Your search keyword '"Manon Buist-Homan"' showing total 22 results

1. Scopoletin and umbelliferone protect hepatocytes against palmitate- and bile acid-induced cell death by reducing endoplasmic reticulum stress and oxidative stress

Author

Zongmei Wu, Yana Geng, Manon Buist-Homan, Han Moshage, Pharmaceutical Technology and Biopharmacy, Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, Cell death, Palmitates, Apoptosis, Toxicology, Antioxidants, TOXICITY, Bile Acids and Salts, Umbelliferone, ACTIVATION, PATHWAY, Necrosis, RELEVANCE, Glycochenodeoxycholic Acid, INFLAMMATION, Non-alcoholic Fatty Liver Disease, Cell Line, Tumor, NAFLD, Animals, Humans, Umbelliferones, Rats, Wistar, INDUCED APOPTOSIS, Pharmacology, Scopoletin, FATTY LIVER, Hep G2 Cells, Endoplasmic Reticulum Stress, Rats, ALPHA, Oxidative Stress, HEPATIC LIPID-ACCUMULATION, Hepatocytes, SURVIVAL, Reactive Oxygen Species, ER stress, Lipotoxicity, Signal Transduction

Abstract

BACKGROUND: The number of patients with non-alcoholic fatty liver disease (NAFLD) is rapidly increasing due to the growing epidemic of obesity. Non-alcoholic steatohepatitis (NASH), the inflammatory stage of NAFLD, is characterized by lipid accumulation in hepatocytes, chronic inflammation and hepatocyte cell death. Scopoletin and umbelliferone are coumarin-like molecules and have antioxidant, anti-cancer and anti-inflammatory effects. Cytoprotective effects of these compounds have not been described in hepatocytes and the mechanisms of the beneficial effects of scopoletin and umbelliferone are unknown.AIM: To investigate whether scopoletin and/or umbelliferone protect hepatocytes against palmitate-induced cell death. For comparison, we also tested the cytoprotective effect of scopoletin and umbelliferone against bile acid-induced cell death.METHODS: Primary rat hepatocytes were exposed to palmitate (1 mmol/L) or the hydrophobic bile acid glycochenodeoxycholic acid (GCDCA; 50 μmol/L). Apoptosis was assessed by caspase-3 activity assay, necrosis by Sytox green assay, mRNA levels by qPCR, protein levels by Western blot and production of reactive oxygen species (ROS) by fluorescence assay.RESULTS: Both scopoletin and umbelliferone protected against palmitate and GCDCA-induced cell death. Both palmitate and GCDCA induced the expression of ER stress markers. Scopoletin and umbelliferone decreased palmitate- and GCDCA-induced expression of ER stress markers, phosphorylation of the cell death signaling intermediate JNK as well as ROS production.CONCLUSION: Scopoletin and umbelliferone protect against palmitate and bile acid-induced cell death of hepatocytes by inhibition of ER stress and ROS generation and decreasing phosphorylation of JNK. Scopoletin and umbelliferone may hold promise as a therapeutic modality for the treatment of NAFLD.

Published

2022

2. Hydrogen sulfide stimulates activation of hepatic stellate cells through increased cellular bio-energetics

Author

Mengfan Zhang, Harry van Goor, Manon Buist-Homan, Klaas Nico Faber, Turtushikh Damba, Han Moshage, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Center for Liver, Digestive and Metabolic Diseases (CLDM), Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Restoring Organ Function by Means of Regenerative Medicine (REGENERATE), and Lifestyle Medicine (LM)

Subjects

Male, EXPRESSION, 0301 basic medicine, Cystathionine gamma-lyase, Cancer Research, LIVER, Physiology, Clinical Biochemistry, INHIBITION, CSE, Inflammation, Endogeny, 030204 cardiovascular system & hematology, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Hepatic stellate cells, Fibrosis, HSCs, medicine, Animals, FIBROSIS, Rats, Wistar, OXIDATIVE STRESS, GASOTRANSMITTERS, Cells, Cultured, Cell Proliferation, Hydrogen sulfide, biology, H2S, Chemistry, PROLIFERATION, CTH, MITOCHONDRIAL BIOENERGETIC FUNCTION, equipment and supplies, medicine.disease, Hepatic stellate cell activation, Cystathionine beta synthase, Rats, Cell biology, 030104 developmental biology, biology.protein, Hepatic stellate cell, RAT, medicine.symptom, Hepatic fibrosis

Abstract

Hepatic fibrosis is caused by chronic inflammation and characterized as the excessive accumulation of extra cellular matrix (ECM) by activated hepatic stellate cells (HSCs). Gasotransmitters like NO and CO are known to modulate inflammation and fibrosis, however, little is known about the role of the gasotransmitter hydrogen sulfide (H2S) in liver fibrogenesis and stellate cell activation. Endogenous H2S is produced by the enzymes cystathionine beta-synthase (CBS), cystathionine gamma-lyase (CTH) and 3-mercaptopyruvate sulfur transferase (MPST) [1]. The aim of this study was to elucidate the role of endogenously produced and/or exogenously administered H2S on rat hepatic stellate cell activation and fibrogenesis. Primary rat HSCs were culture-activated for 7 days and treated with different H2S releasing donors (slow releasing donor GYY4137, fast releasing donor NaHS) or inhibitors of the H2S producing enzymes CTH and CBS (DL-PAG, AOAA). The main message of our study is that mRNA and protein expression level of H2S synthesizing enzymes are low in HSCs compared to hepatocytes and Kupffer cells. However, H2S promotes hepatic stellate cell activation. This conclusion is based on the fact that production of H2S and mRNA and protein expression of its producing enzyme CTH are increased during hepatic stellate cell activation. Furthermore, exogenous H2S increased HSC proliferation while inhibitors of endogenous H2S production reduce proliferation and fibrotic makers of HSCs. The effect of H2S on stellate cell activation correlated with increased cellular bioenergetics. Our results indicate that the H2S generation in hepatic stellate cells is a target for anti-fibrotic intervention and that systemic interventions with H2S should take into account cell-specific effects of H2S.

Published

2019

3. Elevated cAMP Protects against Diclofenac-Induced Toxicity in Primary Rat Hepatocytes: A Protective Effect Mediated by the Exchange Protein Directly Activated by cAMP/cAMP-Regulated Guanine Nucleotide Exchange Factors

Author

Manon Buist-Homan, Martina Schmidt, Xiaodong Cheng, Nshunge Musheshe, Han Moshage, Asmaa Oun, Frank Lezoualc'h, Fabio Alejandro Aguilar Mora, Molecular Pharmacology, Groningen Research Institute for Asthma and COPD (GRIAC), Restoring Organ Function by Means of Regenerative Medicine (REGENERATE), and Center for Liver, Digestive and Metabolic Diseases (CLDM)

Subjects

0301 basic medicine, Male, EXPRESSION, Programmed cell death, IBMX, Diclofenac, INHIBITION, Pharmacology, Mitochondrion, MECHANISMS, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Cyclic AMP, MITOCHONDRIAL TOXICITY, KINASE, Animals, Guanine Nucleotide Exchange Factors, Humans, CELL, Rats, Wistar, Protein kinase A, Liver injury, Forskolin, INDUCED LIVER-INJURY, EPAC, Anti-Inflammatory Agents, Non-Steroidal, medicine.disease, Rats, APOPTOSIS, 030104 developmental biology, HEK293 Cells, chemistry, Apoptosis, Hepatocytes, Molecular Medicine, Signal transduction, 030217 neurology & neurosurgery

