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1. Exposure to Gulf war illness-related chemicals exacerbates alcohol-induced liver damage in rodents

Author

Anca D. Petrescu, Juliet Venter, Daria D. Danilenko, Daniela Medina, Stephanie Grant, Su Yeon An, Elaina Williams, Patrick Mireles, Kathryn Rhodes, Matthew Tjahja, and Sharon DeMorrow

Subjects
Medicine, Science
Abstract

Abstract Gulf War Illness (GWI) describes a series of symptoms suffered by veterans of the Gulf war, consisting of cognitive, neurological and gastrointestinal dysfunctions. Two chemicals associated with GWI are the insecticide permethrin (PER) and the nerve gas prophylactic pyridostigmine-bromide (PB). In this study we assessed the effects of PER and PB exposure on the pathology and subsequent alcohol (EtOH)-induced liver injury, and the influence of a macrophage depletor, PLX3397, on EtOH-induced liver damage in PER/PB-treated mice. Male C57BL/6 mice were injected daily with vehicle or PER/PB for 10 days, followed by 4 months recovery, then treatment with PLX3397 and a chronic-plus-single-binge EtOH challenge for 10 days. PER/PB exposure resulted in the protracted increase in liver transaminases in the serum and induced chronic low-level microvesicular steatosis and inflammation in GWI vs Naïve mice up to 4 months after cessation of exposure. Furthermore, prior exposure to PER/PB also resulted in exacerbated response to EtOH-induced liver injury, with enhanced steatosis, ductular reaction and fibrosis. The enhanced EtOH-induced liver damage in GWI-mice was attenuated by strategies designed to deplete macrophages in the liver. Taken together, these data suggest that exposure to GWI-related chemicals may alter the liver’s response to subsequent ethanol exposure.

Published
2024
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2. Ghrelin reverses ductular reaction and hepatic fibrosis in a rodent model of cholestasis

Author

Anca D. Petrescu, Stephanie Grant, Elaina Williams, Gabriel Frampton, Evan H. Reinhart, Amy Nguyen, Suyeon An, Matthew McMillin, and Sharon DeMorrow

Subjects
Medicine, Science
Abstract

Abstract The orexigenic peptide ghrelin (Ghr) stimulates hunger signals in the hypothalamus via growth hormone secretagogue receptor (GHS-R1a). Gastric Ghr is synthetized as a preprohormone which is proteolytically cleaved, and acylated by a membrane-bound acyl transferase (MBOAT). Circulating Ghr is reduced in cholestatic injuries, however Ghr’s role in cholestasis is poorly understood. We investigated Ghr’s effects on biliary hyperplasia and hepatic fibrosis in Mdr2-knockout (Mdr2KO) mice, a recognized model of cholestasis. Serum, stomach and liver were collected from Mdr2KO and FVBN control mice treated with Ghr, des-octanoyl-ghrelin (DG) or vehicle. Mdr2KO mice had lower expression of Ghr and MBOAT in the stomach, and lower levels of circulating Ghr compared to WT-controls. Treatment of Mdr2KO mice with Ghr improved plasma transaminases, reduced biliary and fibrosis markers. In the liver, GHS-R1a mRNA was expressed predominantly in cholangiocytes. Ghr but not DG, decreased cell proliferation via AMPK activation in cholangiocytes in vitro. AMPK inhibitors prevented Ghr-induced FOXO1 nuclear translocation and negative regulation of cell proliferation. Ghr treatment reduced ductular reaction and hepatic fibrosis in Mdr2KO mice, regulating cholangiocyte proliferation via GHS-R1a, a G-protein coupled receptor which causes increased intracellular Ca2+ and activation of AMPK and FOXO1, maintaining a low rate of cholangiocyte proliferation.

Published
2020
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3. Elevated circulating TGFβ1 during acute liver failure activates TGFβR2 on cortical neurons and exacerbates neuroinflammation and hepatic encephalopathy in mice

Author

Matthew McMillin, Stephanie Grant, Gabriel Frampton, Anca D. Petrescu, Elaina Williams, Brandi Jefferson, Alison Thomas, Ankita Brahmaroutu, and Sharon DeMorrow

Subjects
Acute liver failure, Azoxymethane, Microglia, Neuroinflammation, Necrosis, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Background Acute liver failure resulting from drug-induced liver injury can lead to the development of neurological complications called hepatic encephalopathy (HE). Hepatic transforming growth factor beta 1 (TGFβ1) is upregulated due to liver failure in mice and inhibiting circulating TGFβ reduced HE progression. However, the specific contributions of TGFβ1 on brain cell populations and neuroinflammation during HE are not known. Therefore, the aim of this study was to characterize hepatic and brain TGFβ1 signaling during acute liver failure and its contribution to HE progression using a combination of pharmacological and genetic approaches. Methods C57Bl/6 or neuron-specific transforming growth factor beta receptor 2 (TGFβR2) null mice (TGFβR2ΔNeu) were treated with azoxymethane (AOM) to induce acute liver failure and HE. The activity of circulating TGFβ1 was inhibited in C57Bl/6 mice via injection of a neutralizing antibody against TGFβ1 (anti-TGFβ1) prior to AOM injection. In all mouse treatment groups, liver damage, neuroinflammation, and neurological deficits were assessed. Inflammatory signaling between neurons and microglia were investigated in in vitro studies through the use of pharmacological inhibitors of TGFβ1 signaling in HT-22 and EOC-20 cells. Results TGFβ1 was expressed and upregulated in the liver following AOM injection. Pharmacological inhibition of TGFβ1 after AOM injection attenuated neurological decline, microglia activation, and neuroinflammation with no significant changes in liver damage. TGFβR2ΔNeu mice administered AOM showed no effect on liver pathology but significantly reduced neurological decline compared to control mice. Microglia activation and neuroinflammation were attenuated in mice with pharmacological inhibition of TGFβ1 or in TGFβR2ΔNeu mice. TGFβ1 increased chemokine ligand 2 (CCL2) and decreased C-X3-C motif ligand 1 (CX3CL1) expression in HT-22 cells and reduced interleukin-1 beta (IL-1ß) expression, tumor necrosis factor alpha (TNFα) expression, and phagocytosis activity in EOC-20 cells. Conclusion Increased circulating TGFβ1 following acute liver failure results in activation of neuronal TGFβR2 signaling, driving neuroinflammation and neurological decline during AOM-induced HE.

