| Literature DB >> 26852110 |
Xiaoqian Wang1, Yinxiang Wei2, He Xiao1, Xiaoling Liu3, Yu Zhang4, Gencheng Han1, Guojiang Chen1, Chunmei Hou1, Li Zhang5, Ning Ma6, Beifen Shen1, Yan Li1, Charles E Egwuagu7, Renxi Wang8.
Abstract
Interleukin 10 (IL-10)-producing regulatory B-cells (Bregs) suppress inflammatory responses that mediate autoimmune diseases. However, it is unknown whether Bregs derive from a pre-existing dedicated B-cell lineage or if any B-cell can differentiate into Bregs in response to BCR or TLR activation. GL7(+) B-cells are antigen-experienced differentiated B-cells while GL7(-/lo) are at an early stage of B-cell differentiation. While both GL7(-/lo) and GL7(+) B cells can produce IL-10, differentiation of GL7(-) B-cells into Bregs does not require CD19- or Bcl6-induced signals, suggesting that BCR-induced proliferation or Ig class-switching is not necessary for generation of Breg cells. Of particular importance, we show that GL7(-) Breg cells are dramatically expanded in lupus-like mice and GL7(-) Bregs suppressed inflammatory responses in lupus-like mice by inducing expansion of Foxp3(+)Treg cells. Taken together, these results suggest that pre-existing GL7(-)IL-10(+) cells are expanded during inflammation, differentiate into GL7(+) Bregs and contribute to immune-regulation in lupus-like mice.Entities:
Keywords: Bregs; CD19; GL7; Lupus; Tregs
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Year: 2016 PMID: 26852110 DOI: 10.1016/j.molimm.2016.01.011
Source DB: PubMed Journal: Mol Immunol ISSN: 0161-5890 Impact factor: 4.407