Literature DB >> 29735559

Self-Resistance during Muraymycin Biosynthesis: a Complementary Nucleotidyltransferase and Phosphotransferase with Identical Modification Sites and Distinct Temporal Order.

Zheng Cui1, Xia-Chang Wang1, Xiaodong Liu1, Anke Lemke2, Stefan Koppermann2, Christian Ducho2, Jürgen Rohr1, Jon S Thorson1, Steven G Van Lanen3.   

Abstract

Muraymycins are antibacterial natural products from Streptomyces spp. that inhibit translocase I (MraY), which is involved in cell wall biosynthesis. Structurally, muraymycins consist of a 5'-C-glycyluridine (GlyU) appended to a 5″-amino-5″-deoxyribose (ADR), forming a disaccharide core that is found in several peptidyl nucleoside inhibitors of MraY. For muraymycins, the GlyU-ADR disaccharide is further modified with an aminopropyl-linked peptide to generate the simplest structures, annotated as the muraymycin D series. Two enzymes encoded in the muraymycin biosynthetic gene cluster, Mur29 and Mur28, were functionally assigned in vitro as a Mg·ATP-dependent nucleotidyltransferase and a Mg·ATP-dependent phosphotransferase, respectively, both modifying the 3″-OH of the disaccharide. Biochemical characterization revealed that both enzymes can utilize several nucleotide donors as cosubstrates and the acceptor substrate muraymycin also behaves as an inhibitor. Single-substrate kinetic analyses revealed that Mur28 preferentially phosphorylates a synthetic GlyU-ADR disaccharide, a hypothetical biosynthetic precursor of muraymycins, while Mur29 preferentially adenylates the D series of muraymycins. The adenylated or phosphorylated products have significantly reduced (170-fold and 51-fold, respectively) MraY inhibitory activities and reduced antibacterial activities, compared with the respective unmodified muraymycins. The results are consistent with Mur29-catalyzed adenylation and Mur28-catalyzed phosphorylation serving as complementary self-resistance mechanisms, with a distinct temporal order during muraymycin biosynthesis.
Copyright © 2018 American Society for Microbiology.

Entities:  

Keywords:  MraY inhibitor; antibiotic; biosynthesis; nucleoside; resistance; translocase I

Mesh:

Substances:

Year:  2018        PMID: 29735559      PMCID: PMC6021665          DOI: 10.1128/AAC.00193-18

Source DB:  PubMed          Journal:  Antimicrob Agents Chemother        ISSN: 0066-4804            Impact factor:   5.191


  43 in total

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Authors:  Jinshi Zhao; Robert A Gillespie; Ben C Chung; Do-Yeon Kwon; Ziqiang Guan; Jiyong Hong; Pei Zhou; Seok-Yong Lee
Journal:  Science       Date:  2013-08-30       Impact factor: 47.728

2.  Identification of the gene cluster involved in muraymycin biosynthesis from Streptomyces sp. NRRL 30471.

Authors:  Lin Cheng; Wenqing Chen; Lipeng Zhai; Dongmei Xu; Tingting Huang; Shuangjun Lin; Xiufen Zhou; Zixin Deng
Journal:  Mol Biosyst       Date:  2010-12-23

3.  Insights into the Target Interaction of Naturally Occurring Muraymycin Nucleoside Antibiotics.

Authors:  Stefan Koppermann; Zheng Cui; Patrick D Fischer; Xiachang Wang; Jannine Ludwig; Jon S Thorson; Steven G Van Lanen; Christian Ducho
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4.  Mechanistic analysis of muraymycin analogues: a guide to the design of MraY inhibitors.

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Authors:  J E Van Pelt; D B Northrop
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Authors:  L C Pedersen; M M Benning; H M Holden
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Authors:  Ben C Chung; Ellene H Mashalidis; Tetsuya Tanino; Mijung Kim; Akira Matsuda; Jiyong Hong; Satoshi Ichikawa; Seok-Yong Lee
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Review 10.  Muraymycin nucleoside-peptide antibiotics: uridine-derived natural products as lead structures for the development of novel antibacterial agents.

Authors:  Daniel Wiegmann; Stefan Koppermann; Marius Wirth; Giuliana Niro; Kristin Leyerer; Christian Ducho
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Review 4.  Identification and characterization of enzymes involved in the biosynthesis of pyrimidine nucleoside antibiotics.

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5.  Characterization of the Self-Resistance Mechanism to Dityromycin in the Streptomyces Producer Strain.

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7.  Conserved Mechanism of 2'-Phosphorylation-Aided Amide Ligation in Peptidyl Nucleoside Biosynthesis.

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  8 in total

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