Your search keyword '"Glenn H. Cantor"' showing total 20 results

1. Discovery and structure activity relationships of 7-benzyl triazolopyridines as stable, selective, and reversible inhibitors of myeloperoxidase

Author

Arathi Krishnakumar, Lisa M. Kopcho, Michael Basso, Benjamin P. Vokits, Glenn H. Cantor, Sutjano Jusuf, Lei Zhao, Lynn M. Abell, Ashok Dongre, Javed Khan, Steven A. Spronk, Gregory A. Locke, Gerald J. Duke, Andrew Quoc Viet, Scott A. Shaw, Franck Duclos, Ellen K. Kick, Joelle M. Onorato, Charles G. Clark, Ruth R. Wexler, Dilger Andrew K, and Ji Gao

Subjects

Hypochlorous acid, Pyridines, Clinical Biochemistry, Pharmaceutical Science, Endogeny, 01 natural sciences, Biochemistry, chemistry.chemical_compound, Structure-Activity Relationship, Thyroid peroxidase, In vivo, DNA Repair Protein, Drug Discovery, Humans, Enzyme Inhibitors, Molecular Biology, Peroxidase, biology, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Organic Chemistry, Triazoles, Antimicrobial, 0104 chemical sciences, Molecular Docking Simulation, 010404 medicinal & biomolecular chemistry, chemistry, Myeloperoxidase, biology.protein, Molecular Medicine, Triazolopyridine

Abstract

Myeloperoxidase (MPO) is a heme peroxidase found in neutrophils, monocytes and macrophages that efficiently catalyzes the oxidation of endogenous chloride into hypochlorous acid for antimicrobial activity. Chronic MPO activation can lead to indiscriminate protein modification causing tissue damage, and has been associated with chronic inflammatory diseases, atherosclerosis, and acute cardiovascular events. Triazolopyrimidine 5 is a reversible MPO inhibitor; however it suffers from poor stability in acid, and is an irreversible inhibitor of the DNA repair protein methyl guanine methyl transferase (MGMT). Structure-based drug design was employed to discover benzyl triazolopyridines with improved MPO potency, as well as acid stability, no reactivity with MGMT, and selectivity against thyroid peroxidase (TPO). Structure-activity relationships, a crystal structure of the MPO-inhibitor complex, and acute in vivo pharmacodynamic data are described herein.

Published

2020

2. Beneficial and Adverse Effects of an LXR Agonist on Human Lipid and Lipoprotein Metabolism and Circulating Neutrophils

Author

Lisa Salvador, Richard Martin, Raju Mohan, Philip Wastall, Zhaoqing Wang, John A. Lupisella, Kamelia Behnia, Paul G. Sleph, Todd G. Kirchgessner, Petia Shipkova, Gayani Fernando, Jane Zhang, Carol S. Ryan, Rongan Zhang, Shuyan Du, Tong Li, Harold Malone, Ellen K. Kick, Glenn H. Cantor, Jun Zhu, Yu Chen Barrett, Jacek Ostrowski, Long Yuan, Denise Grimm, Aiqing He, John S. Lee, Robert J.A. Frost, Mohit D. Gandhi, Ricardo Garcia, Robert J. Garmise, and Xiaoqin Liu

Subjects

Male, 0301 basic medicine, Apolipoprotein E, Apolipoprotein B, Neutrophils, Physiology, Leukocyte Count, chemistry.chemical_compound, 0302 clinical medicine, Cell Movement, Mononuclear Phagocyte System, ATP Binding Cassette Transporter, Subfamily G, Member 1, Liver X Receptors, biology, Reverse cholesterol transport, Imidazoles, Healthy Volunteers, 3. Good health, Cholesterol, Adipose Tissue, lipids (amino acids, peptides, and proteins), ATP Binding Cassette Transporter 1, Adult, Agonist, medicine.medical_specialty, Adolescent, medicine.drug_class, Lipoproteins, Hypercholesterolemia, Young Adult, 03 medical and health sciences, Therapeutic index, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Liver X receptor, Molecular Biology, Triglycerides, Macrophages, Lipid metabolism, Cell Biology, Lipid Metabolism, Rats, Mice, Inbred C57BL, Macaca fascicularis, 030104 developmental biology, Endocrinology, chemistry, biology.protein, Hydroxymethylglutaryl-CoA Reductase Inhibitors, 030217 neurology & neurosurgery

Abstract

The development of LXR agonists for the treatment of coronary artery disease has been challenged by undesirable properties in animal models. Here we show the effects of an LXR agonist on lipid and lipoprotein metabolism and neutrophils in human subjects. BMS-852927, a novel LXRβ-selective compound, had favorable profiles in animal models with a wide therapeutic index in cynomolgus monkeys and mice. In healthy subjects and hypercholesterolemic patients, reverse cholesterol transport pathways were induced similarly to that in animal models. However, increased plasma and hepatic TG, plasma LDL-C, apoB, apoE, and CETP and decreased circulating neutrophils were also evident. Furthermore, similar increases in LDL-C were observed in normocholesterolemic subjects and statin-treated patients. The primate model markedly underestimated human lipogenic responses and did not predict human neutrophil effects. These studies demonstrate both beneficial and adverse LXR agonist clinical responses and emphasize the importance of further translational research in this area.

