Your search keyword '"Chromans toxicity"' showing total 119 results

1. Toxicological assessments of an ethanol extract complex of Descurainia sophia and Peucedanum praeruptorum: Subacute oral toxicity and genotoxicity studies.

Author

Cho ES, Shin S, Lee YJ, Kim NS, Kim J, Lee SJ, Son HY, Lee WJ, and Bang OS

Subjects

Administration, Oral, Animals, Dose-Response Relationship, Drug, Female, Male, Mice, Mice, Inbred ICR, Models, Animal, Plant Extracts administration & dosage, Plant Roots chemistry, Seeds chemistry, Toxicity Tests, Antineoplastic Agents toxicity, Apiaceae chemistry, Brassicaceae chemistry, Chromans toxicity, Colorectal Neoplasms drug therapy, DNA Damage drug effects, Plant Extracts toxicity

Abstract

An ethanol extract complex of Descurainia sophia seeds and Peucedanum praeruptorum roots, called BP10A, has antitumor potential against colorectal cancer. In the present study, we evaluated the 28-day oral toxicity and the genotoxicity of BP10A. The subacute toxicity test was done through oral administration to mice. ICR mice (n = 10) received daily oral BP10A doses of 0, 500, 1000 and 2000 mg/kg for 28 consecutive days. During administration, general clinical signs, food consumption, organ weights, and hematologic, biochemical and histopathological parameters in male and female mice were assessed. No significant adverse effects up to the highest dose (2000 mg/kg) were found. The genotoxicity was evaluated using a battery of tests, including an in vitro bacterial reverse mutation (Ames) test, an in vivo micronucleus test using bone marrow cells in ICR mice and a chromosomal aberration test using CHL/IU cells. BP10A did not show any genotoxic signs in the Ames (up to 5000 μg/plate), micronucleus (up to 5000 mg/kg) and the chromosomal aberration tests (550-1750 μg/mL). Therefore, BP10A was considered safe based on the subacute toxicity and genotoxicity results, indicating that it is a useful pharmaceutical material with no adverse toxicity., (© 2020 John Wiley & Sons, Ltd.)

Published

2020

2. A multi-signal mitochondria-targeted fluorescent probe for real-time visualization of cysteine metabolism in living cells and animals.

Author

Yang X, Liu W, Tang J, Li P, Weng H, Ye Y, Xian M, Tang B, and Zhao Y

Subjects

Acrylates chemical synthesis, Acrylates metabolism, Acrylates toxicity, Animals, Cell Line, Tumor, Chromans chemical synthesis, Chromans metabolism, Chromans toxicity, Coumarins chemical synthesis, Coumarins metabolism, Coumarins toxicity, Cysteine metabolism, Fluorescence, Fluorescent Dyes chemical synthesis, Fluorescent Dyes metabolism, Fluorescent Dyes toxicity, Humans, Limit of Detection, Liver metabolism, Mice, Microscopy, Confocal methods, Microscopy, Fluorescence methods, Sulfites analysis, Sulfites chemistry, Sulfur Dioxide metabolism, Zebrafish, Acrylates chemistry, Chromans chemistry, Coumarins chemistry, Cysteine analysis, Fluorescent Dyes chemistry, Mitochondria metabolism, Sulfur Dioxide analysis

Abstract

In this study, we developed a multi-signal mitochondria-targeted fluorescent probe (NIR-Cys) for simultaneous detection of Cys and its metabolite, SO2. In the design of the probe, the acrylate group and the C[double bond, length as m-dash]C of the coumarin ring were used as the recognizing moiety for Cys and SO2, respectively. The probe exhibited high sensitivity, excellent specificity, and fast response. NIR-Cys was found to precisely target and visualize Cys metabolism in mitochondria of living cells with a multi-fluorescence signal. This probe is expected to be a useful tool for understanding Cys metabolism.

Published

2018

3. Increased susceptibility to troglitazone-induced mitochondrial permeability transition in type 2 diabetes mellitus model rat.

Author

Segawa M, Sekine S, Sato T, and Ito K

Subjects

Animals, Cardiolipins metabolism, Chromans adverse effects, Disease Models, Animal, Glutathione metabolism, Hepatocytes drug effects, Hypoglycemic Agents adverse effects, Male, Membrane Potential, Mitochondrial drug effects, Mitochondria, Liver metabolism, Mitochondrial Permeability Transition Pore, Oxidative Phosphorylation drug effects, Oxygen Consumption drug effects, Phospholipids metabolism, Rats, Zucker, Thiazolidinediones adverse effects, Troglitazone, Chromans toxicity, Diabetes Mellitus, Type 2 metabolism, Hypoglycemic Agents toxicity, Lipid Peroxidation, Mitochondria, Liver drug effects, Mitochondrial Membrane Transport Proteins metabolism, Thiazolidinediones toxicity

Abstract

Troglitazone, a member of the thiazolidinedione class of antidiabetic drugs, was withdrawn from the market because it causes severe liver injury. One of the mechanisms for this adverse effect is thought to be mitochondrial toxicity. To investigate the characteristics of troglitazone-induced liver toxicity in more depth, the toxicological effects of troglitazone on hepatocytes and liver mitochondria were investigated using a rat model of type 2 diabetes mellitus (T2DM). Troglitazone was found to increase mitochondrial permeability transition (MPT) in the liver mitochondria of diabetic rats to a greater extent than in control rats, whereas mitochondrial membrane potential and oxidative phosphorylation were not affected. To identify the factors associated with this increase in susceptibility to MPT in diabetic rats, we assessed the oxidative status of the liver mitochondria and found a decrease in mitochondrial glutathione content and an increase in phospholipid peroxidation. Moreover, incorporation of oxidized cardiolipin, a mitochondrion-specific phospholipid, was involved in the troglitazone-induced alteration in susceptibility to MPT. In conclusion, liver mitochondria display disease-associated mitochondrial lipid peroxidation in T2DM, which facilitates the higher susceptibility to troglitazone-induced MPT. Thus, greater susceptibility of liver mitochondria may be a host factor leading to troglitazone-induced hepatotoxicity in T2DM.

Published

2018

4. Individual serum bile acid profiling in rats aids in human risk assessment of drug-induced liver injury due to BSEP inhibition.

Author

Cepa S, Potter D, Wong L, Schutt L, Tarrant J, Pang J, Zhang X, Andaya R, Salphati L, Ran Y, An L, Morgan R, and Maher J

Subjects

Animals, Chromans toxicity, Female, Male, Rats, Rats, Sprague-Dawley, Thiazolidinediones toxicity, Troglitazone, ATP Binding Cassette Transporter, Subfamily B, Member 11 antagonists & inhibitors, Bile Acids and Salts blood, Chemical and Drug Induced Liver Injury etiology, Risk Assessment

Abstract

Drug-induced liver injury (DILI) has been the most frequent cause of post-marketing drug withdrawals in the last 50years. The multifactorial nature of events that precede severe liver injury in human patients is difficult to model in rodents due to a variety of confounding or contributing factors that include disease state, concurrent medications, and translational species differences. In retrospective analyses, a consistent risk factor for DILI has been the inhibition of the Bile Salt Export Pump (BSEP). One compound known for potent BSEP inhibition and severe DILI is troglitazone. The purpose of the current study is to determine if serum profiling of 19 individual bile acids by liquid chromatography-mass spectrometry (LC/MS) can detect perturbations in bile acid homeostasis in rats after acute intravenous (IV) administration of vehicle or 5, 25, or 50mg/kg troglitazone. Minimal serum transaminase elevations (approximately two-fold) were observed with no evidence of microscopic liver injury. However, marked changes in individual serum bile acids occurred, with dose-dependent increases in the majority of the bile acids profiled. When compared to predose baseline values, tauromuricholic acid and taurocholic acid had the most robust increase in serum levels and dynamic range, with a maximum fold increase from baseline of 34-fold and 29-fold, respectively. Peak bile acid increases occurred within 2hours (h) after dosing and returned to baseline values before 24h. In conclusion, serum bile acid profiling can potentially identify a mechanistic risk of clinical DILI that could be poorly detected by traditional toxicity endpoints., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2018

5. Rational Design and Multibiological Profiling of Novel Donepezil-Trolox Hybrids against Alzheimer's Disease, with Cholinergic, Antioxidant, Neuroprotective, and Cognition Enhancing Properties.

Author

Cai P, Fang SQ, Yang XL, Wu JJ, Liu QH, Hong H, Wang XB, and Kong LY

Subjects

Amyloid beta-Peptides drug effects, Animals, Antioxidants pharmacology, Antioxidants toxicity, Blood-Brain Barrier, Cell Line, Central Nervous System Agents pharmacology, Central Nervous System Agents toxicity, Chelating Agents pharmacology, Chelating Agents therapeutic use, Chelating Agents toxicity, Cholinesterase Inhibitors pharmacology, Cholinesterase Inhibitors toxicity, Chromans pharmacology, Chromans toxicity, Copper, Donepezil, Drug Design, Drug Evaluation, Preclinical, Humans, Indans pharmacology, Indans toxicity, Male, Mice, Inbred ICR, Microglia drug effects, Molecular Docking Simulation, Monoamine Oxidase Inhibitors pharmacology, Monoamine Oxidase Inhibitors toxicity, Neurotoxins toxicity, Oxidants toxicity, PC12 Cells, Peptide Fragments drug effects, Piperidines pharmacology, Piperidines toxicity, Protein Aggregation, Pathological drug therapy, Rats, Structure-Activity Relationship, Alzheimer Disease drug therapy, Antioxidants therapeutic use, Central Nervous System Agents therapeutic use, Cholinesterase Inhibitors therapeutic use, Chromans therapeutic use, Indans therapeutic use, Monoamine Oxidase Inhibitors therapeutic use, Piperidines therapeutic use

Abstract

A novel series of donepezil-trolox hybrids were designed, synthesized, and evaluated as multifunctional ligands against Alzheimer's disease (AD). Biological assays showed that these derivatives possessed moderate to good inhibitory activities against acetylcholinesterase (AChE) and monoamine oxidase B (MAO-B) as well as remarkable antioxidant effects. The optimal compound 6d exhibited balanced functions with good inhibition against hAChE (IC 50 = 0.54 μM) and hMAO-B (IC 50 = 4.3 μM), significant antioxidant activity (41.33 μM IC 50 by DPPH method, 1.72 and 1.79 trolox equivalent by ABTS and ORAC methods), excellent copper chelation, and Aβ 1-42 aggregation inhibition effect. Furthermore, cellular tests indicated that 6d has very low toxicity and is capable of combating oxidative toxin (H 2 O 2 , rotenone, and oligomycin-A) induced neurotoxicity. Most importantly, oral administration of 6d demonstrated notable improvements on cognition and spatial memory against scopolamine-induced acute memory deficit as well as d-galactose (d-gal) and AlCl 3 induced chronic oxidative stress in a mouse model without acute toxicity and hepatotoxicity. In summary, both in vitro and in vivo results suggested that 6d is a valuable candidate for the development of a safe and effective anti-Alzheimer's drug.

Published

2017

6. Bis-spirochromanones as potent inhibitors of Mycobacterium tuberculosis: synthesis and biological evaluation.

Author

Dongamanti A, Aamate VK, Devulapally MG, Gundu S, Balabadra S, Manga V, Yogeeswari P, Sriram D, and Balasubramanian S

Subjects

Antitubercular Agents metabolism, Antitubercular Agents toxicity, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Chemistry Techniques, Synthetic, Chromans metabolism, Chromans toxicity, HEK293 Cells, Humans, Microbial Sensitivity Tests, Molecular Docking Simulation, Mycobacterium tuberculosis metabolism, Protein Conformation, Structure-Activity Relationship, Antitubercular Agents chemical synthesis, Antitubercular Agents pharmacology, Chromans chemical synthesis, Chromans pharmacology, Mycobacterium tuberculosis drug effects, Spiro Compounds chemistry

Abstract

On the basis of reported antimycobacterial property of chroman-4-one pharmacophore, a series of chemically modified bis-spirochromanones were synthesized starting from 2-hydroxyacetophenone and 1,4-dioxaspiro[4.5] decan-8-one using a Kabbe condensation approach. The synthesized bis-spirochromanones were established based on their spectral data and X-ray crystal structure of 6e. All synthesized compounds were evaluated against Mycobacterium tuberculosis H37Rv (ATCC 27294) strain, finding that some products exhibited good antimycobacterial activity with minimum inhibitory concentration as low as [Formula: see text]. Docking studies were carried out to identify the binding interactions of compounds II, 6a and 6n with FtsZ. Compounds exhibiting good in vitro potency in the MTB MIC assay were further evaluated for toxicity using the HEK cell line.

