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New neoadjuvant regimen for locally advanced rectal cancer is efficacious
A new sequential neoadjuvant regimen using short-course radiation offers a similarly effective and more convenient treatment option for locally advanced rectal cancer when compared with standard chemoradiation, finds a randomized phase III trial being reported at the Gastrointestinal Cancers Symposium.
The trial, known as Polish II, was conducted among 515 patients from centers throughout Poland who had stage cT4 or fixed cT3 disease but no distant metastases.
Those in the investigational arm received a short course of radiation therapy lasting just 5 days, followed by three cycles of FOLFOX-4 chemotherapy given over 6 weeks. Those in the control arm received chemoradiation consisting of 5.5 weeks of radiation with fluorouracil, leucovorin, and oxaliplatin. After a rest, all patients underwent surgery at 12 weeks from the start of treatment.
The trial failed to meet its primary endpoint of a significantly higher rate of radical resection with the new regimen vs. chemoradiation, according to data reported in a presscast held before the symposium. However, it did find a lower rate of acute toxicity and, with 35 months of follow-up, an absolute 8% improvement in the 3-year rate of overall survival.
“Despite the fact that the trial was negative ... we show for the first time an alternative to the standard chemoradiation lasting for 5 and a half weeks,” said study coauthor Dr. Lucjan Wyrwicz, head of the Medical Oncology Unit in the Department of Gastrointestinal Cancer at the Maria Sklodowska-Curie Memorial Cancer Center and Institute of Oncology in Warsaw.
The new regimen may be preferable in some clinical scenarios, he noted. For example, the short course of radiation may appeal to patients who want to minimize time off from work, and it may be advantageous when cost or lack of insurance is an issue, and in low-resource countries where there are not enough radiation therapy facilities to go around.
Additionally, the regimen is a more attractive option in patients who have metastases, as they can get some full chemotherapy upfront. In contrast, with chemoradiation, it is typically delayed until several weeks after surgery, essentially leaving metastases uncontrolled in the meantime.
“Having two standards is better than having one standard. We need to try to personalize medicine,” Dr. Wyrwicz summarized.
A caveat to the trial was the use of oxaliplatin, which was included in the protocol before other trials showed that it did not improve outcomes but did add toxicity, he noted. The protocol was amended partway through to allow its omission, but about two-thirds of patients in both arms received the drug. However, findings were much the same whether patients received oxaliplatin or not, he said ahead of the symposium, which was sponsored by ASCO, ASTRO, the American Gastroenterological Association, and the Society of Surgical Oncology.
ASCO expert and presscast moderator Dr. Smitha Krishnamurthi commented, “This is a randomized comparison of short-course radiation with chemotherapy that is demonstrating equal efficacy to traditional chemoradiation. Giving patients a shorter, more convenient, less expensive radiation, and moving the chemotherapy (some of it) upfront appears to be equally active to the chemoradiation. So it does give patients another choice.”
The finding of a lower rate of acute toxicity with the new regimen should be viewed with caution, given the use of oxaliplatin in chemoradiation, which would not be done today, she said.
Uptake of short-course radiation has been greater in Europe than in the United States, according to Dr. Krishnamurthi of Case Western Reserve University, Cleveland. This is possibly because of data from an earlier trial by the Trans Tasman Radiation Oncology Group showing a nonsignificantly higher rate of local recurrence with the short course in patients with less advanced disease.
“There are some other randomized trials which are ongoing, so there’s a lot of interest in this short-course radiation. And I think when we have all of this data together, we will be in a much better position to incorporate it,” she concluded.
In the Polish II trial, the rate of radical (R0) resection did not differ significantly between the new short-course regimen and chemoradiation, although there was a trend favoring the former (77% vs. 71%; P = .081), Dr. Wyrwicz reported.
Patients given the new regimen were less likely to experience acute toxicities (75% vs. 83%; P = .006) but not specifically grade 3 and 4 toxicities. The rate of pathologic complete response did not differ significantly.
The 3-year overall survival rate was higher with the new short-course regimen (73% vs. 65%; P = .046). The groups did not differ significantly with respect to disease-free survival or the incidences of local failure and distant metastases.
A new sequential neoadjuvant regimen using short-course radiation offers a similarly effective and more convenient treatment option for locally advanced rectal cancer when compared with standard chemoradiation, finds a randomized phase III trial being reported at the Gastrointestinal Cancers Symposium.
The trial, known as Polish II, was conducted among 515 patients from centers throughout Poland who had stage cT4 or fixed cT3 disease but no distant metastases.
Those in the investigational arm received a short course of radiation therapy lasting just 5 days, followed by three cycles of FOLFOX-4 chemotherapy given over 6 weeks. Those in the control arm received chemoradiation consisting of 5.5 weeks of radiation with fluorouracil, leucovorin, and oxaliplatin. After a rest, all patients underwent surgery at 12 weeks from the start of treatment.
The trial failed to meet its primary endpoint of a significantly higher rate of radical resection with the new regimen vs. chemoradiation, according to data reported in a presscast held before the symposium. However, it did find a lower rate of acute toxicity and, with 35 months of follow-up, an absolute 8% improvement in the 3-year rate of overall survival.
“Despite the fact that the trial was negative ... we show for the first time an alternative to the standard chemoradiation lasting for 5 and a half weeks,” said study coauthor Dr. Lucjan Wyrwicz, head of the Medical Oncology Unit in the Department of Gastrointestinal Cancer at the Maria Sklodowska-Curie Memorial Cancer Center and Institute of Oncology in Warsaw.
The new regimen may be preferable in some clinical scenarios, he noted. For example, the short course of radiation may appeal to patients who want to minimize time off from work, and it may be advantageous when cost or lack of insurance is an issue, and in low-resource countries where there are not enough radiation therapy facilities to go around.
Additionally, the regimen is a more attractive option in patients who have metastases, as they can get some full chemotherapy upfront. In contrast, with chemoradiation, it is typically delayed until several weeks after surgery, essentially leaving metastases uncontrolled in the meantime.
“Having two standards is better than having one standard. We need to try to personalize medicine,” Dr. Wyrwicz summarized.
A caveat to the trial was the use of oxaliplatin, which was included in the protocol before other trials showed that it did not improve outcomes but did add toxicity, he noted. The protocol was amended partway through to allow its omission, but about two-thirds of patients in both arms received the drug. However, findings were much the same whether patients received oxaliplatin or not, he said ahead of the symposium, which was sponsored by ASCO, ASTRO, the American Gastroenterological Association, and the Society of Surgical Oncology.
ASCO expert and presscast moderator Dr. Smitha Krishnamurthi commented, “This is a randomized comparison of short-course radiation with chemotherapy that is demonstrating equal efficacy to traditional chemoradiation. Giving patients a shorter, more convenient, less expensive radiation, and moving the chemotherapy (some of it) upfront appears to be equally active to the chemoradiation. So it does give patients another choice.”
The finding of a lower rate of acute toxicity with the new regimen should be viewed with caution, given the use of oxaliplatin in chemoradiation, which would not be done today, she said.
Uptake of short-course radiation has been greater in Europe than in the United States, according to Dr. Krishnamurthi of Case Western Reserve University, Cleveland. This is possibly because of data from an earlier trial by the Trans Tasman Radiation Oncology Group showing a nonsignificantly higher rate of local recurrence with the short course in patients with less advanced disease.
“There are some other randomized trials which are ongoing, so there’s a lot of interest in this short-course radiation. And I think when we have all of this data together, we will be in a much better position to incorporate it,” she concluded.
In the Polish II trial, the rate of radical (R0) resection did not differ significantly between the new short-course regimen and chemoradiation, although there was a trend favoring the former (77% vs. 71%; P = .081), Dr. Wyrwicz reported.
Patients given the new regimen were less likely to experience acute toxicities (75% vs. 83%; P = .006) but not specifically grade 3 and 4 toxicities. The rate of pathologic complete response did not differ significantly.
The 3-year overall survival rate was higher with the new short-course regimen (73% vs. 65%; P = .046). The groups did not differ significantly with respect to disease-free survival or the incidences of local failure and distant metastases.
A new sequential neoadjuvant regimen using short-course radiation offers a similarly effective and more convenient treatment option for locally advanced rectal cancer when compared with standard chemoradiation, finds a randomized phase III trial being reported at the Gastrointestinal Cancers Symposium.
The trial, known as Polish II, was conducted among 515 patients from centers throughout Poland who had stage cT4 or fixed cT3 disease but no distant metastases.
Those in the investigational arm received a short course of radiation therapy lasting just 5 days, followed by three cycles of FOLFOX-4 chemotherapy given over 6 weeks. Those in the control arm received chemoradiation consisting of 5.5 weeks of radiation with fluorouracil, leucovorin, and oxaliplatin. After a rest, all patients underwent surgery at 12 weeks from the start of treatment.
The trial failed to meet its primary endpoint of a significantly higher rate of radical resection with the new regimen vs. chemoradiation, according to data reported in a presscast held before the symposium. However, it did find a lower rate of acute toxicity and, with 35 months of follow-up, an absolute 8% improvement in the 3-year rate of overall survival.
“Despite the fact that the trial was negative ... we show for the first time an alternative to the standard chemoradiation lasting for 5 and a half weeks,” said study coauthor Dr. Lucjan Wyrwicz, head of the Medical Oncology Unit in the Department of Gastrointestinal Cancer at the Maria Sklodowska-Curie Memorial Cancer Center and Institute of Oncology in Warsaw.
The new regimen may be preferable in some clinical scenarios, he noted. For example, the short course of radiation may appeal to patients who want to minimize time off from work, and it may be advantageous when cost or lack of insurance is an issue, and in low-resource countries where there are not enough radiation therapy facilities to go around.
Additionally, the regimen is a more attractive option in patients who have metastases, as they can get some full chemotherapy upfront. In contrast, with chemoradiation, it is typically delayed until several weeks after surgery, essentially leaving metastases uncontrolled in the meantime.
“Having two standards is better than having one standard. We need to try to personalize medicine,” Dr. Wyrwicz summarized.
A caveat to the trial was the use of oxaliplatin, which was included in the protocol before other trials showed that it did not improve outcomes but did add toxicity, he noted. The protocol was amended partway through to allow its omission, but about two-thirds of patients in both arms received the drug. However, findings were much the same whether patients received oxaliplatin or not, he said ahead of the symposium, which was sponsored by ASCO, ASTRO, the American Gastroenterological Association, and the Society of Surgical Oncology.
ASCO expert and presscast moderator Dr. Smitha Krishnamurthi commented, “This is a randomized comparison of short-course radiation with chemotherapy that is demonstrating equal efficacy to traditional chemoradiation. Giving patients a shorter, more convenient, less expensive radiation, and moving the chemotherapy (some of it) upfront appears to be equally active to the chemoradiation. So it does give patients another choice.”
The finding of a lower rate of acute toxicity with the new regimen should be viewed with caution, given the use of oxaliplatin in chemoradiation, which would not be done today, she said.
Uptake of short-course radiation has been greater in Europe than in the United States, according to Dr. Krishnamurthi of Case Western Reserve University, Cleveland. This is possibly because of data from an earlier trial by the Trans Tasman Radiation Oncology Group showing a nonsignificantly higher rate of local recurrence with the short course in patients with less advanced disease.
“There are some other randomized trials which are ongoing, so there’s a lot of interest in this short-course radiation. And I think when we have all of this data together, we will be in a much better position to incorporate it,” she concluded.
In the Polish II trial, the rate of radical (R0) resection did not differ significantly between the new short-course regimen and chemoradiation, although there was a trend favoring the former (77% vs. 71%; P = .081), Dr. Wyrwicz reported.
Patients given the new regimen were less likely to experience acute toxicities (75% vs. 83%; P = .006) but not specifically grade 3 and 4 toxicities. The rate of pathologic complete response did not differ significantly.
The 3-year overall survival rate was higher with the new short-course regimen (73% vs. 65%; P = .046). The groups did not differ significantly with respect to disease-free survival or the incidences of local failure and distant metastases.
FROM THE GASTROINTESTINAL CANCERS SYMPOSIUM
Key clinical point: A regimen of short-course radiation followed by chemotherapy offers a new treatment option for patients with locally advanced rectal cancer.
Major finding: Compared with chemoradiation, the new regimen did not significantly improve local disease outcomes but did yield a significantly better 3-year overall survival rate (73% vs. 65%).
Data source: A randomized phase III trial among 515 patients with locally advanced rectal cancer (Polish II trial).
Disclosures: Dr. Wyrwicz disclosed that he had no relevant conflicts of interest. The study received funding from the Polish Ministry of Science and Higher Education.
Everolimus is effective across diverse patients with GI neuroendocrine tumors
Everolimus improves outcomes in patients with advanced, progressive neuroendocrine tumors of gastrointestinal (GI) or unknown origin regardless of primary location and prior therapy, according to new subgroup analyses of the RADIANT-4 trial.
The phase III trial is the largest of its type in patients with nonfunctioning GI tract or lung neuroendocrine tumors. The subgroup findings for those whose tumors originated in the GI tract or an unknown site (but suspected to be GI) were presented in a presscast held in advance of the Gastrointestinal Cancers Symposium.
Compared with placebo, everolimus prolonged progression-free survival by 6-9 months, corresponding to a 46%-48% relative reduction in the risk of progression or death, reported lead study author Dr. Simron Singh of Sunnybrook’s Odette Cancer Centre in Toronto. Benefit was similar regardless of whether patients had midgut or non-midgut tumors, and whether they had previously received a somatostatin analog or not.
“In my opinion, this study in advanced, progressive neuroendocrine patients [shows] an effective, new and exciting treatment option in a disease where we’ve had very few treatments to date,” Dr. Singh said ahead of the symposium, which was sponsored by ASCO, ASTRO, the American Gastroenterological Association, and the Society of Surgical Oncology.
ASCO expert and presscast moderator Dr. Smitha Krishnamurthi of Case Western Reserve University, Cleveland, agreed, saying that everolimus could help address an unmet need in this disease.
“Patients with GI neuroendocrine tumors have had very few treatment options. Once they have progressed on somatostatin analogues, there really are no good systemic treatments,” she said. “So this finding is very important, that the mTOR inhibitor everolimus has demonstrated an improvement in risk of progression by over 40% and with very little severe toxicity. This is a welcome finding for these patients who have limited systemic treatment options.”
Patients enrolled in RADIANT-4 had lung, GI, or unknown-origin neuroendocrine tumors that had progressed on other therapies, including somatostatin analogs, surgery, or chemotherapy.
They were randomly assigned in 2:1 ratio to receive everolimus (Afinitor) or placebo, each in addition to best supportive care. Everolimus is currently approved by the Food and Drug Administration for the treatment of pancreatic neuroendocrine tumors, as well as breast and kidney cancer, and subependymal giant cell astrocytoma.
Results for the entire trial population have been previously reported and showed that everolimus prolonged progression-free survival by 7.1 months, reducing the risk of events by 52% (Lancet. 2015 Dec 15. doi.org/10.1016/S0140-6736[15]01234-9).
The new subgroup analyses were restricted to the patients with tumors originating in the GI tract (n =175) or an unknown site generally thought to be the GI tract (n = 36).
Among the group with GI tumors, median progression-free survival was 13.1 months with everolimus versus 5.4 months with placebo, Dr. Singh reported. Among the group with tumors of unknown origin, it was 13.6 and 7.5 months, respectively.
Relative to placebo, everolimus prolonged progression-free survival by 6.41 months, reducing the risk of events by 29%, in patients whose tumors originated in the midgut (duodenum, ileum, jejunum, cecum, or appendix). The relative benefit was 6.17 months, with a reduction in the risk of events of 73%, in patients whose tumors originated in non-midgut sites (stomach, colon, and rectum).
In addition, everolimus prolonged progression-free survival by 6.73 months, reducing the risk of events by 46%, in patients who had previously received somatostatin analogues, and by 9.07 months, reducing the risk by 48%, in patients who had not received these agents.
The safety profile of everolimus was consistent with that expected based on the use of this agent in other patient populations, according to Dr. Singh. The most common adverse events were stomatitis, infections, diarrhea, peripheral edema, and fatigue. No new safety signals were seen.
Dr. Singh disclosed that he receives honoraria from, has a consulting or advisory role with, and receives research funding (institutional) and travel, accommodations, and expenses from Novartis. The study received funding from Novartis Pharmaceuticals.
Everolimus improves outcomes in patients with advanced, progressive neuroendocrine tumors of gastrointestinal (GI) or unknown origin regardless of primary location and prior therapy, according to new subgroup analyses of the RADIANT-4 trial.
The phase III trial is the largest of its type in patients with nonfunctioning GI tract or lung neuroendocrine tumors. The subgroup findings for those whose tumors originated in the GI tract or an unknown site (but suspected to be GI) were presented in a presscast held in advance of the Gastrointestinal Cancers Symposium.
Compared with placebo, everolimus prolonged progression-free survival by 6-9 months, corresponding to a 46%-48% relative reduction in the risk of progression or death, reported lead study author Dr. Simron Singh of Sunnybrook’s Odette Cancer Centre in Toronto. Benefit was similar regardless of whether patients had midgut or non-midgut tumors, and whether they had previously received a somatostatin analog or not.
“In my opinion, this study in advanced, progressive neuroendocrine patients [shows] an effective, new and exciting treatment option in a disease where we’ve had very few treatments to date,” Dr. Singh said ahead of the symposium, which was sponsored by ASCO, ASTRO, the American Gastroenterological Association, and the Society of Surgical Oncology.
ASCO expert and presscast moderator Dr. Smitha Krishnamurthi of Case Western Reserve University, Cleveland, agreed, saying that everolimus could help address an unmet need in this disease.
“Patients with GI neuroendocrine tumors have had very few treatment options. Once they have progressed on somatostatin analogues, there really are no good systemic treatments,” she said. “So this finding is very important, that the mTOR inhibitor everolimus has demonstrated an improvement in risk of progression by over 40% and with very little severe toxicity. This is a welcome finding for these patients who have limited systemic treatment options.”
Patients enrolled in RADIANT-4 had lung, GI, or unknown-origin neuroendocrine tumors that had progressed on other therapies, including somatostatin analogs, surgery, or chemotherapy.
They were randomly assigned in 2:1 ratio to receive everolimus (Afinitor) or placebo, each in addition to best supportive care. Everolimus is currently approved by the Food and Drug Administration for the treatment of pancreatic neuroendocrine tumors, as well as breast and kidney cancer, and subependymal giant cell astrocytoma.
Results for the entire trial population have been previously reported and showed that everolimus prolonged progression-free survival by 7.1 months, reducing the risk of events by 52% (Lancet. 2015 Dec 15. doi.org/10.1016/S0140-6736[15]01234-9).
