Nitrosative Stress and Lipid Homeostasis as a Mechanism for Zileuton Hepatotoxicity and Resistance in Genetically Sensitive Mice

Abstract Zileuton is an orally active inhibitor of leukotriene synthesis for maintenance treatment of asthma, for which clinical usage has been associated with idiosyncratic liver injury. Mechanistic understanding of zileuton toxicity is hampered by the rarity of the cases and lack of an animal model. A promising model for mechanistic study of rare liver injury is the Diversity Outbred (J:DO) mouse population, with genetic variation similar to that found in humans. In this study, female DO mice were administered zileuton or vehicle daily for 7 days (i.g.). Serum liver enzymes were elevated in the zileuton group, with marked interindividual variability in response. Zileuton exposure-induced findings in susceptible DO mice included microvesicular fatty change, hepatocellular mitosis, and hepatocellular necrosis. Inducible nitric oxide synthase and nitrotyrosine abundance were increased in livers of animals with necrosis and those with fatty change, implicating nitrosative stress as a possible injury mechanism. Conversely, DO mice lacking adverse liver pathology following zileuton exposure experienced decreased hepatic concentrations of resistin and increased concentrations of insulin and leptin, providing potential clues into mechanisms of toxicity resistance. Transcriptome pathway analysis highlighted mitochondrial dysfunction and altered fatty acid oxidation as key molecular perturbations associated with zileuton exposure, and suggested that interindividual differences in cytochrome P450 metabolism, glutathione-mediated detoxification, and farnesoid X receptor signaling may contribute to zileuton-induced liver injury (ZILI). Taken together, DO mice provided a platform for investigating mechanisms of toxicity and resistance in context of ZILI which may lead to targeted therapeutic interventions.

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Faculty Opinions recommendation of Mouse population-guided resequencing reveals that variants in CD44 contribute to acetaminophen-induced liver injury in humans.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.1160848.622265 ◽

2009 ◽

Author(s):

Michael Cunningham

Keyword(s):

Liver Injury ◽

Mouse Population

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Faculty Opinions recommendation of Farnesoid X Receptor Protects Against Low-dose Carbon Tetrachloride-induced Liver Injury Through the Taurocholate-JNK Pathway.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.727616019.793532324 ◽

2017 ◽

Author(s):

Grace Guo

Keyword(s):

Carbon Tetrachloride ◽

Liver Injury ◽

Low Dose ◽

Farnesoid X Receptor ◽

Jnk Pathway

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Depdc5 deficiency exacerbates alcohol-induced hepatic steatosis via suppression of PPARα pathway

Cell Death and Disease ◽

10.1038/s41419-021-03980-6 ◽

2021 ◽

Vol 12 (7) ◽

Author(s):

Lin Xu ◽

Xinge Zhang ◽

Yue Xin ◽

Jie Ma ◽

Chenyan Yang ◽

...

Keyword(s):

Liver Injury ◽

Hepatic Steatosis ◽

Liver Steatosis ◽

Pharmacological Intervention ◽

Acid Oxidation ◽

Peroxisome Proliferator ◽

Pathological Effect ◽

Mtorc1 Pathway

AbstractAlcohol-related liver disease (ALD), a condition caused by alcohol overconsumption, occurs in three stages of liver injury including steatosis, hepatitis, and cirrhosis. DEP domain-containing protein 5 (DEPDC5), a component of GAP activities towards Rags 1 (GATOR1) complex, is a repressor of amino acid-sensing branch of the mammalian target of rapamycin complex 1 (mTORC1) pathway. In the current study, we found that aberrant activation of mTORC1 was likely attributed to the reduction of DEPDC5 in the livers of ethanol-fed mice or ALD patients. To further define the in vivo role of DEPDC5 in ALD development, we generated Depdc5 hepatocyte-specific knockout mouse model (Depdc5-LKO) in which mTORC1 pathway was constitutively activated through loss of the inhibitory effect of GATOR1. Hepatic Depdc5 ablation leads to mild hepatomegaly and liver injury and protects against diet-induced liver steatosis. In contrast, ethanol-fed Depdc5-LKO mice developed severe hepatic steatosis and inflammation. Pharmacological intervention with Torin 1 suppressed mTORC1 activity and remarkably ameliorated ethanol-induced hepatic steatosis and inflammation in both control and Depdc5-LKO mice. The pathological effect of sustained mTORC1 activity in ALD may be attributed to the suppression of peroxisome proliferator activated receptor α (PPARα), the master regulator of fatty acid oxidation in hepatocytes, because fenofibrate (PPARα agonist) treatment reverses ethanol-induced liver steatosis and inflammation in Depdc5-LKO mice. These findings provide novel insights into the in vivo role of hepatic DEPDC5 in the development of ALD.

