The Impact of Duration versus Extent of TCR Occupancy on T Cell Activation: A Revision of the Kinetic Proofreading Model

The widely accepted kinetic proofreading theory proposes that rapid TCR dissociation from a peptide/MHC ligand allows for stimulation of early but not late T cell activation events, explaining why low-affinity TCR ligands are poor agonists. We identified a low-affinity TCR ligand which stimulated la...

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Veröffentlicht in:Immunity (Cambridge, Mass.) Mass.), 2001-07, Vol.15 (1), p.59-70
Hauptverfasser: Rosette, Caridad, Werlen, Guy, Daniels, Mark A, Holman, Philmore O, Alam, S.Munir, Travers, Paul J, Gascoigne, Nicholas R.J, Palmer, Ed, Jameson, Stephen C
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Sprache:eng
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Zusammenfassung:The widely accepted kinetic proofreading theory proposes that rapid TCR dissociation from a peptide/MHC ligand allows for stimulation of early but not late T cell activation events, explaining why low-affinity TCR ligands are poor agonists. We identified a low-affinity TCR ligand which stimulated late T cell responses but, contrary to predictions from kinetic proofreading, inefficiently induced early activation events. Furthermore, responses induced by this ligand were kinetically delayed compared to its high-affinity counterpart. Using peptide/MHC tetramers, we showed that activation characteristics could be dissociated from TCR occupancy by the peptide/MHC ligands. Our data argue that T cell responses are triggered by a cumulative signal which is reached at different time points for different TCR ligands.
ISSN:1074-7613
1097-4180
DOI:10.1016/S1074-7613(01)00173-X