Your search keyword '"Clinical Pharmacokinetics"' showing total 39 results

1. Novel omeprazole delayed release orally disintegrating tablets for enhanced patient compliance: a case of model informed formulation development.

Author

Boddu R, Kollipara S, Kambam V, Khan SM, Behera S, Murty NN, Baheti N, Choudhury AA, and Ahmed T

Subjects

Humans, Administration, Oral, Patient Compliance, Models, Biological, Pilot Projects, Drug Liberation, Omeprazole pharmacokinetics, Omeprazole administration & dosage, Omeprazole chemistry, Tablets, Delayed-Action Preparations

Abstract

The advanced in silico simulation tools, such as physiologically based biopharmaceutics models (PBBM) or physiologically based pharmacokinetic models (PBPK), play critical role in model informed formulation development. This approach has been successfully implemented in the present case for development of novel omeprazole delayed-release orally disintegrating tablets (ODT) formulation, aimed to enhance patient compliance.PBBM was developed using physicochemical, biopharmaceutical, and dissolution data. The dissolution studies for pilot formulations were conducted in biopredictive media in fasting (0.1 N HCl followed by pH 6.8) and fed (pH 5 followed by pH 6.8) conditions. The model was extensively validated in three stages: pilot fasted, pilot fed virtual bioequivalence and food effect assessments. Impressively, the model was able to predict both passed and failed batches appropriately.Based on insights from the pilot study, a higher scale pivotal formulation was optimised. Prospective predictions were made for pivotal formulations using validated model and bio results were found to be in line with model predictions in fasting condition.Overall, a rationale and patient compliant formulation was developed using innovative modelling approach and filed to regulatory agency. The novel omeprazole formulation enhanced patient compliance through ease of administration thereby circumventing challenges of conventional formulation.

Published

2024

2. An in vitro study of metformin adsorption to activated charcoal.

Author

Tomoda Y and Kobayashi M

Subjects

Adsorption, Hypoglycemic Agents chemistry, Hypoglycemic Agents toxicity, Drug Overdose drug therapy, Humans, Charcoal chemistry, Charcoal therapeutic use, Metformin chemistry, Metformin toxicity

Abstract

Introduction: Metformin is a biguanide used to manage patients with type 2 diabetes mellitus. However, metabolic acidosis with an elevated lactate concentration and death caused by metformin overdoses are toxicological concerns. Although activated charcoal has been widely used for gastrointestinal decontamination in cases of acute poisoning, there is no evidence regarding its efficacy in treating metformin overdoses. We therefore evaluated the adsorptive capacity of activated charcoal for metformin in vitro ., Methods: Activated charcoal (specific surface area: 1,080 m 2 /g) mixed with various concentrations of metformin solution was dissolved in simulated gastric and intestinal fluids at 37° Celsius. The suspension was then filtered and the metformin concentration in the filtrate was determined using high-performance liquid chromatography. The maximum adsorptive capacity for metformin was calculated using the Langmuir adsorption isotherm equation., Results: The amount of metformin adsorbed per gram of activated charcoal ranged from 0.7 to 8.1 mg/g at pH 1.2, and from 8.4 to 48.2 mg/g at pH 6.8. The corresponding maximum adsorptive capacities were 10.6 mg/g and 55.9 mg/g respectively., Discussion: The maximum adsorptive capacity of activated charcoal for metformin was similar to that of its capacity for other poorly adsorbed substances. This is likely because metformin is water-soluble and has high polarity-factors that correlate with poor adsorption on activated charcoal., Conclusions: The maximum adsorption of metformin by activated charcoal was low. Therefore, activated charcoal may not be effective for treating patients with metformin overdose.

Published

2024

3. The metabolism of the orexin-1 selective receptor antagonist nivasorexant.

Author

Treiber A, Seeland S, Haschimi B, Weigel A, Williams JT, and Gabillet J

Subjects

Humans, Rats, Animals, Orexins metabolism, Orexins pharmacology, Cytochrome P-450 Enzyme System metabolism, Hydroxylation, Cytochrome P-450 CYP3A metabolism, Microsomes, Liver metabolism, Cytochrome P-450 CYP2C19 metabolism, Aryl Hydrocarbon Hydroxylases metabolism

Abstract

Nivasorexant was the first orexin-1 selective receptor antagonist entering clinical development. Despite encouraging preclinical evidence in animal models, a proof-of-concept trial in binge-eating patients recently failed to demonstrate its clinical utility in this population.Across species, nivasorexant clearance was driven by metabolism along seven distinct pathways, five of which were hydroxylation reactions in various locations of the molecule. The exact sites of metabolism were identified by means of mass spectrometry, the use of deuterated analogues, and finally confirmed by chemical references.CYP3A4 was the main cytochrome P450 enzyme involved in nivasorexant metabolism in vitro and accounting for about 90% of turnover in liver microsomes. Minor roles were taken by CYP2C9 and CYP2C19 but individually did not exceed 3-7%.In the rat, nivasorexant was mostly excreted via the bile after extensive metabolism, while urinary excretion was negligible. Only traces of the parent drug were detected in urine, bile, or faeces.