Abstract

Chronic consumption of the nonsteroidal anti-inflammatory drug diclofenac may induce drug-induced liver injury (DILI). The mechanism of diclofenac-induced liver injury is partially elucidated and involves mitochondrial damage. Elevated cAMP protects hepatocytes against bile acid-induced injury. However, it is unknown whether cAMP protects against DILI and, if so, which downstream targets of cAMP are implicated in the protective mechanism, including the classic protein kinase A (PKA) pathway or alternative pathways like the exchange protein directly activated by cAMP (EPAC). The aim of this study was to investigate whether cAMP and/or its downstream targets protect against diclofenac-induced injury in hepatocytes. Rat hepatocytes were exposed to 400 µmol/l diclofenac. Apoptosis and necrosis were measured by caspase-3 activity assay and Sytox green staining, respectively. Mitochondrial membrane potential (MMP) was measured by JC-10 staining. mRNA and protein expression were assessed by quantitative polymerase chain reaction (qPCR) and Western blot, respectively. The cAMP-elevating agent 7β-acetoxy-8,13-epoxy-1α,6β,9α-trihydroxylabd-14-en-11-one (forskolin), the pan-phosphodiesterase inhibitor IBMX, and EPAC inhibitors 5,7-dibromo-6-fluoro-3,4-dihydro-2-methyl-1(2H)-quinoline carboxaldehyde (CE3F4) and ESI-O5 were used to assess the role of cAMP and its effectors, PKA or EPAC. Diclofenac exposure induced apoptotic cell death and loss of MMP in hepatocytes. Both forskolin and IBMX prevented diclofenac-induced apoptosis. EPAC inhibition but not PKA inhibition abolished the protective effect of forskolin and IBMX. Forskolin and IBMX preserved the MMP, whereas both EPAC inhibitors diminished this effect. Both EPAC1 and EPAC2 were expressed in hepatocytes and localized in mitochondria. cAMP elevation protects hepatocytes against diclofenac-induced cell death, a process primarily involving EPACs. The cAMP/EPAC pathway may be a novel target for treatment of DILI. SIGNIFICANCE STATEMENT: This study shows two main highlights. First, elevated cAMP levels protect against diclofenac-induced apoptosis in primary hepatocytes via maintenance of mitochondrial integrity. In addition, this study proposes the existence of mitochondrial cAMP-EPAC microdomains in rat hepatocytes, opening new avenues for targeted therapy in drug-induced liver injury (DILI). Both EPAC1 and EPAC2, but not protein kinase A, are responsible for this protective effect. Our findings present cAMP-EPAC as a potential target for the treatment of DILI and liver injury involving mitochondrial dysfunction.

Published

2021

4. Hesperetin protects against palmitate-induced cellular toxicity via induction of GRP78 in hepatocytes

Author

Hans Blokzijl, Han Moshage, Yana Geng, Zongmei Wu, Manon Buist-Homan, Pharmaceutical Technology and Biopharmacy, Restoring Organ Function by Means of Regenerative Medicine (REGENERATE), and Center for Liver, Digestive and Metabolic Diseases (CLDM)

Subjects

0301 basic medicine, GRP78, Male, Programmed cell death, Palmitates, Caspase 3, LIPOTOXICITY, Toxicology, Unfolded protein response, ACTIVATION, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, ENDOPLASMIC-RETICULUM STRESS, medicine, Hesperetin, INJURY, Animals, Hepatocyte, Gene Silencing, RNA, Small Interfering, Rats, Wistar, Cells, Cultured, Heat-Shock Proteins, Pharmacology, Dose-Response Relationship, Drug, Chemistry, Endoplasmic reticulum, SATURATED FATTY-ACIDS, Hesperidin, DEATH, HEPG2 CELLS, Molecular biology, Rats, 030104 developmental biology, medicine.anatomical_structure, Lipotoxicity, Gene Expression Regulation, 030220 oncology & carcinogenesis, OBESITY, Hepatic stellate cell, Hepatocytes, Non-alcoholic fatty liver disease, RESPONSES, Signal Transduction

Abstract

Lipotoxicity plays a critical role in the pathogenesis of non-alcoholic fatty liver disease (NAFLD). Hesperetin, a flavonoid derivative, has anti-oxidant, anti-inflammatory and cytoprotective properties. In the present study, we aim to examine whether hesperetin protects against palmitate-induced lipotoxic cell death and to investigate the underlying mechanisms in hepatocytes. Primary rat hepatocytes and HepG2 cells were pretreated with hesperetin for 30 min and then exposed to palmitate (1.0 mmol/L in primary rat hepatocytes; 0.5 mmol/L in HepG2 cells) in the presence or absence of hesperetin. Necrotic cell death was measured via Sytox green nuclei staining and quantified by LDH release assay. Apoptotic cell death was determined by caspase 3/7 activity and the protein level of cleaved-PARP. The unfolded protein response (UPR) was assessed by measuring the expression of GRP78, sXBP1, ATF4 and CHOP. Results show that hesperetin (50 μmol/L and 100 μmol/L) protected against palmitate-induced cell death and inhibited palmitate-induced endoplasmic reticulum (ER) stress in both primary rat hepatocytes and HepG2 cells. Hesperetin (100 μmol/L) significantly activated sXBP1/GRP78 signaling, whereas a high concentration of hesperetin (200 μmol/L) activated p-eIF2α and caused hepatic cell death. Importantly, GRP78 knockdown via siRNA abolished the protective effects of hesperetin in HepG2 cells. In conclusion, hesperetin protected against palmitate-induced hepatic cell death via activation of the sXBP1/GRP78 signaling pathway, thus inhibiting palmitate-induced ER stress. Moreover, high concentrations of hesperetin induce ER stress and subsequently cause cell death in hepatocytes.

Published

2020

5. Protective effect of metformin against palmitate-induced hepatic cell death

Author

Alejandra Hernández Villanueva, Hans Blokzijl, Han Moshage, Klaas Nico Faber, Asmaa Oun, Amalia M. Dolga, Yana Geng, Manon Buist-Homan, Molecular Pharmacology, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), Groningen Research Institute for Asthma and COPD (GRIAC), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Programmed cell death, Necrosis, endocrine system diseases, Palmitates, Apoptosis, Protective Agents, 03 medical and health sciences, 0302 clinical medicine, Non-alcoholic Fatty Liver Disease, Cell Line, Tumor, Internal medicine, medicine, Animals, Humans, Rats, Wistar, Molecular Biology, Cell Death, Superoxide Dismutase, business.industry, Fatty liver, nutritional and metabolic diseases, Hep G2 Cells, Lipid Metabolism, medicine.disease, Metformin, digestive system diseases, Mitochondria, Rats, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Liver, Lipotoxicity, 030220 oncology & carcinogenesis, Hepatocyte, Hepatocytes, Hepatic stellate cell, Molecular Medicine, medicine.symptom, Reactive Oxygen Species, business, Signal Transduction, medicine.drug

Abstract

Lipotoxicity causes hepatic cell death and therefore plays an important role in the pathogenesis of non-alcoholic fatty liver disease (NAFLD). Metformin, a first-line anti-diabetic drug, has shown a potential protective effect against NAFLD. However, the underlying mechanism is still not clear. In this study, we aim to understand the molecular mechanism of the protective effect of metformin in NAFLD, focusing on lipotoxicity. Cell death was studied in HepG2 cells and primary rat hepatocytes exposed to palmitate and metformin. Metformin ameliorated palmitate-induced necrosis and apoptosis (decreased caspase-3/7 activity by 52% and 57% respectively) in HepG2 cells. Metformin also reduced palmitate-induced necrosis in primary rat hepatocytes (P

Published

2020

6. α-1 Adrenergic receptor antagonist doxazosin reverses hepatic stellate cells activation via induction of senescence

Author

Sandra A. Serna-Salas, Johanna C. Arroyave-Ospina, Mengfan Zhang, Turtushikh Damba, Manon Buist-Homan, Martin H. Muñoz-Ortega, Javier Ventura-Juárez, Han Moshage, Restoring Organ Function by Means of Regenerative Medicine (REGENERATE), and Center for Liver, Digestive and Metabolic Diseases (CLDM)

Subjects

Liver Cirrhosis, Aging, Liver fibrosis, INHIBITION, SECRETORY PHENOTYPE, Senescence, Norepinephrine, Protein kinase C, Phospholipase C, Receptors, Adrenergic, alpha-1, a1-Adrenergic signaling, Hepatic Stellate Cells, Animals, FIBROSIS, Cells, Cultured, Cellular Senescence, Cell proliferation, Sulfonamides, Doxazosin, PROLIFERATION, Cell Cycle Checkpoints, Rats, Adrenergic alpha-1 Receptor Antagonists, Stellate cells, GROWTH, Senescence-Associated Secretory Phenotype, Adrenergic alpha-Agonists, Signal Transduction, Developmental Biology

Abstract

BACKGROUND: Activated hepatic stellate cells (aHSCs) are the main effector cells during liver fibrogenesis. α-1 adrenergic antagonist doxazosin (DX) was shown to be anti-fibrotic in an in vivo model of liver fibrosis (LF), but the mechanism remains to be elucidated. Recent studies suggest that reversion of LF can be achieved by inducing cellular senescence characterized by irreversible cell-cycle arrest and acquisition of the senescence-associated secretory phenotype (SASP).AIM: To elucidate the mechanism of the anti-fibrotic effect of DX and determine whether it induces senescence.METHODS: Primary culture-activated rat HSCs were used. mRNA and protein expression were measured by qPCR and Western blot, respectively. Cell proliferation was assessed by BrdU incorporation and xCelligence analysis. TGF-β was used for maximal HSC activation. Norepinephrine (NE), PMA and m-3M3FBS were used to activate alpha-1 adrenergic signaling.RESULTS: Expression of Col1α1 was significantly decreased by DX (10 µmol/L) at mRNA (-30 %) and protein level (-50 %) in TGF-β treated aHSCs. DX significantly reduced aHSCs proliferation and increased expression of senescence and SASP markers. PMA and m-3M3FBS reversed the effect of DX on senescence markers.CONCLUSION: Doxazosin reverses the fibrogenic phenotype of aHSCs and induces the senescence phenotype.

