Human dendritic cells skew isotype switching of CD40-activated naive B cells towards IgA(1) and IgA(2)

被引:188
作者
Fayette, J [1 ]
Dubois, B [1 ]
Vandenabeele, S [1 ]
Bridon, JM [1 ]
Vanbervliet, B [1 ]
Durand, I [1 ]
Banchereau, J [1 ]
Caux, C [1 ]
Briere, F [1 ]
机构
[1] SCHERING PLOUGH CORP, LAB IMMUNOL RES, F-69571 DARDILLY, FRANCE
关键词
D O I
10.1084/jem.185.11.1909
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Within T cell-rich areas of secondary lymphoid organs, interdigitating dendritic cells recruit antigen-specific T cells that then induce B cells to secrete Igs. This study investigates the possible role(s) of. dendritic cells in the regulation of human B cell responses. In the absence of exogenous cytokines, in vitro generated dendritic cells (referred to as Dendritic Langerhans cells, D-Lc) induced surface IgA expression on similar to 10% of CD40-activated naive sIgD(+) B cells. In the presence of IL-10 and TGF-beta, a combination of cytokines previously identified for its capacity to induce IgA switch, D-Lc strongly potentiated the induction of sIgA on CD40-activated naive B cells from 5% to 40-50%. D-Lc alone did not induce the secretion of IgA by CD40-activated naive B cells, which required further addition of IL-10 Furthermore, D-Lc skewed towards the IgA isotype at the expense of IgG, the Ig production oi CD40-activated naive B cells cultured in the presence of IL-10 and TGF-beta. Importantly, under these culture conditions, both IgA(1) and IgA(2) were detected. In the presence of IL-10, secretion of IgA2 by CD40-activated naive B cells could be detected only in response to D-Lc and was further enhanced by TGF-beta. Collectively, these results suggest that in addition to activating T cells in the extrafollicular areas of secondary lymphoid organs, human D-Lc also directly modulate T cell-dependent B cell growth and differentiation, by inducing the IgA isotype switch.
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页码:1909 / 1918
页数:10
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