Phosphatidylinositol 3-kinase (PI3K) is one of the most important signaling pathways regulating cell growth, migration and survival. When activated, the PI3K pathway contributes to tumor growth and resistance to therapy. It is why this pathway has become a target for several new cancer drugs, including ones to treat CLL.
For this study, Moffitt investigators used mouse models to evaluate three PI3K inhibitors: two that are Food and Drug Administration approved — idelalisib and duvelisib — and one investigational drug, umbralisib.
“Toxicities for this class of PI3K inhibitors are thought to be immune-mediated, but we know little about what is going on within the immune system to cause these reactions,” said Eva Sahakian, Ph.D., study author and research scientist in Moffitt’s Immunology Program. “Our study sought to answer that question, looking specifically at how these drugs suppressed regulatory T cells and other immune cells.”
Regulatory T cells (Tregs) are a small subset of cells that are actively involved in suppressing anti-tumor immune response through the targeting of other immune cells. They are thought to play a significant role in the progression of cancer and are generally increased in CLL patients.
The research team found that while all three PI3K inhibitors were effective in the treatment of CLL, idelalisib and duvelisib led to increased immune-mediated toxicities, as well as impaired function and a reduced number of Tregs. However, Treg volume and function were well maintained with umbralisib. The researchers believe this is because in addition to inhibiting PI3K, umbralisib is a dual inhibitor that also targets CK1ε, a protein essential to regulating cell division and tumor growth.
“Our findings show the immune-mediated adverse reactions seen in CLL patients following PI3K inhibitor therapy can be counteracted with the addition of CK1ε inhibition. The dual PI3K/ CK1ε inhibitor umbralisib offers an improved safety profile for CLL patients,” says Javier Pinilla-Ibarz, M.D., Ph.D., study author, senior member and head of the Lymphoma Section of the Malignant Hematology Department at Moffitt.
The researchers suggest dual PI3K/CK1ε inhibitor therapy could possibly be used in the treatment of other types of cancer. They would also like to investigate CK1ε inhibitor therapy by itself and in combination with other therapies once an investigational drug becomes available.
This work was supported in part through a sponsored research agreement with TG Therapeutics and funds from the National Institutes of Health (P30-CA076292) and the state of Florida.
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 51 National Cancer Institute-designated Comprehensive Cancer Centers, a distinction that recognizes Moffitt’s scientific excellence, multidisciplinary research, and robust training and education. Moffitt is a Top 10 cancer hospital and has been nationally ranked by U.S. News & World Report since 1999. Moffitt’s expert nursing staff is recognized by the American Nurses Credentialing Center with Magnet® status, its highest distinction. With more than 6,500 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.
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