Your search keyword '"Ketoconazole metabolism"' showing total 203 results

1. Quantitative prediction of CYP3A-mediated drug-drug interactions by correctly estimating fraction metabolized using human liver chimeric mice.

Author

Miyake T, Mochizuki T, Nakagawa T, Nakamura M, Emoto C, Komiyama N, Hirabayashi M, Tsuruta S, Shimojo T, Terao K, and Tachibana T

Subjects

Humans, Mice, Animals, Mice, SCID, Liver metabolism, Drug Interactions, Cytochrome P-450 CYP3A metabolism, Ketoconazole metabolism

Abstract

Background and Purpose: Fraction metabolized (f m ) and fraction transported (f t ) are important for understanding drug-drug interactions (DDIs) in drug discovery and development. However, current in vitro systems cannot accurately estimate in vivo f m due to inability to reflect the f t by efflux transporters (f t,efflux ). This study demonstrates how CYP3A-mediated DDI for CYP3A/P-gp substrates can be predicted using Hu-PXB mice as human liver chimeric mice., Experimental Approach: For estimating human in vitro f m by CYP3A enzyme (f m,CYP3A,in vitro ), six drugs, including CYP3A/P-gp substrates (alprazolam, cyclosporine, docetaxel, midazolam, prednisolone, and theophylline) and human hepatocytes were incubated with or without ketoconazole as a CYP3A inhibitor. We calculated f m,CYP3A,in vitro based on hepatic intrinsic clearance. To estimate human in vivo f m,CYP3A (f m,CYP3A,in vivo ), we collected information on clinical DDI caused by ketoconazole for these six drugs. We calculated f m,CYP3A,in vivo using the change of total clearance (CL total ). For evaluating the human DDI predictability, the six drugs were administered intravenously to Hu-PXB and SCID mice with or without ketoconazole. We calculated the change of CL total caused by ketoconazole. We compared the CL total change in humans with that in Hu-PXB and SCID mice., Key Results: The f m,CYP3A,in vitro was overestimated compared to the f m,CYP3A,in vivo . Hu-PXB mice showed much better correlation in the change of CL total with humans (R 2  = 0.95) compared to SCID mice (R 2  = 0.0058)., Conclusions and Implications: CYP3A-mediated DDI can be predicted by correctly estimating human f m,CYP3A,in vivo using Hu-PXB mice. These mice could be useful predicting hepatic f m and f t,efflux ., (© 2023 British Pharmacological Society.)

Published

2024

2. Enhancing drug-drug Interaction Prediction by Integrating Physiologically-Based Pharmacokinetic Model with Fraction Metabolized by CYP3A4.

Author

Jiang P, Chen T, Chu LF, Xu RP, Gao JT, Wang L, Liu Q, Tang L, Wan H, Li M, and Ren HC

Subjects

Humans, Models, Biological, Drug Interactions, Microsomes, Liver metabolism, Computer Simulation, Cytochrome P-450 CYP3A metabolism, Ketoconazole metabolism

Abstract

Background: Enhancing the precision of drug-drug interaction (DDI) prediction is essential for improving drug safety and efficacy. The aim is to identify the most effective fraction metabolized by CY3A4 ( f m ) for improving DDI prediction using physiologically based pharmacokinetic (PBPK) models., Research Design and Methods: The f m values were determined for 33 approved drugs using a human liver microsome for in vitro measurements and the ADMET Predictor software for in silico predictions. Subsequently, these f m values were integrated into PBPK models using the GastroPlus platform. The PBPK models, combined with a ketoconazole model, were utilized to predict AUCR (AUC combo with ketoconazole /AUC dosing alone ), and the accuracy of these predictions was evaluated by comparison with observed AUCR., Results: The integration of in vitro f m method demonstrates superior performance compared to the in silico f m method and f m of 100% method. Under the Guest-limits criteria, the integration of in vitro f m achieves an accuracy of 76%, while the in silico f m and f m of 100% methods achieve accuracies of 67% and 58%, respectively., Conclusions: Our study highlights the importance of in vitro f m data to improve the accuracy of predicting DDIs and demonstrates the promising potential of in silico f m in predicting DDIs.

Published

2023

3. In Vitro and In Vivo Metabolic Activation of Tolterodine Mediated by CYP3A.

Author

Wang A, Zhao Q, Liu M, Wang Y, Zhao G, Li W, Peng Y, and Zheng J

Subjects

Humans, Rats, Mice, Animals, Activation, Metabolic, Tolterodine Tartrate metabolism, Cysteine metabolism, Ketoconazole metabolism, Microsomes, Liver metabolism, Glutathione metabolism, Cytochrome P-450 CYP3A metabolism, Chemical and Drug Induced Liver Injury metabolism

Abstract

Tolterodine (TOL) is an antimuscarinic drug used for the treatment of patients with overactive bladder presenting urinary frequency, urgency, and urge incontinence. During the clinical use of TOL, adverse events such as liver injury took place. The present study aimed at the investigation of the metabolic activation of TOL possibly associated with its hepatotoxicity. One GSH conjugate, two NAC conjugates, and two cysteine conjugates were found in both mouse and human liver microsomal incubations supplemented with TOL, GSH/NAC/cysteine, and NADPH. The detected conjugates suggest the production of a quinone methide intermediate. The same GSH conjugate was also observed in mouse primary hepatocytes and in the bile of rats receiving TOL. One of the urinary NAC conjugates was observed in rats administered TOL. One of the cysteine conjugates was found in a digestion mixture containing hepatic proteins from animals administered TOL. The observed protein modification was dose-dependent. CYP3A primarily catalyzes the metabolic activation of TOL. Ketoconazole (KTC) pretreatment reduced the generation of the GSH conjugate in mouse liver and cultured primary hepatocytes after TOL treatment. In addition, KTC reduced the susceptibility of primary hepatocytes to TOL cytotoxicity. The quinone methide metabolite may be involved in TOL-induced hepatotoxicity and cytotoxicity.

Published

2023

4. Relationships between Isomeric Metabolism and Regioselective Toxicity of Hydroxychrysenes in Embryos of Japanese Medaka ( Oryzias latipes ).

Author

Tanabe P, Pampanin DM, Tiruye HM, Jørgensen KB, Hammond RI, Gadepalli RS, Rimoldi JM, and Schlenk D

Subjects

Animals, Ketoconazole metabolism, Embryo, Nonmammalian chemistry, Embryo, Nonmammalian metabolism, Oryzias physiology, Water Pollutants, Chemical toxicity, Polycyclic Aromatic Hydrocarbons toxicity

Abstract

Oxygenated polycyclic aromatic hydrocarbons (oxy-PAHs) are ubiquitous contaminants that can be formed through oxidation of parent PAHs. Our previous studies found 2-hydroxychrysene (2-OHCHR) to be significantly more toxic to Japanese medaka embryos than 6-hydroxychrysene (6-OHCHR), an example of regioselective toxicity. We have also previously identified a sensitive developmental window to 2-OHCHR toxicity that closely coincided with liver development, leading us to hypothesize that differences in metabolism may play a role in the regioselective toxicity. To test this hypothesis, Japanese medaka embryos were treated with each isomer for 24 h during liver development (52-76 hpf). Although 6-OHCHR was absorbed 97.2 ± 0.18% faster than 2-OHCHR, it was eliminated 57.7 ± 0.36% faster as a glucuronide conjugate. Pretreatment with cytochrome P450 inhibitor, ketoconazole, reduced anemia by 96.8 ± 3.19% and mortality by 95.2 ± 4.76% in 2-OHCHR treatments. Formation of chrysene-1,2-diol (1,2-CAT) was also reduced by 64.4 ± 2.14% by ketoconazole pretreatment. While pretreatment with UDP-glucuronosyltransferase inhibitor, nilotinib, reduced glucuronidation of 2-OHCHR by 52.4 ± 2.55% and of 6-OHCHR by 63.7 ± 3.19%, it did not alter toxicity for either compound. These results indicate that CYP-mediated activation, potentially to 1,2-CAT, may explain the isomeric differences in developmental toxicity of 2-OHCHR.

Published

2023

5. Identification of a window of androgen sensitivity for somatic cell function in human fetal testis cultured ex vivo.

Author

Lundgaard Riis M, Matilionyte G, Nielsen JE, Melau C, Greenald D, Juul Hare K, Langhoff Thuesen L, Dreisler E, Aaboe K, Brenøe PT, Andersson AM, Albrethsen J, Frederiksen H, Rajpert-De Meyts E, Juul A, Mitchell RT, and Jørgensen A

Subjects

Humans, Male, Androgens pharmacology, Androgens metabolism, Flutamide pharmacology, Flutamide metabolism, Ketoconazole metabolism, Ketoconazole pharmacology, Receptors, Androgen metabolism, Testosterone pharmacology, Testicular Hormones metabolism, Testicular Hormones pharmacology, Testis

Abstract

Background: Reduced androgen action during early fetal development has been suggested as the origin of reproductive disorders comprised within the testicular dysgenesis syndrome (TDS). This hypothesis has been supported by studies in rats demonstrating that normal male development and adult reproductive function depend on sufficient androgen exposure during a sensitive fetal period, called the masculinization programming window (MPW). The main aim of this study was therefore to examine the effects of manipulating androgen production during different timepoints during early human fetal testis development to identify the existence and timing of a possible window of androgen sensitivity resembling the MPW in rats., Methods: The effects of experimentally reduced androgen exposure during different periods of human fetal testis development and function were examined using an established and validated human ex vivo tissue culture model. The androgen production was reduced by treatment with ketoconazole and validated by treatment with flutamide which blocks the androgen receptor. Testicular hormone production ex vivo was measured by liquid chromatography-tandem mass spectrometry or ELISA assays, and selected protein markers were assessed by immunohistochemistry., Results: Ketoconazole reduced androgen production in testes from gestational weeks (GW) 7-21, which were subsequently divided into four age groups: GW 7-10, 10-12, 12-16 and 16-21. Additionally, reduced secretion of testicular hormones INSL3, AMH and Inhibin B was observed, but only in the age groups GW 7-10 and 10-12, while a decrease in the total density of germ cells and OCT4 + gonocytes was found in the GW 7-10 age group. Flutamide treatment in specimens aged GW 7-12 did not alter androgen production, but the secretion of INSL3, AMH and Inhibin B was reduced, and a reduced number of pre-spermatogonia was observed., Conclusions: This study showed that reduced androgen action during early development affects the function and density of several cell types in the human fetal testis, with similar effects observed after ketoconazole and flutamide treatment. The effects were only observed within the GW 7-14 period-thereby indicating the presence of a window of androgen sensitivity in the human fetal testis., (© 2022. The Author(s).)

Published

2022

6. Evidence for Metabolic Activation of Omeprazole In Vitro and In Vivo.

Author

Zhao Y, Sun C, Su M, Shi J, Hu Z, Peng Y, and Zheng J

Subjects

Acetylcysteine metabolism, Activation, Metabolic, Animals, Benzoquinones metabolism, Glutathione metabolism, Humans, Imines metabolism, Ketoconazole metabolism, Microsomes, Liver metabolism, Proton Pump Inhibitors metabolism, Rats, Cytochrome P-450 CYP3A metabolism, Omeprazole metabolism, Omeprazole pharmacology

Abstract

Omeprazole (OPZ) is a proton pump inhibitor commonly used for the treatment of gastric acid hypersecretion. Studies have revealed that use of OPZ can induce hepatotoxicity, but the mechanisms by which it induces liver injury are unclear. This study aimed to identify reactive metabolites of OPZ, determine the pathways of the metabolic activation, and define the correlation of the bioactivation with OPZ cytotoxicity. Quinone imine-derived glutathione (GSH), N -acetylcysteine (NAC), and cysteine (Cys) conjugates were detected in OPZ-fortified rat and human liver microsomal incubations captured with GSH, NAC, or Cys. The same GSH conjugates were detected in bile of rats and cultured liver primary cells after exposure to OPZ. Similarly, the same NAC conjugates were detected in urine of OPZ-treated rats. The resulting quinone imine was found to react with Cys residues of hepatic protein. CYP3A4 dominated the metabolic activation of OPZ. Exposure to OPZ resulted in decreased cell survival in cultured primary hepatocytes. Pretreatment with ketoconazole attenuated the susceptibility of hepatocytes to the cytotoxicity of OPZ.

Published

2022

7. In Vitro Evaluation of P-gp-Mediated Drug-Drug Interactions Using the RPTEC/TERT1 Human Renal Cell Model.

Author

Saib S, Hodin S, Bin V, Ollier E, and Delavenne X

Subjects

Drug Interactions, Humans, Ketoconazole metabolism, Reproducibility of Results, Kidney metabolism, Rivaroxaban pharmacokinetics

Abstract

Background and Objectives: In vitro evaluation of the P-glycoprotein (P-gp) inhibitory potential is an important issue when predicting clinically relevant drug-drug interactions (DDIs). Located within all physiological barriers, including intestine, liver, and kidneys, P-gp plays a major role in the pharmacokinetics of various therapeutic classes. However, few data are available about DDIs involving renal transporters during the active tubular secretion of drugs. In this context, the present study was designed to investigate the application of the human renal cell line RPTEC/TERT1 to study drug interactions mediated by P-gp., Methods: The P-gp inhibitory potentials of a panel of drugs were first determined by measuring the intracellular accumulation of rhodamine 123 in RPTEC/TERT1 cells. Then four drugs were selected to assess the half-maximal inhibitor concentration (IC50) values by measuring the intracellular accumulation of two P-gp-substrate drugs, apixaban and rivaroxaban. Finally, according to the FDA guidelines, the [I 1 ]/IC50 ratio was calculated for each combination of drugs to assess the clinical relevance of the DDIs., Results: The data showed that drugs which are known P-gp inhibitors, including cyclosporin A, ketoconazole, and verapamil, caused great increases in rhodamine 123 retention, whereas noninhibitors did not affect the intracellular accumulation of the P-gp substrate. The determined IC50 values were in accordance with the inhibition profiles observed in the rhodamine 123 accumulation assays, confirming the reliability of the RPTEC/TERT1 model., Conclusions: Taken together, the data demonstrate the feasibility of the application of the RPTEC/TERT1 model for evaluating the P-gp inhibitory potentials of drugs and consequently predicting renal drug interactions., (© 2021. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published

2022

8. Permeabilized Cryopreserved Human Hepatocytes as an Exogenous Metabolic System in a Novel Metabolism-Dependent Cytotoxicity Assay for the Evaluation of Metabolic Activation and Detoxification of Drugs Associated with Drug-Induced Liver Injuries: Results with Acetaminophen, Amiodarone, Cyclophosphamide, Ketoconazole, Nefazodone, and Troglitazone.

