Your search keyword '"Ketoconazole pharmacology"' showing total 115 results

1. Pharmacokinetics, Safety, Tolerability, and Pharmacodynamics of Alicapistat, a Selective Inhibitor of Human Calpains 1 and 2 for the Treatment of Alzheimer Disease: An Overview of Phase 1 Studies.

Author

Lon HK, Mendonca N, Goss S, Othman AA, Locke C, Jin Z, and Rendenbach-Mueller B

Subjects

Alzheimer Disease enzymology, Clinical Trials, Phase I as Topic, Cognition drug effects, Dose-Response Relationship, Drug, Enzyme Inhibitors adverse effects, Enzyme Inhibitors blood, Healthy Volunteers, Humans, Ketoconazole adverse effects, Ketoconazole pharmacokinetics, Pyrrolidines adverse effects, Pyrrolidines pharmacokinetics, Randomized Controlled Trials as Topic, Sleep drug effects, Alzheimer Disease drug therapy, Calpain antagonists & inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Pyrrolidines pharmacology

Abstract

Alicapistat is an orally active selective inhibitor of calpain 1 and 2 whose overactivation has been linked to Alzheimer disease (AD). Three studies were conducted in healthy subjects (18-55 years), 1 in healthy elderly subjects (≥65 years), and 1 in patients with mild to moderate AD. Four studies assessed pharmacokinetics, 1 study in healthy subjects assessed pharmacodynamics (sleep parameters, particularly rapid eye movement [REM], as a measure of central nervous system [CNS] penetration and activity), and all studies assessed safety. Participants received single doses or multiple twice-daily doses of alicapistat for up to 14 days. Maximum alicapistat plasma concentrations were reached in 2 to 5 hours; half-life was 7 to 12 hours postdose. Alicapistat exposure was dose proportional in the alicapistat 50- to 1000-mg dose range. Exposure of the alicapistat R,S diastereomer was approximately 2-fold greater than exposure of the R,R diastereomer in healthy young and elderly subjects and patients with AD. Alicapistat at 400- or 800-mg twice-daily doses had no effect on REM sleep parameters, whereas the active control, donepezil at 10 mg twice daily, affected sleep parameters. Across all trials, the incidence of treatment-emergent adverse events was similar in the placebo and alicapistat groups. There were no clinically significant changes in vital signs and laboratory measurements. The lack of an effect of alicapistat on sleep suggests that concentrations in the CNS were inadequate or that preclinical studies do not predict alicapistat effects in humans., (© 2018, The American College of Clinical Pharmacology.)

Published

2019

2. Effect of enzyme inhibition on perampanel pharmacokinetics: Why study design matters.

Author

Gidal BE, Maganti R, Laurenza A, Yang H, Verbel DA, Schuck E, and Ferry J

Subjects

Adult, Analysis of Variance, Anticonvulsants blood, Area Under Curve, Computer Simulation, Cross-Over Studies, Drug Interactions, Healthy Volunteers, Humans, Ketoconazole pharmacology, Male, Models, Chemical, Nitriles, Pyridones blood, Therapeutic Equivalency, Time Factors, Young Adult, Anticonvulsants pharmacokinetics, Cytochrome P-450 CYP3A Inhibitors pharmacology, Enzyme Inhibitors pharmacology, Pyridones pharmacokinetics

Abstract

Objectives: Perampanel, a selective, noncompetitive AMPA receptor antagonist, is indicated as adjunctive therapy for the treatment of partial seizures with or without secondarily generalized seizures and primary generalized tonic-clonic seizures in patients with epilepsy aged 12years and older. In vitro studies and Phase I trials indicate that perampanel is metabolized almost exclusively by CYP3A, with an elimination half-life (t 1/2 ) averaging approximately 105h. Understanding of pharmacokinetic (PK) interactions-enzyme inhibition or induction-and anticipating their occurrence are important for management of patients with epilepsy. Here we report PK results from a Phase I drug-drug interaction (DDI) study (Study 005) combining perampanel with the CYP3A inhibitor ketoconazole, as well as supplementary in silico predictions further exploring this interaction., Methods: A Phase I, randomized, open-label, two-period, two-treatment, two-way crossover study was conducted in 26 healthy adult male volunteers. Subjects were randomized to 1 of 2 treatment sequences. In one period, subjects received a single 1-mg fasting dose of perampanel (Day1); in the other period, subjects received ketoconazole 400mg once daily for 10days with a single 1-mg perampanel dose while fasting (Day3). Blood samples were drawn at multiple time points up to 288h after the perampanel dose. Pharmacokinetic parameters of perampanel were calculated by noncompartmental analysis, and safety was recorded. An integrated, physiologically based PK model built in Simcyp ® provided additional insight into this interaction. Drug-drug interaction intensity was measured by the ratio of systemic exposure (area under plasma concentration-time curve [AUC]) of perampanel in the presence or absence of concomitant ketoconazole., Results: Single oral doses of 1mg perampanel and once-daily oral doses of ketoconazole 400mg were safe and well tolerated. Maximum perampanel plasma concentration (C max ) and time to C max showed no apparent differences when perampanel was administered alone versus with ketoconazole. Ketoconazole co-administration resulted in an approximate 20% increase in perampanel AUC (P<0.001). This increase, although statistically significant, was a<2.0-fold AUC change and alone would suggest a modest effect of ketoconazole. To further explore these results, DDI simulations were performed to query the findings and test additional study conditions. Using the actual trial conditions of Study 005, the simulations also predicted an AUC ratio increase <2-fold, providing verification of the simulation assumptions and the modest effect of ketoconazole for 10days. Simulations further suggested that an interaction effect of ketoconazole on perampanel exposure (>2-fold) of potential clinical significance could be predicted when using larger doses of ketoconazole (e.g., 200mg every 6h) coadministered for a greater time period (e.g., 30days), with AUC ratio as high as 3.36. Additionally, simulations suggested that a significant interaction with co-administration of perampanel and an inhibitor more potent than ketoconazole (such as itraconazole) could not be ruled out., Conclusions: Selecting an appropriate study design is critical to fully characterize the PK interaction for drugs such as perampanel that have a long t 1/2 . Although a negligible effect on perampanel PK was observed following co-administration of ketoconazole 400mg/day for 10days, this is likely due in part to the relatively brief co-administration period of ketoconazole and perampanel (<3 times the t 1/2 of perampanel). While short-term administration of a CYP3A inhibitor may not significantly increase perampanel exposure, such increases may be expected following chronic and larger dosing or with a more potent inhibitor., (Copyright © 2017 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published

2017

3. Investigation into CYP3A4-mediated drug-drug interactions on midostaurin in healthy volunteers.

Author

Dutreix C, Munarini F, Lorenzo S, Roesel J, and Wang Y

Subjects

Adult, Antineoplastic Agents administration & dosage, Antineoplastic Agents pharmacology, Chromatography, Liquid, Cytochrome P-450 CYP3A biosynthesis, Cytochrome P-450 CYP3A Inhibitors, Drug Administration Schedule, Drug Interactions, Enzyme Induction drug effects, Enzyme Inhibitors administration & dosage, Female, Humans, Ketoconazole pharmacology, Male, Midazolam pharmacology, Middle Aged, Rifampin pharmacology, Staurosporine administration & dosage, Staurosporine pharmacokinetics, Staurosporine pharmacology, Tandem Mass Spectrometry, Young Adult, Antineoplastic Agents pharmacokinetics, Cytochrome P-450 CYP3A metabolism, Enzyme Inhibitors pharmacology, Staurosporine analogs & derivatives

Abstract

Purpose: Midostaurin (PKC412), a multitargeted tyrosine kinase inhibitor that targets FMS-related tyrosine kinase 3 and KIT, is in clinical trials for the treatment for acute myeloid leukemia and advanced systemic mastocytosis. In vitro studies showed that midostaurin is predominantly metabolized by cytochrome P450 3A4 (CYP3A4) and that midostaurin inhibits and/or induces the same enzyme. Here, we address the clinical relevance of CYP3A4-related drug-drug interactions with midostaurin as either a "victim" or "perpetrator.", Methods: Three phase I studies in healthy volunteers evaluated the effects of a CYP3A4 inhibitor (ketoconazole 400 mg daily for 10 days) or CYP3A4 inducer (rifampicin 600 mg daily for 14 days) on concentrations of midostaurin and its metabolites following a single 50-mg dose of midostaurin and the effects of midostaurin as a single dose (100 mg) and multiple doses (50 mg twice daily) on midazolam (a sensitive CYP3A4 probe) concentration. The plasma concentrations of midostaurin and its 2 active metabolites, CGP62221 and CGP52421, were determined using a sensitive liquid chromatography/tandem mass spectrometry method., Results: Inhibition of CYP3A4 by ketoconazole increased midostaurin exposure more than tenfold, and induction of CYP3A4 by rifampicin decreased midostaurin exposure by more than tenfold. Midostaurin did not appreciably affect the concentrations of midazolam or its metabolite, 1'-hydroxymidazolam, at single or multiple doses., Conclusion: The pharmacokinetics of midostaurin and its metabolites was affected substantially by ketoconazole and rifampicin, suggesting that midostaurin is a sensitive CYP3A4 substrate. Midostaurin did not appear to inhibit or induce CYP3A4 in vivo.

Published

2013

4. Co-administration of rivaroxaban with drugs that share its elimination pathways: pharmacokinetic effects in healthy subjects.

Author

Mueck W, Kubitza D, and Becka M

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, Adolescent, Adult, Anticoagulants administration & dosage, Clarithromycin administration & dosage, Clarithromycin pharmacokinetics, Clarithromycin pharmacology, Cytochrome P-450 CYP2J2, Cytochrome P-450 CYP3A administration & dosage, Cytochrome P-450 Enzyme Inhibitors, Drug Interactions, Enzyme Inhibitors administration & dosage, Enzyme Inhibitors pharmacology, Erythromycin administration & dosage, Erythromycin pharmacokinetics, Erythromycin pharmacology, Humans, Ketoconazole administration & dosage, Ketoconazole pharmacokinetics, Ketoconazole pharmacology, Metabolic Clearance Rate, Midazolam administration & dosage, Midazolam pharmacokinetics, Midazolam pharmacology, Middle Aged, Morpholines administration & dosage, Rivaroxaban, Substrate Specificity, Thiophenes administration & dosage, Young Adult, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Anticoagulants pharmacokinetics, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 Enzyme System metabolism, Enzyme Inhibitors pharmacokinetics, Morpholines pharmacokinetics, Thiophenes pharmacokinetics

Abstract

Aims: The anticoagulant rivaroxaban is an oral, direct Factor Xa inhibitor for the management of thromboembolic disorders. Metabolism and excretion involve cytochrome P450 3A4 (CYP3A4) and 2J2 (CYP2J2), CYP-independent mechanisms, and P-glycoprotein (P-gp) and breast cancer resistance protein (Bcrp) (ABCG2)., Methods: The pharmacokinetic effects of substrates or inhibitors of CYP3A4, P-gp and Bcrp (ABCG2) on rivaroxaban were studied in healthy volunteers., Results: Rivaroxaban did not interact with midazolam (CYP3A4 probe substrate). Exposure to rivaroxaban when co-administered with midazolam was slightly decreased by 11% (95% confidence interval [CI] -28%, 7%) compared with rivaroxaban alone. The following drugs moderately affected rivaroxaban exposure, but not to a clinically relevant extent: erythromycin (moderate CYP3A4/P-gp inhibitor; 34% increase [95% CI 23%, 46%]), clarithromycin (strong CYP3A4/moderate P-gp inhibitor; 54% increase [95% CI 44%, 64%]) and fluconazole (moderate CYP3A4, possible Bcrp [ABCG2] inhibitor; 42% increase [95% CI 29%, 56%]). A significant increase in rivaroxaban exposure was demonstrated with the strong CYP3A4, P-gp/Bcrp (ABCG2) inhibitors (and potential CYP2J2 inhibitors) ketoconazole (158% increase [95% CI 136%, 182%] for a 400 mg once daily dose) and ritonavir (153% increase [95% CI 134%, 174%])., Conclusions: Results suggest that rivaroxaban may be co-administered with CYP3A4 and/or P-gp substrates/moderate inhibitors, but not with strong combined CYP3A4, P-gp and Bcrp (ABCG2) inhibitors (mainly comprising azole-antimycotics, apart from fluconazole, and HIV protease inhibitors), which are multi-pathway inhibitors of rivaroxaban clearance and elimination., (© 2013 Bayer Pharma AG. British Journal of Clinical Pharmacology © 2013 The British Pharmacological Society.)

Published

2013

5. Optimization of drug-drug interaction study design: comparison of minimal physiologically based pharmacokinetic models on prediction of CYP3A inhibition by ketoconazole.

Author

Han B, Mao J, Chien JY, and Hall SD

Subjects

Area Under Curve, Dose-Response Relationship, Drug, Drug Interactions, Humans, Models, Biological, Research Design, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Midazolam pharmacokinetics

Abstract

Ketoconazole is a potent CYP3A inhibitor used to assess the contribution of CYP3A to drug clearance and quantify the increase in drug exposure due to a strong inhibitor. Physiologically based pharmacokinetic (PBPK) models have been used to evaluate treatment regimens resulting in maximal CYP3A inhibition by ketoconazole but have reached different conclusions. We compare two PBPK models of the ketoconazole-midazolam interaction, model 1 (Chien et al., 2006) and model 2 implemented in Simcyp (version 11), to predict 16 published treatment regimens. With use of model 2, 41% of the study point estimates of area under the curve (AUC) ratio and 71% of the 90% confidence intervals were predicted within 1.5-fold of the observed, but these increased to 82 and 100%, respectively, with model 1. For midazolam, model 2 predicted a maximal midazolam AUC ratio of 8 and a hepatic fraction metabolized by CYP3A (f(m)) of 0.97, whereas model 1 predicted 17 and 0.90, respectively, which are more consistent with observed data. On the basis of model 1, ketoconazole (400 mg QD) for at least 3 days and substrate administration within 2 hours is required for maximal CYP3A inhibition. Ketoconazole treatment regimens that use 200 mg BID underestimate the systemic fraction metabolized by CYP3A (0.86 versus 0.90) for midazolam. The systematic underprediction also applies to CYP3A substrates with high bioavailability and long half-lives. The superior predictive performance of model 1 reflects the need for accumulation of ketoconazole at enzyme site and protracted inhibition. Model 2 is not recommended for inferring optimal study design and estimation of fraction metabolized by CYP3A.

