PLoS ONE (Jan 2012)

Regulation of CD4⁺ and CD8⁺ effector responses by Sprouty-1.

  • Sam Collins,
  • Adam Waickman,
  • Albert Basson,
  • Abraham Kupfer,
  • Jonathan D Licht,
  • Maureen R Horton,
  • Jonathan D Powell

DOI
https://doi.org/10.1371/journal.pone.0049801
Journal volume & issue
Vol. 7, no. 11
p. e49801

Abstract

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TCR-induced NF-AT activation leads to the expression of both activating and inhibitory proteins. Previously, we had identified Egr-2 and Egr-3 as NF-AT-induced transcription factors which promote the inhibition of T cell activation. In this report we identify Sprouty1 as a downstream target of Egr-3. CD4⁺ T cells lacking Spry1 demonstrate enhanced proliferation and cytokine production. Likewise, Spry1(Flox/Flox) Lck Cre CD8⁺ T cells display increased cytolytic activity. Mechanistically, Spry1 acts at the level of PLC-γ promoting the inhibition of both Ca⁺⁺ induced NF-AT activation and MAP-kinase induced AP-1 activation while sparing NF-κB signaling. In vivo, mice in which Spry1 is selectively deleted in T cells demonstrate enhanced responses to a tumor vaccine and subsequently reject tumors more robustly than Wt mice. These findings suggest that targeting Spry1 might prove to be a novel means of enhancing tumor immunotherapy.