Published

2017

7. Exploring Chronic Drug Effects on Microengineered Human Liver Cultures Using Global Gene Expression Profiling.

Author

Ware BR, McVay M, Sunada WY, and Khetani SR

Subjects

3T3 Cells, Animals, Cells, Cultured, Chemical and Drug Induced Liver Injury genetics, Chromans toxicity, Coculture Techniques, Dose-Response Relationship, Drug, Fibroblasts cytology, Gene Expression Profiling, Hepatocytes cytology, Humans, Mice, Oxidative Stress drug effects, Oxidative Stress genetics, Primary Cell Culture, Rosiglitazone, Thiazolidinediones toxicity, Toxicogenetics, Troglitazone, Chemical and Drug Induced Liver Injury etiology, Fibroblasts drug effects, Hepatocytes drug effects, Liver drug effects, Transcriptome drug effects

Abstract

Global gene expression profiling is useful for elucidating a drug's mechanism of action on the liver; however, such profiling in rats is not very sensitive for predicting human drug-induced liver injury, while dedifferentiated monolayers of primary human hepatocytes (PHHs) do not permit chronic drug treatment. In contrast, micropatterned cocultures (MPCCs) containing PHH colonies and 3T3-J2 fibroblasts maintain a stable liver phenotype for 4-6 weeks. Here, we used MPCCs to test the hypothesis that global gene expression patterns in stable PHHs can be used to distinguish clinical hepatotoxic drugs from their non-liver-toxic analogs and understand the mechanism of action prior to the onset of overt hepatotoxicity. We found that MPCCs treated with the clinical hepatotoxic/non-liver-toxic pair, troglitazone/rosiglitazone, at each drug's reported and non-toxic Cmax (maximum concentration in human plasma) for 1, 7, and 14 days displayed a total of 12, 269, and 628 differentially expressed genes, respectively, relative to the vehicle-treated control. Troglitazone modulated >75% of transcripts across pathways such as fatty acid and drug metabolism, oxidative stress, inflammatory response, and complement/coagulation cascades. Escalating rosiglitazone's dose to that of troglitazone's Cmax increased modulated transcripts relative to the lower dose; however, over half the identified transcripts were still exclusively modulated by troglitazone. Last, other hepatotoxins (nefazodone, ibufenac, and tolcapone) also induced a greater number of differentially expressed genes in MPCCs than their non-liver-toxic analogs (buspirone, ibuprofen, and entacapone) following 7 days of treatment. In conclusion, MPCCs allow evaluation of time- and dose-dependent gene expression patterns in PHHs treated chronically with analog drugs., (© The Author 2017. Published by Oxford University Press on behalf of the Society of Toxicology. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published

2017

8. Development of a cell viability assay to assess drug metabolite structure-toxicity relationships.

Author

Rana P, Will Y, Nadanaciva S, and Jones LH

Subjects

Adenosine Triphosphate metabolism, Benzbromarone analogs & derivatives, Benzbromarone metabolism, Benzbromarone toxicity, Cell Line, Cell Survival drug effects, Chromans metabolism, Chromans toxicity, Cytochrome P-450 CYP2C9 metabolism, Cytochrome P-450 CYP2D6 metabolism, Cytochrome P-450 CYP3A metabolism, Humans, Thiazolidinediones metabolism, Thiazolidinediones toxicity, Troglitazone, Cytochrome P-450 Enzyme System metabolism, Pharmaceutical Preparations metabolism

Abstract

Many adverse drug reactions are caused by the cytochrome P450 (CYP)-dependent activation of drugs into reactive metabolites. In order to reduce attrition due to metabolism-induced toxicity and to improve the safety of drug candidates, we developed a simple cell viability assay by combining a bioactivation system (human CYP3A4, CYP2D6 and CYP2C9) with Hep3B cells. We screened a series of drugs to explore structural motifs that may be responsible for CYP450-dependent activation caused by reactive metabolite formation, which highlighted specific liabilities regarding certain phenols and anilines., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

9. New in vitro model for proarrhythmia safety screening: IKs inhibition potentiates the QTc prolonging effect of IKr inhibitors in isolated guinea pig hearts.

Author

Kui P, Orosz S, Takács H, Sarusi A, Csík N, Rárosi F, Csekő C, Varró A, Papp JG, Forster T, Farkas AS, and Farkas A

Subjects

Animals, Catecholamines pharmacology, Chromans toxicity, Cisapride toxicity, Coronary Circulation drug effects, Delayed Rectifier Potassium Channels drug effects, Drug Interactions, Electrocardiography drug effects, Female, Guinea Pigs, Heart Rate drug effects, In Vitro Techniques, Phenethylamines toxicity, Sulfonamides toxicity, Torsades de Pointes chemically induced, Arrhythmias, Cardiac chemically induced, Drug Evaluation, Preclinical methods, Heart drug effects, Long QT Syndrome chemically induced, Potassium Channel Blockers toxicity

Abstract

Introduction: Preclinical in vivo QT measurement as a proarrhythmia essay is expensive and not reliable enough. The aim of the present study was to develop a sensitive, cost-effective, Langendorff perfused guinea pig heart model for proarrhythmia safety screening., Methods: Low concentrations of dofetilide and cisapride (inhibitors of the rapid delayed rectifier potassium current, IKr) were tested alone and co-perfused with HMR-1556 (inhibitor of the slow delayed rectifier potassium current, IKs) in Langendorff perfused guinea pig hearts. The electrocardiographic rate corrected QT (QTc) interval, the Tpeak-Tend interval and the beat-to-beat variability and instability (BVI) of the QT interval were determined in sinus rhythm., Results: Dofetilide and HMR-1556 alone or co-perfused, prolonged the QTc interval by 20±2%, 10±1% and 55±10%, respectively. Similarly, cisapride and HMR-1556 alone or co-perfused, prolonged the QTc interval by 11±3%, 11±4% and 38±6%, respectively. Catecholamine-induced fast heart rate abolished the QTc prolonging effects of the IKr inhibitors, but augmented the QTc prolongation during IKs inhibition. None of the drug perfusions increased significantly the Tpeak-Tend interval and the sinus BVI of the QT interval., Discussion: IKs inhibition increased the QTc prolonging effect of IKr inhibitors in a super-additive (synergistic) manner, and the QTc interval was superior to other proarrhythmia biomarkers measured in sinus rhythm in isolated guinea pig hearts. The effect of catecholamines on the QTc facilitated differentiation between IKr and IKs inhibitors. Thus, QTc measurement in Langendorff perfused guinea pig hearts with pharmacologically attenuated repolarization reserve and periodic catecholamine perfusion seems to be suitable for preclinical proarrhythmia screening., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

10. Development of an optimized cytotoxicity assay system for CYP3A4-mediated metabolic activation via modified piggyBac transposition.

Author

Huang L, Zou S, Deng J, Dai T, Jiang J, Jia Y, Dai R, and Xie S

Subjects

Acetaminophen toxicity, Activation, Metabolic, Chromans toxicity, Citric Acid toxicity, Cytochrome P-450 CYP3A genetics, DNA Transposable Elements, Galactosamine toxicity, Hep G2 Cells, Humans, Thiazolidinediones toxicity, Troglitazone, Biological Assay, Cell Survival drug effects, Cytochrome P-450 CYP3A metabolism, Nerve Tissue Proteins genetics

Abstract

Drug-induced hepatotoxicity is often caused by cytochrome P450 (CYP)-dependent metabolism of drugs into reactive metabolites. Assessment of hepatotoxicity induced by bioactive compounds is hampered by low CYP expression within in vitro cell lines. To overcome this limitation, piggyBac transposition and monoclonal expansion were used to generate a HepG2 cell line with stable and homogenously high expression of CYP3A4, a prominent CYP isoform. Our studies demonstrate the generated line's constant CYP3A4 expression and activity for over 40 cell passages; to date, it has been in subculture for more than a year without addition of Puromycin. This cell line was utilized to evaluate cytotoxicity of two bioactive (troglitazone and acetaminophen) and two non-bioactive (citrate and galactosamine) compounds by MTT assay. Cell viability significantly decreased upon treatment with bioactive drugs. Moreover, cell lines used in the present study were more sensitive to toxic effects of troglitazone than previously reported. Therefore, this HepG2 cell-based assay system may provide a suitable hepatic model for predicting CYP3A4-mediated hepatotoxicity during preclinical drug development., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2016

11. In Vivo Detection of Mitochondrial Dysfunction Induced by Clinical Drugs and Disease-Associated Genes Using a Novel Dye ZMJ214 in Zebrafish.

Author

Sasagawa S, Nishimura Y, Koiwa J, Nomoto T, Shintou T, Murakami S, Yuge M, Kawaguchi K, Kawase R, Miyazaki T, and Tanaka T

Subjects

Animals, Anti-Bacterial Agents toxicity, Anticonvulsants toxicity, Benzophenones toxicity, Chromans toxicity, Disease Models, Animal, Hypoglycemic Agents toxicity, Nitrophenols toxicity, Oligomycins toxicity, Pioglitazone, Thiazolidinediones toxicity, Tolcapone, Toxicity Tests methods, Troglitazone, Zebrafish genetics, Zebrafish Proteins genetics, Carbocyanines chemistry, Fluorescent Dyes chemistry, Membrane Potential, Mitochondrial drug effects, Mitochondria drug effects, Mitochondria pathology, Optical Imaging methods

Abstract

Mitochondrial dysfunction has been implicated in various drug-induced toxicities and genetic disorders. Recently, the zebrafish has emerged as a versatile animal model for both chemical and genetic screenings. Taking advantage of its transparency, various in vivo fluorescent imaging methods have been developed to identify novel functions of chemicals and genes in zebrafish. However, there have not been fluorescent probes that can detect mitochondrial membrane potential in living zebrafish. In this study, we identified a novel cyanine dye called ZMJ214 that detects mitochondrial membrane potential in living zebrafish from 4 to 8 days post fertilization and is administered by simple immersion. The fluorescence intensity of ZMJ214 in zebrafish was increased and decreased by oligomycin and FCCP, respectively, suggesting a positive correlation between ZMJ214 fluorescence and mitochondrial membrane potential. In vivo imaging of zebrafish stained with ZMJ214 allowed for the detection of altered mitochondrial membrane potential induced by the antidiabetic drug troglitazone and the antiepileptic drug tolcapone, both of which have been withdrawn from the market due to mitochondrial toxicity. In contrast, pioglitazone and entacapone, which are similar to troglitazone and tolcapone, respectively, and have been used commercially, did not cause a change in mitochondrial membrane potential in zebrafish stained with ZMJ214. Live imaging of zebrafish stained with ZMJ214 also revealed that knock-down of slc25a12, a mitochondrial carrier protein associated with autism, dysregulated the mitochondrial membrane potential. These results suggest that ZMJ214 can be a useful tool to identify chemicals and genes that cause mitochondrial dysfunction in vivo.

Published

2016

12. Usefulness of in vitro combination assays of mitochondrial dysfunction and apoptosis for the estimation of potential risk of idiosyncratic drug induced liver injury.

Author

Goda K, Takahashi T, Kobayashi A, Shoda T, Kuno H, and Sugai S

Subjects

Acetaminophen toxicity, Biomarkers metabolism, Caspase 3 metabolism, Caspase 7 metabolism, Cells, Cultured, Chemical and Drug Induced Liver Injury metabolism, Chemical and Drug Induced Liver Injury pathology, Chromans toxicity, Diclofenac toxicity, Dose-Response Relationship, Drug, Ethanol toxicity, Hepatocytes metabolism, Hepatocytes pathology, Humans, Isoxazoles toxicity, Leflunomide, Liver metabolism, Liver pathology, Mitochondria, Liver metabolism, Mitochondria, Liver pathology, Oxygen Consumption drug effects, Primary Cell Culture, Ranitidine toxicity, Risk Assessment, Thiazolidinediones toxicity, Time Factors, Troglitazone, Apoptosis drug effects, Biological Assay, Chemical and Drug Induced Liver Injury etiology, Hepatocytes drug effects, Liver drug effects, Mitochondria, Liver drug effects, Toxicity Tests methods

Abstract

Drug-induced liver injury (DILI) is one of the serious and frequent drug-related adverse events. This adverse event is a main reason for regulatory action pertaining to drugs, including restrictions in clinical indications and withdrawal from clinical trials or the marketplace. Idiosyncratic DILI especially has become a major clinical concern because of its unpredictable nature, frequent hospitalization, need for liver transplantation and high mortality. The estimation of the potential for compounds to induce idiosyncratic DILI is very difficult in non-clinical studies because the precise mechanism of idiosyncratic DILI is still unknown. Recently, many in vitro assays which indicate a possibility of the prediction of the idiosyncratic DILI have been reported. Among these, some in vitro assays focus on the effects of compounds on mitochondrial function and the apoptotic effects of compounds on human hepatocytes. In this study, we measured oxygen consumption rate (OCR) and caspase-3/7 activity as an endpoint of mitochondrial dysfunction and apoptosis, respectively, with human hepatocytes after treatment with compounds causing idiosyncratic DILI (troglitazone, leflunomide, ranitidine and diclofenac). Troglitazone and leflunomide decreased the OCR but did not affect caspase-3/7 activity. Ranitidine increased caspase-3/7 activity but did not affect the OCR. Diclofenac decreased the OCR and increased caspase-3/7 activity. Acetaminophen and ethanol, which are also hepatotoxicants but do not induce idiosyncratic DILI, did not affect the OCR or caspase-3/7 activity. These results indicate that a combination assay of mitochondrial dysfunction and apoptosis is useful for the estimation of potential risk of compounds to induce idiosyncratic DILI.

Published

2016

13. Determination of liver specific toxicities in rat hepatocytes by high content imaging during 2-week multiple treatment.

