1. Analysis of Immature (CD4–CD8–) Thymic Subsets in T-Cell Receptor αß Transgenic Mice
- Author
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Hanspeter Pircher, MacDonald Hr, Ohashi P, and Wilson A
- Subjects
CD8 Antigens ,Receptors, Antigen, T-Cell, alpha-beta ,Cellular differentiation ,Transgene ,Immunology ,Mice, Transgenic ,chemical and pharmacologic phenomena ,Thymus Gland ,T-cell development ,transgenic mice ,Biology ,Mice ,Antigen ,T-Lymphocyte Subsets ,immature thymocytes ,Animals ,Cytotoxic T cell ,T-cell receptor ,IL-2 receptor ,Antibodies, Monoclonal ,Cell Differentiation ,hemic and immune systems ,T-Cell Receptor Alpha-Beta ,Molecular biology ,Gene Expression Regulation ,CD4 Antigens ,CD8 ,Research Article ,Developmental Biology - Abstract
Introduction of a transgenic alpha beta TCR (V alpha 2, V beta 8.1) specific for lymphocytic choriomeningitis virus (LCMV), in the context of H-2Db into the genome of C57BL/6 mice, has many effects on the development and selection of T cells in both the thymus and the periphery. These mice produce increased numbers of CD4-8+ mature T cells, all of which express the transgenic TCR, and small numbers of CD4+8- cells using endogenous TCRs are also produced. This study follows the intrathymic development of T cells in these TCR alpha beta transgenic mice, in particular the earliest CD4-8- stages. As expected, the transgenic TCR is expressed on the cell surface at an earlier developmental stage than endogenous TCRs in nontransgenic littermate controls. Of the three major subsets expressing the heat-stable antigen (HSA), only the most mature, the CD25-CD44- expresses the transgenic TCR, and the earlier CD25-CD44+ and CD25+CD44- do not. Furthermore, in contrast to other TCR alpha beta transgenic lines, TCR gamma delta lineage cells appear to develop normally.
- Published
- 1992
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