成人囊性纤维化患者中 Elexacaftor、Tezacaftor 和 Ivacaftor 的治疗药物监测。

IF 3 3区 医学 Q2 HEALTH CARE SCIENCES & SERVICES
Susanne Naehrig, Christina Shad, Magdalena Breuling, Melanie Goetschke, Katharina Habler, Sarah Sieber, Johanna Kastenberger, Alexandra Katharina Kunzelmann, Olaf Sommerburg, Uwe Liebchen, Juergen Behr, Michael Vogeser, Michael Paal
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引用次数: 0

摘要

背景/目的:Elexacaftor、tezacaftor和ivacaftor(ETI)可显著改善囊性纤维化患者(pwCF)的肺功能。尽管在大多数病例中都取得了显著改善,但与治疗相关的受试者间变异和药物间相互作用使调节剂治疗复杂化的情况也有报道:本回顾性分析报告了 2021 年 8 月至 2023 年 12 月期间,通过常规治疗药物监测 (TDM) 获得的全量或减量治疗 pwCF 的 ETI 血清浓度数据。这些数据与制药公司产品特征概要中的最大药物浓度(Cmax)进行了比较:共分析了来自 155 名重症肌无力患者(女性占 41%,男性占 59%)的 786 份血液样本。检查结果分为四组:在给定最大剂量范围内的全剂量(占所有测量结果的 38.5%)、最大剂量范围外的全剂量(29%)、最大剂量范围内的减剂量(19.2%)和最大剂量范围外的减剂量(13.2%)。在接受全剂量治疗并在tmax内采血的pwCF中,发现分别有45.3%的依来卡夫托血清浓度、51.1%的伊伐卡夫托血清浓度和8.9%的特扎卡夫托血清浓度高于Cmax。在tmax范围内服用减量剂量的患者中,分别有24.5%、23.2%和2.5%的患者的血清中依来卡夫托、伊伐卡夫托和替扎卡夫托的浓度高于Cmax:许多接受 ETI 治疗的 pwCF 的 elexacaftor 和 ivacaftor 的 Cmax 值超过了推荐范围,甚至在减少剂量或达到 tmax 之前也是如此。这凸显了 TDM 计划的价值。有必要开展进一步的药代动力学研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Therapeutic Drug Monitoring of Elexacaftor, Tezacaftor, and Ivacaftor in Adult People with Cystic Fibrosis.

Background/objectives: Elexacaftor, tezacaftor, and ivacaftor (ETI) have significantly improved lung function in people with cystic fibrosis (pwCF). Despite exceptional improvements in most cases, treatment-related inter-subject variability and drug-drug interactions that complicate modulator therapy have been reported.

Methods: This retrospective analysis presents data on the serum concentration of ETI in our pwCF with full or reduced dosage from August 2021 to December 2023 via routine therapeutic drug monitoring (TDM). The data were compared with the maximum drug concentrations (Cmax) from the pharmaceutical company's summary of product characteristics.

Results: A total of 786 blood samples from 155 pwCF (41% female, 59% male) were analyzed. The examinations were divided into four groups: full dose within the given tmax (38.5% of all measurements), full dose outside the tmax (29%), reduced dose within the tmax (19.2%), and reduced dose outside the tmax (13.2%). In pwCF receiving the full dose and blood taken within the tmax, 45.3% of serum concentrations of elexacaftor, 51.1% of serum concentrations of ivacaftor, and 8.9% of serum concentrations of tezacaftor were found to be above the Cmax, respectively. For those on reduced doses within the tmax, 24.5% had a serum concentration of elexacaftor, 23.2% had a serum concentration of ivacaftor, and 2.5% had a serum concentration of tezacaftor above the Cmax, respectively.

Conclusions: Many pwCF under ETI therapy have Cmax values for elexacaftor and ivacaftor above the recommended range, even on reduced doses or before the tmax was reached. This highlights the value of a TDM program. Further pharmacokinetic studies are necessary.

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来源期刊
Journal of Personalized Medicine
Journal of Personalized Medicine Medicine-Medicine (miscellaneous)
CiteScore
4.10
自引率
0.00%
发文量
1878
审稿时长
11 weeks
期刊介绍: Journal of Personalized Medicine (JPM; ISSN 2075-4426) is an international, open access journal aimed at bringing all aspects of personalized medicine to one platform. JPM publishes cutting edge, innovative preclinical and translational scientific research and technologies related to personalized medicine (e.g., pharmacogenomics/proteomics, systems biology). JPM recognizes that personalized medicine—the assessment of genetic, environmental and host factors that cause variability of individuals—is a challenging, transdisciplinary topic that requires discussions from a range of experts. For a comprehensive perspective of personalized medicine, JPM aims to integrate expertise from the molecular and translational sciences, therapeutics and diagnostics, as well as discussions of regulatory, social, ethical and policy aspects. We provide a forum to bring together academic and clinical researchers, biotechnology, diagnostic and pharmaceutical companies, health professionals, regulatory and ethical experts, and government and regulatory authorities.
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