Author

Germano D, Uteng M, Pognan F, Chibout SD, and Wolf A

Subjects

Amiodarone administration & dosage, Amiodarone toxicity, Animals, Cells, Cultured, Chlorpromazine administration & dosage, Chlorpromazine toxicity, Chromans administration & dosage, Chromans toxicity, Culture Techniques, Cyclosporine administration & dosage, Cyclosporine toxicity, Dopamine Antagonists administration & dosage, Dopamine Antagonists toxicity, Gene Expression Regulation drug effects, Hypoglycemic Agents administration & dosage, Hypoglycemic Agents toxicity, Immunosuppressive Agents administration & dosage, Immunosuppressive Agents toxicity, Male, Potassium Channel Blockers administration & dosage, Potassium Channel Blockers toxicity, Rats, Rats, Wistar, Thiazolidinediones administration & dosage, Thiazolidinediones toxicity, Troglitazone, Hepatocytes drug effects

Abstract

DILI is a major safety issue during drug development and one of the leading causes for market withdrawal. Despite many efforts made in the past, the prediction of DILI using in vitro models remains very unreliable. In the present study, the well-established hepatocyte Collagen I-Matrigel™ sandwich culture was used, mimicking chronic drug treatment after multiple incubations for 14 days. Ten drugs associated with different types of specific preclinical and clinical liver injury were evaluated at non-cytotoxic concentrations. Mrp2-mediated transport, intracellular accumulation of neutral lipids and phospholipids were selected as functional endpoints by using Cellomics™ Arrayscan® technology and assessed at five timepoints (day 1, 3, 7, 10, 14). Liver specific functional impairments after drug treatment were enhanced over time and could be monitored by HCI already after few days and before cytotoxicity. Phospholipidosis-inducing drugs Chlorpromazine and Amiodarone displayed the same response as in vivo. Cyclosporin A, Chlorpromazine, and Troglitazone inhibited Mrp2-mediated biliary transport, correlating with in vivo findings. Steatosis remained difficult to be reproduced under the current in vitro testing conditions, resulting into false negative and positive responses. The present results suggest that the repeated long-term treatment of rat hepatocytes in the Collagen I-Matrigel™ sandwich configuration might be a suitable tool for safety profiling of the potential to induce phospholipidosis and impair Mrp2-mediated transport processes, but not to predict steatosis., (Copyright © 2014 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2015

14. Tacrine-Trolox Hybrids: A Novel Class of Centrally Active, Nonhepatotoxic Multi-Target-Directed Ligands Exerting Anticholinesterase and Antioxidant Activities with Low In Vivo Toxicity.

Author

Nepovimova E, Korabecny J, Dolezal R, Babkova K, Ondrejicek A, Jun D, Sepsova V, Horova A, Hrabinova M, Soukup O, Bukum N, Jost P, Muckova L, Kassa J, Malinak D, Andrs M, and Kuca K

Subjects

Acetylcholinesterase chemistry, Animals, Antioxidants toxicity, Blood-Brain Barrier, Catalysis, Cholinesterase Inhibitors toxicity, Chromans toxicity, Drug Design, Free Radical Scavengers chemical synthesis, Free Radical Scavengers pharmacology, Hepatocytes drug effects, Humans, Injections, Intramuscular, Kinetics, Ligands, Male, Microsomes, Liver drug effects, Microsomes, Liver metabolism, Models, Molecular, Rats, Rats, Wistar, Tacrine toxicity, Antioxidants chemical synthesis, Antioxidants pharmacology, Cholinesterase Inhibitors chemical synthesis, Cholinesterase Inhibitors pharmacology, Chromans chemistry, Chromans pharmacology, Tacrine chemistry, Tacrine pharmacology

Abstract

Coupling of two distinct pharmacophores, tacrine and trolox, endowed with different biological properties, afforded 21 hybrid compounds as novel multifunctional candidates against Alzheimer's disease. Several of them showed improved inhibitory properties toward acetylcholinesterase (AChE) in relation to tacrine. These hybrids also scavenged free radicals. Molecular modeling studies in tandem with kinetic analysis exhibited that these hybrids target both catalytic active site as well as peripheral anionic site of AChE. In addition, incorporation of the moiety bearing antioxidant abilities displayed negligible toxicity on human hepatic cells. This striking effect was explained by formation of nontoxic metabolites after 1 h incubation in human liver microsomes system. Finally, tacrine-trolox hybrids exhibited low in vivo toxicity after im administration in rats and potential to penetrate across blood-brain barrier. All of these outstanding in vitro results in combination with promising in vivo outcomes highlighted derivative 7u as the lead structure worthy of further investigation.

Published

2015

15. Hepatotoxicants induce cytokine imbalance in response to innate immune system.

Author

Goto S, Deguchi J, Nishio N, Nomura N, and Funabashi H

Subjects

Animals, Cells, Cultured, Chemokines metabolism, Down-Regulation drug effects, Interleukin-10 metabolism, Interleukin-1beta metabolism, Interleukin-6 metabolism, Kupffer Cells metabolism, Male, Nitric Oxide metabolism, Rats, Sprague-Dawley, Reactive Oxygen Species metabolism, Troglitazone, Up-Regulation drug effects, Acetaminophen toxicity, Chemical and Drug Induced Liver Injury immunology, Chromans toxicity, Cytokines metabolism, Fluoroquinolones toxicity, Immunity, Innate immunology, Inflammation Mediators metabolism, Kupffer Cells immunology, Naphthyridines toxicity, Thiazolidinediones toxicity

Abstract

In recent years, attention has been paid to innate immune systems as mechanisms to initiate or promote drug-induced liver injury (DILI). Kupffer cells are hepatic resident macrophages and might be involved in the pathogenesis of DILI by release of pro- and anti-inflammatory mediators such as cytokines, chemokines, reactive oxygen species, and/or nitric oxides. The purpose of this study was to investigate alterations in mediator levels induced by hepatotoxic compounds in isolated Kupffer cells and discuss the relation between balance of each cytokine or chemokine and potential of innate immune-mediated DILI. Primary cultured rat Kupffer cells were treated with hepatotoxic (acetaminophen, troglitazone, trovafloxacin) or non-hepatotoxic (pioglitazone, levofloxacin) compounds with or without lipopolysaccharide (LPS). After 24 hr treatment, cell supernatants were collected and various levels of mediators released by Kupffer cells were examined. Although hepatotoxicants had no effect on the LPS-induced tumor necrosis factor-alpha (TNF-α) secretion, they enhanced the release of pro-inflammatory cytokine interleukin-1 beta (IL-1β) and suppressed the anti-inflammatory cytokines interleukin-6 (IL-6) and interleukin-10 (IL-10) induced by LPS. These cytokine shifts were not associated with switching the phenotypes of M1 and M2 macrophages in Kupffer cells. In conclusion, the present study suggested that the levels of some specific cytokines are affected by DILI-related drugs with LPS stimulation, and imbalance between pro- and anti-inflammatory cytokines, induced by the up-regulation of IL-1β and the down-regulation of IL-6 or IL-10, plays a key role in innate immune-mediated DILI.

Published

2015

16. Drug-induced cholestasis detection in cryopreserved rat hepatocytes in sandwich culture.

Author

Oorts M, Richert L, and Annaert P

Subjects

Animals, Bile Acids and Salts pharmacology, Cell Survival drug effects, Cell Survival physiology, Cells, Cultured, Cholestasis pathology, Hepatocytes pathology, Male, Rats, Rats, Wistar, Troglitazone, Cholestasis chemically induced, Chromans toxicity, Cryopreservation methods, Cyclosporine toxicity, Hepatocytes drug effects, Thiazolidinediones toxicity

Abstract

Introduction: In vitro identification of compounds that cause cholestasis in vivo still remains a problem in pharmaceutical R&D. Currently existing in vitro systems show poor predictivity towards the clinical situation. Recently, our research group developed a model, based on sandwich-cultured (rat) hepatocytes (SC(R)H), to detect compounds causing cholestasis via altered bile acid (BA) homeostasis (Chatterjee et al., 2014). In the present study, we assessed whether this model performs equally well with freshly-isolated and cryopreserved hepatocytes., Methods: We exposed sandwich cultures from rat hepatocytes before and after cryopreservation to the cholestatic compounds, cyclosporin A (CsA) and troglitazone (Tro), in the presence and in the absence of a BA mixture. At the end of the incubations, the capability of the hepatocytes to produce urea was measured to determine changes in the drug-induced cholestasis index (DICI)., Results: The mean (± SEM) urea production was significantly higher in sandwich cultures from freshly-isolated hepatocytes (27.88 (± 0.96) nmol/cm(2)), compared to cultures from cryopreserved hepatocytes (22.86 (± 1.91) nmol urea/cm(2)). However, after normalization for confluence rate (based on light microscopic image analysis), it appeared that the urea production was similar for all the batches of SCRH. The mean (± SEM) DICI values for CsA 10 μM and Tro 75 μM were 0.89 (± 0.03) and 0.93 (± 0.03), respectively. Higher concentrations, CsA (≥ 15 μM) and Tro (≥ 100 μM), elicited a significant decrease in urea production when incubated in the presence of a BA mixture compared to the compound alone. This was the case for all the batches of SCRH, irrespective of cryopreservation history., Discussion: In conclusion, no significant differences were seen when the previously described in vitro cholestasis model was applied in SCRH before or after cryopreservation. This study demonstrates the robustness of the model, which implies that it can be used with SCRH obtained from both freshly-isolated and cryopreserved hepatocytes., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2015

17. Characterizing the mechanism of thiazolidinedione-induced hepatotoxicity: An in vitro model in mitochondria.

Author

Hu D, Wu CQ, Li ZJ, Liu Y, Fan X, Wang QJ, and Ding RG

Subjects

Cell Line, Tumor, Chromans toxicity, DNA, Mitochondrial genetics, Electron Transport drug effects, Humans, Hypoglycemic Agents toxicity, Liver metabolism, Membrane Potential, Mitochondrial drug effects, Mitochondria metabolism, Oxidative Stress drug effects, Pioglitazone, Reactive Oxygen Species metabolism, Rosiglitazone, Troglitazone, Liver drug effects, Mitochondria drug effects, Thiazolidinediones toxicity

Abstract

Objective: To characterize the mechanism of action of thiazolidinedione (TZD)-induced liver mitochondrial toxicity caused by troglitazone, rosiglitazone, and pioglitazone in HepaRG cells., Methods: Human hepatoma cells (HepaRG) were treated with troglitazone, rosiglitazone, or pioglitazone (12.5, 25, and 50μM) for 48h. The Seahorse Biosciences XF24 Flux Analyzer was used to measure mitochondrial oxygen consumption. The effect of TZDs on reactive oxygen species (ROS) and mitochondrial membrane potential (MMP) were detected by flow cytometry. The mitochondrial ultrastructure of HepaRG cells was observed under a transmission electrical microscope (TEM). mtDNA content was evaluated by real-time PCR, and ATP content and mitochondrial respiratory chain (MRC) complex I, II, III, IV activity were measured via chemiluminescence. Results were considered statistically significant at p<0.05., Results: Among the three drugs, troglitazone exhibited the highest potency, followed by rosiglitazone, and then pioglitazone. The TZDs caused varying degrees of mitochondrial respiratory function disorders including decreases in oxygen consumption, MRC activity, and ATP level, and an elevation in ROS level. TZD treatment resulted in mtDNA content decline, reduction in MMP, and alterations of mitochondrial structure., Conclusion: All investigated TZDs show a certain degree of mitochondrial toxicity, with troglitazone exhibiting the highest potency. The underlying mechanism of TZD-induced hepatotoxicity may be associated with alterations in mitochondrial respiratory function disorders, oxidative stress, and changes in membrane permeability. These parameters may be used early in drug development to further optimize risk:benefit profiles., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2015

18. Systems pharmacology modeling predicts delayed presentation and species differences in bile acid-mediated troglitazone hepatotoxicity.

Author

Yang K, Woodhead JL, Watkins PB, Howell BA, and Brouwer KL

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 11, ATP-Binding Cassette Transporters physiology, Alanine Transaminase blood, Animals, Humans, Male, Models, Biological, Rats, Regression Analysis, Species Specificity, Troglitazone, Bile Acids and Salts physiology, Chemical and Drug Induced Liver Injury etiology, Chromans toxicity, Hypoglycemic Agents toxicity, Thiazolidinediones toxicity

Abstract

Troglitazone (TGZ) causes delayed, life-threatening drug-induced liver injury in some patients but was not hepatotoxic in rats. This study investigated altered bile acid homeostasis as a mechanism of TGZ hepatotoxicity using a systems pharmacology model incorporating drug/metabolite disposition, bile acid physiology/pathophysiology, hepatocyte life cycle, and liver injury biomarkers. In the simulated human population, TGZ (200-600 mg/day × 6 months) resulted in delayed increases in serum alanine transaminase >3× the upper limit of normal in 0.3-5.1%, with concomitant bilirubin elevations >2× the upper limit of normal in 0.3-3.6%, of the population. By contrast, pioglitazone (15-45 mg/day × 6 months) did not elicit hepatotoxicity, consistent with clinical data. TGZ was not hepatotoxic in the simulated rat population. In summary, mechanistic modeling based only on bile acid effects accurately predicted the incidence, delayed presentation, and species differences in TGZ hepatotoxicity, in addition to predicting the relative liver safety of pioglitazone. Systems pharmacology models integrating physiology and experimental data can evaluate drug-induced liver injury mechanisms and may be useful to predict the hepatotoxic potential of drug candidates.

Published

2014

19. Rationally designed less toxic SPD-304 analogs and preliminary evaluation of their TNF inhibitory effects.

Author

Alexiou P, Papakyriakou A, Ntougkos E, Papaneophytou CP, Liepouri F, Mettou A, Katsoulis I, Maranti A, Tsiliouka K, Strongilos A, Chaitidou S, Douni E, Kontopidis G, Kollias G, Couladouros E, and Eliopoulos E

Subjects

Animals, Anti-Inflammatory Agents metabolism, Anti-Inflammatory Agents toxicity, Biotransformation, Cell Line, Tumor, Cell Survival drug effects, Chromans metabolism, Chromans toxicity, Humans, Indoles metabolism, Indoles toxicity, Mice, Molecular Docking Simulation, Molecular Structure, Receptors, Tumor Necrosis Factor, Type I antagonists & inhibitors, Receptors, Tumor Necrosis Factor, Type I metabolism, Structure-Activity Relationship, Anti-Inflammatory Agents chemical synthesis, Anti-Inflammatory Agents pharmacology, Chromans chemical synthesis, Chromans pharmacology, Drug Design, Indoles chemical synthesis, Indoles pharmacology, Tumor Necrosis Factor-alpha antagonists & inhibitors

Abstract

SPD-304 was discovered as a promising tumor necrosis factor alpha (TNF) antagonist that promotes dissociation of TNF trimers and therefore blocks the interaction of TNF and its receptor. However, SPD-304 contains a potentially toxic 3-alkylindole moiety, which can be bioactivated to a reactive electrophilic intermediate. A series of SPD-304 analogs was synthesized with the aim to diminish its toxicophore groups while maintaining the binding affinity for TNF. Incorporation of electron-withdrawing substituents at the indole moiety, in conjunction with elimination of the 6'-methyl group of the 4-chromone moiety, led to a significantly less toxic and equally potent TNF inhibitor., (© 2014 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2014

20. Application of systems pharmacology to explore mechanisms of hepatotoxicity.

Author

Shon J and Abernethy DR

Subjects

Animals, Humans, Male, Troglitazone, Bile Acids and Salts physiology, Chemical and Drug Induced Liver Injury etiology, Chromans toxicity, Hypoglycemic Agents toxicity, Thiazolidinediones toxicity

Abstract

Advances in systems biology have allowed the development of a highly characterized systems pharmacology model to study mechanisms of drug-induced hepatotoxicity. In this issue of CPT, Yang et al. describe a model, DILIsym, used to characterize mechanisms of hepatotoxicity of troglitazone. Their modeling approach has provided new insight into troglitazone-induced hepatotoxicity in humans but is not associated with hepatotoxicity in rats, consistent with preclinical data for this drug.

