Your search keyword '"Daniel Y. Hung"' showing total 23 results

1. Novel CD8+ T-Cell Subsets Demonstrating Plasticity in Patients with Inflammatory Bowel Disease

Author

Daniel Y. Hung, Herman W. Barkema, Ronald Chan, Paul L. Beck, Ji Li, Aito Ueno, Miriam Fort Gasia, Marietta Iacucci, Shem Chenoo, Michael R. Tom, Humberto Jijon, Gilaad G. Kaplan, Vijay Yajnik, Subrata Ghosh, Remo Panaccione, and Andre G. Buret

Subjects

0301 basic medicine, Adult, Male, Biopsy, Cell Plasticity, CD8-Positive T-Lymphocytes, Inflammatory bowel disease, Peripheral blood mononuclear cell, T-Lymphocytes, Regulatory, 03 medical and health sciences, Interferon-gamma, Young Adult, Calcitriol, Crohn Disease, Immunology and Allergy, Medicine, Cytotoxic T cell, Humans, Interferon gamma, Lymphocyte Count, Intestinal Mucosa, Cells, Cultured, Aged, business.industry, Interleukin-17, Gastroenterology, FOXP3, Forkhead Transcription Factors, Vitamins, Middle Aged, medicine.disease, Ulcerative colitis, digestive system diseases, 030104 developmental biology, Case-Control Studies, Immunology, Th17 Cells, Colitis, Ulcerative, Female, Interleukin 17, business, CD8, medicine.drug

Abstract

BACKGROUND Distinct CD8+ T-cell subsets such as interleukin-17-expressing Tc17 and Foxp3-expressing Tcreg are functionally similar to CD4+ T cells. Though CD4+ T cells are dysregulated in patients with inflammatory bowel disease (IBD), CD8+ T cells are not well investigated. Vitamin D is an environmental factor which influences T-cell subsets. We assessed the prevalence of CD8+ T-cell subsets among peripheral blood mononuclear cells (PBMC) and lamina propria mononuclear cells (LPMC) of patients with Crohn's disease, patients with ulcerative colitis, and healthy controls. We then tested the effect of 1α,25-dihydroxyvitamin D3 on CD8+ T-cell subsets. METHODS A total of 73 patients with Crohn's disease, 49 patients with ulcerative colitis, and 47 healthy controls were studied. LPMC or PBMC were isolated and flow cytometry was performed. CD3+ T cells, isolated from PBMC, were cultured with or without 1α,25-dihydroxyvitamin D3, before flow cytometry. RESULTS In LPMC, the prevalence of Tcreg was higher in patients with IBD (P < 0.05), whereas Tc17 were higher in patients with ulcerative colitis compared with patients with Crohn's disease and healthy controls (P < 0.05). In PBMC, both Tcreg and Tc17 were higher in patients with IBD (P < 0.01). Double-expressing interferon-γ+ interleukin-17+ and Foxp3+ interleukin-17+ CD8+ T cells were also identified indicating possible CD8+ plasticity. 1α,25-dihydroxyvitamin D3 decreased interferon-γ-expressing Tc1 (P < 0.05), but had no effect on Tc17 or Tcreg. CONCLUSIONS The prevalence of novel CD8+ T-cell subsets is altered in patients with IBD. Double-expressing cells indicate plasticity and were identified in patients with IBD. Vitamin D may have a limited effect on CD8+ T cells by decreasing interferon-γ expression.

Published

2016

2. Physiologically Based Synthetic Models of Hepatic Disposition

Author

C. Anthony Hunt, Glen E. P. Ropella, Michael S. Roberts, Daniel Y. Hung, Li Yan, Hunt, Anthony, Ropella, Glen, Yan, Li, Hung, D, and Roberts, Michael Stephen

Subjects

Physiologically based pharmacokinetic modelling, Computer science, media_common.quotation_subject, Context (language use), liver, Machine learning, computer.software_genre, Models, Biological, Hepatic disposition, Modeling and simulation, Drug pharmacokinetics, Pharmacokinetics, Humans, discrete event, modeling (modelling), agent-based, Pharmaceutical sciences, Representation (mathematics), Function (engineering), media_common, Pharmacology, Heuristic, business.industry, Event (computing), physiologically based, simulation, discreteevent, Pharmacology and Pharmaceutical Sciences, Liver, Discrete time and continuous time, Artificial intelligence, business, computer

Abstract

Current Physiologically based pharmacokinetic (PBPK) models are inductive. We present an additional, different approach that is based on the synthetic rather than the inductive approach to modeling and simulation. It relies on object-oriented programming A model of the referent system in its experimental context is synthesized by assembling objects that represent components such as molecules, cells, aspects of tissue architecture, catheters, etc. The single pass perfused rat liver has been well described in evaluating hepatic drug pharmacokinetics (PK) and is the system on which we focus. In silico experiments begin with administration of objects representing actual compounds. Data are collected in a manner analogous to that in the referent PK experiments. The synthetic modeling method allows for recognition and representation of discrete event and discrete time processes, as well as heterogeneity in organization, function, and spatial effects. An application is developed for sucrose and antipyrine, administered separately and together PBPK modeling has made extensive progress in characterizing abstracted PK properties but this has also been its limitation. Now, other important questions and possible extensions emerge. How are these PK properties and the observed behaviors generated? The inherent heuristic limitations of traditional models have hindered getting meaningful, detailed answers to such questions. Synthetic models of the type described here are specifically intended to help answer such questions. Analogous to wet-lab experimental models, they retain their applicability even when broken apart into sub-components. Having and applying this new class of models along with traditional PK modeling methods is expected to increase the productivity of pharmaceutical research at all levels that make use of modeling and simulation.

