Clinical Cancer Research Joint Metastasis Research Society-AACR Conference on Metastasis Translational Cancer Medicine 2008: Cancer Clinical Trials and Personalized Medicine
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Clinical Cancer Research Vol. 11, 4653-4657, July 1, 2005
© 2005 American Association for Cancer Research

Human Cancer Biology

Testosterone and Dihydrotestosterone Tissue Levels in Recurrent Prostate Cancer

Mark A. Titus4, Michael J. Schell3,4, Fred B. Lih5, Kenneth B. Tomer5 and James L. Mohler1,2,4,6,7

Authors' Affiliations: Departments of 1 Pathology and Laboratory Medicine, 2 Surgery, and 3 Biostatistics, 4 UNC Lineberger Comprehensive Cancer Center, University of North Carolina School of Medicine, Chapel Hill, 5 Laboratory of Structural Biology, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina, 6 Department of Urologic Oncology, Roswell Park Cancer Institute, and 7 Department of Urology, University at Buffalo School of Medicine and Biotechnology, Buffalo, New York

Requests for reprints: Mark A. Titus, UNC Lineberger Comprehensive Cancer Center, University of North Carolina School of Medicine, Chapel Hill, NC 27599-7295. Phone: 919-966-9257; Fax: 919-966-3015; E-mail: matitus{at}med.unc.edu.

Purpose: Prostate cancer eventually recurs during androgen deprivation therapy despite castrate levels of serum androgens. Expression of androgen receptor and androgen receptor–regulated proteins suggests androgen receptor activation in recurrent prostate cancer. Many groups have pursued mechanisms of ligand-independent androgen receptor activation but we found high levels of testicular androgens in recurrent prostate cancer tissue using RIA.

Experimental Designs: Prostate specimens from 36 men were procured preserving blood flow to prevent ischemia and cyropreserved immediately. Recurrent prostate cancer specimens from 18 men whose cancer recurred locally during androgen deprivation therapy and androgen-stimulated benign prostate specimens from 18 men receiving no hormonal treatments were studied. Tissue levels of testosterone and dihydrotestosterone were measured in each specimen using liquid chromatography/electrospray tandem mass spectrometry. Testosterone and dihydrotestosterone levels were compared with clinical variables and treatment received.

Results: Testosterone levels were similar in recurrent prostate cancer (3.75 pmol/g tissue) and androgen-stimulated benign prostate (2.75 pmol/g tissue, Wilcoxon two-sided, P = 0.30). Dihydrotestosterone levels decreased 91% in recurrent prostate cancer (1.25 pmol/g tissue) compared with androgen-stimulated benign prostate (13.7 pmol/g tissue; Wilcoxon two-sided, P < 0.0001) although dihydrotestosterone levels in most specimens of recurrent prostate cancer were sufficient for androgen receptor activation. Testosterone or dihydrotestosterone levels were not related to metastatic status, antiandrogen treatment, or survival (Wilcoxon rank sum, all P > 0.2).

Conclusions: Recurrent prostate cancer may develop the capacity to biosynthesize testicular androgens from adrenal androgens or cholesterol. This surprising finding suggests intracrine production of dihydrotestosterone and should be exploited for novel treatment of recurrent prostate cancer.




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Copyright © 2005 by the American Association for Cancer Research.