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The survival and function of IL-10-producing regulatory B cells are negatively controlled by SLAMF5

Nat Commun. 2021-03; 
Lihi Radomir, Matthias P Kramer, Michal Perpinial, Nofar Schottlender, Stav Rabani, Keren David, Anna Wiener, Hadas Lewinsky, Shirly Becker-Herman, Rina Aharoni, Ron Milo, Claudia Mauri, Idit Shachar
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Catalog Peptides Mice were injected subcutaneously with 200 μg MOG35-55, (synthesized by Genscript) in incomplete Freund’s adjuvant supplemented with 3 mg ml−1 heat‐inactivated Mycobacterium tuberculosis (Sigma-Aldrich) Get A Quote

摘要

B cells have essential functions in multiple sclerosis and in its mouse model, experimental autoimmune encephalomyelitis, both as drivers and suppressors of the disease. The suppressive effects are driven by a regulatory B cell (Breg) population that functions, primarily but not exclusively, via the production of IL-10. However, the mechanisms modulating IL-10-producing Breg abundance are poorly understood. Here we identify SLAMF5 for controlling IL-10 Breg maintenance and function. In EAE, the deficiency of SLAMF5 in B cells causes accumulation of IL10 Bregs in the central nervous system and periphery. Blocking SLAMF5 in vitro induces both human and mouse IL-10-producing Breg cells and increases their survival... More

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