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Mitochondrial Fatty Acid Oxidation and Susceptibility to Endotoxin in Acute Liver Injury

Journal of Bacteriology ◽

10.1128/jb.90.5.1365-1372.1965 ◽

1965 ◽

Vol 90 (5) ◽

pp. 1365-1372 ◽

Cited By ~ 2

Author(s):

W. Edmund Farrar ◽

Laurence M. Corwin ◽

Thomas H. Kent

Keyword(s):

Fatty Acid ◽

Liver Injury ◽

Fatty Acid Oxidation ◽

Acute Liver Injury ◽

Acid Oxidation ◽

Mitochondrial Fatty Acid Oxidation ◽

Mitochondrial Fatty Acid

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Arbutin Alleviates the Liver Injury of α-Naphthylisothiocyanate-induced Cholestasis Through Farnesoid X Receptor Activation

Frontiers in Cell and Developmental Biology ◽

10.3389/fcell.2021.758632 ◽

2021 ◽

Vol 9 ◽

Author(s):

Peijie Wu ◽

Ling Qiao ◽

Han Yu ◽

Hui Ming ◽

Chao Liu ◽

...

Keyword(s):

Bile Acid ◽

Liver Injury ◽

Protective Effect ◽

Bile Acids ◽

Liver Toxicity ◽

Enterohepatic Circulation ◽

Receptor Activation ◽

Farnesoid X Receptor ◽

Bile Acid Metabolism ◽

Cholestatic Diseases

Cholestasis is a kind of stressful syndrome along with liver toxicity, which has been demonstrated to be related to fibrosis, cirrhosis, even cholangiocellular or hepatocellular carcinomas. Cholestasis usually caused by the dysregulated metabolism of bile acids that possess high cellular toxicity and synthesized by cholesterol in the liver to undergo enterohepatic circulation. In cholestasis, the accumulation of bile acids in the liver causes biliary and hepatocyte injury, oxidative stress, and inflammation. The farnesoid X receptor (FXR) is regarded as a bile acid–activated receptor that regulates a network of genes involved in bile acid metabolism, providing a new therapeutic target to treat cholestatic diseases. Arbutin is a glycosylated hydroquinone isolated from medicinal plants in the genus Arctostaphylos, which has a variety of potentially pharmacological properties, such as anti-inflammatory, antihyperlipidemic, antiviral, antihyperglycemic, and antioxidant activity. However, the mechanistic contributions of arbutin to alleviate liver injury of cholestasis, especially its role on bile acid homeostasis via nuclear receptors, have not been fully elucidated. In this study, we demonstrate that arbutin has a protective effect on α-naphthylisothiocyanate–induced cholestasis via upregulation of the levels of FXR and downstream enzymes associated with bile acid homeostasis such as Bsep, Ntcp, and Sult2a1, as well as Ugt1a1. Furthermore, the regulation of these functional proteins related to bile acid homeostasis by arbutin could be alleviated by FXR silencing in L-02 cells. In conclusion, a protective effect could be supported by arbutin to alleviate ANIT-induced cholestatic liver toxicity, which was partly through the FXR pathway, suggesting arbutin may be a potential chemical molecule for the cholestatic disease.

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Dietary β-Cryptoxanthin Inhibits High-Refined Carbohydrate Diet–Induced Fatty Liver via Differential Protective Mechanisms Depending on Carotenoid Cleavage Enzymes in Male Mice

Journal of Nutrition ◽

10.1093/jn/nxz106 ◽

2019 ◽

Vol 149 (9) ◽

pp. 1553-1564 ◽

Cited By ~ 5

Author(s):

Ji Ye Lim ◽

Chun Liu ◽

Kang-Quan Hu ◽

Donald E Smith ◽

Dayong Wu ◽

...

