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• W295776039 abstract "In male rats a sex-dependent protein fraction in the liver is found to disappear on treatment with cyproterone or reserpine. This protein fraction is dependent on the endogenous testosterone production. Besides this effect the interaction of testosterone and cyproterone was investigated in the prostate gland of the rat. The activity of prostatic nuclear aggregates to synthesize RNA was retarded in castrated rats. This could be brought to normal by exogenous testosterone. Simultaneous treatment with cyproterone inhibited the testosterone action completely. To look for more simple biological systems we investigated the anti-androgenic action of cyproterone, reserpine and other compounds in microbial systems. Using testosterone as inducer for the synthesis of 20ß-hydroxy steroid dehydrogenase (HSDase) in Streptomyces hydrogenans, HSDase- induction was found to be very sensitive to the addition of cyproterone, reserpine, ergocornine and diethylstilbestrol. In the presence of cyproterone induction of HSDase-synthesis is significantly inhibited, which may be due to a competition at the specific receptor. However, no antagonism between progesterone and cyproterone is observed in animals and in Streptomyces. The primary response of an inducer is accompanied by its initial binding to the receptor, which is found in Streptomyces hydrogenans as an acidic protein. Its molecular weight is estimated to be 150 000 or more and it does not contain any strongly bound nucleic acids or nucleotides. After proteolytic digestion this protein fraction loses bound steroids. After in vivo incubation bound steroids are partly altered. There is no final conclusion about the number or heterogeneity of the binding protein(s) for inducing steroids. The steroid binding protein shows binding capacity for steroids in cell free system by equilibrium dialysis too." @default.
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• W295776039 date "1969-01-01" @default.
• W295776039 modified "2023-09-23" @default.
• W295776039 title "Steroid Antagonists: Their Mechanism of Action" @default.
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• W295776039 doi "https://doi.org/10.1016/b978-0-08-006942-5.50019-9" @default.
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