T-LYMPHOCYTE T-CELL B-CELL ACTIVATING MOLECULE CD40-L MOLECULES INDUCE NORMAL B-CELLS OR CHRONIC LYMPHOCYTIC-LEUKEMIA B-CELLS TO EXPRESS CD80 (B7/BB-1) AND ENHANCE THEIR COSTIMULATORY ACTIVITY

被引:0
|
作者
YELLIN, MJ [1 ]
SINNING, J [1 ]
COVEY, LR [1 ]
SHERMAN, W [1 ]
LEE, JJ [1 ]
GLICKMANNIR, E [1 ]
SIPPEL, KC [1 ]
ROGERS, J [1 ]
CLEARY, AM [1 ]
PARKER, M [1 ]
CHESS, L [1 ]
LEDERMAN, S [1 ]
机构
[1] COLUMBIA UNIV, COLL PHYS & SURG, DEPT MED, DIV ONCOL, NEW YORK, NY 10032 USA
来源
JOURNAL OF IMMUNOLOGY | 1994年 / 153卷 / 02期
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中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Activation-induced cell surface molecules are involved in mediating bidirectional T-B lymphocyte signaling that is important in the induction of T or B lymphocyte effector functions. In this regard, T-BAM/CD40-L is an activation-induced CD4(+) T cell surface molecule known to be important in inducing B cell effector functions. This report demonstrates that T-BAM/CD40-L molecules on a Jurkat T cell leukemia subclone (D1.1) or nonlymphoid 293 kidney cell transfectants induce B cells or B-CLL cells to express CD80 (B7/BB-1) in a manner that is specifically inhibited by anti-T-BAM/CD4O-L mAb 5C8. Because activation-induced B cell surface molecules, such as CD80, deliver costimulatory signals to T cells that augment T cell proliferation, the functional costimulatory capacity of T-BAM/CD4O-L-primed B cells and B-CLL cells was studied. T-BAM/CD40-L-primed B cells or B-CLL cells augment the proliferative responses of allogenic T cells. Furthermore, T-BAM/CD40-L priming is specifically inhibited by mAb 5C8. Together, these studies demonstrate that T-BAM/CD40-L induces CD80 expression on resting B cells or B-CLL cells. Moreover, T-BAM/CD40-L signaling enhances B cell costimulatory capacity. These studies suggest that T-BAM/CD40-L molecules not only induce B cell differentiative processes that result in Ab secretion, but also enable B cells to prime Ag-specific T cells for subsequent clonal expansion.
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页码:666 / 674
页数:9
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