Defective HNF4alpha-dependent gene expression as a driver of hepatocellular failure in alcoholic hepatitis

Alcoholic hepatitis (AH) is a life-threatening condition characterized by profound hepatocellular dysfunction for which targeted treatments are urgently needed. Identification of molecular drivers is hampered by the lack of suitable animal models. By performing RNA sequencing in livers from patients...

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Published in	Nature communications Vol. 10; no. 1; pp. 3126 - 19
Main Authors	Argemi, Josepmaria, Latasa, Maria U., Atkinson, Stephen R., Blokhin, Ilya O., Massey, Veronica, Gue, Joel P., Cabezas, Joaquin, Lozano, Juan J., Van Booven, Derek, Bell, Aaron, Cao, Sheng, Vernetti, Lawrence A., Arab, Juan P., Ventura-Cots, Meritxell, Edmunds, Lia R., Fondevila, Constantino, Stärkel, Peter, Dubuquoy, Laurent, Louvet, Alexandre, Odena, Gemma, Gomez, Juan L., Aragon, Tomas, Altamirano, Jose, Caballeria, Juan, Jurczak, Michael J., Taylor, D. Lansing, Berasain, Carmen, Wahlestedt, Claes, Monga, Satdarshan P., Morgan, Marsha Y., Sancho-Bru, Pau, Mathurin, Philippe, Furuya, Shinji, Lackner, Carolin, Rusyn, Ivan, Shah, Vijay H., Thursz, Mark R., Mann, Jelena, Avila, Matias A., Bataller, Ramon
Format	Journal Article
Language	English
Published	London Nature Publishing Group UK 16.07.2019 Nature Publishing Group Nature Portfolio
Series	Nature Communications
Subjects	13/1 13/109 13/51 13/89 14 38/15 38/91 45/61 631/114/2114 692/4020/4021/1607/1608 692/4020/4021/288/2032 Adult Aged Alcoholic beverages Animal models Animals Biopsy Chromatin Assembly and Disassembly Chromatin remodeling Deoxyribonucleic acid Disease Progression DNA DNA Methylation Epigenesis, Genetic Epigenetics Female Gene expression Gene Expression Profiling Gene Expression Regulation Gene polymorphism Gene sequencing Hepatitis Hepatitis, Alcoholic - genetics Hepatitis, Alcoholic - pathology Hepatocyte nuclear factor 4 Hepatocyte Nuclear Factor 4 - genetics Hepatocyte Nuclear Factor 4 - metabolism Hepatocytes Hepatocytes - pathology Humanities and Social Sciences Humans Life Sciences Liver Liver - cytology Liver - pathology Liver diseases Male Middle Aged multidisciplinary Phenotypes Polymorphism, Genetic Ribonucleic acid RNA Science Sequence Analysis, RNA Transcription factors Transcriptomes Transforming Growth Factor beta1 - genetics Transforming Growth Factor beta1 - metabolism Transforming growth factor-b1 Transforming Growth Factor beta1 RNA Humans Liver Middle Aged Gene Expression Regulation Chromatin Assembly and Disassembly Genetic Male Gene Expression Profiling Disease Progression Hepatitis DNA Methylation Animals Hepatocytes Biopsy Alcoholic Adult Female Aged Epigenesis Hepatocyte Nuclear Factor 4 Sequence Analysis Polymorphism
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Abstract	Alcoholic hepatitis (AH) is a life-threatening condition characterized by profound hepatocellular dysfunction for which targeted treatments are urgently needed. Identification of molecular drivers is hampered by the lack of suitable animal models. By performing RNA sequencing in livers from patients with different phenotypes of alcohol-related liver disease (ALD), we show that development of AH is characterized by defective activity of liver-enriched transcription factors (LETFs). TGF β 1 is a key upstream transcriptome regulator in AH and induces the use of HNF4 α P2 promoter in hepatocytes, which results in defective metabolic and synthetic functions. Gene polymorphisms in LETFs including HNF4 α are not associated with the development of AH. In contrast, epigenetic studies show that AH livers have profound changes in DNA methylation state and chromatin remodeling, affecting HNF4 α -dependent gene expression. We conclude that targeting TGF β 1 and epigenetic drivers that modulate HNF4 α -dependent gene expression could be beneficial to improve hepatocellular function in patients with AH. Alcoholic hepatitis, a common cause of liver failure, lacks effective treatment. Here, the authors show altered hepatic HNF4a isoform expression and hypermethylation of its target genes in patients. HNF4a dysregulation is improved in vitro by TGFb or PPARg modulation suggesting potential therapeutic avenues.
