Antimycotic activity of fengycin C biosurfactant and its interaction with phosphatidylcholine model membranes

Lipopeptide biosurfactants constitute one of the most promising groups of compounds for the treatment and prevention of fungal diseases in plants. Bacillus subtilis strain EA-CB0015 produces iturin A, fengycin C and surfactin and it has been proven useful for the treatment of black Sigatoka disease...

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Veröffentlicht in:Colloids and surfaces, B, Biointerfaces B, Biointerfaces, 2017-08, Vol.156, p.114-122
Hauptverfasser: González-Jaramillo, Lina María, Aranda, Francisco José, Teruel, José Antonio, Villegas-Escobar, Valeska, Ortiz, Antonio
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container_start_page 114
container_title Colloids and surfaces, B, Biointerfaces
container_volume 156
creator González-Jaramillo, Lina María
Aranda, Francisco José
Teruel, José Antonio
Villegas-Escobar, Valeska
Ortiz, Antonio
description Lipopeptide biosurfactants constitute one of the most promising groups of compounds for the treatment and prevention of fungal diseases in plants. Bacillus subtilis strain EA-CB0015 produces iturin A, fengycin C and surfactin and it has been proven useful for the treatment of black Sigatoka disease in banana plants, an important pathology caused by the fungus Mycosphaerella fijiensis (Morelet). We have found that B. subtilis EA-CB0015 cell free supernatants and purified fractions inhibit M. fijiensis cellular growth. The effect of the purified lipopeptides mentioned above on fungal growth has been also evaluated, observing that iturin A and fengycin C inhibit mycelial growth and ascospore germination, whereas surfactin is not effective. On the hypothesis that the antifungal action of the lipopeptides is associated to their incorporation into biological membranes, ultimately leading to membrane permeabilization, a detailed biophysical study on the interaction of a new isoform of fengycin C with model dipalmitoyphosphatidylcholine (DPPC) membranes has been carried out. Differential scanning calorimetry shows that fengycin C alters the thermotropic phase transitions of DPPC, and is laterally segregated in the fluid bilayer forming domains. Fluorescent probe polarization measurements show that fengycin C does not affect the hydrophobic interior of the membrane. This latter perturbation is concomitant with a strong dehydration of the polar region of DPPC, as shown by FTIR. Fengycin-rich domains, where the surrounding DPPC molecules are highly dehydrated, may well constitute sites of membrane permeabilization leading to a leaky target membrane. These results are a solid support to explain the membrane perturbing action of fengycin, which has been related to its antifungal activity.
doi_str_mv 10.1016/j.colsurfb.2017.05.021
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Differential scanning calorimetry shows that fengycin C alters the thermotropic phase transitions of DPPC, and is laterally segregated in the fluid bilayer forming domains. Fluorescent probe polarization measurements show that fengycin C does not affect the hydrophobic interior of the membrane. This latter perturbation is concomitant with a strong dehydration of the polar region of DPPC, as shown by FTIR. Fengycin-rich domains, where the surrounding DPPC molecules are highly dehydrated, may well constitute sites of membrane permeabilization leading to a leaky target membrane. 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subjects Fungi - drug effects
Fungi - growth & development
Lipopeptides - chemistry
Lipopeptides - pharmacology
Membranes, Artificial
Microbial Sensitivity Tests
Phosphatidylcholines - chemistry
Surface-Active Agents - chemistry
Surface-Active Agents - pharmacology
title Antimycotic activity of fengycin C biosurfactant and its interaction with phosphatidylcholine model membranes
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