Keyword(s):

Fatty Liver ◽

Farnesoid X Receptor ◽

Receptor Protein ◽

Acid Oxidation ◽

Peroxisome Proliferator ◽

Double Knockout ◽

Carbohydrate Diet ◽

Peroxisome Proliferator Activated Receptor ◽

Nonalcoholic Fatty Liver ◽

Β Carotene

ABSTRACT Background β-Cryptoxanthin (BCX), a provitamin A carotenoid shown to protect against nonalcoholic fatty liver disease (NAFLD), can be cleaved by β-carotene-15,15′-oxygenase (BCO1) to generate vitamin A, and by β-carotene-9′,10′-oxygenase (BCO2) to produce bioactive apo-carotenoids. BCO1/BCO2 polymorphisms have been associated with variations in plasma carotenoid amounts in both humans and animals. Objectives We investigated whether BCX feeding inhibits high refined-carbohydrate diet (HRCD)-induced NAFLD, dependent or independent of BCO1/BCO2. Methods Six-week-old male wild-type (WT) and BCO1−/−/BCO2−/− double knockout (DKO) mice were randomly fed HRCD (66.5% of energy from carbohydrate) with or without BCX (10 mg/kg diet) for 24 wk. Pathological and biochemical variables were analyzed in the liver and mesenteric adipose tissues (MATs). Data were analyzed by 2-factor ANOVA. Results Compared to their respective HRCD controls, BCX reduced hepatic steatosis severity by 33‒43% and hepatic total cholesterol by 43‒70% in both WT and DKO mice (P < 0.01). Hepatic concentrations of BCX, but not retinol and retinyl palmitate, were 33-fold higher in DKO mice than in WT mice (P < 0.001). BCX feeding increased the hepatic fatty acid oxidation protein peroxisome proliferator-activated receptor-α, and the cholesterol efflux gene ATP-binding cassette transporter5, and suppressed the lipogenesis gene acetyl-CoA carboxylase 1 (Acc1) in the MAT of WT mice but not DKO mice (P < 0.05). BCX feeding decreased the hepatic lipogenesis proteins ACC and stearoyl-CoA desaturase-1 (3-fold and 5-fold) and the cholesterol synthesis genes 3-hydroxy-3-methyl-glutaryl-coenzyme A reductase and HMG-CoA synthase 1 (2.7-fold and 1.8-fold) and increased the cholesterol catabolism gene cholesterol 7α-hydroxylase (1.9-fold) in the DKO but not WT mice (P < 0.05). BCX feeding increased hepatic protein sirtuin1 (2.5-fold) and AMP-activated protein kinase (9-fold) and decreased hepatic farnesoid X receptor protein (80%) and the inflammatory cytokine gene Il6 (6-fold) in the MAT of DKO mice but not WT mice (P < 0.05). Conclusion BCX feeding mitigates HRCD-induced NAFLD in both WT and DKO mice through different mechanisms in the liver-MAT axis, depending on the presence or absence of BCO1/BCO2.

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Protective Role of Shiitake Mushroom-Derived Exosome-Like Nanoparticles in D-Galactosamine and Lipopolysaccharide-Induced Acute Liver Injury in Mice

Nutrients ◽

10.3390/nu12020477 ◽

2020 ◽

Vol 12 (2) ◽

pp. 477 ◽

Cited By ~ 3

Author(s):

Baolong Liu ◽

Yizhu Lu ◽

Xingyi Chen ◽

Philma Glora Muthuraj ◽

Xingzhi Li ◽

...

Keyword(s):

Liver Injury ◽

Nlrp3 Inflammasome ◽

Acute Liver Injury ◽

Therapeutic Potential ◽

Disease Model ◽

Protective Role ◽

Therapeutic Interventions ◽

Inflammasome Activation ◽

Mrna Levels ◽

Shiitake Mushroom

Fulminant hepatic failure (FHF) is a rare, life-threatening liver disease with a poor prognosis. Administration of D-galactosamine (GalN) and lipopolysaccharide (LPS) triggers acute liver injury in mice, simulating many clinical features of FHF in humans; therefore, this disease model is often used to investigate potential therapeutic interventions to treat FHF. Recently, suppression of the nucleotide-binding domain and leucine-rich repeat related (NLR) family, pyrin domain containing 3 (NLRP3) inflammasome, was shown to alleviate the severity of GalN/LPS-induced liver damage in mice. Therefore, the goal of this study was to find dietary exosome-like nanoparticles (ELNs) with therapeutic potential in curbing FHF by suppressing the NLRP3 inflammasome. Seven commonly consumed mushrooms were used to extract ELNs. These mushrooms were found to contain ELNs composed of RNAs, proteins, and lipids. Among these mushroom-derived ELNs, only shiitake mushroom-derived ELNs (S-ELNs) substantially inhibited NLRP3 inflammasome activation by preventing inflammasome formation in primary macrophages. S-ELNs also suppressed the secretion of interleukin (IL)-6, as well as both protein and mRNA levels of the Il1b gene. Remarkably, pre-treatment with S-ELNs protected mice from GalN/LPS-induced acute liver injury. Therefore, S-ELNs, identified as potent new inhibitors of the NLRP3 inflammasome, represent a promising class of agents with the potential to combat FHF.

