Gastrointestinal Cancers Symposium 2013

SAN FRANCISCO – Adding bevacizumab to capecitabine for first-line therapy for elderly patients with metastatic colorectal cancer significantly delayed disease progression and improved treatment response rates compared with capecitabine alone in a study of 280 patients.

The study is the first prospective, phase III clinical trial of a biologic agent (bevacizumab) for metastatic colorectal cancer in patients aged 70 years or older, who comprise many patients with this disease and generally are underrepresented in clinical trials, Dr. David Cunningham said.

Courtesy the American Society of Clinical Oncology

Median progression-free survival rates were 5.1 months with capecitabine (Xeloda, Roche) and 9.1 months with capecitabine plus bevacizumab (Avastin, Roche/Genentech), an intent-to-treat analysis showed. Patients were followed for a median of 22 months in the monotherapy arm and 25 months in the combination therapy arm.

Among secondary outcomes, overall response rates were significantly better with the combination regimen (19%) compared with monotherapy (10%), he and his associates reported at a meeting on gastrointestinal cancers sponsored by the American Society of Clinical Oncology.

The capecitabine/bevacizumab group also showed improved median overall survival (20.7 months) compared with the control group (16.8 months). This difference did not reach statistical significance, but the study was not powered to show a difference in overall survival. The primary outcome was progression-free survival, said Dr. Cunningham, head of the gastrointestinal unit at Royal Marsden Hospital, London.

The benefits were seen across all subgroups, he added.

The Avastin in the Elderly with Xeloda (AVEX) trial randomized elderly patients from 10 countries to first-line treatment with capecitabine 1,000 mg/m² b.i.d. on days 1-4 with or without bevacizumab 7.5 mg/kg every 3 weeks. Patients had a median age of 76 years at enrollment and an Eastern Cooperative Oncology Group performance status of 0-2. The study recruited patients who were not considered optimal candidates for combination therapy including irinotecan or oxaliplatin. Baseline characteristics were similar between treatment groups.

Grade 3 or higher adverse events occurred in 59% of patients on the combination therapy, compared with 44% on capecitabine alone, a safety analysis on 270 patients found. Rates of any serious adverse events were 31% with combination therapy and 32% with monotherapy. Adverse events led to death in 8% of the combination group and 12% on monotherapy.

"As a clinician, I was impressed with how well tolerated this combination was," Dr. Cunningham said. No signals of unusual adverse events were seen in this older population.

Among grade 3 or higher adverse events of special interest with bevacizumab or related to chemotherapy, hypertension developed in 2.2% on the combination and 1.5% on monotherapy, venous thromboembolic events were seen in 8.2% on the combination and 4.4% on monotherapy, arterial thromboembolic events occurred in 3.7% on the combination and 1.5% on monotherapy, and proteinuria was seen in 1.5% on the combination and in no patients on monotherapy. Grade 3 or higher bleeding, pulmonary hemorrhage, or heart failure occurred in less than 1% on monotherapy and no patients on combination treatment.

Patients on the combination therapy were exposed to treatment for a longer duration (5.8 months) compared with those on monotherapy (4.2 months). The capecitabine-plus-bevacizumab group underwent a median of nine cycles of therapy compared with six cycles in the capecitabine group.

The combination treatment was "effective, generally well tolerated, and produced meaningful disease control and good survival," Dr. Cunningham said. Because the multicenter study included patients from around the world, "these results should be transferable" and generalizable to elderly patients with metastatic colorectal cancer, he added.

Thirty-seven percent of patients in each treatment group received subsequent therapy for metastatic colorectal cancer.

Bevacizumab is considered part of standard care for metastatic colorectal cancer in general, and prior studies had suggested that elderly patients would benefit from adding bevacizumab to chemotherapy, he said.

The meeting was cosponsored by ASCO, the American Gastroenterological Association Institute, the American Society for Radiation Oncology, and the Society of Surgical Oncology.

Dr. Cunningham reported receiving research funding from Roche, which markets capecitabine and bevacizumab, and from AstraZeneca and Merck KGaA. Several of his associates in the study were employees, leaders, or stockholders in Roche.

s.boschert@elsevier.com

On Twitter @sherryboschert

SAN FRANCISCO – Adding bevacizumab to capecitabine for first-line therapy for elderly patients with metastatic colorectal cancer significantly delayed disease progression and improved treatment response rates compared with capecitabine alone in a study of 280 patients.

The study is the first prospective, phase III clinical trial of a biologic agent (bevacizumab) for metastatic colorectal cancer in patients aged 70 years or older, who comprise many patients with this disease and generally are underrepresented in clinical trials, Dr. David Cunningham said.

Courtesy the American Society of Clinical Oncology

Median progression-free survival rates were 5.1 months with capecitabine (Xeloda, Roche) and 9.1 months with capecitabine plus bevacizumab (Avastin, Roche/Genentech), an intent-to-treat analysis showed. Patients were followed for a median of 22 months in the monotherapy arm and 25 months in the combination therapy arm.

Among secondary outcomes, overall response rates were significantly better with the combination regimen (19%) compared with monotherapy (10%), he and his associates reported at a meeting on gastrointestinal cancers sponsored by the American Society of Clinical Oncology.

The capecitabine/bevacizumab group also showed improved median overall survival (20.7 months) compared with the control group (16.8 months). This difference did not reach statistical significance, but the study was not powered to show a difference in overall survival. The primary outcome was progression-free survival, said Dr. Cunningham, head of the gastrointestinal unit at Royal Marsden Hospital, London.

The benefits were seen across all subgroups, he added.

The Avastin in the Elderly with Xeloda (AVEX) trial randomized elderly patients from 10 countries to first-line treatment with capecitabine 1,000 mg/m² b.i.d. on days 1-4 with or without bevacizumab 7.5 mg/kg every 3 weeks. Patients had a median age of 76 years at enrollment and an Eastern Cooperative Oncology Group performance status of 0-2. The study recruited patients who were not considered optimal candidates for combination therapy including irinotecan or oxaliplatin. Baseline characteristics were similar between treatment groups.