Published

2016

3. Hepatitis C Virus NS5A Replication Complex Inhibitors: The Discovery of Daclatasvir

Author

Donald R. O'Boyle, Anjaneya Chimalakonda, Benjamin M. Johnson, Lavoie Rico, Alain Martel, James Clint A, Denis R. St. Laurent, Julie A. Lemm, Van N. Nguyen, David R. Langley, Henry S. Wong, Fukang Yang, Robert A. Fridell, Deon Daniel H, Juliang Zhu, Glenn H. Cantor, Lawrence B. Snyder, Jeffrey L. Romine, Makonen Belema, Lopez Omar D, Kenneth S. Santone, Carol Bachand, Goodrich Jason, Ruediger Edward H, Richard J. Colonno, Stephen P. Adams, Nicholas A. Meanwell, Min Gao, Aberra Fura, Lawrence G. Hamann, Dawn D. Parker, and Jay O. Knipe

Subjects

Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, Pyrrolidines, Daclatasvir, Hepatitis C virus, Hepacivirus, Viral Nonstructural Proteins, Pharmacology, Virus Replication, medicine.disease_cause, Antiviral Agents, Structure-Activity Relationship, Dogs, Pharmacokinetics, Drug Discovery, medicine, Animals, Structure–activity relationship, Replicon, Enzyme Inhibitors, NS5A, EC50, Chemistry, Drug discovery, Imidazoles, Valine, Virology, Rats, Area Under Curve, Molecular Medicine, Carbamates, medicine.drug

Abstract

The biphenyl derivatives 2 and 3 are prototypes of a novel class of NS5A replication complex inhibitors that demonstrate high inhibitory potency toward a panel of clinically relevant HCV strains encompassing genotypes 1-6. However, these compounds exhibit poor systemic exposure in rat pharmacokinetic studies after oral dosing. The structure-activity relationship investigations that improved the exposure properties of the parent bis-phenylimidazole chemotype, culminating in the identification of the highly potent NS5A replication complex inhibitor daclatasvir (33) are described. An element critical to success was the realization that the arylglycine cap of 2 could be replaced with an alkylglycine derivative and still maintain the high inhibitory potency of the series if accompanied with a stereoinversion, a finding that enabled a rapid optimization of exposure properties. Compound 33 had EC50 values of 50 and 9 pM toward genotype-1a and -1b replicons, respectively, and oral bioavailabilities of 38-108% in preclinical species. Compound 33 provided clinical proof-of-concept for the NS5A replication complex inhibitor class, and regulatory approval to market it with the NS3/4A protease inhibitor asunaprevir for the treatment of HCV genotype-1b infection has recently been sought in Japan.

Published

2014

4. Discovery of (R)-N-(3-(7-methyl-1H-indazol-5-yl)-1-(4-(1-methylpiperidin-4-yl)-1-oxopropan-2-yl)-4-(2-oxo-1,2-dihydroquinolin-3-yl)piperidine-1-carboxamide (BMS-742413): A potent human CGRP antagonist with superior safety profile for the treatment of migraine through intranasal delivery

Author

John E. Macor, Chaturvedula Prasad, Rex Denton, Gene M. Dubowchik, Paul Moench, Valerie J. Whiterock, Charlie M. Conway, Cen Xu, Neil Mathias, Glenn H. Cantor, Robert Macci, Richard Schartman, Laura J. Signor, Stephen E. Mercer, George Thalody, Carl D. Davis, Deborah Keavy, and Sokhom S. Pin

Subjects

Indazoles, medicine.drug_class, Migraine Disorders, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Peptide, Carboxamide, Respiratory Mucosa, Quinolones, Calcitonin gene-related peptide, Pharmacology, Biochemistry, chemistry.chemical_compound, Calcitonin Gene-Related Peptide Receptor Antagonists, Drug Discovery, medicine, Animals, Humans, Receptor, Molecular Biology, Administration, Intranasal, chemistry.chemical_classification, Organic Chemistry, Antagonist, Callithrix, Amides, Coronary Vessels, Rats, chemistry, Calcitonin, Face, Molecular Medicine, Nasal administration, Rabbits, Piperidine, Caco-2 Cells, Receptors, Calcitonin Gene-Related Peptide

Abstract

Calcitonin gene-related peptide (CGRP) receptor antagonists have been shown to be efficacious as abortive migraine therapeutics with the absence of cardiovascular liabilities that are associated with triptans. Herein, we report the discovery of a highly potent CGRP receptor antagonist, BMS-742413, with the potential to provide rapid onset of action through intranasal delivery. The compound displays excellent aqueous solubility, oxidative stability, and toxicological profile. BMS-742413 has good intranasal bioavailability in the rabbit and shows a robust, dose-dependent inhibition of CGRP-induced increases in marmoset facial blood flow.

Published

2013

5. Discovery of Highly Potent Liver X Receptor β Agonists

Author

William C. Stevens, John A. Lupisella, Venkataiah Bollu, Richard Martin, Denise Grimm, Rangaraj Narayanan, Max H. Nanao, Ruth R. Wexler, Raju Mohan, Xiaoping Hou, Meriah Neissel Valente, Brant Clayton Boren, Grace Yan, James Smalley, Brett B. Busch, Jacek Ostrowski, Paul G. Sleph, Yinong Xie, Barry Brock, Ira G. Schulman, A. David Rodrigues, Artur Plonowski, Glenn H. Cantor, Michael Charles Nyman, Huiping Zhang, Lam Nguyen, Ellen K. Kick, Todd G. Kirchgessner, and Kamelia Behnia

Subjects

0301 basic medicine, Agonist, biology, medicine.drug_class, Organic Chemistry, Liver X receptor alpha, Pharmacology, Biochemistry, Blood proteins, Sulfone, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, ABCG1, chemistry, ABCA1, Drug Discovery, biology.protein, medicine, lipids (amino acids, peptides, and proteins), Liver X receptor, Whole blood

Abstract

Introducing a uniquely substituted phenyl sulfone into a series of biphenyl imidazole liver X receptor (LXR) agonists afforded a dramatic potency improvement for induction of ATP binding cassette transporters, ABCA1 and ABCG1, in human whole blood. The agonist series demonstrated robust LXRβ activity (>70%) with low partial LXRα agonist activity (

Published

2016

6. Mechanistic Aspects and Novel Biomarkers of Responder and Non-Responder Phenotypes in Galactosamine-Induced Hepatitis

Author

John C. Lindon, Hector C. Keun, Michael D. Reily, Young-Shick Hong, Alan L Metz, Glenn H. Cantor, Donald G. Robertson, Jeremy K. Nicholson, Muireann Coen, Elizabeth J. Want, T. Andrew Clayton, Cynthia M Rhode, and Elaine Holmes

