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1. Pregnane X Receptor Activation Triggers Rapid ATP Release in Primed Macrophages That Mediates NLRP3 Inflammasome Activation

Author: Kyle L. Flannigan, Simon A. Hirota, Sridhar Mani, Daniel A. Muruve, Christina F. Sandall, Vivek Krishna Pulakazhi Venu, Grace Marie Hudson, Thomas K. H. Chang, Laurie Alston, and Justin A. MacDonald
Subjects: 0301 basic medicine, Inflammasomes, Interleukin-1beta, Nerve Tissue Proteins, Ligands, digestive system, Connexins, Mice, 03 medical and health sciences, Adenosine Triphosphate, 0302 clinical medicine, Cell Line, Tumor, NLR Family, Pyrin Domain-Containing 3 Protein, medicine, Animals, Humans, Receptor, Pharmacology, Pregnane X receptor, Innate immune system, Kinase, Chemistry, Macrophages, Caspase 1, Pregnane X Receptor, Inflammasome, P2RX7, Inflammation, Immunopharmacology, and Asthma, digestive system diseases, Cell biology, Enzyme Activation, Kinetics, src-Family Kinases, 030104 developmental biology, Nuclear receptor, Molecular Medicine, Receptors, Purinergic P2X7, Efflux, 030217 neurology & neurosurgery, medicine.drug
Abstract: The pregnane X receptor (PXR) is a ligand-activated nuclear receptor that acts as a xenobiotic sensor, responding to compounds of foreign origin, including pharmaceutical compounds, environmental contaminants, and natural products, to induce transcriptional events that regulate drug detoxification and efflux pathways. As such, the PXR is thought to play a key role in protecting the host from xenobiotic exposure. More recently, the PXR has been reported to regulate the expression of innate immune receptors in the intestine and modulate inflammasome activation in the vasculature. In the current study, we report that activation of the PXR in primed macrophages triggers caspase-1 activation and interleukin-1β release. Mechanistically, we show that this response is nucleotide-binding oligomerization domain, leucine-rich repeat, and pyrin domain-containing 3-dependent and is driven by the rapid efflux of ATP and P2X purinoceptor 7 activation following PXR stimulation, an event that involves pannexin-1 gating, and is sensitive to inhibition of Src-family kinases. Our findings identify a mechanism whereby the PXR drives innate immune signaling, providing a potential link between xenobiotic exposure and the induction of innate inflammatory responses.
Published: 2019

2. Nuclear Receptor Regulation of Hepatic Cytochrome P450 Enzymes

Author: David J. Waxman and Thomas K. H. Chang
Subjects: Nuclear receptor, Biochemistry, Chemistry, Hepatic cytochrome, P450 Enzymes
Published: 2020

3. Constitutive androstane receptor regulates the intestinal mucosal response to injury

Author: Fernando A. Vicentini, Thomas K. H. Chang, Grace Marie Hudson, Alexandra D. Zamponi, Simon A. Hirota, Laurie Alston, Christina L. Hirota, Kevin P. Rioux, Kyle L. Flannigan, Subrata Ghosh, Sridhar Mani, Sarah L. Erickson, and Christophe Altier
Subjects: 0301 basic medicine, Pharmacology, Pregnane X receptor, business.industry, Cell migration, medicine.disease, Ulcerative colitis, 3. Good health, 03 medical and health sciences, 030104 developmental biology, Intestinal mucosa, Constitutive androstane receptor, medicine, Cancer research, Colitis, business, Wound healing, Receptor
Abstract: Background and Purpose The pathogenesis of the inflammatory bowel diseases (IBD), comprising Crohn's disease (CD) and ulcerative colitis (UC), involves aberrant interactions between a genetically susceptible individual, their microbiota and environmental factors. Alterations in xenobiotic receptor expression and function are associated with increased risk for IBD. Here, we have assessed the role of the constitutive androstane receptor (CAR), a xenobiotic receptor closely related to the pregnane X receptor, in the regulation of intestinal mucosal homeostasis. Experimental Approach CAR expression was assessed in intestinal mucosal biopsies obtained from CD and UC patients, and in C57/Bl6 mice exposed to dextran sulphate sodium (DSS; 3.5% w/v in drinking water) to evoke intestinal inflammation and tissue damage. CAR-deficient mice were exposed to DSS and mucosal healing assessed. Modulation of wound healing by CAR was assessed in vitro. The therapeutic potential of CAR activation was evaluated, using 3,3′,5,5′-tetrachloro-1,4-bis(pyridyloxy)benzene (TCPOBOP), a selective rodent CAR agonist. Key Results CAR expression was reduced in CD and UC samples, compared with expression in healthy controls. This was reproduced in our DSS studies, where CAR expression was reduced in colitic mice. CAR-deficient mice exhibited reduced healing following DSS exposure. In vitro, CAR activation accelerated intestinal epithelial wound healing by enhancing cell migration. Lastly, treating mice with TCPOBOP, following induction of colitis, enhanced mucosal healing. Conclusion and Implications Our results support the notion that xenobiotic sensing is altered during intestinal inflammation, and suggest that CAR activation may prove effective in enhancing mucosal healing in patients with IBD.
Published: 2017

4. Negative Regulation of Human Pregnane X Receptor by MicroRNA-18a-5p: Evidence for Suppression of MicroRNA-18a-5p Expression by Rifampin and Rilpivirine

Author: Abdullah A. Turkistani, Zhaoming Xu, Catherine Hu, Thomas K. H. Chang, Wenjun Chang, and Devinder Sharma
Subjects: 0301 basic medicine, Receptors, Steroid, Gene Expression, Steroid biosynthesis, Biology, 03 medical and health sciences, Cell Line, Tumor, microRNA, Gene expression, Humans, Transcription factor, Luciferases, Renilla, Pharmacology, Pregnane X receptor, Reporter gene, Dose-Response Relationship, Drug, Rilpivirine, Pregnane X Receptor, Transfection, Molecular biology, Cell biology, MicroRNAs, 030104 developmental biology, Nuclear receptor, Reverse Transcriptase Inhibitors, Molecular Medicine, Rifampin
Abstract: Small noncoding microRNAs act as post-transcriptional regulators of gene expression involved in diverse biologic functions. Pregnane X receptor (PXR, NR1I2), a member of the superfamily of nuclear receptors, is a transcription factor governing the transport and biotransformation of various drugs and other chemicals. In the present study, we identified a specific microRNA (miR) involved in regulating the expression and functionality of human PXR (hPXR). According to bioinformatics analysis employing three commonly used algorithms (TargetScan, miRanda, and DIANA-microT-CDS), miR-18a-5p was predicted to be the top candidate microRNA regulator of hPXR. Consequently, this microRNA was selected for detailed experimental investigation. As shown in cell-based dual-luciferase reporter gene assays, functional interaction occurred between miR-18a-5p and the microRNA recognition element of miR-18a-5p in the 3'-untranslated region of hPXR mRNA. Transfection of LS180 human colorectal adenocarcinoma cells with an miR-18a-5p mimic decreased hPXR mRNA and protein expression, whereas transfection of LS180 cells with an miR-18a-5p inhibitor increased hPXR mRNA and protein expression. The decrease in hPXR expression by the miR-18a-5p mimic was associated with a reduction in the extent of hPXR target gene (CYP3A4) induction by rifampin and rilpivirine. Treatment of untransfected LS180 cells with either of these hPXR agonists decreased endogenous expression of miR-18a-5p, and this preceded the onset of CYP3A4 induction. In conclusion, miR-18a-5p is a negative regulator of hPXR expression and the hPXR agonists rifampin and rilpivirine are chemical suppressors of miR-18a-5p expression.
Published: 2017

5. The xenobiotic sensing pregnane X receptor regulates tissue damage and inflammation triggered by C difficile toxins

Author: Thomas K. H. Chang, Kyle L. Flannigan, Simon A. Hirota, K Nieves, Sridhar Mani, Sarah L. Erickson, and Laurie Alston
Subjects: 0301 basic medicine, Bacterial Toxins, Clostridium difficile toxin A, Clostridium difficile toxin B, Inflammation, Biochemistry, 03 medical and health sciences, Enterotoxins, Mice, 0302 clinical medicine, Immune system, Bacterial Proteins, neutrophils, Genetics, Medicine, Animals, Colitis, toxin, Molecular Biology, Enterocolitis, Pseudomembranous, Research Articles, Mice, Knockout, Nr1i2, Pregnane X receptor, Innate immune system, business.industry, Clostridioides difficile, Pregnane X Receptor, Clostridium difficile, medicine.disease, 3. Good health, Toll-Like Receptor 4, 030104 developmental biology, Immunology, eosinophils, medicine.symptom, business, 030217 neurology & neurosurgery, Biotechnology, Signal Transduction, Research Article
Abstract: Clostridioides difficile (formerly Clostridium difficile; C difficile), the leading cause of nosocomial antibiotic‐associated colitis and diarrhea in the industrialized world, triggers colonic disease through the release two toxins, toxin A (TcdA) and toxin B (TcdB), glucosyltransferases that modulate monomeric G‐protein function and alter cytoskeletal function. The initial degree of the host immune response to C difficile and its pathogenic toxins is a common indicator of disease severity and infection recurrence. Thus, targeting the intestinal inflammatory response during infection could significantly decrease disease morbidity and mortality. In the current study, we sought to interrogate the influence of the pregnane X receptor (PXR), a modulator of xenobiotic and detoxification responses, which can sense and respond to microbial metabolites and modulates inflammatory activity, during exposure to TcdA and TcdB. Following intrarectal exposure to TcdA/B, PXR‐deficient mice (Nr1i2−/−) exhibited reduced survival, an effect that was associated with increased levels of innate immune cell influx. This exacerbated response was associated with a twofold increase in the expression of Tlr4. Furthermore, while broad‐spectrum antibiotic treatment (to deplete the intestinal microbiota) did not alter the responses in Nr1i2−/− mice, blocking TLR4 signaling significantly reduced TcdA/B‐induced disease severity and immune responses in these mice. Lastly, to assess the therapeutic potential of targeting the PXR, we activated the PXR with pregnenolone 16α‐carbonitrile (PCN) in wild‐type mice, which greatly reduced the severity of TcdA/B‐induced damage and intestinal inflammation. Taken together, these data suggest that the PXR plays a role in the host's response to TcdA/B and may provide a novel target to dampen the inflammatory tissue damage in C difficile infections.
Published: 2019

6. Cell-based and in silico evidence against quercetin and structurally-related flavonols as activators of vitamin D receptor

Author: Thomas K. H. Chang, Guixiang Yang, Aik Jiang Lau, and Regina Politi
Subjects: 0301 basic medicine, Endocrinology, Diabetes and Metabolism, Receptor expression, Clinical Biochemistry, Disaccharides, Biochemistry, Calcitriol receptor, Mice, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Transactivation, 0302 clinical medicine, Endocrinology, Calcitriol, Animals, Humans, Transgenes, Kaempferols, Vitamin D3 24-Hydroxylase, Molecular Biology, Isorhamnetin, Flavonoids, Syringetin, Hep G2 Cells, Cell Biology, 3. Good health, Molecular Docking Simulation, Galangin, Tamarixetin, HEK293 Cells, 030104 developmental biology, Gene Expression Regulation, chemistry, 030220 oncology & carcinogenesis, Receptors, Calcitriol, Molecular Medicine, Osteopontin, Quercetin, Myricetin, Caco-2 Cells
Abstract: It has been reported that quercetin is an activator of rat vitamin D receptor (rVDR). However, the conclusion was based on experiments performed without all the appropriate control groups, raising the possibility of a false-positive finding. Furthermore, distinct differences exist in the chemical structures of quercetin and 1α,25-dihydroxyvitamin D3, which is a prototypic agonist of VDR. Therefore, we investigated systematically whether quercetin and other flavonols are agonists of rVDR, mouse VDR (mVDR), or human VDR (hVDR). Quercetin, 3-hydroxyflavone, galangin, datiscetin, kaempferol, morin, isorhamnetin, tamarixetin, myricetin, and syringetin did not activate rVDR, mVDR, or hVDR in HEK-293 and HepG2 cells transfected with the corresponding receptor expression plasmid and either the secreted phosphoprotein 1 (Spp1) or cytochrome P450 24A1 (CYP24A1) reporter plasmid, when compared to the respective empty vector control group transfected with one or the other reporter plasmid and treated with one of the flavonols. Control analysis indicated that lithocholic acid and 1α,25-dihydroxyvitamin D3, but not rifampicin, activated rVDR, mVDR, and hVDR. As shown in transfected HEK293 and HepG2 cells, the flavonols did not influence hVDR ligand binding domain transactivation, steroid receptor coactivator-1 recruitment, or hVDR target gene expression (transient receptor potential cation channel 6 and CYP24A1) in hVDR-expressing Caco-2 or LS180 cells. The cumulative data from the cell-based experiments were corroborated by results obtained from molecular docking analysis. In conclusion, quercetin, 3-hydroxyflavone, galangin, datiscetin, kaempferol, morin, isorhamnetin, tamarixetin, myricetin, and syringetin are not agonists of rVDR, mVDR, or hVDR, as judged by cell-based and in silico evidence.
Published: 2016

7. Pregnane X Receptor Activation Attenuates Inflammation-Associated Intestinal Epithelial Barrier Dysfunction by Inhibiting Cytokine-Induced Myosin Light-Chain Kinase Expression and c-Jun N-Terminal Kinase 1/2 Activation

