Testosterone replacement for hypogonadism after treatment of early prostate cancer with brachytherapy

Abstract

BACKGROUND.

Controversy and a notable paucity of published clinical data best characterize the current knowledge of testosterone‐replacement therapy (TRT) for hypogonadism after treatment for early, localized prostate cancer. The objective of this study was to assess the risk of biochemical failure with TRT after treatment of early prostate cancer with permanent transperineal brachytherapy with or without external beam therapy in patients with low serum levels of testosterone and clinical symptoms of hypogonadism.

METHODS.

Patients who underwent prostate brachytherapy from 1996 to 2004 and received subsequent TRT for symptomatic hypogonadism were reviewed to detail cancer characteristics and treatment as well as pre‐ and post‐TRT serum testosterone and prostate‐specific antigen (PSA) values.

RESULTS.

Thirty‐one men received TRT after prostate brachytherapy for 0.5 to 8.5 years (median, 4.5 years), with a follow‐up that ranged from 1.5 years to 9.0 years (median, 5.0 years) postbrachytherapy. TRT was started from 0.5 years to 4.5 years (median, 2.0 years) after brachytherapy. Serum total testosterone levels ranged from 30 ng/dL to 255 ng/dL (median, 188 ng/dL) before TRT and rose to 365 ng/dL to 1373 ng/dL (median, 498 ng/dL) on TRT. Transient rises in PSA were observed in 1 patient. The most recent PSA level was <0.1 ng/mL in 23 patients (74.2%), <0.5 ng/mL in 30 patients (96.7%), and <1 ng/mL in 31 patients (100%). No patients stopped TRT because of cancer recurrence or documented cancer progression.

CONCLUSIONS.

For patients with low serum testosterone levels and symptoms of hypogonadism, TRT may be used with caution and close follow‐up after prostate brachytherapy. Cancer 2007;109:536–541. © 2006 American Cancer Society.