Author

Wei H and Li AP

Subjects

Acetaminophen metabolism, Activation, Metabolic, Cyclophosphamide metabolism, Cytochrome P-450 Enzyme System metabolism, Glutathione metabolism, HEK293 Cells, Hepatocytes metabolism, Humans, Ketoconazole metabolism, Piperazines, Triazoles, Troglitazone, Amiodarone metabolism, Chemical and Drug Induced Liver Injury metabolism

Abstract

We report here a novel in vitro experimental system, the metabolism-dependent cytotoxicity assay (MDCA), for the definition of the roles of hepatic drug metabolism in toxicity. MDCA employs permeabilized cofactor-supplemented cryopreserved human hepatocytes (MetMax Human Hepatocytes, MMHH), as an exogenous metabolic activating system, and human embryonic kidney 293 (HEK293) cells, a cell line devoid of drug-metabolizing enzyme activity, as target cells for the quantification of drug toxicity. The assay was performed in the presence and absence of cofactors for key drug metabolism pathways known to play key roles in drug toxicity: NADPH/NAD+ for phase 1 oxidation, uridine 5'-diphosphoglucuronic acid (UDPGA) for uridine 5'-diphospho-glucuronosyltransferase (UGT) mediated glucuronidation, 3'-phosphoadenosine-5'-phosphosulfate (PAPS) for cytosolic sulfotransferase (SULT) mediated sulfation, and glutathione (GSH) for glutathione S-transferase (GST) mediated GSH conjugation. Six drugs with clinically significant hepatoxicity, resulting in liver failure or a need for liver transplantation: acetaminophen, amiodarone, cyclophosphamide, ketoconazole, nefazodone, and troglitazone were evaluated. All six drugs exhibited cytotoxicity enhancement by NADPH/NAD+, suggesting metabolic activation via phase 1 oxidation. Attenuation of cytotoxicity by UDPGA was observed for acetaminophen, ketoconazole, and troglitazone, by PAPS for acetaminophen, ketoconazole, and troglitazone, and by GSH for all six drugs. Our results suggest that MDCA can be applied toward the elucidation of metabolic activation and detoxification pathways, providing information that can be applied in drug development to guide structure optimization to reduce toxicity and to aid the assessment of metabolism-based risk factors for drug toxicity. GSH detoxification represents an endpoint for the identification of drugs forming cytotoxic reactive metabolites, a key property of drugs with idiosyncratic hepatotoxicity. SIGNIFICANCE STATEMENT: Application of the metabolism-dependent cytotoxicity assay (MDCA) for the elucidation of the roles of metabolic activation and detoxification pathways in drug toxicity may provide information to guide structure optimization in drug development to reduce hepatotoxic potential and to aid the assessment of metabolism-based risk factors. Glutathione (GSH) detoxification represents an endpoint for the identification of drugs forming cytotoxic reactive metabolites that may be applied toward the evaluation of idiosyncratic hepatotoxicity., (Copyright © 2022 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2022

9. Arylacetamide deacetylase knockout mice are sensitive to ketoconazole-induced hepatotoxicity and adrenal insufficiency.

Author

Nagaoka M, Fukami T, Kisui F, Yamada T, Sakai Y, Tashiro K, Ogiso T, Konishi K, Honda S, Hirosawa K, Nakano M, and Nakajima M

Subjects

Adrenal Insufficiency enzymology, Adrenal Insufficiency etiology, Animals, Area Under Curve, Carboxylic Ester Hydrolases metabolism, Chemical and Drug Induced Liver Injury enzymology, Chemical and Drug Induced Liver Injury etiology, Cytochrome P-450 CYP3A Inhibitors metabolism, Cytochrome P-450 CYP3A Inhibitors toxicity, Gene Expression Regulation, Enzymologic, Hydrolysis, Ketoconazole metabolism, Ketoconazole pharmacokinetics, Liver metabolism, Liver pathology, Male, Mice, Inbred C57BL, Mice, Knockout, Microsomes, Liver metabolism, Reverse Transcriptase Polymerase Chain Reaction, Mice, Adrenal Insufficiency genetics, Carboxylic Ester Hydrolases genetics, Chemical and Drug Induced Liver Injury genetics, Ketoconazole toxicity

Abstract

Orally administered ketoconazole may rarely induce liver injury and adrenal insufficiency. A metabolite formed by arylacetamide deacetylase (AADAC)-mediated hydrolysis has been observed in cellulo studies, and it is relevant to ketoconazole-induced cytotoxicity. This study tried to examine the significance of AADAC in ketoconazole-induced toxicity in vivo using Aadac knockout mice. Oral administration of 150 mg/kg ketoconazole resulted in the area under the plasma concentration-time curve values of ketoconazole and N-deacetylketoconazole, a hydrolyzed metabolite of ketoconazole, in Aadac knockout mice being significantly higher and lower than those in wild-type mice, respectively. With the administration of ketoconazole (300 mg/kg/day) for 7 days, Aadac knockout mice showed higher mortality (100%) than wild-type mice (42.9%), and they also showed significantly higher plasma alanine transaminase and lower corticosterone levels, thus representing liver injury and steroidogenesis inhibition, respectively. It was suggested that a higher plasma ketoconazole concentration likely accounts for the inhibition of the synthesis of corticosterone, which has anti-inflammatory effects, in the adrenal gland in Aadac KO mice. In Aadac knockout mice, hepatic mRNA levels of immune- and inflammation-related factors were increased by the administration of 300 mg/kg ketoconazole, and the increase was restored by the replenishment of corticosterone (40 mg/kg, s.c.) along with recoveries of plasma alanine transaminase levels. In conclusion, Aadac defects exacerbate ketoconazole-induced liver injury by inhibiting glucocorticoid synthesis and enhancing the inflammatory response. This in vivo study revealed that the hydrolysis of ketoconazole by AADAC can mitigate ketoconazole-induced toxicities., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2022

10. Effects of nanoplastic on toxicity of azole fungicides (ketoconazole and fluconazole) in zebrafish embryos.

Author

Bhagat J, Zang L, Nakayama H, Nishimura N, and Shimada Y

Subjects

Animals, Embryo, Nonmammalian metabolism, Fluconazole metabolism, Fluconazole toxicity, Ketoconazole metabolism, Ketoconazole toxicity, Oxidative Stress, Zebrafish, Azoles metabolism, Azoles toxicity, Fungicides, Industrial metabolism, Fungicides, Industrial toxicity, Microplastics, Water Pollutants, Chemical metabolism, Water Pollutants, Chemical toxicity

Abstract

The ubiquity of nanoplastics (NPs) raises concerns about their interactions and combined toxicity with other common contaminants. Although azoles are present throughout the natural environment, their interactions with NP are not well known. We investigated the effects of polystyrene (PS) NP on the toxicity of ketoconazole (KCZ) and fluconazole (FCZ) in zebrafish embryos using the developmental toxicity, oxidative-stress-related biochemical parameters, and expression of genes related to neurotoxicity (ache), cardiotoxicity (gata4, bmp4), inflammation (il1b), oxidative stress (sod1, sod2, cyp1a), and apoptosis (bax, bcl2). Co-exposure to NP (1 mg/L) and KCZ/FCZ (1 mg/L) for 96 h reduced the hatching rate, survival rate, and heart rate and increased the malformation rate and catalase activity. The bax/bcl2 ratio, an apoptosis indicator, was higher after NP, KCZ, or FCZ treatment. However, the bax/bcl2 ratio after exposure to NP + KCZ or NP + FCZ was much higher than that after single exposure. Overall, the results indicated that NP aggravated the toxicity of azole by significantly increasing the reactive oxygen species, lipid peroxidation and altering the expression of oxidative-stress- and apoptosis-related genes. The interactive toxicity of PS NP with KCZ/FCZ reported in this study emphasises the need for caution in the release of azole fungicides in the environment., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

11. Analyzing Potential Intestinal Transporter Drug-Drug Interactions: Reevaluating Ticagrelor Interaction Studies.

Author

Liu S, Sodhi JK, and Benet LZ

Subjects

Citrus paradisi, Cyclosporine pharmacokinetics, Cytochrome P-450 CYP3A Inhibitors pharmacokinetics, Diltiazem metabolism, Drug Interactions, Fruit and Vegetable Juices, Humans, Intestinal Absorption, Intestines, Ketoconazole metabolism, Rifampin metabolism, Ticagrelor pharmacokinetics, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Cyclosporine metabolism, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors metabolism, Ticagrelor metabolism

Abstract

Purpose: Previous studies evaluating ticagrelor drug-drug interactions have not differentiated intestinal versus systemic mechanisms, which we do here., Methods: Using recently published methodologies from our laboratory to differentiate metabolic- from transporter-mediated drug-drug interactions, a critical evaluation of five published ticagrelor drug-drug interactions was carried out to investigate the purported clinical significance of enzymes and transporters in ticagrelor disposition., Results: The suggested CYP3A4 inhibitors, ketoconazole and diltiazem, displayed unchanged mean absorption time (MAT) and time of maximum concentration (T max ) values as was expected, i.e., the interactions were mainly mediated by metabolic enzymes. The potential CYP3A4/P-gp inhibitor cyclosporine also showed an unchanged MAT value. Further analysis assuming there was no P-gp effect suggested that the increased AUC and unchanged t 1/2 for ticagrelor after cyclosporine administration were attributed to the inhibition of intestinal CYP3A4 rather than P-gp. Rifampin, an inducer of CYP3As after multiple dosing, unexpectedly showed decreased MAT and T max values, which cannot be completely explained. In contrast, grapefruit juice, an intestinal CYP3A/P-gp/OATP inhibitor, significantly increased MAT and T max values for ticagrelor, which may be due to activation of P-gp or inhibition of OATPs expressed in intestine., Conclusions: This study provides new insight into the role of transporter pathways in ticagrelor intestinal absorption by examining potential MAT and T max changes mediated by drug-drug interactions., (© 2021. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2021

12. Ketoconazole-p aminobenzoic cocrystal, an improved antimycotic drug formulation, does not induce skin sensitization on the skin of BALBc mice.

Author

Danescu S, Filip GA, Moldovan R, Olteanu D, Nagy A, Filip X, Martin F, Kacso I, and Baldea I

Subjects

4-Aminobenzoic Acid chemical synthesis, 4-Aminobenzoic Acid metabolism, Administration, Topical, Animals, Anti-Bacterial Agents chemical synthesis, Anti-Bacterial Agents metabolism, Crystallization methods, Female, Inflammation Mediators antagonists & inhibitors, Inflammation Mediators metabolism, Ketoconazole chemical synthesis, Ketoconazole metabolism, Mice, Mice, Inbred BALB C, Skin metabolism, 4-Aminobenzoic Acid administration & dosage, Anti-Bacterial Agents administration & dosage, Drug Compounding methods, Ketoconazole administration & dosage, Skin drug effects

Abstract

Fungal infections are a growing global health problem. Therefore, our group has synthetized and characterized an improved antimycotic by co-crystallization of ketoconazole and para-amino benzoic acid, named KET-PABA. The aim was to increase bioavailability, biocompatibility, and efficiency of the parent drug-ketoconazole. Based on our previous results showing the cocrystal improved physical properties, such as stability in suspension, solubility, as well as antimycotic efficiency compared to ketoconazole, the current study investigated the local possible side effects induced on the skin of BALBc mice by the application of KET-PABA cocrystal, in view of a further use as a topically applied antimycotic drug. A specific test (mouse ear-swelling test) was used, combined with the histopathological examination and the measurement of pro and anti-inflammatory cytokines and inflammation mediators. KET-PABA application was safe, without signs of skin sensitization shown by the mouse ear sensitization test, or histopathology. KET-PABA strongly inhibited proinflammatory cytokines such as IL1 α, IL1 β, IL6 and TNF α, and other proinflammatory inducers such as NRF2, compared to vehicle. KET-PABA had no effect on the levels of the anti-inflammatory cytokine IL10, or proinflammatory enzyme COX2 and had minimal effects on the activation of the NF-κB pathway. Overall, KET-PABA application induced no sensitization, moreover, it decreased the skin levels of proinflammatory molecules. The lack of skin sensitization effects on BALBc mice skin along with the inhibition of the proinflammatory markers show a good safety profile for topical applications of KET-PABA and show promise for a further clinical use in the treatment of cutaneous mycosis.

Published

2021

13. Tertiary Oxidation of Deoxycholate Is Predictive of CYP3A Activity in Dogs.

Author

Zeng W, Gui L, Tan X, Zhu P, Hu Y, Wu Q, Li X, Yang L, Jia W, Liu C, and Lan K

Subjects

Adult, Animals, Cytochrome P-450 CYP3A Inhibitors pharmacology, Dogs, Enzyme Activation drug effects, Enzyme Activation physiology, Female, Forecasting, GABA Modulators metabolism, GABA Modulators pharmacology, Humans, Ketoconazole metabolism, Ketoconazole pharmacology, Male, Microsomes, Liver drug effects, Midazolam metabolism, Midazolam pharmacology, Oxidation-Reduction drug effects, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors metabolism, Deoxycholic Acid metabolism, Microsomes, Liver metabolism

Abstract

Deoxycholic acid (DCA, 3 α , 12 α -dihydroxy-5 β -cholan-24-oic acid) is the major circulating secondary bile acid, which is synthesized by gut flora in the lower gut and selectively oxidized by CYP3A into tertiary metabolites, including 1 β ,3 α ,12 α -trihydroxy-5 β -cholan-24-oic acid (DCA-1 β -ol) and 3 α ,5 β ,12 α -trihydroxy-5 β -cholan-24-oic acid (DCA-5 β -ol) in humans. Since DCA has the similar exogenous nature and disposition mechanisms as xenobiotics, this work aimed to investigate whether the tertiary oxidations of DCA are predictive of in vivo CYP3A activities in beagle dogs. In vitro metabolism of midazolam (MDZ) and DCA in recombinant canine CYP1A1, 1A2, 2B11, 2C21, 2C41, 2D15, 3A12, and 3A26 enzymes clarified that CYP3A12 was primarily responsible for either the oxidation elimination of MDZ or the regioselective oxidation metabolism of DCA into DCA-1 β -ol and DCA-5 β -ol in dog liver microsomes. Six male dogs completed the CYP3A intervention studies including phases of baseline, inhibition (ketoconazole treatments), recovery, and induction (rifampicin treatments). The oral MDZ clearance after a single dose was determined on the last day of the baseline, inhibition, and induction phases, and subjected to correlation analysis with the tertiary oxidation ratios of DCA detected in serum and urine samples. The results confirmed that the predosing serum ratios of DCA oxidation, DCA-5 β -ol/DCA, and DCA-1 β -ol/DCA were significantly and positively correlated both intraindividually and interindividually with oral MDZ clearance. It was therefore concluded that the tertiary oxidation of DCA is predictive of CYP3A activity in beagle dogs. Clinical transitional studies following the preclinical evidence are promising to provide novel biomarkers of the enterohepatic CYP3A activities. SIGNIFICANCE STATEMENT: Drug development, clinical pharmacology, and therapeutics are under insistent demands of endogenous CYP3A biomarkers that avoid unnecessary drug exposure and invasive sampling. This work has provided the first proof-of-concept preclinical evidence that the CYP3A catalyzed tertiary oxidation of deoxycholate, the major circulating secondary bile acid synthesized in the lower gut by bacteria, may be developed as novel in vivo biomarkers of the enterohepatic CYP3A activities., (Copyright © 2021 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2021

14. Topical application of nanoparticles integrated supramolecular hydrogels for the potential treatment of seborrhoeic dermatitis.

