Degradation-Independent Inhibition of APOBEC3G by the HIV-1 Vif Protein.

Viruses Pub Date : 2021-04-03 DOI:10.3390/v13040617

Benjamin Stupfler, Cédric Verriez, Sarah Gallois-Montbrun, Roland Marquet, Jean-Christophe Paillart

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引用次数: 7

Abstract

The ubiquitin-proteasome system plays an important role in the cell under normal physiological conditions but also during viral infections. Indeed, many auxiliary proteins from the (HIV-1) divert this system to its own advantage, notably to induce the degradation of cellular restriction factors. For instance, the HIV-1 viral infectivity factor (Vif) has been shown to specifically counteract several cellular deaminases belonging to the apolipoprotein B mRNA-editing enzyme catalytic polypeptide-like (APOBEC3 or A3) family (A3A to A3H) by recruiting an E3-ubiquitin ligase complex and inducing their polyubiquitination and degradation through the proteasome. Although this pathway has been extensively characterized so far, Vif has also been shown to impede A3s through degradation-independent processes, but research on this matter remains limited. In this review, we describe our current knowledge regarding the degradation-independent inhibition of A3s, and A3G in particular, by the HIV-1 Vif protein, the molecular mechanisms involved, and highlight important properties of this small viral protein.

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HIV-1 Vif蛋白对APOBEC3G的降解非依赖性抑制

在正常生理条件下，泛素-蛋白酶体系统在细胞中起着重要的作用，在病毒感染过程中也起着重要的作用。事实上，来自HIV-1的许多辅助蛋白使该系统转向其自身优势，特别是诱导细胞限制因子的降解。例如，HIV-1病毒感染因子(Vif)已被证明通过招募e3 -泛素连接酶复合物并通过蛋白酶体诱导它们的多泛素化和降解，特异性地对抗几种属于载脂蛋白B mrna编辑酶催化多肽样(APOBEC3或A3)家族(A3A至A3H)的细胞脱氨酶。尽管到目前为止这一途径已经被广泛表征，Vif也被证明通过不依赖降解的过程阻碍a3，但对这一问题的研究仍然有限。在这篇综述中，我们描述了目前关于HIV-1 Vif蛋白对A3s，特别是A3G的降解非依赖性抑制的知识，所涉及的分子机制，并强调了这种小病毒蛋白的重要特性。

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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Viruses

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