4.7 Review

Employing the promiscuity of lantibiotic biosynthetic machineries to produce novel antimicrobials

Journal

FEMS MICROBIOLOGY REVIEWS
Volume 41, Issue 1, Pages 5-18

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/femsre/fuw034

Keywords

RiPPs: ribosomally produced and post-translationally modified peptides; PTM: post-translational modifications; lantibiotics; antimicrobial

Categories

Funding

  1. Aard- een Levenswetenschappen-Nederlandse Organisatie voor Weternschappelijk Onderzoek ALW-NWO project SynMod [855.01.162]
  2. EU FW7 SynPeptide
  3. Nederlandse Organisatie voor Wetenschappelijk Onderzoek-Stichting voor de Technische Wetenschappen NWO-STW program GenBiotics [10466]

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As the number of new antibiotics that reach the market is decreasing and the demand for them is rising, alternative sources of novel antimicrobials are needed. Lantibiotics are potent peptide antimicrobials that are ribosomally synthesized and stabilized by post-translationally introduced lanthionine rings. Their ribosomal synthesis and enzymatic modifications provide excellent opportunities to design and engineer a large variety of novel antimicrobial compounds. The research conducted in this area demonstrates that the modularity present in both the peptidic rings as well as in the combination of promiscuous modification enzymes can be exploited to further increase the diversity of lantibiotics. Various approaches, where the modifying enzymes and corresponding leader peptides are decoupled from their natural core peptide and integrated in designed plug-and-play production systems, enable the production of modified peptides that are either derived from vast genomic data or designed using functional parts from a wide diversity of core peptides. These approaches constitute a powerful discovery platform to develop novel antimicrobials with high therapeutic potential.

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