Prostate Cancer Clinical Trial
Official title:
A Pilot Study of Parenteral Testosterone and Oral Etoposide as Therapy for Men With Castration Resistant Prostate Cancer
The objective of the study is to determine if men with evidence of progressive prostate
cancer while on chronic androgen ablation of ≥ 1 year duration will exhibit a clinical
response following administration of parenteral testosterone and oral etoposide.
Treatment Plan: Eligible patients will continue on androgen ablative therapy with
luteinizing hormone-releasing hormone (LHRH) agonist (i.e. Zoladex or Lupron) if not
surgically castrated. Patients will receive intramuscular injection with testosterone
cypionate at a dose of 400 mg every month for a total of 3 injections (i.e. 3 months of
therapy). This dose was selected based on data demonstrating that it produces an initial
supraphysiologic serum level of testosterone (i.e. > 3-5 times normal level) with eugonadal
levels achieved at the end of two weeks. Beginning the day of the testosterone injection,
patients will also receive oral etoposide 100 mg/day in divided doses (50 mg q 12h) x 14
days out of 28 days per cycle. After 3 months on therapy, patients will have repeat prostate
specific antigen (PSA) and bone/computed tomography (CT) scans to establish the effect of
combined testosterone and etoposide treatment on these parameters (i.e. "testosterone effect
baseline"). Patients with sustained elevations in PSA ≥ 50% above pre-testosterone treatment
PSA levels after the initial three months of testosterone and etoposide therapy will not
receive continued therapy and will come off study. Patients with PSA levels less than the
peak serum PSA level seen over the three month period (PSA decline) or patients with PSA ≤
50% of pretreatment baseline will receive a second 3 month course of monthly testosterone
and etoposide therapy until evidence of disease progression. Disease progression is defined
as a PSA increase above the PSA level obtained after 3 months on testosterone treatment over
two successive measurements 2 weeks apart or evidence of new lesions or progression on
bone/CT scans compared to baseline studies. Patients who respond to initial treatment with
testosterone and etoposide and then show signs of progression will have the option of
retreatment with testosterone alone after a period of 3 months or greater off of the
original therapy.
Based on our preclinical data, high levels of androgens can lead to significant growth suppressive effects in prostate cancer cells in vitro and in vivo. Mechanistic data in in vitro models suggests that this growth suppression may be due to the accumulation of androgen induced TOP2B mediated double strand breaks at AR target sites occurring after stimulation of prostate cancer cells with high levels of androgens. Provocatively, the number of double strand breaks was significantly increased (Figure 3 B) if the cells were treated with etoposide, an agent that leads to formation of double strand breaks at TOP2 target sites, concurrently with high-dose androgen stimulation. We hypothesize that co-administration of testosterone with etoposide could produce high levels of double strand breaks in prostate cancer cells, overwhelming DNA repair and survival mechanisms and leading to cancer cell death or growth arrest. To test whether this possibility holds promise for therapy of advanced prostate cancer, we propose the following clinical trial of parenteral testosterone therapy in combination with oral etoposide in men with evidence of progressive prostate cancer during chronic androgen ablation. ;
Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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