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首页> 外文期刊>Virus Research: An International Journal of Molecular and Cellular Virology >Characterization of the caprine arthritis encephalitis virus (CAEV) rev N-terminal elements required for efficient interaction with the RRE.
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Characterization of the caprine arthritis encephalitis virus (CAEV) rev N-terminal elements required for efficient interaction with the RRE.

机译:有效与RRE相互作用所需的山羊关节炎脑炎病毒(CAEV)rev N末端元件的表征。

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The Caprine Arthritis Encephalitis Virus (CAEV) genome encodes three structural (gag, pol, and env) and three accessory (rev, tat, and vif) genes. The Rev-C protein regulates Gag, Pol and Env expression by transporting their mRNAs to the cytoplasm. Rev trans-activation requires binding of Rev to an RNA structure called the Rev Response Element (RRE-C). Previous mutational analyses have shown that two domains of Rev are required for its function. The basic domain mediates RRE binding and multimer formation, and the nuclear export signal (NES) mediates trans-activation. Preliminary experiments demonstrate that Rev-C N-terminal deletion mutants bind the RRE less avidly than does wildtype Rev. As a result, it was hypothesized that an additional domain located in the N-terminal exon of Rev-C was required for optimal RRE binding. To test this hypothesis, Rev-C alanine scanning mutants were generated and in vitro RRE binding assays were performed. Alteration of Rev-C amino acids K13, E14, N15, V19, T20, M21 and R27 dramatically decreased affinity for RRE-C. These data demonstrate that Rev-C N-terminal amino acids are required for optimal RRE-C binding and suggest that a third functional domain exists within the N-terminus of Rev-C.
机译:山羊关节炎脑炎病毒(CAEV)基因组编码三个结构性基因(gag,pol和env)和三个辅助性基因(rev,tat和vif)。 Rev-C蛋白通过将其mRNA转运到细胞质来调节Gag,Pol和Env的表达。 Rev反式激活需要将Rev结合到称为Rev Response Element(RRE-C)的RNA结构上。先前的突变分析表明,Rev的功能需要两个域。基本域介导RRE结合和多聚体形成,核输出信号(NES)介导反式激活。初步实验表明,Rev-C N末端缺失突变体与野生型Rev结合的亲和力较小。因此,据推测,为了实现最佳RRE结合,Rev-C N末端外显子需要一个额外的结构域。为了检验该假设,产生了Rev-C丙氨酸扫描突变体,并进行了体外RRE结合测定。 Rev-C氨基酸K13,E14,N15,V19,T20,M21和R27的改变显着降低了对RRE-C的亲和力。这些数据表明,Rev-C N末端氨基酸是最佳RRE-C结合所必需的,并且表明Rev-C的N端内存在第三个功能域。

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