首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >Structure-function studies of STAR family quaking proteins bound to their in vivo RNA target sites
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Structure-function studies of STAR family quaking proteins bound to their in vivo RNA target sites

机译:STAR家族蛋白与体内RNA靶位点结合的结构功能研究

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Mammalian Quaking (QKI) and its Caenorhabditis elegans homolog, GLD-1 (defective in germ line development), are evolutionarily conserved RNA-binding proteins, which post-transcriptionally regulate target genes essential for developmental processes and myelination. We present X-ray structures of the STAR (signal transduction and activation of RNA) domain, composed of Qua1, K homology (KH), and Qua2 motifs of QKI and GLD-1 bound to high-affinity in vivo RNA targets containing YUAAY RNA recognition elements (RREs). The KH and Qua2 motifs of the STAR domain synergize to specifically interact with bases and sugar-phosphate backbones of the bound RRE. Qua1-mediated homodimerization generates a scaffold that enables concurrent recognition of two RREs, thereby plausibly targeting tandem RREs present in many QKI-targeted transcripts. Structure-guided mutations reduced QKI RNA-binding affinity in vitro and in vivo, and expression of QKI mutants in human embryonic kidney cells (HEK293) significantly decreased the abundance of QKI target mRNAs. Overall, our studies define principles underlying RNA target selection by STAR homodimers and provide insights into the post-transcriptional regulatory function of mammalian QKI proteins.
机译:哺乳动物Quaking(QKI)及其秀丽隐杆线虫的同系物GLD-1(在种系发育中有缺陷)是进化上保守的RNA结合蛋白,在转录后调节靶基因对发育过程和髓鞘形成至关重要。我们目前的X射线结构的STAR(信号转导和RNA激活)域,由QKI和GLD-1的Qua1,K同源性(KH)和Qua2图案组成,与包含YUAAY RNA的高亲和力体内RNA靶结合识别元素(RRE)。 STAR结构域的KH和Qua2基序协同作用,与结合的RRE的碱基和糖磷酸主链特异性相互作用。 Qua1介导的均二聚作用产生了一个支架,该支架能够同时识别两个RRE,从而有可能靶向许多QKI靶向转录物中存在的串联RRE。结构指导的突变降低了体内和体外QKI RNA的结合亲和力,并且QKI突变体在人胚胎肾细胞(HEK293)中的表达显着降低了QKI目标mRNA的丰度。总体而言,我们的研究确定了STAR同型二聚体选择RNA靶标的基本原理,并提供了对哺乳动物QKI蛋白转录后调控功能的见解。

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