Subjects

Male, Galactosamine, Urine, Pharmacology, Biochemistry, Rats, Sprague-Dawley, Toxicology, Feces, chemistry.chemical_compound, medicine, Animals, Humans, Nuclear Magnetic Resonance, Biomolecular, Hepatitis, Molecular Structure, General Chemistry, Metabolism, medicine.disease, Uridine, Rats, Phenotype, Liver, chemistry, Chemical and Drug Induced Liver Injury, Xenobiotic, Viral hepatitis, Biomarkers

Abstract

The amino sugar galactosamine (galN) induces alterations in the hepatic uridine nucleotide pool and has been widely used as a model of human viral hepatitis. Histopathological and clinical chemistry analyses of a cohort of rats following administration of galN revealed extreme interindividual variability in the extent of the toxic response which enabled classification of 'responder' and 'non-responder' phenotypes. An integrative metabolic profiling approach was applied to characterize biomarkers of exposure to galN in urine, serum, feces and liver from responders and non-responders. The presence of N-acetylglucosamine and galN in the urine correlated with the occurrence and extent of toxic response. Conversely, the novel identification of galN-pyrazines in the feces of non-responders and their virtual absence in the feces of responders suggests an alternative means of distribution and metabolism of galN in non-responders. The absence of the UDP-hexosamines in the liver of non-responders further supports differential metabolism of galN and suggests an ability of non-responders to avoid UDP-glucose depletion. An observed disturbance of gut microbial derived metabolites in the urine and feces of non-responders may suggest a role of the microflora in reducing the effective dose of galN. This systems level metabonomic approach has provided new mechanistic insights into differential response to galN and is widely applicable to the study of interindividual variation in metabolism for any xenobiotic intervention.

Published

2009

7. Metabonomic investigations into the global biochemical sequelae of exposure to the pancreatic toxin 1-cyano-2-hydroxy-3-butene in the rat

Author

Muireann Coen, John C. Lindon, Olaf Beckonert, Jeremy K. Nicholson, Béla Noszál, Ákos Rácz, Glenn H. Cantor, Hector C. Keun, John A. Wijsman, Timothy M. D. Ebbels, Eszter Bohus, and Elaine Holmes

Subjects

Chemistry, Toxin, Metabolite, General Chemistry, Nuclear magnetic resonance spectroscopy, Urine, Pharmacology, medicine.disease_cause, medicine.disease, chemistry.chemical_compound, Biochemistry, medicine, Pancreatitis, General Materials Science, Xenobiotic, Two-dimensional nuclear magnetic resonance spectroscopy, Drug metabolism

Abstract

The time-related metabolic effects of 1-cyano-2-hydroxy-3-butene (CHB, crambene), a naturally occurring nitrile and experimental model toxin causing exocrine pancreatitis, have been investigated in rats using high-resolution NMR spectroscopy of urine and serum in combination with pattern recognition analysis. Rats were administered CHB subcutaneously in two doses, 15 mg/kg dose (n = 10) and 150 mg/kg (n = 10), and conventional histopathology and clinical chemistry assessments were performed. Urine samples were collected at − 16 and 0, 8, 24, 48, 72, 96, 120, 144 and 168 h postdosing and serum samples were collected at 48 and 168 h postdosing; these were analyzed using a range of 1D and 2D NMR spectroscopic methods. The metabolic profile perturbations seen throughout the time-course of the study are described, and the application of the spectral correlation technique Statistical TOtal Correlation SpectroscopY (STOCSY) to detect both structural and novel toxicological connectivities between xenobiotic and endogenous metabolite signals is illustrated for the first time. As a result, it is suggested that the STOCSY approach may be of wider application in the identification of toxic versus nontoxic metabolites in drug metabolism studies. Copyright © 2009 John Wiley & Sons, Ltd.

Published

2009

8. Metabonomics evaluation of urine from rats given acute and chronic doses of acetaminophen using NMR and UPLC/MS

Author

Laura K. Schnackenberg, Jinchun Sun, Richard D. Beger, Yvonne P. Dragan, Glenn H. Cantor, Thomas C. Schmitt, and Ricky D. Holland

Subjects

Male, Metabolite, Clinical Biochemistry, medicine.disease_cause, Biochemistry, High-performance liquid chromatography, Mass Spectrometry, Analytical Chemistry, Rats, Sprague-Dawley, Necrosis, chemistry.chemical_compound, Metabolomics, Trigonelline, medicine, Animals, Antipyretic, Nuclear Magnetic Resonance, Biomolecular, Chromatography, High Pressure Liquid, Acetaminophen, Chromatography, Liver Diseases, digestive, oral, and skin physiology, Computational Biology, Cell Biology, General Medicine, Rats, Metabolism, Liver, chemistry, Chemical and Drug Induced Liver Injury, Drug metabolism, Oxidative stress, medicine.drug

Abstract

Urinary metabolic perturbations associated with acute and chronic acetaminophen-induced hepatotoxicity were investigated using nuclear magnetic resonance (NMR) spectroscopy and ultra performance liquid chromatography/mass spectrometry (UPLC/MS) metabonomics approaches to determine biomarkers of hepatotoxicity. Acute and chronic doses of acetaminophen (APAP) were administered to male Sprague-Dawley rats. NMR and UPLC/MS were able to detect both drug metabolites and endogenous metabolites simultaneously. The principal component analysis (PCA) of NMR or UPLC/MS spectra showed that metabolic changes observed in both acute and chronic dosing of acetaminophen were similar. Histopathology and clinical chemistry studies were performed and correlated well with the PCA analysis and magnitude of metabolite changes. Depletion of antioxidants (e.g. ferulic acid), trigonelline, S -adenosyl- l -methionine, and energy-related metabolites indicated that oxidative stress was caused by acute and chronic acetaminophen administration. Similar patterns of metabolic changes in response to acute or chronic dosing suggest similar detoxification and recovery mechanisms following APAP administration.

