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How HIV-1 Gag Manipulates Its Host Cell Proteins: A Focus on Interactors of the Nucleocapsid Domain

机译:HIV-1 GAG如何操纵其宿主细胞蛋白质:专注于核衣壳结构域的交互症

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The human immunodeficiency virus (HIV-1) polyprotein Gag (Group-specific antigen) plays a central role in controlling the late phase of the viral lifecycle. Considered to be only a scaffolding protein for a long time, the structural protein Gag plays determinate and specific roles in HIV-1 replication. Indeed, via its different domains, Gag orchestrates the specific encapsidation of the genomic RNA, drives the formation of the viral particle by its auto-assembly (multimerization), binds multiple viral proteins, and interacts with a large number of cellular proteins that are needed for its functions from its translation location to the plasma membrane, where newly formed virions are released. Here, we review the interactions between HIV-1 Gag and 66 cellular proteins. Notably, we describe the techniques used to evidence these interactions, the different domains of Gag involved, and the implications of these interactions in the HIV-1 replication cycle. In the final part, we focus on the interactions involving the highly conserved nucleocapsid (NC) domain of Gag and detail the functions of the NC interactants along the viral lifecycle.
机译:人免疫缺陷病毒(HIV-1)多蛋白GAG(群体特异性抗原)在控制病毒生命周期的晚期时起着重要作用。被认为只是长期脚手架蛋白质,结构蛋白GAG在HIV-1复制中测定和特异性作用。实际上,通过其不同的结构域,GAG通过其自动组装(多聚化)驱动基因组RNA的特定封装,驱动​​病毒颗粒的形成,结合多种病毒蛋白,并与需要的大量细胞蛋白相互作用从其翻译位置到血浆膜的功能,新形成的病毒群被释放。在这里,我们审查了HIV-1 GAG和66个细胞蛋白之间的相互作用。值得注意的是,我们描述了用于证据这些相互作用的技术,所涉及的GAG的不同域,以及这些相互作用在HIV-1复制周期中的影响。在最后一部分中,我们专注于涉及高度保守的核衣壳(NC)的GAG的相互作用和细节沿着病毒生命周期的NC交互剂的功能。

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