AbstractList	Alcoholic hepatitis (AH) is a life-threatening condition characterized by profound hepatocellular dysfunction for which targeted treatments are urgently needed. Identification of molecular drivers is hampered by the lack of suitable animal models. By performing RNA sequencing in livers from patients with different phenotypes of alcohol-related liver disease (ALD), we show that development of AH is characterized by defective activity of liver-enriched transcription factors (LETFs). TGFβ1 is a key upstream transcriptome regulator in AH and induces the use of HNF4α P2 promoter in hepatocytes, which results in defective metabolic and synthetic functions. Gene polymorphisms in LETFs including HNF4α are not associated with the development of AH. In contrast, epigenetic studies show that AH livers have profound changes in DNA methylation state and chromatin remodeling, affecting HNF4α-dependent gene expression. We conclude that targeting TGFβ1 and epigenetic drivers that modulate HNF4α-dependent gene expression could be beneficial to improve hepatocellular function in patients with AH. Alcoholic hepatitis (AH) is a life-threatening condition characterized by profound hepatocellular dysfunction for which targeted treatments are urgently needed. Identification of molecular drivers is hampered by the lack of suitable animal models. By performing RNA sequencing in livers from patients with different phenotypes of alcohol-related liver disease (ALD), we show that development of AH is characterized by defective activity of liver-enriched transcription factors (LETFs). TGFβ1 is a key upstream transcriptome regulator in AH and induces the use of HNF4α P2 promoter in hepatocytes, which results in defective metabolic and synthetic functions. Gene polymorphisms in LETFs including HNF4α are not associated with the development of AH. In contrast, epigenetic studies show that AH livers have profound changes in DNA methylation state and chromatin remodeling, affecting HNF4α-dependent gene expression. We conclude that targeting TGFβ1 and epigenetic drivers that modulate HNF4α-dependent gene expression could be beneficial to improve hepatocellular function in patients with AH.Alcoholic hepatitis (AH) is a life-threatening condition characterized by profound hepatocellular dysfunction for which targeted treatments are urgently needed. Identification of molecular drivers is hampered by the lack of suitable animal models. By performing RNA sequencing in livers from patients with different phenotypes of alcohol-related liver disease (ALD), we show that development of AH is characterized by defective activity of liver-enriched transcription factors (LETFs). TGFβ1 is a key upstream transcriptome regulator in AH and induces the use of HNF4α P2 promoter in hepatocytes, which results in defective metabolic and synthetic functions. Gene polymorphisms in LETFs including HNF4α are not associated with the development of AH. In contrast, epigenetic studies show that AH livers have profound changes in DNA methylation state and chromatin remodeling, affecting HNF4α-dependent gene expression. We conclude that targeting TGFβ1 and epigenetic drivers that modulate HNF4α-dependent gene expression could be beneficial to improve hepatocellular function in patients with AH. Alcoholic hepatitis (AH) is a life-threatening condition characterized by profound hepatocellular dysfunction for which targeted treatments are urgently needed. Identification of molecular drivers is hampered by the lack of suitable animal models. By performing RNA sequencing in livers from patients with different phenotypes of alcohol-related liver disease (ALD), we show that development of AH is characterized by defective activity of liver-enriched transcription factors (LETFs). TGF β 1 is a key upstream transcriptome regulator in AH and induces the use of HNF4 α P2 promoter in hepatocytes, which results in defective metabolic and synthetic functions. Gene polymorphisms in LETFs including HNF4 α are not associated with the development of AH. In contrast, epigenetic studies show that AH livers