Partial Response to IPI?

COMBINATION REGIMENS

Combined anti-CTLA-4 and anti-PD-1 immunotherapy — The combined administration of anti-CTLA-4 immunotherapy with ipilimumab plus anti-PD-1 immunotherapy with nivolumab appears to have a higher level of anti-melanoma activity that either agent alone and has a manageable toxicity profile [53].

The combination was assessed in a phase I trial in which both drugs were given in successive dose escalation cohorts. In a concurrent therapy cohort, 53 patients with advanced melanoma were treated with both drugs once every three weeks for four doses. Nivolumab was then continued every three weeks through week 24. Subsequently, therapy with both drugs was continued once every 12 weeks for a maximum of eight additional doses. In a separate sequential cohort, nivolumab was given on the same schedule to 33 patients who had received prior ipilimumab.

In the concurrent treatment cohort, 21 of 52 evaluable patients (40 percent) had an objective response, and 16 of the 21 had an 80 percent or greater reduction in the tumor burden. Responses were ongoing in 19 of 21 patients at the time of data analysis, with duration of response up to 72 weeks. Evidence of clinical activity (stable disease or greater for at least 24 weeks) was observed in 65 percent of patients. In the sequenced therapy group (ie, nivolumab given after prior ipilimumab treatment), 6 of 30 patients had an objective response.

Among the patients treated with concurrent nivolumab plus ipilimumab, treatment-related adverse events were observed in 93 percent of cases. The most common events of any degree of severity were rash, pruritus, fatigue, and diarrhea (55, 47, 38, and 34 percent, respectively). Severe treatment related adverse events were reported in 49 percent of cases, including liver, gastrointestinal, and kidney toxicity (15, 9, and 6 percent of cases, respectively). Treatment was discontinued because of adverse events in 11 cases (21 percent).

Additional clinical experience and longer follow-up will be required to determine the optimal dose and schedule for concurrent immune checkpoint therapy as well as its role in the management of patients with advanced melanoma. A phase III trial is studying the combination of nivolumab plus ipilimumab compared with each of these other checkpoint inhibitors as a single agent (NCT01844505).

Ipilimumab plus GM-CSF — The addition of granulocyte-macrophage (GM) colony-stimulating factor (CSF) to ipilimumab was studied in a phase II trial conducted by Eastern Cooperative Oncology Group (ECOG).

In this trial, 245 patients with advanced melanoma were randomly assigned to ipilimumab plus GM-CSF or ipilimumab alone [54]. Ipilimumab was given at a dose of 10 mg/kg every three weeks for four cycles, followed by maintenance every 12 weeks. GM-CSF (250 micrograms/day subcutaneously) was given on days 1 to 14 of each 21 day cycle.

Results of this trial were presented at the 2013 American Society of Clinical Oncology (ASCO) meeting. At a median follow-up of 13 months, there was no difference in the objective response rate with or without GM-CSF (15.5 and 14.8 percent, respectively). There also was no significant difference in the progression-free survival (34.0 versus 29.6 percent at 6 months, hazard ratio [HR] 0.92, 95% CI 0.69-1.23). However, overall survival was significantly improved by the addition of GM-CSF (median 17.5 versus 12.7 months, one-year survival rates 69 versus 53 percent, HR 0.64, p = 0.014).

The addition of GM-CSF resulted in a significant reduction in the incidence of high grade adverse events, particularly related to pulmonary and gastrointestinal toxicity. The extent to which this decrease in toxicity contributed to the improved overall survival is unclear.

It is important to note that this trial used a higher dose of ipilimumab than is currently approved and that maintenance therapy was also included as a component of the protocol. The clinical implications of these results will require further study and confirmation.

OTHER IMMUNE REGULATORY CHECKPOINTS — Monoclonal antibodies targeted against a number of other regulatory checkpoints are being evaluated in patients with advanced melanoma based upon our current understanding of the development of cellular immunity.

4-1BB — 4-1BB (CD137) is a member of the tumor necrosis factor (TNF) family and acts as a costimulatory molecule that causes T cell proliferation. A humanized MAb, BMS-663513, targe

http://www.uptodate.com/contents/immunotherapy-of-advanced-melanoma-with-immune-checkpoint-inhibition

COMBINATION REGIMENS

Combined anti-CTLA-4 and anti-PD-1 immunotherapy — The combined administration of anti-CTLA-4 immunotherapy with ipilimumab plus anti-PD-1 immunotherapy with nivolumab appears to have a higher level of anti-melanoma activity that either agent alone and has a manageable toxicity profile [53].

