| Literature DB >> 24752068 |
Lucia Borriello1, Matthieu Montès2, Yves Lepelletier3, Bertrand Leforban1, Wang-Qing Liu1, Luc Demange1, Brigitte Delhomme4, Serena Pavoni1, Rafika Jarray1, Jean Luc Boucher1, Sylvie Dufour5, Olivier Hermine3, Christiane Garbay1, Réda Hadj-Slimane6, Françoise Raynaud7.
Abstract
Neuropilin-1/-2 (+33 NRPs), VEGF-A165 co-receptors, are over-expressed during cancer progression. Thus, NRPs targeted drug development is challenged using a multistep in silico/in vitro screening procedure. The first fully non-peptidic VEGF-A165/NRPs protein-protein interaction antagonist (IC50=34 μM) without effect on pro-angiogenic kinases has been identified (compound-1). This hit showed breast cancer cells anti-proliferative activity (IC50=0.60 μM). Compound-1 treated NOG-xenografted mice significantly exerted tumor growth inhibition, which is correlated with Ki-67(low) expression and apoptosis. Furthermore, CD31(+)/CD34(+) vessels are reduced in accordance with HUVEC-tube formation inhibition (IC50=0.20 μM). Taking together, compound-1 is the first fully organic inhibitor targeting NRPs.Entities:
Keywords: Fully organic inhibitors; Neuropilin; Protein–protein interaction; Tumor growth inhibition
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Year: 2014 PMID: 24752068 DOI: 10.1016/j.canlet.2014.04.004
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679