have profound changes in DNA methylation state and chromatin remodeling, affecting HNF4 α -dependent gene expression. We conclude that targeting TGF β 1 and epigenetic drivers that modulate HNF4 α -dependent gene expression could be beneficial to improve hepatocellular function in patients with AH. Alcoholic hepatitis, a common cause of liver failure, lacks effective treatment. Here, the authors show altered hepatic HNF4a isoform expression and hypermethylation of its target genes in patients. HNF4a dysregulation is improved in vitro by TGFb or PPARg modulation suggesting potential therapeutic avenues. Alcoholic hepatitis, a common cause of liver failure, lacks effective treatment. Here, the authors show altered hepatic HNF4a isoform expression and hypermethylation of its target genes in patients. HNF4a dysregulation is improved in vitro by TGFb or PPARg modulation suggesting potential therapeutic avenues. Alcoholic hepatitis (AH) is a life-threatening condition characterized by profound hepatocellular dysfunction for which targeted treatments are urgently needed. Identification of molecular drivers is hampered by the lack of suitable animal models. By performing RNA sequencing in livers from patients with different phenotypes of alcohol-related liver disease (ALD), we show that development of AH is characterized by defective activity of liver-enriched transcription factors (LETFs). TGFβ1 is a key upstream transcriptome regulator in AH and induces the use of HNF4α P2 promoter in hepatocytes, which results in defective metabolic and synthetic functions. Gene polymorphisms in LETFs including HNF4α are not associated with the development of AH. In contrast, epigenetic studies show that AH livers have profound changes in DNA methylation state and chromatin remodeling, affecting HNF4α-dependent gene expression. We conclude that targeting TGFβ1 and epigenetic drivers that modulate HNF4α-dependent gene expression could be beneficial to improve hepatocellular function in patients with AH.Alcoholic hepatitis, a common cause of liver failure, lacks effective treatment. Here, the authors show altered hepatic HNF4a isoform expression and hypermethylation of its target genes in patients. HNF4a dysregulation is improved in vitro by TGFb or PPARg modulation suggesting potential therapeutic avenues. Alcoholic hepatitis (AH) is a life-threatening condition characterized by profound hepatocellular dysfunction for which targeted treatments are urgently needed. Identification of molecular drivers is hampered by the lack of suitable animal models. By performing RNA sequencing in livers from patients with different phenotypes of alcohol-related liver disease (ALD), we show that development of AH is characterized by defective activity of liver-enriched transcription factors (LETFs). TGF β 1 is a key upstream transcriptome regulator in AH and induces the use of HNF4 α P2 promoter in hepatocytes, which results in defective metabolic and synthetic functions. Gene polymorphisms in LETFs including HNF4 α are not associated with the development of AH. In contrast, epigenetic studies show that AH livers have profound changes in DNA methylation state and chromatin remodeling, affecting HNF4 α -dependent gene expression. We conclude that targeting TGF β 1 and epigenetic drivers that modulate HNF4 α -dependent gene expression could be beneficial to improve hepatocellular function in patients with AH.
ArticleNumber	3126
Author	Mathurin, Philippe Sancho-Bru, Pau Blokhin, Ilya O. Dubuquoy, Laurent Gomez, Juan L. Arab, Juan P. Shah, Vijay H. Odena, Gemma Altamirano, Jose Massey, Veronica Edmunds, Lia R. Furuya, Shinji Monga, Satdarshan P. Wahlestedt, Claes Rusyn, Ivan Argemi, Josepmaria Aragon, Tomas Jurczak, Michael J. Thursz, Mark R. Lozano, Juan J. Ventura-Cots, Meritxell Caballeria, Juan Morgan, Marsha Y. Avila, Matias A. Atkinson, Stephen R. Gue, Joel P. Louvet, Alexandre Cabezas, Joaquin Bell, Aaron Latasa, Maria U. Lackner, Carolin Van Booven, Derek Vernetti, Lawrence A. Bataller, Ramon Berasain, Carmen Fondevila, Constantino Cao, Sheng Stärkel, Peter Taylor, D. Lansing Mann, Jelena
