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Rational design of new cyclic analogues of the antimicrobial lipopeptide tridecaptin A1.

Ross D BallantineYong-Xin LiPei-Yuan QianStephen A Cochrane
Published in: Chemical communications (Cambridge, England) (2018)
Non-ribosomal peptides (NRPs) are a rich source of antibiotic candidates. However, it was recently discovered that resistance to NRPs can be mediated by d-stereoselective peptidases. The tridecaptins, a class of NRPs that selectively target Gram-negative bacteria, are degraded by the d-peptidase TriF. Through analysis of a solution NMR structure of tridecaptin A1, we have rationally synthesized new cyclic tridecaptin analogues that retain strong antimicrobial activity and are resistant to TriF.
Keyphrases
  • molecular docking
  • solid state
  • magnetic resonance
  • structure activity relationship
  • staphylococcus aureus
  • high resolution
  • molecular dynamics simulations