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101. Valproic acid glucuronidation is associated with increases in 15-F2t-isoprostane in rats

Author

Vincent Tong, Stoyan Karagiozov, Frank S. Abbott, Thomas K. H. Chang, and Xiao Wei Teng

Subjects
Male, medicine.medical_specialty, Magnetic Resonance Spectroscopy, Time Factors, Free Radicals, Glucuronidation, medicine.disease_cause, Dinoprost, Biochemistry, Mass Spectrometry, Lipid peroxidation, Rats, Sprague-Dawley, chemistry.chemical_compound, Glucuronic Acid, Physiology (medical), Internal medicine, medicine, Animals, Vasoconstrictor Agents, Inducer, Valproic Acid, Chromatography, Camphanes, Dose-Response Relationship, Drug, Chemistry, Rats, Dose–response relationship, Oxidative Stress, Endocrinology, Liver, Phenobarbital, lipids (amino acids, peptides, and proteins), Lipid Peroxidation, Glucuronide, Excitatory Amino Acid Antagonists, Oxidative stress, medicine.drug, Chromatography, Liquid
Abstract

Oxidative stress has been associated with valproic acid (VPA) treatment in rats and studies are ongoing to examine the relationship between VPA biotransformation and the increase in the lipid peroxidation biomarker 15-F2t-isoprostane (15-F2t-IsoP). This study investigated the effects of modulating VPA-1-O-acyl glucuronide (VPA-G) formation on 15-F2t-IsoP levels. Adult male Sprague-Dawley rats were pretreated with phenobarbital (PB; 80 mg/kg/day for 4 days), (-)-borneol (320 mg/kg), or a combination of both before VPA treatment (500 mg/kg). Liver VPA-G levels were determined by LC/MS and plasma and liver 15-F2t-IsoP levels were measured using an EIA method. PB, an inducer of VPA glucuronidation, elevated both liver VPA-G and plasma and liver 15-F2t-IsoP levels in VPA-treated rats. (-)-Borneol, an inhibitor of glucuronidation, significantly reduced the levels of liver VPA-G and decreased plasma and liver 15-F2t-IsoP levels in both the VPA and the PB + VPA groups. (-)-Borneol and PB alone did not elevate 15-F2t-IsoP levels compared to the vehicle control groups. The fluorinated analogue of VPA, alpha-fluoro-VPA, was a poor substrate for glucuronidation and did not elevate 15-F2t-IsoP levels. In summary, the VPA-induced formation of 15-F2t-IsoP is apparently associated with VPA glucuronidation.

Published
2004

102. UDP-glucuronosyltransferases and clinical drug-drug interactions

Author

Thomas K. H. Chang, Mary H H Ensom, and Tony K. L. Kiang

Subjects
Drug, UGT1A4, media_common.quotation_subject, Glucuronidation, Diflunisal, Pharmacology, digestive system, Enzyme activator, Glucuronides, medicine, Humans, Pharmacology (medical), Drug Interactions, Enzyme inducer, Glucuronosyltransferase, media_common, Clinical Trials as Topic, Polymorphism, Genetic, biology, Chemistry, Drug interaction, Enzyme Activation, Biochemistry, Pharmaceutical Preparations, Pharmacogenetics, Enzyme Induction, biology.protein, medicine.drug
Abstract

UDP-glucuronosyltransferase (UGT) enzymes catalyze the conjugation of various endogenous substances (e.g., bilirubin) and exogenous compounds (e.g., drugs). The human UGT superfamily is comprised of 2 families (UGT1 and UGT2) and 3 subfamilies (UGT1A, UGT2A, and UGT2B). Many of the individual UGT enzymes are expressed not only in liver but also in extrahepatic tissues, where the extent of glucuronidation can be substantial. Several others (e.g., UGT1A7, UGT1A8, and UGT1A10) are expressed only in extrahepatic tissues. The molecular regulation of UGT enzyme is still not fully understood, but various transcription factors appear to play a regulatory role. The expression of individual UGT enzymes is subject to genetic polymorphism and these enzymes can be inhibited or induced by xenobiotics. Experimental evidence in humans indicates that the glucuronidation of acetaminophen, codeine, zidovudine, carbamazepine, lorazepam, and propafenone can influenced by specific interacting drugs. In contrast, the glucuronidation of diflunisal, morphine, naproxen, and temazepam is not affected appreciably by the drugs investigated to date. In general, UGT-mediated human drug interaction studies are difficult to interpret. The factors that complicate the interpretation of this type of drug interaction data are discussed.