Published

2022

7. Hepatitis C virus core or NS3/4A protein expression preconditions hepatocytes against oxidative stress and endoplasmic reticulum stress

Author

W Alfredo Ríos-Ocampo, María Cristina Navas, Manon Buist-Homan, Toos Daemen, Klaas Nico Faber, Han Moshage, Microbes in Health and Disease (MHD), Targeted Gynaecologic Oncology (TARGON), Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

0301 basic medicine, Male, LIVER, Physiology, Clinical Biochemistry, Apoptosis, Hepacivirus, 030204 cardiovascular system & hematology, Viral Nonstructural Proteins, medicine.disease_cause, Biochemistry, ACTIVATION, chemistry.chemical_compound, 0302 clinical medicine, 4A, Superoxides, cellular stress, oxidative stress, lcsh:QH301-705.5, Endoplasmic Reticulum Chaperone BiP, INDUCED APOPTOSIS, GENE-EXPRESSION, chemistry.chemical_classification, nS3, Chemistry, Superoxide, Caspase 3, Hepatitis C virus, Vitamin K 3, unfolded protein response, RNA REPLICATION, Endoplasmic Reticulum Stress, Cell biology, HCV, DNA-REPAIR, AUTOPHAGY, Core, HEME OXYGENASE-1, ER stress, lcsh:RB1-214, Signal Transduction, Research Article, Blotting, Western, Oxidative phosphorylation, 03 medical and health sciences, Cell Line, Tumor, medicine, lcsh:Pathology, Animals, Humans, Rats, Wistar, Reactive oxygen species, nS3/4A, 030102 biochemistry & molecular biology, RAT HEPATOCYTES, Endoplasmic reticulum, Biochemistry (medical), Autophagy, Cell Biology, Transient expression, Rats, lcsh:Biology (General), Microscopy, Fluorescence, Unfolded protein response, Hepatocytes, Reactive Oxygen Species, Oxidative stress

Abstract

Objectives: The occurrence of oxidative stress and endoplasmic reticulum (ER) stress in hepatitis C virus (HCV) infection has been demonstrated and play an important role in liver injury. During viral infection, hepatocytes must handle not only the replication of the virus, but also inflammatory signals generating oxidative stress and damage. Although several mechanisms exist to overcome cellular stress, little attention has been given to the adaptive response of hepatocytes during exposure to multiple noxious triggers. Methods: In the present study, Huh-7 cells and hepatocytes expressing HCV Core or NS3/4A proteins, both inducers of oxidative and ER stress, were additionally challenged with the superoxide anion generator menadione to mimic external oxidative stress. The production of reactive oxygen species (ROS) as well as the response to oxidative stress and ER stress were investigated. Results: We demonstrate that hepatocytes diminish oxidative stress through a reduction in ROS production, ER-stress markers (HSPA5 [GRP78], sXBP1) and apoptosis (caspase-3 activity) despite external oxidative stress. Interestingly, the level of the autophagy substrate protein p62 was downregulated together with HCV Core degradation, suggesting that hepatocytes can overcome excess oxidative stress through autophagic degradation of one of the stressors, thereby increasing cell survival. Duscussion: In conclusion, hepatocytes exposed to direct and indirect oxidative stress inducers are able to cope with cellular stress associated with viral hepatitis and thus promote cell survival.

Published

2019

8. Sphingosine kinase-1 inhibition protects primary rat hepatocytes against bile salt-induced apoptosis

Author

Klaas Nico Faber, Golnar Karimian, Jan Freark de Boer, Karin Klappe, Martina Schmidt, Han Moshage, Uwe J. F. Tietge, Laurent Combettes, Thierry Tordjmann, Jan Willem Kok, Manon Buist-Homan, Faculteit Medische Wetenschappen/UMCG, Molecular Pharmacology, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), Lifestyle Medicine (LM), Groningen Research Institute for Asthma and COPD (GRIAC), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, Sphingosine kinase, Apoptosis, 1-PHOSPHATE, ACTIVATION, chemistry.chemical_compound, Sphingosine-1 phosphate receptor, Sphingosine, Cells, Cultured, Caspase 3, Reverse Transcriptase Polymerase Chain Reaction, HUMAN HEPATIC MYOFIBROBLASTS, Sphingosine-1 phosphate, Cholestatic liver disease, GAP-JUNCTION PERMEABILITY, Cell biology, Phosphotransferases (Alcohol Group Acceptor), Receptors, Lysosphingolipid, Sphingosine kinase 1, SURVIVAL, Molecular Medicine, Signal transduction, Signal Transduction, Programmed cell death, Blotting, Western, Detergents, ENDOPLASMIC-RETICULUM, Biology, Real-Time Polymerase Chain Reaction, ACID-INDUCED APOPTOSIS, CALCIUM, Bile Acids and Salts, Calcium oscillation, Gastrointestinal Agents, Glycochenodeoxycholic acid, Animals, RNA, Messenger, Sphingosine-1-phosphate, Rats, Wistar, TANDEM MASS-SPECTROMETRY, Molecular Biology, SPHINGOSINE-1-PHOSPHATE, Rats, Thiazoles, chemistry, Hepatocytes, biology.protein, Lysophospholipids

Abstract

Sphingosine kinases (SphKs) and their product sphingosine-1-phosphate (S1P) have been reported to regulate apoptosis and survival of liver cells. Cholestatic liver diseases are characterized by cytotoxic levels of bile salts inducing liver injury. It is unknown whether SphKs and/or S1P play a role in this pathogenic process. Here, we investigated the putative involvement of SphK1 and S1P in bile salt-induced cell death in hepatocytes. Primary rat hepatocytes were exposed to glycochenodeoxycholic acid (GCDCA) to induce apoptosis. GCDCA-exposed hepatocytes were co-treated with S1P, the SphK1 inhibitor Ski-II and/or specific antagonists of S1P receptors (S1PR1 and S1PR2). Apoptosis and necrosis were quantified. Ski-II significantly reduced GCDCA-induced apoptosis in hepatocytes (−70%, P

Published

2013

9. Hepatoprotective Effect of Opuntia robusta and Opuntia streptacantha Fruits against Acetaminophen-Induced Acute Liver Damage

Author

María Consolación Martínez-Saldaña, Ana Rosa Rincón-Sánchez, Herson Antonio González-Ponce, Klaas Nico Faber, María Teresa Sumaya-Martínez, Han Moshage, Fernando Jaramillo-Juárez, Manon Buist-Homan, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), Lifestyle Medicine (LM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

0301 basic medicine, Male, Necrosis, Antioxidant, medicine.medical_treatment, hepatoprotective, medicine.disease_cause, chemistry.chemical_compound, OXIDATIVE STRESS, IN-VIVO, acetaminophen, Nutrition and Dietetics, Traditional medicine, Glycogen, digestive, oral, and skin physiology, Opuntia, Analgesics, Non-Narcotic, CACTUS-PEAR, medicine.anatomical_structure, antioxidants, Biochemistry, Liver, Hepatocyte, nutraceutical, medicine.symptom, Chemical and Drug Induced Liver Injury, lcsh:Nutrition. Foods and food supply, medicine.drug, FICUS-INDICA, lcsh:TX341-641, Biology, Article, 03 medical and health sciences, Nutraceutical, NATURAL-PRODUCTS, medicine, Animals, Rats, Wistar, DIETARY FLAVONOIDS, Opuntia fruits, RAT HEPATOCYTES, Plant Extracts, acute liver failure, ANTIOXIDANT PROPERTIES, Glutathione, PRICKLY PEAR JUICE, Acetaminophen, Rats, 030104 developmental biology, chemistry, CELL-DEATH, Dietary Supplements, Hepatocytes, Oxidative stress, Food Science, Phytotherapy

Abstract

Acetaminophen (APAP)-induced acute liver failure (ALF) is a serious health problem in developed countries. N-acetyl-L-cysteine (NAC), the current therapy for APAP-induced ALF, is not always effective, and liver transplantation is often needed. Opuntia spp. fruits are an important source of nutrients and contain high levels of bioactive compounds, including antioxidants. The aim of this study was to evaluate the hepatoprotective effect of Opuntia robusta and Opuntia streptacantha extracts against APAP-induced ALF. In addition, we analyzed the antioxidant activities of these extracts. Fruit extracts (800 mg/kg/day, orally) were given prophylactically to male Wistar rats before intoxication with APAP (500 mg/kg, intraperitoneally). Rat hepatocyte cultures were exposed to 20 mmol/L APAP, and necrosis was assessed by LDH leakage. Opuntia robusta had significantly higher levels of antioxidants than Opuntia streptacantha. Both extracts significantly attenuated APAP-induced injury markers AST, ALT and ALP and improved liver histology. The Opuntia extracts reversed APAP-induced depletion of liver GSH and glycogen stores. In cultured hepatocytes, Opuntia extracts significantly reduced leakage of LDH and cell necrosis, both prophylactically and therapeutically. Both extracts appeared to be superior to NAC when used therapeutically. We conclude that Opuntia extracts are hepatoprotective and can be used as a nutraceutical to prevent ALF.