Published

2024

4. Improving on in-silico prediction of oral drug bioavailability.

Author

Alqahtani S

Subjects

Humans, Biological Availability, Reproducibility of Results, Administration, Oral, Computer Simulation, Pharmaceutical Preparations, Artificial Intelligence, Models, Biological

Abstract

Introduction: Although significant development has been made in high-throughput screening of oral drug absorption and oral bioavailability, in silico prediction continues to play an important role in prediction of oral bioavailability and assisting in the proper selection of potential drug candidates., Areas Covered: This review describes the improvements and latest modeling methods and algorithms available for the prediction of this important parameter. We performed a PubMed database search with a focus on the literature published in the last 15 years., Expert Opinion: A tremendous efforts have been done in the past several years to develop reliable prediction tools that can provide accurate prediction for oral bioavailability. Several studies demonstrated new methodologies and techniques to develop either web-based in silico predictive tools or integrated PBPK models to predict oral bioavailability for new molecules. Improvements in the databases and the computational power will enhance the in silico prediction accuracy and reliability. Finally, introducing artificial intelligence to the drug development process will help improve the prediction tools.

Published

2023

5. The influence of temperature on the metabolic activity of CYP2C9, CYP2C19, and CYP3A4 genetic variants in vitro .

Author

Kojima M, Machida K, Cho S, Watanabe D, Seki H, Shimoji M, Imaoka A, Yamazaki H, Guengerich FP, Nakamura K, Yamamoto K, Akiyoshi T, and Ohtani H

Subjects

Humans, Cytochrome P-450 CYP2C9 genetics, Cytochrome P-450 CYP2C19 genetics, Temperature, Cytochrome P-450 CYP3A genetics, Aryl Hydrocarbon Hydroxylases genetics

Abstract

1. Temperature is considered to affect the activity of drug-metabolizing enzymes; however, no previous studies have compared temperature dependency among cytochrome P450 genetic variants. This study aimed to analyse warfarin 7-hydroxylation by CYP2C9 variants; omeprazole 5-hydroxylation by CYP2C19 variants; and midazolam 1-hydroxylation by CYP3A4 variants at 34 °C, 37 °C, and 40 °C.2. Compared with that seen at 37 °C, the intrinsic clearance rates ( V max / K m ) of CYP2C9.1 and .2 were decreased (76 ∼ 82%), while that of CYP2C9.3 was unchanged at 34 °C. At 40 °C, CYP2C9.1, .2, and .3 exhibited increased (121%), unchanged and decreased (87%) intrinsic clearance rates, respectively. At 34 °C, the clearance rates of CYP2C19.1A and .10 were decreased (71 ∼ 86%), that of CYP2C19.1B was unchanged, and those of CYP2C19.8 and .23 were increased (130 ∼ 134%). At 40 °C, the clearance rates of CYP2C19.1A, .1B, .10, and .23 remained unaffected, while that of CYP2C19.8 was decreased (74%). At 34 °C, the clearance rates of CYP3A4.1 and .16 were decreased (79 ∼ 84%), those of CYP3A4.2 and .7 were unchanged, and that of CYP3A4.18 was slightly increased (112%). At 40 °C, the clearance rate of CYP3A4.1 remained unaffected, while those of CYP3A4.2, .7, .16, and .18 were decreased (58 ∼ 82%).3. These findings may be clinically useful for dose optimisation in patients with hypothermia or hyperthermia.

Published

2023

6. The metabolism of the dual orexin receptor antagonist daridorexant.

Author

Treiber A, Delahaye S, Weigel A, Aeänismaa P, Gatfield J, and Seeland S

Subjects

Male, Rats, Humans, Mice, Animals, Imidazoles, Pyrrolidines, Orexin Receptor Antagonists, Sleep Initiation and Maintenance Disorders drug therapy

Abstract

Daridorexant is a dual orexin receptor antagonist developed for the treatment of insomnia disorder and has shown improvement in sleep outcomes and daytime functioning. The present work describes its biotransformation pathways in vitro and in vivo and provides a cross-species comparison between the animal species used in preclinical safety assessments and man.Daridorexant clearance is driven by metabolism along seven distinct pathways. Metabolic profiles were characterised by downstream products while primary metabolic products were of minor importance. The metabolic pattern differed between rodent species, with the rat reflecting the human pattern better than the mouse.In rodents, daridorexant is mostly excreted via the bile after extensive metabolism while urinary excretion was negligible in the rat. Only traces of the parent drug were detected in urine, bile, or faeces.Daridorexant has three major metabolites which are well covered in these preclinical safety species. All of them retain some residual affinity towards orexin receptors. However, none of these is considered to contribute to the pharmacological effect of daridorexant as their active concentrations in the human brain are too low.

Published

2023

7. Metabolites identification and species comparison of Oroxylin A, an anti-cancer flavonoid, in vitro and in vivo by HPLC-Q-TOF-MS/MS.

