A microscopic
view of a slow-growing breast cancer tumor that has shrunk in response to
standard hormone therapy and a new experimental Rac1 inhibitor. Credit: Caldon
Lab, Garvan Institute
A new study by the Garvan Institute of Medical Research has uncovered a
hidden mechanism explaining why breast cancer can return many years after
successful treatment. Published in Nature Communications, the research
reveals rogue cells that change their programming to allow them to divide at a
remarkably slow pace, meaning they could form microscopic tumors that silently
tick away in distant organs, evading detection for decades.
This research addresses a major challenge for patients with estrogen
receptor-positive (ER+) breast cancer, where the possibility of relapse can
linger for years after being declared cancer-free. Even after five to 10 years
of initial hormone therapy, up to 30% of patients develop incurable relapse,
heavily contributing to the more than 3,300 women who die from breast cancer in
Australia every year.
Relapse is known to be caused by cancer cells lying dormant in the bone or
other organs before "waking up" to cause metastasis. The new research
provides evidence on a parallel pathway by which stealthy cancer cells develop
into secondary tumors—findings which could uncover new approaches to prevent
metastasis.
"We have become very good at treating primary breast cancer, but late
relapses remain a major challenge," says Associate Professor Liz Caldon,
Lab Head at the Garvan Institute and senior author of the study.
"While we know some cancer cells can go into a state of complete
hibernation, we characterized an important alternative pathway that enables
cells to never truly stop dividing during treatment. Instead, they survive by
growing extremely slowly in the background, until a tiny speck becomes a
pebble."
Even though these cancer cells are slow-growing, they are far from
harmless. Once these "micrometastases"—tiny secondary tumors—cross
the threshold of detection or disrupt a vital organ like the brain or bone,
they can become a life-threatening relapse that is notoriously resistant to
chemotherapy.
"For a long time, the idea that extremely slow-growing cells could
drive relapse was just a theory. We've found evidence for the way this could
happen in ER-positive breast cancer. By identifying the pathways that are
important in these slow-growing cells we have a new lever to potentially
prevent these deadly outcomes," Associate Professor Caldon says.
Escaping therapy by slowing down
While standard hormone treatments are highly effective at clearing out the
vast majority of active breast cancer cells, a tumor is not uniform. The
researchers found that some cancer cells naturally divide at a very
slow rate when treated with therapy, and the slow rate inadvertently protects
them from treatment.
As the treatment successfully neutralizes the fast-growing cancer cells,
these slow-growing survivors are left behind to cause cancer relapse down the
track.
To understand this process, the team spent years isolating and cultivating
exceptionally slow-growing breast cancer cells in the laboratory. When they
introduced these cells into preclinical models, they discovered that a slow
growth rate did not limit the cancer's ability to spread throughout the body.
"It took years to isolate these specific cells because they were
dividing so slowly, almost in defiance of how we typically expect cancer to
behave. But once we observed them in action, we realized that a slow clock
doesn't mean a stopped clock," says Kristine Fernandez, Senior Research
Assistant in the Caldon Lab and first author of the study.
"These cells were migrating to organs like the bone and
lungs, proving that speed isn't everything when it comes to metastasis."
A new target for treatment
The researchers then pinpointed what drives these slow-growing cells—a
cellular communication channel known as the Rac1 pathway. Rac1 is
critical for cell movement, structure, and survival. By using advanced
biosensor imaging, the team visualized the Rac1 pathway activating inside live,
slow-growing cancer cells.
Importantly, the researchers demonstrated that blocking this pathway could
effectively shrink the cancer. Using experimental Rac1 inhibitors, the team
successfully reduced the overall size and number of tumors present in
patient-derived lab models of breast cancer.
Looking ahead, the Caldon Lab is launching new investigations to determine
if Rac1 inhibitors could be used preventatively to stop the cancer coming back.
"If we can understand the specific biology of these slow-growing cells, we might eventually be able to offer better ways to track whether a decade of hormone therapy is actually working and ultimately prevent recurrence for patients living with the threat of relapse," says Associate Professor Caldon.
Provided by Garvan Institute of Medical Research
Source: Slow-dividing breast cancer cells may explain relapses decades after treatment
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