Published

2006

3. Hepatic pharmacokinetics of taurocholate in the normal and cholestatic rat liver

Author

Michael S. Roberts, Ping Chang, Gerhard A. Siebert, and Daniel Y. Hung

Subjects

Pharmacology, Cell physiology, medicine.medical_specialty, Disposition kinetics, Biology, medicine.disease, Pathophysiology, medicine.anatomical_structure, Endocrinology, Pharmacokinetics, Cholestasis, Hepatocyte, Rat liver, Internal medicine, medicine, Efflux

Abstract

1 The disposition kinetics of [H-3] taurocholate ([H-3]TC) in perfused normal and cholestatic rat livers were studied using the multiple indicator dilution technique and several physiologically based pharmacokinetic models. 2 The serum biochemistry levels, the outflow profiles and biliary recovery of [H-3] TC were measured in three experimental groups: (i) control; (ii) 17α-ethynylestradiol (EE)-treated (low dose); and (iii) EE-treated (high dose) rats. EE treatment caused cholestasis in a dose-dependent manner. 3 A hepatobiliary TC transport model, which recognizes capillary mixing, active cellular uptake, and active efflux into bile and plasma described the disposition of [H-3]TC in the normal and cholestatic livers better than the other pharmacokinetic models. 4 An estimated five- and 18-fold decrease in biliary elimination rate constant, 1.7- and 2.7-fold increase in hepatocyte to plasma efflux rate constant, and 1.8- and 2.8-fold decrease in [H-3]TC biliary recovery ratio was found in moderate and severe cholestasis, respectively, relative to normal. 5 There were good correlations between the predicted and observed pharmacokinetic parameters of [H-3]TC based on liver pathophysiology (e.g. serum bilirubin level and biliary excretion of [H-3]TC). In conclusion, these results show that altered hepatic TC pharmacokinetics in cholestatic rat livers can be correlated with the relevant changes in liver pathophysiology in cholestasis.

Published

2005

4. Assessing the cellular transmembrane electrical potential difference on the hepatic uptake of palmitate

Author

Daniel Y. Hung, Frank J. Burczynski, Ping Chang, Michael S. Roberts, Andrew L. Lewis, Gopalan Rajaraman, Guqi Wang, and Bassam M. Elmadhoun

Subjects

Male, Time Factors, Clinical Biochemistry, Palmitates, Palmitic Acid, Buffers, Ligands, Gluconates, Membrane Potentials, Rats, Sprague-Dawley, chemistry.chemical_compound, medicine, Animals, Choline, Molecular Biology, Ions, Membrane potential, Alanine, Membranes, Chromatography, Extraction (chemistry), Albumin, Depolarization, Cell Biology, General Medicine, Hyperpolarization (biology), Binding constant, Rats, Perfusion, medicine.anatomical_structure, Liver, chemistry, Hepatocyte, Hepatocytes, Chlorine, Protein Binding

Abstract

Understanding the driving forces for the hepatic uptake of endogenous and exogenous substrates in isolated cells and organs is fundamental to describing the underlying hepatic physiology/pharmacology. In this study we investigated whether uptake of plasma protein-bound [3H]-palmitate across the hepatocyte wall is governed by the transmembrane electrical potential difference (PD). Uptake was studied in isolated hepatocytes and isolated perfused rat livers (IPL). Protein-binding and vasoactive properties of the different perfusates were determined using in vitro heptane/buffer partitioning studies and the multiple indicator dilution (MID) technique in the IPL, respectively. Altering hepatocyte PD by perfusate ion substitution resulted in either a substantial depolarization (−14 ± 1 mV, n = 12, mean ± S.E., substituting choline for Na+) or hyperpolarization (−46 ± 3 mV, n = 12, mean ± S.E., substituting nitrate for Cl−). Perfusate ion substitution also affected the equilibrium binding constant for the palmitate–albumin complex. IPL studies suggested that, other than with gluconate buffer, hepatic [3H]-palmitate extraction was not affected by the buffer used, implying PD was not a determinant of extraction. [3H]-Palmitate extraction was much lower (p < 0.05) when gluconate was substituted for Cl− ion. This work contrasts with that for the extraction of [3H]-alanine where hepatic extraction fraction was significantly reduced during depolarization. Changing the albumin concentration did not affect hepatocyte PD, and [3H]-palmitate clearance into isolated hepatocytes was not affected by the buffers used. MID studies with vascular and extravascular references revealed that, with the gluconate substituted buffer, the extravascular volume possibly increased the diffusional path length thus explaining reduced [3H]-palmitate extraction fraction in the IPL. (Mol Cell Biochem 270: 115–124, 2005)

Published

2005

5. Reduced hepatic extraction of palmitate in steatosis correlated to lower level of liver fatty acid binding protein

Author

Ping Chang, Frank J. Burczynski, Gerhard A. Siebert, Daniel Y. Hung, Michael S. Roberts, Roberts, Michael Stephen, Hung, D, Siebert, Gerhard, Chang, Ping, and Burczynski, Frank

Subjects

medicine.medical_specialty, Physiology, Medical Physiology, Palmitates, Biology, Ethinyl Estradiol, Fatty Acid-Binding Proteins, Fatty acid-binding protein, Liver Fatty Acid-Binding Protein, Physiology (medical), Internal medicine, Nonalcoholic fatty liver disease, medicine, Hepatic extraction, Animals, Rats, Wistar, Hepatology, Binding protein, Fatty Acids, Fatty liver, Gastroenterology, Albumin, Estrogens, Gastroenterology & Hepatology Physiology 17 Alpha-ethynylestradiol Hepatic Palmitate Disposition Residence Time Distributions Nonalcoholic Steatohepatitis Cryptogenic Cirrhosis Rat Model Transport Disease Albumin Chain Hepatocytes, medicine.disease, Rats, Fatty Liver, Endocrinology, Liver, Female, Steatosis, Carrier Proteins

Abstract

Nonalcoholic fatty liver disease is the most common of all liver diseases. The hepatic disposition [3H]palmitate and its low-molecular-weight metabolites in perfused normal and steatotic rat liver were studied using the multiple indicator dilution technique and a physiologically based slow diffusion/bound pharmacokinetic model. The steatotic rat model was established by administration of 17α-ethynylestradiol to female Wistar rats. Serum biochemistry markers and histology of treated and normal animals were assessed and indicated the presence of steatosis in the treatment group. The steatotic group showed a significantly higher alanine aminotransferase-to-aspartate aminotransferase ratio, lower levels of liver fatty acid binding protein and cytochrome P-450, as well as microvesicular steatosis with an enlargement of sinusoidal space. Hepatic extraction for unchanged [3H]palmitate and production of low-molecular-weight metabolites were found to be significantly decreased in steatotic animals. Pharmacokinetic analysis suggested that the reduced extraction and sequestration for palmitate and its metabolites was mainly attributed to a reduction in liver fatty acid binding protein in steatosis.

