BCL-X(L) AND BCL-2 REPRESS A COMMON PATHWAY OF CELL-DEATH

被引：375

作者：

CHAO, DT

LINETTE, GP

BOISE, LH

WHITE, LS

THOMPSON, CB

KORSMEYER, SJ

机构：

[1] WASHINGTON UNIV, SCH MED,HOWARD HUGHES MED INST,DEPT MED, DIV MOLEC ONCOL, ST LOUIS, MO 63110 USA

[2] WASHINGTON UNIV, SCH MED, HOWARD HUGHES MED INST, DEPT PATHOL, ST LOUIS, MO 63110 USA

[3] UNIV CHICAGO, HOWARD HUGHES MED INST, DEPT MED, CHICAGO, IL 60637 USA

[4] UNIV CHICAGO, HOWARD HUGHES MED INST, DEPT MOLEC GENET, CHICAGO, IL 60637 USA

[5] UNIV CHICAGO, HOWARD HUGHES MED INST, DEPT CELL BIOL, CHICAGO, IL 60637 USA

来源：

JOURNAL OF EXPERIMENTAL MEDICINE | 1995年 / 182卷 / 03期

关键词：

D O I：

10.1084/jem.182.3.821

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

The effect of Bcl-x(L) upon the developmental death of T cells was assessed by generating transgenic mice that expressed Bcl-x(L) within all thymocyte subsets. Bcl-x(L) protected thymocytes from a variety of apoptotic stimuli, including gamma irradiation, glucocorticoids, and anti-CDS treatment. Bcl-x(L) altered thymocyte maturation, resulting in increased numbers of CD3(int/hi) and CD4(-)8(+) thymocytes. Overall, the phenotype of Bcl-x(L) transgenics was essentially indistinguishable from a Bcl-2 transgenic model. Overexpression of Bcl-x(L) or Bcl-2 resulted in the down-regulation of the other molecule, providing further evidence of their reciprocal regulation. In a genetic test of redundancy, the Bcl-x(L) transgene rescued mature T cells in Bcl-2 null mice. Immunoprecipitation indicated that Bcl-x(L), like Bcl-2, heterodimerized with the death-promoting molecule Bar in thymocytes. This in vivo model argues that Bcl-x(L), like Bcl-2, functions in a common pathway to repress cell death.

引用

页码：821 / 828

页数：8

共 20 条

[1] CD28 COSTIMULATION CAN PROMOTE T-CELL SURVIVAL BY ENHANCING THE EXPRESSION OF BCL-X(L)
BOISE, LH
MINN, AJ
NOEL, PJ
JUNE, CH
ACCAVITTI, MA
LINDSTEN, T
THOMPSON, CB
[J]. IMMUNITY, 1995, 3 (01) : 87 - 98
[2] BCL-X, A BCL-2-RELATED GENE THAT FUNCTIONS AS A DOMINANT REGULATOR OF APOPTOTIC CELL-DEATH
BOISE, LH
GONZALEZGARCIA, M
POSTEMA, CE
DING, LY
LINDSTEN, T
TURKA, LA
MAO, XH
NUNEZ, G
THOMPSON, CB
[J]. CELL, 1993, 74 (04) : 597 - 608
[3] BRADFORD MM, 1976, ANAL BIOCHEM, V72, P248, DOI 10.1016/0003-2697(76)90527-3
[4] DISSECTION OF THYMOCYTE SIGNALING PATHWAYS BY INVIVO EXPRESSION OF PERTUSSIS TOXIN ADP-RIBOSYLTRANSFERASE
CHAFFIN, KE
BEALS, CR
WILKIE, TM
FORBUSH, KA
SIMON, MI
PERLMUTTER, RM
[J]. EMBO JOURNAL, 1990, 9 (12) : 3821 - 3829
[5] APOPTOSIS AND PROGRAMMED CELL-DEATH IN IMMUNITY
COHEN, JJ
DUKE, RC
FADOK, VA
SELLINS, KS
[J]. ANNUAL REVIEW OF IMMUNOLOGY, 1992, 10 : 267 - 293
[6] GONZALEZGARCIA M, 1994, DEVELOPMENT, V120, P3033
[7] GRATIOTDEANS J, 1993, J IMMUNOL, V151, P3
[8] KRAJEWSKI S, 1994, CANCER RES, V54, P5501
[9] BCL-2 IS UP-REGULATED AT THE CD4(+)CD8(+) STAGE DURING POSITIVE SELECTION AND PROMOTES THYMOCYTE DIFFERENTIATION AT SEVERAL CONTROL POINTS
LINETTE, GP
GRUSBY, MJ
HEDRICK, SM
HANSEN, TH
GLIMCHER, LH
KORSMEYER, SJ
[J]. IMMUNITY, 1994, 1 (03) : 197 - 205
[10] BCLX REGULATES THE SURVIVAL OF DOUBLE-POSITIVE THYMOCYTES
MA, A
PENA, JC
CHANG, B
MARGOSIAN, E
DAVIDSON, L
ALT, FW
THOMPSON, CB
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (11) : 4763 - 4767

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