Published

2014

21. Acute toxicity of subcutaneously administered vitamin E isomers delta- and gamma-tocotrienol in mice.

Author

Swift SN, Pessu RL, Chakraborty K, Villa V, Lombardini E, and Ghosh SP

Subjects

Administration, Cutaneous, Animals, Dermatitis, Contact pathology, Female, Male, Mice, Skin drug effects, Skin pathology, Toxicity Tests, Acute, Vitamin E toxicity, Chromans toxicity, Dermatitis, Contact etiology, Irritants toxicity, Vitamin E analogs & derivatives

Abstract

The toxicity of parenterally administered vitamin E isomers, delta-tocotrienol (DT3) and gamma-tocotrienol (GT3), was evaluated in male and female CD2F1 mice. In an acute toxicity study, a single dose of DT3 or GT3 was administered subcutaneously in a dose range of 200 to 800 mg/kg. A mild to moderately severe dermatitis was observed clinically and microscopically in animals at the injection site at doses above 200 mg/kg. The severity of the reaction was reduced when the drug concentration was lowered. Neither drug produced detectable toxic effects in any other tissue at the doses tested. Based on histopathological analysis for both DT3 and GT3, and macroscopic observations of inflammation at the injection site, a dose of 300 mg/kg was selected as the lowest toxic dose in a 30-day toxicity study performed in male mice. At this dose, a mild skin irritation occurred at the injection site that recovered completely by the end of the experimental period. At a dose of 300 mg/kg of DT3 or GT3, no adverse effects were observed in any tissues or organs., (© The Author(s) 2014.)

Published

2014

22. Assessment of efficacy of proarrhythmia biomarkers in isolated rabbit hearts with attenuated repolarization reserve.

Author

Orosz S, Sarusi A, Csík N, Papp JG, Varró A, Farkas S, Forster T, Farkas AS, and Farkas A

Subjects

Animals, Arrhythmias, Cardiac physiopathology, Biomarkers metabolism, Chromans administration & dosage, Chromans pharmacology, Dose-Response Relationship, Drug, Electrocardiography, Female, Phenethylamines administration & dosage, Phenethylamines pharmacology, Rabbits, Sulfonamides administration & dosage, Sulfonamides pharmacology, Torsades de Pointes physiopathology, Arrhythmias, Cardiac chemically induced, Chromans toxicity, Phenethylamines toxicity, Sulfonamides toxicity, Torsades de Pointes chemically induced

Abstract

Isolated hearts with reduced repolarization reserve would be suitable for assessing the proarrhythmic liability of drugs. However, it is not known which proarrhythmia biomarkers indicate the increased susceptibility to torsades de pointes arrhythmia (TdP) in such experimental setting. Thus, we estimated the efficacy of proarrhythmia biomarkers in isolated hearts with attenuated repolarization reserve. Langendorff-perfused rabbit hearts were used. Repolarization reserve was reduced by concomitant inhibition of the rapid (IKr) and slow (IKs) delayed rectifier potassium currents by dofetilide and HMR-1556, respectively. Rate corrected QT (QTc) interval and beat-to-beat variability of the QT interval measured in sinus rhythm or irrespective of rhythm even during arrhythmias (sinus and absolute QT variability, respectively) were tested. QTc failed to predict increased proarrhythmic risk. Sinus QT variability indicated proarrhythmic liability when low concentration of dofetilide was used. However, when arrhythmias compromised sinus variability measurement during coperfusion of catecholamines and elevated concentration of dofetilide, only absolute QT variability indicated increased proarrhythmic risk. Absolute QT variability parameters seem to be the most practical and sensitive biomarkers of proarrhythmic liability in rabbit hearts with reduced repolarization reserve. Absolute QT variability parameters could serve as surrogates for torsades de pointes in drug-safety investigations in isolated rabbit hearts with attenuated repolarization reserve.

Published

2014

23. Optimization of troglitazone derivatives as potent anti-proliferative agents: towards more active and less toxic compounds.

Author

Bordessa A, Colin-Cassin C, Grillier-Vuissoz I, Kuntz S, Mazerbourg S, Husson G, Vo M, Flament S, Martin H, Chapleur Y, and Boisbrun M

Subjects

Antineoplastic Agents chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, Chromans chemistry, Hepatocytes cytology, Hepatocytes drug effects, Humans, Thiazolidinediones chemistry, Troglitazone, Antineoplastic Agents pharmacology, Antineoplastic Agents toxicity, Chromans pharmacology, Chromans toxicity, Drug Design, Thiazolidinediones pharmacology, Thiazolidinediones toxicity

Abstract

Δ2-Troglitazone derivatives were shown to exhibit anti-proliferative activity in a PPARγ-independent manner. We prepared various compounds in order to increase their potency and decrease their toxicity towards non-malignant primary cultured hepatocytes. Many compounds induced viabilities less than 20% at 10 μM on various cancer cell lines. Furthermore, five of them showed hepatocyte viability of 80% or more at 200 μM. In addition, compounds 17 and 18 exhibited promising maximum tolerated doses on a murine model, enabling future investigations., (Copyright © 2014 Elsevier Masson SAS. All rights reserved.)

Published

2014

24. Synergistic effect of combined treatment with gamma-tocotrienol and statin on human malignant mesothelioma cells.

Author

Tuerdi G, Ichinomiya S, Sato H, Siddig S, Suwa E, Iwata H, Yano T, and Ueno K

Subjects

Apoptosis drug effects, Atorvastatin, Caspase 3 metabolism, Cell Line, Tumor, Cell Proliferation drug effects, Chromans administration & dosage, Chromans toxicity, Drug Synergism, Endoplasmic Reticulum Chaperone BiP, Endoplasmic Reticulum Stress drug effects, Enzyme Activation drug effects, Heptanoic Acids, Humans, Hydroxymethylglutaryl CoA Reductases genetics, Hydroxymethylglutaryl CoA Reductases metabolism, Hydroxymethylglutaryl-CoA Reductase Inhibitors administration & dosage, Hydroxymethylglutaryl-CoA Reductase Inhibitors toxicity, Mesothelioma genetics, Metabolic Networks and Pathways drug effects, Mevalonic Acid metabolism, Proto-Oncogene Proteins c-bcl-2 metabolism, Pyrroles, Simvastatin, Vitamin E administration & dosage, Vitamin E pharmacology, Vitamin E toxicity, Chromans pharmacology, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Mesothelioma metabolism, Vitamin E analogs & derivatives

Abstract

The present study is the first to demonstrate the synergetic effect of statins (atorvastatin and simvastatin) and gamma-tocotrienol (γ-T3) on human malignant mesothelioma (MM). Statin + γ-T3 combinations induced greater cell growth inhibition more than each single treatment via inhibition of mevalonate pathway, a well-known target of both γ-T3 and statins. γ-T3 was necessary for endoplasmic reticulum stress markers CHOP and GRP78, whereas an intrinsic apoptotic marker, caspase 3 activation was induced only in the presence of statins. Overall, the combination of γ-T3 and statins could be useful for MM therapy and functions in a complementary style., (Copyright © 2013 Elsevier Ireland Ltd. All rights reserved.)

Published

2013

25. A dynamic multi-organ-chip for long-term cultivation and substance testing proven by 3D human liver and skin tissue co-culture.

Author

Wagner I, Materne EM, Brincker S, Süssbier U, Frädrich C, Busek M, Sonntag F, Sakharov DA, Trushkin EV, Tonevitsky AG, Lauster R, and Marx U

Subjects

Biomass, Cell Line, Cell Survival drug effects, Chromans toxicity, Humans, Liver drug effects, Liver metabolism, RNA metabolism, Skin drug effects, Skin metabolism, Thiazolidinediones toxicity, Tissue Culture Techniques, Troglitazone, Coculture Techniques instrumentation, Liver cytology, Microfluidic Analytical Techniques instrumentation, Skin cytology

Abstract

Current in vitro and animal tests for drug development are failing to emulate the systemic organ complexity of the human body and, therefore, to accurately predict drug toxicity. In this study, we present a multi-organ-chip capable of maintaining 3D tissues derived from cell lines, primary cells and biopsies of various human organs. We designed a multi-organ-chip with co-cultures of human artificial liver microtissues and skin biopsies, each a (1)/100,000 of the biomass of their original human organ counterparts, and have successfully proven its long-term performance. The system supports two different culture modes: i) tissue exposed to the fluid flow, or ii) tissue shielded from the underlying fluid flow by standard Transwell® cultures. Crosstalk between the two tissues was observed in 14-day co-cultures exposed to fluid flow. Applying the same culture mode, liver microtissues showed sensitivity at different molecular levels to the toxic substance troglitazone during a 6-day exposure. Finally, an astonishingly stable long-term performance of the Transwell®-based co-cultures could be observed over a 28-day period. This mode facilitates exposure of skin at the air-liquid interface. Thus, we provide here a potential new tool for systemic substance testing.

Published

2013

26. Structure-cytotoxic activity relationship of 3-arylideneflavanone and chromanone (E,Z isomers) and 3-arylflavones.

Author

Kupcewicz B, Balcerowska-Czerniak G, Małecka M, Paneth P, Krajewska U, and Rozalski M

Subjects

Apoptosis drug effects, Cell Line, Tumor, Chromans toxicity, Crystallography, X-Ray, Drug Screening Assays, Antitumor, Flavanones toxicity, HL-60 Cells, Human Umbilical Vein Endothelial Cells, Humans, Molecular Conformation, Quantitative Structure-Activity Relationship, Stereoisomerism, Chromans chemistry, Flavanones chemistry

Abstract

The E,Z-isomers of 3-arylidene substituted flavanone, chromanone and 3-aryl substituted flavone derivatives were tested in vitro for their cytotoxic activity against three cancer cell lines (HL-60, NALM-6, WM-115) and normal cell line (HUVEC). It was observed that substitution at C3 position led to significant enhance in cytotoxicity. Isomeric configuration of 3-arylideneflavanones had an influence on the cytotoxic potential. Multiple regression analysis combined with variable selection by genetic algorithm was used to model relationships between molecular descriptors and the cytotoxic activity. The most accurate QSAR models were based on a combination between energy of LUMO, experimental value of logP and partial charge on carbonyl oxygen (δO2)., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

27. Oral toxicity and pharmacokinetic studies of SHetA2, a new chemopreventive agent, in rats and dogs.

Author

Kabirov KK, Kapetanovic IM, Benbrook DM, Dinger N, Mankovskaya I, Zakharov A, Detrisac C, Pereira M, Martín-Jiménez T, Onua E, Banerjee A, van Breemen RB, Nikolić D, Chen L, and Lyubimov AV

Subjects

Administration, Oral, Adrenal Glands drug effects, Adrenal Glands pathology, Animals, Anticarcinogenic Agents administration & dosage, Area Under Curve, Chromans administration & dosage, Dogs, Eating drug effects, Female, Male, Motor Activity drug effects, No-Observed-Adverse-Effect Level, Organ Size drug effects, Prostate drug effects, Prostate pathology, Rats, Rats, Sprague-Dawley, Species Specificity, Thiones administration & dosage, Toxicity Tests, Weight Gain drug effects, Anticarcinogenic Agents pharmacokinetics, Anticarcinogenic Agents toxicity, Chromans pharmacokinetics, Chromans toxicity, Thiones pharmacokinetics, Thiones toxicity

Abstract

SHetA2 is a heteroarotinoid that has shown selective inhibition of cancer cell growth and an induction of apoptosis without activation of nuclear retinoic acid receptors. In the rat study, SHetA2 was administered in 1% aqueous methylcellulose/0.2% Tween 80 by oral gavage at 0, 100, 500, and 2,000 mg/kg/day for 28 days. The high-dose administration induced decreased activity in male rats, decreased body-weight gains and food consumption, and changes in organ weights. The major metabolite of SHetA2 in rat plasma was monohydroxy SHetA2, which was considerably higher than the parent compound after oral and intravenous administration. Pharmacokinetic analysis showed extremely low (<1%) systemic bioavailability of SHetA2 for all doses tested. The dose of 2,000 mg/kg/day was considered as the lowest observed adverse effect level. The no observed adverse effect level (NOAEL) was 500 mg/kg/day. In the dog study, no toxicity of SHetA2 in 30% aqueous Solutol(®) HS 15 was observed in any tested dose groups (0, 100, 400, and 1,500 mg/kg/day). The major metabolite of SHetA2 in dog plasma was also monohydroxy SHetA2, which was equal to or lower than the parent compound after oral administration. SHetA2 levels in dog plasma were notably higher, when compared to levels in rat plasma. However, exposure was not dose proportional, as exemplified by a lack of proportional increase in maximum concentration or area under the plasma concentration-time curve with increasing dose. The NOAEL was not established and was considered to be above 1,500 mg/kg/day.

