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Lantibiotics and microcins: polypeptides with unusual chemical diversity

机译:羊毛硫抗生素和微霉素:具有异常化学多样性的多肽

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Bacterial-derived antimicrobial polypeptides enjoy a large degree of structural and chemical diversity. Two well-studied examples of such polypeptides are the lanthionine-containing lantibiotics produced by a variety of Gram-positive bacteria, and their Gram-negative counterparts, the microcins. Both groups are produced as gene-encoded precursor peptides and undergo post-translational modification to generate the active moieties. Structure elucidation of novel lantibiotics and microcins has recently uncovered further novel structural and chemical features and, combined with the generation of analogue peptides by genetic manipulation, new insights into structure-function relationships have been gained. Furthermore, study of the mode of action of the lantibiotics nisin and mersacidin has revealed their use of a 'docking molecule' in the target cell to facilitate their biological activities. Meanwhile, in vitro studies with microcin B17 have helped to uncover the molecular mechanisms by which post-translational modification results in the formation of heterocyclic oxazole and thiazole rings. From a practical standpoint, both groups of polypeptides represent new lead structures for future development of antimicrobial agents, whilst the identification of the 'docking molecules' represents a step forward in the search for novel targets for future antibiosis.
机译:细菌衍生的抗菌多肽享有很大程度的结构和化学多样性。这类多肽的两个经过充分研究的例子是各种革兰氏阳性细菌产生的含羊毛硫氨酸羊毛硫抗生素,以及它们的革兰氏阴性细菌微素。两组均作为基因编码的前体肽产生,并进行翻译后修饰以产生活性部分。新型羊毛硫抗生素和微霉素的结构解析最近发现了进一步的新型结构和化学特征,并且与通过基因操作产生的类似肽相结合,获得了对结构-功能关系的新见解。此外,对羊毛硫抗生素乳酸链球菌肽和mersacidin的作用方式的研究表明,它们在靶细胞中使用了“对接分子”来促进其生物学活性。同时,用微霉素B17进行的体外研究有助于揭示分子机制,通过这种机制,翻译后修饰可导致形成杂环恶唑和噻唑环。从实践的角度来看,两组多肽代表了抗微生物剂未来发展的新的先导结构,而“对接分子”的鉴定则代表了寻找新的抗微生物靶标的一步。

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