Author

Garg A, Singh C, Pradhan D, Ghosh G, and Rath G

Subjects

Administration, Topical, Animals, Antifungal Agents administration & dosage, Antifungal Agents chemistry, Antifungal Agents metabolism, Dermatitis, Seborrheic metabolism, Goats, HeLa Cells, Humans, Hydrogels chemistry, Hydrogels metabolism, Ketoconazole administration & dosage, Ketoconazole chemistry, Ketoconazole metabolism, Male, Nanoparticles chemistry, Nanoparticles metabolism, Organ Culture Techniques, Particle Size, Rats, Rats, Wistar, Selenium administration & dosage, Selenium chemistry, Selenium metabolism, Skin Absorption physiology, Treatment Outcome, Dermatitis, Seborrheic drug therapy, Hydrogels administration & dosage, Nanoparticles administration & dosage, Skin Absorption drug effects

Abstract

The current application was aimed to evaluate the therapeutic potential of selenium and ketoconazole nanoparticles loaded hyaluronic acid gel against seborrhoeic dermatitis (SD). Amalgamation of ketoconazole (antifungal medication) and selenium (pro-oxidant) in an optimized formulation setting may help in the treatment of SD. In this study, selenium and ketoconazole nanoparticles loaded hyaluronic acid (HA) hydrogel was prepared by mechanical mixing followed by sonication. Results of the optimized batch showed a mean particle size of 121 ± 12 nm for ketoconazole and 51 ± 7 nm for selenium. SEM and TEM study revealed the prepared nanoparticles are of nanoscale dimension, with smooth spherical outline. Finally, the optimized nanoparticles were incorporated into HA hydrogel. Hydrogel exhibits desirable physical, mechanical and rheological characteristics appropriate for topical application. Optimized gel formulation exhibited an enhanced permeability with better antifungal, and anti-inflammatory activities, compared with the plain drug suspension. The optimized hydrogel with ketoconazole and selenium in nanotemplate could offer a potential strategy for the treatment of SD.

Published

2020

15. Development and Validation of Sample Preparation and an HPLC Analytical Method for Dissolution Testing in Fed-State Simulated Gastric Fluid-Illustrating Its Application for Ibuprofen and Ketoconazole Immediate Release Tablets.

Author

Shah HS, Sardhara R, Nahar K, Xu T, Delvadia P, Siddiqui A, Gao Z, Selen A, and Morris K

Subjects

Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal metabolism, Antifungal Agents chemistry, Antifungal Agents metabolism, Chromatography, High Pressure Liquid methods, Ibuprofen chemistry, Ketoconazole chemistry, Reproducibility of Results, Solubility, Tablets, Drug Development methods, Gastric Acid metabolism, Ibuprofen metabolism, Ketoconazole metabolism

Abstract

Dissolution testing and solubility determinations in different biorelevant media have gained considerable interest in the pharmaceutical industry from early-stage development of new products to forecasting bioequivalence. Among all biorelevant fluids, the preparation of fed-state simulated gastric fluid (FeSSGF) and handling of samples from dissolution/solubility testing in FeSSGF is considered to be relatively challenging. Challenges include maintaining the stability of FeSSGF medium upon sampling, filtration, and mitigating analytical interference of excipients and milk components. To overcome these challenges, standard and uniform working practices are required that are not only helpful in preparation of stable FeSSGF but also serve as a harmonizing guide for the collection of dissolution/solubility samples and their subsequent processing (i.e., handling and assay). The optimization of sample preparation methodology is crucial to reduce method-related variance by ensuring specificity, robustness, and reproducibility with acceptable recovery of the analytes. The sample preparation methodology includes a combination of techniques including filtration, solvent treatment, and centrifugation to remove the interfering media-related components and excipients from the analyte. The analytes of interest were chromatographically separated from the interfering analytes to quantify the drug concentration using the new high-performance liquid chromatography methods with ultraviolet detection. The methods developed allow rapid sample preparation, acceptable specificity, reproducible recoveries (greater than 95% of label claim), and quantification of study drugs (ibuprofen and ketoconazole). The sample preparation technique and method considerations provided here for ibuprofen and ketoconazole can serve as a starting point for solubility and dissolution testing of other small molecules in FeSSGF.

Published

2020

16. Nano-elastic liposomes as multidrug carrier of sodium stibogluconate and ketoconazole: A potential new approach for the topical treatment of cutaneous Leishmaniasis.

Author

Dar MJ, Khalid S, Varikuti S, Satoskar AR, and Khan GM

Subjects

Administration, Topical, Animals, Antimony Sodium Gluconate metabolism, Antiprotozoal Agents metabolism, Drug Carriers administration & dosage, Drug Carriers metabolism, Female, Ketoconazole metabolism, Leishmaniasis, Cutaneous metabolism, Liposomes, Mice, Mice, Inbred BALB C, Nanoparticles metabolism, Organ Culture Techniques, Random Allocation, Skin drug effects, Skin metabolism, Antimony Sodium Gluconate administration & dosage, Antiprotozoal Agents administration & dosage, Elasticity, Ketoconazole administration & dosage, Leishmaniasis, Cutaneous drug therapy, Nanoparticles administration & dosage

Abstract

The present study evaluates the efficacy of sodium stibogluconate (SSG) co-loaded with ketoconazole (KTZ) in nano-elastic liposomes (NELs) for the topical treatment of cutaneous leishmaniasis (CL). SSG-KTZ co-loaded NELs were developed and assessed for various physicochemical properties and anti-leishmanial potential. The optimized nano-vesicles have an average size of 212.8 ± 3.1 nm and entrapment efficiency of 61.2 ± 2.9%. SSG-KTZ co-loaded NELs displayed 5.37-fold higher skin permeation of SSG as compared to drug solution. SSG and KTZ displayed a synergistic interaction and flow cytometry revealed enhanced killing of DsRed Leishmania mexicana in infected macrophages. In-vitro and in-vivo anti-leishmanial studies indicated a 10.67-fold lower IC 50 value and a 35.33-fold reduced parasitic burden as compared with plain SSG solution, respectively. SSG-KTZ co-loaded NELs were found to be a promising approach for the topical treatment of CL., Competing Interests: Declaration of Competing Interest None, (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

17. Piperine Is a Mechanism-Based Inactivator of CYP3A.

Author

Cui T, Wang Q, Tian X, Zhang K, Peng Y, and Zheng J

Subjects

Catalase metabolism, Enzyme Inhibitors metabolism, Humans, Ketoconazole metabolism, Kinetics, Metabolic Clearance Rate physiology, Microsomes, Liver, NADP metabolism, Superoxide Dismutase metabolism, Alkaloids metabolism, Benzodioxoles metabolism, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors metabolism, Piperidines metabolism, Polyunsaturated Alkamides metabolism

Abstract

Piperine (PPR) is the representative alkaloid component of the piper species (family: Piperaceae). Our rapid screening study found PPR caused time-dependent inhibition of cytochrome P450s (CYP) 3A and 2D6, and CYP3A was inactivated the most. Further study demonstrated that PPR is a time-, concentration-, and NADPH-dependent inhibitor of CYP3A, and significant loss (49.5% ± 3.9%) of CYP3A activity was observed after 20minute incubations with 80 μ M PPR at 37°C. The values of K I and k inact were 30.7 μ M and 0.041 minutes -1 , respectively. CYP3A competitive inhibitor ketoconazole showed protective effect against the enzyme inactivation. Superoxide dismutase/catalase and GSH displayed minor protection against the PPR-caused enzyme inactivation. Ferricyanide partially reduced the enzyme inhibition by PPR. Additionally, NADPH-dependent formation of reactive metabolites from PPR were found in human liver microsomal incubation mixtures. An ortho -quinone intermediate was trapped by NAC in microsomal incubations with PPR. DM-PPR, demethylene metabolite of PPR, showed weak enzyme inactivation relative to that caused by PPR. It appears that both carbene and ortho -quinone intermediates were involved in the inactivation of CYP3A caused by PPR. SIGNIFICANCE STATEMENT: CYP3A subfamily members (mainly CYP3A4 and CYP3A5) play a critical role in drug metabolism. Piperine (PPR), a methylenedioxyphenyl derivative combined with an unsaturated ketone, is the major active ingredient of pepper. PPR revealed time-, concentration-, and NADPH-dependent inhibitory effect on CYP3A. Carbene and quinone metabolites were both involved in the observed CYP3A inactivation by PPR. Apparently, the unsaturated ketone moiety did not participate in the enzyme inactivation. The present study sounds an alert of potential risk for food-drug interactions., (Copyright © 2020 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2020

18. Conformational Response of N-Terminally Truncated Cytochrome P450 3A4 to Ligand Binding in Solution.

Author

Chuo SW, Liou SH, Wang LP, Britt RD, Poulos TL, Sevrioukova IF, and Goodin DB

Subjects

Electron Spin Resonance Spectroscopy methods, Humans, Ketoconazole chemistry, Ketoconazole metabolism, Ligands, Protein Binding physiology, Protein Conformation, Protein Structure, Secondary, Ritonavir chemistry, Ritonavir metabolism, Cytochrome P-450 CYP3A chemistry, Cytochrome P-450 CYP3A metabolism, Molecular Dynamics Simulation

Abstract

Human cytochrome P450 3A4 (CYP3A4) is a membrane-associated monooxygenase that is responsible for metabolizing >50% of the pharmaceuticals in the current market, so studying its chemical mechanism and structural changes upon ligand binding will help provide deeper insights into drug metabolism and further drug development. The best-characterized cytochrome P450 is a bacterial form, P450cam, which undergoes significant conformational changes upon binding substrate and its redox partner, putidaredoxin. In contrast, most crystal structures of CYP3A4 with or without ligands have shown few changes, although allosteric effects and multiple-substrate binding in solution are well-documented. In this study, we use double electron-electron resonance (DEER) to measure distances between spatially separated spin-labels on CYP3A4 and molecular dynamics to interpret the DEER data. These methods were applied to a soluble N-terminally truncated CYP3A4 form, and the results show that there are few changes in the average structure upon binding ketoconazole, ritonavir, or midazolam. However, binding of midazolam, but not ketoconazole or ritonavir, resulted in a significant change in the motion and/or disorder in the F/G helix region near the substrate binding pocket. These results suggest that soluble CYP3A4 behaves in a unique way in response to inhibitor and substrate binding.

Published

2019

19. Characterization of Genetic Variation in CYP3A4 on the Metabolism of Cabozantinib in Vitro.

Author

Lin QM, Li YH, Lu XR, Wang R, Pang NH, Xu RA, Cai JP, and Hu GX

Subjects

Alleles, Cytochrome P-450 CYP3A genetics, Genetic Variation genetics, Humans, Ketoconazole metabolism, Kinetics, Liver enzymology, Anilides metabolism, Cytochrome P-450 CYP3A metabolism, Protein Kinase Inhibitors metabolism, Pyridines metabolism

Abstract

Cabozantinib is a multityrosine kinase inhibitor and has a wide range of applications in the clinic, whose metabolism is predominately dependent on CYP3A4. This study was performed to characterize the enzymatic properties of 29 CYP3A4 alleles toward cabozantinib and the functional changes of five selected alleles (the wild-type, CYP3A4.2.8.14 and .15) toward cabozantinib in the presence of ketoconazole. Cabozantinib, 1-100 μM, with/without the presence of ketoconazole and CYP3A4 enzymes in the incubation system went through 30 min incubation at 37 °C, and the concentrations of cabozantinib N-oxide were quantified by UPLC-MS/MS to calculate the corresponding kinetic parameters of each variant. Collectively, without the presence of ketoconazole, most variants displayed defective enzymatic activities in different degrees, and only CYP3A4.14 and .15 showed significantly augmented enzymatic activities. With the presence of ketoconazole, five tested CYP3A4 alleles, even CYP3A4.14 and .15, exhibited obvious reductions in intrinsic clearance. Besides, we compared cabozantinib with regorafenib in relative clearance to confirm that CYP3A4 has the property of substrate specificity. As the first study of CYP3A4 genetic polymorphisms toward cabozantinib, our observations can provide prediction of an individual's capability in response to cabozantinib and guidance for medication and treatment of cabozantinib.

Published

2019

20. Modeling of Hepatic Drug Metabolism and Responses in CYP2C19 Poor Metabolizer Using Genetically Manipulated Human iPS cells.

Author

Deguchi S, Yamashita T, Igai K, Harada K, Toba Y, Hirata K, Takayama K, and Mizuguchi H

Subjects

Cell Differentiation physiology, Cell Line, Cell Survival physiology, Chemical and Drug Induced Liver Injury metabolism, Clopidogrel pharmacology, Hepatocytes metabolism, Humans, Ketoconazole pharmacology, Clopidogrel metabolism, Cytochrome P-450 CYP2C19 metabolism, Induced Pluripotent Stem Cells metabolism, Ketoconazole metabolism, Liver metabolism, Metabolic Clearance Rate physiology

Abstract

Cytochrome P450 family 2 subfamily C member 19 (CYP2C19), in liver, plays important roles in terms of drug metabolism. It is known that CYP2C19 poor metabolizers (PMs) lack CYP2C19 metabolic capacity. Thus, unexpected drug-induced liver injury or decrease of drug efficacy would be caused in CYP2C19 substrate-treated CYP2C19 PMs. However, it is difficult to evaluate the safety and effectiveness of drugs and candidate compounds for CYP2C19 PMs because there is currently no model for this phenotype. Here, using human induced pluripotent stem cells (human iPS cells) and our highly efficient genome-editing and hepatocyte differentiation technologies, we generated CYP2C19-knockout human iPS cell-derived hepatocyte-like cells (CYP2C19-KO HLCs) as a novel CYP2C19 PM model for drug development and research. The gene expression levels of hepatocyte markers were similar between wild-type iPS cell-derived hepatocyte-like cells (WT HLCs) and CYP2C19-KO HLCs, suggesting that CYP2C19 deficiency did not affect the hepatic differentiation potency. We also examined CYP2C19 metabolic activity by measuring S -mephenytoin metabolites using ultra-performance liquid chromatography-tandem mass spectrometry. The CYP2C19 metabolic activity was almost eliminated by CYP2C19 knockout. Additionally, we evaluated whether clopidogrel (CYP2C19 substrate)-induced liver toxicity could be predicted using our model. Unexpectedly, there was no significant difference in cell viability between clopidogrel-treated WT HLCs and CYP2C19-KO HLCs. However, the cell viability in clopidogrel- and ketoconazole (CYP3A4 inhibitor)-treated CYP2C19-KO HLCs was significantly enhanced as compared with that in clopidogrel- and DMSO-treated CYP2C19-KO HLCs. This result suggests that CYP2C19-KO HLCs can predict clopidogrel-induced liver toxicity. We succeeded in generating CYP2C19 PM model cells using human iPS cells and genome-editing technologies for pharmaceutical research. SIGNIFICANCE STATEMENT: Although unexpected drug-induced liver injury or decrease of drug efficacy would be caused in CYP2C19 substrate-treated CYP2C19 poor metabolizers, it is difficult to evaluate the safety and effectiveness of drugs and candidate compounds for CYP2C19 poor metabolizers because there is currently no model for this phenotype. Using human iPS cells and our highly efficient genome editing and hepatocyte differentiation technologies, we generated CYP2C19-knockout human iPS cell-derived hepatocyte-like cells as a novel CYP2C19 poor metabolizer model for drug development and research., (Copyright © 2019 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2019

21. Drug-drug interaction (DDI) assessments of ruxolitinib, a dual substrate of CYP3A4 and CYP2C9, using a verified physiologically based pharmacokinetic (PBPK) model to support regulatory submissions.

