Identification of Novel
Inhibitors of DNA Methylation
by Screening of a Chemical Library
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Abstract
In order to discover new inhibitors of the DNA methyltransferase
3A/3L complex, we used a medium-throughput nonradioactive screen on
a random collection of 1120 small organic compounds. After a primary
hit detection against DNA methylation activity of the murine Dnmt3A/3L
catalytic complex, we further evaluated the EC<sub>50</sub> of the
12 most potent hits as well as their cytotoxicity on DU145 prostate
cancer cultured cells. Interestingly, most of the inhibitors showed
low micromolar activities and little cytotoxicity. Dichlone, a small
halogenated naphthoquinone, classically used as pesticide and fungicide,
showed the lowest EC<sub>50</sub> at 460 nM. We briefly assessed the
selectivity of a subset of our new inhibitors against hDNMT1 and bacterial
Dnmts, including M. SssI and EcoDam, and the protein lysine methyltransferase
PKMT G9a and the mode of inhibition. Globally, the tested molecules
showed a clear preference for the DNA methyltransferases, but poor
selectivity among them. Two molecules including Dichlone efficiently
reactivated YFP gene expression in a stable HEK293 cell line by promoter
demethylation. Their efficacy was comparable to the DNMT inhibitor
of reference 5-azacytidine