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比克替拉韦加替诺福韦艾拉酚胺纳米制剂作为长效暴露前预防方案:建模在设计非人灵长类动物药代动力学实验中的应用

Bictegravir Plus Tenofovir Alafenamide Nanoformulation as a Long-Acting Pre-Exposure Prophylaxis Regimen: Application of Modeling to Design Non-Human Primate Pharmacokinetic Experiments.

作者信息

Perazzolo Simone, Mandal Subhra, Prathipati Pavan K, Destache Christopher J

机构信息

Nanomath LLC and University of Washington, Seattle, WA, United States.

School of Pharmacy, Creighton University, Omaha, NE, United States.

出版信息

Front Pharmacol. 2020 Dec 18;11:603242. doi: 10.3389/fphar.2020.603242. eCollection 2020.

DOI:10.3389/fphar.2020.603242
PMID:33390993
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7775496/
Abstract

Bictegravir (BIC) and tenofovir alafenamide fumarate (TAF), two potent anti-HIV drugs, had been nanoformulated () to achieve once-a-month PrEP coverage. mouse experiments for exhibited favorable subcutaneous (SC) pharmacokinetics. To probe the clinical suitability of the , as the next step, we intend to study in non-human primates (NHP), as the best preclinical model to foster clinical trials. Before entering an expensive NHP study, however, we seek to improve our a priori understanding about in higher species, having just mouse data. The mechanism-based pharmacokinetic modeling (MBPK) has been used as an appropriate method for pharmacokinetic modeling and interspecies scaling for nanoformulations. Via the use of MBPK, in this work, we created a model for able to predict plasma concentration-time curves in NHP. BIKTARVY is a daily oral combination of BIC, TAF, and emtricitabine (Gilead Science, CA), approved for HIV therapy. Using BIKTARVY equivalent dosages (from their NHP studies), we predicted that, following just one SC dose of in NHP, both BIC and tenofovir will have detectable and above efficacy levels for 28 days. Furthermore, the MBPK was able to provide a mechanistic explanation regarding the long-acting mechanism characterizing : nanoparticles stores in the SC space from which drugs slowly dissociate. Dissociated drugs in the SC space then buffer the plasma pool over time, yielding an extended-release effect in the plasma. Overall, we predicted for a promising long-acting pharmacokinetic in NHP, potentially usable as monthly PrEP. These results will help investigators to gain confidence for facing regulatory submissions at early stages.

摘要

比克替拉韦(BIC)和替诺福韦艾拉酚胺富马酸盐(TAF)这两种强效抗HIV药物已制成纳米制剂,以实现每月一次的暴露前预防(PrEP)覆盖。小鼠实验显示皮下(SC)给药具有良好的药代动力学。作为下一步,为探究该纳米制剂的临床适用性,我们打算在非人类灵长类动物(NHP)中进行研究,因为这是推进临床试验的最佳临床前模型。然而,在开展昂贵的NHP研究之前,鉴于仅有小鼠数据,我们希望先增进对该纳米制剂在高等物种中的了解。基于机制的药代动力学建模(MBPK)已被用作纳米制剂药代动力学建模和种间缩放的合适方法。通过使用MBPK,在本研究中,我们创建了一个能够预测NHP血浆浓度 - 时间曲线的模型。必妥维(BIKTARVY)是一种由BIC、TAF和恩曲他滨组成的每日口服复方制剂(吉利德科学公司,加利福尼亚州),已获批用于HIV治疗。使用必妥维等效剂量(来自其NHP研究),我们预测,在NHP中仅皮下注射一剂该纳米制剂后,BIC和替诺福韦在28天内都将具有可检测的且高于有效水平的浓度。此外,MBPK能够就该纳米制剂的长效机制提供一个机理解释:纳米颗粒储存在皮下空间,药物从其中缓慢解离。皮下空间中解离的药物随后随时间缓冲血浆池,在血浆中产生缓释效应。总体而言,我们预测该纳米制剂在NHP中具有有前景的长效药代动力学,有可能用作每月一次的PrEP。这些结果将有助于研究人员在早期阶段面对监管申报时获得信心。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2302/7775496/cc4155a4793b/fphar-11-603242-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2302/7775496/cc4155a4793b/fphar-11-603242-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2302/7775496/cc4155a4793b/fphar-11-603242-g001.jpg

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