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预测女性有效HIV化学预防的模型。

Models for predicting effective HIV chemoprevention in women.

作者信息

Nicol Melanie R, Emerson Cindi W, Prince Heather M A, Nelson Julie A E, Fedoriw Yuri, Sykes Craig, Geller Elizabeth J, Patterson Kristine B, Cohen Myron S, Kashuba Angela D M

机构信息

*Division of Pharmacotherapy and Experimental Therapeutics, Eshelman School of Pharmacy, University of North Carolina at Chapel Hill, Chapel Hill, NC; †Center for AIDS Research, University of North Carolina at Chapel Hill, Chapel Hill, NC; and ‡Departments of Medicine and §Microbiology and Immunology, University of North Carolina at Chapel Hill, Chapel Hill, NC (Melanie R. Nicol is now with the Department of Experimental and Clinical Pharmacology, College of Pharmacy, University of Minnesota, Minneapolis, MN).

出版信息

J Acquir Immune Defic Syndr. 2015 Apr 1;68(4):369-76. doi: 10.1097/QAI.0000000000000472.

Abstract

OBJECTIVE

Model systems that rapidly identify tissue drug concentrations protective of HIV infection could streamline the development of chemoprevention strategies. Tissue models are promising, but limited concentration targets exist, and no systematic comparison to cell models or clinical studies has been performed.

DESIGN

We explored the efficacy of maraviroc (MVC) and tenofovir (TFV) for HIV prevention by comparing Emax models from TZM-bl cells to vaginal tissue explants and evaluated their predictive capabilities with a dose-challenge clinical study.

METHODS

HIV-1JR-CSF was used for viral challenge. Drug efficacy was assessed using a luciferase reporter assay in TZM-bl cells and real-time PCR to quantify spliced RNA in a tissue explant model. Cell and tissue concentrations of MVC, TFV, and the active metabolite tenofovir diphosphate were measured by liquid chromatography with tandem mass spectrometry and used to create Emax models of efficacy. Efficacy after a single oral dose of 600 mg MVC and 600 mg tenofovir disoproxil fumarate was predicted from cell and tissue models and confirmed in a clinical study with viral biopsy challenge postdose.

RESULTS

TFV was >10-fold and MVC >1000-fold, more potent in TZM-bl cells compared with vaginal explant tissue. In the dose-challenge study, tissues from 3 of 6 women were protected from HIV infection, which was 49% lower than predicted by TZM-bl data and 36% higher than predicted by tissue explant data.

CONCLUSIONS

Comparative effective concentration data were generated for TFV and MVC in 3 HIV chemoprophylaxis models. These results provide a framework for future early investigations of antiretroviral efficacy in HIV prevention to optimize dosing strategies in clinical investigations.

摘要

目的

能够快速确定可预防HIV感染的组织药物浓度的模型系统,可简化化学预防策略的开发。组织模型很有前景,但存在有限的浓度靶点,且尚未与细胞模型或临床研究进行系统比较。

设计

我们通过比较TZM-bl细胞与阴道组织外植体的Emax模型,探讨了马拉维若(MVC)和替诺福韦(TFV)预防HIV的效果,并通过剂量挑战临床研究评估了它们的预测能力。

方法

使用HIV-1JR-CSF进行病毒攻击。在TZM-bl细胞中使用荧光素酶报告基因检测评估药物疗效,并在组织外植体模型中使用实时PCR定量剪接RNA。通过液相色谱-串联质谱法测量MVC、TFV和活性代谢物二磷酸替诺福韦的细胞和组织浓度,并用于建立疗效的Emax模型。根据细胞和组织模型预测单次口服600 mg MVC和600 mg富马酸替诺福韦二吡呋酯后的疗效,并在剂量后进行病毒活检挑战的临床研究中得到证实。

结果

与阴道外植体组织相比,TFV在TZM-bl细胞中的效力高10倍以上,MVC高1000倍以上。在剂量挑战研究中,6名女性中有3名的组织受到HIV感染的保护,这比TZM-bl数据预测的低49%,比组织外植体数据预测的高36%。

结论

在3种HIV化学预防模型中生成了TFV和MVC的比较有效浓度数据。这些结果为未来在HIV预防中早期研究抗逆转录病毒疗效以优化临床研究中的给药策略提供了框架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ebbd/4334725/9e06f2ff61f9/nihms645182f1.jpg

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