Outcomes for melanoma patients have vastly improved thanks to new treatment options. However, those with high-risk disease who have their tumors surgically removed still have a substantial chance of relapse. A team of researchers from institutions across the United States, including Moffitt Cancer Center, launched a phase 2 clinical trial evaluating a new treatment option for this patient population. Their results, published in The New England Journal of Medicine, show that treating resectable stage 3 and 4 melanoma patients with the immunotherapy drug pembrolizumab both before and after surgery greatly improves outcomes when compared to pembrolizumab given only after surgery.
Pembrolizumab activates the immune system to target cancer cells for destruction. It is approved to treat many different types of cancer, including melanoma that cannot be surgically removed, or be given as a post-surgery (adjuvant) treatment option. The research team, as part of the Southwest Oncology Group, initiated the phase 2 trial to assess whether pembrolizumab given both before surgery (neoadjuvant) and as adjuvant therapy after surgery could improve outcomes of patients with melanoma that can be surgically removed, compared with the identical number of doses of pembrolizumab given entirely after surgery.
“The dramatic successes we’ve seen with drug treatments for melanoma have led us to use them earlier and earlier in the patient’s course. Neoadjuvant therapy brings the powerful drugs to bear on the tumor even before surgery and has a lot of potential advantages. But many surgeons were reluctant to put off surgery for fear that the tumor would grow or spread and they would miss the opportunity for surgical cure,” said Vernon Sondak, M.D., study co-author and chair of Moffitt’s Department of Cutaneous Oncology.
This trial included 313 patients with resectable stage 3 or 4 melanoma from 90 institutions across the U.S. All patients had tumors that were still present and measurable by CT scans. In other words, they could not have already had all their cancer removed prior to the start of the trial. Patients were randomized into two groups. The first group received pembrolizumab as both neoadjuvant (three doses before surgery) and adjuvant (15 doses after surgery) therapy, while the second group received all 18 doses of pembrolizumab after surgery. With a median follow-up of 14.7 months, the 154 patients in the neoadjuvant-adjuvant group had a significantly longer event-free survival than the 159 patients in the adjuvant only group. The two-year event-free survival rates were 72% in the neoadjuvant-adjuvant group versus 49% in the adjuvant only group. The treatment benefit was observed in all patient subgroups that were analyzed, including groups based on age, sex, performance status and stage of disease. Of particular note, there were fewer postsurgical recurrences in the patients in the neoadjuvant plus adjuvant group.
One concern with neoadjuvant therapy is the potential risk of tumor growth or developing toxicities that would prevent patients from undergoing surgery. In the neoadjuvant-adjuvant group, less than 10% of patients developed progressive disease or toxicities from pembrolizumab neoadjuvant therapy that prevented them from undergoing surgical removal of the tumor. Overall, the rates and types of adverse events were similar between the two treatment groups. The percentage of patients who developed grade 3 or 4 treatment-related adverse events during adjuvant therapy was 12% in the neoadjuvant-adjuvant group and 14% in the adjuvant only group.
“Our trial results shows that the timing of administration of an immune checkpoint inhibitor relative to surgery can have a large effect on patient outcomes. These new landmark data are practice-changing and will impact how clinicians treat patients with advanced melanoma that can be surgically removed. We have been using neoadjuvant therapy extensively for several years now, but these results exceeded even my lofty expectations,” Sondak said. “The next step is to use neoadjuvant therapy to lessen the amount of surgery patients might need and shorten the length of drug treatment they might otherwise require. We’re working on precisely that right now.”
This study was funded by the National Cancer Institute (U10CA180888, U10CA180819, U10CA180820, U0CA180821, U10CA180868, UG1CA233329, UG1CA233328, UG1CA233247, UG1CA233180, UG1CA189860, UG1CA233178, UG1CA233160, UG1CA189821, UG1CA233320, UG1CA233331, UG1CA189850, UG1CA233330, UG1CA233234, UG1CA233193, UG1CA189956, UG1CA239767, UG1CA189869, UG1CA180830, P30CA014089, UG1CA239758, P30CA016042, UG1CA189830, P30CA076292, P30CA033572, R35 CA197633 and P01 CA244118) and Merck Sharp and Dohme.
About Moffitt Cancer Center
Moffitt is dedicated to one lifesaving mission: to contribute to the prevention and cure of cancer. The Tampa-based facility is one of only 53 National Cancer Institute-designated Comprehensive Cancer Centers, a distinction that recognizes Moffitt’s scientific excellence, multidisciplinary research, and robust training and education. Moffitt’s expert nursing staff is recognized by the American Nurses Credentialing Center with Magnet® status, its highest distinction. With more than 7,800 team members, Moffitt has an economic impact in the state of $2.4 billion. For more information, call 1-888-MOFFITT (1-888-663-3488), visit MOFFITT.org, and follow the momentum on Facebook, Twitter, Instagram and YouTube.