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通过体外筛选对人1型T细胞白血病病毒Rex结合元件进行高分辨率图谱绘制。

High-resolution mapping of the human T-cell leukemia virus type 1 Rex-binding element by in vitro selection.

作者信息

Baskerville S, Zapp M, Ellington A D

机构信息

Department of Chemistry and Microbiology, Indiana University, Bloomington 47405, USA.

出版信息

J Virol. 1995 Dec;69(12):7559-69. doi: 10.1128/JVI.69.12.7559-7569.1995.

Abstract

Interactions between the Rex protein of HTLV-1 and the genomic Rex-binding element (XBE) mediate the cytoplasmic transport of viral mRNAs. However, it is uncertain which RNA sequences and structures contribute to Rex recognition. A portion of the viral genome that spanned the XBE was partially randomized, and functional Rex-binding variants were selected. Alignment of selected Rex-binding sequences revealed positions that were functionally conserved between different molecules. A model is presented in which a subset of the selected residues are in direct contact with Rex. Positions that covaried with one another were also found. These covariations support a secondary-structural model in which a central paired stem is symmetrically flanked by two bulge loops. On the basis of this model, site-directed mutations of the XBE were constructed and each half molecule was found to bind independently to Rex. The functional residues and secondary structures in the XBE half molecules bear a remarkable resemblance to the transactivation response region element of HIV-1. Since the transactivation response region element is known to interact specifically with arginine residues in the Tat protein, these results suggest that the XBE binds to the arginine-rich RNA-binding domain of Rex in a similar manner. This model is supported by the selection data.

摘要

人类嗜T淋巴细胞病毒1型(HTLV-1)的Rex蛋白与基因组Rex结合元件(XBE)之间的相互作用介导了病毒mRNA的细胞质运输。然而,尚不清楚哪些RNA序列和结构有助于Rex识别。跨越XBE的病毒基因组部分被部分随机化,并筛选出功能性Rex结合变体。对所选Rex结合序列的比对揭示了不同分子之间功能保守的位置。本文提出了一个模型,其中所选残基的一个子集与Rex直接接触。还发现了相互协变的位置。这些协变支持了一种二级结构模型,其中中央配对茎两侧对称地有两个凸起环。基于该模型,构建了XBE的定点突变体,发现每个半分子都能独立与Rex结合。XBE半分子中的功能残基和二级结构与HIV-1的反式激活应答区元件有显著相似性。由于已知反式激活应答区元件与Tat蛋白中的精氨酸残基特异性相互作用,这些结果表明XBE以类似方式与Rex富含精氨酸的RNA结合结构域结合。该模型得到了筛选数据的支持。

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