| Literature DB >> 30412404 |
Antonella Messore1, Valentina Noemi Madia1, Luca Pescatori1, Francesco Saccoliti1, Valeria Tudino1, Alessandro De Leo1, Martina Bortolami1, Daniela De Vita1, Luigi Scipione1, Federico Pepi1, Roberta Costi1, Silvia Rivara2, Laura Scalvini2, Marco Mor2, Fabiana Fosca Ferrara3, Emiliano Pavoni3, Giuseppe Roscilli3, Giuliana Cassinelli4, Ferdinando M Milazzo5, Gianfranco Battistuzzi5, Roberto Di Santo1, Giuseppe Giannini5.
Abstract
Heparanase is the only mammalian endo-β-d-glucuronidase involved in a variety of major diseases. The up-regulation of heparanase expression increases tumor size, angiogenesis, and metastasis, representing a validated target in the anti-cancer field. To date, only a few small-molecule inhibitors have been described, but none have gotten through pre-clinical development. Previously, we explored 2-(4-(4-(bromo-methoxybenzamido)benzylamino)phenyl) benzazole derivatives as anti-heparanase agents, proposing this scaffold for development of broadly effective heparanase inhibitors. Herein, we report an extended investigation of new symmetrical 2-aminophenyl-benzazolyl-5-acetate derivatives, proving that symmetrical compounds are more effective than asymmetrical analogues, with the most-potent compound, 7g, being active at nanomolar concentration against heparanase. Molecular docking studies were performed on the best-acting compounds 5c and 7g to rationalize their interaction with the enzyme. Moreover, invasion assay confirmed the anti-metastatic potential of compounds 5c, 7a, and 7g, proving the inhibition of the expression of proangiogenic factors in tumor cells.Entities:
Mesh:
Substances:
Year: 2018 PMID: 30412404 DOI: 10.1021/acs.jmedchem.8b01497
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446