Litcius/Paper detail

Antimicrobial peptide activity in asymmetric bacterial membrane mimics

Lisa Marx, Moritz P. K. Frewein, Enrico F. Semeraro, Gerald N. Rechberger, Karl Lohner, Lionel Porcar, Georg Pabst

2021Faraday Discussions23 citationsDOIOpen Access PDF

Abstract

We report on the response of asymmetric lipid membranes composed of palmitoyl oleoyl phosphatidylethanolamine and palmitoyl oleoyl phosphatidylglycerol, to interactions with the frog peptides L18W-PGLa and magainin 2 (MG2a), as well as the lactoferricin derivative LF11-215. In particular we determined the peptide-induced lipid flip-flop, as well as membrane partitioning of L18W-PGLa and LF11-215, and vesicle dye-leakage induced by L18W-PGLa. The ability of L18W-PGLa and MG2a to translocate through the membrane appears to correlate with the observed lipid flip-flop, which occurred at the fastest rate for L18W-PGLa. The higher structural flexibility of LF11-215 in turn allows this peptide to insert into the bilayers without detectable changes of membrane asymmetry. The increased vulnerability of asymmetric membranes to L18W-PGLa in terms of permeability, appears to be a consequence of tension differences between the compositionally distinct leaflets, but not due to increased peptide partitioning.

Topics & Concepts

MagaininMembranePeptidePhosphatidylglycerolChemistryBiophysicsPhosphatidylethanolamineLipid bilayerVesicleMembrane lipidsAntimicrobial peptidesBiochemistryPhospholipidBiologyPhosphatidylcholineAntimicrobial Peptides and ActivitiesLipid Membrane Structure and BehaviorBiochemical and Structural Characterization