Published

2005

6. Disposition Kinetics of Propranolol Isomers in the Perfused Rat Liver

Author

Ping Chang, Michael S. Roberts, Daniel Y. Hung, Gerhard A. Siebert, Yuri German Anissimov, Roberts, Michael Stephen, Hung, D, Siebert, Gerhard, Chang, Ping, and Anissimov, Yuri

Subjects

Male, Kinetics, Propranolol, In Vitro Techniques, Pharmacology, monensin, chemistry.chemical_compound, First pass effect, Isomerism, Pharmacokinetics, medicine, Animals, propranolol, Rats, Wistar, Binding site, Electrochemical gradient, optical enantiomer, Chromatography, Chemistry, Monensin, Pharmacology and Pharmaceutical Sciences, Rats, ion-trapping, Perfusion, hepatic drug distribution, Liver, stereo-selectivity, Microsome, Molecular Medicine, medicine.drug

Abstract

The aim of this study was to define the determinants of the linear hepatic disposition kinetics of propranolol optical isomers using a perfused rat liver. Monensin was used to abolish the lysosomal proton gradient to allow an estimation of propranolol ion trapping by hepatic acidic vesicles. In vitro studies were used for independent estimates of microsomal binding and intrinsic clearance. Hepatic extraction and mean transit time were determined from outflow-concentration profiles using a nonparametric method. Kinetic parameters were derived from a physiologically based pharmacokinetic model. Modeling showed an approximate 34-fold decrease in ion trapping following monensin treatment. The observed model-derived ion trapping was similar to estimated theoretical values. No differences in ion-trapping values was found between R(+)- and S(-)-propranolol. Hepatic propranolol extraction was sensitive to changes in liver perfusate flow, permeability-surface area product, and intrinsic clearance. Ion trapping, microsomal and nonspecific binding, and distribution of unbound propranolol accounted for 47.4, 47.1, and 5.5% of the sequestration of propranolol in the liver, respectively. It is concluded that the physiologically more active S()-propranolol differs from the R(+)-isomer in higher permeability-surface area product, intrinsic clearance, and intracellular binding site values.

Published

2004

7. Ion-Trapping, Microsomal Binding, and Unbound Drug Distribution in the Hepatic Retention of Basic Drugs

Author

Gerhard A. Siebert, Michael S. Roberts, Ping Chang, Daniel Y. Hung, Roberts, Michael Stephen, Siebert, Gerhard, Hung, D, and Chang, Ping

Subjects

Male, Drug, media_common.quotation_subject, Intracellular pH, Propranolol, Pharmacology, Models, Biological, chemistry.chemical_compound, lysosomes, microsomal binding, Pharmacokinetics, lipophilicity, medicine, Animals, Distribution (pharmacology), Rats, Wistar, media_common, ionisation constant, Chemistry, Monensin, Pharmacology and Pharmaceutical Sciences, Hydrogen-Ion Concentration, Atenolol, ion-trapping, Rats, drug distribution, Liver, Lipophilicity, Microsomes, Liver, Molecular Medicine, Antipyrine, medicine.drug

Abstract

This study investigated the relative contribution of ion-trapping, microsomal binding, and distribution of unbound drug as determinants in the hepatic retention of basic drugs in the isolated perfused rat liver. The ionophore monensin was used to abolish the vesicular proton gradient and thus allow an estimation of ion-trapping by acidic hepatic vesicles of cationic drugs. In vitro microsomal studies were used to independently estimate microsomal binding and metabolism. Hepatic vesicular ion-trapping, intrinsic elimination clearance, permeability-surface area product, and intracellular binding were derived using a physiologically based pharmacokinetic model. Modeling showed that the ion-trapping was significantly lower after monensin treatment for atenolol and propranolol, but not for antipyrine. However, no changes induced by monensin treatment were observed in intrinsic clearance, permeability, or binding for the three model drugs. Monensin did not affect binding or metabolic activity in vitro for the drugs. The observed ion-trapping was similar to theoretical values estimated using the pHs and fractional volumes of the acidic vesicles and the pKa values of drugs. Lipophilicity and pKa determined hepatic drug retention: a drug with low pKa and low lipophilicity (e.g., antipyrine) distributes as unbound drug, a drug with high pKa and low lipophilicity (e.g., atenolol) by ion-trapping, and a drug with a high pKa and high lipophilicity (e.g., propranolol) is retained by ion-trapping and intracellular binding. In conclusion, monensin inhibits the ion-trapping of high pKa basic drugs, leading to a reduction in hepatic retention but with no effect on hepatic drug extraction.

Published

2003

8. Fatty acid binding protein is a major determinant of hepatic pharmacokinetics of palmitate and its metabolites

Author

Gerhard A. Siebert, Frank J. Burczynski, Daniel Y. Hung, Paul P. Masci, Ping Chang, Andrew L. Lewis, Michael S. Roberts, and Yuri German Anissimov

Subjects

Male, Cytoplasm, Disposition kinetics, Physiology, Metabolite, Kinetics, Palmitates, Nerve Tissue Proteins, In Vitro Techniques, Biology, Fatty Acid-Binding Proteins, Fatty acid-binding protein, Diffusion, Palmitic acid, chemistry.chemical_compound, Cytochrome P-450 Enzyme System, Pharmacokinetics, Albumins, Physiology (medical), medicine, Animals, Tissue Distribution, Clofibrate, Rats, Wistar, Biotransformation, Hypolipidemic Agents, Hepatology, Binding protein, Gastroenterology, Proteins, Glutathione, Neoplasm Proteins, Rats, Perfusion, Liver, chemistry, Biochemistry, Microsomes, Liver, Carrier Proteins, Fatty Acid-Binding Protein 7, Algorithms, Biomarkers, medicine.drug

Abstract

Disposition kinetics of [3H]palmitate and its low-molecular-weight metabolites in perfused rat livers were studied using the multiple-indicator dilution technique, a selective assay for [3H]palmitate and its low-molecular-weight metabolites, and several physiologically based pharmacokinetic models. The level of liver fatty acid binding protein (L-FABP), other intrahepatic binding proteins (microsomal protein, albumin, and glutathione S-transferase) and the outflow profiles of [3H]palmitate and metabolites were measured in four experimental groups of rats: 1) males; 2) clofibrate-treated males; 3) females; and 4) pregnant females. A slow-diffusion/bound model was found to better describe the hepatic disposition of unchanged [3H]palmitate than other pharmacokinetic models. The L-FABP levels followed the order: pregnant female > clofibrate-treated male > female > male. Levels of other intrahepatic proteins did not differ significantly. The hepatic extraction ratio and mean transit time for unchanged palmitate, as well as the production of low-molecular-weight metabolites of palmitate and their retention in the liver, increased with increasing L-FABP levels. Palmitate metabolic clearance, permeability-surface area product, retention of palmitate by the liver, and cytoplasmic diffusion constant for unchanged [3H]palmitate also increased with increasing L-FABP levels. It is concluded that the variability in hepatic pharmacokinetics of unchanged [3H]palmitate and its low-molecular-weight metabolites in perfused rat livers is related to levels of L-FABP and not those of other intrahepatic proteins.