Author_xml	– sequence: 1 givenname: Josepmaria orcidid: 0000-0003-1696-7753 surname: Argemi fullname: Argemi, Josepmaria organization: Division of Gastroenterology, Hepatology and Nutrition, Pittsburgh Liver Research Center, University of Pittsburgh Medical Center (UPMC), Liver Unit, Clínica Universidad de Navarra, University of Navarra – sequence: 2 givenname: Maria U. orcidid: 0000-0002-0878-1337 surname: Latasa fullname: Latasa, Maria U. organization: Hepatology Program, Center for Applied Medical Research (CIMA), University of Navarra – sequence: 3 givenname: Stephen R. surname: Atkinson fullname: Atkinson, Stephen R. organization: Division of Digestive Diseases, Department of Surgery and Cancer, Imperial College London – sequence: 4 givenname: Ilya O. surname: Blokhin fullname: Blokhin, Ilya O. organization: Center for Therapeutic Innovation and Department of Psychiatry and Behavioral Sciences, University of Miami Miller School of Medicine – sequence: 5 givenname: Veronica surname: Massey fullname: Massey, Veronica organization: Division of Gastroenterology and Hepatology, Departments of Medicine and Nutrition and Bowles Center for Alcohol Studies, University of North Carolina at Chapel Hill – sequence: 6 givenname: Joel P. surname: Gue fullname: Gue, Joel P. organization: Division of Gastroenterology, Hepatology and Nutrition, Pittsburgh Liver Research Center, University of Pittsburgh Medical Center (UPMC) – sequence: 7 givenname: Joaquin orcidid: 0000-0003-0012-484X surname: Cabezas fullname: Cabezas, Joaquin organization: Division of Gastroenterology and Hepatology, Departments of Medicine and Nutrition and Bowles Center for Alcohol Studies, University of North Carolina at Chapel Hill, Departament of Hepatology, Marqués de Valdecilla University Hospital – sequence: 8 givenname: Juan J. surname: Lozano fullname: Lozano, Juan J. organization: Centro de Investigacion Biomedica en Red, Enfermedades Hepáticas y Digestivas (CIBERehd), Institut d’Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS) – sequence: 9 givenname: Derek surname: Van Booven fullname: Van Booven, Derek organization: John P. Hussman Institute of Human Genomics. Miller School of Medicine, University of Miami – sequence: 10 givenname: Aaron orcidid: 0000-0001-6648-0834 surname: Bell fullname: Bell, Aaron organization: Departments of Pathology and Medicine, Pittsburgh Liver Research Center, University of Pittsburgh School of Medicine – sequence: 11 givenname: Sheng surname: Cao fullname: Cao, Sheng organization: Division of Gastroenterology and Hepatology, Mayo Clinic – sequence: 12 givenname: Lawrence A. surname: Vernetti fullname: Vernetti, Lawrence A. organization: University of Pittsburgh Drug Discovery Institute, Department of Computational & Systems Biology, University of Pittsburgh – sequence: 13 givenname: Juan P. orcidid: 0000-0002-8561-396X surname: Arab fullname: Arab, Juan P. organization: Division of Gastroenterology and Hepatology, Mayo Clinic, Departamento de Gastroenterologia, Escuela de Medicina, Pontificia Universidad Catolica de Chile – sequence: 14 givenname: Meritxell orcidid: 0000-0001-9513-2855 surname: Ventura-Cots fullname: Ventura-Cots, Meritxell organization: Division of Gastroenterology, Hepatology and Nutrition, Pittsburgh Liver Research Center, University of Pittsburgh Medical Center (UPMC) – sequence: 15 givenname: Lia R. surname: Edmunds fullname: Edmunds, Lia R. organization: Department of Medicine, Division of Endocrinology and Metabolism, Center for Metabolic and Mitochondrial Medicine, University of Pittsburgh – sequence: 16 givenname: Constantino surname: Fondevila fullname: Fondevila, Constantino organization: Liver Transplant Unit, Department of Surgery, Hospital Clinic, University of Barcelona – sequence: 17 givenname: Peter orcidid: 0000-0003-2938-4442 surname: Stärkel fullname: Stärkel, Peter organization: Service d’Hépato-gastroentérologie, Cliniques Universitaires Saint-Luc and Laboratory of Hepatogastroenterology, Institut de Recherche Expérimentale et Clinique, Université Catholique de Louvain – sequence: 18 givenname: Laurent orcidid: 0000-0003-3596-5497 surname: Dubuquoy fullname: Dubuquoy, Laurent organization: Service des Maladies de l’appareil digestif, CHU Lille. 