Abstract

During the past year, research in the Molecular Immunology Section has been focused on the mechanisms of recognition by human CD8+ T cell antigen-specific receptors (TCRs). Analysis of TCR recognition has been examined using T cell functional assays plus kinetic and thermodynamic binding assays. A particular emphasis of these studies has been on the mechanism of how TCRs recognize the complex of MHC-bound haptenated peptides presented by HLA-A2. The overall conclusion is that there are conserved amino acids on the alpha one (K66) and alpha two (Q155) helices of the HLA-A2 molecule that are key anchor residues that are recognized by most HLA-A2-restricted TCRs, including those that recognize haptenated peptides. For most HLA-A2/peptide complexes whose structures have been solved, the side chains of these key amino acids also contact the bound peptide. These findings demonstrate that the molcular mechanism underlying MHC restriction is that the TCR/MHC interaction cannot be physically separated from the peptide/MHC interaction because key elements of the MHC molecule not only are directly contacted by the TCR but these same MHC elements also contribute to the conformation of the bound peptide. Analysis of TCRs that are specific for structurally diverse haptenated peptides reveals that many TCRs are capable of recognition of quite diverse haptens, and provide a system for analyzing the structural basis of plasticity of TCR recognition. Future studies in this area will focus on the detailed functional analysis of these highly cross-reactive TCRs, the cloning and sequencing of their TCR alpha and beta chain genes, expression of soluble forms of these TCRs for kinetic and thermodynamic binding assays, and crystallographic studies of the TCR/haptenated-peptide/HLA-A2 complexes by our collaborator at the Univ. of Notre Dame. These studies will hopefully provide a biochemical and structural solution to the question of just how much plasticity is associated with TCR cross-reactivity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Intramural Research (Z01)
Project #
1Z01NS002603-20
Application #
6842291
Study Section
(MIS)
Project Start
Project End
Budget Start
Budget End
Support Year
20
Fiscal Year
2003
Total Cost
Indirect Cost

  Institution

Name
National Institute of Neurological Disorders and Stroke
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Gagnon, Susan J; Borbulevych, Oleg Y; Davis-Harrison, Rebecca L et al. (2006) T cell receptor recognition via cooperative conformational plasticity. J Mol Biol 363:228-43
Gagnon, Susan J; Turner, Richard V; Shiue, Michael G et al. (2006) Extensive T cell receptor cross-reactivity on structurally diverse haptenated peptides presented by HLA-A2. Mol Immunol 43:346-56
Gagnon, Susan J; Borbulevych, Oleg Y; Davis-Harrison, Rebecca L et al. (2005) Unraveling a hotspot for TCR recognition on HLA-A2: evidence against the existence of peptide-independent TCR binding determinants. J Mol Biol 353:556-73
Niland, Brian; Banki, Katalin; Biddison, William E et al. (2005) CD8+ T cell-mediated HLA-A*0201-restricted cytotoxicity to transaldolase peptide 168-176 in patients with multiple sclerosis. J Immunol 175:8365-78
Baxter, Tiffany K; Gagnon, Susan J; Davis-Harrison, Rebecca L et al. (2004) Strategic mutations in the class I major histocompatibility complex HLA-A2 independently affect both peptide binding and T cell receptor recognition. J Biol Chem 279:29175-84
Stefanova, Irena; Hemmer, Bernhard; Vergelli, Marco et al. (2003) TCR ligand discrimination is enforced by competing ERK positive and SHP-1 negative feedback pathways. Nat Immunol 4:248-54
Biddison, William E; Turner, Richard V; Gagnon, Susan J et al. (2003) Tax and M1 peptide/HLA-A2-specific Fabs and T cell receptors recognize nonidentical structural features on peptide/HLA-A2 complexes. J Immunol 171:3064-74
Binz, Anne-Kathrin; Rodriguez, Rene C; Biddison, William E et al. (2003) Thermodynamic and kinetic analysis of a peptide-class I MHC interaction highlights the noncovalent nature and conformational dynamics of the class I heterotrimer. Biochemistry 42:4954-61
Tomaru, Utano; Yamano, Yoshihisa; Nagai, Masahiro et al. (2003) Detection of virus-specific T cells and CD8+ T-cell epitopes by acquisition of peptide-HLA-GFP complexes: analysis of T-cell phenotype and function in chronic viral infections. Nat Med 9:469-76
Buslepp, Jennifer; Wang, Huanchen; Biddison, William E et al. (2003) A correlation between TCR Valpha docking on MHC and CD8 dependence: implications for T cell selection. Immunity 19:595-606

Showing the most recent 10 out of 12 publications