Development of inflammation in proteoglycan-induced arthritis is dependent on Fc gamma R regulation of the cytokine/chemokine environment

FcgammaRs are specialized cell surface receptors that coordinately regulate immune responses. Although FcgammaR expression is a prerequisite for the development of several immune complex-mediated diseases, the mechanism responsible for FcgammaR-dependent regulation in autoimmunity remains unclear. T...

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Bibliographic Details
Published in:The Journal of immunology (1950) 2002-11, Vol.169 (10), p.5851-5859
Main Authors: Kaplan, Charles D, O'Neill, Shannon K, Koreny, Tamas, Czipri, Matyas, Finnegan, Alison
Format: Article
Language:English
Subjects:
Adult
Animals
Antibody Specificity - genetics
Antigen-Antibody Complex - metabolism
Antigens, CD - genetics
Arthritis, Experimental - genetics
Arthritis, Experimental - immunology
Arthritis, Experimental - pathology
Arthritis, Experimental - prevention & control
Autoantibodies - biosynthesis
Cartilage, Articular - immunology
Cartilage, Articular - pathology
Chemokines, CC - biosynthesis
Chemokines, CC - genetics
Cytokines - biosynthesis
Cytokines - genetics
Hindlimb
Humans
Inflammation - genetics
Inflammation - immunology
Inflammation - prevention & control
Lymphocyte Activation - genetics
Mice
Mice, Inbred BALB C
Mice, Knockout
Mice, SCID
Proteoglycans - administration & dosage
Proteoglycans - immunology
Proteoglycans - pharmacology
Receptors, IgG - deficiency
Receptors, IgG - genetics
Receptors, IgG - metabolism
Receptors, IgG - physiology
RNA, Messenger - biosynthesis
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Summary:FcgammaRs are specialized cell surface receptors that coordinately regulate immune responses. Although FcgammaR expression is a prerequisite for the development of several immune complex-mediated diseases, the mechanism responsible for FcgammaR-dependent regulation in autoimmunity remains unclear. Therefore, we assessed FcgammaR-dependent regulation of inflammation in proteoglycan-induced arthritis (PGIA) using FcgammaR(-/-) mice. FcgammaRIIb(-/-) mice developed arthritis at an earlier time point and with a greater severity than wild-type (WT) mice. In gamma-chain(-/-) (FcgammaRI(-/-) and FcgammaRIII(-/-)) mice, no clinical or histological evidence of inflammation was observed. Exacerbation of arthritis in FcgammaRIIb(-/-) mice correlated with enhanced PG-specific Ab production, but did not significantly affect PG-specific T cell priming. In gamma-chain(-/-) mice, the absence of arthritis did not correlate with serum Ab responses, as PG-specific Ab production was normal. Although PG-specific T cell proliferation was diminished, spleen cells from gamma-chain(-/-) mice successfully adoptively transferred arthritis into SCID mice. Our studies indicated that the mechanism responsible for FcgammaR regulation of PGIA development was at the level of inflammatory cytokine and beta-chemokine expression within the joint. FcgammaRIIb regulated the development of PGIA by controlling the initiation of cytokine and chemokine expression within the joint before the onset of arthritis, whereas the expression of FcgammaRI and or FcgammaRIII controlled cytokine and chemokine expression late in the development of PGIA during the onset of disease. These results suggest that FcgammaRs are critical for the development of inflammation during PGIA, possibly by maintaining or enhancing inflammatory cytokine and beta-chemokine production.
ISSN:0022-1767
1550-6606
DOI:10.4049/jimmunol.169.10.5851