Treg cells within the immune system work to suppress immune function and when Tregs suppress the immune response, it ceases the cancer-fighting effect.

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Eliminating suppressive Treg cells from the immune system can make the cells even more suppressive.
But eliminating the Tregs doesn't help. Researchers have tried, but a clinical trial testing that idea showed no benefit to patients.
Now, more than a decade after discovering the immunosuppressive role of Tregs in human cancer, a new study published in Nature Immunology finds that eliminating the Treg cells doesn't eliminate their suppressive qualities.
When the Tregs die, instead of being negated, they become even more suppressive. All the cells are dead but the machine is still running.
"It's a double-edged sword: If they do not die, they are suppressive. But if they die, they are even more suppressive," says senior study author Weiping Zou, M.D., Ph.D., Charles B. de Nancrede Professor of surgery, immunology, pathology and cancer biology at the University of Michigan.
Immunotherapy has revolutionized cancer treatment, but limitations and questions remain. One of the biggest questions is why such a small number of patients are responsive.
It turns out, this new study finds, that when Treg cells die, they release a lot of small metabolites called ATP. Usually ATP helps supply the body with energy. But dying Tregs quickly convert ATP to adenosine.
The adenosine then targets T-cells, binding to a receptor on the T-cell surface. This affects the function of the T-cells, making them unhealthy.
Tregs travel to the tumor from throughout the body, which explains Zou's earlier finding that there are many Tregs in a tumor. But while the Tregs proliferate, at the same time they are dying fast. So there are a many Tregs but also many dying Tregs.
Researchers will next look for ways to limit this function by creating a roadblock to prevent the cells from migrating to the tumor microenvironment. They will also investigate options to block or control the suppressive activity.
Source-Eurekalert
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