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本文引用的文献

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The involvement of a spliceosome component in internal initiation of human rhinovirus RNA translation.剪接体成分参与人鼻病毒RNA翻译的内部起始过程。
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A cytoplasmic 57-kDa protein that is required for translation of picornavirus RNA by internal ribosomal entry is identical to the nuclear pyrimidine tract-binding protein.一种通过内部核糖体进入进行微小核糖核酸病毒RNA翻译所必需的57千道尔顿细胞质蛋白,与核嘧啶序列结合蛋白相同。
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The cellular polypeptide p57 (pyrimidine tract-binding protein) binds to multiple sites in the poliovirus 5' nontranslated region.细胞多肽p57(嘧啶序列结合蛋白)与脊髓灰质炎病毒5'非翻译区的多个位点结合。
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Purified lupus antigen La recognizes an oligouridylate stretch common to the 3' termini of RNA polymerase III transcripts.纯化的狼疮抗原La识别RNA聚合酶III转录本3'末端共有的一段寡聚尿苷酸序列。
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细胞蛋白与鼻病毒14型RNA 5'非翻译区内富含多聚嘧啶的线性序列结合。

Cell proteins bind to a linear polypyrimidine-rich sequence within the 5'-untranslated region of rhinovirus 14 RNA.

作者信息

Rojas-Eisenring I A, Cajero-Juarez M, del Angel R M

机构信息

Departamento de Patología Experimental, Instituto Politécnico Nacional, Mexico City, Mexico.

出版信息

J Virol. 1995 Nov;69(11):6819-24. doi: 10.1128/JVI.69.11.6819-6824.1995.

DOI:10.1128/JVI.69.11.6819-6824.1995
PMID:7474094
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC189594/
Abstract

Members of the picornavirus family initiate translation of their RNA genomes by a cap-independent mechanism in which ribosomes bind to an internal site in the 5' untranslated region (5'-UTR). This unique process requires an internal ribosome entry site (IRES), a highly structured RNA whose function is mediated in part by interactions with cell proteins. The IRES element of human rhinovirus 2 (HRV-2) extends from nucleotide (nt) 10 to between nt 544 and 568 and has been shown to interact with two cell proteins, pyrimidine tract-binding protein (pPTB) and p97. To map the specific regions of HRV-14 RNA that bind cell proteins, mobility shift, UV cross-linking and Western immunoblot analyses were performed. The results indicate that an RNA sequence from nt 538 to 591 interacts with pPTB and La, two proteins previously shown to functionally interact with the IRES elements of several picornaviruses. Two additional proteins, p97 and p68, were also cross-linked to nt 538 to 591 RNA. These four proteins interact with a putatively unstructured portion of the 5'-UTR that contains a polypyrimidine tract and has been shown to be present at the 3' border of sequences that are essential for IRES function of HRV-2. These protein-RNA interactions are likely to play a role in internal initiation of translation.

摘要

微小核糖核酸病毒科成员通过一种不依赖帽结构的机制起始其RNA基因组的翻译,在这种机制中,核糖体与5'非翻译区(5'-UTR)的一个内部位点结合。这一独特过程需要一个内部核糖体进入位点(IRES),即一种高度结构化的RNA,其功能部分由与细胞蛋白的相互作用介导。人鼻病毒2型(HRV-2)的IRES元件从核苷酸(nt)10延伸至nt 544与568之间,并且已显示与两种细胞蛋白,即嘧啶区结合蛋白(pPTB)和p97相互作用。为了绘制与细胞蛋白结合的HRV-14 RNA的特定区域,进行了迁移率变动、紫外线交联和蛋白质免疫印迹分析。结果表明,从nt 538到591的RNA序列与pPTB和La相互作用,这两种蛋白先前已显示在功能上与几种微小核糖核酸病毒的IRES元件相互作用。另外两种蛋白,p97和p68,也与nt 538到591的RNA发生交联。这四种蛋白与5'-UTR的一个推测为非结构化的部分相互作用,该部分含有一个多嘧啶区,并且已显示存在于对HRV-2的IRES功能至关重要的序列的3'边界处。这些蛋白-RNA相互作用可能在翻译的内部起始中发挥作用。