Identification of a peptide binding protein that plays a role in antigen presentation.
- 1 March 1987
- journal article
- research article
- Published by Proceedings of the National Academy of Sciences in Proceedings of the National Academy of Sciences
- Vol. 84 (6) , 1659-1663
- https://doi.org/10.1073/pnas.84.6.1659
Abstract
The helper T-cell response to globular proteins appears, in general, to require intracellular processing of the antigen, such that a peptide fragment containing the T-cell antigenic determinant is released and transported to and held on the surface of an Ia-expressing, antigen-presenting cell. However, the molecular details underlying these phenomena are largely unknown. The means by which antigenic peptides are anchored on the antigen-presenting cell surface was investigated. A cell surface protein is identified that was isolated by its ability to bind to a 24-amino acid peptide fragment of pigeon cytochrome c, residues 81-104, containing the major antigenic determinant for B10.A mouse T cells. This peptide binding protein, purified from [35S]methionine-labeled cells, appears as two discrete bands of .apprxeq. 72 and and 74 kDa after NaDodSO4/PAGE. The protein can be eluted from the peptide affinity column with equivalent concentrations of either the antigenic pigeon cytochrome c peptide or the corresponding nonantigenic peptide of mouse cytochrome c. However, it does not bind to the native cytochromes c, either of pigeon or mouse, and thus the protein appears to recognize some structure available only in the free peptides. This protein plays a role in antigen presentation as evidenced by the ability of rabbit antibodies raised against it to block the activation of an antigen-specific T-cell hybrid by antigen-presenting cells and pigeon cytochrome c. Its expression is not major histocompatibility complex-restricted in that the blocking activity of the antisera can be absorbed on spleen cells from mice of different haplotypes. This peptide binding protein can be isolated from a variety of cell types, including B cells, T cells, and fibroblasts. The anchoring of processed peptides on the cell surface by such a protein may play a role in antigen presentation.sbd.facilitating the interaction of antigenic peptides with Ia and/or the T-cell receptor.Keywords
This publication has 28 references indexed in Scilit:
- The epitopes of influenza nucleoprotein recognized by cytotoxic T lymphocytes can be defined with short synthetic peptidesCell, 1986
- T-cell-mediated association of peptide antigen and major histocompatibility complex protein detected by energy transfer in an evanescent wave-fieldNature, 1986
- Peptides related to the antigenic determinant block T cell recognition of the native protein as processed by antigen‐presenting cellsEuropean Journal of Immunology, 1986
- Antigen presentation is a function of all B cell subpopulations separated on the basis of sizeEuropean Journal of Immunology, 1986
- Antigen-specific interaction between T and B cellsNature, 1985
- Gene transfer of H-2 class II genes: Antigen presentation by mouse fibroblast and hamster B-cell linesCell, 1984
- Large-scale purification of murine I-Ak and I-Ek antigens and characterization of the purified proteinsMolecular Immunology, 1983
- Antigen recognition by H-2-restricted T cells. I. Cell-free antigen processing.The Journal of Experimental Medicine, 1983
- The T lymphocyte response to cytochrome c—II.: Molecular characterization of a pigeon cytochrome c determinant recognized by proliferating T lymphocytes of the B10.a mouseMolecular Immunology, 1980
- Cleavage of Structural Proteins during the Assembly of the Head of Bacteriophage T4Nature, 1970