Author

Bian Y, Sun M, Chen H, Ren G, Fu K, Yang N, Zhang M, Zhou N, Lu Y, Li N, Zhang Y, Chen X, and Zhao D

Subjects

Animals, Chromatography, High Pressure Liquid methods, Dogs, Flavonoids, Mice, Rats, Rats, Sprague-Dawley, Neoplasms, Tandem Mass Spectrometry methods

Abstract

Oroxylin A, the main component of Scutellaria baicalensis Georigi has been widely studied due to its well-known pharmacological effects. According to previous studies, Oroxylin A with low bioavailability was converted into glucuronidation and sulphonated metabolites, which had high exposure in plasma and generated certain activities. It is necessary to study the metabolites and metabolic pathways of Oroxylin A.This study aimed to explore the metabolites of Oroxylin A in liver microsomes, primary hepatocyte incubation samples of five different species (human, monkey, dog, mouse, rat), and in bile, urine and faeces of rats.It would provide a systematic description of metabolic pathway of Oroxylin A. Also, a method of high-performance liquid chromatography combined with quadrupole time-of-flight mass spectrometry detector (HPLC-Q-TOF-MS/MS) for identification of each metabolite in various biological matrices was developed.This experiment illustrated that phase II metabolites were the main form of Oroxylin A in vitro and in excretion of rats, accompanied with a small amount of phase I metabolites.Furthermore, there were obvious species differences among the metabolism in vitro , especially in phase II. Monkeys and rats may be more suitable for preclinical research than dogs and mice as non-rodent or rodent species.

Published

2022

8. Pirfenidone 5-hydroxylation is mainly catalysed by CYP1A2 and partly catalysed by CYP2C19 and CYP2D6 in the human liver.

Author

Zhang Y, Sato R, Fukami T, Nakano M, and Nakajima M

Subjects

Catalysis, Cytochrome P-450 CYP1A2 metabolism, Cytochrome P-450 CYP2C19 metabolism, Cytochrome P-450 CYP2D6 metabolism, Humans, Hydroxylation, Liver metabolism, Microsomes, Liver metabolism, Pyridones, Cytochromes metabolism

Abstract

Pirfenidone is a first-line drug for the treatment of idiopathic pulmonary fibrosis. The primary metabolic pathways of pirfenidone in humans are 5-hydroxylation and subsequent oxidation to 5-carboxylpirfenidone. The aims of this study were to determine the cytochrome P450 isoforms responsible for pirfenidone 5-hydroxylation and to evaluate their contributions in human liver microsomes (HLM).Among the recombinant P450 isoforms, CYP1A2, CYP2D6, CYP2C19, CYP2A6, and CYP2B6 were shown to catalyse the 5-hydroxylation of pirfenidone. Pirfenidone 5-hydroxylase activity by HLM was inhibited by α-naphthoflavone (by 45%), 8-methoxypsolaren (by 84%), tranylcypromine (by 53%), and quinidine (by 15%), which are CYP1A2, CYP1A2/CYP2A6/CYP2C19, CYP2A6/CYP2C19, and CYP2D6 inhibitors, respectively.In 17 individual HLM donors, pirfenidone 5-hydroxylase activity was significantly correlated with phenacetin O -deethylase ( r  = 0.89, P  < 0.001) and S -mephenytoin 4'-hydroxylase activities ( r  = 0.51, P  < 0.05), which are CYP1A2 and CYP2C19 marker activities, respectively.By using the relative activity factors, the contributions of CYP1A2, CYP2C19, and CYP2D6 to pirfenidone 5-hydroxylation in the human liver were 72.8%, 11.8%, and 8.9%, respectively.In conclusion, we clearly demonstrated the predominant P450 involved in pirfenidone 5-hydroxylation in the human liver is CYP1A2, with CYP2C19 and CYP2D6 playing a minor role.

Published

2021

9. Changes in neurocognitive assessment scores after initiating dolutegravir- versus elvitegravir-based antiretroviral therapy.

Author

Adams JL, Choi YC, West M, Pontiggia L, Baxter J, and George J

Subjects

Adult, Heterocyclic Compounds, 3-Ring, Humans, Male, Middle Aged, Oxazines, Piperazines, Prospective Studies, Pyridones, Quinolones, HIV Infections drug therapy, HIV Integrase Inhibitors therapeutic use, HIV-1

Abstract

This prospective cohort study enrolled people living with HIV initiating antiretroviral therapy (ART) containing the integrase inhibitors, dolutegravir (DTG) or elvitegravir (EVG) and administered the Montreal Cognitive Assessment (MoCA) at baseline and again after approximately six months to compare changes in MoCA scores. The proportion of patients found to have cognitive impairment, as indicated by a MoCA score <26/30, on each agent were also compared and comparisons were made between changes in each domain assessed by the MoCA (visuospatial/executive, naming, attention, language, abstraction, delayed recall, and orientation). Thirty-five evaluable participants were enrolled, 18 on DTG and 17 on EVG. The median [interquartile range(IQR)] age was 44 (32 to 54) years, 63% were male, 57% were African American. The median (IQR) MoCA score at baseline was 25 (23 to 27) with no difference between groups ( p =0.249). The median (IQR) change in MoCA score was 0 (-1 to 2) for DTG and 1 (0 to 3) for EVG ( p  = 0.183). Of those on DTG, 8 (44%) had MoCA scores <26 on follow-up compared to 11 (65%) on EVG ( p  = 0.229). There were no significant differences in changes in any of the individual MoCA domains.

