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ANALYSIS OF TETANUS TOXIN PEPTIDE DR RECOGNITION BY HUMAN T-CELL RECEPTORS RECONSTITUTED INTO A MURINE T-CELL HYBRIDOMA

被引:67
作者
BLANK, U
BOITEL, B
MEGE, D
ERMONVAL, M
ACUTO, O
机构
[1] Laboratory of Molecular Immunology, Pasteur Institute, Paris
来源
EUROPEAN JOURNAL OF IMMUNOLOGY | 1993年 / 23卷 / 12期
关键词
T-CELL RECEPTOR; HLA-DR; TETANUS TOXIN;
D O I
10.1002/eji.1830231203
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
We have previously reported that human T cell receptors (TcR) selected in the class II-restricted (HLA-DRB1*1302) response to a tetanus toxin peptide (tt830-843) frequently used the Vbeta2 germ-line segment which paired with several Valpha segments and that the putative CDR3 of both alpha and beta chains showed remarkable heterogeneity To analyze the structural basis for recognition of the tt830-843/DR complex, five of these TcR were reconstituted into a murine T cell hybridoma, 58 alpha-beta-, by expressing the human alpha and beta variable regions joined to the mouse alpha and beta constant regions, respectively. The chimeric TcR, expressing the same Vbeta germ-line segment (Vbeta2), two expressing Valpha21.1, two Valpha17.1 and one Valpha8.1 were shown to have the expected antigen specificity and DR restriction. Two lines of evidence suggested that the putative CDR3, although not conserved in these TcR, played a key role in recognition. First, two TcR with identical V germ-line segments but distinct CDR3 showed large differences in their capacity to react with the ligand. Second, interchanging the alpha and beta chains from tt830-843/DR1302-specific TcR which differed in their CDR3 sequences invariably led to loss of recognition. We also asked whether germ-line Valpha17.1 could functionally replace Valpha21.1, as they appear to be related in their primary sequence. However, as in the case of CDR3 exchanges, Valpha replacement abrogated TcR reactivity. Taken together, these data underline the fine interdependence of the structural components of the TcR binding site in defining a given specificity. Four of the TcR studied displaying promiscuous recognition were also tested against different DR alleles and site-directed mutants. The results of these experiments suggested that, in spite of their structural heterogeneity, anti-tt830-843 TcR may have a similar orientation with respect to the peptide/DR complex. The reconstitution system described herein should represent a valuable tool for detailed studies of human TcR specificity.
引用
收藏
页码:3057 / 3065
页数:9
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共 49 条
  • [1] LIMITED HETEROGENEITY OF T-CELL RECEPTORS FROM LYMPHOCYTES MEDIATING AUTOIMMUNE ENCEPHALOMYELITIS ALLOWS SPECIFIC IMMUNE INTERVENTION
    ACHAORBEA, H
    MITCHELL, DJ
    TIMMERMANN, L
    WRAITH, DC
    TAUSCH, GS
    WALDOR, MK
    ZAMVIL, SS
    MCDEVITT, HO
    STEINMAN, L
    [J]. CELL, 1988, 54 (02) : 263 - 273
  • [2] STRUCTURE OF THE HUMAN CLASS-I HISTOCOMPATIBILITY ANTIGEN, HLA-A2
