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大肠杆菌S8核糖体蛋白的RNA结合位点:指数富集的配体系统进化技术(SELEX)和羟自由基探测研究

The RNA binding site of S8 ribosomal protein of Escherichia coli: Selex and hydroxyl radical probing studies.

作者信息

Moine H, Cachia C, Westhof E, Ehresmann B, Ehresmann C

机构信息

UPR 9002 du CNRS, Institut de Biologie Moléculaire et Cellulaire, Strasbourg, France.

出版信息

RNA. 1997 Mar;3(3):255-68.

PMID:9056763
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1369478/
Abstract

The RNA binding site of ribosomal protein S8 of Escherichia coli is confined to a small region within the stem of a hairpin in 16S rRNA (nt 588-605/633-651), and thus represents a model system for understanding RNA/protein interaction rules. The S8 binding site on 16S rRNA was suspected to contain noncanonical features difficult to prove with classical genetical or biochemical means. We performed in vitro iterative selection of RNA aptamers that bind S8. For the different aptamers, the interactions with the protein were probed with hydroxyl radicals. Aptamers that were recognized according to the same structural rules as wild-type RNA, but with variations not found in nature, were identified. These aptamers revealed features in the S8 binding site that had been concealed during previous characterizations by the high base conservation throughout evolution. Our data demonstrate that the core structure of the S8 binding site is composed of three interdependent bases (nt 597/641/643), with an essential intervening adenine nucleotide (position 642). The other elements important for the binding site are a base pair (598/640) above the three interdependent bases and a bulged base at position 595, the identity of which is not important. Possible implications on the geometry of the S8 binding site are discussed with the help of a three-dimensional model.

摘要

大肠杆菌核糖体蛋白S8的RNA结合位点局限于16S rRNA发夹茎内的一个小区域(核苷酸588 - 605/633 - 651),因此代表了一个理解RNA/蛋白质相互作用规则的模型系统。16S rRNA上的S8结合位点被怀疑含有难以用经典遗传学或生化方法证明的非规范特征。我们对结合S8的RNA适体进行了体外迭代筛选。对于不同的适体,用羟自由基探测其与蛋白质的相互作用。鉴定出了根据与野生型RNA相同的结构规则识别,但具有自然界中未发现的变异的适体。这些适体揭示了S8结合位点在先前表征过程中因整个进化过程中高度的碱基保守性而被隐藏的特征。我们的数据表明,S8结合位点的核心结构由三个相互依赖的碱基(核苷酸597/641/643)组成,中间有一个必需的腺嘌呤核苷酸(位置642)。结合位点的其他重要元件是三个相互依赖碱基上方的一个碱基对(598/640)和位置595处的一个凸起碱基,其具体身份并不重要。借助三维模型讨论了对S8结合位点几何形状的可能影响。