p53/p21 pathway activation contributes to the ependymal fate decision downstream of GemC1

Gonzalo Ortiz-Álvarez; Aurélien Fortoul; Ayush Srivastava; Matthieu X. Moreau; Benoît Bouloudi; Caroline Mailhes-Hamon; Nathalie Delgehyr; Marion Faucourt; Mathieu Bahin; Corinne Blugeon; Marielle Breau; Vincent Géli; Frédéric Causeret; Alice Meunier; Nathalie Spassky

doi:10.1016/j.celrep.2022.111810

p53/p21 pathway activation contributes to the ependymal fate decision downstream of GemC1

Gonzalo Ortiz-Álvarez
, Aurélien Fortoul
, Ayush Srivastava
, Matthieu X. Moreau
, Benoît Bouloudi
, Caroline Mailhes-Hamon
, Nathalie Delgehyr
, Marion Faucourt
, Mathieu Bahin
, Corinne Blugeon
, Marielle Breau
, Vincent Géli
, Frédéric Causeret
, Alice Meunier
, Nathalie Spassky

Research output: Contribution to journal › Article › peer-review

Abstract

Multiciliated ependymal cells and adult neural stem cells are components of the adult neurogenic niche, essential for brain homeostasis. These cells share a common glial cell lineage regulated by the Geminin family members Geminin and GemC1/Mcidas. Ependymal precursors require GemC1/Mcidas expression to massively amplify centrioles and become multiciliated cells. Here, we show that GemC1-dependent differentiation is initiated in actively cycling radial glial cells, in which a DNA damage response, including DNA replication-associated damage and dysfunctional telomeres, is induced, without affecting cell survival. Genotoxic stress is not sufficient by itself to induce ependymal cell differentiation, although the absence of p53 or p21 in progenitors hinders differentiation by maintaining cell division. Activation of the p53-p21 pathway downstream of GemC1 leads to cell-cycle slowdown/arrest, which permits timely onset of ependymal cell differentiation in progenitor cells.

Original language	English
Article number	111810
Journal	Cell Reports
Volume	41
Issue number	11
DOIs	https://doi.org/10.1016/j.celrep.2022.111810
Publication status	Published - 13 Dec 2022
Externally published	Yes

Keywords

CP: Developmental biology
DNA damage
GemC1
brain ventricle
cell cycle
cell specification
ependyma
motile cilia
neural stem cell
p53-p21 pathway
telomerase

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10.1016/j.celrep.2022.111810

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Ortiz-Álvarez, G., Fortoul, A., Srivastava, A., Moreau, M. X., Bouloudi, B., Mailhes-Hamon, C., Delgehyr, N., Faucourt, M., Bahin, M., Blugeon, C., Breau, M., Géli, V., Causeret, F., Meunier, A., & Spassky, N. (2022). p53/p21 pathway activation contributes to the ependymal fate decision downstream of GemC1. Cell Reports, 41(11), Article 111810. https://doi.org/10.1016/j.celrep.2022.111810

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title = "p53/p21 pathway activation contributes to the ependymal fate decision downstream of GemC1",

abstract = "Multiciliated ependymal cells and adult neural stem cells are components of the adult neurogenic niche, essential for brain homeostasis. These cells share a common glial cell lineage regulated by the Geminin family members Geminin and GemC1/Mcidas. Ependymal precursors require GemC1/Mcidas expression to massively amplify centrioles and become multiciliated cells. Here, we show that GemC1-dependent differentiation is initiated in actively cycling radial glial cells, in which a DNA damage response, including DNA replication-associated damage and dysfunctional telomeres, is induced, without affecting cell survival. Genotoxic stress is not sufficient by itself to induce ependymal cell differentiation, although the absence of p53 or p21 in progenitors hinders differentiation by maintaining cell division. Activation of the p53-p21 pathway downstream of GemC1 leads to cell-cycle slowdown/arrest, which permits timely onset of ependymal cell differentiation in progenitor cells.",

keywords = "CP: Developmental biology, DNA damage, GemC1, brain ventricle, cell cycle, cell specification, ependyma, motile cilia, neural stem cell, p53-p21 pathway, telomerase",

author = "Gonzalo Ortiz-{\'A}lvarez and Aur{\'e}lien Fortoul and Ayush Srivastava and Moreau, \{Matthieu X.\} and Beno{\^i}t Bouloudi and Caroline Mailhes-Hamon and Nathalie Delgehyr and Marion Faucourt and Mathieu Bahin and Corinne Blugeon and Marielle Breau and Vincent G{\'e}li and Fr{\'e}d{\'e}ric Causeret and Alice Meunier and Nathalie Spassky",

