Your search keyword '"Watkins, S"' showing total 27 results

1. Intravital imaging reveals inflammation as a dominant pathophysiology of age-related hepatovascular changes.

Author

Vats R, Li Z, Ju EM, Dubey RK, Kaminski TW, Watkins S, and Pradhan-Sundd T

Subjects

Animals, Inflammation metabolism, Intravital Microscopy, Mice, Mice, Inbred C57BL, Endothelial Cells, Liver metabolism

Abstract

Aging is the most significant risk factor for the majority of chronic diseases, including liver disease. The cellular, molecular, and pathophysiological mechanisms that promote age-induced hepatovascular changes are unknown due to our inability to visualize changes in liver pathophysiology in live mice over time. We performed quantitative liver intravital microscopy (qLIM) in live C57BL/6J mice to investigate the impact of aging on the hepatovascular system over a 24-mo period. qLIM revealed that age-related hepatic alterations include reduced liver sinusoidal blood flow, increased sinusoidal vessel diameter, and loss of small hepatic vessels. The ductular cell structure deteriorates with age, along with altered expression of hepatic junctional proteins. Furthermore, qLIM imaging revealed increased inflammation in the aged liver, which was linked to increased expression of proinflammatory macrophages, hepatic neutrophils, liver sinusoidal endothelial cells, senescent cells, and procoagulants. Finally, we detected elevated NF-κB pathway activity in aged livers. Overall, these findings emphasize the importance of inflammation in age-related hepatic vasculo-epithelial alterations and highlight the utility of qLIM in studying age-related effects in organ pathophysiology.

Published

2022

2. Compensatory hepatic adaptation accompanies permanent absence of intrahepatic biliary network due to YAP1 loss in liver progenitors.

Author

Molina LM, Zhu J, Li Q, Pradhan-Sundd T, Krutsenko Y, Sayed K, Jenkins N, Vats R, Bhushan B, Ko S, Hu S, Poddar M, Singh S, Tao J, Sundd P, Singhi A, Watkins S, Ma X, Benos PV, Feranchak A, Michalopoulos G, Nejak-Bowen K, Watson A, Bell A, and Monga SP

Subjects

Animals, Cell Transdifferentiation, Genotype, Imaging, Three-Dimensional, Liver embryology, Mice, Mice, Inbred C57BL, Mice, Knockout, Morphogenesis, Regeneration, YAP-Signaling Proteins metabolism, Adaptation, Physiological, Biliary Tract physiology, Liver physiology, Stem Cells metabolism, YAP-Signaling Proteins deficiency

Abstract

Yes-associated protein 1 (YAP1) regulates cell plasticity during liver injury, regeneration, and cancer, but its role in liver development is unknown. We detect YAP1 activity in biliary cells and in cells at the hepatobiliary bifurcation in single-cell RNA sequencing analysis of developing livers. Deletion of Yap1 in hepatoblasts does not impair Notch-driven SOX9+ ductal plate formation but does prevent the formation of the abutting second layer of SOX9+ ductal cells, blocking the formation of a patent intrahepatic biliary tree. Intriguingly, these mice survive for 8 months with severe cholestatic injury and without hepatocyte-to-biliary transdifferentiation. Ductular reaction in the perihilar region suggests extrahepatic biliary proliferation, likely seeking the missing intrahepatic biliary network. Long-term survival of these mice occurs through hepatocyte adaptation via reduced metabolic and synthetic function, including altered bile acid metabolism and transport. Overall, we show YAP1 as a key regulator of bile duct development while highlighting a profound adaptive capability of hepatocytes., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2021 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2021

3. Associations of coffee consumption with markers of liver injury in the insulin resistance atherosclerosis study.

Author

Dickson JC, Liese AD, Lorenzo C, Haffner SM, Watkins SM, Hamren SJ, Stiles JK, Wagenknecht LE, and Hanley AJ

Subjects

Biomarkers blood, Caffeine, Female, Humans, Insulin Resistance, Linear Models, Liver Function Tests, Male, Middle Aged, Non-alcoholic Fatty Liver Disease blood, Protective Factors, Surveys and Questionnaires, Alanine Transaminase blood, Aspartate Aminotransferases blood, Coffee, Diabetes Mellitus, Type 2 blood, Liver pathology, alpha-2-HS-Glycoprotein metabolism

Abstract

Background: Coffee consumption has been associated with reduced risk of developing type 2 diabetes mellitus (T2DM) however, the mechanism for this association has yet to be elucidated. Non-alcoholic fatty liver disease (NAFLD) characterizes and predicts T2DM yet the relationship of coffee with this disorder remains unclear. Our aim was to investigate the associations of coffee with markers of liver injury in 1005 multi-ethnic, non-diabetic adults in the Insulin Resistance Atherosclerosis Study., Methods: Dietary intake was assessed using a validated 114-item food frequency questionnaire. Alanine aminotransferase (ALT), aspartate aminotransferase (AST) and fetuin-A were determined in fasting blood samples and the validated NAFLD liver fat score was calculated. Multivariate linear regression assessed the contribution of coffee to variation in markers of liver injury., Results: Caffeinated coffee showed significant inverse associations with ALT (β = -0.08, p = 0.0111), AST (β = -0.05, p = 0.0155) and NAFLD liver fat score (β = -0.05, p = 0.0293) but not with fetuin-A (β = 0.04, p = 0.17). When the highest alcohol consumers were excluded, these associations remained (ALT β = -0.11, p = 0.0037; AST β = -0.05, p = 0.0330; NAFLD liver fat score β = -0.06, p = 0.0298). With additional adjustment for insulin sensitivity, the relationship with ALT remained significant (ALT β = -0.08, p = 0.0400; AST β = -0.03, p = 0.20; NAFLD liver fat score β = -0.03, p = 0.27). There were no significant associations of decaffeinated coffee with liver markers., Conclusions: These analyses indicate a beneficial impact of caffeinated coffee on liver morphology and/or function, and suggest that this relationship may mediate the well-established inverse association of coffee with risk of T2DM.

Published

2015

4. An autophagy-enhancing drug promotes degradation of mutant alpha1-antitrypsin Z and reduces hepatic fibrosis.

Author

Hidvegi T, Ewing M, Hale P, Dippold C, Beckett C, Kemp C, Maurice N, Mukherjee A, Goldbach C, Watkins S, Michalopoulos G, and Perlmutter DH

Subjects

Animals, Carbamazepine administration & dosage, Carbamazepine therapeutic use, Cell Line, Disease Models, Animal, Endoplasmic Reticulum metabolism, HeLa Cells, Humans, Liver drug effects, Liver pathology, Liver Cirrhosis etiology, Liver Cirrhosis metabolism, Liver Cirrhosis pathology, Mice, Mice, Transgenic, Mutant Proteins chemistry, Mutant Proteins metabolism, Phagosomes drug effects, Phagosomes ultrastructure, Phenotype, Proteasome Endopeptidase Complex metabolism, Protein Folding, Solubility, alpha 1-Antitrypsin chemistry, alpha 1-Antitrypsin genetics, alpha 1-Antitrypsin Deficiency complications, alpha 1-Antitrypsin Deficiency pathology, Autophagy drug effects, Carbamazepine pharmacology, Liver metabolism, Liver Cirrhosis drug therapy, alpha 1-Antitrypsin metabolism, alpha 1-Antitrypsin Deficiency metabolism

Abstract

In the classical form of alpha1-antitrypsin (AT) deficiency, a point mutation in AT alters the folding of a liver-derived secretory glycoprotein and renders it aggregation-prone. In addition to decreased serum concentrations of AT, the disorder is characterized by accumulation of the mutant alpha1-antitrypsin Z (ATZ) variant inside cells, causing hepatic fibrosis and/or carcinogenesis by a gain-of-toxic function mechanism. The proteasomal and autophagic pathways are known to mediate degradation of ATZ. Here we show that the autophagy-enhancing drug carbamazepine (CBZ) decreased the hepatic load of ATZ and hepatic fibrosis in a mouse model of AT deficiency-associated liver disease. These results provide a basis for testing CBZ, which has an extensive clinical safety profile, in patients with AT deficiency and also provide a proof of principle for therapeutic use of autophagy enhancers.

