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From TCR Engagement to T Cell Activation

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Presentation on theme: "From TCR Engagement to T Cell Activation"— Presentation transcript:

1 From TCR Engagement to T Cell Activation
Antonio Lanzavecchia, Giandomenica Iezzi, Antonella Viola  Cell  Volume 96, Issue 1, Pages 1-4 (January 1999) DOI: /S (00)

2 Figure 1 Initiation of TCR Triggering and Signal Transduction
(a–c) Mechanisms that may promote TCR triggering. (a) Oligomerization of TCRs induced by ligand binding; (b) Cross-linking of TCR with the CD8-Lck complex induced by monovalent ligand. (c) Lateral translocation of a single TCR to a kinase-rich domain (raft) induced by actin-driven motility of the T cells and shear stress. The passive mobility of a single TCR complex is transiently decreased upon ligation to a peptide–MHC complex on APC. At the same time the rafts are laterally displaced by actin-driven motility, so that collisions between single TCRs and kinase-rich rafts are promoted. (d) Propagation of signal from the triggered TCR to raft-associated adaptors such as LAT. After TCR triggering is completed the peptide–MHC complex can dissociate and become available for another cycle of engagement and triggering. Cell  , 1-4DOI: ( /S (00) )

3 Figure 2 Serial TCR Triggering by Low-Affinity Ligands
For low-affinity ligands, such as peptide–MHC complexes, the relationship between the number of ligands displayed on an APC and the number of TCRs triggered and downregulated over time is logarithmic, indicating that the efficiency of the process is highest when only a few complexes are displayed on the APC. In contrast, in the case of high-affinity ligands the relationship is linear, indicating that they trigger TCRs on an ∼1:1 basis. TCR antagonists inhibit triggering by low-affinity but not by high-affinity ligands. Furthermore, dependency on CD4 coreceptor is a characteristic of weak agonists. The curves shown illustrate experimental observations. The dotted lines represent T cell activation thresholds in the absence or in the presence of costimulation (upper and lower lines, respectively). Cell  , 1-4DOI: ( /S (00) )

4 Figure 3 A Kinetic Window Defines Strong TCR Agonists
Hypothetical relationship between half-life of TCR-ligand interaction (black axes) and number of TCRs engaged (blue axes) or triggered (red axes) by a single ligand in a given time. Only ligands that engage TCRs within an optimal range of kinetics, that compromises between the stability necessary to perform all the steps required for triggering and the instability necessary for serial engagements, will be effective in the serial triggering process. The stippled vertical line defines the TCR triggering threshold. Cell  , 1-4DOI: ( /S (00) )

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