The histone demethylase Phf2 acts as a molecular checkpoint to prevent NAFLD progression during obesity

Julien Bricambert; Marie Clotilde Alves-Guerra; Pauline Esteves; Carina Prip-Buus; Justine Bertrand-Michel; Hervé Guillou; Christopher J. Chang; Mark N. Vander Wal; François Canonne-Hergaux; Philippe Mathurin; Violeta Raverdy; François Pattou; Jean Girard; Catherine Postic; Renaud Dentin

doi:10.1038/s41467-018-04361-y

The histone demethylase Phf2 acts as a molecular checkpoint to prevent NAFLD progression during obesity

Julien Bricambert
, Marie Clotilde Alves-Guerra
, Pauline Esteves
, Carina Prip-Buus
, Justine Bertrand-Michel
, Hervé Guillou
, Christopher J. Chang
, Mark N. Vander Wal
, François Canonne-Hergaux
, Philippe Mathurin
, Violeta Raverdy
, François Pattou
, Jean Girard
, Catherine Postic
, Renaud Dentin

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

83 Scopus citations

Abstract

Aberrant histone methylation profile is reported to correlate with the development and progression of NAFLD during obesity. However, the identification of specific epigenetic modifiers involved in this process remains poorly understood. Here, we identify the histone demethylase Plant Homeodomain Finger 2 (Phf2) as a new transcriptional co-activator of the transcription factor Carbohydrate Responsive Element Binding Protein (ChREBP). By specifically erasing H3K9me2 methyl-marks on the promoter of ChREBP-regulated genes, Phf2 facilitates incorporation of metabolic precursors into mono-unsaturated fatty acids, leading to hepatosteatosis development in the absence of inflammation and insulin resistance. Moreover, the Phf2-mediated activation of the transcription factor NF-E2-related factor 2 (Nrf2) further reroutes glucose fluxes toward the pentose phosphate pathway and glutathione biosynthesis, protecting the liver from oxidative stress and fibrogenesis in response to diet-induced obesity. Overall, our findings establish a downstream epigenetic checkpoint, whereby Phf2, through facilitating H3K9me2 demethylation at specific gene promoters, protects liver from the pathogenesis progression of NAFLD.

Original language	English (US)
Article number	2092
Journal	Nature communications
Volume	9
Issue number	1
DOIs	https://doi.org/10.1038/s41467-018-04361-y
State	Published - Dec 1 2018
Externally published	Yes

All Science Journal Classification (ASJC) codes

General Chemistry
General Biochemistry, Genetics and Molecular Biology
General
General Physics and Astronomy

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10.1038/s41467-018-04361-y

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Bricambert, J., Alves-Guerra, M. C., Esteves, P., Prip-Buus, C., Bertrand-Michel, J., Guillou, H., Chang, C. J., Vander Wal, M. N., Canonne-Hergaux, F., Mathurin, P., Raverdy, V., Pattou, F., Girard, J., Postic, C., & Dentin, R. (2018). The histone demethylase Phf2 acts as a molecular checkpoint to prevent NAFLD progression during obesity. Nature communications, 9(1), Article 2092. https://doi.org/10.1038/s41467-018-04361-y

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title = "The histone demethylase Phf2 acts as a molecular checkpoint to prevent NAFLD progression during obesity",

abstract = "Aberrant histone methylation profile is reported to correlate with the development and progression of NAFLD during obesity. However, the identification of specific epigenetic modifiers involved in this process remains poorly understood. Here, we identify the histone demethylase Plant Homeodomain Finger 2 (Phf2) as a new transcriptional co-activator of the transcription factor Carbohydrate Responsive Element Binding Protein (ChREBP). By specifically erasing H3K9me2 methyl-marks on the promoter of ChREBP-regulated genes, Phf2 facilitates incorporation of metabolic precursors into mono-unsaturated fatty acids, leading to hepatosteatosis development in the absence of inflammation and insulin resistance. Moreover, the Phf2-mediated activation of the transcription factor NF-E2-related factor 2 (Nrf2) further reroutes glucose fluxes toward the pentose phosphate pathway and glutathione biosynthesis, protecting the liver from oxidative stress and fibrogenesis in response to diet-induced obesity. Overall, our findings establish a downstream epigenetic checkpoint, whereby Phf2, through facilitating H3K9me2 demethylation at specific gene promoters, protects liver from the pathogenesis progression of NAFLD.",

author = "Julien Bricambert and Alves-Guerra, \{Marie Clotilde\} and Pauline Esteves and Carina Prip-Buus and Justine Bertrand-Michel and Herv{\'e} Guillou and Chang, \{Christopher J.\} and \{Vander Wal\}, \{Mark N.\} and Fran{\c c}ois Canonne-Hergaux and Philippe Mathurin and Violeta Raverdy and Fran{\c c}ois Pattou and Jean Girard and Catherine Postic and Renaud Dentin",