The new subgroup analyses were restricted to the patients with tumors originating in the GI tract (n =175) or an unknown site generally thought to be the GI tract (n = 36).
Among the group with GI tumors, median progression-free survival was 13.1 months with everolimus versus 5.4 months with placebo, Dr. Singh reported. Among the group with tumors of unknown origin, it was 13.6 and 7.5 months, respectively.
Relative to placebo, everolimus prolonged progression-free survival by 6.41 months, reducing the risk of events by 29%, in patients whose tumors originated in the midgut (duodenum, ileum, jejunum, cecum, or appendix). The relative benefit was 6.17 months, with a reduction in the risk of events of 73%, in patients whose tumors originated in non-midgut sites (stomach, colon, and rectum).
In addition, everolimus prolonged progression-free survival by 6.73 months, reducing the risk of events by 46%, in patients who had previously received somatostatin analogues, and by 9.07 months, reducing the risk by 48%, in patients who had not received these agents.
The safety profile of everolimus was consistent with that expected based on the use of this agent in other patient populations, according to Dr. Singh. The most common adverse events were stomatitis, infections, diarrhea, peripheral edema, and fatigue. No new safety signals were seen.
Dr. Singh disclosed that he receives honoraria from, has a consulting or advisory role with, and receives research funding (institutional) and travel, accommodations, and expenses from Novartis. The study received funding from Novartis Pharmaceuticals.
Everolimus improves outcomes in patients with advanced, progressive neuroendocrine tumors of gastrointestinal (GI) or unknown origin regardless of primary location and prior therapy, according to new subgroup analyses of the RADIANT-4 trial.
The phase III trial is the largest of its type in patients with nonfunctioning GI tract or lung neuroendocrine tumors. The subgroup findings for those whose tumors originated in the GI tract or an unknown site (but suspected to be GI) were presented in a presscast held in advance of the Gastrointestinal Cancers Symposium.
Compared with placebo, everolimus prolonged progression-free survival by 6-9 months, corresponding to a 46%-48% relative reduction in the risk of progression or death, reported lead study author Dr. Simron Singh of Sunnybrook’s Odette Cancer Centre in Toronto. Benefit was similar regardless of whether patients had midgut or non-midgut tumors, and whether they had previously received a somatostatin analog or not.
“In my opinion, this study in advanced, progressive neuroendocrine patients [shows] an effective, new and exciting treatment option in a disease where we’ve had very few treatments to date,” Dr. Singh said ahead of the symposium, which was sponsored by ASCO, ASTRO, the American Gastroenterological Association, and the Society of Surgical Oncology.
ASCO expert and presscast moderator Dr. Smitha Krishnamurthi of Case Western Reserve University, Cleveland, agreed, saying that everolimus could help address an unmet need in this disease.
“Patients with GI neuroendocrine tumors have had very few treatment options. Once they have progressed on somatostatin analogues, there really are no good systemic treatments,” she said. “So this finding is very important, that the mTOR inhibitor everolimus has demonstrated an improvement in risk of progression by over 40% and with very little severe toxicity. This is a welcome finding for these patients who have limited systemic treatment options.”
Patients enrolled in RADIANT-4 had lung, GI, or unknown-origin neuroendocrine tumors that had progressed on other therapies, including somatostatin analogs, surgery, or chemotherapy.
They were randomly assigned in 2:1 ratio to receive everolimus (Afinitor) or placebo, each in addition to best supportive care. Everolimus is currently approved by the Food and Drug Administration for the treatment of pancreatic neuroendocrine tumors, as well as breast and kidney cancer, and subependymal giant cell astrocytoma.
Results for the entire trial population have been previously reported and showed that everolimus prolonged progression-free survival by 7.1 months, reducing the risk of events by 52% (Lancet. 2015 Dec 15. doi.org/10.1016/S0140-6736[15]01234-9).
The new subgroup analyses were restricted to the patients with tumors originating in the GI tract (n =175) or an unknown site generally thought to be the GI tract (n = 36).
Among the group with GI tumors, median progression-free survival was 13.1 months with everolimus versus 5.4 months with placebo, Dr. Singh reported. Among the group with tumors of unknown origin, it was 13.6 and 7.5 months, respectively.
Relative to placebo, everolimus prolonged progression-free survival by 6.41 months, reducing the risk of events by 29%, in patients whose tumors originated in the midgut (duodenum, ileum, jejunum, cecum, or appendix). The relative benefit was 6.17 months, with a reduction in the risk of events of 73%, in patients whose tumors originated in non-midgut sites (stomach, colon, and rectum).
In addition, everolimus prolonged progression-free survival by 6.73 months, reducing the risk of events by 46%, in patients who had previously received somatostatin analogues, and by 9.07 months, reducing the risk by 48%, in patients who had not received these agents.
The safety profile of everolimus was consistent with that expected based on the use of this agent in other patient populations, according to Dr. Singh. The most common adverse events were stomatitis, infections, diarrhea, peripheral edema, and fatigue. No new safety signals were seen.
Dr. Singh disclosed that he receives honoraria from, has a consulting or advisory role with, and receives research funding (institutional) and travel, accommodations, and expenses from Novartis. The study received funding from Novartis Pharmaceuticals.
FROM THE GASTROINTESTINAL CANCERS SYMPOSIUM
Key clinical point: Everolimus reduces the risk of progression or death across subgroups of patients who have advanced, progressive neuroendocrine tumors arising in the GI tract or an unknown site.
Major finding: Compared with placebo, everolimus prolonged median progression-free survival by 6-9 months in patients with midgut and non-midgut tumors, and in patients who had and had not received somatostatin analogues.
Data source: A subgroups analysis of a phase III trial among 211 patients with advanced, progressive nonfunctioning neuroendocrine tumors originating in the GI tract or an unknown site (RADIANT-4 trial).
Disclosures: Dr. Singh disclosed that he receives honoraria from, has a consulting or advisory role with, and receives research funding (institutional) and travel, accommodations, and expenses from Novartis. The study received funding from Novartis Pharmaceuticals.
Radiolabeled somatostatin analog has good showing in midgut neuroendocrine tumors
The radiolabeled somatostatin analog 177Lu-Dotatate is efficacious and safe in patients with previously treated advanced midgut neuroendocrine tumors, according to results of the randomized NETTER-1 trial.
Among the 230 patients studied in the phase III trial, compared with peers given high-dose octreotide LAR, patients given 177Lu-Dotatate had a 79% reduction in the risk of progression or death, lead study author Dr. Jonathan R. Strosberg reported in a presscast leading up to the Gastrointestinal Cancers Symposium.
In addition, 18% of patients had a complete or partial response to the radiolabeled analog, which is considered to be a type of peptide receptor radiotherapy. And there was a trend toward better survival with the radiolabeled analog in an interim analysis.
177Lu-Dotatate had a good safety profile, with somewhat higher rates of gastrointestinal adverse events (likely related to an amino acid infusion given along with the agent) and lymphopenia. Regarding leukemia and myelodysplastic syndrome, “the bottom line is that there were only two very questionable myelodysplastic symptom events seen so far. It’s not clear whether it’s true MDS or whether it’s related to therapy,” said Dr. Strosberg of the Moffitt Cancer Center, Tampa, Fla.
“While there have been few available systemic treatment options for patients progressing on first-line somatostatin analogs, [177Lu-Dotatate] appears to have a major therapeutic benefit in this patient population,” he said ahead of the symposium, which was sponsored by ASCO, ASTRO, the American Gastroenterological Association, and the Society of Surgical Oncology.
Everolimus is also likely to be increasingly used in this therapeutic space, given positive results of the RADIANT-4 trial, including a subgroup analysis being reported at the symposium, Dr. Strosberg acknowledged.
“I think there is going to be a lot of debate on whether 177Lu-Dotatate or everolimus should be used in the average patient that progresses on a first-line somatostatin analog,” he said. “I would argue if there is a predictive factor, it may be somatostatin receptor expression. Patients who express a lot of somatostatin receptors on their scans will probably have a high likelihood of doing well with peptide receptor radiotherapy.”
ASCO expert and presscast moderator Dr. Smitha Krishnamurthi of Case Western Reserve University, Cleveland, said, “177Lu-Dotatate showed impressive ability to slow the growth of midgut neuroendocrine tumors that have progressed on somatostatin analog therapy. Also notable was that the 177Lu-Dotatate resulted in a response rate of 18% in these tumors, which are typically unresponsive to systemic therapy. The trend toward improvement in overall survival was also encouraging.
“This tumor-targeted peptide receptor radionuclide therapy represents a new modality of anticancer treatment,” she maintained.
Patients were eligible for NETTER-1 – the first randomized trial of a radiolabeled somatostatin analog in this setting – if they had inoperable, somatostatin receptor–positive neuroendocrine tumors of the midgut (small intestine or proximal colon) that had progressed despite treatment with octreotide LAR at the standard dose of 30 mg.
They were randomized evenly to 177Lu-Dotatate (Lutathera), one treatment every 8 weeks for a total of four treatments, or to octreotide LAR (Sandostatin LAR) 60 mg every 4 weeks.
In results that Dr. Strosberg called “extremely impressive,” median estimated progression-free survival was not reached but expected to be about 40 months with 177Lu-Dotatate, compared with 8 months with high-dose octreotide. The difference corresponded to a sharply reduced risk of events with the radiolabeled analog (hazard ratio, 0.21; P less than .0001).
The objective response rate was 18% with 177Lu-Dotatate, compared with just 3% with high-dose octreotide (P = .0008).
“Most studies have shown response rates in the single digits,” he noted. “This is really the only large study that has shown a double-digit objective response rate in a population with midgut neuroendocrine tumors.”
An interim analysis of overall survival found that there were 13 deaths with 177Lu-Dotatate and 22 with high-dose octreotide, but longer follow-up is needed.
Grade 3 or 4 lymphopenia was more common with the radiolabeled analog (9% vs. 0%), as were grade 3 or 4 nausea (4% vs. 2%) and vomiting (7% vs. 0%).
“I would say most of the gastrointestinal side effects are related actually to the amino acid infusions that were used as nephroprotective drugs in combination with the [177Lu-Dotatate]. The trial mandated use of commercial formulations of the drugs, which are quite nauseating,” Dr. Strosberg said. “In Europe, they use modified amino acid formulations, which are much less nauseating.”
“The good thing is that the nausea and vomiting typically resolved when the amino acid infusion was discontinued,” he added.
The radiolabeled somatostatin analog 177Lu-Dotatate is efficacious and safe in patients with previously treated advanced midgut neuroendocrine tumors, according to results of the randomized NETTER-1 trial.
Among the 230 patients studied in the phase III trial, compared with peers given high-dose octreotide LAR, patients given 177Lu-Dotatate had a 79% reduction in the risk of progression or death, lead study author Dr. Jonathan R. Strosberg reported in a presscast leading up to the Gastrointestinal Cancers Symposium.
In addition, 18% of patients had a complete or partial response to the radiolabeled analog, which is considered to be a type of peptide receptor radiotherapy. And there was a trend toward better survival with the radiolabeled analog in an interim analysis.
177Lu-Dotatate had a good safety profile, with somewhat higher rates of gastrointestinal adverse events (likely related to an amino acid infusion given along with the agent) and lymphopenia. Regarding leukemia and myelodysplastic syndrome, “the bottom line is that there were only two very questionable myelodysplastic symptom events seen so far. It’s not clear whether it’s true MDS or whether it’s related to therapy,” said Dr. Strosberg of the Moffitt Cancer Center, Tampa, Fla.
“While there have been few available systemic treatment options for patients progressing on first-line somatostatin analogs, [177Lu-Dotatate] appears to have a major therapeutic benefit in this patient population,” he said ahead of the symposium, which was sponsored by ASCO, ASTRO, the American Gastroenterological Association, and the Society of Surgical Oncology.
Everolimus is also likely to be increasingly used in this therapeutic space, given positive results of the RADIANT-4 trial, including a subgroup analysis being reported at the symposium, Dr. Strosberg acknowledged.
“I think there is going to be a lot of debate on whether 177Lu-Dotatate or everolimus should be used in the average patient that progresses on a first-line somatostatin analog,” he said. “I would argue if there is a predictive factor, it may be somatostatin receptor expression. Patients who express a lot of somatostatin receptors on their scans will probably have a high likelihood of doing well with peptide receptor radiotherapy.”
ASCO expert and presscast moderator Dr. Smitha Krishnamurthi of Case Western Reserve University, Cleveland, said, “177Lu-Dotatate showed impressive ability to slow the growth of midgut neuroendocrine tumors that have progressed on somatostatin analog therapy. Also notable was that the 177Lu-Dotatate resulted in a response rate of 18% in these tumors, which are typically unresponsive to systemic therapy. The trend toward improvement in overall survival was also encouraging.
“This tumor-targeted peptide receptor radionuclide therapy represents a new modality of anticancer treatment,” she maintained.
Patients were eligible for NETTER-1 – the first randomized trial of a radiolabeled somatostatin analog in this setting – if they had inoperable, somatostatin receptor–positive neuroendocrine tumors of the midgut (small intestine or proximal colon) that had progressed despite treatment with octreotide LAR at the standard dose of 30 mg.
They were randomized evenly to 177Lu-Dotatate (Lutathera), one treatment every 8 weeks for a total of four treatments, or to octreotide LAR (Sandostatin LAR) 60 mg every 4 weeks.
In results that Dr. Strosberg called “extremely impressive,” median estimated progression-free survival was not reached but expected to be about 40 months with 177Lu-Dotatate, compared with 8 months with high-dose octreotide. The difference corresponded to a sharply reduced risk of events with the radiolabeled analog (hazard ratio, 0.21; P less than .0001).
The objective response rate was 18% with 177Lu-Dotatate, compared with just 3% with high-dose octreotide (P = .0008).
“Most studies have shown response rates in the single digits,” he noted. “This is really the only large study that has shown a double-digit objective response rate in a population with midgut neuroendocrine tumors.”
An interim analysis of overall survival found that there were 13 deaths with 177Lu-Dotatate and 22 with high-dose octreotide, but longer follow-up is needed.
Grade 3 or 4 lymphopenia was more common with the radiolabeled analog (9% vs. 0%), as were grade 3 or 4 nausea (4% vs. 2%) and vomiting (7% vs. 0%).
“I would say most of the gastrointestinal side effects are related actually to the amino acid infusions that were used as nephroprotective drugs in combination with the [177Lu-Dotatate]. The trial mandated use of commercial formulations of the drugs, which are quite nauseating,” Dr. Strosberg said. “In Europe, they use modified amino acid formulations, which are much less nauseating.”
“The good thing is that the nausea and vomiting typically resolved when the amino acid infusion was discontinued,” he added.
The radiolabeled somatostatin analog 177Lu-Dotatate is efficacious and safe in patients with previously treated advanced midgut neuroendocrine tumors, according to results of the randomized NETTER-1 trial.
Among the 230 patients studied in the phase III trial, compared with peers given high-dose octreotide LAR, patients given 177Lu-Dotatate had a 79% reduction in the risk of progression or death, lead study author Dr. Jonathan R. Strosberg reported in a presscast leading up to the Gastrointestinal Cancers Symposium.
In addition, 18% of patients had a complete or partial response to the radiolabeled analog, which is considered to be a type of peptide receptor radiotherapy. And there was a trend toward better survival with the radiolabeled analog in an interim analysis.
177Lu-Dotatate had a good safety profile, with somewhat higher rates of gastrointestinal adverse events (likely related to an amino acid infusion given along with the agent) and lymphopenia. Regarding leukemia and myelodysplastic syndrome, “the bottom line is that there were only two very questionable myelodysplastic symptom events seen so far. It’s not clear whether it’s true MDS or whether it’s related to therapy,” said Dr. Strosberg of the Moffitt Cancer Center, Tampa, Fla.
“While there have been few available systemic treatment options for patients progressing on first-line somatostatin analogs, [177Lu-Dotatate] appears to have a major therapeutic benefit in this patient population,” he said ahead of the symposium, which was sponsored by ASCO, ASTRO, the American Gastroenterological Association, and the Society of Surgical Oncology.
Everolimus is also likely to be increasingly used in this therapeutic space, given positive results of the RADIANT-4 trial, including a subgroup analysis being reported at the symposium, Dr. Strosberg acknowledged.
“I think there is going to be a lot of debate on whether 177Lu-Dotatate or everolimus should be used in the average patient that progresses on a first-line somatostatin analog,” he said. “I would argue if there is a predictive factor, it may be somatostatin receptor expression. Patients who express a lot of somatostatin receptors on their scans will probably have a high likelihood of doing well with peptide receptor radiotherapy.”
ASCO expert and presscast moderator Dr. Smitha Krishnamurthi of Case Western Reserve University, Cleveland, said, “177Lu-Dotatate showed impressive ability to slow the growth of midgut neuroendocrine tumors that have progressed on somatostatin analog therapy. Also notable was that the 177Lu-Dotatate resulted in a response rate of 18% in these tumors, which are typically unresponsive to systemic therapy. The trend toward improvement in overall survival was also encouraging.
“This tumor-targeted peptide receptor radionuclide therapy represents a new modality of anticancer treatment,” she maintained.
Patients were eligible for NETTER-1 – the first randomized trial of a radiolabeled somatostatin analog in this setting – if they had inoperable, somatostatin receptor–positive neuroendocrine tumors of the midgut (small intestine or proximal colon) that had progressed despite treatment with octreotide LAR at the standard dose of 30 mg.
They were randomized evenly to 177Lu-Dotatate (Lutathera), one treatment every 8 weeks for a total of four treatments, or to octreotide LAR (Sandostatin LAR) 60 mg every 4 weeks.
In results that Dr. Strosberg called “extremely impressive,” median estimated progression-free survival was not reached but expected to be about 40 months with 177Lu-Dotatate, compared with 8 months with high-dose octreotide. The difference corresponded to a sharply reduced risk of events with the radiolabeled analog (hazard ratio, 0.21; P less than .0001).
The objective response rate was 18% with 177Lu-Dotatate, compared with just 3% with high-dose octreotide (P = .0008).
“Most studies have shown response rates in the single digits,” he noted. “This is really the only large study that has shown a double-digit objective response rate in a population with midgut neuroendocrine tumors.”
An interim analysis of overall survival found that there were 13 deaths with 177Lu-Dotatate and 22 with high-dose octreotide, but longer follow-up is needed.
Grade 3 or 4 lymphopenia was more common with the radiolabeled analog (9% vs. 0%), as were grade 3 or 4 nausea (4% vs. 2%) and vomiting (7% vs. 0%).
