Small but Highly Versatile: The Viral Accessory Protein Vpu.

IF 8.1 1区 医学 Q1 VIROLOGY
Annual Review of Virology Pub Date : 2023-09-29 Epub Date: 2023-07-05 DOI:10.1146/annurev-virology-111821-100816
Meta Volcic, Lisa Wiesmüller, Frank Kirchhoff
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引用次数: 0

Abstract

Human and simian immunodeficiency viruses (HIVs and SIVs, respectively) encode several small proteins (Vif, Vpr, Nef, Vpu, and Vpx) that are called accessory because they are not generally required for viral replication in cell culture. However, they play complex and important roles for viral immune evasion and spread in vivo. Here, we discuss the diverse functions and the relevance of the viral protein U (Vpu) that is expressed from a bicistronic RNA during the late stage of the viral replication cycle and found only in HIV-1 and closely related SIVs. It is well established that Vpu counteracts the restriction factor tetherin, mediates degradation of the primary viral CD4 receptors, and inhibits activation of the transcription factor nuclear factor kappa B. Recent studies identified additional activities and provided new insights into the sophisticated mechanisms by which Vpu enhances and prolongs the release of fully infectious viral particles. In addition, it has been shown that Vpu prevents superinfection not only by degrading CD4 but also by modulating DNA repair mechanisms to promote degradation of nuclear viral complementary DNA in cells that are already productively infected.

小但高度通用:病毒辅助蛋白Vpu。
人类和猴免疫缺陷病毒(分别为HIVs和SIV)编码几种小蛋白(Vif、Vpr、Nef、Vpu和Vpx),这些小蛋白被称为辅助蛋白,因为它们通常不是细胞培养中病毒复制所必需的。然而,它们在病毒免疫逃避和体内传播中发挥着复杂而重要的作用。在这里,我们讨论了病毒蛋白U(Vpu)的不同功能和相关性,该蛋白在病毒复制周期的后期由双顺反子RNA表达,仅在HIV-1和密切相关的SIV中发现。众所周知,Vpu对抗限制性因子栓系蛋白,介导原代病毒CD4受体的降解,并抑制转录因子核因子κB的激活。最近的研究确定了额外的活性,并为Vpu增强和延长完全传染性病毒颗粒释放的复杂机制提供了新的见解。此外,已经表明Vpu不仅通过降解CD4,而且通过调节DNA修复机制来防止重叠感染,以促进已经有效感染的细胞中核病毒互补DNA的降解。
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来源期刊
CiteScore
19.40
自引率
0.90%
发文量
28
期刊介绍: The Annual Review of Virology serves as a conduit for disseminating thrilling advancements in our comprehension of viruses spanning animals, plants, bacteria, archaea, fungi, and protozoa. Its reviews illuminate novel concepts and trajectories in basic virology, elucidating viral disease mechanisms, exploring virus-host interactions, and scrutinizing cellular and immune responses to virus infection. These reviews underscore the exceptional capacity of viruses as potent probes for investigating cellular function.
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