| Literature DB >> 28186757 |
Paola Vianello1, Luca Sartori1, Federica Amigoni1, Anna Cappa1, Giovanni Fagá1, Raimondo Fattori1, Elena Legnaghi1, Giuseppe Ciossani2, Andrea Mattevi2, Giuseppe Meroni1, Loris Moretti1, Valentina Cecatiello3,4, Sebastiano Pasqualato3, Alessia Romussi1, Florian Thaler1, Paolo Trifiró1, Manuela Villa1, Oronza A Botrugno1, Paola Dessanti1, Saverio Minucci1,5, Stefania Vultaggio1, Elisa Zagarrí1, Mario Varasi1, Ciro Mercurio1,6.
Abstract
The balance of methylation levels at histone H3 lysine 4 (H3K4) is regulated by KDM1A (LSD1). KDM1A is overexpressed in several tumor types, thus representing an emerging target for the development of novel cancer therapeutics. We have previously described ( Part 1, DOI 10.1021.acs.jmedchem.6b01018 ) the identification of thieno[3,2-b]pyrrole-5-carboxamides as novel reversible inhibitors of KDM1A, whose preliminary exploration resulted in compound 2 with biochemical IC50 = 160 nM. We now report the structure-guided optimization of this chemical series based on multiple ligand/KDM1A-CoRest cocrystal structures, which led to several extremely potent inhibitors. In particular, compounds 46, 49, and 50 showed single-digit nanomolar IC50 values for in vitro inhibition of KDM1A, with high selectivity in secondary assays. In THP-1 cells, these compounds transcriptionally affected the expression of genes regulated by KDM1A such as CD14, CD11b, and CD86. Moreover, 49 and 50 showed a remarkable anticlonogenic cell growth effect on MLL-AF9 human leukemia cells.Entities:
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Year: 2017 PMID: 28186757 DOI: 10.1021/acs.jmedchem.6b01019
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446