| Literature DB >> 27427228 |
John R Horton1, Xu Liu1, Molly Gale2, Lizhen Wu2, John R Shanks1, Xing Zhang1, Philip J Webber3, Joshua S K Bell4, Stephen C Kales5, Bryan T Mott5, Ganesha Rai5, Daniel J Jansen5, Mark J Henderson5, Daniel J Urban5, Matthew D Hall5, Anton Simeonov5, David J Maloney5, Margaret A Johns3, Haian Fu6, Ajit Jadhav5, Paula M Vertino7, Qin Yan8, Xiaodong Cheng9.
Abstract
The KDM5/JARID1 family of Fe(II)- and α-ketoglutarate-dependent demethylases removes methyl groups from methylated lysine 4 of histone H3. Accumulating evidence supports a role for KDM5 family members as oncogenic drivers. We compare the in vitro inhibitory properties and binding affinity of ten diverse compounds with all four family members, and present the crystal structures of the KDM5A-linked Jumonji domain in complex with eight of these inhibitors in the presence of Mn(II). All eight inhibitors structurally examined occupy the binding site of α-ketoglutarate, but differ in their specific binding interactions, including the number of ligands involved in metal coordination. We also observed inhibitor-induced conformational changes in KDM5A, particularly those residues involved in the binding of α-ketoglutarate, the anticipated peptide substrate, and intramolecular interactions. We discuss how particular chemical moieties contribute to inhibitor potency and suggest strategies that might be utilized in the successful design of selective and potent epigenetic inhibitors.Entities:
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Year: 2016 PMID: 27427228 PMCID: PMC4958579 DOI: 10.1016/j.chembiol.2016.06.006
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116