Apalutamide slows development of prostate cancer metastases
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Apalutamide conferred a 72% reduced risk for metastasis or death compared with placebo among men with nonmetastatic castration-resistant prostate cancer at high risk for developing metastatic disease, according to the randomized phase 3 SPARTAN study scheduled for presentation at the Genitourinary Cancers Symposium.
“To date there has been no therapy approved for this disease state, and the aim of this study was to see if the development of metastases in the transition from nonmetastatic to metastatic could be slowed,” Eric J. Small, MD, FASCO, professor of medicine at University of California, San Francisco, said during a press cast. “Frequently, these patients receive unproven, older generation, second-line hormone therapy, and none of those agents have demonstrated an impact on outcome. It is a big unmet need.”
As HemOnc Today previously reported, apalutamide (ARN-509; Janssen, Aragon Pharmaceuticals) — which inhibits the action of testosterone in prostate cancer cells and prevents androgen from binding to the androgen receptor — received priority review by the FDA in January for the treatment of nonmetastatic castration-resistant prostate cancer.
Some physicians advocate active surveillance for these patients; however, men whose PSA score rapidly rises — based on a PSA doubling time of less than 8 to 10 months — while on androgen deprivation therapy are at increased risk for developing metastases or death. This group represented the 1,207 men enrolled in the SPARTAN study conducted at 332 institutions worldwide.
Researchers randomly assigned men with nonmetastatic castration-resistant prostate cancer who had stopped responding to ADT and were at high risk for metastasis based on PSA doubling time to 240 mg daily apalutamide or placebo added to ongoing ADT.
At the time of development of metastases, patients received standard second therapies at their physician’s discretion and had an option to receive on-study abiraterone acetate (Zytiga, Janssen) and prednisone.
Metastasis-free survival — defined as the time from randomization to first radiographic distant metastasis or death — served as the primary endpoint. Time to metastasis, PFS, time to symptomatic progression and OS served as secondary endpoints.
The median PSA doubling time at study entry was approximately 4.5 months in both the apalutamide and placebo groups.
Apalutamide decreased the risk for metastasis and death by 72% compared with placebo (HR = 0.28; 95% CI, 0.23-0.35) and significantly prolonged the median metastasis-free survival by 2 years (40.5 months vs. 16.2 months).
Researchers also noted a trend favoring improved OS for men receiving apalutamide, although the difference was not statistically significant.
Time to metastasis, PFS and time to symptomatic progress also improved. At a median follow-up of 20.3 months, 61% of the apalutamide group and 30% of the placebo group remained on treatment.
Following the analysis of metastasis-free survival, study treatment was unblinded in July 2017 following the recommendations of an independent data monitoring committee, and all patients were offered open-label apalutamide.
Of those whose disease progressed, 80% of placebo patients and 52% of apalutamide patients received therapy for metastatic disease.
Apalutamide was well tolerated, with 10.7% of men discontinuing treatment due to adverse events, compared with 6.3% of men receiving placebo. Men who received apalutamide in addition to ADT maintained their quality-of-life scores.
“We concluded that apalutamide reduced the risk [for] metastases by 72% and prolonged the median metastases-free survival in these men by more than 2 years,” Small said. “The trend is certainly encouraging. Overall, these data suggest that apalutamide should now be considered a new standard of care for men with high-risk, nonmetastatic castration-resistant prostate cancer.”
Researchers noted future studies should analyze molecular and circulating markers from blood samples to identify patients who benefit most from apalutamide. – by Chuck Gormley
Disclosures: Aragon Pharmaceuticals funded the study. Small reports consultant/advisory roles with Fortis, Gilead Sciences and Valeant Pharmaceuticals International; stock ownership in Fortis and Harpoon Therapeutics; honoraria from Janssen-Cilag; and researching funding from Janssen. Please see the abstract for all other authors’ relevant financial disclosures.