Journal of Enzyme Inhibition and Medicinal Chemistry (Jan 2020)

Design of new disubstituted imidazo[1,2-b]pyridazine derivatives as selective Haspin inhibitors. Synthesis, binding mode and anticancer biological evaluation

  • Jonathan Elie,
  • Omid Feizbakhsh,
  • Nathalie Desban,
  • Béatrice Josselin,
  • Blandine Baratte,
  • Amandine Bescond,
  • Julien Duez,
  • Xavier Fant,
  • Stéphane Bach,
  • Dominique Marie,
  • Matthieu Place,
  • Sami Ben Salah,
  • Agnes Chartier,
  • Sabine Berteina-Raboin,
  • Apirat Chaikuad,
  • Stefan Knapp,
  • Fabrice Carles,
  • Pascal Bonnet,
  • Frédéric Buron,
  • Sylvain Routier,
  • Sandrine Ruchaud

DOI
https://doi.org/10.1080/14756366.2020.1825408
Journal volume & issue
Vol. 35, no. 1
pp. 1840 – 1853

Abstract

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Haspin is a mitotic protein kinase required for proper cell division by modulating Aurora B kinase localisation and activity as well as histone phosphorylation. Here a series of imidazopyridazines based on the CHR-6494 and Structure Activity Relationship was established. An assessment of the inhibitory activity of the lead structures on human Haspin and several other protein kinases is presented. The lead structure was rapidly optimised using a combination of crystal structures and effective docking models, with the best inhibitors exhibiting potent inhibitory activity on Haspin with IC50 between 6 and 100 nM in vitro. The developed inhibitors displayed anti-proliferative properties against various human cancer cell lines in 2D and spheroid cultures and significantly inhibited the migration ability of osteosarcoma U-2 OS cells. Notably, we show that our lead compounds are powerful Haspin inhibitors in human cells, and did not block G2/M cell cycle transition due to improved selectivity against CDK1/CyclinB.

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