Published

2013

6. Steroid synthesis by Taenia crassiceps WFU cysticerci is regulated by enzyme inhibitors.

Author

Aceves-Ramos A, Valdez RA, Gaona B, Willms K, and Romano MC

Subjects

Androstenedione analogs & derivatives, Androstenedione pharmacology, Animals, Chromatography, Thin Layer, Danazol pharmacology, Desoxycorticosterone pharmacology, Estradiol metabolism, Ketoconazole pharmacology, Enzyme Inhibitors pharmacology, Steroids metabolism, Taenia drug effects, Taenia metabolism

Abstract

Cysticerci and tapeworms from Taenia crassiceps WFU, ORF and Taenia solium synthesize sex-steroid hormones in vitro. Corticosteroids increase the 17β-estradiol synthesis by T. crassiceps cysticerci. T. crassiceps WFU cysticerci synthesize corticosteroids, mainly 11-deoxycorticosterone (DOC). The aim of this work was to investigate whether classical steroidogenic inhibitors modify the capacity of T. crassiceps WFU cysticerci to synthesize corticosteroids and sex steroid hormones. For this purpose, T. crassiceps WFU cysticerci were obtained from the abdominal cavity of mice, pre-cultured for 24h in DMEM+antibiotics/antimycotics and cultured in the presence of tritiated progesterone ((3)H-P4), androstendione ((3)H-A4), or dehydroepiandrosterone ((3)H-DHEA) plus different doses of the corresponding inhibitors, for different periods. Blanks with the culture media adding the tritiated precursors were simultaneously incubated. At the end of the incubation period, parasites were separated and media extracted with ether. The resulting steroids were separated by thin layer chromatography (TLC). Data were expressed as percent transformation of the tritiated precursors. Results showed that after 2h of exposure of the cysticerci to 100 μM formestane, the (3)H-17β-estradiol synthesis from tritiated androstenedione was significantly inhibited. The incubation of cysticerci in the presence of (3)H-DHEA and danazol (100 nM) resulted in (3)H-androstenediol accumulation and a significant reduction of the 17β-estradiol synthesis. The cysticerci (3)H-DOC synthesis was significantly inhibited when the parasites were cultured in the presence of different ketoconazole dosis. The drug treatments did not affect parasite's viability. The results of this study showed that corticosteroid and sex steroid synthesis in T. crassiceps WFU cysticerci can be modified by steroidogenic enzyme inhibitors. As was shown previously by our laboratory and others, parasite survival and development depends on sex steroids, therefore the inhibition of their synthesis is a good starting point exploited in situations where the inhibition of steroidogenesis could help to control the infection for the development of new treatments, or replacement of the usual therapy in resistant parasite infections. We raise the possibility that these drug actions may be beneficially., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

7. Effect of ketoconazole on the pharmacokinetics of the 11β-hydroxysteroid dehydrogenase type 1 inhibitor ABT-384 and its two active metabolites in healthy volunteers: population analysis of data from a drug-drug interaction study.

Author

An G, Liu W, Katz DA, Marek G, Awni W, and Dutta S

Subjects

Adamantane pharmacokinetics, Area Under Curve, Drug Interactions, Humans, Models, Theoretical, Reference Values, 11-beta-Hydroxysteroid Dehydrogenase Type 1 antagonists & inhibitors, Adamantane analogs & derivatives, Antifungal Agents pharmacology, Enzyme Inhibitors pharmacokinetics, Ketoconazole pharmacology, Piperazines pharmacokinetics

Abstract

ABT-384 [1-piperazineacetamide, N-[5-(aminocarbonyl) tricyclo[3.3.1.13,7]dec-2-yl]-α,α-dimethyl-4-[5-(trifluoromethyl)-2-pyridinyl]-,stereoisomer] is a potent and selective inhibitor of 11β-hydroxysteroid dehydrogenase type 1 (HSD-1). ABT-384 has been shown to be safe and well tolerated in humans at doses up to 100 mg daily, and to fully inhibit both peripheral and brain HSD-1 at a dose of 2 mg daily. The effect of ketoconazole on the pharmacokinetics of ABT-384 and its two active metabolites, A-1331480 and A-847082, was investigated in healthy volunteers. When 10 mg of ABT-384 was coadministered with ketoconazole, ABT-384 exposures increased 18-fold for area under the plasma concentration-time curve from time 0 to infinity and 3.5-fold for Cmax. The results suggest that ABT-384 is a sensitive substrate of CYP3A. After ketoconazole coadministration, exposures of A-1331480 and A-847082 were also greatly increased. A population pharmacokinetic model was constructed for ABT-384 and its metabolites using NonMEM. A two-compartment model with three transit absorption compartments best described ABT-384 data. The model predicted a 69.3% decrease in ABT-384 clearance and 91.1% increase in the volume of distribution of ABT-384 in the presence of ketoconazole. A-1331480 was shown to be formation rate-limited and A-847082 was elimination rate-limited. Both metabolites were characterized by a one-compartment model with first-order rate constants of formation and elimination. Overall the model adequately captured the concentration-time profiles of ABT-384, A-1331480, and A-847082 in both ABT-384-alone and ketoconazole-coadministration conditions. Although ABT-384 exposures were greatly increased in the presence of ketoconazole, coadministration of ABT-384 with ketoconazole or other strong/moderate CYP3A inhibitors is not expected to contribute to any major clinical safety issues considering the favorable safety profile of ABT-384.

Published

2013

8. A thorough QTc study of 3 doses of iloperidone including metabolic inhibition via CYP2D6 and/or CYP3A4 and a comparison to quetiapine and ziprasidone.

Author

Potkin SG, Preskorn S, Hochfeld M, and Meng X

Subjects

Adolescent, Adult, Aged, Antipsychotic Agents administration & dosage, Antipsychotic Agents blood, Antipsychotic Agents pharmacokinetics, Cytochrome P-450 CYP2D6 genetics, Cytochrome P-450 CYP2D6 metabolism, Cytochrome P-450 CYP3A metabolism, Dibenzothiazepines administration & dosage, Dibenzothiazepines blood, Dibenzothiazepines pharmacokinetics, Drug Administration Schedule, Drug Interactions, Drug Monitoring, Electrocardiography, Female, Genotype, Humans, Isoxazoles administration & dosage, Isoxazoles blood, Isoxazoles pharmacokinetics, Ketoconazole pharmacology, Linear Models, Long QT Syndrome diagnosis, Long QT Syndrome physiopathology, Male, Middle Aged, Paroxetine pharmacology, Pharmacogenetics, Phenotype, Piperazines administration & dosage, Piperazines blood, Piperazines pharmacokinetics, Piperidines administration & dosage, Piperidines blood, Piperidines pharmacokinetics, Quetiapine Fumarate, Thiazoles administration & dosage, Thiazoles blood, Thiazoles pharmacokinetics, United States, Young Adult, Antipsychotic Agents adverse effects, Cytochrome P-450 CYP2D6 Inhibitors, Cytochrome P-450 CYP3A Inhibitors, Dibenzothiazepines adverse effects, Enzyme Inhibitors pharmacology, Heart Rate drug effects, Isoxazoles adverse effects, Long QT Syndrome chemically induced, Piperazines adverse effects, Piperidines adverse effects, Thiazoles adverse effects

Abstract

The potential for iloperidone, a D2/5-HT2A antipsychotic, to affect the heart rate-corrected QT interval (QTc) was assessed in the absence and presence of metabolic inhibitors in a randomized, open-label, multicenter study. QT interval prolongation by medications, including both conventional and atypical antipsychotic drugs, can predispose patients to cardiac arrhythmias and result in sudden death. Adults with schizophrenia or schizoaffective disorder and normal electrocardiograms at baseline (N = 188) were randomized 1:1:1:1:1 to iloperidone, 8 mg twice daily (BID), 12 mg BID, 24 mg once daily (QD); quetiapine, 375 mg BID; or ziprasidone, 80 mg BID during period 1 (no metabolic inhibitors present). Iloperidone BID produced mean changes in QTc Fridericia correction (QTcF) interval (8.5-9.0 milliseconds [ms]) similar to those produced by ziprasidone (9.6 ms) and higher than those produced by quetiapine (1.3 ms). Iloperidone, 24 mg QD, produced a mean QTcF change of 15.4 ms. Coadministration of metabolic inhibitors with iloperidone during periods 2 (paroxetine) and 3 (paroxetine and ketoconazole) resulted in greater increases in the QTc interval. Increased QTc was observed in individuals with specific cytochrome P450 2D6 polymorphisms. Up to 10% of patients on iloperidone experienced QTc intervals of 60 ms or longer in the presence of metabolic inhibition and QD dosing. However, no patients experienced QTc changes of clinical concern (QTc ≥ 500 ms). The most common adverse events with iloperidone were headache, anxiety, and dyspepsia. The only cardiovascular adverse events with iloperidone were non-concentration-dependent tachycardia that was mild in most patients and did not lead to further sequelae. Pharmacogenetics and recommendations are discussed.

Published

2013

9. The effect of CYP3A inhibitors and inducers on the pharmacokinetics of telaprevir in healthy volunteers.

Author

Garg V, Chandorkar G, Yang Y, Adda N, McNair L, Alves K, Smith F, and van Heeswijk RP

Subjects

Adult, Alkynes, Area Under Curve, Clinical Trials as Topic, Cyclopropanes, Drug Combinations, Drug Interactions, Female, Humans, Male, Middle Aged, Benzoxazines pharmacology, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Oligopeptides pharmacokinetics, Rifampin pharmacology

Abstract

Aim: To evaluate the effects of ketoconazole, rifampicin and efavirenz on the pharmacokinetics of telaprevir in healthy volunteers., Method: Results from three clinical studies are described. (1) Volunteers received a single 750 mg dose telaprevir with and without a single 400 mg dose ketoconazole. (2) Volunteers received (a) 1250 mg telaprevir followed by three 750 mg doses given every 8 h and (b) four 1250 mg telaprevir doses given every 8 h, with a single 400 mg dose ketoconazole given with the fourth dose of telaprevir. (3) Volunteers received either a single 750 mg dose telaprevir with or without 600 mg once daily rifampicin, or 750 mg every 8 h telaprevir with and without 600 mg once daily efavirenz., Results: A single 400 mg dose of ketoconazole increased single dose telaprevir exposure: the geometric least-squares mean ratio (GLSMR, with 90% confidence limits) was 1.24 (1.10, 1.41) for C(max) and 1.62 (1.45, 1.81) for AUC(0,∞). However, after multiple doses of telaprevir, there was no discernible effect of ketoconazole on telaprevir exposure. Co-administration of rifampicin at steady-state markedly reduced single dose telaprevir exposure with GLSMRs of 0.14 (0.11, 0.18) for C(max) and 0.08 (0.07, 0.11) for AUC(0,∞), whereas efavirenz had a smaller effect on telaprevir exposure when both drugs were co-administered at steady-state, with GLSMRs of 0.91 (0.81, 1.02) for C(max) , 0.53 (0.44, 0.65) for C(min), and 0.74 (0.65, 0.84) for AUC(0,8 h)., Conclusion: CYP3A inducers, rifampicin and efavirenz, can reduce telaprevir exposure to varying degrees based on their potency. The effect of ketoconazole as an inhibitor of telaprevir metabolism is more pronounced after a single dose of telaprevir than after repeated administration., (© 2012 Vertex Pharmaceuticals Incorporated. British Journal of Clinical Pharmacology © 2012 The British Pharmacological Society.)

Published

2013

10. Trypanosoma cruzi response to sterol biosynthesis inhibitors: morphophysiological alterations leading to cell death.

Author

Kessler RL, Soares MJ, Probst CM, and Krieger MA

Subjects

Cell Death drug effects, Chagas Disease metabolism, Chagas Disease parasitology, Ketoconazole pharmacology, Lovastatin pharmacology, Mitochondria drug effects, Mitochondria metabolism, Mitochondria pathology, Permeability, Trypanosoma cruzi growth & development, Trypanosoma cruzi ultrastructure, Biosynthetic Pathways drug effects, Enzyme Inhibitors pharmacology, Sterols biosynthesis, Trypanocidal Agents pharmacology, Trypanosoma cruzi drug effects, Trypanosoma cruzi metabolism

Abstract

The protozoan parasite Trypanosoma cruzi displays similarities to fungi in terms of its sterol lipid biosynthesis, as ergosterol and other 24-alkylated sterols are its principal endogenous sterols. The sterol pathway is thus a potential drug target for the treatment of Chagas disease. We describe here a comparative study of the growth inhibition, ultrastructural and physiological changes leading to the death of T. cruzi cells following treatment with the sterol biosynthesis inhibitors (SBIs) ketoconazole and lovastatin. We first calculated the drug concentration inhibiting epimastigote growth by 50% (EC(50)/72 h) or killing all cells within 24 hours (EC(100)/24 h). Incubation with inhibitors at the EC(50)/72 h resulted in interesting morphological changes: intense proliferation of the inner mitochondrial membrane, which was corroborated by flow cytometry and confocal microscopy of the parasites stained with rhodamine 123, and strong swelling of the reservosomes, which was confirmed by acridine orange staining. These changes to the mitochondria and reservosomes may reflect the involvement of these organelles in ergosterol biosynthesis or the progressive autophagic process culminating in cell lysis after 6 to 7 days of treatment with SBIs at the EC(50)/72 h. By contrast, treatment with SBIs at the EC(100)/24 h resulted in rapid cell death with a necrotic phenotype: time-dependent cytosolic calcium overload, mitochondrial depolarization and reservosome membrane permeabilization (RMP), culminating in cell lysis after a few hours of drug exposure. We provide the first demonstration that RMP constitutes the "point of no return" in the cell death cascade, and propose a model for the necrotic cell death of T. cruzi. Thus, SBIs trigger cell death by different mechanisms, depending on the dose used, in T. cruzi. These findings shed new light on ergosterol biosynthesis and the mechanisms of programmed cell death in this ancient protozoan parasite.

Published

2013

11. The effects on metabolic clearance when administering a potent CYP3A autoinducer with the prototypic CYP3A inhibitor, ketoconazole.

Author

Ayan-Oshodi MA, Willis BA, Annes WF, Lowe SL, Friedrich S, de la Peña A, Zhang W, Brown T, Wise SD, and Hall SD

Subjects

Administration, Oral, Adult, Aged, Alanine administration & dosage, Alanine pharmacokinetics, Alanine pharmacology, Amyloid Precursor Protein Secretases antagonists & inhibitors, Area Under Curve, Azepines administration & dosage, Azepines pharmacokinetics, Cells, Cultured, Drug Interactions, Enzyme Induction, Enzyme Inhibitors administration & dosage, Enzyme Inhibitors pharmacokinetics, Female, Half-Life, Hepatocytes enzymology, Humans, Hydroxylation, Ketoconazole administration & dosage, Ketoconazole pharmacokinetics, Male, Metabolic Clearance Rate, Midazolam administration & dosage, Midazolam pharmacokinetics, Middle Aged, Models, Biological, Nifedipine administration & dosage, Nifedipine pharmacokinetics, Testosterone metabolism, Young Adult, Alanine analogs & derivatives, Azepines pharmacology, Cytochrome P-450 CYP3A biosynthesis, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Hepatocytes drug effects, Ketoconazole pharmacology

Abstract

Ketoconazole is recognized as the prototypical CYP3A inhibitor and is often used to determine the metabolic CYP3A liabilities of new chemical entities in preclinical and clinical studies. Ketoconazole has been commercially available for approximately 30 years and was marketed before drug-metabolizing enzymes were well characterized; consequently, little is known about its metabolic profile. Semagacestat, a γ-secretase inhibitor investigated as a potential therapy for Alzheimer's disease, was determined to be a potent CYP3A autoinducer in human hepatocytes. Two human studies were conducted to assess the induction potential of semagacestat. In the first study (study 1, n = 20), semagacestat increased the mean apparent clearance (CL/F) of oral midazolam (76-324 l/h) and nifedipine (63-229 l/h) as predicted from hepatocytes. In a second (steady-state) study (study 2, n = 20), semagacestat CL/F increased from 22 after a single dose to 31 l/h. Ketoconazole decreased semagacestat CL/F by 32% after a single dose of semagacestat [geometric means ratio estimate, 0.68; 90% confidence interval (CI). 0.64, 0.73] and 46% at steady state (geometric means ratio estimate. 0.54; 90% CI, 0.51, 0.58). Ketoconazole area under the concentration-time curve over 8 h decreased 49% from first to last day of semagacestat dosing. Semagacestat significantly increases the oral clearance of CYP3A substrates, confirming its inducer designation. More importantly, when administered with a potent CYP3A inducer at steady state, ketoconazole's plasma exposure decreased, indicating that it may also be cleared by CYP3A, other inducible enzymes or transporters, or both.

