Vaccinia-specific cytotoxic T-cell responses in the context of H-2 antigens not encountered in thymus may reflect aberrant recognition of a virus-H-2 complex.

Author:

Doherty P C,Bennink J C

Abstract

BALB/c (H-2Kd-Dd) spleen and lymph node populations were specifically depleted of alloreactive potential by filtration through H-2 different, irradiated recipients. These negatively selected T cells were then stimulated with vaccinia virus in mice expressing the foreign H-2 determinants encountered previously in the filter environment. Strong virus-immune cytotoxic T-cell responses were seen in the context of H-2Kk and H-2Ks, but not 2H-2Kb. The T cells generated were not cross-reactive for the H-2Kk and H-2Kd alleles, and responsiveness was independent of concurrent presence of effector populations operating at H-2D. These findings are consisent with the idea that recognition is mediated via a complex receptor, part of which is specific for virus and part for self H-2. The capacity to interact with allogeneic, virus-infected cells may then reflect aberrant recognition of a virus-H-2-antigen complex by this single, large binding site. For instance, the T cell which would normally recognize H-2Kd-virus x, or H-2Dd-minor histocompatibility antigen Z, may now show specificity for H-2Kk-vaccinia virus. Implications for both the selective role of the thymus and for mechanisms of tolerance are discussed.

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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1. Functional CD8+ but not CD4+ T cell responses develop independent of thymic epithelial MHC;Proceedings of the National Academy of Sciences;2006-09-18

2. On ‘reactivity’ versus ‘tolerance’;Immunology & Cell Biology;2004-07-28

3. Negative selection imparts peptide specificity to the mature T cell repertoire;Proceedings of the National Academy of Sciences;2003-09-22

4. Efficient T cell repertoire selection in tetraparental chimeric mice independent of thymic epithelial MHC;Proceedings of the National Academy of Sciences;2003-02-06

5. On the role of thymic epithelium vs. bone marrow-derived cells in repertoire selection of T cells;Proceedings of the National Academy of Sciences;1999-07-06

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