使用美国食品药品监督管理局不良事件报告系统(FAERS)对FLT3抑制剂安全性进行的不均衡性分析。
A disproportionality analysis for assessing the safety of FLT3 inhibitors using the FDA Adverse Event Reporting System (FAERS).
作者信息
Zhou Jie, Zhang Jinping, Wang Qiaoyun, Peng Miaoxin, Qian Yun, Wu Fang, Rao Qi, DanZhen Laji, Yang Yonggong, Wang Siliang, Liu Mengying
机构信息
Department of Pharmacy, Nanjing Drum Tower Hospital, School of Basic Medicine and Clinical Pharmacy, China Pharmaceutical University, Nanjing, China.
Department of Pharmacy, Nanjing Drum Tower Hospital, Affiliated Hospital of Medical School, Nanjing University, Nanjing, China.
出版信息
Ther Adv Drug Saf. 2024 Oct 4;15:20420986241284105. doi: 10.1177/20420986241284105. eCollection 2024.
OBJECTIVES
This pharmacovigilance analysis was conducted to assess the safety signals of FMS-related tyrosine kinase 3 (FLT3) inhibitors in a real-world setting using the United States Food and Drug Administration Adverse Event Reporting System (FAERS).
DESIGN
We analyzed adverse event (AE) reports related to FLT3 inhibitors submitted to the FAERS database from the first quarter of 2015 to the fourth quarter of 2022. Disproportionality analysis was used to identify AEs of FLT3 inhibitors in the FAERS database.
RESULTS
A total of 55,393 AE reports were identified, of which 5938, 44,013, and 5442 were attributed to midostaurin, sorafenib, and gilteritinib, respectively, as primary suspects. Compared to the full database, significant safety signals at the system organ class level were observed for midostaurin (blood and lymphatic system disorders and hepatobiliary disorders), sorafenib (skin and subcutaneous tissue disorders and hepatobiliary disorders), and gilteritinib (investigations, blood and lymphatic system disorders, infections and infestations, and hepatobiliary disorders). All the drugs studied were associated with hepatobiliary disorders. The most prominent AEs associated with midostaurin, sorafenib, and gilteritinib were cytopenia, palmar-plantar erythrodysesthesia syndrome, and increased blast cell count, respectively. Compared with chemotherapy, midostaurin and gilteritinib showed a higher risk of electrocardiogram QT prolongation, gastrointestinal hemorrhage, cerebral hemorrhage, and increased white blood cell count. Gilteritinib had the highest overall death percentage (30.28%), whereas sorafenib had the lowest (23.06%).
CONCLUSION
Mining AE signals using the FAERS database provides a method for analyzing the safety of FLT3 inhibitors in post-marketing. We found several significant AE signals that corresponded to previous studies; however, some AE signals were not mentioned in the drug instructions. Our study could provide a direction for follow-up real-world studies to verify the results further.
目的
本药物警戒分析旨在使用美国食品药品监督管理局不良事件报告系统(FAERS)在真实世界环境中评估FMS相关酪氨酸激酶3(FLT3)抑制剂的安全信号。
设计
我们分析了2015年第一季度至2022年第四季度提交至FAERS数据库的与FLT3抑制剂相关的不良事件(AE)报告。采用不成比例分析来识别FAERS数据库中FLT3抑制剂的不良事件。
结果
共识别出55393份AE报告,其中分别有5938份、44013份和5442份报告将米哚妥林、索拉非尼和吉列替尼列为主要可疑药物。与完整数据库相比,在系统器官分类水平上观察到米哚妥林(血液和淋巴系统疾病以及肝胆疾病)、索拉非尼(皮肤和皮下组织疾病以及肝胆疾病)和吉列替尼(检查、血液和淋巴系统疾病、感染和寄生虫感染以及肝胆疾病)存在显著的安全信号。所有研究药物均与肝胆疾病相关。与米哚妥林、索拉非尼和吉列替尼相关的最突出不良事件分别是血细胞减少、手足红斑感觉异常综合征和原始细胞计数增加。与化疗相比,米哚妥林和吉列替尼出现心电图QT间期延长、胃肠道出血、脑出血和白细胞计数增加的风险更高。吉列替尼的总体死亡百分比最高(30.28%),而索拉非尼最低(23.06%)。
结论
使用FAERS数据库挖掘AE信号为分析FLT3抑制剂上市后的安全性提供了一种方法。我们发现了一些与先前研究相符的显著AE信号;然而,一些AE信号在药品说明书中未被提及。我们的研究可为后续真实世界研究进一步验证结果提供方向。
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