A SPECIFIC INTERCELLULAR PATHWAY OF APOPTOTIC CELL-DEATH IS DEFECTIVE IN THE MATURE PERIPHERAL T-CELLS OF AUTOIMMUNE LPR AND GLD MICE

被引:67
作者
GILLETTEFERGUSON, I [1 ]
SIDMAN, CL [1 ]
机构
[1] UNIV CINCINNATI, COLL MED, DEPT MOLEC GENET BIOCHEM & MICROBIOL, CINCINNATI, OH 45267 USA
来源
EUROPEAN JOURNAL OF IMMUNOLOGY | 1994年 / 24卷 / 05期
关键词
APOPTOSIS; AUTOIMMUNITY; GLD; LPR; T CELLS;
D O I
10.1002/eji.1830240526
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Homozygosity for either of the unlinked murine autosomal recessive mutations Ipl or gld leads to autoimmunity characterized by peripheral accumulation of CD4(-)/CD8(-) ''double-negative'' T cells, autoantibodies and various forms of tissue pathology. Recently, the gene affected by lpr was identified as fas, whose product acts as a trigger for programmed cell death or apoptosis. Data reported here indicate that the Fas receptor and its ligand, the wild-type form of the gld gene product, are essential for antigen-stimulated peripheral T cell apoptosis. Furthermore, the wild-type gld gene product is a non-cell-autonomous protein that is produced by activated T cells. Apoptotic elimination of antigen-receptor-triggered peripheral T cells appears to be abnormal in Epr and gld mice, and this deficiency causes peripheral T cells to accumulate resulting in lymphadenopathy. These findings support the importance of apoptotic regulation of lymphocyte persistence after antigen encounter in vivo.
引用
收藏
页码:1181 / 1185
页数:5
相关论文
共 38 条
[1]   DIFFERENCES DEFINED BY BONE-MARROW TRANSPLANTATION SUGGEST THAT LPR AND GLD ARE MUTATIONS OF GENES ENCODING AN INTERACTING PAIR OF MOLECULES [J].
ALLEN, RD ;
MARSHALL, JD ;
ROTHS, JB ;
SIDMAN, CL .
JOURNAL OF EXPERIMENTAL MEDICINE, 1990, 172 (05) :1367-1375
[2]   SPONTANEOUS MURINE LUPUS-LIKE SYNDROMES - CLINICAL AND IMMUNOPATHOLOGICAL MANIFESTATIONS IN SEVERAL STRAINS [J].
ANDREWS, BS ;
EISENBERG, RA ;
THEOFILOPOULOS, AN ;
IZUI, S ;
WILSON, CB ;
MCCONAHEY, PJ ;
MURPHY, ED ;
ROTHS, JB ;
DIXON, FJ .
JOURNAL OF EXPERIMENTAL MEDICINE, 1978, 148 (05) :1198-1215
[3]  
BERDEN JHM, 1983, J IMMUNOL, V130, P1699
[4]  
BUDD RC, 1987, J IMMUNOL, V139, P2200
[5]   LPR AND GLD - SINGLE GENE MODELS OF SYSTEMIC AUTOIMMUNITY AND LYMPHOPROLIFERATIVE DISEASE [J].
COHEN, PL ;
EISENBERG, RA .
ANNUAL REVIEW OF IMMUNOLOGY, 1991, 9 :243-269
[6]   THYMIC AND PERIPHERAL APOPTOSIS OF ANTIGEN-SPECIFIC T-CELLS MIGHT COOPERATE IN ESTABLISHING SELF TOLERANCE [J].
DADAMIO, L ;
AWAD, KM ;
REINHERZ, EL .
EUROPEAN JOURNAL OF IMMUNOLOGY, 1993, 23 (03) :747-753
[7]  
DAVIDSON WF, 1986, J IMMUNOL, V136, P4075
[8]  
DAVIGNON JL, 1985, J IMMUNOL, V135, P2423
[9]  
Green D R, 1992, Semin Immunol, V4, P379
[10]   UNIQUE CELL-SURFACE PHENOTYPES OF PROLIFERATING LYMPHOCYTES IN MICE HOMOZYGOUS FOR IPR AND GLD MUTATIONS, DEFINED BY MONOCLONAL-ANTIBODIES TO MRL/MP-IPR/IPR T-CELLS [J].
ISHIDA, Y ;
UEDA, G ;
NOGUCHI, K ;
NAGASAWA, R ;
HIROSE, S ;
SATO, H ;
SHIRAI, T .
CELLULAR IMMUNOLOGY, 1987, 105 (01) :136-146
1234