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Patterns and plasticity in RNA-protein interactions enable recruitment of multiple proteins through a single site

机译:RNA-蛋白质相互作用的模式和可塑性可通过单个位点募集多种蛋白质

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摘要

mRNA control hinges on the specificity and affinity of proteins for their RNA binding sites. Regulatory proteins must bind their own sites and reject even closely related noncognate sites. In the PUF [Pumilio and fem-3 binding factor (FBF)] family of RNA binding proteins, individual proteins discriminate differences in the length and sequence of binding sites, allowing each PUF to bind a distinct battery of mRNAs. Here, we show that despite these differences, the pattern of RNA interactions is conserved among PUF proteins: the two ends of the PUF protein make critical contacts with the two ends of the RNA sites. Despite this conserved “two-handed” pattern of recognition, the RNA sequence is flexible. Among the binding sites of yeast Puf4p, RNA sequence dictates the pattern in which RNA bases are flipped away from the binding surface of the protein. Small differences in RNA sequence allow new modes of control, recruiting Puf5p in addition to Puf4p to a single site. This embedded information adds a new layer of biological meaning to the connections between RNA targets and PUF proteins.
机译:mRNA控制取决于蛋白质对其RNA结合位点的特异性和亲和力。调节蛋白必须结合自己的位点,甚至排斥紧密相关的非同源位点。在RNA结合蛋白的PUF [Pumilio和fem-3结合因子(FBF)]家族中,单个蛋白区分结合位点的长度和序列的差异,从而使每个PUF都能结合不同的电池mRNA。在这里,我们显示,尽管存在这些差异,但PUF蛋白之间的RNA相互作用模式却是保守的:PUF蛋白的两端与RNA位点的两端形成关键接触。尽管这种保守的“双手”识别模式,RNA序列还是灵活的。在酵母Puf4p的结合位点中,RNA序列决定了RNA碱基从蛋白质结合表面翻转离开的模式。 RNA序列的微小差异允许采用新的控制模式,除了Puf4p外,还将Puf5p募集到单个位点。这种嵌入的信息为RNA靶标与PUF蛋白之间的连接增加了新的生物学意义。

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