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病毒3'非翻译RNA假结内的一个系统发育保守序列调控翻译。

A phylogenetically conserved sequence within viral 3' untranslated RNA pseudoknots regulates translation.

作者信息

Leathers V, Tanguay R, Kobayashi M, Gallie D R

机构信息

Department of Biochemistry, University of California, Riverside 92521-0129.

出版信息

Mol Cell Biol. 1993 Sep;13(9):5331-47. doi: 10.1128/mcb.13.9.5331-5347.1993.

Abstract

Both the 68-base 5' leader (omega) and the 205-base 3' untranslated region (UTR) of tobacco mosaic virus (TMV) promote efficient translation. A 35-base region within omega is necessary and sufficient for the regulation. Within the 3' UTR, a 52-base region, composed of two RNA pseudoknots, is required for regulation. These pseudoknots are phylogenetically conserved among seven viruses from two different viral groups and one satellite virus. The pseudoknots contained significant conservation at the secondary and tertiary levels and at several positions at the primary sequence level. Mutational analysis of the sequences determined that the primary sequence in several conserved positions, particularly within the third pseudoknot, was essential for function. The higher-order structure of the pseudoknots was also required. Both the leader and the pseudoknot region were specifically recognized by, and competed for, the same proteins in extracts made from carrot cell suspension cells and wheat germ. Binding of the proteins is much stronger to omega than the pseudoknot region. Synergism was observed between the TMV 3' UTR and the cap and to a lesser extent between omega and the 3' UTR. The functional synergism and the protein binding data suggest that the cap, TMV 5' leader, and 3' UTR interact to establish an efficient level of translation.

摘要

烟草花叶病毒(TMV)的68个碱基的5'前导序列(ω)和205个碱基的3'非翻译区(UTR)均能促进高效翻译。ω内一个35个碱基的区域对这种调控是必要且充分的。在3'UTR内,一个由两个RNA假结组成的52个碱基的区域是调控所必需的。这些假结在来自两个不同病毒组的七种病毒和一种卫星病毒中在系统发育上是保守的。这些假结在二级和三级水平以及一级序列的几个位置上都有显著的保守性。对这些序列的突变分析确定,几个保守位置的一级序列,特别是在第三个假结内,对功能至关重要。假结的高阶结构也是必需的。在胡萝卜细胞悬浮液和小麦胚芽制备的提取物中,前导序列和假结区域都能被相同的蛋白质特异性识别并与之竞争。蛋白质与ω的结合比对假结区域的结合要强得多。在TMV 3'UTR与帽结构之间观察到协同作用,在ω与3'UTR之间协同作用较弱。功能协同作用和蛋白质结合数据表明,帽结构、TMV 5'前导序列和3'UTR相互作用以建立高效的翻译水平。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/01d4/360232/3a84c8d98200/molcellb00021-0220-a.jpg

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