Published

2010

5. A new antidiabetic compound attenuates inflammation and insulin resistance in Zucker diabetic fatty rats.

Author

Lu M, Patsouris D, Li P, Flores-Riveros J, Frincke JM, Watkins S, Schenk S, and Olefsky JM

Subjects

Adult, Analysis of Variance, Animals, Blood Glucose metabolism, Blotting, Western, Cell Movement drug effects, Chemokines metabolism, Cytokines metabolism, Dehydroepiandrosterone pharmacology, Female, Gene Expression, Gluconeogenesis drug effects, Glucose Clamp Technique, Glucose Tolerance Test, Humans, Immunohistochemistry, Inflammation metabolism, Lipids blood, Lipopolysaccharides, Liver metabolism, Macrophages metabolism, Male, Mice, Middle Aged, Muscle, Skeletal drug effects, Muscle, Skeletal metabolism, Obesity metabolism, Rats, Rats, Zucker, Dehydroepiandrosterone analogs & derivatives, Inflammation drug therapy, Insulin Resistance, Liver drug effects, Macrophages drug effects, Obesity drug therapy

Abstract

Tissue macrophage inflammatory pathways contribute to obesity-associated insulin resistance. Here, we have examined the efficacy and mechanisms of action of a novel anti-inflammatory compound (HE3286) in vitro and in vivo. In primary murine macrophages, HE3286 attenuates LPS- and TNFalpha-stimulated inflammation. In Zucker diabetic fatty rats, inflammatory cytokine/chemokine expression was downregulated in liver and adipose tissue by HE3286 treatment, as was macrophage infiltration into adipose tissue. In line with reduced inflammation, HE3286 treatment normalized fasting and fed glucose levels, improved glucose tolerance, and enhanced skeletal muscle and liver insulin sensitivity, as assessed by hyperinsulinemic euglycemic clamp studies. In phase 2 clinical trials, HE3286 treatment led to an enhancement in insulin sensitivity in humans. Gluconeogenic capacity was also reduced by HE3286 treatment, as evidenced by a reduced glycemic response during pyruvate tolerance tests and decreased basal hepatic glucose production (HGP) rates. Since serum levels of gluconeogenic substrates were decreased by HE3286, it indicates that the reduction of both intrinsic gluconeogenic capacity and substrate availability contributes to the decrease in HGP. Lipidomic analysis revealed that HE3286 treatment reduced liver cholesterol and triglyceride content, leading to a feedback elevation of LDL receptor and HMG-CoA reductase expression. Accordingly, HE3286 treatment markedly decreased total serum cholesterol. In conclusion, HE3286 is a novel anti-inflammatory compound, which displays both glucose-lowering and cholesterol-lowering effects.

Published

2010

6. Superoxide-induced apoptosis of activated rat hepatic stellate cells.

Author

Thirunavukkarasu C, Watkins S, Harvey SA, and Gandhi CR

Subjects

Animals, Caspase Inhibitors, Cell Survival drug effects, Cells, Cultured, Extracellular Fluid enzymology, Free Radical Scavengers metabolism, Heat-Shock Proteins metabolism, Heme Oxygenase (Decyclizing), Liver cytology, Liver enzymology, Male, Oxygenases metabolism, Protease Inhibitors pharmacology, Rats, Rats, Sprague-Dawley, Superoxide Dismutase metabolism, Apoptosis, Liver drug effects, Liver physiology, Superoxides pharmacology

Abstract

Background/aims: During liver injury, reactive oxygen species (ROS) are produced by the resident macrophages (Kupffer cells) and infiltrating blood cells such as neutrophils. ROS cause transformation of desmin-positive quiescent hepatic stellate cells (HSCs) into the proliferating activated phenotype that expresses alpha-smooth muscle actin (alpha-SMA). The highly fibrogenic and contractile activated HSCs (aHSCs) produce various cytokines and growth factors, and play important role in the pathophysiology of chronic liver disease. However, apoptotic aHSCs are also observed during active fibrogenesis in the injured liver. Therefore, we investigated the mechanisms of apoptosis of aHSCs in relation to ROS., Methods: HSCs, isolated from normal rat liver, were activated in culture and effects of superoxide were determined between subcultures 3 and 5., Results: Treatment with superoxide caused apoptosis of aHSCs as determined by flow cytometry, TUNEL assay and DNA laddering analysis. The mechanisms of superoxide-induced apoptosis involved release of cytochrome c, increased Bax expression, increased caspase-3 activity, and hydrolysis of polyADP-ribose polymerase. Superoxide also increased the expression of antiapoptotic Bcl-xL and nuclear translocation of NFkappaB. Caspase-3 inhibitor (DEVD-fmk) and antioxidants (N-acetylcysteine, vitamin E and superoxide dismutase) inhibited superoxide-induced apoptosis., Conclusions: Superoxide-induced apoptosis of aHSCs may be a novel mechanism of limiting chronic fibrotic liver injury.

Published

2004

7. The roles of iNOS in liver ischemia-reperfusion injury.

Author

Lee VG, Johnson ML, Baust J, Laubach VE, Watkins SC, and Billiar TR

Subjects

Alanine Transaminase blood, Animals, Disease Models, Animal, Gene Expression Regulation, Enzymologic, Kinetics, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Nitric Oxide Synthase deficiency, Nitric Oxide Synthase genetics, Nitric Oxide Synthase Type II, Time Factors, Transcription, Genetic, Liver blood supply, Nitric Oxide Synthase metabolism, Reperfusion Injury enzymology

Abstract

To determine the contribution of the inducible nitric oxide synthase (iNOS) to hepatic injury following warm ischemia-reperfusion, we developed a model of partial hepatic ischemia-reperfusion in mice and studied the injury response in iNOS knockout (KO) mice. Compared with wild types, iNOS KO animals exhibited lower plasma transaminase levels after 1 and 6 h of reperfusion following 1 h of ischemia. At the 3-h time point, enzyme levels were not different between the two groups. iNOS mRNA was not detectable in the ischemic hepatic lobes of wild-type mice until 3 h of reperfusion; however, perfusion studies identified a significant delay in reperfusion of the ischemic lobe in the iNOS KO mice at the 1-h time point with similar perfusion rates at 3 and 6 h compared with wild type. By way of comparison, mice deficient in the endothelial NOS (eNOS) were also assessed for the degree of hepatic damage 3 h post-reperfusion. Plasma transaminase levels were significantly increased in eNOS KO animals compared with wild-type controls. These data suggest that systemic as well as local sources of iNOS regulate reperfusion, and local iNOS contributes to hepatic injury, while eNOS is protective in warm hepatic ischemia-reperfusion.

