GLD/GLD MICE ARE UNABLE TO EXPRESS A FUNCTIONAL LIGAND FOR FAS

被引：159

作者：

RAMSDELL, F ^{[1
]}

SEAMAN, MS ^{[1
]}

MILLER, RE ^{[1
]}

TOUGH, TW ^{[1
]}

ALDERSON, MR ^{[1
]}

LYNCH, DH ^{[1
]}

机构：

[1] IMMUNEX RES & DEV CORP,DEPT CELLULAR IMMUNOL,SEATTLE,WA 98101

来源：

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

关键词：

LPR; GLD; FAS; T CELL;

D O I：

10.1002/eji.1830240422

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Mice homozygous for either the lpr or gld genes develop phenotypically identical autoimmune disorders. The gene responsible for the pathology in lpr/lpr mice encodes the Fas antigen, a protein associated with the induction of programmed cell death. To determine if the defect associated with gld represents a mutation in the ligand for Fas, we have assessed the ability of lymphoid cells from homozygous gld/gld mice to lyse target cells in a Fas-dependent manner. Using an antagonistic antibody to Fas, we demonstrate that activated T cells from normal and lpr mice are capable of inducing Fas-mediated lysis of tumor target cells. In contrast, activated T cells from gld/gld mice fail to induce lysis of tumor targets, although cells from gld mice are able to lyse specific allogeneic targets following mixed lymphocyte culture. In addition, activated T cells from gld/gld homozygous animals are not capable of binding to a Fas. Fc fusion protein at high levels, whereas activated T cells from normal and lpr/lpr animals bind Fas. Fc efficiently. These data indicate that mice homozygous for gld are unable to express a functional ligand for Fas.

引用

页码：928 / 933

页数：6

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