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Structure analysis of free and bound states of an RNA aptamer against ribosomal protein S8 from Bacillus anthracis

机译:抗炭疽芽孢杆菌核糖体蛋白S8的RNA适体的自由和结合状态的结构分析

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摘要

Several protein-targeted RNA aptamers have been identified for a variety of applications and although the affinities of numerous protein-aptamer complexes have been determined, the structural details of these complexes have not been widely explored. We examined the structural accommodation of an RNA aptamer that binds bacterial r-protein S8. The core of the primary binding site for S8 on helix 21 of 16S rRNA contains a pair of conserved base triples that mold the sugar-phosphate backbone to S8. The aptamer, which does not contain the conserved sequence motif, is specific for the rRNA binding site of S8. The protein-free RNA aptamer adopts a helical structure with multiple non-canonical base pairs. Surprisingly, binding of S8 leads to a dramatic change in the RNA conformation that restores the signature S8 recognition fold through a novel combination of nucleobase interactions. Nucleotides within the non-canonical core rearrange to create a G-(G-C) triple and a U-(A-U)-U quartet. Although native-like S8-RNA interactions are present in the aptamer-S8 complex, the topology of the aptamer RNA differs from that of the helix 21-S8 complex. This is the first example of an RNA aptamer that adopts substantially different secondary structures in the free and protein-bound states and highlights the remarkable plasticity of RNA secondary structure.
机译:已经鉴定了几种针对蛋白质的RNA适体,可用于多种应用,尽管已确定了许多蛋白质适体复合物的亲和力,但尚未广泛探索这些复合物的结构细节。我们检查了结合细菌r蛋白S8的RNA适体的结构调节。 16S rRNA的螺旋21上S8的主要结合位点的核心含有一对保守的碱基三元组,将糖磷酸骨架形成S8。不包含保守序列基序的适体对S8的rRNA结合位点具有特异性。不含蛋白质的RNA适体采用具有多个非经典碱基对的螺旋结构。出人意料的是,S8的结合导致RNA构象的巨大变化,该变化通过核碱基相互作用的新颖组合恢复了签名S8的识别折叠。非规范核心中的核苷酸重排以创建G-(G-C)三元组和U-(A-U)-U四重奏。尽管适体-S8复合物中存在天然的S8-RNA相互作用,但适体RNA的拓扑结构与21-S8螺旋复合物的拓扑结构不同。这是RNA适体的第一个例子,其在游离态和蛋白质结合态采用基本上不同的二级结构,并突出了RNA二级结构的显着可塑性。

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