委内瑞拉马脑炎病毒 nsP3 蛋白高变区突变差异影响病毒复制。
Mutations in Hypervariable Domain of Venezuelan Equine Encephalitis Virus nsP3 Protein Differentially Affect Viral Replication.
机构信息
Department of Microbiology, University of Alabama at Birmingham, Birmingham, Alabama, USA.
Department of Microbiology, University of Alabama at Birmingham, Birmingham, Alabama, USA
出版信息
J Virol. 2020 Jan 17;94(3). doi: 10.1128/JVI.01841-19.
Venezuelan equine encephalitis virus (VEEV) is one of the important human and animal pathogens. It forms replication enzyme complexes (RCs) containing viral nonstructural proteins (nsPs) that mediate the synthesis of virus-specific RNAs. The assembly and associated functions of RC also depend on the presence of a specific set of host proteins. Our study demonstrates that the hypervariable domain (HVD) of VEEV nsP3 interacts with the members of the FXR family of cellular proteins and also binds the Src homology 3 (SH3) domain-containing proteins CD2AP and SH3KBP1. Interactions with FXR family members are mediated by the C-terminal repeating peptide of HVD. A single short, minimal motif identified in this study is sufficient for driving efficient VEEV replication in the absence of HVD interactions with other host proteins. The SH3 domain-containing proteins bind to another fragment of VEEV HVD. They can promote viral replication in the absence of FXR-HVD interactions albeit less efficiently. VEEV replication can be also switched from an FXR-dependent to a chikungunya virus-specific, G3BP-dependent mode. The described modifications of VEEV HVD have a strong impact on viral replication and pathogenesis. Their effects on viral pathogenesis depend on mouse age and the genetic background of the virus. The replication of alphaviruses is determined by specific sets of cellular proteins, which mediate the assembly of viral replication complexes. Some of these critical host factors interact with the hypervariable domain (HVD) of alphavirus nsP3. In this study, we have explored binding sites of host proteins, which are specific partners of nsP3 HVD of Venezuelan equine encephalitis virus. We also define the roles of these interactions in viral replication both and A mechanistic understanding of the binding of CD2AP, SH3KBP1, and FXR protein family members to VEEV HVD uncovers important aspects of alphavirus evolution and determines new targets for the development of alphavirus-specific drugs and directions for viral attenuation and vaccine development.
委内瑞拉马脑炎病毒(VEEV)是一种重要的人类和动物病原体。它形成包含病毒非结构蛋白(nsPs)的复制酶复合物(RCs),介导病毒特异性 RNA 的合成。RC 的组装和相关功能也依赖于特定的一组宿主蛋白的存在。我们的研究表明,VEEV nsP3 的超变区(HVD)与细胞蛋白的 FXR 家族成员相互作用,并且还与包含 SH3 结构域的蛋白 CD2AP 和 SH3KBP1 结合。与 FXR 家族成员的相互作用是由 HVD 的 C 端重复肽介导的。本研究中鉴定的单个短的最小基序足以在没有 HVD 与其他宿主蛋白相互作用的情况下驱动 VEEV 的有效复制。包含 SH3 结构域的蛋白结合到 VEEV HVD 的另一个片段。尽管效率较低,但它们可以在没有 FXR-HVD 相互作用的情况下促进病毒复制。VEEV 的复制也可以从依赖 FXR 的模式切换为依赖基孔肯雅病毒的、G3BP 依赖的模式。所描述的 VEEV HVD 的修饰对病毒复制和发病机制有很大影响。它们对病毒发病机制的影响取决于小鼠的年龄和病毒的遗传背景。甲病毒的复制由特定的细胞蛋白决定,这些蛋白介导病毒复制复合物的组装。其中一些关键的宿主因子与甲病毒 nsP3 的超变区(HVD)相互作用。在这项研究中,我们探索了宿主蛋白的结合位点,这些宿主蛋白是委内瑞拉马脑炎病毒 nsP3 HVD 的特定伴侣。我们还定义了这些相互作用在病毒复制中的作用,以及。对 CD2AP、SH3KBP1 和 FXR 蛋白家族成员与 VEEV HVD 的结合的机制理解揭示了甲病毒进化的重要方面,并确定了开发甲病毒特异性药物的新靶标以及病毒减毒和疫苗开发的方向。
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