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苜蓿花叶病毒中特定RNA-外壳蛋白肽相互作用的RNA决定因素:等轴不稳环斑病毒RNAs中同源特征的保守性

RNA determinants of a specific RNA-coat protein peptide interaction in alfalfa mosaic virus: conservation of homologous features in ilarvirus RNAs.

作者信息

Ansel-McKinney P, Gehrke L

机构信息

Department of Microbiology and Molecular Genetics, Harvard Medical School, Boston, MA 02115, USA.

出版信息

J Mol Biol. 1998 May 15;278(4):767-85. doi: 10.1006/jmbi.1998.1656.

Abstract

Alfalfa mosaic virus (AMV) coat protein and tobacco streak virus (TSV) coat protein bind specifically to the 3' untranslated regions of the viral RNAs and are required with the genomic RNAs to initiate virus replication. A combination of nucleotide substitutions, hydroxyl radical footprinting, and ethylation and chemical modification interference analysis has been used to define the RNA determinants important for the specific binding of the 3'-terminal 39 nucleotides of AMV RNA 3/4 (AMV843-881) to an amino-terminal coat protein peptide (CP26). The results demonstrate that potential phosphate and base-specific contacts as well as ribose moieties protected upon peptide binding cluster in lower hairpin stems and flanking AUGC sequences of the viral RNA, without direct involvement of loop nucleotides. Nucleotides identified in the modification-interference analyses as important for RNA-protein interactions are highly conserved among AMV and the ilarvirus RNAs. This RNA sequence homology, coupled with the recent identification of an RNA binding consensus sequence for AMV and ilarvirus coat proteins, provides a framework for understanding the functional equivalence of AMV and TSV coat proteins in binding RNA and activating virus replication and may explain why heterologous AMV and ilarvirus coat protein-RNA mixtures are infectious.

摘要

苜蓿花叶病毒(AMV)外壳蛋白和烟草线条病毒(TSV)外壳蛋白特异性结合病毒RNA的3'非翻译区,并且与基因组RNA一起启动病毒复制。通过核苷酸取代、羟自由基足迹分析以及乙基化和化学修饰干扰分析相结合的方法,已确定了对于AMV RNA 3/4(AMV843 - 881)的3'末端39个核苷酸与氨基末端外壳蛋白肽(CP26)特异性结合重要的RNA决定簇。结果表明,潜在的磷酸和碱基特异性接触以及肽结合后受到保护的核糖部分聚集在病毒RNA的下部发夹茎和侧翼AUGC序列中,而环核苷酸没有直接参与。在修饰干扰分析中确定的对RNA - 蛋白质相互作用重要的核苷酸在AMV和等轴不稳环斑病毒RNA中高度保守。这种RNA序列同源性,再加上最近鉴定出的AMV和等轴不稳环斑病毒外壳蛋白的RNA结合共有序列,为理解AMV和TSV外壳蛋白在结合RNA和激活病毒复制方面的功能等效性提供了框架,并可能解释为什么异源AMV和等轴不稳环斑病毒外壳蛋白 - RNA混合物具有感染性。

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