Author: Sridhar Mani, Laurie Alston, Angela Zhao, Thomas K. H. Chang, Sarah L. Erickson, Aik Jiang Lau, Simon A. Hirota, Aditya Garg, and Subhajit Mukherjee
Subjects: Male, 0301 basic medicine, Receptors, Steroid, medicine.medical_specialty, Myosin light-chain kinase, Inflammation, Biology, digestive system, Gene Expression Regulation, Enzymologic, Interferon-gamma, Mice, 03 medical and health sciences, Internal medicine, medicine, Animals, Humans, Mitogen-Activated Protein Kinase 9, Mitogen-Activated Protein Kinase 8, Intestinal Mucosa, Receptor, Myosin-Light-Chain Kinase, Barrier function, Pharmacology, Pregnane X receptor, Tumor Necrosis Factor-alpha, Kinase, Dextran Sulfate, c-jun, NF-kappa B, Pregnane X Receptor, Hep G2 Cells, Colitis, digestive system diseases, Cell biology, Enzyme Activation, Toll-Like Receptor 4, 030104 developmental biology, Endocrinology, Cytokines, Molecular Medicine, Tumor necrosis factor alpha, Caco-2 Cells, medicine.symptom, Gastrointestinal, Hepatic, Pulmonary, and Renal, Signal Transduction
Abstract: The inflammatory bowel diseases (IBDs) are chronic inflammatory disorders with a complex etiology. IBD is thought to arise in genetically susceptible individuals in the context of aberrant interactions with the intestinal microbiota and other environmental risk factors. Recently, the pregnane X receptor (PXR) was identified as a sensor for microbial metabolites, whose activation can regulate the intestinal epithelial barrier. Mutations in NR1I2, the gene that encodes the PXR, have been linked to IBD, and in animal models, PXR deletion leads to barrier dysfunction. In the current study, we sought to assess the mechanism(s) through which the PXR regulates barrier function during inflammation. In Caco-2 intestinal epithelial cell monolayers, tumor necrosis factor-α/interferon-γ exposure disrupted the barrier and triggered zonula occludens-1 relocalization, increased expression of myosin light-chain kinase (MLCK), and activation of c-Jun N-terminal kinase 1/2 (JNK1/2). Activation of the PXR [rifaximin and [[3,5-Bis(1,1-dimethylethyl)-4-hydroxyphenyl]ethenylidene]bis-phosphonic acid tetraethyl ester (SR12813); 10 μM] protected the barrier, an effect that was associated with attenuated MLCK expression and JNK1/2 activation. In vivo, activation of the PXR [pregnenolone 16α-carbonitrile (PCN)] attenuated barrier disruption induced by toll-like receptor 4 activation in wild-type, but not Pxr-/-, mice. Furthermore, PCN treatment protected the barrier in the dextran-sulfate sodium model of experimental colitis, an effect that was associated with reduced expression of mucosal MLCK and phosphorylated JNK1/2. Together, our data suggest that the PXR regulates the intestinal epithelial barrier during inflammation by modulating cytokine-induced MLCK expression and JNK1/2 activation. Thus, targeting the PXR may prove beneficial for the treatment of inflammation-associated barrier disruption in the context of IBD.
Published: 2016

8. Differential activation of human constitutive androstane receptor and its SV23 and SV24 splice variants by rilpivirine and etravirine

Author: Aik Jiang Lau, Matthew A. Sherman, Thomas K. H. Chang, and Devinder Sharma
Subjects: Pharmacology, Nevirapine, Efavirenz, Chemistry, virus diseases, Etravirine, 3. Good health, Transactivation, chemistry.chemical_compound, Rilpivirine, Constitutive androstane receptor, medicine, Delavirdine, Receptor, medicine.drug
Abstract: Background and Purpose Rilpivirine and etravirine are second-generation non-nucleoside reverse transcriptase inhibitors (NNRTIs) indicated for the treatment of HIV/AIDS. The constitutive androstane receptor (CAR) regulates the expression of genes involved in various biological processes, including the transport and biotransformation of drugs. We investigated the effect of rilpivirine and etravirine on the activity of the wild-type human CAR (hCAR-WT) and its hCAR-SV23 and hCAR-SV24 splice variants, and compared it with first-generation NNRTIs (efavirenz, nevirapine, and delavirdine). Experimental Approach Receptor activation, ligand-binding domain (LBD) transactivation, and co-activator recruitment were investigated in transiently transfected, NNRTI-treated HepG2 cells. Nuclear translocation of green fluorescent protein-tagged hCAR-WT and CYP2B6 gene expression were assessed in NNRTI-treated human hepatocytes. Key Results Rilpivirine and etravirine activated hCAR-WT, but not hCAR-SV23 or hCAR-SV24, and without transactivating the LBD or recruiting steroid receptor coactivators SRC-1, SRC-2, or SRC-3. Among the first-generation NNRTIs investigated, only efavirenz activated hCAR-WT, hCAR-SV23, and hCAR-SV24, but none of them transactivated the LBD of these receptors or substantively recruited SRC-1, SRC-2, or SRC-3. Rilpivirine, etravirine, and efavirenz triggered nuclear translocation of hCAR-WT and increased hCAR target gene (CYP2B6) expression. Conclusion and Implications NNRTIs activate hCAR-WT, hCAR-SV23, and hCAR-SV24 in a drug-specific and isoform-selective manner. The activation occurs by a mechanism that does not appear to involve binding to the LBD or recruitment of SRC-1, SRC-2, or SRC-3.
Published: 2015

9. Comparative analysis of ginsenosides in human glucocorticoid receptor binding, transactivation, and transrepression

Author: Catherine Hu, Thomas K. H. Chang, RuiQi Wang, and Aik Jiang Lau
Subjects: 0301 basic medicine, Agonist, Transcriptional Activation, medicine.medical_specialty, Ginsenosides, medicine.drug_class, Pharmacology, Ligands, Glucocorticoid receptor binding, 03 medical and health sciences, Transactivation, chemistry.chemical_compound, 0302 clinical medicine, Glucocorticoid receptor, Receptors, Glucocorticoid, Protein Domains, Internal medicine, medicine, Enzyme-linked receptor, Humans, Receptor, Transrepression, Hep G2 Cells, 030104 developmental biology, Endocrinology, chemistry, 030220 oncology & carcinogenesis, Protopanaxadiol, Protein Binding
Abstract: Conflicting data exist on the effect of ginsenosides on transactivation of human glucocorticoid receptor α (herein referred to as glucocorticoid receptor), and relatively little is known regarding the effect of these chemicals on transrepression of this receptor. We investigated the effect of 20(S)-protopanaxadiol (PPD), PPD-type ginsenosides (Rb1, Rb2, Rc, Rd, Rh2, and Compound K), 20(S)-protopanaxatriol (PPT), and PPT-type ginsenosides (Re, Rf, Rg1, and Rh1) on glucocorticoid receptor binding, transactivation, and transrepression. Each ginsenoside was less efficacious than dexamethasone (positive control) in binding to the ligand-binding domain of glucocorticoid receptor. Among the ginsenosides investigated, Rh2 had the smallest IC50 value (15 ± 1µM), whereas it was 0.02 ± 0.01µM for dexamethasone. In contrast to dexamethasone, none of the ginsenosides influenced glucocorticoid receptor transactivation or transrepression in LS180 human colorectal adenocarcinoma cells, as assessed in a dual-luciferase reporter gene assay. Rh2 did not affect the endogenous mRNA level of tyrosine aminotransferase (marker for glucocorticoid receptor transactivation) or corticosteroid-binding globulin (marker for glucocorticoid receptor transrepression) in HepG2 human hepatocellular carcinoma cells. This chemical also did not alter the response by a glucocorticoid receptor agonist (dexamethasone or Compound A) in the dual-luciferase reporter gene assay or target gene expression assay. In conclusion, ginsenosides were less efficacious and less potent than dexamethasone in binding to the ligand-binding domain of glucocorticoid receptor. The number of glycosylated groups was associated with a decrease in receptor binding potency. PPD-type and PPT-type ginsenosides are not modulators of glucocorticoid receptor transactivation or transrepression in LS180 and HepG2 cells.
Published: 2017

10. The Microbial Metabolite Sensor Pregnane X Receptor (PXR) Restrains Fibroblasts from Promoting Gastrointestinal Inflammation and Fibrosis in Mice

Author: Simon A. Hirota, Laurie Alston, Kyle L. Flannigan, Sridhar Mani, and Thomas K. H. Chang
Subjects: Pregnane X receptor, Chemistry, Fibrosis, Genetics, medicine, Gastrointestinal inflammation, Pharmacology, Microbial metabolite, medicine.disease, Molecular Biology, Biochemistry, Biotechnology
Published: 2017

11. Fetal bovine serum and human constitutive androstane receptor: Evidence for activation of the SV23 splice variant by artemisinin, artemether, and arteether in a serum-free cell culture system

Author: Aik Jiang Lau and Thomas K. H. Chang
Subjects: Serum, medicine.medical_specialty, Time Factors, Cell Survival, Cell, Cell Culture Techniques, Ligands, Transfection, Toxicology, Basal (phylogenetics), Genes, Reporter, Internal medicine, Constitutive androstane receptor, medicine, Humans, Protein Isoforms, Receptor, Pharmacology, Reporter gene, Dose-Response Relationship, Drug, Chemistry, fungi, Reproducibility of Results, Hep G2 Cells, respiratory system, equipment and supplies, Artemisinins, Endocrinology, medicine.anatomical_structure, Biochemistry, Receptors, Androgen, Cell culture, Biological Assay, Artemether, sense organs, Fetal bovine serum
Abstract: The naturally occurring SV23 splice variant of human constitutive androstane receptor (hCAR-SV23) is activated by di-(2-ethylhexyl)phthalate (DEHP), which is detected as a contaminant in fetal bovine serum (FBS). In our initial experiment, we compared the effect of dialyzed FBS, charcoal-stripped, dextran-treated FBS (CS-FBS), and regular FBS on the basal activity and ligand-activation of hCAR-SV23 in a cell-based reporter gene assay. In transfected HepG2 cells cultured in medium supplemented with 10% FBS, basal hCAR-SV23 activity varied with the type of FBS (regular>dialyzed>CS). DEHP increased hCAR-SV23 activity when 10% CS-FBS, but not regular FBS or dialyzed FBS, was used. With increasing concentrations (1-10%) of regular FBS or CS-FBS, hCAR-SV23 basal activity increased, whereas in DEHP-treated cells, hCAR-SV23 activity remained similar (regular FBS) or slightly increased (CS-FBS). Subsequent experiments identified a serum-free culture condition to detect DEHP activation of hCAR-SV23. Under this condition, artemisinin, artemether, and arteether increased hCAR-SV23 activity, whereas they decreased it in cells cultured in medium supplemented with 10% regular FBS. By comparison, FBS increased the basal activity of the wild-type isoform of hCAR (hCAR-WT), whereas it did not affect the basal activity of the SV24 splice variant (hCAR-SV24) or ligand activation of hCAR-SV24 and hCAR-WT by 6-(4-chlorophenyl)imidazo[2,1-b][1,3]thiazole-5-carbaldehyde O-(3,4-dichlorobenzyl)oxime (CITCO). The use of serum-free culture condition was suitable for detecting CITCO activation of hCAR-WT and hCAR-SV24. In conclusion, FBS leads to erroneous classification of pharmacological ligands of hCAR-SV23 in cell-based assays, but investigations on functional ligands of hCAR isoforms can be conducted in serum-free culture condition.
Published: 2014

12. Indirect activation of the SV23 and SV24 splice variants of human constitutive androstane receptor: analysis with 3-hydroxyflavone and its analogues

Author: Thomas K. H. Chang and Aik Jiang Lau
Subjects: Pharmacology, Biology, Molecular biology, Galangin, Nuclear receptor coactivator 1, chemistry.chemical_compound, Transactivation, Tamarixetin, chemistry, Biochemistry, Constitutive androstane receptor, Nuclear receptor coactivator 3, Nuclear receptor coactivator 2, Isorhamnetin
Abstract: Background and Purpose Naturally occurring splice variants of human CAR (hCAR), including hCAR-SV23 (insertion of amino acids SPTV) and hCAR-SV24 (APYLT), have been shown to be expressed in liver. However, little is known regarding how hCAR-SV23 and hCAR-SV24 are activated. Therefore, we investigated the mode of activation of these hCAR splice variants. Experimental Approach Cell-based reporter gene assays, including ligand-binding domain transactivation assays and coactivator recruitment assays, were conducted on cultured HepG2 cells transfected with various constructs and treated with 3-hydroxyflavone or a hydroxylated (galangin, datiscetin, kaempferol, morin, quercetin or myricetin) or methylated (isorhamnetin, tamarixetin, or syringetin) analogue. Key Results Among the flavonols investigated, only 3-hydroxyflavone increased hCAR-SV23 and hCAR-SV24 activities. 3-Hydroxyflavone did not transactivate the ligand-binding domain of these isoforms or recruit steroid receptor coactivators (SRC-1, SRC-2, or SRC-3). By comparison, 3-hydroxyflavone, galangin, datiscetin, kaempferol, quercetin, isorhamnetin and tamarixetin activated hCAR-WT, whereas none of the flavonols activated hCAR-SV25 (both SPTV and APYLT insertions). The flavonols 3-Hydroxyflavone, galangin, quercetin and tamarixetin transactivated the ligand-binding domain of hCAR-WT, but only 3-hydroxyflavone recruited SRC-1, SRC-2 and SRC-3 to the receptor. Conclusion and Implications hCAR-SV23 and hCAR-SV24 can be activated by a mechanism that does not involve the ligand-binding domain of the receptor or recruitment of SRC-1, SRC-2, or SRC-3. 3-Hydroxyflavone and its structural analogues activated hCAR in an isoform-selective and chemical-specific manner. Overall, our study provides insight into a novel mode of ligand activation of hCAR-SV23 and hCAR-SV24.
Published: 2013

13. A rapid and sensitive assay to quantify valproyl 1-O-acyl glucuronide in supernatants of sandwich-cultured rat hepatocytes using ultra-high performance liquid chromatography–tandem mass spectrometry

