Your search keyword '"Gabriel Frampton"' showing total 96 results

1. Generating Shigella that internalize into glioblastoma cells

Author

Austin Shipley, Gabriel Frampton, Bryan W. Davies, and Benjamin J. Umlauf

Subjects

Shigella, glioblastoma, drug delivery, microbial factories, myristoylation, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

IntroductionThe use of microorganisms as drug delivery systems to treat cancer has expanded recently, including FDA approval of certain viruses as oncolytics. Microorganisms have several unique benefits compared to traditional pharmacologic agents including dose independence, the ability to produce therapeutic proteins locally within the tumor, and simplicity of administration. However, current microbial delivery systems such as AAV9 and herpes virus have limited cassette sizes, minimal cancer cell selectivity, and low innate cytotoxicity. To address these issues, we sought to generate a strain of Shigella flexneri to selectively internalize into glioblastoma (GBM) brain tumor cells as an initial step to generating a bacterial-based drug delivery system.MethodsWe generated S. flexneri that selectively internalize into GBM cells using iterative co-cultured assays.ResultsAfter 50 rounds of co-culture, the new strain infected 95 percent of GBM cells in 2 hours. GBM-infecting Shigella demonstrate a 124-fold preference for internalizing in nine different GBM cell lines compared to Normal Astrocytes (NA) controls. Additionally, we developed an in-cell western to identify GBM-infecting Shigella clones that preferentially internalize in patient samples without iterative co-culture. Finally, we demonstrate internalization into GBM cells is mediated via a factor modified by myristoylation.DiscussionIn conclusion, here we present a novel bacterial platform that preferentially internalizes in brain tumor cells. This system provides numerous potential benefits over current interventions and other microbial strategies for treating brain tumors.

Published

2023

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

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

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

5. Bile Acid-Mediated Sphingosine-1-Phosphate Receptor 2 Signaling Promotes Neuroinflammation during Hepatic Encephalopathy in Mice

Author

Matthew McMillin, Gabriel Frampton, Stephanie Grant, Shamyal Khan, Juan Diocares, Anca Petrescu, Amy Wyatt, Jessica Kain, Brandi Jefferson, and Sharon DeMorrow

Subjects

microglia, cytokines, CCL2, acute liver failure, neurons, S1PR2, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Hepatic encephalopathy (HE) is a neuropsychiatric complication that occurs due to deteriorating hepatic function and this syndrome influences patient quality of life, clinical management strategies and survival. During acute liver failure, circulating bile acids increase due to a disruption of the enterohepatic circulation. We previously identified that bile acid-mediated signaling occurs in the brain during HE and contributes to cognitive impairment. However, the influences of bile acids and their downstream signaling pathways on HE-induced neuroinflammation have not been assessed. Conjugated bile acids, such as taurocholic acid (TCA), can activate sphingosine-1-phosphate receptor 2 (S1PR2), which has been shown to promote immune cell infiltration and inflammation in other models. The current study aimed to assess the role of bile-acid mediated S1PR2 signaling in neuroinflammation and disease progression during azoxymethane (AOM)-induced HE in mice. Our findings demonstrate a temporal increase of bile acids in the cortex during AOM-induced HE and identified that cortical bile acids were elevated as an early event in this model. In order to classify the specific bile acids that were elevated during HE, a metabolic screen was performed and this assay identified that TCA was increased in the serum and cortex during AOM-induced HE. To reduce bile acid concentrations in the brain, mice were fed a diet supplemented with cholestyramine, which alleviated neuroinflammation by reducing proinflammatory cytokine expression in the cortex compared to the control diet-fed AOM-treated mice. S1PR2 was expressed primarily in neurons and TCA treatment increased chemokine ligand 2 mRNA expression in these cells. The infusion of JTE-013, a S1PR2 antagonist, into the lateral ventricle prior to AOM injection protected against neurological decline and reduced neuroinflammation compared to DMSO-infused AOM-treated mice. Together, this identifies that reducing bile acid levels or S1PR2 signaling are potential therapeutic strategies for the management of HE.

Published

2017

6. 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

7. Supplementary Table 1 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Author

Sharon DeMorrow, Antonio Benedetti, Marco Marzioni, Sum P. Lee, Domenico Alvaro, Gabriel Frampton, Monique Coufal, Antonio Franchitto, Paolo Onori, Francesca Bernuzzi, Shelley Kopriva, Julie Venter, Eugenio Gaudio, Pietro Invernizzi, and Gianfranco Alpini

Abstract

Supplementary Table 1 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Published

2023

8. Supplementary Figure 5 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Author

Sharon DeMorrow, Antonio Benedetti, Marco Marzioni, Sum P. Lee, Domenico Alvaro, Gabriel Frampton, Monique Coufal, Antonio Franchitto, Paolo Onori, Francesca Bernuzzi, Shelley Kopriva, Julie Venter, Eugenio Gaudio, Pietro Invernizzi, and Gianfranco Alpini

Abstract

Supplementary Figure 5 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Published

2023

9. Supplementary Figure 1 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Author

Sharon DeMorrow, Antonio Benedetti, Marco Marzioni, Sum P. Lee, Domenico Alvaro, Gabriel Frampton, Monique Coufal, Antonio Franchitto, Paolo Onori, Francesca Bernuzzi, Shelley Kopriva, Julie Venter, Eugenio Gaudio, Pietro Invernizzi, and Gianfranco Alpini

Abstract

Supplementary Figure 1 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Published

2023

10. Supplementary Figure 2 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Author

Sharon DeMorrow, Antonio Benedetti, Marco Marzioni, Sum P. Lee, Domenico Alvaro, Gabriel Frampton, Monique Coufal, Antonio Franchitto, Paolo Onori, Francesca Bernuzzi, Shelley Kopriva, Julie Venter, Eugenio Gaudio, Pietro Invernizzi, and Gianfranco Alpini

Abstract

Supplementary Figure 2 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Published

2023

11. Supplementary Figure Legends 1-5 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Author

Sharon DeMorrow, Antonio Benedetti, Marco Marzioni, Sum P. Lee, Domenico Alvaro, Gabriel Frampton, Monique Coufal, Antonio Franchitto, Paolo Onori, Francesca Bernuzzi, Shelley Kopriva, Julie Venter, Eugenio Gaudio, Pietro Invernizzi, and Gianfranco Alpini

