| Literature DB >> 26841869 |
Alejandra Macias-Garcia1, Beate Heizmann2, MacLean Sellars1, Patricia Marchal1, Hayet Dali3, Jean-Louis Pasquali4, Sylviane Muller5, Philippe Kastner6, Susan Chan7.
Abstract
B1 B cells secrete most of the circulating natural antibodies and are considered key effector cells of the innate immune response. However, B1 cell-associated antibodies often cross-react with self-antigens, which leads to autoimmunity, and B1 cells have been implicated in cancer. How B1 cell activity is regulated remains unclear. We show that the Ikaros transcription factor is a major negative regulator of B1 cell development and function. Using conditional knock-out mouse models to delete Ikaros at different locations, we show that Ikaros-deficient mice exhibit specific and significant increases in splenic and bone marrow B1 cell numbers, and that the B1 progenitor cell pool is increased ∼10-fold in the bone marrow. Ikaros-null B1 cells resemble WT B1 cells at the molecular and cellular levels, but show a down-regulation of signaling components important for inhibiting proliferation and immunoglobulin production. Ikaros-null B1 cells hyper-react to TLR4 stimulation and secrete high amounts of IgM autoantibodies. These results indicate that Ikaros is required to limit B1 cell homeostasis in the adult.Entities:
Keywords: B cells; Ikaros; autoimmune disease; differentiation; gene regulation; immunology; leukemia
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Year: 2016 PMID: 26841869 PMCID: PMC4861476 DOI: 10.1074/jbc.M115.704239
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157