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首页> 外文期刊>Angewandte Chemie >Dissecting Bottromycin Biosynthesis Using Comparative Untargeted Metabolomics
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Dissecting Bottromycin Biosynthesis Using Comparative Untargeted Metabolomics

机译:使用比较未靶制的代谢组科对Bottromycin生物合成

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摘要

Bottromycin A(2) is a structurally unique ribosomally synthesized and post-translationally modified peptide (RiPP) that possesses potent antibacterial activity towards multidrug-resistant bacteria. The structural novelty of bottromycin stems from its unprecedented macrocyclic amidine and rare beta-methylated amino acid residues. The N-terminus of a precursor peptide (BtmD) is converted into bottromycin A(2) by tailoring enzymes encoded in the btm gene cluster. However, little was known about key transformations in this pathway, including the unprecedented macrocyclization. To understand the pathway in detail, an untargeted metabolomic approach that harnesses mass spectral networking was used to assess the metabolomes of a series of pathway mutants. This analysis has yielded key information on the function of a variety of previously uncharacterized biosynthetic enzymes, including a YcaO domain protein and a partner protein that together catalyze the macrocyclization.
机译:Bottromycin A(2)是结构独特的核糖体合成和翻译后修饰的肽(RIPP),其具有抗抗多药细菌的有效抗菌活性。 Bottromycin的结构新颖性来自其前所未有的大环脒和稀有β-甲基化氨基酸残基。 前体肽(BTMD)的N-末端通过在BTM基因簇中编码的鉴定酶转化为Bottromycin A(2)。 但是,关于该途径的关键转化知之甚少,包括前所未有的宏次数。 为了详细了解途径,利用利用质谱网络的未确定代谢方法评估一系列途径突变体的代谢。 该分析产生了有关各种先前未表征的生物合成酶的功能的关键信息,包括YcoO结构域蛋白和共同催化宏核的伴侣蛋白。

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