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:10.1080/14756366.2020.1811701

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

Affiliations

Daniele Pala: Dipartimento di Scienze degli Alimenti e del Farmaco, Università degli Studi di Parma
Laura Scalvini: Dipartimento di Scienze degli Alimenti e del Farmaco, Università degli Studi di Parma
Gian Marco Elisi: Dipartimento di Scienze degli Alimenti e del Farmaco, Università degli Studi di Parma
Alessio Lodola: Dipartimento di Scienze degli Alimenti e del Farmaco, Università degli Studi di Parma
Marco Mor: Dipartimento di Scienze degli Alimenti e del Farmaco, Università degli Studi di Parma
Gilberto Spadoni: Dipartimento di Scienze Biomolecolari, Università degli Studi di Urbino “Carlo Bo”
Fabiana F. Ferrara: Takis s.r.l
Emiliano Pavoni: Takis s.r.l
Giuseppe Roscilli: Takis s.r.l
Ferdinando M. Milazzo: R&D Alfasigma S.p.A
Gianfranco Battistuzzi: R&D Alfasigma S.p.A
Silvia Rivara: Dipartimento di Scienze degli Alimenti e del Farmaco, Università degli Studi di Parma
Giuseppe Giannini: R&D Alfasigma S.p.A

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.

Published in Journal of Enzyme Inhibition and Medicinal Chemistry

ISSN: 1475-6366 (Print); 1475-6374 (Online)
Publisher: Taylor & Francis Group
Country of publisher: United Kingdom
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: https://www.tandfonline.com/journals/ienz

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