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Stem cells hold key to blood development
FOR THE first time, scientists have demonstrated that
undifferentiated human embryonic stem cells can be teased down a
developmental pathway to become blood cells. The work, conducted
by a team of researchers at the University of Wisconsin-Madison,
is important because it demonstrates the potential for creating
in the laboratory a novel source of blood cells for
transplantation and transfusion. The work was reported in the
Proceedings of The National Academy of Sciences (PNAS). Finding
out how to direct embryonic stem cells -- blank-slate cells that
arise at the earliest stages of development, to become blood,
bone, skin, nerve and other cell types -- is one of the biggest
technical challenges facing scientists as they work to advance
stem cell technology.
Learning how blood arises from embryonic stem cells has been a
fundamental question in biology. The accomplishment reported by
the Wisconsin scientists shows that undifferentiated stem cells
can be coaxed to become primitive types of blood cells that later
develop into more mature types of blood cells that, one day, may
be used for transfusion or transplant technologies.
``These results show an effective and efficient way to derive
blood cells from these early precursors,'' says Dan Kaufman, a
haematology fellow at the UW-Madison Medical School and the lead
author of the PNAS paper. Kaufman emphasizes that while the work
shows great promise toward the ultimate goal of taming embryonic
stem cells in the lab, the work reported today still represents
early-stages of the science and that clinical application remains
years in the future.
The new research, however, holds promise for illuminating the
process of human development as generic embryonic cells begin
down developmental pathways to become any of the 220 types of
cells and tissue that make up the human body.
Moreover, the ability to create supplies of blood in the lab has
obvious implications for augmenting human blood supplies for
transfusion and for transplant therapies to treat cancers of the
blood and bone marrow such as leukemias and myelomas.
``This is not something that's going to be available tomorrow or
next year,'' Kaufman says, but the research does represent a key
step forward in the quest to direct stem cells to become a
specific cell type.
Writing in PNAS, Kaufman and his colleagues show that stem cells
can be directed to become what are known to scientists as
haematopoietic precursor cells (or haematopoietic colony-forming
cells), cells that display distinct biochemical markers and gene
products characteristic of blood and bone marrow cells in the
body.
Moreover, these precursor cells go on to form colonies of white
blood cells, red blood cells and platelets, cells identical to
those that arise from human bone marrow.
If perfected, the technology could significantly improve human
blood supplies. ``There is generally a shortage of blood,'' says
Kaufman, and if the technology matures it ``may one day be
possible to augment that blood supply.''
The work at Wisconsin was accomplished in tissue culture by
exposing undifferentiated stem cells to bone marrow and other
cells as well as growth factors in order to encourage them down
the developmental pathway to becoming blood.
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