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通过过度确定的氢键作用激活glmS核酶亲核试剂。

Activation of the glmS Ribozyme Nucleophile via Overdetermined Hydrogen Bonding.

作者信息

Bingaman Jamie L, Gonzalez Inanllely Y, Wang Bo, Bevilacqua Philip C

机构信息

Department of Chemistry, Pennsylvania State University , University Park, Pennsylvania 16802, United States.

Center for RNA Molecular Biology, Pennsylvania State University , University Park, Pennsylvania 16802, United States.

出版信息

Biochemistry. 2017 Aug 22;56(33):4313-4317. doi: 10.1021/acs.biochem.7b00662. Epub 2017 Aug 8.

Abstract

RNA enzymes, or ribozymes, catalyze internal phosphodiester bond cleavage using diverse catalytic strategies. These include the four classic strategies: in-line nucleophilic attack, deprotonation of the 2'-OH nucleophile, protonation of the 5'-O leaving group, and stabilization of developing charge on the nonbridging oxygen atoms of the scissile phosphate. In addition, we recently identified two additional ribozyme strategies: acidification of the 2'-OH and release of the 2'-OH from inhibitory interactions. Herein, we report inverse thio effects in the presence of glmS ribozyme variants and a 1-deoxyglucosamine 6-phosphate cofactor analogue and demonstrate that activation of the 2'-OH nucleophile is promoted by competitive hydrogen bonding among diverse ribozyme moieties for the pro-R nonbridging oxygen. We conclude that the glmS ribozyme uses an overdetermined set of competing hydrogen bond donors in its active site to ensure potent activation and regulation by the cofactor. Nucleophile activation through competitive, overdetermined hydrogen bonding could be a general strategy for ribozyme activation and may be applicable for controlling the function of ribozymes and riboswitches in the laboratory.

摘要

RNA酶,即核酶,利用多种催化策略催化内部磷酸二酯键的断裂。这些策略包括四种经典策略:线性亲核攻击、2'-OH亲核试剂的去质子化、5'-O离去基团的质子化以及对断裂磷酸的非桥连氧原子上发展电荷的稳定作用。此外,我们最近还发现了另外两种核酶策略:2'-OH的酸化以及2'-OH从抑制性相互作用中的释放。在此,我们报道了在glmS核酶变体和1-脱氧葡糖胺6-磷酸辅因子类似物存在下的反向硫代效应,并证明了2'-OH亲核试剂的激活是由不同核酶部分之间对前-R非桥连氧的竞争性氢键作用所促进的。我们得出结论,glmS核酶在其活性位点使用一组过度确定的竞争性氢键供体,以确保辅因子的有效激活和调节。通过竞争性、过度确定的氢键作用进行亲核试剂激活可能是核酶激活的一种通用策略,并且可能适用于在实验室中控制核酶和核糖开关的功能。

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