Published

2013

28. Integrative toxicoproteomics implicates impaired mitochondrial glutathione import as an off-target effect of troglitazone.

Author

Lee YH, Goh WW, Ng CK, Raida M, Wong L, Lin Q, Boelsterli UA, and Chung MC

Subjects

Animals, Dicarboxylic Acid Transporters antagonists & inhibitors, Dicarboxylic Acid Transporters genetics, Dicarboxylic Acid Transporters metabolism, Female, Forkhead Box Protein O3, Forkhead Transcription Factors agonists, Forkhead Transcription Factors genetics, Forkhead Transcription Factors metabolism, Gene Expression Regulation drug effects, Glutathione metabolism, Humans, Ion Transport drug effects, MAP Kinase Kinase 4 genetics, MAP Kinase Kinase 4 metabolism, MAP Kinase Kinase Kinase 5 genetics, MAP Kinase Kinase Kinase 5 metabolism, Male, Mice, Mice, Knockout, Mitochondria genetics, Mitochondria metabolism, Mitochondrial Proteins metabolism, Oxidative Stress drug effects, Signal Transduction, Superoxide Dismutase deficiency, Superoxide Dismutase genetics, Troglitazone, Chromans toxicity, Glutathione antagonists & inhibitors, Hypoglycemic Agents toxicity, Mitochondria drug effects, Mitochondrial Proteins genetics, Proteomics, Thiazolidinediones toxicity

Abstract

Troglitazone, a first-generation thiazolidinedione of antihyperglycaemic properties, was withdrawn from the market due to unacceptable idiosyncratic hepatotoxicity. Despite intensive research, the underlying mechanism of troglitazone-induced liver toxicity remains unknown. Here we report the use of the Sod2(+/-) mouse model of silent mitochondrial oxidative-stress-based and quantitative mass spectrometry-based proteomics to track the mitochondrial proteome changes induced by physiologically relevant troglitazone doses. By quantitative untargeted proteomics, we first globally profiled the Sod2(+/-) hepatic mitochondria proteome and found perturbations including GSH metabolism that enhanced the toxicity of the normally nontoxic troglitazone. Short- and long-term troglitazone administration in Sod2(+/-) mouse led to a mitochondrial proteome shift from an early compensatory response to an eventual phase of intolerable oxidative stress, due to decreased mitochondrial glutathione (mGSH) import protein, decreased dicarboxylate ion carrier (DIC), and the specific activation of ASK1-JNK and FOXO3a with prolonged troglitazone exposure. Furthermore, mapping of the detected proteins onto mouse specific protein-centered networks revealed lipid-associated proteins as contributors to overt mitochondrial and liver injury when under prolonged exposure to the lipid-normalizing troglitazone. By integrative toxicoproteomics, we demonstrated a powerful systems approach in identifying the collapse of specific fragile nodes and activation of crucial proteome reconfiguration regulators when targeted by an exogenous toxicant.

Published

2013

29. 3D organotypic cultures of human HepaRG cells: a tool for in vitro toxicity studies.

Author

Gunness P, Mueller D, Shevchenko V, Heinzle E, Ingelman-Sundberg M, and Noor F

Subjects

ATP Binding Cassette Transporter, Subfamily B metabolism, Acetaminophen toxicity, Albumins metabolism, Cell Line, Tumor, Chromans toxicity, Cytochrome P-450 Enzyme System biosynthesis, Cytochrome P-450 Enzyme System metabolism, Cytochrome P450 Family 2, Hepatocytes enzymology, Hepatocytes metabolism, High-Throughput Screening Assays, Humans, Liver enzymology, Liver metabolism, Multidrug Resistance-Associated Protein 2, Rosiglitazone, Spheroids, Cellular enzymology, Spheroids, Cellular metabolism, Thiazolidinediones toxicity, Troglitazone, Urea metabolism, ATP-Binding Cassette Sub-Family B Member 4, Cell Culture Techniques methods, Hepatocytes drug effects, Liver drug effects, Spheroids, Cellular drug effects, Toxicity Tests, Acute methods

Abstract

Drug-induced human hepatotoxicity is difficult to predict using the current in vitro systems. In this study, long-term 3D organotypic cultures of the human hepatoma HepaRG cell line were prepared using a high-throughput hanging drop method. The organotypic cultures were maintained for 3 weeks and assessed for (1) liver specific functions, including phase I enzyme and transporter activities, (2) expression of liver-specific proteins, and (3) responses to three drugs (acetaminophen, troglitazone, and rosiglitazone). Our results show that the organotypic cultures maintain high liver-specific functionality during 3 weeks of culture. The immunohistochemistry analyses illustrate that the organotypic cultures express liver-specific markers such as albumin, CYP3A4, CYP2E1, and MRP-2 throughout the cultivation period. Accordingly, the production rates of albumin and glucose, as well as CYP2E1 activity, were significantly higher in the 3D versus the 2D cultures. Toxicity studies show that the organotypic cultures are more sensitive to acetaminophen- and rosiglitazone-induced toxicity but less sensitive to troglitazone-induced toxicity than the 2D cultures. Furthermore, the EC50 value (2.7mM) for acetaminophen on the 3D cultures was similar to in vivo toxicity. In summary, the results from our study suggest that the 3D organotypic HepaRG culture is a promising in vitro tool for more accurate assessment of acute and also possibly for chronic drug-induced hepatotoxicity.

Published

2013

30. Pyrrolidinediones reduce the toxicity of thiazolidinediones and modify their anti-diabetic and anti-cancer properties.

Author

Saha S, Chan DS, Lee CY, Wong W, New LS, Chui WK, Yap CW, Chan EC, and Ho HK

Subjects

3T3-L1 Cells, Animals, Antineoplastic Agents chemistry, Antineoplastic Agents metabolism, Biotransformation, Caspase 3 metabolism, Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, Chromans toxicity, Dose-Response Relationship, Drug, Fatty Acid-Binding Proteins genetics, Fatty Acid-Binding Proteins metabolism, Gene Expression Regulation, Glutathione metabolism, Humans, Hypoglycemic Agents chemistry, Hypoglycemic Agents metabolism, Liver Neoplasms metabolism, Liver Neoplasms pathology, Mice, Microsomes, Liver drug effects, Microsomes, Liver metabolism, Molecular Structure, PPAR gamma agonists, PPAR gamma metabolism, Phosphorylation, Pioglitazone, Protein Carbonylation drug effects, Receptor Protein-Tyrosine Kinases drug effects, Receptor Protein-Tyrosine Kinases metabolism, Receptors, Peptide metabolism, Rosiglitazone, Structure-Activity Relationship, Succinimides chemistry, Succinimides metabolism, Thiazolidinediones chemistry, Thiazolidinediones metabolism, Troglitazone, Antineoplastic Agents toxicity, Drug Design, Hypoglycemic Agents toxicity, Succinimides toxicity, Thiazolidinediones toxicity

Abstract

Thiazolidinediones have been established as a drug class of significant importance in the treatment of Type II diabetes mellitus and have more recently displayed emergent potential as anti-cancer agents. However, their toxicity has hampered clinical development and usage in both therapeutic areas. Studies to date have implicated that the thiazolidinedione ring is responsible for the generation of reactive metabolites after metabolism. As an attempt to improve their safety profiles, we considered the bioisosteric replacement of the thiazolidinedione ring with a chemically conserved pyrrolidinedione heterocyclic system. Using pyrrolidinedione analogs of the thiazolidinedione drugs troglitazone (TGZ), rosiglitazone (RGZ), and pioglitazone (PGZ), we evaluated their PPAR(γ) activities, anti-cancer properties as well as toxicological effects. Of significance, both pyrrolidinedione analogs demonstrated reduced toxicity. Pharmacologically, they also displayed diminished PPAR(γ) binding and ap2 gene expression in a mouse pre-adipocyte cell line 3T3-L1, but enhanced anti-cancer properties based on the suppression of liver cancer cell line (Huh-7) proliferation and the expression of tumor marker, afp. Overall, this study ascertains the general contribution of the thiazolidinedione ring to their cytotoxicity and proposes the applicability of the pyrrolidinedione ring as a selective and safer choice in anti-diabetic and cancer chemotherapeutics for future drug design., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

31. Differential effect of troglitazone on the human bile acid transporters, MRP2 and BSEP, in the PXB hepatic chimeric mouse.

Author

Foster JR, Jacobsen M, Kenna G, Schulz-Utermoehl T, Morikawa Y, Salmu J, and Wilson ID

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 11, Animals, Child, Preschool, Cytochrome P-450 Enzyme System metabolism, Disease Models, Animal, Down-Regulation drug effects, Female, Hepatocytes metabolism, Hepatocytes transplantation, Hepatocytes ultrastructure, Humans, Liver metabolism, Liver pathology, Male, Mice, Mice, SCID, Mice, Transgenic, Multidrug Resistance-Associated Protein 2, Organ Size drug effects, PPAR gamma agonists, Species Specificity, Troglitazone, ATP-Binding Cassette Transporters metabolism, Chromans toxicity, Hepatocytes drug effects, Liver drug effects, Multidrug Resistance-Associated Proteins metabolism, Thiazolidinediones toxicity, Transplantation Chimera

Abstract

The aims of this study were to assess the utility of the PXB mouse model of a chimeric human/mouse liver in studying human-specific effects of an important human hepatotoxic drug, the PPARγ agonist, troglitazone. When given orally by gavage for 7 days, at dose levels of 300 and 600 ppm, troglitazone induced specific changes in the human hepatocytes of the chimeric liver without an effect on the murine hepatic portions. The human hepatocytes, in the vehicle-treated PXB mouse, showed an accumulation of electron-dense lipid droplets that appeared as clear vacuoles under the light microscope in H&E-stained sections. Following dosing with troglitazone, there was a loss of the large lipid droplets in the human hepatocytes, a decrease in the amount of lipid as observed in frozen sections of liver stained by Oil-red-O, and a decrease in the expression of two bile acid transporters, BSEP and MRP2. None of these changes were observed in the murine remnants of the chimeric liver. No changes were observed in the expression of three CYPs, CYP 3A2, CYP 1A1, and CYP 2B1, in either the human or murine hepatocytes, even though the baseline expression of the enzymes differed significantly between the two hepatocyte species with the mouse hepatocytes consistently showing increased expression of the protein of all three enzymes. This study has shown that the human hepatocytes, in the PXB chimeric mouse liver, retain an essentially normal phenotype in the mouse liver and, the albeit limited CYP enzymes studied show a more human, rather than a murine, expression pattern. In line with this conclusion, the study has shown a differential response of the human versus the mouse hepatocytes, and the effects observed are highly suggestive of a differential handling of the compound by the two hepatocyte species although the exact reasons are not as yet clear. The PXB chimeric mouse system therefore holds the clear potential to explore human hepatic-specific features, such as metabolism, prior to dosing human subjects, and as such should have considerable utility in drug discovery and development.

Published

2012

32. Real-time concurrent monitoring of apoptosis, cytosolic calcium, and mitochondria permeability transition for hypermulticolor high-content screening of drug-induced mitochondrial dysfunction-mediated hepatotoxicity.

Author

Kim JA, Han E, Eun CJ, Tak YK, and Song JM

Subjects

Apoptosis drug effects, Apoptosis physiology, Calcium metabolism, Caspase 3 metabolism, Chemical and Drug Induced Liver Injury metabolism, Chemical and Drug Induced Liver Injury pathology, Hep G2 Cells, Humans, Image Processing, Computer-Assisted, Liver cytology, Liver metabolism, Microscopy, Fluorescence methods, Mitochondria, Liver metabolism, Mitochondrial Membrane Transport Proteins drug effects, Mitochondrial Membrane Transport Proteins metabolism, Mitochondrial Permeability Transition Pore, Piperazines, Tolcapone, Troglitazone, Benzophenones toxicity, Chemical and Drug Induced Liver Injury etiology, Chromans toxicity, Imidazoles toxicity, Liver drug effects, Mitochondria, Liver drug effects, Nitrophenols toxicity, Thiazolidinediones toxicity, Triazoles toxicity

Abstract

A quantitative high-content screening (HCS) was suggested for the real-time monitoring of drug-induced mitochondrial dysfunction-mediated hepatotoxicity. This HCS is very advantageous in that it allows simultaneous observation of drug-induced activations of hepatotoxic pathways using hypermulticolor cellular imaging. The mitochondrial permeability transition (MPT), cytosolic calcium, and caspase-3 were selected as functional markers to verify drug-induced hepatotoxicity and were concurrently monitored in HepG2 cells in a real-time manner. Nefazodone, tolcapone, and troglitazone caused mitochondrial dysfunction and subsequent apoptotic HepG2 cell death in addition to marked cytosolic calcium increase. On the other hand, extrinsic pathway-mediated apoptotic cell death was monitored when HepG2 cells were treated with piroxicam. It was found that piroxicam-treated HepG2 cells showed apoptotic cell death without the MPT formation, while a cytosolic calcium increase was clearly observed. This finding was confirmed by the caspase-8 inhibition assay. These results demonstrated the unique potential of real-time hypermulticolor HCS to screen hepatotoxic drugs at the in vitro stage rather than the later in vivo stage based on an animal model and to ultimately reduce the probability of drug failure., (Copyright © 2012 Elsevier Ireland Ltd. All rights reserved.)

