Discovery of Isoxazole Amides as Potent and Selective SMYD3 Inhibitors

Dai-Shi Su; Junya Qu; Mark Schulz; Chuck W Blackledge; Hongyi Yu; Jenny Zeng; Joelle Burgess; Alexander Reif; Melissa Stern; Raman Nagarajan; Melissa Baker Pappalardi; Kristen Wong; Alan P Graves; William Bonnette; Liping Wang; Patricia Elkins; Beth Knapp-Reed; Jeffrey D Carson; Charles McHugh; Helai Mohammad; Ryan Kruger; Juan Luengo; Dirk A Heerding; Caretha L Creasy

doi:10.1021/acsmedchemlett.9b00493

Discovery of Isoxazole Amides as Potent and Selective SMYD3 Inhibitors

ACS Med Chem Lett. 2019 Dec 27;11(2):133-140. doi: 10.1021/acsmedchemlett.9b00493. eCollection 2020 Feb 13.

Authors

Dai-Shi Su¹, Junya Qu¹, Mark Schulz¹, Chuck W Blackledge¹, Hongyi Yu¹, Jenny Zeng¹, Joelle Burgess¹, Alexander Reif¹, Melissa Stern¹, Raman Nagarajan¹, Melissa Baker Pappalardi¹, Kristen Wong¹, Alan P Graves¹, William Bonnette¹, Liping Wang¹, Patricia Elkins¹, Beth Knapp-Reed¹, Jeffrey D Carson¹, Charles McHugh¹, Helai Mohammad¹, Ryan Kruger¹, Juan Luengo¹, Dirk A Heerding¹, Caretha L Creasy¹

Affiliation

¹ Medicinal Chemistry, Medicine Design, Oncology R&D, Data and Computational Sciences, and Protein Cellular and Structural Sciences, Medicine Design, Medicinal Science and Technology, GlaxoSmithKline, 1250 South Collegeville Road, Collegeville, Pennsylvania 19426, United States.

Abstract

We report herein the discovery of isoxazole amides as potent and selective SET and MYND Domain-Containing Protein 3 (SMYD3) inhibitors. Elucidation of the structure-activity relationship of the high-throughput screening (HTS) lead compound 1 provided potent and selective SMYD3 inhibitors. The SAR optimization, cocrystal structures of small molecules with SMYD3, and mode of inhibition (MOI) characterization of compounds are described. The synthesis and biological and pharmacokinetic profiles of compounds are also presented.