New discovery offers hope for stopping childhood brain tumors before they start

Scientists at The Hospital for Sick Children (SickKids) have discovered a way to stop tumor growth before it starts for a subtype of medulloblastoma, the most common childhood malignant brain cancer. 

Brain cancer presents a unique set of challenges for researchers – by the time a person experiences symptoms, the tumors are often so complex that the fundamental mechanisms driving the tumor growth are no longer easy to identify. A research team led by Dr. Peter Dirks is working to combat this challenge for sonic hedgehog (SHH) medulloblastoma. 

In a new study published in Nature Communications, the researchers identify that a protein is responsible for the waking up of ‘sleeping’ stem cells and driving SHH medulloblastoma tumor formation and regrowth. By blocking this protein and preventing the stem cells from waking, the study demonstrates what could be a pivotal treatment strategy for the cancer, utilizing cutting-edge genomic approaches in combination with functional experiments in a preclinical model. 

Our findings offer a novel strategy to target cancer stem cells, providing hope for more effective treatments against aggressive brain tumors.”

Dr. Peter Dirks, Senior Scientist in the Developmental, Stem Cell & Cancer Biology program and Chief of the Division of Neurosurgery

Cancer interception in action 

The research team began by examining cellular transitions that drove the development of SHH medulloblastoma tumors. They found that early in tumor development and after conventional treatments, a protein called OLIG2 would activate ‘sleeping’ stem cells, causing them to divide and grow into a tumor. 

“There is order to how the cancer initiating stem cells undergo fate changes to form tumors. We can target an early transition event and intercept the entire process – essentially stopping the cancer in its earliest form,” says first author Dr. Kinjal Desai, a postdoctoral researcher in the Dirks lab. 

During these transitions, the researchers uncovered a key window during which tumor progression could be blocked. By combining a previously established treatment with a small molecule called CT-179, which disrupts the OLIG2 protein, the research team were able to target the residual stem cells left after treatment and prevent them from re-awakening, effectively preventing tumor relapse. 

Similarly for early-stage SHH medulloblastoma, CT-179 prevented the tumor from forming and significantly increased survival rates in the preclinical model. 

Together with additional preclinical models in a study published simultaneously in Nature Communications from colleagues at Children’s Healthcare of Atlanta and QIMR Berghofer Medical Research Institute in Australia, the findings showcase what could be an effective new treatment for SHH medulloblastoma, as well as other brain cancers including diffuse intrinsic pontine glioma (DIPG). 

The study complements recent research from the Dirks Lab in Nature, which describes the early stages of glioblastoma development. While future research will expand these findings into clinical trials for patients, particularly among those being monitored for relapse, the Dirks lab, part of the Arthur and Sonia Labatt Brain tumor Research Centre (BTRC), is excited for the diagnostic potential this discovery presents. 

“At SickKids, we’re already genetically testing every child with cancer to inform their diagnosis and treatments – our study goes beyond genetic testing to precision biology,” says Dirks. “I am excited for a future where this ‘magic bullet’ for early treatment could be combined with diagnostic tests to potentially prevent the cancer from developing at all.” 

This study is funded by Canadian Institutes of Health Research (CIHR), Ontario Institute for Cancer Research, Terry Fox Research Institute, Canadian Cancer Society, Cancer Research UK, Stand Up to Cancer, Jessica’s Footprint Foundation, Hopeful Minds Foundation, b.r.a.i.n.child, Meagan’s Walk, Garron Family Cancer Centre, the Bresler family, and SickKids Foundation.