Published

2001

8. Scavenging nitric oxide reduces hepatocellular injury after endotoxin challenge.

Author

Nadler EP, Dickinson EC, Beer-Stolz D, Alber SM, Watkins SC, Pratt DW, and Ford HR

Subjects

Animals, Electron Spin Resonance Spectroscopy, Endotoxemia drug therapy, Endotoxemia pathology, Gene Expression physiology, Hepatocytes metabolism, Hepatocytes pathology, Hepatocytes ultrastructure, Interleukin-6 genetics, Kupffer Cells metabolism, Kupffer Cells pathology, Lipopolysaccharides pharmacology, Liver chemistry, Liver pathology, Male, Microscopy, Electron, Neutrophils immunology, Nitric Oxide Synthase metabolism, Nitric Oxide Synthase Type II, RNA, Messenger analysis, Rats, Rats, Sprague-Dawley, Sorbitol analogs & derivatives, Tumor Necrosis Factor-alpha analysis, Endotoxemia metabolism, Free Radical Scavengers pharmacology, Liver metabolism, Nitric Oxide metabolism, Nitric Oxide pharmacology

Abstract

Sustained upregulation of inducible nitric oxide (NO) synthase in the liver after endotoxin [lipopolysaccharide (LPS)] challenge may result in hepatocellular injury. We hypothesized that administration of a NO scavenger, NOX, may attenuate LPS-induced hepatocellular injury. Sprague-Dawley rats received NOX or saline via subcutaneous osmotic pumps, followed 18 h later by LPS challenge. Hepatocellular injury was assessed using biochemical assays, light, and transmission electron microscopy (TEM). Interleukin (IL)-6 mRNA was measured by RT-PCR. Tumor necrosis factor (TNF)-alpha protein expression was determined by immunohistochemistry. NOX significantly reduced serum levels of ornithine carbamoyltransferase and aspartate aminotransferase. TNF-alpha and IL-6 expression were increased in the livers of saline-treated but not NOX-treated rats. Although there was no difference between groups by light microscopy, TEM revealed obliteration of the space of Disse in saline-treated but not in NOX-treated animals. Electron paramagnetic resonance showed the characteristic mononitrosyl complex in NOX-treated rats. We conclude that NOX reduces hepatocellular injury after endotoxemia. NOX may be useful in the management of hepatic dysfunction secondary to sepsis or other diseases associated with excessive NO production.

Published

2001

9. Liver-derived DEC205+B220+CD19- dendritic cells regulate T cell responses.

Author

Lu L, Bonham CA, Liang X, Chen Z, Li W, Wang L, Watkins SC, Nalesnik MA, Schlissel MS, Demestris AJ, Fung JJ, and Qian S

Subjects

Animals, Apoptosis immunology, Cell Differentiation immunology, Cell Movement immunology, Cytokines biosynthesis, Dendritic Cells metabolism, Dendritic Cells transplantation, Gene Rearrangement, B-Lymphocyte, Heavy Chain, Gene Rearrangement, B-Lymphocyte, Light Chain, Graft Survival immunology, Heart Transplantation immunology, Immunophenotyping, Liver metabolism, Lymphocyte Activation immunology, Lymphocyte Culture Test, Mixed, Male, Mice, Mice, Inbred BALB C, Mice, Inbred C3H, Mice, Inbred C57BL, Minor Histocompatibility Antigens, Protein Tyrosine Phosphatase, Non-Receptor Type 1, T-Lymphocyte Subsets cytology, T-Lymphocyte Subsets immunology, T-Lymphocytes cytology, T-Lymphocytes, Helper-Inducer classification, T-Lymphocytes, Helper-Inducer cytology, T-Lymphocytes, Helper-Inducer immunology, Antigens, CD, Antigens, CD19 biosynthesis, Dendritic Cells immunology, Lectins, C-Type, Leukocyte Common Antigens biosynthesis, Liver cytology, Liver immunology, Membrane Glycoproteins biosynthesis, Receptors, Cell Surface biosynthesis, T-Lymphocytes immunology

Abstract

Leukocytes resident in the liver may play a role in immune responses. We describe a cell population propagated from mouse liver nonparenchymal cells in IL-3 and anti-CD40 mAb that exhibits a distinct surface immunophenotype and function in directing differentiation of naive allogeneic T cells. After culture, such cells are DEC-205(bright)B220+CD11c-CD19-, and negative for T (CD3, CD4, CD8alpha), NK (NK 1.1) cell markers, and myeloid Ags (CD11b, CD13, CD14). These liver-derived DEC205+B220+ CD19- cells have a morphology and migratory capacity similar to dendritic cells. Interestingly, they possess Ig gene rearrangements, but lack Ig molecule expression on the cell surface. They induce low thymidine uptake of allogeneic T cells in MLR due to extensive apoptosis of activated T cells. T cell proliferation is restored by addition of the common caspase inhibitor peptide, benzyloxycarbonyl-Val-Ala-Asp-fluoromethyl ketone (zVAD-fmk). T cells stimulated by liver-derived DEC205+B220+D19- cells release both IL-10 and IFN-gamma, small amounts of TGF-beta, and no IL-2 or IL-4, a cytokine profile resembling T regulatory type 1 cells. Expression of IL-10 and IFN-gamma, but not bioactive IL-12 in liver DEC205+B220+CD19- cells was demonstrated by RNase protection assay. In vivo administration of liver DEC205+B220+CD19- cells significantly prolonged the survival of vascularized cardiac allografts in an alloantigen-specific manner.

Published

2001

10. Interaction of estrogen and 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) with hepatic fatty acid synthesis and metabolism of male chickens (Gallus domesticus).

Author

Stanton B, Watkins S, German JB, and Lasley B

Subjects

Animals, Chromatography, Gas, Chromatography, Thin Layer, Dose-Response Relationship, Drug, Drug Antagonism, Liver drug effects, Male, Phospholipids metabolism, Polychlorinated Dibenzodioxins metabolism, Triglycerides metabolism, Wasting Syndrome chemically induced, Wasting Syndrome veterinary, Chickens metabolism, Environmental Pollutants pharmacology, Estrogen Antagonists pharmacology, Fatty Acids metabolism, Liver metabolism, Polychlorinated Dibenzodioxins pharmacology

Abstract

This study tested the hypothesis that 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) antagonizes estrogen-induced hepatic lipid synthesis and metabolism in birds. Twenty immature male chickens (Gallus domesticus) were divided evenly into four groups: (1) vehicle control; (2) estrogen alone (1.0 mg/kg estradiol cypionate injected on three consecutive days); (3) TCDD alone (50 microg/kg injected on the fourth day); and (4) a combination of the estrogen and TCDD treatments. On day 14, liver samples were collected for quantitative fatty acid analysis by capillary gas chromatography. Birds treated with estrogen alone had increased total triacylglyceride concentrations with specific increases in the Delta9 desaturase products 16:1n7, 18:1n7, 18:1n9, and 20:1n9. In addition, estrogen treatment specifically increased 22:6n3 concentrations in both triacylglycerides and phospholipids. However, these increases in Delta9 desaturase products or 22:6n3 did not occur for birds treated with estrogen in combination with TCDD. TCDD and estrogen plus TCDD treatments increased phospholipid concentrations of the diet-derived polyunsaturated fatty acids 18:2n6, 18:3n6, 20:3n6, 18:3n3, and 20:5n3, although only the estrogen plus TCDD group had significantly increased total phospholipids. In cholesterol esters, all three treatments decreased concentrations of total fatty acids, saturated fatty acids, and Delta9 desaturase products compared to the control group.

