1. Academic Validation
  2. Peptidomimetic analogues of an Arg-Trp-x-x-Trp motif responsible for interaction of translocase MraY with bacteriophage ϕX174 lysis protein E

Peptidomimetic analogues of an Arg-Trp-x-x-Trp motif responsible for interaction of translocase MraY with bacteriophage ϕX174 lysis protein E

  • Bioorg Med Chem. 2021 Dec 15;52:116502. doi: 10.1016/j.bmc.2021.116502.
Rachel V Kerr 1 Julia A Fairbairn 1 Andrew T Merritt 2 Timothy D H Bugg 3
Affiliations

Affiliations

  • 1 Department of Chemistry, University of Warwick, Coventry CV4 7AL, UK.
  • 2 LifeArc, SBC Open Innovation Campus, Stevenage, Herts SG1 2FX, UK.
  • 3 Department of Chemistry, University of Warwick, Coventry CV4 7AL, UK. Electronic address: T.D.Bugg@warwick.ac.uk.
Abstract

Translocase MraY is the target for bacteriophage ϕX174 lysis protein E, which interacts via a protein-protein interaction mediated by Phe-288 and Glu-287 of E. coli MraY, and an Arg-Trp-x-x-Trp motif on protein E, also found in several cationic antimicrobial Peptides. Analogues of Arg-Trp-octyl ester, found previously to show antimicrobial activity, were tested for antimicrobial activity, with Lys-Trp-oct (MIC50P. fluorescens 5 µg/mL) and Arg-Trp-decyl ester (MIC50P. fluorescens 3 µg/mL) showing enhanced antimicrobial activity. Synthesis and testing of α-helix peptidomimetic analogues for this motif revealed improved Antibacterial activity (MIC50E. coli 4-7 µg/mL) for analogues containing two aromatic substituents, mimicking the Arg-Trp-x-x-Trp motif, and MraY inhibition (IC50 140 µM) by one such peptidomimetic. Investigation of mechanism of action using the Alamar Blue membrane permeabilisation assay revealed bacteriostatic and bacteriocidal mechanisms in different members of this set of compounds, raising the possibility of more than one biological target. The observed antimicrobial activity and MraY inhibition shown by peptidomimetic compounds confirms that this site could be targeted by drug-like molecules.

Keywords

Antibacterial; Antimicrobial peptide; Peptidomimetic; Protein–protein interaction; translocase MraY.

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