Published

2016

10. Caveolin-1 Is Enriched in the Peroxisomal Membrane of Rat Hepatocytes

Author

Robert H. Henning, Fiona A.J. van den Heuvel, Manon Buist-Homan, Krzysztof P. Rembacz, Jannes Woudenberg, Carlos Enrich, Han Moshage, Titia E. Woudenberg-Vrenken, Mark Hoekstra, Leo E. Deelman, Klaas Nico Faber, M Geuken, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), Groningen Kidney Center (GKC), Vascular Ageing Programme (VAP), Restoring Organ Function by Means of Regenerative Medicine (REGENERATE), and Groningen Institute for Organ Transplantation (GIOT)

Subjects

Male, EXPRESSION, LIVER-REGENERATION, Caveolin 1, HEPATIC CELLS, Membrane transport and intracellular motility [NCMLS 5], Biology, Peroxins, Mice, Membrane Microdomains, Fenofibrate, Caveolae, Organelle, medicine, Peroxisomes, Animals, ACID N-ACYLTRANSFERASE, SINUSOIDAL CELLS, Molecular gastro-enterology and hepatology [IGMD 2], Rats, Wistar, Lipid raft, Renal disorder [IGMD 9], Mice, Knockout, Hepatology, MAMMALIAN PEROXISOMES, Peroxisomal matrix, Lipid microdomain, Membrane Proteins, PARTIAL-HEPATECTOMY, Lipid metabolism, IN-VITRO, Peroxisome, Cell biology, Rats, medicine.anatomical_structure, Biochemistry, Hepatocyte, LIPID BODIES, Hepatocytes, ATP-Binding Cassette Transporters, DOMINANT-NEGATIVE MUTANT, Acyltransferases, Subcellular Fractions

Abstract

Item does not contain fulltext Caveolae are a subtype of cholesterol-enriched lipid microdomains/rafts that are routinely detected as vesicles pinching off from the plasma membrane. Caveolin-1 is an essential component of caveolae. Hepatic caveolin-1 plays an important role in liver regeneration and lipid metabolism. Expression of caveolin-1 in hepatocytes is relatively low, and it has been suggested to also reside at other subcellular locations than the plasma membrane. Recently, we found that the peroxisomal membrane contains lipid microdomains. Like caveolin-1, hepatic peroxisomes are involved in lipid metabolism. Here, we analyzed the subcellular location of caveolin-1 in rat hepatocytes. The subcellular location of rat hepatocyte caveolin-1 was analyzed by cell fractionation procedures, immunofluorescence, and immuno-electron microscopy. Green fluorescent protein (GFP)-tagged caveolin-1 was expressed in rat hepatocytes. Lipid rafts were characterized after Triton X-100 or Lubrol WX extraction of purified peroxisomes. Fenofibric acid-dependent regulation of caveolin-1 was analyzed. Peroxisome biogenesis was studied in rat hepatocytes after RNA interference-mediated silencing of caveolin-1 and caveolin-1 knockout mice. Cell fractionation and microscopic analyses reveal that caveolin-1 colocalizes with peroxisomal marker proteins (catalase, the 70 kDa peroxisomal membrane protein PMP70, the adrenoleukodystrophy protein ALDP, Pex14p, and the bile acid-coenzyme A:amino acid N-acyltransferase BAAT) in rat hepatocytes. Artificially expressed GFP-caveolin-1 accumulated in catalase-positive organelles. Peroxisomal caveolin-1 is associated with detergent-resistant microdomains. Caveolin-1 expression is strongly repressed by the peroxisome proliferator-activated receptor-alpha agonist fenofibric acid. Targeting of peroxisomal matrix proteins and peroxisome number and shape were not altered in rat hepatocytes with 70%-80% reduced caveolin-1 levels and in livers of caveolin-1 knockout mice. CONCLUSION: Caveolin-1 is enriched in peroxisomes of hepatocytes. Caveolin-1 is not required for peroxisome biogenesis, but this unique subcellular location may determine its important role in hepatocyte proliferation and lipid metabolism. 01 mei 2010

Published

2010

11. Superoxide anions and hydrogen peroxide inhibit proliferation of activated rat stellate cells and induce different modes of cell death

Author

Jan Freark de Boer, Klaas Nico Faber, Sandra Dunning, Han Moshage, Rebekka A. Hannivoort, Manon Buist-Homan, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

MAP Kinase Kinase 4, RESISTANCE-ASSOCIATED PROTEINS, Apoptosis, medicine.disease_cause, p38 Mitogen-Activated Protein Kinases, HEPATOCYTES, chemistry.chemical_compound, Menadione, Superoxides, 4-NAPHTHOQUINONE, GLUTATHIONE, FIBROSIS, Organic Chemicals, OXIDATIVE STRESS, Hydrogen peroxide, INDUCED APOPTOSIS, chemistry.chemical_classification, reactive oxygen species, Reverse Transcriptase Polymerase Chain Reaction, Superoxide, HUMAN HEPATIC MYOFIBROBLASTS, Vitamin K 3, Cell biology, cell death, signal transduction, MENADIONE 2-METHYL-1, EXPRESSION, stellate cells, p38 mitogen-activated protein kinases, proliferation, Blotting, Western, Statistics, Nonparametric, MENADIONE 2-METHYL-1,4-NAPHTHOQUINONE, Hepatic Stellate Cells, medicine, Animals, ANTIFIBROGENIC PROTEIN, Cell Proliferation, DNA Primers, Reactive oxygen species, Hepatology, Hydrogen Peroxide, Glutathione, Molecular biology, Acridine Orange, Rats, Enzyme Activation, chemistry, Hepatic stellate cell, Oxidative stress

Abstract

In chronic liver injury, hepatic stellate cells (HSCs) proliferate and produce excessive amounts of connective tissue causing liver fibrosis and cirrhosis. Oxidative stress has been implicated as a driving force of HSC activation and proliferation, although contradictory results have been described.To determine the effects of oxidative stress on activated HSC proliferation, survival and signalling pathways.Serum-starved culture-activated rat HSCs were exposed to the superoxide anion donor menadione (5-25 mu mol/L) or hydrogen peroxide (0.2-5 mmol/L). Haem oxygenase-1 mRNA expression, glutathione status, cell death, phosphorylation of mitogen-activated protein (MAP) kinases and proliferation were investigated.Menadione induced apoptosis in a dose- and time-dependent, but caspase-independent manner. Hydrogen peroxide induced necrosis only at extremely high concentrations. Both menadione and hydrogen peroxide activated Jun N-terminal kinase (JNK) and p38. Hydrogen peroxide also activated extracellular signal-regulated protein. Menadione, but not hydrogen peroxide, reduced cellular glutathione levels. Inhibition of JNK or supplementation of glutathione reduced menadione-induced apoptosis. Non-toxic concentrations of menadione or hydrogen peroxide inhibited platelet-derived growth factor- or/and serum-induced proliferation.Reactive oxygen species (ROS) inhibit HSC proliferation and promote HSC cell death in vitro. Different ROS induce different modes of cell death. Superoxide anion-induced HSC apoptosis is dependent on JNK activation and glutathione status.

