(Press-News.org) Harvard stem cell scientists have a new theory for how stem cells decide whether to become
liver or pancreatic cells during development. A cell's fate, the researchers found, is determined by
the nearby presence of prostaglandin E2, a messenger molecule best known for its role in
inflammation and pain. The discovery, published in the journal Developmental Cell, could potentially
make liver and pancreas cells easier to generate both in the lab and for future cell therapies.
Wolfram Goessling, MD, PhD, and Trista North, PhD, both principal faculty members of the
Harvard Stem Cell Institute (HSCI), identified a gradient of prostaglandin E2 in the region of
zebrafish embryos where stem cells differentiate into the internal organs. Experiments conducted by
postdoctoral fellow Sahar Nissim, MD, PhD, in the Goessling lab showed how liver-or-pancreas-fated
stem cells have specific receptors on their membranes to detect the amount of prostaglandin E2
hormone present and coerce the cell into differentiating into a specific organ type.
"Cells that see more prostaglandin become liver and the cells that see less prostaglandin
become pancreas," said Goessling, a Harvard Medical School Assistant Professor of Medicine at
Brigham and Women's Hospital and Dana-Farber Cancer Institute. "This is the first time that
prostaglandin is being reported as a factor that can lead this fate switch and essentially instruct
what kind of identity a cell is going to be."
The researchers next collaborated with the laboratory of HSCI Affiliated Faculty member
Richard Maas, MD, PhD, Director of the Genetics Division at Brigham and Women's Hospital, to see
whether prostaglandin E2 has a similar function in mammals. Richard Sherwood, PhD, a former graduate
student of HSCI Co-director Doug Melton, was successfully able to instruct mouse stem cells to
become either liver or pancreas cells by exposing them to different amounts of the hormone. Other
experiments showed that prostaglandin E2 could also enhance liver growth and regeneration of liver
cells.
Goessling and his research partner North, a Harvard Medical School Assistant Professor of
Pathology at Beth Israel Deaconess Hospital, first became intrigued by prostaglandin E2 in 2005, as
postdoctoral fellows in the lab of HSCI Executive Committee Chair Leonard Zon, MD. It caught their
attention during a chemical screen exposing 2,500 known drugs to zebrafish embryos to find any that
could amplify blood stem cell populations. Prostaglandin E2 was the most successful hit —the first
molecule discovered in any system to have such an effect—and recently successfully completed Phase
1b clinical trials as a therapeutic to improve cord blood transplants.
"Prostaglandin might be a master regulator of cell growth in different organs," Goessling
said. "It's used in cord blood, as we have shown, it works in the liver, and who knows what other
organs might be affected by it."
With evidence of how prostaglandin E2 works in the liver, the researchers next want to
calibrate how it can be used in the laboratory to instruct induced pluripotent stem cells—mature
cells that have been reprogrammed into a stem-like state—to become liver or pancreas cells. The
scientists predict that such a protocol could benefit patients who need liver cells for
transplantation or who have had organ injury.
INFORMATION: END
Harvard scientists find cell fate switch that decides liver, or pancreas?
2014-02-14
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