Author: Thomas K. H. Chang, Xiao Wei Teng, András Szeitz, Jayakumar Surendradoss, and Frank S. Abbott
Subjects: Male, Electrospray ionization, Clinical Biochemistry, Glucuronidation, Mass spectrometry, Biochemistry, High-performance liquid chromatography, Analytical Chemistry, Rats, Sprague-Dawley, Glucuronides, Limit of Detection, Tandem Mass Spectrometry, Liquid chromatography–mass spectrometry, Animals, Selected ion monitoring, Chromatography, Chemistry, Valproic Acid, Selected reaction monitoring, Cell Biology, General Medicine, Rats, Hepatocytes, Anticonvulsants, lipids (amino acids, peptides, and proteins), Glucuronide, Chromatography, Liquid
Abstract: A rapid and sensitive ultra-high performance liquid chromatography-tandem mass spectrometry (UHPLC-MS/MS) method was developed and validated for the determination of valproyl-1-O-acyl glucuronide (VPA-G) levels in hepatocyte culture medium. Chromatographic separation was achieved using a Waters Acquity UPLC(®) BEH C18 column (1.7μm, 2.1mm×50mm) with gradient elution and a total run time of 4min. [(2)H6]-VPA-G was used as internal standard (IS). Quantification was performed in the multiple reaction monitoring (MRM) mode using the total ion current of the MRM transition pairs m/z 319.1→142.7 and m/z 319.1→175.2 for VPA-G, and m/z 325.1→149.3 and m/z 325.1→174.9 for the IS under negative electrospray ionization mode. The assay was linear over the VPA-G concentrations of 0.5-500ng/mL, with a r(2) value of 0.995±0.002 (mean±SD). The intra- and inter-day accuracy (% deviation) ranged from -10.2% to 11.1%, whereas the intra- and inter-day precision (% RSD) were ≤7.43%. The method was applied successfully to the quantification of VPA-G levels in culture supernatants of sandwich-cultured rat hepatocytes treated with valproic acid (VPA). No significant difference in the levels of VPA-G over a culture period of 6 days was observed in an experiment that investigated the effect of the age of hepatocyte culture on the extent of VPA glucuronidation. The method presented here for the direct quantification of VPA-G is an improvement of existing methods in the literature and offers a shorter run time and greater sensitivity that enables the use of small volumes of sample. To the best of our knowledge, this is the first validated UHPLC-MS/MS method applied to the quantification of VPA-G in cell culture supernatants.
Published: 2013

14. Agonism of human pregnane X receptor by rilpivirine and etravirine: Comparison with first generation non-nucleoside reverse transcriptase inhibitors

Author: Aik Jiang Lau, Thomas K. H. Chang, Devinder Sharma, and Matthew A. Sherman
Subjects: Receptors, Steroid, Nevirapine, Efavirenz, Etravirine, Pharmacology, Hydroxylation, Real-Time Polymerase Chain Reaction, Biochemistry, Nucleoside Reverse Transcriptase Inhibitor, chemistry.chemical_compound, Genes, Reporter, Cell Line, Tumor, Two-Hybrid System Techniques, Nitriles, Fluorescence Resonance Energy Transfer, medicine, Humans, Delavirdine, Pregnane X receptor, Dose-Response Relationship, Drug, Reverse Transcriptase Polymerase Chain Reaction, Rilpivirine, Pregnane X Receptor, Virology, Pyridazines, Discovery and development of non-nucleoside reverse-transcriptase inhibitors, Pyrimidines, chemistry, Steroid Hydroxylases, Reverse Transcriptase Inhibitors, medicine.drug
Abstract: Rilpivirine and etravirine are second generation non-nucleoside reverse transcriptase inhibitors approved recently by the United States Food and Drug Administration for the treatment of human immunodeficiency virus-1 infection. Pregnane X receptor (PXR) is a member of the superfamily of nuclear receptors that regulate the expression of various genes controlling diverse biological functions. The present study investigated the effects of rilpivirine and etravirine on the activity of human PXR (hPXR), including the mode of activation, and compared them to those of efavirenz, nevirapine, and delavirdine, which are first generation non-nucleoside reverse transcriptase inhibitors. In transiently transfected HepG2 cells, rilpivirine, etravirine, and efavirenz, but not nevirapine or delavirdine, activated human, mouse, and rat PXR. Results from mechanistic studies indicated that rilpivirine, etravirine, and efavirenz, but not nevirapine or delavirdine, bound to the ligand-binding domain of hPXR, as assessed by a transactivation assay and by a competitive ligand-binding assay using time-resolved fluorescence resonance energy transfer; triggered nuclear translocation of a green fluorescence protein-tagged hPXR, as visualized by confocal imaging; and recruited steroid receptor coactivator-1 (SRC-1), SRC-2, and SRC-3 to hPXR, as demonstrated by mammalian two-hybrid assays. Rilpivirine, etravirine, and efavirenz, but not nevirapine or delavirdine, increased hPXR target gene (CYP3A4) expression in primary cultures of human hepatocytes. In summary, select non-nucleoside reverse transcriptase inhibitors activated human and rodent PXR. Rilpivirine, etravirine, and efavirenz, but not nevirapine or delavirdine, were identified as agonists of hPXR, as assessed in mechanistic experiments, and inducers of CYP3A4, as determined in primary cultures of human hepatocytes.
Published: 2013

15. Evaluation of Ginkgo biloba extract as an activator of human glucocorticoid receptor

Author: Ganesh Rajaraman, Thomas K. H. Chang, Guixiang Yang, Aik Jiang Lau, and Christie C. Baucom
Subjects: Receptors, Steroid, Receptors, Cytoplasmic and Nuclear, Pharmacology, complex mixtures, 03 medical and health sciences, chemistry.chemical_compound, Receptors, Glucocorticoid, 0302 clinical medicine, Glucocorticoid receptor, Bilobalide, Genes, Reporter, Drug Discovery, Constitutive androstane receptor, medicine, Cytochrome P-450 CYP3A, Humans, RNA, Messenger, Receptor, Cells, Cultured, Constitutive Androstane Receptor, 030304 developmental biology, 0303 health sciences, Pregnane X receptor, biology, Plant Extracts, Ginkgo biloba, Chemistry, Pregnane X Receptor, Oxidoreductases, N-Demethylating, Hep G2 Cells, biology.organism_classification, 3. Good health, Cytochrome P-450 CYP2B6, Gene Expression Regulation, 030220 oncology & carcinogenesis, Hepatocytes, Ginkgolide, Aryl Hydrocarbon Hydroxylases, Glucocorticoid, medicine.drug
Abstract: Ethnopharmacological relevance Ginkgo biloba, which is one of the most frequently used herbal medicines, is commonly used in the management of several conditions, including memory impairment. Previously, it was reported to decrease the expression of peripheral benzodiazepine receptor and the biosynthesis of glucocorticoids, thereby regulating glucocorticoid levels. However, it is not known whether Ginkgo biloba extract regulates the function of the glucocorticoid receptor. Aim of the study We determined whether Ginkgo biloba extract and several of its chemical constituents affect the activity of human glucocorticoid receptor (hGR). Materials and methods A hGR-dependent reporter gene assay was conducted in HepG2 human hepatocellular carcinoma cells and hGR target gene expression assays were performed in primary cultures of human hepatocytes. Results Multiple lots and concentrations of the extract and several of its chemical constituents (ginkgolide A, ginkgolide B, ginkgolide C, ginkgolide J, and bilobalide) did not increase hGR activity, as assessed by a cell-based luciferase reporter gene assay. The extract did not influence the expression of hGR target genes, including tyrosine aminotransferase (hTAT), constitutive androstane receptor (hCAR), or pregnane X receptor (hPXR), in primary cultures of human hepatocytes. Moreover, hGR antagonism by mifepristone (also known as RU486) did not attenuate the extent of induction of hCAR- and hPXR-regulated target genes CYP2B6 and CYP3A4 by Ginkgo biloba extract. Conclusion Ginkgo biloba extract, ginkgolide A, ginkgolide B, ginkgolide C, ginkgolide J, and bilobalide are not activators of hGR. Furthermore, the extract does not influence the hGR-hCAR or the hGR-hPXR signaling pathway in primary cultures of human hepatocytes.
Published: 2013

16. An Isocratic High-Performance Liquid Chromatography Assay for CYP7A1-Catalyzed Cholesterol 7α-Hydroxylation

Author: David J, Waxman and Thomas K H, Chang
Abstract: A normal-phase, isocratic high-performance liquid chromatography assay is described for cholesterol 7α-hydroxylation catalyzed by CYP7A1, which corresponds to the first and rate-limiting step in the conversion of cholesterol into bile acids. This method is based on the conversion of the primary cytochrome P450 metabolite, 7α-hydroxycholesterol, into 7α-hydroxy-4-cholesten-3-one in a reaction catalyzed by exogenous cholesterol oxidase, followed by chromatographic separation with monitoring at 254 nm. This technique is applicable to enzymatic studies for determination of cholesterol 7α- hydroxylation activity catalyzed by cDNA-expressed CYP7A1 and animal or human liver microsomes.
Published: 2016

17. Thin-Layer Chromatography Analysis of Human CYP3A-Catalyzed Testosterone 6β-Hydroxylation

Author: David J, Waxman and Thomas K H, Chang
Abstract: Testosterone and other steroid hormones have been studied as prototypic examples of endogenous substrates for hepatic cytochrome P450 (P450) enzymes. CYP3A enzymes from various species, including human, metabolize testosterone by a 6β-hydroxylation reaction, which is unique to this P450 subfamily. A thin-layer chromatographic method is described for the determination of 6β-hydroxytestosterone formed enzymatically by incubation of [
Published: 2016

18. High-Performance Liquid Chromatography Analysis of CYP2C8-Catalyzed Paclitaxel 6α-Hydroxylation

Author: Charles L, Crespi, Thomas K H, Chang, and David J, Waxman
Abstract: Paclitaxel (Taxol) is a naturally occurring member of the taxane family of antitumor drugs, which act by stabilizing microtubules. Paclitaxel is inactivated in human liver by a cytochrome P450 (P450)-catalyzed 6α-hydroxylation reaction. A reverse-phase, high-performance liquid chromatographic assay is described for the analysis of paclitaxel 6α-hydroxylation catalyzed by human liver microsomes or cDNA-expressed P450 enzyme CYP2C8. Analytical separations are achieved using a C
Published: 2016

19. Assessment of the role of in situ generated (E)-2,4-diene-valproic acid in the toxicity of valproic acid and (E)-2-ene-valproic acid in sandwich-cultured rat hepatocytes

Author: Jayakumar Surendradoss, Thomas K. H. Chang, and Frank S. Abbott
Subjects: Male, Cell Culture Techniques, Pharmacology, Toxicology, medicine.disease_cause, Rats, Sprague-Dawley, chemistry.chemical_compound, Cytochrome P-450 Enzyme System, Dichlorofluorescein, Lactate dehydrogenase, medicine, Animals, Cytochrome P-450 Enzyme Inhibitors, Valproic Acid, Molecular Structure, Glutathione, Triazoles, Rats, medicine.anatomical_structure, chemistry, Biochemistry, Enzyme Induction, Phenobarbital, Hepatocyte, Toxicity, Hepatocytes, lipids (amino acids, peptides, and proteins), Oxidative stress, medicine.drug
Abstract: Valproic acid (VPA) undergoes cytochrome P450-mediated desaturation to form 4-ene-VPA, which subsequently yields (E)-2,4-diene-VPA by β-oxidation. Another biotransformation pathway involves β-oxidation of VPA to form (E)-2-ene-VPA, which also generates (E)-2,4-diene-VPA by cytochrome P450-mediated desaturation. Although the synthetic form of (E)-2,4-diene-VPA is more hepatotoxic than VPA as shown in various experimental models, there is no conclusive evidence to implicate the in situ generated (E)-2,4-diene-VPA in VPA hepatotoxicity. The present study investigated the effects of modulating the in situ formation of (E)-2,4-diene-VPA on markers of oxidative stress (formation of 2',7'-dichlorofluorescein; DCF), steatosis (accumulation of BODIPY 558/568 C₁₂), necrosis (release of lactate dehydrogenase; LDH), and on cellular total glutathione (GSH) levels in sandwich-cultured rat hepatocytes treated with VPA or (E)-2-ene-VPA. Treatment with either of these chemicals alone increased each of the toxicity endpoints. In VPA-treated hepatocytes, (E)-2,4-diene-VPA was detected only at trace levels, even after phenobarbital (PB) pretreatment and there was no effect on the toxicity of VPA. Furthermore, pretreatment with a cytochrome P450 enzyme inhibitor, 1-aminobenzotriazole (1-ABT), did not influence the extent of VPA toxicity in both PB-pretreated and vehicle-pretreated hepatocytes. However, in (E)-2-ene-VPA-treated hepatocytes, PB pretreatment greatly enhanced the levels of (E)-2,4-diene-VPA and this was accompanied by a further enhancement of the effects of (E)-2-ene-VPA on DCF formation, BODIPY accumulation, LDH release, and GSH depletion. Pretreatment with 1-ABT reduced the concentrations of (E)-2,4-diene-VPA and the extent of (E)-2-ene-VPA toxicity; however, this occurred in PB-pretreated hepatocytes, but not in control hepatocytes. In conclusion, in situ generated (E)-2,4-diene-VPA is not responsible for the hepatocyte toxicity of VPA, whereas it contributes to the toxicity of (E)-2-ene-VPA in PB-pretreated rat hepatocytes.
Published: 2012

20. Estradiol-mediated suppression of CYP1B1 expression in mouse MA-10 Leydig cells is independent of protein kinase A and estrogen receptor

