PHILADELPHIA - Radiotherapy destroys cancer cells using high-energy ionizing radiation to damage DNA and induce cell death. About two million patients per year in the United States – more than 50 percent of all cancer patients -- receive radiotherapy at some stage during their illness, either alone or in combination with chemotherapy, surgery, and targeted medicines.
Radiotherapy targets tumor cells but also causes damage to nearby healthy tissues. While this side effect has been improved by computer-assisted guidance, patients who receive radiation remain at high risk of losing bone density and suffering from broken bones within the radiation field during their lifetimes.
New research from Perelman School of Medicine at the University of Pennsylvania and the Children’s Hospital of Philadelphia may hold a clue to curtailing this feared side effect: suppressing a bone specific protein via its neutralizing antibody alleviates radiation-induced bone loss in an animal model. “Our study showed that activating the Wnt/b-catenin pathway can overcome radiation-induced DNA damage and death of bone-making cells,” said senior author Ling Qin, PhD, an associate professor of Orthopaedic Surgery at Penn. “This study has clinical relevance in that it demonstrates an antibody that can block sclerostin(Scl-Ab), a circulating factor that can inhibit bone formation, can ameliorate radiotherapy-induced osteoporosis.” The team published their findings in the Journal of Bone & Mineral Research.
A Phase II study underway at other centers using Romosozumab (Scl-Ab) for general osteoporosis is showing promise and this encouraged the team to determine whether weekly treatment with Scl-Ab could prevent radiotherapy-induced osteoporosis in mice.
They found that Scl-Ab blocked deterioration of trabecular, or spongy, bone after radiation by partially preserving the number and activity of bone-forming cells. Scl-Ab accelerated DNA repair in bone cells after radiation by reducing the number of DNA double-strand-break markers and increasing the amount of DNA-repair proteins. This protected the bone cells from turning on a radiation-induced, cell-death process.
Using cell-lineage tracing, the team demonstrated that radiation damage to progenitor bone cells mainly involves shifting their fate to become fat cells and stops their ability to proliferate, but not inducing cell death. Scl-Ab treatment partially blocked the lineage shift, but had no effect on the loss of proliferation potential.
Penn coauthors are Abhishek Chandra , Tiao Lin, Tiffany Young , Wei Tong , Xiaoyuan Ma, Wei-Ju Tseng, Yejia Zhang, Keith Cengel, and X. Sherry Liu, and Michael A. Levine at the Children’s Hospital of Philadelphia.
This study was supported in part by the National Institutes of Health (R01AR066098, R01DK095803, K01AR066743, P30AR050950, 1K08HD049598).
Penn Medicine is one of the world’s leading academic medical centers, dedicated to the related missions of medical education, biomedical research, excellence in patient care, and community service. The organization consists of the University of Pennsylvania Health System and Penn’s Raymond and Ruth Perelman School of Medicine, founded in 1765 as the nation’s first medical school.
The Perelman School of Medicine is consistently among the nation's top recipients of funding from the National Institutes of Health, with $550 million awarded in the 2022 fiscal year. Home to a proud history of “firsts” in medicine, Penn Medicine teams have pioneered discoveries and innovations that have shaped modern medicine, including recent breakthroughs such as CAR T cell therapy for cancer and the mRNA technology used in COVID-19 vaccines.
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