CD3 COMPONENTS AT THE SURFACE OF PRO-T CELLS CAN MEDIATE PRE-T CELL-DEVELOPMENT IN-VIVO

被引：147

作者：

JACOBS, H

VANDEPUTTE, D

TOLKAMP, L

DEVRIES, E

BORST, J

BERNS, A

机构：

[1] NETHERLANDS CANC INST,DIV MOLEC GENET,1066 CX AMSTERDAM,NETHERLANDS

[2] NETHERLANDS CANC INST,DIV CELLULAR BIOCHEM,1066 CX AMSTERDAM,NETHERLANDS

[3] NETHERLANDS CANC INST,DEPT ANIM,1066 CX AMSTERDAM,NETHERLANDS

来源：

EUROPEAN JOURNAL OF IMMUNOLOGY | 1994年 / 24卷 / 04期

关键词：

RAG-1(-/-) MICE; PRE-T CELL DEVELOPMENT; PRE-T RECEPTOR COMPLEX; CD3-MEDIATED SIGNAL TRANSDUCTION;

D O I：

10.1002/eji.1830240423

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Developmentally arrested pro-T cells (CD4(-)8(-), IL-2R(+), HSA(++)) of RAG-1-deficient mice appear to express low levels of CD3 molecules in the absence of T cell receptor (TcR) chains at their surface, while developmentally arrested pre-T cells of TcR alpha-deficient mice express low levels of a disulfide-linked TcR beta chain in association with CD3 molecules. Cross-linking of the CD3 modules on pro-T cells of RAG-1(-/-) mice in vivo, with either of two different CD3 epsilon-specific monoclonal antibodies, induces differentiation of these pro-T cells into pre-T cells (CD4(+)8(+), IL-2R(-), HSA(+)), concomitant with a rapid expansion of the thymic T cell compartment, up to 175-fold within 12 days. The same effects can be produced by introduction of a mutant TcR beta transgene lacking most of the variable domain (Delta V-TcR beta) into the RAG-1(-/-) background. These experiments suggest that cross-linking of the CD3 modules on pro-T cells mimics the signaling function expected of the pre-TcR complex, which is found at the surface of pre-T cells prior to functional TcR alpha gene rearrangement. The variable domain of the TcR beta chain is apparently not essential for inducing these aspects of T cell development.

引用

页码：934 / 939

页数：6

共 38 条

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