Effects of Staphylococcus aureus -hemolysin A on calcium signalling in immortalized human airway epithelial cells

Abstract Part of the innate defence of bronchial epithelia against bacterial colonization is secretion of salt and water which generally depends on coordinated actions of receptor-mediated cAMP- and calcium signalling. The hypothesis that Staphylococcus aureus -virulence factors interfere with endog...

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Veröffentlicht in:Cell calcium (Edinburgh) 2009-02, Vol.45 (2), p.165-176
Hauptverfasser: Eichstaedt, Stefanie, Gäbler, Karoline, Below, Sabine, Müller, Christian, Kohler, Christian, Engelmann, Susanne, Hildebrandt, Petra, Völker, Uwe, Hecker, Michael, Hildebrandt, Jan-Peter
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Sprache:eng
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Zusammenfassung:Abstract Part of the innate defence of bronchial epithelia against bacterial colonization is secretion of salt and water which generally depends on coordinated actions of receptor-mediated cAMP- and calcium signalling. The hypothesis that Staphylococcus aureus -virulence factors interfere with endogenous signals in host cells was tested by measuring agonist-mediated changes in [Ca2+ ]i in S9 cells upon pre-incubation with bacterial secretory products. S9 cells responded to mAChR-activation with calcium release from intracellular stores and capacitative calcium influx. Treatment of cells with culture supernatants of S. aureus (COL) or with recombinant α-hemolysin (Hla) resulted in time- and concentration-dependent changes in [Ca2+ ]i . High concentrations of Hla (2000 ng/ml) resulted in elevations in [Ca2+ ]i elicited by accelerated calcium influx. A general Hla-mediated permeabilization of S9 cell membranes to small molecules, however, did not occur. Lower concentrations of Hla (200 ng/ml) induced a reduction in [Ca2+ ]i -levels during the sustained plateau phase of receptor-mediated calcium signalling which was abolished by pre-incubation of cells with carboxyeosin, an inhibitor of the plasma membrane calcium-ATPase. This indicates that low concentrations of Hla change calcium signalling by accelerating pump-driven extrusion of Ca2+ ions. In vivo , such a mechanism may result in attenuation of calcium-mediated cellular defence functions and facilitation of bacterial adherence to the bronchial epithelium.
ISSN:0143-4160
1532-1991
DOI:10.1016/j.ceca.2008.09.001