Newswise, March 3, 2016– Over the past decade, studies have
found that obesity and eating a high-fat, high-calorie diet are significant
risk factors for many types of cancer. Now, a new study from Whitehead
Institute and MIT’s Koch Institute for Integrative Cancer Research reveals how
a high-fat diet makes the cells of the intestinal lining more likely to become
cancerous.
The study of mice suggests that a high-fat diet drives a
population boom of intestinal stem cells and also generates a pool of other
cells that behave like stem cells — that is, they can reproduce themselves
indefinitely and differentiate into other cell types.
These stem cells and “stem-like” cells are more likely to give
rise to intestinal tumors, says Omer Yilmaz, an MIT assistant professor of
biology and co-leader of the research team.
“Not only does the high-fat diet change the biology of stem
cells, it also changes the biology of non-stem-cell populations, which
collectively leads to an increase in tumor formation,” says Yilmaz, who is a
Koch Institute member and a gastrointestinal pathologist at Massachusetts
General Hospital.
“Under a high-fat diet, these non-stem cells acquire the
properties of stem cells so that when they are transformed they become
tumorigenic,” says Whitehead Member David Sabatini, who is also an MIT
professor of biology and an investigator of the Howard Hughes Medical
Institute.
Sabatini and Yilmaz, who previously collaborated on research
into the effects of caloric restriction on stemness in the intestine, are the
senior authors of the study, which appears in Nature on March 2.
People who are obese have a greater risk of developing
colorectal cancer, according to previous studies. Sabatini and Yilmaz, whose
labs study the relationship between diet and cancer, set out to uncover the
cellular mechanisms underpinning the enhanced risk of colon cancer.
“We wanted to understand how a long-term high-fat diet
influences the biology of stem cells, and how such diet-induced changes that
occur in stem cells impact tumor initiation in the intestine,” Yilmaz says.
Recent studies have shown that intestinal stem cells, which
last a lifetime, are the cells most likely to accumulate the mutations that
give rise to colon cancer.
These stem cells live in the lining of the intestine, known as
the epithelium, and generate all of the different cell types that make up the
epithelium.
To investigate a possible link between these stem cells and
obesity-linked cancer, researchers fed healthy mice a diet made up of 60
percent fat for nine to 12 months.
This diet, according to the scientists, is much higher in fat
than the typical American diet, which is usually about 20 to 40 percent fat.
During this period, the mice on the high-fat diet gained 30 to
50 percent more body mass than mice fed a normal diet, and they developed more
intestinal tumors than mice on a normal diet.
These mice also showed some distinctive changes in their
intestinal stem cells, the researchers discovered. First, they found that the
mice on a high-fat diet had many more intestinal stem cells than mice on a
normal diet. These stem cells were also able to operate without input from
neighboring cells.
Normally, intestinal stem cells are surrounded by support or
“niche” cells, which regulate stem cell activity and tell them when to generate
stem cells or differentiated cells.
However, the stem cells from mice on a high-fat diet were more
able to function on their own. When these stem cells were removed from the mice
and grown in a culture dish without their niche cells, they gave rise to
“mini-intestines” much more readily than intestinal stem cells from mice on a
normal diet.
“You have more stem cells and they’re able to operate
independent of inputs coming from their microenvironment,” Yilmaz says.
The researchers also found that another population known as
progenitor cells — differentiated daughter cells of stem cells — started to
behave like stem cells:
They began to live much longer than their usual lifespan of a
few days, and they could also generate mini-intestines when grown outside of
the body.
“This is really important because it’s known that stem cells
are often the cells in the intestine that acquire the mutations that go on to
give rise to tumors,” Yilmaz says.
“Not only do you have
more of the traditional stem cells (on a high-fat diet), but now you have
non-stem-cell populations that have the ability to acquire mutations that give
rise to tumors.”
The researchers also identified a nutrient-sensing pathway
that is hyper-activated by the high-fat diet. The fatty acid sensor, known as
PPAR-delta, responds to high levels of fat by turning on a metabolic process that
enables cells to burn fat as an energy source instead of their usual
carbohydrates and sugars.
“Indeed, small-molecule agonists of PPAR-delta mimic the
effects of a high-fat diet in animals fed a normal diet,” Sabatini says.
In addition to activating this metabolic program, PPAR-delta
also appears to turn on a set of genes that are important for stem cell
identity, Yilmaz says. His lab is now further investigating how this happens in
hopes of identifying possible cancer drug targets for tumors that arise in
obesity.
This work was supported by the National Institutes of Health
(grants R01 CA103866, AI47389, K08 CA198002, R00 AG045144, R00 AG041765,
DK0433051, P30-CA14051), Department of Defense PRCRP Career Development Award
CA120198, the Howard Hughes Medical Institute, the Ellison Medical Foundation,
American Federation of Aging Research, Kathy and Curt Marble Cancer Research
Fund, V Foundation, Koch MIT Ludwig Center, Massachusetts General Hospital, and
the Damon Runyon Cancer Research Foundation
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