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Accession IconGSE15561

Generation of parthenogenetic iPS cells from parthenogenetic neural stem cell

Organism Icon Mus musculus
Sample Icon 10 Downloadable Samples
Technology Badge IconIllumina MouseRef-8 v2.0 expression beadchip

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Description
In pluripotential reprogramming, a pluripotent state is established within somatic cells. In this study, we have generated induced pluripotent stem (iPS) cells from bi-maternal (uniparental) parthenogenetic neural stem cells (pNSCs) by transduction with four (Oct4, Klf4, Sox2, and c-Myc) or two (Oct4 and Klf4) transcription factors. The parthenogenetic iPS (piPS) cells directly reprogrammed from pNSCs were able to generate germline-competent himeras, and hierarchical clustering analysis showed that piPS cells were clustered more closer to parthenogenetic ES cells than normal female ES cells. Interestingly, piPS cells showed loss of parthenogenetic-specific imprinting patterns of donor cells. Microarray data also showed that the maternally imprinted genes, which were not expressed in pNSCs, were upregulated in piPS cells, indicating that pluripotential reprogramming lead to induce loss of imprinting as well as re-establishment of various features of pluripotent cells in parthenogenetic somatic cells.
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10

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piPS-2F rep2
parthenogenetic
pluripotent cells, derived from nsc overexpressing oct4 and klf5
piPS-2F rep1
parthenogenetic
pluripotent cells, derived from nsc overexpressing oct4 and klf4
fNSC rep1
female
neural stem cell
pNSC rep1
parthenogenetic
neural stem cell
pESC-B rep2
parthenogenetic
embryonic stem cell, ssea-1 sorted
pNSC rep2
parthenogenetic
neural stem cell
fNSC rep2
female
neural stem cell
pESC-B rep1
parthenogenetic
embryonic stem cell, ssea-1 sorted
fESC-B rep1
female
embryonic stem cell og2
fESC-B rep2
female
embryonic stem cell og2
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