS) scale. Drug risks were further quantified [odds ratios (OR) with 95% confidence intervals (CI)] in a case-control design with unconditional logistic regression analysis. Drug intake in the last 28 days before index date was considered for the analysis.
The study corroborated hepatotoxic risks for a number of drugs, including phenprocoumon (OR 3.3, 95% CI 1.5, 6.7), amiodarone (OR 5.5, 95% CI 1.3, 21.2), clozapine (OR 34.6, 95% CI 2.8, 824.9) and flupirtine (OR 40.2, 95% CI 5.5, 856.9). Increased risks were also suggested for less commonly reported substances such as angiotensin II receptor blockers, atypical antipsychotics and for biperiden, a drug never before reported to be hepatotoxic.
Our study identified a large number of drugs as possible causes of hepatotoxicity. The observed risk for seldom reported substances highlights the need for further post-authorization safety studies not exclusively focusing on drugs already labelled as potentially hepatotoxic.
药物性肝损伤(DILI)常导致急性肝衰竭、药物撤市、加框警告或药物未获批。因此,我们开展了一项病例对照研究,以确定多种药物的肝毒性风险。
柏林病例对照监测研究FAKOS纳入了医院网络中的所有51家柏林医院。在2002年至2011年期间,确定了198例急性特发性肝炎患者、377例住院对照和708例门诊对照。通过既往史、临床、实验室和组织学数据对病例患者进行全面验证。通过面对面访谈获取药物暴露情况。采用更新后的国际医学科学组织理事会(CIOMS)量表对个体患者评估可能的药物病因。在病例对照设计中,采用无条件逻辑回归分析进一步量化药物风险[比值比(OR)及95%置信区间(CI)]。分析时考虑索引日期前最后28天内的药物摄入情况。
该研究证实了多种药物的肝毒性风险,包括苯丙香豆素(OR 3.3,95% CI 1.5,6.7)、胺碘酮(OR 5.5,95% CI 1.3,21.2)、氯氮平(OR 34.6,95% CI 2.8,824.9)和氟吡汀(OR 40.2,95% CI 5.5,856.9)。对于血管紧张素II受体阻滞剂、非典型抗精神病药物等较少报告的物质以及从未报告有肝毒性的比哌立登,也提示存在风险增加。
我们的研究确定了大量药物可能是肝毒性的原因。观察到的较少报告物质的风险凸显了开展进一步的上市后安全性研究的必要性,这些研究不应仅关注已被标记为潜在肝毒性的药物。