Published
2019
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4. FXR-Mediated Cortical Cholesterol Accumulation Contributes to the Pathogenesis of Type A Hepatic Encephalopathy

Author

Matthew McMillin, Stephanie Grant, Gabriel Frampton, Anca D. Petrescu, Jessica Kain, Elaina Williams, Rebecca Haines, Lauren Canady, and Sharon DeMorrow

Subjects
Cytochrome p450 46A1, Farnesoid X Receptor, Acute Liver Failure, Azoxymethane, Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Hepatic encephalopathy is a serious neurologic complication of acute and chronic liver diseases. We previously showed that aberrant bile acid signaling contributes to the development of hepatic encephalopathy via farnesoid X receptor (FXR)-mediated mechanisms in neurons. In the brain, a novel alternative bile acid synthesis pathway, catalyzed by cytochrome p450 46A1 (Cyp46A1), is the primary mechanism by which the brain regulates cholesterol homeostasis. The aim of this study was to determine if FXR activation in the brain altered cholesterol homeostasis during hepatic encephalopathy. Methods: Cyp7A1-/- mice or C57Bl/6 mice pretreated with central infusion of FXR vivo morpholino, 2-hydroxypropyl-β-cyclodextrin, or fed a cholestyramine-supplemented diet were injected with azoxymethane (AOM). Cognitive and neuromuscular impairment as well as liver damage and expression of Cyp46A1 were assessed using standard techniques. The subsequent cholesterol content in the frontal cortex was measured using commercially available kits and by Filipin III and Nile Red staining. Results: There was an increase in membrane-bound and intracellular cholesterol in the cortex of mice treated with AOM that was associated with decreased Cyp46A1 expression. Strategies to inhibit FXR signaling prevented the down-regulation of Cyp46A1 and the accumulation of cholesterol. Treatment of mice with 2-hydroxypropyl-β-cyclodextrin attenuated the AOM-induced cholesterol accumulation in the brain and the cognitive and neuromuscular deficits without altering the underlying liver pathology. Conclusions: During hepatic encephalopathy, FXR signaling increases brain cholesterol and contributes to neurologic decline. Targeting cholesterol accumulation in the brain may be a possible therapeutic target for the management of hepatic encephalopathy.

Published
2018
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5. Leptin Enhances Hepatic Fibrosis and Inflammation in a Mouse Model of Cholestasis

Author

Anca D. Petrescu, Stephanie Grant, Elaina Williams, Su Yeon An, Nikhil Seth, Mark Shell, Tyson Amundsen, Christopher Tan, Yusra Nadeem, Matthew Tjahja, Lancaster Weld, Christopher S. Chu, Julie Venter, Gabriel Frampton, Matthew McMillin, and Sharon DeMorrow

Subjects
Inflammation, Leptin, Liver Cirrhosis, Male, Mice, Knockout, Cholestasis, Hyperplasia, Regular Article, Antibodies, Neutralizing, Pathology and Forensic Medicine, Disease Models, Animal, Mice, Liver, Hepatic Stellate Cells, Animals, Cytokines, Receptors, Leptin, Female, Proto-Oncogene Proteins c-akt
Abstract

Leptin is an adipokine with roles in food intake and energy metabolism through its actions on neurons in the hypothalamus. The role of leptin in obesity and cardiovascular disorders is well documented. However, its influence on liver conditions such as cholestasis is poorly understood. The effects of exogenous leptin and leptin-neutralizing antibody on biliary hyperplasia, hepatic fibrosis, and inflammation in the multidrug resistance protein 2 knockout (Mdr2KO) mouse model of cholestasis were assessed by quantifying markers specific for cholangiocytes, activated hepatic stellate cells (HSCs), and cytokines. Serum and hepatic leptin were increased in Mdr2KO mice compared with FVB/NJ (FVBN) controls, and exogenous leptin enhanced biliary hyperplasia and liver fibrosis in Mdr2KO and FVBN mice. Leptin administration increased hepatic expression of C-C motif chemokine ligand 2 and IL-6 in Mdr2KO mice. In contrast, leptin-neutralizing antibody reduced intrahepatic bile duct mass and decreased HSC activation in Mdr2KO mice compared with FVBN controls. Sex-related differences were noted, with female Mdr2KO mice having more leptin than males. In cholangiocytes and LX2 cells in vitro, leptin increased phosphorylated Akt and stimulated cell proliferation. Leptin receptor siRNA and inhibitors of Akt phosphorylation impaired leptin-induced cell proliferation and proinflammatory cytokines. The current data suggest that leptin is abnormally increased in cholestatic mice, and excess leptin increases ductular reaction, hepatic fibrosis, and inflammation via leptin receptor–mediated phosphorylation of Akt in cholangiocytes and HSCs.