“I would say most of the gastrointestinal side effects are related actually to the amino acid infusions that were used as nephroprotective drugs in combination with the [177Lu-Dotatate]. The trial mandated use of commercial formulations of the drugs, which are quite nauseating,” Dr. Strosberg said. “In Europe, they use modified amino acid formulations, which are much less nauseating.”
“The good thing is that the nausea and vomiting typically resolved when the amino acid infusion was discontinued,” he added.
FROM THE GASTROINTESTINAL CANCERS SYMPOSIUM
Key clinical point: 177Lu-Dotatate appears efficacious and safe for the treatment of advanced midgut neuroendocrine tumors.
Major finding: Median progression-free survival was expected to be about 40 months with 177Lu-Dotatate, compared with 8 months with high-dose octreotide LAR.
Data source: A randomized phase III trial among 230 patients with previously treated advanced midgut neuroendocrine tumors (NETTER-1 trial).
Disclosures: Dr. Strosberg disclosed that he had no relevant conflicts of interest. The study received funding from Advanced Accelerator Applications.
Hypofractionated radiation emerges as new standard of care for prostate cancer
SAN FRANCISCO – Hypofractionated radiation therapy, which delivers fewer, larger fractions relative to conventional radiation therapy, can be considered a new standard of care for localized prostate cancer, according to a pair of phase III noninferiority randomized trials reported at the Genitourinary Cancers Symposium.
The Radiation Therapy Oncology Group’s 0415 trial, conducted among men with low-risk disease, found that the 5-year rate of disease-free survival with a 70-Gy hypofractionated regimen was noninferior to that with a conventional regimen (86% vs. 85%). And a trial conducted by the U.K. CHHiP Trial Management Group among men with mainly intermediate-risk disease found that the 5-year rate of freedom from biochemical failure or prostate cancer recurrence with a 60-Gy hypofractionated regimen was noninferior to that with a conventional regimen (90.6% vs. 88.3%).
The trade-offs were small increases in the rates of some gastrointestinal and genitourinary toxicities with the hypofractionated regimens.
“Both of these trials now clearly establish that modest hypofractionated regimens are noninferior for biochemical failure, with modest to no change in toxicity. This is probably ready for prime time,” contended invited discussant Dr. Daniel A. Hamstra, a radiation oncologist with Texas Oncology in Irving. “Hypofractionation provides a cost- and resource-effective treatment that is easier and more convenient for patients.”
Among the points yet to be ironed out are identification of the optimal regimen and implementation of hypofractionation in the United States, he noted; uptake of hypofractionated radiation therapy in breast cancer has been slow, even though research there is about 5 to 10 years ahead of that in prostate cancer. “It will be intriguing to see what happens in the United States, whether or not this type of modest hypofractionation takes off,” he said at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
RTOG 0415 trial
In the first trial, NRG Oncology’s RTOG 0415, investigators led by Dr. W. Robert Lee, a radiation oncologist at Duke University, Durham, N.C., randomized 1,115 men with low-risk prostate cancer to a conventional regimen (73.8 Gy given in 41 fractions over 8.2 weeks) or a hypofractionated regimen (70 Gy given in 28 fractions over 5.6 weeks). None received androgen suppression.
With a median follow-up of 5.8 years, the 5-year rate of disease-free survival (the trial’s primary endpoint) was 85% with conventional radiation therapy and 86% with hypofractionated radiation therapy. The absolute difference of 1% and the hazard ratio of 0.85 in favor of hypofractionation fell well within the predefined noninferiority margins of 7.65%, and 1.52, respectively.
The 5-year rates of biochemical recurrence were 8% with conventional radiation and 6% with hypofractionated radiation (hazard ratio, 0.77).
The two regimens did not differ significantly with respect to the rates of grade 3 or 4 early gastrointestinal and genitourinary adverse events. The hypofractionated regimen was associated with a higher rate of late gastrointestinal adverse events (P = .002), driven by more grade 2 events (18.3% vs. 11.4%), and a trend toward a higher rate of late genitourinary adverse events (P = .06), also driven mainly by more grade 2 events (26.2% vs. 20.5%).
“In men with low-risk prostate cancer, 70 Gy in 28 fractions is not inferior to 73.8 Gy in 41 fractions, albeit with a slight increase in grade 2 GI or GU toxicity,” Dr. Lee concluded. “It will be of great interest to determine if the small increase in grade 2 toxicity is manifest in patient-reported quality of life.”
When asked by an attendee whether the evidence from the two trials is sufficient to make hypofractionation standard of care, he said, “If you have a regimen that has been demonstrated in multiple phase III studies to be better or equivalent, then that can be considered a standard of care.”
Dr. Lee speculated that concerns that 5 years is not a sufficient follow-up may stem from past events in the field. “It’s perhaps related to the worry that radiation oncology really deservedly has about large dose per fraction given our history in the ‘70s and ‘80s when we tried to do things quicker. But if you remember, those toxicities were seen very early,” he elaborated.
“And my question back is, how many patients for how long do you need?” he said, given the more than 4,000 patients with 5-year follow-up in the two trials reported, plus an additional 1,700 expected from a similar Canadian study shortly. “How many patients are enough? Do you need 10,000 patients for 15 years?”
CHHiP trial
In the second trial – Conventional or Hypofractionated High-Dose, Intensity-Modulated Radiotherapy for Prostate Cancer (CHHiP) – Dr. David P. Dearnaley, leader of the Clinical Academic Radiotherapy Team at the Institute of Cancer Research, London, and his colleagues studied 3,216 men who predominantly had intermediate-risk disease, most of whom first received hormone treatment.
They were randomized evenly to three radiation therapy regimens: a conventional regimen of 74 Gy in 37 fractions over 7.4 weeks, a hypofractionated regimen of 60 Gy in 20 fractions over 4 weeks, or a hypofractionated regimen of 57 Gy in 19 fractions over 3.8 weeks.
With a median follow-up of 62 months, the 5-year rate of freedom from biochemical failure or prostate cancer recurrence was 88.3% with the conventional regimen, 90.6% with the 60-Gy hypofractionated regimen, and 85.9% with the 57-Gy hypofractionated regimen.
Compared with the conventional regimen, the 60-Gy hypofractionated schedule yielded a hazard ratio of 0.84, which fell well within the predefined hazard ratio of 1.208 for noninferiority (P = .004). In contrast, the 57-Gy hypofractionated schedule yielded a hazard ratio of 1.20, which was inconclusive.
When the two hypofractionated regimens were compared with each other, the 57-Gy one was inferior to the 60-Gy one, yielding a higher risk of biochemical failure or prostate cancer recurrence (HR, 1.44; P = .003).
Results for prostate cancer mortality and all-cause mortality did not differ significantly, but numbers of events were fairly small, so “we’ll have to wait and see,” Dr. Dearnaley said.
The three regimens yielded similar rates of acute bladder toxicity of various grades, but the timing of the peak rate was earlier with hypofractionation. In contrast, acute bowel toxicity occurred not only earlier, but also at higher rates (P less than .001) with the hypofractionated regimens.
At 5 years, late bowel toxicity with the hypofractionated regimens did not differ from that with the conventional regimen; however, comparing the hypofractionation regimens, the 60-Gy one yielded a higher rate than the 57-Gy one. Similarly, for late bladder toxicity, the rate of grade 2 or worse events was higher with 60 Gy.
The trial population was somewhat heterogeneous, Dr. Dearnaley acknowledged. “We will be doing a multivariate analysis to look at all of these very detailed histopathological features, in addition to a translational study where we want to look at molecular characterization of these patients. We’ve got biopsies on most of them for that.”
“We believe that modest hypofractionation using 60 Gy in 20 fractions delivered with high-quality radiotherapy techniques can now be recommended as a new standard of care in patients with this type of intermediate- and low- and high-risk cancer,” he concluded.
“As we move toward image-guided radiotherapy – and I don’t mean just by using fiducials, I mean by using the MR scans – we can start to boost dominant lesions. And I think the effectiveness of 57 Gy in treating lower amounts of volume of cancer within the prostate may mean that we can get the best therapeutic ratio by lowering the dose a little bit to 57 Gy, but boosting our dominant lesions,” Dr. Dearnaley added.
He agreed with Dr. Lee that collectively, the findings at 5 years of follow-up are sufficient to propel hypofractionation into standard of care, noting that trials of dose escalation show that the hazard ratio for biochemical control remains stable between 5 and 10 years. Additionally, in his opinion, survival is not the right endpoint when it comes to investigating fractionation.
“So because the [prostate-specific antigen] data is robust and I don’t think that’s going to change, the critical issue is actually that of side effects. You can get late, late side effects, and I do think we have to be a little bit cautious about those,” Dr. Dearnaley said, although data from the first patients enrolled in CHHiP in 2001 have not raised any concerns.
“My view is the evidence is sufficiently robust in that large number of patients to change practice now,” he concluded.
SAN FRANCISCO – Hypofractionated radiation therapy, which delivers fewer, larger fractions relative to conventional radiation therapy, can be considered a new standard of care for localized prostate cancer, according to a pair of phase III noninferiority randomized trials reported at the Genitourinary Cancers Symposium.
The Radiation Therapy Oncology Group’s 0415 trial, conducted among men with low-risk disease, found that the 5-year rate of disease-free survival with a 70-Gy hypofractionated regimen was noninferior to that with a conventional regimen (86% vs. 85%). And a trial conducted by the U.K. CHHiP Trial Management Group among men with mainly intermediate-risk disease found that the 5-year rate of freedom from biochemical failure or prostate cancer recurrence with a 60-Gy hypofractionated regimen was noninferior to that with a conventional regimen (90.6% vs. 88.3%).
The trade-offs were small increases in the rates of some gastrointestinal and genitourinary toxicities with the hypofractionated regimens.
“Both of these trials now clearly establish that modest hypofractionated regimens are noninferior for biochemical failure, with modest to no change in toxicity. This is probably ready for prime time,” contended invited discussant Dr. Daniel A. Hamstra, a radiation oncologist with Texas Oncology in Irving. “Hypofractionation provides a cost- and resource-effective treatment that is easier and more convenient for patients.”
Among the points yet to be ironed out are identification of the optimal regimen and implementation of hypofractionation in the United States, he noted; uptake of hypofractionated radiation therapy in breast cancer has been slow, even though research there is about 5 to 10 years ahead of that in prostate cancer. “It will be intriguing to see what happens in the United States, whether or not this type of modest hypofractionation takes off,” he said at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
RTOG 0415 trial
In the first trial, NRG Oncology’s RTOG 0415, investigators led by Dr. W. Robert Lee, a radiation oncologist at Duke University, Durham, N.C., randomized 1,115 men with low-risk prostate cancer to a conventional regimen (73.8 Gy given in 41 fractions over 8.2 weeks) or a hypofractionated regimen (70 Gy given in 28 fractions over 5.6 weeks). None received androgen suppression.
With a median follow-up of 5.8 years, the 5-year rate of disease-free survival (the trial’s primary endpoint) was 85% with conventional radiation therapy and 86% with hypofractionated radiation therapy. The absolute difference of 1% and the hazard ratio of 0.85 in favor of hypofractionation fell well within the predefined noninferiority margins of 7.65%, and 1.52, respectively.
The 5-year rates of biochemical recurrence were 8% with conventional radiation and 6% with hypofractionated radiation (hazard ratio, 0.77).
The two regimens did not differ significantly with respect to the rates of grade 3 or 4 early gastrointestinal and genitourinary adverse events. The hypofractionated regimen was associated with a higher rate of late gastrointestinal adverse events (P = .002), driven by more grade 2 events (18.3% vs. 11.4%), and a trend toward a higher rate of late genitourinary adverse events (P = .06), also driven mainly by more grade 2 events (26.2% vs. 20.5%).
“In men with low-risk prostate cancer, 70 Gy in 28 fractions is not inferior to 73.8 Gy in 41 fractions, albeit with a slight increase in grade 2 GI or GU toxicity,” Dr. Lee concluded. “It will be of great interest to determine if the small increase in grade 2 toxicity is manifest in patient-reported quality of life.”
When asked by an attendee whether the evidence from the two trials is sufficient to make hypofractionation standard of care, he said, “If you have a regimen that has been demonstrated in multiple phase III studies to be better or equivalent, then that can be considered a standard of care.”
Dr. Lee speculated that concerns that 5 years is not a sufficient follow-up may stem from past events in the field. “It’s perhaps related to the worry that radiation oncology really deservedly has about large dose per fraction given our history in the ‘70s and ‘80s when we tried to do things quicker. But if you remember, those toxicities were seen very early,” he elaborated.
“And my question back is, how many patients for how long do you need?” he said, given the more than 4,000 patients with 5-year follow-up in the two trials reported, plus an additional 1,700 expected from a similar Canadian study shortly. “How many patients are enough? Do you need 10,000 patients for 15 years?”
CHHiP trial
In the second trial – Conventional or Hypofractionated High-Dose, Intensity-Modulated Radiotherapy for Prostate Cancer (CHHiP) – Dr. David P. Dearnaley, leader of the Clinical Academic Radiotherapy Team at the Institute of Cancer Research, London, and his colleagues studied 3,216 men who predominantly had intermediate-risk disease, most of whom first received hormone treatment.
They were randomized evenly to three radiation therapy regimens: a conventional regimen of 74 Gy in 37 fractions over 7.4 weeks, a hypofractionated regimen of 60 Gy in 20 fractions over 4 weeks, or a hypofractionated regimen of 57 Gy in 19 fractions over 3.8 weeks.
With a median follow-up of 62 months, the 5-year rate of freedom from biochemical failure or prostate cancer recurrence was 88.3% with the conventional regimen, 90.6% with the 60-Gy hypofractionated regimen, and 85.9% with the 57-Gy hypofractionated regimen.
Compared with the conventional regimen, the 60-Gy hypofractionated schedule yielded a hazard ratio of 0.84, which fell well within the predefined hazard ratio of 1.208 for noninferiority (P = .004). In contrast, the 57-Gy hypofractionated schedule yielded a hazard ratio of 1.20, which was inconclusive.
When the two hypofractionated regimens were compared with each other, the 57-Gy one was inferior to the 60-Gy one, yielding a higher risk of biochemical failure or prostate cancer recurrence (HR, 1.44; P = .003).
Results for prostate cancer mortality and all-cause mortality did not differ significantly, but numbers of events were fairly small, so “we’ll have to wait and see,” Dr. Dearnaley said.
The three regimens yielded similar rates of acute bladder toxicity of various grades, but the timing of the peak rate was earlier with hypofractionation. In contrast, acute bowel toxicity occurred not only earlier, but also at higher rates (P less than .001) with the hypofractionated regimens.
At 5 years, late bowel toxicity with the hypofractionated regimens did not differ from that with the conventional regimen; however, comparing the hypofractionation regimens, the 60-Gy one yielded a higher rate than the 57-Gy one. Similarly, for late bladder toxicity, the rate of grade 2 or worse events was higher with 60 Gy.
The trial population was somewhat heterogeneous, Dr. Dearnaley acknowledged. “We will be doing a multivariate analysis to look at all of these very detailed histopathological features, in addition to a translational study where we want to look at molecular characterization of these patients. We’ve got biopsies on most of them for that.”
“We believe that modest hypofractionation using 60 Gy in 20 fractions delivered with high-quality radiotherapy techniques can now be recommended as a new standard of care in patients with this type of intermediate- and low- and high-risk cancer,” he concluded.
“As we move toward image-guided radiotherapy – and I don’t mean just by using fiducials, I mean by using the MR scans – we can start to boost dominant lesions. And I think the effectiveness of 57 Gy in treating lower amounts of volume of cancer within the prostate may mean that we can get the best therapeutic ratio by lowering the dose a little bit to 57 Gy, but boosting our dominant lesions,” Dr. Dearnaley added.
He agreed with Dr. Lee that collectively, the findings at 5 years of follow-up are sufficient to propel hypofractionation into standard of care, noting that trials of dose escalation show that the hazard ratio for biochemical control remains stable between 5 and 10 years. Additionally, in his opinion, survival is not the right endpoint when it comes to investigating fractionation.
“So because the [prostate-specific antigen] data is robust and I don’t think that’s going to change, the critical issue is actually that of side effects. You can get late, late side effects, and I do think we have to be a little bit cautious about those,” Dr. Dearnaley said, although data from the first patients enrolled in CHHiP in 2001 have not raised any concerns.
“My view is the evidence is sufficiently robust in that large number of patients to change practice now,” he concluded.
SAN FRANCISCO – Hypofractionated radiation therapy, which delivers fewer, larger fractions relative to conventional radiation therapy, can be considered a new standard of care for localized prostate cancer, according to a pair of phase III noninferiority randomized trials reported at the Genitourinary Cancers Symposium.
The Radiation Therapy Oncology Group’s 0415 trial, conducted among men with low-risk disease, found that the 5-year rate of disease-free survival with a 70-Gy hypofractionated regimen was noninferior to that with a conventional regimen (86% vs. 85%). And a trial conducted by the U.K. CHHiP Trial Management Group among men with mainly intermediate-risk disease found that the 5-year rate of freedom from biochemical failure or prostate cancer recurrence with a 60-Gy hypofractionated regimen was noninferior to that with a conventional regimen (90.6% vs. 88.3%).
The trade-offs were small increases in the rates of some gastrointestinal and genitourinary toxicities with the hypofractionated regimens.
“Both of these trials now clearly establish that modest hypofractionated regimens are noninferior for biochemical failure, with modest to no change in toxicity. This is probably ready for prime time,” contended invited discussant Dr. Daniel A. Hamstra, a radiation oncologist with Texas Oncology in Irving. “Hypofractionation provides a cost- and resource-effective treatment that is easier and more convenient for patients.”
Among the points yet to be ironed out are identification of the optimal regimen and implementation of hypofractionation in the United States, he noted; uptake of hypofractionated radiation therapy in breast cancer has been slow, even though research there is about 5 to 10 years ahead of that in prostate cancer. “It will be intriguing to see what happens in the United States, whether or not this type of modest hypofractionation takes off,” he said at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
RTOG 0415 trial
In the first trial, NRG Oncology’s RTOG 0415, investigators led by Dr. W. Robert Lee, a radiation oncologist at Duke University, Durham, N.C., randomized 1,115 men with low-risk prostate cancer to a conventional regimen (73.8 Gy given in 41 fractions over 8.2 weeks) or a hypofractionated regimen (70 Gy given in 28 fractions over 5.6 weeks). None received androgen suppression.
