军队卫生系统中厄洛替尼和吉非替尼药物相互作用的回顾性评价。

Federal practitioner : for the health care professionals of the VA, DoD, and PHS Pub Date : 2023-08-01 Epub Date: 2023-08-15 DOI:10.12788/fp.0401

Thu-Lan T Luong, Chelsea N Powers, Brian J Reinhardt, Michael J McAnulty, Peter J Weina, Karen J Shou, Caban B Ambar

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摘要

背景:厄洛替尼和吉非替尼是表皮生长因子受体酪氨酸激酶抑制剂，已被美国食品和药物管理局批准用于治疗非小细胞肺癌。药物-药物相互作用(ddi)与这些药物是模糊的，知之甚少。由于ddi会对临床结果产生影响，我们的目的是确定与厄洛替尼或吉非替尼相互作用的药物，并描述其临床表现。方法:对美国国防部癌症登记处(检索于2021年9月)、综合门诊/专业就诊记录和药房数据交易服务数据库(均检索于2022年5月)中患者的健康记录进行回顾性分析。提取患者的病史、诊断和人口统计数据，并分析这些药物单独使用与与其他处方药合用时不良反应的差异。提取患者的诊断和处方药使用情况，以比较完成治疗组和停止治疗组，确定通常与厄洛替尼或吉非替尼共同使用的药物，并评估ddi与抗抑郁药。结果:387例使用厄洛替尼的患者中，264例完成治疗;使用吉非替尼的33名患者中有28名完成了治疗。厄洛替尼单独与合用时停药的P值< 0.001，吉非替尼停药的P值为0.06。服用厄洛替尼或吉非替尼同时服用大量处方药的患者比服用较少药物的患者停药率更高。完成组患者处方药物1 ~ 75种，完成组患者处方药物3 ~ 103种。那些停止治疗的人比那些完成治疗的人有更多的诊断出的医学问题。结论:本综述不能得出与处方药同时使用会导致厄洛替尼或吉非替尼停药的结论。厄洛替尼或吉非替尼与抗抑郁药之间没有明显的ddi。

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Retrospective Evaluation of Drug-Drug Interactions With Erlotinib and Gefitinib Use in the Military Health System.

Background: Erlotinib and gefitinib are epidermal growth factor receptor-tyrosine kinase inhibitors approved for non-small cell lung cancer treatment by the US Food and Drug Administration. Drug-drug interactions (DDIs) with these agents are vague and poorly understood. Because DDIs can have an effect on clinical outcomes, we aimed to identify drugs that interact with erlotinib or gefitinib and describe their clinical manifestations.

Methods: A retrospective analysis was performed on the health records of patients in the US Department of Defense Cancer Registry (retrieved September 2021), Comprehensive Ambulatory/Professional Encounter Records, and Pharmacy Data Transaction Service database (both retrieved May 2022). Patients' medical history, diagnoses, and demographics were extracted and analyzed for differences in adverse effects when these agents were used alone vs concomitantly with other prescription drugs. Patients' diagnoses and prescription drug use were extracted to compare completed vs discontinued treatment groups, identify medications commonly co-administered with erlotinib or gefitinib, and evaluate DDIs with antidepressants.

Results: Of 387 patients using erlotinib, 264 completed treatments; 28 of 33 patients using gefitinib completed treatment. The P value for erlotinib discontinuation when used alone vs concomitantly was < .001, and the P value for gefitinib discontinuation was .06. Patients who took erlotinib or gefitinib concomitantly with a greater number of prescription drugs had a higher rate of treatment discontinuation than those who received fewer medications. Patients in the completed group received 1 to 75 prescription drugs, and those in the completed group were prescribed 3 to 103. Those who discontinued treatment had more diagnosed medical issues than those who completed treatment.

Conclusions: This review cannot conclude that concomitant use with prescription drug(s) resulted in erlotinib or gefitinib discontinuation. There were no significant DDIs determined between erlotinib or gefitinib and antidepressants.

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Federal practitioner : for the health care professionals of the VA, DoD, and PHS

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