Author

Umehara K, Huth F, Jin Y, Schiller H, Aslanis V, Heimbach T, and He H

Subjects

Administration, Oral, Caco-2 Cells, Drug Interactions, Erythromycin administration & dosage, Erythromycin metabolism, Erythromycin pharmacokinetics, Humans, Ketoconazole administration & dosage, Ketoconazole metabolism, Ketoconazole pharmacokinetics, Nitriles, Pyrazoles administration & dosage, Pyrimidines, Rifampin administration & dosage, Rifampin metabolism, Rifampin pharmacokinetics, Cytochrome P-450 CYP2C9 metabolism, Cytochrome P-450 CYP3A metabolism, Models, Biological, Pyrazoles metabolism, Pyrazoles pharmacokinetics

Abstract

Ruxolitinib is mainly metabolized by cytochrome P450 (CYP) enzymes CYP3A4 and CYP2C9 followed by minor contributions of other hepatic CYP enzymes in vitro. A physiologically based pharmacokinetic (PBPK) model was established to evaluate the changes in the ruxolitinib systemic exposures with co-administration of CYP3A4 and CYP2C9 perpetrators. The fractions metabolized in the liver via oxidation by CYP enzymes (fm,CYP3A4 = 0.75, fm,CYP2C9 = 0.19, and fm,CYPothers = 0.06) for an initial ruxolitinib model based on in vitro data were optimized (0.43, 0.56, and 0.01, respectively) using the observed exposure changes of ruxolitinib (10 mg) with co-administered ketoconazole (200 mg). The reduced amount of fm,CYP3A4 was distributed to fm,CYP2C9. For the initial ruxolitinib model with co-administration of ketoconazole, the area under the curve (AUC) increase of 2.60-fold was over-estimated compared with the respective observation (1.91-fold). With the optimized fm values, the predicted AUC ratio was 1.82. The estimated AUC ratios of ruxolitinib by co-administration of the moderate CYP3A4 inhibitor erythromycin (500 mg) and the strong CYP3A4 inducer rifampicin (600 mg) were within a 20% error compared with the clinically observed values. The PBPK modeling results may provide information on the labeling, i.e. supporting a dose reduction by half for co-administration of strong CYP3A4 inhibitors. Furthermore, an AUC increase of ruxolitinib in the absence or presence of the dual CYP3A4 and CYP2C9 inhibitor fluconazole (100-400 mg) was prospectively estimated to be 1.94- to 4.31-fold. Fluconazole simulation results were used as a basis for ruxolitinib dose adjustment when co-administering perpetrator drugs. A ruxolitinib PBPK model with optimized fm,CYP3A4 and fm,CYP2C9 was established to evaluate victim DDI risks. The previous minimal PBPK model was supported by the FDA for the dose reduction strategy, halving the dose with the concomitant use of strong CYP3A4 inhibitors and dual inhibitors on CYP2C9 and CYP3A4, such as fluconazole at ≤200 mg. Fluconazole simulation results were used as supportive evidence in discussions with the FDA and EMA about ruxolitinib dose adjustment when co-administering perpetrator drugs. Thus, this study demonstrated that PBPK modeling can support characterizing DDI liabilities to inform the drug label and might help reduce the number of clinical DDI studies by simulations of untested scenarios, when a robust PBPK model is established.

Published

2019

22. Simultaneous Prediction of Intestinal Absorption and Metabolism Using the Mini-Ussing Chamber System.

Author

Kondo S and Miyake M

Subjects

Animals, Drug Delivery Systems methods, Ketoconazole metabolism, Male, Midazolam metabolism, Nifedipine metabolism, Permeability, Rats, Rats, Sprague-Dawley, Intestinal Absorption physiology, Intestinal Mucosa metabolism, Pharmaceutical Preparations metabolism

Abstract

The purpose of this study was to investigate the possibility of simultaneous prediction of the intestinal absorption and metabolism in a mini-Ussing chamber equipped with rat intestinal tissues, based on the transport index (TI). TI value was defined as the sum of drug amounts, by mass balance method, transported to the basal-side component and drug amounts accumulated in the tissue, which are normalized by area under the curve of the drug in the apical compartment. Midazolam and nifedipine with high permeability were used as typical P450 substrates to examine the possibility of simultaneous prediction of intestinal absorption and metabolism. The metabolite formation of both compounds was observed and ketoconazole strongly inhibited the metabolite formation of both compounds in rat intestinal tissues, leading to the improvement of the TI value to a statistically significant extent for both compounds. TI ratio of nifedipine between in the presence and absence of ketoconazole was larger than that of midazolam, which was consistent with the reported lower value of fraction absorbed multiplied by intestinal availability of nifedipine. Therefore, the mini-Ussing chamber, equipped with animal intestinal tissues, showed potential to predict the intestinal absorption and metabolism simultaneously., (Copyright © 2019 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2019

23. Cytochromes P450 1A2 and 3A4 Catalyze the Metabolic Activation of Sunitinib.

Author

Amaya GM, Durandis R, Bourgeois DS, Perkins JA, Abouda AA, Wines KJ, Mohamud M, Starks SA, Daniels RN, and Jackson KD

Subjects

Biocatalysis, Chromatography, High Pressure Liquid, Cytochrome P-450 CYP1A2 chemistry, Cytochrome P-450 CYP1A2 genetics, Cytochrome P-450 CYP3A chemistry, Cytochrome P-450 CYP3A genetics, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Glutathione chemistry, Humans, Ketoconazole chemistry, Ketoconazole metabolism, Kinetics, Microsomes, Liver metabolism, Quinones chemistry, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Recombinant Proteins isolation & purification, Spectrophotometry, Ultraviolet, Sunitinib analysis, Tandem Mass Spectrometry, Cytochrome P-450 CYP1A2 metabolism, Cytochrome P-450 CYP3A metabolism, Sunitinib metabolism

Abstract

Sunitinib is a multitargeted tyrosine kinase inhibitor associated with idiosyncratic hepatotoxicity. The mechanisms of this toxicity are unknown. We hypothesized that sunitinib undergoes metabolic activation to form chemically reactive, potentially toxic metabolites which may contribute to development of sunitinib-induced hepatotoxicity. The purpose of this study was to define the role of cytochrome P450 (P450) enzymes in sunitinib bioactivation. Metabolic incubations were performed using individual recombinant P450s, human liver microsomal fractions, and P450-selective chemical inhibitors. Glutathione (GSH) and dansylated GSH were used as trapping agents to detect reactive metabolite formation. Sunitinib metabolites were analyzed by liquid chromatography-tandem mass spectrometry. A putative quinoneimine-GSH conjugate (M5) of sunitinib was detected from trapping studies with GSH and dansyl-GSH in human liver microsomal incubations, and M5 was formed in an NADPH-dependent manner. Recombinant P450 1A2 generated the highest levels of defluorinated sunitinib (M3) and M5, with less formation by P450 3A4 and 2D6. P450 3A4 was the major enzyme forming the primary active metabolite N-desethylsunitinib (M1). In human liver microsomal incubations, P450 3A inhibitor ketoconazole reduced formation of M1 by 88%, while P450 1A2 inhibitor furafylline decreased generation of M5 by 62% compared to control levels. P450 2D6 and P450 3A inhibition also decreased M5 by 54 and 52%, respectively, compared to control. In kinetic assays, recombinant P450 1A2 showed greater efficiency for generation of M3 and M5 compared to that of P450 3A4 and 2D6. Moreover, M5 formation was 2.7-fold more efficient in human liver microsomal preparations from an individual donor with high P450 1A2 activity compared to a donor with low P450 1A2 activity. Collectively, these data suggest that P450 1A2 and 3A4 contribute to oxidative defluorination of sunitinib to generate a reactive, potentially toxic quinoneimine. Factors that alter P450 1A2 and 3A activity may affect patient risk for sunitinib toxicity.

Published

2018

24. Metabolism of a 5HT 6 Antagonist, 2-Methyl-1-(Phenylsulfonyl)-4-(Piperazin-1-yl)-1H-Benzo[d]imidazole (SAM-760): Impact of Sulfonamide Metabolism on Diminution of a Ketoconazole-Mediated Clinical Drug-Drug Interaction.

Author

Sawant-Basak A, Obach RS, Doran A, Lockwood P, Schildknegt K, Gao H, Mancuso J, Tse S, and Comery TA

Subjects

Cytochrome P-450 CYP2C19 metabolism, Cytochrome P-450 CYP2D6 metabolism, Cytochrome P-450 CYP3A Inhibitors metabolism, Hepatocytes metabolism, Humans, Isoenzymes metabolism, Microsomes, Liver metabolism, Piperazine, Drug Interactions physiology, Imidazoles metabolism, Ketoconazole metabolism, Piperazines metabolism, Receptors, Serotonin metabolism, Selective Serotonin Reuptake Inhibitors metabolism, Sulfonamides metabolism

Abstract

SAM-760 [(2-methyl-1-(phenylsulfonyl)-4-(piperazin-1-yl)-1H-benzo[d]imidazole)], a 5HT 6 antagonist, was investigated in humans for the treatment of Alzheimer's disease. In liver microsomes and recombinant cytochrome P450 (P450) isozymes, SAM-760 was predominantly metabolized by CYP3A (∼85%). Based on these observations and an expectation of a 5-fold magnitude of interaction with moderate to strong CYP3A inhibitors, a clinical DDI study was performed. In the presence of ketoconazole, the mean C max and area under the plasma concentration-time curve from time zero extrapolated to infinite time values of SAM-760 showed only a modest increase by 30% and 38%, respectively. In vitro investigation of this unexpectedly low interaction was undertaken using [ 14 C]SAM-760. Radiometric profiling in human hepatocytes confirmed all oxidative metabolites previously observed with unlabeled SAM-760; however, the predominant radiometric peak was an unexpected polar metabolite that was insensitive to the pan-P450 inhibitor 1-aminobenzotriazole. In human hepatocytes, radiometric integration attributed 43% of the total metabolism of SAM-760 to this non-P450 pathway. Using an authentic standard, this predominant metabolite was confirmed as benzenesulfinic acid. Additional investigation revealed that the benzenesulfinic acid metabolite may be a novel, nonenzymatic, thiol-mediated reductive cleavage of an aryl sulfonamide group of SAM-760. We also determined the relative contribution of P450 to the metabolism of SAM-760 in human hepatocytes by following the rate of formation of oxidative metabolites in the presence and absence of P450 isoform-specific inhibitors. The P450-mediated oxidative metabolism of SAM-760 was still primarily attributed to CYP3A (33%), with minor contributions from P450 isoforms CYP2C19 and CYP2D6. Thus, the disposition of [ 14 C]SAM-760 in human hepatocytes via novel sulfonamide metabolism and CYP3A verified the lower than expected clinical DDI when SAM-760 was coadministered with ketoconazole., (Copyright © 2018 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2018

25. Development and applications of a physiologically-based model of paediatric oral drug absorption.

Author

Johnson TN, Bonner JJ, Tucker GT, Turner DB, and Jamei M

Subjects

Acetaminophen chemistry, Acetaminophen metabolism, Administration, Oral, Adolescent, Adult, Biopharmaceutics methods, Chemistry, Pharmaceutical methods, Child, Child, Preschool, Gastrointestinal Tract metabolism, Humans, Infant, Infant, Newborn, Intestinal Absorption drug effects, Ketoconazole chemistry, Ketoconazole metabolism, Solubility drug effects, Theophylline chemistry, Theophylline metabolism, Young Adult, Pharmaceutical Preparations chemistry, Pharmaceutical Preparations metabolism

Abstract

There is increasing interest in paediatric drug absorption and the development of biopharmaceutics tools to facilitate the development of oral formulations for neonates, infants and children. We describe the development and application of a physiologically-based model of paediatric drug absorption applicable from full term birth onwards. Paediatric age-specific parameters were included for salivary flow, gastric pH, gastric emptying (and associated food effects) and duodenal bile salt concentrations and the associated algorithms were integrated into a dissolution, absorption and metabolism model as part of a PBPK platform. For other parameters, there was either evidence for no age-related changes or a lack of data, so that adult values were applied. An initial assessment of the model was carried out by simulating the oral absorption of theophylline, paracetamol and ketoconazole over a range of paediatric ages. The absorption of the first two drugs, both BCS class 1 compounds, was predicted to be slower in early neonates compared to older age groups (median t max values of 3 vs 2h, respectively), but with invariant fraction absorbed (fa). This is in agreement with clinical observations. The t max of ketoconazole, a BCS class 2 compound, was predicted to be about 1h in both neonates and adults, but the fa value was higher in the former (0.87 vs 0.69). There is clearly a need to expand the components of the model as new information on the ontogeny of GI tract parameters becomes available, and to assess it against more in vivo data with evidence of specific age-related changes in oral drug absorption., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

26. Simultaneous Physiologically Based Pharmacokinetic (PBPK) Modeling of Parent and Active Metabolites to Investigate Complex CYP3A4 Drug-Drug Interaction Potential: A Case Example of Midostaurin.