With a median follow-up of 5.8 years, the 5-year rate of disease-free survival (the trial’s primary endpoint) was 85% with conventional radiation therapy and 86% with hypofractionated radiation therapy. The absolute difference of 1% and the hazard ratio of 0.85 in favor of hypofractionation fell well within the predefined noninferiority margins of 7.65%, and 1.52, respectively.
The 5-year rates of biochemical recurrence were 8% with conventional radiation and 6% with hypofractionated radiation (hazard ratio, 0.77).
The two regimens did not differ significantly with respect to the rates of grade 3 or 4 early gastrointestinal and genitourinary adverse events. The hypofractionated regimen was associated with a higher rate of late gastrointestinal adverse events (P = .002), driven by more grade 2 events (18.3% vs. 11.4%), and a trend toward a higher rate of late genitourinary adverse events (P = .06), also driven mainly by more grade 2 events (26.2% vs. 20.5%).
“In men with low-risk prostate cancer, 70 Gy in 28 fractions is not inferior to 73.8 Gy in 41 fractions, albeit with a slight increase in grade 2 GI or GU toxicity,” Dr. Lee concluded. “It will be of great interest to determine if the small increase in grade 2 toxicity is manifest in patient-reported quality of life.”
When asked by an attendee whether the evidence from the two trials is sufficient to make hypofractionation standard of care, he said, “If you have a regimen that has been demonstrated in multiple phase III studies to be better or equivalent, then that can be considered a standard of care.”
Dr. Lee speculated that concerns that 5 years is not a sufficient follow-up may stem from past events in the field. “It’s perhaps related to the worry that radiation oncology really deservedly has about large dose per fraction given our history in the ‘70s and ‘80s when we tried to do things quicker. But if you remember, those toxicities were seen very early,” he elaborated.
“And my question back is, how many patients for how long do you need?” he said, given the more than 4,000 patients with 5-year follow-up in the two trials reported, plus an additional 1,700 expected from a similar Canadian study shortly. “How many patients are enough? Do you need 10,000 patients for 15 years?”
CHHiP trial
In the second trial – Conventional or Hypofractionated High-Dose, Intensity-Modulated Radiotherapy for Prostate Cancer (CHHiP) – Dr. David P. Dearnaley, leader of the Clinical Academic Radiotherapy Team at the Institute of Cancer Research, London, and his colleagues studied 3,216 men who predominantly had intermediate-risk disease, most of whom first received hormone treatment.
They were randomized evenly to three radiation therapy regimens: a conventional regimen of 74 Gy in 37 fractions over 7.4 weeks, a hypofractionated regimen of 60 Gy in 20 fractions over 4 weeks, or a hypofractionated regimen of 57 Gy in 19 fractions over 3.8 weeks.
With a median follow-up of 62 months, the 5-year rate of freedom from biochemical failure or prostate cancer recurrence was 88.3% with the conventional regimen, 90.6% with the 60-Gy hypofractionated regimen, and 85.9% with the 57-Gy hypofractionated regimen.
Compared with the conventional regimen, the 60-Gy hypofractionated schedule yielded a hazard ratio of 0.84, which fell well within the predefined hazard ratio of 1.208 for noninferiority (P = .004). In contrast, the 57-Gy hypofractionated schedule yielded a hazard ratio of 1.20, which was inconclusive.
When the two hypofractionated regimens were compared with each other, the 57-Gy one was inferior to the 60-Gy one, yielding a higher risk of biochemical failure or prostate cancer recurrence (HR, 1.44; P = .003).
Results for prostate cancer mortality and all-cause mortality did not differ significantly, but numbers of events were fairly small, so “we’ll have to wait and see,” Dr. Dearnaley said.
The three regimens yielded similar rates of acute bladder toxicity of various grades, but the timing of the peak rate was earlier with hypofractionation. In contrast, acute bowel toxicity occurred not only earlier, but also at higher rates (P less than .001) with the hypofractionated regimens.
At 5 years, late bowel toxicity with the hypofractionated regimens did not differ from that with the conventional regimen; however, comparing the hypofractionation regimens, the 60-Gy one yielded a higher rate than the 57-Gy one. Similarly, for late bladder toxicity, the rate of grade 2 or worse events was higher with 60 Gy.
The trial population was somewhat heterogeneous, Dr. Dearnaley acknowledged. “We will be doing a multivariate analysis to look at all of these very detailed histopathological features, in addition to a translational study where we want to look at molecular characterization of these patients. We’ve got biopsies on most of them for that.”
“We believe that modest hypofractionation using 60 Gy in 20 fractions delivered with high-quality radiotherapy techniques can now be recommended as a new standard of care in patients with this type of intermediate- and low- and high-risk cancer,” he concluded.
“As we move toward image-guided radiotherapy – and I don’t mean just by using fiducials, I mean by using the MR scans – we can start to boost dominant lesions. And I think the effectiveness of 57 Gy in treating lower amounts of volume of cancer within the prostate may mean that we can get the best therapeutic ratio by lowering the dose a little bit to 57 Gy, but boosting our dominant lesions,” Dr. Dearnaley added.
He agreed with Dr. Lee that collectively, the findings at 5 years of follow-up are sufficient to propel hypofractionation into standard of care, noting that trials of dose escalation show that the hazard ratio for biochemical control remains stable between 5 and 10 years. Additionally, in his opinion, survival is not the right endpoint when it comes to investigating fractionation.
“So because the [prostate-specific antigen] data is robust and I don’t think that’s going to change, the critical issue is actually that of side effects. You can get late, late side effects, and I do think we have to be a little bit cautious about those,” Dr. Dearnaley said, although data from the first patients enrolled in CHHiP in 2001 have not raised any concerns.
“My view is the evidence is sufficiently robust in that large number of patients to change practice now,” he concluded.
AT THE GENITOURINARY CANCERS SYMPOSIUM
Key clinical point: Hypofractionated radiation therapy was not inferior to conventional radiation therapy in men with low-risk or predominantly intermediate-risk prostate cancer.
Major finding: The 5-year rate of disease-free survival with a 70-Gy hypofractionated regimen was noninferior to that with a conventional regimen (86% vs. 85%). The 5-year rate of freedom from biochemical failure or prostate cancer recurrence with a 60-Gy hypofractionated regimen was noninferior to that with a conventional regimen (90.6% vs. 88.3%).
Data source: A pair of randomized phase 3 trials among 1,115 men with low-risk prostate cancer (RTOG 0415 trial) and 3,216 men with predominantly intermediate-risk prostate cancer (CHHiP trial).
Disclosures: Dr. Lee disclosed that he had no relevant conflicts of interest. Dr. Dearnaley disclosed that he had no relevant conflicts of interest. Dr. Hamstra disclosed that he receives honoraria from Varian Medical Systems.
Testicular cancer patients who fare well early on have smooth sailing thereafter
SAN FRANCISCO – Men who undergo treatment for metastatic testicular cancer and are alive and disease free a few years later have an excellent prognosis, regardless of their initial risk group, and don’t need CT surveillance, new data suggest.
In the apparent first conditional survival analysis to stratify adult patients according to the International Germ Cell Cancer Collaborative Group (IGCCCG) risk classification system, investigators led by Dr. Jenny J. Ko studied 942 men with this cancer treated over a 22-year period.
Results reported at the 2016 Genitourinary Cancers Symposium sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology showed that those who were still alive and free of disease at 2 years after diagnosis had a 98%-99% probability of remaining so over the next 2 years.
“This study has implications for survivorship, including counseling of patients; applying for life, disability, or medical insurance; and determining the frequency of surveillance imaging post therapy,” said Dr. Ko of the British Columbia Cancer Agency, Abbotsford. “Our study provides support for no further routine CT imaging beyond 2 years post first-line curative treatment in this patient population, which is consistent with the [National Comprehensive Cancer Network] guideline,” she said.
In additional findings, the patients had better outcomes than those seen in the original study used to derive the IGCCCG risk classification system nearly two decades ago (J Clin Oncol. 1997;15:594-603). This improvement “may be due to the better supportive care, standardized use of modern chemotherapy regimens, and better risk stratification in the contemporary cohort,” she proposed.
Invited discussant Dr. Christian K. Kollmannsberger, a medical oncologist with the BC Cancer Agency’s Vancouver Cancer Centre and the University of British Columbia, Vancouver, noted that the findings are consistent with those of other contemporary studies in this patient population, showing that most relapses occur in the first 2 years and that outcomes have improved in recent years.
The NCCN guidelines therefore endorse a lower frequency of clinical exams and imaging after 2 years, “but I think the other guidelines need to follow, and we need to really adopt our guidelines based on the results we have and lighten the burden for our patients,” he maintained.
Additionally, the overall better outcomes for patients in the contemporary era should be taken into consideration when designing new trials, according to Dr. Kollmannsberger.
“We have had numerous discussions in the past how to best statistically design our first-line trials. Should we use the IGCCCG classification data or not? And I think it’s time to move away from that and to use the updated data in order to design the appropriate trial,” he said, adding that the risk classification system is being revised to incorporate new data.
In their study, Dr. Ko and her colleagues reviewed the charts of men with a diagnosis of metastatic testicular germ cell tumors treated at five tertiary cancer centers in Canada, the United States, and Australia between 1990 and 2012.
At increments of 6 months (corresponding to typical assessment time points in men receiving first-line therapy), they calculated the probability of subsequently remaining alive among survivors and the probability of subsequently remaining alive without disease among survivors who had not experienced relapse.
Results for the entire population showed that, with a median follow-up of 99 months, the 5-year rate of overall survival was 95%, 93%, and 64% among patients with, respectively, favorable-, intermediate-, and poor-risk disease at diagnosis according to IGCCCG criteria, she reported. The corresponding disease-free survival rates were 88%, 81%, and 54%.
At baseline, the 2-year conditional overall survival was 97%, 94%, and 71% in patients with favorable-, intermediate-, and poor-risk disease, respectively. The differences diminished over time, and by 2 years out, corresponding values were 99%, 99%, and 93%, and no longer significantly different.
Similarly, at baseline, the 2-year conditional disease-free survival rate was 91%, 84%, and 55% in patients with favorable-, intermediate-, and poor-risk disease, respectively. By 2 years out, it was 98%, 99%, and 98%.
Findings were similar for men with seminoma and with nonseminoma tumor types.
Dr. Ko disclosed that she had no relevant conflicts of interest. Dr. Kollmannsberger disclosed that he receives honoraria from Bristol-Myers Squibb, Novartis, and Pfizer, and that he has consulting or advisory roles with Bristol-Myers Squibb, Novartis, Pfizer, and Seattle Genetics.
SAN FRANCISCO – Men who undergo treatment for metastatic testicular cancer and are alive and disease free a few years later have an excellent prognosis, regardless of their initial risk group, and don’t need CT surveillance, new data suggest.
In the apparent first conditional survival analysis to stratify adult patients according to the International Germ Cell Cancer Collaborative Group (IGCCCG) risk classification system, investigators led by Dr. Jenny J. Ko studied 942 men with this cancer treated over a 22-year period.
Results reported at the 2016 Genitourinary Cancers Symposium sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology showed that those who were still alive and free of disease at 2 years after diagnosis had a 98%-99% probability of remaining so over the next 2 years.
“This study has implications for survivorship, including counseling of patients; applying for life, disability, or medical insurance; and determining the frequency of surveillance imaging post therapy,” said Dr. Ko of the British Columbia Cancer Agency, Abbotsford. “Our study provides support for no further routine CT imaging beyond 2 years post first-line curative treatment in this patient population, which is consistent with the [National Comprehensive Cancer Network] guideline,” she said.
In additional findings, the patients had better outcomes than those seen in the original study used to derive the IGCCCG risk classification system nearly two decades ago (J Clin Oncol. 1997;15:594-603). This improvement “may be due to the better supportive care, standardized use of modern chemotherapy regimens, and better risk stratification in the contemporary cohort,” she proposed.
Invited discussant Dr. Christian K. Kollmannsberger, a medical oncologist with the BC Cancer Agency’s Vancouver Cancer Centre and the University of British Columbia, Vancouver, noted that the findings are consistent with those of other contemporary studies in this patient population, showing that most relapses occur in the first 2 years and that outcomes have improved in recent years.
The NCCN guidelines therefore endorse a lower frequency of clinical exams and imaging after 2 years, “but I think the other guidelines need to follow, and we need to really adopt our guidelines based on the results we have and lighten the burden for our patients,” he maintained.
Additionally, the overall better outcomes for patients in the contemporary era should be taken into consideration when designing new trials, according to Dr. Kollmannsberger.
“We have had numerous discussions in the past how to best statistically design our first-line trials. Should we use the IGCCCG classification data or not? And I think it’s time to move away from that and to use the updated data in order to design the appropriate trial,” he said, adding that the risk classification system is being revised to incorporate new data.
In their study, Dr. Ko and her colleagues reviewed the charts of men with a diagnosis of metastatic testicular germ cell tumors treated at five tertiary cancer centers in Canada, the United States, and Australia between 1990 and 2012.
At increments of 6 months (corresponding to typical assessment time points in men receiving first-line therapy), they calculated the probability of subsequently remaining alive among survivors and the probability of subsequently remaining alive without disease among survivors who had not experienced relapse.
Results for the entire population showed that, with a median follow-up of 99 months, the 5-year rate of overall survival was 95%, 93%, and 64% among patients with, respectively, favorable-, intermediate-, and poor-risk disease at diagnosis according to IGCCCG criteria, she reported. The corresponding disease-free survival rates were 88%, 81%, and 54%.
At baseline, the 2-year conditional overall survival was 97%, 94%, and 71% in patients with favorable-, intermediate-, and poor-risk disease, respectively. The differences diminished over time, and by 2 years out, corresponding values were 99%, 99%, and 93%, and no longer significantly different.
Similarly, at baseline, the 2-year conditional disease-free survival rate was 91%, 84%, and 55% in patients with favorable-, intermediate-, and poor-risk disease, respectively. By 2 years out, it was 98%, 99%, and 98%.
Findings were similar for men with seminoma and with nonseminoma tumor types.
Dr. Ko disclosed that she had no relevant conflicts of interest. Dr. Kollmannsberger disclosed that he receives honoraria from Bristol-Myers Squibb, Novartis, and Pfizer, and that he has consulting or advisory roles with Bristol-Myers Squibb, Novartis, Pfizer, and Seattle Genetics.
SAN FRANCISCO – Men who undergo treatment for metastatic testicular cancer and are alive and disease free a few years later have an excellent prognosis, regardless of their initial risk group, and don’t need CT surveillance, new data suggest.
In the apparent first conditional survival analysis to stratify adult patients according to the International Germ Cell Cancer Collaborative Group (IGCCCG) risk classification system, investigators led by Dr. Jenny J. Ko studied 942 men with this cancer treated over a 22-year period.
Results reported at the 2016 Genitourinary Cancers Symposium sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology showed that those who were still alive and free of disease at 2 years after diagnosis had a 98%-99% probability of remaining so over the next 2 years.
“This study has implications for survivorship, including counseling of patients; applying for life, disability, or medical insurance; and determining the frequency of surveillance imaging post therapy,” said Dr. Ko of the British Columbia Cancer Agency, Abbotsford. “Our study provides support for no further routine CT imaging beyond 2 years post first-line curative treatment in this patient population, which is consistent with the [National Comprehensive Cancer Network] guideline,” she said.
In additional findings, the patients had better outcomes than those seen in the original study used to derive the IGCCCG risk classification system nearly two decades ago (J Clin Oncol. 1997;15:594-603). This improvement “may be due to the better supportive care, standardized use of modern chemotherapy regimens, and better risk stratification in the contemporary cohort,” she proposed.
Invited discussant Dr. Christian K. Kollmannsberger, a medical oncologist with the BC Cancer Agency’s Vancouver Cancer Centre and the University of British Columbia, Vancouver, noted that the findings are consistent with those of other contemporary studies in this patient population, showing that most relapses occur in the first 2 years and that outcomes have improved in recent years.
The NCCN guidelines therefore endorse a lower frequency of clinical exams and imaging after 2 years, “but I think the other guidelines need to follow, and we need to really adopt our guidelines based on the results we have and lighten the burden for our patients,” he maintained.
Additionally, the overall better outcomes for patients in the contemporary era should be taken into consideration when designing new trials, according to Dr. Kollmannsberger.
“We have had numerous discussions in the past how to best statistically design our first-line trials. Should we use the IGCCCG classification data or not? And I think it’s time to move away from that and to use the updated data in order to design the appropriate trial,” he said, adding that the risk classification system is being revised to incorporate new data.
In their study, Dr. Ko and her colleagues reviewed the charts of men with a diagnosis of metastatic testicular germ cell tumors treated at five tertiary cancer centers in Canada, the United States, and Australia between 1990 and 2012.
At increments of 6 months (corresponding to typical assessment time points in men receiving first-line therapy), they calculated the probability of subsequently remaining alive among survivors and the probability of subsequently remaining alive without disease among survivors who had not experienced relapse.
Results for the entire population showed that, with a median follow-up of 99 months, the 5-year rate of overall survival was 95%, 93%, and 64% among patients with, respectively, favorable-, intermediate-, and poor-risk disease at diagnosis according to IGCCCG criteria, she reported. The corresponding disease-free survival rates were 88%, 81%, and 54%.
At baseline, the 2-year conditional overall survival was 97%, 94%, and 71% in patients with favorable-, intermediate-, and poor-risk disease, respectively. The differences diminished over time, and by 2 years out, corresponding values were 99%, 99%, and 93%, and no longer significantly different.
Similarly, at baseline, the 2-year conditional disease-free survival rate was 91%, 84%, and 55% in patients with favorable-, intermediate-, and poor-risk disease, respectively. By 2 years out, it was 98%, 99%, and 98%.
Findings were similar for men with seminoma and with nonseminoma tumor types.
Dr. Ko disclosed that she had no relevant conflicts of interest. Dr. Kollmannsberger disclosed that he receives honoraria from Bristol-Myers Squibb, Novartis, and Pfizer, and that he has consulting or advisory roles with Bristol-Myers Squibb, Novartis, Pfizer, and Seattle Genetics.
AT THE GENITOURINARY CANCERS SYMPOSIUM
Key clinical point: The longer men lived without any recurrence, the greater their probability of remaining alive and disease free in the future.
Major finding: Men who were still alive and disease free at 2 years after diagnosis had a 98% to 99% probability of remaining so for at least the next 2 years.
Data source: A retrospective cohort study of 942 men with metastatic testicular germ cell tumor treated between 1990 and 2012.
Disclosures: Dr. Ko disclosed that she had no relevant conflicts of interest. Dr. Kollmannsberger disclosed that he receives honoraria from Bristol-Myers Squibb, Novartis, and Pfizer, and that he has consulting or advisory roles with Bristol-Myers Squibb, Novartis, Pfizer, and Seattle Genetics.