Grade 3 or higher adverse events occurred in 59% of patients on the combination therapy, compared with 44% on capecitabine alone, a safety analysis on 270 patients found. Rates of any serious adverse events were 31% with combination therapy and 32% with monotherapy. Adverse events led to death in 8% of the combination group and 12% on monotherapy.

"As a clinician, I was impressed with how well tolerated this combination was," Dr. Cunningham said. No signals of unusual adverse events were seen in this older population.

Among grade 3 or higher adverse events of special interest with bevacizumab or related to chemotherapy, hypertension developed in 2.2% on the combination and 1.5% on monotherapy, venous thromboembolic events were seen in 8.2% on the combination and 4.4% on monotherapy, arterial thromboembolic events occurred in 3.7% on the combination and 1.5% on monotherapy, and proteinuria was seen in 1.5% on the combination and in no patients on monotherapy. Grade 3 or higher bleeding, pulmonary hemorrhage, or heart failure occurred in less than 1% on monotherapy and no patients on combination treatment.

Patients on the combination therapy were exposed to treatment for a longer duration (5.8 months) compared with those on monotherapy (4.2 months). The capecitabine-plus-bevacizumab group underwent a median of nine cycles of therapy compared with six cycles in the capecitabine group.

The combination treatment was "effective, generally well tolerated, and produced meaningful disease control and good survival," Dr. Cunningham said. Because the multicenter study included patients from around the world, "these results should be transferable" and generalizable to elderly patients with metastatic colorectal cancer, he added.

Thirty-seven percent of patients in each treatment group received subsequent therapy for metastatic colorectal cancer.

Bevacizumab is considered part of standard care for metastatic colorectal cancer in general, and prior studies had suggested that elderly patients would benefit from adding bevacizumab to chemotherapy, he said.

The meeting was cosponsored by ASCO, the American Gastroenterological Association Institute, the American Society for Radiation Oncology, and the Society of Surgical Oncology.

Dr. Cunningham reported receiving research funding from Roche, which markets capecitabine and bevacizumab, and from AstraZeneca and Merck KGaA. Several of his associates in the study were employees, leaders, or stockholders in Roche.

s.boschert@elsevier.com

On Twitter @sherryboschert

SAN FRANCISCO – Adding bevacizumab to capecitabine for first-line therapy for elderly patients with metastatic colorectal cancer significantly delayed disease progression and improved treatment response rates compared with capecitabine alone in a study of 280 patients.

The study is the first prospective, phase III clinical trial of a biologic agent (bevacizumab) for metastatic colorectal cancer in patients aged 70 years or older, who comprise many patients with this disease and generally are underrepresented in clinical trials, Dr. David Cunningham said.

Courtesy the American Society of Clinical Oncology

Median progression-free survival rates were 5.1 months with capecitabine (Xeloda, Roche) and 9.1 months with capecitabine plus bevacizumab (Avastin, Roche/Genentech), an intent-to-treat analysis showed. Patients were followed for a median of 22 months in the monotherapy arm and 25 months in the combination therapy arm.

Among secondary outcomes, overall response rates were significantly better with the combination regimen (19%) compared with monotherapy (10%), he and his associates reported at a meeting on gastrointestinal cancers sponsored by the American Society of Clinical Oncology.

The capecitabine/bevacizumab group also showed improved median overall survival (20.7 months) compared with the control group (16.8 months). This difference did not reach statistical significance, but the study was not powered to show a difference in overall survival. The primary outcome was progression-free survival, said Dr. Cunningham, head of the gastrointestinal unit at Royal Marsden Hospital, London.

The benefits were seen across all subgroups, he added.

The Avastin in the Elderly with Xeloda (AVEX) trial randomized elderly patients from 10 countries to first-line treatment with capecitabine 1,000 mg/m² b.i.d. on days 1-4 with or without bevacizumab 7.5 mg/kg every 3 weeks. Patients had a median age of 76 years at enrollment and an Eastern Cooperative Oncology Group performance status of 0-2. The study recruited patients who were not considered optimal candidates for combination therapy including irinotecan or oxaliplatin. Baseline characteristics were similar between treatment groups.

Grade 3 or higher adverse events occurred in 59% of patients on the combination therapy, compared with 44% on capecitabine alone, a safety analysis on 270 patients found. Rates of any serious adverse events were 31% with combination therapy and 32% with monotherapy. Adverse events led to death in 8% of the combination group and 12% on monotherapy.

"As a clinician, I was impressed with how well tolerated this combination was," Dr. Cunningham said. No signals of unusual adverse events were seen in this older population.

Among grade 3 or higher adverse events of special interest with bevacizumab or related to chemotherapy, hypertension developed in 2.2% on the combination and 1.5% on monotherapy, venous thromboembolic events were seen in 8.2% on the combination and 4.4% on monotherapy, arterial thromboembolic events occurred in 3.7% on the combination and 1.5% on monotherapy, and proteinuria was seen in 1.5% on the combination and in no patients on monotherapy. Grade 3 or higher bleeding, pulmonary hemorrhage, or heart failure occurred in less than 1% on monotherapy and no patients on combination treatment.

Patients on the combination therapy were exposed to treatment for a longer duration (5.8 months) compared with those on monotherapy (4.2 months). The capecitabine-plus-bevacizumab group underwent a median of nine cycles of therapy compared with six cycles in the capecitabine group.

The combination treatment was "effective, generally well tolerated, and produced meaningful disease control and good survival," Dr. Cunningham said. Because the multicenter study included patients from around the world, "these results should be transferable" and generalizable to elderly patients with metastatic colorectal cancer, he added.

Thirty-seven percent of patients in each treatment group received subsequent therapy for metastatic colorectal cancer.

Bevacizumab is considered part of standard care for metastatic colorectal cancer in general, and prior studies had suggested that elderly patients would benefit from adding bevacizumab to chemotherapy, he said.

The meeting was cosponsored by ASCO, the American Gastroenterological Association Institute, the American Society for Radiation Oncology, and the Society of Surgical Oncology.