Published
2022

6. Coordinated Targeting of Galanin Receptors on Cholangiocytes and Hepatic Stellate Cells Ameliorates Liver Fibrosis in Multidrug Resistance Protein 2 Knockout Mice

Author

Gabriel Frampton, Stephanie Grant, Elaina Williams, Evan Reinhart, Matthew McMillin, Rebekah John, Marcus Davies, Hanna Blaney, Sharon DeMorrow, Anca D. Petrescu, and Natalie Parks

Subjects
Liver Cirrhosis, 0301 basic medicine, ATP Binding Cassette Transporter, Subfamily B, Cholangiocyte proliferation, Galanin, Article, Pathology and Forensic Medicine, Mice, 03 medical and health sciences, 0302 clinical medicine, Hepatic Stellate Cells, Animals, Receptor, Cell Proliferation, Mice, Knockout, Cholestasis, Chemistry, Liver cell, Epithelial Cells, Molecular biology, Receptor, Galanin, Type 1, Receptor, Galanin, Type 2, Disease Models, Animal, 030104 developmental biology, Liver, 030220 oncology & carcinogenesis, Knockout mouse, Hepatic stellate cell, Female, Bile Ducts, Hepatic fibrosis, Immunostaining
Abstract

Galanin (Gal) is a peptide with a role in neuroendocrine regulation of the liver. In this study, we assessed the role of Gal and its receptors, Gal receptor 1 (GalR1) and Gal receptor 2 (GalR2), in cholangiocyte proliferation and liver fibrosis in multidrug resistance protein 2 knockout (Mdr2KO) mice as a model of chronic hepatic cholestasis. The distribution of Gal, GalR1, and GalR2 in specific liver cell types was assessed by laser-capture microdissection and confocal microscopy. Galanin immunoreactivity was detected in cholangiocytes, hepatic stellate cells (HSCs), and hepatocytes. Cholangiocytes expressed GalR1, whereas HSCs and hepatocytes expressed GalR2. Strategies were used to either stimulate or block GalR1 and GalR2 in FVB/N (wild-type) and Mdr2KO mice and measure biliary hyperplasia and hepatic fibrosis by quantitative PCR and immunostaining of specific markers. Galanin treatment increased cholangiocyte proliferation and fibrogenesis in both FVB/N and Mdr2KO mice. Suppression of GalR1, GalR2, or both receptors in Mdr2KO mice resulted in reduced bile duct mass and hepatic fibrosis. In vitro knockdown of GalR1 in cholangiocytes reduced α-smooth muscle actin expression in LX-2 cells treated with cholangiocyte-conditioned media. A GalR2 antagonist inhibited HSC activation when Gal was administered directly to LX-2 cells, but not via cholangiocyte-conditioned media. These data demonstrate that Gal contributes not only to cholangiocyte proliferation but also to liver fibrogenesis via the coordinate activation of GalR1 in cholangiocytes and GalR2 in HSCs.

Published
2020

7. A CRITICAL REVIEW OF BILE ACIDS AND THEIR RECEPTORS IN HEPATIC ENCEPHALOPATHY

Author

Sharon DeMorrow, Elaina Williams, and Christopher Chu

Subjects
Pathology, medicine.medical_specialty, medicine.drug_class, Biophysics, Receptors, Cytoplasmic and Nuclear, Inflammation, Biochemistry, Article, Pathogenesis, Bile Acids and Salts, medicine, Animals, Humans, Receptor, Molecular Biology, Hepatic encephalopathy, Neuroinflammation, Bile acid, business.industry, Hyperammonemia, Cell Biology, medicine.disease, G protein-coupled bile acid receptor, Hepatic Encephalopathy, medicine.symptom, business
Abstract

Hepatic encephalopathy describes an array of neurological complications that arise due to liver insufficiency. The pathogenesis of hepatic encephalopathy shares a longstanding association with hyperammonemia and inflammation, and recently, aberrant bile acid signaling has been implicated in the development of key features of hepatic encephalopathy. These key features include neuronal dysfunction, neuroinflammation and blood-brain barrier permeability. This review summarizes the findings of recent studies demonstrating a role for bile acids in the pathogenesis of hepatic encephalopathy via one of three main bile acid receptors and speculates on the possible downstream consequences of aberrant bile acid signaling.

Published
2021

8. Glucocorticoids Cause Gender-Dependent Reversal of Hepatic Fibrosis in the MDR2-Knockout Mouse Model

Author

Anca D. Petrescu, Stephanie Grant, Gabriel Frampton, Jessica Kain, Karam Hadidi, Elaina Williams, Matthew McMillin, and Sharon DeMorrow

Subjects
hypothalamic-pituitary-adrenal (HPA) axis, corticosterone, glucocorticoid receptor, hepatic cholestasis, liver fibrosis, cholangiocytes, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Hepatic cholestasis is associated with a significant suppression of the hypothalamus-pituitary-adrenal axis (HPA). In the present study, we tested the hypothesis that activation of the HPA axis by corticosterone treatment can reverse liver inflammation and fibrosis in a multidrug resistance protein 2 knockout (MDR2KO) transgenic mouse model of hepatic cholestasis. Friend Virus B NIH-Jackson (FVBN) control and MDR2KO male and female mice were treated with vehicle or corticosterone for two weeks, then serum and liver analyses of hepatic cholestasis markers were performed. Indicators of inflammation, such as increased numbers of macrophages, were determined. MDR2KO mice had lower corticotropin releasing hormone and corticosterone levels than FVBN controls in the serum. There was a large accumulation of CD68 and F4/80 macrophages in MDR2KO mice livers, which indicated greater inflammation compared to FVBNs, an effect reversed by corticosterone treatment. Intrahepatic biliary duct mass, collagen deposition and alpha smooth muscle actin (αSMA) were found to be much higher in livers of MDR2KO mice than in controls; corticosterone treatment significantly decreased these fibrosis markers. When looking at the gender-specific response to corticosterone treatment, male MDR2KO mice tended to have a more pronounced reversal of liver fibrosis than females treated with corticosterone.