Author

Gu H, Dutreix C, Rebello S, Ouatas T, Wang L, Chun DY, Einolf HJ, and He H

Subjects

Adult, Biomarkers metabolism, Cytochrome P-450 CYP3A Inducers metabolism, Cytochrome P-450 CYP3A Inducers pharmacokinetics, Cytochrome P-450 CYP3A Inhibitors metabolism, Cytochrome P-450 CYP3A Inhibitors pharmacokinetics, Female, Humans, Hydroxycholesterols metabolism, Ketoconazole metabolism, Ketoconazole pharmacokinetics, Male, Midazolam metabolism, Midazolam pharmacokinetics, Middle Aged, Models, Biological, Rifampin metabolism, Rifampin pharmacokinetics, Staurosporine metabolism, Staurosporine pharmacokinetics, Young Adult, Cytochrome P-450 CYP3A metabolism, Drug Interactions physiology, Staurosporine analogs & derivatives

Abstract

Midostaurin (PKC412) is being investigated for the treatment of acute myeloid leukemia (AML) and advanced systemic mastocytosis (advSM). It is extensively metabolized by CYP3A4 to form two major active metabolites, CGP52421 and CGP62221. In vitro and clinical drug-drug interaction (DDI) studies indicated that midostaurin and its metabolites are substrates, reversible and time-dependent inhibitors, and inducers of CYP3A4. A simultaneous pharmacokinetic model of parent and active metabolites was initially developed by incorporating data from in vitro, preclinical, and clinical pharmacokinetic studies in healthy volunteers and in patients with AML or advSM. The model reasonably predicted changes in midostaurin exposure after single-dose administration with ketoconazole (a 5.8-fold predicted versus 6.1-fold observed increase) and rifampicin (90% predicted versus 94% observed reduction) as well as changes in midazolam exposure (1.0 predicted versus 1.2 observed ratio) after daily dosing of midostaurin for 4 days. The qualified model was then applied to predict the DDI effect with other CYP3A4 inhibitors or inducers and the DDI potential with midazolam under steady-state conditions. The simulated midazolam area under the curve ratio of 0.54 and an accompanying observed 1.9-fold increase in the CYP3A4 activity of biomarker 4 β -hydroxycholesterol indicated a weak-to-moderate CYP3A4 induction by midostaurin and its metabolites at steady state in patients with advSM. In conclusion, a simultaneous parent-and-active-metabolite modeling approach allowed predictions under steady-state conditions that were not possible to achieve in healthy subjects. Furthermore, endogenous biomarker data enabled evaluation of the net effect of midostaurin and its metabolites on CYP3A4 activity at steady state and increased confidence in DDI predictions., (Copyright © 2018 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2018

27. Modulation of the interaction between human P450 3A4 and B. megaterium reductase via engineered loops.

Author

Castrignanò S, D'Avino S, Di Nardo G, Catucci G, Sadeghi SJ, and Gilardi G

Subjects

Bacillus megaterium enzymology, Bacterial Proteins antagonists & inhibitors, Bacterial Proteins genetics, Bacterial Proteins metabolism, Binding Sites, Cytochrome P-450 CYP3A genetics, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors metabolism, Gene Expression, Humans, Ketoconazole metabolism, Kinetics, Ligands, Molecular Docking Simulation, NADPH-Ferrihemoprotein Reductase antagonists & inhibitors, NADPH-Ferrihemoprotein Reductase genetics, NADPH-Ferrihemoprotein Reductase metabolism, Protein Binding, Protein Conformation, alpha-Helical, Protein Conformation, beta-Strand, Protein Engineering, Protein Interaction Domains and Motifs, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Structure-Activity Relationship, Substrate Specificity, Testosterone chemistry, Testosterone metabolism, Bacillus megaterium genetics, Bacterial Proteins chemistry, Cytochrome P-450 CYP3A chemistry, Cytochrome P-450 CYP3A Inhibitors chemistry, Ketoconazole chemistry, NADPH-Ferrihemoprotein Reductase chemistry, Recombinant Fusion Proteins chemistry

Abstract

Chimerogenesis involving cytochromes P450 is a successful approach to generate catalytically self-sufficient enzymes. However, the connection between the different functional modules should allow a certain degree of flexibility in order to obtain functional and catalytically efficient proteins. We previously applied the molecular Lego approach to develop a chimeric P450 3A4 enzyme linked to the reductase domain of P450 BM3 (BMR). Three constructs were designed with the connecting loop containing no glycine, 3 glycine or 5 glycine residues and showed a different catalytic activity and coupling efficiency. Here we investigate how the linker affects the ability of P450 3A4 to bind substrates and inhibitors. We measure the electron transfer rates and the catalytic properties of the enzyme also in the presence of ketoconazole as inhibitor. The data show that the construct 3A4-5GLY-BMR with the longest loop better retains the binding ability and cooperativity for testosterone, compared to P450 3A4. In both 3A4-3GLY-BMR and 3A4-5GLY-BMR, the substrate induces an increase in the first electron transfer rate and a shorter lag phase related to a domain rearrangements, when compared to the construct without Gly. These data are consistent with docking results and secondary structure predictions showing a propensity to form helical structures in the loop of the 3A4-BMR and 3A4-3GLY-BMR. All three chimeras retain the ability to bind the inhibitor ketoconazole and show an IC 50 comparable with those reported for the wild type protein. This article is part of a Special Issue entitled: Cytochrome P450 biodiversity and biotechnology, edited by Erika Plettner, Gianfranco Gilardi, Luet Wong, Vlada Urlacher, Jared Goldstone., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

28. The Combination of GIS and Biphasic to Better Predict In Vivo Dissolution of BCS Class IIb Drugs, Ketoconazole and Raloxifene.

Author

Tsume Y, Igawa N, Drelich AJ, Amidon GE, and Amidon GL

Subjects

Chemistry, Pharmaceutical methods, Computer Simulation, Drug Liberation physiology, Humans, Intestinal Absorption physiology, Models, Biological, Permeability, Solubility, Gastrointestinal Tract metabolism, Ketoconazole chemistry, Ketoconazole metabolism, Raloxifene Hydrochloride chemistry, Raloxifene Hydrochloride metabolism

Abstract

The formulation developments and the in vivo assessment of Biopharmaceutical Classification System (BCS) class II drugs are challenging due to their low solubility and high permeability in the human gastrointestinal (GI) tract. Since the GI environment influences the drug dissolution of BCS class II drugs, the human GI characteristics should be incorporated into the in vitro dissolution system to predict bioperformance of BCS class II drugs. An absorptive compartment may be important in dissolution apparatus for BCS class II drugs, especially for bases (BCS IIb) because of high permeability, precipitation, and supersaturation. Thus, the in vitro dissolution system with an absorptive compartment may help predicting the in vivo phenomena of BCS class II drugs better than compendial dissolution apparatuses. In this study, an absorptive compartment (a biphasic device) was introduced to a gastrointestinal simulator. This addition was evaluated if this in vitro system could improve the prediction of in vivo dissolution for BCS class IIb drugs, ketoconazole and raloxifene, and subsequent absorption. The gastrointestinal simulator is a practical in vivo predictive tool and exhibited an improved in vivo prediction utilizing the biphasic format and thus a better tool for evaluating the bioperformance of BCS class IIb drugs than compendial apparatuses., (Copyright © 2018. Published by Elsevier Inc.)

Published

2018

29. Evaluation of intestinal metabolism and absorption using the Ussing chamber system equipped with intestinal tissue from rats and dogs.

Author

Miyake M, Kondo S, Koga T, Yoda N, Nakazato S, Emoto C, Mukai T, and Toguchi H

Subjects

Animals, Biological Transport drug effects, Dogs, Male, Permeability drug effects, Rats, Rats, Sprague-Dawley, Intestinal Absorption physiology, Intestinal Mucosa metabolism, Ketoconazole metabolism

Abstract

The purpose of this study was to evaluate the intestinal metabolism and absorption in a mini-Ussing chamber equipped with animal intestinal tissues, based on the transport index (TI). TI value was defined as the sum of drug amounts transported to the basal-side component (X corr ) and drug amounts accumulated in the tissue (T corr ), which are normalized by AUC of a drug in the apical compartment, as an index for drug absorption. Midazolam was used as a test compound for the evaluation of intestinal metabolism and absorption. The metabolite formulation of midazolam was observed in both rats and dogs. Ketoconazole inhibited the intestinal metabolism of midazolam in rats and improved its intestinal absorption to a statistically significant extent. Therefore, the mini-Ussing chamber, equipped with animal intestinal tissues, showed potential to use the evaluation of the intestinal metabolism and absorption, including the assessment of species differences., (Copyright © 2017. Published by Elsevier B.V.)

Published

2018

30. Comparison of Oral Voriconazole Versus Oral Ketoconazole as an Adjunct to Topical Natamycin in Severe Fungal Keratitis: A Randomized Controlled Trial.

Author

Sharma N, Singhal D, Maharana PK, Sinha R, Agarwal T, Upadhyay AD, Velpandian T, Satpathy G, and Titiyal JS

Subjects

Administration, Oral, Administration, Topical, Adult, Aged, Antifungal Agents metabolism, Chemotherapy, Adjuvant, Drug Therapy, Combination, Female, Humans, Keratitis microbiology, Ketoconazole metabolism, Male, Middle Aged, Ophthalmic Solutions therapeutic use, Tears metabolism, Visual Acuity, Voriconazole metabolism, Antifungal Agents administration & dosage, Eye Infections, Fungal drug therapy, Keratitis drug therapy, Ketoconazole administration & dosage, Natamycin administration & dosage, Voriconazole administration & dosage

Abstract

Purpose: To compare the efficacy of oral voriconazole (VCZ) with oral ketoconazole (KCZ) as an adjunct to topical natamycin in severe fungal keratitis., Methods: Fifty eyes of 50 patients with proven severe fungal keratitis, (>5 mm size, involving >4 mm central cornea and >50% stromal depth), smear, and/or culture positive were randomized to receive either oral VCZ (n = 25) or oral KCZ (n = 25) 200 mg twice a day. Both groups received topical natamycin along with oral medication. The primary outcome measure was best spectacle-corrected visual acuity (BSCVA) at 3 months of follow-up. Secondary outcomes were the percentage of healed cases and scar size., Results: The mean BSCVA after treatment was 1.3 ± 0.35 logarithm of minimum angle of resolution units in the VCZ group and 1.6 ± 0.39 logarithm of minimum angle of resolution units in the KCZ group [P = 0.004, 95% confidence interval (CI), -0.10 to 0.54]. The final mean scar size was smaller for oral VCZ than for oral KCZ (P = 0.04, 95% CI, -0.01 to 0.93 mm). The percentage of cases healed were 80% and 72% in VCZ and KCZ groups, respectively (P = 0.51, 95% CI, -0.15 to 0.31). The ratio of tear film to serum concentration of oral VCZ was better than oral KCZ at days 14 (P = 0.002) and 21 (P = 0.006)., Conclusions: Although the duration and percentage of healing was similar in both groups, oral VCZ attained a significantly better tear film concentration with a smaller scar size and better BSCVA compared with oral KCZ. Thus, oral VCZ may be preferred over oral KCZ in severe fungal keratitis.

Published

2017

31. Ocular ketoconazole-loaded proniosomal gels: formulation, ex vivo corneal permeation and in vivo studies.

Author

Abdelbary GA, Amin MM, and Zakaria MY

Subjects

Animals, Antifungal Agents administration & dosage, Cornea drug effects, Drug Carriers administration & dosage, Drug Liberation, Gels, Ketoconazole administration & dosage, Liposomes administration & dosage, Male, Organ Culture Techniques, Permeability drug effects, Prodrugs administration & dosage, Rabbits, Antifungal Agents metabolism, Cornea metabolism, Drug Carriers metabolism, Ketoconazole metabolism, Liposomes metabolism, Prodrugs metabolism

Abstract

Context: Vesicular drug carriers for ocular delivery have gained a real potential. Proniosomal gels as ocular drug carriers have been proven to be an effective way to improve bioavailability and patient compliance., Objective: Formulation and in vitro/ex vivo/in vivo characterization of ketoconazole (KET)-loaded proniosomal gels for the treatment of ocular keratitis., Materials and Methods: The effect of formulation variables; HLB value, type and concentration of non-ionic surfactants (Tweens, Spans, Brijs and Pluronics) with or without lecithin on the entrapment efficiency (EE%), vesicle size and in vitro KET release was evaluated. An ex vivo corneal permeation study to determine the level of KET in the external eye tissue of albino rabbits and an in vivo assessment of the level of KET in the aqueous humors were performed., Results and Discussion: In vivo evaluation showed an increase in bioavailability up to 20-folds from the optimum KET proniosomal gel formula in the aqueous humor compared to drug suspension (KET-SP). The selected formulae were composed of spans being hydrophobic suggesting the potential use of a more hydrophobic surfactant as Span during the formulation of formulae. Factors that stabilize the vesicle membrane and increase the entrapment efficiency of KET (namely low HLB, long alkyl chain, high phase transition temperature) slowed down the release profile., Conclusions: Proniosomal gels as drug delivery carriers were proven to be a promising approach to increase corneal contact and permeation as well as retention time in the eye resulting in a sustained action and enhanced bioavailability.

Published

2017

32. Characterization of 1-Aminobenzotriazole and Ketoconazole as Novel Inhibitors of Monoamine Oxidase (MAO): An In Vitro Investigation.

Author

Shaik AN, LeDuc BW, and Khan AA

Subjects

Animals, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 Enzyme Inhibitors metabolism, Cytochrome P-450 Enzyme Inhibitors pharmacology, Humans, Isoenzymes metabolism, Ketoconazole metabolism, Kinetics, Liver metabolism, Mice, Microsomes, Liver metabolism, Monoamine Oxidase Inhibitors metabolism, Rats, Triazoles metabolism, Ketoconazole pharmacology, Monoamine Oxidase metabolism, Monoamine Oxidase Inhibitors pharmacology, Triazoles pharmacology

Abstract

Background and Objectives: 1-Aminobenzotriazole, a known time-dependent inhibitor of cytochrome P450 (CYP) enzymes, and ketoconazole, a strong inhibitor of the human CYP3A4 isozyme, are used as standard probe inhibitors to characterize the CYP and/or non-CYP-mediated metabolism of xenobiotics. In the present investigation, 1-Aminobenzotriazole and ketoconazole are characterized as potent monoamine oxidase (MAO) inhibitors in vitro using mouse, rat and human liver microsomes and S9 fractions., Methods: Inhibition potential of 1-aminobenzotriazole and ketoconazole was studied in mice, rat and human liver microsomes, S9 fractions, MAO-A and MAO-B expressed enzymes by monitoring the formation of 4-hydroxyquinoline (4-HQ) from kynuramine, a specific substrate of MAO by liquid chromatography-tandem mass spectrometry (LC-MS/MS). Mechanism of MAO inhibition was studied by incubating varying concentration of kynuramine with mouse, rat and human S9 fractions at varying concentration of 1-aminobenzatriazole and ketoconazole and monitoring the formation of 4-HQ., Results: 1-aminobenzotriazole and ketoconazole inhibited both MAO isozymes (MAO-A and MAO-B) with more specificity towards MAO-B. Kynuramine substrate kinetics in mouse, rat and human S9 fractions with varying 1-aminobenzotriazole and ketoconazole concentrations showed decreased maximum rate (V max ) for 4-HQ formation without affecting the Michaelis-Menten constant (K m ). A non-competitive inhibition model was constructed and inhibition constants (K i ) for 1-aminobenzotriazole (7.87 ± 0.61, 8.61 ± 0.92, 65.2 ± 1.61 µM for mice, rat and humans, respectively) and ketoconazole (0.12 ± 0.01, 2.04 ± 0.08, 5.52 ± 0.47 µM for mice, rat and humans, respectively) were determined., Conclusions: 1-Aminobenzotriazole and ketoconazole are characterized as non-competitive inhibitors of mice, rat and human MAO in vitro and the extent of their MAO inhibition potential is species specific. 1-Aminobenzotriazole or ketoconazole can be used as a probe inhibitor in vitro for screening the involvement of MAO-dependent metabolism of new chemical entities (NCE) in early drug discovery.

