eLife (Jan 2017)

PKCθ links proximal T cell and Notch signaling through localized regulation of the actin cytoskeleton

  • Graham J Britton,
  • Rachel Ambler,
  • Danielle J Clark,
  • Elaine V Hill,
  • Helen M Tunbridge,
  • Kerrie E McNally,
  • Bronwen R Burton,
  • Philomena Butterweck,
  • Catherine Sabatos-Peyton,
  • Lea A Hampton-O’Neil,
  • Paul Verkade,
  • Christoph Wülfing,
  • David Cameron Wraith

DOI
https://doi.org/10.7554/eLife.20003
Journal volume & issue
Vol. 6

Abstract

Read online

Notch is a critical regulator of T cell differentiation and is activated through proteolytic cleavage in response to ligand engagement. Using murine myelin-reactive CD4 T cells, we demonstrate that proximal T cell signaling modulates Notch activation by a spatiotemporally constrained mechanism. The protein kinase PKCθ is a critical mediator of signaling by the T cell antigen receptor and the principal costimulatory receptor CD28. PKCθ selectively inactivates the negative regulator of F-actin generation, Coronin 1A, at the center of the T cell interface with the antigen presenting cell (APC). This allows for effective generation of the large actin-based lamellum required for recruitment of the Notch-processing membrane metalloproteinase ADAM10. Such enhancement of Notch activation is critical for efficient T cell proliferation and Th17 differentiation. We reveal a novel mechanism that, through modulation of the cytoskeleton, controls Notch activation at the T cell:APC interface thereby linking T cell receptor and Notch signaling pathways.

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