Author: Stelvio M. Bandiera, Grace S. Leung, Thomas K. H. Chang, Subrata Deb, and Jenny K. Tai
Subjects: Male, medicine.medical_specialty, CYP1B1, Clinical Biochemistry, Estrogen receptor, Biology, Cell Line, Rats, Sprague-Dawley, Mice, Estrogen Receptor Modulators, Downregulation and upregulation, Internal medicine, medicine, Animals, RNA, Messenger, Protein kinase A, Fulvestrant, Molecular Biology, Messenger RNA, Sheep, Estradiol, luteinizing hormone/choriogonadotropin receptor, Antagonist, Leydig Cells, Cell Biology, General Medicine, Receptors, LH, Cyclic AMP-Dependent Protein Kinases, Rats, Mice, Inbred C57BL, body regions, Endocrinology, Gene Expression Regulation, Receptors, Estrogen, Cytochrome P-450 CYP1B1, Aryl Hydrocarbon Hydroxylases, Luteinizing hormone, hormones, hormone substitutes, and hormone antagonists
Abstract: Estrogens have multifaceted roles in mammalian testis. In the present study, we focused on estradiol as a potential regulator of testicular cytochrome P450 1B1 (CYP1B1) expression and investigated the possible mechanisms involved in the estradiol-mediated suppression. CYP1B1 protein levels were measured in the testes of rats that were treated with 17β-estradiol benzoate (1.5 mg/kg) at different stages of development. In addition, CYP1B1 mRNA levels were measured in mouse MA-10 Leydig tumor cells treated with (a) various concentrations of 17β-estradiol benzoate, (b) 17β-estradiol benzoate in the presence of exogenous luteinizing hormone (LH), or (c) 17β-estradiol benzoate in the presence of ICI 182,780, a competitive steroidal antagonist of estrogen receptors (ERs). Treatment of neonatal, pubertal, or adult rats with 17β-estradiol benzoate was associated with a reduction of approximately 90% in testicular CYP1B1 protein content compared to age-matched controls. Treatment of MA-10 cells with 17β-estradiol benzoate (10-500 nM) produced a concentration- and time-dependent decrease in CYP1B1 mRNA levels, but had no effect on LH receptor mRNA levels or on protein kinase A (PKA) activity. However, 17β-estradiol benzoate (10-500 nM), regardless of the concentration tested, failed to attenuate the LH-elicited increase in CYP1B1 mRNA or PKA activity in MA-10 cells that were co-treated with LH and estradiol. Similarly, ICI 182,780 (10-1000 µM) did not reverse the suppressive effect of estradiol on CYP1B1 mRNA expression in MA-10 cells co-treated with estradiol and ICI 182,780. The results indicate that downregulation of testicular CYP1B1 by estradiol was independent of PKA activity and was not mediated by ERs in MA-10 cells.
Published: 2011

21. Effects of Valproic Acid on Organic Acid Metabolism in Children: A Metabolic Profiling Study

Author: James F. Bale, Robin E. Pearce, Kristin E Price, Robert M. Ward, Uttam Garg, Janice E. Sullivan, JS Leeder, Mary Jayne Kennedy, Laurie D. Smith, Frank S. Abbott, Thomas K. H. Chang, and B.A. Heese
Subjects: Male, Adolescent, Urinary system, Carboxylic Acids, Biology, Pharmacology, medicine.disease_cause, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Metabolome, Humans, Pharmacology (medical), Lactic Acid, Child, Retrospective Studies, 030304 developmental biology, chemistry.chemical_classification, Principal Component Analysis, 0303 health sciences, Valproic Acid, Age Factors, Infant, Carbamazepine, 3. Good health, Lactic acid, Treatment Outcome, chemistry, Child, Preschool, Toxicity, Female, lipids (amino acids, peptides, and proteins), 030217 neurology & neurosurgery, Oxidative stress, Organic acid, medicine.drug
Abstract: Young children are at increased risk for valproic acid (VPA) hepatotoxicity. Urinary organic acid profiles, as a surrogate of mitochondrial function, were obtained in children 1.9 to 17.3 years of age (n = 52) who were undergoing treatment with VPA for seizure disorders. Age-matched patients receiving treatment with carbamazepine (CBZ; n = 50) and healthy children not undergoing treatment (n = 22) served as controls. Age-related changes in organic acid profiles were observed in all three groups. Although the untreated and CBZ control groups were indistinguishable from each other with respect to the principal-component analysis (PCA) score plots of the subjects, a distinct boundary was apparent between the VPA and each of the control groups. Interindividual variability was observed in the VPA-induced alterations in endogenous pathways corresponding to branched-chain amino acid metabolism and oxidative stress. The data suggest that more detailed metabolomic analysis may provide novel insights into biological mechanisms and predictive biomarkers for children at highest risk for serious toxicity. Clinical Pharmacology & Therapeutics (2011) 89 6, 867–874. doi:10.1038/clpt.2011.47
Published: 2011

22. CYP1B1 expression in rat testis and Leydig cells is not inducible by aryl hydrocarbon receptor agonists

Author: Subrata Deb, Masahiko Kawai, Thomas K. H. Chang, and Stelvio M. Bandiera
Subjects: Male, endocrine system, medicine.medical_specialty, Polychlorinated Dibenzodioxins, Health, Toxicology and Mutagenesis, CYP1B1, Immunoblotting, Toxicology, Biochemistry, Gene Expression Regulation, Enzymologic, Cell Line, Rats, Sprague-Dawley, Mice, chemistry.chemical_compound, Internal medicine, Benzo(a)pyrene, medicine, Animals, Pharmacology, Messenger RNA, Dose-Response Relationship, Drug, biology, Leydig Cells, General Medicine, Aryl hydrocarbon receptor, Rats, body regions, Endocrinology, Receptors, Aryl Hydrocarbon, Mrna level, chemistry, Cytochrome P-450 CYP1B1, biology.protein, Pyrene, Aryl Hydrocarbon Hydroxylases, Methylcholanthrene
Abstract: 1. Cytochrome P450 1B1 (CYP1B1) is highly expressed in testis, but there is conflicting information regarding the inducibility of testicular CYP1B1 by aryl hydrocarbon receptor (AhR) agonists. 2. To assess AhR-mediated regulation, testicular CYP1B1 expression was measured following treatment of adult rats with 3-methylcholanthrene and various dosages of benzo[a]pyrene and 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD). The effect of TCDD on CYP1B1 expression in R2C rat Leydig and MA-10 mouse Leydig cells in culture was also determined. 3. Immunoblot analysis showed that treatment with benzo[a]pyrene at dosages up to 200 mg/kg/day and 3-methylcholanthrene at 25 mg/kg/day did not induce testicular CYP1B1 expression. Treatment with TCDD at dosages of 1, 5 or 100 microg/kg had no effect, but testicular CYP1B1 protein levels were increased by approximately 50% at dosages of 10 and 50 microg/kg. 4. CYP1B1 mRNA levels in MA-10 and CYP1B1 protein levels in R2C cells were not induced by exposure to TCDD (10-1000 nM). 5. Overall, the results indicate that rodent testicular CYP1B1 is not inducible by AhR agonists.
Published: 2010

23. Inhibition of procarcinogen-bioactivating human CYP1A1, CYP1A2 and CYP1B1 enzymes by melatonin

Author: Thomas K. H. Chang, Jie Chen, Eugene Y. H. Yeung, and Guixiang Yang
Subjects: Mixed inhibition, Pharmacology, Polymerase Chain Reaction, Cell Line, Cytochrome P-450 CYP2A6, Hydroxylation, Melatonin, chemistry.chemical_compound, Endocrinology, Cytochrome P-450 CYP1A2, Oxazines, Cytochrome P-450 CYP1A1, medicine, Humans, Benzopyrenes, Enzyme Inhibitors, Cells, Cultured, Carcinogen, biology, Chemistry, CYP1A2, Cytochrome P450, Enzyme Activation, Biochemistry, Benzo(a)pyrene, Cytochrome P-450 CYP1B1, Microsomes, Liver, Microsome, biology.protein, Aryl Hydrocarbon Hydroxylases, Plasmids, medicine.drug
Abstract: Administration of melatonin to rodents decreases the incidence of tumorigenesis initiated by benzo[a]pyrene or 7,12-dimethylbenz[a]anthracene, which requires bioactivation by cytochrome P450 enzymes, such as CYP1A1, CYP1A2 and CYP1B1, to produce carcinogenic metabolites. The present study tested the hypothesis that melatonin is a modulator of human CYP1 catalytic activity and gene expression. As a comparison, we also investigated the effect of melatonin on the catalytic activity of CYP2A6, which is also a procarcinogen-bioactivating enzyme. Melatonin (3-300 microm) decreased 7-ethoxyresorufin O-dealkylation catalyzed by human hepatic microsomes and recombinant CYP1A1, CYP1A2 and CYP1B1, whereas it did not affect coumarin 7-hydroxylation catalyzed by hepatic microsomes or recombinant CYP2A6. Melatonin inhibited CYP1 enzymes by mixed inhibition, with apparent K(i) values (mean +/- S.E.M.) of 59 +/- 1 (CYP1A1), 12 +/- 1 (CYP1A2), 14 +/- 2 (CYP1B1) and 46 +/- 8 microm (hepatic microsomes). Additional experiments indicated that melatonin decreased benzo[a]pyrene hydroxylation catalyzed by hepatic microsomes and CYP1A2 but not by CYP1A1 or CYP1B1. Treatment of MCF-10A human mammary epithelial cells with melatonin (up to 300 microm) did not affect basal or benzo[a]pyrene-inducible CYP1A1 or CYP1B1 gene expression. Consistent with this finding, melatonin did not influence reporter activity in aryl hydrocarbon receptor-dependent pGudluc6.1-transfected MCF-10A cells treated with or without benzo[a]pyrene, as assessed in an in vitro cell-based luciferase reporter gene assay. Overall, melatonin is an in vitro inhibitor of human CYP1 catalytic activity, and it may be useful to develop potent analogues of melatonin as potential cancer chemopreventive agents that block CYP1-mediated chemical carcinogenesis.
Published: 2010

24. Effect of Ginkgo biloba extract on oxidative metabolism of valproic acid in hepatic microsomes from donors with the CYP2C91/1 genotypeThis article is one of a selection of papers published in this special issue (part 1 of 2) on the Safety and Efficacy of Natural Health Products

Author: Thomas K. H. Chang, Andrew M. NumaA.M. Numa, and Frank S. Abbott
Subjects: Pharmacology, biology, Physiology, Ginkgo biloba, General Medicine, biology.organism_classification, chemistry.chemical_compound, Aglycone, Bilobalide, chemistry, Biochemistry, Physiology (medical), Microsome, Ginkgolide, Quercetin, Kaempferol, Isorhamnetin
Abstract: We investigated the effect of Ginkgo biloba extracts and some of its individual constituents on the oxidative metabolism of valproic acid (VPA) in hepatic microsomes from donors with the CYP2C9*1/*1 genotype. G. biloba extract decreased 4-ene-VPA, 3-OH-VPA, 4-OH-VPA, and 5-OH-VPA formation with mean (± SE) IC50 values of 340 ± 40 μg/mL, 370 ± 100 μg/mL, 180 ± 30 μg/mL, and 210 ± 20 μg/mL, respectively. This was associated with inhibition of not only CYP2C9*1, but also CYP2A6 and CYP2B6. Bilobalide, ginkgolide A, ginkgolide B, ginkgolide C, ginkgolide J, quercetin-3-O-rutinoside, kaempferol-3-O-rutinoside, and isorhamnetin-3-O-rutinoside were not responsible for the inhibition of VPA metabolism by the extract. When analyzed as the sum of the aglycone and total glycosides present in the extract, quercetin decreased 4-ene-VPA, 4-OH-VPA, and 5-OH-VPA formation by 76%, 51%, and 70%, respectively, kaempferol decreased 4-ene-VPA, 4-OH-VPA, and 5-OH-VPA formation by 65%, 46%, and 49%, respectively, and isorhamnetin decreased 4-ene-VPA, 4-OH-VPA, and 5-OH-VPA formation by 29%, 26%, and 31%, respectively. The 3 aglycones did not affect 3-OH-VPA formation. In summary, G. biloba extract decreased hepatic microsomal formation of 4-ene-VPA, 4-OH-VPA, 5-OH-VPA, and 3-OH-VPA, but the effect was not due to the terpene trilactones or flavonol glycosides investigated in our study.
Published: 2007

25. In Vitro Inhibition of Rat CYP1A1 and CYP1A2 by Piceatannol, a Hydroxylated Metabolite of trans-Resveratrol

Author: Thomas K. H. Chang, Chia-ting Yu, and Jie Chen
Subjects: Male, animal structures, Cytochrome P-450 CYP1A2 Inhibitors, Metabolite, Clinical Biochemistry, Pharmaceutical Science, Mixed inhibition, Pharmacology, Rats, Sprague-Dawley, chemistry.chemical_compound, Stilbenes, Cytochrome P-450 CYP1A1, Animals, Pharmacology (medical), Enzyme Inhibitors, Piceatannol, biology, Trans-resveratrol, Biochemistry (medical), CYP1A2, Enzyme assay, In vitro, Rats, chemistry, Biochemistry, Resveratrol, embryonic structures, Microsomes, Liver, biology.protein, Microsome
Abstract: Piceatannol and its parent compound, trans-resveratrol, decreased the in vitro catalytic activity of rat CYP1A1 and CYP1A2 by mixed inhibition. trans-Resveratrol was not a mechanism-based inactivator of rat CYP1A in vitro and the administration of this compound (50 mg/kg) to rats did not affect hepatic microsomal CYP1A-mediated enzyme activity.
Published: 2007

26. 3-Hydroxyflavone and structural analogues differentially activate pregnane X receptor: Implication for inflammatory bowel disease