Published
2017
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9. Gulf War Illness‐related Chemicals Increase Hepatic Steatosis and Enhance Chronic Ethanol‐induced Liver Damage in Mice

Author

Ashok K. Shetty, Stephanie Grant, Sharon DeMorrow, Anca D. Petrescu, Suyeon An, Elaina Williams, and Laura K. Fonken

Subjects
medicine.medical_specialty, Ethanol, business.industry, medicine.disease, Gulf war, Biochemistry, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, Genetics, Medicine, Liver damage, Steatosis, business, Molecular Biology, Biotechnology
Published
2021

10. Leptin Enhances Hepatic Fibrosis and Inflammation in a Mouse Model of Cholestasis

Author

Stephanie Grant, Sharon DeMorrow, Anca D. Petrescu, Suyeon An, and Elaina Williams

Subjects
medicine.medical_specialty, business.industry, Leptin, Inflammation, medicine.disease, Biochemistry, Endocrinology, Cholestasis, Internal medicine, Genetics, medicine, medicine.symptom, Hepatic fibrosis, business, Molecular Biology, Biotechnology
Published
2021

14. Direct Comparison of the Thioacetamide and Azoxymethane Models of Type A Hepatic Encephalopathy in Mice

Author

Jessica Kain, Elaina Williams, Sharon DeMorrow, Anca D. Petrescu, Matthew McMillin, Gabriel Frampton, Stephanie Grant, and Victoria Jaeger

Subjects
Male, 0301 basic medicine, medicine.medical_specialty, medicine.drug_class, Azoxymethane, Thioacetamide, Article, Cerebral edema, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, Genetics, medicine, Animals, Molecular Biology, Hepatic encephalopathy, Neuroinflammation, Liver injury, Bile acid, business.industry, Brain, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Endocrinology, Liver, chemistry, Hepatic Encephalopathy, Toxicity, business, Biomarkers, 030217 neurology & neurosurgery
Abstract

Acute liver failure is a devastating consequence of hepatotoxic liver injury that can lead to the development of hepatic encephalopathy. There is no consensus on the best model to represent these syndromes in mice, and therefore the aim of this study was to classify hepatic and neurological consequences of azoxymethane- and thioacetamide-induced liver injury. Azoxymethane-treated mice were euthanized at time points representing absence of minor and significant stages of neurological decline. Thioacetamide-treated mice had tissue collected at up to 3 days following daily injections. Liver histology, serum chemistry, bile acids, and cytokine levels were measured. Reflexes, grip strength measurement, and ataxia were calculated for all groups. Brain ammonia, bile acid levels, cerebral edema, and neuroinflammation were measured. Finally, in vitro and in vivo assessments of blood‐brain barrier function were performed. Serum transaminases and liver histology demonstrate that both models generated hepatotoxic liver injury. Serum proinflammatory cytokine levels were significantly elevated in both models. Azoxymethane-treated mice had progressive neurological deficits, while thioacetamide-treated mice had inconsistent neurological deficits. Bile acids and cerebral edema were increased to a higher degree in azoxymethane-treated mice, while cerebral ammonia and neuroinflammation were greater in thioacetamide-treated mice. Blood‐brain barrier permeability exists in both models but was likely not due to direct toxicity of azoxymethane or thioacetamide on brain endothelial cells. In conclusion, both models generate acute liver injury and hepatic encephalopathy, but the requirement of a single injection and the more consistent neurological decline make azoxymethane treatment a better model for acute liver failure with hepatic encephalopathy.

Published
2018

15. FXR-Mediated Cortical Cholesterol Accumulation Contributes to the Pathogenesis of Type A Hepatic Encephalopathy

Author

Lauren Canady, Jessica Kain, Sharon DeMorrow, Elaina Williams, Gabriel Frampton, Stephanie Grant, Anca D. Petrescu, Matthew McMillin, and Rebecca Haines

Subjects
0301 basic medicine, medicine.medical_specialty, Morpholino, medicine.drug_class, Acute Liver Failure, Azoxymethane, Pathogenesis, 03 medical and health sciences, chemistry.chemical_compound, Internal medicine, medicine, lcsh:RC799-869, Hepatic encephalopathy, Farnesoid X Receptor, Hepatology, Bile acid, biology, business.industry, Cholesterol, Gastroenterology, Cytochrome P450, medicine.disease, Cytochrome p450 46A1, 030104 developmental biology, Endocrinology, chemistry, biology.protein, Farnesoid X receptor, lcsh:Diseases of the digestive system. Gastroenterology, business
Abstract

Background & Aims Hepatic encephalopathy is a serious neurologic complication of acute and chronic liver diseases. We previously showed that aberrant bile acid signaling contributes to the development of hepatic encephalopathy via farnesoid X receptor (FXR)-mediated mechanisms in neurons. In the brain, a novel alternative bile acid synthesis pathway, catalyzed by cytochrome p450 46A1 (Cyp46A1), is the primary mechanism by which the brain regulates cholesterol homeostasis. The aim of this study was to determine if FXR activation in the brain altered cholesterol homeostasis during hepatic encephalopathy. Methods Cyp7A1-/- mice or C57Bl/6 mice pretreated with central infusion of FXR vivo morpholino, 2-hydroxypropyl-β-cyclodextrin, or fed a cholestyramine-supplemented diet were injected with azoxymethane (AOM). Cognitive and neuromuscular impairment as well as liver damage and expression of Cyp46A1 were assessed using standard techniques. The subsequent cholesterol content in the frontal cortex was measured using commercially available kits and by Filipin III and Nile Red staining. Results There was an increase in membrane-bound and intracellular cholesterol in the cortex of mice treated with AOM that was associated with decreased Cyp46A1 expression. Strategies to inhibit FXR signaling prevented the down-regulation of Cyp46A1 and the accumulation of cholesterol. Treatment of mice with 2-hydroxypropyl-β-cyclodextrin attenuated the AOM-induced cholesterol accumulation in the brain and the cognitive and neuromuscular deficits without altering the underlying liver pathology. Conclusions During hepatic encephalopathy, FXR signaling increases brain cholesterol and contributes to neurologic decline. Targeting cholesterol accumulation in the brain may be a possible therapeutic target for the management of hepatic encephalopathy.

