B cell–specific MHC class II deletion reveals multiple nonredundant roles for B cell antigen presentation in murine lupus

JR Giles, M Kashgarian, PA Koni… - The Journal of …, 2015 - journals.aai.org
JR Giles, M Kashgarian, PA Koni, MJ Shlomchik
The Journal of Immunology, 2015journals.aai.org
B cells have both Ab-dependent and Ab-independent functions in systemic autoimmune
diseases, including systemic lupus erythematosus (SLE). Ab-independent functions are
known to be important, because mice with B cells but no secreted Ig have severe disease.
These functions could include roles in lymphoid development, cytokine secretion, and Ag
presentation; however, these possibilities have not been directly tested in SLE models. In
this study, we show by lineage-specific ablation of MHC class II (MHCII) that B cell Ag …
Abstract
B cells have both Ab-dependent and Ab-independent functions in systemic autoimmune diseases, including systemic lupus erythematosus (SLE). Ab-independent functions are known to be important, because mice with B cells but no secreted Ig have severe disease. These functions could include roles in lymphoid development, cytokine secretion, and Ag presentation; however, these possibilities have not been directly tested in SLE models. In this study, we show by lineage-specific ablation of MHC class II (MHCII) that B cell Ag presentation plays a nonredundant role in CD4+ T cell activation and effector differentiation in the MRL. Fas lpr mouse model of SLE. MHCII-mediated interactions between B and T cells further promote B cell proliferation and differentiation, and, in fact, inefficient MHCII deletion on B cells led to strong selection of escaped cells in activated and plasmablast compartments, further underscoring the central role of B cell Ag presentation. Despite the leakiness in the system, B cell–specific MHCII deletion resulted in substantially ameliorated clinical disease. Hence, B cell Ag presentation is critical for T and B cell activation and differentiation, as well as target organ damage.
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