Investigational drug with immunotherapy may provide new therapeutic opportunity for patients previously treated for kidney and lung cancer

Pegilodecakin with pembrolizumab and nivolumab shown to be safe in Phase 1B study

UNIVERSITY OF TEXAS M. D. ANDERSON CANCER CENTER

HOUSTON — Pegilodecakin, a first-in-class drug currently in clinical trials, has shown positive safety results and may offer a potential new treatment avenue for patients with non-small cell lung cancer (NSCLC) and kidney cancer. The study, led by The University of Texas MD Anderson Cancer Center, demonstrated that the drug, in combination with two leading anti-PD-1 monoclonal antibodies, pembrolizumab and nivolumab, achieved measurable responses for these patients.

IMAGE: THIS IS AUNG NAING, M.D. CREDIT: MD ANDERSON CANCER CENTER

Findings from a multi-center Phase Ib study was published in the Sept. 25 online issue of The Lancet Oncology.

“Pegilodecakin with anti-PD-1 monoclonal antibodies had a manageable toxicity profile and promising anti-tumor activity,” said Aung Naing, M.D., associate professor of Investigational Cancer Therapeutics. “Our study showed this combination demonstrated favorable response in NSCLC and kidney cancer patients who previously had been treated when compared to those treated with anti-PD-1 monoclonal antibodies alone.”

The study was designed to assess the safety, tolerability and maximal tolerated dose of pegilodecakin in combination with pembrolizumab or nivolumab, while also investigating biomarkers to identify patients likely to respond to treatment.

The study, which took place from February 2015 to September 2017, followed 111 kidney cancer, NSCLC and melanoma patients with advanced malignant solid tumors. The most common side effects were anemia, fatigue, low blood platelet counts and high triglycerides.

Objective responses were seen in 43% of NSCLC patients, 40% of kidney cancer patients and 10% of melanoma patients. Patients received pegilodecakin with pembrolizumab or nivolumab until disease progression, toxicity necessitating treatment discontinuation, patient withdrawal of consent or study end. Patients continued to receive combination therapy or pegilodecakin alone after disease progression if the investigator determined that the patient would continue to benefit.

Pegilodecakin is comprised of recombinant interleukin-10 (IL-10) which is linked to a molecule called polyethylene glycol (PEG). IL-10 is a protein that regulates activity of various immune cells, and high concentrations of IL-10 activate an immune response against cancer cells. The attachment of PEG to IL-10 increases its size, which prevents or delays its breakdown to prolong the time it circulates in the body.

The drug works by stimulating the survival, proliferation and “killing” potential of CD8+ T cells, known for their ability to recognize and destroy cancer cells. Increasing the amount of CD8+ T cells within the tumor is thought to improve prognosis and survival of the patient. The immune stimulatory effect of pegilodecakin complements the action of anti-PD-1 monoclonal antibodies that blocks the immune suppressive effect on T cells.

“The activity of pegilodecakin in combination with anti-PD-1 monoclonal antibodies introduces a new class of drugs to the treatment of advanced solid tumors,” said Naing. “Future randomized trials hopefully will determine the tolerability and clinical benefits of pegilodecakin as a single agent and in combinations in a range of cancers.”

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MD Anderson study team participants included Shubham Pant, M.D., of the Department of Investigational Cancer Therapeutics; Naval Daver, M.D., of the Department of Leukemia; Adi Diab, M.D., of the Department of Melanoma Medical Oncology; and Nizar Tannir, M.D., of the Department of Genitourinary Medical Oncology.

Other participating institutions included the David Geffen School of Medicine at the University of California Los Angeles; the Sarah Cannon Research Institute/Tennessee Oncology, Nashville. Tenn.; the University of California San Francisco; the Stephenson Cancer Center at the University of Oklahoma, Oklahoma City; the START Center for Cancer Care, San Antonio; Memorial Sloan Kettering Cancer Center, New York; ARMO Biosciences, Redwood City, Calif.; Eli Lilly and Company, New York; and Synthekine Inc., Menlo Park, Calif.

The study was funded by ARMO Biosciences. Naing received travel and accommodation reimbursement from ARMO in addition to research funding for this study.

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