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ZO-FAST: Immediate Zoledronic Acid Beats Delayed Tx in Early Breast Cancer

SAN ANTONIO – Immediate treatment with zoledronic acid in postmenopausal women with hormone receptor–positive breast cancer initiating letrozole therapy was associated with a 34% reduction in recurrence risk and 31% improvement in overall survival, compared with women of similar status who received the bisphosphonate later, according to new data from the ZO-FAST trial.

This study assessed the impact of zoledronic acid (Zometa) on aromatase inhibitor-associated bone loss after surgery for early breast cancer.

Additional disease-free and overall survival benefits were observed among the subgroup of patients who had been postmenopausal for at least 5 years, Dr. Richard de Boer reported yesterday at the San Antonio Breast Cancer Symposium.

The findings update those previously reported by Dr. de Boer of the Royal Melbourne Hospital and colleagues in the ZO-FAST (Zometa-Femara Adjuvant Synergy Trial), demonstrating that early zoledronic acid significantly improved bone mineral density and improved breast cancer disease-free survival.

The new, long-term data confirm the overall survival benefits, and the results of an exploratory subgroup analysis based on menopausal status indicates that the addition of zoledronic acid confers the most benefit to women who are truly menopausal at diagnosis, Dr. de Boer reported.

The study involved 1,065 postmenopausal women with hormone receptor–positive early breast cancer with a bone mineral density T-score of –2. In addition to receiving adjuvant endocrine therapy with 2.5 mg of letrozole (Femara) four times daily for 5 years, the women were randomized to receive 4 mg of zoledronic acid every 6 months either immediately or when their post-baseline T score dipped below –2 or they suffered a nontraumatic/asymptomatic fracture. Patients were included in the analysis if they had established menopause at the time of diagnosis or if they became menopausal as a consequence of chemotherapy or ovarian suppression, Dr. de Boer explained.

At 60 months follow-up, the hazard ratios for recurrence and mortality in the immediate treatment group were 0.66 and 0.69 respectively, with only the former representing a statistically significant improvement over the delayed treatment patients, Dr. de Boer reported. Exploratory analyses of the 670 women who were postmenopausal for more than 5 years or older than 60 years at study entry showed that immediate zoledronic acid treatment significantly improved disease-free survival, with a hazard ratio of 0.63, and significantly prolonged overall survival, with a hazard ratio of 0.50, compared with the delayed treatment group.

With respect to lumbar spine bone mineral density, "the benefits observed in the immediate therapy group early on, when bone loss is at it greatest, continued out over 5 years, with a net difference of 10% favoring the immediate zoledronic acid group," Dr. de Boer said, noting that similar results were observed in total hip bone mineral density, "with an overall change of close to 6% in the immediate group at the 5-year time point."

In a subset analysis comparing the immediate treatment group with the 27% of patients who initiated zoledronic acid, "we observed a hazard ratio 0.62 for recurrence in favor of the up-front zoledronic acid group," Dr. de Boer said. "Bone was the most common site of recurrence, and this favored the immediate group, with 14 events compared with 24 in the delayed group."

In a comparison of patients who did and did not initiate therapy, "the hazard ratio for disease-free survival was in favor of those who did initiate treatment, suggesting a delay in bisphosphonate initiation could still have an impact on disease outcomes," Dr. de Boer said.

In terms of safety, there were three confirmed cases of osteonecrosis of the jaw in the trial, all in the immediate group. "This compares favorably with published results of studies in which zoledronic acid was administered on a 6-month schedule," according to Dr. de Boer. "The AZURE [Adjuvant Zoledronic Acid to Reduce Recurrence] study had a more intensive administration schedule, and thus had more cases of jaw osteonecrosis."

The findings of this study, together with those of other recent studies including the AZURE trial, "support the hypothesis that the anticancer benefits of zoledronic acid may best be realized in a low-estrogen environment," Dr. de Boer concluded.

The additional anticancer benefit observed in the truly vs. recently postmenopausal women in this study warrants additional investigation, according to Dr. James Ingle of the Mayo Clinic in Rochester, Minn., the discussant for the session. "The study met its primary analysis endpoint, which was bone mineral density improvement, but it was not powered nor designed to detect a difference in breast events," he said. "Although the findings demonstrate the value of zoledronic acid, they are based on an unplanned analysis and thus insufficient on their own to support zoledronic acid as standard of care in postmenopausal women."

 

 

Dr. de Boer is on the speakers’ bureau for Novartis. Dr. Ingle said he had no financial conflicts to disclose.

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SAN ANTONIO – Immediate treatment with zoledronic acid in postmenopausal women with hormone receptor–positive breast cancer initiating letrozole therapy was associated with a 34% reduction in recurrence risk and 31% improvement in overall survival, compared with women of similar status who received the bisphosphonate later, according to new data from the ZO-FAST trial.

This study assessed the impact of zoledronic acid (Zometa) on aromatase inhibitor-associated bone loss after surgery for early breast cancer.