Published
2018

16. The TGFβ1 Receptor Antagonist GW788388 Reduces JNK Activation and Protects Against Acetaminophen Hepatotoxicity in Mice

Author

Matthew McMillin, Sharon DeMorrow, Gabriel Frampton, Stephanie Grant, Anca D. Petrescu, Brandi Jefferson, and Elaina Williams

Subjects
0301 basic medicine, Male, Necrosis, medicine.medical_treatment, Apoptosis, Pharmacology, Toxicology, medicine.disease_cause, Antioxidants, Mice, 0302 clinical medicine, Transforming Growth Factor beta, Medicine, Phosphorylation, Liver injury, biology, Cell Death, digestive, oral, and skin physiology, Glutathione, medicine.anatomical_structure, Cytokine, Liver, 030220 oncology & carcinogenesis, Hepatocyte, Benzamides, medicine.symptom, Chemical and Drug Induced Liver Injury, medicine.drug, Signal Transduction, Programmed cell death, Protective Agents, 03 medical and health sciences, Animals, Regeneration, Acetaminophen, Inflammation, business.industry, JNK Mitogen-Activated Protein Kinases, Transforming growth factor beta, Liver Failure, Acute, medicine.disease, Mice, Inbred C57BL, Oxidative Stress, 030104 developmental biology, Organ Specific Toxicology, biology.protein, Hepatocytes, Pyrazoles, business, Oxidative stress
Abstract

Acute liver failure is a serious consequence of acetaminophen (APAP)-induced hepatotoxic liver injury with high rates of morbidity and mortality. Transforming growth factor beta 1 (TGFβ1) is elevated during liver injury and influences hepatocyte senescence during APAP-induced hepatotoxicity. This study investigated TGFβ1 signaling in the context of inflammation, necrotic cell death, and oxidative stress during APAP-induced liver injury. Male C57Bl/6 mice were injected with 600 mg/kg APAP to generate liver injury in the presence or absence of the TGFβ receptor 1 inhibitor, GW788388, 1 h prior to APAP administration. Acetaminophen-induced liver injury was characterized using histological and biochemical measures. Transforming growth factor beta 1 expression and signal transduction were assessed using immunohistochemistry, Western blotting and ELISA assays. Hepatic necrosis, liver injury, cell proliferation, hepatic inflammation, and oxidative stress were assessed in all mice. Acetaminophen administration significantly induced necrosis and elevated serum transaminases compared with control mice. Transforming growth factor beta 1 staining was observed in and around areas of necrosis with phosphorylation of SMAD3 observed in hepatocytes neighboring necrotic areas in APAP-treated mice. Pretreatment with GW788388 prior to APAP administration in mice reduced hepatocyte cell death and stimulated regeneration. Phosphorylation of SMAD3 was reduced in APAP mice pretreated with GW788388 and this correlated with reduced hepatic cytokine production and oxidative stress. These results support that TGFβ1 signaling plays a significant role in APAP-induced liver injury by influencing necrotic cell death, inflammation, oxidative stress, and hepatocyte regeneration. In conclusion, targeting TGFβ1 or downstream signaling may be a possible therapeutic target for the management of APAP-induced liver injury.

Published
2019

17. Elevated circulating TGFβ1 during acute liver failure activates TGFβR2 on cortical neurons and exacerbates neuroinflammation and hepatic encephalopathy in mice

Author

Anca D. Petrescu, Ankita Brahmaroutu, Gabriel Frampton, Stephanie Grant, Sharon DeMorrow, Brandi Jefferson, Matthew McMillin, Elaina Williams, and Alison Thomas

Subjects
0301 basic medicine, Chemokine, Pyridines, Pharmacology, lcsh:RC346-429, Mice, 0302 clinical medicine, Neuroinflammation, Hepatic encephalopathy, Cell Line, Transformed, Cerebral Cortex, Neurons, Liver injury, Microglia, biology, General Neuroscience, Up-Regulation, 3. Good health, medicine.anatomical_structure, Liver, Neurology, Benzamides, Tumor necrosis factor alpha, Signal Transduction, Immunology, Azoxymethane, Mice, Transgenic, Antibodies, Transforming Growth Factor beta1, Necrosis, 03 medical and health sciences, Cellular and Molecular Neuroscience, Phagocytosis, medicine, Animals, Pyrroles, CX3CL1, lcsh:Neurology. Diseases of the nervous system, Inflammation, business.industry, Research, Receptor, Transforming Growth Factor-beta Type II, Transforming growth factor beta, Liver Failure, Acute, Isoquinolines, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Hepatic Encephalopathy, Carcinogens, biology.protein, Pyrazoles, business, Acute liver failure, 030217 neurology & neurosurgery
Abstract