Abstract

Supplementary Figure Legends 1-5 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Published

2023

12. Supplementary Figure 3 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Author

Sharon DeMorrow, Antonio Benedetti, Marco Marzioni, Sum P. Lee, Domenico Alvaro, Gabriel Frampton, Monique Coufal, Antonio Franchitto, Paolo Onori, Francesca Bernuzzi, Shelley Kopriva, Julie Venter, Eugenio Gaudio, Pietro Invernizzi, and Gianfranco Alpini

Abstract

Supplementary Figure 3 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Published

2023

13. Supplementary Figure 4 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Author

Sharon DeMorrow, Antonio Benedetti, Marco Marzioni, Sum P. Lee, Domenico Alvaro, Gabriel Frampton, Monique Coufal, Antonio Franchitto, Paolo Onori, Francesca Bernuzzi, Shelley Kopriva, Julie Venter, Eugenio Gaudio, Pietro Invernizzi, and Gianfranco Alpini

Abstract

Supplementary Figure 4 from Serotonin Metabolism Is Dysregulated in Cholangiocarcinoma, which Has Implications for Tumor Growth

Published

2023

14. 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

15. Characterization of Hepatic Injury During the Azoxymethane Model of Acute Liver Failure

Author

Matthew McMillin, Ashwin Jhawer, Gabriel Frampton, Shadikchhya M. Bhattarai, and Eleonora Troyanovskaya

Subjects

Genetics, Molecular Biology, Biochemistry, Biotechnology

Published

2022

16. LPS‐induced endotoxemia promotes blood‐brain barrier permeability via TSP1‐dependent TGFβ1 activation

Author

Shadikchhya M. Bhattarai, Gabriel Frampton, Ashwin Jhawer, Eleonora Troyanovskaya, and Matthew McMillin

Subjects

Genetics, Molecular Biology, Biochemistry, Biotechnology

Published

2022

17. 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

18. Thrombospondin-1 Exacerbates Acute Liver Failure and Hepatic Encephalopathy Pathology in Mice by Activating Transforming Growth Factor β1

Author

Sarah Andry, Malaika Ali, Michaela Ploof, Brandi Jefferson, Gabriel Frampton, Matthew McMillin, Stephanie Grant, and Sharon DeMorrow

Subjects

0301 basic medicine, endocrine system, medicine.medical_specialty, Azoxymethane, Caspase 3, Article, Pathology and Forensic Medicine, Cerebral edema, Thrombospondin 1, Transforming Growth Factor beta1, Pathogenesis, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, immune system diseases, Internal medicine, otorhinolaryngologic diseases, Animals, Medicine, Hepatic encephalopathy, Mice, Knockout, Liver injury, Cell Death, business.industry, virus diseases, Liver Failure, Acute, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Endocrinology, chemistry, Hepatic Encephalopathy, Carcinogens, Hepatic stellate cell, business, 030217 neurology & neurosurgery, Signal Transduction, Transforming growth factor

Abstract

Severe hepatic insults can lead to acute liver failure and hepatic encephalopathy (HE). Transforming growth factor β1 (TGFβ1) has been shown to contribute to HE during acute liver failure; however, TGFβ1 must be activated to bind its receptor and generate downstream effects. One protein that can activate TGFβ1 is thrombospondin-1 (TSP-1). Therefore, the aim of this study was to assess TSP-1 during acute liver failure and HE pathogenesis. C57Bl/6 or TSP-1 knockout (TSP-1(−/−)) mice were injected with azoxymethane (AOM) to induce acute liver failure and HE. Liver damage, neurologic decline, and molecular analyses of TSP-1 and TGFβ1 signaling were performed. AOM-treated mice had increased TSP-1 and TGFβ1 mRNA and protein expression in the liver. TSP-1(−/−) mice administered AOM had reduced liver injury as assessed by histology and serum transaminase levels compared with C57Bl/6 AOM-treated mice. TSP-1(−/−) mice treated with AOM had reduced TGFβ1 signaling that was associated with less hepatic cell death as assessed by terminal deoxynucleotidyl transferase-mediated dUTP nick-end labeling staining and cleaved caspase 3 expression. TSP-1(−/−) AOM-treated mice had a reduced rate of neurologic decline, less cerebral edema, and a decrease in microglia activation in comparison with C57Bl/6 mice treated with AOM. Taken together, TSP-1 is an activator of TGFβ1 signaling during AOM-induced acute liver failure and contributes to both liver pathology and HE progression.

Published

2020

19. Thrombospondin‐1 Inhibition Reduces Nrf2 Activity and Increases Liver Injury during Acetaminophen‐Induced Hepatotoxicity

Author

Matthew McMillin and Gabriel Frampton

Subjects

Liver injury, business.industry, Thrombospondin 1, Genetics, medicine, Pharmacology, business, medicine.disease, Molecular Biology, Biochemistry, Biotechnology, Acetaminophen, medicine.drug

Published

2021

20. Inhibition of thrombospondin-1 reduces glutathione activity and worsens acute liver injury during acetaminophen hepatotoxicity in mice

Author

Matthew McMillin, Malaika Ali, Durreshahwar Khan, Brandi Jefferson, Priyanka Reddy, and Gabriel Frampton

Subjects

0301 basic medicine, Programmed cell death, NF-E2-Related Factor 2, SMAD, Pharmacology, Toxicology, medicine.disease_cause, Article, Antioxidants, Thrombospondin 1, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, medicine, Animals, Phosphorylation, Acetaminophen, Liver injury, Cell Death, Chemistry, digestive, oral, and skin physiology, Glutathione, Liver Failure, Acute, medicine.disease, Liver regeneration, Liver Regeneration, Mice, Inbred C57BL, Oxidative Stress, 030104 developmental biology, medicine.anatomical_structure, Liver, 030220 oncology & carcinogenesis, Hepatocyte, Hepatocytes, Chemical and Drug Induced Liver Injury, Reactive Oxygen Species, Oxidative stress, medicine.drug, Signal Transduction

