This was long suspected but simply unproven. We have that now and a clear pathway analysis. This all leads to better research options.
Hopefully this leads to better suppression as well.
All Good.
.
Cancer Cells Can Poison Normal Cells
Like bacteria and viruses, cancer cells have the potential to infect normal cells and promote cancer progression.
Released:
30-Nov-2015
http://www.newswise.com/articles/view/643967/?sc=dwhn
Newswise — Cancer cells are continuously produced in our bodies,
where most of them are recognized by our immune systems and destroyed.
Some, however, escape this innate surveillance system and find a place
to survive and grow.
Several factors expelled by tumor cells are
concentrated in the area immediately surrounding the tumor, called the
tumor microenvironment. While it is established that these factors
support and enhance cancer cell growth and multiplication, it was not
known whether these factors influence neighboring normal cells.
Now a team of researchers from the University of Delaware,
Nemours/A.I. duPont Hospital for Children, St. Joseph’s Hospital and
Medical Center in Phoenix and Therapy Architects LLC in Wilmington,
Delaware, has reported that cancer cells can actually cause neighboring
normal cells to become cancerous. The research is documented in the
current online edition of the Journal of Cell Science.
The
researchers used a three-dimensional co-culture system where they grew
normal cells and cancer cells together, mimicking the situation inside
the body.
They found that cancer cells produce an enzyme—a
protease—which splits a cell-cell adhesion molecule called E-cadherin
from normal cells. The action of the protease liberates the segment of
E-cadherin that projects outside the cells. This segment, designated
soluble E-cadherin, or sE-cad, then associates with a signaling molecule
called epidermal growth factor receptor on normal cells and converts
them to cancerous cells.
“The serum of adult cancer patients
contains high levels of sE-cad,” says Pratima Patil, who received her
doctorate in biological sciences from UD earlier this year. “Our finding
documents that tumor cells modify normal epithelial cells, disrupting
their cellular architecture, and use them as accomplices to generate
sE-cad, which is known to facilitate tumor progression.”
Ayyappan
Rajasekaran, adjunct professor in materials science and engineering and
president of Therapy Architects, says this is the first time research
has demonstrated that a cancer cell can sequentially induce early and
late stages of cancer development in neighboring normal cells—a
fundamental finding that can inform future studies.
“Like bacteria and viruses, cancer cells have the potential to infect normal cells and promote cancer progression,” he adds.
This
finding opens up new cancer research areas, including determining how
cancer cells interact with neighboring normal cells and promote cancer
development.
From a clinical perspective, the discovery raises
the question of whether reducing sE-cad levels in cancer patients will
slow the progression of cancer and improve treatment options.
“These future studies should give a new dimension to our understanding of cancer development and treatment,” Rajasekaran says.
The
paper, “Carcinoma Cells Induce Lumen Filling and EMT in Epithelial
Cells by soluble E-cadherin-Mediated Activation of EGFR,” was
co-authored by Pratima Patil, Julia D’Ambrosio, Landon Inge, Robert
Mason, and Ayyappan Rajasekaran. A PDF OF THE ARTICLE IS AVAILABLE FOR
DOWNLOAD HERE.
This
research was supported by funds from the National Institutes of Health
(NIH grant DK56216), Nemours Research Programs and COBRE grant
P20GM103464.
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