Halogenated Flavonoid Derivatives Display Antiangiogenic Activity

Overview

Journal Molecules

Publisher MDPI

Specialty Biology

Date 2022 Jul 28

PMID 35897938

Authors

Mai Khater

Kimberly A Watson

Samuel Y Boateng

Francesca Greco

Helen M I Osborn

Affiliations

Soon will be listed here.

Abstract

Antiangiogenic agents attenuate tumours' growth and metastases and are therefore beneficial as an adjuvant or standalone cancer regimen. Drugs with dual antiproliferative and antiangiogenic activities can achieve anticancer efficacy and overcome acquired resistance. In this study, synthetic flavones (,) with reported anticancer activity, and derivatives ( and ), exhibited significant inhibition of endothelial cell tube formation (40-55%, 12 h) at 1 µM, which is comparable to sunitinib (50% inhibition at 1 µM, 48 h). Flavones (, , and ) also showed 25-37% reduction in HUVECs migration at 10 µM. In a Western blotting assay, and subdued VEGFR2 phosphorylation by 37% and 57%, respectively, suggesting that VEGFR2 may be their main antiangiogenic target. displayed the best docking fit with VEGFR2 in an in silico study, followed by , emphasizing the importance of the 7-hydroxyl group accompanied by a 4-C=S for activity. Conversely, derivatives with a 4-carbonyl moiety fitted poorly into the target's binding pocket, suggesting that their antiangiogenic activity depends on a different target. This study provides valuable insight into the Structure Activity Relationships (SAR) and modes of action of halogenated flavones with VEGFR2 and highlights their therapeutic potential as antiangiogenic/anticancer lead compounds.

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