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Lansing organization: University of Pittsburgh Drug Discovery Institute, Department of Computational & Systems Biology, University of Pittsburgh – sequence: 27 givenname: Carmen orcidid: 0000-0001-7075-2476 surname: Berasain fullname: Berasain, Carmen organization: Hepatology Program, Center for Applied Medical Research (CIMA), University of Navarra, Centro de Investigacion Biomedica en Red, Enfermedades Hepáticas y Digestivas (CIBERehd) – sequence: 28 givenname: Claes orcidid: 0000-0003-4471-5916 surname: Wahlestedt fullname: Wahlestedt, Claes organization: Center for Therapeutic Innovation and Department of Psychiatry and Behavioral Sciences, University of Miami Miller School of Medicine – sequence: 29 givenname: Satdarshan P. orcidid: 0000-0002-8437-3378 surname: Monga fullname: Monga, Satdarshan P. organization: Departments of Pathology and Medicine, Pittsburgh Liver Research Center, University of Pittsburgh School of Medicine – sequence: 30 givenname: Marsha Y. surname: Morgan fullname: Morgan, Marsha Y. organization: UCL Institute for Liver and Digestive Health, Division of Medicine, Royal Free Campus, University College London – sequence: 31 givenname: Pau orcidid: 0000-0001-5569-9259 surname: Sancho-Bru fullname: Sancho-Bru, Pau organization: Centro de Investigacion Biomedica en Red, Enfermedades Hepáticas y Digestivas (CIBERehd), Institut d’Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS) – sequence: 32 givenname: Philippe surname: Mathurin fullname: Mathurin, Philippe organization: Service des Maladies de l’appareil digestif, CHU Lille. 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BackLink	https://www.ncbi.nlm.nih.gov/pubmed/31311938$$D View this record in MEDLINE/PubMed https://hal.univ-lille.fr/hal-03113100$$DView record in HAL
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Keywords	Transforming Growth Factor beta1 RNA Humans Liver Middle Aged Gene Expression Regulation Chromatin Assembly and Disassembly Genetic Male Gene Expression Profiling Disease Progression Hepatitis DNA Methylation Animals Hepatocytes Biopsy Alcoholic Adult Female Aged Epigenesis Hepatocyte Nuclear Factor 4 Sequence Analysis Polymorphism
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Snippet	Alcoholic hepatitis (AH) is a life-threatening condition characterized by profound hepatocellular dysfunction for which targeted treatments are urgently... Alcoholic hepatitis, a common cause of liver failure, lacks effective treatment. Here, the authors show altered hepatic HNF4a isoform expression and...
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SubjectTerms	13/1 13/109 13/51 13/89 14 38/15 38/91 45/61 631/114/2114 692/4020/4021/1607/1608 692/4020/4021/288/2032 Adult Aged Alcoholic beverages Animal models Animals Biopsy Chromatin Assembly and Disassembly Chromatin remodeling Deoxyribonucleic acid Disease Progression DNA DNA Methylation Epigenesis, Genetic Epigenetics Female Gene expression Gene Expression Profiling Gene Expression Regulation Gene polymorphism Gene sequencing Hepatitis Hepatitis, Alcoholic - genetics Hepatitis, Alcoholic - pathology Hepatocyte nuclear factor 4 Hepatocyte Nuclear Factor 4 - genetics Hepatocyte Nuclear Factor 4 - metabolism Hepatocytes Hepatocytes - pathology Humanities and Social Sciences Humans Life Sciences Liver Liver - cytology Liver - pathology Liver diseases Male Middle Aged multidisciplinary Phenotypes Polymorphism, Genetic Ribonucleic acid RNA Science Sequence Analysis, RNA Transcription factors Transcriptomes Transforming Growth Factor beta1 - genetics Transforming Growth Factor beta1 - metabolism Transforming growth factor-b1
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Title	Defective HNF4alpha-dependent gene expression as a driver of hepatocellular failure in alcoholic hepatitis
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