Abstract

Acetaminophen (N-Acetyl-p-Aminophenol or APAP)-induced hepatotoxicity is the most common cause of acute liver failure in the United States and Western Europe. Previous studies have shown that TGFβ1 is elevated during APAP-induced hepatotoxicity and promotes liver injury by reducing liver regeneration while inducing hepatocyte senescence. At this time, little is known about the role of proteins that activate latent TGFβ1 and their effects during APAP-induced hepatotoxicity. Thrombospondin-1 (TSP1) is a homotrimeric protein that can not only activate latent TGFβ1 but can also interact with other proteins including Nrf2 to induce antioxidant signaling. The aim of the current study was to assess the role of thrombospondin-1 (TSP1) in both TGFβ1 activation and its contribution to APAP-induced liver injury. C57Bl/6 mice or TSP1 null mice (TSP1−/−) were administered 300 mg/kg or 600 mg/kg of APAP. TGFβ1 signaling, TSP1 expression, measures of hepatic injury, Nrf2 expression, measures of oxidative/nitrosative stress and GSH metabolism were assessed. The expression of TGFβ1, TSP1 and phosphorylation of SMAD proteins increased in APAP-treated mice compared to controls. TSP1−/− mice had reduced TGFβ1 expression and phosphorylation of SMAD proteins but increased liver injury. Hepatocyte cell death was increased in TSP1−/− mice and this was associated with decreased Nrf2 activity, decreased GSH levels and increased oxidative stress in comparison to wild-type C57Bl/6 mice. Together, these data demonstrate that elimination of TSP1 protein in APAP-treated mice reduces TGFβ1 signaling but leads to increased liver injury by reducing Nrf2 expression and GSH activity, ultimately resulting in increased cell death.

Published

2020

21. Gulf war illness-related chemicals increase CD11b/c+ monocyte infiltration into the liver and aggravate hepatic cholestasis in a rodent model

Author

Jessica Kain, Anca D. Petrescu, Sharon DeMorrow, Ashok K. Shetty, Maheedhar Kodali, Gabriel Frampton, Stephanie Grant, and Matthew McMillin

Subjects

0301 basic medicine, medicine.medical_specialty, lcsh:Medicine, Inflammation, Systemic inflammation, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Cholestasis, Internal medicine, medicine, lcsh:Science, Multidisciplinary, business.industry, Biliary hyperplasia, Monocyte, lcsh:R, medicine.disease, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, lcsh:Q, medicine.symptom, Ligation, business, Hepatic fibrosis, Infiltration (medical), 030217 neurology & neurosurgery

Abstract

Gulf War Illness (GWI) is a chronic multisymptom disorder affecting veterans of the 1990–91 Gulf war. GWI was linked with exposure to chemicals including the nerve gas prophylactic drug pyridostigmine-bromide (PB) and pesticides (DEET, permethrin). Veterans with GWI exhibit prolonged, low-level systemic inflammation, though whether this impacts the liver is unknown. While no evidence exists that GWI-related chemicals are hepatotoxic, the prolonged inflammation may alter the liver’s response to insults such as cholestatic injury. We assessed the effects of GWI-related chemicals on macrophage infiltration and its subsequent influence on hepatic cholestasis. Sprague Dawley rats were treated daily with PB, DEET and permethrin followed by 15 minutes of restraint stress for 28 days. Ten weeks afterward, GWI rats or naïve age-matched controls underwent bile duct ligation (BDL) or sham surgeries. Exposure to GWI-related chemicals alone increased IL-6, and CD11b+F4/80− macrophages in the liver, with no effect on biliary mass or hepatic fibrosis. However, pre-exposure to GWI-related chemicals enhanced biliary hyperplasia and fibrogenesis caused by BDL, compared to naïve rats undergoing the same surgery. These data suggest that GWI patients could be predisposed to developing worse liver pathology due to sustained low-level inflammation of the liver when compared to patients without GWI.

Published

2018

22. 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

23. 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

24. The Neuropeptide Galanin Is Up-Regulated during Cholestasis and Contributes to Cholangiocyte Proliferation

Author

Matthew McMillin, Gabriel Frampton, Stephanie Grant, and Sharon DeMorrow

Subjects

Male, 0301 basic medicine, CAMP Responsive Element Binding Protein, medicine.medical_specialty, Cholangiocyte proliferation, Neuropeptide, Galanin, Biology, Cell Line, Morpholinos, Pathology and Forensic Medicine, Rats, Sprague-Dawley, Mice, 03 medical and health sciences, Internal medicine, medicine, Animals, Phosphorylation, Cyclic AMP Response Element-Binding Protein, Ligation, Cell Proliferation, Inflammation, Cholestasis, Kinase, Biliary hyperplasia, Regular Article, YAP-Signaling Proteins, DNA, Up-Regulation, 030104 developmental biology, Endocrinology, Bile Ducts, Signal transduction, Apoptosis Regulatory Proteins, Receptors, Galanin, Biomarkers, Signal Transduction, Galanin receptor 1

Abstract

During the course of cholestatic liver diseases, mitotically dormant cholangiocytes proliferate and subsequently acquire a neuroendocrine phenotype. Galanin is a neuroendocrine factor responsible for regulation of physiological responses, such as feeding behavior and mood, and has been implicated in the development of fatty liver disease, although its role in biliary hyperplasia is unknown. Biliary hyperplasia was induced in rats via bile duct ligation (BDL) surgery, and galanin was increased in serum and liver homogenates from BDL rats. Treatment of sham and BDL rats with recombinant galanin increased cholangiocyte proliferation and intrahepatic biliary mass, liver damage, and inflammation, whereas blocking galanin expression with specific vivo-morpholino sequences inhibited hyperplastic cholangiocyte proliferation, liver damage, inflammation, and subsequent fibrosis. The proliferative effects of galanin were via activation of galanin receptor 1 expressed specifically on cholangiocytes and were associated with an activation of extracellular signal-regulated kinase 1/2, and ribosomal S6 kinase 1 signal transduction pathways and subsequent increase in cAMP responsive element binding protein DNA-binding activity and induction of Yes-associated protein expression. Strategies to inhibit extracellular signal-regulated kinase 1/2, ribosomal S6 kinase 1, or cAMP responsive element binding protein DNA-binding activity prevented the proliferative effects of galanin. Taken together, these data suggest that targeting galanin signaling may be effective for the maintenance of biliary mass during cholestatic liver diseases.