Published

2021

10. An updated review of pharmacokinetic drug interactions and pharmacogenetics of statins.

Author

Hirota T, Fujita Y, and Ieiri I

Subjects

Animals, Carrier Proteins genetics, Carrier Proteins metabolism, Cytochrome P-450 Enzyme System genetics, Cytochrome P-450 Enzyme System metabolism, Humans, Hydroxymethylglutaryl-CoA Reductase Inhibitors adverse effects, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacokinetics, Hypercholesterolemia drug therapy, Muscle, Skeletal drug effects, Muscle, Skeletal pathology, Muscular Diseases chemically induced, Polymorphism, Genetic, Drug Interactions, Hydroxymethylglutaryl-CoA Reductase Inhibitors administration & dosage, Pharmacogenetics

Abstract

Introduction: Hydroxymethylglutaryl-coenzyme A reductase inhibitors (statins) lower cholesterol synthesis in patients with hypercholesterolemia. Increased statin exposure is an important risk factor for skeletal muscle toxicity. Potent inhibitors of cytochrome P450 (CYP) 3A4 significantly increase plasma concentrations of the active forms of simvastatin, lovastatin, and atorvastatin. Fluvastatin is metabolized by CYP2C9, whereas pravastatin, rosuvastatin, and pitavastatin are unaffected by inhibition by either CYP. Statins also have different affinities for membrane transporters involved in processes such as intestinal absorption, hepatic absorption, biliary excretion, and renal excretion., Areas Covered: In this review, the pharmacokinetic aspects of drug-drug interactions with statins and genetic polymorphisms of CYPs and drug transporters involved in the pharmacokinetics of statins are discussed., Expert Opinion: Understanding the mechanisms underlying statin interactions can help minimize drug interactions and reduce the adverse side effects caused by statins. Since recent studies have shown the involvement of drug transporters such as OATP and BCRP as well as CYPs in statin pharmacokinetics, further clinical studies focusing on the drug transporters are necessary. The establishment of biomarkers based on novel mechanisms, such as the leakage of microRNAs into the peripheral blood associated with the muscle toxicity, is important for the early detection of statin side effects.

Published

2020

11. Effects of the ABCB1 and ABCG2 polymorphisms on the pharmacokinetics of afatinib in healthy Chinese volunteers.

Author

Tan Y, Cao K, Ren G, Qin Z, Zhao D, Li N, Chen X, Xia Y, and Lu Y

Subjects

ATP Binding Cassette Transporter, Subfamily B genetics, Adult, Asian People, China, Female, Genotype, Healthy Volunteers, Humans, Male, Polymorphism, Single Nucleotide, ATP Binding Cassette Transporter, Subfamily G, Member 2 genetics, Afatinib pharmacokinetics, Antineoplastic Agents pharmacokinetics, Neoplasm Proteins genetics

Abstract

1. Afatinib is an oral, selective tyrosine kinase inhibitor (TKI) primarily transported by P-glycoprotein (MDR1, gene code ABCB1 ) and breast cancer resistance protein (BCRP, gene code ABCG2 ). In the present study, the effects of ABCB1 and ABCG2 genetic polymorphisms on the pharmacokinetics of afatinib in healthy Chinese were investigated.2. Blood samples from 24 healthy participants who received afatinib were used for genotyping ABCB1 (1236C>T, 2677G > T/A, 3435C>T) and ABCG2 (34G>A, 421C>A) polymorphisms. Subsequently, the association between afatinib plasma concentrations and target single-nucleotide polymorphisms (SNPs) was analyzed.3. Among the five polymorphisms, plasma concentrations of afatinib in healthy subjects with ABCB1 1236CC-3435CC were remarkably higher than in other genotype subjects. No significant differences of afatinib exposure were found between the ABCG2 wild-type and heterozygous groups.4. The ABCB1 genetic polymorphism influenced the plasma exposure of afatinib, and gene testing before drug administration may be useful for clinically individualized use of afatinib. Our data suggest the usefulness of afatinib pharmacogenetics in treatment optimization.

Published

2020

12. The prominent impairment of liver/intestinal cytochrome P450 and intestinal drug transporters in sepsis-induced acute kidney injury over acute and chronic renal ischemia, a mouse model comparison.

Author

Sukkummee W, Jittisak P, Wonganan P, Wittayalertpanya S, Chariyavilaskul P, and Leelahavanichkul A

Subjects

ATP Binding Cassette Transporter, Subfamily B metabolism, Acute Kidney Injury etiology, Animals, Chemokines, CC metabolism, Cytochrome P-450 CYP3A metabolism, Disease Models, Animal, Hep G2 Cells, Humans, Interleukin-6 metabolism, Intestines pathology, Liver pathology, Macrophage Inflammatory Proteins metabolism, Male, Membrane Proteins metabolism, Mice, Mice, Inbred ICR, Organic Anion Transporters metabolism, Renal Insufficiency, Chronic etiology, Reperfusion Injury etiology, Acute Kidney Injury pathology, Renal Insufficiency, Chronic pathology, Reperfusion Injury pathology, Sepsis complications

