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核黄素类似物核糖嘧啶的原子分辨率机制研究:一种对大肠杆菌FMN核糖开关具有高度选择性的非天然配体模拟物。

Atomic resolution mechanistic studies of ribocil: A highly selective unnatural ligand mimic of the E. coli FMN riboswitch.

作者信息

Howe John A, Xiao Li, Fischmann Thierry O, Wang Hao, Tang Haifeng, Villafania Artjohn, Zhang Rumin, Barbieri Christopher M, Roemer Terry

机构信息

a Merck Research Laboratories , Kenilworth , NJ , USA.

出版信息

RNA Biol. 2016 Oct 2;13(10):946-954. doi: 10.1080/15476286.2016.1216304. Epub 2016 Aug 2.

Abstract

Bacterial riboswitches are non-coding RNA structural elements that direct gene expression in numerous metabolic pathways. The key regulatory roles of riboswitches, and the urgent need for new classes of antibiotics to treat multi-drug resistant bacteria, has led to efforts to develop small-molecules that mimic natural riboswitch ligands to inhibit metabolic pathways and bacterial growth. Recently, we reported the results of a phenotypic screen targeting the riboflavin biosynthesis pathway in the Gram-negative bacteria Escherichia coli that led to the identification of ribocil, a small molecule inhibitor of the flavin mononucleotide (FMN) riboswitch controlling expression of this biosynthetic pathway. Although ribocil is structurally distinct from FMN, ribocil functions as a potent and highly selective synthetic mimic of the natural ligand to repress riboswitch-mediated ribB gene expression and inhibit bacterial growth both in vitro and in vivo. Herein, we expand our analysis of ribocil; including mode of binding in the FMN binding pocket of the riboswitch, mechanisms of resistance and structure-activity relationship guided efforts to generate more potent analogs.

摘要

细菌核糖开关是非编码RNA结构元件,可在众多代谢途径中指导基因表达。核糖开关的关键调控作用,以及迫切需要新型抗生素来治疗多重耐药细菌,促使人们努力开发小分子,以模拟天然核糖开关配体来抑制代谢途径和细菌生长。最近,我们报道了针对革兰氏阴性细菌大肠杆菌中核黄素生物合成途径的表型筛选结果,该筛选导致了核糖嘧啶的鉴定,核糖嘧啶是一种小分子抑制剂,可抑制控制该生物合成途径表达的黄素单核苷酸(FMN)核糖开关。尽管核糖嘧啶在结构上与FMN不同,但核糖嘧啶作为天然配体的有效且高度选择性的合成模拟物发挥作用,以抑制核糖开关介导的ribB基因表达,并在体外和体内抑制细菌生长。在此,我们扩展了对核糖嘧啶的分析;包括在核糖开关的FMN结合口袋中的结合模式、抗性机制以及构效关系,以指导生成更有效类似物的努力。

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