Author: Aik Jiang Lau and Thomas K. H. Chang
Subjects: Receptors, Steroid, Pharmacology, Ligands, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, 0302 clinical medicine, Genes, Reporter, Cell Line, Tumor, Humans, RNA, Messenger, Receptor, Isorhamnetin, 030304 developmental biology, Flavonoids, 0303 health sciences, Pregnane X receptor, Syringetin, Pregnane X Receptor, Hep G2 Cells, Inflammatory Bowel Diseases, digestive system diseases, Galangin, Tamarixetin, chemistry, Nuclear receptor, 030220 oncology & carcinogenesis, Myricetin
Abstract: Pregnane X receptor (PXR; NR1I2) is a member of the superfamily of nuclear receptors that regulates the expression of genes involved in various biological processes, including drug transport and biotransformation. In the present study, we investigated the effect of 3-hydroxyflavone and its structurally-related analogues on PXR activity. 3-Hydroxyflavone, galangin, kaempferol, querceetin, isorhamnetin, and tamarixetin, but not but not datiscetin, morin, myricetin, or syringetin, activated mouse PXR, as assessed in a cell-based reporter gene assay. By comparison, 3-hydroxyflavone activated rat PXR, whereas 3-hydroxyflavone, galangin, quercetin, isorhamnetin, and tamarixetin activated human PXR (hPXR). A time-resolved fluorescence resonance energy transfer competitive ligand-binding assay showed binding to the ligand-binding domain of hPXR by 3-hydroxyflavone, galangin, quercetin, isorhamnetin, and tamarixetin. 3-Hydroxyflavone and galangin, but not quercetin, isorhamnetin, or tamarixetin, recruited steroid receptor coactivator (SRC)-1, SRC-2, and SRC-3 to hPXR. In LS180 human colon adenocarcinoma cells, 3-hydroxyflavone, quercetin, and tamarixetin increased CYP3A4, CYP3A5, and ABCB1 mRNA expression, whereas galangin and isorhamnetin increased CYP3A4 and ABCB1 but not CYP3A5 mRNA expression. Datiscetin, kaempferol, morin, myricetin, and syringetin did not attenuate the extent of hPXR activation by rifampicin, suggesting they are not hPXR antagonists. Overall, flavonols activate PXR in an analogue-specific and species-dependent manner. Substitution at the C2' or C5' position of 3-hydroxyflavone with a hydroxyl or methoxy group rendered it incapable of activating hPXR. Understanding the structure-activity relationship of flavonols in hPXR activation may facilitate nutraceutical development efforts in the treatment of PXR-associated intestinal diseases, such as inflammatory bowel disease.
Published: 2015

27. Contribution of CYP2C9, CYP2A6, and CYP2B6 to Valproic Acid Metabolism in Hepatic Microsomes from Individuals with the CYP2C91/1 Genotype

Author: Tony K. L. Kiang, Thomas K. H. Chang, M. Reza Anari, Frank S. Abbott, Ping C. Ho, and Vincent Tong
Subjects: DNA, Complementary, CYP2B6, In Vitro Techniques, Pharmacology, Toxicology, Sulfaphenazole, Gene Expression Regulation, Enzymologic, Mixed Function Oxygenases, Cytochrome P-450 CYP2A6, medicine, Humans, CYP2A6, Cytochrome P-450 CYP2C9, chemistry.chemical_classification, biology, Valproic Acid, CYP1A2, Cytochrome P450, Oxidoreductases, N-Demethylating, CYP2E1, Cytochrome P-450 CYP2B6, Enzyme, Biochemistry, chemistry, Microsomes, Liver, biology.protein, Microsome, Anticonvulsants, lipids (amino acids, peptides, and proteins), Aryl Hydrocarbon Hydroxylases, medicine.drug
Abstract: The present study investigated the role of specific human cytochrome P450 (CYP) enzymes in the in vitro metabolism of valproic acid (VPA) by a complementary approach that used individual cDNA-expressed CYP enzymes, chemical inhibitors of specific CYP enzymes, CYP-specific inhibitory monoclonal antibodies (MAbs), individual human hepatic microsomes, and correlational analysis. cDNA-expressed CYP2C9*1, CYP2A6, and CYP2B6 were the most active catalysts of 4-ene-VPA, 4-OH-VPA, and 5-OH-VPA formation. The extent of 4-OH-VPA and 5-OH-VPA formation by CYP1A1, CYP1A2, CYP1B1, CYP2C8, CYP2C19, CYP2D6, CYP2E1, CYP4A11, CYP4F2, CYP4F3A, and CYP4F3B was only 1-8% of the levels by CYP2C9*1. CYP2A6 was the most active in catalyzing VPA 3-hydroxylation, whereas CYP1A1, CYP2B6, CYP4F2, and CYP4F3B were less active. Correlational analyses of VPA metabolism with CYP enzyme-selective activities suggested a potential role for hepatic microsomal CYP2A6 and CYP2C9. Chemical inhibition experiments with coumarin (CYP2A6 inhibitor), triethylenethiophosphoramide (CYP2B6 inhibitor), and sulfaphenazole (CYP2C9 inhibitor) and immunoinhibition experiments (including combinatorial analysis) with MAb-2A6, MAb-2B6, and MAb-2C9 indicated that the CYP2C9 inhibitors reduced the formation of 4-ene-VPA, 4-OH-VPA, and 5-OH-VPA by 75-80% in a panel of hepatic microsomes from donors with the CYP2C9*1/*1 genotype, whereas the CYP2A6 and CYP2B6 inhibitors had a small effect. Only the CYP2A6 inhibitors reduced VPA 3-hydroxylation (by approximately 50%). The extent of inhibition correlated with the catalytic capacity of these enzymes in each microsome sample. Overall, our novel findings indicate that in human hepatic microsomes, CYP2C9*1 is the predominant catalyst in the formation of 4-ene-VPA, 4-OH-VPA, and 5-OH-VPA, whereas CYP2A6 contributes partially to 3-OH-VPA formation.
Published: 2006

28. Effect of Ginkgo biloba extract on procarcinogen-bioactivating human CYP1 enzymes: Identification of isorhamnetin, kaempferol, and quercetin as potent inhibitors of CYP1B1

Author: Eugene Y. H. Yeung, Thomas K. H. Chang, and Jie Chen
Subjects: Flavonols, Cytochrome P-450 CYP1A2 Inhibitors, Flavonoid, In Vitro Techniques, Hydroxylation, Toxicology, Catalysis, chemistry.chemical_compound, Bilobalide, Cytochrome P-450 CYP1A2, Benzo(a)pyrene, Cytochrome P-450 CYP1A1, Humans, heterocyclic compounds, Kaempferols, Isorhamnetin, Pharmacology, chemistry.chemical_classification, Dose-Response Relationship, Drug, biology, Plant Extracts, Ginkgo biloba, Glycoside, biology.organism_classification, Recombinant Proteins, chemistry, Biochemistry, Dealkylation, Cytochrome P-450 CYP1B1, Carcinogens, Microsomes, Liver, Quercetin, Aryl Hydrocarbon Hydroxylases, Kaempferol
Abstract: In the present study, we investigated the effect of Ginkgo biloba extracts and some of its individual constituents on the catalytic activity of human cytochrome P450 enzymes CYP1B1, CYP1A1, and CYP1A2. G. biloba extract of known abundance of terpene trilactones and flavonol glycosides inhibited 7-ethoxyresorufin O-dealkylation catalyzed by human recombinant CYP1B1, CYP1A1, and CYP1A2, and human liver microsomes, with apparent Ki values of 2 +/- 0.3, 5 +/- 0.5, 16 +/- 1.4, and 39 +/- 1.2 microg/ml (mean +/- SE), respectively. In each case, the mode of inhibition was of the mixed type. Bilobalide, ginkgolides A, B, C, and J, quercetin 3-O-rutinoside, kaempferol 3-O-rutinoside, and isorhamentin 3-O-rutinoside were not responsible for the inhibition of CYP1 enzymes by G. biloba extract, as determined by experiments with these individual chemicals at the levels present in the extract. In contrast, the aglycones of quercetin, kaempferol, and isorhamentin inhibited CYP1B1, CYP1A1, and CYP1A2. Among the three flavonol aglycones, isorhamentin was the most potent in inhibiting CYP1B1 (apparent Ki = 3 +/- 0.1 nM), whereas quercetin was the least potent in inhibiting CYP1A2 (apparent Ki = 418 +/- 50 nM). The mode of inhibition was competitive, noncompetitive, or mixed, depending on the enzyme and the flavonol. G. biloba extract also reduced benzo[a]pyrene hydroxylation, and the effect was greater with CYP1B1 than with CYP1A1 as the catalyst. Overall, our novel findings indicate that G. biloba extract and the flavonol aglycones isorhamnetin, kaempferol, and quercetin preferentially inhibit the in vitro catalytic activity of human CYP1B1.
Published: 2006

29. Synthetic Drugs and Natural Products as Modulators of Constitutive Androstane Receptor (Car) and Pregnane X Receptor (PXR)

Author: David J. Waxman and Thomas K. H. Chang
Subjects: Receptors, Steroid, Receptors, Cytoplasmic and Nuclear, Pharmacology, digestive system, Meclizine, chemistry.chemical_compound, Constitutive androstane receptor, Animals, Humans, Inverse agonist, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, Receptor, Transcription factor, Biotransformation, Constitutive Androstane Receptor, Pregnane X receptor, biology, Pregnane X Receptor, Cytochrome P450, digestive system diseases, Liver, chemistry, Biochemistry, Nuclear receptor, biology.protein, Androstane, human activities, Transcription Factors
Abstract: Constitutive androstane receptor (CAR) and pregnane X receptor (PXR) are members of the nuclear receptor superfamily. These transcription factors are predominantly expressed in the liver, where they are activated by structurally diverse compounds, including many drugs and endogenous substances. CAR and PXR regulate the expression of a broad range of genes, which contribute to transcellular transport, bioactivation, and detoxification of numerous xenochemicals and endogenous substances. This article discusses the importance of these receptors for pharmacology and toxicology, emphasizing the role of individual drugs and natural products as agonists, indirect activators, inverse agonists, and antagonists of CAR and PXR.
Published: 2006

30. LACK OF EVIDENCE FOR INDUCTION OF CYP2B1, CYP3A23, AND CYP1A2 GENE EXPRESSION BY Panax ginseng AND Panax quinquefolius EXTRACTS IN ADULT RATS AND PRIMARY CULTURES OF RAT HEPATOCYTES

Author: Vincent Tong, Thomas K. H. Chang, Xiao Wei Teng, Jie Chen, and Chia-ting Yu
Subjects: Male, Panax, Pharmaceutical Science, Pharmacology, Gene Expression Regulation, Enzymologic, Rats, Sprague-Dawley, Ginseng, chemistry.chemical_compound, Cytochrome P-450 CYP1A2, Oral administration, Gene expression, medicine, Animals, Cytochrome P-450 CYP3A, Cells, Cultured, Dexamethasone, biology, Plant Extracts, CYP1A2, biology.organism_classification, Rats, chemistry, Ginsenoside, Enzyme Induction, Cytochrome P-450 CYP2B1, Hepatocytes, Araliaceae, Phenobarbital, Aryl Hydrocarbon Hydroxylases, medicine.drug
Abstract: Treatment of rats with a single oral dose (10-30 mg/kg) of a crude Panax ginseng extract of unknown ginsenoside content has been reported to modestly increase hepatic microsomal cytochrome P450-mediated aminopyrine N-demethylation activity. In the present study, we compared the effect of P. ginseng and Panax quinquefolius extracts on rat hepatic CYP2B1, CYP3A23, and CYP1A2 gene expression. Adult male Sprague-Dawley rats (250-275 g) received, by oral gavage or i.p., P. ginseng extract [4% (w/w) total ginsenosides; 30 or 100 mg/kg/day for 1 or 4 days], P. quinquefolius extract [10% (w/w) total ginsenosides; 100 or 400 mg/kg/day for 21 consecutive days), or an equivalent volume (2 ml/kg) of the vehicle (0.9% NaCl or 0.3% carboxymethylcellulose) and were terminated 1 day after the last dose. P. ginseng and P. quinquefolius extracts did not affect body weight gain, absolute or relative liver weight, hepatic CYP2B1, CYP3A23, or CYP1A2 mRNA expression, or microsomal CYP2B-mediated 7-benzyloxyresorufin O-dealkylation (BROD) or CYP1A-mediated 7-ethoxyresorufin O-dealkylation (EROD) activity. In contrast, results from positive control experiments indicated that phenobarbital increased CYP2B1 mRNA and BROD activity, dexamethasone increased CYP3A23 mRNA, and beta-naphthoflavone increased CYP1A2 mRNA and EROD activity levels. Treatment of primary cultures of rat hepatocytes with either of the ginseng extracts (0.1-1000 microg/ml for 2 days) also did not affect CYP2B1 or CYP3A23 mRNA expression. Overall, our data indicate that P. ginseng and P. quinquefolius extracts do not increase rat hepatic CYP2B1, CYP3A23, or CYP1A2 gene expression.
Published: 2004

