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一种冠状病毒核衣壳蛋白的N端和C端结构域的X射线晶体结构:对核衣壳形成的影响

X-ray structures of the N- and C-terminal domains of a coronavirus nucleocapsid protein: implications for nucleocapsid formation.

作者信息

Jayaram Hariharan, Fan Hui, Bowman Brian R, Ooi Amy, Jayaram Jyothi, Collisson Ellen W, Lescar Julien, Prasad B V Venkataram

机构信息

Verna and Marrs McLean Department of Biochemistry and Molecular Biology, Baylor College of Medicine, One Baylor Plaza, Houston, TX 77030-3498, USA.

出版信息

J Virol. 2006 Jul;80(13):6612-20. doi: 10.1128/JVI.00157-06.

Abstract

Coronaviruses cause a variety of respiratory and enteric diseases in animals and humans including severe acute respiratory syndrome. In these enveloped viruses, the filamentous nucleocapsid is formed by the association of nucleocapsid (N) protein with single-stranded viral RNA. The N protein is a highly immunogenic phosphoprotein also implicated in viral genome replication and in modulating cell signaling pathways. We describe the structure of the two proteolytically resistant domains of the N protein from infectious bronchitis virus (IBV), a prototype coronavirus. These domains are located at its N- and C-terminal ends (NTD and CTD, respectively). The NTD of the IBV Gray strain at 1.3-A resolution exhibits a U-shaped structure, with two arms rich in basic residues, providing a module for specific interaction with RNA. The CTD forms a tightly intertwined dimer with an intermolecular four-stranded central beta-sheet platform flanked by alpha helices, indicating that the basic building block for coronavirus nucleocapsid formation is a dimeric assembly of N protein. The variety of quaternary arrangements of the NTD and CTD revealed by the analysis of the different crystal forms delineates possible interfaces that could be used for the formation of a flexible filamentous ribonucleocapsid. The striking similarity between the dimeric structure of CTD and the nucleocapsid-forming domain of a distantly related arterivirus indicates a conserved mechanism of nucleocapsid formation for these two viral families.

摘要

冠状病毒可导致动物和人类出现多种呼吸道和肠道疾病,包括严重急性呼吸综合征。在这些包膜病毒中,丝状核衣壳由核衣壳(N)蛋白与单链病毒RNA结合形成。N蛋白是一种高度免疫原性的磷蛋白,也与病毒基因组复制以及调节细胞信号通路有关。我们描述了传染性支气管炎病毒(IBV,一种典型的冠状病毒)N蛋白的两个抗蛋白酶解结构域的结构。这些结构域分别位于其N端和C端(分别为NTD和CTD)。IBV Gray株的NTD在1.3埃分辨率下呈现出U形结构,有两条富含碱性残基的臂,为与RNA的特异性相互作用提供了一个模块。CTD形成一个紧密缠绕的二聚体,有一个分子间的四链中央β-折叠平台,两侧为α螺旋,这表明冠状病毒核衣壳形成的基本构建单元是N蛋白的二聚体组装。通过对不同晶体形式的分析揭示的NTD和CTD的多种四级排列描绘了可能用于形成柔性丝状核糖核衣壳的界面。CTD的二聚体结构与远亲动脉炎病毒的核衣壳形成结构域之间的显著相似性表明这两个病毒家族的核衣壳形成机制是保守的。

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