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Light-based tuning of ligand half-life supports kinetic proofreading model of T cell signaling.

eLife (2019-04-06)
Doug K Tischer, Orion David Weiner
RESUMEN

T cells are thought to discriminate self from foreign peptides by converting small differences in ligand binding half-life into large changes in cell signaling. Such a kinetic proofreading model has been difficult to test directly, as existing methods of altering ligand binding half-life also change other potentially important biophysical parameters, most notably the mechanical stability of the receptor-ligand interaction. Here we develop an optogenetic approach to specifically tune the binding half-life of a chimeric antigen receptor without changing other binding parameters and provide direct evidence of kinetic proofreading in T cell signaling. This half-life discrimination is executed in the proximal signaling pathway, downstream of ZAP70 recruitment and upstream of diacylglycerol accumulation. Our methods represent a general tool for temporal and spatial control of T cell signaling and extend the reach of optogenetics to probe pathways where the individual molecular kinetics, rather than the ensemble average, gates downstream signaling.

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Sigma-Aldrich
Acetona, histological grade, ≥99.5%
Sigma-Aldrich
Maleimide, 99%
Hellmanex III, Special Cleaning Concentrate for cuvettes
BRAND® glass staining trough, Coplin pattern, soda-lime glass
Sigma-Aldrich
PP2, ≥98% (HPLC)