Intestinal
Cells Can Be Stimulated To Make Insulin
A
new source of beta cells can provide an answer to the shortage in
Edmonton Protocols
An
international research team has discovered a new source of cells to
combat diabetes. Scientists at the University of Calgary and Japan’s
Shiga University find that intestinal cells produce insulin.
Dr.
Norman Wong, a University of Calgary physician-scientist, and his
colleagues, Drs. Takaaki Nakamura and Atsunori Kashiwagi,
clinician-scientists of Shiga University in Japan, have completed
studies which demonstrate that intestinal cells can be stimulated into
producing insulin –- a hormone that millions of diabetics are
lacking.
The
team’s findings are published in the May edition of Diabetes,
a prestigious international research journal.
“Scientists
the world over are studying how to manipulate cells in order to
convert them into pancreatic cells, which may be used to treat
diabetes mellitus,” says Wong, professor, medicine, and biochemistry
& molecular biology, University of Calgary Faculty of Medicine,
and director, Libin Gene Therapy Unit. “My colleagues and I decided
to investigate whether we could make islet cells by altering
intestinal cells so that they would transform into pancreatic islet
cells and produce insulin.”
Type
1 diabetes mellitus, previously known as juvenile diabetes mellitus,
is caused by the destruction of insulin-producing beta cells in the
pancreas. This destruction occurs when the immune system mistakenly
attacks the beta cells. The absence of insulin means that people with
diabetes have high blood glucose and associated complications that
affect vital organs including: kidney, eye and nerve conditions as
well as heart and vascular disease.
This
research stems from the understanding that pancreatic cells and
intestinal cells share a common origin in the embryo. Armed with that
knowledge, the team began exploring whether conducting a series of
experiments on intestinal cells would stimulate those cells into
performing the functions normally provided by pancreatic cells.
The
scientists first exposed the intestinal cells of rats to a
transcription factor called PDX-1. This factor has been previously
shown to be important for insulin gene expression. Secondly, the team
exposed the PDX-1 expressing intestinal cells to a growth factor
called Betacellulin. “We discovered that the combination of those
two steps enabled us to fire up the intestinal cells so that they
produced insulin,” says Wong.
“The
advantage of using intestinal cells to perform the work of pancreatic
cells is that people have available to them a nearly limitless supply
of their own intestinal cells -– whereas pancreatic cells are
extremely scarce,” says Wong. “That’s what’s so exciting about
these results –- we have taken the first step in finding a man-made
way to produce pancreatic cells. These findings may provide an
important source of cells for the Edmonton islet cell transplantation
protocol.”
Wong’s
research is supported by: Canadian Diabetes Association, Alberta
Heritage Foundation for Medical Research, and Canadian Institutes of
Health Research. - By Karen Thomas
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