Effect of Antimicrobial Peptides Divergicin M35 and Nisin A on <Emphasis Type="Italic">Listeria monocytogenes</Emphasis> LSD530 Potassium Channels

The aim of this work was to study the effect of antimicrobial peptides: divergicin M35 and nisin A on Listeria monocytogenes LSD 530 potassium (K⁺) channels: ATP-sensitive (K_ATP), calcium-activated (BK_Ca), and depolarization-activated (K_v) types. Increase on K⁺ efflux and inhibition of cellular growth were observed after adding K⁺ channel activators pinacidil, NS1619, and cromakalim to divergicin M35. Increase in K⁺ efflux from log-phase cells was about 18 ± 1.1, 11 ± 0.63, and nmol mg⁻¹ of cell dry weight (CDW) for pinacidil and NS1619, respectively, over the efflux obtained with divergicin M35 alone. Increases in K⁺ efflux obtained by adding the same K⁺ channel activators to nisin A fit a completely different profile. Divergicin M35 activates K⁺ channels, particularly of the K_v and BK_Ca types and to a lesser extent the K_ATP type, causing K⁺ efflux and consequently cell death.