Published
2004

107. Enzymatic Analysis of cDNA-Expressed Human CYPIAI, CYPlA2, and CYPIBI with 7-Ethoxyresorufin as Substrate

Author

Thomas K. H. Chang and David J. Waxman

Subjects
chemistry.chemical_classification, Enzyme, Biochemistry, biology, chemistry, CYP1B1, Complementary DNA, CYP1A2, biology.protein, Substrate (chemistry), Cytochrome P450, Metabolism, Fluorescence
Abstract

Cytochrome P450 (P450) enzymes belonging to the CYP1 family are highly inducible by polycyclic aromatic hydrocarbons and other environmental chemicals and play a major role in the metabolism of many foreign chemicals and endogenous substances. We describe a spectrofluorometric method for determining 7-ethoxyresorufin O-dealkylation catalyzed by CYP1A1, CYP1A2, and CYPB1. The formation of the enzymatic product, resorufin, is monitored continuously by fluorescence using an excitation wavelength of 530 nm and an emission wavelength of 580 nm. This method can be applied to assay P450-catalyzed formation of resorufin from other alkoxyresorufins, such as 7-methoxyresorufin, 7-benzyloxyresorufin, and 7-pentoxyresorufin. It can also be used to assay 7-ethoxyresorufin O-dealkylation activity in isolated hepatocytes and cultured cells that express this P450 activity.

Published
2003

109. CYP2D6-Dependent Bufuralol 1 '-Hydroxylation Assayed by Reversed-Phase Ion-Pair High-Performance Liquid Chromatography with Fluorescence Detection

Author

Charles L. Crespi, Thomas K. H. Chang, and David J. Waxman

Subjects
Hydroxylation, chemistry.chemical_compound, Chromatography, chemistry, Phase (matter), Bufuralol, Perchloric acid, Mass spectrometry, Acetonitrile, High-performance liquid chromatography, Fluorescence
Abstract

A reverse-phase, high-performance liquid chromatography method is described for the quantification of 1'-hydroxybufuralol formed enzymatically by the incubation of bufuralol with cDNA-expressed CYP2D6 or human liver microsomes. Analytical separation is achieved using a C18 column and a mobile phase consisting of 30% acetonitrile and 2 mM perchloric acid, with detection by fluorescence using an excitation wavelength of 252 nm and an emission wavelength of 302 nm. This method is applicable to enzymatic studies for determination of CYP2D6-catalyzed bufuralol 1'-hydroxylation activity.

Published
2003

110. Determination of CYP2CSGatalyzed Diclofenac 4'-Hydroxylation by High-Performance Liquid Chromatography

Author

David J. Waxman, Charles L. Crespi, and Thomas K. H. Chang

Subjects
Hydroxylation, chemistry.chemical_compound, Chromatography, Diclofenac, chemistry, Microsome, medicine, Perchloric acid, Methanol, Acetonitrile, High-performance liquid chromatography, Catalysis, medicine.drug
Abstract

A reverse-phase, high-performance liquid chromatography method is described for quantification of diclofenac 4'-hydroxylation catalyzed by human liver microsomes or cDNA-expressed CYP2C9. Analytical separation is achieved using a C18 column developed with a gradient of 30% acetonitrile and 2 mM perchloric acid in water to 100% methanol, with detection at 280 nm. This method is applicable to enzymatic studies for determination of CYP2C9-catalyzed diclofenac 4'-hydroxylation activity.

