Literature DB >> 33393905

Dentate gyrus development requires a cortical hem-derived astrocytic scaffold.

Alessia Caramello1, Christophe Galichet1, Karine Rizzoti1, Robin Lovell-Badge1.   

Abstract

During embryonic development, radial glial cells give rise to neurons, then to astrocytes following the gliogenic switch. Timely regulation of the switch, operated by several transcription factors, is fundamental for allowing coordinated interactions between neurons and glia. We deleted the gene for one such factor, SOX9, early during mouse brain development and observed a significantly compromised dentate gyrus (DG). We dissected the origin of the defect, targeting embryonic Sox9 deletion to either the DG neuronal progenitor domain or the adjacent cortical hem (CH). We identified in the latter previously uncharacterized ALDH1L1+ astrocytic progenitors, which form a fimbrial-specific glial scaffold necessary for neuronal progenitor migration toward the developing DG. Our results highlight an early crucial role of SOX9 for DG development through regulation of astroglial potential acquisition in the CH. Moreover, we illustrate how formation of a local network, amidst astrocytic and neuronal progenitors originating from adjacent domains, underlays brain morphogenesis.
© 2021, Caramello et al.

Entities:  

Keywords:  dentate gyrus; developmental biology; embryo; mouse; neuroscience; sox9

Mesh:

Year:  2021        PMID: 33393905      PMCID: PMC7806271          DOI: 10.7554/eLife.63904

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.140


  71 in total

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