Abstract

The objective of this work has been to understand the details of the interaction of self and foreign peptides with MHC molecules, as studied both by in vitro binding methods and by assays of T cell activation. As this project has developed, we have developed a system in which the binding of the antigenic peptide to the MHC class I molecule H-2Ld is measured and in which we can in parallel measure the interaction of the MHC/peptide complex with the T cell receptor. Current experiments have investigated the influence of the coreceptor molecule, CD8, on the MHC/TCR interaction as well as the nature of the early signaling events that are elicited by the stimulation of the T cell with peptide/MHC complexes and those containing variant peptides. Attention has been focused on a paradoxical result: the identification of a single peptide variant that complexes with the mouse MHC class I molecule H-2Ld, serves as an effective sensitizing peptide, but fails to form a complex in which we can detect binding by surface plasmon resonance. The variant peptide seems to form a complex that activates the T cells to cytolysis, lymphokine production, or now, as studied by Dr. M. Jelonek in collaboration with Dr. I. Stefanova by early phosphorylation events. Since there has been such a discrepancy in the ability of the variant peptide/H-2Ld complex to bind the TCR in vitro it is remarkable that the T cell response seems to show only minor kinetic and quantitative differences in early phosphorylation patterns. Attempts to evaluate the contribution of CD8 (produced by Australian collaborators Brendan Classon and Peter Hudson) to the binding reaction of H-2Ld/peptide complexes with the cognate TCR revealed interaction of the CD8 to H-2Ld molecules devoid of peptide. This suggested that an H-2Ld peptide motif in the amino terminal region of the CD8 protein was mediating binding to the MHC molecule through the MHC's peptide binding groove. A variety of direct binding and competition experiments have confirmed that H-2Ld can carry out this mode of binding to the mature CD8.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Intramural Research (Z01)
Project #
1Z01AI000622-06
Application #
6160663
Study Section
Special Emphasis Panel (LI)
Project Start
Project End
Budget Start
Budget End
Support Year
6
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
National Institute of Allergy and Infectious Diseases
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Margulies, David H (2009) Antigen-processing and presentation pathways select antigenic HIV peptides in the fight against viral evolution. Nat Immunol 10:566-8
Dzutsev, Amiran K; Belyakov, Igor M; Isakov, Dmitry V et al. (2008) Estimation of low frequency antigen-presenting cells with a novel RELISPOT assay. J Immunol Methods 333:71-8
Belyakov, Igor M; Kozlowski, Steven; Mage, Michael et al. (2007) Role of alpha3 domain of class I MHC molecules in the activation of high- and low-avidity CD8+ CTLs. Int Immunol 19:1413-20
Dzutsev, Amiran H; Belyakov, Igor M; Isakov, Dmitry V et al. (2007) Avidity of CD8 T cells sharpens immunodominance. Int Immunol 19:497-507
Mans, Janet; Natarajan, Kannan; Balbo, Andrea et al. (2007) Cellular expression and crystal structure of the murine cytomegalovirus major histocompatibility complex class I-like glycoprotein, m153. J Biol Chem 282:35247-58
Natarajan, Kannan; Hicks, Ashleigh; Mans, Janet et al. (2006) Crystal structure of the murine cytomegalovirus MHC-I homolog m144. J Mol Biol 358:157-71
Hu, Jin-Shan; Plaksin, Daniel; Margulies, David H (2005) Backbone and side chain resonance assignmentsof a TRAV14-3 mouse T cell receptor domain. J Biomol NMR 31:271-2
Kuribayashi, Hideki; Wakabayashi, Ayako; Shimizu, Masumi et al. (2004) Resistance to viral infection by intraepithelial lymphocytes in HIV-1 P18-I10-specific T-cell receptor transgenic mice. Biochem Biophys Res Commun 316:356-63
Dam, Julie; Guan, Rongjin; Natarajan, Kannan et al. (2003) Variable MHC class I engagement by Ly49 natural killer cell receptors demonstrated by the crystal structure of Ly49C bound to H-2K(b). Nat Immunol 4:1213-22
Lukashev, Dmitriy E; Caldwell, Charles C; Chen, Pearl et al. (2003) A serine/threonine phosphorylation site in the ectodomain of a T cell receptor beta chain is required for activation by superantigen. J Recept Signal Transduct Res 23:33-52

Showing the most recent 10 out of 31 publications