Published

2008

9. Metabonomic evaluation of idiosyncrasy-like liver injury in rats cotreated with ranitidine and lipopolysaccharide

Author

George G. Harrigan, Glenn H. Cantor, Gary L. Cockerell, Robert A. Roth, Patricia E. Ganey, Roy H. Bible, Gregory N. Cosma, James P. Luyendyk, Alan P. Breau, Jane F. Maddox, and Royston Goodacre

Subjects

Lipopolysaccharides, Male, Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, Lipopolysaccharide, medicine.drug_class, Biology, Pharmacology, Ranitidine, Toxicology, Rats, Sprague-Dawley, chemistry.chemical_compound, Liver Function Tests, medicine, Animals, Aspartate Aminotransferases, Liver injury, Principal Component Analysis, medicine.diagnostic_test, Discriminant Analysis, Alanine Transaminase, medicine.disease, Receptor antagonist, Rats, Histamine H2 Antagonists, Liver, chemistry, Alanine transaminase, Toxicity, biology.protein, Chemical and Drug Induced Liver Injury, Liver function tests, Histamine, medicine.drug

Abstract

Idiosyncratic liver injury occurs in a small fraction of people on certain drug regimens. The cause of idiosyncratic hepatotoxicity is not known; however, it has been proposed that environmental factors such as concurrent inflammation initiated by bacterial lipopolysaccharide (LPS) increase an individual's susceptibility to drug toxicity. Ranitidine (RAN), a histamine-2 receptor antagonist, causes idiosyncratic liver injury in humans. In a previous report, idiosyncrasy-like liver toxicity was created in rats by cotreating them with LPS and RAN. In the present study, the ability of metabonomic techniques to distinguish animals cotreated with LPS and RAN from those treated with each agent individually was investigated. Rats were treated with LPS or its vehicle and with RAN or its vehicle, and urine was collected for nuclear magnetic resonance (NMR)- and mass spectroscopy-based metabonomic analyses. Blood and liver samples were also collected to compare metabonomic results with clinical chemistry and histopathology. NMR metabonomic analysis indicated changes in the pattern of metabolites consistent with liver damage that occurred only in the LPS/RAN cotreated group. Principal component analysis of urine spectra by either NMR or mass spectroscopy produced a clear separation of the rats treated with LPS/RAN from the other three groups. Clinical chemistry (serum alanine aminotransferase and aspartate aminotransferase activities) and histopathology corroborated these results. These findings support the potential use of a noninvasive metabonomic approach to identify drug candidates with potential to cause idiosyncratic liver toxicity with inflammagen coexposure.

Published

2006

10. Unique Gene Expression and Hepatocellular Injury in the Lipopolysaccharide-Ranitidine Drug Idiosyncrasy Rat Model: Comparison with Famotidine

Author

Jane F. Maddox, David M. Nelson, Patricia E. Ganey, Vasanthi Bhaskaran, Glenn H. Cantor, Robert A. Roth, Bruce D. Car, Lois D. Lehman-McKeeman, James P. Luyendyk, and Timothy P. Reilly

Subjects

Lipopolysaccharides, Male, Lipopolysaccharide, Enzyme-Linked Immunosorbent Assay, Inflammation, Pharmacology, Ranitidine, Toxicology, Polymerase Chain Reaction, Rats, Sprague-Dawley, chemistry.chemical_compound, Gene expression, medicine, Animals, Drug Interactions, Interleukin 6, Oligonucleotide Array Sequence Analysis, Liver injury, biology, business.industry, Gene Expression Profiling, Famotidine, medicine.disease, Rats, Gene expression profiling, Gene Expression Regulation, Histamine H2 Antagonists, Liver, chemistry, Plasminogen activator inhibitor-1, Immunology, biology.protein, medicine.symptom, business, medicine.drug

Abstract

Rats cotreated with lipopolysaccharide (LPS) and ranitidine (RAN) but not LPS and famotidine (FAM) develop hepatocellular injury in an animal model of idiosyncratic drug reactions. Evaluation of liver gene expression in rats given LPS and/or RAN led to confirmation that the hemostatic system, hypoxia, and neutrophils (PMNs) are critical mediators in LPS/RAN-induced liver injury. We tested the hypothesis that unique gene expression changes distinguish LPS/RAN-treated rats from rats given LPS or RAN alone and from those cotreated with LPS/FAM. Rats were treated with a nonhepatotoxic dose of LPS (44.4 x 10(6) endotoxin units/kg, iv) or its vehicle. Two hours thereafter they were given RAN (30 mg/kg, iv), FAM (either 6 mg/kg, a pharmacologically equi-efficacious dose, or 28.8 mg/kg, an equimolar dose, iv), or vehicle. They were killed 2 or 6 h after drug treatment for evaluation of hepatotoxicity (2 and 6 h) and liver gene expression (2 h only). At a time before the onset of hepatocellular injury, hierarchical clustering distinguished rats treated with LPS/RAN from those given LPS alone. 205 probesets were expressed differentially to a greater or lesser degree only in LPS/RAN-treated rats compared to LPS/FAM or LPS alone, which did not develop liver injury. These included VEGF, EGLN3, MAPKAPK-2, BNIP3, MIP-2, COX-2, EGR-1, PAI-1, IFN-gamma, and IL-6. Expression of these genes was confirmed by real-time PCR. Serum concentrations of MIP-2, PAI-1, IFN-gamma, and IL-6 correlated with their respective gene expression patterns. Overall, the expression of several gene products capable of controlling requisite mediators of injury (i.e., hemostasis, hypoxia, PMNs) in this model were enhanced in livers of LPS/RAN-treated rats. Furthermore, enhanced expression of MAPKAPK-2 in RAN-treated rats and its target genes in LPS/RAN-treated rats suggests that p38/MAPKAPK-2 signaling is a regulation point for enhancement of LPS-induced gene expression by RAN.

