How Immune Cells Survive Cancer Battles

Augmenting critical survival factors could help the body eliminate tumors

Colorful digital illustration showing T cells attacking a cancer cell

T cells attacking cancer cell. Image: royaltystockphoto/iStock/Getty Images Plus

The body’s immune system can recognize and attack cancer cells, but when cancer cells are able to overcome this assault malignant tumors develop in patients.

New research led by Harvard Medical School investigators at Massachusetts General Hospital has uncovered some of the key factors that are needed for survival of immune cells in the battle against cancer.

The findings, published in Cell, point to potential therapeutic targets that could tip the scales so that the immune system can effectively defeat aggressive cancers.

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Cytotoxic T lymphocytes (CTL) are the cells that recognize and destroy cancer cells, and they’re first activated in tumor-draining lymph nodes. From there, they enter the bloodstream to reach tumors and battle malignant cells.

Tumors, however, are hostile environments for CTLs. When researchers used imaging techniques to examine what goes on there, they found that to survive in tumors, CTLs must spend time in regions adjacent to blood vessels in the tissue surrounding cancer cells.

“Within these niches, they are able to interact with a highly activated population of so-called dendritic cells that provide survival signals that CTLs depend on,” explained senior author Thorsten Mempel, HMS professor of medicine and associate director of the Center for Immunology and Inflammatory Diseases at Mass General.

“Such signals, including the cytokine IL-15, enable CTLs to survive long enough to effectively eliminate cancer cells and, under ideal conditions, reject the tumors entirely,” Mempel said.
Mempel and his colleagues also wondered how CTLs find their way into these survival niches.

They suspected a major role for chemokines, which are chemotactic guidance factors that direct the migration of immune cells and help them find each other within tissues.

“We discovered that one chemokine called CXCL16 is highly expressed by those activated dendritic cells that occupy the blood vessel–associated niches, and that the receptor for this chemokine, called CXCR6, helps CTLs to accumulate in the niches and is thereby critical for their survival in tumors,” said lead author Mauro Di Pilato, assistant professor of immunology at the University of Texas MD Anderson Cancer Center.

This detailed understanding may help scientists develop more effective immunotherapies for patients with cancer.

In parallel studies, one of the research groups involved has already engineered CTLs to express more CXCR6. This alteration increased the cells’ ability to control tumor growth in animal models of cancer.

This work was funded by the National Institutes of Health, Melanoma Research Alliance, Melanoma Research Foundation, European Molecular Biology Organization, European Commission, German Research Foundation, Swiss National Science Foundation, and American Association of Cancer Research.

Adapted from a Mass General news release.