Prescription patterns of comedications associated with drug-drug interactions risk in HCV-infected patients undergoing direct-acting antiviral treatment: an analysis of an administrative claims database in Japan.

IF 1.2 Q4 PHARMACOLOGY & PHARMACY

Journal of Pharmaceutical Health Care and Sciences Pub Date : 2025-04-18 DOI:10.1186/s40780-025-00442-5

Daisuke Nakamoto, Yi Piao, Hajime Mizutani, Ryozo Wakabayashi, Satoshi Otokita, Alice Stead, Candido Hernandez, Masahisa Jinushi

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Abstract

Introduction: While direct-acting antivirals (DAA) are effective treatment for hepatitis C virus (HCV) patients, concerns about drug-drug interactions (DDIs) remain a significant challenge. Although there are several studies investigating the risk of DDIs associated with DAA therapy, there is limited research evaluating DDIs of DAA therapy in real-world settings in Japan. We investigated prescription patterns of comedication associated with DDIs risk in HCV patients receiving DAA therapy using a large Japanese database.

Methods: This was a descriptive epidemiological study, using the Japanese administrative claims database provided by DeSC Healthcare, Inc. Patients who initiated sofosbuvir/velpatasvir (SOF/VEL) or glecaprevir/pibrentasvir (GLE/PIB) between April 2017 and August 2023 were identified from the data. The primary outcome was DDIs associated with comedications which were assessed based on both Japanese package inserts and the Liverpool HEP Drug Interaction Checker (Liverpool HEP checker).

Results: Patients included in this study were 7,338, with 467 prescribed SOF/VEL and 6,871 prescribed GLE/PIB. The mean age of the patients was 69.9 years (SD = 13.1), with 50% being male. The median number of comedications was higher in the SOF/VEL group (14.0; IQR = 14.0) than in the GLE/PIB group (9.0; IQR = 12.0) and based on package insert and Liverpool HEP checker, the DDI risk was present in 59.3% (277) of the SOF/VEL group and 51.5% (3,542) of the GLE/PIB group. DDI risk involving two or more medications in combination with a DAA was 14.1% (66) in the SOF/VEL group and 24.0% (1,648) in the GLE/PIB group. In terms of DDI severity, in the SOF/VEL group there were no patients identified under the level "Contraindication (Red)" category, indicating medications that do not co-administered, in contrast with the 1.7% (115) in the GLE/PIB group who were identified as "contraindication (red)".

Conclusion: A considerable proportion of patients were prescribed medications with DDI risk during DAA treatment. A small but notable proportion of patients were on "Contraindication (Red)" medications. Consideration of the potential DDI risks associated with comedications by healthcare professionals is advised, referring not only to package inserts but also tools such as Liverpool HEP checker to guide safe prescribing when initiating DAA therapy for HCV patients.

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在接受直接作用抗病毒治疗的hcv感染患者中，与药物相互作用风险相关的药物处方模式：对日本行政索赔数据库的分析

导论：虽然直接作用抗病毒药物（DAA）是丙型肝炎病毒（HCV）患者的有效治疗方法，但对药物-药物相互作用（ddi）的担忧仍然是一个重大挑战。虽然有几项研究调查了与DAA治疗相关的ddi风险，但在日本，评估DAA治疗的ddi的研究有限。我们使用日本大型数据库调查了接受DAA治疗的HCV患者与ddi风险相关的药物处方模式。方法：这是一项描述性流行病学研究，使用由DeSC Healthcare， Inc.提供的日本行政索赔数据库。从数据中确定了2017年4月至2023年8月期间使用索非布韦/维帕他韦（SOF/VEL）或glecaprevir/pibrentasvir （GLE/PIB）的患者。主要终点是与药物相关的ddi，根据日本药品说明书和利物浦HEP药物相互作用检查器（利物浦HEP检查器）进行评估。结果：本研究纳入患者7338例，其中467例使用SOF/VEL， 6871例使用GLE/PIB。患者平均年龄69.9岁（SD = 13.1），男性占50%。SOF/VEL组用药中位数较高(14.0；IQR = 14.0)高于GLE/PIB组(9.0；IQR = 12.0)，根据说明书和利物浦HEP检查，SOF/VEL组的DDI风险为59.3% (277)，GLE/PIB组的DDI风险为51.5%（3542）。两种或两种以上药物联合DAA的DDI风险在SOF/VEL组为14.1%(66)，在GLE/PIB组为24.0%（1648）。在DDI严重程度方面，SOF/VEL组中没有患者被确定为“禁忌症（红色）”类别，这表明药物不能共同给药，而GLE/PIB组中有1.7%（115）的患者被确定为“禁忌症（红色）”。结论：相当比例的患者在DAA治疗过程中使用了有DDI风险的药物。一小部分但值得注意的患者使用“禁忌症（红色）”药物。建议卫生保健专业人员考虑与药物相关的潜在DDI风险，不仅参考包装说明书，而且参考利物浦HEP检查器等工具，以指导HCV患者开始DAA治疗时的安全处方。

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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