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首页> 外文期刊>Angewandte Chemie >Total Synthesis of Albicidin: A Lead Structure from Xanthomonas albilineans for Potent Antibacterial Gyrase Inhibitors
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Total Synthesis of Albicidin: A Lead Structure from Xanthomonas albilineans for Potent Antibacterial Gyrase Inhibitors

机译:阿比西丁的全合成:一种来自黄单胞菌的强效抗菌促旋酶抑制剂的铅结构。

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摘要

The peptide antibiotic albicidin, which is synthesized by the plant pathogenic bacterium Xanthomonas albilineans, displays remarkable antibacterial activity against various Gram-positive and Gram-negative microorganisms. The low amounts of albicidin obtainable from the producing organism or through heterologous expression are limiting factors in providing sufficient material for bioactivity profiling and structure-activity studies. Therefore, we developed a convergent total synthesis route toward albicidin. The unexpectedly difficult formation of amide bonds between the aromatic amino acids was achieved through a triphosgene-mediated coupling strategy. The herein presented synthesis of albicidin confirms the previously determined chemical structure and underlines the extraordinary antibacterial activity of this compound. The synthetic protocol will provide multigram amounts of albicidin for further profiling of its drug properties.
机译:由植物病原性细菌黄单胞菌(Xanthomonas albilineans)合成的肽抗生素短杆菌肽对多种革兰氏阳性和革兰氏阴性微生物表现出显着的抗菌活性。可从生产生物体或通过异源表达获得的少量苦豆素是为生物活性谱和结构活性研究提供足够材料的限制因素。因此,我们开发了趋向白粉菌素的聚合全合成路线。通过三光气介导的偶联策略实现了芳族氨基酸之间酰胺键意外地难以形成。本文提出的阿比西丁合成证实了先前确定的化学结构,并强调了该化合物的非凡抗菌活性。合成方案将提供数克量的杀菌素,以进一步分析其药物特性。

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