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Home › Dataset Library › Geminin-regulated genes during neural fate acquisition of mouse embryonic stem cells

Dataset: Geminin-regulated genes during neural fate acquisition of mouse embryonic stem cells

Formation of the complex vertebrate nervous system begins when pluripotent cells of the early embryo are directed to acquire a neural...

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Formation of the complex vertebrate nervous system begins when pluripotent cells of the early embryo are directed to acquire a neural fate. Although cell intrinsic controls play an important role in this process, the molecular nature of this regulation is not well defined. Here we assessed the role for Geminin, a nuclear protein expressed in embryonic cells, in neural fate acquisition from mouse embryonic stem (ES) cells. While Geminin knockdown does not affect the ability of ES cells to maintain or exit pluripotency, we found that it significantly impairs their ability to acquire a neural fate. Conversely, Geminin overexpression promotes neural gene expression, even in the presence of growth factor signaling that antagonizes neural transcriptional responses. These data demonstrate that Geminin’s activity contributes to mammalian neural cell fate acquisition. We investigated the mechanistic basis of this phenomenon and found that Geminin maintains a hyperacetylated and open chromatin conformation at neural genes. Interestingly, recombinant Geminin protein also rapidly alters chromatin acetylation and accessibility even when Geminin is combined with nuclear extract and chromatin in vitro. These findings define a novel activity for Geminin in regulation of chromatin structure. Together, these data support a role for Geminin as a cell intrinsic regulator of neural fate acquisition that promotes expression of neural genes by regulating chromatin accessibility and histone acetylation. Mouse embryonic stem cells were differentiated for two days in N2B27 medium, with or without Doxycycline-inducible shRNAmir knockdown of Geminin and compared by microarray. Three independent experiments were conducted, using two different mouse embryonic stem cell lines for Doxycycline-inducible knockdown of Geminin. The two ES lines express unique shRNAmir sequences targeting Geminin (shRNAmir #9 and #11) to control for off-target effects.

Species:
mouse

Samples:
6

Source:
E-GEOD-25737

PubMed:
21300881

Updated:
Dec.12, 2014

Registered:
Nov.11, 2014


Factors: (via ArrayExpress)
Sample TREATMENT
GSM632119 Geminin knockdown, shRNAmir #11
GSM632120 control, shRNAmir #11
GSM63212 Geminin knockdown, shRNAmir #9
GSM632122 control, shRNAmir #9
GSM632119 Geminin knockdown, shRNAmir #11
GSM632120 control, shRNAmir #11

Tags

  • cell
  • chromatin
  • embryo
  • embryonic stem cell
  • histone
  • nervous system
  • neural cell
  • protein
  • stem cell

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