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Human oligodendrocytes from embryonic stem cells: conserved SHH signaling networks and divergent FGF effects.


ABSTRACT: Human embryonic stem cells (hESCs) offer a platform to bridge what we have learned from animal studies to human biology. Using oligodendrocyte differentiation as a model system, we show that sonic hedgehog (SHH)-dependent sequential activation of the transcription factors OLIG2, NKX2.2 and SOX10 is required for sequential specification of ventral spinal OLIG2-expressing progenitors, pre-oligodendrocyte precursor cells (pre-OPCs) and OPCs from hESC-derived neuroepithelia, indicating that a conserved transcriptional network underlies OPC specification in human as in other vertebrates. However, the transition from pre-OPCs to OPCs is protracted. FGF2, which promotes mouse OPC generation, inhibits the transition of pre-OPCs to OPCs by repressing SHH-dependent co-expression of OLIG2 and NKX2.2. Thus, despite the conservation of a similar transcriptional network across vertebrates, human stem/progenitor cells may respond differently to those of other vertebrates to certain extrinsic factors.

SUBMITTER: Hu BY 

PROVIDER: S-EPMC2674255 | biostudies-literature | 2009 May

REPOSITORIES: biostudies-literature

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Human oligodendrocytes from embryonic stem cells: conserved SHH signaling networks and divergent FGF effects.

Hu Bao-Yang BY   Du Zhong-Wei ZW   Li Xue-Jun XJ   Ayala Melvin M   Zhang Su-Chun SC  

Development (Cambridge, England) 20090501 9


Human embryonic stem cells (hESCs) offer a platform to bridge what we have learned from animal studies to human biology. Using oligodendrocyte differentiation as a model system, we show that sonic hedgehog (SHH)-dependent sequential activation of the transcription factors OLIG2, NKX2.2 and SOX10 is required for sequential specification of ventral spinal OLIG2-expressing progenitors, pre-oligodendrocyte precursor cells (pre-OPCs) and OPCs from hESC-derived neuroepithelia, indicating that a conser  ...[more]

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