Bacterial species selective toxicity of two isomeric / -peptides: Role of membrane lipids

We have studied how membrane interactions of two synthetic cationic antimicrobial peptides with alternating - and -amino acid residues (" / -peptides") impact toxicity to different prokaryotes. Electron microscopic examination of thin sections of Escherichia coli and of Bacillus subtilis e...

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Bibliographic Details
Published inMolecular membrane biology Vol. 22; no. 6; pp. 457 - 469
Main Authors Epand, Raquel F., Schmitt, Margaret A., Gellman, Samuel H., Sen, Arindam, Auger, Michèle, Hughes, Donald W., Epand, Richard M.
Format Journal Article
LanguageEnglish
Published Informa UK Ltd 2005
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Summary:We have studied how membrane interactions of two synthetic cationic antimicrobial peptides with alternating - and -amino acid residues (" / -peptides") impact toxicity to different prokaryotes. Electron microscopic examination of thin sections of Escherichia coli and of Bacillus subtilis exposed to these two / -peptides reveals different structural changes in the membranes of these bacteria. These two peptides also have very different effects on the morphology of liposomes composed of phosphatidylethanolamine and phosphatidylglycerol in a 2:1 molar ratio. Freeze fracture electron microscopy indicates that with this lipid mixture, / -peptide I induces the formation of a sponge phase. 31P NMR and X-ray diffraction are consistent with this conclusion. In contrast, with / -peptide II and this same lipid mixture, a lamellar phase is maintained, but with a drastically reduced d-spacing. / -Peptide II is more lytic to liposomes composed of these lipids than is I. These findings are consistent with the greater toxicity of / -peptide II, relative to / -peptide I, to E. coli, a bacterium having a high content of phosphatidylethanolamine. In contrast, both / -peptides display similar toxicity toward B. subtilis, in accord with the greater anionic lipid composition in its membrane. This work shows that variations in the selectivity of these peptidic antimicrobial peptides toward different strains of bacteria can be partly determined by the lipid composition of the bacterial cell membrane.
ISSN:0968-7688
1464-5203
DOI:10.1080/09687860500370562