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首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Discovery of platencin, a dual FabF and FabH inhibitor with in vivo antibiotic properties
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Discovery of platencin, a dual FabF and FabH inhibitor with in vivo antibiotic properties

机译:发现具有体内抗生素特性的双重FabF和FabH抑制剂Platencin

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Emergence of bacterial resistance is a major issue for all classes of antibiotics; therefore, the identification of new classes is critically needed. Recently we reported the discovery of platensimycin by screening natural product extracts using a target-based whole-cell strategy with antisense silencing technology in concert with cell free biochemical validations. Continued screening efforts led to the discovery of platencin, a novel natural product that is chemically and biologically related but different from platensimycin. Platencin exhibits a broad-spectrum Gram-positive antibacterial activity through inhibition of fatty acid biosynthesis. It does not exhibit cross-resistance to key antibiotic resistant strains tested, including methicillin-resistant Staphylococcus aureus, vancomycin-interme-diate S. aureus, and vancomycin-resistant Enterococci. Platencin shows potent in vivo efficacy without any observed toxicity. It targets two essential proteins, β-ketoacyl-[acyl carrier protein (ACP)] synthase Ⅱ (FabF) and Ⅲ (FabH) with IC_(50) values of 1.95 and 3.91 μg/ml, respectively, whereas platensimycin targets only FabF (IC_(50) = 0.13 μg/ml) in S. aureus, emphasizing the fact that more antibiotics with novel structures and new modes of action can be discovered by using this antisense differential sensitivity whole-cell screening paradigm.
机译:细菌耐药性的出现是所有类型抗生素的主要问题。因此,迫切需要识别新类别。最近,我们报道了通过使用基于靶标的全细胞策略和反义沉默技术与无细胞生化验证相结合的方法筛选天然产物提取物,发现了板霉素的发现。持续的筛选工作导致发现了Platencin,这是一种化学和生物学相关但与Platensimycin不同的新型天然产物。血小板素通过抑制脂肪酸的生物合成表现出广谱的革兰氏阳性抗菌活性。它对测试的关键抗生素抗性菌株没有交叉耐药性,包括耐甲氧西林的金黄色葡萄球菌,中间万古霉素的金黄色葡萄球菌和耐万古霉素的肠球菌。 Platencin显示有效的体内功效,没有观察到毒性。它靶向两种必需蛋白,β-酮酰基-[酰基载体蛋白(ACP)]合酶Ⅱ(FabF)和Ⅲ(FabH),IC_(50)值分别为1.95和3.91μg/ ml,而板霉素仅靶向FabF(金黄色葡萄球菌的IC_(50)= 0.13μg/ ml)强调了这样一个事实,即通过使用这种反义差异敏感性全细胞筛选范例可以发现更多具有新颖结构和新作用方式的抗生素。

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