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在没有可靠给药史的情况下估算替诺福韦的群体药代动力学参数,并应用模拟策略追溯给药史。

Estimation of tenofovir's population pharmacokinetic parameters without reliable dosing histories and application to tracing dosing history using simulation strategies.

作者信息

Chaturvedula Ayyappa, Fossler Michael J, Hendrix Craig W

机构信息

Departments of Pharmacy Practice & Pharmaceutical Sciences, Mercer University College of Pharmacy, Atlanta, GA, USA.

出版信息

J Clin Pharmacol. 2014 Feb;54(2):150-60. doi: 10.1002/jcph.221. Epub 2013 Nov 30.

Abstract

The objectives of this analysis were to develop a population pharmacokinetic model (PPK) for tenofovir without using potentially unreliable patient reported dosing records and to retrace patient dosing history using pharmacokinetic simulations conditioned on protocol design constraints to assess patient adherence. MTN-001 is a multi-center, open label, 3-way cross over study comparing oral, vaginal and combination (oral and vaginal) administration of tenofovir in healthy women. It was reported that self-reported adherence in this study was high (94%), but serum concentrations indicated only 64% of participants used tablets consistently. A method based on superposition was applied to develop the population PPK considering only observable clinic visit dosing information. A two compartment model described the data well and the parameters agree with the literature reported values. Race was not a significant covariate on clearance. Retracing of the dosing history with 3-past dose resolution was not successful. Trial simulations with full adherence assumption predict a median Cmin of 68 ng/mL, which is in agreement with literature reports. Non-adherence at 25% resulted in 37-51% reduction in Cmin using one coin and two coin models, respectively. Population analyses should consider some method of correction for non-adherence to avoid biased estimates.

摘要

本分析的目的是建立一个替诺福韦的群体药代动力学模型(PPK),不使用可能不可靠的患者报告给药记录,并利用基于方案设计约束条件的药代动力学模拟追溯患者给药历史,以评估患者的依从性。MTN-001是一项多中心、开放标签、三臂交叉研究,比较替诺福韦在健康女性中的口服、阴道给药及联合(口服和阴道)给药情况。据报道,本研究中自我报告的依从性较高(94%),但血清浓度表明只有64%的参与者持续使用片剂。应用一种基于叠加的方法,仅考虑可观察到的临床访视给药信息来建立群体PPK。一个二室模型能很好地描述数据,且参数与文献报道值一致。种族不是清除率的显著协变量。以3个既往剂量分辨率追溯给药历史未成功。完全依从假设下的试验模拟预测中位Cmin为68 ng/mL,这与文献报道一致。分别使用单硬币和双硬币模型,25%的不依从导致Cmin降低37% - 51%。群体分析应考虑某种校正不依从的方法,以避免估计偏差。

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