Discovery of OICR12694: A Novel, Potent, Selective, and Orally Bioavailable BCL6 BTB Inhibitor.
Ahmed MamaiAnh M ChauBrian J WilsonIain D WatsonBabu B JosephPandiaraju R SubramanianMonzur M MorshedJustin A MorinMichael A PrakeschTianbao LuPete ConnollyDouglas A KuntzNeil C PomroyGennady PodaKong NguyenRichard MarcellusGraig StrathdeeBrigitte TheriaultRatheesh SubramaniamMohammed MohammedAyome AbibiManuel ChanJeffrey WinstonTaira KiyotaElijus UndzysAhmed M AmanNigel AustinMarc Du JardinKathryn PackmanUlrike PhillipparRiccardo AttarJames EdwardsJeff O'MearaDavid E UehlingRima Al-AwarGilbert G PrivéMethvin B IsaacPublished in: ACS medicinal chemistry letters (2023)
B cell lymphoma 6 (BCL6), a highly regulated transcriptional repressor, is deregulated in several forms of non-Hodgkin lymphoma (NHL), most notably in diffuse large B-cell lymphoma (DLBCL). The activities of BCL6 are dependent on protein-protein interactions with transcriptional co-repressors. To find new therapeutic interventions addressing the needs of patients with DLBCL, we initiated a program to identify BCL6 inhibitors that interfere with co-repressor binding. A virtual screen hit with binding activity in the high micromolar range was optimized by structure-guided methods, resulting in a novel and highly potent inhibitor series. Further optimization resulted in the lead candidate 58 (OICR12694/JNJ-65234637), a BCL6 inhibitor with low nanomolar DLBCL cell growth inhibition and an excellent oral pharmacokinetic profile. Based on its overall favorable preclinical profile, OICR12694 is a highly potent, orally bioavailable candidate for testing BCL6 inhibition in DLBCL and other neoplasms, particularly in combination with other therapies.