Morphological diversification and functional maturation of human astrocytes in glia-enriched cortical organoid transplanted in mouse brain

Astrocytes, the most abundant glial cell type in the brain, are underrepresented in traditional cortical organoid models due to the delayed onset of cortical gliogenesis. Here we introduce a new glia-enriched cortical organoid model that exhibits accelerated astrogliogenesis. We demonstrated that in...

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Veröffentlicht in:Nature biotechnology 2024-02
Hauptverfasser: Wang, Meiyan, Zhang, Lei, Novak, Sammy Weiser, Yu, Jingting, Gallina, Iryna S, Xu, Lynne L, Lim, Christina K, Fernandes, Sarah, Shokhirev, Maxim N, Williams, April E, Saxena, Monisha D, Coorapati, Shashank, Parylak, Sarah L, Quintero, Cristian, Molina, Elsa, Andrade, Leonardo R, Manor, Uri, Gage, Fred H
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Sprache:eng
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Zusammenfassung:Astrocytes, the most abundant glial cell type in the brain, are underrepresented in traditional cortical organoid models due to the delayed onset of cortical gliogenesis. Here we introduce a new glia-enriched cortical organoid model that exhibits accelerated astrogliogenesis. We demonstrated that induction of a gliogenic switch in a subset of progenitors enabled the rapid derivation of astroglial cells, which account for 25-31% of the cell population within 8-10 weeks of differentiation. Intracerebral transplantation of these organoids reliably generated a diverse repertoire of cortical neurons and anatomical subclasses of human astrocytes. Spatial transcriptome profiling identified layer-specific expression patterns among distinct subclasses of astrocytes within organoid transplants. Using an in vivo acute neuroinflammation model, we identified a subpopulation of astrocytes that rapidly activates pro-inflammatory pathways upon cytokine stimulation. Additionally, we demonstrated that CD38 signaling has a crucial role in mediating metabolic and mitochondrial stress in reactive astrocytes. This model provides a robust platform for investigating human astrocyte function.
ISSN:1087-0156
1546-1696
1546-1696
DOI:10.1038/s41587-024-02157-8