Published

2006

11. Coagulation-Dependent Gene Expression and Liver Injury in Rats Given Lipopolysaccharide with Ranitidine but Not with Famotidine

Author

Jane F. Maddox, David M. Nelson, Bruce D. Car, Lois D. Lehman-McKeeman, James P. Luyendyk, Timothy P. Reilly, Vasanthi Bhaskaran, Glenn H. Cantor, Patricia E. Ganey, Robert A. Roth, and Xiaomin Deng

Subjects

Lipopolysaccharides, Male, Lipopolysaccharide, Gene Expression, Inflammation, Pharmacology, Ranitidine, Rats, Sprague-Dawley, chemistry.chemical_compound, Gene expression, medicine, Animals, RNA, Messenger, Blood Coagulation, Oligonucleotide Array Sequence Analysis, Liver injury, Heparin, business.industry, Famotidine, medicine.disease, Rats, Histamine H2 Antagonists, Liver, chemistry, Immunology, Molecular Medicine, Chemical and Drug Induced Liver Injury, medicine.symptom, business, Plasminogen activator, medicine.drug

Abstract

In an animal model of drug idiosyncrasy, rats cotreated with nonhepatotoxic doses of lipopolysaccharide (LPS) and ranitidine (RAN) develop hepatocellular injury, whereas rats treated with LPS and famotidine (FAM) do not. The coagulation system and neutrophils (PMNs) are requisite mediators of LPS/RAN-induced liver injury. We tested the hypothesis that unique gene expression in LPS/RAN-treated rats requires coagulation system activation and that these changes are absent in rats given LPS and FAM. Rats were treated with a nonhepatotoxic dose of LPS (44.4 x 10(6) endotoxin units/kg i.v.) or its vehicle, and then 1 h later, they were treated with heparin (3000 U/kg) or its vehicle. One hour thereafter, they were given RAN (30 mg/kg), FAM (6 mg/kg, a pharmacologically equiefficacious dose, or 28.8 mg/kg, an equimolar dose), or vehicle (i.v.). They were killed 2 or 6 h after drug treatment for evaluation of hepatotoxicity, coagulation system activation, and liver gene expression (2 h only). Statistical filtering of gene array results and real-time polymerase chain reaction identified groups of genes expressed in LPS/RAN-treated rats but not LPS/FAM-treated rats that were either changed or unchanged by heparin administration. For example, LPS/RAN-induced mRNA expression of the inflammatory mediators interleukin-6, cyclooxygenase-2, and macrophage inflammatory protein-2 (MIP-2) was reduced by anticoagulation. Enhancement of serum MIP-2 and plasminogen activator inhibitor-1 concentrations in LPS/RAN-treated rats was prevented by anticoagulation. The results suggest cross-talk between hemostasis-induced gene expression and inflammation (e.g., PMN function) in the genesis of hepatocellular injury in LPS/RAN-treated rats. In contrast, neither the expression of such genes nor hepatocellular necrosis occurred in rats treated with LPS/FAM.

Published

2006

12. Integrated histopathological and urinary metabonomic investigation of the pathogenesis of microcystin-LR toxicosis

Author

John C. Lindon, Roy H. Bible, Mary E. Bollard, J. A. Wijsman, Olaf Beckonert, Hector C. Keun, Glenn H. Cantor, Elaine Holmes, Timothy M. D. Ebbels, Jeremy K. Nicholson, Alan P. Breau, Henrik Antti, and Gary L. Cockerell

Subjects

Male, Magnetic Resonance Spectroscopy, Microcystis, Time Factors, Microcystins, Urinary system, Physiology, Endogeny, Microcystin-LR, Urine, Biology, medicine.disease_cause, Kidney, Pathogenesis, Neovascularization, Bile Acids and Salts, Rats, Sprague-Dawley, chemistry.chemical_compound, medicine, Animals, Metabolomics, Enzyme Inhibitors, General Veterinary, Toxin, Urocanic Acid, Rats, chemistry, Biochemistry, Liver, Biomarker (medicine), Marine Toxins, medicine.symptom, Injections, Intraperitoneal

Abstract

Patterns of change of endogenous metabolites may closely reflect systemic and organ-specific toxic changes. The authors examined the metabolic effects of the cyanobacterial (blue-green algal) toxin microcystin-LR by 1H-nuclear magnetic resonance (NMR) analysis of urinary endogenous metabolites. Rats were treated with a single sublethal dose, either 20 or 80 µg/kg intraperitoneally, and sacrificed at 2 or 7 days post dosing. Changes in the high-dose, 2-day sacrifice group included centrilobular hepatic necrosis and congestion, accompanied in some animals by regeneration and neovascularization. By 7 days, animals had recovered, the necrotizing process had ended, and the centrilobular areas had been replaced by regenerative, usually hypertrophic hepatocytes. There was considerable interanimal variation in the histologic process and severity, which correlated with the changes in patterns of endogenous metabolites in the urine, thus providing additional validation of the biomarker and biochemical changes. Similarity of the shape of the metabolic trajectories suggests that the mechanisms of toxic effects and recovery are similar among the individual animals, albeit that the magnitude and timing are different for the individual animals. Initial decreases in urinary citrate, 2-oxoglutarate, succinate, and hippurate concentrations were accompanied by a temporary increase in betaine and taurine, then creatine from 24 to 48 hours. Further changes were an increase in guanidinoacetate, dimethylglycine, urocanic acid, and bile acids. As a tool, urine can be repeatedly and noninvasively sampled and metabonomics utilized to study the onset and recovery after toxicity, thus identifying time points of maximal effect. This can help to employ histopathological examination in a guided and effective fashion.

Published

2012

13. Urinary metabolites of 2-bromoethanamine identified by stable isotope labelling: evidence for carbamoylation and glutathione conjugation

Author

Serhiy Hnatyshyn, John C. Lindon, Nelly Aranibar, Lois D. Lehman-McKeeman, Glenn H. Cantor, Muireann Coen, Petia Shipkova, T. Andrew Clayton, Jeremy K. Nicholson, Jeffrey D. Vassallo, Elaine Holmes, Mark Sanders, and Haiying Zhang

Subjects

Male, Time Factors, Health, Toxicology and Mutagenesis, Renal papillary necrosis, Toxicology, Kidney, Biochemistry, Nephrotoxicity, Rats, Sprague-Dawley, chemistry.chemical_compound, Liquid chromatography–mass spectrometry, Labelling, medicine, Ethylamines, Animals, Amino Acids, Pharmacology, chemistry.chemical_classification, Chemistry, General Medicine, Metabolism, Glutathione, medicine.disease, Amino acid, Rats, Isotope Labeling, Toxicity, Carbamates

