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Dysregulation of the SIRT1/OCT6 Axis Contributes to Environmental Stress-Induced Neural Induction Defects.


ABSTRACT: Environmental stresses are increasingly acknowledged as core causes of abnormal neural induction leading to neural tube defects (NTDs). However, the mechanism responsible for environmental stress-triggered neural induction defects remains unknown. Here, we report that a spectrum of environmental stresses, including oxidative stress, starvation, and DNA damage, profoundly activate SIRT1, an NAD+-dependent lysine deacetylase. Both mouse embryos and in vitro differentiated embryonic stem cells (ESCs) demonstrated a negative correlation between the expression of SIRT1 and that of OCT6, a key neural fate inducer. Activated SIRT1 radically deacetylates OCT6, triggers an OCT6 ubiquitination/degradation cascade, and consequently increases the incidence of NTD-like phenotypes in mice or hinders neural induction in both human and mouse ESCs. Together, our results suggest that early exposure to environmental stresses results in the dysregulation of the SIRT1/OCT6 axis and increases the risk of NTDs.

SUBMITTER: Li G 

PROVIDER: S-EPMC5425630 | biostudies-literature | 2017 May

REPOSITORIES: biostudies-literature

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Dysregulation of the SIRT1/OCT6 Axis Contributes to Environmental Stress-Induced Neural Induction Defects.

Li Guoping G   Jiapaer Zeyidan Z   Weng Rong R   Hui Yi Y   Jia Wenwen W   Xi Jiajie J   Wang Guiying G   Zhu Songcheng S   Zhang Xin X   Feng Dandan D   Liu Ling L   Zhang Xiaoqing X   Kang Jiuhong J  

Stem cell reports 20170420 5


Environmental stresses are increasingly acknowledged as core causes of abnormal neural induction leading to neural tube defects (NTDs). However, the mechanism responsible for environmental stress-triggered neural induction defects remains unknown. Here, we report that a spectrum of environmental stresses, including oxidative stress, starvation, and DNA damage, profoundly activate SIRT1, an NAD<sup>+</sup>-dependent lysine deacetylase. Both mouse embryos and in vitro differentiated embryonic stem  ...[more]

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