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  4. Coreceptor scanning by the T cell receptor provides a mechanism for T cell tolerance
 
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Coreceptor scanning by the T cell receptor provides a mechanism for T cell tolerance

Date Issued
2014-01-01
Author(s)
Stepanek, Ondrej
Prabhakar, Arvind S.
Osswald, Celine
King, Carolyn G.  
Bulek, Anna
Naeher, Dieter
Beaufils-Hugot, Marina
Abanto, Michael L.
Galati, Virginie
Hausmann, Barbara
Lang, Rosemarie
Cole, David K.
Huseby, Eric S.
Sewell, Andrew K.
Chakraborty, Arup K.
Palmer, Ed  
DOI
10.1016/j.cell.2014.08.042
Abstract
In the thymus, high-affinity, self-reactive thymocytes are eliminated from the pool of developing T cells, generating central tolerance. Here, we investigate how developing T cells measure self-antigen affinity. We show that very few CD4 or CD8 coreceptor molecules are coupled with the signal-initiating kinase, Lck. To initiate signaling, an antigen-engaged T cell receptor (TCR) scans multiple coreceptor molecules to find one that is coupled to Lck; this is the first and rate-limiting step in a kinetic proofreading chain of events that eventually leads to TCR triggering and negative selection. MHCII-restricted TCRs require a shorter antigen dwell time (0.2 s) to initiate negative selection compared to MHCI-restricted TCRs (0.9 s) because more CD4 coreceptors are Lck-loaded compared to CD8. We generated a model (Lck come&stay/signal duration) that accurately predicts the observed differences in antigen dwell-time thresholds used by MHCI- and MHCII-restricted thymocytes to initiate negative selection and generate self-tolerance.
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