Published

2003

9. Quantitative evaluation of altered hepatic spaces and membrane transport in fibrotic rat liver

Author

Clay Winterford, Ping Chang, Michael S. Roberts, Daniel Y. Hung, and Kee Cheung

Subjects

Volume of distribution, Pathology, medicine.medical_specialty, Liquid diet, Hepatology, Bile acid, medicine.drug_class, Albumin, Biology, medicine.disease, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Fibrosis, Permeability (electromagnetism), Hepatocyte, medicine, Carbon tetrachloride

Abstract

Four animal models were used to quantitatively evaluate hepatic alterations in this study: (1) a carbon tetrachloride control group (phenobarbital treatment only), (2) a CCl(4)-treated group (phenobarbital with CCl(4) treatment), (3) an alcohol-treated group (liquid diet with alcohol treatment), and (4) a pair-fed alcohol control group (liquid diet only). At the end of induction, single-pass perfused livers were used to conduct multiple indicator dilution (MID) studies. Hepatic spaces (vascular space, extravascular albumin space, extravascular sucrose space, and cellular distribution volume) and water hepatocyte permeability/surface area product were estimated from nonlinear regression of outflow concentration versus time profile data. The hepatic extraction ratio of (3)H-taurocholate was determined by the nonparametric moments method. Livers were then dissected for histopathologic analyses (e.g., fibrosis index, number of fenestrae). In these 4 models, CCl(4)-treated rats were found to have the smallest vascular space, extravascular albumin space, (3)H-taurocholate extraction, and water hepatocyte permeability/surface area product but the largest extravascular sucrose space and cellular distribution volume. In addition, a linear relationship was found to exist between histopathologic analyses (fibrosis index or number of fenestrae) and hepatic spaces. The hepatic extraction ratio of (3)H-taurocholate and water hepatocyte permeability/surface area product also correlated to the severity of fibrosis as defined by the fibrosis index. In conclusion, the multiple indicator dilution data obtained from the in situ perfused rat liver can be directly related to histopathologic analyses.

Published

2002

10. Cytoplasmic binding and disposition kinetics of diclofenac in the isolated perfused rat liver

Author

Olaf Kuhlmann, Daniel Y. Hung, Michael S. Roberts, and Michael Weiss

Subjects

Pharmacology, Cytosol, chemistry.chemical_compound, chemistry, Biochemistry, Kinetics, Extracellular fluid, Biophysics, Albumin, Extracellular, Buffer solution, Intracellular, Receptor–ligand kinetics

Abstract

1 The binding kinetics of diclofenac to hepatocellular structures were evaluated in the perfused rat liver using the multiple indicator dilution technique and a stochastic model of organ transit time density. 2 The single-pass, in situ rat liver preparation was perfused with buffer solution (containing 2% albumin) at 30 ml min(-1) Diclofenac and [C-14]-sucrose (extracellular reference) were injected simultaneously as a bolus dose into the portal vein (six experiments in three rats). An analogous series of experiments was performed with [C-14]-diclofenac and [H-3]-sucrose. 3 The diclofenac outflow data were analysed using three models of intracellular distribution kinetics, assuming (1) instantaneous distribution and binding (well-mixed model), (2) 'slow' binding at specific intracellular sites after instantaneous distribution throughout the cytosol (slow binding model), and (3) 'slowing' of cytoplasmic diffusion due to instantaneous binding (slow diffusion model). 4 The slow binding model provided the best description of the data. The rate constants for cellular influx and sequestration were 0.126+/-0.026 and 0.013+/-0.009 s(-1), respectively. The estimated ratio of cellular initial distribution volume to extracellular volume of 2.82 indicates an almost instantaneous distribution in the cellular water space, while the corresponding ratio of 5.54 estimated for the apparent tissue distribution volume suggests a relatively high hepatocellular binding. The non-instantaneous intracellular equilibration process was characterized by time constants of the binding and unbinding process of 53.8 and 49.5 s, respectively. The single-pass availability of diclofenac was 86%. The results obtained with [C-14]-diclofenac and [H-3]-sucrose were not statistically different.

Published

2000

11. Hepatic structure-pharmacokinetic relationships: The hepatic disposition and metabolite kinetics of a homologous series of O-acyl derivatives of salicylic acid

Author

George D. Mellick, Daniel Y. Hung, Michael Weiss, Yuri German Anissimov, and Michael S. Roberts

Subjects

Pharmacology, Stereochemistry, Metabolite, Metabolism, High-performance liquid chromatography, Acetaminophen, chemistry.chemical_compound, chemistry, Pharmacokinetics, Lipophilicity, medicine, Salicylic acid, Drug metabolism, medicine.drug

Abstract

1. The hepatic disposition and metabolite kinetics of a homologous series of O-acyl (acetyl, propionyl, butanoyl, pentanoyl, hexanoyl and octanoyl) esters of salicylic acid (C2SA, C3SA, C4SA, C5SA, C6SA and C8SA, respectively) was determined using a single-pass, in-situ rat liver preparation. 2. The hepatic venous outflow profiles for the parent esters and the generated metabolite, salicylic acid (SA) were analysed by HPLC. Non-parametric moments analysis was used to determine the area under the curve (AUC'), mean transit time (MTT) and normalized variance (CV2) for the parent esters and generated SA. 3. Pregenerated SA ([14C]-salicylic acid) was injected into each liver with the parent ester to determine its distribution characteristics. 4. The overall recovery of ester plus metabolite was 89% of the ester dose injected and independent of the ester carbon number, suggesting that ester extraction was due to hepatic metabolism to salicylic acid. 5. The metabolite AUC' value increased directly with the lipophilicity of the parent ester (from 0.12 for C2SA to 0.95 for C8SA). By contrast, the parent AUC' decreased with the lipophilicity (from 0.85 for C2SA to zero for C8SA). The metabolite MTT value also showed a trend to increase with the lipophilicity of the parent ester (from 15.72 s for C3SA to 61.97 s for C8SA). However, the parent MTT value shows no significant change across the series. 6. The two-compartment dispersion model was used to derive the kinetic parameters for parent ester, pregenerated SA and generated SA. Consequently, these parameters were used to estimate the values of AUC', MTT and CV2 for the parent ester and metabolite. The moments values obtained using the two-compartment dispersion model show similar trends to the corresponding moments values obtained from the outflow profiles using a non-parametric approach. 7. The more lipophilic aspirin analogues are more confined to the portal circulation after oral administration than aspirin due to their more extensive hepatic elimination avoiding systemic prostacyclin inhibition. Given that aspirin's selectivity as an anti-thrombotic agent has been postulated to be due to selective anti-platelet effects in the portal circulation, the more lipophilic and highly extracted analogues are potentially more selective anti-thrombotic agents than aspirin.