Abstract

Drug dosing adjustment in sepsis-induced acute kidney injury (sepsis-AKI) is currently adjusted based on renal function. Sepsis is a multiorgan injury, and thus, drug metabolism in sepsis-AKI might be interfered by non-renal factors such as changes in functions of drug-metabolizing enzymes in the liver and functions of intestinal drug transporters. We compared the defect on mouse CYP3A11 (human CYP3A4 representative) in liver and intestine along with several intestinal drug transporters (MDR1a, MRP2, and OATP3) in three mouse models; chronic ischemic reperfusion injury (Chr I/R; 4-week), acute ischemic reperfusion injury (Acute I/R; 24-h), and cecal ligation and puncture (CLP; 24-h) as representative of sepsis-AKI. Decreased expression of CYP3A11 and drug transporters was demonstrated in all models. Among these models, sepsis-AKI had the least severe renal injury (increased BUN and Scr) with the most severe liver injury (increased ALT and changes in liver histopathology), the most severe intestinal leakage (increased serum (1→3)-β-D-glucan) and the highest increase in serum IL-6. A reduced expression and activity of liver and intestinal CYP3A11 along with intestinal efflux-drug transporter expressions (MDR1a and MRP2), but not drug uptake transporter (OATP3), was predominant in sepsis-AKI compared with acute I/R. Additionally, a reduction of CYP3A4 expression with IL-6 was demonstrated on HepG2 cells implying a direct injury of IL-6 on human liver cells. Differences in drug metabolism were reported between sepsis-AKI and ischemic-AKI confirming that drug dosing adjustment in sepsis-AKI depends not just only on renal function but also on several non-renal factors. Further studies are warranted.

Published

2019

13. Metabolic characteristics of Tanshinone I in human liver microsomes and S9 subcellular fractions.

Author

Li Y, Fan Y, Su H, Wang Q, Li GF, Hu Y, Jiang J, Tan B, and Qiu F

Subjects

Abietanes pharmacokinetics, Biotransformation, Chromatography, High Pressure Liquid, Cytochrome P-450 CYP2A6 metabolism, Cytochrome P-450 CYP2A6 physiology, Glucuronosyltransferase metabolism, Humans, Hydroxylation, Mass Spectrometry, Metabolic Networks and Pathways, NAD(P)H Dehydrogenase (Quinone) metabolism, NADP metabolism, Protein Isoforms metabolism, Protein Isoforms physiology, Subcellular Fractions metabolism, Abietanes metabolism, Microsomes, Liver metabolism

Abstract

Tanshinone I (TSI) is a lipophilic diterpene in Salvia miltiorrhiza with versatile pharmacological activities. However, metabolic pathway of TSI in human is unknown. In this study, we determined major metabolites of TSI using a preparation of human liver microsomes (HLMs) by HPLC-UV and Q-Trap mass spectrometer. A total of 6 metabolites were detected, which indicated the presence of hydroxylation, reduction as well as glucuronidation. Selective chemical inhibition and purified cytochrome P450 (CYP450) isoform screening experiments revealed that CYP2A6 was primarily responsible for TSI Phase I metabolism. Part of generated hydroxylated TSI was glucuronidated via several glucuronosyltransferase (UGT) isoforms including UGT1A1, UGT1A3, UGT1A7, UGT1A9, as well as extrahepatic expressed isoforms UGT1A8 and UGT1A10. TSI could be reduced to a relatively unstable hydroquinone intermediate by NAD(P)H: quinone oxidoreductase 1 (NQO1), and then immediately conjugated with glucuronic acid by a panel of UGTs, especially UGT1A9, UGT1A1 and UGT1A8. Additionally, NQO1 could also reduce hydroxylated TSI to a hydroquinone intermediate, which was immediately glucuronidated by UGT1A1. The study demonstrated that hydroxylation, reduction as well as glucuronidation were the major pathways for TSI biotransformation, and six metabolites generated by CYPs, NQO1 and UGTs were found in HLMs and S9 subcellular fractions.

Published

2019

14. Evaluation of the pharmacokinetics, tissue distribution and excretion studies of YMR-65, a tubulin polymerization inhibitor with potential anticancer activity, in rats using UPLC-MS/MS.

Author

Fan A, Zhang Y, Zhang Q, Wei J, Lu X, Ren G, Zhao D, Li N, Zhu H, and Chen X

Subjects

Administration, Intravenous, Administration, Oral, Animals, Antineoplastic Agents pharmacokinetics, Area Under Curve, Chromatography, Liquid, Indoles administration & dosage, Male, Pyrazoles administration & dosage, Rats, Sprague-Dawley, Reproducibility of Results, Tandem Mass Spectrometry methods, Tissue Distribution, Tubulin Modulators administration & dosage, Indoles pharmacokinetics, Pyrazoles pharmacokinetics, Tubulin Modulators pharmacokinetics

