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ASCO 2014: Addition of docetaxel to initial hormone therapy substantially improves survival in metastatic, hormone-sensitive prostate cancer

1 Jun 2014
ASCO 2014: Addition of docetaxel to initial hormone therapy substantially improves survival in metastatic, hormone-sensitive prostate cancer

Findings from a federally funded phase III study, E3805, indicate that adding the chemotherapy drug docetaxel to standard hormone therapy extends survival for men with newly diagnosed hormone-sensitive prostate cancer by roughly 10 months.

The survival benefit is even greater for the subset of men with extensive disease spread (high-extent disease).

“Hormone therapy has been a standard treatment for prostate cancer since the 1950s,” said lead study author Christopher Sweeney, MBBS, medical oncologist at the Lank Center of Genitourinary Oncology at the Dana-Farber Cancer Institute in Boston, MA.

“This is the first study to identify a strategy that prolongs survival in newly diagnosed metastatic prostate cancer. The benefit is substantial and warrants this being a new standard treatment for men who have high-extent disease and are fit for chemotherapy.”

Androgen hormones fuel prostate cancer growth.

Hormonal therapy – also called androgen deprivation therapy (ADT) – alone is the standard first-line treatment for hormone-sensitive prostate cancer.

Although ADT is effective, the disease eventually becomes resistant to the therapy in most patients.

About 30,000 patients die of hormone-resistant prostate cancer in the United States every year.

Chemotherapy is typically initiated only after the disease progresses despite ADT.

In this National Cancer Institute-led study, 790 men with newly diagnosed metastatic prostate cancer were randomly assigned to receive either ADT alone or ADT with docetaxel over a period of 18 weeks.

Approximately two-thirds of patients had high-extent disease, meaning that the cancer had spread to major organs and/or the patient had bone metastases.

When the disease worsened, 45 patients in the ADT plus docetaxel group received additional docetaxel.

In the ADT only group, 123 patients received docetaxel at disease progression.

At a median follow-up of 29 months, there were 136 deaths in the ADT-alone group vs. 101 in the ADT plus docetaxel group.

The median overall survival was 44 months in the ADT group and 57.6 months in the ADT plus docetaxel group.

The relative improvement in median overall survival was even larger among the 520 patients with high-extent disease (32.2 months vs. 49.2 months).

The median overall survival for the subset with low-extent disease takes longer to reach as these patients respond better to ADT, and the median survival has not yet been reached.

Docetaxel also delayed disease progression, assessed by either PSA rise or appearance of new metastases or symptom worsening.

At one year, the proportion of patients with PSA levels less than 0.2ng/mL (a PSA level of less than 0.2 is considered a sign of a better remission) was 11.7 percent in the ADT group vs. 22.7 percent in the ADT plus docetaxel group.

The median time to clinical progression (new symptoms or metastases detected on a scan) was 19.8 months in the ADT group vs. 32.7 months in the ADT plus docetaxel group.

This new treatment paradigm will entail earlier, multidisciplinary care involving the collaboration of both urologists and oncologists, who both commonly treat men with prostate cancer, Dr. Sweeney said.

Follow-up of patients will continue to assess survival benefits for patients with low-extent disease.

Quality-of-life data from this study will be analysed and reported at a later time.

Watch the press conference or interview for more.

Source: ASCO