Published

2017

33. Utility of CYP3A4 and PXR-CAR-CYP3A4/3A7 Transgenic Mouse Models To Assess the Magnitude of CYP3A4 Mediated Drug-Drug Interactions.

Author

Ly JQ, Messick K, Qin A, Takahashi RH, and Choo EF

Subjects

Alprazolam metabolism, Aniline Compounds metabolism, Animals, Chromatography, Liquid, Constitutive Androstane Receptor, Crizotinib, Dasatinib metabolism, Female, Humans, Itraconazole metabolism, Ketoconazole metabolism, Mice, Mice, Transgenic, Nitriles metabolism, Piperidines metabolism, Pyrazoles metabolism, Pyridines metabolism, Quinazolines metabolism, Quinolines metabolism, Rifampin metabolism, Tandem Mass Spectrometry, Triazolam metabolism, Cytochrome P-450 CYP3A metabolism, Drug Interactions

Abstract

Species differences in the expression, activity, regulation, and substrate specificity of metabolizing enzymes preclude the use of animal models to predict clinical drug-drug interactions (DDIs). The objective of this work is to determine if the transgenic (Tg) Cyp3a -/- Tg-3A4 Hep/Int and Nr1i2/Nr1i3 -/- -Cyp3a -/- Tg-PXR-CAR-3A4/3A7 Hep/Int (PXR-CAR-CYP3A4/3A7) mouse models could be used to predict in vivo DDI of 10 drugs; alprazolam, bosutinib, crizotinib, dasatinib, gefitinib, ibrutinib, regorafenib, sorafenib, triazolam, and vandetinib (as victims); with varying magnitudes of reported CYP3A4 clinical DDI. As an assessment of the effect of CYP3A4 inhibition, these drugs were coadministered to Cyp3a -/- Tg-3A4 Hep/Int mice with the CYP3A inhibitor, itraconazole. For crizotinib, regorafenib, sorafenib, and vandetanib, there was no significant increase of AUC observed; with alprazolam, bosutinib, ibrutinib, dasatinib, and triazolam, pretreatment with itraconazole resulted in a 2-, 4-, 17-, 7-, and 15-fold increase in AUC, respectively. With the exception of gefinitib for which the DDI effect was overpredicted (12-fold in Tg-mice vs 2-fold in the clinic), the magnitude of AUC increase observed in this study was consistent (within 2-fold) with the clinical DDI observed following administration with itraconazole/ketoconazole. As an assessment of CYP3A4 induction, following rifampin pretreatment to PXR-CAR-3A4/3A7 Hep/Int mice, an 8% decrease in vandetanib mean AUC was observed; 39-52% reduction in AUC were observed for dasatinib, ibrutinib, regorafenib, and sorafenib compared to vehicle treated mice. The greatest effect of rifampin induction was observed with alprazolam, bosutinib, crizotinib, gefitinib, and triazolam where 72-91% decrease in AUC were observed. With the exception of vandetanib for which rifampin induction was under-predicted, the magnitude of induction observed in this study was consistent (within 2-fold) with clinical observations. These data sets suggest that, with two exceptions, these transgenic mice models were able to exclude or capture the magnitude of CYP3A4 clinical inhibition and induction. Data generated in transgenic mice may be used to gain confidence and complement in vitro and in silico methods for assessing DDI potential/liability.

Published

2017

34. In vitro ocular metabolism and bioactivation of ketoconazole in rat, rabbit and human.

Author

Cirello AL, Dumouchel JL, Gunduz M, Dunne CE, and Argikar UA

Subjects

Administration, Ophthalmic, Animals, Humans, Ketoconazole chemistry, Male, Molecular Structure, Rabbits, Rats, Rats, Sprague-Dawley, Eye metabolism, Ketoconazole administration & dosage, Ketoconazole metabolism

Abstract

Oral ketoconazole is clinically administered for treatment of severe cases for fungal keratitis. Pharmacodynamics and efficacy of oral and topical (ocular) ketoconazole have been explored in rabbit. However, metabolism of ketoconazole in the eye in any species is not well explored in any preclinical species or human. An understanding of ocular drug metabolism in the eye is crucial for ocular therapeutics to facilitate the risk assessment and development of potential drug candidates for the clinic. We aimed to investigate the metabolism of ketoconazole in rat, rabbit and human ocular S9 fractions. Metabolism in liver S9 fractions was also studied for a direct comparison. Eleven putative metabolites were identified in the in vitro incubations. Of these metabolites, six were present in rat ocular S9 whereas eight were present in rabbit and human ocular matrices. Metabolic pathways in rabbit and human ocular fractions suggested the formation of reactive intermediates in rabbit and human liver and ocular S9 incubations, which was confirmed with trapping studies. Herein, we report eight human ocular metabolites of ketoconazole for the first time. To the best of our knowledge, this is the first report of ocular metabolic pathways and ocular bioactivation of ketoconazole in preclinical species and human., (Copyright © 2016 The Japanese Society for the Study of Xenobiotics. Published by Elsevier Ltd. All rights reserved.)

Published

2017

35. Characterization of chemical-induced sterile inflammation in vitro: application of the model compound ketoconazole in a human hepatic co-culture system.

Author

Wewering F, Jouy F, Wissenbach DK, Gebauer S, Blüher M, Gebhardt R, Pirow R, von Bergen M, Kalkhof S, Luch A, and Zellmer S

Subjects

Chemical and Drug Induced Liver Injury metabolism, Coculture Techniques, Hep G2 Cells drug effects, Humans, Interleukin-8 metabolism, Ketoconazole analogs & derivatives, Ketoconazole metabolism, Ketoconazole pharmacokinetics, Membrane Potential, Mitochondrial drug effects, NF-kappa B metabolism, Proteins analysis, Proteins metabolism, Reactive Oxygen Species metabolism, Tumor Necrosis Factor-alpha metabolism, Chemical and Drug Induced Liver Injury pathology, Ketoconazole adverse effects, Toxicity Tests methods

Abstract

Liver injury as a result of a sterile inflammation is closely linked to the activation of immune cells, including macrophages, by damaged hepatocytes. This interaction between immune cells and hepatocytes is as yet not considered in any of the in vitro test systems applied during the generation of new drugs. Here, we established and characterized a novel in vitro co-culture model with two human cell lines, HepG2 and differentiated THP-1. Ketoconazole, an antifungal drug known for its hepatotoxicity, was used as a model compound in the testing of the co-culture. Single cultures of HepG2 and THP-1 cells were studied as controls. Different metabolism patterns of ketoconazole were observed for the single and co-culture incubations as well as for the different cell types. The main metabolite N-deacetyl ketoconazole was found in cell pellets, but not in supernatants of cell cultures. Global proteome analysis showed that the NRF2-mediated stress response and the CXCL8 (IL-8) pathway were induced by ketoconazole treatment under co-culture conditions. The upregulation and ketoconazole-induced secretion of several pro-inflammatory cytokines, including CXCL8, TNF-α and CCL3, was observed in the co-culture system only, but not in single cell cultures. Taking together, we provide evidence that the co-culture model applied might be suitable to serve as tool for the prediction of chemical-induced sterile inflammation in liver tissue in vivo.

Published

2017

36. Methoxy poly (ethylene glycol)-b-poly (δ-valerolactone) copolymeric micelles for improved skin delivery of ketoconazole.

Author

Deng P, Teng F, Zhou F, Song Z, Meng N, and Feng R

Subjects

Animals, Antifungal Agents chemistry, Antifungal Agents metabolism, Antifungal Agents pharmacology, Drug Liberation, Ketoconazole pharmacology, Mice, Permeability, Drug Carriers chemistry, Ketoconazole chemistry, Ketoconazole metabolism, Micelles, Polyethylene Glycols chemistry, Pyrones chemistry, Skin metabolism

Abstract

Ketoconazole is a broad spectrum imidazole antifungal drug. For the treatment of superficial fungal infections with ketoconazole, it needs to be permeated to deep skin layers. In order to develop topical formulation of ketoconazole for improving its skin deposition and water-solubility, ketoconazole-loaded methoxy poly (ethylene glycol)-b-poly (δ-valerolactone) micelles were developed through thin-film hydration method. Particle size, drug loading capacity, infrared spectrum and X-ray diffraction of drug-loaded micelles were characterized. The optimal drug formulation was selected for skin delivery and deposition investigation performed by use of mice skin, and its in vitro release and antifungal activity were also investigated. Penetration and distribution in the skin were also visualized using fluorescein-loaded micelles and fluorescence microscopy. The drug-loaded micelles were obtained with encapsulation efficiency of 86.39% and particle diameter of about 12 nm. The micelles made ketoconazole aqueous solubility increase to 86-fold higher than crude one. Ketoconazole-loaded micelles showed no skin permeation of ketoconazole, obviously enhance skin deposition and demonstrated similar antifungal activity as compared with marketed ketoconazole cream. Fluorescein-loaded micelles displayed higher skin deposition than fluorescein water solution. These results demonstrate that the MPEG-PVL micelle is a potential delivery system for ketoconazole in the field of skin delivery.

Published

2017

37. Allosteric activation of midazolam CYP3A5 hydroxylase activity by icotinib - Enhancement by ketoconazole.

Author

Zhuang X, Zhang T, Yue S, Wang J, Luo H, Zhang Y, Li Z, Che J, Yang H, Li H, Zhu M, and Lu C

Subjects

Allosteric Regulation, Animals, Antineoplastic Agents metabolism, Crown Ethers metabolism, Dogs, Dose-Response Relationship, Drug, Drug Interactions, Haplorhini, Humans, In Vitro Techniques, Ketoconazole metabolism, Mice, Microsomes, Liver drug effects, Microsomes, Liver enzymology, Quinazolines metabolism, Rats, Species Specificity, Substrate Specificity, Antineoplastic Agents pharmacology, Crown Ethers pharmacology, Cytochrome P-450 CYP3A metabolism, Ketoconazole pharmacology, Microsomes, Liver metabolism, Midazolam metabolism, Quinazolines pharmacology

Abstract

Icotinib (ICO), a novel small molecule and a tyrosine kinase inhibitor, was developed and approved recently in China for non-small cell lung cancer. During screening for CYP inhibition potential in human liver microsomes (HLM), heterotropic activation toward CYP3A5 was revealed. Activation by icotinib was observed with CYP3A-mediated midazolam hydroxylase activity in HLM (∼40% over the baseline) or recombinant human CYP3A5 (rhCYP3A5) (∼70% over the baseline), but not in the other major CYPs including rhCYP3A4. When co-incubated with selective CYP3A4 inhibitor CYP3cide or monoclonal human CYP3A4 inhibitory antibody in HLM, the activation was extended to ∼60%, suggesting CYP3A5 might be the isozyme involved. Further, the relative activation was enhanced to ∼270% in rhCYP3A5 in the presence of ketoconazole. The activation was substrate and pathway dependent and observed only in the formation of 1'-OH-midazolam, and not 4-OH-midazolam, 6β-OH-testosterone, or oxidized nifedipine. The activation requires the presence of cytochrome b5 and it is only observed in the liver microsomes of dogs, monkeys, and humans, but not in rats and mice. Kinetic analyses of 1'-OH-midazolam formation showed that ICO increased the V max values in HLM and rhCYP3A5 with no significant changes in K m values. By adding CYP3cide with ICO to the incubation, the V max values increased 2-fold over the CYP3cide control. Addition of ketoconazole with ICO alone or ICO plus CYP3cide resulted in an increase in V max values and decrease in K m values compared to their controls. This phenomenon may be attributed to a new mechanism of CYP3A5 heterotropic activation, which warrants further investigation., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

38. Membrane Fluidity Modulates Thermal Stability and Ligand Binding of Cytochrome P4503A4 in Lipid Nanodiscs.

Author

McClary WD, Sumida JP, Scian M, Paço L, and Atkins WM

Subjects

Calorimetry, Differential Scanning, Circular Dichroism, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors metabolism, Cytochrome P-450 CYP3A Inhibitors pharmacology, Dimyristoylphosphatidylcholine chemistry, Enzyme Stability drug effects, Humans, Ketoconazole metabolism, Ketoconazole pharmacology, Lipid Bilayers chemistry, Lipid Bilayers metabolism, Models, Molecular, Phosphatidylcholines chemistry, Protein Binding, Protein Denaturation, Protein Domains, Testosterone metabolism, Thermodynamics, Cytochrome P-450 CYP3A chemistry, Lipids chemistry, Membrane Fluidity, Nanostructures chemistry, Temperature

Abstract

Cytochrome P4503A4 (CYP3A4) is a peripheral membrane protein that plays a major role in enzymatic detoxification of many drugs and toxins. CYP3A4 has an integral membrane N-terminal helix and a localized patch comprised of the G' and F' helix regions that are embedded in the membrane, but the effects of membrane composition on CYP3A4 function are unknown. Here, circular dichroism and differential scanning calorimetry were used to compare the stability of CYP3A4 in lipid bilayer nanodiscs with varying ratios of 1-palmitoyl-2-oleoyl-sn-glycero-3-phosphocholine to 1,2-dimyristoyl-sn-glycero-3-phosphocholine (DMPC). These lipids differ in the acyl-chain length and their degree of unsaturation. The thermal denaturation of CYP3A4 in nanodiscs occurs in a temperature range distinct from that of the nanodisc denaturation so it can be monitored calorimetrically. Melting temperatures (T m ), heat capacities (ΔC p ), and calorimetric enthalpies (ΔH cal ) for denaturation of CYP3A4 each increased with an increasing fraction of DMPC, with a maximum at 50% DMPC, before decreasing at 75% DMPC. Addition of the inhibitor ketoconazole results in increased thermal stability, and larger ΔC p and ΔH cal values, with different sensitivities to lipid composition. Effects of lipid composition on ligand binding dynamics were also studied. Equilibrium binding affinities of both ketoconazole (KTZ) and testosterone (TST) were minimally affected by lipid composition. However, stopped-flow analyses indicate that the rates of KTZ binding reach a maximum in membranes containing 50% DMPC, whereas the rate of TST binding decreases continuously with an increasing DMPC concentration. These results indicate that CYP3A4 is highly sensitive to the acyl-chain composition of the lipids and fluidity of the membrane in which it is embedded.

