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Discrete LAT condensates encode antigen information from single pMHC:TCR binding events.


ABSTRACT: LAT assembly into a two-dimensional protein condensate is a prominent feature of antigen discrimination by T cells. Here, we use single-molecule imaging techniques to resolve the spatial position and temporal duration of each pMHC:TCR molecular binding event while simultaneously monitoring LAT condensation at the membrane. An individual binding event is sufficient to trigger a LAT condensate, which is self-limiting, and neither its size nor lifetime is correlated with the duration of the originating pMHC:TCR binding event. Only the probability of the LAT condensate forming is related to the pMHC:TCR binding dwell time. LAT condenses abruptly, but after an extended delay from the originating binding event. A LAT mutation that facilitates phosphorylation at the PLC-γ1 recruitment site shortens the delay time to LAT condensation and alters T cell antigen specificity. These results identify a function for the LAT protein condensation phase transition in setting antigen discrimination thresholds in T cells.

SUBMITTER: McAffee DB 

PROVIDER: S-EPMC9718779 | biostudies-literature | 2022 Dec

REPOSITORIES: biostudies-literature

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Discrete LAT condensates encode antigen information from single pMHC:TCR binding events.

McAffee Darren B DB   O'Dair Mark K MK   Lin Jenny J JJ   Low-Nam Shalini T ST   Wilhelm Kiera B KB   Kim Sungi S   Morita Shumpei S   Groves Jay T JT  

Nature communications 20221202 1


LAT assembly into a two-dimensional protein condensate is a prominent feature of antigen discrimination by T cells. Here, we use single-molecule imaging techniques to resolve the spatial position and temporal duration of each pMHC:TCR molecular binding event while simultaneously monitoring LAT condensation at the membrane. An individual binding event is sufficient to trigger a LAT condensate, which is self-limiting, and neither its size nor lifetime is correlated with the duration of the origina  ...[more]

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