| Literature DB >> 32075099 |
Clemens Zwergel1,2, Rossella Fioravanti1, Giulia Stazi1, Federica Sarno2, Cecilia Battistelli3, Annalisa Romanelli1, Angela Nebbioso2, Eduarda Mendes4, Alexandra Paulo4, Raffaele Strippoli3,5, Marco Tripodi3,5,6, Dany Pechalrieu7, Paola B Arimondo7,8, Teresa De Luca9, Donatella Del Bufalo9, Daniela Trisciuoglio9,10, Lucia Altucci2, Sergio Valente1, Antonello Mai1.
Abstract
DNA methyltransferases (DNMTs) play a relevant role in epigenetic control of cancer cell survival and proliferation. Since only two DNMT inhibitors (azacitidine and decitabine) have been approved to date for the treatment of hematological malignancies, the development of novel potent and specific inhibitors is urgent. Here we describe the design, synthesis, and biological evaluation of a new series of compounds acting at the same time as DNMTs (mainly DNMT3A) inhibitors and degraders. Tested against leukemic and solid cancer cell lines, 2a-c and 4a-c (the last only for leukemias) displayed up to submicromolar antiproliferative activities. In HCT116 cells, such compounds induced EGFP gene expression in a promoter demethylation assay, confirming their demethylating activity in cells. In the same cell line, 2b and 4c chosen as representative samples induced DNMT1 and -3A protein degradation, suggesting for these compounds a double mechanism of DNMT3A inhibition and DNMT protein degradation.Entities:
Keywords: DNA methyltransferase; apoptosis; drug discovery; enzyme inhibition; medicinal chemistry; protein degradation
Year: 2020 PMID: 32075099 DOI: 10.3390/cancers12020447
Source DB: PubMed Journal: Cancers (Basel) ISSN: 2072-6694 Impact factor: 6.639