Dr. Cunningham reported receiving research funding from Roche, which markets capecitabine and bevacizumab, and from AstraZeneca and Merck KGaA. Several of his associates in the study were employees, leaders, or stockholders in Roche.

s.boschert@elsevier.com

On Twitter @sherryboschert

SAN FRANCISCO – A phase II/III clinical trial of adding cetuximab to chemoradiotherapy for localized esophageal cancer was stopped early when interim results showed greater toxicity, less completion of chemoradiotherapy, and worse survival with cetuximab.

Patients had been randomized to potentially curative treatment with cisplatin, capecitabine, and radiation, with or without cetuximab (Erbitux). Six months of follow-up on 258 patients found significantly lower median overall survival in the cetuximab arm compared with the control group (22.1 months vs. 25.4 months) and fewer patients free of treatment failure (66% vs. 77%), Dr. Thomas Crosby reported at a meeting on gastrointestinal cancers sponsored by the American Society of Clinical Oncology (ASCO).

Sherry Boschert/IMNG Medical Media

The number of patients lost to follow-up before 26 weeks was similar between groups: 10 in the cetuximab group and 8 in the control group, he added.

Significantly fewer patients in the cetuximab arm were able to receive the full protocol dose of radiotherapy compared with the control arm (75% vs. 86%) and to complete all four cycles of cisplatin and capecitabine at full doses (77% vs. 90%) or reduced doses (69% vs. 85%), reported Dr. Crosby of Velindre Hospital, Cardiff, Wales.

The cetuximab group also showed significantly higher rates of grade 3 or 4 nonhematologic toxicities (78%) compared with the control arm (63%), primarily because of increases in cardiac toxicities (6% vs. 2%), dermatologic toxicities (22% vs. 4%), and metabolic toxicities (24% vs. 11%).

"The addition of cetuximab cannot be recommended to standard definitive chemoradiotherapy in the treatment of unselected patients with esophageal cancer," Dr. Crosby said.

All patients were to receive four cycles of cisplatin 60 mg/m² on day 1 and capecitabine 625 mg/m² daily on days 1-21, with cycles three and four given concurrently with radiotherapy (60 Gy in 25 fractions). The cetuximab group also received 400 mg/m² of the drug on day 1 of cycle three, followed by cetuximab 250 mg/m² weekly.

Patients in the multicenter study, known as the SCOPE 1 trial, had a median age of 67 years in both groups.

Survival outcomes associated with chemoradiotherapy for localized, poor-prognosis esophageal cancer in SCOPE 1 were better than results previously reported in trials of radiotherapy or surgery for these cancers, he noted. Future research should look at improving definitive chemoradiotherapy by identifying biomarkers to help select patients for treatment and incorporating newer radiology techniques to intensify treatment, he suggested.

Definitive chemoradiotherapy is used in the United Kingdom predominantly for patients with esophageal cancer who are not candidates for surgery and is considered a standard of care for patients with localized squamous cell carcinoma of the esophagus, Dr. Crosby said.

Other previous studies have reported that cetuximab improved outcomes when added to chemotherapy for advanced colorectal or head and neck cancers, and when added to radiotherapy for localized squamous cell carcinomas of the head and neck, he said. A separate study recently reported worse outcomes when cetuximab was added to first-line chemotherapy for gastric cancer.

Dr. Crosby reported having no relevant financial disclosures. Cetuximab is a product of ImClone, a subsidiary of Eli Lilly and Bristol-Myers Squibb, that is licensed to Merck KGaA for marketing outside the United States. Some of his associates reported receiving research funding from Merck, AstraZeneca, or Roche.

s.boschert@elsevier.com

On Twitter @sherryboschert

SAN FRANCISCO – A phase II/III clinical trial of adding cetuximab to chemoradiotherapy for localized esophageal cancer was stopped early when interim results showed greater toxicity, less completion of chemoradiotherapy, and worse survival with cetuximab.

Patients had been randomized to potentially curative treatment with cisplatin, capecitabine, and radiation, with or without cetuximab (Erbitux). Six months of follow-up on 258 patients found significantly lower median overall survival in the cetuximab arm compared with the control group (22.1 months vs. 25.4 months) and fewer patients free of treatment failure (66% vs. 77%), Dr. Thomas Crosby reported at a meeting on gastrointestinal cancers sponsored by the American Society of Clinical Oncology (ASCO).

Sherry Boschert/IMNG Medical Media

The number of patients lost to follow-up before 26 weeks was similar between groups: 10 in the cetuximab group and 8 in the control group, he added.

Significantly fewer patients in the cetuximab arm were able to receive the full protocol dose of radiotherapy compared with the control arm (75% vs. 86%) and to complete all four cycles of cisplatin and capecitabine at full doses (77% vs. 90%) or reduced doses (69% vs. 85%), reported Dr. Crosby of Velindre Hospital, Cardiff, Wales.

The cetuximab group also showed significantly higher rates of grade 3 or 4 nonhematologic toxicities (78%) compared with the control arm (63%), primarily because of increases in cardiac toxicities (6% vs. 2%), dermatologic toxicities (22% vs. 4%), and metabolic toxicities (24% vs. 11%).

"The addition of cetuximab cannot be recommended to standard definitive chemoradiotherapy in the treatment of unselected patients with esophageal cancer," Dr. Crosby said.

All patients were to receive four cycles of cisplatin 60 mg/m² on day 1 and capecitabine 625 mg/m² daily on days 1-21, with cycles three and four given concurrently with radiotherapy (60 Gy in 25 fractions). The cetuximab group also received 400 mg/m² of the drug on day 1 of cycle three, followed by cetuximab 250 mg/m² weekly.

Patients in the multicenter study, known as the SCOPE 1 trial, had a median age of 67 years in both groups.

Survival outcomes associated with chemoradiotherapy for localized, poor-prognosis esophageal cancer in SCOPE 1 were better than results previously reported in trials of radiotherapy or surgery for these cancers, he noted. Future research should look at improving definitive chemoradiotherapy by identifying biomarkers to help select patients for treatment and incorporating newer radiology techniques to intensify treatment, he suggested.

Definitive chemoradiotherapy is used in the United Kingdom predominantly for patients with esophageal cancer who are not candidates for surgery and is considered a standard of care for patients with localized squamous cell carcinoma of the esophagus, Dr. Crosby said.