Abstract

2-Bromoethanamine (BEA) causes renal papillary necrosis (RPN) in rats after a single dose and has been widely used as a model compound for studying the lesion. Although the metabolism of BEA may be an important determinant of toxicity, the metabolic fate of the compound has not been fully elucidated. To date, the only identified BEA metabolites are aziridine, 2-oxazolidone and 5-hydroxy-2-oxazolidone. In this study, stable isotope labelling (SIL) of BEA analogs ((¹³C and ²H) were used to differentiate generated BEA metabolites from endogenous molecules which enabled the accurate liquid chromatography mass spectrometry detection of more than 180 novel metabolites. BEA metabolism was evaluated in rats after acute administration of a non-toxic dose (50 mg/kg) and a toxic dose (250 mg/kg) that caused frank RPN and polyuria. Newly identified metabolites include three carbamoylation products, two mercapturic acids and a group of amino acid conjugates. Overall, the results indicate that BEA metabolism is very complex, suggest the potential formation of reactive intermediates and establish that BEA is subject to conjugation with glutathione. The results also demonstrate the utility and sensitivity of the SIL approach for identification of metabolites from small, reactive compounds.

Published

2010

14. Bacterial- and viral-induced inflammation increases sensitivity to acetaminophen hepatotoxicity

Author

James J. Pestka, Christopher F. Cuff, Glenn H. Cantor, Erica M. Sparkenbaugh, Sandra W. Newport, Patricia E. Ganey, Maoxiang Li, Robert A. Roth, Chidozie J. Amuzie, and Jane F. Maddox

Subjects

Lipopolysaccharides, Male, Lipopolysaccharide, Neutrophils, Health, Toxicology and Mutagenesis, Inflammation, Pharmacology, Toxicology, chemistry.chemical_compound, Mice, Medicine, Animals, Acetaminophen, Liver injury, Mice, Inbred BALB C, Dose-Response Relationship, Drug, business.industry, Tumor Necrosis Factor-alpha, Centrilobular necrosis, digestive, oral, and skin physiology, medicine.disease, Glutathione, Reoviridae Infections, Mice, Inbred C57BL, Dose–response relationship, chemistry, Liver, Immunology, Cytokines, Tumor necrosis factor alpha, Female, medicine.symptom, business, Viral hepatitis, medicine.drug

Abstract

Acetaminophen (APAP)-induced hepatotoxicity accounts for nearly half of acute liver failure cases in the United States. The doses that produce hepatotoxicity vary considerably and many risk factors have been proposed, including liver inflammation from viral hepatitis. Interestingly, inflammatory stress from another stimulus, bacterial endotoxin (lipopolysaccharide, LPS), renders the liver more sensitive to hepatotoxicity from numerous xenobiotic agents. The purpose of these studies was to test the hypothesis that inflammation induced by LPS or infection with reovirus increases sensitivity to APAP-induced liver injury. For LPS-induced inflammation, C57BL/6J mice were treated with either saline or LPS (44 x 10(6) EU/kg, ip) 2 h before treatment with APAP (100-400 mg/kg, ip) or saline. No elevation in serum alanine aminotransferase (ALT) activity was observed in mice that received vehicle or LPS alone. LPS co-treatment produced a leftward shift of the dose-response curve for APAP-induced hepatotoxicity and led to significantly greater tumor necrosis factor-alpha (TNF) production than APAP alone. Reovirus serotype 1 (10(8) PFU, iv) induced inflammation in Balb/c mice as evidenced by increases in hepatic mRNAs for macrophage inhibitory protein-2, interleukin-6, and TNF. Co-administration of reovirus and APAP at doses of 450 and 700 mg/kg (2 h after reovirus) led to increases in serum ALT activity, whereas neither reovirus nor APAP alone produced liver injury. Consistent with the increases in serum ALT activity, histopathologic examination revealed centrilobular necrosis with marked neutrophilic accumulation only in livers of mice treated with LPS/APAP or with reovirus/APAP. The results suggest that normally noninjurious doses of APAP are rendered hepatotoxic by modest inflammation, whether bacterial or viral in origin.

Published

2009

15. NMR-based metabolic profiling identifies biomarkers of liver regeneration following partial hepatectomy in the rat

Author

Hector C. Keun, Timothy M. D. Ebbels, Mary E. Bollard, Olaf Beckonert, John C. Lindon, Leon M. Smith, Glenn H. Cantor, Lois D. Lehman-McKeeman, Nancy R Contel, Jeremy K. Nicholson, and Elaine Holmes

Subjects

Male, Taurine, medicine.medical_specialty, medicine.medical_treatment, Biology, Urine, Creatine, Biochemistry, Dimethylglycine, Rats, Sprague-Dawley, chemistry.chemical_compound, Internal medicine, medicine, Choline, Animals, Hepatectomy, Metabolomics, Nuclear Magnetic Resonance, Biomolecular, Histocytochemistry, Fatty liver, Body Weight, Lipid metabolism, General Chemistry, Organ Size, medicine.disease, Liver regeneration, Liver Regeneration, Rats, Endocrinology, chemistry, Liver, Biomarkers, Blood Chemical Analysis

Abstract

Tissue injury and repair are often overlapping consequences of disease or toxic exposure, but are not often considered as distinct processes in molecular studies. To establish the systemic metabolic response to liver regeneration, the partial hepatectomy (PH) model has been studied in the rat by an integrated metabonomics strategy, utilizing (1)H NMR spectroscopy of urine, liver and serum. Male Sprague-Dawley rats were subjected to either surgical removal of approximately two-thirds of the liver, sham operated (SO) surgery, or no treatment (n = 10/group) and samples collected over a 7 day period. A number of urinary metabolic perturbations were observed in PH rats compared with SO and control animals, including elevated levels of taurine, hypotaurine, creatine, guanidinoacetic acid, betaine, dimethylglycine and bile acids. Serum betaine and creatine were also elevated after PH, while levels of triglyceride were reduced. In the liver, triglycerides, cholesterol, alanine and betaine were elevated after PH, while choline and its derivatives were reduced. Upon examining the dynamic pattern of urinary response (the 'metabolic trajectory'), several metabolites could be categorized into groups likely to reflect perturbations to different processes such as dietary intake or hepatic 1-carbon metabolism. Several of the urinary perturbations observed during the regenerative phase of the PH model have also been observed after exposure to liver toxins, indicating that hepatic regeneration may make a contribution to the systemic alterations in metabolism associated with hepatotoxicity. The observed changes in 1-carbon and lipid metabolism are consistent with the proposed role of these pathways in the activation of a regenerative response and provide further evidence regarding the utility of urinary NMR profiles in the detection of liver-specific pathology. Biofluid (1)H NMR-based metabolic profiling provides new insight into the role of metabolism of liver regeneration, and suggests putative biomarkers for the noninvasive monitoring of the regeneration process.

