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Elucidating the Interacting Domains of Chandipura Virus Nucleocapsid Protein

机译:阐明昌迪普拉病毒核壳蛋白的相互作用域

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摘要

The nucleocapsid (N) protein of Chandipura virus (CHPV) plays a crucial role in viral life cycle, besides being an important structural component of the virion through proper organization of its interactions with other viral proteins. In a recent study, the authors had mapped the associations among CHPV proteins and shown that N protein interacts with four of the viral proteins: N, phosphoprotein (P), matrix protein (M), and glycoprotein (G). The present study aimed to distinguish the regions of CHPV N protein responsible for its interactions with other viral proteins. In this direction, we have generated the structure of CHPV N protein by homology modeling using SWISS-MODEL workspace and Accelrys Discovery Studio client 2.55 and mapped the domains of N protein using PiSQRD. The interactions of N protein fragments with other proteins were determined by ZDOCK rigid-body docking method and validated by yeast two-hybrid and ELISA. The study revealed a unique binding site, comprising of amino acids 1–30 at the N terminus of the nucleocapsid protein (N1) that is instrumental in its interactions with N, P, M, and G proteins. It was also observed that N2 associates with N and G proteins while N3 interacts with N, P, and M proteins.
机译:Chandipura病毒(CHPV)的核衣壳(N)蛋白在病毒的生命周期中起着至关重要的作用,此外它还通过适当地组织与其他病毒蛋白的相互作用而成为病毒体的重要结构组成部分。在最近的研究中,作者绘制了CHPV蛋白之间的关联关系,并显示N蛋白与四种病毒蛋白相互作用:N,磷蛋白(P),基质蛋白(M)和糖蛋白(G)。本研究旨在区分CHPV N蛋白与其他病毒蛋白相互作用的区域。在这个方向上,我们已经通过使用SWISS-MODEL工作区和Accelrys Discovery Studio客户端2.55进行同源建模,生成了CHPV N蛋白的结构,并使用PiSQRD绘制了N蛋白的结构域。通过ZDOCK刚体对接方法确定N蛋白片段与其他蛋白的相互作用,并通过酵母双杂交和ELISA验证。这项研究揭示了一个独特的结合位点,该位点在核衣壳蛋白(N1)的N端包含1至30个氨基酸,这有助于其与N,P,M和G蛋白相互作用。还观察到N2与N和G蛋白缔合,而N3与N,P和M蛋白相互作用。

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