Properly Substituted Analogues of BIX-01294 Lose Inhibition of G9a Histone Methyltransferase and Gain Selective Anti-DNA Methyltransferase 3A Activity

Dante Rotili,Domenico Tarantino,Biagina Marrocco,Christina Gros,Véronique Masson,Valérie Poughon,Frédéric Ausseil,Yanqi Chang,Donatella Labella,Sandro Cosconati,Salvatore Di Maro,Ettore Novellino,Michael Schnekenburger,Cindy Grandjenette,Céline Bouvy,Marc Diederich,Xiaodong Cheng,Paola B. Arimondo,Antonello Mai

Properly Substituted Analogues of BIX-01294 Lose Inhibition of G9a Histone Methyltransferase and Gain Selective Anti-DNA Methyltransferase 3A Activity

2014

Dante Rotili
Domenico Tarantino
Biagina Marrocco
Christina Gros
Véronique Masson
Valérie Poughon
Frédéric Ausseil
Yanqi Chang
Donatella Labella
Sandro Cosconati
Salvatore Di Maro
Ettore Novellino
Michael Schnekenburger
Cindy Grandjenette
Céline Bouvy
Marc Diederich
Xiaodong Cheng
Paola B. Arimondo
Antonello Mai

Chemical manipulations performed on the histone H3 lysine 9 methyltransferases (G9a/GLP) inhibitor BIX-01294 afforded novel desmethoxyquinazolines able to inhibit the DNA methyltransferase DNMT3A at low micromolar levels without any significant inhibition of DNMT1 and G9a. In KG-1 cells such compounds, when tested at sub-toxic doses, induced the luciferase re-expression in a stable construct controlled by a cytomegalovirus (CMV) promoter silenced by methylation (CMV-luc assay). Finally, in human lymphoma U-937 and RAJI cells, the N-(1-benzylpiperidin-4-yl)-2-(4-phenylpiperazin-1yl)quinazolin-4-amine induced the highest proliferation arrest and cell death induction starting from 10 mM, in agreement with its DNMT3A inhibitory potency.

Keywords:

Histone H3
Methylation
DNMT1
Luciferase
DNA methyltransferase
Raji cell
Methyltransferase
Histone methyltransferase
Molecular biology
Biochemistry
Biology
Histone
DNA methylation

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