BCL-2 TRANSGENE INHIBITS T-CELL DEATH AND PERTURBS THYMIC SELF-CENSORSHIP

被引:1071
作者
STRASSER, A
HARRIS, AW
CORY, S
机构
[1] Institute of Medical Research Royal Melbourne Hospital Post Office Victoria, 3050, Walter and Eliza Hall
来源
CELL | 1991年 / 67卷 / 05期
关键词
D O I
10.1016/0092-8674(91)90362-3
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Early death is the fate of most developing T lymphocytes. Because bcl-2 can promote cell survival, we tested its impact in mice expressing an E-mu-bcl-2 transgene within the T lymphoid compartment. The T cells showed remarkably sustained viability and some spontaneous differentiation in vitro. They also resisted killing by lymphotoxic agents. Although total T cell numbers and the rate of thymic involution were unaltered, the response to immunization was enhanced, consistent with reduced death of activated T cells. No T cells reactive with self-superantigens appeared in the lymph nodes, but an excess was found in the thymus. These observations, together with previous findings on B cells, suggest that modulated bcl-2 expression is a determinant of life and death in normal lymphocytes.
引用
收藏
页码:889 / 899
页数:11
相关论文
共 60 条
[1]   CYTO-TOXIC T-CELL CLONE-SPECIFIC MONOCLONAL-ANTIBODIES USED TO SELECT CLONOTYPIC ANTIGEN-SPECIFIC CYTO-TOXIC T-CELLS [J].
ACHAORBEA, H ;
ZINKERNAGEL, RM ;
HENGARTNER, H .
EUROPEAN JOURNAL OF IMMUNOLOGY, 1985, 15 (01) :31-36
[2]   CLONAL DELETION OF V-BETA 14-BEARING T-CELLS IN MICE TRANSGENIC FOR MAMMARY-TUMOR VIRUS [J].
ACHAORBEA, H ;
SHAKHOV, AN ;
SCARPELLINO, L ;
KOLB, E ;
MULLER, V ;
VESSAZSHAW, A ;
FUCHS, R ;
BLOCHLINGER, K ;
ROLLINI, P ;
BILLOTTE, J ;
SARAFIDOU, M ;
MACDONALD, HR ;
DIGGELMANN, H .
NATURE, 1991, 350 (6315) :207-211
[3]   CLONING THE CHROMOSOMAL BREAKPOINT OF T(14-18) HUMAN LYMPHOMAS - CLUSTERING AROUND JH ON CHROMOSOME-14 AND NEAR A TRANSCRIPTIONAL UNIT ON 18 [J].
BAKHSHI, A ;
JENSEN, JP ;
GOLDMAN, P ;
WRIGHT, JJ ;
MCBRIDE, OW ;
EPSTEIN, AL ;
KORSMEYER, SJ .
CELL, 1985, 41 (03) :899-906
[4]   MURINE T-CELL RECEPTOR MUTANTS WITH DELETIONS OF BETA-CHAIN VARIABLE REGION GENES [J].
BEHLKE, MA ;
CHOU, HS ;
HUPPI, K ;
LOH, DY .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1986, 83 (03) :767-771
[5]   THE ROLE OF THE T-CELL RECEPTOR IN POSITIVE AND NEGATIVE SELECTION OF DEVELOPING T-CELLS [J].
BLACKMAN, M ;
KAPPLER, J ;
MARRACK, P .
SCIENCE, 1990, 248 (4961) :1335-1341
[6]   THE BCL-2 CANDIDATE PROTO-ONCOGENE PRODUCT IS A 24-KILODALTON INTEGRAL-MEMBRANE PROTEIN HIGHLY EXPRESSED IN LYMPHOID-CELL LINES AND LYMPHOMAS CARRYING THE T(14,18) TRANSLOCATION [J].
CHENLEVY, Z ;
NOURSE, J ;
CLEARY, ML .
MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (02) :701-710
[7]   A SUPERANTIGEN ENCODED IN THE OPEN READING FRAME OF THE 3' LONG TERMINAL REPEAT OF MOUSE MAMMARY-TUMOR VIRUS [J].
CHOI, YW ;
KAPPLER, JW ;
MARRACK, P .
NATURE, 1991, 350 (6315) :203-207
[8]   CLONING AND STRUCTURAL-ANALYSIS OF CDNAS FOR BCL-2 AND A HYBRID BCL-2/IMMUNOGLOBULIN TRANSCRIPT RESULTING FROM THE T(14-18) TRANSLOCATION [J].
CLEARY, ML ;
SMITH, SD ;
SKLAR, J .
CELL, 1986, 47 (01) :19-28
[9]   T-CELL RECEPTOR GENE DIVERSITY AND SELECTION [J].
DAVIS, MM .
ANNUAL REVIEW OF BIOCHEMISTRY, 1990, 59 :475-496
[10]   SUPERANTIGENS INTERACT WITH MHC CLASS-II MOLECULES OUTSIDE OF THE ANTIGEN GROOVE [J].
DELLABONA, P ;
PECCOUD, J ;
KAPPLER, J ;
MARRACK, P ;
BENOIST, C ;
MATHIS, D .
CELL, 1990, 62 (06) :1115-1121
123456