PLoS ONE (Jan 2014)

CKIP-1 is an intrinsic negative regulator of T-cell activation through an interaction with CARMA1.

  • Takashi Sakamoto,
  • Masayuki Kobayashi,
  • Kohei Tada,
  • Masanobu Shinohara,
  • Katsuhiro Io,
  • Kayoko Nagata,
  • Fumie Iwai,
  • Yoko Takiuchi,
  • Yasuyuki Arai,
  • Kouhei Yamashita,
  • Keisuke Shindo,
  • Norimitsu Kadowaki,
  • Yoshio Koyanagi,
  • Akifumi Takaori-Kondo

DOI
https://doi.org/10.1371/journal.pone.0085762
Journal volume & issue
Vol. 9, no. 1
p. e85762

Abstract

Read online

The transcription factor NF-κB plays a key regulatory role in lymphocyte activation and generation of immune response. Stimulation of T cell receptor (TCR) induces phosphorylation of CARMA1 by PKCθ, resulting in formation of CARMA1-Bcl10-MALT1 (CBM) complex at lipid rafts and subsequently leading to NF-κB activation. While many molecular events leading to NF-κB activation have been reported, it is less understood how this activation is negatively regulated. We performed a cell-based screening for negative regulators of TCR-mediated NF-κB activation, using mutagenesis and complementation cloning strategies. Here we show that casein kinase-2 interacting protein-1 (CKIP-1) suppresses PKCθ-CBM-NF-κB signaling. We found that CKIP-1 interacts with CARMA1 and competes with PKCθ for association. We further confirmed that a PH domain of CKIP-1 is required for association with CARMA1 and its inhibitory effect. CKIP-1 represses NF-κB activity in unstimulated cells, and inhibits NF-κB activation induced by stimulation with PMA or constitutively active PKCθ, but not by stimulation with TNFα. Interestingly, CKIP-1 does not inhibit NF-κB activation induced by CD3/CD28 costimulation, which caused dissociation of CKIP-1 from lipid rafts. These data suggest that CKIP-1 contributes maintenance of a resting state on NF-κB activity or prevents T cells from being activated by inadequate signaling. In conclusion, we demonstrate that CKIP-1 interacts with CARMA1 and has an inhibitory effect on PKCθ-CBM-NF-κB signaling.