Poorer survival of African Americans with kidney cancer may be due to genomic differences
SAN FRANCISCO – African American patients with clear-cell renal cell carcinoma may have poorer survival in part because of genomic factors that render tumors more aggressive and less sensitive to anti-angiogenic therapy, suggests a study reported at the Genitourinary Cancers Symposium.
Genomic analysis in 438 patients with metastatic disease found that African Americans were about half as likely as Caucasians to have mutations of the von Hippel–Lindau (VHL) tumor suppressor gene, reported lead investigator Dr. Tracy Lynn Rose, a hematology-oncology fellow at the University of North Carolina at Chapel Hill and Lineberger Comprehensive Cancer Center. Mutational inactivation of this gene leads to increased signaling in the vascular endothelial growth factor (VEGF) pathway.
African Americans also were more likely to have the clear cell B molecular subtype and had less up-regulation of pathways associated with hypoxia-inducible factor (HIF), which collectively suggest a less angiogenic profile and activation of non-VEGF pathways.
A companion analysis of 35,152 patients treated during a 14-year period found that African American patients with metastatic renal cell carcinoma still had a higher risk of death than white peers in the contemporary era, after introduction of multiple agents that target the VEGF pathway and similar increases in receipt of systemic therapy.
“Our findings indicate clear differences in the biology of clear-cell renal cell carcinoma between African Americans and Caucasians. These differences could suggest a larger proportion of tumors from African Americans have a HIF- and VEGF-independent propensity for aggressiveness, and they also suggest perhaps increased resistance of African Americans to VEGF-targeted therapy,” Dr. Rose said at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
“Overall, our data lend support to a role for tumor biology in the survival disparity observed between African American and Caucasian patients,” she said.
The study may be a step toward precision medicine, whereby race is used to guide treatment decisions, according to invited discussant Dr. Guru Sonpavde, director of the Genitourinary Malignancy Program at the University of Alabama at Birmingham. “That’s an exciting possibility,” he said.
“It is plausible that African American patients are less VEGF driven, less responsive to VEGF inhibitors, but I think the results right now are not ready for use in the clinic,” he further commented. “We need validation in a larger number of African American patients. But even more importantly, we need to focus more on molecular measures of VEGF-driven tumors, to select patients for VEGF inhibitors since we don’t have any biomarkers of this sort in the clinic today.”
“Finally, somatic differences may be driven by differences in the germline, and we may want to focus on integrating the germline and somatic alterations into a molecular panel which might be even better at predicting benefit from specific agents,” he concluded.
Previous studies have found a small but consistent elevation of the risk of death for African American patients with renal cell carcinoma, Dr. Rose noted when introducing the study. Initial hypotheses were that this disparity might be due to differences in comorbidities and use of nephrectomy.
She and her colleagues performed genomic analyses in a discovery cohort of 438 African American and Caucasian patients with metastatic clear-cell renal cell carcinoma from The Cancer Genome Atlas database.
Results indicated that African Americans in this discovery cohort were less likely to have a VHL mutation (17% vs. 50%, P = .036), a finding that was confirmed in a validation cohort of 135 similar patients (40% vs. 81%, P = .008).
African American patients were less likely to have several VEGF and HIF signatures relative to Caucasian counterparts. On the other hand, they were more likely to have the clear cell B molecular subtype (79% vs. 45%, P less than .01), which has been associated with decreased activation of angiogenic pathways and poorer prognosis.
The investigators next analyzed data from the National Cancer Database, assessing survival among 35,152 patients who received a diagnosis of metastatic clear-cell renal cell carcinoma between 1998 and 2011.
The proportion receiving systemic therapy over time was similar for African American and Caucasian patients, with both seeing a rise in 2006, corresponding to the introduction of VEGF-targeted therapies. The poorer median survival for African American versus Caucasian patients seen during 1998-2004 (6.0 vs. 7.6 months; adjusted hazard ratio, 1.07; P less than .01) was still evident in 2006-2011 (6.5 vs. 9.2 months; adjusted hazard ratio, 1.08; P less than .01).
SAN FRANCISCO – African American patients with clear-cell renal cell carcinoma may have poorer survival in part because of genomic factors that render tumors more aggressive and less sensitive to anti-angiogenic therapy, suggests a study reported at the Genitourinary Cancers Symposium.
Genomic analysis in 438 patients with metastatic disease found that African Americans were about half as likely as Caucasians to have mutations of the von Hippel–Lindau (VHL) tumor suppressor gene, reported lead investigator Dr. Tracy Lynn Rose, a hematology-oncology fellow at the University of North Carolina at Chapel Hill and Lineberger Comprehensive Cancer Center. Mutational inactivation of this gene leads to increased signaling in the vascular endothelial growth factor (VEGF) pathway.
African Americans also were more likely to have the clear cell B molecular subtype and had less up-regulation of pathways associated with hypoxia-inducible factor (HIF), which collectively suggest a less angiogenic profile and activation of non-VEGF pathways.
A companion analysis of 35,152 patients treated during a 14-year period found that African American patients with metastatic renal cell carcinoma still had a higher risk of death than white peers in the contemporary era, after introduction of multiple agents that target the VEGF pathway and similar increases in receipt of systemic therapy.
“Our findings indicate clear differences in the biology of clear-cell renal cell carcinoma between African Americans and Caucasians. These differences could suggest a larger proportion of tumors from African Americans have a HIF- and VEGF-independent propensity for aggressiveness, and they also suggest perhaps increased resistance of African Americans to VEGF-targeted therapy,” Dr. Rose said at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
“Overall, our data lend support to a role for tumor biology in the survival disparity observed between African American and Caucasian patients,” she said.
The study may be a step toward precision medicine, whereby race is used to guide treatment decisions, according to invited discussant Dr. Guru Sonpavde, director of the Genitourinary Malignancy Program at the University of Alabama at Birmingham. “That’s an exciting possibility,” he said.
“It is plausible that African American patients are less VEGF driven, less responsive to VEGF inhibitors, but I think the results right now are not ready for use in the clinic,” he further commented. “We need validation in a larger number of African American patients. But even more importantly, we need to focus more on molecular measures of VEGF-driven tumors, to select patients for VEGF inhibitors since we don’t have any biomarkers of this sort in the clinic today.”
“Finally, somatic differences may be driven by differences in the germline, and we may want to focus on integrating the germline and somatic alterations into a molecular panel which might be even better at predicting benefit from specific agents,” he concluded.
Previous studies have found a small but consistent elevation of the risk of death for African American patients with renal cell carcinoma, Dr. Rose noted when introducing the study. Initial hypotheses were that this disparity might be due to differences in comorbidities and use of nephrectomy.
She and her colleagues performed genomic analyses in a discovery cohort of 438 African American and Caucasian patients with metastatic clear-cell renal cell carcinoma from The Cancer Genome Atlas database.
Results indicated that African Americans in this discovery cohort were less likely to have a VHL mutation (17% vs. 50%, P = .036), a finding that was confirmed in a validation cohort of 135 similar patients (40% vs. 81%, P = .008).
African American patients were less likely to have several VEGF and HIF signatures relative to Caucasian counterparts. On the other hand, they were more likely to have the clear cell B molecular subtype (79% vs. 45%, P less than .01), which has been associated with decreased activation of angiogenic pathways and poorer prognosis.
The investigators next analyzed data from the National Cancer Database, assessing survival among 35,152 patients who received a diagnosis of metastatic clear-cell renal cell carcinoma between 1998 and 2011.
The proportion receiving systemic therapy over time was similar for African American and Caucasian patients, with both seeing a rise in 2006, corresponding to the introduction of VEGF-targeted therapies. The poorer median survival for African American versus Caucasian patients seen during 1998-2004 (6.0 vs. 7.6 months; adjusted hazard ratio, 1.07; P less than .01) was still evident in 2006-2011 (6.5 vs. 9.2 months; adjusted hazard ratio, 1.08; P less than .01).
SAN FRANCISCO – African American patients with clear-cell renal cell carcinoma may have poorer survival in part because of genomic factors that render tumors more aggressive and less sensitive to anti-angiogenic therapy, suggests a study reported at the Genitourinary Cancers Symposium.
Genomic analysis in 438 patients with metastatic disease found that African Americans were about half as likely as Caucasians to have mutations of the von Hippel–Lindau (VHL) tumor suppressor gene, reported lead investigator Dr. Tracy Lynn Rose, a hematology-oncology fellow at the University of North Carolina at Chapel Hill and Lineberger Comprehensive Cancer Center. Mutational inactivation of this gene leads to increased signaling in the vascular endothelial growth factor (VEGF) pathway.
African Americans also were more likely to have the clear cell B molecular subtype and had less up-regulation of pathways associated with hypoxia-inducible factor (HIF), which collectively suggest a less angiogenic profile and activation of non-VEGF pathways.
A companion analysis of 35,152 patients treated during a 14-year period found that African American patients with metastatic renal cell carcinoma still had a higher risk of death than white peers in the contemporary era, after introduction of multiple agents that target the VEGF pathway and similar increases in receipt of systemic therapy.
“Our findings indicate clear differences in the biology of clear-cell renal cell carcinoma between African Americans and Caucasians. These differences could suggest a larger proportion of tumors from African Americans have a HIF- and VEGF-independent propensity for aggressiveness, and they also suggest perhaps increased resistance of African Americans to VEGF-targeted therapy,” Dr. Rose said at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
“Overall, our data lend support to a role for tumor biology in the survival disparity observed between African American and Caucasian patients,” she said.
The study may be a step toward precision medicine, whereby race is used to guide treatment decisions, according to invited discussant Dr. Guru Sonpavde, director of the Genitourinary Malignancy Program at the University of Alabama at Birmingham. “That’s an exciting possibility,” he said.
“It is plausible that African American patients are less VEGF driven, less responsive to VEGF inhibitors, but I think the results right now are not ready for use in the clinic,” he further commented. “We need validation in a larger number of African American patients. But even more importantly, we need to focus more on molecular measures of VEGF-driven tumors, to select patients for VEGF inhibitors since we don’t have any biomarkers of this sort in the clinic today.”
“Finally, somatic differences may be driven by differences in the germline, and we may want to focus on integrating the germline and somatic alterations into a molecular panel which might be even better at predicting benefit from specific agents,” he concluded.
Previous studies have found a small but consistent elevation of the risk of death for African American patients with renal cell carcinoma, Dr. Rose noted when introducing the study. Initial hypotheses were that this disparity might be due to differences in comorbidities and use of nephrectomy.
She and her colleagues performed genomic analyses in a discovery cohort of 438 African American and Caucasian patients with metastatic clear-cell renal cell carcinoma from The Cancer Genome Atlas database.
Results indicated that African Americans in this discovery cohort were less likely to have a VHL mutation (17% vs. 50%, P = .036), a finding that was confirmed in a validation cohort of 135 similar patients (40% vs. 81%, P = .008).
African American patients were less likely to have several VEGF and HIF signatures relative to Caucasian counterparts. On the other hand, they were more likely to have the clear cell B molecular subtype (79% vs. 45%, P less than .01), which has been associated with decreased activation of angiogenic pathways and poorer prognosis.
The investigators next analyzed data from the National Cancer Database, assessing survival among 35,152 patients who received a diagnosis of metastatic clear-cell renal cell carcinoma between 1998 and 2011.
The proportion receiving systemic therapy over time was similar for African American and Caucasian patients, with both seeing a rise in 2006, corresponding to the introduction of VEGF-targeted therapies. The poorer median survival for African American versus Caucasian patients seen during 1998-2004 (6.0 vs. 7.6 months; adjusted hazard ratio, 1.07; P less than .01) was still evident in 2006-2011 (6.5 vs. 9.2 months; adjusted hazard ratio, 1.08; P less than .01).
AT THE GENITOURINARY CANCERS SYMPOSIUM
Key clinical point: The poorer survival of African American patients vs. Caucasian patients with clear-cell renal cell carcinoma may be due in part to genomic factors.
Major finding: Compared with Caucasian patients, African American patients were less likely to have mutations of the VHL gene (17% vs. 50%) and more likely to have the clear cell B molecular subtype (79% vs. 45%).
Data source: Analyses of a genomic cohort of 438 patients with metastatic clear-cell renal cell carcinoma from The Cancer Genome Atlas database and a survival cohort of 35,152 from the National Cancer Database.
Disclosures: Dr. Rose disclosed that she had no relevant conflicts of interest. Dr. Sonpavde disclosed that he has a consulting or advisory role with Bayer, Genentech, Merck, Novartis, Pfizer, and Sanofi, and that his institution receives research funding from Bayer, Boehringer Ingelheim, and Onyx.
Combination of celecoxib, zoledronic acid benefits some with hormone-sensitive prostate cancer
SAN FRANCISCO – Men with metastatic hormone-naive prostate cancer have better outcomes when given the nonsteroidal anti-inflammatory drug celecoxib and the bisphosphonate zoledronic acid in addition to standard therapy, according to data from the randomized STAMPEDE trial.
The 1,245 men treated on three trial arms had high-risk locally advanced or metastatic prostate cancer and had not previously received any hormone therapy.
Prespecified analyses showed that when added to standard of care (androgen deprivation therapy and, optionally, radiation therapy), neither celecoxib alone nor the combination of celecoxib and zoledronic acid improved outcomes in the entire trial population, Dr. Nicholas D. James reported at the 2016 Genitourinary Cancers Symposium sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology. But among men who had metastases at baseline, the combination reduced the risk of failure-free survival events by 23% and the risk of death by 24%.
“At the very least, we feel that this data merits further evaluation, particularly as these drugs are widely used and widely available,” commented Dr. James, director of the cancer research unit at the University of Warwick, Coventry, England.
The findings help provide a big picture when viewed together with those from previously reported STAMPEDE trial arms that tested addition of docetaxel (found effective) and of zoledronic acid alone (found ineffective), he noted (Lancet. 2015 Dec 21).
“It does look as though there is a possibility of [a] synergistic or an additive effect here” of celecoxib and zoledronic acid in the patients with metastases, he said. Also, the magnitude of benefit with the combination was similar to that of docetaxel when it came to overall survival, albeit somewhat less when it came to failure-free survival.
Invited discussant Dr. A. Oliver Sartor, the Laborde Professor for Cancer Research and medical director at the Tulane Cancer Center in New Orleans, commented, “We now know from a number of studies that docetaxel and ADT [androgen deprivation therapy] prolong survival, and I believe it should be the standard of care for ‘chemo-fit’ patients with metastatic hormone-sensitive disease.”
Implications of the new findings are unclear, he said. “Neither zoledronic acid nor celecoxib is standard of care today within these hormone-sensitive patients, and I just suspect this combination is unlikely to become standard of care going forward.” In particular, celecoxib has a black box warning for cardiovascular events, which makes its use problematic in the litigious U.S. environment.
At the end of the day, there are likely higher-priority research questions to be addressed in hormone-sensitive disease, according to Dr. Sartor. “Abiraterone, enzalutamide, and radium all need testing,” he said. “And from a global perspective, this disease state is incredibly important. North America and Western Europe are not really the center of the universe. There are lots of people out there who get diagnosed with hormone-sensitive metastatic disease, and they need better therapies than ADT, which is the standard worldwide.”
Giving some background to the research, Dr. James explained that zoledronic acid (Zometa) was chosen because it is known to reduce skeletal-related events in men with bone metastases of castration-refractory disease and was being studied for prevention of metastases. Celecoxib (Celebrex) was chosen in part because it inhibits cyclo-oxygenase-2 (COX-2), which is associated with tumor growth and invasiveness, along with epidemiologic data linking use of nonsteroidal anti-inflammatory drugs with lower prostate cancer risk.
The new analyses were based on 622 men who received only standard of care, 312 who additionally received celecoxib, and 311 who additionally received celecoxib plus zoledronic acid. Overall, 61% had metastases at baseline.
With a median follow-up of 63 months, 55% of men were alive, 36% had died of prostate cancer, and 9% had died of other causes, Dr. James reported.
The addition of celecoxib alone did not improve failure-free survival or overall survival, compared with standard of care alone, either in the whole trial population or in the subgroups with and without metastases.
And the addition of both celecoxib and zoledronic acid did not improve either outcome in the entire trial population overall. But here, there were interaction trends according to the presence of metastases.
Patients with metastases who received celecoxib and zoledronic acid had reductions in the risks of failure-free survival events (hazard ratio, 0.77; P = .008) and overall survival events (hazard ratio, 0.78; P = .04) relative to peers who received standard of care alone. In contrast, patients without metastases did not benefit.
Adverse events of grades 3-5 occurred in about one-third of patients in each treatment arm, with no significant differences in incidence. “In particular, for cardiac disorders, there is no evidence of cardiac toxicity,” Dr. James noted. “But we had excluded patients with a significant history of MIs, heart failure, and so on, so these are patients with a good cardiovascular status going into the trial.”
In terms of salvage therapies, the three arms were essentially the same with respect to the time to first subsequent therapy post progression and the time to first life-prolonging therapy. And among the patients receiving life-prolonging therapies, there was similar exposure to various agents, such as docetaxel and abiraterone.
Dr. James and Dr. Sartor disclosed that they receive honoraria and/or have consulting or advisory roles with numerous pharmaceutical companies.
SAN FRANCISCO – Men with metastatic hormone-naive prostate cancer have better outcomes when given the nonsteroidal anti-inflammatory drug celecoxib and the bisphosphonate zoledronic acid in addition to standard therapy, according to data from the randomized STAMPEDE trial.
The 1,245 men treated on three trial arms had high-risk locally advanced or metastatic prostate cancer and had not previously received any hormone therapy.
Prespecified analyses showed that when added to standard of care (androgen deprivation therapy and, optionally, radiation therapy), neither celecoxib alone nor the combination of celecoxib and zoledronic acid improved outcomes in the entire trial population, Dr. Nicholas D. James reported at the 2016 Genitourinary Cancers Symposium sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology. But among men who had metastases at baseline, the combination reduced the risk of failure-free survival events by 23% and the risk of death by 24%.
“At the very least, we feel that this data merits further evaluation, particularly as these drugs are widely used and widely available,” commented Dr. James, director of the cancer research unit at the University of Warwick, Coventry, England.
The findings help provide a big picture when viewed together with those from previously reported STAMPEDE trial arms that tested addition of docetaxel (found effective) and of zoledronic acid alone (found ineffective), he noted (Lancet. 2015 Dec 21).
