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“We performed the first-ever cost effectiveness analysis in acquired TTP and found that the addition of caplacizumab to standard of care treatment is not cost effective at its current drug pricing,” said George Goshua, MD, lead author of the study and a clinical fellow in the Hematology/Oncology fellowship training program at YCC. “This raises the question: Are we doing the right thing for our patients, for our community, and for our health system?”
TTP is a life-threatening, rare blood disorder where blood clots form in small blood vessels throughout the body. The clots can limit or block the flow of oxygen-rich blood to the body’s organs, such as the brain, kidneys, and heart. Caplacizumab, the first drug approved by the U.S. Food and Drug Administration for treatment of TTP, is used in combination with plasma exchange and immunosuppressive therapy to treat the disorder.
In the study, to analyze the cost effectiveness of adding caplacizumab to standard of care (SOC) in acquired TTP, Goshua and his colleagues developed several cost models using data from two major clinical trials studying TTP (TITAN and HERCULES). The models incorporated the cost of caplacizumab and other SOC treatments for TTP, including therapeutic plasma exchange, the immunosuppressive medication rituximab, number of days in the hospital and in the intensive care unit, TTP recurrence rates, and deaths. In both the TITAN and HERCULES trials, the addition of caplacizumab to SOC yielded a higher cost of treatment, and an improvement in quality-adjusted life years, compared to SOC alone. The incremental cost effectiveness ratio for adding caplacizumab to SOC versus SOC alone was $1.5 million dollars at 5 years with a 95% confidence interval of $1.3-1.7 million, far above the current U.S. standard of $195,330.
“We hope to conduct additional studies utilizing longer-term follow-up data once they become available to assess the full impact of caplacizumab on the cost of treating TTP,” added Goshua. “In the short term these patients do have increased relapses and more bleeding with the use of caplacizumab in the clinical trials, so we need to be conscious of the fact that we do not know enough in the TTP field about the long-term effects of caplacizumab.”
Senior author on the paper is Alfred Ian Lee, MD, PhD. Co-authors on the paper include Jeanne E. Hendrickson, MD, Christopher Tormey, MD, Pranay Sinha, MD, and Pavan K. Bendapudi, MD.
The study was funded by a donation from Jack Levin to the Benign Hematology program at Yale, a grant from the National Institutes of Health, and the Luick Family Fund of Massachusetts General Hospital.
About Yale Cancer Center and Smilow Cancer Hospital Yale Cancer Center (YCC) is one of only 51 National Cancer Institute-designated comprehensive cancer centers in the nation and the only such center in Connecticut. Cancer treatment for patients is available at Smilow Cancer Hospital through 13 multidisciplinary teams and at 15 Smilow Cancer Hospital Care Centers in Connecticut and Rhode Island. Comprehensive cancer centers play a vital role in the advancement of the NCI’s goal of reducing morbidity and mortality from cancer through scientific research, cancer prevention, and innovative cancer treatment.
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