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黄瓜花叶病毒3a蛋白的C末端33个氨基酸影响病毒运动、RNA结合以及对感染和翻译的抑制。

The C-terminal 33 amino acids of the cucumber mosaic virus 3a protein affect virus movement, RNA binding and inhibition of infection and translation.

作者信息

Kim Sang Hyon, Kalinina Natalia O, Andreev Igor, Ryabov Eugene V, Fitzgerald Alexander G, Taliansky Michael E, Palukaitis Peter

机构信息

Scottish Crop Research Institute, Invergowrie, Dundee DD2 5DA, UK.

A.N. Belozersky Institute of Physico-chemical Biology, Moscow State University, Moscow 119899, Russia.

出版信息

J Gen Virol. 2004 Jan;85(Pt 1):221-230. doi: 10.1099/vir.0.19583-0.

Abstract

The capsid protein (CP) of Cucumber mosaic virus (CMV) is required for cell-to-cell movement, mediated by the 3a movement protein (MP). Deletion of the C-terminal 33 amino acids of the CMV 3a MP (in the mutant designated 3aDeltaC33 MP) resulted in CP-independent cell-to-cell movement, but not long-distance movement. RNA-binding studies done in vitro using isolated bacterially expressed MP showed that the 3aDeltaC33 MP bound RNA more strongly, with fewer regions sensitive to RNase and formed cooperatively bound complexes at lower ratios of protein : RNA than the wild-type (wt) 3a MP. Analysis of the architecture of the complexes by atomic force microscopy showed that the wt 3a MP formed a single type of complex with RNA, resembling beads on a string. By contrast, the 3aDeltaC33 MP formed several types of complexes, including complexes with virtually no MP bound or thicker layers of MP bound to the RNA. Assays showed that protein-RNA complexes containing high levels of either MP inhibited the infectivity and in vitro translatability of viral RNAs. The 3aDeltaC33 MP inhibited these processes at lower ratios of protein : RNA than the wt 3a MP, consistent with its stronger binding properties. The apparent contradiction between these inhibition data and the CP-independent cell-to-cell movement of CMV expressing the 3aDeltaC33 MP is discussed.

摘要

黄瓜花叶病毒(CMV)的衣壳蛋白(CP)是由3a运动蛋白(MP)介导的细胞间运动所必需的。删除CMV 3a MP的C末端33个氨基酸(在突变体3aDeltaC33 MP中)导致了不依赖CP的细胞间运动,但不是长距离运动。使用分离的细菌表达的MP进行的体外RNA结合研究表明,与野生型(wt)3a MP相比,3aDeltaC33 MP与RNA的结合更强,对RNase敏感的区域更少,并且在更低的蛋白质:RNA比例下形成协同结合的复合物。通过原子力显微镜对复合物结构的分析表明,wt 3a MP与RNA形成单一类型的复合物,类似于串珠。相比之下,3aDeltaC33 MP形成了几种类型的复合物,包括几乎没有MP结合的复合物或与RNA结合的较厚MP层。试验表明,含有高水平任一MP的蛋白质-RNA复合物会抑制病毒RNA的感染性和体外翻译能力。与wt 3a MP相比,3aDeltaC33 MP在更低的蛋白质:RNA比例下抑制这些过程,这与其更强的结合特性一致。讨论了这些抑制数据与表达3aDeltaC33 MP的CMV不依赖CP的细胞间运动之间明显的矛盾。

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