Finding by Montefiore Einstein
Comprehensive Cancer Center Could Point to New
Approach
for Preventing or Treating Metastatic
Disease
BRONX,
N.Y., Oct. 7, 2024 /PRNewswire/ -- Metastatic
disease—when cancer spreads from the primary tumor to other parts
of the body—is the cause of most cancer deaths. While researchers
understand how cancer cells escape the primary site to seed new
tumors, it's not well understood why some of these wayward cancer
cells spawn new tumors— sometimes decades later—while others do
not.
Now, a research team at the National Cancer Institute-designated
Montefiore Einstein Comprehensive Cancer Center (MECCC) has
discovered a natural immune mechanism in mice that stops escaped
cancer cells from developing into tumors elsewhere in the body. The
findings were published today in the journal Cell.
"Preventing or curing metastases is the most critical challenge
in cancer," said study leader Julio
Aguirre-Ghiso, Ph.D., director of MECCC's Cancer Dormancy
Institute. "We think our findings have the potential to point to
new therapies to prevent or treat metastatic disease." The study's
co-first authors are Erica Dalla,
Ph.D., a former student, and Michael
Papanicolaou, Ph.D., a postdoctoral fellow in Dr.
Aguirre-Ghiso's lab.
The Role of Dormancy in Cancer
Cells that migrate from
primary tumors and seed metastatic tumors are called disseminated
cancer cells (DCCs). Some DCCs behave aggressively, immediately
starting tumors in new tissue, while others remain in a state of
suspended animation referred to as dormancy.
"It's long been a mystery how some DCCs can remain in tissues
for decades and never cause metastases, and we believe we've found
the explanation," said Dr. Aguirre-Ghiso, who is also professor of
cell biology, of oncology, and of medicine and the Rose C.
Falkenstein Chair in Cancer Research at Albert Einstein College of Medicine.
Breast cancer and many other types of cancer metastasize to the
lungs. In research involving three mouse models of metastatic
breast cancer, Dr. Aguirre-Ghiso and colleagues determined that
when breast cancer DCCs spread to the lung's air sacs (alveoli),
they are kept in a dormant state by immune cells known as alveolar
macrophages.
Insight into the Immune System
"Alveolar macrophages
are the lung's first responders, defending the organ against
bacteria and dangerous substances like environmental pollutants,"
said Dr. Aguirre-Ghiso. These specialized macrophages, he notes,
appear early in embryonic development and reside within lung tissue
for life.
"Our findings demonstrate a new role for these macrophages, in
which they recognize DCCs and actively interact with them, and—by
secreting a protein called TGF-β2—produce signals in the cancer
cells that keep them in a dormant state," Dr. Aguirre-Ghiso said.
"Since every organ in the body has its own set of tissue-resident
macrophages, they may function to keep DCCs in check in those
organs as well. Our study has shown for the first time that these
specialized macrophages function to actively induce dormancy in
DCCs."
Confirming the importance of alveolar macrophages in keeping
DCCs dormant, Dr. Aguirre-Ghiso and his team found that depleting
them in the mice significantly increased the number of activated
DCCs and subsequent metastases in their lungs compared to mice with
normal levels of the immune cells.
As DCCs become more aggressive, the researchers found, they
become resistant to the pro-dormancy signals produced by alveolar
macrophages. Ultimately, this evasion mechanism enables some DCCs
to "wake up" from dormancy and reactivate to form metastases.
"Understanding how immune cells keep DCCs in check could lead to
new anti-metastatic cell therapies among other strategies," Dr.
Aguirre-Ghiso said. For example, he noted, it may be possible to
strengthen macrophage signaling so that DCCs never awaken from
dormancy or find ways to prevent older DCCs from becoming resistant
to dormancy signaling.
The study is titled, "Lung resident alveolar macrophages
regulate the timing of breast cancer metastasis." Additional
authors from MECCC include: Nicole Barth Ph.D (also at University of Edinburgh, UK), Deisy Segura-Villalobos, Ph.D., Luis Valencia-Salazar, B.A., Dan Sun Ph.D., and
David Entenberg, Ph.D. Other authors
include: Matthew Park, Ph.D., and
Miriam Merad, M.D., Ph.D., at Icahn
School of Medicine at Mount Sinai, New
York, NY, Rui Hou, Ph.D., and
Alistair R. R. Forrest, Ph.D., at
The University of Western
Australia, Nedlands, Australia, and Maria
Casanova-Acebes, Ph.D., at Spanish National Cancer Centre,
Madrid, Spain.
About Montefiore Einstein Comprehensive Cancer
Center
Montefiore Einstein Comprehensive Cancer Center
(MECCC) is a National Cancer Institute (NCI)-designated
comprehensive cancer center and a national leader in cancer
research and care located in the racially and ethnically diverse
borough of the Bronx, N.Y. MECCC
combines the exceptional science of Albert
Einstein College of Medicine with the multidisciplinary and
team-based approach to cancer clinical care at Montefiore Health
System. Founded in 1971 and a NCI-designated cancer center since
1972, MECCC is redefining excellence in cancer research, clinical
care, education and training, and community outreach and
engagement. Its mission is to reduce the burden of cancer for all,
especially people from historically underrepresented groups.
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SOURCE Montefiore Einstein Comprehensive Cancer Center