Abstract

1. YMR-65, 5-(5-bromo-1-methyl-1H-indol-3-yl)-3-(3-methoxyphenyl)-4, 5-dihydro-1H-pyrazole-1-carboxamide, is a new tubulin polymerization inhibitor with encouraging anticancer activity. 2. The validated ultra-performance liquid chromatography-tandem mass spectrometer (UPLC-MS/MS) method was successfully applied to the pharmacokinetics, tissue distribution and excretion study of YMR-65 after oral and intravenous administration. The area under concentration-time curve (AUC 0-∞ ) for YMR-65 were 151.67 ± 54.48 and 459.45 ± 49.23 ng/ml*h for oral and intravenous administration at the dosage of 1.5 mg/kg, respectively and the oral bioavailability was about 33.01%. Moreover, YMR-65 was extensively distributed in heart, liver, spleen, lung, kidney, stomach, intestine and testis and the highest were detected in heart, followed by stomach, intestine and liver. The majority of YMR-65 was excreted via feces and its accumulative excretion ratio during the period of 96 h was 19.83 ± 3.01%, but only 1.54 ± 0.37 and 0.215 ± 0.026% for urine within 96 h and bile within 10 h after intravenous administration, respectively, though the fecal and urine excretion were incomplete within 96 h. 3. In summary, this study defined the pharmacokinetic characteristics of YMR-65 in vivo and the important data can be a useful resource for further research and development.

Published

2018

15. Pharmacokinetic evaluation of β-caryophyllene alcohol in rats and beagle dogs.

Author

He J, Zhou S, Li X, Wang C, Yu Y, Chen X, and Lu Y

Subjects

Animals, Dogs, Female, Male, Polycyclic Sesquiterpenes, Rats, Rats, Sprague-Dawley, Sesquiterpenes pharmacokinetics, Sesquiterpenes pharmacology

Abstract

1. β-caryophyllene alcohol (BCPA) has shown therapeutic promise in the treatment of asthma and inflammation with low toxicity. The aim of the current study was to report the pharmacokinetic profiles of BCPA in rats and dogs. 2. Following intravenous administration, BCPA exhibited moderate volumes of distribution (V z ) ranging from 5.63 to 8.97 L/kg in rats and low V z (2.89 ± 1.12 L/kg) in dogs. Systemic plasma clearance was high in both species, resulting in a short elimination half-life ranging from 29.6 to 48.3 min. In rats, the intravenous pharmacokinetics was dose dependent. The measured oral bioavailability was low in rats for BCPA solution (1.17 ± 0.78%), suspension (1.21 ± 0.33%) and PEG formulation (6.22 ± 2.63%). The bioavailability was lower in dogs for BCPA solution (0.12 ± 0.05%) and PEG formulation (0.25 ± 0.07%), indicating significant species difference. However, treatment of plasma samples with β-glucuronidase increased the systematic exposure of BCPA as assessed from AUC (0-∞) by 24.7- or 2.62-fold in rats and dogs, respectively, which suggested glucuronidation was a significant metabolic pathway for BCPA possibly due to first-pass metabolism. 3. In summary, this was the first preclinical pharmacokinetic investigation of BCPA in animals, providing vital knowledge for further preclinical research and subsequent clinical trials.

Published

2018

16. An update on the potential role of intestinal first-pass metabolism for the prediction of drug-drug interactions: the role of PBPK modeling.

Author

Alqahtani S, Bukhari I, Albassam A, and Alenazi M

Subjects

Administration, Oral, Animals, Biological Availability, Humans, Intestinal Absorption, Pharmaceutical Preparations administration & dosage, Drug Interactions, Models, Biological, Pharmaceutical Preparations metabolism

Abstract

Introduction: The intestinal absorption process is a combination of several events that are governed by various factors. Several transport mechanisms are involved in drug absorption through enterocytes via active and/or passive processes. The transported molecules then undergo intestinal metabolism, which together with intestinal transport may affect the systemic availability of drugs. Many studies have provided clear evidence on the significant role of intestinal first-pass metabolism on drug bioavailability and degree of drug-drug interactions (DDIs). Areas covered: This review provides an update on the role of intestinal first-pass metabolism in the oral bioavailability of drugs and prediction of DDIs. It also provides a comprehensive overview and summary of the latest update in the role of physiologically based pharmacokinetic models modeling in prediction of intestinal metabolism and DDIs in humans. Expert opinion: The contribution of intestinal first-pass metabolism in the oral bioavailability of drugs and prediction of DDIs has become more evident over the last few years. Several in vitro, in situ, and in vivo models have been developed to evaluate the role of first-pass metabolism and to predict DDIs. Currently, physiologically based pharmacokinetic modeling is considered the most valuable tool for the prediction of intestinal first-pass metabolism and DDIs.

Published

2018

17. The effect of fenofibric acid on the pharmacokinetics and pharmacodynamics of warfarin in rats.

Author

Guo C, Xue S, Zheng X, Lu Y, Zhao D, Chen X, and Li N

Subjects

Animals, Fenofibrate pharmacology, Male, Rats, Rats, Sprague-Dawley, Anticoagulants pharmacokinetics, Anticoagulants pharmacology, Fenofibrate analogs & derivatives, Warfarin pharmacokinetics, Warfarin pharmacology

