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Metabolic inhibitors of bacterial glycan biosynthesis

机译:细菌聚糖生物合成的代谢抑制剂

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The bacterial cell wall is a quintessential drug target due to its critical role in colonization of the host, pathogen survival, and immune evasion. The dense cell wall glycocalyx contains distinctive monosaccharides that are absent from human cells, and proper assembly of monosaccharides into higher-order glycans is critical for bacterial fitness and pathogenesis. However, the systematic study and inhibition of bacterial glycosylation enzymes remains challenging. Bacteria produce glycans containing rare deoxy amino sugars refractory to traditional glycan analysis, complicating the study of bacterial glycans and the creation of glycosylation inhibitors. To ease the study of bacterial glycan function in the absence of detailed structural or enzyme information, we crafted metabolic inhibitors based on rare bacterial monosaccharide scaffolds. Metabolic inhibitors were assessed for their ability to interfere with glycan biosynthesis and fitness in pathogenic and symbiotic bacterial species. Three metabolic inhibitors led to dramatic structural and functional defects in Helicobacter pylori . Strikingly, these inhibitors acted in a bacteria-selective manner. These metabolic inhibitors will provide a platform for systematic study of bacterial glycosylation enzymes not currently possible with existing tools. Moreover, their selectivity will provide a pathway for the development of novel, narrow-spectrum antibiotics to treat infectious disease. Our inhibition approach is general and will expedite the identification of bacterial glycan biosynthesis inhibitors in a range of systems, expanding the glycochemistry toolkit.
机译:由于其在宿主,病原体存活和免疫逃避的殖民化中的关键作用,细菌细胞壁是一种典型的药物靶标。致密的细胞壁甘油蛋白含有从人细胞中不存在的独特单糖,并且将单糖的适当组装成高阶聚糖对于细菌性能和发病性至关重要。然而,对细菌糖基化酶的系统研究和抑制仍然具有挑战性。细菌产生含有稀有脱氧氨基糖的聚糖对传统聚糖分析的难以解答,使细菌聚糖的研究复杂化和糖基化抑制剂的产生。为了缓解细菌聚糖功能,在没有详细的结构或酶信息的情况下,我们基于稀有细菌单糖支架制作代谢抑制剂。评估代谢抑制剂的能力干扰甘油生物合成和致病性和共生细菌种类的适应性。三种代谢抑制剂导致幽门螺杆菌的戏剧性结构和功能性缺陷。引人注目的是,这些抑制剂以细菌选择性的方式作用。这些代谢抑制剂将提供对现有工具目前不可能的细菌糖基化酶的系统研究平台。此外,它们的选择性将为新颖,窄谱抗生素的发展提供一种治疗传染病的途径。我们的抑制方法是一般的,并加快鉴定在一系列系统中的细菌聚糖生物合成抑制剂,膨胀甘油化学工具包。

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