Published

2017

25. 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

26. 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

27. Neuron‐specific knockout of FXR attenuates the neurological complications of chronic liver disease

Author

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

Subjects

Pathology, medicine.medical_specialty, medicine.anatomical_structure, business.industry, Genetics, medicine, Neuron, Chronic liver disease, medicine.disease, business, Molecular Biology, Biochemistry, Biotechnology

Published

2019

28. Suppression of the HPA Axis During Cholestasis Can Be Attributed to Hypothalamic Bile Acid Signaling

Author

Nisha S Patel, Sharon DeMorrow, Gabriel Frampton, Stephanie Grant, Matthew McMillin, Karen Newell-Rogers, Matthew A. Quinn, and Ali Divan

Subjects

Male, Hypothalamo-Hypophyseal System, endocrine system, medicine.medical_specialty, Corticotropin-Releasing Hormone, medicine.drug_class, Cholestyramine Resin, Hypothalamus, Pituitary-Adrenal System, Biology, Bile Acids and Salts, Rats, Sprague-Dawley, chemistry.chemical_compound, Corticotropin-releasing hormone, Endocrinology, Glucocorticoid receptor, Cholestasis, Bile acid sequestrant, Internal medicine, medicine, Glycochenodeoxycholic acid, Animals, Molecular Biology, Original Research, Cholestyramine, Bile acid, General Medicine, Taurocholic acid, medicine.disease, Rats, chemistry, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

Suppression of the hypothalamic-pituitary-adrenal (HPA) axis has been shown to occur during cholestatic liver injury. Furthermore, we have demonstrated that in a model of cholestasis, serum bile acids gain entry into the brain via a leaky blood brain barrier and that hypothalamic bile acid content is increased. Therefore, the aim of the current study was to determine the effects of bile acid signaling on the HPA axis. The data presented show that HPA axis suppression during cholestatic liver injury, specifically circulating corticosterone levels and hypothalamic corticotropin releasing hormone (CRH) expression, can be attenuated by administration of the bile acid sequestrant cholestyramine. Secondly, treatment of hypothalamic neurons with various bile acids suppressed CRH expression and secretion in vitro. However, in vivo HPA axis suppression was only evident after the central injection of the bile acids taurocholic acid or glycochenodeoxycholic acid but not the other bile acids studied. Furthermore, we demonstrate that taurocholic acid and glycochenodeoxycholic acid are exerting their effects on hypothalamic CRH expression after their uptake through the apical sodium-dependent bile acid transporter and subsequent activation of the glucocorticoid receptor. Taken together with previous studies, our data support the hypothesis that during cholestatic liver injury, bile acids gain entry into the brain, are transported into neurons through the apical sodium-dependent bile acid transporter and can activate the glucocorticoid receptor to suppress the HPA axis. These data also lend themselves to the broader hypothesis that bile acids may act as central modulators of hypothalamic peptides that may be altered during liver disease.

Published

2015

29. Inhibition of thrombospondin‐1 reduces transforming growth factor beta 1 signaling, hepatic fibrosis and neurological deficits during cholestasis in rats

Author

Sharon DeMorrow, Durreshahwar Khan, Gabriel Frampton, Stephanie Grant, and Matthew McMillin

Subjects

medicine.medical_specialty, biology, business.industry, Transforming growth factor beta, medicine.disease, Biochemistry, Endocrinology, Cholestasis, Internal medicine, Thrombospondin 1, Genetics, medicine, biology.protein, business, Hepatic fibrosis, Molecular Biology, Biotechnology

Published

2020

30. Acetaminophen‐induced liver injury in mice can be alleviated by reducing hepatic TGFβ1 signaling

Author

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

Subjects

Liver injury, business.industry, Genetics, medicine, Pharmacology, medicine.disease, business, Molecular Biology, Biochemistry, Biotechnology, Acetaminophen, medicine.drug

Published

2018

31. Gulf war illness-related chemicals increase CD11b/c

Author

Anca D, Petrescu, Stephanie, Grant, Gabriel, Frampton, Matthew, McMillin, Jessica, Kain, Maheedhar, Kodali, Ashok K, Shetty, and Sharon, DeMorrow

Subjects

Inflammation, Male, CD11b Antigen, Cholestasis, Interleukin-6, DEET, Gene Expression, Monocytes, Article, Rats, Rats, Sprague-Dawley, Disease Models, Animal, Immobilization, Liver, Cell Movement, Animals, Humans, Persian Gulf Syndrome, Bile Ducts, Ligation, Permethrin, Stress, Psychological, Pyridostigmine Bromide

Abstract

Gulf War Illness (GWI) is a chronic multisymptom disorder affecting veterans of the 1990–91 Gulf war. GWI was linked with exposure to chemicals including the nerve gas prophylactic drug pyridostigmine-bromide (PB) and pesticides (DEET, permethrin). Veterans with GWI exhibit prolonged, low-level systemic inflammation, though whether this impacts the liver is unknown. While no evidence exists that GWI-related chemicals are hepatotoxic, the prolonged inflammation may alter the liver’s response to insults such as cholestatic injury. We assessed the effects of GWI-related chemicals on macrophage infiltration and its subsequent influence on hepatic cholestasis. Sprague Dawley rats were treated daily with PB, DEET and permethrin followed by 15 minutes of restraint stress for 28 days. Ten weeks afterward, GWI rats or naïve age-matched controls underwent bile duct ligation (BDL) or sham surgeries. Exposure to GWI-related chemicals alone increased IL-6, and CD11b+F4/80− macrophages in the liver, with no effect on biliary mass or hepatic fibrosis. However, pre-exposure to GWI-related chemicals enhanced biliary hyperplasia and fibrogenesis caused by BDL, compared to naïve rats undergoing the same surgery. These data suggest that GWI patients could be predisposed to developing worse liver pathology due to sustained low-level inflammation of the liver when compared to patients without GWI.

