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Sequence-specific interaction between HIV-1 matrix protein and viral genomic RNA revealed by in vitro genetic selection.

机译:HIV-1基质蛋白和病毒基因组RNA之间的序列特异性相互作用通过体外遗传选择揭示。

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摘要

The human immunodeficiency virus type-1 matrix protein (HIV-1 MA) is a multifunctional structural protein synthesized as part of the Pr55 gag polyprotein. We have used in vitro genetic selection to identify an RNA consensus sequence that specifically interacts with MA (Kd = 5 x 10(-7) M). This 13-nt MA binding consensus sequence bears a high degree of homology (77%) to a region (nt 1433-1446) within the POL open reading frame of the HIV-1 genome (consensus sequence from 38 HIV-1 strains). Chemical interference experiments identified the nucleotides within the MA binding consensus sequence involved in direct contact with MA. We further demonstrate that this RNA-protein interaction is mediated through a stretch of basic amino acids within MA. Mutations that disrupt the interaction between MA and its RNA binding site within the HIV-1 genome resulted in a measurable decrease in viral replication.
机译:人类免疫缺陷病毒1型基质蛋白(HIV-1 MA)是作为Pr55 gag多蛋白的一部分合成的多功能结构蛋白。我们已使用体外遗传选择来鉴定与MA特异性相互作用的RNA共有序列(Kd = 5 x 10(-7)M)。该13-nt MA结合共有序列与HIV-1基因组的POL开放阅读框(来自38个HIV-1菌株的共有序列)内的区域(nt 1433-1446)具有高度同源性(77%)。化学干扰实验确定了与MA直接接触的MA结合共有序列中的核苷酸。我们进一步证明这种RNA蛋白质相互作用是通过MA内的一系列碱性氨基酸介导的。破坏MA及其在HIV-1基因组中的RNA结合位点之间相互作用的突变导致病毒复制量明显下降。

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