Published

2012

12. The cytochrome P450 inhibitor, ketoconazole, inhibits oxidized linoleic acid metabolite-mediated peripheral inflammatory pain.

Author

Ruparel S, Green D, Chen P, and Hargreaves KM

Subjects

Animals, Antibodies pharmacology, Behavior, Animal drug effects, Cytochrome P-450 Enzyme System metabolism, Freund's Adjuvant, Hot Temperature, Hyperalgesia drug therapy, Hyperalgesia pathology, Inflammation complications, Inflammation pathology, Linoleic Acids immunology, Linoleic Acids, Conjugated immunology, Mice, Mice, Inbred C57BL, Nociception drug effects, Oxidation-Reduction drug effects, Pain complications, Pain pathology, Rats, Rats, Sprague-Dawley, TRPV Cation Channels agonists, TRPV Cation Channels metabolism, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Inflammation drug therapy, Ketoconazole pharmacology, Linoleic Acid metabolism, Pain drug therapy

Abstract

Background: Oxidized linoleic acid metabolites (OLAMs) are a class of endogenous agonists to the transient receptor potential V1 (TRPV1) receptor. Although TRPV1 mediates inflammatory heat hyperalgesia, it is not known if the OLAMs contribute to the peripheral activation of this receptor during tissue inflammation. In the present study, we evaluated whether the OLAM system is activated during inflammation and whether cytochrome P450 enzymes mediate OLAM contributions to heat hyperalgesia using the complete Freund's adjuvant (CFA) model of inflammation., Results: Our results demonstrate that the intraplantar (ipl) injection of anti-OLAM antibodies significantly reversed CFA-induced heat hyperalgesia. Moreover, application of lipid extracts from inflamed rat skin to cultured sensory neurons triggered a significant release of iCGRP that is blocked by co-treatment with I-RTX, a TRPV1 antagonist. To determine the role of CYP enzymes in mediating OLAM effects, we used a broad spectrum CYP inhibitor, ketoconazole. Pretreatment with ketoconazole inhibited the release of TRPV1 agonists in lipid extracts from inflamed skin and significantly reversed CFA-induced heat hyperalgesia by a peripheral mechanism of action. Moreover, the ipl injection of linoleic acid to rats 24 hr after CFA evoked spontaneous nocifensive behaviors that were significantly reduced by capsazepine, by knockout of the TRPV1 gene, or by pretreatment with either anti-OLAM antibodies or ketoconazole., Conclusions: Taken together, our data suggests that OLAMs contribute to inflammatory nociception in the periphery and that cytochrome P450 enzymes play a crucial role in mediating OLAM contributions to inflammatory heat hyperalgesia.

Published

2012

13. Discovery of a highly selective CYP3A4 inhibitor suitable for reaction phenotyping studies and differentiation of CYP3A4 and CYP3A5.

Author

Li X, Song X, Kamenecka TM, and Cameron MD

Subjects

Cytochrome P-450 CYP3A metabolism, Dose-Response Relationship, Drug, Drug Discovery, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors metabolism, Half-Life, Humans, Hydroxylation, Imidazoles chemical synthesis, Imidazoles metabolism, Ketoconazole pharmacology, Liver enzymology, Microsomes, Liver drug effects, Microsomes, Liver enzymology, Midazolam metabolism, Molecular Structure, Phenotype, Phenylurea Compounds chemical synthesis, Phenylurea Compounds metabolism, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins metabolism, Structure-Activity Relationship, Substrate Specificity, Testosterone metabolism, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Imidazoles pharmacology, Liver drug effects, Phenylurea Compounds pharmacology

Abstract

Current molecular tools lack the ability to differentiate the activity of CYP3A4 and CYP3A5 in biological samples such as human liver microsomes. Kinetic experiments and the CYP3A4 crystal structure indicate that the active sites of both enzymes are large and flexible, and have more than one binding subsite within the active site. 1-(4-Imidazopyridinyl-7phenyl)-3-(4'-cyanobiphenyl) urea (SR-9186) was optimized through several rounds of structural refinement from an initial screening hit to obtain greater than 1000-fold selectivity for the inhibition of CYP3A4 versus CYP3A5. Characterization data demonstrate selectivity using midazolam and testosterone hydroxylation assays with recombinant cytochrome P450, pooled human liver microsomes, and individually genotyped microsomes. Clear differences are seen between individuals with CYP3A5*1 and *3 genotypes. The antifungal drug ketoconazole is the most commonly used CYP3A inhibitor for in vitro and in vivo studies. A direct comparison of SR-9186 and ketoconazole under typical assay conditions used in reaction phenotyping studies demonstrated that SR-9186 had selectivity over CYP1A2, CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C19, CYP2D6, CYP2E1, and CYP3A5 greater than or equal to that of ketoconazole. In addition, the long half-life (106 min) of SR-9186 in incubations containing 1 mg/ml human liver microsomes provided sustained CYP3A4 inhibition.

Published

2012

14. The effect of CYP3A4 inhibition or induction on the pharmacokinetics and pharmacodynamics of orally administered ruxolitinib (INCB018424 phosphate) in healthy volunteers.

Author

Shi JG, Chen X, Emm T, Scherle PA, McGee RF, Lo Y, Landman RR, McKeever EG Jr, Punwani NG, Williams WV, and Yeleswaram S

Subjects

Adult, Antineoplastic Agents adverse effects, Antineoplastic Agents blood, Antineoplastic Agents pharmacology, Drug Interactions, Enzyme Induction drug effects, Erythromycin pharmacology, Female, Half-Life, Humans, Janus Kinase 1 antagonists & inhibitors, Janus Kinase 2 antagonists & inhibitors, Ketoconazole pharmacology, Male, Metabolic Detoxication, Phase I, Middle Aged, Nitriles, Phosphorylation drug effects, Protein Kinase Inhibitors adverse effects, Protein Kinase Inhibitors blood, Protein Kinase Inhibitors pharmacology, Pyrazoles adverse effects, Pyrazoles blood, Pyrazoles pharmacology, Pyrimidines, STAT3 Transcription Factor blood, STAT3 Transcription Factor metabolism, Young Adult, Antineoplastic Agents pharmacokinetics, Cytochrome P-450 CYP3A biosynthesis, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Protein Kinase Inhibitors pharmacokinetics, Pyrazoles pharmacokinetics, Rifampin pharmacology

Abstract

Ruxolitinib, a selective Janus kinase (JAK) 1&2 inhibitor in development for the treatment of myeloproliferative neoplasms, is primarily metabolized by CYP3A4. The effects of inhibition or induction of CYP3A4 on single oral dose ruxolitinib pharmacokinetics (PK) and pharmacodynamics (PD) were evaluated in healthy volunteers. Coadministration of ketoconazole (a potent CYP3A4 inhibitor) and erythromycin (a moderate CYP3A4 inhibitor) increased total ruxolitinib plasma exposure (AUC(0-∞)) by 91% and 27%, respectively, and ruxolitinib PD, as measured by the inhibition of interleukin (IL)-6-stimulated STAT3 phosphorylation in whole blood, was generally consistent with the PK observed. Pretreatment with rifampin, a potent CYP3A4 inducer, decreased ruxolitinib AUC(0-∞) by 71% while resulting in only a 10% decrease in the overall PD activity. This apparent PK/PD discrepancy may be explained, in part, by an increase in the relative abundance of ruxolitinib active metabolites with the rifampin coadministration. The collective PK/PD data suggest that starting doses of ruxolitinib should be reduced by 50% if coadministered with a potent CYP3A4 inhibitor, whereas adjustments in ruxolitinib starting doses may not be needed when coadministered with inducers or mild/moderate inhibitors of CYP3A4. All study doses of ruxolitinib were generally safe and well tolerated when given alone and in combination with ketoconazole, erythromycin, or rifampin.

Published

2012

15. Effects of ketoconazole and valproic acid on the pharmacokinetics of the next generation NNRTI, lersivirine (UK-453,061), in healthy adult subjects.

Author

Langdon G, Davis J, Layton G, Chong CL, Weissgerber G, and Vourvahis M

Subjects

Adult, Area Under Curve, Asian People, Cross-Over Studies, Cytochrome P-450 CYP3A metabolism, Drug Interactions, Glucuronosyltransferase metabolism, Humans, Male, Middle Aged, Nitriles administration & dosage, Pyrazoles administration & dosage, Reverse Transcriptase Inhibitors administration & dosage, Young Adult, Antifungal Agents pharmacology, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Nitriles pharmacokinetics, Pyrazoles pharmacokinetics, Reverse Transcriptase Inhibitors pharmacokinetics, Valproic Acid pharmacology

Abstract

Aims: To investigate the effect of inhibitors of cytochrome P450 (CYP) 3A4 and glucuronidation (UGT2B7) on the pharmacokinetics of lersivirine (UK-453,061), a next generation non-nucleoside reverse transcriptase inhibitor with a unique resistance profile, and to investigate the safety and tolerability of co-administration of lersivirine with these inhibitors., Methods: Two open-label, randomized, placebo-controlled, crossover studies were conducted in healthy subjects. Study 1 investigated the effect of ketoconazole (400 mg once daily) on the pharmacokinetics of lersivirine (250 mg once daily). Subjects received ketoconazole 400 mg once daily or placebo on days 1-2 and received lersivirine 250 mg once daily and ketoconazole 400 mg once daily or placebo on days 3-9. Study 2 investigated the effect of valproic acid (VPA, sodium valproate, 1000 mg once daily) on the PK of lersivirine (500 mg once daily). On days 1-7, subjects received lersivirine 500 mg once daily plus either VPA 1000 mg or placebo., Results: Compared with lersivirine alone, co-administration with ketoconazole increased the lersivirine mean area under the curve (AUC(0,24 h)) and maximum plasma concentration (C(max) ) by 82% (90% CI 74%, 91%) and 61% (90% CI 41%, 83%), respectively. VPA increased the mean lersivirine AUC(0,24 h) by 25% (90% CI 16%, 35%), with little effect on C(max) (2.5%, 90% CI -9%, 16%). There were no serious adverse events and no treatment-related discontinuations from either study., Conclusions: Inhibition of CYP3A4 and UGT2B7 by ketoconazole increased lersivirine exposure. Inhibition of UGT2B7-mediated glucuronidation by VPA had a modest effect on lersivirine exposure. Co-administration of lersivirine with either ketoconazole or VPA appeared to be well tolerated., (© 2011 Pfizer Inc. British Journal of Clinical Pharmacology © 2011 The British Pharmacological Society.)

Published

2012

16. Effects of CYP3A4 inhibition and induction on the pharmacokinetics and pharmacodynamics of tolvaptan, a non-peptide AVP antagonist in healthy subjects.

Author

Shoaf SE, Bricmont P, and Mallikaarjun S

Subjects

14-alpha Demethylase Inhibitors pharmacokinetics, 14-alpha Demethylase Inhibitors pharmacology, Adolescent, Adult, Area Under Curve, Benzazepines urine, Cytochrome P-450 CYP3A metabolism, Dose-Response Relationship, Drug, Double-Blind Method, Drug Interactions, Female, Humans, Ketoconazole pharmacology, Male, Middle Aged, Rifampin pharmacology, Tolvaptan, Urination drug effects, Young Adult, Antidiuretic Hormone Receptor Antagonists, Benzazepines pharmacokinetics, Benzazepines pharmacology, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology

Abstract

What Is Already Known About This Subject: Before these trials were done, the effects of CYP3A4 inhibition and induction on the pharmacokinetics (PK) and pharmacodynamics (PD) of tolvaptan in healthy subjects were unknown. As tolvaptan is a CYP3A4 substrate, knowing the effects of inhibition and induction on CYP3A4-mediated metabolism was important for dosing recommendations., What This Study Adds: This paper describes the changes in tolvaptan PK and PD following inhibition or induction of CYP3A4 and explores the mechanisms behind the disparity seen between tolvaptan PK and effects on urine output. It also discusses the concentrations at which tolvaptan produces its maximal response on urine output and the timing of the onset and offset of this response. AIMS In vitro studies indicated CYP3A4 alone was responsible for tolvaptan metabolism. To determine the effect of a CYP3A4 inhibitor (ketoconazole) and a CYP3A4 inducer (rifampicin) on tolvaptan pharmacokinetics (PK) and pharmacodynamics (PD), two clinical trials were performed., Methods: For CYP3A4 inhibition, a double-blind, randomized (5:1), placebo-controlled trial was conducted in 24 healthy subjects given either a single 30 mg dose of tolvaptan (n= 19) or matching placebo (n= 5) on day 1 with a 72 h washout followed by a 3 day regimen of 200 mg ketoconazole, once daily with 30 mg tolvaptan or placebo also given on day 5. For CYP3A4 induction, 14 healthy subjects were given a single dose of 240 mg tolvaptan with 48 h washout followed by a 7 day regimen of 600 mg rifampicin, once daily, with 240 mg tolvaptan also given on the seventh day., Results: When co-administered with ketoconazole, mean C(max) and AUC(0,∞) of tolvaptan were increased 3.48- and 5.40-fold, respectively. Twenty-four hour urine volume increased from 5.9 to 7.7 l. Erythromycin breath testing showed no difference following a single dose of tolvaptan. With rifampicin, tolvaptan mean C(max) and AUC were reduced to 0.13- and 0.17-fold of tolvaptan administered alone. Twenty-four hour urine volume decreased from 12.3 to 8.8 l., Conclusions: Tolvaptan is a sensitive CYP3A4 substrate with no inhibitory activity. Due to the saturable nature of tolvaptan's effect on urine excretion rate, changes in the pharmacokinetic profile of tolvaptan do not produce proportional changes in urine output., (© 2011 The Authors. British Journal of Clinical Pharmacology © 2011 The British Pharmacological Society.)

Published

2012

17. Predicting drug candidate victims of drug-drug interactions, using microdosing.

Author

Croft M, Keely B, Morris I, Tann L, and Lappin G

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Adult, Area Under Curve, Cross-Over Studies, Cytochrome P-450 Enzyme System metabolism, Dose-Response Relationship, Drug, Drug Interactions, Fluvoxamine pharmacology, Humans, Ketoconazole pharmacology, Male, Middle Aged, ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology

Abstract

Objective: The aim of this crossover human male volunteer study was to investigate the utility of microdosing in the investigation of drug-drug interactions., Methods: A mixture of midazolam, tolbutamide, caffeine and fexofenadine were administered as a microdose (25 μg each) before and after administration of a combined pharmacological dose of ketoconazole (400 mg) and fluvoxamine (100 mg) to inhibit P-glycoprotein and metabolism by cytochrome P450 (CYP) 1A2, CYP3A4 and CYP2C9., Results: When administered alone, pharmacokinetics for all four microdosed compounds scaled well with those reported for therapeutic doses and with previously performed microdose studies. The pharmacokinetics of each compound administered as a microdose were significantly altered after the administration of ketoconazole and fluvoxamine, showing statistically significant (p < 0.01) 12.8-, 8.1- and 3.2-fold increases in the area under the plasma concentration-time curve from time zero to infinity (AUC(∞)) for midazolam, caffeine and fexofenadine, respectively. A 1.8-fold increase (not statistically significant) in AUC(∞) was observed for tolbutamide. The changes in pharmacokinetics mediated by ketoconazole and fluvoxamine were quantitatively consistent with previously reported, non-microdose, drug-drug interaction data from studies including the same compounds., Conclusion: The initial data reported here demonstrate the utility of microdosing to investigate the risk of development drugs being victims of drug-drug interactions.

Published

2012

18. Orteronel (TAK-700), a novel non-steroidal 17,20-lyase inhibitor: effects on steroid synthesis in human and monkey adrenal cells and serum steroid levels in cynomolgus monkeys.

