primordial germ cells
Reprogramming Primordial Germ Cells into Pluripotent Stem Cells
29/10/2008
Specification of primordial germ cells (PGCs) results
in the conversion of pluripotent epiblast cells into
monopotent germ cell lineage. Blimp1/Prmt5 complex
plays a critical role in the specification and
maintenance of the early germ cell lineage. However,
PGCs can be induced to dedifferentiate back to a
pluripotent state as embryonic germ (EG) cells when
exposed to exogenous signaling molecules, FGF-2, LIF
and SCF.
Methodology and Principal Findings
Here we show that Trichostatin A (TSA), an inhibitor of histone deacetylases, is a highly potent agent that can replace FGF-2 to induce dedifferentiation of PGCs into EG cells. A key early event during dedifferentiation of PGCs in response to FGF-2 or TSA is the down-regulation of Blimp1, which reverses and apparently relieves the cell fate restriction imposed by it. Notably, the targets of Blimp1, which include c-Myc and Klf-4, which represent two of the key factors known to promote reprogramming of somatic cells to pluripotent state, are up-regulated. We also found early activation of the LIF/Stat-3 signaling pathway with the translocation of Stat-3 into the nucleus. By contrast, while Prmt5 is retained in EG cells, it translocates from the nucleus to the cytoplasm where it probably has an independent role in regulating pluripotency.
Conclusions/Significance
We propose that dedifferentiation of PGCs into EG cells may provide significant mechanistic insights on early events associated with reprogramming of committed cells to a pluripotent state.
PLoS ONE 3(10): e3531. doi:10.1371/journal.pone.0003531
Methodology and Principal Findings
Here we show that Trichostatin A (TSA), an inhibitor of histone deacetylases, is a highly potent agent that can replace FGF-2 to induce dedifferentiation of PGCs into EG cells. A key early event during dedifferentiation of PGCs in response to FGF-2 or TSA is the down-regulation of Blimp1, which reverses and apparently relieves the cell fate restriction imposed by it. Notably, the targets of Blimp1, which include c-Myc and Klf-4, which represent two of the key factors known to promote reprogramming of somatic cells to pluripotent state, are up-regulated. We also found early activation of the LIF/Stat-3 signaling pathway with the translocation of Stat-3 into the nucleus. By contrast, while Prmt5 is retained in EG cells, it translocates from the nucleus to the cytoplasm where it probably has an independent role in regulating pluripotency.
Conclusions/Significance
We propose that dedifferentiation of PGCs into EG cells may provide significant mechanistic insights on early events associated with reprogramming of committed cells to a pluripotent state.
PLoS ONE 3(10): e3531. doi:10.1371/journal.pone.0003531
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Generation of pluripotent stem cells from adult human testis
09/10/2008
Human primordial germ cells and mouse neonatal and
adult germline stem cells are pluripotent and show
similar properties to embryonic stem cells. Here we
report the successful establishment of human adult
germline stem cells derived from spermatogonial cells
of adult human testis. Cellular and molecular
characterization of these cells revealed many
similarities to human embryonic stem cells, and the
germline stem cells produced teratomas after
transplantation into immunodeficient mice. The human
adult germline stem cells differentiated into various
types of somatic cells of all three germ layers when
grown under conditions used to induce the
differentiation of human embryonic stem cells. We
conclude that the generation of human adult germline
stem cells from testicular biopsies may provide
simple and non-controversial access to individual
cell-based therapy without the ethical and
immunological problems associated with human
embryonic stem cells.
Nature advance online publication 8 October 2008 | doi:10.1038/nature07404
Nature advance online publication 8 October 2008 | doi:10.1038/nature07404