Population Pharmacokinetics of Cobicistat and its Effect on the Pharmacokinetics of the Anticancer Drug Olaparib.

IF 4 2区医学 Q1 PHARMACOLOGY & PHARMACY

Clinical Pharmacokinetics Pub Date : 2025-03-01 Epub Date: 2025-02-05 DOI:10.1007/s40262-025-01480-w

Joanneke K Overbeek, Nielka P van Erp, David M Burger, Alfons A den Broeder, Stijn L W Koolen, Alwin D R Huitema, Rob Ter Heine

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引用次数: 0

Abstract

Objectives: Pharmacokinetic (PK) boosting is the intentional use of strong inhibitors of metabolic enzymes or transporters to boost the systemic exposure of a therapeutic drug. PK boosting is expanding to therapeutic areas outside human immunodeficiency virus (HIV) therapy. Data on the PK of the booster cobicistat and its effect on CYP3A-substrates outside of HIV therapy are lacking. This study aimed to describe the PK of once- and twice-daily cobicistat regimens in healthy volunteers and patients with rheumatoid arthritis, cancer, or HIV infection and to investigate the interplay between cobicistat and the anticancer drug olaparib.

Methods: Cobicistat levels from 683 samples from 66 subjects in four clinical trials were included in the analysis. For olaparib, 261 samples from 12 subjects from one trial were included. Population PK analysis was performed by nonlinear mixed-effects modelling.

Results: Both cobicistat and olaparib PK were adequately described by a well-stirred liver model with one central compartment and Erlang type absorption. Cobicistat PK was similar across patient populations and dosing regimens. Cobicistat increased olaparib prehepatic bioavailability 1.65-fold (RSE 6%) and decreased intrinsic clearance 0.34-fold (RSE 6.5%). A correlation between olaparib PK and cobicistat exposure could not be identified. The interindividual variability in olaparib clearance was lower with cobicistat than without cobicistat.

Conclusions: The developed pharmacokinetic models adequately described cobicistat and olaparib plasma concentrations. PK boosting with cobicistat at 150 mg twice daily led to an increase in olaparib bioavailability and decrease in clearance. This effect was not correlated with cobicistat exposure, which may reflect saturation of the boosting effect of cobicistat at this dose.

Trial registration numbers (date of registration): NCT02565888 (30-09-2015), NCT00825929 (19-01-2009), Netherlands Trial Register NL7766 (18-12-2018), NCT05078671 (22-09-2021).

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可比司他的群体药动学及其对抗癌药奥拉帕尼的影响。

目的：药代动力学（PK）增强是有意使用代谢酶或转运蛋白的强抑制剂来增加治疗药物的全身暴露。PK增强正在扩展到人类免疫缺陷病毒（HIV）治疗以外的治疗领域。关于辅助剂cobicistat的PK及其在HIV治疗之外对cyp3a底物的影响的数据尚缺乏。本研究旨在描述健康志愿者和类风湿关节炎、癌症或HIV感染患者每日一次和两次的共存司他方案的PK，并调查共存司他与抗癌药物奥拉帕尼之间的相互作用。方法：对4项临床试验66例受试者683份样本的Cobicistat水平进行分析。对于奥拉帕尼，一项试验纳入了来自12名受试者的261份样本。种群PK分析采用非线性混合效应模型。结果：可比司他和奥拉帕尼的PK均被充分描述为一个中心室和二郎型吸收的搅拌良好的肝脏模型。不同患者群体和给药方案的Cobicistat PK相似。可比司他提高奥拉帕尼肝前生物利用度1.65倍（RSE 6%），降低内在清除率0.34倍（RSE 6.5%）。不能确定奥拉帕尼PK与共存司他暴露之间的相关性。与未使用共存司他时相比，使用共存司他时奥拉帕尼清除率的个体间变异性更低。结论：建立的药代动力学模型充分描述了共存司他和奥拉帕尼的血药浓度。cobicistat每日两次，每次150 mg，增加PK，导致奥拉帕尼生物利用度增加，清除率降低。该效应与可比司他暴露无关，这可能反映了可比司他在该剂量下的增强效应饱和。试验注册号（注册日期）：NCT02565888 (30-09-2015), NCT00825929(19-01-2009)，荷兰试验注册号NL7766 (18-12-2018), NCT05078671（22-09-2021）。

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.