Published

1998

12. Hepatic Disposition and Metabolite Kinetics of a Homologous Series of Diflunisal Esters

Author

Michael Weiss, Michael S. Roberts, Yuri German Anissimov, George D. Mellick, and Daniel Y. Hung

Subjects

Chemical Phenomena, Stereochemistry, Metabolite, Pharmaceutical Science, Diflunisal, In Vitro Techniques, Models, Biological, High-performance liquid chromatography, Rats, Sprague-Dawley, chemistry.chemical_compound, Homologous series, medicine, Animals, Tissue Distribution, Biotransformation, Chromatography, Chemistry, Physical, Hydrolysis, Anti-Inflammatory Agents, Non-Steroidal, Albumin, Rats, Bioavailability, Perfusion, Liver, chemistry, Area Under Curve, Lipophilicity, Microsomes, Liver, Female, Algorithms, Salicylic acid, medicine.drug

Abstract

The hepatic disposition and metabolite kinetics of a homologous series of diflunisal O-acyl esters (acetyl, butanoyl, pentanoyl, anti hexanoyl) were determined using a single-pass perfused in situ rat liver preparation. The experiments were conducted using 2% BSA Krebs-Henseleit buffer (pH 7.4), and perfusions were performed at 30 mL/min in each liver. O-Acyl esters of diflunisal and pregenerated diflunisal were injected separately into the portal vein. The venous outflow samples containing the esters and metabolite diflunisal were analyzed by high performance liquid chromatography (HPLC). The normalized outflow concentration-time profiles for each parent ester and the formed metabolite, diflunisal, were analyzed using statistical moments analysis and the two-compartment dispersion model. Data (presented as mean +/- standard error for triplicate experiments) was compared using ANOVA repeated measures, significance level P < 0.05. The hepatic availability (AUC'), the fraction of the injected dose recovered in the outflowing perfusate, for O-acetyldiflunisal (C2D = 0.21 +/- 0.03) was significantly lower than the other esters (0.34-0.38). However, R-N/f(u), the removal efficiency number R-N divided by the unbound fraction in perfusate f(u), which represents the removal efficiency of unbound ester by the liver, was significantly higher for the most lipophilic ester (O-hexanoyldiflunisal, C6D = 16.50 +/- 0.22) compared to the other members of the series (9.57 to 11.17). The most lipophilic ester, C6D, had the largest permeability surface area (PS) product (94.52 +/- 38.20 mt min-l g-l liver) and tissue distribution value VT (35.62 +/- 11.33 mL g(-1) liver) in this series. The MTT of these O-acyl esters of diflunisal were not significantly different from one another. However, the metabolite diflunisal MTTs tended to increase with the increase in the parent ester lipophilicity (11.41 +/- 2.19 s for C2D to 38.63 +/- 9.81 s for C6D). The two-compartment dispersion model equations adequately described the outflow profiles for the parent esters and the metabolite diflunisal formed from the O-acyl esters of diflunisal in the liver.

Published

1998

13. Synthesis, identification, characterization, stability, solubility, and protein binding of ester derivatives of salicylic acid and diflunisal

Author

Richard J Prankerd, Daniel Y. Hung, George D. Mellick, and Michael S. Roberts

Subjects

biology, Pharmaceutical Science, Diflunisal, Chemical synthesis, chemistry.chemical_compound, Hydrolysis, Acyl chloride, chemistry, biology.protein, Side chain, medicine, Organic chemistry, Bovine serum albumin, Solubility, Salicylic acid, medicine.drug

Abstract

O-Acyl esters were prepared from salicylic acid and diflunisal by esterification with the appropriate acyl anhydride (in the presence of sulfuric acid at 80°C) or acyl chloride (in the presence of pyridine at 0°C). Synthesis, identification and characterization of these compounds is described. In vitro hydrolysis, solubility and protein binding studies of these O-acyl esters were performed. For the diflunisal esters, the melting points fell as the side chain was increased from ethyl to pentyl. The melting points showed no significant difference as the length of the side chain was increased from pentyl to heptyl. The aspirin analogues showed a similar trend. The relationship between solubility and carbon chain length agreed closely with that for the melting points with carbon chain length. In vitro non-enzymatic hydrolysis studies concluded that: (1) hydrolysis rate constants generally decreased with carbon chain length; (2) the diflunisal esters have shorter half lives compared with their salicylate counterparts; and (3) the in vitro hydrolysis of these compounds was retarded by the presence of bovine serum albumin. Protein binding experiments showed that the strength of binding of the aspirin and diflunisal analogues to bovine serum albumin increased with carbon chain length.

Published

1997

14. Kinetic analysis of saturable hepatic uptake of digoxin and its inhibition by rifampicin

Author

Michael S. Roberts, Daniel Y. Hung, Michael Weiss, Klaus Poenicke, Weiss, M, Hung, D, Poenicke, Klaus, and Roberts, Michael Stephen

Subjects

Male, Digoxin, Organic anion transporter 1, Kinetics, Pharmaceutical Science, Organic Anion Transporters, Pharmacology, Michaelis–Menten kinetics, High-performance liquid chromatography, Models, Biological, polycyclic compounds, medicine, Animals, Rats, Wistar, Antibacterial agent, Protein synthesis inhibitor, biology, Chemistry, Rats, Perfusion, Liver, biology.protein, Rifampin, Rifampicin, medicine.drug

Abstract

Although the organic anion transporter Oatp2 plays a critical role in determining the hepatic clearance of some drugs, little quantitative information exists about its functional characteristics in relation to inhibition of sinusoidal drug uptake. We investigated the uptake kinetics of the Oatp2 substrate digoxin in the isolated perfused rat liver. In the single-pass perfused liver three consecutive digoxin doses of 15, 30 and 45 micorg were administered in the presence or absence of rifampicin (100 micorM), an inhibitor of Oatp2. Digoxin was determined in the outflow samples by HPLC and all data were analyzed by simultaneous nonlinear regression assuming a Michaelis-Menten uptake mechanism. Hepatocellular uptake of digoxin was concentration-dependent with a Michaelis constant (K(M)) of 577.8 ng/ml. Rifampicin significantly reduced uptake (K(M) increased 2.5-fold) without affecting other parameters.