Published

2012

33. Chimeric mice with a humanized liver as an animal model of troglitazone-induced liver injury.

Author

Kakuni M, Morita M, Matsuo K, Katoh Y, Nakajima M, Tateno C, and Yokoi T

Subjects

Animals, Buthionine Sulfoximine pharmacology, Dose-Response Relationship, Drug, Glutathione metabolism, Humans, Liver metabolism, Liver pathology, Mice, Troglitazone, Antineoplastic Agents toxicity, Chemical and Drug Induced Liver Injury pathology, Chromans toxicity, Thiazolidinediones toxicity, Transplantation Chimera metabolism

Abstract

Troglitazone (Tro) is a thiazolidinedione antidiabetic drug that was withdrawn from the market due to its association with idiosyncratic severe liver injury. Tro has never induced liver injury in experimental animals in vivo. It was assumed that the species differences between human and experimental animals in the pharmaco- or toxicokinetics of Tro might be associated with these observations. In this study, we investigated whether a chimeric mouse with a humanized liver that we previously established, whose replacement index with human hepatocytes is up to 92% can reproduce Tro-induced liver injury. When the chimeric mice were orally administered Tro for 14 or 23 days (1000mg/kg/day), serum alanine aminotransferase (ALT) was significantly increased by 2.1- and 3.6-fold, respectively. Co-administration of l-buthionine sulfoximine (10mM in drinking water), an inhibitor of glutathione (GSH) synthesis, unexpectedly prevented the Tro-dependent increase of ALT, which suggests that the GSH scavenging pathway will not be involved in Tro-induced liver injury. To elucidate the mechanism of the onset of liver injury, hepatic GSH content, the level of oxidative stress markers and phase I and phase II drug metabolizing enzymes were determined. However, these factors were not associated with Tro-induced liver injury. An immune-mediated reaction may be associated with Tro-induced liver toxicity in vivo, because the chimeric mouse is derived from an immunodeficient SCID mouse. In conclusion, we successfully reproduced Tro-induced liver injury using chimeric mice with a humanized liver, which provides a new animal model for studying idiosyncratic drug-induced liver injury., (Copyright © 2012 Elsevier Ireland Ltd. All rights reserved.)

Published

2012

34. Mouse precision-cut liver slices as an ex vivo model to study idiosyncratic drug-induced liver injury.

Author

Hadi M, Chen Y, Starokozhko V, Merema MT, and Groothuis GM

Subjects

Animals, Benzodiazepines chemistry, Benzodiazepines toxicity, Biomarkers metabolism, Carbamazepine chemistry, Carbamazepine toxicity, Cell Survival drug effects, Chemical and Drug Induced Liver Injury metabolism, Chemokines metabolism, Chromans chemistry, Chromans toxicity, Clozapine chemistry, Clozapine toxicity, Cytokines metabolism, Diclofenac chemistry, Diclofenac toxicity, Drug Synergism, Female, Glutathione metabolism, Granulocyte Colony-Stimulating Factor metabolism, Granulocyte-Macrophage Colony-Stimulating Factor metabolism, In Vitro Techniques, Ketoconazole chemistry, Ketoconazole toxicity, Lipopolysaccharides toxicity, Mice, Mice, Inbred C57BL, Nitrogen Oxides metabolism, Olanzapine, Pyrimidines chemistry, Pyrimidines toxicity, Thiazolidinediones chemistry, Thiazolidinediones toxicity, Triazoles chemistry, Triazoles toxicity, Troglitazone, Voriconazole, Chemical and Drug Induced Liver Injury pathology

Abstract

Idiosyncratic drug-induced liver injury (IDILI) has been the top reason for withdrawing drugs from the market or for black box warnings. IDILI may arise from the interaction of a drug's reactive metabolite with a mild inflammation that renders the liver more sensitive to injury resulting in increased toxicity (inflammatory stress hypothesis). Aiming to develop a robust ex vivo screening method to study inflammatory stress-related IDILI mechanisms and to find biomarkers that can detect or predict IDILI, mouse precision-cut liver slices (mPCLS) were coincubated for 24 h with IDILI-related drugs and lipopolysaccharide. Lipopolysaccharide exacerbated ketoconazole (15 μM) and clozapine (45 μM) toxicity but not their non-IDILI-related comparators, voriconazole (1500 μM) and olanzapine (45 μM). However, the other IDILI-related drugs tested [diclofenac (200 μM), carbamazepine (400 μM), and troglitazone (30 μM)] did not cause synergistic toxicity with lipopolysaccharide after 24 h of incubation. Lipopolysaccharide further decreased the reduced glutathione levels caused by ketoconazole or clozapine in mPCLS after 24 h of incubation, which was not the case for the other drugs. Lipopolysaccharide significantly increased nitric oxide (NO), cytokine, and chemokine release into the mPCLS media, while the treatment with the drugs alone did not cause any substantial change. All seven drugs drastically reduced lipopolysaccharide-induced NO production. Interestingly, only ketoconazole and clozapine increased the lipopolysaccharide-induced granulocyte colony-stimulating factor (G-CSF) and granulocyte-macrophage colony-stimulating factor (GM-CSF) release. Pilot experiments showed that diclofenac and troglitazone, but not carbamazepine, demonstrated synergistic toxicity with lipopolysaccharide after a longer incubation of 48 h in mPCLS. In conclusion, we have developed an ex vivo model to detect inflammatory stress-related liver toxicity and identified ketoconazole, clozapine, troglitazone, and diclofenac as drugs that showed synergistic toxicity with lipopolysaccharide. Reduced glutathione, G-CSF, and GM-CSF were identified to be potential biomarkers for IDILI-inducing drugs mediated by inflammatory stress, and mPCLS appear to be a promising screening tool to further unravel the mechanism of IDILI.

Published

2012

35. Genotoxicity of the cancer chemopreventive drug candidates CP-31398, SHetA2, and phospho-ibuprofen.

Author

Doppalapudi RS, Riccio ES, Davis Z, Menda S, Wang A, Du N, Green C, Kopelovich L, Rao CV, Benbrook DM, and Kapetanovic IM

Subjects

Animals, CHO Cells, Chromosome Aberrations, Cricetinae, Cricetulus, Dose-Response Relationship, Drug, Female, Humans, Ibuprofen toxicity, Mice, Micronucleus Tests, Mutagenicity Tests methods, Rats, Rats, Inbred F344, Salmonella typhimurium genetics, Anticarcinogenic Agents toxicity, Chromans toxicity, DNA Damage drug effects, Ibuprofen analogs & derivatives, Mutagens toxicity, Organophosphates toxicity, Pyrimidines toxicity, Thiones toxicity

Abstract

The genotoxic activities of three cancer chemopreventive drug candidates, CP-31398 (a cell permeable styrylquinazoline p53 modulator), SHetA2 (a flexible heteroarotinoid), and phospho-ibuprofen (PI, a derivative of ibuprofen) were tested. None of the compounds were mutagenic in the Salmonella/Escherichia coli/microsome plate incorporation test. CP-31398 and SHetA2 did not induce chromosomal aberrations (CA) in Chinese hamster ovary (CHO) cells, either in the presence or absence of rat hepatic S9 (S9). PI induced CA in CHO cells, but only in the presence of S9. PI, its parent compound ibuprofen, and its moiety diethoxyphosphoryloxybutyl alcohol (DEPBA) were tested for CA and micronuclei (MN) in CHO cells in the presence of S9. PI induced CA as well as MN, both kinetochore-positive (Kin+) and -negative (Kin-), in the presence of S9 at ≤100μg/ml. Ibuprofen was negative for CA, positive for MN with Kin+ at 250μg/ml, and positive for MN with Kin- at 125 and 250μg/ml. DEPBA induced neither CA nor MN at ≤5000μg/ml. The induction of chromosomal damage in PI-treated CHO cells in the presence of S9 may be due to its metabolites. None of the compounds were genotoxic, in the presence or absence of S9, in the GADD45α-GFP Human GreenScreen assay and none induced MN in mouse bone marrow erythrocytes., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

36. The development of subcutaneous sarcomas in rodents exposed to peroxisome proliferators agonists: hypothetical mechanisms of action and de-risking attitude.

Author

Pruimboom-Brees IM, Francone O, Pettersen JC, Kerlin RL, Will Y, Amacher DE, Boucher GG, and Morton D

Subjects

Adipogenesis drug effects, Adipose Tissue, Brown drug effects, Adipose Tissue, Brown metabolism, Adipose Tissue, White drug effects, Adipose Tissue, White metabolism, Animals, Cell Differentiation, Chromans toxicity, DNA Damage drug effects, Diabetes Mellitus, Type 2 physiopathology, Diabetes Mellitus, Type 2 therapy, Glycine analogs & derivatives, Glycine toxicity, Ion Channels genetics, Ion Channels metabolism, Mice, Mitochondria drug effects, Mitochondria metabolism, Mitochondrial Proteins genetics, Mitochondrial Proteins metabolism, Oxazoles toxicity, Oxidative Stress drug effects, PPAR alpha genetics, PPAR alpha metabolism, PPAR gamma genetics, PPAR gamma metabolism, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Pioglitazone, RNA-Binding Proteins genetics, RNA-Binding Proteins metabolism, Rats, Rodentia metabolism, Rosiglitazone, Sarcoma pathology, Thermogenesis drug effects, Thiazolidinediones toxicity, Transcription Factors genetics, Transcription Factors metabolism, Troglitazone, Uncoupling Protein 1, Hypoglycemic Agents toxicity, PPAR alpha agonists, PPAR gamma agonists, Sarcoma chemically induced

Abstract

Peroxisome proliferator-activated receptors (PPARs) represent therapeutic targets for the management of type 2 diabetes mellitus and dyslipidemia. Rodent carcinogenicity studies have revealed a link between γ and dual γ/α PPAR agonist treatment and the increased incidence of subcutaneous (SC) liposarcomas/fibrosarcomas or hemangiosarcomas, but very little has been reported for potent and selective PPARα agonists. We present a mode of action framework for the development of SC mesenchymal tumors in rodents given PPAR agonists. (1) Tumor promotion results from pharmacologically mediated recruitment (proliferation and differentiation), thermogenesis and adipogenesis of stromovascular cells, and subsequent generation of oxidative free radicals. (2) Tumor initiation consists of chemotype-driven mitochondrial dysfunction causing uncontrolled oxidative stress and permanent DNA damage. Promotion is characterized by enhanced adipogenesis in the SC adipose tissue, where the baseline PPARγ expression and responsiveness to PPARγ ligands is the highest, and by thermogenesis through expression of the uncoupling protein 1 (UCP-1) and the PPARγ co-activator 1 α (PGC-1α), two factors more highly expressed in brown versus white adipose tissue. Initiation is supported by the demonstration of mitochondrial uncoupling and OXPHOS Complexes dysfunction (Complexes III, IV and V) by compounds associated with increased incidences of sarcomas (muraglitazar and troglitazone), but not others lacking malignant tumor effects (pioglitazone, rosiglitazone).

Published

2012

37. δ- and γ-tocotrienols induce classical ultrastructural apoptotic changes in human T lymphoblastic leukemic cells.

Author

Wong RS, Radhakrishnan AK, Ibrahim TA, and Cheong SK

Subjects

Cell Line, Tumor, Cell Nucleus ultrastructure, Cell Survival drug effects, Chromatin ultrastructure, Humans, Microscopy, Electron, Transmission, T-Lymphocytes physiology, T-Lymphocytes ultrastructure, Tocotrienols, Vitamin E toxicity, Apoptosis, Chromans toxicity, T-Lymphocytes drug effects, Vitamin E analogs & derivatives

Abstract

Tocotrienols are isomers of the vitamin E family, which have been reported to exert cytotoxic effects in various cancer cells. Although there have been some reports on the effects of tocotrienols in leukemic cells, ultrastructural evidence of tocotrienol-induced apoptotic cell death in leukemic cells is lacking. The present study investigated the effects of three isomers of tocotrienols (alpha, delta, and gamma) on a human T lymphoblastic leukemic cell line (CEM-SS). Cell viability assays showed that all three isomers had cytotoxic effects (p < 0.05) on CEM-SS cells with delta-tocotrienol being the most potent. Transmission electron microscopy showed that the cytotoxic effects by delta- and gamma-tocotrienols were through the induction of an apoptotic pathway as demonstrated by the classical ultrastructural apoptotic changes characterized by peripheral nuclear chromatin condensation and nuclear fragmentation. These findings were confirmed biochemically by the demonstration of phosphatidylserine externalization via flow cytometry analysis. This is the first study showing classical ultrastructural apoptotic changes induced by delta- and gamma-tocotrienols in human T lymphoblastic leukemic cells.

Published

2012

38. Synthesis of new troglitazone derivatives: anti-proliferative activity in breast cancer cell lines and preliminary toxicological study.

Author

Salamone S, Colin C, Grillier-Vuissoz I, Kuntz S, Mazerbourg S, Flament S, Martin H, Richert L, Chapleur Y, and Boisbrun M

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, Chromans chemical synthesis, Chromans chemistry, Hepatocytes cytology, Hepatocytes drug effects, Humans, Thiazolidinediones chemical synthesis, Thiazolidinediones chemistry, Troglitazone, Antineoplastic Agents pharmacology, Antineoplastic Agents toxicity, Breast Neoplasms pathology, Chemistry Techniques, Synthetic, Chromans pharmacology, Chromans toxicity, Thiazolidinediones pharmacology, Thiazolidinediones toxicity, Toxicity Tests

Abstract

Breast cancer is the most prevalent cancer in women. The development of resistances to therapeutic agents and the absence of targeted therapy for triple negative breast cancer motivate the search for alternative treatments. With this aim in mind, we synthesised new derivatives of troglitazone, a compound which was formerly used as an anti-diabetic agent and which exhibits anti-proliferative activity on various cancer cell lines. Among the compounds prepared, some displayed micromolar activity against hormone-dependent and hormone-independent breast cancer cells. Furthermore, the influence of the compounds on the viability of primary cultures of human hepatocytes was evaluated. This enabled us to obtain for the first time interesting structure-toxicity relationships in this family of compounds, resulting in 6b and 8b, which show good anti-proliferative activities and poor toxicity towards hepatocytes, compared to troglitazone., (Copyright © 2012 Elsevier Masson SAS. All rights reserved.)

