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DOI: 10.1055/s-0029-1210534
© J. A. Barth Verlag in Georg Thieme Verlag KG Stuttgart · New York
Assignment of Anabolic-Androgenic and Antiandrogenic Properties to Some Chlorine-Substituted Steroids on the Basis of Their Binding Characteristics to the Androgen Receptor of the Rat Seminal Vesicle1)
1) Presented at the 3rd Symposium on Biochemical Aspects of Steroid Research, October 1—6, 1984, Weimar/GDRPublication History
1984
Publication Date:
16 July 2009 (online)
Summary
In this study we investigated the affinity of several 4-chlorinated and 1-ene derivatives of 17α-methyltestosterone (MT) and 17α-methyl-5α-dihydrotestosterone (MDHT) to the androgen receptor, and, additionally, the effect of a few MT-derived steroids on the activity of the 5α-reductase enzyme present in the rat seminal vesicle. From our results we conclude, that 1. Δ1 or/and Δ4 double bonds in ring A counteract the inhibition of receptor-binding caused by chlorine-substitution at C4; 2. the dissociation of myotropic and androgenic effects [=M/A dissociation] of 4-chloro-MT (as compared to MT) is due to its inactivation by 5α-reductase in androgen target organs and/or to the inhibition of the conversion of endogenous testosterone to DHT; 3. the M/A dissociation of 1-ene-MT and 4-chloro-l-ene-MT may be explained by their inability to be activated by 5α-reductase; 4. for the same reason, M/A dissociation can be assigned to the effects of 4α-chloro-l-ene-DHT.
We determined the short-term and long-term competition of cyproterone acetate and chlormadinone acetate with [3H]DHT for receptor binding at 0°C and showed, that the complexes formed by these antiandrogens with the androgen receptor have equally reduced stabilities compared to the DHT-receptor complex.
Key words
Chloro-steroids - Androgen receptor affinity - 5α-reductase - Seminal vesicle