评估富马酸替诺福韦二酯/恩曲他滨HIV暴露前预防用药的临床试验模拟。

IF 2.3 Q2 PUBLIC, ENVIRONMENTAL & OCCUPATIONAL HEALTH Frontiers in reproductive health Pub Date : 2023-09-27 eCollection Date: 2023-01-01 DOI:10.3389/frph.2023.1224580
Rachel K Scott, Yifan Yu, Mark A Marzinke, Jenell S Coleman, Craig W Hendrix, Robert Bies
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引用次数: 0

摘要

目的:评估妊娠期间向上调整富马酸替诺福韦二酯(TDF)/恩曲他滨(FTC)暴露前预防(PrEP)给药,以维持与HIV保护相关的目标血浆浓度。设计:群体药代动力学(PK)建模和临床试验模拟(CTS)。材料和方法:我们使用合作伙伴示范项目的数据和Coleman等人对顺性别女性TDF/FTC的PK研究开发了TFV和FTC的群体药代学模型,并进行了计算机模拟。在优化的最终模型中,妊娠期被确定为表观清除率的显著协变量。我们模拟了1000名孕妇开始标准的每日口服TDF/FTC(300 mg/200 mg)。怀孕后,模拟患者被分为两组:一组持续标准剂量,另一组在整个妊娠期接受双倍标准剂量。结果:与妊娠前相比,妊娠期的标准剂量谷TFV浓度显著降低,谷血浆浓度分别有34.0%、43.8%和65.1%低于预期谷浓度的下限,这被认为是妊娠期第1、2和3个月的保护阈值。相比之下,在模拟双剂量组中,分别有10.7%、14.4%和27.8%的谷浓度在第一、第二和第三个月低于估计的保护阈值。妊娠期间的FTC谷血浆浓度也低于妊娠前,45.2%的稳态谷浓度低于FTC的估计保护性谷浓度。在妊娠调整双剂量组中,24.1%的谷血浆浓度低于保护水平。结论:我们的模拟显示,超过50%的标准剂量的研究参与者在妊娠晚期的谷血浆TFV浓度低于与保护相关的水平。该模拟为妊娠期前瞻性TDF/FTC研究的设计提供了定量基础,以评估妊娠调整剂量的安全性和适当性。
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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Clinical trial simulation to evaluate tenofovir disoproxil fumarate/emtricitabine HIV pre-exposure prophylaxis dosing during pregnancy.

Objective: To evaluate upward-adjustment of tenofovir disoproxil fumarate (TDF)/emtricitabine (FTC) pre-exposure prophylaxis (PrEP) dosing during pregnancy in order to maintain target plasma concentrations associated with HIV protection.

Design: Population pharmacokinetic (PK) modeling and clinical trial simulation (CTS).

Material and methods: We developed population pharmacokinetic models for TFV and FTC using data from the Partners Demonstration Project and a PK study of TDF/FTC among cisgender women by Coleman et al., and performed an in-silico simulation. Pregnancy-trimester was identified as a significant covariate on apparent clearance in the optimized final model. We simulated 1,000 pregnant individuals starting standard daily oral TDF/FTC (300 mg/200 mg) prior to pregnancy. Upon becoming pregnant, simulated patients were split into two study arms: one continuing standard-dose and the other receiving double standard-dose throughout pregnancy.

Results: Standard-dose trough TFV concentrations were significantly lower in pregnancy compared to pre-pregnancy, with 34.0%, 43.8%, and 65.1% of trough plasma concentrations below the lower bound of expected trough concentrations presumed to be the protective threshold in the 1st, 2nd, and 3rd trimesters, respectively. By comparison, in the simulated double-dose group, 10.7%, 14.4%, and 27.8% of trough concentrations fell below the estimated protective thresholds in the 1st, 2nd, and 3rd trimesters, respectively. The FTC trough plasma concentration during pregnancy was also lower than pre-pregnancy, with 45.2% of the steady-state trough concentrations below the estimated protective trough concentrations of FTC. In the pregnancy-adjusted double-dose group, 24.1% of trough plasma concentrations were lower than protective levels.

Conclusions: Our simulation shows >50% of research participants on standard dosing would have 3rd trimester trough plasma TFV concentrations below levels associated with protection. This simulation provides the quantitative basis for the design of prospective TDF/FTC studies during pregnancy to evaluate the safety and appropriateness of pregnancy-adjusted dosing.

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