Published

2012

39. Species-specific toxicity of troglitazone on rats and human by gel entrapped hepatocytes.

Author

Shen C, Meng Q, and Zhang G

Subjects

Animals, Cells, Cultured, Hepatocytes ultrastructure, Humans, Male, Rats, Rats, Sprague-Dawley, Species Specificity, Troglitazone, Chromans toxicity, Hepatocytes drug effects, Hypoglycemic Agents toxicity, Thiazolidinediones toxicity

Abstract

Troglitazone, despite passing preclinical trials on animals, was shortly withdrawn from market due to its severe hepatotoxicity in clinic. As rat hepatocyte monolayer consistently showed sensitive troglitazone toxicity as human hepatocyte monolayer in contrast to the species-specific toxicity in vivo, this paper utilized both hepatocytes in three-dimensional culture of gel entrapment to reflect the species difference on hepatotoxicity. Rat hepatocytes in gel entrapment did not show obvious cellular damage even under a long-term exposure for 21 days while gel entrapped human hepatocytes significantly displayed oxidative stress, steatosis, mitochondrial damage and cell death at a short exposure for 4 days. As a result, the detected species-specific toxicity of troglitazone between gel entrapped rat and human hepatocytes consisted well with the situation in vivo but was in a sharp contrast to the performance of two hepatocytes by monolayer culture. Such contradictory toxicity of rat hepatocytes between monolayer and gel entrapment culture could be explained by the fact that troglitazone was cleared more rapidly in gel entrapment than in monolayer culture. Similarly, the differential clearance of troglitazone in rat and human might also explain its species-specific toxicity. Therefore, gel entrapment of hepatocytes might serve as a platform for evaluation of drug toxicity at early stage of drug development by reducing costs, increasing the likelihood of clinical success and limiting human exposure to unsafe drugs., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2012

40. Toxicogenomics and metabolomics of pentamethylchromanol (PMCol)-induced hepatotoxicity.

Author

Parman T, Bunin DI, Ng HH, McDunn JE, Wulff JE, Wang A, Swezey R, Rasay L, Fairchild DG, Kapetanovic IM, and Green CE

Subjects

Animals, Biomarkers blood, Biomarkers urine, Chromans blood, Chromans urine, Gene Expression drug effects, Gene Expression Profiling, Kidney drug effects, Kidney metabolism, Kidney pathology, Liver metabolism, Liver pathology, Male, Metabolomics, Molecular Structure, Oligonucleotide Array Sequence Analysis, Organ Size drug effects, Rats, Rats, Sprague-Dawley, Real-Time Polymerase Chain Reaction, Toxicogenetics, Chemical and Drug Induced Liver Injury genetics, Chemical and Drug Induced Liver Injury metabolism, Chemical and Drug Induced Liver Injury pathology, Chromans toxicity, Liver drug effects

Abstract

Pentamethyl-6-chromanol (PMCol), a chromanol-type compound related to vitamin E, was proposed as an anticancer agent with activity against androgen-dependent cancers. In repeat dose-toxicity studies in rats and dogs, PMCol caused hepatotoxicity, nephrotoxicity, and hematological effects. The objectives of this study were to determine the mechanisms of the observed toxicity and identify sensitive early markers of target organ injury by integrating classical toxicology, toxicogenomics, and metabolomic approaches. PMCol was administered orally to male Sprague-Dawley rats at 200 and 2000 mg/kg daily for 7 or 28 days. Changes in clinical chemistry included elevated alanine aminotransferase, total bilirubin, cholesterol and triglycerides-indicative of liver toxicity that was confirmed by microscopic findings (periportal hepatocellular hydropic degeneration and cytomegaly) in treated rats. Metabolomic evaluations of liver revealed time- and dose-dependent changes, including depletion of total glutathione and glutathione conjugates, decreased methionine, and increased S-adenosylhomocysteine, cysteine, and cystine. PMCol treatment also decreased cofactor levels, namely, FAD and increased NAD(P)+. Microarray analysis of liver found that differentially expressed genes were enriched in the glutathione and cytochrome P450 pathways by PMCol treatment. Reverse transcription-polymerase chain reaction of six upregulated genes and one downregulated gene confirmed the microarray results. In conclusion, the use of metabolomics and toxicogenomics demonstrates that chronic exposure to high doses of PMCol induces liver damage and dysfunction, probably due to both direct inhibition of glutathione synthesis and modification of drug metabolism pathways. Depletion of glutathione due to PMCol exposure ultimately results in a maladaptive response, increasing the consumption of hepatic dietary antioxidants and resulting in elevated reactive oxygen species levels associated with hepatocellular damage and deficits in liver function.

Published

2011

41. Evaluation of PPARγ agonists on rodent endothelial cell proliferation.

Author

Kakiuchi-Kiyota S, Arnold LL, Yokohira M, Suzuki S, Pennington KL, and Cohen SM

Subjects

Adipose Tissue drug effects, Adipose Tissue pathology, Animals, Apoptosis drug effects, Body Weight drug effects, Cell Proliferation drug effects, DNA biosynthesis, Endothelial Cells physiology, Female, Hepatocytes drug effects, Mice, Organ Size drug effects, Pioglitazone, Rats, Rats, Wistar, Troglitazone, Chromans toxicity, Endothelial Cells drug effects, PPAR gamma agonists, Thiazolidinediones toxicity

Abstract

The PPARγ agonist troglitazone (TG) induced an increased incidence of hemangiosarcomas in mice but was not carcinogenic in rats. In contrast, pioglitazone (PIO) did not induce hemangiosarcomas or any other tumors in mice. We previously demonstrated that TG increased the proliferation of endothelial cells (ECs) in liver and adipose tissue in mice, and acted as a mitogenic stimulant and an inhibitor of apoptosis in vitro in mouse, but not human, ECs. In the present study, we investigated whether TG had any effect on the proliferation of ECs in rats. We also evaluated the in vivo and in vitro effects of PIO on ECs in mice. In rats, TG did not increase the Ki-67 labeling index (LI) of ECs in liver or adipose tissue at doses used in the two-year bioassay, and did not increase hepatocyte proliferation. PIO administered to mice did not increase the Ki-67 LI of hepatocytes or ECs in liver or white adipose tissue, but slightly increased the EC proliferation in brown adipose tissue. PIO was slightly mitogenic on cultured mouse ECs after 3 days of treatment but not after 6 days, and there was no inhibition of apoptosis, in contrast to what was seen with TG. The data support the conclusion that sustained EC proliferation in mice is necessary, for the induction of hemangiosarcomas by TG, and these short-term and long-term effects are not seen with TG in the rat or with PIO in mice, treatments that also are not related to the induction of hemangiosarcomas in two-year bioassays., (Copyright © 2011 Elsevier Ireland Ltd. All rights reserved.)

Published

2011

42. Toxic metabolite formation from Troglitazone (TGZ): new insights from a DFT study.

Author

Dixit VA and Bharatam PV

Subjects

Chromans chemistry, Chromans toxicity, Hydrogen Peroxide chemistry, Indolequinones toxicity, Oxidation-Reduction, Quantum Theory, Quinones chemistry, Thermodynamics, Thiazolidinediones toxicity, Troglitazone, Chromans metabolism, Thiazolidinediones metabolism

Abstract

The hepatotoxicity of Troglitazone (TGZ) has been ascribed to the formation of reactive metabolites, and the primary reactive metabolite of TGZ has been confirmed to be an o-quinone methide. Oxidation of the chromane moiety is also known to produce quinone containing metabolites. Quantum chemical studies have been performed to analyze the possible reaction pathways for the metabolism of the TGZ side chain, 6-hydroxy-2,2,5,7,8-pentamethylchromane (HPMC). From this analysis, a new pathway including oxidation at the C13 and C14 atoms of HPMC has been proposed for the formation of o-quinone methide (M2), while oxidation at the hydroxyl group leads to the formation of the quinone metabolite (M7). o-Quinone methide reactive metabolites have been shown to be more electrophilic at the reactive methylene center using quantum chemically estimated parameters., (© 2011 American Chemical Society)

Published

2011

43. A comparative integrated transcript analysis and functional characterization of differential mechanisms for induction of liver hypertrophy in the rat.

Author

Boitier E, Amberg A, Barbié V, Blichenberg A, Brandenburg A, Gmuender H, Gruhler A, McCarthy D, Meyer K, Riefke B, Raschke M, Schoonen W, Sieber M, Suter L, Thomas CE, and Sajot N

Subjects

Animals, Hypertrophy, Male, Proteomics methods, Rats, Rats, Wistar, Troglitazone, Chemical and Drug Induced Liver Injury genetics, Chemical and Drug Induced Liver Injury pathology, Chromans toxicity, Gene Expression Profiling methods, Gene Regulatory Networks physiology, Thiazolidinediones toxicity

Abstract

The main goal of the present work was to better understand the molecular mechanisms underlying liver hypertrophy (LH), a recurrent finding observed following acute or repeated drug administration to animals, using transcriptomic technologies together with the results from conventional toxicology methods. Administration of 5 terminated proprietary drug candidates from participating companies involved in the EU Innomed PredTox Project or the reference hepatotoxicant troglitazone to rats for up to a 14-day duration induced LH as the main liver phenotypic toxicity outcome. The integrated analysis of transcriptomic liver expression data across studies turned out to be the most informative approach for the generation of mechanistic models of LH. In response to a xenobiotic stimulus, a marked increase in the expression of xenobiotic metabolizing enzymes (XME) was observed in a subset of 4 studies. Accumulation of these newly-synthesized proteins within the smooth endoplasmic reticulum (SER) would suggest proliferation of this organelle, which most likely is the main molecular process underlying the LH observed in XME studies. In another subset of 2 studies (including troglitazone), a marked up-regulation of genes involved in peroxisomal fatty acid β-oxidation was noted, associated with induction of genes involved in peroxisome proliferation. Therefore, an increase in peroxisome abundance would be the main mechanism underlying LH noted in this second study subset. Together, the use of transcript profiling provides a means to generate putative mechanistic models underlying the pathogenesis of liver hypertrophy, to distinguish between subtle variations in subcellular organelle proliferation and creates opportunities for improved mechanism-based risk assessment., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

44. Differential disposition of chenodeoxycholic acid versus taurocholic acid in response to acute troglitazone exposure in rat hepatocytes.

Author

Marion TL, Perry CH, St Claire RL 3rd, Yue W, and Brouwer KL

Subjects

ATP-Binding Cassette Transporters antagonists & inhibitors, ATP-Binding Cassette Transporters genetics, Animals, Biological Transport, Carbon Radioisotopes, Cells, Cultured, Chemical and Drug Induced Liver Injury etiology, Chemical and Drug Induced Liver Injury metabolism, Chromatography, High Pressure Liquid, Hepatocytes metabolism, Male, Propionates pharmacology, Quinolines pharmacology, Rats, Rats, Wistar, Tandem Mass Spectrometry, Troglitazone, Chenodeoxycholic Acid metabolism, Chromans toxicity, Hepatocytes drug effects, PPAR gamma agonists, Taurocholic Acid metabolism, Thiazolidinediones toxicity

Abstract

Inhibition of bile acid (BA) transport may contribute to the hepatotoxicity of troglitazone (TRO), a peroxisome proliferator-activated receptor gamma agonist. Typically, studies use taurocholic acid (TCA) as a model substrate to investigate effects of xenobiotics on BA disposition. However, TRO may differentially affect the transport of individual BAs, potentially causing hepatocyte accumulation of more cytotoxic BAs. The effects of TRO on the disposition of [(14)C]-labeled chenodeoxycholic acid ([(14)C]CDCA), an unconjugated cytotoxic BA, were determined in suspended hepatocytes and sandwich-cultured hepatocytes (SCH) from rats. (E)-3-[[[3-[2-(7-chloro-2-quinolinyl)ethenyl]phenyl][[3-(dimethylamino)-3-oxopropyl]thio]methyl]thio]-propanoic acid (MK571), a multidrug resistance-associated protein (MRP) inhibitor, was included to evaluate involvement of MRPs in CDCA disposition. Accumulation in cells + bile of total [(14)C]CDCA species in SCH was sixfold greater than [(3)H]TCA and unaffected by 1 and 10μM TRO; 100μM TRO and 50μM MK571 ablated biliary excretion and significantly increased intracellular accumulation of total [(14)C]CDCA species. Results were similar in Mrp2-deficient TR(-) rat hepatocytes. Liquid chromatography-tandem mass spectrometry (LC-MS/MS) analysis revealed that taurine- and glycine-conjugated CDCA, in addition to unconjugated CDCA, accumulated in hepatocytes during the 10-min incubation. In suspended rat hepatocytes, initial [(14)C]CDCA uptake was primarily Na(+)-independent, whereas initial [(3)H]TCA uptake was primarily Na(+)-dependent; TRO and MK571 decreased [(14)C]CDCA uptake to a lesser extent than [(3)H]TCA. Unexpectedly, MK571 inhibited Na(+)-taurocholate cotransporting polypeptide and bile salt export pump. Differential effects on uptake and efflux of individual BAs may contribute to TRO hepatotoxicity. Although TCA is the prototypic BA used to investigate the effects of xenobiotics on BA transport, it may not be reflective of other BAs.