Additional disease-free and overall survival benefits were observed among the subgroup of patients who had been postmenopausal for at least 5 years, Dr. Richard de Boer reported yesterday at the San Antonio Breast Cancer Symposium.

The findings update those previously reported by Dr. de Boer of the Royal Melbourne Hospital and colleagues in the ZO-FAST (Zometa-Femara Adjuvant Synergy Trial), demonstrating that early zoledronic acid significantly improved bone mineral density and improved breast cancer disease-free survival.

The new, long-term data confirm the overall survival benefits, and the results of an exploratory subgroup analysis based on menopausal status indicates that the addition of zoledronic acid confers the most benefit to women who are truly menopausal at diagnosis, Dr. de Boer reported.

The study involved 1,065 postmenopausal women with hormone receptor–positive early breast cancer with a bone mineral density T-score of –2. In addition to receiving adjuvant endocrine therapy with 2.5 mg of letrozole (Femara) four times daily for 5 years, the women were randomized to receive 4 mg of zoledronic acid every 6 months either immediately or when their post-baseline T score dipped below –2 or they suffered a nontraumatic/asymptomatic fracture. Patients were included in the analysis if they had established menopause at the time of diagnosis or if they became menopausal as a consequence of chemotherapy or ovarian suppression, Dr. de Boer explained.

At 60 months follow-up, the hazard ratios for recurrence and mortality in the immediate treatment group were 0.66 and 0.69 respectively, with only the former representing a statistically significant improvement over the delayed treatment patients, Dr. de Boer reported. Exploratory analyses of the 670 women who were postmenopausal for more than 5 years or older than 60 years at study entry showed that immediate zoledronic acid treatment significantly improved disease-free survival, with a hazard ratio of 0.63, and significantly prolonged overall survival, with a hazard ratio of 0.50, compared with the delayed treatment group.

With respect to lumbar spine bone mineral density, "the benefits observed in the immediate therapy group early on, when bone loss is at it greatest, continued out over 5 years, with a net difference of 10% favoring the immediate zoledronic acid group," Dr. de Boer said, noting that similar results were observed in total hip bone mineral density, "with an overall change of close to 6% in the immediate group at the 5-year time point."

In a subset analysis comparing the immediate treatment group with the 27% of patients who initiated zoledronic acid, "we observed a hazard ratio 0.62 for recurrence in favor of the up-front zoledronic acid group," Dr. de Boer said. "Bone was the most common site of recurrence, and this favored the immediate group, with 14 events compared with 24 in the delayed group."

In a comparison of patients who did and did not initiate therapy, "the hazard ratio for disease-free survival was in favor of those who did initiate treatment, suggesting a delay in bisphosphonate initiation could still have an impact on disease outcomes," Dr. de Boer said.

In terms of safety, there were three confirmed cases of osteonecrosis of the jaw in the trial, all in the immediate group. "This compares favorably with published results of studies in which zoledronic acid was administered on a 6-month schedule," according to Dr. de Boer. "The AZURE [Adjuvant Zoledronic Acid to Reduce Recurrence] study had a more intensive administration schedule, and thus had more cases of jaw osteonecrosis."

The findings of this study, together with those of other recent studies including the AZURE trial, "support the hypothesis that the anticancer benefits of zoledronic acid may best be realized in a low-estrogen environment," Dr. de Boer concluded.

The additional anticancer benefit observed in the truly vs. recently postmenopausal women in this study warrants additional investigation, according to Dr. James Ingle of the Mayo Clinic in Rochester, Minn., the discussant for the session. "The study met its primary analysis endpoint, which was bone mineral density improvement, but it was not powered nor designed to detect a difference in breast events," he said. "Although the findings demonstrate the value of zoledronic acid, they are based on an unplanned analysis and thus insufficient on their own to support zoledronic acid as standard of care in postmenopausal women."

 

 

Dr. de Boer is on the speakers’ bureau for Novartis. Dr. Ingle said he had no financial conflicts to disclose.

SAN ANTONIO – Immediate treatment with zoledronic acid in postmenopausal women with hormone receptor–positive breast cancer initiating letrozole therapy was associated with a 34% reduction in recurrence risk and 31% improvement in overall survival, compared with women of similar status who received the bisphosphonate later, according to new data from the ZO-FAST trial.

This study assessed the impact of zoledronic acid (Zometa) on aromatase inhibitor-associated bone loss after surgery for early breast cancer.

Additional disease-free and overall survival benefits were observed among the subgroup of patients who had been postmenopausal for at least 5 years, Dr. Richard de Boer reported yesterday at the San Antonio Breast Cancer Symposium.

The findings update those previously reported by Dr. de Boer of the Royal Melbourne Hospital and colleagues in the ZO-FAST (Zometa-Femara Adjuvant Synergy Trial), demonstrating that early zoledronic acid significantly improved bone mineral density and improved breast cancer disease-free survival.