    BJORKMAN, PJ
    SAPER, MA
    SAMRAOUI, B
    BENNETT, WS
    STROMINGER, JL
    WILEY, DC
    [J]. NATURE, 1987, 329 (6139) : 506 - 512
  • [3] PREFERENTIAL V-BETA-GENE USAGE AND LACK OF JUNCTIONAL SEQUENCE CONSERVATION AMONG HUMAN T-CELL RECEPTORS SPECIFIC FOR A TETANUS TOXIN DERIVED PEPTIDE - EVIDENCE FOR A DOMINANT ROLE OF A GERMLINE-ENCODED V-REGION IN ANTIGEN MAJOR HISTOCOMPATIBILITY COMPLEX RECOGNITION
    BOITEL, B
    ERMONVAL, M
    PANINABORDIGNON, P
    MARIUZZA, RA
    LANZAVECCHIA, A
    ACUTO, O
    [J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1992, 175 (03) : 765 - 777
  • [4] INVOLVEMENT OF BOTH T-CELL RECEPTOR V-ALPHA AND V-BETA VARIABLE REGION DOMAINS AND ALPHA-CHAIN JUNCTIONAL REGION IN VIRAL-ANTIGEN RECOGNITION
    BRANDLE, D
    BURKI, K
    WALLACE, VA
    ROHRER, UH
    MAK, TW
    MALISSEN, B
    HENGARTNER, H
    PIRCHER, H
    [J]. EUROPEAN JOURNAL OF IMMUNOLOGY, 1991, 21 (09) : 2195 - 2202
  • [5] A HYPOTHETICAL MODEL OF THE FOREIGN ANTIGEN-BINDING SITE OF CLASS-II HISTOCOMPATIBILITY MOLECULES
    BROWN, JH
    JARDETZKY, T
    SAPER, MA
    SAMRAOUI, B
    BJORKMAN, PJ
    WILEY, DC
    [J]. NATURE, 1988, 332 (6167) : 845 - 850
  • [6] 3-DIMENSIONAL STRUCTURE OF THE HUMAN CLASS-II HISTOCOMPATIBILITY ANTIGEN HLA-DR1
    BROWN, JH
    JARDETZKY, TS
    GORGA, JC
    STERN, LJ
    URBAN, RG
    STROMINGER, JL
    WILEY, DC
    [J]. NATURE, 1993, 364 (6432) : 33 - 39
  • [7] T-CELL RECEPTOR SELECTION BY AND RECOGNITION OF 2 CLASS-I MAJOR HISTOCOMPATIBILITY COMPLEX RESTRICTED ANTIGENIC PEPTIDES THAT DIFFER AT A SINGLE POSITION
    CASANOVA, JL
    MARTINON, F
    GOURNIER, H
    BARRA, C
    PANNETIER, C
    REGNAULT, A
    KOURILSKY, P
    CEROTTINI, JC
    MARYANSKI, JL
    [J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1993, 177 (03) : 811 - 820
  • [8] H-2-RESTRICTED CYTOLYTIC LYMPHOCYTES-T SPECIFIC FOR HLA DISPLAY T-CELL RECEPTORS OF LIMITED DIVERSITY
    CASANOVA, JL
    CEROTTINI, JC
    MATTHES, M
    NECKER, A
    GOURNIER, H
    BARRA, C
    WIDMANN, C
    MACDONALD, HR
    LEMONNIER, F
    MALISSEN, B
    MARYANSKI, JL
    [J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1992, 176 (02) : 439 - 447
  • [9] T-CELL RECEPTOR GENES IN A SERIES OF CLASS-I MAJOR HISTOCOMPATIBILITY COMPLEX-RESTRICTED CYTOTOXIC LYMPHOCYTE-T CLONES SPECIFIC FOR A PLASMODIUM-BERGHEI NONAPEPTIDE - IMPLICATIONS FOR T-CELL ALLELIC EXCLUSION AND ANTIGEN-SPECIFIC REPERTOIRE
    CASANOVA, JL
    ROMERO, P
    WIDMANN, C
    KOURILSKY, P
    MARYANSKI, JL
    [J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1991, 174 (06) : 1371 - 1383
  • [10] SELECTIVE EXPANSION OF T-CELLS EXPRESSING V-BETA-2 IN TOXIC SHOCK SYNDROME
    CHOI, YW
    LAFFERTY, JA
    CLEMENTS, JR
    TODD, JK
    GELFAND, EW
    KAPPLER, J
    MARRACK, P
    KOTZIN, BL
    [J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1990, 172 (03) : 981 - 984
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