Author

Yamaoka M, Hara T, Hitaka T, Kaku T, Takeuchi T, Takahashi J, Asahi S, Miki H, Tasaka A, and Kusaka M

Subjects

Adrenal Glands drug effects, Androgen Antagonists pharmacology, Androgens metabolism, Animals, Cell Line, Tumor, Cells, Cultured, Dehydroepiandrosterone antagonists & inhibitors, Dehydroepiandrosterone blood, Humans, Hydrocortisone antagonists & inhibitors, Hydrocortisone blood, Imidazoles blood, Ketoconazole pharmacology, Macaca fascicularis, Male, Naphthalenes blood, Orchiectomy, Steroid 17-alpha-Hydroxylase metabolism, Testosterone antagonists & inhibitors, Testosterone blood, Adrenal Glands cytology, Enzyme Inhibitors pharmacology, Imidazoles pharmacology, Naphthalenes pharmacology, Steroid 17-alpha-Hydroxylase antagonists & inhibitors, Steroids blood, Steroids metabolism

Abstract

Surgical or pharmacologic methods to control gonadal androgen biosynthesis are effective approaches in the treatment of a variety of non-neoplastic and neoplastic diseases. For example, androgen ablation and its consequent reduction in circulating levels of testosterone is an effective therapy for advanced prostate cancers. Unfortunately, the therapeutic effectiveness of this approach is often temporary because of disease progression to the 'castration resistant' (CRPC) state, a situation for which there are limited treatment options. One mechanism thought to be responsible for the development of CRPC is extra-gonadal androgen synthesis and the resulting impact of these residual extra-gonadal androgens on prostate tumor cell proliferation. An important enzyme responsible for the synthesis of extra-gonadal androgens is CYP17A1 which possesses both 17,20-lyase and 17-hydroxylase catalytic activities with the 17,20-lyase activity being key in the androgen biosynthetic process. Orteronel (TAK-700), a novel, selective, and potent inhibitor of 17,20-lyase is under development as a drug to inhibit androgen synthesis. In this study, we quantified the inhibitory activity and specificity of orteronel for testicular and adrenal androgen production by evaluating its effects on CYP17A1 enzymatic activity, steroid production in monkey adrenal cells and human adrenal tumor cells, and serum levels of dehydroepiandrosterone (DHEA), cortisol, and testosterone after oral dosing in castrated and intact male cynomolgus monkeys. We report that orteronel potently suppresses androgen production in monkey adrenal cells but only weakly suppresses corticosterone and aldosterone production; the IC(50) value of orteronel for cortisol was ~3-fold higher than that for DHEA. After single oral dosing, serum levels of DHEA, cortisol, and testosterone were rapidly suppressed in intact cynomolgus monkeys. In castrated monkeys treated twice daily with orteronel, suppression of DHEA and testosterone persisted throughout the treatment period. In both in vivo models and in agreement with our in vitro data, suppression of serum cortisol levels following oral dosing was less than that seen for DHEA. In terms of human CYP17A1 and human adrenal tumor cells, orteronel inhibited 17,20-lyase activity 5.4 times more potently than 17-hydroxylase activity in cell-free enzyme assays and DHEA production 27 times more potently than cortisol production in human adrenal tumor cells, suggesting greater specificity of inhibition between 17,20-lyase and 17-hydroxylase activities in humans vs monkeys. In summary, orteronel potently inhibited the 17,20-lyase activity of monkey and human CYP17A1 and reduced serum androgen levels in vivo in monkeys. These findings suggest that orteronel may be an effective therapeutic option for diseases where androgen suppression is critical, such as androgen sensitive and CRPC., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

19. Effects of cytochrome P450 inhibitors on peroxidase activity.

Author

Martinkova M, Kubickova B, and Stiborova M

Subjects

Benzoflavones chemistry, Benzoflavones pharmacology, Disulfiram chemistry, Disulfiram pharmacology, Ditiocarb chemistry, Ditiocarb pharmacology, Ellipticines chemistry, Ellipticines pharmacology, Enzyme Activation drug effects, Enzyme Inhibitors chemistry, Horseradish Peroxidase metabolism, Humans, Ketoconazole chemistry, Ketoconazole pharmacology, Metyrapone chemistry, Metyrapone pharmacology, Piperonyl Butoxide chemistry, Piperonyl Butoxide pharmacology, Proadifen chemistry, Proadifen pharmacology, Quinidine chemistry, Quinidine pharmacology, Structure-Activity Relationship, Substrate Specificity drug effects, Sulfaphenazole chemistry, Sulfaphenazole pharmacology, Triazoles chemistry, Troleandomycin chemistry, Troleandomycin pharmacology, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Horseradish Peroxidase antagonists & inhibitors, Triazoles pharmacology

Abstract

Objectives: Of several enzymes metabolizing xenobiotics, cytochrome P450 (CYP) and peroxidase enzymes seem to be most important. One of the major challenges in studies investigating metabolism of xenobiotics is to resolve which of these two groups of enzymes is predominant to metabolize individual xenobiotic compounds. Utilization of selective inhibitors of CYP and peroxidase enzymes might be a useful tool to identify the contribution of these enzymes to metabolism of xenobiotics in samples, where both types of enzymes are present. The aim of this study was to investigate specificities of several known CYP inhibitors to these enzymes; whether they inhibit only the CYP enzymes and do not inhibit peroxidases., Methods: Since the oxidation of o-anisidine catalyzed by a model peroxidase used, horseradish peroxidase (HRP), is a two-substrate reaction, the inhibition potential of tested chemicals was studied with respect to both peroxidase substrates, o-anisidine and hydrogen peroxide. Initial velocities of o-anisidine oxidation by HRP under various conditions were determined spectrophotometrically., Results: The CYP inhibitors metyrapone, troleandomycine, disulfiram, sulfaphenazole, quinidine and 1-aminobenzotriazole do not inhibit o-anisidine oxidation catalyzed by HRP. In contrast, ketoconazole, diethyldithiocarbamate, ellipticine, α-naphtoflavone, proadifen SKF525A, piperonylbutoxide, were found to inhibit not only the CYPs, but also the HRP-mediated oxidation of o-anisidine. Interestingly, α-naphtoflavone inhibits oxidation of o-anisidine by HRP with respect to H2O2, but not with respect to o-anisidine. Diethyldithiocarbamate is the most potent peroxidase inhibitor of o-anisidine oxidation with Ki with respect to o-anisidine of 10 μM and Ki with respect to H2O2 of 60 μM, being even the better peroxidase inhibitor than the classical "peroxidase inhibitor" - propyl gallate (Ki with respect to o-anisidine of 60 μM and Ki with respect to H2O2 of 750 μM)., Conclusions: The results of the present study demonstrate that 1-aminobenzotriazole, a potent inhibitor of various CYP enzymes, seems to be the best candidate suitable for utilization in studies evaluating participation of CYP enzymes in metabolism of xenobiotics in various complex biological materials containing both CYP and peroxidase enzymes. Moreover, precaution to prevent misinterpretation of results is necessary in cases when proadifen SKF525A, piperonylbutoxide, diethyldithiocarbamate, ketoconazole, α-naphtoflavone and ellipticine are used in similar studies (as CYP inhibitors in various complex biological materials containing both CYP and peroxidase enzymes), since these chemicals can except of CYP enzymes inhibit also peroxidase-mediated reactions.

Published

2012

20. Exploring the possible metabolism mediated interaction of Glycyrrhiza glabra extract with CYP3A4 and CYP2D6.

Author

Pandit S, Ponnusankar S, Bandyopadhyay A, Ota S, and Mukherjee PK

Subjects

Animals, Chromatography, High Pressure Liquid, Inhibitory Concentration 50, Ketoconazole pharmacology, Male, Quinidine pharmacology, Rats, Wistar, Rhizome, Cytochrome P-450 CYP2D6 metabolism, Cytochrome P-450 CYP3A metabolism, Enzyme Inhibitors pharmacology, Glycyrrhiza chemistry, Glycyrrhizic Acid pharmacology, Herb-Drug Interactions, Plant Extracts pharmacology

Abstract

The rhizome of Glycyrrhiza glabra L. (licorice) is used very widely in Indian and Chinese traditional medicine, and it is a popular flavor ingredient of drinks, sweets and candies. Its medicinal uses include treating bronchitis, dry cough, respiratory infections, liver disorders and diabetes. Glycyrrhizin is normally considered to be its biologically active marker, so a rapid RP-HPLC method was developed for the quantitative estimation of glycyrrhizin in the extract. The effect of the standardized extract and its marker on drug metabolizing enzymes was evaluated through CYP3A4 and CYP2D6 inhibition assays to evaluate the safety through its drug interaction potential. The inhibition of CYP3A4 and CYP2D6 isozymes was analysed by the fluorescent product formation method. In the CYP450-CO assay, the interaction potential of the standardized extract and pooled microsomes (percentage inhibition 23.23 ± 1.84%), was found to be less than the standard inhibitor. In the fluorimetric assay, G. glabra extracts showed higher IC(50) values than their positive inhibitors, ketoconazole and quinidine for CYP3A4 and CYP2D6, respectively. Furthermore, the interaction potential of the plant extract was greater than the pure compound. The results demonstrate that G. glabra and its principle bioactive compound, glycyrrhizin, when co-administered with conventional medicines showed only a weak interaction potential with drug metabolizing enzymes., (Copyright © 2011 John Wiley & Sons, Ltd.)

Published

2011

21. Effects of CYP inhibitors on precocene I metabolism and toxicity in rat liver slices.

Author

Ly VT and Brock B

Subjects

Adenosine Triphosphate metabolism, Animals, Aspartate Aminotransferases metabolism, Benzopyrans pharmacology, Chromatography, High Pressure Liquid, Cytochrome P-450 Enzyme System metabolism, Ditiocarb pharmacology, Dose-Response Relationship, Drug, Drug Interactions, Enzyme Inhibitors metabolism, Glucuronides metabolism, Glutathione analogs & derivatives, Glutathione metabolism, Hydroxylation, Ketoconazole metabolism, Ketoconazole pharmacology, L-Lactate Dehydrogenase metabolism, Liver enzymology, Male, Mass Spectrometry, Molecular Structure, Necrosis chemically induced, Necrosis metabolism, Rats, Rats, Sprague-Dawley, Sulfaphenazole metabolism, Sulfaphenazole pharmacology, Tranylcypromine pharmacology, Triazoles metabolism, Triazoles pharmacology, Benzopyrans metabolism, Benzopyrans toxicity, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Liver drug effects, Liver metabolism

Abstract

We present a comprehensive in vitro approach to assessing metabolism-mediated hepatotoxicity using male Sprague-Dawley rat liver slices incubated with the well characterized hepatotoxicant, precocene I, and inhibitors of cytochrome P450 (CYP) enzymes. This approach combines liquid chromatography mass spectrometry (LC MS) detection methods with multiple toxicity endpoints to enable identification of critical metabolic pathways for hepatotoxicity. The incubations were performed in the absence and presence of the non-specific CYP inhibitor, 1-aminobenzotriazole (ABT) and isoform-specific inhibitors. The metabolite profile of precocene I in rat liver slices shares some features of the in vivo profile, but also had a major difference in that epoxide dihydrodiol hydrolysis products were not observed to a measurable extent. As examples of our liver slice metabolite identification procedure, a minor glutathione adduct and previously unreported 7-O-desmethyl and glucuronidated metabolites of precocene I are reported. Precocene I induced hepatocellular necrosis in a dose- and time-dependent manner. ABT decreased the toxicity of precocene I, increased exposure to parent compound, and decreased metabolite levels in a dose-dependent manner. Of the isoform-specific CYP inhibitors tested for an effect on the precocene I metabolite profile, only tranylcypromine was noticeably effective, indicating a role of CYPs 2A6, 2C9, 2Cl9, and 2E1. With respect to toxicity, the order of CYP inhibitor effectiveness was ABT>diethyldithiocarbamate∼tranylcypromine>ketoconazole. Furafylline and sulfaphenazole had no effect, while quinidine appeared to augment precocene I toxicity. These results suggest that rat liver slices do not reproduce the reported in vivo biotransformation of precocene I and therefore may not be an appropriate model for precocene I metabolism. However, these results provide an example of how small molecule manipulation of CYP activity in an in vitro model can be used to confirm metabolism-mediated toxicity., (Copyright © 2011 Elsevier Ireland Ltd. All rights reserved.)

Published

2011

22. Higher throughput human hepatocyte assays for the evaluation of time-dependent inhibition of CYP3A4.

Author

Li AP and Doshi U

Subjects

Adult, Cytochrome P-450 CYP3A, Drug Design, Enzyme Inhibitors administration & dosage, Erythromycin administration & dosage, Erythromycin pharmacology, Female, High-Throughput Screening Assays methods, Humans, Inhibitory Concentration 50, Ketoconazole administration & dosage, Ketoconazole pharmacology, Male, Middle Aged, Time Factors, Triazoles administration & dosage, Triazoles pharmacology, Young Adult, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Hepatocytes metabolism

Abstract

Time-dependent or mechanism-based CYP3A4 inhibition is an important adverse drug property that should be carefully managed during drug development. Evaluation of time-dependent inhibition is traditionally performed using liver microsomes or recombinant P450 isoforms. We report here higher throughput approaches to evaluate time-dependent CYP3A4 inhibition assay using cultured cryopreserved human hepatocytes. The assays were performed in human hepatocytes cultured in 96-well plates, with luciferin-IPA as the CYP3A4 specific substrate. The advantages of the approach are as follows: 1. The use of 96-well plates minimizes the quantity of human hepatocytes and test materials required for the assays. 2. The use of luciferin-IPA allows CYP3A4 activity to be quantified rapidly using a plate reader, thereby avoiding the need for LC/MS that is required for traditional substrates such as testosterone and midazolam. 3. The use of cultured (plated) hepatocytes allows effective removal of treatment medium and washing of the cells without the laborious centrifugation step that is required for hepatocytes in suspension. Two assays were developed: 1. IC(50) shift assay; and 2. enzyme kinetic assay. The IC-50 shift assay is intended for general screening purpose with which a time-dependent CYP3A4 inhibitor would be identified by an increase in inhibitory potency (quantified as a decrease in IC(50)) upon a 30 min. pre-incubation of hepatocytes with the inhibitor at 37 deg. C. Results with model inhibitors showed that the IC50 assay readily distinguished the time-dependent inhibitors (1-aminobenzotriazole, erythromycin) from the non-time-dependent inhibitor (ketoconazole). The enzyme kinetic assay is used for the derivation of the kinetic parameters K(I) and k(inact). With this assay, time and concentration dependent inhibition of CYP3A4 were observed for 1-aminobenzotriazole and erythromycin. With hepatocytes from 4 donors, K(I) and k(inact) values were calculated to be 22.0 to 70.7 uM, and 0.09 to 0.51 min(-1), respectively, for 1-aminobenzotriazole; and 47.3 to 75.1 uM, and 0.26 to 1.48, respectively, for erythromycin. DMSO (tested up to 2% v/v) was found to significantly attenuate the time-dependent inhibitory effects of 1-aminobenzotriazole, and had no apparent effects on erythromycin. Acetonitrile and methanol at 1% v/v had no significant effects. The higher throughput assays describe here can to be used routinely for the evaluation of time-dependent CYP3A4 inhibitory potential of drug candidates during early phases of drug development.

Published

2011

23. Enhancement of the drug susceptibility of a triclabendazole-resistant isolate of Fasciola hepatica using the metabolic inhibitor ketoconazole.