Published

2009

12. Carbon monoxide blocks oxidative stress-induced hepatocyte apoptosis via inhibition of the p54 JNK isoform

Author

Rebekka A. Hannivoort, Henk F. Kauffman, Han Moshage, Rick Havinga, Peter L. A. Jansen, Laura Conde de la Rosa, Klaas Nico Faber, Dirk-Jan Slebos, Manon Buist-Homan, TE Vrenken, Faculteit Medische Wetenschappen/UMCG, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), Groningen Research Institute for Asthma and COPD (GRIAC), Restoring Organ Function by Means of Regenerative Medicine (REGENERATE), Amsterdam Gastroenterology Endocrinology Metabolism, and Gastroenterology and Hepatology

Subjects

Programmed cell death, MAP Kinase Kinase 4, caspase, SIGNAL-TRANSDUCTION, medicine.disease_cause, PROTEIN-KINASE PATHWAY, Models, Biological, Biochemistry, ACID-INDUCED APOPTOSIS, Gene Expression Regulation, Enzymologic, carbon monoxide, necrosis, chemistry.chemical_compound, Metabolism, transport and motion [NCMLS 2], Superoxides, Physiology (medical), medicine, Animals, Protein Isoforms, oxidative stress, NITRIC-OXIDE SYNTHASE, Heme, REPERFUSION LUNG INJURY, MAP KINASES, Renal disorder [IGMD 9], Liver injury, biology, RAT HEPATOCYTES, Superoxide, Liver Diseases, NASH, apoptosis, heme oxygenase-1, medicine.disease, Molecular biology, MAPK, Rats, Nitric oxide synthase, Renal disorders [UMCN 5.4], chemistry, CELL-DEATH, Apoptosis, Caspases, Hepatocytes, biology.protein, INK, LIVER-INJURY, Signal transduction, Oxidative stress

Abstract

Most chronic liver diseases are accompanied by oxidative stress, which may induce apoptosis in hepatocytes and liver injury. Oxidative stress induces heme oxygenase-1 (HO-1) expression. This stress-responsive cytoprotective protein is responsible for heme degradation into carbon monoxide (CO), free iron, and biliverdin. CO is an important intracellular messenger; however, the exact mechanisms responsible for its cytoprotective effect are not yet elucidated. Thus, we investigated whether HO-1 and CO protect primary hepatocytes against oxidative-stress-induced apoptosis. In vivo, bile duct ligation was used as model of chronic liver disease. In vitro, primary hepatocytes were exposed to the superoxide anion donor menadione in a normal and in a CO- containing atmosphere. Apoptosis was determined by measuring caspase-9, -6, -3 activity and poly(ADP-ribose) polymerase cleavage, and necrosis was determined by Sytox green staining. The results showed that (1) HO-I is induced in chronic cholestatic liver disease, (2) superoxide anions time- and dose-dependently induce HO-1 activity, (3) HO-1 overexpression inhibits superoxide-anions-induced apoptosis, and (4) CO blocks superoxide-anions-induced JNK phosphorylation and caspase-9, -6, -3 activation and abolishes apoptosis but does not increase necrosis. We conclude that HO-I and CO protect primary hepatocytes against superoxide-anions-induced apoptosis partially via inhibition of JNK activity. CO could represent an important candidate for the treatment of liver diseases. (C) 2007 Elsevier Inc. All rights reserved.

Published

2008

13. The protective effect of the natural compound hesperetin against fulminant hepatitis in vivo and in vitro

Author

Xueting, Bai, Peixuan, Yang, Qiaoling, Zhou, Bozhi, Cai, Manon, Buist-Homan, He, Cheng, Jiyang, Jiang, Daifei, Shen, Lijun, Li, Xiajiong, Luo, Klaas Nico, Faber, Han, Moshage, and Ganggang, Shi

Subjects

Lipopolysaccharides, Male, Biological Products, Dose-Response Relationship, Drug, Hesperidin, Galactosamine, In Vitro Techniques, Liver Failure, Acute, Protective Agents, Research Papers, Rats, Concanavalin A, Animals, Rats, Wistar

Abstract

Liver diseases are mostly accompanied by inflammation and hepatocyte death. Therapeutic approaches targeting both hepatocyte injury and inflammation are not available. Natural compounds are considered as potential treatment for inflammatory liver diseases. Hesperetin, a flavonoid component of citrus fruits, has been reported to have anti-inflammatory properties. The aim of this study was to evaluate the cytoprotective and anti-inflammatory properties of hesperetin both in vitro and in models of fulminant hepatitis.Apoptotic cell death and inflammation were induced in primary cultures of rat hepatocytes by bile acids and cytokine mixture respectively. Apoptosis was quantified by caspase-3 activity and necrosis by LDH release. The concanavalin A (ConA) and D-galactosamine/LPS (D-GalN/LPS) were used as models of fulminant hepatitis. Liver injury was assessed by alanine aminotransferase (ALT) and aspartate aminotransferase (AST) levels, liver histology and TUNEL assay and inflammation by inducible NOS (iNOS) expression.Hesperetin blocked bile acid-induced apoptosis and cytokine-induced inflammation in rat hepatocytes. Moreover, hesperetin improved liver histology and protected against hepatocyte injury in ConA- and D-GalN/LPS-induced fulminant hepatitis, as assessed by TUNEL assay and serum AST and ALT levels. Hesperetin also reduced expression of the inflammatory marker iNOS and the expression and serum levels of TNFα and IFN-γ, the main mediators of cell toxicity in fulminant hepatitis.Hesperetin has anti-inflammatory and cytoprotective actions in models of acute liver toxicity. Hesperetin therefore has therapeutic potential for the treatment of inflammatory liver diseases accompanied by extensive hepatocyte injury, such as fulminant hepatitis.

Published

2016

14. Glutathione and antioxidant enzymes serve complementary roles in protecting activated hepatic stellate cells against hydrogen peroxide-induced cell death

Author

Floris W. Haijer, Marjolein H. Tiebosch, Sandra Dunning, Manon Buist-Homan, Fiona A.J. van den Heuvel, Rebekka A. Hannivoort, Han Moshage, Jannes Woudenberg, Atta ur Rehman, Klaas Nico Faber, Faculteit Medische Wetenschappen/UMCG, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, Antioxidant, medicine.medical_treatment, Fluorescent Antibody Technique, Apoptosis, MOUSE, Antioxidants, DEFICIENT MICE, chemistry.chemical_compound, Hydrogen peroxide, Cells, Cultured, chemistry.chemical_classification, biology, Reverse Transcriptase Polymerase Chain Reaction, Glutathione peroxidase, PROLIFERATION, Oxidants, Catalase, Glutathione, MANGANESE SUPEROXIDE-DISMUTASE, Molecular Medicine, LIVER-INJURY, Cell death, EXPRESSION, Blotting, Western, Superoxide dismutase, Real-Time Polymerase Chain Reaction, MECHANISMS, Necrosis, Hepatic Stellate Cells, medicine, Animals, ANTIFIBROGENIC PROTEIN, RNA, Messenger, Rats, Wistar, Molecular Biology, Cell Proliferation, Reactive oxygen species, Hydrogen Peroxide, Molecular biology, GAMMA-GLUTAMYLCYSTEINE SYNTHETASE, Rats, chemistry, Oxidative stress, biology.protein, Hepatic stellate cell

Abstract

Background: In chronic liver disease, hepatic stellate cells (HSCs) are activated, highly proliferative and produce excessive amounts of extracellular matrix, leading to liver fibrosis. Elevated levels of toxic reactive oxygen species (ROS) produced during chronic liver injury have been implicated in this activation process. Therefore, activated hepatic stellate cells need to harbor highly effective anti-oxidants to protect against the toxic effects of ROS.Aim: To investigate the protective mechanisms of activated HSCs against ROS-induced toxicity.Methods: Culture-activated rat HSCs were exposed to hydrogen peroxide. Necrosis and apoptosis were determined by Sytox Green or acridine orange staining, respectively. The hydrogen peroxide detoxifying enzymes catalase and glutathione-pefoxidase (GPx) were inhibited using 3-amino-1,2,4-triazole and mercaptosuccinic acid, respectively. The anti-oxidant glutathione was depleted by L-buthionine-sulfoximine and repleted with the GSH-analogue GSH-monoethylester (GSH-MEE).Results: Upon activation, HSCs increase their cellular glutathione content and GPx expression, while MnSOD (both at mRNA and protein level) and catalase (at the protein level, but not at the mRNA level) decreased. Hydrogen peroxide did not induce cell death in activated HSCs. Glutathione depletion increased the sensitivity of HSCs to hydrogen peroxide, resulting in 35% and 75% necrotic cells at 0.2 and 1 mmol/L hydrogen peroxide, respectively. The sensitizing effect was abolished by GSH-MEE. Inhibition of catalase or GPx significantly increased hydrogen peroxide-induced apoptosis, which was not reversed by GSH-MEE.Conclusion: Activated HSCs have increased ROS-detoxifying capacity compared to quiescent HSCs. Glutathione levels increase during HSC activation and protect against ROS-induced necrosis, whereas hydrogen peroxide-detoxifying enzymes protect against apoptotic cell death. (C) 2013 Elsevier B.V. All rights reserved.

