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(Dis)similar Analogues of Riboswitch Metabolites as Antibacterial Lead Compounds

机译:Riboswitch代谢产物作为(抗菌)先导化合物的(相异)类似物

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摘要

The rise of antimicrobial resistance in human pathogenic bacteria has increased the necessity for the discovery of novel, yet unexplored antibacterial drug targets. Riboswitches, which are embedded in untranslated regions of bacterial messenger RNA (mRNA), represent such an interesting target structure. These RNA elements regulate gene expression upon binding to natural metabolites, second messengers, and inorganic ions, such as fluoride with high affinity and in a highly discriminative manner. Recently, efforts have been directed toward the identification of artificial riboswitch activators by establishing high-throughput screening assays, fragment-based screening, and structure-guided ligand design approaches. Emphasis in this review is placed on the special requirements and synthesis of new potential antibiotic drugs that target riboswitches in which dissimilarity is an important aspect in the design of potential lead compounds.
机译:人类病原菌中抗菌素耐药性的增加增加了发现新型但尚未探索的抗菌药物靶标的必要性。嵌在细菌信使RNA(mRNA)非翻译区的核糖开关代表了这种有趣的靶标结构。这些RNA元素在与天然代谢物,第二信使和无机离子(例如氟化物)结合时,以高度亲和力和高度区分性的方式调节基因表达。近来,已经通过建立高通量筛选测定,基于片段的筛选和结构指导的配体设计方法来致力于鉴定人工核糖开关激活剂。本文的重点是针对针对核糖开关的新的潜在抗生素药物的特殊要求和合成,其中相异性是潜在铅化合物设计中的重要方面。

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