Published
2003

111. CYP2Cl g-Mediated (S)-Mephenytoin 4'-Hydroxylation Assayed by High-Performance Liquid Chromatography with Radiometric Detection

Author

David J. Waxman, Charles L. Crespi, and Thomas K. H. Chang

Subjects
Hydroxylation, chemistry.chemical_compound, Chromatography, Human liver, Chemistry, Microsome, medicine, Methanol, Mephenytoin, CYP2C19, High-performance liquid chromatography, medicine.drug
Abstract

A reverse-phase, high-performance liquid chromatography method is described for the quantification of 4'-hydroxymephenytoin formed enzymatically from 14C-labeled (S)-mephenytoin following incubation with cDNA-expressed CYP2C19 or human liver microsomes. Analytical separation is achieved using a C18 column developed with a gradient from 10 to 100% methanol, with detection using a scintillation detector. This method is applicable to enzymatic studies for determination of CYP2C19-catalyzed (S)-mephenytoin 4'-hydroxylation activity.

Published
2003

113. Spectrophotometric Analysis of Human CY P2El -Catalyzed pNitrophenol Hydroxylation

Author

David J. Waxman, Thomas K. H. Chang, and Charles L. Crespi

Subjects
chemistry.chemical_classification, Hydroxylation, Nitrophenol, chemistry.chemical_compound, Chromatography, Enzyme, Chemistry, Microsome, CYP2E1, Trichloroacetic acid, Neutralization, Catalysis
Abstract

The cytochrome P450 enzyme CYP2E1 catalyzes the oxidative metabolism of many solvents and other small organic molecules. A spectrophotometric method is described for determination of CYP2E1 activity by monitoring the formation of p-nitrocatechol from p-nitrophenol by cDNA-expressed CYP2E1 or isolated liver microsomes. The enzymatic product, p-nitrocatechol, is assayed at 535 nm after acidification of the reaction mixture with trichloroacetic acid followed by neutralization using 2 M NaOH. This method is applicable to enzymatic studies for determination of P450-catalyzed p-nitrophenol hydroxylation activity.

Published
2003

114. Determination of CYP4All -Catalyzed Laurie Acid 12-Hydroxylation by High-Performance Liquid Chromatography with Radiometric Detection

Author

David J. Waxman, Thomas K. H. Chang, and Charles L. Crespi

Subjects
Hydroxylation, chemistry.chemical_compound, Chromatography, Chemistry, Substrate (chemistry), lipids (amino acids, peptides, and proteins), Perchloric acid, Methanol, Acetonitrile, Lauric acid, High-performance liquid chromatography, Catalysis
Abstract

Lauric acid serves as an endogenous substrate for the cytochrome P450 enzyme CYP4A11. A reverse-phase, high-performance liquid chromatography method is described for the quantification of 12-hydroxylauric acid formed enzymatically by incubation of 14C-labeled lauric acid with cDNA-expressed CYP4A11 or human liver microsomes. Analytical separation is achieved using a C18 column and a gradient of 30% acetonitrile and 2 mM perchloric acid to 100% methanol, using a detection scintillation counter. This method is applicable to enzymatic studies for determination of lauric acid 12-hydroxylation activity.

Published
2003

115. Transcript profiling of cytochrome P450 genes in HL-60 human leukemic cells: upregulation of CYP1B1 by all-trans-retinoic acid

Author

Masahiko, Kawai, Jie, Chen, Catherine Y S, Cheung, and Thomas K H, Chang

Subjects
Receptors, Steroid, DNA, Complementary, Transcription, Genetic, Reverse Transcriptase Polymerase Chain Reaction, Pregnane X Receptor, Receptors, Cytoplasmic and Nuclear, HL-60 Cells, Tretinoin, Up-Regulation, Cytochrome P-450 Enzyme System, Cytochrome P-450 CYP1B1, Humans, RNA, Aryl Hydrocarbon Hydroxylases, RNA, Messenger, Constitutive Androstane Receptor, Transcription Factors
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 microM 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

116. The effect of valproic acid on hepatic and plasma levels of 15-F2t-isoprostane in rats

Author

Thomas K. H. Chang, Jie Chen, Frank S. Abbott, and Vincent Tong

Subjects
Male, medicine.medical_specialty, Lipid Peroxides, medicine.disease_cause, Dinoprost, Biochemistry, Thiobarbituric Acid Reactive Substances, Gas Chromatography-Mass Spectrometry, Lipid peroxidation, Rats, Sprague-Dawley, chemistry.chemical_compound, Cytochrome P-450 Enzyme System, Physiology (medical), Internal medicine, medicine, Animals, Enzyme Inhibitors, Biotransformation, Liver injury, chemistry.chemical_classification, Valproic Acid, Reactive oxygen species, F2-Isoprostanes, biology, Proadifen, Cytochrome P450, Metabolism, Triazoles, medicine.disease, Rats, Oxidative Stress, Endocrinology, chemistry, Liver, Phenobarbital, biology.protein, lipids (amino acids, peptides, and proteins), Anticonvulsants, Oxidative stress, medicine.drug
Abstract