Author

Devine C, Brennan GP, Lanusse CE, Alvarez LI, Trudgett A, Hoey E, and Fairweather I

Subjects

Animals, Drug Synergism, Fasciola hepatica anatomy & histology, Microscopy, Electron, Scanning, Rats, Rats, Sprague-Dawley, Triclabendazole, Anthelmintics pharmacology, Benzimidazoles pharmacology, Drug Resistance, Enzyme Inhibitors pharmacology, Fasciola hepatica drug effects, Ketoconazole pharmacology

Abstract

A study has been carried out to investigate whether the action of triclabendazole (TCBZ) is altered by using the metabolic inhibitor, ketoconazole (KTZ) to inhibit the cytochrome P450 (CYP 450) system within Fasciola hepatica. The Oberon TCBZ-resistant and Cullompton TCBZ-susceptible isolates were used for these experiments. The CYP 450 enzyme system was inhibited by a 2 h pre-incubation in KTZ (40 microM). Flukes were then incubated for a further 22 h in NCTC medium containing either KTZ; KTZ + nicotinamide adenine dinucleotide phosphate (NADPH; 1 nM); KTZ + NADPH + TCBZ (15 microg/ml); or KTZ + NADPH + triclabendazole sulphoxide (TCBZ.SO;15 microg/ml). Morphological changes resulting from drug treatment and following metabolic inhibition were assessed using scanning electron microscopy. After treatment with either TCBZ or TCBZ.SO alone, there was greater disruption to the TCBZ-susceptible isolate than the TCBZ-resistant isolate. However, co-incubation with KTZ and TCBZ/TCBZ.SO led to more severe surface changes to the TCBZ-resistant isolate than with each drug on its own, with greater swelling and blebbing of the tegument and even the loss of the apical plasma membrane in places. With the Cullompton isolate, there was limited potentiation of drug action in combination with KTZ, and only with TCBZ.SO. The results support the concept of altered drug metabolism within TCBZ-resistant isolates and indicate that this process may play a role in the development of drug resistance.

Published

2010

24. Structural basis of human CYP51 inhibition by antifungal azoles.

Author

Strushkevich N, Usanov SA, and Park HW

Subjects

Bacterial Proteins chemistry, Catalytic Domain, Crystallography, X-Ray, Econazole chemistry, Econazole metabolism, Enzyme Inhibitors metabolism, Humans, Ketoconazole chemistry, Ketoconazole metabolism, Models, Molecular, Molecular Structure, Protein Binding, Protein Conformation, Protein Structure, Tertiary, Sterol 14-Demethylase, Cytochrome P-450 Enzyme Inhibitors, Cytochrome P-450 Enzyme System chemistry, Econazole pharmacology, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology

Abstract

The obligatory step in sterol biosynthesis in eukaryotes is demethylation of sterol precursors at the C14-position, which is catalyzed by CYP51 (sterol 14-alpha demethylase) in three sequential reactions. In mammals, the final product of the pathway is cholesterol, while important intermediates, meiosis-activating sterols, are produced by CYP51. Three crystal structures of human CYP51, ligand-free and complexed with antifungal drugs ketoconazole and econazole, were determined, allowing analysis of the molecular basis for functional conservation within the CYP51 family. Azole binding occurs mostly through hydrophobic interactions with conservative residues of the active site. The substantial conformational changes in the B' helix and F-G loop regions are induced upon ligand binding, consistent with the membrane nature of the protein and its substrate. The access channel is typical for mammalian sterol-metabolizing P450 enzymes, but is different from that observed in Mycobacterium tuberculosis CYP51. Comparison of the azole-bound structures provides insight into the relative binding affinities of human and bacterial P450 enzymes to ketoconazole and fluconazole, which can be useful for the rational design of antifungal compounds and specific modulators of human CYP51., ((c) 2010 Elsevier Ltd. All rights reserved.)

Published

2010

25. Testosterone hydroxylation in bovine liver: enzyme kinetic and inhibition study.

Author

Pegolo S, Giantin M, Dacasto M, Montesissa C, and Capolongo F

Subjects

Animals, Antibodies pharmacology, Aryl Hydrocarbon Hydroxylases antagonists & inhibitors, Aryl Hydrocarbon Hydroxylases metabolism, Blotting, Western, Chromatography, High Pressure Liquid, Cytochrome P-450 CYP3A immunology, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors, Hydroxylation, Ketoconazole pharmacology, Kinetics, Peptide Fragments immunology, Steroid Hydroxylases antagonists & inhibitors, Steroid Hydroxylases metabolism, Cattle metabolism, Enzyme Inhibitors pharmacology, Liver enzymology, Testosterone metabolism

Abstract

In order to sort out the involvement of cytochrome P450 (CYP) 3A and possibly CYP2B in testosterone hydroxylation in cattle, enzyme kinetic and inhibition studies were performed. Most relevant kinetic constants (Km and Vmax) for 6beta-, 16beta- and 2beta-testosterone hydroxylase (OHT) activities were determined and accounted for 93.4 +/- 13.8, 36.4 +/- 6.1 and 110.8 +/- 15.2 muM, respectively, for Km and 0.558 +/- 0.03, 0.280 +/- 0.013, and 0.338 +/- 0.017 nmol min-1 mg-1 protein, respectively, for Vmax. Eadie-Hofstee plot analysis pointed out how these enzymatic activities in cattle follow a monophasic kinetic pattern. Preliminary inhibition studies conducted with the CYP3A inhibitor ketoconazole and the CYP2B inhibitors orphenadrine and 9-ethynylphenanthrene seemed to suggest the major involvement of CYP3A in testosterone hydroxylation in cattle. Immuno-inhibition studies with an anti-peptide antibody against bovine CYP3A4 confirmed the predominant role of CYP3A in testosterone hydroxylation in bovine liver, proving the usefulness of anti-peptide antibodies in defining the contribution of specific P450 isoforms in drug metabolism in veterinary species.

Published

2010

26. The effects of ketoconazole and rifampicin on the pharmacokinetics of mirodenafil in healthy Korean male volunteers: an open-label, one-sequence, three-period, three-treatment crossover study.

Author

Shin KH, Kim BH, Kim TE, Kim JW, Yi S, Yoon SH, Cho JY, Shin SG, Jang IJ, and Yu KS

Subjects

Adult, Asian People, Biological Availability, Biotransformation, Chromatography, Liquid, Cross-Over Studies, Cytochrome P-450 CYP3A biosynthesis, Drug Interactions, Enzyme Induction, Enzyme Inhibitors administration & dosage, Humans, Ketoconazole administration & dosage, Korea, Male, Phosphodiesterase Inhibitors administration & dosage, Phosphodiesterase Inhibitors adverse effects, Phosphodiesterase Inhibitors blood, Pyrimidinones administration & dosage, Pyrimidinones adverse effects, Pyrimidinones blood, Rifampin administration & dosage, Sulfonamides administration & dosage, Sulfonamides adverse effects, Sulfonamides blood, Tandem Mass Spectrometry, Young Adult, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Phosphodiesterase 5 Inhibitors, Phosphodiesterase Inhibitors pharmacokinetics, Pyrimidinones pharmacokinetics, Rifampin pharmacology, Sulfonamides pharmacokinetics

Abstract

Background: Mirodenafil, a phosphodiesterase 5 inhibitor reported to be effective in the treatment of erectile dysfunction, is metabolized by cytochrome P450 (CYP) 3A4 to the active metabolite N-dehydroxyethyl mirodenafil. Mirodenafil may have drug-drug interactions with ketoconazole and/or rifampicin., Objective: The aim of this study was to investigate the effects of a potent inhibitor (ketoconazole) and inducer (rifampicin) of the CYP3A4 isozyme on the pharmacokinetics of mirodenafil to meet the regulatory requirements for the marketing of mirodenafil in Korea., Methods: An open-label, 1-sequence, 3-period, 3-treatment crossover study was conducted over 22 days in healthy Korean male volunteers. Each subject received 100 mg of mirodenafil in each of 3 study periods: mirodenafil alone (period 1); mirodenafil after pretreatment with ketoconazole 400 mg once daily for 3 days (period 2); and mirodenafil after pretreatment with rifampicin 600 mg once daily for 10 days (period 3). Serial blood samples were collected for pharmacokinetic analysis after the administration of mirodenafil in each study period. Plasma concentration-time data for mirodenafil and its major metabolite, N-dehydroxyethyl mirodenafil, were determined using LC-MS/MS and analyzed by a noncompartmental method. The results for mirodenafil coadministration with either ketoconazole or rifampicin were compared with those for mirodenafil alone. Adverse events (AEs) were identified by asking general health-related questions of the subjects, by physical examination, and by subject self-report throughout the study period., Results: Nineteen subjects were enrolled (mean [SD] age, 23.2 [2.76] years [range, 19-29 years]; weight, 69.3 [6.50] kg [range, 61.0-84.0 kg]; body mass index, 22.4 [1.77] kg/m(2) [range, 20.0-26.0 kg/m(2)]) and 18 subjects completed the study. One subject discontinued the study due to protocol violation and was replaced. The AUC(0-infinity) of mirodenafil increased 5.04-fold (90% CI, 3.78-6.72) and the metabolic ratio decreased 0.21-fold after pretreatment with ketoconazole compared with mirodenafil alone. After pretreatment with rifampicin, the AUC(0-infinity) of mirodenafil decreased 0.03-fold (90% CI, 0.02-0.05) and the metabolic ratio increased 2.9-fold. Twelve cases of headache, 6 of nasal congestion, 2 of feeling hot, 2 of epistaxis, and 1 each of dizziness, nausea, and somnolence were considered to be related to administration of mirodenafil. Twenty-eight AEs were reported in period 2 (in 68.4% of subjects), during which systemic exposure to mirodenafil was highest, whereas 7 AEs were reported in period 1 (in 31.6% of subjects) and 5 AEs in period 3 (in 16.7% of subjects)., Conclusion: In these healthy Korean male volunteers, the coadministration of ketoconazole and rifampicin resulted in significant changes in systemic exposure to mirodenafil., (Copyright 2009 Excerpta Medica Inc. All rights reserved.)

Published

2009

27. In vitro antimalarial interactions between mefloquine and cytochrome P450 inhibitors.

Author

Wisedpanichkij R, Chaijaroenkul W, Sangsuwan P, Tantisawat J, Boonprasert K, and Na-Bangchang K

Subjects

Animals, Cytochrome P-450 Enzyme Inhibitors, Drug Synergism, Humans, Inhibitory Concentration 50, Antimalarials pharmacology, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Mefloquine pharmacology, Plasmodium falciparum drug effects, Quinidine pharmacology

Abstract

The treatment and control of malaria is becoming increasingly difficult due to resistance of Plasmodium falciparum strains resistance to commonly used antimalarials. Combination therapy is currently the strategy for combating multi-drug resistant falciparum malaria, through exploiting phamacodynamic synergistic effect and delaying the emergence of drug resistance. The objective of the present study was to investigate antimalarial activity of inhibitors of cytochrome P450 (CYP) enzyme including their interactions with the antimalarial mefloquine against chloroquine-resistant (K1) and chloroquine-sensitive (3D7) P. falciparum clones in vitro. Results showed IC(50) (drug concentration which produces 50% schizont maturation inhibition) values [mean (range)] of mefloquine against K1 and 3D7 clones to be 8.6 (8.0-9.3) and 12.1 (10.5-13.8) nM, respectively. The corresponding values for the IC(50) of quinidine were 32.2 (31.9-32.5) and 28.7 (28.4-29.0) nM, and for ketoconazole were 3.9 (3.7-4.1) and 4.8 (4.6-5.1) microM, respectively. Analysis of isobologram revealed a trend of decreasing of fraction IC(50) (FIC), which indicates synergistics of the either quinidine or ketoconazole with mefloquine for both chloroquine-resistant and chloroquine-sensitive clones.

Published

2009

28. Synthesis and biochemical evaluation of a range of sulfonated derivatives of 4-hydroxybenzyl imidazole as highly potent inhibitors of rat testicular 17alpha-hydroxylase/17,20-lyase (P-450(17alpha)).

Author

Ahmed S, Shahid I, Dhanani S, and Owen CP

Subjects

Animals, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Imidazoles chemistry, Imidazoles pharmacology, Ketoconazole pharmacology, Male, Rats, Steroid 17-alpha-Hydroxylase metabolism, Sulfones chemistry, Enzyme Inhibitors chemical synthesis, Imidazoles chemical synthesis, Steroid 17-alpha-Hydroxylase antagonists & inhibitors, Testis enzymology

Abstract

We report the synthesis and biochemical evaluation of a range of 4-sulfonated derivatives of 4-hydroxybenzyl imidazole which has been targetted against the two components of 17alpha-hydroxylase/17,20-lyase (P-450(17alpha)), namely, 17alpha-hydroxylase (17alpha-OHase) and 17,20-lyase (lyase). The results from the biochemical testing suggest that the compounds synthesised are highly potent inhibitors possessing excellent selectivity towards the lyase component.

Published

2009

29. Curcumin modulates efflux mediated by yeast ABC multidrug transporters and is synergistic with antifungals.

Author

Sharma M, Manoharlal R, Shukla S, Puri N, Prasad T, Ambudkar SV, and Prasad R

Subjects

Anisomycin pharmacology, Candida albicans metabolism, Cycloheximide pharmacology, Drug Synergism, Fluconazole pharmacology, Itraconazole pharmacology, Ketoconazole pharmacology, Methotrexate metabolism, Miconazole pharmacology, Pyrimidines pharmacology, Rhodamines metabolism, Saccharomyces cerevisiae metabolism, Triazoles pharmacology, Voriconazole, Antifungal Agents pharmacology, Biological Transport drug effects, Curcumin pharmacology, Enzyme Inhibitors pharmacology, Multidrug Resistance-Associated Proteins metabolism, Saccharomyces cerevisiae drug effects

Abstract

Curcumin (CUR), a natural product of turmeric, from rhizomes of Curcuma longa, is a known agent of reversal of drug resistance phenotypes in cancer cells overexpressing ATP-binding cassette (ABC) transporters, viz., ABCB1, ABCG2, and ABCC1. In the present study, we evaluated whether CUR could also modulate multidrug transporters of yeasts that belong either to the ABC family or to the major facilitator superfamily (MFS). The effect of CUR on multidrug transporter proteins was demonstrated by examining rhodamine 6G (R6G) efflux in Saccharomyces cerevisiae cells overexpressing the Candida albicans ABC transporters Cdr1p and Cdr2p (CaCdr1p and CaCdr2p, respectively) and the MFS transporters CaMdr1p and S. cerevisiae Pdr5p. CUR decreased the extracellular concentration of R6G in ABC transporter-expressing cells but had no effect on methotrexate efflux mediated through the MFS transporter CaMdr1p. CUR competitively inhibited R6G efflux and the photolabeling of CaCdr1p by [(125)I]iodoarylazidoprazosin, a drug analogue of the substrate prazosin (50% inhibitory concentration, 14.2 microM). Notably, the mutant variants of CaCdr1p that displayed abrogated efflux of R6G also showed reduced modulation by CUR. Drug susceptibility testing of ABC protein-expressing cells by spot assays and checkerboard tests revealed that CUR was selectively synergistic with drug substrates such as R6G, ketoconazole, itraconazole, and miconazole but not with fluconazole, voriconazole, anisomycin, cycloheximide, or FK520. Taken together, our results provide the first evidence that CUR modulates only ABC multidrug transporters and could be exploited in combination with certain conventional antifungal drugs to reverse multidrug resistance in Candida cells.

