Molecules (Feb 2019)

Structure-Function Studies of Polymyxin B Lipononapeptides

  • Alejandra Gallardo-Godoy,
  • Karl A. Hansford,
  • Craig Muldoon,
  • Bernd Becker,
  • Alysha G. Elliott,
  • Johnny X. Huang,
  • Ruby Pelingon,
  • Mark S. Butler,
  • Mark A. T. Blaskovich,
  • Matthew A. Cooper

DOI
https://doi.org/10.3390/molecules24030553
Journal volume & issue
Vol. 24, no. 3
p. 553

Abstract

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The emerging threat of infections caused by highly drug-resistant bacteria has prompted a resurgence in the use of the lipodecapeptide antibiotics polymyxin B and colistin as last resort therapies. Given the emergence of resistance to these drugs, there has also been a renewed interest in the development of next generation polymyxins with improved therapeutic indices and spectra of action. We report structure-activity studies of 36 polymyxin lipononapeptides structurally characterised by an exocyclic FA-Thr2-Dab3 lipodipeptide motif instead of the native FA-Dab1-Thr2-Dab3 tripeptide motif found in polymyxin B, removing one of the positively charged residues believed to contribute to nephrotoxicity. The compounds were prepared by solid phase synthesis using an on-resin cyclisation approach, varying the fatty acid and the residues at position 2 (P2), P3 and P4, then assessing antimicrobial potency against a panel of Gram-negative bacteria, including polymyxin-resistant strains. Pairwise comparison of N-acyl nonapeptide and decapeptide analogues possessing different fatty acids demonstrated that antimicrobial potency is strongly influenced by the N-terminal L-Dab-1 residue, contingent upon the fatty acid. This study highlights that antimicrobial potency may be retained upon truncation of the N-terminal L-Dab-1 residue of the native exocyclic lipotripeptide motif found in polymyxin B. The strategy may aid in the design of next generation polymyxins.

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