The mechanism by which valproic acid (VPA) induces liver injury remains unknown, but it is hypothesized to involve the generation of toxic metabolites and/or reactive oxygen species. This study's objectives were to determine the effect of VPA on plasma and hepatic levels of the F(2)-isoprostane, 15-F(2t)-IsoP, a marker for oxidative stress, and to investigate the influence of cytochrome P450- (P450-) mediated VPA biotransformation on 15-F(2t)-IsoP levels in rats. In rats treated with VPA (500 mg/kg), plasma 15-F(2t)-IsoP was increased 2.5-fold at t(max) = 0.5 h. Phenobarbital pretreatment (80 mg/kg/d for 4 d) in VPA-treated rats increased plasma and liver levels of free 15-F(2t)-IsoP by 5-fold and 3-fold, respectively, when compared to control groups. This was accompanied by an elevation in plasma and liver levels of P450-mediated VPA metabolites. Pretreatment with SKF-525A (80 mg/kg) or 1-aminobenzotriazole (100 mg/kg), which inhibited P450-mediated VPA metabolism, did not attenuate the increased levels of plasma 15-F(2t)-IsoP in VPA-treated groups. Plasma and hepatic levels of 15-F(2t)-IsoP were further elevated after 14 d of VPA treatment compared to single-dose treatment. Our data indicate that VPA increases plasma and hepatic levels of 15-F(2t)-IsoP and this effect can be enhanced by phenobarbital by a mechanism not involving P450-catalyzed VPA biotransformation.

Published
2003

117. Dose-dependent protection of cardiac function by propofol during ischemia and early reperfusion in rats: effects on 15-F2t-isoprostane formation

Author

David V. Godin, Zhengyuan Xia, David M. Ansley, and Thomas K. H. Chang

Subjects
Cardiac function curve, Male, Isoprostane, Physiology, medicine.medical_treatment, Ischemia, Myocardial Ischemia, Myocardial Reperfusion Injury, Pharmacology, In Vitro Techniques, Dinoprost, Antioxidants, Ventricular Function, Left, Lipid peroxidation, Rats, Sprague-Dawley, chemistry.chemical_compound, Physiology (medical), medicine, Animals, Saline, Propofol, F2-Isoprostanes, Dose-Response Relationship, Drug, business.industry, Heart, General Medicine, medicine.disease, Rats, Dose–response relationship, chemistry, Anesthesia, Lipid Peroxidation, business, Perfusion, Anesthetics, Intravenous, medicine.drug
Abstract

We examined the effects of propofol (2,6-diisopropylphenol) on functional recovery and 15-F2t-isoprostane generation during ischemia–reperfusion in Langendorff-perfused rat hearts. Before the induction of 40 min of global ischemia, hearts were perfused (10 min) with propofol at 5 (lo-P) or 12 μg/mL (hi-P) in saline or with saline only (control). During ischemia, saline, lo-P, or hi-P was perfused through the aorta at 60 μL/min. During the first 15 min of reperfusion, propofol (5 or 12 μg/mL) was continued, followed by perfusion with 5 μg/mL propofol for 75 min in both propofol-treated groups. After 90 min of reperfusion (Rep-90), heart tissues were harvested for assessment of antioxidant status. In hi-P, we observed increased latency to and greater reduction of ischemic contracture relative to the lo-P or control groups. 15-F2t-Isoprostane concentrations increased during ischemia and were significantly lower in hi-P and lo-P than in control (P < 0.01). At Rep-90, myocardial functional recovery was greater in both propofol-treated groups relative to control, and it correlated positively with tissue antioxidant capacity preservation. Tissue antioxidant capacity was better preserved in hi-P than in lo-P treatment (P < 0.05). We conclude that oxidant injury occurs during ischemia and reperfusion, and propofol provides dose-dependent protection primarily by enhancing tissue antioxidant capacity and reducing lipid peroxidation.Key words: propofol, myocardium, ischemia–reperfusion, 15-F2t-isoprostane.