31. Role of individual human cytochrome P450 enzymes in thein vitrometabolism of hydromorphone

Author: Thomas K. H. Chang, K.M. McErlane, V M Borges, and S A Benetton
Subjects: Furafylline, CYP3A, Health, Toxicology and Mutagenesis, Pharmacology, Toxicology, Sulfaphenazole, Biochemistry, chemistry.chemical_compound, Cytochrome P-450 Enzyme System, medicine, Cytochrome P-450 Enzyme Inhibitors, Humans, Hydromorphone, Troleandomycin, Enzyme Inhibitors, Cells, Cultured, CYP3A4, CYP1A2, General Medicine, Recombinant Proteins, Enzyme Activation, Kinetics, chemistry, Microsomes, Liver, Microsome, Ketoconazole, medicine.drug
Abstract: 1. The aim was to identify the individual human cytochrome P450 (CYP) enzymes responsible for the in vitro N-demethylation of hydromorphone and to determine the potential effect of the inhibition of this metabolic pathway on the formation of other hydromorphone metabolites. 2. Hydromorphone was metabolized to norhydromorphone (apparent Km = 206 - 822 microM, Vmax = 104 - 834 pmol min(-1) mg(-1) protein) and dihydroisomorphine (apparent Km = 62 - 557 microM, Vmax = 17 - 122 pmol min(-1) mg(-1) protein) by human liver microsomes. 5. In pooled human liver microsomes, troleandomycin, ketoconazole and sulfaphenazole reduced norhydromorphone formation by an average of 45, 50 and 25%, respectively, whereas furafylline, quinidine and omeprazole had no effect. In an individual liver microsome sample with a high CYP3A protein content, troleandomycin and ketoconazole inhibited norhydromorphone formation by 80%. 5. The reduction in norhydromorphone formation by troleandomycin and ketoconazole was accompanied by a stimulation in dihydroisomorphine production. Recombinant CYP3A4, CYP3A5, CYP2C9 and CYP2D6, but not CYP1A2, catalysed norhydromorphone formation, whereas none of these enzymes was active in dihydroisomorphine formation. 6. In summary, CYP3A and, to a lesser extent, CYP2C9 catalysed hydromorphone N-demethylation in human liver microsomes. The inhibition of norhydromorphone formation by troleandomycin and ketoconazole resulted in a stimulation of microsomal dihydroisomorphine formation.
Published: 2004

32. Evaluation of a real-time polymerase chain reaction method for the quantification of CYP1B1 gene expression in MCF-7 human breast carcinoma cells

Author: Thomas K. H. Chang, Jie Chen, and Catherine Y.S. Cheung
Subjects: Emodin, Gene Expression, Breast Neoplasms, Adenocarcinoma, Biology, Toxicology, Sensitivity and Specificity, Melting curve analysis, chemistry.chemical_compound, Cytochrome P-450 Enzyme System, beta-Naphthoflavone, Cell Line, Tumor, Complementary DNA, Stilbenes, Gene expression, Humans, RNA, Messenger, RNA, Neoplasm, Enzyme Inhibitors, Pharmacology, Dose-Response Relationship, Drug, Reverse Transcriptase Polymerase Chain Reaction, Reproducibility of Results, Amplicon, Molecular biology, Orders of magnitude (mass), Real-time polymerase chain reaction, chemistry, Resveratrol, Cytochrome P-450 CYP1B1, Agarose gel electrophoresis, Female, Aryl Hydrocarbon Hydroxylases
Abstract: Introduction: Cytochrome P450 1B1 (CYP1B1) catalyzes the bioactivation of numerous procarcinogens and it is expressed in tumor cells, including human breast cancer cells. To study CYP1B1 gene expression, it is important to have an accurate, precise, reproducible, specific, and quantitative method. Methods: MCF-7 human breast carcinoma cells were treated with β-naphthoflavone (BNF; 50 μM), emodin (0.1–3 μM), trans-resveratrol (2.5–20 μM), or 0.1% dimethylsulfoxide (DMSO; vehicle control). Total cellular RNA was isolated and reverse transcribed. cDNA samples were quantified by a fluorescence assay and a constant amount (1 ng) was amplified in a real-time DNA thermal cycler (LightCycler). Results: Melting curve analysis and agarose gel electrophoresis of the amplicons resulted in a single peak and a single band, respectively. The identity of the amplicon was confirmed to be CYP1B1 by sequencing analysis. The standard curve for the real-time PCR amplification of CYP1B1 cDNA was log-linear for at least four orders of magnitude. The limit of quantitation (LOQ) of the assay was 100 copies. At the LOQ, the assay had an accuracy of 8% and a precision of 10%. The intraday (n=4) variability (expressed as percent coefficient of variation) was 9% for a sample with low CYP1B1 mRNA expression (cells treated with 0.1% DMSO; i.e., Sample A) and 3% for a sample with elevated CYP1B1 mRNA expression (cells treated with BNF; i.e., Sample B). The interday (n=4) variability was 16% for Sample A and 15% for Sample B. Emodin increased CYP1B1 mRNA expression in cultured MCF-7 cells (maximal effect of ninefold induction achieved at 1 μM), whereas trans-resveratrol suppressed it (IC50=6.6±1.0 μM, mean±S.E.M., n=3). Discussion: An accurate, precise, reproducible, and specific method is described for the real-time PCR quantification of CYP1B1 gene expression in MCF-7 human breast carcinoma cells.
Published: 2004

33. Constitutive Androstane Receptor and Pregnane X Receptor Gene Expression in Human Liver: Interindividual Variability and Correlation with CYP2B6 mRNA Levels

Author: Stelvio M. Bandiera, Jie Chen, and Thomas K. H. Chang
Subjects: Receptors, Steroid, medicine.medical_specialty, CYP2B6, Receptors, Cytoplasmic and Nuclear, Pharmaceutical Science, Biology, Isozyme, chemistry.chemical_compound, Internal medicine, Gene expression, Constitutive androstane receptor, medicine, Humans, RNA, Messenger, Constitutive Androstane Receptor, Pharmacology, Pregnane X receptor, Pregnane, Pregnane X Receptor, Genetic Variation, Oxidoreductases, N-Demethylating, Cytochrome P-450 CYP2B6, Endocrinology, Gene Expression Regulation, Liver, Nuclear receptor, chemistry, Androstane, Aryl Hydrocarbon Hydroxylases, Transcription Factors
Abstract: The constitutive androstane receptor (CAR) and pregnane X receptor (PXR) mediate the expression of mammalian cytochrome P450 (P450) 2B genes, including CYP2B6 in humans. Large interindividual differences exist in hepatic CYP2B6 expression, but the molecular basis for this variability is not well understood. In the present study, we developed real-time polymerase chain reaction methods to measure CYP2B6, CAR, and PXR mRNA expression and compared the levels in a panel of 12 individual human liver samples. The transcripts of CAR and CYP2B6 were present in all the samples analyzed, whereas those of PXR were detectable in all but one sample. A striking finding was the 240-fold interindividual variability in hepatic CAR mRNA levels, which was similar to the variability (278-fold) in CYP2B6 mRNA levels but greater than the 27-fold variability in PXR mRNA expression. Additional analysis revealed positive and statistically significant correlations between the mRNA levels of CAR and CYP2B6 ( r 2 = 0.63, p = 0.002), PXR and CYP2B6 ( r 2 = 0.75. p < 0.001), and CAR and PXR ( r 2 = 0.86, p < 0.001). In summary, substantial interindividual differences exist in hepatic CAR and, to a lesser extent, PXR gene expression. The variability in the abundance of these transcription factors may contribute to the large interindividual differences in CYP2B6 gene expression in human liver.
Published: 2003

34. [Untitled]

Author: Catherine Y.S. Cheung, Thomas K. H. Chang, Masahiko Kawai, and Jie Chen
Subjects: Pregnane X receptor, CYP3A4, CYP2B6, organic chemicals, CYP1B1, Clinical Biochemistry, Retinoic acid, Cell Biology, General Medicine, Biology, Molecular biology, chemistry.chemical_compound, CYP26A1, chemistry, Downregulation and upregulation, Constitutive androstane receptor, Molecular Biology
Abstract: All-trans-retinoic acid (ATRA) is used in the treatment of promyelocytic acute leukemia. The biotransformation of this drug is catalyzed by various cytochrome P450 (CYP) enzymes, but relatively little is known about the effect of ATRA on CYP enzyme expression in leukemic cells. In the present study, we conducted transcript profiling of CYP and related genes in cultured HL-60 human promyelocytic leukemic cells and determined the effect of ATRA on the expression of these genes. Reverse transcription-polymerase chain reaction (RT-PCR) analysis with a block-cycler indicated the presence of CYP1B1 but not CYP1A1, CYP2B6, CYP2C8, CYP2C9, CYP3A4, CYP3A5, or CYP26A1 transcript in cultured HL-60 cells. ATRA treatment (0.1–40 μM for 3 days) increased CYP1B1 mRNA levels by up to 3 fold, as determined by a quantitative real-time PCR method. The same ATRA treatment also resulted in the detection of CYP26A1 but not CYP1A1, CYP2B6, CYP2C8, CY2C9, CYP3A4, or CYP3A5 mRNA. Additional experiments showed that phenobarbital increased CYP2B6 mRNA expression and that pregnane X receptor (PXR) but not constitutive androstane receptor (CAR) was detected in HL-60 cells. Overall, our novel findings indicate the upregulation of CYP1B1 by ATRA in HL-60 human promyelocytic leukemic cells shown for the first time to express PXR but not CAR mRNA.
Published: 2003

35. Abstract

Author: Douglas D. Snider, Brendan T. Finucane, Donna Clarke, J. Loiselle, G. Doak, B. Anderson, Dan Wood, Sandy Shysh, Michel-Antoine Perrault, Philippe Chouinard, François Fugère, François Girard, Monique Ruel, Wendy C. E. Hall, Jiri Hrazdil, Donald T. Jolly, John C. Galbraith, Maria C. Greacen, Alexander S. Clanachan, Duminda N. Wijeysundera, W. Scott Beattie, Michelle Chochinov, Stephen Halpern, Dolores M. McKeen, Robert T. Nunn, Brendan S. Barrett, G. Allen Finley, Susan Buffett-Jerrott, Sherry Stewart, Donna Millington, Keyvan Karkouti, Yoga R. Rampersaud, Stuart A. McCluskey, Lucia Evans, Mohammed M. Ghannam, Nizar N. Mahomed, Sudha Singh, Patricia Morley-Forster, Mohammed Shamsah, Ian R. Thomson, Aaron D. Brown, Jeffrey I. Freedman, Robert J. Hudson, Murray Hong, Sean Hall, Brian Milne, Louie Wang, Chris Loomis, Ian Gilron, Debbie Tod, Allan Bell, Elizabeth Orr, Gary Dobson, Mustafa Karamanoglu, John V. Tyberg, Frances Chung, Charles Imarengiaye, Angela Rocchi, Lindy Forte, Elizabeth G. Van Den Kerkhof, David H. Goldstein, Mike Rimmer, Hoi Kwan Lee, Isabelle Charest, René Martin, François Plante, Shaheen Shaikh, Damian Yung, Mark Bernstein, Ngozi Imasogie, David Wong, Ken Luk, Suntheralingam Yogendran, Atul Prabhu, Ayman Hendy, Glenn McGuire, Jean Wong, M. Denise Daley, Peter H. Norman, Una Srejic, Thomas Dougherty, Sarah Hogervorst, Thomas M. Hemmerling, Joachim Schmidt, Pierre Beaulieu, Klaus E. Jacobi, Pamela H. Lennox, Kelly V. Mayson, Toshimi Arai, Kaori Saito, Masao Yamashita, Alain Gauthier, Daniel Boudreault, Dominique C. Girard, Louie T. S. Wang, Nancy Sikich, Guy Petroz, Jerrold Lerman, Gregory M. T. Hare, Andrew J. Baker, Kathryn M. Hum, Steve Y. Kim, Aiala Barr, C. David Mazer, Terrance A. Yemen, Thomas Howlett, Andrew Baker, Nicholas Phan, N. Persaud, Min Zhao, Elaine Liu, Michael Fehlings, Davinia E. Withington, T. AlAyed, G. Michael Davis, David M. Ansley, B. S. Dhaliwal, Zhengyuan Xia, Anthony M. -H. Ho, Anna Lee, Elizabeth Ling, Alan Daly, Kevin Teoh, Theodore E. Warkentin, David V. Godin, Thomas K. H. Chang, Joanne D. Fortier, Fadi Basile, Ignacio Prieto, David Mazer, Peter Duke, Barry Finegan, Davy Cheng, Richard Hall, B. Lim, J. Shannon, C. M. Ho, S. K. Tsai, Margaret Srebrnjak, Vivien Walsh, Geena Joseph, Teresa Valois Gomez, Carmen Rivero Fuenmayor, Paul S. Bach, Allaudin Kamani, Joanne Douglas, Mark Esler, Vit Gunka, Pamela Angle, Sam Tang, Dorothy Thompson, Jean Kronberg, Anwar Morgan, Craig H. Leicht, Ivan A. Velickovic, David T. Raphael, Maxim Benbassat, Dimiter Arnaudov, Alex Bohorquez, Bita Nasseri, D. John Doyle, Jacelyn Kolman, Ian Keith, Pamela J. Morgan, Doreen Cleave-Hogg, Susan Eveleigh, Jordan Tarshis, Sharon Davies, John Doyle, Heather Lee Loughlin, J. Patrick O’Connor, John F. Dolman, Fred S. Mikelberg, Gordana Dulovic, Brian G. Feagan, Cindy J. Wong, Alexandra Kirkley, D. W. C. Johnston, Frank C. Smith, Paul Whitsitt, William Li Pi Shanl, Steven B. Backman, Jeffrey Barkun, Peter Metrakos, John Tchervenkov, Mary Jane Salpeter, Leah Jamnicky, Michael Jewett, Ramiro Arellano, Brian Muirhead, Saifundin Rashiq, Meera Shah, Vikki Wilkinson, Samantha J. Woolsey, Barry A. Finegan, Carol Fiorilli, Joel L. Parlow, Nicole D. Avery, George N. Djaiani, Jayanta Muhkerji, Jacek M. Karski, Jo A. Carroll, Stuart McCluskey, Linda Harris, Jan Paton, Emmanuel Kanetos, William G. Williams, Cristina Hurtado, Manoj Gandhi, Sandy Clanachan, Woo Jong Shin, Bruce, D. Winegar, Jae Hang Shim, Woo Jae Jeon, Kyung Hun Kim, Bing Wang, David P. Archer, Naaznin Samanani, Sheldon H. Roth, Claudia Coimbra, Manon Choinière, Denis Babin, Francois Donati, Cynthia L. Henderson, John H. P. Friesen, Michael Jacka, Alan Cheng, Finlay McAlister, Jessie A. Leak, Tao Bui, Dy Nguyen, Alicia Kowalski, Keruyi Popat, Henry Kuerer, Paul Serowka, Kim Turner, Ted Ashbury, Tianlong Wang, Driss El-Kebir, Bernard Hubert, Ruud A. W. Veldhuizen, Dominique Gauvin, Gilbert Blaise, Fan Yang, and Patricia Amicone
Subjects: Anesthesiology and Pain Medicine, General Medicine
Published: 2002