Published

2013

15. Metformin Protects Rat Hepatocytes against Bile Acid-Induced Apoptosis

Author

Han Moshage, Laura Conde de la Rosa, Manon Buist-Homan, Titia E. Woudenberg-Vrenken, Klaas Nico Faber, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

AMPK, Male, endocrine system diseases, lcsh:Medicine, ComputingMilieux_LEGALASPECTSOFCOMPUTING, Nonalcoholic Steatohepatitis, Apoptosis, Pharmacology, AMP-Activated Protein Kinases, KAPPA-B ACTIVATION, chemistry.chemical_compound, Phosphatidylinositol 3-Kinases, AMP-activated protein kinase, Molecular Cell Biology, lcsh:Science, Multidisciplinary, biology, Cell Death, Chemistry, Caspase 3, MTOR, Liver Diseases, TOR Serine-Threonine Kinases, NF-kappa B, Animal Models, Metformin, Medicine, SIGNALING PATHWAY, medicine.drug, Research Article, Signal Transduction, medicine.medical_specialty, Programmed cell death, Drugs and Devices, Drug Research and Development, Acute Liver Failure, Phosphoinositide Signal Transduction, Gastroenterology and Hepatology, Signaling Pathways, Bile Acids and Salts, Necrosis, Model Organisms, Glycochenodeoxycholic Acid, Internal medicine, medicine, Glycochenodeoxycholic acid, DEATH RECEPTORS, Animals, Hypoglycemic Agents, Protein kinase B, Biology, PI3K/AKT/mTOR pathway, FATTY LIVER-DISEASE, Dose-Response Relationship, Drug, lcsh:R, Cell Membrane, nutritional and metabolic diseases, Rats, Endocrinology, MAMMALIAN TARGET, CELLS, biology.protein, KINASE ACTIVATION, Hepatocytes, Rat, lcsh:Q, Liver function, Proto-Oncogene Proteins c-akt

Abstract

This is an open-access article distributed under the terms of the Creative Commons Attribution License., [Background]: Metformin is used in the treatment of Diabetes Mellitus type II and improves liver function in patients with non-alcoholic fatty liver disease (NAFLD). Metformin activates AMP-activated protein kinase (AMPK), the cellular energy sensor that is sensitive to changes in the AMP/ATP-ratio. AMPK is an inhibitor of mammalian target of rapamycin (mTOR). Both AMPK and mTOR are able to modulate cell death. [Aim]: To evaluate the effects of metformin on hepatocyte cell death. [Methods]: Apoptotic cell death was induced in primary rat hepatocytes using either the bile acid glycochenodeoxycholic acid (GCDCA) or TNFα in combination with actinomycin D (actD). AMPK, mTOR and phosphoinositide-3 kinase (PI3K)/Akt were inhibited using pharmacological inhibitors. Apoptosis and necrosis were quantified by caspase activation, acridine orange staining and Sytox green staining respectively. [Results]: Metformin dose-dependently reduces GCDCA-induced apoptosis, even when added 2 hours after GCDCA, without increasing necrotic cell death. Metformin does not protect against TNFα/ActD-induced apoptosis. The protective effect of metformin is dependent on an intact PI3-kinase/Akt pathway, but does not require AMPK/mTOR-signaling. Metformin does not inhibit NF-κB activation. [Conclusion]: Metformin protects against bile acid-induced apoptosis and could be considered in the treatment of chronic liver diseases accompanied by inflammation. © 2013 Woudenberg-Vrenken et al., This work was supported by the Dutch Digestive Foundation and the J.K. de Cock Foundation.

Published

2013

16. Pertussis toxin, an inhibitor of G(αi) PCR, inhibits bile acid- and cytokine-induced apoptosis in primary rat hepatocytes

Author

Klaas Nico Faber, Manon Buist-Homan, Han Moshage, Golnar Karimian, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, Necrosis, LIVER, Time Factors, Nucleotide Receptor Signaling, Cancer Treatment, lcsh:Medicine, Apoptosis, p38 Mitogen-Activated Protein Kinases, Receptors, G-Protein-Coupled, chemistry.chemical_compound, Phosphatidylinositol 3-Kinases, Molecular Cell Biology, Tyrosine Kinase Signaling Cascade, Membrane Receptor Signaling, lcsh:Science, Crosstalk, Protein Kinase C, Apoptotic Signaling Cascade, Cellular Stress Responses, Mitogen-Activated Protein Kinase 1, Multidisciplinary, Mitogen-Activated Protein Kinase 3, Primary Biliary Cirrhosis, Bile acid, Protein Kinase Signaling Cascade, Cell Death, MEMBRANE-PROTEIN, Caspase 3, Liver Diseases, Mechanisms of Signal Transduction, Hep G2 Cells, Hormone Receptor Signaling, Signaling Cascades, Cirrhosis, Oncology, ADP-ribosylation, Cytokines, Medicine, Tumor necrosis factor alpha, medicine.symptom, Biliary Disorders, FARNESOID-X-RECEPTOR, Research Article, Signal Transduction, Programmed cell death, medicine.drug_class, SUBUNIT STRUCTURE, Acute Liver Failure, Cytokine Therapy, Gastroenterology and Hepatology, Biology, Pertussis toxin, Bile Acids and Salts, PROTEIN-COUPLED RECEPTORS, GI-PROTEIN, Glycochenodeoxycholic Acid, Glycochenodeoxycholic acid, medicine, Primary Sclerosing Cholangitis, Animals, Humans, Rats, Wistar, ADP-RIBOSYLATION, ISLET-ACTIVATING PROTEIN, lcsh:R, Molecular biology, Rats, DRUG DISCOVERY, Enzyme Activation, chemistry, CELL-DEATH, Pertussis Toxin, Hepatocytes, lcsh:Q

Abstract

Excessive hepatocyte apoptosis is a common event in acute and chronic liver diseases leading to loss of functional liver tissue. Approaches to prevent apoptosis have therefore high potential for the treatment of liver disease. G-protein coupled receptors (GPCR) play crucial roles in cell fate (proliferation, cell death) and act through heterotrimeric G-proteins. G(alpha i)PCRs have been shown to regulate lipoapoptosis in hepatocytes, but their role in inflammation- or bile acid-induced apoptosis is unknown. Here, we analyzed the effect of inhibiting G(alpha i)PCR function, using pertussis toxin (PT), on bile acid-and cytokine-induced apoptosis in hepatocytes. Primary rat hepatocytes, HepG2-rNtcp cells (human hepatocellular carcinoma cells) or H-4-II-E cells (rat hepatoma cells) were exposed to glycochenodeoxycholic acid (GCDCA) or tumor necrosis factor-alpha (TNF alpha)/actinomycin D (ActD). PT (50-200 nmol/L) was added 30 minutes prior to the apoptotic stimulus. Apoptosis (caspase-3 activity, acridine orange staining) and necrosis (sytox green staining) were assessed. PT significantly reduced GCDCA-and TNF alpha/ActD-induced apoptosis in rat hepatocytes (260%, p, 0.05) in a dose-dependent manner (with no shift to necrosis), but not in HepG2-rNtcp cells or rat H-4-II-E cells. The protective effect of pertussis toxin was independent of the activation of selected cell survival signal transduction pathways, including ERK, p38 MAPK, PI3K and PKC pathways, as specific protein kinase inhibitors did not reverse the protective effects of pertussis toxin in GCDCA-exposed hepatocytes. Conclusion: Pertussis toxin, an inhibitor of G(alpha i)PCRs, protects hepatocytes, but not hepatocellular carcinoma cells, against bile acid-and cytokine-induced apoptosis and has therapeutic potential as primary hepatoprotective drug, as well as adjuvant in anticancer therapy.

Published

2012

17. Anti-oxidants do not prevent bile acid-induced cell death in rat hepatocytes

Author

Titia E, Woudenberg-Vrenken, Manon, Buist-Homan, Laura, Conde de la Rosa, Klaas Nico, Faber, and Han, Moshage

Subjects

Male, Caspase 3, NADPH Oxidases, Apoptosis, Antioxidants, Rats, Rats, Zucker, Necrosis, Oxidative Stress, src-Family Kinases, Glycochenodeoxycholic Acid, Cytoprotection, Heme Oxygenase (Decyclizing), Hepatocytes, Animals, RNA, Messenger, Rats, Wistar, Reactive Oxygen Species, Protein Kinase Inhibitors, Cells, Cultured, Taurolithocholic Acid

Abstract

Bile acids, reactive oxygen species (ROS) and inflammatory cytokines are crucial regulators of cell death in acute and chronic liver diseases. The contribution of each factor to hepatocyte death, either apoptosis or necrosis, has not been clarified as yet. It has been suggested that the generation of oxidative stress by bile acids contributes to hepatocyte death during cholestasis and bile acid toxicity, although the beneficial role of ROS prevention in bile acid-mediated cell death is not fully understood.Study the effects of anti-oxidants in bile acid-induced cell death in vitro.Primary rat hepatocytes were exposed to the bile acids glycochenodeoxycholic acid (GCDCA) or taurolithocholic acid-3 sulphate in the absence or presence of ROS scavengers or anti-oxidants. Haeme oxygenase (HO)-1 mRNA levels were analysed by quantitative polymerase chain reaction. Apoptosis was quantified by acridine orange staining and caspase-3 activity assay. Necrosis was detected by Sytox green staining.Anti-oxidants do not attenuate bile acid-induced cell death. Furthermore, bile acid exposure does not enhance the mRNA expression of the oxidative stress-responsive gene HO-1. The Src-kinase inhibitor, SU6656, does reduce GCDCA-induced apoptosis and necrosis.In hepatocytes, bile acid-induced toxicity is not prevented by scavengers of oxidative stress. The beneficial effects observed in patients might be because of the contribution of ROS and cytokines rather than bile acid-mediated oxidative stress. However, the use of specific Src kinase inhibitors might be a useful tool to prevent bile acid-induced injury in liver diseases.