Background Acute liver failure resulting from drug-induced liver injury can lead to the development of neurological complications called hepatic encephalopathy (HE). Hepatic transforming growth factor beta 1 (TGFβ1) is upregulated due to liver failure in mice and inhibiting circulating TGFβ reduced HE progression. However, the specific contributions of TGFβ1 on brain cell populations and neuroinflammation during HE are not known. Therefore, the aim of this study was to characterize hepatic and brain TGFβ1 signaling during acute liver failure and its contribution to HE progression using a combination of pharmacological and genetic approaches. Methods C57Bl/6 or neuron-specific transforming growth factor beta receptor 2 (TGFβR2) null mice (TGFβR2ΔNeu) were treated with azoxymethane (AOM) to induce acute liver failure and HE. The activity of circulating TGFβ1 was inhibited in C57Bl/6 mice via injection of a neutralizing antibody against TGFβ1 (anti-TGFβ1) prior to AOM injection. In all mouse treatment groups, liver damage, neuroinflammation, and neurological deficits were assessed. Inflammatory signaling between neurons and microglia were investigated in in vitro studies through the use of pharmacological inhibitors of TGFβ1 signaling in HT-22 and EOC-20 cells. Results TGFβ1 was expressed and upregulated in the liver following AOM injection. Pharmacological inhibition of TGFβ1 after AOM injection attenuated neurological decline, microglia activation, and neuroinflammation with no significant changes in liver damage. TGFβR2ΔNeu mice administered AOM showed no effect on liver pathology but significantly reduced neurological decline compared to control mice. Microglia activation and neuroinflammation were attenuated in mice with pharmacological inhibition of TGFβ1 or in TGFβR2ΔNeu mice. TGFβ1 increased chemokine ligand 2 (CCL2) and decreased C-X3-C motif ligand 1 (CX3CL1) expression in HT-22 cells and reduced interleukin-1 beta (IL-1ß) expression, tumor necrosis factor alpha (TNFα) expression, and phagocytosis activity in EOC-20 cells. Conclusion Increased circulating TGFβ1 following acute liver failure results in activation of neuronal TGFβR2 signaling, driving neuroinflammation and neurological decline during AOM-induced HE. Electronic supplementary material The online version of this article (10.1186/s12974-019-1455-y) contains supplementary material, which is available to authorized users.

Published
2019

21. Glucocorticoids Cause Gender-Dependent Reversal of Hepatic Fibrosis in the MDR2-Knockout Mouse Model

Author

Gabriel Frampton, Stephanie Grant, Elaina Williams, Jessica Kain, Matthew McMillin, Anca D. Petrescu, Karam Hadidi, and Sharon DeMorrow

Subjects
Liver Cirrhosis, Male, 0301 basic medicine, Corticotropin-Releasing Hormone, Pituitary-Adrenal System, lcsh:Chemistry, Mice, chemistry.chemical_compound, Corticotropin-releasing hormone, 0302 clinical medicine, Fibrosis, Corticosterone, glucocorticoid receptor, lcsh:QH301-705.5, Spectroscopy, liver fibrosis, Mice, Knockout, Sex Characteristics, hepatic cholestasis, hypothalamic-pituitary-adrenal (HPA) axis, corticosterone, cholangiocytes, General Medicine, 3. Good health, Computer Science Applications, Liver, Knockout mouse, Female, 030211 gastroenterology & hepatology, medicine.symptom, Genetically modified mouse, Hypothalamo-Hypophyseal System, medicine.medical_specialty, ATP Binding Cassette Transporter, Subfamily B, Inflammation, Biology, Article, Catalysis, Inorganic Chemistry, 03 medical and health sciences, Cholestasis, Internal medicine, medicine, Animals, Physical and Theoretical Chemistry, Glucocorticoids, Molecular Biology, Organic Chemistry, medicine.disease, 030104 developmental biology, Endocrinology, chemistry, lcsh:Biology (General), lcsh:QD1-999, Hepatic fibrosis
Abstract

Hepatic cholestasis is associated with a significant suppression of the hypothalamus-pituitary-adrenal axis (HPA). In the present study, we tested the hypothesis that activation of the HPA axis by corticosterone treatment can reverse liver inflammation and fibrosis in a multidrug resistance protein 2 knockout (MDR2KO) transgenic mouse model of hepatic cholestasis. Friend Virus B NIH-Jackson (FVBN) control and MDR2KO male and female mice were treated with vehicle or corticosterone for two weeks, then serum and liver analyses of hepatic cholestasis markers were performed. Indicators of inflammation, such as increased numbers of macrophages, were determined. MDR2KO mice had lower corticotropin releasing hormone and corticosterone levels than FVBN controls in the serum. There was a large accumulation of CD68 and F4/80 macrophages in MDR2KO mice livers, which indicated greater inflammation compared to FVBNs, an effect reversed by corticosterone treatment. Intrahepatic biliary duct mass, collagen deposition and alpha smooth muscle actin (αSMA) were found to be much higher in livers of MDR2KO mice than in controls; corticosterone treatment significantly decreased these fibrosis markers. When looking at the gender-specific response to corticosterone treatment, male MDR2KO mice tended to have a more pronounced reversal of liver fibrosis than females treated with corticosterone.