36. In Vitro Effect of Standardized Ginseng Extracts and Individual Ginsenosides on the Catalytic Activity of Human CYP1A1, CYP1A2, and CYP1B1

Author: Jie Chen, Thomas K. H. Chang, and Salete A. Benetton
Subjects: Ginsenosides, Cytochrome P-450 CYP1A2 Inhibitors, Panax, Pharmaceutical Science, Pharmacology, Catalysis, chemistry.chemical_compound, Ginseng, Non-competitive inhibition, Cytochrome P-450 Enzyme System, Cytochrome P-450 CYP1A2, Oxazines, Cytochrome P-450 CYP1A1, Cytochrome P-450 Enzyme Inhibitors, Humans, American ginseng, Dose-Response Relationship, Drug, biology, Plant Extracts, Chemistry, CYP1A2, Saponins, biology.organism_classification, Asian Ginseng, Kinetics, Ginsenoside, Cytochrome P-450 CYP1B1, Microsomes, Liver, Microsome, Araliaceae, Aryl Hydrocarbon Hydroxylases
Abstract: Ginseng extract has been reported to decrease the incidence of 7,12-dimethylbenz[a]anthracene (DMBA)-initiated tumorigenesis in mice. A potential mechanism for this effect by ginseng is inhibition of DMBA-bioactivating cytochrome P450 (P450) enzymes. In the present in vitro study, we examined the effect of a standardized Panax ginseng (or Asian ginseng) extract (G115), a standardized Panax quinquefolius (or North American ginseng) extract (NAGE), and individual ginsenosides (Rb1, Rb2, Rc, Rd, Re, Rf, and Rg1) on CYP1 catalytic activities, as assessed by 7-ethoxyresorufin O-dealkylation. G115 and NAGE decreased human recombinant CYP1A1, CYP1A2, and CYP1B1 activities in a concentration-dependent manner. Except for the competitive inhibition of CYP1A1 by G115, the mode of inhibition was the mixed-type in the other cases. A striking finding was that NAGE was 45-fold more potent than G115 in inhibiting CYP1A2. Compared with G115, NAGE also preferentially inhibited 7-ethoxyresorufin O-dealkylation activity in human liver microsomes. Rb1, Rb2, Rc, Rd, Re, Rf, and Rg1, either individually or as a mixture and at the levels reflecting those found in an inhibitory concentration (100 microg/ml) of NAGE or G115, did not influence CYP1 activities. However, at a higher ginsenoside concentration (50 microg/ml), Rb1, Rb2, Rc, Rd, and Rf inhibited these activities. Overall, our in vitro findings indicate that standardized NAGE and G115 extracts, which were not treated with calf serum or subjected to acid hydrolysis, inhibited CYP1 catalytic activity in an enzyme-selective and extract-specific manner, but the effects were not due to Rb1, Rb2, Rc, Rd, Re, Rf, or Rg1.
Published: 2002

37. MicroRNA-18a is a Regulator of Human Pregnane X Receptor

Author: Abdullah A. Turkistani, Wenjun Chang, Thomas K. H. Chang, Devinder Sharma, and Zhaoming Xu
Subjects: Pharmacology, Pregnane X receptor, Liver X receptor beta, Chemistry, microRNA, Regulator, Toxicology, Cell biology
Published: 2017

38. Evaluation of in situ generated valproyl 1-O-β-acyl glucuronide in valproic acid toxicity in sandwich-cultured rat hepatocytes

Author: Jayakumar Surendradoss, Thomas K. H. Chang, and Frank S. Abbott
Subjects: Male, Metabolite, Glucuronidation, Pharmaceutical Science, medicine.disease_cause, Rats, Sprague-Dawley, chemistry.chemical_compound, Glucuronides, beta-Naphthoflavone, Lactate dehydrogenase, medicine, Animals, Cells, Cultured, Pharmacology, Camphanes, L-Lactate Dehydrogenase, Valproic Acid, Glutathione, Rats, medicine.anatomical_structure, chemistry, Biochemistry, Hepatocyte, Toxicity, Hepatocytes, lipids (amino acids, peptides, and proteins), Glucuronide, Oxidative stress
Abstract: Acyl glucuronides are reactive electrophilic metabolites implicated in the toxicity of carboxylic acid drugs. Valproyl 1-O-β-acyl glucuronide (VPA-G), which is a major metabolite of valproic acid (VPA), has been linked to the development of oxidative stress in VPA-treated rats. However, relatively little is known about the toxicity of in situ generated VPA-G and its contribution to VPA hepatotoxicity. Therefore, we investigated the effects of modulating the in situ formation of VPA-G on lactate dehydrogenase (LDH) release (a marker of necrosis), BODIPY 558/568 C12 accumulation (a marker of steatosis), and cellular glutathione (GSH) content in VPA-treated sandwich-cultured rat hepatocytes. VPA increased LDH release and BODIPY 558/568 C12 accumulation, whereas it had little or no effect on total GSH content. Among the various uridine 5'-diphospho-glucuronosyltransferase inducers evaluated, β-naphthoflavone produced the greatest increase in VPA-G formation. This was accompanied by an attenuation of the increase in BODIPY 558/568 C12 accumulation, but did not affect the change in LDH release or total GSH content in VPA-treated hepatocytes. Inhibition of in situ formation of VPA-G by borneol was not accompanied by substantive changes in the effects of VPA on any of the toxicity markers. In a comparative study, in situ generated diclofenac glucuronide was not toxic to rat hepatocytes, as assessed using the same chemical modulators, thereby demonstrating the utility of the sandwich-cultured rat hepatocyte model. Overall, in situ generated VPA-G was not toxic to sandwich-cultured rat hepatocytes, suggesting that VPA glucuronidation per se is not expected to be a contributing mechanism for VPA hepatotoxicity.
Published: 2014

39. Differential activation of human constitutive androstane receptor and its SV23 and SV24 splice variants by rilpivirine and etravirine

Author: Devinder, Sharma, Aik Jiang, Lau, Matthew A, Sherman, and Thomas K H, Chang
Subjects: Adult, Male, Adolescent, Dose-Response Relationship, Drug, Molecular Structure, Rilpivirine, Receptors, Cytoplasmic and Nuclear, Hep G2 Cells, Research Papers, Pyridazines, Alternative Splicing, Cytochrome P-450 CYP2B6, Structure-Activity Relationship, Young Adult, Pyrimidines, Nitriles, Hepatocytes, Tumor Cells, Cultured, Humans, Reverse Transcriptase Inhibitors, Female, Constitutive Androstane Receptor, Aged
Abstract: Rilpivirine and etravirine are second-generation non-nucleoside reverse transcriptase inhibitors (NNRTIs) indicated for the treatment of HIV/AIDS. The constitutive androstane receptor (CAR) regulates the expression of genes involved in various biological processes, including the transport and biotransformation of drugs. We investigated the effect of rilpivirine and etravirine on the activity of the wild-type human CAR (hCAR-WT) and its hCAR-SV23 and hCAR-SV24 splice variants, and compared it with first-generation NNRTIs (efavirenz, nevirapine, and delavirdine).Receptor activation, ligand-binding domain (LBD) transactivation, and co-activator recruitment were investigated in transiently transfected, NNRTI-treated HepG2 cells. Nuclear translocation of green fluorescent protein-tagged hCAR-WT and CYP2B6 gene expression were assessed in NNRTI-treated human hepatocytes.Rilpivirine and etravirine activated hCAR-WT, but not hCAR-SV23 or hCAR-SV24, and without transactivating the LBD or recruiting steroid receptor coactivators SRC-1, SRC-2, or SRC-3. Among the first-generation NNRTIs investigated, only efavirenz activated hCAR-WT, hCAR-SV23, and hCAR-SV24, but none of them transactivated the LBD of these receptors or substantively recruited SRC-1, SRC-2, or SRC-3. Rilpivirine, etravirine, and efavirenz triggered nuclear translocation of hCAR-WT and increased hCAR target gene (CYP2B6) expression.NNRTIs activate hCAR-WT, hCAR-SV23, and hCAR-SV24 in a drug-specific and isoform-selective manner. The activation occurs by a mechanism that does not appear to involve binding to the LBD or recruitment of SRC-1, SRC-2, or SRC-3.
Published: 2014

40. Localization of cytochrome P450 and related enzymes in adult rat testis and downregulation by estradiol and bisphenol A

Author: Ravindranath Reddy Gilibili, Thomas K. H. Chang, A. Wayne Vogl, and Stelvio M. Bandiera
Subjects: Male, endocrine system, medicine.medical_specialty, CYP3A, Bisphenol, Down-Regulation, Biology, Toxicology, Rats, Sprague-Dawley, chemistry.chemical_compound, Downregulation and upregulation, Cytochrome P-450 Enzyme System, Phenols, Internal medicine, Microsomes, Testis, medicine, Animals, Benzhydryl Compounds, Cellular localization, Dose-Response Relationship, Drug, Estradiol, Cytochrome P450, Leydig Cells, Seminiferous Tubules, Endocrinology, chemistry, Microsomal epoxide hydrolase, Estradiol benzoate, Microsome, biology.protein
Abstract: There is a growing body of evidence that exposure to endocrine disrupting chemicals and to estrogenic compounds in particular can affect the testis and male fertility. In the present study, the constitutive expression of steroidogenic and non-steroidogenic cytochrome P450 (CYP) and related enzymes in adult rat testis, and their regulation by estradiol and bisphenol A, were investigated. CYP1B1, CYP2A1, NADPH-cytochrome P450 oxidoreductase (POR) and microsomal epoxide hydrolase (mEH) proteins, together with CYP17A1 and 3β-hydroxysteroid dehydrogenase (HSD3B), were detected by immunoblot analysis in testicular microsomes prepared from untreated adult Sprague Dawley rats. In contrast, CYP1A, CYP2B, CYP2E, CYP2D, CYP2C, CYP3A, and CYP4A enzymes were not detected. Immunofluorescence staining of cryosections of perfusion-fixed testes showed that CYP1B1, CYP2A1, CYP17A1, and HSD3B were expressed exclusively or mainly in interstitial cells, whereas mEH and POR protein staining was detected both in interstitial cells and in seminiferous tubules. Testicular CYP1B1 and CYP2A1 protein levels were decreased following treatment of adult rats with estradiol benzoate at 0.004, 0.04, 0.4, or 4 μmol/kg/day or bisphenol A at 400 or 800 μmol/kg/day, for 14 days, whereas expression of HSD3B was unaffected. Testicular CYP17A1, POR, and mEH protein expression was also downregulated at the three highest dosages of estradiol benzoate and at both dosages of bisphenol A. The present study is the first to establish the cellular localization of CYP1B1, mEH, and POR in rat testis and to demonstrate the suppressive effect of bisphenol A on testicular CYP1B1, CYP2A1, mEH, and POR protein levels.
Published: 2014

41. Ginkgo biloba extract potentiates human vitamin D receptor‐mediated increase in CYP2B6 reporter activity by 1α,25‐dihydroxyvitamin D 3 (1141.8)

Author: Aik Jiang Lau and Thomas K. H. Chang
Subjects: 1α 25 dihydroxyvitamin d3, CYP2B6, biology, Chemistry, Ginkgo biloba, Pharmacology, biology.organism_classification, Biochemistry, Calcitriol receptor, 3. Good health, Drug biotransformation, Genetics, Molecular Biology, Gene, Biotechnology
Abstract: Vitamin D receptor (VDR) regulates the expression of a broad array of genes, including those involved in drug biotransformation (e.g. CYP2B6). Ginkgo biloba extract induces CYP2B6, but it is not kn...
Published: 2014

42. Influence of dietary zinc deficiency during development on hepatic CYP2C11, CYP2C12, CYP3A2, CYP3A9, and CYP3A18 expression in postpubertal male rats11Abbreviations: CYP, cytochrome P450; GH, growth hormone; and RT-PCR, reverse transcription-polymerase chain reaction

Author: Thomas K. H. Chang, Masahiko Kawai, Stelvio M. Bandiera, and Zhaoming Xu
Subjects: Pharmacology, medicine.medical_specialty, biology, Cytochrome P450, chemistry.chemical_element, Weanling, Zinc, medicine.disease, Biochemistry, Sexual dimorphism, Endocrinology, Thyroid-stimulating hormone, chemistry, Internal medicine, Gene expression, biology.protein, Zinc deficiency, medicine, Testosterone
Abstract: The present study investigated the effect of dietary zinc deficiency during the developmental period on hepatic cytochrome P450 (CYP) expression in postpubertal male rats. Twenty-one-day-old weanling male Wistar rats were randomly assigned to one of the following dietary groups: zinc-adequate (31 mg zinc/kg diet); marginal zinc-deficient (3 mg zinc/kg diet); severe zinc-deficient (1 mg zinc/kg diet); or pair-fed control for either the marginal or severe zinc-deficient group. All rats were killed at 63 days of age. Compared with the corresponding pair-fed controls, marginal zinc deficiency decreased CYP2C11-mediated testosterone 2α- and 16α-hydroxylase activities by 43 and 42%, respectively, whereas severe zinc deficiency reduced each of these activities by approximately 60%. The decrease in CYP2C11 activity was accompanied by a reduction in CYP2C11 protein and mRNA levels, as assessed by immunoblot and reverse transcription-polymerase chain reaction (RT-PCR) assays, respectively. Additional RT-PCR analysis indicated that severe zinc deficiency decreased CYP3A2 and CYP3A18 mRNA levels by 49 and 43%, respectively, whereas it increased CYP2C12 (253%) and CYP3A9 (238%) mRNA expression. Plasma testosterone concentration was decreased by 67% in the marginal zinc-deficient group when compared with the corresponding pair-fed control group. By comparison, it was below the limit of quantification (0.2 ng/mL) in the severe zinc-deficient rats. Overall, these results indicate that dietary zinc deficiency during the developmental period feminized the hepatic gene expression of the sexually dimorphic CYP2C11, CYP3A2, CYP3A18, CYP2C12, and CYP3A9 in postpubertal male rats.
Published: 2001