“It does look as though there is a possibility of [a] synergistic or an additive effect here” of celecoxib and zoledronic acid in the patients with metastases, he said. Also, the magnitude of benefit with the combination was similar to that of docetaxel when it came to overall survival, albeit somewhat less when it came to failure-free survival.
Invited discussant Dr. A. Oliver Sartor, the Laborde Professor for Cancer Research and medical director at the Tulane Cancer Center in New Orleans, commented, “We now know from a number of studies that docetaxel and ADT [androgen deprivation therapy] prolong survival, and I believe it should be the standard of care for ‘chemo-fit’ patients with metastatic hormone-sensitive disease.”
Implications of the new findings are unclear, he said. “Neither zoledronic acid nor celecoxib is standard of care today within these hormone-sensitive patients, and I just suspect this combination is unlikely to become standard of care going forward.” In particular, celecoxib has a black box warning for cardiovascular events, which makes its use problematic in the litigious U.S. environment.
At the end of the day, there are likely higher-priority research questions to be addressed in hormone-sensitive disease, according to Dr. Sartor. “Abiraterone, enzalutamide, and radium all need testing,” he said. “And from a global perspective, this disease state is incredibly important. North America and Western Europe are not really the center of the universe. There are lots of people out there who get diagnosed with hormone-sensitive metastatic disease, and they need better therapies than ADT, which is the standard worldwide.”
Giving some background to the research, Dr. James explained that zoledronic acid (Zometa) was chosen because it is known to reduce skeletal-related events in men with bone metastases of castration-refractory disease and was being studied for prevention of metastases. Celecoxib (Celebrex) was chosen in part because it inhibits cyclo-oxygenase-2 (COX-2), which is associated with tumor growth and invasiveness, along with epidemiologic data linking use of nonsteroidal anti-inflammatory drugs with lower prostate cancer risk.
The new analyses were based on 622 men who received only standard of care, 312 who additionally received celecoxib, and 311 who additionally received celecoxib plus zoledronic acid. Overall, 61% had metastases at baseline.
With a median follow-up of 63 months, 55% of men were alive, 36% had died of prostate cancer, and 9% had died of other causes, Dr. James reported.
The addition of celecoxib alone did not improve failure-free survival or overall survival, compared with standard of care alone, either in the whole trial population or in the subgroups with and without metastases.
And the addition of both celecoxib and zoledronic acid did not improve either outcome in the entire trial population overall. But here, there were interaction trends according to the presence of metastases.
Patients with metastases who received celecoxib and zoledronic acid had reductions in the risks of failure-free survival events (hazard ratio, 0.77; P = .008) and overall survival events (hazard ratio, 0.78; P = .04) relative to peers who received standard of care alone. In contrast, patients without metastases did not benefit.
Adverse events of grades 3-5 occurred in about one-third of patients in each treatment arm, with no significant differences in incidence. “In particular, for cardiac disorders, there is no evidence of cardiac toxicity,” Dr. James noted. “But we had excluded patients with a significant history of MIs, heart failure, and so on, so these are patients with a good cardiovascular status going into the trial.”
In terms of salvage therapies, the three arms were essentially the same with respect to the time to first subsequent therapy post progression and the time to first life-prolonging therapy. And among the patients receiving life-prolonging therapies, there was similar exposure to various agents, such as docetaxel and abiraterone.
Dr. James and Dr. Sartor disclosed that they receive honoraria and/or have consulting or advisory roles with numerous pharmaceutical companies.
SAN FRANCISCO – Men with metastatic hormone-naive prostate cancer have better outcomes when given the nonsteroidal anti-inflammatory drug celecoxib and the bisphosphonate zoledronic acid in addition to standard therapy, according to data from the randomized STAMPEDE trial.
The 1,245 men treated on three trial arms had high-risk locally advanced or metastatic prostate cancer and had not previously received any hormone therapy.
Prespecified analyses showed that when added to standard of care (androgen deprivation therapy and, optionally, radiation therapy), neither celecoxib alone nor the combination of celecoxib and zoledronic acid improved outcomes in the entire trial population, Dr. Nicholas D. James reported at the 2016 Genitourinary Cancers Symposium sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology. But among men who had metastases at baseline, the combination reduced the risk of failure-free survival events by 23% and the risk of death by 24%.
“At the very least, we feel that this data merits further evaluation, particularly as these drugs are widely used and widely available,” commented Dr. James, director of the cancer research unit at the University of Warwick, Coventry, England.
The findings help provide a big picture when viewed together with those from previously reported STAMPEDE trial arms that tested addition of docetaxel (found effective) and of zoledronic acid alone (found ineffective), he noted (Lancet. 2015 Dec 21).
“It does look as though there is a possibility of [a] synergistic or an additive effect here” of celecoxib and zoledronic acid in the patients with metastases, he said. Also, the magnitude of benefit with the combination was similar to that of docetaxel when it came to overall survival, albeit somewhat less when it came to failure-free survival.
Invited discussant Dr. A. Oliver Sartor, the Laborde Professor for Cancer Research and medical director at the Tulane Cancer Center in New Orleans, commented, “We now know from a number of studies that docetaxel and ADT [androgen deprivation therapy] prolong survival, and I believe it should be the standard of care for ‘chemo-fit’ patients with metastatic hormone-sensitive disease.”
Implications of the new findings are unclear, he said. “Neither zoledronic acid nor celecoxib is standard of care today within these hormone-sensitive patients, and I just suspect this combination is unlikely to become standard of care going forward.” In particular, celecoxib has a black box warning for cardiovascular events, which makes its use problematic in the litigious U.S. environment.
At the end of the day, there are likely higher-priority research questions to be addressed in hormone-sensitive disease, according to Dr. Sartor. “Abiraterone, enzalutamide, and radium all need testing,” he said. “And from a global perspective, this disease state is incredibly important. North America and Western Europe are not really the center of the universe. There are lots of people out there who get diagnosed with hormone-sensitive metastatic disease, and they need better therapies than ADT, which is the standard worldwide.”
Giving some background to the research, Dr. James explained that zoledronic acid (Zometa) was chosen because it is known to reduce skeletal-related events in men with bone metastases of castration-refractory disease and was being studied for prevention of metastases. Celecoxib (Celebrex) was chosen in part because it inhibits cyclo-oxygenase-2 (COX-2), which is associated with tumor growth and invasiveness, along with epidemiologic data linking use of nonsteroidal anti-inflammatory drugs with lower prostate cancer risk.
The new analyses were based on 622 men who received only standard of care, 312 who additionally received celecoxib, and 311 who additionally received celecoxib plus zoledronic acid. Overall, 61% had metastases at baseline.
With a median follow-up of 63 months, 55% of men were alive, 36% had died of prostate cancer, and 9% had died of other causes, Dr. James reported.
The addition of celecoxib alone did not improve failure-free survival or overall survival, compared with standard of care alone, either in the whole trial population or in the subgroups with and without metastases.
And the addition of both celecoxib and zoledronic acid did not improve either outcome in the entire trial population overall. But here, there were interaction trends according to the presence of metastases.
Patients with metastases who received celecoxib and zoledronic acid had reductions in the risks of failure-free survival events (hazard ratio, 0.77; P = .008) and overall survival events (hazard ratio, 0.78; P = .04) relative to peers who received standard of care alone. In contrast, patients without metastases did not benefit.
Adverse events of grades 3-5 occurred in about one-third of patients in each treatment arm, with no significant differences in incidence. “In particular, for cardiac disorders, there is no evidence of cardiac toxicity,” Dr. James noted. “But we had excluded patients with a significant history of MIs, heart failure, and so on, so these are patients with a good cardiovascular status going into the trial.”
In terms of salvage therapies, the three arms were essentially the same with respect to the time to first subsequent therapy post progression and the time to first life-prolonging therapy. And among the patients receiving life-prolonging therapies, there was similar exposure to various agents, such as docetaxel and abiraterone.
Dr. James and Dr. Sartor disclosed that they receive honoraria and/or have consulting or advisory roles with numerous pharmaceutical companies.
AT THE GENITOURINARY CANCERS SYMPOSIUM
Key clinical point: Adding celecoxib and zoledronic acid to standard of care improves outcomes in men with metastatic hormone-naive prostate cancer.
Major finding: Men with metastases had better failure-free survival (hazard ratio, 0.77) and overall survival (hazard ratio, 0.76) when celecoxib and zoledronic acid were added to standard of care.
Data source: An analysis of 1,245 men with hormone-naive prostate cancer treated on three arms of a multiarm, multistage randomized controlled trial (STAMPEDE).
Disclosures: Dr. James and Dr. Sartor disclosed that they receive honoraria and/or have consulting or advisory roles with several pharmaceutical companies.
Atezolizumab generates excitement in advanced urothelial cancer
SAN FRANCISCO – The immune checkpoint inhibitor atezolizumab is highly active and well tolerated in patients with platinum-treated advanced urothelial carcinoma and may in fact change management of this disease, according to a phase II trial reported at the 2016 Genitourinary Cancers Symposium.
The trial, IMvigor 210, was conducted in Europe, Canada, and the United States among patients who had locally advanced or metastatic urothelial carcinoma. Lead investigator Dr. Jean H. Hoffman-Censits reported findings for the trial’s second cohort, which enrolled 310 patients who had had progression on or after platinum-based chemotherapy, with no limit on the number of lines of prior therapy.
At 3-week intervals, the patients received atezolizumab, an investigational antibody that targets programmed death–ligand 1 (PD-L1), preventing it from binding to the programmed death–1 (PD-1) receptor on T cells and thereby enhancing their activity, Dr. Hoffman-Censits reported at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
The overall response rate was 15% in the entire cohort and 26% in the subset of patients whose immune cells had high expression of PD-L1 by immunohistochemistry. Values in all prespecified groups exceeded the bar of 10% that the investigators had selected on the basis of second-line trials, even though many patients in IMvigor were being treated in later lines.
Atezolizumab was well tolerated. Overall, 16% of patients experienced grade 3 or 4 treatment-related adverse events; only 4% of patients stopping treatment because of such events, reported Dr. Hoffman-Censits of the Kimmel Cancer Center, Thomas Jefferson University Hospital in Philadelphia.
“Given the current landscape of chemotherapy options for our patients with urothelial cancer progressing following platinum chemotherapy, this primary analysis of IMvigor 210 demonstrates that atezolizumab has the potential to change the standard of care for metastatic urothelial cancers,” Dr. Hoffman-Censits maintained. “Higher PD-L1 [immune cell] status was associated with higher response rates, but low PD-L1 status or poor prognostic factors did not preclude responses,” she noted.
A pair of ongoing randomized phase III trials are testing atezolizumab in metastatic urothelial carcinoma and as adjuvant therapy in muscle-invasive bladder cancer. Also, there is now an expanded-access trial for patients with platinum-treated metastatic urothelial carcinoma.
“We look forward to the results of these trials, which will continue to define the role of atezolizumab in the treatment of patients with urothelial cancers,” she concluded.
Invited discussant Dr. William Y. Kim of the Lineberger Comprehensive Cancer Center, University of North Carolina, in Chapel Hill, noted that patients given immunotherapies such as atezolizumab can experience both pseudoprogression and delayed response, which may be misclassified with the RECIST criteria used in the trial. However, it is not yet clear whether immune-related response criteria will be useful in urothelial cancers.
“In IMvigor 210, we anxiously await the results of cohort one,” he said, referring to a separate group of patients who were not eligible for platinum chemotherapy. “Follow-up regarding the durability of these responses will be needed as well.”
Atezolizumab’s mechanism of action is attractive in urothelial cancer, Dr. Hoffman-Censits noted when introducing the trial.
“By inhibiting binding of PD-L1 to PD-1 and B7.1, atezolizumab can enhance T-cell priming and reinvigorate suppressed immune cells,” she explained. “However, by leaving the interaction between PD-L2 and PD-1 intact, atezolizumab can preserve peripheral immune homeostasis. Urothelial cancers have a high mutation burden, which potentially can lead to neoantigen formation, and those [new antigens] could be recognized by the immune system.”
Three-fourths of the 310 patients studied had bladder cancer. A total of 41% had previously received two or more therapies for metastatic disease.
Immunohistochemistry showed high PD-L1 staining of immune cells (5% or more positive) in 32% of patients, intermediate staining (between 1% and 5% positive) in 35%, and low staining (less than 1% positive) in 33%.
The overall response rate according to RECIST criteria with central review was 15% in the entire cohort, 18% in patients with intermediate or high PD-L1 staining, and 26% in patients with high PD-L1 staining.
“Surprisingly, complete responses were seen in this group,” Dr. Hoffman-Censits commented. “This is a phenomenon that is incredibly rare in second-line and beyond clinical trials.”
The rate of complete response was 5% in the entire cohort, 6% in patients with intermediate or high PD-L1 staining, and 11% in patients with high PD-L1 staining. Of note, some complete responses were seen even in those with low staining.
With a median follow-up of 11.7 months, the median duration of response had not been reached; fully 84% of patients who initially had a response still had an ongoing response at the time of data cutoff. Stable disease was likewise durable.
When patients were stratified by prognostic factors, the overall response rate was highest, at 23%, among those with lymph nodes as the only site of metastases.
Median progression-free survival was 2.1 months in the entire cohort and also regardless of PD-L1 staining. Median overall survival was 7.9 months in the entire cohort; it was longer for patients with high staining (11.4 months) than for peers with intermediate or low staining (6.7 months).
The 12-month overall survival rate was 36% for the entire cohort, 30% for patients with low or intermediate staining, and 48% for patients with high staining.
“Considering 12-month overall survival estimates for second-line chemo are approximately 20%, these data are truly exciting,” Dr. Hoffman-Censits said.
Analysis of adverse events showed that atezolizumab had a favorable safety profile. In particular, there were no immune-mediated adverse events deemed to be related to treatment.
SAN FRANCISCO – The immune checkpoint inhibitor atezolizumab is highly active and well tolerated in patients with platinum-treated advanced urothelial carcinoma and may in fact change management of this disease, according to a phase II trial reported at the 2016 Genitourinary Cancers Symposium.
The trial, IMvigor 210, was conducted in Europe, Canada, and the United States among patients who had locally advanced or metastatic urothelial carcinoma. Lead investigator Dr. Jean H. Hoffman-Censits reported findings for the trial’s second cohort, which enrolled 310 patients who had had progression on or after platinum-based chemotherapy, with no limit on the number of lines of prior therapy.
At 3-week intervals, the patients received atezolizumab, an investigational antibody that targets programmed death–ligand 1 (PD-L1), preventing it from binding to the programmed death–1 (PD-1) receptor on T cells and thereby enhancing their activity, Dr. Hoffman-Censits reported at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
The overall response rate was 15% in the entire cohort and 26% in the subset of patients whose immune cells had high expression of PD-L1 by immunohistochemistry. Values in all prespecified groups exceeded the bar of 10% that the investigators had selected on the basis of second-line trials, even though many patients in IMvigor were being treated in later lines.
Atezolizumab was well tolerated. Overall, 16% of patients experienced grade 3 or 4 treatment-related adverse events; only 4% of patients stopping treatment because of such events, reported Dr. Hoffman-Censits of the Kimmel Cancer Center, Thomas Jefferson University Hospital in Philadelphia.
“Given the current landscape of chemotherapy options for our patients with urothelial cancer progressing following platinum chemotherapy, this primary analysis of IMvigor 210 demonstrates that atezolizumab has the potential to change the standard of care for metastatic urothelial cancers,” Dr. Hoffman-Censits maintained. “Higher PD-L1 [immune cell] status was associated with higher response rates, but low PD-L1 status or poor prognostic factors did not preclude responses,” she noted.
A pair of ongoing randomized phase III trials are testing atezolizumab in metastatic urothelial carcinoma and as adjuvant therapy in muscle-invasive bladder cancer. Also, there is now an expanded-access trial for patients with platinum-treated metastatic urothelial carcinoma.
“We look forward to the results of these trials, which will continue to define the role of atezolizumab in the treatment of patients with urothelial cancers,” she concluded.
Invited discussant Dr. William Y. Kim of the Lineberger Comprehensive Cancer Center, University of North Carolina, in Chapel Hill, noted that patients given immunotherapies such as atezolizumab can experience both pseudoprogression and delayed response, which may be misclassified with the RECIST criteria used in the trial. However, it is not yet clear whether immune-related response criteria will be useful in urothelial cancers.
“In IMvigor 210, we anxiously await the results of cohort one,” he said, referring to a separate group of patients who were not eligible for platinum chemotherapy. “Follow-up regarding the durability of these responses will be needed as well.”
Atezolizumab’s mechanism of action is attractive in urothelial cancer, Dr. Hoffman-Censits noted when introducing the trial.
“By inhibiting binding of PD-L1 to PD-1 and B7.1, atezolizumab can enhance T-cell priming and reinvigorate suppressed immune cells,” she explained. “However, by leaving the interaction between PD-L2 and PD-1 intact, atezolizumab can preserve peripheral immune homeostasis. Urothelial cancers have a high mutation burden, which potentially can lead to neoantigen formation, and those [new antigens] could be recognized by the immune system.”
Three-fourths of the 310 patients studied had bladder cancer. A total of 41% had previously received two or more therapies for metastatic disease.
Immunohistochemistry showed high PD-L1 staining of immune cells (5% or more positive) in 32% of patients, intermediate staining (between 1% and 5% positive) in 35%, and low staining (less than 1% positive) in 33%.
The overall response rate according to RECIST criteria with central review was 15% in the entire cohort, 18% in patients with intermediate or high PD-L1 staining, and 26% in patients with high PD-L1 staining.
“Surprisingly, complete responses were seen in this group,” Dr. Hoffman-Censits commented. “This is a phenomenon that is incredibly rare in second-line and beyond clinical trials.”
The rate of complete response was 5% in the entire cohort, 6% in patients with intermediate or high PD-L1 staining, and 11% in patients with high PD-L1 staining. Of note, some complete responses were seen even in those with low staining.
With a median follow-up of 11.7 months, the median duration of response had not been reached; fully 84% of patients who initially had a response still had an ongoing response at the time of data cutoff. Stable disease was likewise durable.
When patients were stratified by prognostic factors, the overall response rate was highest, at 23%, among those with lymph nodes as the only site of metastases.
Median progression-free survival was 2.1 months in the entire cohort and also regardless of PD-L1 staining. Median overall survival was 7.9 months in the entire cohort; it was longer for patients with high staining (11.4 months) than for peers with intermediate or low staining (6.7 months).
The 12-month overall survival rate was 36% for the entire cohort, 30% for patients with low or intermediate staining, and 48% for patients with high staining.
“Considering 12-month overall survival estimates for second-line chemo are approximately 20%, these data are truly exciting,” Dr. Hoffman-Censits said.
