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Assembly of a functional Machupo virus polymerase complex

机译:功能性马丘波病毒聚合酶复合物的组装

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Segmented negative-sense viruses of the family Arenaviridae encode a large polymerase (L) protein that contains all of the enzymatic activities required for RNA synthesis. These activities include an RNA-dependent RNA polymerase (RdRP) and an RNA endonu-clease that cleaves capped primers from cellular mRNAs to prime transcription. Using purified catalytically active Machupo virus L, we provide a view of the overall architecture of this multifunctional polymerase and reconstitute complex formation with an RNA template in vitro. The L protein contains a central ring domain that is similar in appearance to the RdRP of dsRNA viruses and multiple accessory appendages that may be responsible for 5' cap formation. RNA template recognition by L requires a sequence-specific motif located at positions 2-5 in the 3' terminus of the viral genome. Moreover, L-RNA complex formation depends on single-stranded RNA, indicating that inter-termini dsRNA interactions must be partially broken for complex assembly to occur. Our results provide a model for arenavirus polymerase-template interactions and reveal the structural organization of a negative-strand RNA virus L protein.
机译:沙眼病毒科的分段负义病毒编码一种大型聚合酶(L)蛋白,该蛋白包含RNA合成所需的所有酶促活性。这些活动包括RNA依赖性RNA聚合酶(RdRP)和RNA内切核酸酶,该酶可将带帽引物从细胞mRNA切割为转录。使用纯化的具有催化活性的马丘波病毒L,我们提供了这种多功能聚合酶的总体结构,并在体外用RNA模板重构了复合物的形成。 L蛋白包含一个中央环结构域,该结构域的外观与dsRNA病毒的RdRP相似,并且具有多个可能引起5'帽形成的附件。通过L识别RNA模板需要在病毒基因组3'末端的2-5位置上有一个序列特异性基序。此外,L-RNA复合物的形成取决于单链RNA,这表明末端dsRNA间的相互作用必须部分破坏才能发生复杂的组装。我们的结果提供了一种用于沙粒病毒聚合酶-模板相互作用的模型,并揭示了负链RNA病毒L蛋白的结构组织。

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