Published

2001

11. Potent antitumor effects of intra-arterial injection of fibroblasts genetically engineered to express IL-12 in liver metastasis model of rat: no additional benefit of using retroviral producer cell.

Author

Iwazawa T, Chau GY, Mori T, Dookeran KA, Rubin JT, Watkins S, Robbins PD, Lotze MT, and Tahara H

Subjects

3T3 Cells, Animals, Base Sequence, Cell Division immunology, Cell Line, Female, Green Fluorescent Proteins, Immunotherapy, Injections, Intra-Arterial, Interleukin-12 genetics, Lac Operon physiology, Liver Neoplasms metabolism, Liver Neoplasms secondary, Luminescent Proteins metabolism, Mice, Molecular Sequence Data, Neoplasm Metastasis, Neoplasm Transplantation, Polymerase Chain Reaction, RNA, Messenger metabolism, Rats, Rats, Inbred F344, Retroviridae genetics, Fibroblasts metabolism, Interleukin-12 metabolism, Liver pathology, Liver Neoplasms therapy

Abstract

Interleukin-12 (IL-12) mediates significant antitumor effects in animal models but associated with dose-dependent toxicity in human. To achieve local expression of IL-12 at the tumor site without systemic toxicity, we performed intra-arterial administration of fibroblasts genetically engineered to produce IL-12 protein with or without retrovirus (CRIP- IL-12 or 3T3-IL-12) in liver metastasis model. Rat breast cancer cells ( MADB - 106) were injected into the portal vein of syngeneic Fisher rats on day 0, and fibroblasts were injected into the hepatic artery on day 7. On day 21, liver weight and number of liver tumors were examined. As controls, CRIP cells expressing retrovirus carrying lacZ marker gene (CRIP-lacZ) or saline (Hanks balanced salt solution, HBSS) were injected. Administration of CRIP-IL-12 significantly reduced tumor metastasis in liver measured by number of foci (CRIP- IL-12: 45.2 +/- 36.7, CRIP-lacZ: >250, HBSS: >250, P<.05) and by liver weight (CRIP-IL-12: 13.0+/-2.5 g, CRIP-lacZ: 30.4+/-8.5 g, HBSS: 26.0+/-7.6 g, P<.05). 3T3-IL-12, which produced only IL-12 protein but not IL-12 retrovirus, also had significant antitumor effects equivalent to CRIP-IL-12. Intra-arterial injection of IL-12--producing fibroblasts into the liver may be an effective therapy for liver tumors reducing systemic toxicity, and could be developed for clinical application.

Published

2001

12. Elevated levels of hepatocyte nuclear factor 3beta in mouse hepatocytes influence expression of genes involved in bile acid and glucose homeostasis.

Author

Rausa FM, Tan Y, Zhou H, Yoo KW, Stolz DB, Watkins SC, Franks RR, Unterman TG, and Costa RH

Subjects

ATP Binding Cassette Transporter, Subfamily B metabolism, ATP-Binding Cassette Transporters metabolism, Animals, Base Sequence, Bile Acids and Salts metabolism, Blotting, Western, Carrier Proteins metabolism, Cell Line, DNA Methylation, Glucose metabolism, Glutathione Transferase metabolism, Glycogen metabolism, Hepatocyte Nuclear Factor 3-beta, Hepatocyte Nuclear Factor 6, Homeodomain Proteins metabolism, Immunohistochemistry, Insulin-Like Growth Factor Binding Protein 1 blood, Insulin-Like Growth Factor Binding Protein 1 metabolism, Ligands, Liver embryology, Liver metabolism, Liver pathology, Mice, Mice, Transgenic, Microscopy, Electron, Models, Genetic, Molecular Sequence Data, Organic Anion Transporters, Sodium-Dependent, Phenotype, Prealbumin genetics, Prealbumin metabolism, Promoter Regions, Genetic, Protein Isoforms, Recombinant Proteins metabolism, Symporters, Time Factors, Trans-Activators metabolism, Transcription, Genetic, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Liver cytology, Membrane Transport Proteins, Nuclear Proteins genetics, Nuclear Proteins metabolism, Transcription Factors

Abstract

The winged helix transcription factor, hepatocyte nuclear factor-3beta (HNF-3beta), mediates the hepatocyte-specific transcription of numerous genes important for liver function. However, the in vivo role of HNF-3beta in regulating these genes remains unknown because homozygous null HNF3beta mouse embryos die in utero prior to liver formation. In order to examine the regulatory function of HNF-3beta, we created transgenic mice in which the -3-kb transthyretin promoter functions to increase hepatocyte expression of the rat HNF-3beta protein. Postnatal transgenic mice exhibit growth retardation, depletion of hepatocyte glycogen storage, and elevated levels of bile acids in serum. The retarded growth phenotype is likely due to a 20-fold increase in hepatic expression of insulin-like growth factor binding protein 1 (IGFBP-1), which results in elevated levels in serum of IGFBP-1 and limits the biological availability of IGFs required for postnatal growth. The defects in glycogen storage and serum bile acids coincide with diminished postnatal expression of hepatocyte genes involved in gluconeogenesis (phosphoenolpyruvate carboxykinase and glycogen synthase) and sinusoidal bile acid uptake (Ntcp), respectively. These changes in gene transcription may result from the disruptive effect of HNF-3beta on the hepatic expression of the endogenous mouse HNF-3alpha,-3beta, -3gamma, and -6 transcription factors. Furthermore, adult transgenic livers lack expression of the canalicular phospholipid transporter, mdr2, which is consistent with ultrastructure evidence of damage to transgenic hepatocytes and bile canaliculi. These transgenic studies represent the first in vivo demonstration that the HNF-3beta transcriptional network regulates expression of hepatocyte-specific genes required for bile acid and glucose homeostasis, as well as postnatal growth.

Published

2000

13. Quantitative biochemical and ultrastructural comparison of mitochondrial permeability transition in isolated brain and liver mitochondria: evidence for reduced sensitivity of brain mitochondria.

Author

Berman SB, Watkins SC, and Hastings TG

Subjects

Animals, Arsenicals pharmacology, Calcium metabolism, Calcium pharmacology, Clonazepam pharmacology, Cyclosporine pharmacology, Dose-Response Relationship, Drug, Enzyme Inhibitors pharmacology, Glutathione metabolism, Intercellular Signaling Peptides and Proteins, Male, Membrane Proteins drug effects, Mitochondria drug effects, Mitochondria, Liver drug effects, Mitochondria, Liver metabolism, Mitochondria, Liver ultrastructure, Mitochondrial Membrane Transport Proteins, Mitochondrial Permeability Transition Pore, Mitochondrial Swelling drug effects, Peptides, Phosphates metabolism, Phosphates pharmacology, Rats, Rats, Sprague-Dawley, Thiazepines pharmacology, Wasp Venoms pharmacology, tert-Butylhydroperoxide pharmacology, Brain metabolism, Clonazepam analogs & derivatives, Ion Channels, Liver metabolism, Membrane Proteins metabolism, Mitochondria metabolism, Mitochondria ultrastructure

Abstract

Opening of the mitochondrial permeability transition pore has increasingly been implicated in excitotoxic, ischemic, and apoptotic cell death, as well as in several neurodegenerative disease processes. However, much of the work directly characterizing properties of the transition pore has been performed in isolated liver mitochondria. Because of suggestions of tissue-specific differences in pore properties, we directly compared isolated brain mitochondria with liver mitochondria and used three quantitative biochemical and ultrastructural measurements of permeability transition. We provide evidence that brain mitochondria do not readily undergo permeability transition upon exposure to conditions that rapidly induce the opening of the transition pore in liver mitochondria. Exposure of liver mitochondria to transition-inducing agents led to a large, cyclosporin A-inhibitable decrease in spectrophotometric absorbance, a loss of mitochondrial glutathione, and morphologic evidence of matrix swelling and disruption, as expected. However, we found that similarly treated brain mitochondria showed very little absorbance change and no loss of glutathione. The absence of response in brain was not simply due to structural limitations, since large-amplitude swelling and release of glutathione occurred when membrane pores unrelated to the transition pore were formed. Additionally, electron microscopy revealed that the majority of brain mitochondria appeared morphologically unchanged following treatment to induce permeability transition. These findings show that isolated brain mitochondria are more resistant to induction of permeability transition than mitochondria from liver, which may have important implications for the study of the mechanisms involved in neuronal cell death., (Copyright 2000 Academic Press.)