Analysis of adverse events showed that atezolizumab had a favorable safety profile. In particular, there were no immune-mediated adverse events deemed to be related to treatment.
SAN FRANCISCO – The immune checkpoint inhibitor atezolizumab is highly active and well tolerated in patients with platinum-treated advanced urothelial carcinoma and may in fact change management of this disease, according to a phase II trial reported at the 2016 Genitourinary Cancers Symposium.
The trial, IMvigor 210, was conducted in Europe, Canada, and the United States among patients who had locally advanced or metastatic urothelial carcinoma. Lead investigator Dr. Jean H. Hoffman-Censits reported findings for the trial’s second cohort, which enrolled 310 patients who had had progression on or after platinum-based chemotherapy, with no limit on the number of lines of prior therapy.
At 3-week intervals, the patients received atezolizumab, an investigational antibody that targets programmed death–ligand 1 (PD-L1), preventing it from binding to the programmed death–1 (PD-1) receptor on T cells and thereby enhancing their activity, Dr. Hoffman-Censits reported at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
The overall response rate was 15% in the entire cohort and 26% in the subset of patients whose immune cells had high expression of PD-L1 by immunohistochemistry. Values in all prespecified groups exceeded the bar of 10% that the investigators had selected on the basis of second-line trials, even though many patients in IMvigor were being treated in later lines.
Atezolizumab was well tolerated. Overall, 16% of patients experienced grade 3 or 4 treatment-related adverse events; only 4% of patients stopping treatment because of such events, reported Dr. Hoffman-Censits of the Kimmel Cancer Center, Thomas Jefferson University Hospital in Philadelphia.
“Given the current landscape of chemotherapy options for our patients with urothelial cancer progressing following platinum chemotherapy, this primary analysis of IMvigor 210 demonstrates that atezolizumab has the potential to change the standard of care for metastatic urothelial cancers,” Dr. Hoffman-Censits maintained. “Higher PD-L1 [immune cell] status was associated with higher response rates, but low PD-L1 status or poor prognostic factors did not preclude responses,” she noted.
A pair of ongoing randomized phase III trials are testing atezolizumab in metastatic urothelial carcinoma and as adjuvant therapy in muscle-invasive bladder cancer. Also, there is now an expanded-access trial for patients with platinum-treated metastatic urothelial carcinoma.
“We look forward to the results of these trials, which will continue to define the role of atezolizumab in the treatment of patients with urothelial cancers,” she concluded.
Invited discussant Dr. William Y. Kim of the Lineberger Comprehensive Cancer Center, University of North Carolina, in Chapel Hill, noted that patients given immunotherapies such as atezolizumab can experience both pseudoprogression and delayed response, which may be misclassified with the RECIST criteria used in the trial. However, it is not yet clear whether immune-related response criteria will be useful in urothelial cancers.
“In IMvigor 210, we anxiously await the results of cohort one,” he said, referring to a separate group of patients who were not eligible for platinum chemotherapy. “Follow-up regarding the durability of these responses will be needed as well.”
Atezolizumab’s mechanism of action is attractive in urothelial cancer, Dr. Hoffman-Censits noted when introducing the trial.
“By inhibiting binding of PD-L1 to PD-1 and B7.1, atezolizumab can enhance T-cell priming and reinvigorate suppressed immune cells,” she explained. “However, by leaving the interaction between PD-L2 and PD-1 intact, atezolizumab can preserve peripheral immune homeostasis. Urothelial cancers have a high mutation burden, which potentially can lead to neoantigen formation, and those [new antigens] could be recognized by the immune system.”
Three-fourths of the 310 patients studied had bladder cancer. A total of 41% had previously received two or more therapies for metastatic disease.
Immunohistochemistry showed high PD-L1 staining of immune cells (5% or more positive) in 32% of patients, intermediate staining (between 1% and 5% positive) in 35%, and low staining (less than 1% positive) in 33%.
The overall response rate according to RECIST criteria with central review was 15% in the entire cohort, 18% in patients with intermediate or high PD-L1 staining, and 26% in patients with high PD-L1 staining.
“Surprisingly, complete responses were seen in this group,” Dr. Hoffman-Censits commented. “This is a phenomenon that is incredibly rare in second-line and beyond clinical trials.”
The rate of complete response was 5% in the entire cohort, 6% in patients with intermediate or high PD-L1 staining, and 11% in patients with high PD-L1 staining. Of note, some complete responses were seen even in those with low staining.
With a median follow-up of 11.7 months, the median duration of response had not been reached; fully 84% of patients who initially had a response still had an ongoing response at the time of data cutoff. Stable disease was likewise durable.
When patients were stratified by prognostic factors, the overall response rate was highest, at 23%, among those with lymph nodes as the only site of metastases.
Median progression-free survival was 2.1 months in the entire cohort and also regardless of PD-L1 staining. Median overall survival was 7.9 months in the entire cohort; it was longer for patients with high staining (11.4 months) than for peers with intermediate or low staining (6.7 months).
The 12-month overall survival rate was 36% for the entire cohort, 30% for patients with low or intermediate staining, and 48% for patients with high staining.
“Considering 12-month overall survival estimates for second-line chemo are approximately 20%, these data are truly exciting,” Dr. Hoffman-Censits said.
Analysis of adverse events showed that atezolizumab had a favorable safety profile. In particular, there were no immune-mediated adverse events deemed to be related to treatment.
AT THE GENITOURINARY CANCERS SYMPOSIUM
Key clinical point: Atezolizumab is active in advanced urothelial cancer, especially in patients whose immune cells have higher expression of PD-L1.
Major finding: The overall response rate was 15% in the entire cohort and 26% in the subset with high PD-L1 staining. The rate of grade 3 or 4 treatment-related adverse events was 16%.
Data source: An analysis of 310 patients with platinum-treated locally advanced or metastatic urothelial carcinoma on a phase II trial (IMvigor 210 trial).
Disclosures: Dr. Hoffman-Censits disclosed that she receives honoraria from and has a consulting or advisory role with Roche/Genentech, and receives research funding from Sanofi. The study was funded by F. Hoffman-LaRoche. Dr. Kim disclosed that he owns stock in Agios, Bristol-Myers Squibb, Johnson & Johnson, Medivation, and Merck, and that he has a patent for the BASE47 bladder cancer subtype classifier.
Nivolumab has survival benefit across diverse RCC patient subgroups
SAN FRANCISCO – The immune checkpoint inhibitor nivolumab has a consistent survival benefit over everolimus among diverse patients with previously treated advanced clear-cell renal cell carcinoma, finds a subgroup analysis of the CheckMate 025 trial reported at the 2016 Genitourinary Cancers Symposium.
Patients in the open-label phase III trial had received one or two prior anti-angiogenic therapies, usually one of the tyrosine kinase inhibitors that target signaling through the vascular endothelial growth factor receptor.
In all, 821 patients were randomized to nivolumab (Opdivo), an antibody to the cell surface receptor programmed death 1 (PD-1), or everolimus (Afinitor), an inhibitor of the mammalian target of rapamycin that is considered a standard of care in this setting.
Previously reported results showed that the trial met its primary endpoint, with an overall survival favoring nivolumab among the entire trial population (hazard ratio, 0.73; P = .0018) (N Engl J Med. 2015;373:1803-13), ultimately resulting in FDA approval of the drug. Nivolumab also yielded a better response rate, fewer grade 3 and 4 adverse events, and improved quality of life.
Findings of the new subgroup analysis showed that compared with everolimus, nivolumab was associated with a roughly 20%-50% reduced risk of death across patients stratified by disease characteristics and prior therapies, reported lead author Dr. Robert J. Motzer of Memorial Sloan Kettering Cancer Center, New York.
“Consistent with the benefit observed in the overall population of CheckMate 025, nivolumab demonstrated an overall survival and objective response benefit across all key subgroups we examined … Nivolumab is a new standard of care for patients with advanced renal cell carcinoma who have received prior anti-angiogenic therapy, and we think it’s a good choice as a second-line agent,” he said at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
In the same session, investigators reported findings of a subgroup analysis of the METEOR trial, which compared cabozantinib (Cometriq), an oral multitargeted tyrosine kinase inhibitor, with everolimus in a similar patient population. Those data were much the same, showing a consistent progression-free survival benefit of cabozantinib across subgroups.
Weighing results of the two trials, session chair Dr. Toni K. Choueiri, director of the Kidney Cancer Center at the Dana-Farber Cancer Institute, Boston, asked, “For patients who progress on a first-line VEGFR TKI, let’s say sunitinib, is your agent of choice nivolumab or cabozantinib?”
“My treatment of choice in that patient would be nivolumab, [because of] the survival benefit, the tolerability, the durability of responses that we see when the responses do occur,” Dr. Motzer replied. “I also am attracted by a change in mechanism. A change in mechanism of action to a different type of drug is what I prefer.”
This choice would remain the same even if the METEOR trial eventually shows an overall survival benefit of cabozantinib, he added.
“Obviously, we have a number of different options here. I don’t think that there is any one right answer … Neither of these drugs has been compared to the other. Neither of them has been compared to axitinib. So it’s really an individual decision. It’s going to be a patient’s decision. It’s going to be a physician’s decision,” he said. “Hopefully, as we get more experience, more data, more trials, we’ll have more evidence to base our decision on.”
A session attendee asked, “Where do we go from here? What will the approval of cabozantinib and the use of cabozantinib mean for the development of the combination of everolimus and lenvatinib, which we’ve been working on?”
“We have a number of drugs that are coming into the armamentarium that are hopefully going to get approved. Nivolumab has been approved. Cabozantinib I anticipate will be approved. I don’t know about lenvatinib –we’ll have to see,” Dr. Motzer said, adding that axitinib is also in the mix.
“We would need some comparative trials. For lenvatinib, what we’d like to see is that going into the first-line setting perhaps combined with a checkpoint inhibitor. We are currently doing a study at our center with lenvatinib and pembrolizumab. I think that will be a great combination,” he added. “So you’re right, it’s a time where suddenly this year, we may have three new drugs for kidney cancer, and we need to sort that out. We have lots of good options for our patients now.”
Results of the CheckMate 025 subgroup analysis showed a lower risk of death with nivolumab compared with everolimus among patients whether their Memorial Sloan Kettering Cancer Center (MSKCC) risk score was favorable (hazard ratio, 0.80), intermediate (hazard ratio, 0.81), or poor (hazard ratio, 0.48).
Benefit was consistent in patients with bone metastases (hazard ratio, 0.72) and liver metastases (hazard ratio, 0.81).
Nivolumab was likewise superior to everolimus in the roughly 60% of patients who had previously received sunitinib (hazard ratio, 0.81) and in the roughly 30% who had previously received pazopanib (hazard ratio, 0.60).
And benefit was essentially the same whether patients had been on first-line therapy for less than 6 months, a poor prognostic marker (hazard ratio, 0.76), or for longer than that (hazard ratio, 0.78).
There was also an overall survival advantage in favor of nivolumab when patients were stratified by International Metastatic Renal Cell Carcinoma Database Consortium (IMDC) risk score, number of sites of metastases, and number of prior anti-angiogenic therapies.
The previously published results showed an advantage in favor of nivolumab regardless of programmed death–ligand 1 (PD-L1) expression, Dr. Motzer noted.
The benefit in terms of overall response rate was also consistently in favor of nivolumab over everolimus across these diverse patient subgroups.
Dr. Motzer disclosed that he has a consulting or advisory role with Eisai, Novartis, and Pfizer; that he receives travel expenses from Bristol-Myers Squibb; and that his institution receives research funding from Bristol-Myers Squibb, Eisai, Genentech/Roche, GlaxoSmithKline, Novartis, and Pfizer. The trial was sponsored in part by Bristol-Myers Squibb in collaboration with Ono Pharmaceutical Co. Ltd.
SAN FRANCISCO – The immune checkpoint inhibitor nivolumab has a consistent survival benefit over everolimus among diverse patients with previously treated advanced clear-cell renal cell carcinoma, finds a subgroup analysis of the CheckMate 025 trial reported at the 2016 Genitourinary Cancers Symposium.
Patients in the open-label phase III trial had received one or two prior anti-angiogenic therapies, usually one of the tyrosine kinase inhibitors that target signaling through the vascular endothelial growth factor receptor.
In all, 821 patients were randomized to nivolumab (Opdivo), an antibody to the cell surface receptor programmed death 1 (PD-1), or everolimus (Afinitor), an inhibitor of the mammalian target of rapamycin that is considered a standard of care in this setting.
Previously reported results showed that the trial met its primary endpoint, with an overall survival favoring nivolumab among the entire trial population (hazard ratio, 0.73; P = .0018) (N Engl J Med. 2015;373:1803-13), ultimately resulting in FDA approval of the drug. Nivolumab also yielded a better response rate, fewer grade 3 and 4 adverse events, and improved quality of life.
Findings of the new subgroup analysis showed that compared with everolimus, nivolumab was associated with a roughly 20%-50% reduced risk of death across patients stratified by disease characteristics and prior therapies, reported lead author Dr. Robert J. Motzer of Memorial Sloan Kettering Cancer Center, New York.
“Consistent with the benefit observed in the overall population of CheckMate 025, nivolumab demonstrated an overall survival and objective response benefit across all key subgroups we examined … Nivolumab is a new standard of care for patients with advanced renal cell carcinoma who have received prior anti-angiogenic therapy, and we think it’s a good choice as a second-line agent,” he said at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
In the same session, investigators reported findings of a subgroup analysis of the METEOR trial, which compared cabozantinib (Cometriq), an oral multitargeted tyrosine kinase inhibitor, with everolimus in a similar patient population. Those data were much the same, showing a consistent progression-free survival benefit of cabozantinib across subgroups.
Weighing results of the two trials, session chair Dr. Toni K. Choueiri, director of the Kidney Cancer Center at the Dana-Farber Cancer Institute, Boston, asked, “For patients who progress on a first-line VEGFR TKI, let’s say sunitinib, is your agent of choice nivolumab or cabozantinib?”
“My treatment of choice in that patient would be nivolumab, [because of] the survival benefit, the tolerability, the durability of responses that we see when the responses do occur,” Dr. Motzer replied. “I also am attracted by a change in mechanism. A change in mechanism of action to a different type of drug is what I prefer.”
This choice would remain the same even if the METEOR trial eventually shows an overall survival benefit of cabozantinib, he added.
“Obviously, we have a number of different options here. I don’t think that there is any one right answer … Neither of these drugs has been compared to the other. Neither of them has been compared to axitinib. So it’s really an individual decision. It’s going to be a patient’s decision. It’s going to be a physician’s decision,” he said. “Hopefully, as we get more experience, more data, more trials, we’ll have more evidence to base our decision on.”
A session attendee asked, “Where do we go from here? What will the approval of cabozantinib and the use of cabozantinib mean for the development of the combination of everolimus and lenvatinib, which we’ve been working on?”
“We have a number of drugs that are coming into the armamentarium that are hopefully going to get approved. Nivolumab has been approved. Cabozantinib I anticipate will be approved. I don’t know about lenvatinib –we’ll have to see,” Dr. Motzer said, adding that axitinib is also in the mix.
“We would need some comparative trials. For lenvatinib, what we’d like to see is that going into the first-line setting perhaps combined with a checkpoint inhibitor. We are currently doing a study at our center with lenvatinib and pembrolizumab. I think that will be a great combination,” he added. “So you’re right, it’s a time where suddenly this year, we may have three new drugs for kidney cancer, and we need to sort that out. We have lots of good options for our patients now.”
Results of the CheckMate 025 subgroup analysis showed a lower risk of death with nivolumab compared with everolimus among patients whether their Memorial Sloan Kettering Cancer Center (MSKCC) risk score was favorable (hazard ratio, 0.80), intermediate (hazard ratio, 0.81), or poor (hazard ratio, 0.48).
Benefit was consistent in patients with bone metastases (hazard ratio, 0.72) and liver metastases (hazard ratio, 0.81).
Nivolumab was likewise superior to everolimus in the roughly 60% of patients who had previously received sunitinib (hazard ratio, 0.81) and in the roughly 30% who had previously received pazopanib (hazard ratio, 0.60).
And benefit was essentially the same whether patients had been on first-line therapy for less than 6 months, a poor prognostic marker (hazard ratio, 0.76), or for longer than that (hazard ratio, 0.78).
There was also an overall survival advantage in favor of nivolumab when patients were stratified by International Metastatic Renal Cell Carcinoma Database Consortium (IMDC) risk score, number of sites of metastases, and number of prior anti-angiogenic therapies.
The previously published results showed an advantage in favor of nivolumab regardless of programmed death–ligand 1 (PD-L1) expression, Dr. Motzer noted.
The benefit in terms of overall response rate was also consistently in favor of nivolumab over everolimus across these diverse patient subgroups.
Dr. Motzer disclosed that he has a consulting or advisory role with Eisai, Novartis, and Pfizer; that he receives travel expenses from Bristol-Myers Squibb; and that his institution receives research funding from Bristol-Myers Squibb, Eisai, Genentech/Roche, GlaxoSmithKline, Novartis, and Pfizer. The trial was sponsored in part by Bristol-Myers Squibb in collaboration with Ono Pharmaceutical Co. Ltd.
SAN FRANCISCO – The immune checkpoint inhibitor nivolumab has a consistent survival benefit over everolimus among diverse patients with previously treated advanced clear-cell renal cell carcinoma, finds a subgroup analysis of the CheckMate 025 trial reported at the 2016 Genitourinary Cancers Symposium.
Patients in the open-label phase III trial had received one or two prior anti-angiogenic therapies, usually one of the tyrosine kinase inhibitors that target signaling through the vascular endothelial growth factor receptor.
In all, 821 patients were randomized to nivolumab (Opdivo), an antibody to the cell surface receptor programmed death 1 (PD-1), or everolimus (Afinitor), an inhibitor of the mammalian target of rapamycin that is considered a standard of care in this setting.
Previously reported results showed that the trial met its primary endpoint, with an overall survival favoring nivolumab among the entire trial population (hazard ratio, 0.73; P = .0018) (N Engl J Med. 2015;373:1803-13), ultimately resulting in FDA approval of the drug. Nivolumab also yielded a better response rate, fewer grade 3 and 4 adverse events, and improved quality of life.
Findings of the new subgroup analysis showed that compared with everolimus, nivolumab was associated with a roughly 20%-50% reduced risk of death across patients stratified by disease characteristics and prior therapies, reported lead author Dr. Robert J. Motzer of Memorial Sloan Kettering Cancer Center, New York.