Published
2017

22. Sa1519 – Neuronal Ablation of Fxr Signaling Attenuates the Dysregulation of Galanin and Neuropeptide Y Resulting in Improved Liver Pathology During Cholestasis

Author

Matthew McMillin, Elaina Williams, Gabriel Frampton, Sharon DeMorrow, Stephanie Grant, Marcus Davis, Anca D. Petrescu, and Hanna Blaney

Subjects
medicine.medical_specialty, Hepatology, business.industry, medicine.medical_treatment, Gastroenterology, medicine.disease, Ablation, Neuropeptide Y receptor, Endocrinology, Cholestasis, Internal medicine, medicine, Galanin, business, Liver pathology
Published
2019

23. 576 – Let-7F Expression is Upregulated in the Frontal Cortex During Acute Liver Failure and Contributes to Hepatic Encephalopathy Via Downregulation of Igf1 Expression

Author

Marcus Davis, Elaina Williams, Matthew McMillin, Anca D. Petrescu, Sharon DeMorrow, Gabriel Frampton, Stephanie Grant, and Hanna Blaney

Subjects
medicine.medical_specialty, Endocrinology, Frontal cortex, Hepatology, Downregulation and upregulation, business.industry, Internal medicine, Gastroenterology, Liver failure, Medicine, business, medicine.disease, Hepatic encephalopathy
Published
2019

24. Sa1522 – Galanin Enhances Hepatic Fibrosis in Mdr2 Knockout Mice Via Co-Ordinate Activation of Galanin Receptors on Cholangiocytes and Hepatic Stellate Cells

Author

Sharon DeMorrow, Elaina Williams, Matthew McMillin, Gabriel Frampton, Stephanie Grant, Anca D. Petrescu, Hanna Blaney, Marcus Davis, and Natalie Parks

Subjects
medicine.medical_specialty, Endocrinology, Hepatology, Chemistry, Co ordinate, Internal medicine, Knockout mouse, Gastroenterology, medicine, Hepatic stellate cell, Galanin, Hepatic fibrosis, Receptor
Published
2019

26. Direct Comparison of the Thioacetamide and Azoxymethane Models of Type A Hepatic Encephalopathy in Mice.

Author

Grant, Stephanie, McMillin, Matthew, Frampton, Gabriel, Petrescu, Anca D., Williams, Elaina, Jaeger, Victoria, Kain, Jessica, and DeMorrow, Sharon

Subjects
THIOACETAMIDE, HEPATIC encephalopathy, LABORATORY mice, LIVER failure, HEPATOTOXICOLOGY, ANIMAL models in research
Abstract

Acute liver failure is a devastating consequence of hepatotoxic liver injury that can lead to the development of hepatic encephalopathy. There is no consensus on the best model to represent these syndromes in mice, and therefore the aim of this study was to classify hepatic and neurological consequences of azoxymethane- and thioacetamide-induced liver injury. Azoxymethane-treated mice were euthanized at time points representing absence of minor and significant stages of neurological decline. Thioacetamide-treated mice had tissue collected at up to 3 days following daily injections. Liver histology, serum chemistry, bile acids, and cytokine levels were measured. Reflexes, grip strength measurement, and ataxia were calculated for all groups. Brain ammonia, bile acid levels, cerebral edema, and neuroinflammation were measured. Finally, in vitro and in vivo assessments of blood-brain barrier function were performed. Serum transaminases and liver histology demonstrate that both models generated hepatotoxic liver injury. Serum proinflammatory cytokine levels were significantly elevated in both models. Azoxymethane-treated mice had progressive neurological deficits, while thioacetamide-treated mice had inconsistent neurological deficits. Bile acids and cerebral edema were increased to a higher degree in azoxymethane-treated mice, while cerebral ammonia and neuroinflammation were greater in thioacetamide-treated mice. Blood-brain barrier permeability exists in both models but was likely not due to direct toxicity of azoxymethane or thioacetamide on brain endothelial cells. In conclusion, both models generate acute liver injury and hepatic encephalopathy, but the requirement of a single injection and the more consistent neurological decline make azoxymethane treatment a better model for acute liver failure with hepatic encephalopathy. [ABSTRACT FROM AUTHOR]

Published
2018
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27. Glucocorticoids Cause Gender-Dependent Reversal of Hepatic Fibrosis in the MDR2-Knockout Mouse Model.

Author

Petrescu, Anca D., Grant, Stephanie, Frampton, Gabriel, Kain, Jessica, Hadidi, Karam, Williams, Elaina, McMillin, Matthew, and DeMorrow, Sharon

Subjects
GLUCOCORTICOIDS, HEPATIC fibrosis, TRANSGENIC mice, LIVER, INFLAMMATION
Abstract

Hepatic cholestasis is associated with a significant suppression of the hypothalamuspituitary- adrenal axis (HPA). In the present study, we tested the hypothesis that activation of the HPA axis by corticosterone treatment can reverse liver inflammation and fibrosis in a multidrug resistance protein 2 knockout (MDR2KO) transgenic mouse model of hepatic cholestasis. Friend Virus B NIH-Jackson (FVBN) control and MDR2KO male and female mice were treated with vehicle or corticosterone for two weeks, then serum and liver analyses of hepatic cholestasis markers were performed. Indicators of inflammation, such as increased numbers of macrophages, were determined. MDR2KO mice had lower corticotropin releasing hormone and corticosterone levels than FVBN controls in the serum. There was a large accumulation of CD68 and F4/80 macrophages in MDR2KO mice livers, which indicated greater inflammation compared to FVBNs, an effect reversed by corticosterone treatment. Intrahepatic biliary duct mass, collagen deposition and alpha smooth muscle actin (αSMA) were found to be much higher in livers of MDR2KO mice than in controls; corticosterone treatment significantly decreased these fibrosis markers. When looking at the gender-specific response to corticosterone treatment, male MDR2KO mice tended to have a more pronounced reversal of liver fibrosis than females treated with corticosterone. [ABSTRACT FROM AUTHOR]

Published
2017
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28. Ghrelin reverses ductular reaction and hepatic fibrosis in a rodent model of cholestasis.

