基于FDA不良事件报告系统数据库的来氟米特致肝损伤病例分析

doi:10.19803/j.1672-8629.2022.04.18

中国药物警戒 ›› 2022, Vol. 19 ›› Issue (4): 426-431.
DOI: 10.19803/j.1672-8629.2022.04.18

基于FDA不良事件报告系统数据库的来氟米特致肝损伤病例分析

崔向丽¹, 张志琪¹, 孙丽莹², 郭明星¹, 曾志贵², 徐菀佚¹

¹首都医科大学附属北京友谊医院药学部,北京 100050;
²首都医科大学附属北京友谊医院普外科肝移植中心,北京 100050

收稿日期:2020-06-15 出版日期:2022-04-15 发布日期:2022-04-15
作者简介:崔向丽,博士,主任药师,临床药学与药事管理。E-mail:cui10@163.com
基金资助:
国家卫健委卫生技术评估重点实验室2019 年度开放基金（FHTA2019-02）; 北京市医院管理中心2020年培育项目（PG2020002）

Leflunomide-induced hepatotoxicity: data analysis based on the FDA adverse event reporting system

CUI Xiangli¹, ZHANG Zhiqi¹, SUN Liying², GUO Mingxing¹, ZENG Zhigui², XU Wanyi¹

¹Department of Pharmacy, Beijing Friendship Hospital, Capital Medical University, Beijing 100050, China;
²Beijing Friendship Hospital, Capital Medical University General Surgery Department, Liver Transplantation Center, Beijing 100050, China

Received:2020-06-15 Online:2022-04-15 Published:2022-04-15

摘要/Abstract

摘要： 目的利用美国食品药品监督管理局不良事件报告系统（FDA adverse event reporting system, FAERS）数据库挖掘来氟米特肝损伤的药品不良反应特点,提示临床用药时应密切监测肝功能,警示此药具肝损伤特点。方法比较各国说明书和指南对肝损伤患者使用来氟米特的推荐意见;利用报告比值比法（report ratio, ROR）和比例报告比值法（proportion report ratio, PRR）对FAERS 数据库1999年1月1日至 2019 年12月31日间来氟米特不良事件报告进行信号挖掘,对其患者人群特点、原发病、合并用药、临床结局等信息进行分析。结果中国来氟米特说明书【禁忌症】中写明了严重肝脏损害禁用,相对其他国家的说明书或指南推荐使用过于宽泛。美国说明书黑框警告有严重肝损伤和致命性肝衰竭的报道,避免用于之前有肝病史或ALT>2倍正常值的患者。FAERS数据库中共检索到来氟米特不良事件28 186例,其中肝损伤不良反应人数4 319例,占17.9%。来氟米特与其他药物肝损伤的ROR和PRR分别是51.6和43.9。肝损伤患者中女性人数约为男性的3.5倍,年龄46~60岁占比最高,达35.1%。治疗原发病以类风湿性关节炎为主,占77.5%。合并用药方面,单用来氟米特患者2 288例,占52.98%,其次是合并使用1~5种药物,占29.22%;合并使用阿达木单抗、糖皮质激素、非甾体抗炎药、甲氨蝶呤的患者例数最多。死亡风险主要与年龄和性别相关,与合并用药种类无显著相关性。男性、高龄,死亡风险增加。结论我国临床使用来氟米特应警惕其引起肝损伤风险,应间隔2~4周监测患者肝功能,尤其与其他有肝损伤风险药物合用时更应该加强监测,有肝病史的患者尽量避免使用。

关键词: 来氟米特, 肝损伤, 美国食品药品监督管理局不良事件报告系统, 药品不良反应

Abstract: Objective To explore the characteristics of adverse drug reactions induced by leflunomide, such as hepatotoxicity, by using the FDA adverse event reporting system (FAERS) data in the United States, and to recommend that liver function should be closely monitored during clinical medication to prevent the hepatotoxicity of leflunomide. Methods The recommendations in the instructions and guidelines for the use of leflunomide among patients with liver damage in different countries were compared. The adverse event reports in FAERS data from January 1, 1999 to December 31, 2019 in the United States were mined by using the report ratio (ROR) method and the proportion report ratio (PRR) method. The signals of liver injury caused by leflunomide were mined, and the demographic characteristics, primary diseases, concomitant medications, clinical outcomes and other information were analyzed. Results Contraindications of leflunomide in Chinese instructions included severe liver damage, which was too broad compared with instructions or guidelines recommended by other countries. The US instructions deliberately added a black box to warn reports of severe liver damage and fatal liver failure to prevent this drug from being used by patients with a previous liver disease history or ALT>2 times the normal value. A total number of 28 186 adverse events of flunomide were retrieved, 4 319 (17.9%) of which were hepatotoxic adverse events. The ROR and PRR of hepatotoxicity of leflunomide and other drugs were 51.6 and 43.9 respectively. There were 3.5 times as many female patients with liver damage as male ones. The percentage of patients aged 46 to 60 was the highest (35.1%). Rheumatoid arthritis was the dominating primary disease, accounting for 77.5%. In terms of combined medication, 2 288 patients were treated with flunomide alone, accounting for 52.98%, while those treated with one to five types of drugs made up 29.22%. The combined use of adalimumab, glucocorticoid, non-steroidal anti-inflammatory drugs and methotrexate was the most common. The risk of death was mainly related to age and gender, and had no obvious correlations with the types of combined drugs, but tended to increase in male and elder patients. Conclusion Clinicians should be alert to the hepatotoxicity of leflunomide in China, and the liver function of patients should be monitored at an intervals of 2~4 weeks. Patients with a history of liver desease should avoid using this drug.

Key words: leflunomide, liver injury, FDA adverse event reporting system (FAERS), adverse drug reaction (ADR)

中图分类号:

R994.11

崔向丽, 张志琪, 孙丽莹, 郭明星, 曾志贵, 徐菀佚. 基于FDA不良事件报告系统数据库的来氟米特致肝损伤病例分析[J]. 中国药物警戒, 2022, 19(4): 426-431.

CUI Xiangli, ZHANG Zhiqi, SUN Liying, GUO Mingxing, ZENG Zhigui, XU Wanyi. Leflunomide-induced hepatotoxicity: data analysis based on the FDA adverse event reporting system[J]. Chinese Journal of Pharmacovigilance, 2022, 19(4): 426-431.

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基于FDA不良事件报告系统数据库的来氟米特致肝损伤病例分析

Leflunomide-induced hepatotoxicity: data analysis based on the FDA adverse event reporting system

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