Other previous studies have reported that cetuximab improved outcomes when added to chemotherapy for advanced colorectal or head and neck cancers, and when added to radiotherapy for localized squamous cell carcinomas of the head and neck, he said. A separate study recently reported worse outcomes when cetuximab was added to first-line chemotherapy for gastric cancer.

Dr. Crosby reported having no relevant financial disclosures. Cetuximab is a product of ImClone, a subsidiary of Eli Lilly and Bristol-Myers Squibb, that is licensed to Merck KGaA for marketing outside the United States. Some of his associates reported receiving research funding from Merck, AstraZeneca, or Roche.

s.boschert@elsevier.com

On Twitter @sherryboschert

SAN FRANCISCO – A phase II/III clinical trial of adding cetuximab to chemoradiotherapy for localized esophageal cancer was stopped early when interim results showed greater toxicity, less completion of chemoradiotherapy, and worse survival with cetuximab.

Patients had been randomized to potentially curative treatment with cisplatin, capecitabine, and radiation, with or without cetuximab (Erbitux). Six months of follow-up on 258 patients found significantly lower median overall survival in the cetuximab arm compared with the control group (22.1 months vs. 25.4 months) and fewer patients free of treatment failure (66% vs. 77%), Dr. Thomas Crosby reported at a meeting on gastrointestinal cancers sponsored by the American Society of Clinical Oncology (ASCO).

Sherry Boschert/IMNG Medical Media

The number of patients lost to follow-up before 26 weeks was similar between groups: 10 in the cetuximab group and 8 in the control group, he added.

Significantly fewer patients in the cetuximab arm were able to receive the full protocol dose of radiotherapy compared with the control arm (75% vs. 86%) and to complete all four cycles of cisplatin and capecitabine at full doses (77% vs. 90%) or reduced doses (69% vs. 85%), reported Dr. Crosby of Velindre Hospital, Cardiff, Wales.

The cetuximab group also showed significantly higher rates of grade 3 or 4 nonhematologic toxicities (78%) compared with the control arm (63%), primarily because of increases in cardiac toxicities (6% vs. 2%), dermatologic toxicities (22% vs. 4%), and metabolic toxicities (24% vs. 11%).

"The addition of cetuximab cannot be recommended to standard definitive chemoradiotherapy in the treatment of unselected patients with esophageal cancer," Dr. Crosby said.

All patients were to receive four cycles of cisplatin 60 mg/m² on day 1 and capecitabine 625 mg/m² daily on days 1-21, with cycles three and four given concurrently with radiotherapy (60 Gy in 25 fractions). The cetuximab group also received 400 mg/m² of the drug on day 1 of cycle three, followed by cetuximab 250 mg/m² weekly.

Patients in the multicenter study, known as the SCOPE 1 trial, had a median age of 67 years in both groups.

Survival outcomes associated with chemoradiotherapy for localized, poor-prognosis esophageal cancer in SCOPE 1 were better than results previously reported in trials of radiotherapy or surgery for these cancers, he noted. Future research should look at improving definitive chemoradiotherapy by identifying biomarkers to help select patients for treatment and incorporating newer radiology techniques to intensify treatment, he suggested.

Definitive chemoradiotherapy is used in the United Kingdom predominantly for patients with esophageal cancer who are not candidates for surgery and is considered a standard of care for patients with localized squamous cell carcinoma of the esophagus, Dr. Crosby said.

Other previous studies have reported that cetuximab improved outcomes when added to chemotherapy for advanced colorectal or head and neck cancers, and when added to radiotherapy for localized squamous cell carcinomas of the head and neck, he said. A separate study recently reported worse outcomes when cetuximab was added to first-line chemotherapy for gastric cancer.

Dr. Crosby reported having no relevant financial disclosures. Cetuximab is a product of ImClone, a subsidiary of Eli Lilly and Bristol-Myers Squibb, that is licensed to Merck KGaA for marketing outside the United States. Some of his associates reported receiving research funding from Merck, AstraZeneca, or Roche.

s.boschert@elsevier.com

On Twitter @sherryboschert

SAN FRANCISCO – A phase III clinical trial of an experimental monoclonal antibody for patients failing first-line treatment of metastatic gastric or gastroesophageal junction adenocarcinoma increased median overall survival to 5.2 months, compared with 3.8 months on placebo.

The difference was statistically significant and the treatment effect generally was consistent across major subgroups of the 355 patients in the international, prospective, double-blind trial. At 6 months, 42% of patients on ramucirumab and 32% on placebo were alive. At 12 months, 18% on ramucirumab and 11% on placebo were alive, Dr. Charles S. Fuchs and his associates reported in a poster presentation at a meeting on gastrointestinal cancers sponsored by the American Society of Clinical Oncology (ASCO).

Courtesy American Society of Clinical Oncology

Ramucirumab is a fully human IgG1 monoclonal antibody receptor antagonist designed to inhibit the receptor for vascular endothelial cell growth factor (VEGF), which is believed to contribute to gastric cancer pathogenesis.

The study randomized 238 patients to second-line treatment with IV ramucirumab 8 mg/kg plus best supportive care or placebo plus best supportive care every 2 weeks until disease progression, unacceptable toxicity, or death. All patients had shown disease progression within 4 months of treatment for metastatic disease or within 6 months of adjuvant therapy using first-line regimens containing platinum and/or fluoropyrimidine.

Among secondary outcomes, patients in the ramucirumab group showed a significantly longer interval to disease progression – 2.1 months, compared with 1.3 months on placebo – the intent-to-treat analysis found. At 12 weeks, 40% of patients in the ramucirumab group and 16% on placebo showed no disease progression, reported Dr. Fuchs, director of the gastrointestinal cancer center at the Dana Farber Cancer Institute, Boston.

Overall, 49% of patients on ramucirumab showed a complete or partial response or stable disease, compared with 23% on placebo, a significant difference.