Published

2016

39. Human arylacetamide deacetylase hydrolyzes ketoconazole to trigger hepatocellular toxicity.

Author

Fukami T, Iida A, Konishi K, and Nakajima M

Subjects

Activation, Metabolic drug effects, Antifungal Agents adverse effects, Biocatalysis drug effects, Carboxylic Ester Hydrolases antagonists & inhibitors, Carboxylic Ester Hydrolases genetics, Cell Line, Tumor, Cells, Cultured, Chemical and Drug Induced Liver Injury metabolism, Chemical and Drug Induced Liver Injury pathology, Cytochrome P-450 CYP3A Inhibitors adverse effects, Enzyme Inhibitors pharmacology, Female, Hepatocytes cytology, Hepatocytes drug effects, Hepatocytes pathology, Humans, Hydrolysis drug effects, Hydroxylation drug effects, Isoflurophate pharmacology, Ketoconazole adverse effects, Ketoconazole analogs & derivatives, Ketoconazole toxicity, Male, Microsomes, Liver drug effects, Microsomes, Liver metabolism, Middle Aged, Oxygenases antagonists & inhibitors, Oxygenases genetics, Oxygenases metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Antifungal Agents metabolism, Carboxylic Ester Hydrolases metabolism, Chemical and Drug Induced Liver Injury enzymology, Cytochrome P-450 CYP3A Inhibitors metabolism, Hepatocytes metabolism, Ketoconazole metabolism, Microsomes, Liver enzymology

Abstract

Ketoconazole (KC), an antifungal agent, rarely causes severe liver injury when orally administered. It has been reported that KC is mainly hydrolyzed to N-deacetyl ketoconazole (DAK), followed by the N-hydroxylation of DAK by flavin-containing monooxygenase (FMO). Although the metabolism of KC has been considered to be associated with hepatotoxicity, the responsible enzyme(s) remain unknown. The purpose of this study was to identify the responsible enzyme(s) for KC hydrolysis in humans and to clarify their relevance to KC-induced toxicity. Kinetic analysis and inhibition studies using human liver microsomes (HLM) and recombinant enzymes revealed that human arylacetamide deacetylase (AADAC) is responsible for KC hydrolysis to form DAK, and confirmed that FMO3 is the enzyme responsible for DAK N-hydroxylation. In HLM, the clearance of KC hydrolysis occurred to the same extent as DAK N-hydroxylation, which indicates that both processes are not rate-limiting pathways. Cytotoxicity of KC and DAK was evaluated using HepaRG cells and human primary hepatocytes. Treatment of HepaRG cells with DAK for 24h showed cytotoxicity in a dose-dependent manner, whereas treatment with KC did not show due to the low expression of AADAC. Overexpression of AADAC in HepaRG cells with an adenovirus expression system elicited the cytotoxicity of KC. Cytotoxicity of KC in human primary hepatocytes was attenuated by diisopropylfluorophosphate, an AADAC inhibitor. In conclusion, the present study demonstrated that human AADAC hydrolyzes KC to trigger hepatocellular toxicity., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

40. Prediction of the precipitation profiles of weak base drugs in the small intestine using a simplified transfer ("dumping") model coupled with in silico modeling and simulation approach.

Author

Kambayashi A, Yasuji T, and Dressman JB

Subjects

Administration, Oral, Computer Simulation, Dipyridamole administration & dosage, Dipyridamole metabolism, Gastric Emptying, Humans, Ketoconazole administration & dosage, Ketoconazole metabolism, Pharmacokinetics, Intestine, Small metabolism, Models, Biological, Pharmaceutical Preparations metabolism

Abstract

Background: Precipitation of poorly soluble, weakly basic drugs upon entering the small intestine may lead to poor bioavailability. It would be useful to be able to predict the extent of in vivo precipitation so that formulation measures to counteract this problem can be taken., Aim: The aim of this research was to characterize the precipitation kinetics of two representative weak base drugs, dipyridamole and ketoconazole in vitro using a simplified transfer model approach, and to establish a predictive model for the total and dissolved concentrations in the small intestine after oral administration using in silico modeling and simulation., Methods: A simplified transfer ("dumping") method based on the USP paddle apparatus was used to obtain the precipitation profiles of the two weak base drugs by adding a solution of the drug in 0.02N hydrochloric acid to FaSSIF-V2. The observed precipitation curves obtained with various initial concentrations were fitted to first order kinetics. An in silico pharmacokinetic model for weak base drugs with precipitation in the small intestine was designed using STELLA® software and coupled with the precipitation profiles in order to simulate the total and dissolved drug concentrations in the small intestinal lumen in the fasted state in humans., Results: The predicted total and dissolved concentration curves in small intestine for the two weak base drugs were similar to the concentration profiles observed in vivo. The fraction precipitated of the drugs in the small intestine was also well predicted, although the precipitation of ketoconazole at higher initial concentrations was somewhat overestimated. A sensitivity analysis conducted on the simulation of the precipitation of the drugs indicated that a higher fraction precipitated when gastric emptying was faster and/or the concentration of the drug in the added solution was higher., Conclusion: The dumping method provides a useful screen for precipitation in the small intestine, especially in the context of early development., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

41. Bioconcentration and metabolism of ketoconazole and effects on multi-biomarkers in crucian carp (Carassius auratus).

Author

Liu J, Lu G, Yang H, Yan Z, Wang Y, and Wang P

Subjects

Acetylcholinesterase metabolism, Animals, Biomarkers metabolism, Cytochrome P-450 CYP1A1 metabolism, Glutathione Transferase metabolism, Ketoconazole pharmacokinetics, Liver metabolism, Superoxide Dismutase metabolism, Tandem Mass Spectrometry, Tissue Distribution, Water Pollutants, Chemical pharmacokinetics, Goldfish metabolism, Ketoconazole metabolism, Water Pollutants, Chemical metabolism

Abstract

The tissue distribution, bioconcentration, metabolism and biological effects of the antifungal medication ketoconazole were investigated in fish, crucian carp (Carassius auratus) were exposed to a series of nominal concentrations (0.2, 2 and 20 μg/L) for 14 days. The ultra-high performance liquid chromatography tandem triple quadrupole mass spectroscopy (UPLC/MS/MS) analysis was used to determine the bioconcentration of ketoconazole and its metabolites in fish. The highest tissue concentration of ketoconazole was observed in the liver with the bioconcentration factor of 257.2, which is lower than the estimated BCF value. The ability of crucian carp to metabolize ketoconazole was confirmed and the results pointed out the existence of seven metabolites likely formed via oxidation of imidazole ring and the metabolic alteration of the piperazine rings. In addition, acetylcholinesterase, 7-ethoxyresorufin O-deethylase, superoxide dismutase and glutathione S-transferase changed significantly after 3, 7 and 14 days of exposure (P < 0.05), which indicated that the accumulation and metabolism of ketoconazole in fish tissues may account for the biological effects., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

42. The Consequence of Drug-Drug Interactions Influencing the Interplay between P-Glycoprotein and Cytochrome P450 3a: An Ex Vivo Study with Rat Precision-Cut Intestinal Slices.

Author

Li M, de Graaf IA, Siissalo S, de Jager MH, van Dam A, and Groothuis GM

Subjects

Animals, Cyclosporins metabolism, Intestinal Absorption, Ketoconazole metabolism, Male, Quinidine metabolism, Rats, Rats, Wistar, Valine metabolism, Verapamil metabolism, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Cytochrome P-450 CYP3A metabolism, Drug Interactions physiology, Ileum metabolism, Jejunum metabolism, Pharmaceutical Preparations metabolism

Abstract

P-glycoprotein (P-gp) and cytochrome P450 3A (CYP3A) are differentially expressed along the intestine and work coordinately to reduce the intracellular concentration of xenobiotics and the absorption of orally taken drugs. Drug-drug interactions (DDIs) based on P-gp/CYP3A interplay are of clinical importance and require preclinical investigation. We investigated the P-gp/Cyp3a interplay and related DDIs with different P-gp inhibitors in the various regions of the rat intestine ex vivo using precision-cut intestinal slices (PCIS) with quinidine (Qi), a dual substrate of P-gp and Cyp3a, as the probe. The results showed that P-gp efflux was the main factor limiting the intracellular Qi content at concentrations below 5µM, whereas both efflux and metabolism were saturated at [Qi] > 50µM. The selective P-gp inhibitors CP100356 [N-(3,4-dimethoxyphenethyl)-4-(6,7-dimethoxy-3,4-dihydroisoquinolin-2[1H]-yl)-6,7-dimethoxyquinazolin-2-amine] and PSC833 [valspodar, 6-[(2S,4R,6E)-4-methyl-2-(methylamino)-3-oxo-6-octenoic acid]-7-l-valine-cyclosporin A] enhanced the Qi accumulation in slices in line with the different P-gp expression in the intestinal regions and, as a result, also enhanced metabolism in the jejunum and ileum. Dual inhibitors of both P-gp and Cyp3a (verapamil and ketoconazole) increased the concentration of Qi in the jejunum and ileum, but less 3-hydroxy-quinidine was produced due to inhibition of Cyp3a. The results indicate that the P-gp/Cyp3a interplay depends on the concentration of the drug and on the intestinal region under study. Furthermore, due to the P-gp/Cyp3a interplay, DDIs can lead to remarkable changes in the intracellular concentration of both the parent drug and the metabolite, which varies among the intestinal regions and depends on the selectivity of the inhibitors, with potentially important implications for disposition and toxicity of drugs and their metabolites., (Copyright © 2016 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2016

43. Effects of gastric pH on oral drug absorption: In vitro assessment using a dissolution/permeation system reflecting the gastric dissolution process.

Author

Kataoka M, Fukahori M, Ikemura A, Kubota A, Higashino H, Sakuma S, and Yamashita S

Subjects

Administration, Oral, Albendazole metabolism, Caco-2 Cells, Cell Line, Diclofenac metabolism, Dipyridamole metabolism, Humans, Hydrogen-Ion Concentration, Ketoconazole metabolism, Permeability, Solubility, Water chemistry, Body Fluids metabolism, Gastric Mucosa metabolism, Intestinal Absorption, Pharmaceutical Preparations metabolism

Abstract

The aim of the present study was to evaluate the effects of gastric pH on the oral absorption of poorly water-soluble drugs using an in vitro system. A dissolution/permeation system (D/P system) equipped with a Caco-2 cell monolayer was used as the in vitro system to evaluate oral drug absorption, while a small vessel filled with simulated gastric fluid (SGF) was used to reflect the gastric dissolution phase. After applying drugs in their solid forms to SGF, SGF solution containing a 1/100 clinical dose of each drug was mixed with the apical solution of the D/P system, which was changed to fasted state-simulated intestinal fluid. Dissolved and permeated amounts on applied amount of drugs were then monitored for 2h. Similar experiments were performed using the same drugs, but without the gastric phase. Oral absorption with or without the gastric phase was predicted in humans based on the amount of the drug that permeated in the D/P system, assuming that the system without the gastric phase reflected human absorption with an elevated gastric pH. The dissolved amounts of basic drugs with poor water solubility, namely albendazole, dipyridamole, and ketoconazole, in the apical solution and their permeation across a Caco-2 cell monolayer were significantly enhanced when the gastric dissolution process was reflected due to the physicochemical properties of basic drugs. These amounts resulted in the prediction of higher oral absorption with normal gastric pH than with high gastric pH. On the other hand, when diclofenac sodium, the salt form of an acidic drug, was applied to the D/P system with the gastric phase, its dissolved and permeated amounts were significantly lower than those without the gastric phase. However, the oral absorption of diclofenac was predicted to be complete (96-98%) irrespective of gastric pH because the permeated amounts of diclofenac under both conditions were sufficiently high to achieve complete absorption. These estimations of the effects of gastric pH on the oral absorption of poorly water-soluble drugs were consistent with observations in humans. In conclusion, the D/P system with the gastric phase may be a useful tool for better predicting the oral absorption of poorly water-soluble basic drugs. In addition, the effects of gastric pH on the oral absorption of poorly water-soluble drugs may be evaluated by the D/P system with and without the gastric phase., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

44. Evaluation of Ketoconazole and Its Alternative Clinical CYP3A4/5 Inhibitors as Inhibitors of Drug Transporters: The In Vitro Effects of Ketoconazole, Ritonavir, Clarithromycin, and Itraconazole on 13 Clinically-Relevant Drug Transporters.

