Interplay Among Constitutes of Ebola Virus: Nucleoprotein, Polymerase L, Viral Proteins

Minchuan Zhang, Peiming He, Jing Su, D. T. Singh, Hailei Su, Haibin Su
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Abstract

Ebola virus is a highly lethal filovirus, claimed thousands of people in its recent outbreak. Seven viral proteins constitute ebola viral structure, and four of them (nucleoprotein (NP), polymerase L, VP35 and VP30) participate majorly in viral replication and transcription. We have elucidated a conformation change of NP cleft by VP35 NP-binding protein domains through superimposing two experimental NP structure images and discussed the function of this conformation change in the replication and transcription with polymerase complex (L, VP35 and VP30). The important roles of VP30 in viral RNA synthesis have also been discussed. A “tapping” model has been proposed in this paper for a better understanding of the interplay among the four viral proteins (NP, polymerase L, VP35 and VP30). Moreover, we have pinpointed some key residue changes on NP (both NP N- and C-terminal) and L between Reston and Zaire by computational studies. Together, this paper provides a description of interactions among ebola viral proteins (NP, L, VP35, VP30 and VP40) in viral replication and transcription, and sheds light on the complex system of viral reproduction.
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埃博拉病毒各组成部分之间的相互作用:核蛋白、聚合酶L、病毒蛋白
埃博拉病毒是一种高度致命的丝状病毒,在最近的疫情中夺走了数千人的生命。七种病毒蛋白构成埃博拉病毒结构,其中四种(核蛋白(NP)、聚合酶L、VP35和VP30)主要参与病毒复制和转录。我们通过叠加两个实验NP结构图像,阐明了VP35 NP结合蛋白结构域对NP裂的构象变化,并讨论了这种构象变化在聚合酶复合物(L、VP35和VP30)复制和转录中的作用。还讨论了VP30在病毒RNA合成中的重要作用。为了更好地理解四种病毒蛋白(NP、聚合酶L、VP35和VP30)之间的相互作用,本文提出了一个“窃听”模型。此外,我们还通过计算研究精确定位了Reston和Zaire之间NP(包括NP的N-和C-末端)和L上的一些关键残基变化。本文共同描述了埃博拉病毒蛋白(NP、L、VP35、VP30和VP40)在病毒复制和转录中的相互作用,并揭示了病毒繁殖的复杂系统。
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