T-cell hybridomas from HLA-transgenic mice as tools for analysis of human antigen processing |
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Authors: | Canaday David H Gehring Adam Leonard Ethan G Eilertson Brandon Schreiber John R Harding Clifford V Boom W Henry |
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Affiliation: | Division of Infectious Disease, Case Western Reserve University and University Hospitals, Cleveland, OH 44106-4984, USA. dxc44@cwru.edu |
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Abstract: | The study of antigen processing and presentation by human antigen presenting cells (APC) has been limited by difficulties of producing and maintaining human T-cell clones. Murine T-cell hybridomas have advantages for detecting specific peptide-MHC complexes on APC. Human antigen-specific immortalized T-cell lines have not been successfully produced. We report and validate the use of transgenic mice with human MHC genes for HLA-A2, DR1 and DR4 to produce murine T-cell hybridomas that are restricted to human HLA alleles and respond to human macrophages, dendritic cells (DC), and B-cell lines. Hybridomas restricted by human MHC-I and -II specific for influenza matrix protein, tetanus toxoid, diphtheria antigen CRM(197), and various M. tuberculosis antigens were produced. Epitope specificity was determined for several hybridomas. T hybridomas recognized peptide-MHC complexes on fixed APC for analysis of kinetics or susceptibility to inhibitors of antigen processing. T hybridomas restricted by human MHC represent convenient and powerful tools for the study of antigen processing by human APC. |
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