CD69 downregulates autoimmune reactivity through active transforming growth factor-β production in collagen-induced arthritis
David Sancho, … , Pilar Lauzurica, Francisco Sánchez-Madrid
David Sancho, … , Pilar Lauzurica, Francisco Sánchez-Madrid
Published September 15, 2003
Citation Information: J Clin Invest. 2003;112(6):872-882. https://doi.org/10.1172/JCI19112.
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Article Immunology

CD69 downregulates autoimmune reactivity through active transforming growth factor-β production in collagen-induced arthritis

Abstract

CD69 is induced after activation of leukocytes at inflammatory sites, but its physiological role during inflammation remains unknown. We explored the role of CD69 in autoimmune reactivity by analyzing a model of collagen-induced arthritis (CIA) in WT and CD69-deficient mice. CD69–/– mice showed higher incidence and severity of CIA, with exacerbated T and B cell immune responses to type II collagen. Levels of TGF-β1 and TGF-β2, which act as protective agents in CIA, were reduced in CD69–/– mice inflammatory foci, correlating with the increase in the proinflammatory cytokines IL-1β and RANTES. Local injection of blocking anti–TGF-β antibodies increased CIA severity and proinflammatory cytokine mRNA levels in CD69+/+ but not in CD69–/– mice. Moreover, in vitro engagement of CD69 induced total and active TGF-β1 production in Concanavalin A–activated splenocyte subsets, mouse and human synovial leukocytes, and Jurkat stable transfectants of human CD69 but not in the parental CD69 negative cell line. Our results show that CD69 is a negative modulator of autoimmune reactivity and inflammation through the synthesis of TGF-β, a cytokine that in turn downregulates the production of various proinflammatory mediators.

Authors

David Sancho, Manuel Gómez, Fernando Viedma, Enric Esplugues, Mónica Gordón-Alonso, María Angeles García-López, Hortensia de la Fuente, Carlos Martínez-A, Pilar Lauzurica, Francisco Sánchez-Madrid

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Local cytokine analysis in joints and purified leukocyte synovial cells ...
Local cytokine analysis in joints and purified leukocyte synovial cells from CII-immunized CD69–/– mice. (a) Real-time quantitative RT-PCR analysis of mRNA from CD69+/+ (white bars) and CD69–/– (black bars) mouse hind paws. Each bar represents the arithmetic mean ± SD of 12 mice per group in two independent experiments. Results for each cytokine are normalized to GAPDH expression measured in parallel in each sample. *P < 0.01 versus CD69+/+ (Mann-Whitney U test). (b) Levels of active and total TGF-β1, IL-1β, TNF-α, and RANTES in synovial washouts from CIA CD69+/+ (white bars) and CD69–/– (black bars) mice. Data correspond to the arithmetic mean ± SD of three independent experiments (six mice per group per experiment). *P < 0.01 versus CD69+/+ (Mann-Whitney U test). (c) Quantitative RT-PCR analysis of mRNA from CD69+/+ (white bars) and CD69–/– (black bars) purified subsets of synovial cells. Each histogram represents the arithmetic mean ± SD of 12 mice per group in two independent experiments. Results of each cytokine are normalized to GAPDH expression measured in parallel in each sample. *P < 0.01 versus CD69+/+ (Mann-Whitney U test).