HLA-restricted recognition of viral antigens in HLA transgenic mice
Cytotoxic T lymphocytes (CTL) recognize antigen in the context of the class-I products of the major histocompatibility complex (MHC). The extensive polymorphism of class-I molecules is thought to be linked to their capacity to present a large variety of foreign antigens. Whether a single T-cell rece...
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Published in: | Nature (London) Vol. 329; no. 6138; pp. 447 - 449 |
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Abstract | Cytotoxic T lymphocytes (CTL) recognize antigen in the context of the class-I products of the major histocompatibility complex (MHC). The extensive polymorphism of class-I molecules is thought to be linked to their capacity to present a large variety of foreign antigens. Whether a single T-cell receptor (TCR) recognizes two separate epitopes (the foreign antigen and an epitope on MHC molecules), or a single epitope resulting from the combination of a foreign antigen and an MHC molecule, has not yet been resolved. In view of the differences between species in primary structure of histocompatibility antigens, it might be predicted that the TCR repertoire would evolve in concert with the diversity of MHC antigens. The mouse and human TCR repertoire would be optimally adapted to engage in productive interactions only with mouse (H-2) and human (HLA) MHC antigens respectively, especially if the more conserved features of histocompatibility antigens, in addition to foreign antigen, were seen by the TCR. Alternatively, only the most variable segments of MHC antigens might be engaged in antigen presentation and thus in interaction with the TCR. In that case, interaction between MHC plus antigen and the TCR might not necessarily be limited by species-specific features. By analysis of the T-cell response against virus-infected cells in HLA-B27/human beta 2-microglobulin double transgenic mice, we report here that the mouse T-cell repertoire is perfectly capable of using the human HLA-B27 antigen as a restriction element. |
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AbstractList | Cytotoxic T lymphocytes (CTL) recognize antigen in the context of the class-I products of the major histocompatibility complex (MHC). The extensive polymorphism of class-I molecules is thought to be linked to their capacity to present a large variety of foreign antigens. Whether a single T-cell receptor (TCR) recognizes two separate epitopes (the foreign antigen and an epitope on MHC molecules), or a single epitope resulting from the combination of a foreign antigen and an MHC molecule, has not yet been resolved. In view of the differences between species in primary structure of histocompatibility antigens, it might be predicted that the TCR repertoire would evolve in concert with the diversity of MHC antigens. The mouse and human TCR repertoire would be optimally adapted to engage in productive interactions only with mouse (H-2) and human (HLA) MHC antigens respectively, especially if the more conserved features of histocompatibility antigens, in addition to foreign antigen, were seen by the TCR. Alternatively, only the most variable segments of MHC antigens might be engaged in antigen presentation and thus in interaction with the TCR. In that case, interaction between MHC plus antigen and the TCR might not necessarily be limited by species-specific features. By analysis of the T-cell response against virus-infected cells in HLA-B27/human beta 2-microglobulin double transgenic mice, we report here that the mouse T-cell repertoire is perfectly capable of using the human HLA-B27 antigen as a restriction element. Cytotoxic T lymphocytes (CTL) recognize antigen in the context of the class-I products of the major histocompatibility complex (MHC). In view of the differences between species in primary structure of histocompatibility antigens, it might be predicted that the TCR repertoire would evolve in concert with the diversity of MHC antigens. By analysis of the T-cell response against virus-infected cells in HLA-B27/human beta sub(2)-microglobulin double transgenic mice, the authors report here that the mouse T-cell repertoire is perfectly capable of using the human HLA-B27 antigen as a restriction element. |
Author | Kievits, Femia Berns, Anton Ploegh, Hidde L Ivanyi, Pavol Krimpenfort, Paul |
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Keywords | Antigen Virus Membrane receptor Major histocompatibility system T-Lymphocyte Transgenic animal Cytotoxicity Infected cell β2»-Microglobulin HLA»-System |
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References | M Cohn (BF329447a0_CR3) 1983; 33 MJ Holterman (BF329447a0_CR18) 1986; 83 L De Waal (BF329447a0_CR8) 1983; 130 JL Maryanski (BF329447a0_CR20) 1986; 136 O Dill (BF329447a0_CR21) 1986; 173 C Bernabeu (BF329447a0_CR15) 1984; 131 MH Breuning (BF329447a0_CR9) 1982; 5 GHA Seemann (BF329447a0_CR11) 1986; 5 E Gomard (BF329447a0_CR17) 1984; 20 BP Babbit (BF329447a0_CR5) 1985; 317 P Krimpenfort (BF329447a0_CR16) 1987; 6 A Herman (BF329447a0_CR14) 1983; 80 P Ferrier (BF329447a0_CR23) 1985; 135 RM Zinkernagel (BF329447a0_CR1) 1979; 27 R Epstein (BF329447a0_CR2) 1986; 163 A Achour (BF329447a0_CR19) 1986; 16 P Matzinger (BF329447a0_CR4) 1981; 292 JD Ashwell (BF329447a0_CR6) 1986; 320 PR Parham (BF329447a0_CR7) 1984; 4 A Toubert (BF329447a0_CR10) 1984; 20 RS Rein (BF329447a0_CR12) 1987; 138 MA Vega (BF329447a0_CR13) 1986; 137 BF329447a0_CR22 |
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Snippet | Cytotoxic T lymphocytes (CTL) recognize antigen in the context of the class-I products of the major histocompatibility complex (MHC). The extensive... By analysis of the T-cell response against virus-infected cells in HLA-B27/human beta sub(2)-microglobulin double transgenic mice, the authors report here that... Cytotoxic T lymphocytes (CTL) recognize antigen in the context of the class-I products of the major histocompatibility complex (MHC). In view of the... |
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SubjectTerms | Analysis of the immune response. Humoral and cellular immunity Animals Antigens, Viral - immunology beta 2-Microglobulin - genetics Biochemistry Biological and medical sciences Blood Cell interactions Fundamental and applied biological sciences. Psychology Fundamental immunology Genetics H-2 Antigens - immunology HLA Antigens - genetics HLA Antigens - immunology HLA-B27 Antigen Humans Immunity (Disease) Immunobiology Influenza A virus - immunology Lymphocytes Medical research Mice Mice, Inbred C57BL Mice, Inbred CBA Mice, Transgenic Parainfluenza Virus 1, Human - immunology Receptors, Antigen, T-Cell - immunology T-Lymphocytes, Cytotoxic - immunology Transfection |
Title | HLA-restricted recognition of viral antigens in HLA transgenic mice |
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