Published
2003

118. Real-time polymerase chain reaction analysis of CYP1B1 gene expression in human liver

Author

Jie Chen, Vincent Pillay, Thomas K. H. Chang, Jeong-Yau Ho, and Stelvio M. Bandiera

Subjects
Adult, Male, Adolescent, CYP1B1, Immunoblotting, Gene Expression, Toxicology, Isozyme, law.invention, law, Cytochrome P-450 CYP1A2, Gene expression, Cytochrome P-450 CYP1A1, Humans, RNA, Messenger, Polymerase chain reaction, Aged, DNA Primers, Messenger RNA, biology, Reverse Transcriptase Polymerase Chain Reaction, Smoking, CYP1A2, Cytochrome P450, Middle Aged, Molecular biology, Real-time polymerase chain reaction, Child, Preschool, Calibration, Cytochrome P-450 CYP1B1, biology.protein, Microsomes, Liver, Electrophoresis, Polyacrylamide Gel, Female, Aryl Hydrocarbon Hydroxylases
Abstract

Procarcinogen-activating cytochrome P450 (CYP) enzymes such as CYP1B1, CYP1A1, and CYP1A2 are considered to play an important role in chemical carcinogenesis. However, conflicting data exist with respect to CYP1B1 expression in human liver. In the present study, we measured CYP1B1 mRNA and protein expression in liver samples from 12 individuals (7 nonsmokers, 4 smokers, and 1 ex-smoker) and compared the levels to those of CYP1A1 and CYP1A2. As analyzed by real-time polymerase chain reaction, CYP1B1 mRNA was present in all samples and the inter-individual variability was 16-fold. The group mean level was 5-fold greater in smokers than nonsmokers (121 +/- 46 vs. 26 +/- 5 molecules/ng double-stranded DNA, p < 0.05). By comparison, CYP1A1 mRNA was detectable in samples from 4 of 7 nonsmokers, 3 of 4 smokers, and one ex-smoker, whereas CYP1A2 mRNA was detectable in samples from 5 nonsmokers, 4 smokers, and the ex-smoker. The mean levels of CYP1A1 and CYP1A2 mRNA were 4-fold and 9-fold greater, respectively, in smokers than nonsmokers, but the differences were not statistically significant. The inter-individual variability in CYP1A1 and CYP1A2 mRNA expression was 26-fold and 500-fold, respectively. Immunoblot analysis using several antibodies and with a larger panel (n = 27) of liver microsomes showed that CYP1A1 and CYP1B1 proteins were undetectable, whereas CYP1A2 was detectable in all samples and quantifiable in 24 of 27 samples. In summary, our novel finding indicates that CYP1B1 mRNA is expressed in human liver and the levels are increased in smokers, but the protein is undetectable.

Published
2003

119. Pharmacogenetics: the therapeutic drug monitoring of the future?

Author

Payal Patel, Mary H H Ensom, and Thomas K. H. Chang

Subjects
Drug, Drug Utilization, medicine.medical_specialty, Cost effectiveness, media_common.quotation_subject, Azathioprine, Pharmacology, Therapeutic index, Pharmacotherapy, Cytochrome P-450 Enzyme System, Drug Therapy, Predictive Value of Tests, Medicine, Humans, Pharmacology (medical), Intensive care medicine, media_common, medicine.diagnostic_test, business.industry, Genetic Variation, Membrane Transport Proteins, Therapeutic drug monitoring, Pharmacogenetics, Drug Monitoring, business, medicine.drug
Abstract