The new, long-term data confirm the overall survival benefits, and the results of an exploratory subgroup analysis based on menopausal status indicates that the addition of zoledronic acid confers the most benefit to women who are truly menopausal at diagnosis, Dr. de Boer reported.

The study involved 1,065 postmenopausal women with hormone receptor–positive early breast cancer with a bone mineral density T-score of –2. In addition to receiving adjuvant endocrine therapy with 2.5 mg of letrozole (Femara) four times daily for 5 years, the women were randomized to receive 4 mg of zoledronic acid every 6 months either immediately or when their post-baseline T score dipped below –2 or they suffered a nontraumatic/asymptomatic fracture. Patients were included in the analysis if they had established menopause at the time of diagnosis or if they became menopausal as a consequence of chemotherapy or ovarian suppression, Dr. de Boer explained.

At 60 months follow-up, the hazard ratios for recurrence and mortality in the immediate treatment group were 0.66 and 0.69 respectively, with only the former representing a statistically significant improvement over the delayed treatment patients, Dr. de Boer reported. Exploratory analyses of the 670 women who were postmenopausal for more than 5 years or older than 60 years at study entry showed that immediate zoledronic acid treatment significantly improved disease-free survival, with a hazard ratio of 0.63, and significantly prolonged overall survival, with a hazard ratio of 0.50, compared with the delayed treatment group.

With respect to lumbar spine bone mineral density, "the benefits observed in the immediate therapy group early on, when bone loss is at it greatest, continued out over 5 years, with a net difference of 10% favoring the immediate zoledronic acid group," Dr. de Boer said, noting that similar results were observed in total hip bone mineral density, "with an overall change of close to 6% in the immediate group at the 5-year time point."

In a subset analysis comparing the immediate treatment group with the 27% of patients who initiated zoledronic acid, "we observed a hazard ratio 0.62 for recurrence in favor of the up-front zoledronic acid group," Dr. de Boer said. "Bone was the most common site of recurrence, and this favored the immediate group, with 14 events compared with 24 in the delayed group."

In a comparison of patients who did and did not initiate therapy, "the hazard ratio for disease-free survival was in favor of those who did initiate treatment, suggesting a delay in bisphosphonate initiation could still have an impact on disease outcomes," Dr. de Boer said.

In terms of safety, there were three confirmed cases of osteonecrosis of the jaw in the trial, all in the immediate group. "This compares favorably with published results of studies in which zoledronic acid was administered on a 6-month schedule," according to Dr. de Boer. "The AZURE [Adjuvant Zoledronic Acid to Reduce Recurrence] study had a more intensive administration schedule, and thus had more cases of jaw osteonecrosis."

The findings of this study, together with those of other recent studies including the AZURE trial, "support the hypothesis that the anticancer benefits of zoledronic acid may best be realized in a low-estrogen environment," Dr. de Boer concluded.

The additional anticancer benefit observed in the truly vs. recently postmenopausal women in this study warrants additional investigation, according to Dr. James Ingle of the Mayo Clinic in Rochester, Minn., the discussant for the session. "The study met its primary analysis endpoint, which was bone mineral density improvement, but it was not powered nor designed to detect a difference in breast events," he said. "Although the findings demonstrate the value of zoledronic acid, they are based on an unplanned analysis and thus insufficient on their own to support zoledronic acid as standard of care in postmenopausal women."

 

 

Dr. de Boer is on the speakers’ bureau for Novartis. Dr. Ingle said he had no financial conflicts to disclose.

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ZO-FAST: Immediate Zoledronic Acid Beats Delayed Tx in Early Breast Cancer
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zoledronic acid, postmenopausal women, hormone receptor–positive, breast cancer, letrozole therapy, ZO-FAST trial, Zometa, aromatase inhibitor-associated bone loss, early breast cancer, Dr. Richard de Boer, San Antonio Breast Cancer Symposium, Zometa-Femara Adjuvant Synergy Trial, bone mineral density, disease-free survival,

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zoledronic acid, postmenopausal women, hormone receptor–positive, breast cancer, letrozole therapy, ZO-FAST trial, Zometa, aromatase inhibitor-associated bone loss, early breast cancer, Dr. Richard de Boer, San Antonio Breast Cancer Symposium, Zometa-Femara Adjuvant Synergy Trial, bone mineral density, disease-free survival,

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FROM THE SAN ANTONIO BREAST CANCER SYMPOSIUM

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Major Finding: Immediate treatment with zoledronic acid reduced recurrence and mortality risk by 34% and 31%, respectively, and improved bone density, compared with women assigned to delayed treatment with the bisphosphonate.

Data Source: The multicenter, multinational Z0-FAST (Zometa-Femara Adjuvant Synergy Trial) of 1,065 postmenopausal women with hormone receptor–positive early breast cancer initiating adjuvant endocrine therapy with letrozole with immediate or delayed zoledronic acid therapy at 5 years.

Disclosures: Dr. de Boer is on the speakers’ bureau for Novartis. Dr. Ingle said he had no financial conflicts to disclose.