Published

2000

14. A novel nitric oxide scavenger decreases liver injury and improves survival after hemorrhagic shock.

Author

Menezes J, Hierholzer C, Watkins SC, Lyons V, Peitzman AB, Billiar TR, Tweardy DJ, and Harbrecht BG

Subjects

Animals, Blood Pressure drug effects, Cytokines genetics, Kidney metabolism, Kidney pathology, Liver metabolism, Male, Neutrophils pathology, Ornithine Carbamoyltransferase blood, Peroxidase metabolism, RNA, Messenger metabolism, Rats, Rats, Sprague-Dawley, Shock, Hemorrhagic physiopathology, Free Radical Scavengers pharmacology, Liver drug effects, Liver pathology, Nitric Oxide antagonists & inhibitors, Shock, Hemorrhagic mortality, Shock, Hemorrhagic pathology, Thiocarbamates pharmacology

Abstract

We tested the ability of a nitric oxide (NO) scavenger to reduce tissue injury in a rodent model of hemorrhagic shock. Rats were hemorrhaged to a mean arterial blood pressure (MAP) of 40 mmHg and then resuscitated when either 30% of their shed blood had been returned (group 1) or after 100 min of continuous shock (group 2). Selected animals were treated with the NO scavenger NOX (30 mg. kg(-1). h(-1)) infused over 4 h. Hemorrhaged rats had a lower MAP after resuscitation compared with sham-shock control rats. NOX treatment significantly increased MAP after resuscitation from hemorrhage. Hemorrhagic shock also increased liver injury as reflected by elevated ornithine carbamoyltransferase (OCT) plasma levels, and NOX treatment significantly reduced OCT release. In addition, NOX was associated with significantly decreased hepatic neutrophil infiltration and improved 24-h survival (n = 8 of 9) compared with saline-treated shock animals (n = 3 of 9). These data suggest that excess NO mediates shock-induced tissue injury and that suppression of NO availability with NO scavengers may reduce the pathophysiological sequelae of severe hemorrhage.

Published

1999

15. Reactive nitrogen and oxygen radicals formed during hepatic ischemia-reperfusion kill weakly metastatic colorectal cancer cells.

Author

Jessup JM, Battle P, Waller H, Edmiston KH, Stolz DB, Watkins SC, Locker J, and Skena K

Subjects

Animals, Humans, Ischemia metabolism, Ischemia pathology, Liver blood supply, Liver metabolism, Mice, Mice, Nude, Neoplasm Transplantation pathology, Nitric Oxide metabolism, Tumor Cells, Cultured, Colorectal Neoplasms pathology, Liver pathology, Reactive Oxygen Species metabolism, Reperfusion Injury pathology

Abstract

Microscopic infarcts develop within the livers of athymic nude mice during the first 24 h after human colorectal carcinoma (CRC) cells arrest within hepatic sinusoids. Because these regions are reperfused, essentially all weakly metastatic clone A and MIP-101 CRC cells die, whereas many highly metastatic CX-1 CRC cells survive. Because hepatic sinusoidal endothelial cells kill tumor cells in vitro by producing nitric oxide, superoxide anion, and other reactive oxygen and nitrogen species, our purpose was to determine whether reoxygenation of ischemic hepatic cultures in vitro forms toxic oxygen and nitrogen radicals that kill weakly but not highly metastatic CRC cells. CRC cells (10(7)) were labeled with rhodamine-dextran and calcein AM, cultured with cells from one mouse liver in a rotating suspension culture system for up to 24 h, and the metabolic activity of the CRC cells was determined. Liver fragments oxygenated normally before harvest were not toxic to either CRC cell line, but coculture with liver made ischemic by a 3-min ligation of the portal vein and hepatic artery in vivo before harvest and then cultured in oxygenated medium killed 50-70% of weakly metastatic clone A and MIP-101 cells at 24 h but <15% of highly metastatic CX-1 cells. Inhibition of nitric oxide synthase, addition of exogenous superoxide dismutase, but not catalase or hypoxia, during coculture blocked the killing of weakly metastatic CRC cells. Thus, reoxygenation of hepatic parenchymal and nonparenchymal cells after ischemia may form toxic species that eliminate weakly metastatic CRCs within 24 h of their arrest in the liver.

Published

1999

16. Morphogenetic events in mixed cultures of rat hepatocytes and nonparenchymal cells maintained in biological matrices in the presence of hepatocyte growth factor and epidermal growth factor.

Author

Michalopoulos GK, Bowen WC, Zajac VF, Beer-Stolz D, Watkins S, Kostrubsky V, and Strom SC

Subjects

Animals, Blotting, Northern, Cell Division drug effects, Cell Fractionation, Cells, Cultured, Collagen, DNA Probes, Drug Combinations, Gene Expression Regulation, Laminin, Liver cytology, Male, Microscopy, Electron, Microscopy, Fluorescence, Proteoglycans, RNA, Messenger biosynthesis, RNA, Messenger genetics, Rats, Rats, Inbred F344, Time Factors, Epidermal Growth Factor pharmacology, Hepatocyte Growth Factor pharmacology, Liver drug effects

Abstract

Hepatocytes were grown in chemically defined hepatocyte growth medium (HGM) containing hepatocyte growth factor (HGF) and epidermal growth factor (EGF) on collagen-coated polystyrene beads in roller bottle cultures, forming clusters of beads, and proliferating hepatocytes and nonparenchymal cells, including fenestrated endothelium-forming vascular structures. Desmin-positive cells surrounded hepatocytes. Collagen types I and III were deposited in a diffuse manner whereas collagen type IV surrounded the clusters of the epithelial cells, forming a basement membrane. When the mixed cell clusters were implanted in Matrigel (Collaborative Research, Bedford, MA), hepatocytes grew in three dimensions, forming plates and ducts. Many single, long plates of hepatocytes were seen, suggesting progressive linear assembly guided by hepatocyte specific structural parameters. HGF, EGF, and transforming growth factor-alpha (TGF-alpha) enhance these phenomena. HGF plus EGF elicited maximal response. TGF-beta1 suppressed formation of the ducts and plates. Within three months in Matrigel, the cultures established monolayers composed of plates, ducts, and a well-delineated canalicular network. The mixed cultures expressed albumin, A1AT, AFP, transferrin, and CYPIIB1. Following implantation of the cell clusters in Matrigel, there was decreased expression of c-met, urokinase, urokinase receptor, and TGF-beta1. Electron microscopy showed differentiated hepatocytes with nearly normal ultrastructure. The proliferating cell nuclear antigen (PCNA) labeling index was high (more than 80%) whereas the Bromo-deoxyaridine labeling index of ongoing DNA synthesis varied from 10% to 15%. These results show that the mixed cultures of proliferating hepatocytes and nonparenchymal cells can reproduce the hallmark structures of hepatic histological architecture while maintaining differentiation and the capacity to proliferate. (HEPATOLOGY 1999;29:90-100.)