Published

2009

30. Revisiting the metabolism of ketoconazole using accurate mass.

Author

Fitch WL, Tran T, Young M, Liu L, and Chen Y

Subjects

Animals, Biotransformation, Chromatography, Liquid, Cytochrome P-450 CYP3A Inhibitors, Cytochrome P-450 Enzyme Inhibitors, Deuterium Exchange Measurement, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Humans, Ketoconazole chemistry, Ketoconazole pharmacology, Liver drug effects, Male, Molecular Structure, Molecular Weight, Rats, Tandem Mass Spectrometry, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 Enzyme System metabolism, Enzyme Inhibitors metabolism, Ketoconazole metabolism, Liver enzymology

Abstract

The microsomal metabolism of ketoconazole is revisited using accurate mass LC/MS(n) and deuterium labelling. Structures for sixteen metabolites are proposed from rat and human microsomal metabolism of commercial ketoconazole. Thirteen of the proposed structures are well determined and consistent with all data; five of the proposed structures are less certain. Ten of the metabolites are described for the first time. Reaction phenotyping shows that most of the metabolites arise from CYP3A4, the enzyme known to be well inhibited by ketoconazole.

Published

2009

31. In vitro inhibition of CYP3A4 by herbal remedies frequently used by cancer patients.

Author

Engdal S and Nilsen OG

Subjects

Agaricus, Chromatography, High Pressure Liquid, Cytochrome P-450 CYP3A, Herbal Medicine, Humans, Ketoconazole pharmacology, Tea adverse effects, Testosterone metabolism, Viscum album adverse effects, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors, Plant Extracts adverse effects

Abstract

The herbal remedies Natto K2, Agaricus, mistletoe, noni juice, green tea and garlic, frequently used by cancer patients, were investigated for their in vitro inhibition potential of cytochrome P-450 3A4 (CYP3A4) metabolism. To our knowledge, only garlic and green tea had available data on the possible inhibition of CYP3A4 metabolism. Metabolic studies were performed with human c-DNA baculovirus expressed CYP3A4. Testosterone was used as a substrate and ketoconazole as a positive quantitative inhibition control. The formation of 6-beta-OH-testosterone was quantified by a validated HPLC methodology. Green tea was the most potent inhibitor of CYP3A4 metabolism (IC(50): 73 microg/mL), followed by Agaricus, mistletoe and noni juice (1324, 3594, >10 000 microg/mL, respectively). All IC(50) values were high compared with those determined for crude extracts of other herbal remedies. The IC(50)/IC(25) ratios for the inhibiting herbal remedies ranged from 2.15 to 2.67, indicating similar inhibition profiles of the herbal inhibitors of CYP3A4. Garlic and Natto K2 were classified as non-inhibitors. Although Agaricus, noni juice, mistletoe and green tea inhibited CYP3A4 metabolism in vitro, clinically relevant systemic or intestinal interactions with CYP3A4 were considered unlikely, except for a probable inhibition of intestinal CYP3A4 by the green tea product., (Copyright 2009 John Wiley & Sons, Ltd.)

Published

2009

32. An inhibition study of beauvericin on human and rat cytochrome P450 enzymes and its pharmacokinetics in rats.

Author

Mei L, Zhang L, and Dai R

Subjects

Administration, Oral, Animals, Antifungal Agents administration & dosage, Antifungal Agents pharmacokinetics, Antifungal Agents pharmacology, Chromatography, High Pressure Liquid, Cytochrome P-450 Enzyme System metabolism, Depsipeptides administration & dosage, Dose-Response Relationship, Drug, Enzyme Inhibitors administration & dosage, Humans, Inhibitory Concentration 50, Ketoconazole administration & dosage, Ketoconazole pharmacokinetics, Ketoconazole pharmacology, Mass Spectrometry, Microsomes, Liver drug effects, Microsomes, Liver enzymology, Microsomes, Liver metabolism, Rats, Rats, Sprague-Dawley, Substrate Specificity, Cytochrome P-450 Enzyme Inhibitors, Depsipeptides pharmacokinetics, Depsipeptides pharmacology, Enzyme Inhibitors pharmacokinetics, Enzyme Inhibitors pharmacology

Abstract

Beauvericin is a secondary metabolite natural product from microorganisms and has been shown to have a new potential antifungal activity. In this study, the metabolism and inhibition of beauvericin in human liver microsomes (HLM) and rat liver microsomes (RLM) were investigated. The apparent K(m) and V(max) of beauvericin in HLM were determined by substrate depletion approach and its inhibitory effects on cytochromes P450 (CYP) activities were evaluated using probe substrates, with IC(50) and the (K(i)) values were 1.2 microM (0.5 microM) and 1.3 microM (1.9 microM), respectively for CYP3A4/5 (midazolam) and CYP2C19 (mephenytoin). Similarly, beauvericin was also a potent inhibitor for CYP3A1/2 (IC(50): 1.3 microM) in RLM. Furthermore, the pharmacokinetics of beauvericin in the rat were studied after p.o administration alone and co-administration with ketoconazole, which indicated a pharmacodynamic function may play a role in the synergistic effect on antifungal activity.

Published

2009

33. Effect of ketoconazole on the pharmacokinetic profile of ambrisentan.

Author

Richards DB, Walker GA, Mandagere A, Magee MH, and Henderson LS

Subjects

Adolescent, Adult, Antifungal Agents adverse effects, Cytochrome P-450 CYP3A Inhibitors, Drug Interactions, Enzyme Inhibitors adverse effects, Humans, Ketoconazole adverse effects, Male, Middle Aged, Phenylpropionates adverse effects, Phenylpropionates metabolism, Pyridazines adverse effects, Pyridazines metabolism, Antifungal Agents pharmacology, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Phenylpropionates pharmacokinetics, Pyridazines pharmacokinetics

Abstract

Ambrisentan is an endothelin type A (ET(A))-selective receptor antagonist that is metabolized primarily by glucuronidation but also undergoes oxidative metabolism by CYP3A4. The potential for ketoconazole, the archetypal strong inhibitor of CYP3A4, to alter the pharmacokinetic profile of ambrisentan and its oxidative metabolite, 4-hydroxymethyl ambrisentan, was assessed in an open-label, nonrandomized, 2-period, single-sequence study in 16 healthy men. Participants received a single dose of ambrisentan 10 mg alone and after 4 days of ketoconazole 400 mg administered once daily. In the presence of multiple doses of ketoconazole, single-dose ambrisentan AUC(0-infinity) estimate was increased by 35.3%, whereas C(max) was increased by 20.0%. For the 4-hydroxymethyl ambrisentan metabolite, AUC(0-infinity) estimate was decreased by 4.0%, whereas C(max) was decreased by 16.5%. Concomitant administration of ambrisentan and ketoconazole was well tolerated. In summary, ketoconazole had no clinically significant effect on the pharmacokinetics or safety profile of ambrisentan; therefore, no changes in ambrisentan dose should be necessary when the drug is administered concomitantly with known CYP3A4 inhibitors.

Published

2009

34. CYP1A1 induction and CYP3A4 inhibition by the fungicide imazalil in the human intestinal Caco-2 cells-comparison with other conazole pesticides.

Author

Sergent T, Dupont I, Jassogne C, Ribonnet L, van der Heiden E, Scippo ML, Muller M, McAlister D, Pussemier L, Larondelle Y, and Schneider YJ

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, ATP Binding Cassette Transporter, Subfamily G, Member 2, ATP-Binding Cassette Transporters antagonists & inhibitors, ATP-Binding Cassette Transporters metabolism, Antifungal Agents pharmacology, Caco-2 Cells, Calcitriol pharmacology, Chromatography, High Pressure Liquid, Cytochrome P-450 CYP3A metabolism, Dose-Response Relationship, Drug, Drug Interactions, Enzyme Induction, Enzyme Inhibitors toxicity, Fungicides, Industrial toxicity, Glutathione Transferase metabolism, Humans, Imidazoles toxicity, Intestinal Mucosa enzymology, Ketoconazole pharmacology, Kinetics, Multidrug Resistance-Associated Protein 2, Multidrug Resistance-Associated Proteins antagonists & inhibitors, Multidrug Resistance-Associated Proteins metabolism, Neoplasm Proteins antagonists & inhibitors, Neoplasm Proteins metabolism, Polychlorinated Dibenzodioxins pharmacology, RNA, Messenger biosynthesis, Receptors, Aryl Hydrocarbon drug effects, Spectrophotometry, Ultraviolet, Triazoles pharmacology, Cytochrome P-450 CYP1A1 biosynthesis, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Food Contamination, Fungicides, Industrial pharmacology, Imidazoles pharmacology, Intestinal Mucosa drug effects

Abstract

Imazalil (IMA) is a widely used imidazole-antifungal pesticide and, therefore, a food contaminant. This compound is also used as a drug (enilconazole). As intestine is the first site of exposure to ingested drugs and pollutants, we have investigated the effects of IMA, at realistic intestinal concentrations, on xenobiotic-metabolizing enzymes and efflux pumps by using Caco-2 cells, as a validated in vitro model of the human intestinal absorptive epithelium. For comparison, other conazole fungicides, i.e. ketoconazole, propiconazole and tebuconazole, were also studied. IMA induced cytochrome P450 (CYP) 1A1 activity to the same extent as benzo(a)pyrene (B(a)P) or 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD), in a dose- and time-dependent manner. Cell-free aryl hydrocarbon receptor (AhR) binding assay and reporter gene assay suggested that IMA is not an AhR-ligand, implying that IMA-mediated induction should involve an AhR-independent pathway. Moreover, IMA strongly inhibited the CYP3A4 activity in 1,25-vitamin D(3)-induced Caco-2 cells. The other fungicides had weak or nil effects on CYP activities. Study of the apical efflux pump activities revealed that ketoconazole inhibited both P-glycoprotein (Pgp) and multidrug resistance-associated protein 2 (MRP-2) or breast cancer resistance protein (BCRP), whereas IMA and other fungicides did not. Our results imply that coingestion of IMA-contaminated food and CYP3A4- or CYP1A1-metabolizable drugs or chemicals could lead to drug bioavailability modulation or toxicological interactions, with possible adverse effects for human health.

Published

2009

35. The combination of chemical and antibody inhibitors for superior P450 3A inhibition in reaction phenotyping studies.

Author

Rock DA, Foti RS, and Pearson JT

Subjects

Antibodies, Monoclonal immunology, Area Under Curve, Cytochrome P-450 CYP3A immunology, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 Enzyme Inhibitors, Cytochrome P-450 Enzyme System metabolism, Drug Interactions, Humans, Hydroxytestosterones metabolism, Ketoconazole pharmacology, Microsomes, Liver drug effects, Midazolam analogs & derivatives, Midazolam metabolism, Protein Isoforms antagonists & inhibitors, Protein Isoforms metabolism, Testosterone analogs & derivatives, Testosterone metabolism, Antibodies, Monoclonal pharmacology, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Microsomes, Liver enzymology

Abstract

Cytochrome P450 (P450) reaction phenotyping is a key process toward accurately determining the contribution of different P450s to the metabolism of new chemical entities. The significance of P450s to drug disposition has led to the identification of selective chemical and antibody inhibitors for individual P450 enzymes. Despite these advances, the maximal inhibition attainable is limited by the use of inhibitor concentrations that maintain selectivity for the individual P450s. Thus, most commercially available inhibitors produce a maximal inhibition of approximately 80%. Herein, the combination of chemical plus antibody inhibitors is explored to find whether P450 3A could be selectively and completely (>99%) inhibited by using both inhibitors simultaneously.

Published

2008

36. Human CYP3A4-introduced HepG2 cells: in vitro screening system of new chemicals for the evaluation of CYP3A4-inhibiting activity.

Author

Araki N, Tsuruoka S, Wang N, Hasegawa G, Yanagihara H, Ando H, Omasa T, Enosawa S, Nagai H, and Fujimura A

Subjects

Ammonia metabolism, Animals, Atorvastatin, Cricetinae, Cytochrome P-450 CYP3A metabolism, Drug Evaluation, Preclinical, Enzyme Inhibitors metabolism, Glutamate-Ammonia Ligase metabolism, Heptanoic Acids metabolism, Heptanoic Acids pharmacology, Humans, Ketoconazole metabolism, Ketoconazole pharmacology, Lidocaine metabolism, Lidocaine pharmacology, Nifedipine metabolism, Nifedipine pharmacology, Pyrroles metabolism, Pyrroles pharmacology, Cell Line, Tumor, Cytochrome P-450 CYP3A genetics, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology

Abstract

1. The aims were to attest whether HepG2-GS-3A4, a cell line into which the human CYP3A4 gene was introduced, can be used for a screening of chemicals that will inhibit CYP3A4 activity. 2. The capacity of the cells for metabolizing CYP3A4 substrates in vitro was evaluated. Also determined was the effect of CYP3A4 inhibitors and non-inhibitors on nifedipine hydroxylation. Western blot, immunohistochemostry and determination of beta-nicotinamide adenine dinucleotide phosphate (NADPH)-reductase activity were performed. 3. HepG2-GS-3A4 selectively metabolized substrates of CYP3A4 (diazepam, nordiazepam, lidocaine, atorvastatin, and nifedipine) to a greater degree than control. The metabolites were easily detected in the culture medium. Values of V(max) of HepG2-GS-3A4 were about 30- to 100-fold higher than those of the control, while values of K(m) were comparable. Pre-incubation of cimetidine and ketoconazole significantly inhibited nifedipine hydroxylation, while addition of inhibitors specific to other isoforms of CYPs had no substantial effect. The HepG2-GS-3A4 expressed a higher amount of CYP3A4 protein and mRNA than control. Most NADPH reductase activity was detected in microsomal fractions. 4 In conclusion, HepG2-GS-3A4 sufficiently and selectively metabolize substrates of CYP3A4, and inhibitors of CYP3A4 reduced the metabolism. Because the metabolites were easily detected in the culture medium, this cell might be useful for the new and easy screening of new drugs for the evaluation of CYP3A4-inhibiting activity in vitro.

Published

2008

37. Microsome biocolloids for rapid drug metabolism and inhibition assessment by LC-MS.

Author

Bajrami B, Krishnan S, and Rusling JF

Subjects

Animals, Chromatography, Liquid methods, Colloids chemistry, Cytochrome P-450 CYP2E1 Inhibitors, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors administration & dosage, Fomepizole, Inhibitory Concentration 50, Ketoconazole administration & dosage, Ketoconazole pharmacology, Microsomes, Liver enzymology, Microsomes, Liver metabolism, Nanoparticles, Pyrazoles administration & dosage, Pyrazoles pharmacology, Rats, Tandem Mass Spectrometry methods, Cytochrome P-450 CYP2E1 metabolism, Cytochrome P-450 CYP3A metabolism, Enzyme Inhibitors pharmacology, Nitroso Compounds metabolism

Abstract

Rat liver microsomes attached to nanoparticles were used for LC-MS studies of CYP3A and 2E1 enzymes in metabolism of N-nitroso compounds. Using these biocolloids, turnover rates were measured within 2 min. Inhibitor IC(50) values for ketoconazole (KET) and 4-methylpyrazole (4-MEP) were estimated.

Published

2008

38. Effects of ketoconazole and quinidine on pharmacokinetics of pactimibe and its plasma metabolite, R-125528, in humans.

