T cell positive selection by a high density, low affinity ligand
- *Howard Hughes Medical Institute, Division of Basic Immunology, Department of Medicine, National Jewish Medical and Research Center, 1400 Jackson Street, Denver, CO 80206; and Departments of ‡Immunology and Medicine and §Biochemistry, Biophysics and Genetics, University of Colorado Health Sciences Center, Denver, CO 80262
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Contributed by John W. Kappler
Abstract
Interaction of the αβ T cell receptor (TCR) with major histocompatibility (MHC) molecules occupied with any of a large collection of peptides derived from self proteins is a critical step in driving T cell “positive” selection in the thymus. Interaction with this same pool of self-peptide/MHC ligands deletes T cells with potential self-reactivity. To examine how T cells survive both of these processes to form a self-tolerant mature repertoire, mice were constructed whose entire class II MHC IEk specific repertoire was positively selected on a single peptide covalently attached to the IEk molecule. In these mice T cells were identified that could respond to a variant of the positively selecting peptide bound to IEk. The affinities of the TCRs from these T cells for the positively selecting ligand were extremely low and at least 10-fold less than those for the activating ligand. These results support the theory that positive selection is driven by TCR affinities lower than those involved in T cell deletion or activation and that, if present at high concentration, even very low affinity ligands can positively select.
Footnotes
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↵ † Present address: 1450 Duarte Road, Hilton Building, Department of Immunology, Beckman Research Institute, City of Hope, Duarte, CA 91010-3000.
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↵ ¶ To whom reprint requests should be addressed. e-mail: Kapplerj{at}njc.org.
- ABBREVIATIONS:
- MHC,
- major histocompatibility complex;
- TCR,
- αβ T cell receptor;
- MCC,
- moth cytochrome c;
- IL,
- interleukin;
- Hb,
- hemoglobin β chain
- Copyright © 1998, The National Academy of Sciences