Published

1999

17. Conformational change of the catalytic subunit of glucose-6-phosphatase in rat liver during the fetal-to-neonatal transition.

Author

Puskás F, Marcolongo P, Watkins SL, Mandl J, Allan BB, Houston P, Burchell A, Benedetti A, and Bánhegyi G

Subjects

Animals, Animals, Newborn, Antibodies immunology, Catalytic Domain, Glucose metabolism, Glucose-6-Phosphatase chemistry, Glucose-6-Phosphatase immunology, Glucose-6-Phosphate metabolism, Liver embryology, Liver growth & development, Male, Microsomes, Liver enzymology, Microsomes, Liver metabolism, Phosphates metabolism, Phosphoric Monoester Hydrolases metabolism, Protein Conformation, Rats, Rats, Sprague-Dawley, Glucose-6-Phosphatase metabolism, Liver enzymology

Abstract

The glucose-6-phosphatase system was investigated in fetal rat liver microsomal vesicles. Several observations indicate that the orientation of the catalytic subunit is different in the fetal liver in comparison with the adult form: (i) the phosphohydrolase activity was not latent using glucose-6-phosphate as substrate, and in the case of other phosphoesters it was less latent; (ii) the intravesicular accumulation of glucose upon glucose-6-phosphate hydrolysis was lower; (iii) the size of the intravesicular glucose-6-phosphate pool was independent of the glucose-6-phosphatase activities; (iv) antibody against the loop containing the proposed catalytic site of the enzyme inhibited the phosphohydrolase activity in fetal but not in adult rat liver microsomes. Glucose-6-phosphate, phosphate, and glucose uptake could be detected by both light scattering and/or rapid filtration method in fetal liver microsomes; however, the intravesicular glucose-6-phosphate and glucose accessible spaces were proportionally smaller than in adult rat liver microsomes. These data demonstrate that the components of the glucose-6-phosphatase system are already present, although to a lower extent, in fetal liver, but they are functionally uncoupled by the extravesicular orientation of the catalytic subunit.

Published

1999

18. Expression of CD14 by hepatocytes: upregulation by cytokines during endotoxemia.

Author

Liu S, Khemlani LS, Shapiro RA, Johnson ML, Liu K, Geller DA, Watkins SC, Goyert SM, and Billiar TR

Subjects

Animals, CHO Cells, Cells, Cultured, Cloning, Molecular, Cricetinae, DNA, Complementary analysis, DNA, Complementary isolation & purification, Gene Expression Regulation drug effects, Gene Expression Regulation immunology, In Situ Hybridization, Interleukin-1 physiology, Lipopolysaccharide Receptors genetics, Lipopolysaccharides pharmacology, Liver cytology, Liver metabolism, Male, RNA, Messenger biosynthesis, Rats, Rats, Sprague-Dawley, Tumor Necrosis Factor-alpha physiology, Up-Regulation drug effects, Cytokines physiology, Endotoxemia immunology, Lipopolysaccharide Receptors biosynthesis, Liver immunology, Up-Regulation immunology

Abstract

Studies were undertaken to examine hepatocyte CD14 expression during endotoxemia. Our results show that lipopolysaccharide (LPS) treatment in vivo caused a marked upregulation in CD14 mRNA and protein levels in rat hepatocytes. Detectable increases in mRNA were seen as early as 1.5 h after LPS treatment; these increases peaked at 20-fold by 3 h and returned to baseline levels by 24 h. In situ hybridization localized the CD14 mRNA expression to hepatocytes both in vitro and in vivo. Increases in hepatic CD14 protein levels were detectable by 3 h and peaked at 12 h. Hepatocytes from LPS-treated animals expressed greater amounts of cell-associated CD14 protein, and more of the soluble CD14 was released by hepatocytes from LPS-treated rats in vitro. The increases in hepatocyte CD14 expression during endotoxemia occurred in parallel to increases of CD14 levels in plasma. To provide molecular identification of the hepatocyte CD14, we cloned the rat liver CD14 cDNA. The longest clone consists of a 1,591-bp insert containing a 1,116-bp open reading frame. The deduced amino acid sequence is 372 amino acids long, has 81.8 and 62.8% homology to the amino acid sequences of mouse and human CD14, respectively, and is identical to the rat macrophage CD14. The expressed CD14 protein from this clone was functional, as indicated by NF-kappaB activation in response to LPS and fluorescein isothiocyanate-LPS binding in CHO cells stably transfected with rat CD14. A nuclear run-on assay showed that CD14 transcription rates were significantly increased in hepatocytes from LPS-treated animals, indicating that the upregulation in CD14 mRNA levels observed in rat hepatocytes after LPS treatment is dependent, in part, on increased transcription. In vitro and in vivo experiments indicated that interleukin-1beta and/or tumor necrosis factor alpha participate in the upregulation of CD14 mRNA levels in hepatocytes. Our data indicate that hepatocytes express CD14 and that hepatocyte CD14 mRNA and protein levels increase rapidly during endotoxemia. Our observations also support the idea that soluble CD14 is an acute-phase protein and that hepatocytes could be a source for soluble CD14 production.

Published

1998

19. An endothelin receptor antagonist TAK-044 ameliorates carbon tetrachloride-induced acute liver injury and portal hypertension in rats.

Author

Gandhi CR, Nemoto EM, Watkins SC, and Subbotin VM

Subjects

Animals, Carbon Tetrachloride toxicity, Cells, Cultured, Endothelin-1 metabolism, Hypertension, Portal chemically induced, Hypertension, Portal pathology, Liver metabolism, Liver Cirrhosis, Experimental chemically induced, Liver Cirrhosis, Experimental pathology, Male, Rats, Rats, Sprague-Dawley, Receptors, Endothelin metabolism, Endothelin Receptor Antagonists, Endothelin-1 antagonists & inhibitors, Hypertension, Portal prevention & control, Liver drug effects, Liver Cirrhosis, Experimental prevention & control, Peptides, Cyclic pharmacology

Abstract

Hepatic levels of a powerful vasoconstrictor endothelin-1 (ET-1) and its receptors increase in human and carbon tetrachloride (CCl4)-induced liver cirrhosis. The aim of this study was to determine whether antagonism of hepatic ET-1 receptors ameliorates CCl4-induced hepatic injury and portal hypertension in rats. Acute liver injury was induced by a single intraperitoneal injection of CCl4 (0.3 ml/kg), whereas cirrhosis and portal hypertension were induced by CCl4 treatment (0.15 ml/kg twice a week) for 8 weeks. Hepatic morphology, ET-1 and its receptors, and portal venous pressures were determined. Increases in ET-1 and its receptors occurred within 24 h of CCl4 administration, and progressively thereafter during the development of cirrhosis. The acute CCl4-induced hepatic injury was characterized by significant increases in portal pressure (from 8.7+/-1.8 to 17.6+/-3.3 mmHg; p<0.01) and serum levels of liver enzymes, as well as massive hepatocellular necrosis (62+/-8%). Intravenous administration of an ET-1 receptor antagonist TAK-044 reduced portal pressure to 13.6+/-2.8 mmHg (p<0.05), and ameliorated hepatocellular necrosis by about 35% (p<0.001). TAK-044 treatment also produced significant reduction in serum levels of liver enzymes. In cirrhotic rats, portal venous infusion of TAK-044 reduced portal hypertension by about 40% (p<0.05). In conclusion, these results indicate involvement of ET-1 in acute liver injury as well as portal hypertension associated with hepatic cirrhosis, and a potential for ET-1 receptor antagonists in the treatment of these pathologic conditions.

