How Oxygen Deprivation Drives Cancer Metastasis


Low oxygen (hypoxia) in tumors triggers changes that help cancer cells spread and survive.

How Oxygen Deprivation Drives Cancer Metastasis

Researchers at the Johns Hopkins Kimmel Cancer Center have identified 16 genes that enable breast cancer cells to survive in the bloodstream after escaping the low-oxygen areas of a tumor. Each of these genes presents a potential target for therapies to prevent cancer recurrence, with one gene, MUC1, already in clinical trials. The research was published in the journal Nature Communications (1 Trusted Source
Hypoxia induces ROS-resistant memory upon reoxygenation in vivo promoting metastasis in part via MUC1-C

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Deep in a tumor, full of rapidly dividing cells, cancer cells are faced with a lack of oxygen, a condition called hypoxia. Cancer cells that survive these tough environments end up seeking what they missed, slowly making their way to the oxygen-rich bloodstream and often seeding metastasis elsewhere in the body, explains lead study author Daniele Gilkes, Ph.D., an assistant professor of oncology at Johns Hopkins.

Uncovering Survival Genes

The team identified 16 genes responsible for this protection from reactive oxygen species, “which is a stress that occurs when the cells enter the bloodstream,” Gilkes says. “Although the hypoxic cells are localized in what we call the perinecrotic region of a tumor – meaning they’re sitting right next to dead cells – we think that they’re able to migrate into higher [oxygen] levels where they can actually find the bloodstream,” she says. “Cells able to survive super-low oxygen concentrations do a better job of surviving in the bloodstream. This is how, even after a tumor is removed, we sometimes find that cancer cells have set up elsewhere in the body. Lower levels of oxygen in a tumor correlate with worse prognosis.”

In laboratory studies, Gilkes’ team color-coded hypoxic cells green, then applied a technique called spatial transcriptomics to identify which genes were turned on in the perinecrotic region, and that stayed on when the cells migrated to more oxygenated tumor regions. They compared cells in the primary tumors of mice with those that had entered the blood stream or the lungs. A subset of hypoxia-induced genes continued to be expressed long after cancer cells escaped the initial tumor.

“The results suggest the potential for a sort of memory of exposure to hypoxic conditions,” says Gilkes.

The new research showed a disparity between what occurs in laboratory models and what happens in the human body, solving a mystery that was puzzling scientists. When cells in a dish are hypoxic and returned to high levels of oxygen in a short time, they tend to stop expressing the (hypoxia-induced) genes and go back to normal. However, in tumors, hypoxia can be more of a chronic condition, not acute. When Gilkes’ team exposed cells to hypoxia for a longer period – five days was usually enough – they mimicked what was happening in the mouse models.

Results were particularly predictive for triple-negative breast cancer (TNBC), which has a high rate of recurrence. The researchers found that patient biopsies from TNBC that had recurred within three years had higher levels of a protein called MUC1.

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As part of their research model, Gilkes and team blocked MUC1 using a compound called GO-203 to see if it would reduce the spread of breast cancer cells to the lung. Their aim was to specifically eliminate aggressive, post-hypoxic metastatic cells.

“If we reduced the level of MUC1 in these hypoxic cells, they were no longer able to survive in the bloodstream or in presence of reactive oxygen species, and they formed fewer metastases in mice,” Gilkes says. However, there are other factors at play, she says, and additional research will be needed to see if this finding is true across cancer types.

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A phase I/II clinical trial targeting MUC1 for patients with advanced cancers across a variety of solid tumor types – including those found in breast, ovarian, and colorectal cancer – is ongoing, Gilkes says.

Reference:

  1. Hypoxia induces ROS-resistant memory upon reoxygenation in vivo promoting metastasis in part via MUC1-C – (https://www.nature.com/articles/s41467-024-51995-2)

Source-Eurekalert



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