AI Article Synopsis

  • Nonribosomal peptide synthetases (NRPSs) make unique chemical products by adding special parts called tailoring domains.
  • A specific type of these enzymes, called linear gramicidin synthetase, starts with a special formylation domain that may have come from a sugar-related gene.
  • Scientists studied a sugar formyltransferase (FT) from Anoxybacillus kamchatkensis and found out how it creates a new compound, using advanced techniques like gene analysis and X-ray crystallography to understand how this enzyme has changed over time to work as part of NRPS.

Article Abstract

Nonribosomal peptide synthetases (NRPSs) increase the chemical diversity of their products by acquiring tailoring domains. Linear gramicidin synthetase starts with a tailoring formylation (F) domain, which likely originated from a sugar formyltransferase (FT) gene. Here, we present studies on an Anoxybacillus kamchatkensis sugar FT representative of the prehorizontal gene transfer FT. Gene cluster analysis reveals that this FT acts on a UDP-sugar in a novel pathway for synthesis of a 7-formamido derivative of CMP-pseudaminic acid. We recapitulate the pathway up to and including the formylation step in vitro, experimentally demonstrating the role of the FT. We also present X-ray crystal structures of the FT alone and with ligands, which unveil contrasts with other structurally characterized sugar FTs and show close structural similarity with the F domain. The structures reveal insights into the adaptations that were needed to co-opt and evolve a sugar FT into a functional and useful NRPS domain.

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Source
http://dx.doi.org/10.1021/acschembio.8b00739DOI Listing

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