Published

1998

20. Differential effects of nonselective nitric oxide synthase (NOS) and selective inducible NOS inhibition on hepatic necrosis, apoptosis, ICAM-1 expression, and neutrophil accumulation during endotoxemia.

Author

Ou J, Carlos TM, Watkins SC, Saavedra JE, Keefer LK, Kim YM, Harbrecht BG, and Billiar TR

Subjects

Animals, Apoptosis drug effects, DNA Fragmentation, Endotoxemia pathology, Liver drug effects, Male, Necrosis, Neutrophils drug effects, Nitrates blood, Nitric Oxide Synthase Type II, Nitric Oxide Synthase Type III, Nitrites blood, Rats, Rats, Sprague-Dawley, Endotoxemia physiopathology, Intercellular Adhesion Molecule-1 biosynthesis, Liver pathology, Liver physiopathology, NG-Nitroarginine Methyl Ester pharmacology, Neutrophils physiology, Nitric Oxide Synthase antagonists & inhibitors, omega-N-Methylarginine pharmacology

Abstract

The roles of nitric oxide derived from either the constitutive endothelial NO synthase (eNOS or NOS3) or the inducible NOS (iNOS or NOS2) in hepatic injury during endotoxemia remain controversial. To investigate this further, rats received a bolus of lipopolysaccharide (LPS) following implantation of osmotic pumps containing one of two nonselective NOS inhibitors (NMA or NAME), one of two inducible NOS inhibitors (NIL or AG), or saline. The inhibitors were infused continuously into the liver via the portal vein. Treatment of LPS-injected rats with NMA and NAME resulted in 106 and 227% increases, respectively, in circulating hepatic enzyme levels compared to LPS-treated control rats. In contrast, infusion of the iNOS-selective inhibitors had no effect on the LPS-induced hepatic necrosis. In rats receiving NAME, LPS induced greater neutrophil infiltration and ICAM-1 expression than in the LPS + saline group, whereas NIL infusion did not. The increased hepatic necrosis and PMN infiltration in the LPS + NAME group was partially prevented by a simultaneous infusion of a liver-selective NO donor. Inhibition of PMN accumulation using an anti-ICAM-1 antibody or by PMN depletion using vinblastine pretreatment, however, did not reverse the increased necrosis with NAME infusion during endotoxemia. In contrast to the assessment for necrosis, increased apoptosis was observed in the livers of LPS-treated rats receiving infusions of either NAME or NIL, but not with LPS alone. These data indicate that NO produced by eNOS may be adequate to prevent necrosis by a mechanism independent of PMN, while induced NO appears to prevent apoptosis.

Published

1997

21. Targeting nitric oxide (NO) delivery in vivo. Design of a liver-selective NO donor prodrug that blocks tumor necrosis factor-alpha-induced apoptosis and toxicity in the liver.

Author

Saavedra JE, Billiar TR, Williams DL, Kim YM, Watkins SC, and Keefer LK

Subjects

Animals, Cell Line, Cyclic GMP biosynthesis, DNA Fragmentation drug effects, Drug Design, Galactosamine pharmacology, Hemodynamics drug effects, Liver metabolism, Male, Mice, Nitric Oxide metabolism, Prodrugs administration & dosage, Prodrugs pharmacology, Rats, Rats, Sprague-Dawley, Tumor Necrosis Factor-alpha pharmacology, Tumor Necrosis Factor-alpha toxicity, Apoptosis drug effects, Drug Delivery Systems, Liver drug effects, Nitric Oxide administration & dosage, Prodrugs chemical synthesis, Pyrrolidines metabolism, Tumor Necrosis Factor-alpha antagonists & inhibitors

Abstract

We have designed a drug that protects the liver from apoptotic cell death by organ-selective pharmacological generation of the bioregulatory agent, nitric oxide (NO). The discovery strategy involved three steps: identifying a diazeniumdiolate ion (R2N[N(O)NO]-, where R2N = pyrrolidinyl) that spontaneously decomposes to NO with a very short half-life (3 s) at physiological pH; converting this ion to a series of potential prodrug derivatives by covalent attachment of protecting groups that we postulated might be rapidly removed by enzymes prevalent in the liver; and screening the prodrug candidates in vitro and in vivo to select a lead and to confirm the desired activity. Of five cell types examined, only cultured hepatocytes metabolized O2-vinyl 1-(pyrrolidin-1-yl)diazen-1-ium-1,2-diolate (V-PYRRO/NO) to NO, triggering cyclic guanosine 3',5'-monophosphate (cGMP) synthesis and protecting the hepatocytes from apoptotic cell death induced by treatment with tumor necrosis factor-alpha (TNF alpha) plus actinomycin D. In vivo, V-PYRRO/NO increased liver cGMP levels while minimally affecting systemic hemodynamics, protecting rats dosed with TNF alpha plus galactosamine from apoptosis and hepatotoxicity. The results illustrate the potential utility of diazeniumdiolates for targeting NO delivery in vivo and suggest a possible therapeutic strategy for hepatic disorders such as fulminant liver failure.

Published

1997

22. Nitric oxide protects cultured rat hepatocytes from tumor necrosis factor-alpha-induced apoptosis by inducing heat shock protein 70 expression.

Author

Kim YM, de Vera ME, Watkins SC, and Billiar TR

Subjects

Animals, Enzyme Inhibitors pharmacology, Glutathione analogs & derivatives, Glutathione metabolism, Glutathione Disulfide, Interferon-gamma pharmacology, Interleukin-1 pharmacology, Liver metabolism, Male, NF-kappa B pharmacology, Nitroso Compounds metabolism, Oligonucleotides, Antisense pharmacology, Penicillamine analogs & derivatives, Penicillamine pharmacology, Platelet Aggregation Inhibitors metabolism, Rats, Rats, Sprague-Dawley, S-Nitroso-N-Acetylpenicillamine, S-Nitrosoglutathione, Apoptosis drug effects, HSP70 Heat-Shock Proteins metabolism, Liver drug effects, Nitric Oxide pharmacology, Tumor Necrosis Factor-alpha pharmacology

Abstract

Nitric oxide (NO) and tumor necrosis factor-alpha (TNFalpha) play important roles in the pathogenesis of liver disease during acute inflammation. The present study was designed to elucidate the effect of NO pre-exposure on TNFalpha-induced hepatotoxicity. Pretreatment of primary cultures of rat hepatocytes with the NO donor S-nitroso-N-acetylpenicillamine (SNAP) induced the expression of heat shock protein 70 (HSP70) mRNA and protein, which was associated with thermotolerance and cytoprotection from TNFalpha+actinomycin D-induced hepatotoxicity and apoptosis. SNAP transiently changed the intracellular redox state by inducing glutathione (GSH) oxidation associated with the formation of S-nitrosoglutathione (GSNO). HSP70 mRNA was also induced by the GSH-oxidizing agent diamide and the GSH-conjugating agent N-ethylmaleimide, suggesting that NO induces HSP70 expression through GSH oxidation. The protective effect of SNAP pretreatment on TNFalpha-induced apoptosis correlated with the level of HSP70 expression. SNAP pretreatment inhibited reactive oxygen intermediate generation and lipid peroxidation effects that were reversed by blocking HSP70 expression using an antisense oligonucleotide to HSP70. Finally, endogenous NO formation, induced in hepatocytes stimulated with interferon-gamma and interleukin-1beta, led to the formation of GSNO and GSSG, induced HSP70, and attenuated TNFalpha-mediated cytotoxicity. These findings demonstrated that NO can induce resistance to TNFalpha-induced hepatotoxicity, possibly through the stimulation of HSP70 expression.

