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Proscar (finasteride) a 5 alpha reductase inhibitor. - online information
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   Saw Palmetto Studies

Comparison of finasteride (Proscar), a 5 alpha reductase inhibitor.

Study

TITLE

Comparison of finasteride (Proscar), a 5 alpha reductase inhibitor, and various commercial plant extracts in in vitro and in vivo 5 alpha reductase inhibition.

AUTHOR

Rhodes L; Primka RL; Berman C; Vergult G; Gabriel M; Pierre-Malice M; Gibelin B

ORGANISATION

Department of Biochemistry, Merck Research Laboratories, Rahway, New Jersey 07065.

SOURCE

Prostate 1993; 22 (1): 43-51

LANGUAGE OF PUBLICATION

English

ABSTRACT

Human prostate was used as a source of 5 alpha reductase. Compounds were incubated with an enzyme preparation and [3H]testosterone. [3H]-dihydrotestosterone production was measured to calculate 5 alpha reductase activity. IC50 values (ng/ml) were finasteride=1; Permixon=5,600; Talso=7,000; Strogen Forte=31,000; Prostagutt=40,000; and Tadenan=63,000. Bazoton and Harzol had no activity at concentrations up to 500,000 ng/ml. In castrate rats stimulated with testosterone (T) or dihydrotestosterone (DHT), finasteride, but not Permixon or Bazoton, inhibited T stimulated prostate growth, while none of the three compounds inhibited DHT stimulated growth. These results demonstrate that finasteride inhibits 5 alpha reductase, while Permixon and Bazoton have neither anti-androgen nor 5 alpha reductase inhibitory activity. In addition, in a 7 day human clinical trial, finasteride, but not Permixon or placebo, decreased serum DHT in men, further confirming the lack of 5 alpha reductase inhibition by Permixon. Finasteride and the plant extracts listed above do not inhibit the binding of DHT to the rat prostatic androgen receptor (concentrations to 100 micrograms/ml). Based on these results, it is unlikely that these plant extracts would shrink the prostate by inhibiting androgen action or 5 alpha reductase. (AUTHOR)

MJTR: Androstenes PD. Azasteroids PD. Plant Extracts PD. Testosterone 5-alpha-Reductase AI.

MNTR: Animal. Comparative Study. Human. In Vitro. Male. Prostate DE. Prostate EN. Rats. Receptors, Androgen DE. Stanolone BL. Testosterone BL. CLINICAL TRIAL. CONTROLLED CLINICAL TRIAL. JOURNAL ARTICLE

RNUM: EC 1.3.99.5 (Testosterone 5-alpha-Reductase); 0 (Androstenes); 0 (Azasteroids); 0 (Permixon); 0 (Plant Extracts); 0 (Receptors, Androgen); 521-18-6 (Stanolone); 57-85-2 (Testosterone); 98319-26-7 (Finasteride)

GEOT: UNITED STATES

IDEN: ISSN: 0270-4137. JOURNAL-CODE: PB4. ENTRY-DATE: 930226. JOURNAL-SUBSET: M X. IM-DATE: 9305.

ACCE: 93149919




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