文摘
We report herein a stereoselective and straightforward methodology for the synthesis of new androgen receptor ligands with (anti)-agonistic activities. Oxygen鈥搉itrogen replacement in bicalutamide-like structures paves the way to the disclosure of a new class of analogues, including cyclized/nitrogen-substituted derivatives, with promising antiandrogen (or anabolic) activity.
Keywords:
androgen receptor; enantiopure antiandrogens; hormone-refractory prostate cancer; sulfinylimino propanamides