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Restoration of An Early, Progressive Defect in Responsiveness to T-Cell Activation in Lupus Mice by Exogenous IL-2

 

作者: PingFang,   StottDavid I.,  

 

期刊: Autoimmunity  (Taylor Available online 1993)
卷期: Volume 15, issue 1  

页码: 19-29

 

ISSN:0891-6934

 

年代: 1993

 

DOI:10.3109/08916939309004835

 

出版商: Taylor&Francis

 

关键词: Con A;IL-2;IL-2R;NZB/W;Mrl/lpr;SLE

 

数据来源: Taylor

 

摘要:

Splenic T-cells from lupus strain (NZB/W F1, Mrl/lpr) mice lack the ability to respond to concanavalin A (Con A) by secretion of IL-2 and hence expression of IL-2 receptor and proliferation. These defects were found not only in an aged group (>5 months) of mice in which obvious clinical‘SLE like’symptoms and elevated levels of serum autoantibodies were observed, but also in mice as young as 4-wk. We demonstrate here that the defective mitogenic activation of T-cells from lupus mice is due to the inability of T-helper cells to produce IL-2 and this defect can be restored by exogenous IL-2in vitro.Con A-induced cell proliferation and IL-2 receptor expression on CD3+cells from lupus mice occur only in the presence of exogenous IL-2, whereas normal T-cells from BALB/c and CBA control mice are activated by the mitogen and undergo complete cell cycling in the absence of exogenous IL-2, as they are able to secrete sufficient endogenous IL-2. The detection of impaired T-helper function in young lupus mice, before development of overt disease, and the reversible nature of the defect indicate that defective IL-2 activity may be fundamental to the mechanism of development of pathology in SLE.

 

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