TITLE
Enzyme activities in tissue of human benign prostatic hyperplasia after
three months' treatment with the Sabal serrulata extract IDS 89 (Strogen) or
placebo.
AUTHOR
Weisser H; Behnke B; Helpap B; Bach D; Krieg M
ORGANISATION
Institute of Clinical Chemistry, Transfusion and Laboratory Medicine,
University Clinic Bergmannsheil, Bochum, Germany.
SOURCE
Eur Urol 1997; 31 (1): 97-101
LANGUAGE OF ORIGIN
English
ABSTRACT
OBJECTIVE: The mechanism of action of plant extracts used for the medical
treatment of human benign prostatic hyperplasia (BPH) is still unknown. In this
prospective, randomized, double-blind trial, we investigated the possible
influence of the Sabal serrulata extract IDS 89 (Strogen) on epithelial and
stromal enzyme activities of BPH tissue.
METHODS: 18 patients with BPH were randomly assigned to receive 3 x 2 capsules
Strogen uno (320 mg/capsule) (n=8) or placebo (n=10) daily for 3 months. The
activity (Vmax and Km) of 5 alpha-reductase. 3 alpha-HSORred, 3 beta-HSORred,
and creatine kinase was determined in mechanically separated epithelium and
stroma of human BPH. RESULTS: The multivariate correlation analysis revealed a
positive correlation between therapy and the following enzyme alterations: (1)
In epithelium, the substrate affinity of the 5 alpha-reductase decreased
slightly (increase of Km value). (2) In stroma, the Vmax value of the 3
alpha-HSORred increased statistically distinctly, leading to a moderate
increase of Vmax/Km. (3) In stroma, the Vmax value of the 3 beta-HSORred
increased moderately, but not statistically significant. (4) In stroma, the
Vmax value of creatine kinase increased significantly, leading to a
statistically distinct increase of Vmax/Km. CONCLUSION: This double-blind,
placebo-controlled clinical trial with the S. serrulata extract IDS 89 revealed
significant biochemical changes at the cellular level of BPH tissue. However,
the alterations are merely moderate, their biochemical causes and consequences
regarding the pathophysiology of BPH rather uncertain. Therefore, more studies
are needed before plant extracts like IDS 89 become valid candidates likewise
synthetic substances already used for medical treatment of human BPH.
(AUTHOR)
MJTR: Enzyme Inhibitors TU. Fatty Acids TU.
Phytosterols TU. Plant Extracts TU. Prostatic Hyperplasia DT. Prostatic
Hyperplasia EN.
MNTR: Aged. Creatine Kinase AI. Creatine
Kinase ME. Double-Blind Method. Human. Male. Middle Age. Prospective Studies.
Prostate EN. Testosterone 5-alpha-Reductase AI. Testosterone 5-alpha-Reductase
ME. Time Factors. 3-Hydroxysteroid Dehydrogenases AI. 3-Hydroxysteroid
Dehydrogenases ME. CLINICAL TRIAL. JOURNAL ARTICLE. RANDOMIZED CONTROLLED
TRIAL
RNUM: EC 1.1.- (3-Hydroxysteroid
Dehydrogenases); EC 1.3.99.5 (Testosterone 5-alpha-Reductase); EC 2.7.3.2
(Creatine Kinase); 0 (Enzyme Inhibitors); 0 (Fatty Acids); 0 (IDS 89 Sabal
serrulata extract); 0 (Phytosterols); 0 (Plant Extracts) PAGE 6 National
Library of Medicine MEDLINE Database
GEOT: SWITZERLAND
IDEN: ISSN: 0302-2838. JOURNAL-CODE: ENM.
ENTRY-DATE: 970603. JOURNAL-SUBSET: M. IM-DATE: 9708.
ACCE: 97184773