AI Article Synopsis

  • - Neural precursor cells (NPCs) in the developing neocortex produce different types of neurons in a specific sequence, and the timing of these changes is crucial for proper cortical structure and function.
  • - The research identifies Ring1B, a component of polycomb group proteins, as a key factor that regulates the end of subcerebral projection neuron (SCPN) production by influencing the expression of Fezf2, which is vital for SCPN identity.
  • - When Ring1B is deleted from NPCs, it leads to prolonged Fezf2 expression and increased generation of SCPNs, highlighting Ring1B's role in timing neuron subtype production in the developing brain.

Article Abstract

In the developing neocortex, neural precursor cells (NPCs) sequentially generate various neuronal subtypes in a defined order. Although the precise timing of the NPC fate switches is essential for determining the number of neurons of each subtype and for precisely generating the cortical layer structure, the molecular mechanisms underlying these switches are largely unknown. Here, we show that epigenetic regulation through Ring1B, an essential component of polycomb group (PcG) complex proteins, plays a key role in terminating NPC-mediated production of subcerebral projection neurons (SCPNs). The level of histone H3 residue K27 trimethylation at and Ring1B binding to the promoter of Fezf2, a fate determinant of SCPNs, increased in NPCs as Fezf2 expression decreased. Moreover, deletion of Ring1B in NPCs, but not in postmitotic neurons, prolonged the expression of Fezf2 and the generation of SCPNs that were positive for CTIP2. These results indicate that Ring1B mediates the timed termination of Fezf2 expression and thereby regulates the number of SCPNs.

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Source
http://dx.doi.org/10.1242/dev.112276DOI Listing

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