Two patients in each group did not receive the drug or placebo. Among 351 patients who did, the proportions that died because of an adverse event were similar between groups – 11% on ramucirumab and 13% on placebo. The two groups did not differ significantly in rates of most individual adverse events, most commonly fatigue, abdominal pain, decreased appetite, or vomiting. Hypertension was more likely to develop in the ramucirumab group than the placebo group (16% vs. 8%), and grade 3 or higher hypertension was more common on ramucirumab (8% vs. 3% on placebo), though no patients on ramucirumab developed grade 4 hypertension.

No unexpected or new findings regarding safety were seen, Dr. Fuchs reported. Hypertension is one of the adverse events generally associated with antiangiogenic agents and therapeutic antibodies. Rates did not differ between groups for other adverse events of special interest with these agents, including bleeding/hemorrhage, arteriothromboembolic or venous thrombolic events, proteinuria, GI perforation, fistula, and others.

Patient characteristics were similar between the groups at baseline.

The study enrolled patients at 120 centers in 30 countries on six continents.

Ramucirumab is a potential new second-line treatment for patients with metastatic adenocarcinoma of the stomach or the gastroesophageal junction, Dr. Fuchs suggested.

The symposium was cosponsored by ASCO, the American Gastroenterological Association Institute, the American Society for Radiation Oncology, and the Society of Surgical Oncology.

The study was funded by ImClone Systems, a subsidiary of Eli Lilly and Co., which is developing ramucirumab. Some of Dr. Fuchs’ associates in the study disclosed employment or other financial relationships with ImClone Systems and stock ownership in Eli Lilly. Dr. Fuchs has been an advisor to Amgen, Bayer, Bristol-Myers Squibb, Genentech, Infinity Pharmaceuticals, Metamark Genetics, Momenta Pharmaceuticals, Pfizer, Roche, and Sanofi.

s.boschert@elsevier.com

On Twitter @sherryboschert

SAN FRANCISCO – A phase III clinical trial of an experimental monoclonal antibody for patients failing first-line treatment of metastatic gastric or gastroesophageal junction adenocarcinoma increased median overall survival to 5.2 months, compared with 3.8 months on placebo.

The difference was statistically significant and the treatment effect generally was consistent across major subgroups of the 355 patients in the international, prospective, double-blind trial. At 6 months, 42% of patients on ramucirumab and 32% on placebo were alive. At 12 months, 18% on ramucirumab and 11% on placebo were alive, Dr. Charles S. Fuchs and his associates reported in a poster presentation at a meeting on gastrointestinal cancers sponsored by the American Society of Clinical Oncology (ASCO).

Courtesy American Society of Clinical Oncology

Ramucirumab is a fully human IgG1 monoclonal antibody receptor antagonist designed to inhibit the receptor for vascular endothelial cell growth factor (VEGF), which is believed to contribute to gastric cancer pathogenesis.

The study randomized 238 patients to second-line treatment with IV ramucirumab 8 mg/kg plus best supportive care or placebo plus best supportive care every 2 weeks until disease progression, unacceptable toxicity, or death. All patients had shown disease progression within 4 months of treatment for metastatic disease or within 6 months of adjuvant therapy using first-line regimens containing platinum and/or fluoropyrimidine.

Among secondary outcomes, patients in the ramucirumab group showed a significantly longer interval to disease progression – 2.1 months, compared with 1.3 months on placebo – the intent-to-treat analysis found. At 12 weeks, 40% of patients in the ramucirumab group and 16% on placebo showed no disease progression, reported Dr. Fuchs, director of the gastrointestinal cancer center at the Dana Farber Cancer Institute, Boston.

Overall, 49% of patients on ramucirumab showed a complete or partial response or stable disease, compared with 23% on placebo, a significant difference.

Two patients in each group did not receive the drug or placebo. Among 351 patients who did, the proportions that died because of an adverse event were similar between groups – 11% on ramucirumab and 13% on placebo. The two groups did not differ significantly in rates of most individual adverse events, most commonly fatigue, abdominal pain, decreased appetite, or vomiting. Hypertension was more likely to develop in the ramucirumab group than the placebo group (16% vs. 8%), and grade 3 or higher hypertension was more common on ramucirumab (8% vs. 3% on placebo), though no patients on ramucirumab developed grade 4 hypertension.

No unexpected or new findings regarding safety were seen, Dr. Fuchs reported. Hypertension is one of the adverse events generally associated with antiangiogenic agents and therapeutic antibodies. Rates did not differ between groups for other adverse events of special interest with these agents, including bleeding/hemorrhage, arteriothromboembolic or venous thrombolic events, proteinuria, GI perforation, fistula, and others.

Patient characteristics were similar between the groups at baseline.

The study enrolled patients at 120 centers in 30 countries on six continents.

Ramucirumab is a potential new second-line treatment for patients with metastatic adenocarcinoma of the stomach or the gastroesophageal junction, Dr. Fuchs suggested.

The symposium was cosponsored by ASCO, the American Gastroenterological Association Institute, the American Society for Radiation Oncology, and the Society of Surgical Oncology.

The study was funded by ImClone Systems, a subsidiary of Eli Lilly and Co., which is developing ramucirumab. Some of Dr. Fuchs’ associates in the study disclosed employment or other financial relationships with ImClone Systems and stock ownership in Eli Lilly. Dr. Fuchs has been an advisor to Amgen, Bayer, Bristol-Myers Squibb, Genentech, Infinity Pharmaceuticals, Metamark Genetics, Momenta Pharmaceuticals, Pfizer, Roche, and Sanofi.

s.boschert@elsevier.com

On Twitter @sherryboschert

SAN FRANCISCO – A phase III clinical trial of an experimental monoclonal antibody for patients failing first-line treatment of metastatic gastric or gastroesophageal junction adenocarcinoma increased median overall survival to 5.2 months, compared with 3.8 months on placebo.

The difference was statistically significant and the treatment effect generally was consistent across major subgroups of the 355 patients in the international, prospective, double-blind trial. At 6 months, 42% of patients on ramucirumab and 32% on placebo were alive. At 12 months, 18% on ramucirumab and 11% on placebo were alive, Dr. Charles S. Fuchs and his associates reported in a poster presentation at a meeting on gastrointestinal cancers sponsored by the American Society of Clinical Oncology (ASCO).

