A small molecule modulates Jumonji histone demethylase activity and selectively inhibits cancer growth

نویسندگان

  • Lei Wang
  • Jianjun Chang
  • Diana Varghese
  • Michael Dellinger
  • Subodh Kumar
  • Anne M. Best
  • Julio Ruiz
  • Richard Bruick
  • Samuel Peña-Llopis
  • Junjie Xu
  • David J. Babinski
  • Doug E. Frantz
  • Rolf A. Brekken
  • Amy M. Quinn
  • Anton Simeonov
  • Johnny Easmon
  • Elisabeth D. Martinez
چکیده

The pharmacological inhibition of general transcriptional regulators has the potential to block growth through targeting multiple tumorigenic signalling pathways simultaneously. Here, using an innovative cell-based screen, we identify a structurally unique small molecule (named JIB-04) that specifically inhibits the activity of the Jumonji family of histone demethylases in vitro, in cancer cells, and in tumours in vivo. Unlike known inhibitors, JIB-04 is not a competitive inhibitor of α-ketoglutarate. In cancer, but not in patient-matched normal cells, JIB-04 alters a subset of transcriptional pathways and blocks viability. In mice, JIB-04 reduces tumour burden and prolongs survival. Importantly, we find that patients with breast tumours that overexpress Jumonji demethylases have significantly lower survival. Thus, JIB-04, a novel inhibitor of Jumonji demethylases in vitro and in vivo, constitutes a unique potential therapeutic and research tool against cancer, and validates the use of unbiased cellular screens to discover chemical modulators with disease relevance.

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عنوان ژورنال:

دوره 4  شماره 

صفحات  -

تاریخ انتشار 2013