Knockdown of Foxg1 in Sox9+ supporting cells increases the trans-differentiation of supporting cells into hair cells in the neonatal mouse utricle

Foxg1 plays important roles in regeneration of hair cell (HC) in the cochlea of neonatal mouse. Here, we used Sox9-CreER to knock down Foxg1 in supporting cells (SCs) in the utricle in order to investigate the role of Foxg1 in HC regeneration in the utricle. We found Sox9 an ideal marker of utricle...

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Autores principales: Zhang, Yuan, Zhang, Shasha, Zhang, Zhonghong, Dong, Ying, Ma, Xiangyu, Qiang, Ruiying, Chen, Yin, Gao, Xia, Zhao, Chunjie, Chen, Fangyi, He, Shuangba, Chai, Renjie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals 2020
Materias:
Priority Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7655167/
https://www.ncbi.nlm.nih.gov/pubmed/33099273
http://dx.doi.org/10.18632/aging.104009
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author Zhang, Yuan
Zhang, Shasha
Zhang, Zhonghong
Dong, Ying
Ma, Xiangyu
Qiang, Ruiying
Chen, Yin
Gao, Xia
Zhao, Chunjie
Chen, Fangyi
He, Shuangba
Chai, Renjie
author_facet Zhang, Yuan
Zhang, Shasha
Zhang, Zhonghong
Dong, Ying
Ma, Xiangyu
Qiang, Ruiying
Chen, Yin
Gao, Xia
Zhao, Chunjie
Chen, Fangyi
He, Shuangba
Chai, Renjie
author_sort Zhang, Yuan
collection PubMed
description Foxg1 plays important roles in regeneration of hair cell (HC) in the cochlea of neonatal mouse. Here, we used Sox9-CreER to knock down Foxg1 in supporting cells (SCs) in the utricle in order to investigate the role of Foxg1 in HC regeneration in the utricle. We found Sox9 an ideal marker of utricle SCs and bred Sox9(CreER/+)Foxg1(loxp/loxp) mice to conditionally knock down Foxg1 in utricular SCs. Conditional knockdown (cKD) of Foxg1 in SCs at postnatal day one (P01) led to increased number of HCs at P08. These regenerated HCs had normal characteristics, and could survive to at least P30. Lineage tracing showed that a significant portion of newly regenerated HCs originated from SCs in Foxg1 cKD mice compared to the mice subjected to the same treatment, which suggested SCs trans-differentiate into HCs in the Foxg1 cKD mouse utricle. After neomycin treatment in vitro, more HCs were observed in Foxg1 cKD mice utricle compared to the control group. Together, these results suggest that Foxg1 cKD in utricular SCs may promote HC regeneration by inducing trans-differentiation of SCs. This research therefore provides theoretical basis for the effects of Foxg1 in trans-differentiation of SCs and regeneration of HCs in the mouse utricle.
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spelling pubmed-76551672020-11-19 Knockdown of Foxg1 in Sox9+ supporting cells increases the trans-differentiation of supporting cells into hair cells in the neonatal mouse utricle Zhang, Yuan Zhang, Shasha Zhang, Zhonghong Dong, Ying Ma, Xiangyu Qiang, Ruiying Chen, Yin Gao, Xia Zhao, Chunjie Chen, Fangyi He, Shuangba Chai, Renjie Aging (Albany NY) Priority Research Paper Foxg1 plays important roles in regeneration of hair cell (HC) in the cochlea of neonatal mouse. Here, we used Sox9-CreER to knock down Foxg1 in supporting cells (SCs) in the utricle in order to investigate the role of Foxg1 in HC regeneration in the utricle. We found Sox9 an ideal marker of utricle SCs and bred Sox9(CreER/+)Foxg1(loxp/loxp) mice to conditionally knock down Foxg1 in utricular SCs. Conditional knockdown (cKD) of Foxg1 in SCs at postnatal day one (P01) led to increased number of HCs at P08. These regenerated HCs had normal characteristics, and could survive to at least P30. Lineage tracing showed that a significant portion of newly regenerated HCs originated from SCs in Foxg1 cKD mice compared to the mice subjected to the same treatment, which suggested SCs trans-differentiate into HCs in the Foxg1 cKD mouse utricle. After neomycin treatment in vitro, more HCs were observed in Foxg1 cKD mice utricle compared to the control group. Together, these results suggest that Foxg1 cKD in utricular SCs may promote HC regeneration by inducing trans-differentiation of SCs. This research therefore provides theoretical basis for the effects of Foxg1 in trans-differentiation of SCs and regeneration of HCs in the mouse utricle. Impact Journals 2020-10-24 /pmc/articles/PMC7655167/ /pubmed/33099273 http://dx.doi.org/10.18632/aging.104009 Text en Copyright: © 2020 Zhang et al. https://creativecommons.org/licenses/by/3.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/3.0/) (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Priority Research Paper
Zhang, Yuan
Zhang, Shasha
Zhang, Zhonghong
Dong, Ying
Ma, Xiangyu
Qiang, Ruiying
Chen, Yin
Gao, Xia
Zhao, Chunjie
Chen, Fangyi
He, Shuangba
Chai, Renjie
Knockdown of Foxg1 in Sox9+ supporting cells increases the trans-differentiation of supporting cells into hair cells in the neonatal mouse utricle
title Knockdown of Foxg1 in Sox9+ supporting cells increases the trans-differentiation of supporting cells into hair cells in the neonatal mouse utricle
title_full Knockdown of Foxg1 in Sox9+ supporting cells increases the trans-differentiation of supporting cells into hair cells in the neonatal mouse utricle
title_fullStr Knockdown of Foxg1 in Sox9+ supporting cells increases the trans-differentiation of supporting cells into hair cells in the neonatal mouse utricle
title_full_unstemmed Knockdown of Foxg1 in Sox9+ supporting cells increases the trans-differentiation of supporting cells into hair cells in the neonatal mouse utricle
title_short Knockdown of Foxg1 in Sox9+ supporting cells increases the trans-differentiation of supporting cells into hair cells in the neonatal mouse utricle
title_sort knockdown of foxg1 in sox9+ supporting cells increases the trans-differentiation of supporting cells into hair cells in the neonatal mouse utricle
topic Priority Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7655167/
https://www.ncbi.nlm.nih.gov/pubmed/33099273
http://dx.doi.org/10.18632/aging.104009
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