Potent Cytolytic Response by a CD8+ CTL Clone to Multiple Peptides from the Same Protein in Association with an Allogeneic Class I MHC Molecule

Kageyama, Shigeki; Tsomides, Theodore J.; Fukusen, Naomi; Papayannopoulos, Ioannis A.; Eisen, Herman N.; Sykulev, Yuri

doi:10.4049/jimmunol.166.5.3028

Cited by 16 publications

(13 citation statements)

References 34 publications

(36 reference statements)

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“…Because prominent recognition of the peptide by the CDR3 region of the TCR would have resulted in altered usage of CDR3 lengths, these results are consistent with the model derived from structural analyses of the molecular interactions involved in direct allorecognition. Indeed, the large number of contacts made by the TCR with the MHC framework (11,12) and the relatively low sensitivity to peptide sequence variations (17,18,43) suggest that direct recognition of nonself-MHC molecules by T cells may be more dependent on interactions of the TCR with the allo-MHC framework determinants than with the peptide itself (20). This low peptide specificity has also been recently suggested by the low contact number between the CDR3 regions of the BM3.3 TCR and an allogeneic MHC-peptide ligand (44).…”

Section: Discussionmentioning

confidence: 99%

Direct Recognition of Foreign MHC Determinants by Naive T Cells Mobilizes Specific Vβ Families Without Skewing of the Complementarity-Determining Region 3 Length Distribution

Sébille

Gagne

Guillet

et al. 2001

The Journal of Immunology

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The capacity of T cells to interact with nonself-APC, also referred to as direct allorecognition, is an essential feature of the cellular response involved in graft rejection. However, there is no study on TCR repertoire biases associated with direct restricted T cell activation. In this paper, we have addressed the impact of direct recognition on the whole naive T cell repertoire, using a new approach that provides, for the first time, an integrated depiction of the quantitative and qualitative alterations in the TCR Vβ transcriptome. This method can differentiate resting patterns from polyclonally activated ones, as evidenced by superantigen usage. According to this new readout, we show that direct recognition of nonself-MHC molecules triggers mRNA accumulation of several TCR Vβ families, specific to the combination studied. Moreover, in marked contrast to the situation that prevails in indirect allorecognition, T cell activation through the direct presentation pathway was not associated with skewing of the complementarity determining region (CDR) 3 length distribution. Altogether, these data argue for the significance of TCR contacts with the MHC framework in direct allorecognition. In addition, the TCR diversity mobilized by this interaction and the massive TCRβ mRNA accumulation observed after a few days of culture suggest that a significant proportion of naive T cells receive a signal leading to TCRβ transcriptional activation even though only a few of them engage in mitosis.

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Section: Discussionmentioning

confidence: 99%

Direct Recognition of Foreign MHC Determinants by Naive T Cells Mobilizes Specific Vβ Families Without Skewing of the Complementarity-Determining Region 3 Length Distribution

Sébille

Gagne

Guillet

et al. 2001

The Journal of Immunology

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“…The answer is not altogether clear. The number of peptide-MHC complexes required for T lymphocyte recognition varies from several thousand per target cell to as few as one [25,[28][29][30][31][32][33], although weak recognition of other peptides may contribute to the T cell activation process [34]. Some studies have shown a direct correlation between cell surface densities of individual peptide antigens and the magnitude of the immune response against them [35][36][37][38][39], but other studies have shown exactly the opposite [25,27,40].…”

Section: Structural Characteristics Of Peptides Displayed By Mhc Molementioning

confidence: 99%

The contributions of mass spectrometry to understanding of immune recognition by T lymphocytes

