B cells expressing IFN‐γ suppress Treg‐cell differentiation and promote autoimmune experimental arthritis |
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| Authors: | Susan A. Olalekan Yanxia Cao Keith M. Hamel Alison Finnegan |
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| Affiliation: | 1. Department of Immunology/Microbiology, Rush University Medical Center, Cohn Research Building, Chicago, IL, USA;2. Department of Internal Medicine, Division of Rheumatology, Rush University Medical Center, Cohn Research Building, Chicago, IL, USA;3. Department of Medicine, Section of Rheumatology, Gwen Knapp Center for Lupus and Immunology Research, The University of Chicago, Chicago, IL, USA |
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| Abstract: | ![]()
Clinical efficacy in the treatment of rheumatoid arthritis with anti‐CD20 (Rituximab)‐mediated B‐cell depletion has garnered interest in the mechanisms by which B cells contribute to autoimmunity. We have reported that B‐cell depletion in a murine model of proteoglycan‐induced arthritis (PGIA) leads to an increase in Treg cells that correlate with decreased autoreactivity. Here, we demonstrate that the increase in Treg cells after B‐cell depletion is due to an increase in the differentiation of naïve CD4+ T cells into Treg cells. Since the development of PGIA is dependent on IFN‐γ and B cells are reported to produce IFN‐γ, we hypothesized that B‐cell‐specific IFN‐γ plays a role in the development of PGIA. Accordingly, mice with B‐cell‐specific IFN‐γ deficiency were as resistant to the induction of PGIA as mice that were completely IFN‐γ deficient. Importantly, despite a normal frequency of IFN‐γ‐producing CD4+ T cells, B‐cell‐specific IFN‐γ‐deficient mice exhibited a higher percentage of Treg cells compared with that in WT mice. These data indicate that B‐cell IFN‐γ production inhibits Treg‐cell differentiation and exacerbates arthritis. Thus, we have established that IFN‐γ, specifically derived from B cells, uniquely contributes to the pathogenesis of autoimmunity through prevention of immunoregulatory mechanisms. |
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| Keywords: | Arthritis Autoimmunity B cells IFN‐γ Treg cells |
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