Yale researchers show in detail how three
genes within human embryonic stem cells regulate development, a finding that
increases understanding of how to grow these cells for therapeutic purposes.
This
process, described in the April 6 issue of the journal Cell Stem Cell, is different
in humans than in mice, highlighting the importance of research using human
embryonic stem cells.
"It
is difficult to deduce from the mouse how these cells work in humans,"
said Natalia Ivanova, assistant professor of genetics in the Yale Stem Cell
Center and senior author of the study. "Human networks organize themselves
quite differently."
Embryonic
stem cells form soon after conception and are special because each cell can
become any type of cell in the body. Cells become increasingly specialized as
development progresses, losing the ability to become other cell types -- except
for the renewal of a few new stem cells. Scientists want to understand the
processes of self-renewal and differentiation in order to treat a host of
diseases characterized by damaged cells such as Parkinson's disease, spinal
cord injury, heart disease, and Alzheimer's.
Scientists
have identified three genes active in early development -- Nanog, Oct 4, and
Sox 2 -- as essential to maintaining the stem cell's ability to self-renew and
prevent premature differentiation into the "wrong" type of cells.
Because of restrictions on the use of human embryonic stem cells, much of the
investigation into how these genes work has been done in mice.
The new
study shows that human embryonic cells operate in fundamentally different ways
in humans than in mouse cells. In humans, for instance, Nanog pairs with Oct 4
to regulate differentiation of so-called neuro-ectoderm cells, a lineage that
gives rise to neurons and other central nervous system cells. Sox 2, by
contrast, inhibits the differentiation of mesoderm -- a lineage that gives rise
to muscles and many other tissue types. Oct 4 cooperates with the other genes
and is crucial in the regulation of all four early cell lineages: ectoderm,
mesoderm, and endoderm -- which gives rise to gut and glands such as liver and
pancreas -- as well as the creation of new stem cells. The self-renewal of stem
cells has been implicated in several forms of cancer.
Ivanova
stresses that many other genes must be involved in regulation of these early
developmental changes, and her lab is investigating that question now.
The
research was supported by a grant from the Connecticut Stem Cell Research
Program.
Source:
Yale University
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