Literature DB >> 10358174

Single amino acid replacements in an antigenic peptide are sufficient to alter the TCR V beta repertoire of the responding CD8+ cytotoxic lymphocyte population.

A M Kalergis1, T Ono, F Wang, T P DiLorenzo, S Honda, S G Nathenson.   

Abstract

Cytotoxic CD8+ T lymphocytes are activated upon the engagement of their Ag-specific receptors by MHC class I molecules loaded with peptides 8-11 amino acids long. T cell responses triggered by certain antigenic peptides are restricted to a limited number of TCR V beta elements. The precise role of the peptide in causing this restricted TCR V beta expansion in vivo remains unclear. To address this issue, we immunized C57BL/6 mice with the immunodominant peptide of the vesicular stomatitis virus (VSV) and several peptide variants carrying single substitutions at TCR-contact residues. We observed the expansion of a limited set of TCR V beta elements responding to each peptide variant. To focus our analysis solely on the TCR beta-chain, we created a transgenic mouse expressing exclusively the TCR alpha-chain from a VSV peptide-specific CD8+ T cell clone. These mice showed an even more restricted TCR V beta usage consequent to peptide immunization. However, in both C57BL/6 and TCR alpha transgenic mice, single amino acid replacements in TCR-contact residues of the VSV peptide could alter the TCR V beta usage of the responding CD8+ T lymphocytes. These results provide in vivo evidence for an interaction between the antigenic peptide and the germline-encoded complementarity-determining region-beta loops that can influence the selection of the responding TCR repertoire. Furthermore, only replacements at residues near the C terminus of the peptide were able to alter the TCR V beta usage, which is consistent with the notion that the TCR beta-chain interacts in vivo preferentially with this region of the MHC/peptide complex.

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Year:  1999        PMID: 10358174

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  8 in total

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3.  Steric recognition of T-cell receptor contact residues is required to map mutant epitopes by immunoinformatical programmes.

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Journal:  Immunology       Date:  2012-06       Impact factor: 7.397

Review 4.  Peptides for Vaccine Development.

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Journal:  Sci Transl Med       Date:  2022-04-13       Impact factor: 19.319

6.  Tuning antiviral CD8 T-cell response via proline-altered peptide ligand vaccination.

Authors:  Adil Doganay Duru; Renhua Sun; Eva B Allerbring; Jesseka Chadderton; Nadir Kadri; Xiao Han; Kaliroi Peqini; Hannes Uchtenhagen; Chaithanya Madhurantakam; Sara Pellegrino; Tatyana Sandalova; Per-Åke Nygren; Stephen J Turner; Adnane Achour
Journal:  PLoS Pathog       Date:  2020-05-04       Impact factor: 6.823

7.  l- to d-Amino Acid Substitution in the Immunodominant LCMV-Derived Epitope gp33 Highlights the Sensitivity of the TCR Recognition Mechanism for the MHC/Peptide Structure and Dynamics.

Authors:  Federico Ballabio; Luca Broggini; Cristina Paissoni; Xiao Han; Kaliroi Peqini; Benedetta Maria Sala; Renhua Sun; Tatyana Sandalova; Alberto Barbiroli; Adnane Achour; Sara Pellegrino; Stefano Ricagno; Carlo Camilloni
Journal:  ACS Omega       Date:  2022-03-07

Review 8.  Modulation of tumor immunity by soluble and membrane-bound molecules at the immunological synapse.

Authors:  Pablo A González; Leandro J Carreño; Pablo F Céspedes; Susan M Bueno; Claudia A Riedel; Alexis M Kalergis
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  8 in total

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