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Structural Insights into Bunyavirus Replication and Its Regulation by the vRNA Promoter

机译:对Bunyavirus复制及其vRNA启动子调控的结构见解

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Segmented negative-strand RNA virus (sNSV) polymerases transcribe and replicate the viral RNA (vRNA) within a ribonucleoprotein particle (RNP). We present cryo-EM and X-ray structures of, respectively, apo-and vRNA bound La Crosse orthobunyavirus (LACV) polymerase that give atomic-resolution insight into how such RNPs perform RNA synthesis. The complementary 3' and 5' vRNA extremities are sequence specifically bound in separate sites on the polymerase. The 5' end binds as a stem-loop, allosterically structuring functionally important polymerase active site loops. Identification of distinct template and product exit tunnels allows proposal of a detailed model for template-directed replication with minimal disruption to the circularised RNP. The similar overall architecture and vRNA binding of monomeric LACV to heterotrimeric influenza polymerase, despite high sequence divergence, suggests that all sNSV polymerases have a common evolutionary origin and mechanism of RNA synthesis. These results will aid development of replication inhibitors of diverse, serious human pathogenic viruses.
机译:分段负链RNA病毒(sNSV)聚合酶转录并复制核糖核蛋白颗粒(RNP)中的病毒RNA(vRNA)。我们目前分别与载脂蛋白和vRNA结合的La Crosse正宗布尼亚病毒(LACV)聚合酶的冷冻EM和X射线结构提供原子分辨率的见解,以了解这种RNPs如何执行RNA合成。互补的3'和5'vRNA末端在聚合酶的不同位点上特异性结合。 5'末端结合为茎环,变构构造功能上重要的聚合酶活性位点环。独特的模板和产品出口通道的鉴定可以为模板导向的复制提供详细的模型建议,同时对环化RNP的破坏最小。尽管序列差异很大,单体LACV与异源三聚体流感聚合酶的总体结构和vRNA结合相似,这表明所有sNSV聚合酶都具有共同的进化起源和RNA合成机制。这些结果将有助于开发多种严重人类致病病毒的复制抑制剂。

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