Published

2008

15. Sa1763 1,25-Dihydroxyvitamin D3 Decreases Th1 and Tc1 Lymphocytes From the Peripheral Blood of IBD Patients and Healthy Controls Ex Vivo but Has No Effect on IL-17 or FoxP3 Expression

Author

Ronald Chan, Aito Ueno, Ji Li, Andre G. Buret, Marietta Iacucci, Shem Chenoo, Michael R. Tom, Paul L. Beck, Christina L. Hirota, Remo Panaccione, Alexander Li, Subrata Ghosh, Mailin Deane, Daniel Y. Hung, Gilaad G. Kaplan, and Miriam Fort Gasia

Subjects

Foxp3 expression, Hepatology, business.industry, Immunology, Gastroenterology, Medicine, Interleukin 17, business, Ex vivo, Peripheral blood

Published

2015

16. Mo1735 Regulation of TREM-1 and TREM-2 Protein Expression by Vitamin D in Monocyte-Derived Macrophages From Ulcerative Colitis Patients

Author

Christina L. Hirota, Daniel Y. Hung, Mailin Deane, Aito Ueno, Subrata Ghosh, Miriam Fort Gasia, Marietta Iacucci, Michael R. Tom, and Ronald Chan

Subjects

Hepatology, business.industry, Monocyte-Derived Macrophages, Immunology, Gastroenterology, Vitamin D and neurology, Medicine, business, medicine.disease, Ulcerative colitis, Protein expression

Published

2015

17. Hepatic pharmacokinetics of propranolol in rats with adjuvant-induced systemic inflammation

Author

Michael W. Whitehouse, Linda M. Fletcher, Ping Chang, Michael S. Roberts, Darrell H. G. Crawford, Gerhard A. Siebert, Daniel Y. Hung, Hung, D, Siebert, Gerhard, Chang, Ping, Whitehouse, Michael, Fletcher, Linda, Crawford, Darrell, and Roberts, Michael Stephen

Subjects

medicine.medical_specialty, Cytochrome, Physiology, Iron, Adrenergic beta-Antagonists, Medical Physiology, Orosomucoid, Propranolol, Pharmacology, In Vitro Techniques, Systemic inflammation, Oxygen Consumption, Pharmacokinetics, Cytochrome P-450 Enzyme System, Physiology (medical), Internal medicine, acidic vesicles, iron overload, ion trapping, medicine, Animals, Aspartate Aminotransferases, Chromatography, High Pressure Liquid, Cytoskeleton, Inflammation, Hepatology, biology, Gastroenterology, Cytochrome P450, Alanine Transaminase, Metabolism, Organ Size, Alkaline Phosphatase, Arthritis, Experimental, Acetaminophen, Rats, Perfusion, Endocrinology, Liver, Data Interpretation, Statistical, biology.protein, Hepatocytes, Female, medicine.symptom, Algorithms, medicine.drug

Abstract

Systemic inflammation is known to affect drug disposition in the liver. This study sought to relate and quantitate changes in hepatic pharmacokinetics of propranolol with changes in hepatic architecture and physiology in adjuvant-treated rats. Transmission electron microscopy was used to assess morphological changes in mitochondria and lysosomes of adjuvant-treated rat livers. The disposition of propranolol was assessed in the perfused rat liver using the multiple indicator dilution technique. Hepatic extraction and mean transit time were determined from outflow-concentration profiles using a nonparametric method. Kinetic parameters were derived from a two-phase physiologically based organ pharmacokinetic model. Possible relationships were then explored between the changes in hepatic drug disposition and cytochrome P-450 activity and iron concentration. Adjuvant treatment induced the appearance of mitochondrial inclusions/tubularization and irregularly shaped lysosomes in rat livers. Livers from adjuvant-treated rats had (relative to normal) significantly higher α1-acid glycoprotein (orosomucoid) and iron tissue concentrations but lower cytochrome P-450 content. The hepatic extraction, metabolism, and ion trapping of propranolol were significantly impaired in adjuvant-treated rats and could be correlated with altered iron store and cytochrome P-450 activity. It is concluded that adjuvant-induced systemic inflammation alters hepatocellular morphology and biochemistry and consequently influences hepatic disposition of propranolol.

Published

2006

18. Therapeutic effects and possible mechanisms of a snake venom preparation in the fibrotic rat liver

Author

Michael S. Roberts, Daniel Y. Hung, Kim R. Bridle, Gerhard A. Siebert, Ping Chang, Roberts, Michael Stephen, Chang, Ping, Hung, D, Siebert, Gerhard, and Bridle, Kim

Subjects

Liver Cirrhosis, Male, Taurocholic Acid, medicine.medical_specialty, Cirrhosis, Physiology, Clinical Sciences, Organic Anion Transporters, Sodium-Dependent, Organic Anion Transporters, Sodium-Independent, digestive system, complex mixtures, Microcirculation, chemistry.chemical_compound, In vivo, Fibrosis, cirrhosis - snake venom - bile salt transporters - fibrinolysis - antithrombotic, Internal medicine, Animals, Bile, Medicine, RNA, Messenger, Rats, Wistar, Carbon Tetrachloride, ATP Binding Cassette Transporter, Subfamily B, Member 11, Dose-Response Relationship, Drug, Symporters, business.industry, Gastroenterology, Fibrinogen, Membrane Transport Proteins, medicine.disease, Taurocholic acid, Rats, Thromboxane B2, Endocrinology, Liver, chemistry, Snake venom, ATP-Binding Cassette Transporters, business, Hepatic fibrosis, Liver Circulation, Snake Venoms

