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The specific T-cell response to antigenic peptides is influenced by bystander peptides |
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| Authors: | Izabela Nowak Elżbieta Pajtasz-Piasecka Bartosz Chmielowski Leszek Ignatowicz Piotr Kuśnierczyk |
| Affiliation: | (1) Laboratory of Immunogenetics, Department of Clinical Immunology, Polish Academy of Sciences, Rudolfa Weigla 12, 53-114 Wrocław, Poland;(2) Laboratory of Experimental Antitumor Therapy, Department of Experimental Oncology, Ludwik Hirszfeld Institute of Immunology and Experimental Therapy, Polish Academy of Sciences, Rudolfa Weigla 12, 53-114 Wrocław, Poland;(3) Center of Biotechnology and Genomic Medicine, Medical College of Georgia, Augusta, Georgia, USA;(4) Jan Długosz Paedagogical University, Cz77ęstochowa, Poland |
| Abstract: | T lymphocytes recognize antigens in the form of peptides presented by major histocompatibility complex (MHC) molecules on the cell surface. Only a small proportion of MHC class I and class II molecules are loaded with foreign antigenic peptides; the vast majority are loaded with thousands of different self peptides. It was suggested that MHC molecules presenting self peptides may serve either to decrease (antagonistic effect) or increase (synergistic effect) the T cell response to a specific antigen. Here, we present our finding that transfected mouse fibroblasts presenting a single antigenic peptide covalently bound to a class II MHC molecule stimulated specific mouse T cell hybridoma cells to an interleukin-2 response less efficiently than fibroblasts presenting a similar amount of antigenic peptide in the presence of class II molecules loaded with heterogenous bystander peptides. |
| Keywords: | Bystander peptide T cell response Transfectants Mouse model |
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