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Conformations of the monomeric hepatitis C virus RNA-dependent RNA polymerase

机译:单体丙型肝炎病毒RNA依赖性RNA聚合酶的构象

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The hepatitis C virus (HCV) RNA-dependent RNA polymerase (RdRp) changes its conformation and oligomerization state in association with the steps in RNA synthesis. Using a human right hand as an analogy, the crystal structure of the HCV RdRp has extensive interactions between the “finger” and “thumb” domains which result in a closed conformation. However, the RdRp must form a partially open conformation to accommodate the nascent and template RNA duplex during RNA synthesis, and to interact with the retinoblastoma protein through residues in the “palm” domain. A motif named the Δ1 loop has been previously proposed to regulate the transition from the closed to the open conformation. We used negative-stain electron microscopy and single particle reconstruction to identify several conformations of the HCV RdRp monomer, from closed to open. An RdRp with five amino acids deleted in the tip of the Δ1 loop resulted in an open conformation, confirming the importance of this loop in regulating RdRp conformations. Bioinformatics analysis of HCV strains focusing on the Δ1 loop and its interacting surfaces further defined the requirements for this gating mechanism in the HCV RdRp. These results provide glimpses into the dynamic conformations of the HCV RdRp and should provide insights into alternative conformations of the HCV polymerase that could serve as targets for antiviral development against HCV.
机译:丙型肝炎病毒(HCV)RNA依赖性RNA聚合酶(RdRp)与RNA合成步骤相关联地改变其构象和寡聚状态。以人类右手为类比,HCV RdRp的晶体结构在“手指”和“拇指”结构域之间具有广泛的相互作用,从而导致闭合构象。但是,RdRp必须形成部分开放的构象,以适应RNA合成过程中新生的RNA和模板RNA双链体,并通过“棕榈”结构域中的残基与成视网膜细胞瘤蛋白相互作用。先前已经提出了称为Δ1环的基序,以调节从闭合构象到开放构象的转变。我们使用负染色电子显微镜和单颗粒重建技术来鉴定HCV RdRp单体从封闭到开放的几种构型。 Δ1环末端缺失5个氨基酸的RdRp导致一个开放的构象,证实了该环在调节RdRp构象中的重要性。专注于Δ1环及其相互作用表面的HCV菌株的生物信息学分析进一步确定了HCV RdRp对这种门控机制的要求。这些结果使人对HCV RdRp的动态构象有所了解,并应提供对HCV聚合酶替代构象的见解,该构象可以作为抗HCV的抗病毒药物的靶标。

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