Abstract

The effects of a Chinese snake venom preparation from Agkistrodon halys pallas, used for treatment of hepatic fibrosis/cirrhosis in China, was investigated in an in vivo rat model and using in situ hepatic perfusion. Four groups were used in the experiments: (i) healthy, (ii) healthy/venom-treated, (iii) carbon tetrachloride (CCl4)-treated, and (iv) CCl4/venom-treated. Treatment effects were assessed by determining hepatic histopathology, biochemistry and fibrosis index parameters, bile production, biliary taurocholate recovery, hepatic mRNA expression of four bile salt transporters (Ntcp, Bsep, Oatp-1, and Oatp-3), comparison of hepatic microcirculation, fibrinolytic activity, and antithrombotic effects. Liver histopathology, biochemistry, and fibrosis index showed a dramatic improvement in venom-treated animals. There were significant differences in bile production between healthy/venom-treated and all other experimental groups and between CCl4/venom-treated and CCl4-treated animals, but no significant differences were found between CCl4/venom-treated and healthy animals. Biliary taurocholate recovery was significantly increased in healthy/venom-treated and CCl4/venom-treated animals. The expression of mRNA levels of the four bile salt transporters showed an increase after venom treatment. The hepatic microcirculation studies showed normalized sinusoidal beds in CCl4/venom-treated animals compared to healthy animals, whereas CCl4-treated animals showed abnormal profiles to the healthy and the CCl4/AHPV-treated animals. The fibrinogen and plasma thromboxane B2 levels of healthy rats decreased with increasing dose after venom treatment. It was concluded that snake venom treatment may be therapeutic in treatment of hepatic fibrosis/cirrhosis by possibly a combination of increased bile flow and improved hepatic microcirculation, changes in bile salt transporter expression, and fibrinolytic and antithrombotic effects of the snake venom preparation.

Published

2005

19. Membrane binding proteins are the major determinants for the hepatocellular transmembrane flux of long-chain fatty acids bound to albumin

Author

Frank J. Burczynski, Michael S. Roberts, Guqi Wang, Gopalan Rajaraman, and Daniel Y. Hung

Subjects

Male, Carcinoma, Hepatocellular, Serum albumin, Palmitic Acid, Pharmaceutical Science, Fatty Acid-Binding Proteins, Rats, Sprague-Dawley, Albumins, Cell Line, Tumor, medicine, Animals, Pharmacology (medical), Bovine serum albumin, Rats, Wistar, Pharmacology, chemistry.chemical_classification, biology, Organic Chemistry, Fatty Acids, Albumin, Fatty acid, Membrane Transport Proteins, Ligand (biochemistry), Transport protein, Rats, Cytosol, medicine.anatomical_structure, Biochemistry, chemistry, Liver, Hepatocyte, biology.protein, Hepatocytes, Molecular Medicine, lipids (amino acids, peptides, and proteins), Female, Biotechnology, Protein Binding

Abstract

The hepatic transmembrane flux of long-chain fatty acids (LCFA) occurs through passive and fatty acid transport protein facilitated processes from blood. The extent that these transport processes can be related to the unbound and protein-bound fractions of LCFA in blood is not clear.We used hepatocyte suspensions, hepatoma monolayers, and perfused rat livers to quantitate the transport of purified [(3)H]palmitate ([(3)H]PA) and 12-(N-methyl)-N-[(7-nitrobenz-2oxa-1,3-diazol-4yl-)amino]octadecanoicacid (12-NBDS) from solutions with a constant unbound LCFA concentration with varying bovine serum albumin (BSA) concentrations and in the presence and absence of antisera raised against cytosolic liver fatty acid binding protein (L-FABP).In the absence of L-FABP antisera, using an unbound ligand concentration that was adjusted to remain constant at each BSA concentration, hepatocyte [(3)H]PA and 12-NBDS uptake rates increased linearly with an increase in BSA concentration (p0.0001). In the presence of L-FABP antisera, [(3)H]PA uptake showed a greater reduction in the presence of 100 muM BSA than 5 muM BSA. The calculated permeability surface area product (PS) confirmed that both unbound and bound fractions of LCFA contributed to the overall flux, but only the PS for the protein-bound fraction was reduced in the presence of L-FABP antisera. In situ rat liver perfusion studies showed that the only rate process for the disposition of [(3)H]PA in the liver inhibited by L-FABP antisera was that for influx, as defined by PS, and that it reduced PS in the perfused liver by 42%.These results suggest that, at physiological albumin concentrations, most of the LCFA uptake is mediated from that bound to albumin by a hepatocyte basolateral membrane transport protein, and uptake of unbound LCFA occurring by passive diffusion contributes a minor component.

Published

2004

20. Cationic drug pharmacokinetics in diseased livers determined by fibrosis index, hepatic protein content, microsomal activity, and nature of drug

Author

Paul P. Masci, Michael Weiss, Ping Chang, Kee Cheung, Michael S. Roberts, Brett C. McWhinney, and Daniel Y. Hung

Subjects

Drug, Liver Cirrhosis, Male, media_common.quotation_subject, CCL4, Orosomucoid, Pharmacology, chemistry.chemical_compound, Pharmacokinetics, Liver Function Tests, Fibrosis, Cations, medicine, Animals, Rats, Wistar, media_common, Binding Sites, biology, Ethanol, Chemistry, Cytochrome P450, Central Nervous System Depressants, Proteins, medicine.disease, Rats, Kinetics, medicine.anatomical_structure, Liver, Pharmaceutical Preparations, Hepatocyte, biology.protein, Carbon tetrachloride, Microsomes, Liver, Molecular Medicine

Abstract

The disposition kinetics of six cationic drugs in perfused diseased and normal rat livers were determined by multiple indicator dilution and related to the drug physicochemical properties and liver histopathology. A carbon tetrachloride (CCl(4))-induced acute hepatocellular injury model had a higher fibrosis index (FI), determined by computer-assisted image analysis, than did an alcohol-induced chronic hepatocellular injury model. The alcohol-treated group had the highest hepatic alpha(1)-acid glycoprotein, microsomal protein (MP), and cytochrome P450 (P450) concentrations. Various pharmacokinetic parameters could be related to the octanol-water partition coefficient (log P(app)) of the drug as a surrogate for plasma membrane partition coefficient and affinity for MP or P450, the dependence being lower in the CCl(4)-treated group and higher in the alcohol-treated group relative to controls. Stepwise regression analysis showed that hepatic extraction ratio, permeability-surface area product, tissue-binding constant, intrinsic clearance, partition ratio of influx (k(in)) and efflux rate constant (k(out)), and k(in)/k(out) were related to physicochemical properties of drug (log P(app) or pK(a)) and liver histopathology (FI, MP, or P450). In addition, hepatocyte organelle ion trapping of cationic drugs was evident in all groups. It is concluded that fibrosis-inducing hepatic disease effects on cationic drug disposition in the liver may be predicted from drug properties and liver histopathology.