Author

Kotsuma M, Tokui T, Freudenthaler S, and Nishimura K

Subjects

Adult, Alkanes blood, Area Under Curve, Cross-Over Studies, Dose-Response Relationship, Drug, Double-Blind Method, Drug Interactions, Enzyme Inhibitors blood, Humans, Indoleacetic Acids blood, Indoles blood, Male, Placebos, Sensitivity and Specificity, Alkanes pharmacokinetics, Enzyme Inhibitors pharmacokinetics, Indoleacetic Acids pharmacokinetics, Indoles pharmacokinetics, Ketoconazole pharmacology, Quinidine pharmacology

Abstract

Pactimibe sulfate is a novel acyl coenzyme A:cholesterol acyltransferase inhibitor developed for the treatment of hypercholesterolemia and atherosclerotic diseases. Pactimibe has two equally dominant clearance pathways forming R-125528 by CYP3A4 and M-1 by CYP2D6 in vitro. R-125528 is a plasma metabolite and is cleared solely by CYP2D6 despite its acidity. To evaluate contributions of the cytochrome P450 enzymes on the pharmacokinetics of pactimibe and R-125528 in humans, drug-drug interaction studies using ketoconazole and quinidine were conducted. Eighteen healthy male subjects were given a single dose of pactimibe sulfate without and with 400 mg of ketoconazole (q.d.). With the concomitant treatment, the area under the plasma concentration-time curve (AUC(0-inf)) of pactimibe modestly increased 1.7-fold and AUC(0-tz) of R-125528 decreased by 55%. In addition, 17 healthy male subjects were given a single dose of pactimibe sulfate without and with 600 mg of quinidine (b.i.d.). With the concomitant treatment, the AUC(0-inf) for pactimibe modestly increased 1.7-fold. On the other hand, the AUC(0-tz) of R-125528 was markedly elevated 5.0-fold, although the AUC(0-inf) could not be adequately defined because the terminal elimination phase of R-125528 was not obtained in the study period up to 72 h. As the f(m CYP3A4) and f(m CYP2D6) values of pactimibe estimated from in vitro studies were 0.40 and 0.33, respectively, AUC increase ratios of pactimibe were estimated to be 1.7 with ketoconazole and 1.5 with quinidine. These values were well in accordance with the values observed in this study. Moreover, the f(m CYP2D6) of R-125528 estimated to be almost 1 would well explain the accumulation of R-125528 observed with the quinidine treatment.

Published

2008

39. Validation and application of Caco-2 assays for the in vitro evaluation of development candidate drugs as substrates or inhibitors of P-glycoprotein to support regulatory submissions.

Author

Elsby R, Surry DD, Smith VN, and Gray AJ

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Caco-2 Cells cytology, Drug Approval, Drug Evaluation, Preclinical methods, Humans, United States, United States Food and Drug Administration, ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, Antifungal Agents pharmacology, Biological Assay methods, Caco-2 Cells metabolism, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Quinidine pharmacology

Abstract

1. An understanding of the role that transporters, in particular P-glycoprotein (P-gp), can play in the absorption, distribution, metabolism and excretion (ADME) of candidate drugs, and an assessment of how these processes might impact on toxicity and the potential for drug-drug interactions in the clinic, is required to support drug development and registration. It is therefore necessary to validate preclinical assays for the in vitro evaluation of candidate drugs as substrates or inhibitors of human P-gp. 2. The present study has characterized a Caco-2 cell monolayer model by determining the bi-directional apparent permeabilities and efflux ratios of the known P-gp substrates ([(3)H]-digoxin, [(3)H]-ketoconazole, [(3)H]-verapamil, [(3)H]-quinidine, dipyridamole and loratidine; 1-100 microM) a non-substrate ([(3)H]-propranolol; 10 microM), or by determining the inhibitory potencies (IC(50)) of inhibitors (verapamil, ketoconazole, quinidine, dipyridamole and probenecid; 0.1-100 microM) on the basolateral-to-apical transport of [(3)H]-digoxin (5 microM), in order to validate methodologies for the identification of substrates or inhibitors of P-gp, respectively. 3. The reproducibility of the [(3)H]-digoxin or verapamil data determined from replicate monolayers across different cell passages indicates that the functional expression of P-gp is consistent across the range of passages (25-40) utilized for transport experiments and that the determination of bi-directional apparent permeability, or IC(50) for inhibition of P-gp, respectively, need only be performed on one occasion for a test compound. [(3)H]-digoxin and [(3)H]-propranolol or verapamil and probenecid were considered to be appropriate positive and negative controls of P-gp-mediated transport, or inhibition of P-gp, respectively, to ensure performance of the assays when assessing candidate drugs. Additionally, the low IC(50) values determined for ketoconazole and quinidine indicated that these inhibitors were suitable to use to confirm the role of P-gp in the efflux of a test compound. 4. These validated Caco-2 assays are robust, reproducible and suitable for routine in vitro evaluation of candidate drugs. They have been successfully applied to development projects resulting in the identification of two candidate drugs as substrates and inhibitors of P-gp, whereas a third was neither a substrate nor an inhibitor of this transporter.

Published

2008

40. Synthesis, biochemical evaluation and rationalisation of the inhibitory activity of a range of phenyl alkyl imidazole-based compounds as potent inhibitors of the enzyme complex 17alpha-hydroxylase/17,20-lyase (P450(17alpha)).

Author

Owen CP, Shahid I, Olusanjo MS, Patel CH, Dhanani S, and Ahmed S

Subjects

17-Hydroxysteroid Dehydrogenases chemistry, 17-Hydroxysteroid Dehydrogenases metabolism, Enzyme Inhibitors chemistry, Imidazoles chemistry, Inhibitory Concentration 50, Isoenzymes chemistry, Isoenzymes metabolism, Ketoconazole pharmacology, Molecular Structure, Structure-Activity Relationship, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Imidazoles chemical synthesis, Imidazoles pharmacology, Mixed Function Oxygenases antagonists & inhibitors, Rationalization, Steroid 17-alpha-Hydroxylase antagonists & inhibitors

Abstract

The cytochrome P450 enzyme, 17alpha-hydroxylase/17,20-lyase (P450(17alpha)), is a potential target in hormone-dependent cancers. We report the synthesis, biochemical evaluation and rationalisation of the inhibitory activity of a number of azole-based compounds as inhibitors of the two components of P450(17alpha), i.e., 17alpha-hydroxylase (17alpha-OHase) and 17,20-lyase (lyase). The results suggest that the imidazole-based compounds are highly potent inhibitors of both components, with N-7-phenyl heptyl imidazole (21) (IC(50)=0.32 microM against 17alpha-OHase and IC(50)=0.10 microM against lyase) and N-8-phenyl octyl imidazole (23) (IC(50)=0.25 microM against 17alpha-OHase and IC(50)=0.21 microM against lyase) being the two most potent compounds within the current study, in comparison to ketoconazole (KTZ) (IC(50)=3.76 microM against 17alpha-OHase and IC(50)=1.66 microM against lyase). Furthermore, consideration of the inhibitory activity against the two components show that the compounds tested are less potent towards the 17alpha-OHase component, a desirable property in the development of novel inhibitors of P450(17alpha). Structure-activity relationship determination of the range of compounds synthesised suggests that logP (log of the partition coefficient) is a key physicochemical factor in determining the overall inhibitory activity. In an effort to determine the viability of these compounds becoming potential drug candidates as well as to show specificity of these compounds, we undertook the biochemical evaluation of the synthesised compounds against two isozymes of 17beta-hydroxysteroid dehydrogenase [namely type 1 (17beta-HSD1) and type 3 (17beta-HSD3)] and 3beta-hydroxysteroid dehydrogenase (3beta-HSD). Consideration of the inhibitory activity possessed by the compounds considered within the current study against 3beta-HSD, 17beta-HSD1 and 17beta-HSD3 shows that there is no clear structure-activity relationship and that the compounds appear to possess similar inhibitory activity against both 3beta-HSD and 17beta-HSD3 whilst against 17beta-HSD1, the compounds appear to possess poor inhibitory activity at [I]=100 microM. Indeed, two of the most potent inhibitors of P450(17alpha), (compounds 21 and 23), were found to possess relatively good levels of inhibition against the three enzymes-compound 21 was found to possess approximately 32%, approximately 21% and approximately 37% inhibition whilst compound 23 was found to possess approximately 38%, approximately 30% and approximately 28% inhibition against 3beta-HSD, 17beta-HSD1 and 17beta-HSD3 respectively. We therefore concluded that the azole-based compounds synthesised within the current study are not suitable for further consideration as potential drug candidates due to their lack of specificity.

Published

2008

41. Differential effects of ketoconazole on exposure to temsirolimus following intravenous infusion of temsirolimus.

Author

Boni JP, Leister C, Burns J, and Hug B

Subjects

Adolescent, Adult, Area Under Curve, Cytochrome P-450 CYP3A, Drug Interactions, Female, Humans, Infusions, Intravenous, Male, Middle Aged, Sirolimus adverse effects, Sirolimus pharmacokinetics, Antineoplastic Agents pharmacokinetics, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Sirolimus analogs & derivatives

Abstract

Intravenous (i.v.) temsirolimus, a novel inhibitor of mammalian target of rapamycin, is approved for the treatment of advanced renal cell carcinoma and is being studied in patients with mantle cell lymphoma. Because temsirolimus and its primary metabolite, sirolimus, are metabolised by the cytochrome P450 3A4 pathway (CYP3A4), the potential exists for pharmacokinetic (PK) drug interactions with the numerous agents that modulate CYP3A4 isozyme activity. We investigated the effects of ketoconazole, a potent CYP3A4 inhibitor, on the PK profile of i.v. temsirolimus in healthy adults. Coadministration of 400 mg oral ketoconazole with 5 mg i.v. temsirolimus had no significant effect on temsirolimus maximum concentration (C(max)) or area under the concentration curve (AUC). However, mean AUC increased 3.1-fold and AUC(sum) (sum of temsirolimus plus sirolimus AUCs) increased 2.3-fold compared with temsirolimus alone. A single 5-mg dose of temsirolimus with ketoconazole was well tolerated, and there were no unexpected safety results. Therefore, in cancer patients receiving 25 mg i.v. temsirolimus, concomitant treatment with agents that have strong CYP3A4 inhibition potential should be avoided. If a concomitant strong CYP3A4 inhibitor is necessary, a temsirolimus dose reduction to 12.5 mg weekly should be considered.

Published

2008

42. Effects of ketoconazole on the pharmacokinetics and pharmacodynamics of morphine in healthy Greyhounds.

Author

Kukanich B and Borum SL

Subjects

Analgesics, Opioid blood, Analgesics, Opioid pharmacology, Animals, Area Under Curve, Dogs blood, Drug Interactions, Female, Half-Life, Male, Morphine blood, Morphine pharmacology, Analgesics, Opioid pharmacokinetics, Dogs metabolism, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Morphine pharmacokinetics

Abstract

Objective: To assess pharmacokinetics and pharmacodynamics of morphine and the effects of ketoconazole on the pharmacokinetics and pharmacodynamics of morphine in healthy Greyhounds., Animals: 6 healthy Greyhounds, 3 male and 3 female., Procedures: Morphine sulfate (0.5 mg/kg. IV) was administered to Greyhounds prior to and after 5 days of ketoconazole (12.7 +/- 0.6 mg/kg, PO) treatment. Plasma samples were obtained from blood samples that were collected at predetermined time points for measurement of morphine and ketoconazole concentrations by mass spectrometry. Pharmacokinetics of morphine were estimated by use of computer software., Results: Pharmacodynamic effects of morphine in Greyhounds were similar to those of other studies in dogs and were similar between treatment groups. Morphine was rapidly eliminated with a half-life of 1.28 hours and a plasma clearance of 32.55 mL/min/kg. The volume of distribution was 3.6 L/kg. No significant differences in the pharmacokinetics of morphine were found after treatment with ketoconazole. Plasma concentrations of ketoconazole were high and persisted longer than expected in Greyhounds., Conclusions and Clinical Relevance: Ketoconazole had no significant effect on morphine pharmacokinetics, and the pharmacodynamics were similar between treatment groups. Plasma concentrations of ketoconazole were higher than expected and persisted longer than expected in Greyhounds.

Published

2008

43. The effects of CYP3A4 inhibition on erlotinib pharmacokinetics: computer-based simulation (SimCYP) predicts in vivo metabolic inhibition.

Author

Rakhit A, Pantze MP, Fettner S, Jones HM, Charoin JE, Riek M, Lum BL, and Hamilton M

Subjects

Adolescent, Adult, Aged, Area Under Curve, Computer Simulation, Cytochrome P-450 CYP3A Inhibitors, Drug Interactions, Erlotinib Hydrochloride, Forecasting, Humans, Ketoconazole pharmacology, Male, Microsomes, Liver metabolism, Middle Aged, Cytochrome P-450 CYP3A metabolism, Enzyme Inhibitors pharmacology, Protein Kinase Inhibitors pharmacokinetics, Quinazolines pharmacokinetics

Abstract

Background: Erlotinib is an orally active antitumor agent. Analyses in vitro using human liver microsomes and recombinant enzymes showed that erlotinib was metabolized primarily by CYP3A4, with a secondary contribution from CYP1A2., Methods: A computer-based simulation model, SimCYP, predicted that CYP3A4 contributed to approximately 70% of the metabolic elimination of erlotinib, with CYP1A2 being responsible for the other approximately 30%. A drug-drug interaction study was therefore conducted for erlotinib and a potent CYP3A4 inhibitor, ketoconazole, in healthy male volunteers to evaluate the impact of CYP3A4 inhibition on erlotinib exposure., Results: Ketoconazole caused an almost two-fold increase in erlotinib plasma area under the concentration curve and in maximum plasma concentration. This is consistent with the SimCYP prediction of a two-fold increase in erlotinib AUC, further validating a primary (approximately 70%) role of CYP3A4 in erlotinib elimination., Conclusion: Prediction of clinically important drug-drug interaction with SimCYP using in vitro human metabolism data can be a powerful tool during early clinical development to ensure safe administration of anticancer drugs, which are often co-administered at maximum tolerated doses with other drugs as part of a palliative treatment regimen.

Published

2008

44. Effect of coadministered ketoconazole, a strong cytochrome P450 3A4 enzyme inhibitor, on the pharmacokinetics of ciclesonide and its active metabolite desisobutyryl-ciclesonide.

Author

Böhmer GM, Drollmann A, Gleiter CH, and Nave R

Subjects

Adult, Anti-Allergic Agents adverse effects, Antifungal Agents adverse effects, Area Under Curve, Biotransformation, Enzyme Inhibitors adverse effects, Female, Humans, Ketoconazole adverse effects, Male, Middle Aged, Pregnenediones adverse effects, Anti-Allergic Agents pharmacokinetics, Antifungal Agents pharmacology, Aryl Hydrocarbon Hydroxylases antagonists & inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Pregnenediones pharmacokinetics

Abstract

Background and Objectives: Cytochrome P450 (CYP) 3A4 isoenzyme has been identified in vitro as the key enzyme to metabolize desisobutyryl-ciclesonide (des-CIC), the pharmacologically active metabolite of the inhaled corticosteroid ciclesonide. This pharmacokinetic drug-drug interaction study was conducted to confirm this major metabolic pathway in vivo by using the strong CYP3A4 inhibitor ketoconazole, and to assess the effect of ketoconazole on the pharmacokinetics of ciclesonide and des-CIC., Methods: Fourteen healthy adults participated in this open-label, nonrandomized, fixed sequence, two-period, repeated-dose pharmacokinetic study. During the first 7-day treatment period, the subjects orally inhaled ciclesonide 320 microg once daily. During the second 7-day treatment period, the subjects continued with the same dose of orally inhaled ciclesonide and concomitantly received oral ketoconazole 400 mg once daily. Pharmacokinetic profiles for ciclesonide and des-CIC were obtained on day 7 of each study period., Results: For the parent compound, ciclesonide, no changes in the pharmacokinetic parameter estimates--the area under the serum concentration-time curve during the dosage interval (AUC(tau)), maximum serum concentration (C(max)) and time to reach the C(max)--were observed. In contrast, the AUC(tau) and C(max) of des-CIC increased approximately 3.5-fold and 2-fold under the influence of the CYP3A4 inhibitor ketoconazole., Conclusions: The CYP3A4 pathway is the major pathway for biotransformation of the active metabolite of ciclesonide in humans. While elimination of des-CIC was reduced by strong CYP3A4 inhibitor coadministration in vivo, activation of the parent compound ciclesonide to des-CIC was not affected. Dose adjustment is not necessary when ciclesonide needs to be coadministered with ketoconazole, because the potency of an inhaled corticosteroid is mediated by topical concentrations in the lung and because ciclesonide has a very low potential to produce systemic adverse effects.

