| Literature DB >> 2374140 |
R G Christiansen1, M R Bell, T E D'Ambra, J P Mallamo, J L Herrmann, J H Ackerman, C J Opalka, R K Kullnig, R C Winneker, B W Snyder.
Abstract
The steroidal sulfonylpyrazole 1 bound to the rat ventral prostate androgen receptor in vitro; it inhibited testosterone propionate induced increases in ventral prostate weight in vivo in the castrated, immature male rat with an ED50 of 15 mg/kg po. Compound 1 lacked androgenic activity in vivo in contrast to the parent steroidal pyrazole 5, which was both androgenic and antiandrogenic. The 2'- and 5'-methylsulfonyl isomers 6 and 6a did not bind to the androgen receptor. Introduction of an alkylsulfonyl at the N-1'-position has served, therefore, to isolate the intrinsic antiandrogenic properties of the steroidal heterocycle free of apparent hormone agonist properties. Structure-activity relationship studies revealed that a methylsulfonyl group at N-1' together with a C-17 alpha-substituent were the optimal combination for in vitro androgen receptor binding, in vivo antiandrogenic potency, and a lack of androgenic activity.Entities:
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Year: 1990 PMID: 2374140 DOI: 10.1021/jm00170a008
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446