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释放腮腺炎病毒核衣壳中封存的基因组RNA。

Releasing the Genomic RNA Sequestered in the Mumps Virus Nucleocapsid.

作者信息

Severin Chelsea, Terrell James R, Zengel James R, Cox Robert, Plemper Richard K, He Biao, Luo Ming

机构信息

Department of Chemistry, Georgia State University, Atlanta, Georgia, USA.

Department of Infectious Diseases, College of Veterinary Medicine, University of Georgia, Athens, Georgia, USA.

出版信息

J Virol. 2016 Oct 28;90(22):10113-10119. doi: 10.1128/JVI.01422-16. Print 2016 Nov 15.

Abstract

In a negative-strand RNA virus, the genomic RNA is sequestered inside the nucleocapsid when the viral RNA-dependent RNA polymerase uses it as the template for viral RNA synthesis. It must require a conformational change in the nucleocapsid protein (N) to make the RNA accessible to the viral polymerase during this process. The structure of an empty mumps virus (MuV) nucleocapsid-like particle was determined to 10.4-Å resolution by cryo-electron microscopy (cryo-EM) image reconstruction. By modeling the crystal structure of parainfluenza virus 5 into the density, it was shown that the α-helix close to the RNA became flexible when RNA was removed. Point mutations in this helix resulted in loss of polymerase activities. Since the core of N is rigid in the nucleocapsid, we suggest that interactions between this region of the mumps virus N and its polymerase, instead of large N domain rotations, lead to exposure of the sequestered genomic RNA. Mumps virus (MuV) infection may cause serious diseases, including hearing loss, orchitis, oophoritis, mastitis, and pancreatitis. MuV is a negative-strand RNA virus, similar to rabies virus or Ebola virus, that has a unique mechanism of viral RNA synthesis. They all make their own RNA-dependent RNA polymerase (RdRp). The viral RdRp uses the genomic RNA inside the viral nucleocapsid as the template to synthesize viral RNAs. Since the template RNA is always sequestered in the nucleocapsid, the viral RdRp must find a way to open it up in order to gain access to the covered template. Our work reported here shows that a helix structural element in the MuV nucleocapsid protein becomes open when the sequestered RNA is released. The amino acids related to this helix are required for RdRp to synthesize viral RNA. We propose that the viral RdRp pulls this helix open to release the genomic RNA.

摘要

在负链RNA病毒中,当病毒RNA依赖的RNA聚合酶将基因组RNA用作病毒RNA合成的模板时,基因组RNA被隔离在核衣壳内部。在此过程中,病毒聚合酶要使用该RNA,核衣壳蛋白(N)必须发生构象变化以使RNA可及。通过冷冻电子显微镜(cryo-EM)图像重建,确定了空的腮腺炎病毒(MuV)核衣壳样颗粒的结构,分辨率达到10.4埃。通过将副流感病毒5的晶体结构模型化到密度图中,结果表明当RNA被去除时,靠近RNA的α螺旋变得灵活。该螺旋中的点突变导致聚合酶活性丧失。由于N的核心在核衣壳中是刚性的,我们认为腮腺炎病毒N的该区域与其聚合酶之间的相互作用,而非N结构域的大幅旋转,导致了被隔离的基因组RNA的暴露。腮腺炎病毒(MuV)感染可能会引发严重疾病,包括听力丧失、睾丸炎、卵巢炎、乳腺炎和胰腺炎。MuV是一种负链RNA病毒,类似于狂犬病病毒或埃博拉病毒,具有独特的病毒RNA合成机制。它们都能产生自身的RNA依赖的RNA聚合酶(RdRp)。病毒RdRp利用病毒核衣壳内的基因组RNA作为模板来合成病毒RNA。由于模板RNA总是被隔离在核衣壳中,病毒RdRp必须找到打开它的方法,以便获取被覆盖的模板。我们在此报告的工作表明,当被隔离的RNA释放时,MuV核衣壳蛋白中的一个螺旋结构元件会打开。RdRp合成病毒RNA需要与该螺旋相关的氨基酸。我们提出,病毒RdRp拉开这个螺旋以释放基因组RNA。

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