学术探索
学术期刊
新闻热点
数据分析
智能评审

PRECOMMITMENT OF CD4+CD8+ THYMOCYTES TO EITHER CD4 OR CD8 LINEAGES

被引:27
作者
CROMPTON, T [1 ]
LEES, RK [1 ]
PIRCHER, H [1 ]
MACDONALD, HR [1 ]
机构
[1] UNIV HOSP ZURICH, INST EXPTL PATHOL, CH-8091 ZURICH, SWITZERLAND
来源
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1993年 / 90卷 / 19期
关键词
D O I
10.1073/pnas.90.19.8982
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
CD4+ and CD8+ mature T cells arise from CD4+CD8+ precursors in the thymus. During this process, cells expressing T-cell receptors (TCRs) reactive with self major histocompatibility complex (MHC) class I or II molecules are positively selected to the CD8 or CD4 lineage, respectively. It is controversial whether lineage commitment of CD4+CD8+ thymocytes is controlled directly by TCR specificity for MHC (instructional model) or, alternatively, by processes that operate independently of TCR specificity (stochastic model). We show here that CD4+CD8+ thymocytes bearing a MHC class I-restricted transgenic TCR can be subject to two alternative developmental fates. One population of CD4+CD8+ cells is positively selected by MHC class I molecules to the CD8 lineage as expected, whereas the other CD4+CD8+ population rearranges endogenous TCR genes and is positively selected by MHC class II molecules to the CD4 lineage. Blocking TCR-MHC class II interactions in vivo does not interfere with the generation of CD4+CD8+ cells expressing endogenous TCRs but does prevent their subsequent maturation to CD4+ cells. These data support a version of the stochastic model in which CD4+CD8+ thymocytes are precommitted to the CD4 or CD8 lineage independently of TCR specificity for MHC and prior to positive selection.
引用
收藏
页码:8982 / 8986
页数:5
相关论文
共 36 条
[11]   DEPLETION OF CD4+ T-CELLS IN MAJOR HISTOCOMPATIBILITY COMPLEX CLASS-II DEFICIENT MICE [J].
GRUSBY, MJ ;
JOHNSON, RS ;
PAPAIOANNOU, VE ;
GLIMCHER, LH .
SCIENCE, 1991, 253 (5026) :1417-1420
[12]   T-CELL RECEPTOR-MEDIATED NEGATIVE SELECTION OF AUTOREACTIVE LYMPHOCYTE-T PRECURSORS OCCURS AFTER COMMITMENT TO THE CD4 OR CD8 LINEAGES [J].
GUIDOS, CJ ;
DANSKA, JS ;
FATHMAN, CG ;
WEISSMAN, IL .
JOURNAL OF EXPERIMENTAL MEDICINE, 1990, 172 (03) :835-845
[13]   DIFFERENT EXPRESSION OF THE RECOMBINATION ACTIVITY GENE RAG-1 IN VARIOUS POPULATIONS OF THYMOCYTES, PERIPHERAL T-CELLS AND GUT THYMUS-INDEPENDENT INTRAEPITHELIAL LYMPHOCYTES SUGGESTS 2 PATHWAYS OF T-CELL RECEPTOR REARRANGEMENT [J].
GUYGRAND, D ;
BROECKE, CV ;
BRIOTTET, C ;
MALASSISSERIS, M ;
SELZ, F ;
VASSALLI, P .
EUROPEAN JOURNAL OF IMMUNOLOGY, 1992, 22 (02) :505-510
[14]   THE ANTIGEN-SPECIFIC, MAJOR HISTOCOMPATIBILITY COMPLEX-RESTRICTED RECEPTOR ON T-CELLS .6. AN ANTIBODY TO A RECEPTOR ALLOTYPE [J].
HASKINS, K ;
HANNUM, C ;
WHITE, J ;
ROEHM, N ;
KUBO, R ;
KAPPLER, J ;
MARRACK, P .
JOURNAL OF EXPERIMENTAL MEDICINE, 1984, 160 (02) :452-471
[15]  
HOWE RC, 1988, J IMMUNOL, V140, P1047
[16]   KINETICS AND EFFICACY OF POSITIVE SELECTION IN THE THYMUS OF NORMAL AND T-CELL RECEPTOR TRANSGENIC MICE [J].
HUESMANN, M ;
SCOTT, B ;
KISIELOW, P ;
VONBOEHMER, H .
CELL, 1991, 66 (03) :533-540
[17]   THE T-CELL RECEPTOR AS A MULTICOMPONENT SIGNALING MACHINE - CD4/CD8 CORECEPTORS AND CD45 IN T-CELL ACTIVATION [J].
JANEWAY, CA .
ANNUAL REVIEW OF IMMUNOLOGY, 1992, 10 :645-674
[18]   ABSENCE OF THE LYT-2-,L3T4+ LINEAGE OF T-CELLS IN MICE TREATED NEONATALLY WITH ANTI-I-A CORRELATES WITH ABSENCE OF INTRATHYMIC I-A-BEARING ANTIGEN-PRESENTING CELL-FUNCTION [J].
KRUISBEEK, AM ;
MOND, JJ ;
FOWLKES, BJ ;
CARMEN, JA ;
BRIDGES, S ;
LONGO, DL .
JOURNAL OF EXPERIMENTAL MEDICINE, 1985, 161 (05) :1029-1047
[19]   T-CELL REPERTOIRE SELECTION DURING DEVELOPMENT [J].
MACDONALD, HR .
CURRENT OPINION IN IMMUNOLOGY, 1989, 2 (02) :199-203
[20]   REGULATION OF TCR-ALPHA AND TCR-BETA GENE ALLELIC EXCLUSION DURING T-CELL DEVELOPMENT [J].
MALISSEN, M ;
TRUCY, J ;
JOUVINMARCHE, E ;
CAZENAVE, PA ;
SCOLLAY, R ;
MALISSEN, B .
IMMUNOLOGY TODAY, 1992, 13 (08) :315-322
1234