Super-enhancer signature reveals key mechanisms associated with resistance to non-alcoholic steatohepatitis in humans with obesity

Hung, Yu‐Han; Sritharan, Ramja; Vohl, Marie‐Claude; Biertho, Laurent; Tchernof, André; White, Phillip J.; Sethupathy, Praveen

doi:10.1101/2021.08.20.457162

Cited by 4 publications

(2 citation statements)

References 159 publications

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“…NFIL3 and JUNB have been reported to play a role in all stages of human NAFLD [43]. NFIL3 was described as part of an enhancer hotspot associated gene in NASH-prone livers [44] and mechanistically affects gluconeogenesis in hepatocytes [45, p. 3] and lipid accumulation [46]. The preference of JunB in for ECM cluster genes (cluster 2) con rmed a recently described positive correlation of JunB levels with liver brosis in human and murine samples [47].…”

Section: Discussionmentioning

confidence: 82%

Alterations in the hepatocyte epigenetic landscape in steatosis

Schulz

Gasparoni

Nordström

et al. 2023

Preprint

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Fatty liver disease or the buildup of fat in the liver, has been reported to affect the global population. This comes with an increased risk for the development of fibrosis, cirrhosis, and hepatocellular carcinoma. Yet, little is known about the effects of fat and alcohol diet towards epigenetic aging, with respect to changes in transcriptional and epigenomic profiles. In this study, we took up a multi-omics approach and integrated gene expression, methylation signals, and chromatin signals to study the epigenomic effects of a high-fat and alcohol-containing diet on mouse hepatocytes. We identified 4 relevant protein-protein interaction network clusters that were associated with relevant pathways that promote steatosis. Using a machine learning approach, we predict specific transcription factors that might be responsible to modulate the functionally relevant clusters. Finally, we discover 4 additional CpG loci and validate that aging related differential CpG methylation. Differential CpG methylation linked to aging showed minimal overlap with altered methylation in steatosis.

show abstract

Section: Discussionmentioning

confidence: 82%

Alterations in the hepatocyte epigenetic landscape in steatosis

Schulz

Gasparoni

Nordström

et al. 2023

Preprint

View full text Add to dashboard Cite

show abstract

“…NFIL3 and JUNB have been reported to play a role in all stages of human NAFLD [ 46 ]. NFIL3 was described as part of an enhancer hotspot associated gene in NASH-prone livers [ 47 ] and mechanistically affects gluconeogenesis in hepatocytes [ 48 , p. 3] and lipid accumulation [ 49 ]. The preference of JunB for ECM cluster genes ( cluster 2) confirmed a recently described positive correlation of JunB levels with liver fibrosis in human and murine samples in hepatic stellate cells [ 50 ].…”

Section: Discussionmentioning

confidence: 99%

Alterations in the hepatocyte epigenetic landscape in steatosis

Maji

Czepukojc

Scherer

et al. 2023

Epigenetics & Chromatin

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Fatty liver disease or the accumulation of fat in the liver, has been reported to affect the global population. This comes with an increased risk for the development of fibrosis, cirrhosis, and hepatocellular carcinoma. Yet, little is known about the effects of a diet containing high fat and alcohol towards epigenetic aging, with respect to changes in transcriptional and epigenomic profiles. In this study, we took up a multi-omics approach and integrated gene expression, methylation signals, and chromatin signals to study the epigenomic effects of a high-fat and alcohol-containing diet on mouse hepatocytes. We identified four relevant gene network clusters that were associated with relevant pathways that promote steatosis. Using a machine learning approach, we predict specific transcription factors that might be responsible to modulate the functionally relevant clusters. Finally, we discover four additional CpG loci and validate aging-related differential CpG methylation. Differential CpG methylation linked to aging showed minimal overlap with altered methylation in steatosis.

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Characterization of regulatory transcriptional mechanisms in hepatocyte lipotoxicity

Pérez-Schindler

Vargas-Fernández

Karrer-Cardel

et al. 2022

Sci Rep

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Non-alcoholic fatty liver disease is a continuum of disorders among which non-alcoholic steatohepatitis (NASH) is particularly associated with a negative prognosis. Hepatocyte lipotoxicity is one of the main pathogenic factors of liver fibrosis and NASH. However, the molecular mechanisms regulating this process are poorly understood. The main aim of this study was to dissect transcriptional mechanisms regulated by lipotoxicity in hepatocytes. We achieved this aim by combining transcriptomic, proteomic and chromatin accessibility analyses from human liver and mouse hepatocytes. This integrative approach revealed several transcription factor networks deregulated by NASH and lipotoxicity. To validate these predictions, genetic deletion of the transcription factors MAFK and TCF4 was performed, resulting in hepatocytes that were better protected against saturated fatty acid oversupply. MAFK- and TCF4-regulated gene expression profiles suggest a mitigating effect against cell stress, while promoting cell survival and growth. Moreover, in the context of lipotoxicity, some MAFK and TCF4 target genes were to the corresponding differentially regulated transcripts in human liver fibrosis. Collectively, our findings comprehensively profile the transcriptional response to lipotoxicity in hepatocytes, revealing new molecular insights and providing a valuable resource for future endeavours to tackle the molecular mechanisms of NASH.

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Super-enhancer signature reveals key mechanisms associated with resistance to non-alcoholic steatohepatitis in humans with obesity

Cited by 4 publications

References 159 publications

Alterations in the hepatocyte epigenetic landscape in steatosis

Alterations in the hepatocyte epigenetic landscape in steatosis

Alterations in the hepatocyte epigenetic landscape in steatosis

Characterization of regulatory transcriptional mechanisms in hepatocyte lipotoxicity

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