Effects of androgen deprivation on chronic bacterial prostatitis in a rat model

Effects of androgen deprivation on chronic bacterial prostatitis in a rat model

Background: Many attempts have been made to improve the treatment success rate of chronic bacterial prostatitis (CBP). However, no treatment modality has achieved complete cure. The growth and development of the prostate is under direct hormonal control, and it is possible that prostatitis may be di...

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Published in:International journal of urology Vol. 10; no. 9; pp. 485 - 491
Main Authors: SEO, SEONG IL, LEE, SEUNG-JU, KIM, JOON CHUL, CHOI, YEONG-JIN, HWANG, TAE KON, CHO, YONG-HYUN
Format: Journal Article
Language:English
Published: Melbourne, Australia Blackwell Science Pty 01-09-2003
Subjects:
Androgen Antagonists - therapeutic use
Animals
Anti-Infective Agents, Urinary - therapeutic use
Castration
chronic bacterial prostatitis
Chronic Disease
Enzyme Inhibitors - pharmacology
Escherichia coli Infections - complications
Escherichia coli Infections - drug therapy
Escherichia coli Infections - urine
Estradiol - pharmacology
estrogen
Estrogens - blood
finasteride
Finasteride - pharmacology
Levofloxacin
Male
Models, Animal
Ofloxacin - pharmacology
Prostatitis - drug therapy
Prostatitis - microbiology
Random Allocation
rat
Rats
Rats, Wistar
Testosterone - blood
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Summary:Background: Many attempts have been made to improve the treatment success rate of chronic bacterial prostatitis (CBP). However, no treatment modality has achieved complete cure. The growth and development of the prostate is under direct hormonal control, and it is possible that prostatitis may be directly influenced by its hormonal milieu in a similar fashion to benign prostatic hyperplasia and prostate cancer. Therefore, the effects of androgen deprivation on the treatment of CBP were investigated in rats. Methods: Experimental CBP was induced in one hundred, male Wistar rats by instillation of bacterial suspension (Escherichia coli Z17, O2: K1: H‐) containing 1 × 108 CFU/µL into the prostatic urethra. Microbiologically and histologically proven CBP was demonstrated in 62% (62 of 100) of the rats after 4 weeks of bacterial instillation. The 62 rats demonstrating CBP were randomly divided into five groups: control; castration; finasteride; estrogen; and levofloxacin groups. All drug treatments were conducted over a period of 4 weeks. Results: Microbiological cultures and histological findings of the prostate and urine samples demonstrated reduced bacterial growth and improved inflammatory responses in all four experimental groups compared with the control group. The castration and estrogen groups showed coherent trends of decrease in bacterial growth and improvements in prostatic inflammation compared with the control group, but not to a statistically significant degree (P > 0.05). However, the finasteride and levofloxacin groups did show statistically significant decreases in bacterial growth and improvements in prostatic inflammation compared with the control group (P < 0.05). Conclusion: These results suggest that androgen deprivation is an effective modality in CBP treatment. In particular, the finasteride treatment reduced the severity of CBP in the animal model without reducing the systemic testosterone level. The combination of finasteride and levofloxacin maybe one of the effective treatment modalities for CBP.
Bibliography:istex:0CEF8D91E91668244D2EFBE324AB6CCC75823480
ark:/67375/WNG-877JSW1J-8
ArticleID:IJU666
ObjectType-Article-1
SourceType-Scholarly Journals-1
ObjectType-Feature-2
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ISSN:0919-8172
1442-2042
DOI:10.1046/j.1442-2042.2003.00666.x