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Using AI, researchers pioneer a potential new immunotherapy approach for treating glioblastoma

by Medical Xpress
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Glioblastoma (histology slide). Credit: Wikipedia/CC BY-SA 3.0

In an innovative study of glioblastoma, scientists used artificial intelligence (AI) to reprogram cancer cells, converting them into dendritic cells (DCs), which can identify cancer cells and direct other immune cells to kill them.

Glioblastoma is the most common brain cancer in adults and also the deadliest, with less than 10% of patients surviving five years after their diagnosis. While new approaches such as immunotherapy have revolutionized treatment for other cancers, they have done little for patients with glioblastoma. That is partly because these hard-to-reach brain tumors hide behind the blood-brain barrier, where immune cells struggle to reach and eliminate them.

But new research, led by the Keck School of Medicine of USC, has leveraged AI to explore which genes control a cell’s fate—whether it develops into a heart cell, a lung cell or a cancer cell, for instance.

The researchers identified genes that can reprogram glioblastoma cells, converting them into immune cells within the tumor itself so they effectively target their kin for destruction.

In mouse models of glioblastoma, the approach increased the chances of survival by up to 75%. The results were published in Cancer Immunology Research.

“This groundbreaking study leverages the power of AI to transform glioblastoma cells into immune-activating cells, marking a significant advancement in cancer immunotherapy,” said the study’s lead author David Tran, MD, Ph.D., an associate professor of neurological surgery and neurology and division chief of neuro-oncology at the Keck School of Medicine.

“By turning the cancer’s own cells against it, we are paving the way for more effective treatments and offering new hope to patients battling this and many other aggressive cancers.”

In addition to their work in animal models, researchers used AI to identify a set of genes that can convert human glioblastoma cells into immune cells. In the future, scientists could deliver that to glioblastoma patients by embedding it within an innocuous virus, a tool known as a viral vector.

“Forcing a cell with 20,000 genes to become something else is incredibly complex. Using traditional molecular approaches, it would be almost impossible to do,” said Tran, who also co-directs the USC Brain Tumor Center at USC Norris Comprehensive Cancer Center. “AI is helping us answer some critical questions and gives us a powerful way to learn how to manipulate a cell’s fate.”

Controlling the fate of a cell

DCs play a central role in activating the immune response: They sample antigens (such as from a cancer cell) and present them to other , including armies of T-cells, effectively triggering a full-scale attack.

Evidence suggests that DCs can fight glioblastoma, but scientists have not yet found a reliable way to get them past the and into the hostile environment of a tumor. By reprogramming cancer cells already located within the tumor, Tran and his team have bypassed this major challenge.

When manipulating the fate of a cell, one important consideration is specificity. Converting healthy brain cells into DCs, for example, could shrink a brain tumor but cause health problems.

“We don’t want to give something to a patient that can convert all sorts of cells into DCs,” Tran said.

The he and his team developed was able to query tens of thousands of genes and millions of gene-to-gene connections and identify those that can specifically target glioblastoma cells and reprogram them to resemble DCs. This AI-driven method differs from previous research, which used what is known as an empirical approach to manually identify genes that control a cell’s fate.

“The high computational power of AI is really helping us accelerate the discovery process,” Tran said.

Used alongside other immunotherapies, reprogramming glioblastoma cells significantly enhanced the and survival rates in mouse models of glioblastoma. When combined with immune checkpoint therapy, the new approach improved the chance of survival by 75%.

When combined with a classic DC vaccine, the new approach doubled the chance of survival. (Used alone, neither immune checkpoint therapy nor a DC vaccine increased the chance of survival in patients with glioblastoma.)

Moving toward clinical trials

In addition to the proof-of-concept study in mice, the researchers used their AI system to identify a set of human genes that can convert human glioblastoma cells into cells resembling DCs. Next, they plan to fine-tune that list, package the genetic material into a viral vector and begin an initial round of safety and efficacy tests in animal models.

“We want to expand the search, using AI to help us find the best possible combinations as we move toward testing in patients,” Tran said.

If the approach is deemed safe and effective—meaning it improves outcomes for models and does not cause unexpected side effects—Tran and his team will apply for approval to begin clinical trials in patients in several years.

Down the line, they also hope to use their AI model to find genes that can reprogram other types of cancer cells to behave like DCs.

More information:
ianyi Liu et al, Machine Learning–Directed Conversion of Glioblastoma Cells to Dendritic Cell–like Antigen-Presenting Cells as Cancer Immunotherapy, Cancer Immunology Research (2024). DOI: 10.1158/2326-6066.CIR-23-0721

Citation:
Using AI, researchers pioneer a potential new immunotherapy approach for treating glioblastoma (2024, August 1)
retrieved 1 August 2024
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