Genetic variability in drug response occurs as a result of molecular alterations at the level of drug-metabolising enzymes, drug targets/receptors, and drug transport proteins. In this paper, we discuss the possibility that therapeutic drug monitoring (TDM) in the future will involve not the mere measurement and interpretation of drug concentrations but will include both traditional TDM and pharmacogenetics-oriented TDM. In contrast to traditional TDM, which cannot be performed until after a drug is administered to the patient. pharmacogenetics-oriented TDM can be conducted even before treatment begins. Other advantages of genotyping over traditional TDM include, but are not limited to, the following: (i) it does not require the assumption of steady-state conditions (or patient compliance) for the interpretation of results; (ii) it can often be performed less invasively (with saliva, hair root or buccal swab samples); (iii) it can provide predictive value for multiple drugs [e.g. a number of cytochrome P450 (CYP) 2D6, CYP2C 19 or CYP2C9 substrates] rather than a single drug; (iv) it provides mechanistic, instead of merely descriptive, information; and (v) it is constant over an individual's lifetime (and not influenced by concurrent drug administration, alteration in hormonal levels or disease states). Pharmacogenetic information can be applied a priori for initial dose stratification and identification of cases where certain drugs are simply not effective. However, traditional TDM will still be required for all of the reasons that we use it now. In current clinical practice, pharmacogenetic testing is performed for only a few drugs (e.g. mercaptopurine, thioguanine, azathioprine, trastuzumab and tacrine) and in a limited number of teaching hospitals and specialist academic centres. We propose that other drugs (e.g. warfarin, phenytoin, codeine, oral hypoglycaemics, tricyclic antidepressants, aminoglycosides, digoxin, cyclosporin, cyclophosphamide, ifosfamide, theophylline and clozapine) are potential candidates for pharmacogenetics-oriented TDM. However, prospective studies of phaymacogenetics-oriented TDM must be performed to determine its efficacy and cost effectiveness in optimising therapeutic effects while minimising toxicity. In the future, in addition to targeting a patient's drug concentrations within a therapeutic range, pharmacists are likely to be making dosage recommendations for individual drugs on the basis of the individual patient's genotype. As we enter the era of personalised drug therapy, we will be able to identify not only the best drug to be administered to a particular patient, but also the most effective and safest dosage from the outset of therapy.

Published
2001

120. Growth hormone regulation and developmental expression of rat hepatic CYP3A18, CYP3A9, and CYP3A2

Author

Stelvio M. Bandiera, Gail D. Bellward, Masahiko Kawai, and Thomas K. H. Chang

Subjects
Male, medicine.medical_specialty, Aging, Hypophysectomy, medicine.medical_treatment, Period (gene), Biology, Biochemistry, Gene Expression Regulation, Enzymologic, Rats, Sprague-Dawley, Mice, Sex Factors, Cytochrome P-450 Enzyme System, Prepuberty, Internal medicine, Gene expression, medicine, Animals, Cytochrome P-450 CYP3A, Testosterone, Pharmacology, Messenger RNA, Cytochrome P450, Gene Expression Regulation, Developmental, Oxidoreductases, N-Demethylating, Rats, Endocrinology, Liver, Growth Hormone, Steroid Hydroxylases, Microsome, biology.protein, Female, Aryl Hydrocarbon Hydroxylases
Abstract

The present study investigated the role of growth hormone (GH) in hepatic CYP3A18 and CYP3A9 expression in prepubertal and adult male rats. For comparison, the effects of GH on CYP3A2 expression were also measured. Initial experiments demonstrated that CYP3A18 mRNA levels were greater during puberty and adulthood than during the prepubertal period, CYP3A9 mRNA was not expressed until puberty and its expression increased in adulthood, and CYP3A2 mRNA levels were relatively constant from prepuberty to adult life. Hypophysectomy, which results in the loss of multiple pituitary factors including GH, increased CYP3A2 and CYP3A18 mRNA expression 3- to 4-fold, but it did not affect CYP3A9 mRNA levels or CYP3A-mediated testosterone 2beta- or 6beta-hydroxylase activity in adult rats. GH administered as twice daily s.c. injections (0.12 microg/g body weight) to hypophysectomized or intact adult rats did not affect CYP3A18 or CYP3A9 mRNA expression. The same treatment decreased CYP3A2 mRNA and protein and testosterone 2beta- and 6beta-hydroxylase activity levels in intact but not hypophysectomized rats. However, in intact prepubertal rats, intermittent GH administration decreased CYP3A18 and CYP3A2 mRNA levels, but a higher dosage (3.6 microg/g) was required to suppress CYP3A2. Overall, the present study demonstrated that: (a) the constitutive expression of CYP3A18, CYP3A9, and CYP3A2 does not require the presence of GH, (b) CYP3A18 is more sensitive than CYP3A9 to GH modulation in adult rats; and (c) CYP3A2 is less sensitive to the suppressive influence of GH during the prepubertal period than during adult life.

