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J Immunol 2015 Feb 1;194(3):983-9

Immune Complexes Suppress IFN-gamma-Induced Responses in Monocytes by Activating Discrete Members of the SRC Kinase Family.

Boekhoudt GH, McGrath AG, Swisher JF, Feldman GM

Abstract

The regulation of the innate and the adaptive immune responses are extensively intertwined and tightly regulated. Ag-driven immune responses that are modulated by immune complexes (ICs) are known to inhibit IFN-gamma-dependent MHC class II expression. We have previously demonstrated that ICs dramatically inhibit IFN-gamma-induced activation of human monocytes through the activation of the FcgammaRI signaling pathway. In the present study we further explore the mechanisms by which ICs regulate IFN-gamma activation of human monocytes. We demonstrate that members of the SRC kinase family (SKF) are key mediators of IFN-gamma pathway suppression: inhibitors of the SKF reverse the ability of ICs to suppress IFN-gamma signaling. Small interfering RNA was used to target specific members of the SKF. The data indicate that SRC and LYN are both required for ICs to elicit their immunosuppressive activity, whereas FYN does not appear to contribute to this function. Similarly, the kinase SYK, though not a member of the SKF, is also demonstrated to be involved in this IC-mediated immunosuppression. Our data suggest a mechanism whereby ICs directly inhibit inflammatory signals by crosslinking FcgammaRI, resulting in the activation of the specific phosphotyrosine kinases SRC, LYN, and SYK and the concomitant suppression of the IFN-gamma signaling pathway.


Category: Journal Article
PubMed ID: #25512601
Includes FDA Authors from Scientific Area(s): Drugs
Entry Created: 2014-12-17 Entry Last Modified: 2015-02-21
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