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反式激活因子(Tat)在HIV潜伏和激活中的作用。

The role of Tat in HIV latency and reactivation.

作者信息

Margolis David M, Browne Edward P

机构信息

Departments of Medicine, Microbiology and Immunology, UNC HIV Cure Center, University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.

出版信息

Front Immunol. 2025 Aug 27;16:1650385. doi: 10.3389/fimmu.2025.1650385. eCollection 2025.

Abstract

HIV persists during therapy due the existence of a latently infected reservoir in which viral gene expression is silenced. This reservoir thus represents the primary barrier to a cure for HIV. To eliminate latently infected cells from people with HIV (PWH) on antiretroviral therapy (ART), small molecules that reverse HIV latency (Latency reversing agents - LRAs) have been previously developed and tested, but these lack specificity for HIV and are typically inefficient at promoting broad reservoir reactivation. As such, more potent and selective tools for latency reversal are needed. Recently, delivery of mRNA encoding the viral protein Tat, which promotes transcriptional elongation, has attracted interest as a possible HIV-specific approach to inducing latency reversal. This review will cover the evidence that Tat plays a key role in both establishment of HIV latency and latency reversal, as well as recent developments in which Tat mRNA delivery has been used to enhance latency reversal approaches. Delivery of Tat to infected cells represents a promising avenue to bypass the limitations of small molecule LRAs and achieve broad reactivation of the clinical reservoir.

摘要

由于存在潜伏感染库,其中病毒基因表达被沉默,所以HIV在治疗期间持续存在。因此,这个储存库是治愈HIV的主要障碍。为了从接受抗逆转录病毒疗法(ART)的HIV感染者(PWH)中消除潜伏感染的细胞,先前已经开发并测试了逆转HIV潜伏的小分子(潜伏逆转剂-LRAs),但这些分子对HIV缺乏特异性,并且在促进广泛的储存库重新激活方面通常效率低下。因此,需要更有效和选择性的潜伏逆转工具。最近,递送编码病毒蛋白Tat的mRNA,其促进转录延伸,作为一种可能的HIV特异性诱导潜伏逆转的方法引起了关注。本综述将涵盖Tat在HIV潜伏建立和潜伏逆转中起关键作用的证据,以及Tat mRNA递送用于增强潜伏逆转方法的最新进展。将Tat递送至感染细胞是绕过小分子LRA的局限性并实现临床储存库广泛重新激活的一条有前途的途径。

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