Engelhard

2007

International Journal of Mass Spectrometry

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Over the last 15 years, the ability of mass spectrometry to analyze complex peptide mixtures and identify individual species has provided unprecedented insights into the repertoire of peptide antigens displayed by MHC molecules and recognized by T lymphocytes. These include: understanding the peptide binding specificity of MHC molecules; understanding of roles of different intracellular components of the antigen processing pathways in determining the peptide display; and identification of a large number of individual peptide antigens associated with infectious diseases, cancer, and transplant rejection that have provided the basis for new immunologically based therapies. This review will summarize the impact that the application of mass spectrometry has had on these advances, with particular attention to the contributions of Professor Donald Hunt and members of his laboratory, and point out the opportunities for future work. Keywordsantigen processing; post-translational modification; peptides; MHC molecules THE NATURE OF ANTIGEN RECOGNITION BY T LYMPHOCYTEST lymphocytes are a branch of the immune system concerned with recognition of antigens that are displayed on the surface of host cells. These antigens are produced through intracellular proteolytic mechanisms that create small peptides, which are then rescued and presented at the cell surface by adaptor proteins called MHC molecules [reviewed in [1-6]. The binding site of each MHC molecule enables it to bind to a wide range of different peptides, and results in the display of a repertoire of such antigens, each recognized by a distinct T lymphocyte. This "antigen processing and presentation" mechanism results in the display of peptides derived from the proteins of pathogens that have infected the cell or been taken up by endocytosis. Their recognition by T lymphocytes results in the development of an immune response, and results in clearance of the pathogen and infected cells from the body. However, antigen processing and presentation pathways operate constitutively on normal cellular proteins as well, resulting in the display of peptide antigens that can be distinguished on tumors and transplanted tissues. Some of these "self-peptides" are also involved in the development of T lymphocytes in the thymus, and their recognition also controls the balance between selftolerance and autoimmune disease. Correspondence: phone: 434-924-2423; fax: 434-924-1221; email: vhe@virginia.edu Publisher's Disclaimer: This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final citable form. Please note that during the production process errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. In most individuals, molecules of each MHC class are expressed from 3 genetic loci that ...

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“…When, however, the target cells expressed L d , background lysis values were higher (ϳ20%) because some naturally occurring (endogenous) cellular peptides associate with L d to form pMHC agonists for 2C cells (10,12). Background lysis values were not subtracted from the reported results.…”

Section: Cytolytic Assaysmentioning

confidence: 99%

A Peptide That Antagonizes TCR-Mediated Reactions with Both Syngeneic and Allogeneic Agonists: Functional and Structural Aspects

Rudolph

Shen

Lamontagne

et al. 2004

The Journal of Immunology

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We identify and consider some characteristics of a peptide antagonist for the Ag-specific receptor on 2C cells (the 2C TCR). The peptide, GNYSFYAL (called GNY), binds to H-2Kb, and a very high-resolution crystal structure of the GNY-Kb complex at 1.35 Å is described. Although the GNY peptide does not bind to Ld, the potency of GNY-Kb as an antagonist is evident from its ability to specifically inhibit 2C TCR-mediated reactions to an allogenic agonist complex (QLSPFPFDL-Ld), as well as to a syngeneic agonist complex (SIYRYYGL-Kb). The crystal structure and the activities of alanine-substituted peptide variants point to the properties of the peptide P4 side chain and the conformation of the Tyr-P6 side chain as the structural determinants of GNYSFYAL antagonist activity.

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Potent Cytolytic Response by a CD8+ CTL Clone to Multiple Peptides from the Same Protein in Association with an Allogeneic Class I MHC Molecule

Cited by 16 publications

References 34 publications

Direct Recognition of Foreign MHC Determinants by Naive T Cells Mobilizes Specific Vβ Families Without Skewing of the Complementarity-Determining Region 3 Length Distribution

Direct Recognition of Foreign MHC Determinants by Naive T Cells Mobilizes Specific Vβ Families Without Skewing of the Complementarity-Determining Region 3 Length Distribution

The contributions of mass spectrometry to understanding of immune recognition by T lymphocytes

A Peptide That Antagonizes TCR-Mediated Reactions with Both Syngeneic and Allogeneic Agonists: Functional and Structural Aspects

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