4.8 Article

Molecular diversity of diencephalic astrocytes reveals adult astrogenesis regulated by Smad4

期刊

EMBO JOURNAL
卷 40, 期 21, 页码 -

出版社

WILEY
DOI: 10.15252/embj.2020107532

关键词

astrocytes; cerebral cortex; de novo astrocyte generation; proliferation; Smad4

资金

  1. DFG, the German Research Foundation [1757]
  2. European Research Council (advanced ERC grant ChroNeuroRepair GA) [340793]
  3. EU consortium NSC Reconstruct [874758, 2145]
  4. [870]
  5. European Research Council (ERC) [340793] Funding Source: European Research Council (ERC)

向作者/读者索取更多资源

Astrocytes exhibit diverse gene expression states related to distinct functions, with some subsets being more widespread while others are regionally restricted. The study also reveals the novel concept of low-level proliferation of astrocytes in the adult diencephalon, with Smad4 identified as a key regulator.
Astrocytes regulate brain-wide functions and also show region-specific differences, but little is known about how general and region-specific functions are aligned at the single-cell level. To explore this, we isolated adult mouse diencephalic astrocytes by ACSA-2-mediated magnetic-activated cell sorting (MACS). Single-cell RNA-seq revealed 7 gene expression clusters of astrocytes, with 4 forming a supercluster. Within the supercluster, cells differed by gene expression related to ion homeostasis or metabolism, with the former sharing gene expression with other regions and the latter being restricted to specific regions. All clusters showed expression of proliferation-related genes, and proliferation of diencephalic astrocytes was confirmed by immunostaining. Clonal analysis demonstrated low level of astrogenesis in the adult diencephalon, but not in cerebral cortex grey matter. This led to the identification of Smad4 as a key regulator of diencephalic astrocyte in vivo proliferation and in vitro neurosphere formation. Thus, astrocytes show diverse gene expression states related to distinct functions with some subsets being more widespread while others are more regionally restricted. However, all share low-level proliferation revealing the novel concept of adult astrogenesis in the diencephalon.

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