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Ed. Note: The following
is a press release from the University of Pittsburgh
PITTSBURGH, Aug. 5, 2005 – Routinely discarded as medical waste,
placental tissue could feasibly provide an abundant source of cells with the
same potential to treat diseases and regenerate tissues as their more
controversial counterparts, embryonic stem cells, suggests a
University of Pittsburgh study
to be published in the journal Stem Cells and available now as an
early online publication in Stem Cells Express.
A part of the placenta called the amnion, or the outer membrane of the
amniotic sac, is comprised of cells that have strikingly similar
characteristics to embryonic stem cells, including the ability to express
two key genes that give embryonic stem cells their unique capability for
developing into any kind of specialized cell, the researchers report. And
according to the results of their studies, these so-called amniotic
epithelial cells could in fact be directed to form liver, pancreas, heart
and nerve cells under the right laboratory conditions.
“If we could develop efficient methods that would allow amnion-derived cells
to differentiate into specific cell types, then placentas would no longer be
relegated to the trashcan. Instead, we’d have a useful source of cells for
transplantation and regenerative medicine,” said senior author Stephen C.
Strom, Ph.D., associate professor of pathology at the University of
Pittsburgh School of Medicine and a researcher at the university’s
McGowan Institute for Regenerative
Medicine.
According to U.S. census figures, there are more than 4 million live births
each year. For each discarded placenta, the researchers calculate there are
about 300 million amniotic epithelial cells that potentially could be
expanded to between 10 and 60 billion cells relatively easily.
“Provided that research advances to the point that we can demonstrate these
cells’ true therapeutic benefit, parents could conceivably choose to bank
their child’s amniotic epithelial cells in the event they may someday be
needed, as is sometimes done now with umbilical cord blood,” commented Dr.
Strom.
The amnion is derived from the embryo and forms as early as eight days after
fertilization, when the fate of cells has yet to be determined, and serves
to protect the developing fetus. According to the researchers’ studies using
placentas from full-term pregnancies, amniotic epithelial cells have many of
the telltale surface markers that define embryonic stem cells, and also
express the Oct-4 and nanog genes that are known to be required for
self-renewal and pluripotency – the ability to develop into any type of
cell.
Yet the authors are careful to point out that despite their remarkable
similarities to embryonic stem cells, amniotic epithelial cells are not stem
cells per se, because they can’t grow indefinitely. This may be due to the
fact that these amnion-derived cells do not express a certain enzyme, called
telomerase, that is important for normal DNA and chromosome replication, and
by extension, ultimately, cell division.
“Perhaps it’s to their advantage that the amnion epithelial cells lack
telomerase expression, because telomerase is associated with many cancers
and one of the main concerns about stem cell therapies is that transplanted
stem cells would replicate in the recipient to form tumors,” noted Toshio
Miki, M.D., Ph.D., first author of the paper and an instructor in the
department of pathology at the School of Medicine.
To help determine if amnion-derived cells that are delivered directly to
tissues would cause tumors, the researchers conducted studies in immune
system-deficient mice and found no evidence that tumors had developed seven
months after the cells were injected into multiple sites.
While amniotic epithelial cells do not share the same capacity for unlimited
replication as do embryonic stem cells, they still can double in population
size about 20 times over without needing another cell type serving as a
feeder cell layer. This is significant, because to replicate, the currently
available embryonic stem cell lines require a bed of mouse cells, traces of
which can end up in each new generation of stem cells. Amniotic epithelial
cells, on the other hand, create their own feeder layer, with some cells
choosing to spread out at the bottom of the culture dish thereby giving
those cells just above them the best environment for replicating and for
retaining their stem cell characteristics.
With the addition of various growth factors, the authors report the
amnion-derived cells could differentiate to become liver cells, heart cells,
the glial and neuronal cells that make up the nervous system, and pancreatic
cells with genetic markers for insulin and glycogen production.
“In this first paper we sought to determine if amniotic epithelial cells
have the potential to differentiate into many different cell types rather
than focusing on ways for optimizing this potential for a specific cell
type. Further studies will be required to better understand if and how they
may be useful in a clinical setting,” Dr. Strom added.
The researchers say their original motivation was, and still is, to identify
cells with the same therapeutic promise as embryonic stem cells. To this
end, they began looking at the viability of amnion as a cell source in late
2001, obtaining discarded placentas from full-term births under an
Institutional Review Board-approved protocol. In 2002, the University of
Pittsburgh licensed the technology to a company now called Stemnion, LLC,
and as part of the agreement, and in keeping with university patent policy,
Drs. Strom and Miki will receive license proceeds. Both have served as paid
consultants and hold equity in Stemnion.
The research was supported by the Alpha-1 Foundation and the National
Institute of Diabetes and Digestive and Kidney Diseases, a part of the
National Institutes of Health. In addition to Drs. Miki and Strom, other
authors are Thomas Lehmann, Ph.D., and Hongbo Cai, M.D., Ph.D., both from
the department of pathology, and Donna Stolz, Ph.D., of the department of
cell biology and physiology.
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