Improving Understanding of Fexofenadine Pharmacokinetics to Assess Pgp Phenotypic Activity in Older Adult Patients Using Population Pharmacokinetic Modeling.

IF 4.6 2区医学 Q1 PHARMACOLOGY & PHARMACY Clinical Pharmacokinetics Pub Date : 2025-02-01 Epub Date: 2025-01-11 DOI:10.1007/s40262-024-01470-4

Frédéric Gaspar, Celestin Jacost-Descombes, Pauline Gosselin, Jean-Luc Reny, Monia Guidi, Chantal Csajka, Caroline Samer, Youssef Daali, Jean Terrier

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Abstract

Background and objective: Fexofenadine is commonly used as a probe substrate to assess P-glycoprotein (Pgp) activity. While its use in healthy volunteers is well documented, data in older adult and polymorbid patients are lacking. Age- and disease-related physiological changes are expected to affect the pharmacokinetics of fexofenadine. This study aims to investigate the pharmacokinetics of fexofenadine in hospitalized older adult patients as a potential marker of Pgp activity, using data from the OptimAT study (ClinicalTrials.gov identifier: NCT03477331).

Methods: Population pharmacokinetic (popPK) modeling was conducted using data from 449 hospitalized patients with a median age of 71 years (range: 25-97) and 10 healthy volunteers (median age: 23 years, range: 20-36). Fexofenadine plasma concentrations were analyzed using a refined two-compartment model with sequential zero/first-order absorption, while investigating the impact of covariates such as age, renal function, and Pgp inhibitors on fexofenadine pharmacokinetics.

Results: Age, renal insufficiency, and Pgp inhibitors significantly influenced fexofenadine exposure. Renal function was a key factor, with AUC_0-6 increasing by 79% in mild-to-moderate and by 154% in moderate-to-severe renal impairment compared with normal renal function. Co-administration of Pgp inhibitors led to a 35% increase in AUC_0-6. Across chronic kidney disease (CKD) stages, age, and Pgp inhibitor status, fexofenadine AUC_0-6 ratio ranged from 1.15 (stage 1, 20-30 years) to 4.59 (stage 5, 91-100 years, with Pgp inhibitors), relative to a reference subject of 20 years, normal renal function, and no Pgp inhibitors.

Conclusion: Clinicians should consider the risk of Pgp substrate accumulation in older adults, particularly those with advanced renal impairment. We propose typical values stratified by age and renal function to assist in interpreting Pgp phenotyping using fexofenadine exposure, thereby supporting drug optimization in this population. Further studies are needed to explore underlying mechanisms, such as reduced Pgp activity or expression.

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利用群体药代动力学模型提高对非索非那定药代动力学的理解以评估老年患者Pgp表型活性。

背景与目的：非索非那定常被用作检测p -糖蛋白（Pgp）活性的探针底物。虽然它在健康志愿者中的使用有很好的记录，但在老年人和多病患者中的数据缺乏。年龄和疾病相关的生理变化预计会影响非索非那定的药代动力学。本研究旨在研究非索非那定在住院老年患者中的药代动力学，作为Pgp活性的潜在标记物，使用OptimAT研究（ClinicalTrials.gov标识：NCT03477331）的数据。方法：采用449例中位年龄为71岁（范围25-97岁）的住院患者和10例健康志愿者（年龄中位为23岁，范围20-36岁）的数据进行人群药代动力学（popPK）建模。非索非那定血药浓度的分析采用了一种精确的双室模型，具有顺序零/一阶吸收，同时研究了协变量如年龄、肾功能和Pgp抑制剂对非索非那定药代动力学的影响。结果：年龄、肾功能不全和Pgp抑制剂显著影响非索非那定暴露。肾功能是一个关键因素，与正常肾功能相比，轻度至中度肾功能损害患者AUC0-6增加79%，中度至重度肾功能损害患者AUC0-6增加154%。同时使用Pgp抑制剂导致AUC0-6增加35%。在慢性肾脏疾病（CKD）分期、年龄和Pgp抑制剂状态中，非索非那定的AUC0-6比值从1.15（1期，20-30年）到4.59（5期，91-100年，有Pgp抑制剂），相对于20岁、肾功能正常、无Pgp抑制剂的对照受试者。结论：临床医生应考虑Pgp底物在老年人中积累的风险，特别是那些有晚期肾功能损害的老年人。我们提出了按年龄和肾功能分层的典型值，以帮助解释使用非索非那定暴露的Pgp表型，从而支持该人群的药物优化。需要进一步的研究来探索潜在的机制，如Pgp活性或表达的降低。

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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来源期刊

Clinical Pharmacokinetics 医学-药学

CiteScore

8.80

自引率

4.40%

发文量

审稿时长

6-12 weeks

期刊介绍： Clinical Pharmacokinetics promotes the continuing development of clinical pharmacokinetics and pharmacodynamics for the improvement of drug therapy, and for furthering postgraduate education in clinical pharmacology and therapeutics. Pharmacokinetics, the study of drug disposition in the body, is an integral part of drug development and rational use. Knowledge and application of pharmacokinetic principles leads to accelerated drug development, cost effective drug use and a reduced frequency of adverse effects and drug interactions.