Published
2000

121. Impact of tamoxifen on peripubertal androgen imprinting of rat hepatic cytochrome P450 2C11, cytochrome P450 3A2, and steroid 5 alpha-reductase

Author

Thomas K. H. Chang, Maureen M.Y. Chan, Susan L. Holsmer, Gail D. Bellward, and Stelvio M. Bandiera

Subjects
Male, medicine.medical_specialty, Sex Differentiation, medicine.drug_class, medicine.medical_treatment, Biochemistry, Steroid, Rats, Sprague-Dawley, 3-Oxo-5-alpha-Steroid 4-Dehydrogenase, Cytochrome P-450 Enzyme System, Internal medicine, medicine, Animals, Cytochrome P-450 CYP3A, Testosterone, Imprinting (psychology), Cytochrome P450 Family 2, Pharmacology, Sexual differentiation, biology, Estradiol, Estrogen Antagonists, Cytochrome P450, Membrane Proteins, Antiestrogen, Androgen, Rats, Tamoxifen, Endocrinology, Steroid 16-alpha-Hydroxylase, Toxicity, Steroid Hydroxylases, biology.protein, Microsomes, Liver, Female, Aryl Hydrocarbon Hydroxylases, medicine.drug
Abstract

Expression of sex-dependent rat hepatic cytochromes P450 and steroid 5 alpha-reductase is regulated mainly by the sex-specific pattern of growth hormone (GH) secretion and is subject to androgen imprinting. Since tamoxifen suppresses GH pulse amplitude and nadir levels, we investigated the effect of tamoxifen on peripubertal testosterone imprinting of hepatic CYP2C11, CYP3A2, CYP2A1, and steroid 5 alpha-reductase. Prepubertal tamoxifen administration (5 mg once daily s.c. on days 28 and 29 of age) to non-ovariectomized female Sprague-Dawley rats did not affect hepatic microsomal CYP2C11-dependent testosterone 2 alpha-hydroxylase, CYP3A-mediated testosterone 6 beta-hydroxylase, CYP2A1-dependent testosterone 7 alpha-hydroxylase, or steroid 5 alpha-reductase activity in adult rats. Testosterone treatment (5 mumol/kg, s.c., once daily) of intact female rats during either puberty (days 35-49 of age) or adult life (days 69-77 of age) had no effect on these enzyme activities in adult (78-day-old) female rats, but the same treatment given during both of these periods induced the male-specific testosterone 2 alpha- and 6 beta-hydroxylase activities and suppressed the female-predominant testosterone 7 alpha-hydroxylase and steroid 5 alpha-reductase activities, indicating that peripubertal testosterone administration imprints the adult androgen responsiveness but not the basal levels of these enzyme activities in non-ovariectomized female rats. However, peripubertal androgen imprinting of the basal levels of testosterone 2 alpha-hydroxylase and steroid 5 alpha-reductase activities was observed in female rats administered tamoxifen prepubertally. Tamoxifen pretreatment also enhanced testosterone imprinting of the adult androgen responsiveness of testosterone 2 alpha- and 6 beta-hydroxylase and steroid 5 alpha-reductase activities. The enhanced testosterone hydroxylase activities were, however, not associated with an increase in microsomal NADPH-cytochrome P450 reductase activity, but were accompanied by elevated hepatic CYP2C11 and CYP3A2 protein levels. Overall, the present study indicates that prepubertal tamoxifen administration does not interfere with the normal sex differentiation of the gender-dependent hepatic cytochromes P450 and steroid 5 alpha-reductase, but this drug modulates peripubertal androgen imprinting of CYP2C11, CYP3A2, and steroid 5 alpha-reductase in adult female rats.

Published
1996

122. Response to Letter to the Editor

Author

Thomas K. H. Chang, Stelvio M. Bandiera, and Jie Chen

Subjects
Pharmacology, Pharmaceutical Science
Published
2003

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