首页> 美国卫生研究院文献>Journal of Virology >Juxtaposition between activation and basic domains of human immunodeficiency virus type 1 Tat is required for optimal interactions between Tat and TAR.
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Juxtaposition between activation and basic domains of human immunodeficiency virus type 1 Tat is required for optimal interactions between Tat and TAR.

机译:Tat和TAR之间的最佳相互作用需要在1型人类免疫缺陷病毒Tat的激活域和基本域之间并置。

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摘要

trans activation of the human immunodeficiency virus type 1 long terminal repeat requires that the viral trans activator Tat interact with the trans-acting responsive region (TAR) RNA. Although the N-terminal 47 amino acids represent an independent activation domain that functions via heterologous nucleic acid-binding proteins, sequences of Tat that are required for interactions between Tat and TAR in cells have not been defined. Although in vitro binding studies suggested that the nine basic amino acids from positions 48 to 57 in Tat bind efficiently to the 5' bulge in the TAR RNA stem-loop, by creating several mutants of Tat and new hybrid proteins between Tat and the coat protein of bacteriophage R17, we determined that this arginine-rich domain is not sufficient for interactions between Tat and TAR in vivo. Rather, the activation domain is also required and must be juxtaposed to the basic domain. Thus, in vitro TAR RNA binding does not translate to function in vivo, which suggests that other proteins are important for specific and productive interactions between Tat and TAR.
机译:人类免疫缺陷病毒1型长末端重复序列的反式激活需要病毒反式激活因子Tat与反式反应区(TAR)RNA相互作用。尽管N末端的47个氨基酸代表通过异源核酸结合蛋白起作用的独立的激活结构域,但是尚未定义细胞中Tat和TAR之间相互作用所需的Tat序列。尽管体外结合研究表明,Tat中第48-57位的9个碱性氨基酸可通过在Tat和外壳蛋白之间产生多个Tat突变体和新的杂合蛋白,与TAR RNA茎环的5'凸起有效结合。对于噬菌体R17,我们确定该富含精氨酸的结构域不足以实现Tat和TAR在体内的相互作用。而是,激活域也是必需的,并且必须与基本域并置。因此,体外TAR RNA结合不能转化为体内功能,这表明其他蛋白质对于Tat与TAR之间的特异性和生产性相互作用也很重要。

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