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Mouse population-guided resequencing reveals that variants in CD44 contribute to acetaminophen-induced liver injury in humans

Genome Research ◽

10.1101/gr.090241.108 ◽

2009 ◽

Vol 19 (9) ◽

pp. 1507-1515 ◽

Cited By ~ 132

Author(s):

A. H. Harrill ◽

P. B. Watkins ◽

S. Su ◽

P. K. Ross ◽

D. E. Harbourt ◽

...

Keyword(s):

Liver Injury ◽

Mouse Population

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Cholestatic Drug Induced Liver Injury: A Function of Bile Salt Export Pump Inhibition and Farnesoid X Receptor Antagonism

Applied In Vitro Toxicology ◽

10.1089/aivt.2018.0011 ◽

2018 ◽

Vol 4 (3) ◽

pp. 265-279 ◽

Cited By ~ 7

Author(s):

Jonathan P. Jackson ◽

Kimberly M. Freeman ◽

Robert L. St. Claire ◽

Chris B. Black ◽

Kenneth R. Brouwer

Keyword(s):

Liver Injury ◽

Bile Salt ◽

Farnesoid X Receptor ◽

Bile Salt Export Pump ◽

Drug Induced ◽

Receptor Antagonism ◽

Drug Induced Liver Injury

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Milk osteopontin, a nutritional approach to prevent alcohol-induced liver injury

AJP Gastrointestinal and Liver Physiology ◽

10.1152/ajpgi.00014.2013 ◽

2013 ◽

Vol 304 (10) ◽

pp. G929-G939 ◽

Cited By ~ 26

Author(s):

Xiaodong Ge ◽

Yongke Lu ◽

Tung-Ming Leung ◽

Esben S. Sørensen ◽

Natalia Nieto

Keyword(s):

Liver Disease ◽

Liver Injury ◽

Neutrophil Infiltration ◽

Therapeutic Interventions ◽

High Concentration ◽

Intestinal Integrity ◽

Enterocyte Proliferation ◽

Factor Α ◽

Key Events ◽

Necrosis Factor

Alcohol consumption is a leading cause of liver disease worldwide; thus, there is an urgent need to develop novel therapeutic interventions. Key events for the onset and progression of alcoholic liver disease result in part from the gut-to-liver interaction. Osteopontin is a cytokine present at high concentration in human milk, umbilical cord, and infants' plasma with beneficial potential. We hypothesized that dietary administration of milk osteopontin could prevent alcohol-induced liver injury perhaps by maintaining gut integrity and averting hepatic inflammation and steatosis. Wild-type mice were fed either the control or the ethanol Lieber-DeCarli diets alone or in combination with milk osteopontin for 3 wk, and parameters of gut and liver damage were measured. Milk osteopontin protected the stomach and the gut by increasing gland height, crypt cell plus enterocyte proliferation, and mucin content in addition to lowering macrophages, plasmacytes, lymphocytes, and neutrophils in the mucosa and submucosa in alcohol-fed mice. Milk osteopontin targeted the gut-liver axis, preserving the expression of tight-junction proteins in alcohol-fed mice thus maintaining intestinal integrity and permeability. There was protection from liver injury since transaminases, the activity scores, triglyceride levels, neutrophil infiltration, 3-nitrotyrosine residues, lipid peroxidation end products, translocation of gram-negative bacteria, lipopolysaccharide levels, and tumor necrosis factor-α were lower in cotreated than in ethanol-fed mice. Furthermore, milk osteopontin diminished ethanol-mediated liver injury in OPN knockout mice. Milk osteopontin could be a simple effective nutritional therapeutic strategy to prevent alcohol hepatotoxicity due, among others, to gut protective, anti-inflammatory, and anti-steatotic actions.

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