Published

2008

45. The cytochrome p450 inhibitor ketoconazole potentiates 5-hydroxytryptamine-induced contraction in rat aorta.

Author

Ogden KK, Falck JR, and Watts SW

Subjects

Animals, Aorta, Thoracic physiology, Catalase physiology, Drug Synergism, Male, Nitric Oxide metabolism, Nitric Oxide Synthase physiology, Nitroarginine pharmacology, Rats, Rats, Sprague-Dawley, Receptor, Serotonin, 5-HT2A physiology, Serotonin metabolism, Superoxides metabolism, Aorta, Thoracic drug effects, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Serotonin pharmacology, Vasoconstriction drug effects

Abstract

5-Hydroxytryptamine (5-HT; serotonin) is a potent vasoconstrictor and smooth muscle mitogen. Substances that produce similar responses also stimulate production of superoxide. We sought to determine whether 5-HT stimulates production of superoxide. 5-HT can be metabolized by cytochrome P450 to nitric oxide (NO), which scavenges superoxide. Thus, we hypothesized that inhibiting cytochrome P450 would potentiate 5-HT-induced contraction and reveal 5-HT-stimulated superoxide. In isolated tissue bath experiments using endotheliumintact rat aorta, the cytochrome P450 inhibitor ketoconazole (KTZ; 1-50 microM) caused a maximum 8-fold leftward shift in the 5-HT concentration-response curve that was not observed when aorta were stimulated with phenylephrine or KCl. 5-HT did not stimulate concentration-dependent increases in superoxide levels as measured by a lucigenin-enhanced chemiluminescent superoxide assay. KTZ (10 microM) did not reveal 5-HT-stimulated superoxide. The NO inhibitor N(omega)-nitro-L-arginine (L-NNA) (100 microM) with or without KTZ (10 microM) potentiated 5-HT-induced contraction independently of NADPH oxidase-derived superoxide but also did not reveal 5-HT-stimulated superoxide. Metabolism of 5-HT to NO depends on catalase, but the catalase inhibitor 3-amino-1,2,4-triazole (50 mM) attenuated 5-HT-induced contraction. Removal of endothelium did not alter the effects of KTZ on 5-HT-induced contraction, and, in endothelium-intact aorta, KTZ did not decrease acetylcholine-induced relaxation. Unlike KTZ, the cytochrome P450 inhibitors 1-aminobenzotriazole (0.5 mM) and clotrimazole (10 microM) did not potentiate 5-HT-induced contraction. Moreover, 14,15-epoxyeicosa-5(Z)-enoic acid (10 microM), an epoxyeicosatrienoic acid antagonist, caused a small rightward shift in the 5-HT concentration-response curve. These data suggest KTZ acts by a potentially novel mechanism to potentiate 5-HT-induced contraction.

Published

2007

46. Use of isolated hepatocyte preparations for cytochrome P450 inhibition studies: comparison with microsomes for Ki determination.

Author

Brown HS, Chadwick A, and Houston JB

Subjects

Animals, Catalysis drug effects, Cells, Cultured, Cytochrome P-450 CYP2D6 metabolism, Cytochrome P-450 CYP2D6 Inhibitors, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme System metabolism, Dextromethorphan metabolism, Dextromethorphan pharmacokinetics, Dextromethorphan pharmacology, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacokinetics, Fluconazole metabolism, Fluconazole pharmacokinetics, Fluconazole pharmacology, Fluoxetine metabolism, Fluoxetine pharmacokinetics, Fluoxetine pharmacology, Fluvoxamine metabolism, Fluvoxamine pharmacokinetics, Fluvoxamine pharmacology, Hepatocytes cytology, Hepatocytes metabolism, Ketoconazole metabolism, Ketoconazole pharmacokinetics, Ketoconazole pharmacology, Kinetics, Male, Miconazole metabolism, Miconazole pharmacokinetics, Miconazole pharmacology, Microsomes, Liver metabolism, Midazolam metabolism, Midazolam pharmacokinetics, Midazolam pharmacology, Phenytoin metabolism, Phenytoin pharmacokinetics, Phenytoin pharmacology, Quinine metabolism, Quinine pharmacokinetics, Quinine pharmacology, Rats, Rats, Sprague-Dawley, Tolbutamide metabolism, Tolbutamide pharmacokinetics, Tolbutamide pharmacology, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Hepatocytes enzymology, Microsomes, Liver enzymology

Abstract

Predicting drug-drug interactions requires an assessment of the drug concentration available to the enzyme active site, both in vivo, and within an in vitro incubation. These predictions are confounded when the inhibitor accumulates within the liver, either as a result of active transport processes or intracellular binding (including lysosomal trapping). In theory, hepatocytes should provide a more accurate estimation of inhibitory potency compared with microsomes for those compounds that undergo hepatic accumulation. However, they are not routinely used for Ki determination and there is limited comparative information available. Therefore, the aims of this study were to compare Ki values determined in rat microsomes and freshly isolated hepatocytes using six cytochrome P450 inhibitors (miconazole, fluconazole, ketoconazole, quinine, fluoxetine, and fluvoxamine) with a range of uptake properties (cell-to-medium concentration ratios 4.2-6000). Inhibition studies were performed using four probe substrates for CYP2C, CYP2D, and CYP3A enzymes (tolbutamide and phenytoin, dextromethorphan and midazolam, respectively). Comparison of unbound Ki values (range 0.05-30 microM) showed good agreement between microsomes and hepatocytes for inhibition of 18 pathways of metabolism. In addition to this, there was no relationship between the cell-to-medium concentration ratios (covering over 3 orders of magnitude) and the microsomal to hepatocyte Ki ratio of these inhibitors. These data suggest that the hepatic accumulation of these inhibitors results from intracellular binding rather than the involvement of uptake transporters and indicate that microsomes and hepatocytes appear to be equivalent for determining the inhibitory potency of the six inhibitors investigated in the present study.

Published

2007

47. The prokinetic cinitapride has no clinically relevant pharmacokinetic interaction and effect on QT during coadministration with ketoconazole.

Author

Robert M, Salvà M, Segarra R, Pavesi M, Esbri R, Roberts D, and Golor G

Subjects

Administration, Oral, Adult, Area Under Curve, Aryl Hydrocarbon Hydroxylases metabolism, Benzamides administration & dosage, Benzamides adverse effects, Biological Availability, Cross-Over Studies, Cytochrome P-450 CYP2C8, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme System metabolism, Double-Blind Method, Drug Interactions, Electrocardiography, Enzyme Inhibitors administration & dosage, Female, Gastrointestinal Agents administration & dosage, Gastrointestinal Agents adverse effects, Heart Rate drug effects, Humans, Ketoconazole administration & dosage, Long QT Syndrome chemically induced, Male, Metabolic Clearance Rate drug effects, Middle Aged, Reference Values, Benzamides pharmacokinetics, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Gastrointestinal Agents pharmacokinetics, Ketoconazole pharmacology

Abstract

The present clinical trial was designed to evaluate the possible pharmacokinetic and electrocardiographic interactions of the gastroenteric prokinetic drug cinitapride with ketoconazole. The safety and tolerability of the study treatments were also evaluated. After a placebo-controlled, double-blind, crossover design, 16 healthy male (n = 8) and female (n = 8) volunteers were randomized into four treatment groups of four subjects (two males and two females): cinitapride (CTP; 1 mg t.i.d.) + ketoconazole (KET; 200 mg b.i.d.), CTP + placebo (PL), PL+KET, and PL+PL. Treatments were given for 7 days with a washout period of 14 days between crossover treatments. Cinitapride is rapidly absorbed after oral administration and is metabolized by the cytochrome P450 CYP3A4 and CYP2C8 isozymes. At steady state, coadministration with ketoconazole, a potent CYP3A4 inhibitor, increased mean C(max,ss) and AUC(tau) by 1.63- and 1.98-fold, respectively. Measurement of mean QTc interval or baseline-corrected QTc intervals on day 7 showed small increases that were due to the effects of ketoconazole alone. Comparing CTP+KET versus PL+KET, the differences between mean increases in the QTc parameters were always less than 2 ms. Finally, no outlier increase of the QTc interval versus baseline >60 ms was identified after any treatment. The study showed that cinitapride, either given alone or after coadministration with ketoconazole 200 mg b.i.d., had no effect on cardiac repolarization as measured by changes in the heart rate-corrected QT interval on the surface electrocardiogram.

Published

2007

48. Possible inhibitory mechanism of Curcuma drugs on CYP3A4 in 1alpha,25 dihydroxyvitamin D3 treated Caco-2 cells.

Author

Hou XL, Takahashi K, Kinoshita N, Qiu F, Tanaka K, Komatsu K, Takahashi K, and Azuma J

Subjects

Caco-2 Cells, Cell Survival drug effects, Curcumin analysis, Curcumin toxicity, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme System biosynthesis, Cytochrome P-450 Enzyme System genetics, Dose-Response Relationship, Drug, Enzyme Induction drug effects, Enzyme Inhibitors chemistry, Enzyme Inhibitors toxicity, Humans, Hydroxylation, Inhibitory Concentration 50, Intestinal Mucosa enzymology, Intestinal Mucosa pathology, Ketoconazole pharmacology, Nifedipine metabolism, Oxidation-Reduction, Plant Extracts chemistry, Plant Extracts pharmacology, RNA, Messenger metabolism, Rhizome, Rifampin pharmacology, Testosterone metabolism, Calcitriol pharmacology, Curcuma chemistry, Curcumin pharmacology, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Herb-Drug Interactions, Intestinal Mucosa drug effects

Abstract

Curcuma longa and C. zedoaria, belonging to genus Curcuma, have become prevalent as supplements in East Asia. Curcumin is the most well-studied bioactive component isolated from rhizomes of C. longa and other Curcuma species except C. zedoaria. In this study, we investigated the affects of C. longa, C. zedoaria from Japan and curcumin on CYP3A4. Caco-2 cells, in which CYP3A4 expression was induced by 1alpha,25-(OH)(2)-D(3), were used to mimic the metabolism of small intestine. Caco-2 cells were treated with methanol extracts from two Curcuma rhizomes (0.1mg/ml) or curcumin (30 microM) for 72 h. Both extracts significantly decreased the activity of CYP3A4 by about 85-98%. The 50% inhibitory concentrations of C. longa and C. zedoaria extracts were 0.019 and 0.014 mg/ml, respectively. They caused a 60-70% decrease in CYP3A4 protein. Otherwise, curcumin treatment caused a 30-40% decrease in CYP3A4 catalytic activity and a 38% decrease in CYP3A4 protein expression. Moreover, it was found that both Curcuma extracts and curcumin treatment had no influence on CYP3A4 mRNA expression. Our results suggested that administration of Curcuma drugs might inhibit the catalytic activity of intestinal CYP3A4. However, curcumin was not the major compound responsible for this inhibitory effect.

Published

2007

49. Cytochrome P450 3A inhibition by ketoconazole affects prasugrel and clopidogrel pharmacokinetics and pharmacodynamics differently.

Author

Farid NA, Payne CD, Small DS, Winters KJ, Ernest CS 2nd, Brandt JT, Darstein C, Jakubowski JA, and Salazar DE

Subjects

Adult, Area Under Curve, Clopidogrel, Cross-Over Studies, Double-Blind Method, Drug Interactions, Female, Humans, Male, Middle Aged, Piperazines administration & dosage, Piperazines pharmacology, Platelet Aggregation drug effects, Platelet Aggregation Inhibitors administration & dosage, Platelet Aggregation Inhibitors pharmacology, Prasugrel Hydrochloride, Thiophenes administration & dosage, Thiophenes pharmacology, Ticlopidine administration & dosage, Ticlopidine pharmacokinetics, Ticlopidine pharmacology, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Piperazines pharmacokinetics, Platelet Aggregation Inhibitors pharmacokinetics, Thiophenes pharmacokinetics, Ticlopidine analogs & derivatives

Abstract

Prasugrel and clopidogrel inhibit platelet aggregation through active metabolite formation. Prasugrel's active metabolite (R-138727) is formed primarily by cytochrome P450 (CYP) 3A and CYP2B6, with roles for CYP2C9 and CYP2C19. Clopidogrel's activation involves two sequential steps by CYP3A, CYP1A2, CYP2C9, CYP2C19, and/or CYP2B6. In a randomized crossover study, healthy subjects received a loading dose (LD) of prasugrel (60 mg) or clopidogrel (300 mg), followed by five daily maintenance doses (MDs) (15 and 75 mg, respectively) with or without the potent CYP3A inhibitor ketoconazole (400 mg/day). Subjects had a 2-week washout between periods. Ketoconazole decreased R-138727 and clopidogrel active metabolite Cmax (maximum plasma concentration) 34-61% after prasugrel and clopidogrel dosing. Ketoconazole did not affect R-138727 exposure or prasugrel's inhibition of platelet aggregation (IPA). Ketoconazole decreased clopidogrel's active metabolite AUC0-24 (area under the concentration-time curve to 24 h postdose) 22% (LD) to 29% (MD) and reduced IPA 28% (LD) to 33% (MD). We conclude that CYP3A4 and CYP3A5 inhibition by ketoconazole affects formation of clopidogrel's but not prasugrel's active metabolite. The decreased formation of clopidogrel's active metabolite is associated with reduced IPA.

Published

2007

50. Effect of ion suppression on judgment of enzyme inhibition and avoidance of error by utilizing a stable isotope-labeled probe substrate: example of CYP3A4 inhibition with [13C4,15N] labeled midazolam as a substrate.

Author

Nakamura K, Watanabe A, Okudaira N, Okazaki O, and Sudo K

Subjects

Carbon Isotopes metabolism, Chromatography, High Pressure Liquid, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme System metabolism, Dextrorphan metabolism, Dose-Response Relationship, Drug, Erythromycin pharmacology, Humans, Hydroxylation, In Vitro Techniques, Liver enzymology, Microsomes, Liver drug effects, Microsomes, Liver enzymology, Nitrogen Isotopes metabolism, Reproducibility of Results, Tandem Mass Spectrometry, Artifacts, Cytochrome P-450 Enzyme Inhibitors, Drug Evaluation, Preclinical methods, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Liver drug effects, Midazolam metabolism, Molecular Probes metabolism

Abstract

An advantage of using LC-MS(/MS) for in vitro CYP inhibition screening is that it does not require extensive sample preparation and chromatographic separation. Attention must be paid, however, to ion suppression effects on analytes caused by the test compound as well as endogenous compounds. In this study, we have shown the ion suppression of 1'-hydroxymidazolam (analyte) and dextrorphan (IS) by erythromycin, as an example, which may cause over- or underestimation of CYP3A4 inhibition. To avoid this kind of effect, we proposed to use a stable isotope-labeled substrate and determine labeled metabolites by using unlabeled authentic compounds of each metabolite. We showed that CYP3A4 activity was determined with high accuracy and precision by using stable isotope-labeled midazolam even in the presence of an ion suppressor at high concentrations in the samples. This method is useful not only for the CYP inhibition screening but also for testing drug candidates to predict changes in metabolite formation by the possible co-administered drugs.

Published

2007