DIFFERENTIAL RESPONSES OF CD4+CD45RA+ AND CD4+CD29+ SUBSETS TO ACTIVATED CD8+ CELLS - ENHANCED STIMULATION OF THE CD4+CD45RA+ SUBSET BY CELLS FROM PATIENTS WITH MULTIPLE-SCLEROSIS

被引:7
|
作者
FREEDMAN, MS [1 ]
BLAIN, M [1 ]
ANTEL, JP [1 ]
机构
[1] MCGILL UNIV, MONTREAL NEUROL INST, DEPT NEUROSURG, MONTREAL H3A 2B4, QUEBEC, CANADA
基金
英国医学研究理事会;
关键词
D O I
10.1016/0008-8749(91)90106-L
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
To examine whether functionally different CD4+ cells respond uniformly to the immunoregulatory influences of allogeneic activated CD8+ cells (*CD8+), we subfractionated the CD4+ population into two subsets, based on the high expression of either CD45RA or CD29. We confirmed that the CD45RA+ cells proliferated poorly in response to soluble anti-CD3 mAb, compared to the vigorous response obtained with the CD29+ subset; the CD45RA+ cells were more responsive to stimulation with Con A. Using normal healthy controls, we found that whereas *CD8+ had a significant suppressive effect on the proliferation of the CD29+ subset, they augmented the mitogen-induced proliferative response of the CD45RA+ cells. We further demonstrated that *CD8+ derived from MS patients augmented the response of the CD45RA+ subset to a significantly higher degree compared to healthy age- and sex-matched controls. There were no significant differences between the degree of suppression exerted by the *CD8+ of either the MS or the control group on the CD29+ cells. These results demonstrate that helper/memory CD4+CD29+ cells are more sensitive to the suppressive influences of *CD8+ compared to the CD4+CD45RA+ subset. In addition, in MS, *CD8+ may contribute to a more pronounced "on" signal for virgin CD4+CD45RA+ cells, which might serve as a means to perpetuate the autoimmune disease process. © 1991.
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页码:306 / 316
页数:11
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