Detergent-Like Activity and α-Helical Structure of Warnericin RK, an Anti- Legionella Peptide
Warnericin RK is the first antimicrobial peptide known to be active against Legionella pneumophila, a pathogen bacterium that is responsible for severe pneumonia. Strikingly, this peptide displays a very narrow range of antimicrobial activity, almost limited to the Legionella genus, and a hemolytic...
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Veröffentlicht in: | Biophysical journal 2009-10, Vol.97 (7), p.1933-1940 |
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Sprache: | eng |
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Zusammenfassung: | Warnericin RK is the first antimicrobial peptide known to be active against
Legionella pneumophila, a pathogen bacterium that is responsible for severe pneumonia. Strikingly, this peptide displays a very narrow range of antimicrobial activity, almost limited to the
Legionella genus, and a hemolytic activity. A similar activity has been described for
δ-lysin, a well-known hemolytic peptide of
Staphylococci that has not been described as antimicrobial. In this study we aimed to understand the mode of action of warnericin RK and to explain its particular target specificity. We found that warnericin RK permeabilizes artificial membranes in a voltage-independent manner. Osmotic protection experiments on erythrocytes showed that warnericin RK does not form well-defined pores, suggesting a detergent-like mode of action, as previously described for
δ-lysin at high concentrations. Warnericin RK also permeabilized
Legionella cells, and these cells displayed a high sensitivity to detergents. Depending on the detergent used,
Legionella was from 10- to 1000-fold more sensitive than the other bacteria tested. Finally, the structure of warnericin RK was investigated by means of circular dichroism and NMR spectroscopy. The peptide adopted an amphiphilic
α-helical structure, consistent with the proposed mode of action. We conclude that the specificity of warnericin RK toward
Legionella results from both the detergent-like mode of action of the peptide and the high sensitivity of these bacteria to detergents. |
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ISSN: | 0006-3495 1542-0086 |
DOI: | 10.1016/j.bpj.2009.06.053 |