Isolation and characterisation of neural progenitor cells from the adult Chx10orJ/orJ central neural retina

I. Kokkinopoulos; R. A. Pearson; A. MacNeil; N. S. Dhomen; R. E. MacLaren; R. R. Ali; J. C. Sowden

doi:10.1016/j.mcn.2008.03.008

Isolation and characterisation of neural progenitor cells from the adult Chx10^orJ/orJ central neural retina

I. Kokkinopoulos, R. A. Pearson, A. MacNeil, N. S. Dhomen, R. E. MacLaren, R. R. Ali, J. C. Sowden^*

^*Corresponding author for this work

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

8 Citations (Scopus)

Abstract

Retinal stem cells have been isolated from the ciliary epithelium (CE) of the mammalian retina. However, the central neural retina (CNR) lacks the capability to regenerate, a phenomenon retained by lower vertebrates. Mutations in the Chx10 homeobox gene cause reduced proliferation of retinal progenitor cells during development, leading to microphthalmia. Recently, we showed that in Chx10^orJ/orJ mice, dividing cells persist in the adult CNR, suggesting the existence of a dormant progenitor population. Here, we show that these cells are proliferative and give rise to neurospheres in vitro, a characteristic of neural stem cells. However, these adult-derived CNR progenitors differ from those of the wildtype CE, leading to de-pigmented, larger and more numerous neurospheres expressing Müller glial cell markers. Our results suggest that lack of Chx10 leads to maintenance of a dormant neural progenitor population in the adult CNR. Furthermore, Chx10 is not required for in vitro proliferation of these progenitors.

Original language	English
Pages (from-to)	359-373
Number of pages	15
Journal	Molecular and Cellular Neuroscience
Volume	38
Issue number	3
DOIs	https://doi.org/10.1016/j.mcn.2008.03.008
Publication status	Published - Jul 2008

Keywords

Adult stem cell
Chx10
Mouse
Müller cell
Müller progenitor
Neural progenitor cell
Neurosphere
Retina

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10.1016/j.mcn.2008.03.008

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title = "Isolation and characterisation of neural progenitor cells from the adult Chx10orJ/orJ central neural retina",

abstract = "Retinal stem cells have been isolated from the ciliary epithelium (CE) of the mammalian retina. However, the central neural retina (CNR) lacks the capability to regenerate, a phenomenon retained by lower vertebrates. Mutations in the Chx10 homeobox gene cause reduced proliferation of retinal progenitor cells during development, leading to microphthalmia. Recently, we showed that in Chx10orJ/orJ mice, dividing cells persist in the adult CNR, suggesting the existence of a dormant progenitor population. Here, we show that these cells are proliferative and give rise to neurospheres in vitro, a characteristic of neural stem cells. However, these adult-derived CNR progenitors differ from those of the wildtype CE, leading to de-pigmented, larger and more numerous neurospheres expressing M{\"u}ller glial cell markers. Our results suggest that lack of Chx10 leads to maintenance of a dormant neural progenitor population in the adult CNR. Furthermore, Chx10 is not required for in vitro proliferation of these progenitors.",

keywords = "Adult stem cell, Chx10, Mouse, M{\"u}ller cell, M{\"u}ller progenitor, Neural progenitor cell, Neurosphere, Retina",

author = "I. Kokkinopoulos and Pearson, {R. A.} and A. MacNeil and Dhomen, {N. S.} and MacLaren, {R. E.} and Ali, {R. R.} and Sowden, {J. C.}",

note = "Funding Information: This work was supported by grants from Fight for Sight, UK, the Medical Research Council UK (G0300341 and G0700438), the Macula Vision Research Foundation and the Scottish National Institute for the War Blinded. IK and NS are Fight for Sight PhD students. RAP is a Royal Society University Research Fellow. REM is a Health Foundation Clinician Scientist. We thank Patrizia Ferretti for critical discussions during the project. Copyright: Copyright 2009 Elsevier B.V., All rights reserved.",

year = "2008",

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doi = "10.1016/j.mcn.2008.03.008",

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AU - MacNeil, A.

AU - Dhomen, N. S.

AU - MacLaren, R. E.

AU - Ali, R. R.

AU - Sowden, J. C.

N1 - Funding Information: This work was supported by grants from Fight for Sight, UK, the Medical Research Council UK (G0300341 and G0700438), the Macula Vision Research Foundation and the Scottish National Institute for the War Blinded. IK and NS are Fight for Sight PhD students. RAP is a Royal Society University Research Fellow. REM is a Health Foundation Clinician Scientist. We thank Patrizia Ferretti for critical discussions during the project. Copyright: Copyright 2009 Elsevier B.V., All rights reserved.

PY - 2008/7

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N2 - Retinal stem cells have been isolated from the ciliary epithelium (CE) of the mammalian retina. However, the central neural retina (CNR) lacks the capability to regenerate, a phenomenon retained by lower vertebrates. Mutations in the Chx10 homeobox gene cause reduced proliferation of retinal progenitor cells during development, leading to microphthalmia. Recently, we showed that in Chx10orJ/orJ mice, dividing cells persist in the adult CNR, suggesting the existence of a dormant progenitor population. Here, we show that these cells are proliferative and give rise to neurospheres in vitro, a characteristic of neural stem cells. However, these adult-derived CNR progenitors differ from those of the wildtype CE, leading to de-pigmented, larger and more numerous neurospheres expressing Müller glial cell markers. Our results suggest that lack of Chx10 leads to maintenance of a dormant neural progenitor population in the adult CNR. Furthermore, Chx10 is not required for in vitro proliferation of these progenitors.

AB - Retinal stem cells have been isolated from the ciliary epithelium (CE) of the mammalian retina. However, the central neural retina (CNR) lacks the capability to regenerate, a phenomenon retained by lower vertebrates. Mutations in the Chx10 homeobox gene cause reduced proliferation of retinal progenitor cells during development, leading to microphthalmia. Recently, we showed that in Chx10orJ/orJ mice, dividing cells persist in the adult CNR, suggesting the existence of a dormant progenitor population. Here, we show that these cells are proliferative and give rise to neurospheres in vitro, a characteristic of neural stem cells. However, these adult-derived CNR progenitors differ from those of the wildtype CE, leading to de-pigmented, larger and more numerous neurospheres expressing Müller glial cell markers. Our results suggest that lack of Chx10 leads to maintenance of a dormant neural progenitor population in the adult CNR. Furthermore, Chx10 is not required for in vitro proliferation of these progenitors.

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Isolation and characterisation of neural progenitor cells from the adult Chx10^orJ/orJ central neural retina

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Keywords

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