Western Regional Blog – BC, YK, AB, NWT and Nunavut
A new combination therapy developed by researchers at the Roswell Park Cancer Institute has showed positive results in 60% of women with recurrent ovarian cancer. To develop the new therapy, researchers took advantage of the fact that ovarian cancer cells have abnormally high a marker called NY-ESO-1 on their surfaces. Researchers gave patients a drug called decitabine to boost NY-ESO-1 levels, and then gave patients a vaccine that tells the patient’s immune system to destroy any tissue showing high levels of the marker NY-ESO-1. Done in combination with chemotherapy, 60% of women tested showed stable disease for several months following treatment. (OCNA http://www.ovariancancer.org/2014/01/07/new-combination-therapy-for-ovarian-cancer-shows-positive-results-in-phase-i-clinical-trials/)
Recurrent ovarian cancers respond to cancer vaccine after ‘reprogramming’ with decitabine
Treatment with the drug decitabine prior to administration of chemotherapy and a cancer vaccine yielded clinical benefit for women with recurrent ovarian cancer, suggesting that this combinatorial chemoimmunotherapy may provide a new treatment option for patients with this disease, according to a study published in Cancer Immunology Research, a journal of the American Association for Cancer Research.
A prerequisite for a patient’s immune system to recognize and attack his or her tumor is the presence of high levels of a protein not normally found in the patient’s healthy cells. Proteins with this profile are called tumor antigens and can be good targets for anticancer vaccines.
“NY-ESO-1 is one of the few tumor antigens that have restricted expression in normal tissues but become aberrantly expressed in epithelial ovarian cancers and other solid tumors, so we focused on this antigen as the lead candidate for development of cancer immunotherapy,” said Kunle Odunsi, M.D., Ph.D., principal investigator of the study, the M. Steven Piver professor and chair of the Department of Gynecologic Oncology, and director of the Center for Immunotherapy at Roswell Park Cancer Institute in Buffalo, N.Y. “However, we observed that this antigen is not uniformly expressed by epithelial ovarian cancers, so our goal was to force the expression of NY-ESO-1 on ovarian cancer cells in order to allow the immune system to recognize and attack them.
“Expression of NY-ESO-1 is regulated by an epigenetic process called DNA methylation. Therefore, we tested the hypothesis that epigenetic reprogramming of NY-ESO-1 using the demethylating agent decitabine will augment vaccine-induced immunity,” he added. “Although clinical results were not a focus of this phase I trial, we saw evidence of clinical benefit in up to 60 percent of the patients with chemotherapy-resistant tumors. The combination of a demethylating agent, chemotherapy, and cancer vaccine may have enabled this remarkable effect.”
Odunsi and colleagues conducted a phase I dose-escalation trial of decitabine, to which they recruited 12 women with epithelial ovarian cancer that had not responded to multiple lines of chemotherapy, with an estimated progression-free survival time of three months. All patients received decitabine on day one, the chemotherapy drug doxorubicin on day eight, and the cancer vaccine (NY-ESO-1 protein with Montanide and GM-CSF) on day 15.
In preclinical analysis reported as part of this study, the investigators established the best sequence of drug administration: decitabine was effective only when administered before chemotherapy, and it was ineffective if given after chemotherapy; vaccine administration was the last step.
The clinical trial participants were randomly assigned to receive a low, middle, or high dose of decitabine.
Of the 10 patients evaluable for clinical response, five had stable disease for up to 7.8 months, and one had a partial response with disease remission that lasted 5.8 months. All patients from the low- and middle-dose cohorts of decitabine showed clinical benefit, whereas one-third of the patients who received the high dose showed benefit. These data suggest that lower doses of decitabine are associated with improved clinical response using this regimen. The treatment was well tolerated, and adverse events included hematologic side effects that were clinically manageable, according to Odunsi.
“One of the most remarkable results in terms of immune responses was that we were able to evoke what we call ‘antigen spreading,'” he said. “Although we immunized against a single target [NY-ES0-1], we analyzed and found that we were able to induce immune responses against three other antigens, against which we did not immunize.
“We propose that patients should actively seek these kinds of combination therapies. Even though the majority of these types of therapies are experimental at this point, there is enough scientific and clinical evidence to indicate that they are likely to be beneficial,” Odunsi added.
To this end, Odunsi and Adam R. Karpf, Ph.D., a co-principal investigator of the study and associate professor at the Eppley Institute and member of the Fred and Pamela Buffett Cancer Center in the University of Nebraska Medical Center in Omaha, are currently planning a phase II trial at Roswell Park Cancer Institute and the Fred and Pamela Buffett Cancer Center to test whether this treatment approach lengthens progression-free survival in patients with ovarian cancer.