人副流感病毒 2 型 L 蛋白与其他病毒蛋白相互作用和 mRNA 加帽所需的区域。
Human parainfluenza virus type 2 L protein regions required for interaction with other viral proteins and mRNA capping.
机构信息
Department of Microbiology, Mie University Graduate School of Medicine, 2-174, Edobashi, Tsu, Mie 514-8507, Japan.
出版信息
J Virol. 2011 Jan;85(2):725-32. doi: 10.1128/JVI.01226-10. Epub 2010 Nov 10.
Abstract
The large RNA polymerase (L) protein of human parainfluenza virus type 2 (hPIV2) binds the nucleocapsid, phosphoprotein, and V protein, as well as itself, and these interactions are essential for transcription and replication of the viral RNA genome. Although all of these interactions were found to be mediated through the domains within the N terminus of L, the C terminus of the L protein was also required for minigenome reporter gene expression. We have identified a highly conserved rubulavirus domain near the C terminus of the L protein that is required for mRNA synthesis but not for genome replication. Remarkably, this region of L shares homology with a conserved region of cellular capping enzymes that binds GTP and forms a lysyl-GMP enzyme intermediate, the first step in the cellular capping reaction. We propose that this conserved region of L also binds GTP (or GDP) to carry out the second step of the unconventional nonsegmented negative-strand virus capping reaction.
摘要
人副流感病毒 2 型(hPIV2)的大 RNA 聚合酶(L)蛋白与核衣壳、磷蛋白和 V 蛋白结合,以及与自身结合,这些相互作用对于病毒 RNA 基因组的转录和复制是必不可少的。尽管所有这些相互作用都被发现是通过 L 蛋白 N 端的结构域介导的,但 L 蛋白的 C 端对于小基因报告基因的表达也是必需的。我们已经确定了 L 蛋白 C 端附近的一个高度保守的 rubulavirus 结构域,该结构域对于 mRNA 合成而不是基因组复制是必需的。值得注意的是,L 蛋白的这一区域与细胞加帽酶的保守区域具有同源性,后者结合 GTP 并形成赖氨酸-GMP 酶中间产物,这是细胞加帽反应的第一步。我们提出,L 的这一保守区域也结合 GTP(或 GDP)以执行非常规的非节段负链病毒加帽反应的第二步。
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