Development and in vivo evaluation of fused benzazole analogs of anti-melanoma agent HA15

Author:

Millet Antoine1,Filho Mauro Safir1ORCID,Hamouda-Tekaya Nedra2,Cavazza Elisa2,Abbe Patricia2,Rüdiger Johanna1,Plaisant Magali2,Mayen Julie1,Rocchi Stéphane2ORCID,Ronco Cyril1ORCID,Benhida Rachid13ORCID

Affiliation:

1. Institut de Chimie de Nice CRNS UMR7272, Université Côte d’Azur, 28 Avenue Valrose, Nice, 06108, France

2. Centre Méditerranéen de Médecine Moléculaire (C3M), INSERM, U1065, Team 12, Université Côte d’Azur, 151 Route de Saint-Antoine de Ginestière, Nice, 06200, France

3. Mohamed VI Polytechnic University, UM6P, Department of Chemical and Biochemical Sciences, Green ProcessEngineering, CBS, Ben Guerir, 43150, Morocco

Abstract

Background: In line with our recent discovery of an efficient anticancer thiazolebenzenesulfonamide framework HA15 (1) based on a remarkable endoplasmic reticulum stress inducement mode of action, we report herein a series of innovative constrained HA15 analogs, featuring four types of bicylic derivatives. Results: The structure–activity relationship analysis, using a cell line assay, led us to identify a novel version of HA15: a new benzothiazole derivative (10b) exhibiting important anti-melanoma effect against sensitive and resistant melanoma cells. Meanwhile, compound 10b induced a significant tumor growth inhibition in vivo with no apparent signs of toxicity. Conclusion: These results consistently open new directions to improve and develop more powerful anticancer therapeutics harboring this type of fused framework.

Funder

Université Côte d’Azur

Institut National Du Cancer

Cancéropôle PACA

Publisher

Future Science Ltd

Subject

Drug Discovery,Pharmacology,Molecular Medicine

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