The combination was assessed in a phase I trial in which both drugs were given in successive dose escalation cohorts. In a concurrent therapy cohort, 53 patients with advanced melanoma were treated with both drugs once every three weeks for four doses. Nivolumab was then continued every three weeks through week 24. Subsequently, therapy with both drugs was continued once every 12 weeks for a maximum of eight additional doses. In a separate sequential cohort, nivolumab was given on the same schedule to 33 patients who had received prior ipilimumab.

In the concurrent treatment cohort, 21 of 52 evaluable patients (40 percent) had an objective response, and 16 of the 21 had an 80 percent or greater reduction in the tumor burden. Responses were ongoing in 19 of 21 patients at the time of data analysis, with duration of response up to 72 weeks. Evidence of clinical activity (stable disease or greater for at least 24 weeks) was observed in 65 percent of patients. In the sequenced therapy group (ie, nivolumab given after prior ipilimumab treatment), 6 of 30 patients had an objective response.

Among the patients treated with concurrent nivolumab plus ipilimumab, treatment-related adverse events were observed in 93 percent of cases. The most common events of any degree of severity were rash, pruritus, fatigue, and diarrhea (55, 47, 38, and 34 percent, respectively). Severe treatment related adverse events were reported in 49 percent of cases, including liver, gastrointestinal, and kidney toxicity (15, 9, and 6 percent of cases, respectively). Treatment was discontinued because of adverse events in 11 cases (21 percent).

Additional clinical experience and longer follow-up will be required to determine the optimal dose and schedule for concurrent immune checkpoint therapy as well as its role in the management of patients with advanced melanoma. A phase III trial is studying the combination of nivolumab plus ipilimumab compared with each of these other checkpoint inhibitors as a single agent (NCT01844505).

Ipilimumab plus GM-CSF — The addition of granulocyte-macrophage (GM) colony-stimulating factor (CSF) to ipilimumab was studied in a phase II trial conducted by Eastern Cooperative Oncology Group (ECOG).

In this trial, 245 patients with advanced melanoma were randomly assigned to ipilimumab plus GM-CSF or ipilimumab alone [54]. Ipilimumab was given at a dose of 10 mg/kg every three weeks for four cycles, followed by maintenance every 12 weeks. GM-CSF (250 micrograms/day subcutaneously) was given on days 1 to 14 of each 21 day cycle.

Results of this trial were presented at the 2013 American Society of Clinical Oncology (ASCO) meeting. At a median follow-up of 13 months, there was no difference in the objective response rate with or without GM-CSF (15.5 and 14.8 percent, respectively). There also was no significant difference in the progression-free survival (34.0 versus 29.6 percent at 6 months, hazard ratio [HR] 0.92, 95% CI 0.69-1.23). However, overall survival was significantly improved by the addition of GM-CSF (median 17.5 versus 12.7 months, one-year survival rates 69 versus 53 percent, HR 0.64, p = 0.014).

The addition of GM-CSF resulted in a significant reduction in the incidence of high grade adverse events, particularly related to pulmonary and gastrointestinal toxicity. The extent to which this decrease in toxicity contributed to the improved overall survival is unclear.

It is important to note that this trial used a higher dose of ipilimumab than is currently approved and that maintenance therapy was also included as a component of the protocol. The clinical implications of these results will require further study and confirmation.

OTHER IMMUNE REGULATORY CHECKPOINTS — Monoclonal antibodies targeted against a number of other regulatory checkpoints are being evaluated in patients with advanced melanoma based upon our current understanding of the development of cellular immunity.

4-1BB — 4-1BB (CD137) is a member of the tumor necrosis factor (TNF) family and acts as a costimulatory molecule that causes T cell proliferation. A humanized MAb, BMS-663513, targe

http://www.uptodate.com/contents/immunotherapy-of-advanced-melanoma-with-immune-checkpoint-inhibition

COMBINATION REGIMENS

Combined anti-CTLA-4 and anti-PD-1 immunotherapy — The combined administration of anti-CTLA-4 immunotherapy with ipilimumab plus anti-PD-1 immunotherapy with nivolumab appears to have a higher level of anti-melanoma activity that either agent alone and has a manageable toxicity profile [53].

The combination was assessed in a phase I trial in which both drugs were given in successive dose escalation cohorts. In a concurrent therapy cohort, 53 patients with advanced melanoma were treated with both drugs once every three weeks for four doses. Nivolumab was then continued every three weeks through week 24. Subsequently, therapy with both drugs was continued once every 12 weeks for a maximum of eight additional doses. In a separate sequential cohort, nivolumab was given on the same schedule to 33 patients who had received prior ipilimumab.

