Login / Signup

Polyether Cyclization Cascade Alterations in Response to Monensin Polyketide Synthase Mutations.

Sascha HeinrichMarius GroteSonja SieversSusanna KushnirFrank Schulz
Published in: Chembiochem : a European journal of chemical biology (2021)
The targeted manipulation of polyketide synthases has in recent years led to numerous new-to-nature polyketides. For type I polyketide synthases the response of post-polyketide synthases (PKS) processing enzymes onto the most frequently polyketide backbone manipulations is so far insufficiently studied. In particular, complex processes such as the polyether cyclisation in the biosynthesis of ionophores such as monensin pose interesting objects of research. We present here a study of the substrate promiscuity of the polyether cyclisation cascade enzymes in monensin biosynthesis in the conversion of redox derivatives of the nascent polyketide chain. LC-HRMS/MS2 -based studies revealed a remarkable flexibility of the post-PKS enzymes. They acted on derivatized polyketide backbones based on the three possible polyketide redox states within two different modules and gave rise to an altered polyether structure. One of these monensin derivatives was isolated and characterized by 2D-NMR spectroscopy, crystallography, and bioactivity studies.
Keyphrases
  • mass spectrometry
  • drug delivery
  • case control
  • high resolution
  • cancer therapy
  • amino acid