2018
DOI: 10.1016/j.cell.2018.03.063
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Single-Cell Transcriptomics and Fate Mapping of Ependymal Cells Reveals an Absence of Neural Stem Cell Function

Abstract: Ependymal cells are multi-ciliated cells that form the brain's ventricular epithelium and a niche for neural stem cells (NSCs) in the ventricular-subventricular zone (V-SVZ). In addition, ependymal cells are suggested to be latent NSCs with a capacity to acquire neurogenic function. This remains highly controversial due to a lack of prospective in vivo labeling techniques that can effectively distinguish ependymal cells from neighboring V-SVZ NSCs. We describe a transgenic system that allows for targeted label… Show more

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Cited by 167 publications
(160 citation statements)
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“…A) or in neuroblasts (not shown) . Because we have demonstrated the presence of Sox2 protein in ependymal cells, qNSCs, aNSCs, and neuroblasts , as well as the expression of Sox2 mRNA in these populations (Fig. A), it may be that TF activity is regulated post‐translationally perhaps at the level of chromatin remodeling.…”
Section: What Underlies Functional Divergence In the Adult Nsc Niche?mentioning
confidence: 81%
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“…A) or in neuroblasts (not shown) . Because we have demonstrated the presence of Sox2 protein in ependymal cells, qNSCs, aNSCs, and neuroblasts , as well as the expression of Sox2 mRNA in these populations (Fig. A), it may be that TF activity is regulated post‐translationally perhaps at the level of chromatin remodeling.…”
Section: What Underlies Functional Divergence In the Adult Nsc Niche?mentioning
confidence: 81%
“…Although expression of most transcription factors (Sox2, Sox9, Klf9, Hes1 etc.) was similar across ependymal cells and qNSCs [17], there were several highly discrepant GRNs between these cell types ( Fig. 1B-D).…”
Section: What Underlies Functional Divergence In the Adult Nsc Niche?mentioning
confidence: 86%
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“…B. Johansson et al, 1999). Since then, there have been a number of studies that support both ideas (Kaur, Rathnasamy, & Ling, 2016;Luo et al, 2015;Mirzadeh et al, 2008;Shah et al, 2018). At the end, it has turned out that the soma and/or apical processes of NSCs actually reside in both the ependymal and subependymal regions, and, thus, cells with a NSCs capacity and typical ependymal cells with motile multi cilia coexist in the ependymal layer (Abdelhamed et al, 2018;Coletti et al, 2018;Del Bigio, 2010;Guo et al, 2010;S.…”
Section: Box 1 Impacts Of Non-neuronal/glial Cell Types On Postnatal mentioning
confidence: 98%
“…Although adult NSCs retain key epithelial properties of their progenitors, radial glial cells (Mirzadeh, Merkle, Soriano‐Navarro, Garcia‐Verdugo, & Alvarez‐Buylla, ), the ventricular surface in the adult brain displays a completely different pattern, as the small apical domains of NSCs are surrounded by the large apical surfaces of multiciliated ependymal cells (Mirzadeh et al, ). In contrast to NSCs, ependymal cells remain post‐mitotic and do not possess progenitor properties under physiological conditions (Shah et al, ; Spassky et al, ).…”
Section: Introductionmentioning
confidence: 99%