Keap1 represses nuclear activation of antioxidant responsive elements by Nrf2 through binding to the amino-terminal Neh2 domain

  • Itoh, Ken (Center for Tsukuba Advanced Research Alliance and Institute of Basic Medical Sciences, University of Tsukuba) ;
  • Wakabayashi, Nobunao (Center for Tsukuba Advanced Research Alliance and Institute of Basic Medical Sciences, University of Tsukuba) ;
  • Katoh, Yasutake (Center for Tsukuba Advanced Research Alliance and Institute of Basic Medical Sciences, University of Tsukuba) ;
  • Ishii, Tetsuro (Center for Tsukuba Advanced Research Alliance and Institute of Basic Medical Sciences, University of Tsukuba) ;
  • Igarashi, Kazuhiko (Center for Tsukuba Advanced Research Alliance and Institute of Basic Medical Sciences, University of Tsukuba) ;
  • Engel, James Douglas (Center for Tsukuba Advanced Research Alliance and Institute of Basic Medical Sciences, University of Tsukuba) ;
  • Yamamoto, Masayuki (Center for Tsukuba Advanced Research Alliance and Institute of Basic Medical Sciences, University of Tsukuba)
  • Published : 2002.05.24

Abstract

Transcription factor Nrf2 is essential for the antioxidant responsive element (ARE)-mediated induction of phase II detoxifying and oxidative stress enzyme genes. Detailed analysis of differential Nrf2 activity displayed in transfected cell lines ultimately led to the identification of a new protein, which we named Keap1, that suppresses Nrf2 transcriptional activity by specific binding to its evolutionarily conserved amino-terminal regulatory domain. The closest homolog of Keap1 is a Drosophila actin-binding protein called Kelch, implying that Keap1 might be a Nrf2 cytoplasmic effector. We then showed that electrophilic agents antagonize Keap1 inhibition of Nrf2 activity in vivo, allowing Nrf2 to traverse from the cytoplasm to the nucleus and potentiate the ARE response. We postulate that Keap1 and Nrf2 constitute a crucial cellular sensor for oxidative stress, and together mediate a key step in the signaling pathway that leads to transcriptional activation by this novel Nrf2 nuclear shuttling mechanism. The activation of Nrf2 leads in turn to the induction of phase II enzyme and antioxidative stress genes in response to electrophiles and reactive oxygen species.

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