Published

2002

21. Focused antithrombotic therapy: novel anti-platelet salicylates with reduced ulcerogenic potential and higher first-pass detoxification than aspirin in rats

Author

George D. Mellick, Paul P. Masci, Michael W. Whitehouse, Michael S. Roberts, A.N. Whitaker, and Daniel Y. Hung

Subjects

Blood Platelets, Platelet Aggregation, Anti-Inflammatory Agents, Diflunisal, Prostacyclin, Pharmacology, In Vitro Techniques, Pathology and Forensic Medicine, Thromboxane A2, chemistry.chemical_compound, Fibrinolytic Agents, In vivo, medicine, Animals, Platelet, Stomach Ulcer, Rats, Wistar, Aspirin, biology, Dose-Response Relationship, Drug, General Medicine, Arthritis, Experimental, Rats, chemistry, Biochemistry, Liver, Gastric Mucosa, Inactivation, Metabolic, biology.protein, Female, Steroids, Cyclooxygenase, Salicylic acid, Platelet Aggregation Inhibitors, medicine.drug

Abstract

The use of aspirin as an anti-platelet drug is limited by its propensity to induce gastric injury and by its adverse effect on vascular prostacyclin formation. Two phenolic non-steroidal anti-inflammatory drugs (salicylic acid and diflunisal) were modified by esterification with a series of O-acyl moieties. The short-term ulcerogenic in vitro and in vivo anti-platelet properties, pharmacodynamic profiles, and extent of hepatic extraction of these phenolic esters were compared with aspirin (acetylsalicylic acid). The more lipophilic esters (longer carbon chain length in O-acyl group) show significantly less gastrotoxicity in stressed rats than does aspirin after a single oral dose. The in vitro and in vivo anti-platelet studies show that these phenolic esters inhibited (1) arachidonate-triggered human platelet aggregation and (2) thrombin-stimulated rat serum thromboxane A2 production by platelets in the clotting process almost as effectively as aspirin. The hepatic extractions of these O-acyl derivatives are significantly higher than those of aspirin. The pharmacodynamic studies show that these O-acyl derivatives of salicylic acid and diflunisal probably bind to, or combine with, the same site on the platelet cyclooxygenase as aspirin. Replacing the O-acetyl group with longer chain O-acyl moiety in this series of phenolic esters markedly reduced the potential of these agents to induce short-term gastric injury but did not lessen their activity as inhibitors of platelet aggregation. These non-acetyl salicylates may therefore represent a novel class of anti-platelet drugs with less ulcerogenic potential.

Published

1998

22. The effect of protein binding on the hepatic first pass of O-acyl salicylate derivatives in the rat

Author

Michael S. Roberts, Daniel Y. Hung, Benjamin D. Whitehead, and George D. Mellick

Subjects

Pharmacology, Chromatography, Chemistry, Albumin, Pharmaceutical Science, Serum Albumin, Bovine, Plasma protein binding, Salicylates, Bioavailability, Rats, Rats, Sprague-Dawley, First pass effect, chemistry.chemical_compound, Pharmacokinetics, Liver, Mediated transport, Lipophilicity, Animals, Female, Salicylic acid, Protein Binding

Abstract

In this work the in-situ perfused rat liver has been used to examine the effect of changing the protein content of the perfusate on the hepatic extraction of O-acyl esters of salicylic acid. The hepatic availability (F) of these solutes was studied at a flow-rate of 30 mL min−1 with perfusate albumin concentrations of 0, 2, and 4% w/v. The hepatic availability of the esters was shown to decrease with increasing carbon-chain length in the O-acyl group; for all the esters the hepatic availability increased with increasing albumin concentration in the perfusate. The dispersion-model-derived efficiency number (RN) of the esters was shown to increase with increasing lipophilicity and decrease with increasing albumin concentration in the perfusate. The unbound fraction (fu) of the esters decreased with lipophilicity. RN/fu for acetylsalicylic acid remained relatively constant as the albumin concentration was increased. However, RN/fu for n-pentanoyl-and n-hexanoylsalicylic acids increased significantly as albumin concentration increased from 0% to 4%. Thus, for the more lipophilic solutes (n-pentanoyl- and n-hexanoylsalicylic acids) the presence of albumin apparently facilitates the uptake of unbound solute relative to acetylsalicylic acid.

Published

1998

23. Therapeutic Effects and Possible Mechanisms of a Snake Venom Preparation in the Fibrotic Rat Liver.

Author

Ping Chang, Daniel Y. Hung, Gerhard A. Siebert, Kim Bridle, and Michael S. Roberts

Abstract

Abstract The effects of a Chinese snake venom preparation from Agkistrodon halys pallas, used for treatment of hepatic fibrosis/cirrhosis in China, was investigated in an {in vivo} rat model and using in situ hepatic perfusion. Four groups were used in the experiments: (i) healthy, (ii) healthy/venom-treated, (iii) carbon tetrachloride (CCl4)-treated, and (iv) CCl4/venom-treated. Treatment effects were assessed by determining hepatic histopathology, biochemistry and fibrosis index parameters, bile production, biliary taurocholate recovery, hepatic mRNA expression of four bile salt transporters (Ntcp, Bsep, Oatp-1, and Oatp-3), comparison of hepatic microcirculation, fibrinolytic activity, and antithrombotic effects. Liver histopathology, biochemistry, and fibrosis index showed a dramatic improvement in venom-treated animals. There were significant differences in bile production between healthy/venom-treated and all other experimental groups and between CCl4/venom-treated and CCl4-treated animals, but no significant differences were found between CCl4/venom-treated and healthy animals. Biliary taurocholate recovery was significantly increased in healthy/venom-treated and CCl4/venom-treated animals. The expression of mRNA levels of the four bile salt transporters showed an increase after venom treatment. The hepatic microcirculation studies showed normalized sinusoidal beds in CCl4/venom-treated animals compared to healthy animals, whereas CCl4-treated animals showed abnormal profiles to the healthy and the CCl4/AHPV-treated animals. The fibrinogen and plasma thromboxane B2 levels of healthy rats decreased with increasing dose after venom treatment. It was concluded that snake venom treatment may be therapeutic in treatment of hepatic fibrosis/cirrhosis by possibly a combination of increased bile flow and improved hepatic microcirculation, changes in bile salt transporter expression, and fibrinolytic and antithrombotic effects of the snake venom preparation. [ABSTRACT FROM AUTHOR]

Published

2005