January 07, 2015
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Active surveillance safe for favorable-risk prostate cancer

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Active surveillance appeared safe and feasible for patients with favorable-risk prostate cancer, according to long-term follow-up of a prospective single-arm cohort study.

Perspective from

Active surveillance has gained acceptance for patients with favorable-risk prostate cancer because it may reduce the risk for overtreatment of clinically insignificant disease, while still allowing for definitive therapy for patients whose risk appears to increase over time. However, long-term follow-up on this approach is lacking, according to background information provided by researchers.

In the current study, Laurence Klotz, MD, FRCS(C), chief of the division of urology at Sunnybrook Health Sciences Centre and professor in the department of surgery at the University of Toronto, and colleagues reported long-term outcomes of a large cohort of men who underwent active surveillance.

The study included 993 men (median age, 67.8 years; range, 41-89) with favorable- or intermediate-risk prostate cancer treated at a single academic health sciences center.

Researchers measured patients’ PSA levels in stable patients every 3 months for 2 years, and every 6 months thereafter. Intervention was offered for those whose PSA levels doubled in less than 3 years, those who demonstrated Gleason score progression and those who demonstrated unequivocal Gleason score progression.

About one-quarter of patients (28.6%; n=267) required intervention. The most common reasons for intervention were short PSA doubling time, grade progression and patient preference.

At the time of analysis, 149 (15%) patients had died, including 15 (1.5%) who died from prostate cancer. All 15 patients who died from prostate cancer had developed metastatic disease.

Another 25 patients were lost to follow-up. Of the 819 patients who were still alive at the time of analysis, median follow-up from first biopsy was 6.4 years (range, 0.2-19.8).

Researchers reported cause-specific survival rates of 98.1% at 10 years and 94.3% at 15 years.

Thirteen patients (1.3%) developed metastatic disease; of these patients, nine remained alive with confirmed metastases at the time of analysis and four had died of other causes.

The percentage of patients who remained untreated and on surveillance was 75.7% at 5 years, 63.5% at 10 years, and 55% at 15 years.

Researchers calculated a cumulative HR for nonprostate-to-prostate cancer mortality of 9.2 to 1.

“Active surveillance for favorable-risk and select early intermediate-risk prostate cancer is feasible and seems to be safe over 15 years,” Klotz and colleagues concluded. “This strategy provides the benefit of a personalized approach based on the demonstrated risk of clinical or biochemical progression with time … Although prostate cancer mortality increased with longer followup, only 2.8% of patients have developed metastatic disease and 1.5% have died of prostate cancer. These findings are consistent with expected mortality in favorable-risk patients managed with initial definitive intervention.”

Although the results showed how many men in a surveillance cohort died of prostate cancer, they do not show how many ultimately died because they opted for surveillance and “thereby missed the window of opportunity for cure,” Matthew R. Cooperberg, MD, MPH, associate professor of urology, epidemiology and biostatistics at University of California, San Francisco, wrote in an accompanying editorial.

“Whatever this number truly is, it is greater than zero,” Cooperberg wrote. “These deaths by definition are preventable, and as sins of omission are particularly galling to cancer-focused clinicians. But in the alternative paradigm of immediate intervention for all low-risk tumors, they are vastly outnumbered by men harmed substantially by entirely avoidable treatments.”

The effort to reduce overtreatment must be balanced with attempts to identify patients with potentially lethal tumors while at a curable stage, Cooperberg wrote.

“The future of active surveillance — and of prostate cancer treatment in general — must be found at the frontiers of precision medicine,” Cooperberg said. “Both the timing and intensity of intervention should be customized based on maximal information reflecting clinical tumor characteristics; patient health and comorbidity; and, where appropriate, novel imaging and genomic assessment. Prostate cancer has evolved to a diagnosis now recognized to reflect an extraordinary range of biology and prognostic risk, and its management must reflect this diversity.”

Disclosure: See the full study for a list of the researchers’ relevant financial disclosures.