AI Article Synopsis

  • Researchers discovered a new polyketide, NOCAP, from strains linked to nocardiosis using a reconstituted polyketide synthase (PKS).
  • The structure of the NOCAP aglycone features a unique resorcylaldehyde headgroup and a 15-carbon tail with multiple conjugated all-trienes.
  • This work marks the first successful reconstitution of a -acyltransferase assembly line PKS and helps clarify how this compound might benefit the bacteria during human infections.

Article Abstract

Several strains associated with nocardiosis, a potentially life-threatening disease, house a nonamodular assembly line polyketide synthase (PKS) that presumably synthesizes an unknown polyketide. Here, we report the discovery and structure elucidation of the NOCAP (nocardiosis-associated polyketide) aglycone by first fully reconstituting the NOCAP synthase from purified protein components followed by heterologous expression in and spectroscopic analysis of the purified products. The NOCAP aglycone has an unprecedented structure comprised of a substituted resorcylaldehyde headgroup linked to a 15-carbon tail that harbors two conjugated all- trienes separated by a stereogenic hydroxyl group. This report is the first example of reconstituting a -acyltransferase assembly line PKS and of using these approaches to "deorphanize" a complete assembly line PKS identified via genomic sequencing. With the NOCAP aglycone in hand, the stage is set for understanding how this PKS and associated tailoring enzymes confer an advantage to their native hosts during human infections.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7329362PMC
http://dx.doi.org/10.1021/jacs.0c00904DOI Listing

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