Published

2018

32. P: 5 Let7f Expression Is Upregulated in the Frontal Cortex During Acute Liver Failure and Contributes to Hepatic Encephalopathy via Downregulation of IGF1 Expression

Author

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

Subjects

Pathology, medicine.medical_specialty, Frontal cortex, Hepatology, Downregulation and upregulation, business.industry, Gastroenterology, Liver failure, Medicine, business, medicine.disease, Hepatic encephalopathy

Published

2019

33. P: 60 Characterization of a Novel Mouse Model of Type A Hepatic Encephalopathy

Author

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

Subjects

Pathology, medicine.medical_specialty, Hepatology, business.industry, Gastroenterology, medicine, medicine.disease, business, Hepatic encephalopathy

Published

2019

34. 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

35. TGFβ1 exacerbates blood–brain barrier permeability in a mouse model of hepatic encephalopathy via upregulation of MMP9 and downregulation of claudin-5

Author

Nisha S Patel, Sharon DeMorrow, Amber Jacobs, Andrew P Seiwell, Matthew McMillin, and Gabriel Frampton

Subjects

Male, Pathology, medicine.medical_specialty, Down-Regulation, Pharmacology, Article, Cell Line, Pathology and Forensic Medicine, Capillary Permeability, Transforming Growth Factor beta1, Mice, chemistry.chemical_compound, Downregulation and upregulation, medicine, Animals, Claudin-5, Smad3 Protein, Claudin, Molecular Biology, Hepatic encephalopathy, Tight junction, Azoxymethane, business.industry, Cell Biology, medicine.disease, Extravasation, Up-Regulation, Mice, Inbred C57BL, Endothelial stem cell, Matrix Metalloproteinase 9, chemistry, Blood-Brain Barrier, Hepatic Encephalopathy, business, Transforming growth factor

Abstract

Recent studies have found that vasogenic brain edema is present during hepatic encephalopathy following acute liver failure and is dependent upon increased matrix metalloproteinase 9 (MMP9) activity and downregulation of tight junction proteins. Furthermore, circulating transforming growth factor β1 (TGFβ1) is increased following liver damage and may promote endothelial cell permeability. This study aimed to assess if increased circulating TGFβ1 drives changes in tight junction protein expression and MMP9 activity following acute liver failure. Blood-brain barrier permeability was assessed in azoxymethane (AOM)-treated mice at 6, 12, and 18 hours post-injection via Evan’s blue extravasation. Monolayers of immortalized mouse brain endothelial cells (bEnd.3) were treated with recombinant TGFβ1 (rTGFβ1) and permeability to fluorescein isothiocyanate-dextran (FITC-dextran), MMP9 and claudin-5 expression were assessed. Antagonism of TGFβ1 signaling was performed in vivo to determine its role in blood-brain barrier permeability. Blood-brain barrier permeability was increased in mice at 18 hours following AOM injection. Treatment of bEnd.3 cells with rTGFβ1 led to a dose-dependent increase of MMP9 expression as well as a suppression of claudin-5 expression. These effects of rTGFβ1 on MMP9 and claudin-5 expression could be reversed following treatment with a SMAD3 inhibitor. AOM-treated mice injected with neutralizing antibodies against TGFβ demonstrated significantly reduced blood-brain barrier permeability. Blood-brain barrier permeability is induced in AOM mice via a mechanism involving the TGFβ1-driven SMAD3-dependent upregulation of MMP9 expression and decrease of claudin-5 expression. Therefore, treatment modalities aimed at reducing TGFβ1 levels or SMAD3 activity may be beneficial in promoting blood-brain barrier integrity following liver failure.

Published

2015

36. The specific serotonin reuptake inhibitors sertraline and fluoxetine promote tumor growth in a mouse xenograft model of cholangiocarcinoma

Author

Amy Wyatt, Jessica Kain, Anca D. Petrescu, Gabriel Frampton, Matthew McMillin, Stephanie Grant, Sharon DeMorrow, Hope Shin, and Jenny Smith

Subjects

Sertraline, Fluoxetine, Mouse xenograft, business.industry, medicine, Tumor growth, Pharmacology, Serotonin reuptake, business, Biliary cancer, medicine.drug

Published

2017

37. Bile Acid-Mediated Sphingosine-1-Phosphate Receptor 2 Signaling Promotes Neuroinflammation during Hepatic Encephalopathy in Mice

Author

Juan P. Diocares, Gabriel Frampton, Stephanie Grant, Shamyal Khan, Anca D. Petrescu, Amy Wyatt, Matthew McMillin, Jessica Kain, Sharon DeMorrow, and Brandi Jefferson

Subjects

0301 basic medicine, medicine.medical_specialty, Chemokine, medicine.drug_class, microglia, neurons, Biology, lcsh:RC321-571, Proinflammatory cytokine, 03 medical and health sciences, chemistry.chemical_compound, Cellular and Molecular Neuroscience, 0302 clinical medicine, Internal medicine, medicine, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Enterohepatic circulation, Neuroinflammation, S1PR2, Original Research, Cholestyramine, Bile acid, acute liver failure, Taurocholic acid, cytokines, 030104 developmental biology, Endocrinology, chemistry, biology.protein, 030217 neurology & neurosurgery, CCL2, medicine.drug, Neuroscience

Abstract

Hepatic encephalopathy (HE) is a neuropsychiatric complication that occurs due to deteriorating hepatic function and this syndrome influences patient quality of life, clinical management strategies and survival. During acute liver failure, circulating bile acids increase due to a disruption of the enterohepatic circulation. We previously identified that bile acid-mediated signaling occurs in the brain during HE and contributes to cognitive impairment. However, the influences of bile acids and their downstream signaling pathways on HE-induced neuroinflammation have not been assessed. Conjugated bile acids, such as taurocholic acid (TCA), can activate sphingosine-1-phosphate receptor 2 (S1PR2), which has been shown to promote immune cell infiltration and inflammation in other models. The current study aimed to assess the role of bile-acid mediated S1PR2 signaling in neuroinflammation and disease progression during azoxymethane (AOM)-induced HE in mice. Our findings demonstrate a temporal increase of bile acids in the cortex during AOM-induced HE and identified that cortical bile acids were elevated as an early event in this model. In order to classify the specific bile acids that were elevated during HE, a metabolic screen was performed and this assay identified that TCA was increased in the serum and cortex during AOM-induced HE. To reduce bile acid concentrations in the brain, mice were fed a diet supplemented with cholestyramine, which alleviated neuroinflammation by reducing proinflammatory cytokine expression in the cortex compared to the control diet-fed AOM-treated mice. S1PR2 was expressed primarily in neurons and TCA treatment increased chemokine ligand 2 mRNA expression in these cells. The infusion of JTE-013, a S1PR2 antagonist, into the lateral ventricle prior to AOM injection protected against neurological decline and reduced neuroinflammation compared to DMSO-infused AOM-treated mice. Together, this identifies that reducing bile acid levels or S1PR2 signaling are potential therapeutic strategies for the management of HE.

