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Results of the TEST-PD Study

Michael S. Okun, MD; Hubert H. Fernandez, MD; Ramon L. Rodriguez, MD; Janet Romrell, PA-C; Michele Suelter, BS; Sarah Munson, BS; Elan D. Louis, MD; Thomas Mulligan, MD; Paul S. Foster, PhD; Brian V. Shenal, PhD; Sheyan J. Armaghani, BS; Charles Jacobson, BS; Samuel Wu, PhD; Gregory Crucian, PhD

Arch Neurol. 2006;63:729-735.

Background  Testosterone deficiency has been reported in patients with Parkinson disease (PD), Alzheimer disease, and Huntington disease. It is not known whether testosterone therapy (TT) in men with borderline hypogonadism and neurodegenerative diseases will be of substantial benefit. Previously, we reported that testosterone deficiency is more common in patients with PD compared with age-matched control subjects, and we also reported in 2 small open-label studies that some nonmotor symptoms responded favorably to TT.

Objective  To define the effects of TT on nonmotor and motor symptoms in men with PD and probable testosterone deficiency.

Design  Double-masked, placebo-controlled, parallel-group, single-center trial.

Patients  Two experimental groups: patients with PD who were receiving either TT or placebo.

Interventions  Participants received either the study drug by intramuscular injection (200 mg/mL of testosterone enanthate every 2 weeks for 8 weeks) or placebo (isotonic sodium chloride solution injections). In patients in each group, the testosterone serum concentration was obtained at each study visit. During 2 study visits, testosterone levels were blindly evaluated and the intramuscular testosterone dose was increased by 200 mg/mL if the free testosterone value failed to double from the baseline value.

Main Outcome Measures  The primary outcome variable was the St Louis Testosterone Deficiency Questionnaire, and secondary outcome measures included measures of mood, cognition, fatigue, motor function, and frequency of adverse events. At the end of the double-blind phase, all patients were offered open-label TT and were followed up after 3 and 6 months.

Results  Fifteen patients in the placebo group (mean age, 69.9 years), receiving a mean total levodopa equivalent dose of 924 mg/d, had a baseline free testosterone level of 47.91 pg/mL, compared with 15 patients in the TT group (mean age, 66.7 years), receiving an average total levodopa equivalent dose of 734 mg/d, who had a baseline free testosterone level of 63.49 pg/mL. Testosterone was generally well tolerated. More subjects in the TT group experienced lower extremity edema (40% vs 20%). In 2 patients, 1 in each group, prostate-specific antigen levels were elevated from baseline. The improvement in the TT group compared with the placebo group (1.7 vs 1.1) on the St Louis Testosterone Deficiency Scale was not statistically significant. In addition, there were no significant differences in motor and nonmotor features of PD between the 2 groups, although a few subscales showed improvements (Hopkins Verbal Learning Test, P<.04; and Backward Visual Span subtrial, P<.03). However, long-term open-label TT resulted in delayed but sustained improvement in subjects in the TT group who continued to receive treatment (n = 6) compared with subjects in the placebo group who elected not to receive TT (n = 3).

Conclusions  Testosterone therapy was generally well tolerated in elderly men with PD and probable testosterone deficiency. While there was no significant difference in the motor and nonmotor scales between the TT and placebo groups at the end of 8 weeks compared with baseline, this may be due to several study limitations, including small sample size, a strong placebo effect with intramuscular therapy, and short follow-up that did not allow measurement of delayed effects of TT in some subjects. Until more definitive studies are reported, practitioners should be particularly cautious in treatment of low testosterone concentrations in men with PD and borderline testosterone deficiency, and careful consideration should be given to the risks vs the benefits of TT.

Author Affiliations: Departments of Neurology (Drs Okun, Fernandez, Rodriguez, Foster, Shenal, and Crucian, Messrs Armaghani and Jacobson, and Mss Romrell, Suelter, and Munson), Neurosurgery (Dr Okun), and Psychiatry (Dr Okun), University of Florida Movement Disorders Center, McKnight Brain Institute, Gainesville; Gertude H. Sergievsky Center, College of Physicians and Surgeons, Columbia University Medical Center, New York, NY (Drs Okun and Louis); Departments of Medicine and Geriatrics, Geriatric Research, Education, and Clinical Center, Malcolm Randall Veterans Affairs Hospital and University of Florida (Dr Mulligan); and Division of Biostatistics, College of Medicine, University of Florida (Dr Wu).