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细胞蛋白与丙型肝炎病毒RNA基因组3'非翻译区的聚(U)序列结合。

Cellular proteins bind to the poly(U) tract of the 3' untranslated region of hepatitis C virus RNA genome.

作者信息

Luo G

机构信息

Department of Virology, Bristol-Myers Squibb Pharmaceutical Research Institute, 5 Research Parkway, Wallingford, Connecticut 06492, USA.

出版信息

Virology. 1999 Mar 30;256(1):105-18. doi: 10.1006/viro.1999.9639.

Abstract

UV cross-linking analyses were performed in an attempt to determine cellular protein-viral RNA interactions with the 3' untranslated region (3' UTR) of the hepatitis C virus RNA genome. Two cellular proteins, with estimated molecular masses of 58 kDa (p58) and 35 kDa (p35), respectively, were found to specifically bind to the 3' UTR. The p58 protein was determined to be the polypyrimidine tract-binding protein. In addition to binding to the conserved 98 nucleotides (nt) of the 3' UTR, p58 also binds to the poly(U) tract of the 3' UTR. The p35 protein was found to interact only with the poly(U) tract of the 3' UTR. These conclusions are supported by the following findings: (1) p58, and not p35, binds to the 3' end conserved 98 nt, (2) both p58 and p35 bind to a 3' UTR RNA with a deletion of the conserved 98 nt, (3) the 98-nt deletion mutant 3' UTR competed out both p58 and p35 binding, (4) a poly(U) homopolymer competed out both p58 and p35 binding, (5) a 3' UTR RNA with deletion of the poly(U) tract competed out only p58 binding but not p35 binding, and (6) an RNA containing the variable region of the 3' UTR with a deletion of both poly(U) tract and 98 nt failed to compete for binding of either p58 or p35. Interaction of these cellular proteins with the HCV 3' UTR is probably involved in regulation of translation and/or replication of the HCV RNA genome.

摘要

进行紫外线交联分析,以确定细胞蛋白与丙型肝炎病毒RNA基因组3'非翻译区(3'UTR)之间的相互作用。发现两种细胞蛋白分别与3'UTR特异性结合,其估计分子量分别为58 kDa(p58)和35 kDa(p35)。确定p58蛋白为多嘧啶序列结合蛋白。除了与3'UTR保守的98个核苷酸(nt)结合外,p58还与3'UTR的聚尿苷序列结合。发现p35蛋白仅与3'UTR的聚尿苷序列相互作用。这些结论得到以下发现的支持:(1)p58而非p35与3'端保守的98个nt结合;(2)p58和p35都与缺失保守98个nt的3'UTR RNA结合;(3)98个nt缺失的突变体3'UTR竞争抑制p58和p35的结合;(4)聚尿苷同聚物竞争抑制p58和p35的结合;(5)缺失聚尿苷序列的3'UTR RNA仅竞争抑制p58的结合,而不竞争抑制p35的结合;(6)含有3'UTR可变区且缺失聚尿苷序列和98个nt的RNA不能竞争p58或p35的结合。这些细胞蛋白与HCV 3'UTR的相互作用可能参与了HCV RNA基因组翻译和/或复制的调控。

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