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Blood dendritic cells interact with splenic marginal zone B cells to initiate T-independent immune responses.

机译:血液树突状细胞与脾边缘B区细胞相互作用,以启动T依赖性免疫应答。

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摘要

Marginal zone (MZ) and B1 B lymphocytes participate jointly in the early immune response against T-independent (TI) particulate antigens. Here we show that blood-derived neutrophil granulocytes and CD11c(lo) immature dendritic cells (DC) are the primary cells that efficiently capture and transport particulate bacteria to the spleen. In a systemic infection, CD11c(lo) DC, but not neutrophils, provide critical survival signals, which can be inhibited by TACI-Fc, to antigen-specific MZ B cells and promote their differentiation into IgM-secreting plasmablasts. In a local TI response, peritoneal cavity macrophages provide similar support to B1 B-derived Ag-specific blasts. In the absence of soluble TACI ligands, Ag-activated MZ- and B1-derived blasts lack survival signals and undergo apoptosis, resulting in severely impaired antibody responses.
机译:边缘区(MZ)和B1 B淋巴细胞共同参与针对T非依赖性(TI)颗粒抗原的早期免疫反应。在这里,我们显示血液来源的嗜中性粒细胞和CD11c(lo)未成熟树突状细胞(DC)是有效捕获和运输颗粒细菌到脾脏的主要细胞。在全身性感染中,CD11c(lo)DC而非嗜中性粒细胞向抗原特异性MZ B细胞提供关键的生存信号,这些信号可以被TACI-Fc抑制,并促进其分化为分泌IgM的浆母细胞。在局部TI反应中,腹膜腔巨噬细胞提供与B1 B衍生的Ag特异性胚细胞相似的支持。在没有可溶性TACI配体的情况下,Ag激活的MZ和B1衍生的原始细胞缺乏存活信号,并发生凋亡,从而导致抗体反应严重受损。

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