Courtesy American Society of Clinical Oncology

Ramucirumab is a fully human IgG1 monoclonal antibody receptor antagonist designed to inhibit the receptor for vascular endothelial cell growth factor (VEGF), which is believed to contribute to gastric cancer pathogenesis.

The study randomized 238 patients to second-line treatment with IV ramucirumab 8 mg/kg plus best supportive care or placebo plus best supportive care every 2 weeks until disease progression, unacceptable toxicity, or death. All patients had shown disease progression within 4 months of treatment for metastatic disease or within 6 months of adjuvant therapy using first-line regimens containing platinum and/or fluoropyrimidine.

Among secondary outcomes, patients in the ramucirumab group showed a significantly longer interval to disease progression – 2.1 months, compared with 1.3 months on placebo – the intent-to-treat analysis found. At 12 weeks, 40% of patients in the ramucirumab group and 16% on placebo showed no disease progression, reported Dr. Fuchs, director of the gastrointestinal cancer center at the Dana Farber Cancer Institute, Boston.

Overall, 49% of patients on ramucirumab showed a complete or partial response or stable disease, compared with 23% on placebo, a significant difference.

Two patients in each group did not receive the drug or placebo. Among 351 patients who did, the proportions that died because of an adverse event were similar between groups – 11% on ramucirumab and 13% on placebo. The two groups did not differ significantly in rates of most individual adverse events, most commonly fatigue, abdominal pain, decreased appetite, or vomiting. Hypertension was more likely to develop in the ramucirumab group than the placebo group (16% vs. 8%), and grade 3 or higher hypertension was more common on ramucirumab (8% vs. 3% on placebo), though no patients on ramucirumab developed grade 4 hypertension.

No unexpected or new findings regarding safety were seen, Dr. Fuchs reported. Hypertension is one of the adverse events generally associated with antiangiogenic agents and therapeutic antibodies. Rates did not differ between groups for other adverse events of special interest with these agents, including bleeding/hemorrhage, arteriothromboembolic or venous thrombolic events, proteinuria, GI perforation, fistula, and others.

Patient characteristics were similar between the groups at baseline.

The study enrolled patients at 120 centers in 30 countries on six continents.

Ramucirumab is a potential new second-line treatment for patients with metastatic adenocarcinoma of the stomach or the gastroesophageal junction, Dr. Fuchs suggested.

The symposium was cosponsored by ASCO, the American Gastroenterological Association Institute, the American Society for Radiation Oncology, and the Society of Surgical Oncology.

The study was funded by ImClone Systems, a subsidiary of Eli Lilly and Co., which is developing ramucirumab. Some of Dr. Fuchs’ associates in the study disclosed employment or other financial relationships with ImClone Systems and stock ownership in Eli Lilly. Dr. Fuchs has been an advisor to Amgen, Bayer, Bristol-Myers Squibb, Genentech, Infinity Pharmaceuticals, Metamark Genetics, Momenta Pharmaceuticals, Pfizer, Roche, and Sanofi.

s.boschert@elsevier.com

On Twitter @sherryboschert

Results of a phase III trial support a common clinical practice – giving docetaxel as second-line chemotherapy to patients with advanced adenocarcinomas of the stomach or esophagus that progressed after first-line chemotherapy.

The randomized, controlled, open-label study showed significantly longer overall survival in 84 patients who received docetaxel (a median of 5.2 months), compared with 84 patients who received only "active symptom control" as second-line therapy (3.6 months), Dr. Hugo Ford reported. Active symptom control could include anything that the treating clinicians felt might be appropriate to manage symptoms, including radiotherapy, steroids, and supportive medications.

The finding bolsters previous, weaker evidence of survival benefit from second-line chemotherapy in these patients. Perhaps more important, though, is the current study’s finding of improved quality of life in patients who underwent second-line chemotherapy with docetaxel, compared with no second-line chemotherapy, he said.

Although scores for global quality of life and function did not differ significantly between groups, pain scores were significantly better in the treatment group than the control group, Dr. Ford said during a press briefing sponsored by the American Society for Clinical Oncology (ASCO).

"This is the first trial to show a quality of life benefit" from second-line chemotherapy in patients with esophagogastric cancer, "which is a very important finding in terms of informing patients about the likely benefits of the treatment we’re offering them," added Dr. Ford, director of cancer services at Addenbrooke’s Hospital, Cambridge, England. "Docetaxel should be a standard second-line treatment for esophagogastric adenocarcinoma."

He will present the findings in San Francisco on Jan. 24 at a meeting on gastrointestinal cancers sponsored by ASCO.

Clinicians in the United States and Europe commonly give second-line chemotherapy to patients with advanced esophagogastric cancers that progress after first-line treatment, despite a lack of strong evidence for the practice. Without second-line chemotherapy, the median survival time of patients who relapse after first-line chemotherapy for advanced esophagogastric adenocarcinoma is 3-4 months, previous data suggest.

Two separate trials recently reported small survival benefits from second-line chemotherapy using other drugs. A German study using irinotecan was too small (only 40 patients) to be considered robust evidence, Dr. Ford said. A Korean study used either irinotecan or docetaxel for second-line therapy but included only gastric cancers in patients who were Asian and younger and fitter than patients normally seen in U.S. practices, he added.

Paclitaxel also is used commonly as second-line chemotherapy for esophagogastric cancers and similar to docetaxel. Although there are no randomized data showing benefits from second-line paclitaxel, compared with supportive care, "one would be reasonable extrapolating a benefit there," he said.

The current trial enrolled patients with locally advanced or metastatic esophagogastric cancer who had a performance status of 0-2 and whose cancer had progressed within 6 months of first-line chemotherapy with platinum/fluoropyrimidine. Patients randomized to second-line docetaxel received IV 75 mg/m² every 3 weeks for up to six cycles.

Only 19 patients in the docetaxel group completed six cycles of the chemotherapy (23%); the median number of cycles was three per patient. Disease progression and toxicity were the main reasons for not completing six cycles. Grade 4 toxicity occurred in 18 patients on docetaxel (21%).