Published

2017

38. The Hippo signaling functions through the Notch signaling to regulate intrahepatic bile duct development in mammals

Author

Gianfranco Alpini, Duojia Pan, Ying Wan, Tiaohao Zhou, Quy Nguyen, Haibo Bai, Sharon DeMorrow, Nan Wu, Julie Venter, Gabriel Frampton, Fanyin Meng, and Shannon Glaser

Subjects

0301 basic medicine, Male, medicine.medical_specialty, endocrine system, Neurofibromatosis 2, Cell, Notch signaling pathway, Intrahepatic bile ducts, Biology, Protein Serine-Threonine Kinases, Article, Pathology and Forensic Medicine, 03 medical and health sciences, Mice, Mediator, Internal medicine, medicine, Animals, Hippo Signaling Pathway, Receptor, Notch2, Molecular Biology, Mice, Knockout, Hippo signaling pathway, Bile duct, Effector, Cell Biology, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Bile Ducts, Intrahepatic, Hippo signaling, Female

Abstract

The Hippo signaling pathway and the Notch signaling pathway are evolutionary conserved signaling cascades that have important roles in embryonic development of many organs. In murine liver, disruption of either pathway impairs intrahepatic bile duct development. Recent studies suggested that the Notch signaling receptor Notch2 is a direct transcriptional target of the Hippo signaling pathway effector YAP, and the Notch signaling is a major mediator of the Hippo signaling in maintaining biliary cell characteristics in adult mice. However, it remains to be determined whether the Hippo signaling pathway functions through the Notch signaling in intrahepatic bile duct development. We found that loss of the Hippo signaling pathway tumor suppressor Nf2 resulted in increased expression levels of the Notch signaling pathway receptor Notch2 in cholangiocytes but not in hepatocytes. When knocking down Notch2 on the background of Nf2 deficiency in mouse livers, the excessive bile duct development induced by Nf2 deficiency was suppressed by heterozygous and homozygous deletion of Notch2 in a dose-dependent manner. These results implicated that Notch signaling is one of the downstream effectors of the Hippo signaling pathway in regulating intrahepatic bile duct development.

Published

2017

39. Bile acids permeabilize the blood brain barrier after bile duct ligation in rats via Rac1-dependent mechanisms

Author

Matthew McMillin, Hae Yong Pae, Gabriel Frampton, Sharon DeMorrow, Matthew A. Quinn, and Cheryl Galindo

Subjects

medicine.medical_specialty, Hepatology, Tight junction, business.industry, Deoxycholic acid, Gastroenterology, Occludin, medicine.disease, Blood–brain barrier, chemistry.chemical_compound, Endocrinology, medicine.anatomical_structure, Biochemistry, chemistry, Cholestasis, Internal medicine, Chenodeoxycholic acid, medicine, Phosphorylation, business, Ligation

Abstract

Background The blood brain barrier tightly regulates the passage of molecules into the brain and becomes leaky following obstructive cholestasis. The aim of this study was to determine if increased serum bile acids observed during cholestasis permeabilize the blood brain barrier.

Published

2014

40. Overexpression of membrane metalloendopeptidase inhibits substance P stimulation of cholangiocarcinoma growth

Author

Kelly McDaniel, Syeda H. Afroze, Lindsey Kennedy, Shannon Glaser, Sharon DeMorrow, Micheleine Guerrier, Yuyan Han, Gianfranco Alpini, Laura Hargrove, Shanika Avila, Heather Francis, Debolina Ray, Holly Standeford, Julie Venter, Gabriel Frampton, Fanyin Meng, Matthew McMillin, and Morgan Quezada

Subjects

Male, Vascular Endothelial Growth Factor A, medicine.medical_specialty, Time Factors, Physiology, Mice, Nude, Substance P, Biology, Transfection, Gene Expression Regulation, Enzymologic, Cholangiocyte, Cholangiocarcinoma, Mice, Neurokinin-1 Receptor Antagonists, In vivo, Cell Line, Tumor, Proliferating Cell Nuclear Antigen, Physiology (medical), Internal medicine, parasitic diseases, medicine, Animals, Humans, Secretion, Autocrine signalling, Neprilysin, Cell Proliferation, Keratin-19, Mice, Inbred BALB C, Dose-Response Relationship, Drug, Hepatology, Cell growth, Gastroenterology, Receptors, Neurokinin-1, Xenograft Model Antitumor Assays, Molecular biology, Tumor Burden, Up-Regulation, Gene Expression Regulation, Neoplastic, Liver and Biliary Tract, Vascular endothelial growth factor A, Bile Ducts, Intrahepatic, Endocrinology, Bile Duct Neoplasms, Cell culture

Abstract

Substance P (SP) promotes cholangiocyte growth during cholestasis by activating its receptor, NK1R. SP is a proteolytic product of tachykinin (Tac1) and is deactivated by membrane metalloendopeptidase (MME). This study aimed to evaluate the functional role of SP in the regulation of cholangiocarcinoma (CCA) growth. NK1R, Tac1, and MME expression and SP secretion were assessed in human CCA cells and nonmalignant cholangiocytes. The proliferative effects of SP (in the absence/presence of the NK1R inhibitor, L-733,060) and of L-733,060 were evaluated. In vivo, the effect of L-733,060 treatment or MME overexpression on tumor growth was evaluated by using a xenograft model of CCA in nu/nu nude mice. The expression of Tac1, MME, NK1R, PCNA, CK-19, and VEGF-A was analyzed in the resulting tumors. Human CCA cell lines had increased expression of Tac1 and NK1R, along with reduced levels of MME compared with nonmalignant cholangiocytes, resulting in a subsequent increase in SP secretion. SP treatment increased CCA cell proliferation in vitro, which was blocked by L-733,060. Treatment with L-733,060 alone inhibited CCA proliferation in vitro and in vivo. Xenograft tumors derived from MME-overexpressed human Mz-ChA-1 CCA cells had a slower growth rate than those derived from control cells. Expression of PCNA, CK-19, and VEGF-A decreased, whereas MME expression increased in the xenograft tumors treated with L-733,060 or MME-overexpressed xenograft tumors compared with controls. The study suggests that SP secreted by CCA promotes CCA growth via autocrine pathway. Blockade of SP secretion and NK1R signaling may be important for the management of CCA.

