Mechanism of a Prototypical Synthetic Membrane-Active Antimicrobial: Efficient Hole-Punching Via Interaction With Negative Intrinsic Curvature Lipids

Yang, L; Gordon, V D; Trinkle, D R; Schmidt, N W; Davis, M A; DeVries, C; Som, A; Cronan, Jr, J E; Tew, G N; Wong, G C.L.

Title: Mechanism of a Prototypical Synthetic Membrane-Active Antimicrobial: Efficient Hole-Punching Via Interaction With Negative Intrinsic Curvature Lipids

Journal Article · Thu May 28 00:00:00 EDT 2009 · Proc. Nat. Acad. Sci. 105:20595,2008

OSTI ID:953515

Yang, L; Gordon, V D; Trinkle, D R; Schmidt, N W; Davis, M A; DeVries, C; Som, A; Cronan, Jr, J E; Tew, G N; Wong, G C.L.

Phenylene ethynylenes comprise a prototypical class of synthetic antimicrobial compounds that mimic antimicrobial peptides produced by eukaryotes and have broad-spectrum antimicrobial activity. We show unambiguously that bacterial membrane permeation by these antimicrobials depends on the presence of negative intrinsic curvature lipids, such as phosphatidylethanolamine (PE) lipids, found in high concentrations within bacterial membranes. Plate-killing assays indicate that a PE-knockout mutant strain of Escherichia coli drastically out-survives the wild type against the membrane-active phenylene ethynylene antimicrobials, whereas the opposite is true when challenged with traditional metabolic antibiotics. That the PE deletion is a lethal mutation in normative environments suggests that resistant bacterial strains do not evolve because a lethal mutation is required to gain immunity. PE lipids allow efficient generation of negative curvature required for the circumferential barrel of an induced membrane pore; an inverted hexagonal HII phase, which consists of arrays of water channels, is induced by a small number of antimicrobial molecules. The estimated antimicrobial occupation in these water channels is nonlinear and jumps from {approx}1 to 3 per 4 nm of induced water channel length as the global antimicrobial concentration is increased. By comparing to exactly solvable 1D spin models for magnetic systems, we quantify the cooperativity of these antimicrobials.

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Research Organization:: SLAC National Accelerator Lab., Menlo Park, CA (United States)

Sponsoring Organization:: USDOE

DOE Contract Number:: AC02-76SF00515

OSTI ID:: 953515

Report Number(s):: SLAC-REPRINT-2009-368; PNASA6; TRN: US201002%%1343

Journal Information:: Proc. Nat. Acad. Sci. 105:20595,2008, Vol. 105, Issue 52; ISSN 0027-8424

Country of Publication:: United States

Language:: English

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60 APPLIED LIFE SCIENCES
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MOLECULES
MUTANTS
PEPTIDES
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OTHER
CHEM

Title: Mechanism of a Prototypical Synthetic Membrane-Active Antimicrobial: Efficient Hole-Punching Via Interaction With Negative Intrinsic Curvature Lipids

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