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Structural basis for recognition of AU-rich element RNA by the HuD protein

机译:HuD蛋白识别富含AU的元素RNA的结构基础

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摘要

Hu proteins bind to adenosine-uridine (AU)-rich elements (AREs) in the 3' untranslated regions of many short-lived mRNAs, thereby stabilizing them, Here we report the crystal structures of the first two RNA recognition motif (RRM) domains of the HuD protein in complex with an 11-nucleotide fragment of a class I ARE (the c-fos ARE; to 1.8 Angstrom), and with an 11-nucleotide fragment of a class II ARE (the tumor necrosis factor alpha ARE; to 2.3 Angstrom). These structures reveal a consensus RNA recognition sequence that suggests a preference for pyrimidine-rich sequences and a requirement for a central uracil residue in the clustered AUUUA repeats found in class II AREs, Comparison to structures of other RRM domain-nucleic acid complexes reveals two base recognition pockets in all the structures that interact with bases using residues in conserved ribonucleoprotein motifs and at the C-terminal ends of RRM domains. Different conformations of nucleic acid can be bound by RRM domains by using different combinations of base recognition pockets and multiple RRM domains. [References: 34]
机译:Hu蛋白与许多短寿命mRNA的3'非翻译区中的富含腺苷-尿苷(AU)的元素结合,从而使其稳定。在这里,我们报道前两个RNA识别基序(RRM)域的晶体结构HuD蛋白与I类ARE的11个核苷酸片段(c-fos ARE;至1.8埃)和II类ARE的11个核苷酸片段(肿瘤坏死因子αARE; 2.3埃)。这些结构揭示了一个共有的RNA识别序列,该序列暗示了对富含嘧啶的序列的偏爱,以及对在II类ARE中发现的成簇AUUUA重复序列中中央尿嘧啶残基的要求,与其他RRM域-核酸复合物的结构比较揭示了两个碱基使用保守的核糖核蛋白基序和RRM结构域C末端的残基,可与碱基相互作用的所有结构中的识别口袋。通过使用碱基识别口袋和多个RRM结构域的不同组合,核酸的不同构象可以被RRM结构域结合。 [参考:34]

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