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FIV 衣壳 RNA 的结构分析揭示了一个潜在的结构开关,该开关可能控制病毒包装和基因组二聚化。

SHAPE analysis of the FIV Leader RNA reveals a structural switch potentially controlling viral packaging and genome dimerization.

机构信息

University of Cambridge Department of Medicine, Box 157, Level 5 Addenbrooke's Hospital, Hills Rd, Cambridge, CB20QQ, UK.

出版信息

Nucleic Acids Res. 2011 Aug;39(15):6692-704. doi: 10.1093/nar/gkr252. Epub 2011 May 5.

Abstract

Feline immunodeficiency virus (FIV) infects many species of cat, and is related to HIV, causing a similar pathology. High-throughput selective 2' hydroxyl acylation analysed by primer extension (SHAPE), a technique that allows structural interrogation at each nucleotide, was used to map the secondary structure of the FIV packaging signal RNA. Previous studies of this RNA showed four conserved stem-loops, extensive long-range interactions (LRIs) and a small, palindromic stem-loop (SL5) within the gag open reading frame (ORF) that may act as a dimerization initiation site (DIS), enabling the virus to package two copies of its genome. Our analyses of wild-type (wt) and mutant RNAs suggest that although the four conserved stem-loops are static structures, the 5' and 3' regions previously shown to form LRI also adopt an alternative, yet similarly conserved conformation, in which the putative DIS is occluded, and which may thus favour translational and splicing functions over encapsidation. SHAPE and in vitro dimerization assays were used to examine SL5 mutants. Dimerization contacts appear to be made between palindromic loop sequences in SL5. As this stem-loop is located within the gag ORF, recognition of a dimeric RNA provides a possible mechanism for the specific packaging of genomic over spliced viral RNAs.

摘要

猫免疫缺陷病毒(FIV)感染多种猫科动物,与 HIV 相关,可引起类似的病理学改变。使用高通量选择性 2' 羟基乙酰化分析引物延伸(SHAPE)技术来绘制 FIV 包装信号 RNA 的二级结构。该 RNA 的先前研究表明,在 gag 开放阅读框(ORF)内存在四个保守的茎环、广泛的长程相互作用(LRIs)和一个小的、发夹状的茎环(SL5),可能作为二聚化起始位点(DIS),使病毒能够包装其基因组的两个拷贝。我们对野生型(wt)和突变型 RNA 的分析表明,尽管四个保守的茎环是静态结构,但先前显示形成 LRI 的 5' 和 3' 区域也采用了替代的、但同样保守的构象,其中假定的 DIS 被掩盖,这可能有利于翻译和剪接功能而不是封装。使用 SHAPE 和体外二聚化测定来检查 SL5 突变体。二聚体接触似乎是在 SL5 中的发夹环序列之间形成的。由于这个茎环位于 gag ORF 内,识别二聚体 RNA 提供了一种可能的机制,用于特异性包装基因组 RNA 而不是剪接的病毒 RNA。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2654/3159445/710476570058/gkr252f1.jpg

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