Abstract

1. Case reports have shown that coadministration of fenofibric acid (FA) could increase bleeding risks of warfarin, but the mechanisms remained unknown. We therefore investigated the pharmacokinetic and pharmacodynamic interaction between warfarin and FA in rats. 2. Rats received warfarin alone (2 mg/kg) or coadministered with FA (100 mg/kg). FA significantly increased the exposure to warfarin, and decreased that to 7-hydroxywarfarin in rats nearly by two-fold, meanwhile increased C max and prolonged t 1/2 of warfarin. Anticoagulant activity significantly increased, with prothrombin time (PT) up to 199 ± 33 s in coadministered group (approximately ten-fold compared with rats received warfarin alone). Incubation experiments illustrated FA inhibited CYP2C6 and CYP3A1/2 with the IC50 values of 6.98 and 16.14 μM, and inhibited the metabolism of warfarin (K i value of 2.21 μM). Meanwhile, FA decreased the plasma protein binding of warfarin in vitro. 3. Our data suggested that the altered pharmacokinetics and pharmacodynamics of warfarin in rats was primarily attributed to the inhibition of metabolism. Anticoagulant activity monitoring or warfarin dose lowering needs to be considered when patients are coadministered with FA.

Published

2018

18. Non-alcoholic fatty liver disease (NAFLD) - pathogenesis, classification, and effect on drug metabolizing enzymes and transporters.

Author

Cobbina E and Akhlaghi F

Subjects

Animals, Humans, Non-alcoholic Fatty Liver Disease enzymology, Non-alcoholic Fatty Liver Disease etiology, Pharmacokinetics, Non-alcoholic Fatty Liver Disease classification, Non-alcoholic Fatty Liver Disease metabolism

Abstract

Non-alcoholic fatty liver disease (NAFLD) is a spectrum of liver disorders. It is defined by the presence of steatosis in more than 5% of hepatocytes with little or no alcohol consumption. Insulin resistance, the metabolic syndrome or type 2 diabetes and genetic variants of PNPLA3 or TM6SF2 seem to play a role in the pathogenesis of NAFLD. The pathological progression of NAFLD follows tentatively a "three-hit" process namely steatosis, lipotoxicity and inflammation. The presence of steatosis, oxidative stress and inflammatory mediators like TNF-α and IL-6 has been implicated in the alterations of nuclear factors such as CAR, PXR, PPAR-α in NAFLD. These factors may result in altered expression and activity of drug metabolizing enzymes (DMEs) or transporters. Existing evidence suggests that the effect of NAFLD on CYP3A4, CYP2E1 and MRP3 is more consistent across rodent and human studies. CYP3A4 activity is down-regulated in NASH whereas the activity of CYP2E1 and the efflux transporter MRP3 is up-regulated. However, it is not clear how the majority of CYPs, UGTs, SULTs and transporters are influenced by NAFLD either in vivo or in vitro. The alterations associated with NAFLD could be a potential source of drug variability in patients and could have serious implications for the safety and efficacy of xenobiotics. In this review, we summarize the effects of NAFLD on the regulation, expression and activity of major DMEs and transporters. We also discuss the potential mechanisms underlying these alterations.

Published

2017

19. Biocompatible complex coated with glycosaminoglycan for gene delivery.

Author

Iwanaga M, Kodama Y, Muro T, Nakagawa H, Kurosaki T, Sato K, Nakamura T, Kitahara T, and Sasaki H

Subjects

Animals, Cell Line, Tumor, Gene Expression, Liver metabolism, Lung metabolism, Male, Melanoma, Experimental therapy, Mice, Microscopy, Fluorescence, Spleen metabolism, Coated Materials, Biocompatible, Gene Transfer Techniques, Glycosaminoglycans

Abstract

The purpose of this study was to develop a ternary complex of plasmid DNA (pDNA) electrostatically assembled with dendrigraft poly-l-lysine (DGL) and biodegradable glycosaminoglycan for effective and secure gene delivery. High gene expression of pDNA/DGL complex was confirmed with slight cytotoxicity and erythrocyte agglutination. Anionic ternary complexes of 55.4-223.8 nm were formed by the addition of a glycosaminoglycan such as chondroitin sulfate A (CS-A), chondroitin sulfate B (CS-B), chondroitin sulfate C (CS-C) or hyaluronic acid (HA). Using the cell line B16-F10, most of the ternary complexes showed only weak gene expression and little cytotoxicity, although the pDNA/DGL/CS-A complexes maintained a certain level of gene expression. In particular, the pDNA/DGL/CS-A8 complexes showed significantly higher gene expression than pDNA/DGL complexes in the presence of fetal bovine serum. Gene expression from the pDNA/DGL/CS-A8 complex was inhibited by a high concentration of CS-A and endocytosis inhibitors. After intravenous administration of the pDNA/DGL/CS-A8 complex and the pDNA/DGL complex into ddY mice, high gene expression was observed in the reticuloendothelial systems, the pDNA/DGL/CS-A complex is expected to be useful for gene therapy.

