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程序化迭代控制抗生素莫匹罗星壬酸侧链的组装。

Programmed Iteration Controls the Assembly of the Nonanoic Acid Side Chain of the Antibiotic Mupirocin.

作者信息

Winter Ashley J, Rowe Matthew T, Weir Angus N M, Akter Nahida, Mbatha Sbusisiwe Z, Walker Paul D, Williams Christopher, Song Zhongshu, Race Paul R, Willis Christine L, Crump Matthew P

机构信息

School of Chemistry University of Bristol Bristol BS8 1TS UK.

School of Biochemistry University of Bristol Bristol BS8 1TD UK.

出版信息

Angew Chem Weinheim Bergstr Ger. 2022 Dec 12;134(50):e202212393. doi: 10.1002/ange.202212393. Epub 2022 Nov 10.

Abstract

Mupirocin is a clinically important antibiotic produced by NCIMB 10586 that is assembled by a complex -AT polyketide synthase. The polyketide fragment, monic acid, is esterified by a 9-hydroxynonanoic acid (9HN) side chain which is essential for biological activity. The ester side chain assembly is initialised from a 3-hydroxypropionate (3HP) starter unit attached to the acyl carrier protein (ACP) MacpD, but the fate of this species is unknown. Herein we report the application of NMR spectroscopy, mass spectrometry, chemical probes and in vitro assays to establish the remaining steps of 9HN biosynthesis. These investigations reveal a complex interplay between a novel iterative or "stuttering" KS-AT didomain (MmpF), the multidomain module MmpB and multiple ACPs. This work has important implications for understanding the late-stage biosynthetic steps of mupirocin and will be important for future engineering of related -AT biosynthetic pathways (e.g. thiomarinol).

摘要

莫匹罗星是由NCIMB 10586产生的一种具有临床重要性的抗生素,它由一种复杂的聚酮合酶装配而成。聚酮片段莫尼酸被一个对生物活性至关重要的9-羟基壬酸(9HN)侧链酯化。酯侧链的装配从连接到酰基载体蛋白(ACP)MacpD上的3-羟基丙酸(3HP)起始单元开始,但该物种的命运未知。在此,我们报告了应用核磁共振光谱、质谱、化学探针和体外测定来确定9HN生物合成的其余步骤。这些研究揭示了一种新型迭代或“口吃”的KS-AT双结构域(MmpF)、多结构域模块MmpB和多个ACP之间的复杂相互作用。这项工作对于理解莫匹罗星的后期生物合成步骤具有重要意义,并且对于未来相关聚酮合酶生物合成途径(如硫代马菌素)的工程改造也将具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c2c6/10947060/d64df6943441/ANGE-134-0-g010.jpg

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