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CNOT3-Dependent mRNA Deadenylation Safeguards the Pluripotent State

Poly(A) tail length and mRNA deadenylation play important roles in gene regulation. However, how they regulate embryonic development and pluripotent cell fate is not fully understood. Here we present evidence that CNOT3-dependent mRNA deadenylation governs the pluripotent state. We show that CNOT3,...

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Autores principales: Zheng, Xiaofeng, Yang, Pengyi, Lackford, Brad, Bennett, Brian D., Wang, Li, Li, Hui, Wang, Yu, Miao, Yiliang, Foley, Julie F., Fargo, David C., Jin, Ying, Williams, Carmen J., Jothi, Raja, Hu, Guang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5106518/
https://www.ncbi.nlm.nih.gov/pubmed/27746116
http://dx.doi.org/10.1016/j.stemcr.2016.09.007
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author Zheng, Xiaofeng
Yang, Pengyi
Lackford, Brad
Bennett, Brian D.
Wang, Li
Li, Hui
Wang, Yu
Miao, Yiliang
Foley, Julie F.
Fargo, David C.
Jin, Ying
Williams, Carmen J.
Jothi, Raja
Hu, Guang
author_facet Zheng, Xiaofeng
Yang, Pengyi
Lackford, Brad
Bennett, Brian D.
Wang, Li
Li, Hui
Wang, Yu
Miao, Yiliang
Foley, Julie F.
Fargo, David C.
Jin, Ying
Williams, Carmen J.
Jothi, Raja
Hu, Guang
author_sort Zheng, Xiaofeng
collection PubMed
description Poly(A) tail length and mRNA deadenylation play important roles in gene regulation. However, how they regulate embryonic development and pluripotent cell fate is not fully understood. Here we present evidence that CNOT3-dependent mRNA deadenylation governs the pluripotent state. We show that CNOT3, a component of the Ccr4-Not deadenylase complex, is required for mouse epiblast maintenance. It is highly expressed in blastocysts and its deletion leads to peri-implantation lethality. The epiblast cells in Cnot3 deletion embryos are quickly lost during diapause and fail to outgrow in culture. Mechanistically, CNOT3 C terminus is required for its interaction with the complex and its function in embryonic stem cells (ESCs). Furthermore, Cnot3 deletion results in increases in the poly(A) tail lengths, half-lives, and steady-state levels of differentiation gene mRNAs. The half-lives of CNOT3 target mRNAs are shorter in ESCs and become longer during normal differentiation. Together, we propose that CNOT3 maintains the pluripotent state by promoting differentiation gene mRNA deadenylation and degradation, and we identify poly(A) tail-length regulation as a post-transcriptional mechanism that controls pluripotency.
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spelling pubmed-51065182016-11-17 CNOT3-Dependent mRNA Deadenylation Safeguards the Pluripotent State Zheng, Xiaofeng Yang, Pengyi Lackford, Brad Bennett, Brian D. Wang, Li Li, Hui Wang, Yu Miao, Yiliang Foley, Julie F. Fargo, David C. Jin, Ying Williams, Carmen J. Jothi, Raja Hu, Guang Stem Cell Reports Article Poly(A) tail length and mRNA deadenylation play important roles in gene regulation. However, how they regulate embryonic development and pluripotent cell fate is not fully understood. Here we present evidence that CNOT3-dependent mRNA deadenylation governs the pluripotent state. We show that CNOT3, a component of the Ccr4-Not deadenylase complex, is required for mouse epiblast maintenance. It is highly expressed in blastocysts and its deletion leads to peri-implantation lethality. The epiblast cells in Cnot3 deletion embryos are quickly lost during diapause and fail to outgrow in culture. Mechanistically, CNOT3 C terminus is required for its interaction with the complex and its function in embryonic stem cells (ESCs). Furthermore, Cnot3 deletion results in increases in the poly(A) tail lengths, half-lives, and steady-state levels of differentiation gene mRNAs. The half-lives of CNOT3 target mRNAs are shorter in ESCs and become longer during normal differentiation. Together, we propose that CNOT3 maintains the pluripotent state by promoting differentiation gene mRNA deadenylation and degradation, and we identify poly(A) tail-length regulation as a post-transcriptional mechanism that controls pluripotency. Elsevier 2016-10-13 /pmc/articles/PMC5106518/ /pubmed/27746116 http://dx.doi.org/10.1016/j.stemcr.2016.09.007 Text en http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Zheng, Xiaofeng
Yang, Pengyi
Lackford, Brad
Bennett, Brian D.
Wang, Li
Li, Hui
Wang, Yu
Miao, Yiliang
Foley, Julie F.
Fargo, David C.
Jin, Ying
Williams, Carmen J.
Jothi, Raja
Hu, Guang
CNOT3-Dependent mRNA Deadenylation Safeguards the Pluripotent State
title CNOT3-Dependent mRNA Deadenylation Safeguards the Pluripotent State
title_full CNOT3-Dependent mRNA Deadenylation Safeguards the Pluripotent State
title_fullStr CNOT3-Dependent mRNA Deadenylation Safeguards the Pluripotent State
title_full_unstemmed CNOT3-Dependent mRNA Deadenylation Safeguards the Pluripotent State
title_short CNOT3-Dependent mRNA Deadenylation Safeguards the Pluripotent State
title_sort cnot3-dependent mrna deadenylation safeguards the pluripotent state
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5106518/
https://www.ncbi.nlm.nih.gov/pubmed/27746116
http://dx.doi.org/10.1016/j.stemcr.2016.09.007
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