Litcius/Paper detail

Discovery of the First-in-Class G9a/GLP Covalent Inhibitors

Kwang‐Su Park, Yan Xiong, Hyerin Yim, Julia Velez, Nicolas Babault, Prashasti Kumar, Jing Liu, Jian Jin

2022Journal of Medicinal Chemistry45 citationsDOIOpen Access PDF

Abstract

The highly homologous protein lysine methyltransferases G9a and GLP, which catalyze mono- and dimethylation of histone H3 lysine 9 (H3K9), have been implicated in various human diseases. To investigate functions of G9a and GLP in human diseases, we and others reported several noncovalent reversible small-molecule inhibitors of G9a and GLP. Here, we report the discovery of the first-in-class G9a/GLP covalent irreversible inhibitors, 1 and 8 (MS8511), by targeting a cysteine residue at the substrate binding site. We characterized these covalent inhibitors in enzymatic, mass spectrometry based and cellular assays and using X-ray crystallography. Compared to the noncovalent G9a/GLP inhibitor UNC0642, covalent inhibitor 8 displayed improved potency in enzymatic and cellular assays. Interestingly, compound 8 also displayed potential kinetic preference for covalently modifying G9a over GLP. Collectively, compound 8 could be a useful chemical tool for studying the functional roles of G9a and GLP by covalently modifying and inhibiting these methyltransferases.

Topics & Concepts

ChemistryCovalent bondLysineMethyltransferaseCysteineEnzymeBiochemistryNon-covalent interactionsSmall moleculeResidue (chemistry)MethylationAmino acidMoleculeHydrogen bondOrganic chemistryGeneEpigenetics and DNA MethylationCancer-related gene regulationHIV Research and Treatment