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Study
shows blood stem cells originate, are nurtured in the placenta
Wednesday, March 5, 2008
Findings could be used to
develop treatments for various blood diseases
Dr.
Hanna Mikkola
Researcher
with the Eli and Edythe Broad Center of Regenerative
Medicine and Stem Cell Research
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Credit:
UCLA newsroom
Solving a longstanding
biological mystery, UCLA stem cell researchers have discovered
that blood stem cells — the cells that later differentiate
into all the cells in the blood supply — originate and are
nurtured in the placenta.
The discovery may allow
researchers to mimic the specific embryonic microenvironment
necessary for the development of blood stem cells in cell
cultures and grow them for use in treating diseases like leukemia
and aplastic anemia, said Dr. Hanna Mikkola, a researcher with
the Eli and Edythe Broad Center of Regenerative Medicine and Stem
Cell Research at UCLA and senior author of the study.
"It was a big mystery,
where these cells originated," Mikkola said. "This is
the first time we can really say definitively that blood stem
cells are generated in the placenta. There's no more
speculation."
The study appears March 6 in
the journal Cell Stem Cell. Researchers in Mikkola's lab are
working now to replicate this mouse-model research in humans.
"If we want to fully
harness the potential of embryonic stem cells to treat disease,
it's critical for us to learn how to make tissue-specific stem
cells," said Mikkola, who also is a researcher at UCLA's
Jonsson Comprehensive Cancer Center and an assistant professor of
molecular, cell and developmental biology. "We can learn
that by studying what happens during embryonic development."
Currently, scientists can take
embryonic stem cells — cells that can become any tissue
type in the body — and coax them into becoming all the
cells in the blood supply, such as red and white blood cells and
platelets. However, they can't make blood stem cells that
self-renew, or make more of themselves, and don't differentiate
prematurely when transplanted into patients. The only way this
can now be achieved is by manipulating the cell's nuclear
regulatory machinery with genes using retroviruses. To generate
blood stem cells that are safe for use in patients, it is
imperative that scientists learn how to generate self-renewing
blood stem cells in a more natural way, by providing the correct
developmental cues from the environment in which the cells
develop.
Patients with certain types of
leukemia currently have one shot at a cure — a bone marrow
transplant. However, there aren't nearly enough bone marrow
donors to provide patients with perfect matches, and the use of
less-than-perfect matches carries the risk of graft-versus-host
disease, in which the immune cells from the donated marrow attack
the body of the transplant patient. Cord blood contains blood
stem cells, but not in large enough quantities for adult patient
transplants, Mikkola said.
If researchers could grow blood
stem cells, those cells could be transplanted into these
patients. The blood stem cells would then differentiate into a
new and healthy blood supply. And with the recent success in
creating induced pluripotent stem cells (iPS) from human skin
cells, a patient's own skin cells could perhaps be used to create
iPS cells. These cells could then be transformed into blood stem
cells, creating an immune-compatible source of blood supply that
eliminates the risk of graft-versus-host disease.
In her previous research,
Mikkola and collaborators at Harvard University and in France
discovered that the placenta contained a large pool of blood stem
cells, but it was unclear whether these cells had originated
elsewhere and migrated to the placenta to self-renew. Using a
unique mouse model (a mouse embryo without a heartbeat) Mikkola
and her team were able to find the blood stem cells at their site
of origin, since there was no circulation of blood through the
body.
"Using this model, we
identified that the placenta has the potential to make
hematopoietic (blood) stem cells with full differentiation
ability to create all the major lineages of blood cells,"
Mikkola said. "The placenta acts as a sort of kindergarten
for these newly made blood stem cells, giving them the first
education they need."
It was previously known that
blood stem cells could be found in the dorsal aorta, but there
were so few located there that scientists reasoned it could not
be the sole source of blood stem cells in the embryo. Mikkola's
discovery indicates that the blood stem cells are generated in
the large arteries of the embryo and placenta, and then move to a
specific site, or niche, where they expand and mature.
This recent study indicates
that the first niche for expansion of blood stem cells is the
placenta's vascular labyrinth, where oxygen and nutrients are
exchanged between the mother and the fetus. The findings show
that the placenta harbors two different microenvironments —
one area where blood stem cells originate and another, the
labyrinth, that nurtures them, allowing them to expand in number.
These niches serve different roles and could provide clues to
researchers seeking to grow blood stem cells.
Mikkola now is seeking to
uncover the critical biological signals and cues during embryonic
development that drive blood stem cell generation and expansion
and keep the cells from differentiating prematurely.
"The labyrinth is a source
of many growth factors and cytokines," Mikkola said. "We
just need to identify what those signaling molecules and cues are
that are nurturing those cells when in the placenta."
Mikkola is confident the study
can be confirmed in humans.
"Everything we're learning
suggests we will find the same thing in the human placenta,"
she said.
UCLA's stem cell center was
launched in 2005 with a UCLA commitment of $20 million over five
years. A $20 million gift from the Eli and Edythe Broad
Foundation in 2007 resulted in the renaming of the center.
Source:
University of California, Los Angeles / Kim Irwin

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