Identification and optimization of hydrazone-gallate derivatives as specific inhibitors of DNA methyltransferase 3A

Author:

Erdmann Alexandre1,Menon Yoann1,Gros Christina1,Masson Véronique1,Aussagues Yannick1,Ausseil Fréderic1,Novosad Natacha1,Schambel Philippe2,Baltas Michel34,Arimondo Paola B1

Affiliation:

1. Unité de Service et de Recherche CNRS-Pierre Fabre USR n°3388, ETaC, CRDPF, 31100 Toulouse, France

2. Institut de Recherche Pierre Fabre, 81106 Castres, France

3. CNRS, Laboratoire de Synthèse et Physico-Chimie de Molécules d’Intérêt Biologique, SPCMIB, UMR-5068, 118 Route de Narbonne, 31062 Toulouse cedex 9, France

4. Université de Toulouse, UPS, Laboratoire de Synthèse et Physico-Chimie de Molécules d’Intérêt Biologique, SPCMIB, 118 route de Narbonne,31062 Toulouse cedex 9, France

Abstract

DNA methylation is the most studied epigenetic event. Since the methylation profile of the genome is widely modified in cancer cells, DNA methyltransferases are the target of new anticancer therapies. Nucleosidic inhibitors suffer from toxicity and chemical stability, while non-nucleosidic inhibitors lack potency. Here, we found a novel DNMT inhibitor scaffold by enzymatic screening and structure–activity relationship studies. The optimization studies led to an inhibitor containing three fragments: a gallate frame, a hydrazone linker and a benzothiazole moiety. Interestingly, the compound inhibits DNMT3A with micromolar potency (EC50 = 1.6 μM) and does not inhibit DNMT1; this DNMT3A selectivity is supported by a docking study. Finally, the compound reactivates a reporter gene in leukemia KG-1 cells.

Publisher

Future Science Ltd

Subject

Drug Discovery,Pharmacology,Molecular Medicine

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