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A transient α-helix in the N-terminal RNA recognition motif of polypyrimidine tract binding protein senses RNA secondary structure

机译:聚嘧啶束结合蛋白N端RNA识别基序中的瞬时α螺旋感应RNA二级结构

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摘要

The polypyrimidine tract binding protein (PTB) is a multi-domain protein involved in alternative splicing, mRNA localization, stabilization, polyadenylation and translation initiation from internal ribosome entry sites (IRES). In this latter process, PTB promotes viral translation by interacting extensively with complex structured regions in the 5′-untranslated regions of viral RNAs at pyrimidine-rich targets located in single strand and hairpin regions. To better understand how PTB recognizes structured elements in RNA targets, we solved the solution structure of the N-terminal RNA recognition motif (RRM) in complex with an RNA hairpin embedding the loop sequence UCUUU, which is frequently found in IRESs of the picornovirus family. Surprisingly, a new three-turn α3 helix C-terminal to the RRM, folds upon binding the RNA hairpin. Although α3 does not mediate any contacts to the RNA, it acts as a sensor of RNA secondary structure, suggesting a role for RRM1 in detecting pyrimidine tracts in the context of structured RNA. Moreover, the degree of helix formation depends on the RNA loop sequence. Finally, we show that the α3 helix region, which is highly conserved in vertebrates, is crucial for PTB function in enhancing Encephalomyocarditis virus IRES activity.
机译:聚嘧啶束结合蛋白(PTB)是一种多域蛋白,涉及内部核糖体进入位点(IRES)的可变剪接,mRNA定位,稳定化,聚腺苷酸化和翻译起始。在后面的过程中,PTB通过与位于单链和发夹区域的富含嘧啶的靶标的病毒RNA的5'-非翻译区中的复杂结构区广泛相互作用,促进病毒翻译。为了更好地了解PTB如何识别RNA靶标中的结构元件,我们解决了N末端RNA识别基序(RRM)的溶液结构,该蛋白与嵌有环序列UCUUU的RNA发夹配合使用,该序列通常在微微小病毒家族的IRES中发现。出人意料的是,在结合RNA发夹后,RRM的新的三匝α3螺旋C端折叠了。尽管α3不介导与RNA的任何接触,但它充当RNA二级结构的传感器,这提示RRM1在结构化RNA的背景下检测嘧啶束中的作用。此外,螺旋形成的程度取决于RNA环序列。最后,我们证明了在脊椎动物中高度保守的α3螺旋区对于PTB在增强脑心肌炎病毒IRES活性中的功能至关重要。

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