INTRACELLULAR CALCIUM LEVELS ARE DIFFERENTIALLY REGULATED IN T-LYMPHOCYTES TRIGGERED BY ANTI-CD2 AND ANTI-CD3 MONOCLONAL-ANTIBODIES

被引：7

作者：

SPINOZZI, F

AGEA, E

BISTONI, O

BELIA, S

TRAVETTI, A

GERLI, R

MUSCAT, C

BERTOTTO, A

机构：

[1] UNIV PERUGIA,DEPT INTERNAL MED,I-06100 PERUGIA,ITALY

[2] UNIV PERUGIA,DEPT CELLULAR BIOL,I-06100 PERUGIA,ITALY

[3] UNIV PERUGIA,DEPT PEDIAT,I-06100 PERUGIA,ITALY

来源：

CELLULAR SIGNALLING | 1995年 / 7卷 / 03期

关键词：

INTRACELLULAR CALCIUM CD3 AND CD2 STIMULATION; T LYMPHOCYTES; JURKAT T CELLS; IP3; GENERATION; CA2+/MG2+ ATPASE;

D O I：

10.1016/0898-6568(94)00079-Q

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

Antigen and/or mitogen-driven T-cell activation is mediated by a rise in intracellular free Ca2+, as second messenger. A regulatory key role for this process is represented by membrane-associated [Ca2+/Mg2+] ATP-ase that is mainly devoted to extrusion of intracellular ion excess. In the present study we have investigated the kinetics of Ca2+ fluxes in both resting and already activated (Jurkat T-cell line) T lymphocytes after CD3 and CD2 (T11(2) and T11(3)) triggering and focused our attention on plasma membrane [Ca2+/Mg2+] ATP-ase activity. In both resting T cells and Jurkat cell line, the CD2 stimulation was able to determine a rise in intracellular free Ca2+ higher than that observed after CD3 triggering. In addition, this calcium signal was independent of negative feedback control exerted by [Ca2+/Mg2+] ATP-ase, as well as of IP3 generation. Thus the CD2 molecular system may, together with cell-adhesion properties, act as an amplifier of Ca2+ signals that, if delivered in the context of other molecular systems, such as CD3 or MHC class II antigens, are essentially devoted to the polyclonal co-stimulatory recruitment of a larger cellular repertoire.

引用

页码：287 / 293

页数：7

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