Scientists reprogram skin cells into insulin-producing pancreas cells

By Dr. Matthew Watson

PUBLIC RELEASE DATE:

6-Feb-2014

Contact: Anne Holden anne.holden@gladstone.ucsf.edu 415-734-2534 Gladstone Institutes

SAN FRANCISCO, CAFebruary 6, 2014A cure for type 1 diabetes has long eluded even the top experts. Not because they do not know what must be donebut because the tools did not exist to do it. But now scientists at the Gladstone Institutes, harnessing the power of regenerative medicine, have developed a technique in animal models that could replenish the very cells destroyed by the disease. The team's findings, published online today in the journal Cell Stem Cell, are an important step towards freeing an entire generation of patients from the life-long injections that characterize this devastating disease.

Type 1 diabetes, which usually manifests during childhood, is caused by the destruction of -cells, a type of cell that normally resides in the pancreas and produces a hormone called insulin. Without insulin, the body's organs have difficulty absorbing sugars, such as glucose, from the blood. Once a death sentence, the disease can now be managed with regular glucose monitoring and insulin injections. A more permanent solution, however, would be to replace the missing -cells. But these cells are hard to come by, so researchers have looked towards stem cell technology as a way to make them.

"The power of regenerative medicine is that it can potentially provide an unlimited source of functional, insulin-producing -cells that can then be transplanted into the patient," said Dr. Ding, who is also a professor at the University of California, San Francisco (UCSF), with which Gladstone is affiliated. "But previous attempts to produce large quantities of healthy -cellsand to develop a workable delivery systemhave not been entirely successful. So we took a somewhat different approach."

One of the major challenges to generating large quantities of -cells is that these cells have limited regenerative ability; once they mature it's difficult to make more. So the team decided to go one step backwards in the life cycle of the cell.

The team first collected skin cells, called fibroblasts, from laboratory mice. Then, by treating the fibroblasts with a unique 'cocktail' of molecules and reprogramming factors, they transformed the cells into endoderm-like cells. Endoderm cells are a type of cell found in the early embryo, and which eventually mature into the body's major organsincluding the pancreas.

"Using another chemical cocktail, we then transformed these endoderm-like cells into cells that mimicked early pancreas-like cells, which we called PPLC's," said Gladstone Postdoctoral Scholar Ke Li, PhD, the paper's lead author. "Our initial goal was to see whether we could coax these PPLC's to mature into cells that, like -cells, respond to the correct chemical signals andmost importantlysecrete insulin. And our initial experiments, performed in a petri dish, revealed that they did."

The research team then wanted to see whether the same would occur in live animal models. So they transplanted PPLC's into mice modified to have hyperglycemia (high glucose levels), a key indicator of diabetes.

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Scientists reprogram skin cells into insulin-producing pancreas cells

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