Nfix Regulates Fetal-Specific Transcription in Developing Skeletal Muscle

Graziella Messina; Stefano Biressi; Stefania Monteverde; Alessandro Magli; Marco Cassano; Laura Perani; Elena Roncaglia; Enrico Tagliafico; Linda Starnes; Christine E. Campbell; Milena Grossi; David J. Goldhamer; Richard M. Gronostajski; Giulio Cossu

doi:10.1016/j.cell.2010.01.027

Nfix Regulates Fetal-Specific Transcription in Developing Skeletal Muscle

Graziella Messina, Stefano Biressi, Stefania Monteverde, Alessandro Magli, Marco Cassano, Laura Perani, Elena Roncaglia, Enrico Tagliafico, Linda Starnes, Christine E. Campbell, Milena Grossi, David J. Goldhamer, Richard M. Gronostajski, Giulio Cossu

Medicine - Cardiology Division

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

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Abstract

Skeletal myogenesis, like hematopoiesis, occurs in successive developmental stages that involve different cell populations and expression of different genes. We show here that the transcription factor nuclear factor one X (Nfix), whose expression is activated by Pax7 in fetal muscle, in turn activates the transcription of fetal specific genes such as MCK and β-enolase while repressing embryonic genes such as slow myosin. In the case of the MCK promoter, Nfix forms a complex with PKC theta that binds, phosphorylates, and activates MEF2A. Premature expression of Nfix activates fetal and suppresses embryonic genes in embryonic muscle, whereas muscle-specific ablation of Nfix prevents fetal and maintains embryonic gene expression in the fetus. Therefore, Nfix acts as a transcriptional switch from embryonic to fetal myogenesis.

Original language	English (US)
Pages (from-to)	554-566
Number of pages	13
Journal	Cell
Volume	140
Issue number	4
DOIs	https://doi.org/10.1016/j.cell.2010.01.027
State	Published - Feb 19 2010

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DEVBIO

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title = "Nfix Regulates Fetal-Specific Transcription in Developing Skeletal Muscle",

abstract = "Skeletal myogenesis, like hematopoiesis, occurs in successive developmental stages that involve different cell populations and expression of different genes. We show here that the transcription factor nuclear factor one X (Nfix), whose expression is activated by Pax7 in fetal muscle, in turn activates the transcription of fetal specific genes such as MCK and β-enolase while repressing embryonic genes such as slow myosin. In the case of the MCK promoter, Nfix forms a complex with PKC theta that binds, phosphorylates, and activates MEF2A. Premature expression of Nfix activates fetal and suppresses embryonic genes in embryonic muscle, whereas muscle-specific ablation of Nfix prevents fetal and maintains embryonic gene expression in the fetus. Therefore, Nfix acts as a transcriptional switch from embryonic to fetal myogenesis.",

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AU - Messina, Graziella

AU - Biressi, Stefano

AU - Monteverde, Stefania

AU - Magli, Alessandro

AU - Cassano, Marco

AU - Perani, Laura

AU - Roncaglia, Elena

AU - Tagliafico, Enrico

AU - Starnes, Linda

AU - Campbell, Christine E.

AU - Grossi, Milena

AU - Goldhamer, David J.

AU - Gronostajski, Richard M.

AU - Cossu, Giulio

PY - 2010/2/19

Y1 - 2010/2/19

N2 - Skeletal myogenesis, like hematopoiesis, occurs in successive developmental stages that involve different cell populations and expression of different genes. We show here that the transcription factor nuclear factor one X (Nfix), whose expression is activated by Pax7 in fetal muscle, in turn activates the transcription of fetal specific genes such as MCK and β-enolase while repressing embryonic genes such as slow myosin. In the case of the MCK promoter, Nfix forms a complex with PKC theta that binds, phosphorylates, and activates MEF2A. Premature expression of Nfix activates fetal and suppresses embryonic genes in embryonic muscle, whereas muscle-specific ablation of Nfix prevents fetal and maintains embryonic gene expression in the fetus. Therefore, Nfix acts as a transcriptional switch from embryonic to fetal myogenesis.

AB - Skeletal myogenesis, like hematopoiesis, occurs in successive developmental stages that involve different cell populations and expression of different genes. We show here that the transcription factor nuclear factor one X (Nfix), whose expression is activated by Pax7 in fetal muscle, in turn activates the transcription of fetal specific genes such as MCK and β-enolase while repressing embryonic genes such as slow myosin. In the case of the MCK promoter, Nfix forms a complex with PKC theta that binds, phosphorylates, and activates MEF2A. Premature expression of Nfix activates fetal and suppresses embryonic genes in embryonic muscle, whereas muscle-specific ablation of Nfix prevents fetal and maintains embryonic gene expression in the fetus. Therefore, Nfix acts as a transcriptional switch from embryonic to fetal myogenesis.

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JF - Cell

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Nfix Regulates Fetal-Specific Transcription in Developing Skeletal Muscle

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