Published

2009

16. Comparative metabonomics of differential hydrazine toxicity in the rat and mouse

Author

Mary E. Bollard, Olaf Beckonert, John P. Shockcor, Jeremy K. Nicholson, Hector C. Keun, Glenn H. Cantor, Elaine Holmes, Timothy M. D. Ebbels, Henrik Antti, John C. Lindon, Andrew W. Nicholls, and Greg Stevens

Subjects

Male, Magnetic Resonance Spectroscopy, Time Factors, Hydrochloride, Ratón, Administration, Oral, Urine, Pharmacology, Toxicology, Mass Spectrometry, Excretion, Rats, Sprague-Dawley, chemistry.chemical_compound, Mice, Species Specificity, Liquid chromatography–mass spectrometry, Citrulline, Toxicity Tests, Acute, Animals, Hydrazine (antidepressant), Principal Component Analysis, Liver Diseases, Organ Size, Rats, Hydrazines, chemistry, Biochemistry, Liver, Toxicity, Chemical and Drug Induced Liver Injury, Chromatography, Liquid

Abstract

Interspecies variation between rats and mice has been studied for hydrazine toxicity using a novel metabonomics approach. Hydrazine hydrochloride was administered to male Sprague-Dawley rats (30 mg/kg, n = 10 and 90 mg/kg, n = 10) and male B6C3F mice (100 mg/kg, n = 8 and 250 mg/kg, n = 8) by oral gavage. In each species, the high dose was selected to produce the major histopathologic effect, hepatocellular lipid accumulation. Urine samples were collected at sequential time points up to 168 h post dose and analyzed by 1H NMR spectroscopy. The metabolites of hydrazine, namely diacetyl hydrazine and 1,4,5,6-tetrahydro-6-oxo-3-pyridazine carboxylic acid (THOPC), were detected in both the rat and mouse urine samples. Monoacetyl hydrazine was detected only in urine samples from the rat and its absence in the urine of the mouse was attributed to a higher activity of N-acetyl transferases in the mouse compared with the rat. Differential metabolic effects observed between the two species included elevated urinary beta-alanine, 3-D-hydroxybutyrate, citrulline, N-acetylcitrulline, and reduced trimethylamine-N-oxide excretion unique to the rat. Metabolic principal component (PC) trajectories highlighted the greater degree of toxic response in the rat. A data scaling method, scaled to maximum aligned and reduced trajectories (SMART) analysis, was used to remove the differences between the metabolic starting positions of the rat and mouse and varying magnitudes of effect, to facilitate comparison of the response geometries between the rat and mouse. Mice followed "biphasic" open PC trajectories, with incomplete recovery 7 days after dosing, whereas rats followed closed "hairpin" time profiles, indicating functional reversibility. The greater magnitude of metabolic effects observed in the rat was supported by the more pronounced effect on liver pathology in the rat when compared with the mouse.

Published

2004

17. Contemporary issues in toxicology the role of metabonomics in toxicology and its evaluation by the COMET project

Author

Hector C. Keun, Timothy M. D. Ebbels, Alan P. Breau, John C. Lindon, Donald G. Robertson, Peter Luke, Mary E. Bollard, Olaf Beckonert, Ali Loukaci, Elaine Holmes, Steen Møller Laursen, Henrik Antti, Jeremy K. Nicholson, Urs Niederhauser, Bruce D. Car, Michael D. Reily, Hans Senn, Ulla G. Sidelmann, Lois D. Lehman-McKeeman, Roy H. Bible, Glenn H. Cantor, Adrienne A. Tymiak, Craig E. Thomas, Gregory J. Stevens, Jean-Marie Colet, and Goetz Schlotterbeck

Subjects

Pharmacology, Magnetic Resonance Spectroscopy, Kidney Toxicity, Databases, Factual, Chemistry, Liver and kidney, Drug Evaluation, Preclinical, Serum samples, Toxicology, Rats, Xenobiotics, Chemometrics, Mice, Blood serum, Metabolism, Biological variation, Toxicity, Biochemical composition, Animals, Humans

Abstract

The role that metabonomics has in the evaluation of xenobiotic toxicity studies is presented here together with a brief summary of published studies. To provide a comprehensive assessment of this approach, the Consortium for Metabonomic Toxicology (COMET) has been formed between six pharmaceutical companies and Imperial College of Science, Technology and Medicine (IC), London, UK. The objective of this group is to define methodologies and to apply metabonomic data generated using H-1 NMR spectroscopy of urine and blood serum for preclinical toxicological screening of candidate drugs. This is being achieved by generating databases of results for a wide range of model toxins which serve as the raw material for computer-based expert systems for toxicity prediction. The project progress on the generation of comprehensive metabonomic databases and multivariate statistical models for prediction of toxicity, initially for Ever and kidney toxicity in the rat and mouse, is reported. Additionally, both the analytical and biological variation which might arise through the use of metabonomics has been evaluated. An evaluation of intersite NMR analytical reproducibility has revealed a high degree of robustness. Second, a detailed comparison has been made of the ability of the six companies to provide consistent urine and serum samples using a study of the toxicity of hydrazine at two doses in the male rat, this study showing a high degree of consistency between samples from the various companies in terms of spectral patterns and biochemical composition. Differences between samples from the various companies were small compared to the biochemical effects of the toxin. A metabonomic model has been constructed for urine from control rats, enabling identification of outlier samples and the metabolic reasons for the deviation. Building on this success, and with the completion of studies on approximately 80 model toxins, first expert systems for prediction of liver and kidney toxicity have been generated. (C) 2003 Elsevier Science (USA). All rights reserved.