Nearly a third of patients in the docetaxel group received either one round or no chemotherapy, which points to the generally poor prognosis with this aggressive disease and the fact that a significant number of patients will not benefit from chemotherapy, Dr. Ford said.

"For me, it makes the case that in those people that are benefitting from chemotherapy, the benefits are probably more marked even than we saw in the trial," he said.

The study was unable to identify any subgroup as being less likely to benefit from second-line chemotherapy. Future studies may try to find ways to identify patients who won’t benefit from the treatment, he said.

"Docetaxel should be standard second-line treatment for esophagogastric adenocarcinoma, and we think it’s likely to be the standard arm against which future treatments should be compared," Dr. Ford said.

After second-line chemotherapy, 7% of patients had a partial response, and 46% had stable disease.

The median age in the study was 65 years, and 81% of patients were male. The performance status at randomization was 0 in 27% of patients, 1 in 57%, and 2 in 15%. A total of 46% of cancers were in the stomach, 34% were in the esophagogastric junction, and 20% were in the esophagus. The disease had metastasized in 86% of patients.

Disease progression occurred during primary chemotherapy in 43% of patients, within 3 months of finishing primary chemotherapy in 28%, and between 3 and 6 months after primary chemotherapy in 29% of patients.

Dr. Ford and his associates now are analyzing cost-effectiveness data collected during the study.

Approximately 39,000 new cases of esophagogastric cancer are diagnosed each year in the United States and 1.5 million cases worldwide, most commonly adenocarcinomas. All patients with esophagogastric adenocarcinoma who present with advanced disease and 60%-70% of patients who present with local disease will relapse after first-line chemotherapy.

The gastrointestinal cancers meeting, where Dr. Ford will present the results, is cosponsored by ASCO, the American Gastroenterological Association Institute, the American Society for Radiation Oncology, and the Society of Surgical Oncology.

The charity Cancer Research UK funded the study. Sanofi-Aventis, which makes docetaxel, provided the drug for free. Some of Dr. Ford’s associates in the study have been consultants or advisers to Sanofi and/or received honoraria or research funding from the company.

Results of a phase III trial support a common clinical practice – giving docetaxel as second-line chemotherapy to patients with advanced adenocarcinomas of the stomach or esophagus that progressed after first-line chemotherapy.

The randomized, controlled, open-label study showed significantly longer overall survival in 84 patients who received docetaxel (a median of 5.2 months), compared with 84 patients who received only "active symptom control" as second-line therapy (3.6 months), Dr. Hugo Ford reported. Active symptom control could include anything that the treating clinicians felt might be appropriate to manage symptoms, including radiotherapy, steroids, and supportive medications.

The finding bolsters previous, weaker evidence of survival benefit from second-line chemotherapy in these patients. Perhaps more important, though, is the current study’s finding of improved quality of life in patients who underwent second-line chemotherapy with docetaxel, compared with no second-line chemotherapy, he said.

Although scores for global quality of life and function did not differ significantly between groups, pain scores were significantly better in the treatment group than the control group, Dr. Ford said during a press briefing sponsored by the American Society for Clinical Oncology (ASCO).

"This is the first trial to show a quality of life benefit" from second-line chemotherapy in patients with esophagogastric cancer, "which is a very important finding in terms of informing patients about the likely benefits of the treatment we’re offering them," added Dr. Ford, director of cancer services at Addenbrooke’s Hospital, Cambridge, England. "Docetaxel should be a standard second-line treatment for esophagogastric adenocarcinoma."

He will present the findings in San Francisco on Jan. 24 at a meeting on gastrointestinal cancers sponsored by ASCO.

Clinicians in the United States and Europe commonly give second-line chemotherapy to patients with advanced esophagogastric cancers that progress after first-line treatment, despite a lack of strong evidence for the practice. Without second-line chemotherapy, the median survival time of patients who relapse after first-line chemotherapy for advanced esophagogastric adenocarcinoma is 3-4 months, previous data suggest.

Two separate trials recently reported small survival benefits from second-line chemotherapy using other drugs. A German study using irinotecan was too small (only 40 patients) to be considered robust evidence, Dr. Ford said. A Korean study used either irinotecan or docetaxel for second-line therapy but included only gastric cancers in patients who were Asian and younger and fitter than patients normally seen in U.S. practices, he added.

Paclitaxel also is used commonly as second-line chemotherapy for esophagogastric cancers and similar to docetaxel. Although there are no randomized data showing benefits from second-line paclitaxel, compared with supportive care, "one would be reasonable extrapolating a benefit there," he said.

The current trial enrolled patients with locally advanced or metastatic esophagogastric cancer who had a performance status of 0-2 and whose cancer had progressed within 6 months of first-line chemotherapy with platinum/fluoropyrimidine. Patients randomized to second-line docetaxel received IV 75 mg/m² every 3 weeks for up to six cycles.

Only 19 patients in the docetaxel group completed six cycles of the chemotherapy (23%); the median number of cycles was three per patient. Disease progression and toxicity were the main reasons for not completing six cycles. Grade 4 toxicity occurred in 18 patients on docetaxel (21%).

Nearly a third of patients in the docetaxel group received either one round or no chemotherapy, which points to the generally poor prognosis with this aggressive disease and the fact that a significant number of patients will not benefit from chemotherapy, Dr. Ford said.

"For me, it makes the case that in those people that are benefitting from chemotherapy, the benefits are probably more marked even than we saw in the trial," he said.

The study was unable to identify any subgroup as being less likely to benefit from second-line chemotherapy. Future studies may try to find ways to identify patients who won’t benefit from the treatment, he said.

"Docetaxel should be standard second-line treatment for esophagogastric adenocarcinoma, and we think it’s likely to be the standard arm against which future treatments should be compared," Dr. Ford said.

After second-line chemotherapy, 7% of patients had a partial response, and 46% had stable disease.

The median age in the study was 65 years, and 81% of patients were male. The performance status at randomization was 0 in 27% of patients, 1 in 57%, and 2 in 15%. A total of 46% of cancers were in the stomach, 34% were in the esophagogastric junction, and 20% were in the esophagus. The disease had metastasized in 86% of patients.