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year = "2022",

month = dec,

day = "13",

doi = "10.1016/j.celrep.2022.111810",

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Ortiz-Álvarez, G, Fortoul, A, Srivastava, A, Moreau, MX, Bouloudi, B, Mailhes-Hamon, C, Delgehyr, N, Faucourt, M, Bahin, M, Blugeon, C, Breau, M, Géli, V, Causeret, F, Meunier, A & Spassky, N 2022, 'p53/p21 pathway activation contributes to the ependymal fate decision downstream of GemC1', Cell Reports, vol. 41, no. 11, 111810. https://doi.org/10.1016/j.celrep.2022.111810

TY - JOUR

T1 - p53/p21 pathway activation contributes to the ependymal fate decision downstream of GemC1

AU - Ortiz-Álvarez, Gonzalo

AU - Fortoul, Aurélien

AU - Srivastava, Ayush

AU - Moreau, Matthieu X.

AU - Bouloudi, Benoît

AU - Mailhes-Hamon, Caroline

AU - Delgehyr, Nathalie

AU - Faucourt, Marion

AU - Bahin, Mathieu

AU - Blugeon, Corinne

AU - Breau, Marielle

AU - Géli, Vincent

AU - Causeret, Frédéric

AU - Meunier, Alice

AU - Spassky, Nathalie

PY - 2022/12/13

Y1 - 2022/12/13

N2 - Multiciliated ependymal cells and adult neural stem cells are components of the adult neurogenic niche, essential for brain homeostasis. These cells share a common glial cell lineage regulated by the Geminin family members Geminin and GemC1/Mcidas. Ependymal precursors require GemC1/Mcidas expression to massively amplify centrioles and become multiciliated cells. Here, we show that GemC1-dependent differentiation is initiated in actively cycling radial glial cells, in which a DNA damage response, including DNA replication-associated damage and dysfunctional telomeres, is induced, without affecting cell survival. Genotoxic stress is not sufficient by itself to induce ependymal cell differentiation, although the absence of p53 or p21 in progenitors hinders differentiation by maintaining cell division. Activation of the p53-p21 pathway downstream of GemC1 leads to cell-cycle slowdown/arrest, which permits timely onset of ependymal cell differentiation in progenitor cells.

AB - Multiciliated ependymal cells and adult neural stem cells are components of the adult neurogenic niche, essential for brain homeostasis. These cells share a common glial cell lineage regulated by the Geminin family members Geminin and GemC1/Mcidas. Ependymal precursors require GemC1/Mcidas expression to massively amplify centrioles and become multiciliated cells. Here, we show that GemC1-dependent differentiation is initiated in actively cycling radial glial cells, in which a DNA damage response, including DNA replication-associated damage and dysfunctional telomeres, is induced, without affecting cell survival. Genotoxic stress is not sufficient by itself to induce ependymal cell differentiation, although the absence of p53 or p21 in progenitors hinders differentiation by maintaining cell division. Activation of the p53-p21 pathway downstream of GemC1 leads to cell-cycle slowdown/arrest, which permits timely onset of ependymal cell differentiation in progenitor cells.

KW - CP: Developmental biology

KW - DNA damage

KW - GemC1

KW - brain ventricle

KW - cell cycle

KW - cell specification

KW - ependyma

KW - motile cilia

KW - neural stem cell

KW - p53-p21 pathway

KW - telomerase

U2 - 10.1016/j.celrep.2022.111810

DO - 10.1016/j.celrep.2022.111810

M3 - Article

C2 - 36516767

AN - SCOPUS:85143875369

SN - 2211-1247

VL - 41

JO - Cell Reports

JF - Cell Reports

IS - 11

M1 - 111810

ER -

p53/p21 pathway activation contributes to the ependymal fate decision downstream of GemC1

Abstract

Keywords

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