Published

2003

18. Bovine leukemia virus gp30 transmembrane (TM) protein is not tyrosine phosphorylated: examining potential interactions with host tyrosine-mediated signaling

Author

Suzanne M. Pritchard, Glenn H. Cantor, Diana M. Stone, and Valerie T Hamilton

Subjects

Cancer Research, viruses, Molecular Sequence Data, Retroviridae Proteins, Oncogenic, Receptors, Antigen, B-Cell, Protein tyrosine phosphatase, Lymphocyte Activation, Receptor tyrosine kinase, Cell Line, chemistry.chemical_compound, Mice, Viral Envelope Proteins, LYN, Virology, Immunoreceptor tyrosine-based activation motif, Leukemia Virus, Bovine, Animals, Receptors, Amino Acid, Amino Acid Sequence, Tyrosine, Phosphorylation, Receptors, Immunologic, B-Lymphocytes, biology, Bovine leukemia virus, Tyrosine phosphorylation, Enzootic Bovine Leukosis, biology.organism_classification, Cell biology, Infectious Diseases, chemistry, biology.protein, Cattle, Signal Transduction

Abstract

Bovine leukemia virus (BLV) causes persistent lymphocytosis, a preneoplastic, polyclonal expansion of B lymphocytes. The expansion increases viral transmission to new hosts, but the mechanisms of this expansion have not been determined. We hypothesized that BLV infection contributes to B-cell expansion by signaling initiated via viral transmembrane protein motifs undergoing tyrosine phosphorylation. Viral mimicry of host cell proteins is a well-demonstrated mechanism by which viruses may increase propagation or decrease recognition by the host immune system. The cytoplasmic tail of BLV transmembrane protein gp30 (TM) has multiple areas of homology to motifs of host cell signaling proteins, including two immunoreceptor tyrosine-based activation motifs (ITAMs) and two immunoreceptor tyrosine-based inhibition motifs (ITIMs), which are homologous to B-cell receptor and inhibitory co-receptor motifs. Signaling by these motifs in B cells typically relies on tyrosine phosphorylation, followed by interactions with Src-homology-2 (SH2) domains of nonreceptor protein tyrosine kinases or phosphatases. Phosphorylation of tyrosine residues in the cytoplasmic tail of TM was tested in four systems including ex vivo cultured peripheral blood mononuclear cells from BLV infected cows, BLV-expressing fetal lamb kidney cell and bat lung cell lines, and DT40 B cells transfected with a fusion of mouse extracellular CD8alpha and cytoplasmic TM. No phosphorylation of TM was detected in our experiments in any of the cell types utilized, or with various stimulation methods. Detection was attempted by immunoblotting for phosphotyrosines, or by metabolic labeling of cells. Thus BLV TM is not likely to modify host signal pathways through interactions between phosphorylated tyrosines of the ITAM or ITIM motifs and host-cell tyrosine kinases or phosphatases.

Published

2002

19. Bovine leukemia virus transmembrane protein gp30 physically associates with the down-regulatory phosphatase SHP-1

Author

Glenn H. Cantor, Oto Orlik, Suzanne M. Pritchard, William C. Davis, Raymond Reeves, and Gary A. Splitter

Subjects

Immunology, Phosphatase, Molecular Sequence Data, Retroviridae Proteins, Oncogenic, Down-Regulation, Protein Tyrosine Phosphatase, Non-Receptor Type 11, chemistry.chemical_compound, Retrovirus, Viral Envelope Proteins, medicine, Animals, Humans, Amino Acid Sequence, B-Lymphocytes, biology, Bovine leukemia virus, Protein Tyrosine Phosphatase, Non-Receptor Type 6, CD22, Intracellular Signaling Peptides and Proteins, Tyrosine phosphorylation, Enzootic Bovine Leukosis, biology.organism_classification, medicine.disease, Molecular biology, Precipitin Tests, Transmembrane protein, Lymphoma, Leukemia, chemistry, Cancer research, Cattle, Female, Protein Tyrosine Phosphatases, Protein Binding

Abstract

In B lymphocytes, the down-regulatory phosphatase SHP-1 associates with CD22 and CD32b (also known as FcγRIIB) and acts as a critical negative regulator of B-cell receptor signaling. Bovine leukemia virus, a retrovirus of the HTLV/BLV group, causes persistently increased numbers of peripheral blood B lymphocytes, known as persistent lymphocytosis (PL) and, in some animals, progression to B-cell leukemia and/or lymphoma. Here, we show that SHP-1 associates with the bovine leukemia virus transmembrane protein, gp30. This interaction is either direct or indirect. The interaction is dependent on tyrosine phosphorylation, and the interaction increases after cell stimulation with sodium pervanadate. The gp30–SHP-1 interaction is seen in all of the BLV-infected, PL animals tested, but is not seen in uninfected animals or in most BLV-infected, non-PL animals, which do not express significant quantities of gp30. However, one BLV-infected, non-PL animal expressed large quantities of gp30, yet no gp30–SHP-1 interaction was detected, suggesting that there may be other factors in cells from the PL animals that facilitate the gp30–SHP-1 interaction. The association of gp30 and SHP-1 suggests the hypothesis that gp30 may act as a decoy to sequester SHP-1, resulting in up-regulation of B-cell receptor signaling. The implication of this could be a novel mechanism of viral activation of lymphocytes by removal of a down-regulatory phosphatase.

Published

1999

20. Corrigendum to 'Metabonomics evaluation of urine from rats given acute and chronic doses of acetaminophen using NMR and UPLC/MS' [J. Chromatogr. B 871 (2008) 328]

Author

Jinchun Sun, Ricky D. Holland, Laura K. Schnackenberg, Richard D. Beger, Glenn H. Cantor, Thomas C. Schmitt, and Yvonne P. Dragan

Subjects

Chromatography, Chemistry, Clinical Biochemistry, medicine, Uplc ms ms, Cell Biology, General Medicine, Urine, Pharmacology, Biochemistry, Analytical Chemistry, Acetaminophen, medicine.drug

Published

2009