Published

2014

41. P: 61 Attenuation of Neurological Symptoms of Type C Hepatic Encephalopathy by Selective Ablation of Neuronal FXR Expression

Author

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

Subjects

Pathology, medicine.medical_specialty, Hepatology, business.industry, Selective ablation, Gastroenterology, medicine, medicine.disease, business, Hepatic encephalopathy

Published

2019

42. P: 79 Central Inhibition of IGFBP3 Attenuates Symptoms of Hepatic Encephalopathy in a Mouse Model of Acute Liver Failure

Author

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

Subjects

medicine.medical_specialty, Hepatology, business.industry, Internal medicine, Gastroenterology, medicine, IGFBP3, Liver failure, medicine.disease, business, Hepatic encephalopathy

Published

2019

43. P: 57 Thrombospondin-1 Worsens Azoxymethane-Induced Hepatic Encephalopathy Through Activation of Transforming Growth Factor Beta 1

Author

Gabriel Frampton, Sharon DeMorrow, Stephanie Grant, Matthew McMillin, and Brandi Jefferson

Subjects

Hepatology, biology, business.industry, Azoxymethane, Gastroenterology, Transforming growth factor beta, medicine.disease, chemistry.chemical_compound, chemistry, Thrombospondin 1, biology.protein, Cancer research, Medicine, business, Hepatic encephalopathy

Published

2019

44. 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

45. 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

46. 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

47. Neuropeptide Y inhibits biliary hyperplasia of cholestatic rats by paracrine and autocrine mechanisms

Author

Gabriel Frampton, Fanyin Meng, Romina Mancinelli, Paolo Onori, Kelly McDaniel, Julie Venter, Dinorah Leyva-Illades, Gianfranco Alpini, Matthew A. Quinn, Shannon Glaser, Antonio Franchitto, Eugenio Gaudio, Hae Yong Pae, Heather Francis, and Sharon DeMorrow

Subjects

Male, medicine.medical_specialty, Physiology, proliferation, Paracrine Communication, Biology, Autocrine Communication, digestive system, neurotransmitters, Cell Line, Paracrine signalling, Proliferating Cell Nuclear Antigen, Physiology (medical), Internal medicine, mental disorders, medicine, Animals, Homeostasis, Neuropeptide Y, RNA, Messenger, Autocrine signalling, Receptor, Cell Proliferation, Cholestasis, Hyperplasia, Hepatology, biliary epithelium, Biliary hyperplasia, Gastroenterology, Neuropeptide Y receptor, Antibodies, Neutralizing, Rats, Inbred F344, humanities, Rats, Receptors, Neuropeptide Y, Liver and Biliary Tract, Bile Ducts, Intrahepatic, Endocrinology, cell cycle, Signal transduction, Signal Transduction

Abstract

Neuropeptide Y (NPY) exerts its functions through six subtypes of receptors (Y1–Y6). Biliary homeostasis is regulated by several factors through autocrine/paracrine signaling. NPY inhibits cholangiocarcinoma growth; however, no information exists regarding the autocrine/paracrine role of NPY on biliary hyperplasia during cholestasis. The aims of this study were to determine: 1) the expression of NPY and Y1–Y5 in cholangiocytes and 2) the paracrine/autocrine effects of NPY on cholangiocyte proliferation. Normal or bile duct ligation (BDL) rats were treated with NPY, neutralizing anti-NPY antibody, or vehicle for 7 days. NPY and NPY receptor (NPYR) expression was assessed in liver sections and isolated cholangiocytes. NPY secretion was assessed in serum and bile from normal and BDL rats, as well as supernatants from normal and BDL cholangiocytes and normal rat cholangiocyte cell line [intrahepatic normal cholangiocyte culture (NRICC)]. We evaluated intrahepatic bile ductal mass (IBDM) in liver sections and proliferation in cholangiocytes. With the use of NRICC, the effects of NPY or anti-NPY antibody on cholangiocyte proliferation were determined. The expression of NPY and all NPYR were increased after BDL. NPY levels were lower in serum and cholangiocyte supernatant from BDL compared with normal rats. NPY secretion from NRICC was detected at both the basolateral and apical domains. Chronic NPY treatment decreased proliferating cellular nuclear antigen (PCNA) expression and IBDM in BDL rats. Administration of anti-NPY antibody to BDL rats increased cholangiocyte proliferation and IBDM. NPY treatment of NRICC decreased PCNA expression and increased the cell cycle arrest, whereas treatment with anti-NPY antibody increased proliferation. Therapies targeting NPY-mediated signaling may prove beneficial for the treatment of cholangiopathies.

Published

2013

48. The novel growth factor, progranulin, stimulates mouse cholangiocyte proliferation via sirtuin-1-mediated inactivation of FOXO1

Author

Cheryl Galindo, Matthew McMillin, Hae Yong Pae, Gabriel Frampton, Sharon DeMorrow, Matthew A. Quinn, Dinorah Leyva-Illades, and Yoshiyuki Ueno

Subjects

Male, medicine.medical_specialty, Physiology, medicine.medical_treatment, Cholangiocyte proliferation, FOXO1, Biology, Cholangiocyte, Cholangiocarcinoma, Small hairpin RNA, Mice, Progranulins, Sirtuin 1, Downregulation and upregulation, Physiology (medical), Internal medicine, medicine, Animals, Ligation, Cell Proliferation, Granulins, Hepatology, Forkhead Box Protein O1, Cell growth, Growth factor, Gastroenterology, Forkhead Transcription Factors, Cell biology, Mice, Inbred C57BL, Liver and Biliary Tract, Endocrinology, biology.protein, Intercellular Signaling Peptides and Proteins, Bile Ducts