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Bricambert, J, Alves-Guerra, MC, Esteves, P, Prip-Buus, C, Bertrand-Michel, J, Guillou, H, Chang, CJ, Vander Wal, MN, Canonne-Hergaux, F, Mathurin, P, Raverdy, V, Pattou, F, Girard, J, Postic, C & Dentin, R 2018, 'The histone demethylase Phf2 acts as a molecular checkpoint to prevent NAFLD progression during obesity', Nature communications, vol. 9, no. 1, 2092. https://doi.org/10.1038/s41467-018-04361-y

TY - JOUR

T1 - The histone demethylase Phf2 acts as a molecular checkpoint to prevent NAFLD progression during obesity

AU - Bricambert, Julien

AU - Alves-Guerra, Marie Clotilde

AU - Esteves, Pauline

AU - Prip-Buus, Carina

AU - Bertrand-Michel, Justine

AU - Guillou, Hervé

AU - Chang, Christopher J.

AU - Vander Wal, Mark N.

AU - Canonne-Hergaux, François

AU - Mathurin, Philippe

AU - Raverdy, Violeta

AU - Pattou, François

AU - Girard, Jean

AU - Postic, Catherine

AU - Dentin, Renaud

PY - 2018/12/1

Y1 - 2018/12/1

N2 - Aberrant histone methylation profile is reported to correlate with the development and progression of NAFLD during obesity. However, the identification of specific epigenetic modifiers involved in this process remains poorly understood. Here, we identify the histone demethylase Plant Homeodomain Finger 2 (Phf2) as a new transcriptional co-activator of the transcription factor Carbohydrate Responsive Element Binding Protein (ChREBP). By specifically erasing H3K9me2 methyl-marks on the promoter of ChREBP-regulated genes, Phf2 facilitates incorporation of metabolic precursors into mono-unsaturated fatty acids, leading to hepatosteatosis development in the absence of inflammation and insulin resistance. Moreover, the Phf2-mediated activation of the transcription factor NF-E2-related factor 2 (Nrf2) further reroutes glucose fluxes toward the pentose phosphate pathway and glutathione biosynthesis, protecting the liver from oxidative stress and fibrogenesis in response to diet-induced obesity. Overall, our findings establish a downstream epigenetic checkpoint, whereby Phf2, through facilitating H3K9me2 demethylation at specific gene promoters, protects liver from the pathogenesis progression of NAFLD.

AB - Aberrant histone methylation profile is reported to correlate with the development and progression of NAFLD during obesity. However, the identification of specific epigenetic modifiers involved in this process remains poorly understood. Here, we identify the histone demethylase Plant Homeodomain Finger 2 (Phf2) as a new transcriptional co-activator of the transcription factor Carbohydrate Responsive Element Binding Protein (ChREBP). By specifically erasing H3K9me2 methyl-marks on the promoter of ChREBP-regulated genes, Phf2 facilitates incorporation of metabolic precursors into mono-unsaturated fatty acids, leading to hepatosteatosis development in the absence of inflammation and insulin resistance. Moreover, the Phf2-mediated activation of the transcription factor NF-E2-related factor 2 (Nrf2) further reroutes glucose fluxes toward the pentose phosphate pathway and glutathione biosynthesis, protecting the liver from oxidative stress and fibrogenesis in response to diet-induced obesity. Overall, our findings establish a downstream epigenetic checkpoint, whereby Phf2, through facilitating H3K9me2 demethylation at specific gene promoters, protects liver from the pathogenesis progression of NAFLD.

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JF - Nature communications

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The histone demethylase Phf2 acts as a molecular checkpoint to prevent NAFLD progression during obesity

Abstract

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