43. Effect of exogenous growth hormone on somatic growth, gonadal development, and hepatic CYP2C11 and CYP2C12 expression in prepubertal intact male rats

Author: Gail D. Bellward, Stelvio M. Bandiera, Thomas K. H. Chang, and Masahiko Kawai
Subjects: Pharmacology, medicine.medical_specialty, Physiology, Somatic cell, Preputial gland, Cytochrome P450, General Medicine, Biology, Testicle, Sexual dimorphism, Endocrinology, medicine.anatomical_structure, Physiology (medical), Internal medicine, Gene expression, medicine, biology.protein, Development of the gonads, Hormone
Abstract: The influence of exogenous growth hormone (GH) on pubertal maturation, as assessed by growth, age of preputial separation, testicular development, and hepatic expression of sexually dimorphic cytochrome P450 (CYP) enzymes, was investigated. Treatment of 22-day old prepubertal intact male rats with twice daily subcutaneous (sc) injections of rat recombinant GH (0.12 µg/g body weight) for 12 or 21 days did not affect body weight, skeletal growth, or testicular weight. By comparison, GH suppressed hepatic CYP2C11 enzyme activity, protein, and mRNA levels but induced CYP2C12 expression. GH suppressed CYP2C11 expression by approximately 60% in prepubertal rats as compared with 30% in adult rats, whereas it increased CYP2C12 levels to 80% of the normal female levels but had no effect in adult male rats. Twice daily intravenous injections of GH suppressed CYP2C11 only. Increasing the sc dose of GH 30-fold produced little or no additional change in CYP2C11 or CYP2C12 expression, whereas it modestly increased body weight and skeletal growth and reduced testicular weight. Overall, the present study provides the first demonstration that prepubertal administration (22-33 days of age) of GH at a pharmacologically relevant dose (0.12 µg/g twice daily) suppressed hepatic expression of CYP2C11 in 34-day-old intact male rats, suggesting that in this age group the liver is intrinsically responsive to transcription factors involved in the regulation of GH-dependent, sex-specific CYP gene expression. A higher dose (3.6 µg/g) of GH administered during the prepubertal period was required to elicit a modest effect on somatic growth and gonadal development.Key words: cytochrome P450, CYP2C11, CYP2C12, growth hormone, preputial separation, pubertal development, testosterone.
Published: 2001

44. Effect oftrans-resveratrol on 7-benzyloxy-4-trifluoromethylcoumarinO-dealkylation catalyzed by human recombinant CYP3A4 and CYP3A5

Author: Thomas K. H. Chang and Rosita K. Y. Yeung
Subjects: Pharmacology, Wine, CYP3A4, biology, Physiology, Stereochemistry, Chemistry, food and beverages, Cytochrome P450, General Medicine, Alkylation, law.invention, Catalysis, Biochemistry, Polyphenol, law, Physiology (medical), biology.protein, Recombinant DNA, CYP3A5
Abstract: Red wine concentrate has been reported to inhibit the catalytic activity of human recombinant cytochrome P450 (CYP) 3A4. Wine contains many polyphenolic compounds, including trans-resveratrol, which is also available commercially as a nutraceutical product. In the present study, we examined the in vitro effect of trans-resveratrol on human CYP3A catalytic activity by employing recombinant CYP3A4 and CYP3A5 as model enzymes and 7-benzyloxy-4-trifluoromethylcoumarin (BFC) as a CYP3A substrate. Trans-resveratrol inhibited BFC O-dealkylation catalyzed by CYP3A4 and CYP3A5 in a concentration-dependent manner. In each case, the inhibition was noncompetitive, as determined by Lineweaver-Burk and Dixon plots of the enzyme kinetic data. The apparent Kivalues (mean ± SEM) for the inhibition by trans-resveratrol of BFC O-dealkylation catalyzed by CYP3A4 and CYP3A5 were 10.2 ± 1.1 µM and 14.7 ± 0.3 µM, respectively. Preincubation of trans-resveratrol with NADPH and CYP3A4 or CYP3A5 for 10 or 15 min prior to initiation of substrate oxidation did not enhance the inhibitory effect, suggesting that this compound was not a mechanism-based inactivator of CYP3A4 or CYP3A5 when BFC was used as the substrate. Overall, our study provides the first demonstration that trans-resveratrol inhibits, in vitro, a substrate oxidation reaction catalyzed by human recombinant CYP3A4 and CYP3A5.Key words: 7-benzyloxy-4-trifluoromethylcoumarin, cytochrome P450, CYP3A4, CYP3A5, 7-hydroxy-4-trifluoromethylcoumarin, nutraceutical, trans-resveratrol.
Published: 2001

45. Trans-resveratrol modulates the catalytic activity and mRNA expression of the procarcinogen-activating human cytochrome P450 1B1

Author: Thomas K. H. Chang, Hin Hin Ko, and Wendy B. K. Lee
Subjects: Pharmacology, chemistry.chemical_classification, Physiology, CYP1B1, Cytochrome P450, General Medicine, Biology, Resveratrol, Molecular biology, Enzyme assay, body regions, chemistry.chemical_compound, Enzyme, chemistry, Biochemistry, Cell culture, Physiology (medical), Gene expression, biology.protein, Cytochrome P-450 Enzyme Inhibitors
Abstract: The present study was performed to determine if trans-resveratrol (3,5,4'-trihydroxy-trans-stilbene) modulates the catalytic activity and gene expression of cytochrome P450 1B1 (CYP1B1). In vitro, trans-resveratrol decreased human recombinant CYP1B1-catalyzed 7-ethoxyresorufin O-dealkylation activity, with an IC50 value of 1.4 +/- 0.2 microM (mean +/- SEM). Enzyme kinetic analysis indicated that trans-resveratrol inhibited CYP1B1 enzyme activity by a mixed-type inhibition and the apparent Ki was 0.75 +/- 0.06 microM. To determine if trans-resveratrol modulates constitutive CYP1B1 gene expression, cultured MCF-7 human breast carcinoma cells were treated with trans-resveratrol. As indicated by RT-PCR analysis, treatment of MCF-7 cells with 10 microM trans-resveratrol decreased relative CYP1B1 mRNA levels after 5 h, but not after 1.5 or 3 h, of exposure. trans-Resveratrol treatment at 5, 7.5, 10, or 20 microM for 5 h produced a concentration-dependent decrease in CYP1B1 mRNA levels. The extent of suppression was approximately 50% at 20 microM concentration. The suppressive effect was not a consequence of a toxic response to the compound as assessed by a cell proliferation assay. Overall, our novel finding that trans-resveratrol inhibits the catalytic activity and suppresses the constitutive gene expression of CYP1B1 leads to the possibility that this nutraceutical confers protection against toxicity and carcinogenicity induced by compounds that undergo CYP1B1-catalyzed bioactivation.
Published: 2000

46. Functional analysis of splice variants of human constitutive androstane receptor: Investigation with flavonol (3‐hydroxyflavone) and its metabolites

Author: Thomas K. H. Chang and Aik Jiang Lau
Subjects: 0303 health sciences, Functional analysis, 3-Hydroxyflavone, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Constitutive androstane receptor, Genetics, splice, Molecular Biology, 030217 neurology & neurosurgery, 030304 developmental biology, Biotechnology
Published: 2013

47. Indirect activation of the SV23 and SV24 splice variants of human constitutive androstane receptor: analysis with 3-hydroxyflavone and its analogues

Author: Aik Jiang, Lau and Thomas K H, Chang
Subjects: Flavonoids, Receptors, Cytoplasmic and Nuclear, Hep G2 Cells, Ligands, Transfection, Research Papers, Nuclear Receptor Coactivator 3, Nuclear Receptor Coactivator 2, Nuclear Receptor Coactivator 1, Liver, Genes, Reporter, Humans, Protein Isoforms, Constitutive Androstane Receptor
Abstract: Naturally occurring splice variants of human CAR (hCAR), including hCAR-SV23 (insertion of amino acids SPTV) and hCAR-SV24 (APYLT), have been shown to be expressed in liver. However, little is known regarding how hCAR-SV23 and hCAR-SV24 are activated. Therefore, we investigated the mode of activation of these hCAR splice variants.Cell-based reporter gene assays, including ligand-binding domain transactivation assays and coactivator recruitment assays, were conducted on cultured HepG2 cells transfected with various constructs and treated with 3-hydroxyflavone or a hydroxylated (galangin, datiscetin, kaempferol, morin, quercetin or myricetin) or methylated (isorhamnetin, tamarixetin, or syringetin) analogue.Among the flavonols investigated, only 3-hydroxyflavone increased hCAR-SV23 and hCAR-SV24 activities. 3-Hydroxyflavone did not transactivate the ligand-binding domain of these isoforms or recruit steroid receptor coactivators (SRC-1, SRC-2, or SRC-3). By comparison, 3-hydroxyflavone, galangin, datiscetin, kaempferol, quercetin, isorhamnetin and tamarixetin activated hCAR-WT, whereas none of the flavonols activated hCAR-SV25 (both SPTV and APYLT insertions). The flavonols 3-Hydroxyflavone, galangin, quercetin and tamarixetin transactivated the ligand-binding domain of hCAR-WT, but only 3-hydroxyflavone recruited SRC-1, SRC-2 and SRC-3 to the receptor.hCAR-SV23 and hCAR-SV24 can be activated by a mechanism that does not involve the ligand-binding domain of the receptor or recruitment of SRC-1, SRC-2, or SRC-3. 3-Hydroxyflavone and its structural analogues activated hCAR in an isoform-selective and chemical-specific manner. Overall, our study provides insight into a novel mode of ligand activation of hCAR-SV23 and hCAR-SV24.
Published: 2013

48. Selective Activation of Human Pregnane X Receptor, Glucocorticoid Receptor, and Constitutive Androstane Receptor by Individual Ginkgolides

Author: Thomas K. H. Chang, Guixiang Yang, and Aik Jiang Lau
Subjects: 0303 health sciences, medicine.medical_specialty, Pregnane X receptor, Chemistry, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Glucocorticoid receptor, Internal medicine, Constitutive androstane receptor, Genetics, medicine, Ginkgolides, Molecular Biology, 030217 neurology & neurosurgery, 030304 developmental biology, Biotechnology
Published: 2012

49. Evaluating In Situ (E)‐2,4‐Diene‐Valproic Acid in the Toxicity of Valproic Acid and (E)‐2‐Ene‐Valproic Acid in Sandwich‐Cultured Rat Hepatocytes

Author: Jayakumar Surendradoss, Frank S. Abbott, and Thomas K. H. Chang
Subjects: In situ, 0303 health sciences, Valproic Acid, Diene, Biochemistry, Medicinal chemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Toxicity, Genetics, medicine, Molecular Biology, 030217 neurology & neurosurgery, Ene reaction, 030304 developmental biology, Biotechnology, medicine.drug
Published: 2012

50. Selective agonism of human pregnane X receptor by individual ginkgolides

Author: Thomas K. H. Chang, Aik Jiang Lau, Guixiang Yang, and Chun Wei Yap
Subjects: Pharmacology, Pregnane X receptor, Receptors, Steroid, Chemistry, Pregnane X Receptor, Pharmaceutical Science, Hep G2 Cells, Ligand (biochemistry), Crystallography, X-Ray, chemistry.chemical_compound, Structure-Activity Relationship, Glucocorticoid receptor, Ginkgolides, Nuclear receptor, Constitutive androstane receptor, Ginkgolide, Tumor Cells, Cultured, Humans, Receptor, Luciferases, Renilla, Protein Binding
Abstract: Ginkgolide A, ginkgolide B, ginkgolide C, and ginkgolide J are structurally related terpene trilactones present in Ginkgo biloba extract. Pregnane X receptor (PXR), glucocorticoid receptor (GR), and constitutive androstane receptor (CAR) regulate the expression of genes involved in diverse biological functions. In the present study, we investigated the effects of individual ginkgolides as single chemical entities on the function of human PXR (hPXR), human GR (hGR), and human CAR (hCAR). In cell-based reporter gene assays, none of the ginkgolides activated hGR or hCAR (wild-type and its SV23, SV24, and SV25 splice variants). Concentration-response experiments showed that ginkgolide A and ginkgolide B activated hPXR and rat PXR to a greater extent than ginkgolide C, whereas ginkgolide J had no effect. As determined by a time-resolved fluorescence resonance energy transfer competitive binding assay, ginkgolide A and ginkgolide B, but not ginkgolide C or ginkgolide J, were shown to bind to the ligand-binding domain of hPXR, consistent with molecular docking data. Compared with tetraethyl 2-(3,5-di-tert-butyl-4-hydroxyphenyl)ethenyl-1,1-bisphosphonate (SR12813) (a known agonist of hPXR), ginkgolide A and ginkgolide B were considerably less potent in binding to hPXR. These two ginkgolides recruited steroid receptor coactivator-1 to hPXR and increased hPXR target gene (CYP3A4) expression, as assessed by a mammalian two-hybrid assay and real-time polymerase chain reaction, respectively. In conclusion, the individual ginkgolides regulate the function of nuclear receptors in a receptor-selective and chemical-dependent manner. This study identifies ginkgolide A and ginkgolide B as naturally occurring agonists of hPXR and provides mechanistic insight into the structure-activity relationship in ligand activation of hPXR.
Published: 2012

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