“Consistent with the benefit observed in the overall population of CheckMate 025, nivolumab demonstrated an overall survival and objective response benefit across all key subgroups we examined … Nivolumab is a new standard of care for patients with advanced renal cell carcinoma who have received prior anti-angiogenic therapy, and we think it’s a good choice as a second-line agent,” he said at the symposium, sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
In the same session, investigators reported findings of a subgroup analysis of the METEOR trial, which compared cabozantinib (Cometriq), an oral multitargeted tyrosine kinase inhibitor, with everolimus in a similar patient population. Those data were much the same, showing a consistent progression-free survival benefit of cabozantinib across subgroups.
Weighing results of the two trials, session chair Dr. Toni K. Choueiri, director of the Kidney Cancer Center at the Dana-Farber Cancer Institute, Boston, asked, “For patients who progress on a first-line VEGFR TKI, let’s say sunitinib, is your agent of choice nivolumab or cabozantinib?”
“My treatment of choice in that patient would be nivolumab, [because of] the survival benefit, the tolerability, the durability of responses that we see when the responses do occur,” Dr. Motzer replied. “I also am attracted by a change in mechanism. A change in mechanism of action to a different type of drug is what I prefer.”
This choice would remain the same even if the METEOR trial eventually shows an overall survival benefit of cabozantinib, he added.
“Obviously, we have a number of different options here. I don’t think that there is any one right answer … Neither of these drugs has been compared to the other. Neither of them has been compared to axitinib. So it’s really an individual decision. It’s going to be a patient’s decision. It’s going to be a physician’s decision,” he said. “Hopefully, as we get more experience, more data, more trials, we’ll have more evidence to base our decision on.”
A session attendee asked, “Where do we go from here? What will the approval of cabozantinib and the use of cabozantinib mean for the development of the combination of everolimus and lenvatinib, which we’ve been working on?”
“We have a number of drugs that are coming into the armamentarium that are hopefully going to get approved. Nivolumab has been approved. Cabozantinib I anticipate will be approved. I don’t know about lenvatinib –we’ll have to see,” Dr. Motzer said, adding that axitinib is also in the mix.
“We would need some comparative trials. For lenvatinib, what we’d like to see is that going into the first-line setting perhaps combined with a checkpoint inhibitor. We are currently doing a study at our center with lenvatinib and pembrolizumab. I think that will be a great combination,” he added. “So you’re right, it’s a time where suddenly this year, we may have three new drugs for kidney cancer, and we need to sort that out. We have lots of good options for our patients now.”
Results of the CheckMate 025 subgroup analysis showed a lower risk of death with nivolumab compared with everolimus among patients whether their Memorial Sloan Kettering Cancer Center (MSKCC) risk score was favorable (hazard ratio, 0.80), intermediate (hazard ratio, 0.81), or poor (hazard ratio, 0.48).
Benefit was consistent in patients with bone metastases (hazard ratio, 0.72) and liver metastases (hazard ratio, 0.81).
Nivolumab was likewise superior to everolimus in the roughly 60% of patients who had previously received sunitinib (hazard ratio, 0.81) and in the roughly 30% who had previously received pazopanib (hazard ratio, 0.60).
And benefit was essentially the same whether patients had been on first-line therapy for less than 6 months, a poor prognostic marker (hazard ratio, 0.76), or for longer than that (hazard ratio, 0.78).
There was also an overall survival advantage in favor of nivolumab when patients were stratified by International Metastatic Renal Cell Carcinoma Database Consortium (IMDC) risk score, number of sites of metastases, and number of prior anti-angiogenic therapies.
The previously published results showed an advantage in favor of nivolumab regardless of programmed death–ligand 1 (PD-L1) expression, Dr. Motzer noted.
The benefit in terms of overall response rate was also consistently in favor of nivolumab over everolimus across these diverse patient subgroups.
Dr. Motzer disclosed that he has a consulting or advisory role with Eisai, Novartis, and Pfizer; that he receives travel expenses from Bristol-Myers Squibb; and that his institution receives research funding from Bristol-Myers Squibb, Eisai, Genentech/Roche, GlaxoSmithKline, Novartis, and Pfizer. The trial was sponsored in part by Bristol-Myers Squibb in collaboration with Ono Pharmaceutical Co. Ltd.
AT THE GENITOURINARY CANCERS SYMPOSIUM
Key clinical point: Nivolumab was superior to everolimus regardless of disease characteristics and prior therapies.
Major finding: All subgroups had a reduced risk of death, ranging from roughly 20% to 50%, with nivolumab versus everolimus.
Data source: A subgroup analysis of a randomized phase III trial of 821 patients with pretreated advanced clear-cell renal cell carcinoma who had received prior anti-angiogenic therapy (CheckMate 025).
Disclosures: Dr. Motzer disclosed that he has a consulting or advisory role with Eisai, Novartis, and Pfizer; that he receives travel expenses from Bristol-Myers Squibb; and that his institution receives research funding from Bristol-Myers Squibb, Eisai, Genentech/Roche, GlaxoSmithKline, Novartis, and Pfizer. The trial was sponsored in part by Bristol-Myers Squibb in collaboration with Ono Pharmaceutical Co. Ltd.
Liquid biopsy may help guide treatment decisions in prostate cancer
Analysis of the phenotypic and genotypic profile of circulating tumor cells (CTCs) – a so-called liquid biopsy – may help guide treatment decisions in men with castration-resistant metastatic prostate cancer, according to a cohort study being reported at the Genitourinary Cancers Symposium.
Investigators analyzed CTCs in 221 blood samples from 179 patients with metastatic prostate cancer about to begin either hormonal therapy (enzalutamide or abiraterone) or chemotherapy based on a taxane (docetaxel or cabazitaxel).
Among patients given hormonal therapy, those whose CTCs exhibited high versus low scores for phenotypic heterogeneity had poorer radiographic progression-free survival (5 months vs. 17 months) and overall survival (9 months vs. not reached), first author Dr. Howard I. Scher reported in a press briefing held before the 2016 genitourinary cancers symposium sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
In contrast, among those given chemotherapy, heterogeneity score did not affect these outcomes.
In other key findings, the heterogeneity score increased with each additional line of therapy patients received in the metastatic setting.
“We were able to show that single cell morphology, protein, and genomic characterization is feasible and can be used to assess tumor heterogeneity,” commented Dr. Scher of the Genitourinary Oncology Service at the Memorial Sloan Kettering Cancer Center (MSKCC) in New York. “For characterizing disease at the point of decision making, a noninvasive liquid biopsy that enables the characterization of individual cells from a patient with metastatic prostate cancer can be used to guide treatment selection. Clinical trials to validate these findings are currently in development.”
He speculated that CTC heterogeneity was important only for hormonal therapy because it is a targeted therapy; as the disease becomes more diverse, essentially evolving into multiple diseases, this therapy is less likely to be effective. “The mechanism of taxanes is more general and not quite as targeted as these specific agents, which is why we believe they are more effective in a more diverse population,” he explained.
ASCO spokesperson and moderator of the press briefing Dr. Sumanta K. Pal, commented, “This is really fascinating work. We’ve always relied on a patient’s tumor to get genetic information, but that can be incredibly complicated for a number of reasons.” Among them, metastases may be located in hard-to-biopsy locations, and it is not practical to repeatedly perform needle biopsies over time.
The new findings show that “prostate cancer appears to get more complex over time as the disease evolves. The genetic diversity, quote unquote, increases, potentially suggesting that the cancer cell is crafting machinery to resist treatment,” he said.
From the clinical perspective, the ability to link CTC characteristics to response or lack thereof to a given therapy “is of incredible value,” according to Dr. Pal of the City of Hope, Duarte, Calif. “We have a number of new treatments for advanced prostate cancer and right now, we have little means of personalizing them and offering the right treatment to the right patient. With the studies that Dr. Scher has proposed to potentially validate this modality, we would have this personalized selection tool in our hands.”
Giving some background to the research, Dr. Scher noted, “Tissues are composed of a mixture of cells that differ morphologically and biologically. The result is diversity at single sites and multiple sites, broadly termed heterogeneity, so that we are not treating a single disease but a collection of diseases, and that is one reason we have difficulty achieving cures.”
“One could think of the blood as sampling, at least in theory, from all of the metastatic sites that are present. And we think you’ll have a greater chance of getting a more relevant characterization of the disease as a whole, in particular, by looking at the individual cells,” he further noted.
In the study, the investigators collected CTCs from blood samples, deposited them onto slides, stained them with DAPI and for various proteins (cytokeratin, androgen receptor, and CD45), and then scanned them, using a commercial platform (Epic Sciences).
They analyzed morphologic and phenotypic features of 9,225 single CTCs, splitting them into 15 distinct subtypes. They also performed whole-genome sequencing in a subset of 741 CTCs to assess copy number variation, clonality, and gene amplifications and deletions.
“The samples can be run quickly, and you can get results within 48 hours, which is important if you are trying to make a treatment decision,” Dr. Scher noted.
Findings showed that among patients given hormonal therapy, a high versus low CTC heterogeneity score was associated with much greater risks of radiographic progression-free survival events (hazard ratio, 2.2; P = .00182) and death (HR, 5.5; P less than .0001). In contrast, among patients who received taxane-based chemotherapy, CTC heterogeneity did not significantly affect either outcome.
Analysis of the phenotypic and genotypic profile of circulating tumor cells (CTCs) – a so-called liquid biopsy – may help guide treatment decisions in men with castration-resistant metastatic prostate cancer, according to a cohort study being reported at the Genitourinary Cancers Symposium.
Investigators analyzed CTCs in 221 blood samples from 179 patients with metastatic prostate cancer about to begin either hormonal therapy (enzalutamide or abiraterone) or chemotherapy based on a taxane (docetaxel or cabazitaxel).
Among patients given hormonal therapy, those whose CTCs exhibited high versus low scores for phenotypic heterogeneity had poorer radiographic progression-free survival (5 months vs. 17 months) and overall survival (9 months vs. not reached), first author Dr. Howard I. Scher reported in a press briefing held before the 2016 genitourinary cancers symposium sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
In contrast, among those given chemotherapy, heterogeneity score did not affect these outcomes.
In other key findings, the heterogeneity score increased with each additional line of therapy patients received in the metastatic setting.
“We were able to show that single cell morphology, protein, and genomic characterization is feasible and can be used to assess tumor heterogeneity,” commented Dr. Scher of the Genitourinary Oncology Service at the Memorial Sloan Kettering Cancer Center (MSKCC) in New York. “For characterizing disease at the point of decision making, a noninvasive liquid biopsy that enables the characterization of individual cells from a patient with metastatic prostate cancer can be used to guide treatment selection. Clinical trials to validate these findings are currently in development.”
He speculated that CTC heterogeneity was important only for hormonal therapy because it is a targeted therapy; as the disease becomes more diverse, essentially evolving into multiple diseases, this therapy is less likely to be effective. “The mechanism of taxanes is more general and not quite as targeted as these specific agents, which is why we believe they are more effective in a more diverse population,” he explained.
ASCO spokesperson and moderator of the press briefing Dr. Sumanta K. Pal, commented, “This is really fascinating work. We’ve always relied on a patient’s tumor to get genetic information, but that can be incredibly complicated for a number of reasons.” Among them, metastases may be located in hard-to-biopsy locations, and it is not practical to repeatedly perform needle biopsies over time.
The new findings show that “prostate cancer appears to get more complex over time as the disease evolves. The genetic diversity, quote unquote, increases, potentially suggesting that the cancer cell is crafting machinery to resist treatment,” he said.
From the clinical perspective, the ability to link CTC characteristics to response or lack thereof to a given therapy “is of incredible value,” according to Dr. Pal of the City of Hope, Duarte, Calif. “We have a number of new treatments for advanced prostate cancer and right now, we have little means of personalizing them and offering the right treatment to the right patient. With the studies that Dr. Scher has proposed to potentially validate this modality, we would have this personalized selection tool in our hands.”
Giving some background to the research, Dr. Scher noted, “Tissues are composed of a mixture of cells that differ morphologically and biologically. The result is diversity at single sites and multiple sites, broadly termed heterogeneity, so that we are not treating a single disease but a collection of diseases, and that is one reason we have difficulty achieving cures.”
“One could think of the blood as sampling, at least in theory, from all of the metastatic sites that are present. And we think you’ll have a greater chance of getting a more relevant characterization of the disease as a whole, in particular, by looking at the individual cells,” he further noted.
In the study, the investigators collected CTCs from blood samples, deposited them onto slides, stained them with DAPI and for various proteins (cytokeratin, androgen receptor, and CD45), and then scanned them, using a commercial platform (Epic Sciences).
They analyzed morphologic and phenotypic features of 9,225 single CTCs, splitting them into 15 distinct subtypes. They also performed whole-genome sequencing in a subset of 741 CTCs to assess copy number variation, clonality, and gene amplifications and deletions.
“The samples can be run quickly, and you can get results within 48 hours, which is important if you are trying to make a treatment decision,” Dr. Scher noted.
Findings showed that among patients given hormonal therapy, a high versus low CTC heterogeneity score was associated with much greater risks of radiographic progression-free survival events (hazard ratio, 2.2; P = .00182) and death (HR, 5.5; P less than .0001). In contrast, among patients who received taxane-based chemotherapy, CTC heterogeneity did not significantly affect either outcome.
Analysis of the phenotypic and genotypic profile of circulating tumor cells (CTCs) – a so-called liquid biopsy – may help guide treatment decisions in men with castration-resistant metastatic prostate cancer, according to a cohort study being reported at the Genitourinary Cancers Symposium.
Investigators analyzed CTCs in 221 blood samples from 179 patients with metastatic prostate cancer about to begin either hormonal therapy (enzalutamide or abiraterone) or chemotherapy based on a taxane (docetaxel or cabazitaxel).
Among patients given hormonal therapy, those whose CTCs exhibited high versus low scores for phenotypic heterogeneity had poorer radiographic progression-free survival (5 months vs. 17 months) and overall survival (9 months vs. not reached), first author Dr. Howard I. Scher reported in a press briefing held before the 2016 genitourinary cancers symposium sponsored by the American Society of Clinical Oncology, ASTRO, and the Society of Urologic Oncology.
In contrast, among those given chemotherapy, heterogeneity score did not affect these outcomes.
In other key findings, the heterogeneity score increased with each additional line of therapy patients received in the metastatic setting.
“We were able to show that single cell morphology, protein, and genomic characterization is feasible and can be used to assess tumor heterogeneity,” commented Dr. Scher of the Genitourinary Oncology Service at the Memorial Sloan Kettering Cancer Center (MSKCC) in New York. “For characterizing disease at the point of decision making, a noninvasive liquid biopsy that enables the characterization of individual cells from a patient with metastatic prostate cancer can be used to guide treatment selection. Clinical trials to validate these findings are currently in development.”
He speculated that CTC heterogeneity was important only for hormonal therapy because it is a targeted therapy; as the disease becomes more diverse, essentially evolving into multiple diseases, this therapy is less likely to be effective. “The mechanism of taxanes is more general and not quite as targeted as these specific agents, which is why we believe they are more effective in a more diverse population,” he explained.
ASCO spokesperson and moderator of the press briefing Dr. Sumanta K. Pal, commented, “This is really fascinating work. We’ve always relied on a patient’s tumor to get genetic information, but that can be incredibly complicated for a number of reasons.” Among them, metastases may be located in hard-to-biopsy locations, and it is not practical to repeatedly perform needle biopsies over time.
The new findings show that “prostate cancer appears to get more complex over time as the disease evolves. The genetic diversity, quote unquote, increases, potentially suggesting that the cancer cell is crafting machinery to resist treatment,” he said.
From the clinical perspective, the ability to link CTC characteristics to response or lack thereof to a given therapy “is of incredible value,” according to Dr. Pal of the City of Hope, Duarte, Calif. “We have a number of new treatments for advanced prostate cancer and right now, we have little means of personalizing them and offering the right treatment to the right patient. With the studies that Dr. Scher has proposed to potentially validate this modality, we would have this personalized selection tool in our hands.”
Giving some background to the research, Dr. Scher noted, “Tissues are composed of a mixture of cells that differ morphologically and biologically. The result is diversity at single sites and multiple sites, broadly termed heterogeneity, so that we are not treating a single disease but a collection of diseases, and that is one reason we have difficulty achieving cures.”
“One could think of the blood as sampling, at least in theory, from all of the metastatic sites that are present. And we think you’ll have a greater chance of getting a more relevant characterization of the disease as a whole, in particular, by looking at the individual cells,” he further noted.
In the study, the investigators collected CTCs from blood samples, deposited them onto slides, stained them with DAPI and for various proteins (cytokeratin, androgen receptor, and CD45), and then scanned them, using a commercial platform (Epic Sciences).
They analyzed morphologic and phenotypic features of 9,225 single CTCs, splitting them into 15 distinct subtypes. They also performed whole-genome sequencing in a subset of 741 CTCs to assess copy number variation, clonality, and gene amplifications and deletions.
“The samples can be run quickly, and you can get results within 48 hours, which is important if you are trying to make a treatment decision,” Dr. Scher noted.
Findings showed that among patients given hormonal therapy, a high versus low CTC heterogeneity score was associated with much greater risks of radiographic progression-free survival events (hazard ratio, 2.2; P = .00182) and death (HR, 5.5; P less than .0001). In contrast, among patients who received taxane-based chemotherapy, CTC heterogeneity did not significantly affect either outcome.
FROM THE GENITOURINARY CANCERS SYMPOSIUM
Key clinical point: In patients with castration-resistant metastatic prostate cancer, CTC heterogeneity affects the response to hormonal therapy but not to chemotherapy.
Major finding: A high vs. low CTC heterogeneity score was associated with shorter median progression-free survival (5 vs. 17 months) and overall survival (9 months vs. not reached) with hormonal therapy but did not affect these outcomes with chemotherapy.
Data source: A cohort study of 179 patients with castration-resistant metastatic prostate cancer about to begin either hormonal therapy or taxane-based chemotherapy.
Disclosures: Dr. Scher disclosed that he has a consulting or advisory role, and receives travel, accommodations, and/or expenses from numerous pharmaceutical companies. He receives research funding (institutional) from BIND Biosciences, Exelixis, Janssen Pharmaceuticals, Medivation, Janssen Diagnostics, and Innocrin Pharmaceuticals. The study received funding from the Prostate Cancer Foundation, MSKCC SPORE, and MSKCC Core Grant. Dr. Pal disclosed that he receives honoraria from Astellas Pharma, Medivation, and Novartis; that he has a consulting or advisory role with Aveo, Genentech, Myriad Pharmaceuticals, Novartis, and Pfizer; and that he receives research funding from Medivation.