FXR-dependent Rubicon induction impairs autophagy in models of human cholestasis

Katrin Panzitt; Emilian Jungwirth; Elisabeth Krones; Jae Man Lee; Marion Pollheimer; Gerhard G Thallinger; Dagmar Kolb-Lenz; Rui Xiao; Anders Thorell; Michael Trauner; Peter Fickert; Hanns-Ulrich Marschall; David D Moore; Martin Wagner

doi:10.1016/j.jhep.2020.01.014

FXR-dependent Rubicon induction impairs autophagy in models of human cholestasis

J Hepatol. 2020 Jun;72(6):1122-1131. doi: 10.1016/j.jhep.2020.01.014. Epub 2020 Jan 28.

Authors

Affiliations

¹ Division of Gastroenterology and Hepatology, Medical University Graz, Graz, Austria; Research Unit for Translational Nuclear Receptor Research, Medical University Graz, Graz, Austria.
² Division of Gastroenterology and Hepatology, Medical University Graz, Graz, Austria; Research Unit for Translational Nuclear Receptor Research, Medical University Graz, Graz, Austria; Omics Center Graz, BioTechMed Graz, Austria; Institute of Computational Biotechnology, University of Technology, Graz, Austria.
³ Division of Gastroenterology and Hepatology, Medical University Graz, Graz, Austria.
⁴ Department of Biochemistry and Cell Biology, Cell and Matrix Research Institute, BK21 Plus KNU Biomedical Convergence Program, Department of Biomedical Science, School of Medicine, Kyungpook National University, Daegu, South Korea.
⁵ Institute of Pathology, Medical University Graz, Graz, Austria.
⁶ Omics Center Graz, BioTechMed Graz, Austria; Institute of Computational Biotechnology, University of Technology, Graz, Austria.
⁷ Center for Medical Research Medical University Graz and Division of Cell Biology, Histology and Embryology, Gottfried Schatz Research Center for Cell Signaling, Metabolism and Aging, Medical University of Graz, Austria.
⁸ Molecular and Human Genetics, Baylor College of Medicine, Houston, TX, USA.
⁹ Karolinska Institutet, Department of Clinical Science, Danderyd Hospital and Department of Surgery, Ersta Hospital, Stockholm, Sweden.
¹⁰ Division of Gastroenterology and Hepatology, Department of Medicine III, Medical University of Vienna, Vienna, Austria.
¹¹ Department of Molecular and Clinical Medicine, University of Gothenburg and Sahlgrenska University Hospital, Gothenburg, Sweden.
¹² Department of Molecular and Cellular Biology, Baylor College of Medicine, Houston, TX, USA.
¹³ Division of Gastroenterology and Hepatology, Medical University Graz, Graz, Austria; Research Unit for Translational Nuclear Receptor Research, Medical University Graz, Graz, Austria; Omics Center Graz, BioTechMed Graz, Austria. Electronic address: martin.wagner@medunigraz.at.

PMID: 32001325
DOI: 10.1016/j.jhep.2020.01.014

Abstract

Background & aims: Cholestasis comprises a spectrum of liver diseases characterized by the accumulation of bile acids. Bile acids and activation of the farnesoid X receptor (FXR) can inhibit autophagy, a cellular self-digestion process necessary for cellular homeostasis and regeneration. In mice, autophagy appears to be impaired in cholestasis and induction of autophagy may reduce liver injury.

Methods: Herein, we explored autophagy in human cholestasis in vivo and investigated the underlying molecular mechanisms in vitro. FXR chromatin immunoprecipitation-sequencing and qPCR were performed in combination with luciferase promoter studies to identify functional FXR binding targets in a human cholestatic liver sample.

Results: Autophagic processing appeared to be impaired in patients with cholestasis and in individuals treated with the FXR ligand obeticholic acid (OCA). In vitro, chenodeoxycholic acid and OCA inhibited autophagy at the level of autophagosome to lysosome fusion in an FXR-dependent manner. Rubicon, which inhibits autophago-lysosomal maturation, was identified as a direct FXR target that is induced in cholestasis and by FXR-agonistic bile acids. Genetic inhibition of Rubicon reversed the bile acid-induced impairment of autophagic flux. In contrast to OCA, ursodeoxycholic acid (UDCA), which is a non-FXR-agonistic bile acid, induced autophagolysosome formation independently of FXR, enhanced autophagic flux and was associated with reduced Rubicon levels.

Conclusion: In models of human cholestasis, autophagic processing is impaired in an FXR-dependent manner, partly resulting from the induction of Rubicon. UDCA is a potent inducer of hepatic autophagy. Manipulating autophagy and Rubicon may represent a novel treatment concept for cholestatic liver diseases.

Lay summary: Autophagy, a cellular self-cleansing process, is impaired in various forms of human cholestasis. Bile acids, which accumulate in cholestatic liver disease, induce Rubicon, a protein that inhibits proper execution of autophagy. Ursodeoxycholic acid, which is the first-line treatment option for many cholestatic liver diseases, induces hepatic autophagy along with reducing Rubicon.

Keywords: Bile acids; Nuclear receptors; Obeticholic acid; Ursodeoxycholic acid; Vesicle trafficking.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Autophagosomes / metabolism
Autophagy / drug effects
Autophagy / genetics*
Autophagy-Related Proteins / genetics
Autophagy-Related Proteins / metabolism*
Chenodeoxycholic Acid / analogs & derivatives
Chenodeoxycholic Acid / metabolism
Chenodeoxycholic Acid / pharmacology
Chenodeoxycholic Acid / therapeutic use
Cholestasis / drug therapy
Cholestasis / metabolism*
Cytotoxins
Gene Knockdown Techniques
Hep G2 Cells
Humans
Liver / metabolism
Liver / pathology
Lysosomes / metabolism
Receptors, Cytoplasmic and Nuclear / agonists
Receptors, Cytoplasmic and Nuclear / antagonists & inhibitors
Receptors, Cytoplasmic and Nuclear / genetics
Receptors, Cytoplasmic and Nuclear / metabolism*
Retrospective Studies
Signal Transduction / genetics*
Transfection
Ursodeoxycholic Acid / metabolism
Ursodeoxycholic Acid / pharmacology

Substances

Autophagy-Related Proteins
Cytotoxins
RUBCN protein, human
Receptors, Cytoplasmic and Nuclear
obeticholic acid
farnesoid X-activated receptor
Chenodeoxycholic Acid
Ursodeoxycholic Acid

Grants and funding

P 30482/FWF_/Austrian Science Fund FWF/Austria