Novel Oxindole Sulfonamides and Sulfamides: EPZ031686, the First Orally Bioavailable Small Molecule SMYD3 Inhibitor

Lorna H Mitchell; P Ann Boriack-Sjodin; Sherri Smith; Michael Thomenius; Nathalie Rioux; Michael Munchhof; James E Mills; Christine Klaus; Jennifer Totman; Thomas V Riera; Alejandra Raimondi; Suzanne L Jacques; Kip West; Megan Foley; Nigel J Waters; Kevin W Kuntz; Tim J Wigle; Margaret Porter Scott; Robert A Copeland; Jesse J Smith; Richard Chesworth

doi:10.1021/acsmedchemlett.5b00272

Novel Oxindole Sulfonamides and Sulfamides: EPZ031686, the First Orally Bioavailable Small Molecule SMYD3 Inhibitor

ACS Med Chem Lett. 2015 Aug 27;7(2):134-8. doi: 10.1021/acsmedchemlett.5b00272. eCollection 2016 Feb 11.

Authors

Lorna H Mitchell¹, P Ann Boriack-Sjodin¹, Sherri Smith¹, Michael Thomenius¹, Nathalie Rioux¹, Michael Munchhof¹, James E Mills¹, Christine Klaus¹, Jennifer Totman¹, Thomas V Riera¹, Alejandra Raimondi¹, Suzanne L Jacques¹, Kip West¹, Megan Foley¹, Nigel J Waters¹, Kevin W Kuntz¹, Tim J Wigle¹, Margaret Porter Scott¹, Robert A Copeland¹, Jesse J Smith¹, Richard Chesworth¹

Affiliation

¹ Epizyme Inc. , Fourth Floor, 400 Technology Square, Cambridge, Massachusetts 02139, United States.

Abstract

SMYD3 has been implicated in a range of cancers; however, until now no potent selective small molecule inhibitors have been available for target validation studies. A novel oxindole series of SMYD3 inhibitors was identified through screening of the Epizyme proprietary histone methyltransferase-biased library. Potency optimization afforded two tool compounds, sulfonamide EPZ031686 and sulfamide EPZ030456, with cellular potency at a level sufficient to probe the in vitro biology of SMYD3 inhibition. EPZ031686 shows good bioavailability following oral dosing in mice making it a suitable tool for potential in vivo target validation studies.

Keywords: KMT; SMYD3; methyltransferase; oncology; oxindole; tool compound.