The discovery of potent ribosomal S6 kinase inhibitors by high-throughput screening and structure-guided drug design

نویسندگان

  • Sylvain Couty
  • Isaac M. Westwood
  • Andrew Kalusa
  • Celine Cano
  • Jon Travers
  • Kathy Boxall
  • Chiau Ling Chow
  • Sam Burns
  • Jessica Schmitt
  • Lisa Pickard
  • Caterina Barillari
  • P. Craig McAndrew
  • Paul A. Clarke
  • Spiros Linardopoulos
  • Roger J. Griffin
  • G. Wynne Aherne
  • Florence I. Raynaud
  • Paul Workman
  • Keith Jones
  • Rob L.M. van Montfort
چکیده

The ribosomal P70 S6 kinases play a crucial role in PI3K/mTOR regulated signalling pathways and are therefore potential targets for the treatment of a variety of diseases including diabetes and cancer. In this study we describe the identification of three series of chemically distinct S6K1 inhibitors. In addition, we report a novel PKA-S6K1 chimeric protein with five mutations in or near its ATP-binding site, which was used to determine the binding mode of two of the three inhibitor series, and provided a robust system to aid the optimisation of the oxadiazole-substituted benzimidazole inhibitor series. We show that the resulting oxadiazole-substituted aza-benzimidazole is a potent and ligand efficient S6 kinase inhibitor, which blocks the phosphorylation of RPS6 at Ser235/236 in TSC negative HCV29 human bladder cancer cells by inhibiting S6 kinase activity and thus provides a useful tool compound to investigate the function of S6 kinases.

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عنوان ژورنال:

دوره 4  شماره 

صفحات  -

تاریخ انتشار 2013