Antigen perception in T cells by long-term Erk and NFAT signaling dynamics

Author:

Wither Matthew J.1ORCID,White William L.1ORCID,Pendyala Sriram2ORCID,Leanza Paul J.1,Fowler Douglas M.2,Kueh Hao Yuan13ORCID

Affiliation:

1. University of Washington, Department of Bioengineering, Seattle, WA 98195

2. University of Washington, Department of Genome Sciences, Seattle, WA 98195

3. Institute for Stem Cell and Regenerative Medicine, University of Washington, Seattle, WA 98109

Abstract

Immune system threat detection hinges on T cells’ ability to perceive varying peptide–major histocompatibility complex (pMHC) antigens. As the Erk and NFAT pathways link T cell receptor engagement to gene regulation, their signaling dynamics may convey information about pMHC inputs. To test this idea, we developed a dual reporter mouse strain and a quantitative imaging assay that, together, enable simultaneous monitoring of Erk and NFAT dynamics in live T cells over day-long timescales as they respond to varying pMHC inputs. Both pathways initially activate uniformly across various pMHC inputs but diverge only over longer (9+ h) timescales, enabling independent encoding of pMHC affinity and dose. These late signaling dynamics are decoded via multiple temporal and combinatorial mechanisms to generate pMHC-specific transcriptional responses. Our findings underscore the importance of long timescale signaling dynamics in antigen perception and establish a framework for understanding T cell responses under diverse contexts.

Funder

NIH/NIBIB

NIH/NHGRI

NSF

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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