Login / Signup

Spirocyclic Thiohydantoin Antagonists of F877L and Wild-Type Androgen Receptor for Castration-Resistant Prostate Cancer.

Zhuming ZhangPeter J ConnollyLuis Trabalón EscolarChristian RocaboyVineet PandeLieven MeerpoelHeng-Keang LimJonathan R BranchJanine OndrusIan HicksonTammy L BushJames R BischoffGilles Bignan
Published in: ACS medicinal chemistry letters (2021)
Androgen receptor (AR) transcriptional reactivation plays a key role in the development and progression of lethal castration-resistant prostate cancer (CRPC). Recurrent alterations in the AR enable persistent AR pathway signaling and drive resistance to the treatment of second-generation antiandrogens. AR F877L, a point mutation in the ligand binding domain of the AR, was identified in patients who acquired resistance to enzalutamide or apalutamide. In parallel to our previous structure-activity relationship (SAR) studies of compound 4 (JNJ-pan-AR) and clinical stage compound 5 (JNJ-63576253), we discovered additional AR antagonists that provide opportunities for future development. Here we report a highly potent series of spirocyclic thiohydantoins as AR antagonists for the treatment of the F877L mutant and wild-type CRPC.
Keyphrases
  • wild type
  • prostate cancer
  • gene expression
  • smoking cessation