首页> 外文期刊>Nucleic Acids Research >Recognition of a cognate RNA aptamer by neomycin B: quantitative evaluation of hydrogen bonding and electrostatic interactions.
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Recognition of a cognate RNA aptamer by neomycin B: quantitative evaluation of hydrogen bonding and electrostatic interactions.

机译:新霉素B对同源RNA适体的识别:氢键和静电相互作用的定量评估。

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摘要

Aminoglycosides are an important class of antibiotic that selectively target RNA structural motifs. Recently we have demonstrated copper derivatives of amino-glycosides to be efficient cleavage agents for cognate RNA motifs. To fully develop their potential as pharmaceutical agents it is necessary to understand both the structural mechanisms used by aminoglycosides to target RNA, and the relative contributions of hydrogen bonding and electrostatic interactions to recognition selectivity. Herein we report results from a calorimetric analysis of a stem-loop 23mer RNA aptamer complexed to the aminoglycoside neomycin B. Key thermodynamic parameters for complex formation have been determined by isothermal titration calorimetry, and from the metal-ion dependence of these binding parameters the relative contributions of electrostatics and hydrogen bonding toward binding affinity have been assessed. The principal mechanism for recognition and binding of neomycin B to the RNA major groove is mediated by hydrogen bonding.
机译:氨基糖苷是一类重要的抗生素,可以选择性地靶向RNA结构基序。最近,我们已经证明氨基糖苷的铜衍生物是有效的同源RNA图案切割剂。为了充分发挥其作为药物的潜力,有必要了解氨基糖苷类用于靶向RNA的结构机制,以及氢键和静电相互作用对识别选择性的相对贡献。在本文中,我们报告了与氨基糖苷新霉素B复合的茎环23mer RNA适体的量热分析结果。通过等温滴定量热法确定了复合物形成的关键热力学参数,并且根据这些结合参数对金属离子的依赖性已经评估了静电和氢键对结合亲和力的贡献。识别和结合新霉素B到RNA大沟的主要机制是通过氢键介导的。

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