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联合抗逆转录病毒疗法和免疫压力导致体内 HIV-1 与原始病毒基因组发生重组。

Combined antiretroviral therapy and immune pressure lead to in vivo HIV-1 recombination with ancestral viral genomes.

机构信息

Hospital Universitari Germans Trias i Pujol, Universitat Autònoma de Barcelona, Badalona, Spain.

出版信息

J Acquir Immune Defic Syndr. 2011 Jun 1;57(2):109-17. doi: 10.1097/QAI.0b013e318215ab0a.

Abstract

BACKGROUND

Studies on drug interruption have provided new insights on the adaptive evolution of rebounding HIV-1 during antiretroviral pressure. We investigated the origin of new viral variants after discontinuation of protease (PR) inhibitors as a treatment remained exclusively based on reverse transcriptase inhibitors, and whether drug susceptibility, viral fitness, and neutralizing antibodies could be major driving forces for the evolution of virus populations.

METHODS

The study comprised 3 treatment-experienced subjects. Phylogenetic analysis of the PR, reverse transcriptase, and the viral envelope were carried out to ascertain the origin of the new viral variants with samples obtained over a 10-year period before and after a PR inhibitor withdrawal. In addition, drug susceptibility, replication capacity, and neutralization assays were performed.

RESULTS

New viral variants from all 3 subjects were derived through recombination with ancestral quasispecies. Computerized recombination models confirmed these results. Recombination was demonstrated by increased replication capacity, decreased drug susceptibility, and neutralization of ancestral virus envelope by contemporaneous plasma samples.

CONCLUSIONS

These findings demonstrate the relevance of HIV-1 reservoirs in adaptive evolution throughout recombination in response to selective pressure, such as antiretroviral therapy and immune responses. This result might assist in the design of new treatment strategies for patients experiencing treatment failure.

摘要

背景

药物中断研究为抗逆转录病毒压力下 HIV-1 反弹的适应性进化提供了新的见解。我们研究了在完全基于逆转录酶抑制剂的治疗方案中停止使用蛋白酶抑制剂后新病毒变异体的起源,以及药物敏感性、病毒适应性和中和抗体是否可能是病毒群体进化的主要驱动力。

方法

本研究包括 3 名有治疗经验的受试者。对 PR、逆转录酶和病毒包膜进行系统发育分析,以确定在停止使用 PR 抑制剂前后 10 年期间获得的样本中,新病毒变异体的起源。此外,还进行了药物敏感性、复制能力和中和测定。

结果

所有 3 名受试者的新病毒变异体均通过与祖先准种重组产生。计算机重组模型证实了这些结果。重组通过增加复制能力、降低药物敏感性以及同时代血浆样本对祖先病毒包膜的中和作用得到证实。

结论

这些发现表明,在抗逆转录病毒治疗和免疫反应等选择性压力下,HIV-1 储库在适应性进化中通过重组起重要作用。这一结果可能有助于为治疗失败的患者设计新的治疗策略。

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