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Hantavirus Gn and Gc Envelope Glycoproteins: Key Structural Units for Virus Cell Entry and Virus Assembly

机译:汉坦病毒Gn和Gc包膜糖蛋白:病毒细胞进入和病毒组装的关键结构单位

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摘要

In recent years, ultrastructural studies of viral surface spikes from three different genera within the Bunyaviridae family have revealed a remarkable diversity in their spike organization. Despite this structural heterogeneity, in every case the spikes seem to be composed of heterodimers formed by Gn and Gc envelope glycoproteins. In this review, current knowledge of the Gn and Gc structures and their functions in virus cell entry and exit is summarized. During virus cell entry, the role of Gn and Gc in receptor binding has not yet been determined. Nevertheless, biochemical studies suggest that the subsequent virus-membrane fusion activity is accomplished by Gc. Further, a class II fusion protein conformation has been predicted for Gc of hantaviruses, and novel crystallographic data confirmed such a fold for the Rift Valley fever virus (RVFV) Gc protein. During virus cell exit, the assembly of different viral components seems to be established by interaction of Gn and Gc cytoplasmic tails (CT) with internal viral ribonucleocapsids. Moreover, recent findings show that hantavirus glycoproteins accomplish important roles during virus budding since they self-assemble into virus-like particles. Collectively, these novel insights provide essential information for gaining a more detailed understanding of Gn and Gc functions in the early and late steps of the hantavirus infection cycle.
机译:近年来,对来自Bunyaviridae家族三个不同属的病毒表面刺突的超微结构研究表明,它们的刺突组织具有显着的多样性。尽管存在这种结构异质性,但在每种情况下,刺突似乎都是由Gn和Gc包膜糖蛋白形成的异二聚体组成。在这篇综述中,总结了有关Gn和Gc结构及其在病毒细胞进入和退出中的功能的当前知识。在病毒细胞进入过程中,尚未确定Gn和Gc在受体结合中的作用。然而,生化研究表明,随后的病毒-膜融合活性是由Gc完成的。此外,已经预测汉坦病毒的Gc具有II类融合蛋白构象,并且新的晶体学数据证实了裂谷热病毒(RVFV)Gc蛋白的这种折叠。在病毒细胞退出期间,似乎通过Gn和Gc细胞质尾巴(CT)与内部病毒核糖核衣壳的相互作用而建立了不同病毒组分的装配体。此外,最近的发现表明,汉坦病毒糖蛋白在病毒出芽期间起重要作用,因为它们自组装成病毒样颗粒。总的来说,这些新颖的见解为在汉坦病毒感染周期的早期和晚期阶段获得对Gn和Gc功能的更详细的了解提供了必要的信息。

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