Abstract

Progranulin (PGRN), a secreted growth factor, regulates the proliferation of various epithelial cells. Its mechanism of action is largely unknown. Sirtuin 1 (Sirt1) is a protein deacetylase that is known to regulate the transcriptional activity of the forkhead receptor FOXO1, thereby modulating the balance between proapoptotic and cell cycle-arresting genes. We have shown that PGRN is overexpressed in cholangiocarcinoma and stimulates proliferation. However, its effects on hyperplastic cholangiocyte proliferation are unknown. In the present study, the expression of PGRN and its downstream targets was determined after bile duct ligation (BDL) in mice and in a mouse cholangiocyte cell line after stimulation with PGRN. The effects of PGRN on cholangiocyte proliferation were assessed in sham-operated (sham) and BDL mice treated with PGRN or by specifically knocking down endogenous PGRN expression using Vivo-Morpholinos or short hairpin RNA. PGRN expression and secretion were upregulated in proliferating cholangiocytes isolated after BDL. Treatment of mice with PGRN increased biliary mass and cholangiocyte proliferation in vivo and in vitro and enhanced cholangiocyte proliferation observed after BDL. PGRN treatment decreased Sirt1 expression and increased the acetylation of FOXO1, resulting in the cytoplasmic accumulation of FOXO1 in cholangiocytes. Overexpression of Sirt1 in vitro prevented the proliferative effects of PGRN. Conversely, knocking down PGRN expression in vitro or in vivo inhibited cholangiocyte proliferation. In conclusion, these data suggest that the upregulation of PGRN may be a key feature stimulating cholangiocyte proliferation. Modulating PGRN levels may be a viable technique for regulating the balance between ductal proliferation and ductopenia observed in a variety of cholangiopathies.

Published

2012

49. Monoamine oxidase A expression is suppressed in human cholangiocarcinoma via coordinated epigenetic and IL-6-driven events

Author

Wei Chen, Gabriel Frampton, Matthew McMillin, Sharon DeMorrow, Kun Song Zhang, Matthew A. Quinn, Li Huang, Li Jian Liang, Kimberly Walker, Brianne Culbreath, Arundhati Rao, Jia Ming Lai, Michelle K. Bradley, Xiao Yu Yin, and Dinorah Leyva-Illades

Subjects

Male, Chromatin Immunoprecipitation, Serotonin, Cell Survival, Sp1 Transcription Factor, Dopamine, Mice, Nude, Repressor, digestive system, Gene Expression Regulation, Enzymologic, Article, Pathology and Forensic Medicine, Cholangiocarcinoma, Mice, Cell Line, Tumor, medicine, Animals, Humans, Epigenetics, Promoter Regions, Genetic, Interleukin 6, Monoamine Oxidase, neoplasms, Molecular Biology, R1 repressor, DNA methylation, biology, Interleukin-6, Cell Biology, Immunohistochemistry, digestive system diseases, Gene Expression Regulation, Neoplastic, Repressor Proteins, Bile Ducts, Intrahepatic, SP-1, Bile Duct Neoplasms, Cell culture, Case-Control Studies, Choledochal Cyst, biliary cancer, biology.protein, Cancer research, Monoamine oxidase A, medicine.drug

Abstract

Objectives The secretion of dopamine and serotonin is increased in cholangiocarcinoma, which has growth-promoting effects. Monoamine oxidase A (MAOA), the degradation enzyme of serotonin and dopamine, is suppressed in cholangiocarcinoma via an unknown mechanism. The aims of this study were to (i) correlate MAOA immunoreactivity with pathophysiological parameters of cholangiocarcinoma, (ii) determine the mechanism by which MAOA expression is suppressed and (iii) evaluate the consequences of restored MAOA expression in cholangiocarcinoma. Design MAOA expression was assessed in cholangiocarcinoma and non-malignant controls. The control of MAOA expression by promoter hypermethylation was evaluated and the contribution of IL-6 signaling to the suppression of MAOA expression was determined. The effects of MAOA overexpression on cholangiocarcinoma growth and invasion were also assessed. Results MAOA expression is correlated with differentiation, invasion and survival in cholangiocarcinoma. The MAOA promoter was hypermethylated immediately upstream of the start codon in cholangiocarcinoma samples and cell lines but not in non-malignant counterparts. IL-6 signaling also decreased MAOA expression via a mechanism independent of hypermethylation, involving the regulation of the balance between SP-1 transcriptional activity and its inhibitor, R1 repressor. Inhibition of both IL-6 signaling and DNA methylation restored MAOA levels to those observed in cholangiocytes. Forced MAOA overexpression inhibited cholangiocarcinoma growth and invasion. Conclusions MAOA expression is suppressed by the coordinated control of promoter hypermethylation and IL-6 signaling. MAOA may be a useful prognostic marker in the management of cholangiocarcinoma, and therapies designed to increase MAOA expression might prove beneficial in the treatment of cholangiocarcinoma.

Published

2012

50. Hepatic alterations are accompanied by changes to bile acid transporter-expressing neurons in the hypothalamus after traumatic brain injury

Author

Sanjib Mukherjee, Matthew McMillin, Sharon DeMorrow, Damir Nizamutdinov, Gabriel Frampton, Suzanne Zeitouni, Lee A. Shapiro, Jacob Hurst, Paul Clint S. Bricker, and Jessica Kain

Subjects

0301 basic medicine, medicine.medical_specialty, Time Factors, medicine.drug_class, Traumatic brain injury, Hypothalamus, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, Internal medicine, Brain Injuries, Traumatic, medicine, Animals, Receptor, Acute-Phase Reaction, Stroke, Neurons, Multidisciplinary, Membrane Glycoproteins, Bile acid, business.industry, Acute-phase protein, Transporter, medicine.disease, nervous system diseases, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Endocrinology, nervous system, Liver, business, Carrier Proteins, 030217 neurology & neurosurgery

Abstract

Annually, there are over 2 million incidents of traumatic brain injury (TBI) and treatment options are non-existent. While many TBI studies have focused on the brain, peripheral contributions involving the digestive and immune systems are emerging as factors involved in the various symptomology associated with TBI. We hypothesized that TBI would alter hepatic function, including bile acid system machinery in the liver and brain. The results show activation of the hepatic acute phase response by 2 hours after TBI, hepatic inflammation by 6 hours after TBI and a decrease in hepatic transcription factors, Gli 1, Gli 2, Gli 3 at 2 and 24 hrs after TBI. Bile acid receptors and transporters were decreased as early as 2 hrs after TBI until at least 24 hrs after TBI. Quantification of bile acid transporter, ASBT-expressing neurons in the hypothalamus, revealed a significant decrease following TBI. These results are the first to show such changes following a TBI, and are compatible with previous studies of the bile acid system in stroke models. The data support the emerging idea of a systemic influence to neurological disorders and point to the need for future studies to better define specific mechanisms of action.

Published

2016