Ingestion of opsonized pathogens by professional phagocytes results in the generation and release of microbicidal products that are essential for normal host defense. Because these products can result in significant tissue injury, phagocytosis must be regulated to limit damage to the host while allowing for optimal clearance and destruction of opsonized pathogens. To pursue negative regulation of phagocytosis, we assessed the effect of the Src kinase family member, Fgr, on opsonin-dependent phagocytosis by mouse macrophages. We chose Fgr because it is present in high concentrations in circulating phagocytes but is not essential for Fcγ receptor–mediated ingestion by mouse macrophages. Although expression of Fgr both in a macrophage cell line and in primary macrophages significantly attenuates ingestion mediated by Fcγ receptors and CR3, it does not affect macropinocytosis or receptor-mediated endocytosis. This selective effect of Fgr is independent of its tyrosine kinase function. After Fcγ receptor cross-linking, Fgr becomes associated with the immunoreceptor tyrosine-based inhibition motif (ITIM)–containing receptor, SIRPα (a member of the signal-regulatory protein family, also known as Src homology 2 domain–containing protein tyrosine phosphatase [SHP] substrate 1 [SHPS-1], brain immunoglobulin-like molecule with tyrosine-based activation motifs [BIT], and P84) and potentiates the association of the phosphatase SHP-1 with SIRPα. This association is responsible, at least in part, for decreasing positive signaling essential for optimal phagocytosis. These data demonstrate an important negative regulatory role for this Src kinase family member and suggest that this homeostatic function must be overcome for optimal uptake and clearance of opsonized pathogens.
Negative Regulation of Phagocytosis in Murine Macrophages by the Src Kinase Family Member, Fgr
Abbreviations used in this paper: AI, attachment index; CSF-1, colony stimulating factor 1; ECL, enhanced chemiluminescence; EC3bi, EIgG2a, EIgG2b, and EIgGr, C3bi-, IgG2a-, IgG2b-, and rabbit IgG–opsonized erythrocyte(s); HRP, horseradish peroxidase; HSA, human serum albumin; IAP, integrin-associated protein; ITIM, immunoreceptor tyrosine-based inhibition motif; LCM, L cell–conditioned medium; MCF, mean channel of fluorescence; PDBu, phorbol dibutyrate; PECAM-1, platelet-endothelial cell adhesion molecule 1; PI, phagocytic index; PI 3-kinase, phosphatidylinositol 3-kinase; PIR-B, paired Ig-like receptor B; SH, Src homology; SHP, SH2 domain–containing protein tyrosine phosphatase; SIRPα, signal regulatory protein of the α subtype; VBS, veronal-buffered saline.
Hattie D. Gresham, Benjamin M. Dale, Jeffrey W. Potter, Peter W. Chang, Charlotte M. Vines, Clifford A. Lowell, Carl F. Lagenaur, Cheryl L. Willman; Negative Regulation of Phagocytosis in Murine Macrophages by the Src Kinase Family Member, Fgr. J Exp Med 7 February 2000; 191 (3): 515–528. doi: https://doi.org/10.1084/jem.191.3.515
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