Journal of Enzyme Inhibition and Medicinal Chemistry (Jan 2020)

New classes of potent heparanase inhibitors from ligand-based virtual screening

  • Daniele Pala,
  • Laura Scalvini,
  • Gian Marco Elisi,
  • Alessio Lodola,
  • Marco Mor,
  • Gilberto Spadoni,
  • Fabiana F. Ferrara,
  • Emiliano Pavoni,
  • Giuseppe Roscilli,
  • Ferdinando M. Milazzo,
  • Gianfranco Battistuzzi,
  • Silvia Rivara,
  • Giuseppe Giannini

DOI
https://doi.org/10.1080/14756366.2020.1811701
Journal volume & issue
Vol. 35, no. 1
pp. 1685 – 1696

Abstract

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Heparanase is a validated target in cancer therapy and a potential target for several inflammatory pathologies. A ligand-based virtual screening of commercial libraries was performed to expand the chemical space of small-molecule inhibitors. The screening was based on similarity with known inhibitors and was performed in several runs, starting from literature compounds and progressing through newly discovered inhibitors. Among the fifty-five tested compounds, nineteen had IC50 values lower than 5 µM and some showed remarkable potencies. Importantly, tere- and isophthalamides derivatives belong to new structural classes of heparanase inhibitors and some of them showed enzyme affinities (61 and 63, IC50 = 0.32 and 0.12 µM, respectively) similar to those of the most potent small-molecule inhibitors reported so far. Docking studies provided a comprehensive binding hypothesis shared by compounds with significant structural diversity. The most potent inhibitors reduced cell invasiveness and inhibited the expression of proangiogenic factors in tumour cell lines.

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