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Identification of Low-Molecular-Weight Compounds Inhibiting Growth of Corynebacteria: Potential Lead Compounds for Antibiotics

机译:抑制棒状杆菌生长的低分子量化合物的鉴定:抗生素的潜在先导化合物

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The bacterial genus Corynebacteria contains several pathogenic species that cause diseases such as diphtheria in humans and "cheesy gland" in goats and sheep. Thus, identifying new therapeutic targets to treat Corynebacteria infections is both medically and economically important. CG2496, a functionally uncharacterized protein from Corynebacterium glutamicum, was evaluated using an NMR ligand-affinity screen. A total of 11 compounds from a library of 460 biologically active compounds were shown to selectively bind CG2496 in a highly conserved region of the protein. The best binder was identified to be methiothepin (K_D = 54±19 u.m), an FDA-approved serotonin receptor antagonist. Methiothepin was also shown to inhibit the growth of C glutamicum, but not bacteria that lack CG2496 homologs. Our results suggest that CG2496 is a novel therapeutic target and methiothepin is a potential lead compound or structural scaffold for developing new antibiotics specifically targeting Corynebacteria.
机译:棒状杆菌属细菌包含几种致病菌,可引起人类白喉和山羊和绵羊“俗气的腺体”等疾病。因此,确定治疗棒状杆菌感染的新治疗靶标在医学和经济上都是重要的。使用NMR配体亲和力筛选仪评估了CG2496,这是一种来自谷氨酸棒杆菌的功能上未表征的蛋白质。已显示来自460种生物活性化合物的库中的总共11种化合物在蛋白质的高度保守区域中选择性结合CG2496。最好的结合剂被确定为美托西平(K_D = 54±19 u.m),这是一种FDA批准的5-羟色胺受体拮抗剂。还显示了甲硫平可以抑制谷氨酸丙氨酸的生长,但不能抑制缺乏CG2496同源物的细菌。我们的研究结果表明,CG2496是一种新型治疗靶标,而美索西平是开发专门针对棒状杆菌的新型抗生素的潜在先导化合物或结构支架。

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