Published

1997

23. Inhibition of nitric oxide synthase during hemorrhagic shock increases hepatic injury.

Author

Harbrecht BG, Wu B, Watkins SC, Marshall HP Jr, Peitzman AB, and Billiar TR

Subjects

Analysis of Variance, Animals, Arginine toxicity, Blood Pressure drug effects, Disease Models, Animal, Infusions, Intravenous, Liver blood supply, Liver enzymology, Male, NG-Nitroarginine Methyl Ester, Rats, Rats, Sprague-Dawley, Resuscitation, Shock, Hemorrhagic pathology, Shock, Hemorrhagic therapy, Time Factors, Arginine analogs & derivatives, Enzyme Inhibitors toxicity, Liver drug effects, Liver Circulation drug effects, Nitric Oxide biosynthesis, Nitric Oxide Synthase antagonists & inhibitors, Shock, Hemorrhagic physiopathology

Abstract

The function of nitric oxide (NO) in hemorrhagic shock is controversial. Increased NO synthesis has been temporally correlated with severe shock and has been associated with vascular hyporeactivity to vasoconstrictor agents in isolated vascular rings. Its role in local tissue perfusion, however, is unknown. We studied the role of NO in shock-induced hepatic injury in a rodent model of decompensated hemorrhagic shock by inhibiting its synthesis with Nw-nitro-L-arginine methyl ester (L-NAME). L-NAME infusion (5 micrograms/kg/min) increased the shock-induced hepatic injury and this effect was reversible with L-arginine. L-NAME had only transient effects on systemic mean arterial blood pressure, which quickly returned to pre-L-NAME levels. We conclude that NO synthesis serves a protective function in preventing shock-induced hepatic injury and we postulate that this effect may be due to modulation of the local hepatic circulation.

Published

1995

24. Propagation of dendritic cell progenitors from normal mouse liver using granulocyte/macrophage colony-stimulating factor and their maturational development in the presence of type-1 collagen.

Author

Lu L, Woo J, Rao AS, Li Y, Watkins SC, Qian S, Starzl TE, Demetris AJ, and Thomson AW

Subjects

Animals, Antibodies, Monoclonal, Antigens, Surface analysis, Bone Marrow Cells, Cell Adhesion, Cell Aggregation, Cell Division, Cell Separation, Cells, Cultured, Culture Techniques methods, Dendritic Cells drug effects, Dendritic Cells ultrastructure, Histocompatibility Antigens Class II analysis, Immunophenotyping, Kinetics, Liver physiology, Male, Mice, Mice, Inbred C57BL, Mice, Inbred Strains, Microscopy, Electron, Recombinant Proteins pharmacology, Sheep, Stem Cells drug effects, Stem Cells ultrastructure, Collagen pharmacology, Dendritic Cells cytology, Granulocyte-Macrophage Colony-Stimulating Factor pharmacology, Liver cytology, Phagocytosis, Stem Cells cytology

Abstract

Within 1 wk of liquid culture in granulocyte/macrophage colony-stimulating factor (GM-CSF), normal B10 BR (H-2k I-E+) mouse liver nonparenchymal cells (NPC) formed loosely adherent myeloid cell clusters that have been shown to contain dendritic cell (DC) progenitors in similar studies of mouse blood or bone marrow. Mononuclear cell progeny released from these clusters at and beyond 4 d exhibited distinct dendritic morphology and were actively phagocytic. After 6-10 d of culture, these cells strongly expressed CD45, CD11b, heat stable antigen, and CD44. However, the intensity of expression of the DC-restricted markers NLDC 145, 33D1, and N418, and the macrophage marker F4/80, intercellular adhesion molecule 1, and Fc gamma RII was low to moderate, whereas the cells were negative for CD3, CD45RA, and NK1.1. Splenocytes prepared in the same way also had a similar range and intensity of expression of these immunophenotypic markers. Unlike the splenic DC, however, most of the GM-CSF-propagated putative liver DC harvested at 6-10 d expressed only a low level of major histocompatibility complex (MHC) class II (I-Ek), and they failed to induce primary allogeneic responses in naive T cells, even when propagated additionally in GM-CSF and tumor necrosis alpha and/or interferon gamma-supplemented medium. However, when 7-d cultured GM-CSF-stimulated liver cells were maintained additionally for three or more days on type-1 collagen-coated plates in the continued presence of GM-CSF, they exhibited characteristics of mature DC: MHC class II expression was markedly upregulated, mixed leukocyte reaction stimulatory activity was increased, and phagocytic function was decreased. Similar observations were made when Ia+ cells were depleted from the GM-CSF-propagated cells before exposure to collagen. Further evidence that the GM-CSF-stimulated class IIdim or class II-depleted hepatic NPC were immature DC was obtained by injecting them into allogeneic B10 (H-2b I-E-) recipients. They "homed" to T cell-dependent areas of lymph nodes and spleen where they strongly expressed donor MHC class II antigen 1-5 d later. These observations provide insight into the regulation of DC maturation, and are congruent with the possibility that the migration of immature DC from normal liver and perhaps other organ allografts may help explain their inherent tolerogenicity.

Published

1994

25. Cross species graft-versus-host disease induces hepatic injury in association with a donor-derived cellular immune response.

Author

Cooper MH, Nalesnik MA, Watkins SC, Schachter MJ, and Ildstad ST

Subjects

Animals, Bone Marrow Transplantation pathology, Chimera, Histocompatibility Antigens Class I immunology, Liver immunology, Mice, Rats, Transplantation, Heterologous pathology, Bone Marrow Transplantation immunology, Graft vs Host Disease immunology, Graft vs Host Disease pathology, Immunity, Cellular, Liver pathology, Transplantation, Heterologous immunology

Published

1993

26. Degradation of extracellular protein by the isolated perfused rat liver. A biochemical and autoradiographic study.

Author

Watkins S, Clark MG, Rogers AW, Hopgood MF, and Ballard FJ

Subjects

Animals, Autoradiography, Endocytosis, In Vitro Techniques, Kinetics, Kupffer Cells metabolism, Liver ultrastructure, Lysosomes metabolism, Male, Organoids metabolism, Protein Denaturation, Rats, Serum Albumin, Bovine metabolism, Liver metabolism, Phosphoenolpyruvate Carboxykinase (GTP) metabolism, Serum Albumin metabolism

Published

1979

27. Identification of cobalt protoporphyrin IX formation in vivo following cobalt administration to rats.

Author

Watkins S, Baron J, and Tephly TR

Subjects

Animals, Cobalt analysis, Male, Protoporphyrins analysis, Rats, Cobalt metabolism, Liver metabolism, Porphyrins metabolism, Protoporphyrins metabolism

Published

1980