Disease progression occurred during primary chemotherapy in 43% of patients, within 3 months of finishing primary chemotherapy in 28%, and between 3 and 6 months after primary chemotherapy in 29% of patients.

Dr. Ford and his associates now are analyzing cost-effectiveness data collected during the study.

Approximately 39,000 new cases of esophagogastric cancer are diagnosed each year in the United States and 1.5 million cases worldwide, most commonly adenocarcinomas. All patients with esophagogastric adenocarcinoma who present with advanced disease and 60%-70% of patients who present with local disease will relapse after first-line chemotherapy.

The gastrointestinal cancers meeting, where Dr. Ford will present the results, is cosponsored by ASCO, the American Gastroenterological Association Institute, the American Society for Radiation Oncology, and the Society of Surgical Oncology.

The charity Cancer Research UK funded the study. Sanofi-Aventis, which makes docetaxel, provided the drug for free. Some of Dr. Ford’s associates in the study have been consultants or advisers to Sanofi and/or received honoraria or research funding from the company.

Results of a phase III trial support a common clinical practice – giving docetaxel as second-line chemotherapy to patients with advanced adenocarcinomas of the stomach or esophagus that progressed after first-line chemotherapy.

The randomized, controlled, open-label study showed significantly longer overall survival in 84 patients who received docetaxel (a median of 5.2 months), compared with 84 patients who received only "active symptom control" as second-line therapy (3.6 months), Dr. Hugo Ford reported. Active symptom control could include anything that the treating clinicians felt might be appropriate to manage symptoms, including radiotherapy, steroids, and supportive medications.

The finding bolsters previous, weaker evidence of survival benefit from second-line chemotherapy in these patients. Perhaps more important, though, is the current study’s finding of improved quality of life in patients who underwent second-line chemotherapy with docetaxel, compared with no second-line chemotherapy, he said.

Although scores for global quality of life and function did not differ significantly between groups, pain scores were significantly better in the treatment group than the control group, Dr. Ford said during a press briefing sponsored by the American Society for Clinical Oncology (ASCO).

"This is the first trial to show a quality of life benefit" from second-line chemotherapy in patients with esophagogastric cancer, "which is a very important finding in terms of informing patients about the likely benefits of the treatment we’re offering them," added Dr. Ford, director of cancer services at Addenbrooke’s Hospital, Cambridge, England. "Docetaxel should be a standard second-line treatment for esophagogastric adenocarcinoma."

He will present the findings in San Francisco on Jan. 24 at a meeting on gastrointestinal cancers sponsored by ASCO.

Clinicians in the United States and Europe commonly give second-line chemotherapy to patients with advanced esophagogastric cancers that progress after first-line treatment, despite a lack of strong evidence for the practice. Without second-line chemotherapy, the median survival time of patients who relapse after first-line chemotherapy for advanced esophagogastric adenocarcinoma is 3-4 months, previous data suggest.

Two separate trials recently reported small survival benefits from second-line chemotherapy using other drugs. A German study using irinotecan was too small (only 40 patients) to be considered robust evidence, Dr. Ford said. A Korean study used either irinotecan or docetaxel for second-line therapy but included only gastric cancers in patients who were Asian and younger and fitter than patients normally seen in U.S. practices, he added.

Paclitaxel also is used commonly as second-line chemotherapy for esophagogastric cancers and similar to docetaxel. Although there are no randomized data showing benefits from second-line paclitaxel, compared with supportive care, "one would be reasonable extrapolating a benefit there," he said.

The current trial enrolled patients with locally advanced or metastatic esophagogastric cancer who had a performance status of 0-2 and whose cancer had progressed within 6 months of first-line chemotherapy with platinum/fluoropyrimidine. Patients randomized to second-line docetaxel received IV 75 mg/m² every 3 weeks for up to six cycles.

Only 19 patients in the docetaxel group completed six cycles of the chemotherapy (23%); the median number of cycles was three per patient. Disease progression and toxicity were the main reasons for not completing six cycles. Grade 4 toxicity occurred in 18 patients on docetaxel (21%).

Nearly a third of patients in the docetaxel group received either one round or no chemotherapy, which points to the generally poor prognosis with this aggressive disease and the fact that a significant number of patients will not benefit from chemotherapy, Dr. Ford said.

"For me, it makes the case that in those people that are benefitting from chemotherapy, the benefits are probably more marked even than we saw in the trial," he said.

The study was unable to identify any subgroup as being less likely to benefit from second-line chemotherapy. Future studies may try to find ways to identify patients who won’t benefit from the treatment, he said.

"Docetaxel should be standard second-line treatment for esophagogastric adenocarcinoma, and we think it’s likely to be the standard arm against which future treatments should be compared," Dr. Ford said.

After second-line chemotherapy, 7% of patients had a partial response, and 46% had stable disease.

The median age in the study was 65 years, and 81% of patients were male. The performance status at randomization was 0 in 27% of patients, 1 in 57%, and 2 in 15%. A total of 46% of cancers were in the stomach, 34% were in the esophagogastric junction, and 20% were in the esophagus. The disease had metastasized in 86% of patients.

Disease progression occurred during primary chemotherapy in 43% of patients, within 3 months of finishing primary chemotherapy in 28%, and between 3 and 6 months after primary chemotherapy in 29% of patients.

Dr. Ford and his associates now are analyzing cost-effectiveness data collected during the study.

Approximately 39,000 new cases of esophagogastric cancer are diagnosed each year in the United States and 1.5 million cases worldwide, most commonly adenocarcinomas. All patients with esophagogastric adenocarcinoma who present with advanced disease and 60%-70% of patients who present with local disease will relapse after first-line chemotherapy.

The gastrointestinal cancers meeting, where Dr. Ford will present the results, is cosponsored by ASCO, the American Gastroenterological Association Institute, the American Society for Radiation Oncology, and the Society of Surgical Oncology.

The charity Cancer Research UK funded the study. Sanofi-Aventis, which makes docetaxel, provided the drug for free. Some of Dr. Ford’s associates in the study have been consultants or advisers to Sanofi and/or received honoraria or research funding from the company.