Cpeb4-Mediated Translational Regulatory Circuitry Controls Terminal Erythroid Differentiation

Wenqian Hu; Bingbing Yuan; Harvey F. Lodish

doi:10.1016/j.devcel.2014.07.008

Cpeb4-Mediated Translational Regulatory Circuitry Controls Terminal Erythroid Differentiation

Wenqian Hu, Bingbing Yuan, Harvey F. Lodish

Biochemistry and Molecular Biology

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

30 Scopus citations

Abstract

While we have considerable understanding of the transcriptional networks controlling mammalian cell differentiation, our knowledge of posttranscriptional regulatory events is very limited. Using differentiation of primary erythroid cells as a model, we show thatthe sequence-specific mRNA-binding protein Cpeb4 is strongly induced by the erythroid-important transcription factors Gata1 and Tal1 and is essential for terminal erythropoiesis. By interacting with the translation initiation factor eIF3, Cpeb4 represses the translation of a large set of mRNAs, including its own mRNA. Thus, transcriptional induction and translational repression combine to form a negative feedback loop to control Cpeb4 protein levels within a specific range that is required for terminal erythropoiesis. Our study provides an example of how translational control is integrated with transcriptional regulation to precisely control gene expression during mammalian cell differentiation.

Original language	English (US)
Pages (from-to)	660-672
Number of pages	13
Journal	Developmental Cell
Volume	30
Issue number	6
DOIs	https://doi.org/10.1016/j.devcel.2014.07.008
State	Published - Sep 29 2014

ASJC Scopus subject areas

Molecular Biology
Biochemistry, Genetics and Molecular Biology(all)
Developmental Biology
Cell Biology

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10.1016/j.devcel.2014.07.008

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title = "Cpeb4-Mediated Translational Regulatory Circuitry Controls Terminal Erythroid Differentiation",

abstract = "While we have considerable understanding of the transcriptional networks controlling mammalian cell differentiation, our knowledge of posttranscriptional regulatory events is very limited. Using differentiation of primary erythroid cells as a model, we show thatthe sequence-specific mRNA-binding protein Cpeb4 is strongly induced by the erythroid-important transcription factors Gata1 and Tal1 and is essential for terminal erythropoiesis. By interacting with the translation initiation factor eIF3, Cpeb4 represses the translation of a large set of mRNAs, including its own mRNA. Thus, transcriptional induction and translational repression combine to form a negative feedback loop to control Cpeb4 protein levels within a specific range that is required for terminal erythropoiesis. Our study provides an example of how translational control is integrated with transcriptional regulation to precisely control gene expression during mammalian cell differentiation.",

author = "Wenqian Hu and Bingbing Yuan and Lodish, {Harvey F.}",

note = "Funding Information: We thank Drs. Juan Alvarez, Jiahai Shi, Stephen Eichhorn, and Barry Paw for assistance on experiments and reagents; Dr. George Bell for critical reading of this manuscript; and the flow cytometry core at the Whitehead Institute and the Biopolymers & Proteomics Lab at MIT for technical support. W.H. is a Merck Fellow of the Life Sciences Research Foundation and is supported by a Pathway to Independence Award (1K99HL118157) from the NIH. This research was supported by NIH grants R01DK068348 and 5P01HL066105 to H.F.L. Publisher Copyright: {\textcopyright} 2014 Elsevier Inc.",

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N2 - While we have considerable understanding of the transcriptional networks controlling mammalian cell differentiation, our knowledge of posttranscriptional regulatory events is very limited. Using differentiation of primary erythroid cells as a model, we show thatthe sequence-specific mRNA-binding protein Cpeb4 is strongly induced by the erythroid-important transcription factors Gata1 and Tal1 and is essential for terminal erythropoiesis. By interacting with the translation initiation factor eIF3, Cpeb4 represses the translation of a large set of mRNAs, including its own mRNA. Thus, transcriptional induction and translational repression combine to form a negative feedback loop to control Cpeb4 protein levels within a specific range that is required for terminal erythropoiesis. Our study provides an example of how translational control is integrated with transcriptional regulation to precisely control gene expression during mammalian cell differentiation.

AB - While we have considerable understanding of the transcriptional networks controlling mammalian cell differentiation, our knowledge of posttranscriptional regulatory events is very limited. Using differentiation of primary erythroid cells as a model, we show thatthe sequence-specific mRNA-binding protein Cpeb4 is strongly induced by the erythroid-important transcription factors Gata1 and Tal1 and is essential for terminal erythropoiesis. By interacting with the translation initiation factor eIF3, Cpeb4 represses the translation of a large set of mRNAs, including its own mRNA. Thus, transcriptional induction and translational repression combine to form a negative feedback loop to control Cpeb4 protein levels within a specific range that is required for terminal erythropoiesis. Our study provides an example of how translational control is integrated with transcriptional regulation to precisely control gene expression during mammalian cell differentiation.

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Cpeb4-Mediated Translational Regulatory Circuitry Controls Terminal Erythroid Differentiation

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