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Deficiency of Ttyh1 downstream to Notch signaling results in precocious differentiation of neural stem cells

Mammalian neural stem cells (NSCs) are not only responsible for normal development of the central nervous system (CNS), but also participate in brain homeostasis and repair, thus hold promising clinical potentials in the treatment of neurodegenerative diseases and trauma. However the molecular netwo...

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Published in:Biochemical and biophysical research communications 2019-06, Vol.514 (3), p.842-847
Main Authors: Wu, Hai-Ning, Cao, Xiu-Li, Fang, Zheng, Zhang, Yu-Fei, Han, Wen-Juan, Yue, Kang-Yi, Cao, Yuan, Zheng, Min-Hua, Wang, Li-Li, Han, Hua
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cited_by cdi_FETCH-LOGICAL-c356t-fc726621b154c58471050de503b907ea25e8380bfaa4c8bd435bb12c1fa0da1c3
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container_title Biochemical and biophysical research communications
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creator Wu, Hai-Ning
Cao, Xiu-Li
Fang, Zheng
Zhang, Yu-Fei
Han, Wen-Juan
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Cao, Yuan
Zheng, Min-Hua
Wang, Li-Li
Han, Hua
description Mammalian neural stem cells (NSCs) are not only responsible for normal development of the central nervous system (CNS), but also participate in brain homeostasis and repair, thus hold promising clinical potentials in the treatment of neurodegenerative diseases and trauma. However the molecular networks regulating the stemness and differentiation of NSCs have not been fully understood. In this study, we show that Tweety-homolog 1 (Ttyh1), a five-pass transmembrane protein specifically expressed in mouse brain, is involved in maintaining stemness of murine NSCs. Blocking or activating Notch signal led to downregulation and upregulation of Ttyh1 in cultured NSCs, respectively, suggesting that Ttyh1 is under the control of Notch signaling. Knockdown of Ttyh1 in cultured NSCs resulted in a transient increase in the number and size of neurospheres, followed by a decrease of stemness as manifested by compromised neurosphere formation, downregulated stem cell markers, and increased neuronal differentiation. We generated Ttyh1 knockout mice by deleting its exon 4 using the CRISPR-Cas9 technology. Surprisingly, in contrast to a previous report, Ttyh1 knockout did not result in embryonic lethality. NSCs derived from Ttyh1 knockout mice phenocopied NSCs transfected with Ttyh1 siRNA. Immunofluorescence showed that loss of Ttyh1 leads to the increase of neurogenesis in adult mice. Taken together, these findings indicate that Ttyh1, which is likely downstream to Notch signaling, plays an important role in regulating NSCs. •In our study, Ttyh1 is required for the maintenance of stemness in NSCs.•Ttyh1 is a Notch downstream gene in NSCs.•Ttyh1 deficiency damages NSCs without embryonic lethality.•Increased neurogenesis occurs in the absence of Ttyh1 in adult mice.
doi_str_mv 10.1016/j.bbrc.2019.04.181
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subjects Neural stem cells (NSCs)
Notch
Stemness
Ttyh1
title Deficiency of Ttyh1 downstream to Notch signaling results in precocious differentiation of neural stem cells
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