根据血浆暴露量对进展期转移性钙化抗性前列腺癌患者进行阿比特龙个体内剂量递增:OPTIMABI试验结果。

IF 4.6 2区 医学 Q1 PHARMACOLOGY & PHARMACY Clinical Pharmacokinetics Pub Date : 2024-07-01 Epub Date: 2024-07-04 DOI:10.1007/s40262-024-01396-x
Jérôme Alexandre, Stephane Oudard, Lisa Golmard, Luca Campedel, Mourad Mseddi, Sylvain Ladoire, Ahmed Khalil, Denis Maillet, Christophe Tournigand, Blaise Pasquiers, Françoise Goirand, Joseph Berthier, Jérôme Guitton, Charles Dariane, Florence Joly, Evanguelos Xylinas, Jean Louis Golmard, Hendy Abdoul, Alicja Puszkiel, Xavier Decleves, Edith Carton, Audrey Thomas, Michel Vidal, Olivier Huillard, Benoit Blanchet
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引用次数: 0

摘要

背景和目的:8.4纳克/毫升的阿比特龙低浓度(ABI Cmin)已被确定为转移性去势抵抗性前列腺癌(mCRPC)患者的适当疗效阈值。OPTIMABI II 期研究旨在评估药代动力学(PK)指导下的醋酸阿比特龙(AA)剂量递增对未充分暴露且肿瘤早期进展的 mCRPC 患者的疗效:这项多中心、非随机研究包括两个连续步骤。第一步,所有患者开始接受每天一次、每次 1000 毫克 AA 的治疗。在治疗的前 12 周内,每月在最后一次服药后 22-26 小时测量阿比特龙 Cmin。在步骤 2 中,未充分暴露的患者(Cmin < 8.4 纳克/毫升)在治疗的前 6 个月内出现肿瘤进展,这些患者将接受每日两次、每次 1000 毫克的 AA 治疗。主要终点是剂量加倍后 12 周的无进展率。在步骤1中,使用Girerd自我报告问卷对ABI治疗的依从性进行了评估。采用贝叶斯法对在采样指南(22-26 h)外采集的样本的Cmin进行估计,对药代动力学(PK)数据进行了事后分析:在意向治疗分析(ITT)中,有 81 名患者被纳入步骤 1。共有 21 名患者(26%)在第一步中暴露不足,其中 8 名患者(38%)在最初 6 个月内肿瘤进展。共有 71 名患者(88%)填写了 Girerd 自我报告问卷。其中,62%的患者得分为0分,38%的患者得分为1分或2分(轻度依从性失败),两组患者的平均ABI Cmin无显著差异。有四名患者进入了第二步,在加倍剂量后,他们都达到了暴露目标(Cmin > 8.4 ng/mL),但没有一人达到主要终点。在对PK数据进行的事后分析中,有32名患者(39%)暴露不足,ABI Cmin与无进展生存期的恶化独立相关[危险比(HR)2.50,95%置信区间(CI)1.07-5.81;P = 0.03],这与ITT分析形成鲜明对比:ITT和按方案分析表明,在mCRPC患者中,ABI暴露不足与早期肿瘤进展风险增加之间没有统计学关联,而贝叶斯估算器显示两者之间存在关联。不过,除了在病情进展时加大剂量外,还需要对其他策略进行评估。在本研究中,治疗依从性似乎一致良好。最后,使用贝叶斯方法恢复在预定采血时间窗外采集的样本,将有利于开展基于药物监测的临床试验。OPTIMABI试验已注册为国家临床试验,编号为NCT03458247,EudraCT编号为2017-000560-15)。
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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Intra-individual Dose Escalation of Abiraterone According to Its Plasma Exposure in Patients with Progressive Metastatic Castration-Resistant Prostate Cancer: Results of the OPTIMABI Trial.

Background and objective: Trough abiraterone concentration (ABI Cmin) of 8.4 ng/mL has been identified as an appropriate efficacy threshold in patients treated for metastatic castration-resistant prostate cancer (mCRPC). The aim of the phase II OPTIMABI study was to evaluate the efficacy of pharmacokinetics (PK)-guided dose escalation of abiraterone acetate (AA) in underexposed patients with mCRPC with early tumour progression.

Methods: This multicentre, non-randomised study consisted of two sequential steps. In step 1, all patients started treatment with 1000 mg of AA once daily. Abiraterone Cmin was measured 22-26 h after the last dose intake each month during the first 12 weeks of treatment. In step 2, underexposed patients (Cmin < 8.4 ng/mL) with tumour progression within the first 6 months of treatment were enrolled and received AA 1000 mg twice daily. The primary endpoint was the rate of non-progression at 12 weeks after the dose doubling. During step 1, adherence to ABI treatment was assessed using the Girerd self-reported questionnaire. A post-hoc analysis of pharmacokinetic (PK) data was conducted using Bayesian estimation of Cmin from samples collected outside the sampling guidelines (22-26 h).

Results: In the intention-to-treat analysis (ITT), 81 patients were included in step 1. In all, 21 (26%) patients were underexposed in step 1, and 8 of them (38%) experienced tumour progression within the first 6 months. A total of 71 patients (88%) completed the Girerd self-reported questionnaire. Of the patients, 62% had a score of 0, and 38% had a score of 1 or 2 (minimal compliance failure), without a significant difference in mean ABI Cmin in the two groups. Four patients were enrolled in step 2, and all reached the exposure target (Cmin > 8.4 ng/mL) after doubling the dose, but none met the primary endpoint. In the post-hoc analysis of PK data, 32 patients (39%) were underexposed, and ABI Cmin was independently associated with worse progression-free survival [hazard ratio (HR) 2.50, 95% confidence interval (CI) 1.07-5.81; p = 0.03], in contrast to the ITT analysis.

Conclusion: The ITT and per-protocol analyses showed no statistical association between ABI underexposure and an increased risk of early tumour progression in patients with mCRPC, while the Bayesian estimator showed an association. However, other strategies than dose escalation at the time of progression need to be evaluated. Treatment adherence appeared to be uniformly good in the present study. Finally, the use of a Bayesian approach to recover samples collected outside the predefined blood collection time window could benefit the conduct of clinical trials based on drug monitoring. OPTIMABI trial is registered as National Clinical Trial number NCT03458247, with the EudraCT number 2017-000560-15).

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来源期刊
CiteScore
8.80
自引率
4.40%
发文量
86
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.
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