Author

Petrescu, Anca D., Grant, Stephanie, Williams, Elaina, Frampton, Gabriel, Reinhart, Evan H., Nguyen, Amy, An, Suyeon, McMillin, Matthew, and DeMorrow, Sharon

Subjects
CHOLESTASIS, HEPATIC fibrosis, HYPOTHALAMUS, SOMATOTROPIN, HYPERPLASIA
Abstract

The orexigenic peptide ghrelin (Ghr) stimulates hunger signals in the hypothalamus via growth hormone secretagogue receptor (GHS-R1a). Gastric Ghr is synthetized as a preprohormone which is proteolytically cleaved, and acylated by a membrane-bound acyl transferase (MBOAT). Circulating Ghr is reduced in cholestatic injuries, however Ghr's role in cholestasis is poorly understood. We investigated Ghr's effects on biliary hyperplasia and hepatic fibrosis in Mdr2-knockout (Mdr2KO) mice, a recognized model of cholestasis. Serum, stomach and liver were collected from Mdr2KO and FVBN control mice treated with Ghr, des-octanoyl-ghrelin (DG) or vehicle. Mdr2KO mice had lower expression of Ghr and MBOAT in the stomach, and lower levels of circulating Ghr compared to WT-controls. Treatment of Mdr2KO mice with Ghr improved plasma transaminases, reduced biliary and fibrosis markers. In the liver, GHS-R1a mRNA was expressed predominantly in cholangiocytes. Ghr but not DG, decreased cell proliferation via AMPK activation in cholangiocytes in vitro. AMPK inhibitors prevented Ghr-induced FOXO1 nuclear translocation and negative regulation of cell proliferation. Ghr treatment reduced ductular reaction and hepatic fibrosis in Mdr2KO mice, regulating cholangiocyte proliferation via GHS-R1a, a G-protein coupled receptor which causes increased intracellular Ca2+ and activation of AMPK and FOXO1, maintaining a low rate of cholangiocyte proliferation. [ABSTRACT FROM AUTHOR]

Published
2020
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29. Elevated circulating TGFβ1 during acute liver failure activates TGFβR2 on cortical neurons and exacerbates neuroinflammation and hepatic encephalopathy in mice.

Author

Jefferson, Brandi, McMillin, Matthew, Frampton, Gabriel, Grant, Stephanie, Petrescu, Anca D., Williams, Elaina, DeMorrow, Sharon, Thomas, Alison, and Brahmaroutu, Ankita

Subjects
HEPATIC encephalopathy, LIVER failure, TRANSFORMING growth factors-beta, TUMOR necrosis factors, HYDROXYETHYL starch, NEURONS
Abstract

Background: Acute liver failure resulting from drug-induced liver injury can lead to the development of neurological complications called hepatic encephalopathy (HE). Hepatic transforming growth factor beta 1 (TGFβ1) is upregulated due to liver failure in mice and inhibiting circulating TGFβ reduced HE progression. However, the specific contributions of TGFβ1 on brain cell populations and neuroinflammation during HE are not known. Therefore, the aim of this study was to characterize hepatic and brain TGFβ1 signaling during acute liver failure and its contribution to HE progression using a combination of pharmacological and genetic approaches.Methods: C57Bl/6 or neuron-specific transforming growth factor beta receptor 2 (TGFβR2) null mice (TGFβR2ΔNeu) were treated with azoxymethane (AOM) to induce acute liver failure and HE. The activity of circulating TGFβ1 was inhibited in C57Bl/6 mice via injection of a neutralizing antibody against TGFβ1 (anti-TGFβ1) prior to AOM injection. In all mouse treatment groups, liver damage, neuroinflammation, and neurological deficits were assessed. Inflammatory signaling between neurons and microglia were investigated in in vitro studies through the use of pharmacological inhibitors of TGFβ1 signaling in HT-22 and EOC-20 cells.Results: TGFβ1 was expressed and upregulated in the liver following AOM injection. Pharmacological inhibition of TGFβ1 after AOM injection attenuated neurological decline, microglia activation, and neuroinflammation with no significant changes in liver damage. TGFβR2ΔNeu mice administered AOM showed no effect on liver pathology but significantly reduced neurological decline compared to control mice. Microglia activation and neuroinflammation were attenuated in mice with pharmacological inhibition of TGFβ1 or in TGFβR2ΔNeu mice. TGFβ1 increased chemokine ligand 2 (CCL2) and decreased C-X3-C motif ligand 1 (CX3CL1) expression in HT-22 cells and reduced interleukin-1 beta (IL-1ß) expression, tumor necrosis factor alpha (TNFα) expression, and phagocytosis activity in EOC-20 cells.Conclusion: Increased circulating TGFβ1 following acute liver failure results in activation of neuronal TGFβR2 signaling, driving neuroinflammation and neurological decline during AOM-induced HE. [ABSTRACT FROM AUTHOR]

Published
2019
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31. Cobra Pose

Subjects
Global economy, Yoga, Library and information science, Publishing industry
Abstract

Cobra Pose Susan Rogers and John Roosen G-EMS PTY LTD and PS LLC 9780645413625, $6.99 ebook https://www.amazon.com/Cobra-Pose-Mysteries-suspense-adventure-ebook/dp/B0BTJV4V1H Cobra Pose, the second book in the Yoga Mat Mysteries series, benefits from [...]

Published
2023

32. Data on Liver Fibrosis Detailed by Researchers at Central Texas Veterans Health Care System (Coordinated Targeting of Galanin Receptors On Cholangiocytes and Hepatic Stellate Cells Ameliorates Liver Fibrosis In Multidrug Resistance Protein 2 ...)

Subjects
Medical research, Medicine, Experimental, Fibrosis, Drug resistance in microorganisms, Liver, Neuropeptides, Liver diseases, Health
Abstract

2021 APR 19 (NewsRx) -- By a News Reporter-Staff News Editor at Gastroenterology Week -- New research on Liver Diseases and Conditions - Liver Fibrosis is the subject of a [...]

Published
2021

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