AUTHOR=Bratti Manuela , Vibhushan Shamila , Longé Cyril , Koumantou Despoina , Ménasché Gaël , Benhamou Marc , Varin-Blank Nadine , Blank Ulrich , Saveanu Loredana , Ben Mkaddem Sanae 

TITLE=Insulin-regulated aminopeptidase contributes to setting the intensity of FcR-mediated inflammation

JOURNAL=Frontiers in Immunology

VOLUME=13

YEAR=2022

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2022.1029759

DOI=10.3389/fimmu.2022.1029759

ISSN=1664-3224

ABSTRACT=<p>The function of intracellular trafficking in immune-complex triggered inflammation remains poorly understood. Here, we investigated the role of Insulin-Regulated Amino Peptidase (IRAP)-positive endosomal compartments in Fc receptor (FcR)-induced inflammation. Less severe FcγR-triggered arthritis, active systemic anaphylaxis and FcεRI-triggered passive systemic anaphylaxis were observed in IRAP-deficient <italic>versus</italic> wild-type mice. In mast cells FcεRI stimulation induced rapid plasma membrane recruitment of IRAP-positive endosomes. IRAP-deficient cells exhibited reduced secretory responses, calcium signaling and activating Syk<sup>Y519/520</sup> phosphorylation albeit receptor tyrosine phosphorylation on β and γ subunits was not different. By contrast, in the absence of IRAP, SHP1-inactivating phosphorylation on Ser<sup>591</sup> that controls Syk activity was decreased. <italic>Ex-vivo</italic> cell profiling after FcγR-triggered anaphylaxis confirmed decreased phosphorylation of both Syk<sup>Y519/520</sup> and SHP-1<sup>S591</sup> in IRAP-deficient neutrophils and monocytes. Thus, IRAP-positive endosomal compartments, in promoting inhibition of SHP-1 during FcR signaling, control the extent of phosphorylation events at the plasma membrane and contribute to setting the intensity of immune-complex triggered inflammatory diseases.</p>