Published

2010

18. Unconjugated bile salts shuttle through hepatocyte peroxisomes for taurine conjugation

Author

Jannes Woudenberg, Miguel A. Miranda, Krzysztof P. Rembacz, Klaas Nico Faber, Fiona A.J. van den Heuvel, Mark Hoekstra, Jana Rohacova, M. Luisa Marin, Titia E. Woudenberg-Vrenken, Elles Jonkers, Frans Stellaard, Manon Buist-Homan, Han Moshage, Faculteit Medische Wetenschappen/UMCG, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

EXPRESSION, Male, Taurine, Apoptosis, Digitonin, Biology, ACTIVATION, Bile Acids and Salts, chemistry.chemical_compound, Tandem Mass Spectrometry, Glyceraldehyde, HUMAN LIVER, medicine, BAAT, Peroxisomes, Animals, ACID N-ACYLTRANSFERASE, Molecular gastro-enterology and hepatology [IGMD 2], Rats, Wistar, Enterohepatic circulation, Cells, Cultured, INDUCED APOPTOSIS, Hepatology, Cholic acid, MASS-SPECTROMETRY, IN-VITRO, Peroxisome, TRANSPORT, Rats, medicine.anatomical_structure, Biochemistry, chemistry, Hepatocyte, Hepatocytes, MEMBRANE, PROTECTS RAT HEPATOCYTES, Cholates, Acyltransferases, Chromatography, Liquid

Abstract

Item does not contain fulltext Bile acid-CoA:amino acid N-acyltransferase (BAAT) conjugates bile salts to glycine or taurine, which is the final step in bile salt biosynthesis. In addition, BAAT is required for reconjugation of bile salts in the enterohepatic circulation. Recently, we showed that BAAT is a peroxisomal protein, implying shuttling of bile salts through peroxisomes for reconjugation. However, the subcellular location of BAAT remains a topic of debate. The aim of this study was to obtain direct proof for reconjugation of bile salts in peroxisomes. Primary rat hepatocytes were incubated with deuterium-labeled cholic acid (D(4)CA). Over time, media and cells were collected and the levels of D(4)CA, D(4)-tauro-CA (D(4)TCA), and D(4)-glyco-CA (D(4)GCA) were quantified by liquid chromatography-tandem mass spectrometry (LC/MS/MS). Subcellular accumulation of D(4)-labeled bile salts was analyzed by digitonin permeabilization assays and subcellular fractionation experiments. Within 24 hours, cultured rat hepatocytes efficiently (>90%) converted and secreted 100 muM D(4)CA to D(4)TCA and D(4)GCA. The relative amounts of D(4)TCA and D(4)GCA produced were dependent on the presence of glycine or taurine in the medium. Treatment of D(4)CA-exposed hepatocytes with 30-150 mug/mL digitonin led to the complete release of D(4)CA, D(4)GCA, and glyceraldehyde 3-phosphate dehydrogenase (GAPDH) (cytosolic marker). Full release of D(4)TCA, catalase, and BAAT was only observed at 500 mug/mL digitonin, indicating the presence of D(4)TCA in membrane-enclosed organelles. D(4)TCA was detected in fractions of purified peroxisomes, which did not contain D(4)CA and D(4)GCA. Conclusion: We established a novel assay to study conjugation and intra- and transcellular transport of bile salts. Using this assay, we show that cholic acid shuttles through peroxisomes for taurine-conjugation. 01 december 2010

Published

2010

19. Multidrug resistance-associated proteins are crucial for the viability of activated rat hepatic stellate cells

Author

Albert Geerts, Sandra Dunning, Fiona A.J. van den Heuvel, Jannes Woudenberg, M Geuken, Manon Buist-Homan, Tania Roskams, Sara Vander Borght, Klaas Nico Faber, Rebekka A. Hannivoort, Fiona Oakley, Ben Schroyen, Han Moshage, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, ATP Binding Cassette Transporter, Subfamily B, Cell Survival, Cell, Interleukin-1beta, ATP-binding cassette transporter, LIVER FIBROSIS, Biology, Liver Cirrhosis, Experimental, DISEASE, Flow cytometry, MECHANISMS, MDR1B EXPRESSION, Interferon-gamma, medicine, INJURY, Animals, Humans, Viability assay, RNA, Messenger, Molecular gastro-enterology and hepatology [IGMD 2], Rats, Wistar, Cells, Cultured, Hepatology, medicine.diagnostic_test, Tumor Necrosis Factor-alpha, Multidrug resistance-associated protein 2, INDUCTION, Transporter, TRANSPORTERS, Cell biology, APOPTOSIS, Rats, Oxidative Stress, medicine.anatomical_structure, Biochemistry, PROGENITOR CELLS, Genetic defects of metabolism [UMCN 5.1], Liver, Hepatic stellate cell, Hepatocytes, ATP-Binding Cassette Transporters, Multidrug Resistance-Associated Proteins

Abstract

Hepatic stellate cells (HSCs) survive and proliferate in the chronically injured liver. ATP-binding cassette (ABC) transporters play a crucial role in cell viability by transporting toxic metabolites or xenobiotics out of the cell. ABC transporter expression in HSCs and its relevance to cell viability and/or activation have not been reported so far. The aim of this study was to investigate the expression, regulation, and function of multidrug resistance–associated protein (Mrp)-type and multidrug resistance protein (Mdr)–type ABC transporters in activated rat HSCs. Rat HSCs were exposed to cytokines or oxidative stress. ABC transporter expression was determined by quantitative polymerase chain reaction and immunohistochemistry. HSCs were exposed to the Mdr inhibitors verapamil and PSC-833 and the Mrp inhibitor MK571. Mdr and Mrp transporter function was evaluated with flow cytometry. Apoptosis was determined by activated caspase-3 and acridine orange staining, and necrosis was determined by Sytox green nuclear staining. An in vivo model of carbon tetrachloride (CCl4)–induced liver fibrosis was used. With respect to hepatocytes, activated HSCs expressed high levels of Mrp1 and comparable levels of Mrp3, Mrp4, Mdr1a, and Mdr1b but not the hepatocyte-specific transporters bile salt export pump, Mrp2, and Mrp6. Mrp1 protein staining correlated with desmin staining in livers from CCl4-treated rats. Mrp1 expression increased upon activation of HSCs. Cytokines induced Mdr1b expression only. Oxidative stress was not a major regulator of Mdr and Mrp transporter expression. Activated HSCs became necrotic when exposed to the Mrp inhibitors. Conclusion: Activated HSCs contain relatively high levels of Mrp1. Mrp-type transporters are required for the viability of activated HSCs. Mrp-dependent export of endogenous metabolites is important for the survival of activated HSCs in chronic liver diseases. (HEPATOLOGY 2008.)

Published

2008

20. The active metabolite of leflunomide, A77 1726, protects rat hepatocytes against bile acid-induced apoptosis

Author

Manon Buist-Homan, TE Vrenken, Andries Kalsbeek, Han Moshage, Klaas Nico Faber, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, Hydroxybutyrates, Apoptosis, Pharmacology, Signal transduction, ACTIVATION, chemistry.chemical_compound, TYROSINE PHOSPHORYLATION, Aniline Compounds, Bile acid, FAMILY KINASE YES, Anti-Inflammatory Agents, Non-Steroidal, NF-kappa B, SALT-INDUCED APOPTOSIS, FACTOR-KAPPA-B, medicine.anatomical_structure, Hepatocyte, Mitogen-activated protein kinase, Caspases, Crotonates, LIVER-INJURY, Leflunomide, medicine.medical_specialty, Programmed cell death, Toluidines, medicine.drug_class, MAP Kinase Signaling System, p38 mitogen-activated protein kinases, INHIBITION, Biology, In Vitro Techniques, Bile Acids and Salts, Necrosis, Glycochenodeoxycholic Acid, Internal medicine, Nitriles, medicine, Glycochenodeoxycholic acid, Animals, Rats, Wistar, Protein kinase B, Hepatology, Tumor Necrosis Factor-alpha, Isoxazoles, Bile acids, RHEUMATOID-ARTHRITIS, Rats, MITOCHONDRIAL PERMEABILITY TRANSITION, Oxidative Stress, Endocrinology, chemistry, biology.protein, Hepatocytes, GROWTH-FACTOR RECEPTOR