In the concurrent treatment cohort, 21 of 52 evaluable patients (40 percent) had an objective response, and 16 of the 21 had an 80 percent or greater reduction in the tumor burden. Responses were ongoing in 19 of 21 patients at the time of data analysis, with duration of response up to 72 weeks. Evidence of clinical activity (stable disease or greater for at least 24 weeks) was observed in 65 percent of patients. In the sequenced therapy group (ie, nivolumab given after prior ipilimumab treatment), 6 of 30 patients had an objective response.

Among the patients treated with concurrent nivolumab plus ipilimumab, treatment-related adverse events were observed in 93 percent of cases. The most common events of any degree of severity were rash, pruritus, fatigue, and diarrhea (55, 47, 38, and 34 percent, respectively). Severe treatment related adverse events were reported in 49 percent of cases, including liver, gastrointestinal, and kidney toxicity (15, 9, and 6 percent of cases, respectively). Treatment was discontinued because of adverse events in 11 cases (21 percent).

Additional clinical experience and longer follow-up will be required to determine the optimal dose and schedule for concurrent immune checkpoint therapy as well as its role in the management of patients with advanced melanoma. A phase III trial is studying the combination of nivolumab plus ipilimumab compared with each of these other checkpoint inhibitors as a single agent (NCT01844505).

Ipilimumab plus GM-CSF — The addition of granulocyte-macrophage (GM) colony-stimulating factor (CSF) to ipilimumab was studied in a phase II trial conducted by Eastern Cooperative Oncology Group (ECOG).

In this trial, 245 patients with advanced melanoma were randomly assigned to ipilimumab plus GM-CSF or ipilimumab alone [54]. Ipilimumab was given at a dose of 10 mg/kg every three weeks for four cycles, followed by maintenance every 12 weeks. GM-CSF (250 micrograms/day subcutaneously) was given on days 1 to 14 of each 21 day cycle.

Results of this trial were presented at the 2013 American Society of Clinical Oncology (ASCO) meeting. At a median follow-up of 13 months, there was no difference in the objective response rate with or without GM-CSF (15.5 and 14.8 percent, respectively). There also was no significant difference in the progression-free survival (34.0 versus 29.6 percent at 6 months, hazard ratio [HR] 0.92, 95% CI 0.69-1.23). However, overall survival was significantly improved by the addition of GM-CSF (median 17.5 versus 12.7 months, one-year survival rates 69 versus 53 percent, HR 0.64, p = 0.014).

The addition of GM-CSF resulted in a significant reduction in the incidence of high grade adverse events, particularly related to pulmonary and gastrointestinal toxicity. The extent to which this decrease in toxicity contributed to the improved overall survival is unclear.

It is important to note that this trial used a higher dose of ipilimumab than is currently approved and that maintenance therapy was also included as a component of the protocol. The clinical implications of these results will require further study and confirmation.

OTHER IMMUNE REGULATORY CHECKPOINTS — Monoclonal antibodies targeted against a number of other regulatory checkpoints are being evaluated in patients with advanced melanoma based upon our current understanding of the development of cellular immunity.

4-1BB — 4-1BB (CD137) is a member of the tumor necrosis factor (TNF) family and acts as a costimulatory molecule that causes T cell proliferation. A humanized MAb, BMS-663513, targe

http://www.uptodate.com/contents/immunotherapy-of-advanced-melanoma-with-immune-checkpoint-inhibition

Janet, 

rumor has it that Dr Weber (Moffitt) has a few slots in a new PD1 trial. People have certainly seen great success when it works. I had at best, a partial response. I am now on dabrafenib/Mekinist (and v600d), not sure if it's working, should find out soon, but this is certainly an option. Unfortunately partial responses are not uncommon with any of these drugs.  

Blessings, 

Amy

Janet, 

rumor has it that Dr Weber (Moffitt) has a few slots in a new PD1 trial. People have certainly seen great success when it works. I had at best, a partial response. I am now on dabrafenib/Mekinist (and v600d), not sure if it's working, should find out soon, but this is certainly an option. Unfortunately partial responses are not uncommon with any of these drugs.  

Blessings, 

Amy

Janet, 

rumor has it that Dr Weber (Moffitt) has a few slots in a new PD1 trial. People have certainly seen great success when it works. I had at best, a partial response. I am now on dabrafenib/Mekinist (and v600d), not sure if it's working, should find out soon, but this is certainly an option. Unfortunately partial responses are not uncommon with any of these drugs.  

Blessings, 

Amy