Published

2011

45. Chromanols from Sargassum siliquastrum and their antioxidant activity in HT 1080 cells.

Author

Lee JI and Seo Y

Subjects

Antioxidants isolation & purification, Antioxidants toxicity, Cell Line, Tumor, Chromans isolation & purification, Chromans toxicity, Glutathione metabolism, Humans, Lipid Peroxidation drug effects, Magnetic Resonance Spectroscopy, Reactive Oxygen Species metabolism, Antioxidants chemistry, Chromans chemistry, Sargassum chemistry

Abstract

Six meroterpenoids (compounds 1-6) of chromene class, including three known compounds (1-3), were isolated from Sargassum siliquastrum. The structure of these compounds was established by extensive 2D-NMR experiments such as (1)H gradient double quantum filtered correlation spectroscopy (gDQCOSY), total correlation spectroscopy (TOCSY), nuclear Overhauser effect spectroscopy (NOESY), gradient heteronuclear multiple quantum coherence (gHMQC), and gradient heteronuclear multiple bond correlation (gHMBC), and by comparison with published spectral data. The antioxidant activity of these compounds was evaluated by various antioxidant tests, such as scavenging effects on generation of intracellular reactive oxygen species (ROS), increments of intracellular glutathione (GSH) level, and inhibitory effects on lipid peroxidation in human fibrosarcoma HT 1080 cells. Compounds (1-6) significantly decreased generation of intracellular ROS and inhibited lipid peroxidation while they increased levels of intracellular GSH at a concentration of 5 µg/ml.

Published

2011

46. Multiple mechanisms underlying troglitazone-induced mitochondrial permeability transition.

Author

Okuda T, Norioka M, Shitara Y, and Horie T

Subjects

Animals, Apoptosis physiology, Dose-Response Relationship, Drug, Mitochondria, Liver metabolism, Mitochondrial Permeability Transition Pore, Mitochondrial Swelling drug effects, Mitochondrial Swelling physiology, Rats, Rats, Sprague-Dawley, Reactive Oxygen Species metabolism, Troglitazone, Apoptosis drug effects, Chromans toxicity, Mitochondria, Liver drug effects, Mitochondrial Membrane Transport Proteins metabolism, Thiazolidinediones toxicity

Abstract

Troglitazone, a thiazolidinedione class antidiabetic drug, was withdrawn from the market because of its severe idiosyncratic hepatotoxicity. It causes a mitochondrial permeability transition (MPT), which may in part contribute to its hepatotoxicity. In the present study, the mechanism of troglitazone mitochondrial toxicity was investigated in isolated rat liver mitochondria. Mitochondrial swelling induced by 10 μM troglitazone was attenuated by bromoenol lactone (BEL), an inhibitor of Ca²+-independent phospholipase A₂ (iPLA₂). In contrast, that induced by 50 μM troglitazone was exacerbated by BEL. This exacerbation was diminished by addition of 2mM glutathione, an antioxidant. Oxygen consumption by state 3 respiration in isolated mitochondria was also decreased by troglitazone, but it was not affected by BEL. Mitochondrial swelling induced by 10 μM troglitazone was completely attenuated in the absence of Ca²+ while that induced by 50 μM troglitazone was not affected. Addition of 1 μM cyclosporin A (CsA), an inhibitor of MPT pores, completely attenuated swelling induced by 10 μM troglitazone while it only partly diminished that induced by 50 μM troglitazone. Thus, the MPT induced by 10 and 50 μM troglitazone are regulated by different mechanism; the MPT induced by 10 μM troglitazone is regulated by the activation of iPLA₂ and caused by the opening of CsA-regulating MPT pores followed by accumulation of Ca²+ in mitochondria, while that induced by 50 μM troglitazone is partly regulated by reactive oxygen species and mainly caused by the opening of CsA-insensitive MPT pores., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2010

47. Troglitazone induces cytotoxicity in part by promoting the degradation of peroxisome proliferator-activated receptor γ co-activator-1α protein.

Author

Liao X, Wang Y, and Wong CW

Subjects

Adenosine Triphosphate metabolism, Apoptosis drug effects, Carrier Proteins drug effects, Carrier Proteins metabolism, Cell Survival drug effects, Gene Expression Regulation drug effects, Heat-Shock Proteins metabolism, Hep G2 Cells, Humans, Mitochondria, Liver metabolism, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Pioglitazone, RNA-Binding Proteins, Reactive Oxygen Species metabolism, Rosiglitazone, Transcription Factors metabolism, Troglitazone, Chromans toxicity, Heat-Shock Proteins drug effects, Hypoglycemic Agents toxicity, Mitochondria, Liver drug effects, Thiazolidinediones toxicity, Transcription Factors drug effects

Abstract

Background and Purpose: Troglitazone (Tro), rosiglitazone (Rosi) and pioglitazone (Pio) are anti-diabetic thiazolidinediones that function as ligands for peroxisome proliferator-activated receptor γ (PPARγ); however, Tro has been withdrawn from the market due to liver toxicity issues. Mitochondrial dysfunction induced by Tro has been suggested to be an important mechanism behind its cytotoxicity. Constitutively active nuclear hormone receptors, oestrogen-related receptor α and γ are thought to regulate mitochondrial mass and oxidative phosphorylation together with their co-activators PPARγ co-activator-1α and -1β (PGC-1α and PGC-1β). Hence, in this study, we investigated whether Tro affects the expression and activity levels of these regulators., Experimental Approach: Cellular viability was measured by an ATP-based assay. Mitochondrial mass and reactive oxygen species (ROS) were quantified by two different fluorogenic probes. Apoptosis was measured by an Annexin-V-based kit. Gene expression at the levels of mRNA and protein was measured by quantitative RT-PCR and Western analysis. Over-expression of PGC-1α was mediated by an adenovirus., Key Results: Tro, but not Rosi or Pio, selectively stimulated PGC-1α protein degradation. As a result, Tro reduced mitochondrial mass, and superoxide dismutases 1 and 2 expressions, but induced ROS to initiate apoptosis. Using a ubiquitin-proteasome inhibitor MG132, it was established that blocking PGC-1α degradation partially suppressed the reduction of mitochondrial mass. Importantly, over-expressing PGC-1α partially restored the Tro-suppressed mitochondrial mass and attenuated the cytotoxic effects of Tro., Conclusions and Implications: Collectively, these results suggest that PGC-1α degradation is an important mechanism behind the cytotoxic effects of Tro in the liver., (© 2010 The Authors. British Journal of Pharmacology © 2010 The British Pharmacological Society.)

Published

2010

48. Assessment of oral toxicity and safety of pentamethylchromanol (PMCol), a potential chemopreventative agent, in rats and dogs.

Author

Lindeblad M, Kapetanovic IM, Kabirov KK, Detrisac CJ, Dinger N, Mankovskaya I, Zakharov A, and Lyubimov AV

Subjects

Administration, Oral, Animals, Anticarcinogenic Agents administration & dosage, Chromans administration & dosage, Dogs, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Female, Male, Organ Size drug effects, Rats, Toxicity Tests, Anticarcinogenic Agents toxicity, Chromans toxicity

Abstract

2,2,5,7,8-Pentamethyl-6-chromanol (PMCol) was administered by gavage in rats for 28 days at dose levels of 0, 100, 500, and 2000mg/kg/day. PMCol administration induced decreases in body weight gains and food consumption, hepatotoxicity (increased TBILI, ALB, ALT, TP; increased relative liver weights; increased T4 and TSH), nephrotoxicity (increased BUN and BUN/CREAT, histopathology lesions), effect on lipid metabolism (increased CHOL), anemia, increase in WBC counts (total and differential), coagulation (FBGN upward arrow and PT downward arrow) and hyperkeratosis of the nonglandular stomach in the 2000mg/kg/day dose group (in one or both sexes). In the 500mg/kg/day dose group, toxicity was seen to a lesser extent. In the 100mg/kg/day dose group, only increased CHOL (females) was observed. To assess the toxicity of PMCol in male dogs it was administered orally by capsule administration for 28 days at dose levels of 0, 50, 200 and 800mg/kg/day (four male dogs/dose group). PMCol treatment at 800mg/kg/day resulted in pronounced toxicity to the male dogs. Target organs of toxicity were liver and thymus. Treatment at 200mg/kg/day resulted in toxicity consistent with slight adverse effect on the liver only. The results of the safety pharmacology study indicate that doses of 0, 50, 200 and 800mg/kg administered orally did not have an effect on the QT interval, blood pressures and body temperatures following dosing over a 24-h recording period. Under the conditions of this study, the no-observed-adverse effect level (NOAEL) for daily oral administration of PMCol by gavage for 28 days to male rats was 100mg/kg/day and 50mg/kg in male dogs. In female rats, the NOAEL was not established due to statistically significant and biologically meaningful increases in CHOL level seen in the 100mg/kg/day dose group. The results of these studies indicated that administration of PMCol at higher dose levels resulted in severe toxicity in dogs and moderate toxicity in rats, however, administration at lower levels is considered to be less likely to result in toxicity following 28 days of exposure. Sex-related differences were seen in rats. Male rats appeared to have greater sensitivity to nephrotoxicity, while female animals had a greater incidence of hepatoxicity and changes in hematological parameters evaluated, especially at a dose of 500mg/kg/day, which correlated to the higher plasma drug levels in female rats. It appeared that dogs were generally more sensitive than rats to oral administration of PMCol. Further examination of the potential toxic effects of PMCol in longer term studies is required prior to understanding the full risks of PMCol administration as a chemopreventative agent.

Published

2010

49. Direct toxicity effects of sulfo-conjugated troglitazone on human hepatocytes.

Author

Saha S, New LS, Ho HK, Chui WK, and Chan EC

Subjects

Cell Line, Cell Survival drug effects, Chromans toxicity, Glutathione metabolism, Hepatocytes enzymology, Hepatocytes metabolism, Humans, Hypoglycemic Agents chemistry, Oxidative Stress drug effects, Protein Carbonylation drug effects, Sulfotransferases antagonists & inhibitors, Sulfuric Acid Esters chemistry, Thiazolidinediones chemistry, Troglitazone, Hepatocytes drug effects, Hypoglycemic Agents toxicity, Sulfuric Acid Esters toxicity, Thiazolidinediones toxicity

Abstract

Troglitazone (TGZ), an orally active hypoglycemic agent, was found to be associated with severe drug-induced liver failure and was withdrawn from the market in 2000. Although the exact mechanism is not clear, it has been postulated that the formation of its major sulfo-conjugated metabolite (TGZS) plays an important role in its toxicity. TGZS inhibits bile salt export pump (BSEP) that causes accumulation of bile salts in liver. High concentration of bile salts causes cell death and mitochondrial dysfunction via detergent properties. One question arises whether TGZS has direct toxicity effect on human liver cells in addition to BSEP inhibition. In this study, both TGZ and chemically synthesized TGZS were incubated with normal human hepatocytes (THLE-2 cells) for measuring their cytotoxicity in vitro using the MTT assay. Glutathione (GSH) and protein carbonyl (PC) assays were further performed to measure the oxidative stress generated by these two compounds during incubation with THLE-2 cells. The results from this study indicated that TGZS (EC(50)=21.74+/-5.38 microM) was more toxic than TGZ (EC(50)=41.12+/-4.3 microM) in THLE-2 cells. The GSH and PC data further confirmed that TGZS produced greater oxidative stress in THLE-2 cells as compared to TGZ. In conclusion, our study demonstrated for the first time that TGZS has direct toxicity effect on human liver cells and may be partially responsible for the hepatotoxicity of TGZ., (Copyright 2010 Elsevier Ireland Ltd. All rights reserved.)

Published

2010

50. Contribution of high basolateral bile salt efflux to the lack of hepatotoxicity in rat in response to drugs inducing cholestasis in human.

Author

Jemnitz K, Veres Z, and Vereczkey L

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 11, ATP-Binding Cassette Transporters antagonists & inhibitors, Animals, Biological Transport drug effects, Chemical and Drug Induced Liver Injury prevention & control, Humans, Male, Organic Anion Transporters, Sodium-Dependent antagonists & inhibitors, Rats, Rats, Wistar, Species Specificity, Symporters antagonists & inhibitors, Troglitazone, Cholagogues and Choleretics metabolism, Cholestasis, Intrahepatic chemically induced, Chromans toxicity, Hypoglycemic Agents toxicity, Taurocholic Acid metabolism, Thiazolidinediones toxicity

Abstract

Intrahepatic bile acid accumulation due to inhibition of the bile salt export pump (BSEP) has been proposed as a mechanism for drug-induced cholestasis. Many cholestatic drugs do not initiate hepatotoxicity in rats, although they inhibit rat Bsep and cause elevated serum bile acid concentration. In this study, we examined changes in the taurocholate (TC) transport in response to cholestatic drug treatments in human and rat sandwich-cultured hepatocytes. Our experimental setup allows studying the basolateral and canalicular efflux simultaneously, thus comparing drug-induced changes in the vectorial efflux of TC. We found that TC elimination highly differs in human and rat hepatocytes. In human hepatocytes, an equal fraction of TC(uptake) was eliminated by basolateral (34.8%) and canalicular (34.4%) transporters and remained in the cells (30.5%), while in the case of rats, the basolateral transport was dominant (71.7%) and intracellular TC accumulation was negligible (6.9%). The inhibition of BSEP/Bsep resulted in significantly higher intracellular TC(conc) in humans than in rats. The 15-fold difference in intracellular TC(conc) of control in human versus rat hepatocytes was increased 25-fold by troglitazone treatment. MK571 and indomethacin decreased the basolateral efflux and significantly increased the intracellular TC(conc) in rats. In rat hepatocytes, the highest intracellular TC(conc) was observed with cyclosporine A and glibenclamide, which inhibited TC elimination in both directions. Nevertheless, the basolateral transport remained dominant. We conclude that in rats, the higher rate of basolateral bile salt efflux represents an additional protective mechanism in cholestasis, which contributes to species differences in response to hepatotoxic drugs.

Published

2010