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Structure-function studies of FMRP RGG peptide recognition of an RNA duplex-quadruplex junction

机译:FMRP RGG肽识别RNA双链-四链连接的结构功能研究

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摘要

We have determined the solution structure of the complex between an arginine-glycine-rich RGG peptide from the human fragile X mental retardation protein (FMRP) and an in vitro-selected guanine-rich (G-rich) sc1 RNA. The bound RNA forms a newly discovered G-quadruplex separated from the flanking duplex stem by a mixed junctional tetrad. The RGG peptide is positioned along the major groove of the RNA duplex, with the G-quadruplex forcing a sharp turn of R 10 GGGGR 15 at the duplex-quadruplex junction. Arg10 and Arg15 form cross-strand specificity-determining intermolecular hydrogen bonds with the major-groove edges of guanines of adjacent Watson-Crick G-C pairs. Filter-binding assays on RNA and peptide mutations identify and validate contributions of peptide-RNA intermolecular contacts and shape complementarity to molecular recognition. These findings on FMRP RGG domain recognition by a combination of G-quadruplex and surrounding RNA sequences have implications for the recognition of other genomic G-rich RNAs.
机译:我们已经确定了来自人类脆弱的X智力低下蛋白(FMRP)的富含精氨酸-甘氨酸的RGG肽与体外选择的富含鸟嘌呤(富含G)的sc1 RNA之间的复合物的溶液结构。结合的RNA形成新发现的G-四链体,其通过混合连接四联体与侧翼双链体茎分开。 RGG肽沿着RNA双链体的主要凹槽定位,G-四链体迫使R 10 GGGGR 15在双链体-四链体连接处急剧转向。 Arg10和Arg15与相邻的Watson-Crick G-C对的鸟嘌呤的主要沟槽边缘形成确定链间氢键的跨链特异性。 RNA和肽突变的滤膜结合测定法可识别和验证肽-RNA分子间接触的贡献以及形状互补性对分子识别的作用。 G-四链体和周围RNA序列相结合的关于FMRP RGG域识别的这些发现对其他富含G的基因组RNA的识别具有重要意义。

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