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Structure of tandem RNA recognition motifs from polypyrimidine tract binding protein reveals novel features of the RRM fold

机译:聚嘧啶束结合蛋白的串联RNA识别基序的结构揭示了RRM折叠的新特征

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摘要

Polypyrimidine tract binding protein (PTB), an RNA binding protein containing four RNA recognition motifs (RRMs), is involved in both pre-mRNA splicing and translation initiation directed by picornaviral internal ribosome entry sites. Sequence comparisons previously indicated that PTB is a non-canonical RRM protein. The solution structure of a PTB fragment containing RRMs 3 and 4 shows that the protein consists of two domains connected by a long, flexible linker. The two domains tumble independently in solution, having no fixed relative orientation. In addition to the βαββαβ topology, which is characteristic of RRM domains, the C-terminal extension of PTB RRM-3 incorporates an unanticipated fifth β-strand, which extends the RNA binding surface. The long, disordered polypeptide connecting β4 and β5 in RRM-3 is poised above the RNA binding surface and is likely to contribute to RNA recognition. Mutational analyses show that both RRM-3 and RRM-4 contribute to RNA binding specificity and that, despite its unusual sequence, PTB binds RNA in a manner akin to that of other RRM proteins.
机译:聚嘧啶束结合蛋白(PTB)是一种含有四个RNA识别基序(RRM)的RNA结合蛋白,既参与前mRNA剪接,又受皮甲病毒内部核糖体进入位点的翻译起始。序列比较以前表明PTB是非规范的RRM蛋白。包含RRM 3和4的PTB片段的溶液结构表明,该蛋白由两个结构域组成,这些结构域由一个长而灵活的接头连接。这两个域在解决方案中独立滚动,没有固定的相对方向。除具有RRM结构域特征的βαββαβ拓扑结构外,PTB RRM-3的C末端延伸还掺入了未预期的第五个β链,该链延伸了RNA结合表面。 RRM-3中连接β4和β5的长无序多肽位于RNA结合表面上方,可能有助于RNA识别。突变分析表明,RRM-3和RRM-4都有助于RNA结合特异性,尽管序列不寻常,但PTB仍以与其他RRM蛋白类似的方式结合RNA。

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