Abstract

Background/Aims: Leflunomide is used in the treatment of autoimmune diseases as an anti-inflammatory agent. Leflunomide and its active metabolite A77 1726 modulate mitogen-activated protein kinases (MAPK), Src kinases, the phosphoinositide-3 kinase (PI3K)/Akt-pathway and nuclear factor (NF)-kappa B activation. Both cell protective and cytotoxic effects of leflunomide have been described. Since leflunomide affects pathways involved in hepatocyte cell survival, we examined the effects of A77 1726 on hepatocyte cell death.Methods: Primary rat hepatocytes were exposed to the bile acid glycochenodeoxycholic acid (GCDCA), the superoxide anion donor menadione, or tumor necrosis factor (TNF) alpha in combination with actinomycin D. Activation of MAP-kinases was determined by Western blot analysis. Apoptosis and necrosis were analyzed by acridine orange staining and caspase activity and Sytox Green staining, respectively.Results: A77 1726 dose-dependently reduces GCDCA-induced apoptosis and necrosis, but not menadione- or TNF alpha/ActD-induced apoptosis. The hepatoprotective effect of A77 1726 does not involve ERK1/2, p38 or PI3K/Akt activation. A77 1726 does not inhibit NF-kappa B activation in hepatocytes.Conclusions: Since A77 1726 inhibits bile acid-induced apoptosis and does not sensitize hepatocytes to TNF alpha, our results suggest that A77 1726 could be considered for the treatment of chronic liver diseases accompanied by elevated bile acid levels and inflammation. (C) 2008 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.

Published

2007

21. Superoxide anions and hydrogen peroxide induce hepatocyte death by different mechanisms: involvement of JNK and ERK MAP kinases

Author

TE Vrenken, MH Schoemaker, Manon Buist-Homan, Peter L.M. Jansen, Han Moshage, Rick Havinga, Laura Conde de la Rosa, Amsterdam Gastroenterology Endocrinology Metabolism, Gastroenterology and Hepatology, and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, necrosis, chemistry.chemical_compound, Menadione, Superoxides, 4-NAPHTHOQUINONE, oxidative stress, glutathione, Extracellular Signal-Regulated MAP Kinases, Cells, Cultured, Caspase, chemistry.chemical_classification, N-TERMINAL KINASE, INDUCED LIVER-INJURY, biology, Chemistry, Superoxide, NF-kappa B, apoptosis, Vitamin K 3, Free Radical Scavengers, Vitamins, Oxidants, Specific Pathogen-Free Organisms, FACTOR-KAPPA-B, PREVENTS APOPTOSIS, Caspases, Mitogen-activated protein kinase, signal transduction, MENADIONE 2-METHYL-1, Programmed cell death, MAP Kinase Signaling System, caspase, SIGNAL-TRANSDUCTION, ACID-INDUCED APOPTOSIS, Superoxide dismutase, MENADIONE 2-METHYL-1,4-NAPHTHOQUINONE, Animals, Rats, Wistar, NITRIC-OXIDE SYNTHASE, Reactive oxygen species, RAT HEPATOCYTES, Hepatology, JNK Mitogen-Activated Protein Kinases, Hydrogen Peroxide, Molecular biology, Rats, Apoptosis, Hepatocytes, biology.protein, Reactive Oxygen Species

Abstract

Background/Aims: In liver diseases, reactive oxygen species (ROS) are involved in cell death and liver injury, but the mechanisms are not completely elucidated. To elucidate the mechanisms of hepatocyte cell death induced by the ROS superoxide anions and hydrogen peroxide, primary cultures of hepatocytes were exposed to the superoxide anion donor menadione (10-50 mu mol/L) or H(2)O(2) (1-5 mmol/L). Hepatocytes were also treated with caspases and MAPKs inhibitors, superoxide dismutase (PEG-SOD) and SNAP, a nitric oxide donor. Apoptosis was determined by measuring caspase-9, -6, -3 activation and cleaved PARP, and necrotic cell death by Sytox Green staining.Results: (1) Menadione (50 mu mol/L) induces JNK phosphorylation, caspase-9, -6, -3 activation, PARP cleavage and apoptosis. Superoxide anions-induced apoptosis is dependent on JNK activity. Menadione (50 mu mol/L) induces the phosphorylation of ERK1/2 and this attenuates cell death. (2) H(2)O(2) increases necrotic cell death at high concentration or when H(2)O(2) detoxification is impaired. H202 does not activate MAPKs signalling. (3) PEG-SOD prevents ERK1/2-, JNK- phosphorylation, caspase activation and apoptosis induced by menadione. Glutathione depletion increases menadione-induced apoptosis. (4) SNAP abolishes menadione-induced apoptosis but increases necrotic cell death.Conclusions: In normal hepatocytes, superoxide anions-induced caspase activation and apoptosis is dependent on JNK activity and totally abolished by superoxide scavengers. (c) 2005 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.

Published

2006

22. Angiotensin II Protects Primary Rat Hepatocytes against Bile Salt-Induced Apoptosis

Author

Klaas Nico Faber, Bojana Mikus, Golnar Karimian, Robert H. Henning, Han Moshage, Manon Buist-Homan, Groningen Kidney Center (GKC), Vascular Ageing Programme (VAP), Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Center for Liver, Digestive and Metabolic Diseases (CLDM), Restoring Organ Function by Means of Regenerative Medicine (REGENERATE), and Groningen Institute for Organ Transplantation (GIOT)

Subjects

Male, MAPK/ERK pathway, lcsh:Medicine, Apoptosis, LIVER FIBROSIS, Signal transduction, ERK signaling cascade, Phosphatidylinositol 3-Kinases, chemistry.chemical_compound, Molecular cell biology, ENDOPLASMIC-RETICULUM STRESS, OXIDATIVE STRESS, lcsh:Science, Receptor, Cells, Cultured, Protein Kinase C, Cellular Stress Responses, TRIGGERS APOPTOSIS, Primary Biliary Cirrhosis, Multidisciplinary, Cell Death, Caspase 3, Liver Diseases, Angiotensin II, Clinical Pharmacology, Signaling cascades, Vitamin K 3, ER STRESS, Endoplasmic Reticulum Stress, medicine.anatomical_structure, Hepatocyte, Dactinomycin, Medicine, Biliary Disorders, Research Article, Taurolithocholic Acid, Drugs and Devices, medicine.medical_specialty, Programmed cell death, MAPK signaling cascades, MAP Kinase Signaling System, Primary Cell Culture, Gastroenterology and Hepatology, HEPATIC STELLATE CELLS, Biology, ACID-INDUCED APOPTOSIS, Receptor, Angiotensin, Type 1, Apoptotic signaling cascade, Adverse Reactions, Glycochenodeoxycholic Acid, Internal medicine, Primary Sclerosing Cholangitis, medicine, Glycochenodeoxycholic acid, Animals, Rats, Wistar, CHOP GADD153, Cell Shape, RECEPTOR BLOCKER, Tumor Necrosis Factor-alpha, lcsh:R, Rats, Enzyme Activation, Endocrinology, chemistry, Hepatocytes, Hepatic stellate cell, lcsh:Q, Reactive Oxygen Species, INDUCED HEPATOTOXICITY

Abstract

UNLABELLED: Angiotensin II (AT-II) is a pro-fibrotic compound that acts via membrane-bound receptors (AT-1R/AT-2R) and thereby activates hepatic stellate cells (HSCs). AT-II receptor blockers (ARBs) are thus important candidates in the treatment of liver fibrosis. However, multiple case reports suggest that AT-1R blockers may induce hepatocyte injury. Therefore, we investigated the effect of AT-II and its receptor blockers on cytokine-, oxidative stress- and bile salt-induced cell death in hepatocytes. Primary rat hepatocytes were exposed to TNF-α/Actinomycin D, the ROS-generating agent menadione or the bile salts: glycochenodeoxycholic acid (GCDCA) and tauro-lithocholic acid-3 sulfate (TLCS), to induce apoptosis. AT-II (100 nmol/L) was added 10 minutes prior to the cell death-inducing agent. AT-1R antagonists (Sartans) and the AT-2R antagonist PD123319 were used at 1 µmol/L. Apoptosis (caspase-3 activity, acridine orange staining) and necrosis (Sytox green staining) were quantified. Expression of CHOP (marker for ER stress) and AT-II receptor mRNAs were quantified by Q-PCR. AT-II dose-dependently reduced GCDCA-induced apoptosis of hepatocytes (-50%, p

Published

2012