An important feature of the role of
IgA in protection against
infection and disease at the level of the mucosal surfaces might be the elimination of pathogens without induction of a strong inflammatory reaction. In the present study we addressed the question whether
IgA has a regulatory effect on the generation of
reactive oxygen intermediates in human neutrophils and monocytes (i.e. the respiratory burst). Cells were stimulated with heat-inactivated Haemophilus influenzae type b or
phorbol myristate acetate, stimuli known to use different recognition structures or signal transduction pathways. Concentrations of
IgA as low as 10 mg/L significantly inhibited the receptor-dependent Haemophilus influenzae-induced respiratory burst in granulocytes, as assessed by measuring
luminol-enhanced chemiluminescence. Furthermore,
IgA had a dose-dependent inhibitory effect on the receptor-independent induction of the respiratory burst, as examined by flow cytometry in monocytes and granulocytes activated with
phorbol myristate acetate. Our results therefore indicate that inhibition of receptor-
ligand interaction is not a sufficient explanation for the
IgA-mediated modulation of the respiratory burst in human phagocytic cells. In addition,
IgA might directly regulate the activation of the respiratory burst at the level or downstream of
protein kinase C activation. By modulating the release of
mediators of inflammation such as
reactive oxygen intermediates, the inflammatory response could be down-regulated at the level of the mucosal surfaces, thereby preventing the development of sequelae of an exaggerated inflammatory response potentially leading to local or systemic pathology.