Author

Vermeer LM, Isringhausen CD, Ogilvie BW, and Buckley DB

Subjects

Biological Transport physiology, Cell Line, Drug Interactions physiology, HEK293 Cells, Humans, Clarithromycin metabolism, Cytochrome P-450 CYP3A Inhibitors metabolism, Itraconazole metabolism, Ketoconazole metabolism, Membrane Transport Proteins metabolism, Ritonavir metabolism

Abstract

Ketoconazole is a potent CYP3A4/5 inhibitor and, until recently, recommended by the Food and Drug Administration (FDA) and the European Medicines Agency as a strong CYP3A4/5 inhibitor in clinical drug-drug interaction (DDI) studies. Ketoconazole sporadically causes liver injury or adrenal insufficiency. Because of this, the FDA and European Medicines Agency recommended suspension of ketoconazole use in DDI studies in 2013. The FDA specifically recommended use of clarithromycin or itraconazole as alternative strong CYP3A4/5 inhibitors in clinical DDI studies, but many investigators have also used ritonavir as an alternative. Although the effects of these clinical CYP3A4/5 inhibitors on other CYPs are largely established, reports on the effects on the broad range of drug transporter activities are sparse. In this study, the inhibitory effects of ketoconazole, clarithromycin, ritonavir, and itraconazole (and its CYP3A4-inhibitory metabolites, hydroxy-, keto-, and N-desalkyl itraconazole) toward 13 drug transporters (OATP1B1, OATP1B3, OAT1, OAT3, OCT1, OCT2, MATE1, MATE2-K, P-gp, BCRP, MRP2, MRP3, and BSEP) were systematically assessed in transporter-expressing HEK-293 cell lines or membrane vesicles. In vitro findings were translated into clinical context with the basic static model approaches outlined by the FDA in its 2012 draft guidance on DDIs. The results indicate that, like ketoconazole, the alternative clinical CYP3A4/5 inhibitors ritonavir, clarithromycin, and itraconazole each have unique transporter inhibition profiles. None of the alternatives to ketoconazole provided a clean inhibition profile toward the 13 drug transporters evaluated. The results provide guidance for the selection of clinical CYP3A4/5 inhibitors when transporters are potentially involved in a victim drug's pharmacokinetics., (Copyright © 2016 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2016

45. CYP450 mediated inhibition potential of Swertia chirata: An herb from Indian traditional medicine.

Author

Ahmmed SM, Mukherjee PK, Bahadur S, Harwansh RK, Kar A, Bandyopadhyay A, Al-Dhabi NA, and Duraipandiyan V

Subjects

Animals, Chromatography, High Pressure Liquid methods, Cytochrome P-450 Enzyme Inhibitors chemistry, Herb-Drug Interactions physiology, India, Inhibitory Concentration 50, Ketoconazole metabolism, Ketoconazole pharmacology, Male, Medicine, Traditional methods, Microsomes, Liver drug effects, Microsomes, Liver metabolism, Plant Extracts metabolism, Rats, Rats, Wistar, Triterpenes chemistry, Triterpenes metabolism, Triterpenes pharmacology, Ursolic Acid, Cytochrome P-450 CYP2D6 metabolism, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 Enzyme Inhibitors pharmacology, Plant Extracts chemistry, Plant Extracts pharmacology, Swertia chemistry

Abstract

Ethnopharmacological Relevance: An Ayurvedic herb, Swertia chirata (SC) have been used in treating various ailments such as hyperglycemia, leishmania, liver infections, inflammation, abdominal pain, bacterial infection, malaria etc. in Indian Systems of Medicine (ISM)., Aim of the Study: Study was designed to investigate the inhibition potential of the standardized SC extract along with its bioactive molecule ursolic acid on hepatic drug metabolizing isozymes (CYP3A4 and CYP2D6) and further some heavy metals were also analysed of the plant material., Materials and Methods: The hydro-alcoholic extract was standardized with standard ursolic acid by reverse phase-high performance liquid chromatography (RP-HPLC) method and the heavy metals content were analyzed through atomic absorption spectroscopy (AAS). The effect of extract on rat liver microsome (RLM) and individual CYP isozymes (CYP3A4 and CYP2D6) was investigated through CYP450-CO complex assay and fluorescence microplate assay respectively., Results: The content of ursolic acid was found to be 2.66% (w/w) in the SC extract and heavy metal contents along with trace elements were within the prescribed limits as per WHO guidelines. The inhibitory potential of SC extract on RLM was found to be 23.64±1.80%. CYP3A4 and CYP2D6 inhibitory effect of SC and ursolic acid (IC50: 197.49±2.68, 211.45±3.54 and IC50: 229.25±2.52, 212.66±1.26 µg/mL) was less as compared to that known inhibitors, ketoconazole and quinidine respectively., Conclusions: The current study revealed that S. chirata has less inhibition potential with two major drug metabolizing isozymes CYP3A4 and CYP2D6. SC extract and ursolic acid showed significantly (P<0.001) less inhibitory potential on RLM. The Ayurvedic herb (SC) has shown less inhibitory activity in a concentration dependent manner against the tested two CYP450 enzymes. The tested heavy metals and trace elements present SC was within limit. Therefore, the traditional use of S. chirata may be safe in respect of both tested isozymes., (Copyright © 2015 Elsevier Ireland Ltd. All rights reserved.)

Published

2016

46. An in vitro biorelevant gastrointestinal transfer (BioGIT) system for forecasting concentrations in the fasted upper small intestine: Design, implementation, and evaluation.

Author

Kourentas A, Vertzoni M, Stavrinoudakis N, Symillidis A, Brouwers J, Augustijns P, Reppas C, and Symillides M

Subjects

Fasting, Gastric Mucosa metabolism, Gastrointestinal Tract, In Vitro Techniques, Dipyridamole metabolism, Intestine, Small metabolism, Ketoconazole metabolism, Models, Biological, Ranitidine metabolism, Triazoles metabolism

Abstract

Purpose: Design an in vitro methodology for studying gastrointestinal transfer in the fasted state and implement the methodology in vitro by using a biorelevant gastrointestinal transfer system(BioGIT); evaluate the usefulness of BioGIT in predicting luminal concentrations of lipophilic weak bases in the fasted upper small intestine., Methods: The methodology was designed after modeling existing luminal data. Its implementation in vitro was based on a three compartment setup. Reproducibility of the transfer process was evaluated under conditions where solutions and/or suspensions were present in gastric and/or duodenal compartment and by using ranitidine, dipyridamole, ketoconazole, and posaconazole as model drugs. The transfer process as well as concentrations of dipyridamole, ketoconazole and posaconazole measured in the duodenal compartment were compared with data previously collected in the upper small intestine, after administration of identical preparations/dosage forms to fasted adults., Results: Using BioGIT, the transfer process was performed reproducibly in all cases (RSD b 12.9%); data with dipyridamole and ketoconazole were in line with luminal data in humans. Dipyridamole, ketoconazole and posaconazole concentrations in duodenal compartment were also in line with previously measured concentrations in the fasted upper small intestine of healthy adults., Conclusions: BioGIT system could be useful for the evaluation of the impact of gastrointestinal transfer on concentrations in the upper intestinal lumen during the first hour, after oral administration of dispersing/solution dosage forms of lipophilic weak bases.

Published

2016

47. Optimized on-line enantioselective capillary electrophoretic method for kinetic and inhibition studies of drug metabolism mediated by cytochrome P450 enzymes.

Author

Řemínek R, Glatz Z, and Thormann W

Subjects

Dexmedetomidine metabolism, Dexmedetomidine pharmacokinetics, Ketamine metabolism, Ketamine pharmacokinetics, Ketoconazole metabolism, Ketoconazole pharmacokinetics, Stereoisomerism, gamma-Cyclodextrins metabolism, gamma-Cyclodextrins pharmacokinetics, Cytochrome P-450 Enzyme Inhibitors pharmacology, Cytochrome P-450 Enzyme System metabolism, Electrophoresis, Capillary methods

Abstract

Pharmacokinetic and pharmacodynamic properties of a chiral drug can significantly differ between application of the racemate and single enantiomers. During drug development, the characteristics of candidate compounds have to be assessed prior to clinical testing. Since biotransformation significantly influences drug actions in an organism, metabolism studies represent a crucial part of such tests. Hence, an optimized and economical capillary electrophoretic method for on-line studies of the enantioselective drug metabolism mediated by cytochrome P450 enzymes was developed. It comprises a diffusion-based procedure, which enables mixing of the enzyme with virtually any compound inside the nanoliter-scale capillary reactor and without the need of additional optimization of mixing conditions. For CYP3A4, ketamine as probe substrate and highly sulfated γ-cyclodextrin as chiral selector, improved separation conditions for ketamine and norketamine enantiomers compared to a previously published electrophoretically mediated microanalysis method were elucidated. The new approach was thoroughly validated for the CYP3A4-mediated N-demethylation pathway of ketamine and applied to the determination of its kinetic parameters and the inhibition characteristics in presence of ketoconazole and dexmedetomidine. The determined parameters were found to be comparable to literature data obtained with different techniques. The presented method constitutes a miniaturized and cost-effective tool, which should be suitable for the assessment of the stereoselective aspects of kinetic and inhibition studies of cytochrome P450-mediated metabolic steps within early stages of the development of a new drug., (© 2014 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2015

48. Synergetic skin targeting effect of hydroxypropyl-β-cyclodextrin combined with microemulsion for ketoconazole.

Author

Che J, Wu Z, Shao W, Guo P, Lin Y, Pan W, Zeng W, Zhang G, Wu C, and Xu Y

Subjects

2-Hydroxypropyl-beta-cyclodextrin, Administration, Cutaneous, Animals, Antifungal Agents chemistry, Antifungal Agents metabolism, Candida drug effects, Candida growth & development, Chemistry, Pharmaceutical, Emulsions, Ethylene Glycols chemistry, Glycerides chemistry, Hydrogen-Ion Concentration, Ketoconazole chemistry, Ketoconazole metabolism, Kinetics, Microscopy, Confocal, Particle Size, Permeability, Polyethylene Glycols chemistry, Proton Magnetic Resonance Spectroscopy, Rats, Wistar, Solubility, Stearic Acids chemistry, Surface-Active Agents chemistry, Technology, Pharmaceutical methods, Viscosity, Antifungal Agents administration & dosage, Drug Carriers, Ketoconazole administration & dosage, Skin metabolism, Skin Absorption, beta-Cyclodextrins chemistry

Abstract

The objective was to develop a ternary skin targeting system for ketoconazole (KET) using a combined strategy of microemulsion (ME) and cyclodextrin (HP-β-CD), i.e., KET-CD-ME, which exploits both virtues of cyclodextrin complex and ME to obtain the synergetic effect. KET-CD-ME was formulated using Labrafil M 1944 CS as oil phase, Solutol HS 15 as surfactant, Transcutol P as cosurfactant, and HP-β-CD solution as aqueous phase. The formulation of KET-CD-ME was optimized and the optimal formulation was characterized in terms of particle size, size distribution, pH value, and viscosity. Long term stability experiment showed that HP-β-CD could increase the physical stability of ternary system and KET chemical stability. Percutaneous permeation of KET from KET-CD-ME in vitro through rat skin was investigated in comparison with KET microemulsion (KET-ME), KET HP-β-CD inclusion solution (KET-CD), KET aqueous suspension, and commercial KET cream; the results showed that the combination of ME with HP-β-CD exhibited significantly synergistic effect on KET deposition within the skin (29.38 ± 1.79 μg/cm(2)) and a slightly synergistic effect on KET penetration through the skin (11.3 μg/cm(2)/h). The enhancement of the combination on skin deposition was further visualized by confocal laser scanning microscope (CLSM). In vitro sensitivity against Candida parapsilosis test indicated that KET-CD-ME enhanced KET antifungal activity mainly owing to the solubilization of HP-β-CD on KET in the ternary system. Moreover, the interactions between HP-β-CD and KET in the ternary system were elucidated through microScale thermophoresis (MST) and 2D (1)H NMR spectroscopy. The profiles from MST confirmed the host-guest interactions of HP-β-CD with KET in the ternary system and a deep insight into the interactions between KET and HP-β-CD were obtained by means of 2D (1)H NMR spectroscopy. The results indicate that the ternary system of ME combination with HP-β-CD may be a promising approach for skin targeting delivery of KET., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2015

49. Pi-pi Stacking Mediated Cooperative Mechanism for Human Cytochrome P450 3A4.

Author

Fa B, Cong S, and Wang J

Subjects

Antifungal Agents metabolism, Binding Sites, Crystallography, X-Ray, Cytochrome P-450 CYP3A ultrastructure, Humans, Hydrophobic and Hydrophilic Interactions, Ketoconazole metabolism, Models, Molecular, Molecular Dynamics Simulation, Protein Binding, Antifungal Agents chemistry, Cytochrome P-450 CYP3A chemistry, Ketoconazole chemistry

Abstract

Human Cytochrome P450 3A4 (CYP3A4) is an important member of the cytochrome P450 superfamily with responsibility for metabolizing ~50% of clinical drugs. Experimental evidence showed that CYP3A4 can adopt multiple substrates in its active site to form a cooperative binding model, accelerating substrate metabolism efficiency. In the current study, we constructed both normal and cooperative binding models of human CYP3A4 with antifungal drug ketoconazoles (KLN). Molecular dynamics simulation and free energy calculation were then carried out to study the cooperative binding mechanism. Our simulation showed that the second KLN in the cooperative binding model had a positive impact on the first one binding in the active site by two significant pi-pi stacking interactions. The first one was formed by Phe215, functioning to position the first KLN in a favorable orientation in the active site for further metabolism reactions. The second one was contributed by Phe304. This pi-pi stacking was enhanced in the cooperative binding model by the parallel conformation between the aromatic rings in Phe304 and the dioxolan moiety of the first KLN. These findings can provide an atomic insight into the cooperative binding in CYP3A4, revealing a novel pi-pi stacking mechanism for drug-drug interactions.

Published

2015

50. A simple construction of electrochemical liver microsomal bioreactor for rapid drug metabolism and inhibition assays.

Author

Walgama C, Nerimetla R, Materer NF, Schildkraut D, Elman JF, and Krishnan S

Subjects

Biocatalysis, Carbon chemistry, Cytochrome P-450 Enzyme Inhibitors chemistry, Cytochrome P-450 Enzyme Inhibitors metabolism, Electrodes, Humans, Ketoconazole chemistry, Ketoconazole pharmacology, Kinetics, Microsomes, Liver enzymology, Structure-Activity Relationship, Bioreactors, Cytochrome P-450 Enzyme Inhibitors pharmacology, Cytochrome P-450 Enzyme System metabolism, Electrochemical Techniques, Ketoconazole metabolism, Microsomes, Liver chemistry, Microsomes, Liver metabolism

Abstract

In order to design a green microsomal bioreactor on suitably identified carbon electrodes, it is important to understand the direct electrochemical properties at the interfaces between various carbon electrode materials and human liver microsomes (HLM). The novelty of this work is on the investigation of directly adsorbed HLM on different carbon electrodes with the goal to develop a simple, rapid, and new bioanalytical platform of HLM useful for drug metabolism and inhibition assays. These novel biointerfaces are designed in this study by a one step adsorption of HLM directly onto polished basal plane pyrolytic graphite (BPG), edge plane pyrolytic graphite (EPG), glassy carbon (GC), or high-purity graphite (HPG) electrodes. The estimated direct electron transfer (ET) rate constant of HLM on the smooth GC surface was significantly greater than that of the other electrodes. On the other hand, the electroactive surface coverage and stability of microsomal films were greater on highly surface defective, rough EPG and HPG electrodes compared to the smooth GC and less defective hydrophobic BPG surfaces. The presence of significantly higher oxygen functionalities and flatness of the GC surface is attributed to favoring faster ET rates of the coated layer of thin HLM film compared to other electrodes. The cytochrome P450 (CYP)-specific bioactivity of the liver microsomal film on the catalytically superior, stable HPG surface was confirmed by monitoring the electrocatalytic conversion of testosterone to 6β-hydroxytestosterone and its inhibition by the CYP-specific ketoconazole inhibitor. The identification of optimal HPG and EPG electrodes to design biologically active interfaces with liver microsomes is suggested to have immense significance in the design of one-step, green bioreactors for stereoselective drug metabolite synthesis and drug metabolism and inhibition assays.

Published

2015