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Cell Type-Specific Transcriptional Control of Gsk3β in the Developing Mammalian Neocortex

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Temporal control of neurogenesis is central for the development and evolution of species-specific brain architectures. The balance between progenitor expansion and neuronal differentiation is tightly coordinated by cell-intrinsic and cell-extrinsic cues. Wnt signaling plays pivotal roles in the proliferation and differentiation of neural progenitors in a temporal manner. However, regulatory mechanisms that adjust intracellular signaling amplitudes according to cell fate progression remain to be elucidated. Here, we report the transcriptional controls of Gsk3β, a critical regulator of Wnt signaling, in the developing mouse neocortex. Gsk3β expression was higher in ventricular neural progenitors, while it gradually declined in differentiated neurons. We identified active cis-regulatory module (CRM) of Gsk3β that responded to cell type-specific transcription factors, such as Sox2, Sox9, and Neurogenin2. Furthermore, we found extensive conservation of the CRM among mammals but not in non-mammalian amniotes. Our data suggest that a mammalian-specific CRM drives the cell type-specific activity of Gsk3β to fine tune Wnt signaling, which contributes to the tight control of neurogenesis during neocortical development.
Title: Cell Type-Specific Transcriptional Control of Gsk3β in the Developing Mammalian Neocortex
Description:
Temporal control of neurogenesis is central for the development and evolution of species-specific brain architectures.
The balance between progenitor expansion and neuronal differentiation is tightly coordinated by cell-intrinsic and cell-extrinsic cues.
Wnt signaling plays pivotal roles in the proliferation and differentiation of neural progenitors in a temporal manner.
However, regulatory mechanisms that adjust intracellular signaling amplitudes according to cell fate progression remain to be elucidated.
Here, we report the transcriptional controls of Gsk3β, a critical regulator of Wnt signaling, in the developing mouse neocortex.
Gsk3β expression was higher in ventricular neural progenitors, while it gradually declined in differentiated neurons.
We identified active cis-regulatory module (CRM) of Gsk3β that responded to cell type-specific transcription factors, such as Sox2, Sox9, and Neurogenin2.
Furthermore, we found extensive conservation of the CRM among mammals but not in non-mammalian amniotes.
Our data suggest that a mammalian-specific CRM drives the cell type-specific activity of Gsk3β to fine tune Wnt signaling, which contributes to the tight control of neurogenesis during neocortical development.

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