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Unexpected immune response may hold key to long-term cancer remission

by Medical Xpress
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From left to right: Co-authors Weilin Li, Tom Enbar, Li Tang, and Lucia Bonati. Credit: Alain Herzog

Results from a preclinical study in mice led by EPFL, and a collaborative clinical study in patients show that the type 2 immune response—associated with parasitic infection and thought to play a negative role in cancer immunity—is positively correlated with long-term cancer remission.

In 2012, 7-year-old Emily Whitehead became the first pediatric patient to receive pioneering (CAR-T) therapy to fight the recurrence of acute lymphoblastic leukemia (ALL). Twelve years later, Emily is in remission and a student at the University of Pennsylvania, where the therapy was developed. But for many others, the fight continues: More than half of ALL patients experience a relapse within one year following CAR-T therapy.

Now, samples from the same pioneering have been used in a new study, recently published in Nature in collaboration with EPFL, Yale University, University of Pennsylvania and Cleveland Clinic, that could again signal a paradigm shift in .

“For this study, the goal was to determine if the CAR-T cells of long-surviving ALL patients like Emily had a certain profile, or signature, that distinguished them from patients who relapsed,” explains Li Tang, head of the Laboratory of Biomaterials for Immunoengineering in EPFL’s School of Engineering.

In CAR-T therapy, called T cells are extracted and engineered to express certain proteins that better target a patient’s . The modified CAR-T cells are then transferred back to the patient, with some retained for research.

For the Nature study, scientists used nearly 700,000 CAR-T cells from 82 ALL patients, plus six healthy controls, and created a gene expression atlas to analyze each individual cell. This atlas showed that the cells of long-term ALL survivors indeed had something special: They contained certain proteins—notably the cytokine IL-4, among others—usually associated with something called a type 2 immune response.

Unlike a type 1 immune response, which has traditionally been the target of cancer therapies like CAR-T, type 2 responses are mobilized to fight parasitic immune threats like worms.

Until now, researchers thought that type 2 immune factors were not useful in fighting cancer, and could even promote tumor growth. But the cell atlas data showed otherwise. The researchers notably observed a statistically significant correlation between the presence of type 2 immune factors and eight-year relapse-free remission from ALL.

Unexpected immune response may hold key to long-term cancer remission
Single-cell atlas of 695,819 CAR T cells from 82 patients and 6 HDs. Credit: Nature (2024). DOI: 10.1038/s41586-024-07762-w

An energy boost in the race against cancer

Tang emphasizes that the results of the cell atlas study, while significant, are correlational. “We did not show a causal relationship between type 2 immunity and cancer remission,” he says. But a second study, led by Tang’s lab and simultaneously published in Nature, suggests that IL-4 may alter the metabolism of T cells, “reinvigorating” them as they fight tumors.

For this second study, designed to investigate the mechanism of type 2 immunity, the researchers compared the effect of type 1 CAR-T immunotherapy alone with that of a combined type 1/type 2 immunotherapy on tumors in mice. This combined therapy included a modified, longer-lasting version of the IL-4 cytokine.

The mice receiving the combined treatment not only had a greater curative response rate (86%), but also showed improved survival even after their immune systems were re-challenged with cancer cells, thanks to immune memory.

Closer analysis of these data revealed that the modified IL-4 appeared to be promoting glycolysis—an essential metabolic pathway that provides energy to cells. Like a carbohydrate snack in the middle of a marathon, the researchers theorize that type 2 immunity factors like IL-4 give exhausted T cells an energy boost, revitalizing their ability to fight cancer.

“We wanted to see if we could harness type 2 immunity to enhance current immunotherapy, which is all type 1-centric. Our results show that type 1 and type 2 immunity can be thought of in terms of synergy, like yin and yang,” Tang says.

“Our study not only sheds light on the synergy between these two types of , but also unveils an innovative strategy for advancing next-generation cancer immunotherapy by integrating type 2 immune factors.

“Overall, I hope that these two studies—one preclinical mechanistic and one clinical—will inspire the field to challenge the type 1-centric paradigm in cancer immunotherapy, and re-examine the role of type 2 immunity.”

More information:
Zhiliang Bai et al, Single-cell CAR T atlas reveals type 2 function in 8-year leukaemia remission, Nature (2024). DOI: 10.1038/s41586-024-07762-w

Bing Feng et al, The type 2 cytokine Fc–IL-4 revitalizes exhausted CD8+ T cells against cancer, Nature (2024). DOI: 10.1038/s41586-024-07962-4

Citation:
Unexpected immune response may hold key to long-term cancer remission (2024, September 26)
retrieved 26 September 2024
from https://medicalxpress.com/news/2024-09-unexpected-immune-response-key-term.html

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