The Ubiquitin Ligase c-Cbl Down-Regulates FcγRIIa Activation in Human Neutrophils

Little is known about the mechanisms that arrest Fc-gamma RIIa signaling in human neutrophils once engaged by immune complexes or opsonized pathogens. In our previous studies, we observed a loss of immunoreactivity of Abs directed against Fc gamma RIIa following its cross-linking. In this study, we report on the mechanisms involved in this event. A stimulated internalization of Fc gamma RIIa leading to the down-regulation of its surface expression was observed by How cytometry and confocal microscopy. Immunoprecipitation of the receptor showed that Fc gamma RIIa is ubiquitinated after stimulation. MG132 and clasto-lactacystin beta-lactone inhibited the loss of immunoreactivity of Fc gamma RIIa, suggesting that this receptor was down-regulated via the proteasomal pathway. The E3 ubiquitin ligase c-Cbl was found to translocate from the cytosol to the plasma membrane following receptor cross-linking. Furthermore, c-Cbl was recruited to the same subset of high-density, detergent-resistant membrane fractions as stimulated Fc gamma RIIa itself. Silencing the expression of c-Cbl by small interfering RNA decreased Fc gamma RIIa ubiquitination and prevented its degradation without affecting the internalisation process. It also prolonged the stimulation of the tyrosine phosphorylation response to the cross-linking of the receptor. We conclude that c-Cbl mediates the ubiquitination of stimulated Fc gamma RIIa and thereby contributes to the termination of Fc gamma RIIa signaling via its proteasomal degradation, thus leading to the down-regulation of neutrophil signalisation and function (phagocytosis) through this receptor. The Journal of Immunology, 2009, 182: 2374-2384.