Journal of Medicinal Chemistry p. 6546 - 6573 (2018)
Update date:2022-08-15
Topics:
Rabal, Obdulia
Sánchez-Arias, Juan Antonio
José-Enériz, Edurne San
Agirre, Xabier
De Miguel, Irene
Garate, Leire
Miranda, Estibaliz
Sáez, Elena
Roa, Sergio
Martínez-Climent, José Angel
Liu, Yingying
Wu, Wei
Xu, Musheng
Prosper, Felipe
Oyarzabal, Julen
Epigenetic regulators that exhibit aberrant enzymatic activities or expression profiles are potential therapeutic targets for cancers. Specifically, enzymes responsible for methylation at histone-3 lysine-9 (like G9a) and aberrant DNA hypermethylation (DNMTs) have been implicated in a number of cancers. Recently, molecules bearing a 4-aminoquinoline scaffold were reported as dual inhibitors of these targets and showed a significant in vivo efficacy in animal models of hematological malignancies. Here, we report a detailed exploration around three growing vectors born by this chemotype. Exploring this chemical space led to the identification of features to navigate G9a and DNMT1 biological spaces: not only their corresponding exclusive areas, selective compounds, but also common spaces. Thus, we identified from selective G9a and first-in-class DNMT1 inhibitors, >1 log unit between their IC50 values, with IC50 < 25 nM (e.g., 43 and 26, respectively) to equipotent inhibitors with IC50 < 50 nM for both targets (e.g., 13). Their ADME/Tox profiling and antiproliferative efficacies, versus some cancer cell lines, are also reported.
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