Identification of a discrete subpopulation of spinal cord ependymal cells with neural stem cell properties

Moa Stenudd; Hanna Sabelström; Enric Llorens-Bobadilla; Margherita Zamboni; Hans Blom; Hjalmar Brismar; Shupei Zhang; Onur Basak; Hans Clevers; Christian Göritz; Fanie Barnabé-Heider; Jonas Frisén

doi:10.1016/j.celrep.2022.110440

Identification of a discrete subpopulation of spinal cord ependymal cells with neural stem cell properties

Moa Stenudd, Hanna Sabelström, Enric Llorens-Bobadilla, Margherita Zamboni, Hans Blom, Hjalmar Brismar, Shupei Zhang, Onur Basak, Hans Clevers, Christian Göritz, Fanie Barnabé-Heider, Jonas Frisén

Onderzoeksoutput: Bijdrage aan tijdschrift › Artikel › peer review

30 Citaten (Scopus)

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Spinal cord ependymal cells display neural stem cell properties in vitro and generate scar-forming astrocytes and remyelinating oligodendrocytes after injury. We report that ependymal cells are functionally heterogeneous and identify a small subpopulation (8% of ependymal cells and 0.1% of all cells in a spinal cord segment), which we denote ependymal A (EpA) cells, that accounts for the in vitro stem cell potential in the adult spinal cord. After spinal cord injury, EpA cells undergo self-renewing cell division as they give rise to differentiated progeny. Single-cell transcriptome analysis revealed a loss of ependymal cell gene expression programs as EpA cells gained signaling entropy and dedifferentiated to a stem-cell-like transcriptional state after an injury. We conclude that EpA cells are highly differentiated cells that can revert to a stem cell state and constitute a therapeutic target for spinal cord repair.

Originele taal-2	Engels
Artikelnummer	110440
Pagina's (van-tot)	110440
Tijdschrift	Cell reports
Volume	38
Nummer van het tijdschrift	9
DOI's	https://doi.org/10.1016/j.celrep.2022.110440
Status	Gepubliceerd - 1 mrt. 2022
Extern gepubliceerd	Ja

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10.1016/j.celrep.2022.110440

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Stenudd, M., Sabelström, H., Llorens-Bobadilla, E., Zamboni, M., Blom, H., Brismar, H., Zhang, S., Basak, O., Clevers, H., Göritz, C., Barnabé-Heider, F., & Frisén, J. (2022). Identification of a discrete subpopulation of spinal cord ependymal cells with neural stem cell properties. Cell reports, 38(9), 110440. Artikel 110440. https://doi.org/10.1016/j.celrep.2022.110440

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title = "Identification of a discrete subpopulation of spinal cord ependymal cells with neural stem cell properties",

abstract = "Spinal cord ependymal cells display neural stem cell properties in vitro and generate scar-forming astrocytes and remyelinating oligodendrocytes after injury. We report that ependymal cells are functionally heterogeneous and identify a small subpopulation (8\% of ependymal cells and 0.1\% of all cells in a spinal cord segment), which we denote ependymal A (EpA) cells, that accounts for the in vitro stem cell potential in the adult spinal cord. After spinal cord injury, EpA cells undergo self-renewing cell division as they give rise to differentiated progeny. Single-cell transcriptome analysis revealed a loss of ependymal cell gene expression programs as EpA cells gained signaling entropy and dedifferentiated to a stem-cell-like transcriptional state after an injury. We conclude that EpA cells are highly differentiated cells that can revert to a stem cell state and constitute a therapeutic target for spinal cord repair.",

keywords = "EpA cells, ependymal cells, neural stem cells, spinal cord injury, Neural Stem Cells/metabolism, Cell Differentiation/physiology, Humans, Neuroglia, Spinal Cord/metabolism, Spinal Cord Injuries/metabolism",

author = "Moa Stenudd and Hanna Sabelstr{\"o}m and Enric Llorens-Bobadilla and Margherita Zamboni and Hans Blom and Hjalmar Brismar and Shupei Zhang and Onur Basak and Hans Clevers and Christian G{\"o}ritz and Fanie Barnab{\'e}-Heider and Jonas Fris{\'e}n",

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doi = "10.1016/j.celrep.2022.110440",

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Stenudd, M, Sabelström, H, Llorens-Bobadilla, E, Zamboni, M, Blom, H, Brismar, H, Zhang, S, Basak, O, Clevers, H, Göritz, C, Barnabé-Heider, F & Frisén, J 2022, 'Identification of a discrete subpopulation of spinal cord ependymal cells with neural stem cell properties', Cell reports, vol. 38, nr. 9, 110440, blz. 110440. https://doi.org/10.1016/j.celrep.2022.110440

TY - JOUR

T1 - Identification of a discrete subpopulation of spinal cord ependymal cells with neural stem cell properties

AU - Stenudd, Moa

AU - Sabelström, Hanna

AU - Llorens-Bobadilla, Enric

AU - Zamboni, Margherita

AU - Blom, Hans

AU - Brismar, Hjalmar

AU - Zhang, Shupei

AU - Basak, Onur

AU - Clevers, Hans

AU - Göritz, Christian

AU - Barnabé-Heider, Fanie

AU - Frisén, Jonas

PY - 2022/3/1

Y1 - 2022/3/1

N2 - Spinal cord ependymal cells display neural stem cell properties in vitro and generate scar-forming astrocytes and remyelinating oligodendrocytes after injury. We report that ependymal cells are functionally heterogeneous and identify a small subpopulation (8% of ependymal cells and 0.1% of all cells in a spinal cord segment), which we denote ependymal A (EpA) cells, that accounts for the in vitro stem cell potential in the adult spinal cord. After spinal cord injury, EpA cells undergo self-renewing cell division as they give rise to differentiated progeny. Single-cell transcriptome analysis revealed a loss of ependymal cell gene expression programs as EpA cells gained signaling entropy and dedifferentiated to a stem-cell-like transcriptional state after an injury. We conclude that EpA cells are highly differentiated cells that can revert to a stem cell state and constitute a therapeutic target for spinal cord repair.

AB - Spinal cord ependymal cells display neural stem cell properties in vitro and generate scar-forming astrocytes and remyelinating oligodendrocytes after injury. We report that ependymal cells are functionally heterogeneous and identify a small subpopulation (8% of ependymal cells and 0.1% of all cells in a spinal cord segment), which we denote ependymal A (EpA) cells, that accounts for the in vitro stem cell potential in the adult spinal cord. After spinal cord injury, EpA cells undergo self-renewing cell division as they give rise to differentiated progeny. Single-cell transcriptome analysis revealed a loss of ependymal cell gene expression programs as EpA cells gained signaling entropy and dedifferentiated to a stem-cell-like transcriptional state after an injury. We conclude that EpA cells are highly differentiated cells that can revert to a stem cell state and constitute a therapeutic target for spinal cord repair.

KW - EpA cells

KW - ependymal cells

KW - neural stem cells

KW - spinal cord injury

KW - Neural Stem Cells/metabolism

KW - Cell Differentiation/physiology

KW - Humans

KW - Neuroglia

KW - Spinal Cord/metabolism

KW - Spinal Cord Injuries/metabolism

UR - https://www.scopus.com/pages/publications/85125224331

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DO - 10.1016/j.celrep.2022.110440

M3 - Article

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AN - SCOPUS:85125224331

SN - 2211-1247

VL - 38

SP - 110440

JO - Cell reports

JF - Cell reports

IS - 9

M1 - 110440

ER -

Identification of a discrete subpopulation of spinal cord ependymal cells with neural stem cell properties

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