Published

2017

20. Epigenetic regulation of drug transporter expression in human tissues.

Author

Hirota T, Tanaka T, Takesue H, and Ieiri I

Subjects

Animals, Biological Transport genetics, Biomarkers metabolism, DNA Methylation genetics, Gene Expression Regulation, Histone Code genetics, Humans, MicroRNAs genetics, Epigenesis, Genetic, Membrane Transport Proteins genetics, Pharmaceutical Preparations metabolism

Abstract

Introduction: Drug transporters are expressed in a number of tissues such as the intestine, liver, and kidney, and play key roles in drug absorption, distribution, and excretion. Variations in drug transporter gene expression significantly contribute to interindividual differences in drug responses. Epigenetic regulation of drug transporter genes has recently emerged as an important mechanism. Epigenetic regulation alters the expression of genes without changing DNA sequences. Epigenetic control mechanisms are associated with DNA methylation, histone modifications, and microRNAs. Herein we discuss recent advances in the study of the transcriptional and post-transcriptional mechanisms of drug transporters with a focus on epigenetic regulation. Areas covered: This review summarizes recent research on the epigenetic regulation of drug transporter genes, and highlights the importance of identifying novel biomarkers based on epigenetics for use in individualized drug therapy. Expert opinion: Researchers are actively attempting to elucidate the epigenetic mechanisms that control the expression of drug transporters, which affect the pharmacokinetics of drugs. Current evidence suggests that epigenetic changes play an important role in drug transporter function. A clearer understanding of epigenetic regulation in drug transporter genes will provide an insight into novel approaches to individualized drug therapy.

Published

2017

21. Drug-drug interactions that interfere with statin metabolism.

Author

Hirota T and Ieiri I

Subjects

Anticholesteremic Agents adverse effects, Atherosclerosis drug therapy, Cytochrome P-450 Enzyme Inhibitors adverse effects, Cytochrome P-450 Enzyme Inhibitors pharmacology, Cytochrome P-450 Enzyme System genetics, Cytochrome P-450 Enzyme System metabolism, Drug Interactions, Humans, Hydroxymethylglutaryl-CoA Reductase Inhibitors adverse effects, Muscular Diseases chemically induced, Polymorphism, Genetic, Rhabdomyolysis chemically induced, Anticholesteremic Agents pharmacokinetics, Cytochrome P-450 Enzyme System drug effects, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacokinetics

Abstract

Introduction: Lipid-lowering drugs, especially hydroxymethylglutaryl-CoA reductase inhibitors (statins), are widely used in the treatment and prevention of atherosclerotic diseases. The benefits of statins are well documented. However, myotoxic side effects, which can sometimes be severe, including myopathy or rhabdomyolysis, have been associated with the use of statins. In some cases, this toxicity is associated with pharmacokinetic alterations. Potent inhibitors of CYP 3A4 significantly increase plasma concentrations of the active forms of simvastatin, lovastatin and atorvastatin. Fluvastatin is metabolized by CYP2C9, while pravastatin, rosuvastatin and pitavastatin are not susceptible to inhibition by any CYP., Areas Covered: This review discusses the pharmacokinetic aspects of the drug-drug interaction with statins and genetic polymorphisms in CYPs, which are involved in the metabolism of statins, and highlights the importance of establishing a system utilizing electronic medical information practically to avoid adverse drug reactions., Expert Opinion: An understanding of the mechanisms underlying statin interactions will help to minimize drug interactions and develop statins that are less prone to adverse interactions. Quantitatively analyzed information for the low-density lipoprotein cholesterol lowering effects of statin based on electronic medical records may be useful for avoiding the adverse effect of statins.

Published

2015

22. Mechanism of the 24-hour rhythm of tumor necrosis factor-alpha formed by onset of rheumatoid arthritis.

Author

Yoshimatsu H, Okazaki F, Ieiri I, and To H

Subjects

Animals, Arthritis, Rheumatoid genetics, Arthritis, Rheumatoid immunology, Biomarkers blood, Cells, Cultured, Disease Models, Animal, Down-Regulation, Lymphotoxin-alpha blood, Lymphotoxin-beta blood, Male, Mice, Inbred MRL lpr, Promoter Regions, Genetic, Serum Amyloid A Protein metabolism, Time Factors, Transcription, Genetic, Transfection, Tumor Necrosis Factor-alpha genetics, Arthritis, Rheumatoid blood, Circadian Rhythm, Inflammation Mediators blood, Tumor Necrosis Factor-alpha blood

Abstract

Objective: Morning stiffness and plasma cytokine levels in rheumatoid arthritis (RA) patients exhibit 24-hour variations. Tumor necrosis factor-α (TNF-α) plays a central role in RA clinical conditions, including the invasion of inflammatory cells, destruction of cartilage, systemic inflammatory response and its levels show a 24-hour rhythm after the onset of RA. In this study, we investigated what cytokines and/or transcriptional factors are involved in the formation of 24-hour variations in TNF-α levels after the onset of RA using MRL/Mpj-Tnfrsf6(lpr) (MRL/lpr) mice., Method: Blood was drawn at six different times from MRL/lpr mice to measure cytokines, serum amyloid A (SAA), IgG rheumatoid factor (IgG-RF) and corticosterone levels. Cytokine and transcriptional factor levels at the different times were measured in 10- and/or 15-week-old MRL/lpr mice. The promoter activity of TNF-α by lymphotoxins (LTs) was investigated using a dual-luciferase assay., Results: SAA and TNF-α concentrations clearly exhibited 24-hour rhythms with higher levels at the light phase and lower levels at the dark phase after RA crisis. The expression of LT-α and LT-β showed significant 24-hour rhythms in 15-week-old MRL/lpr mice and the phases of LT-α and LT-β levels were antiphase compared with that of TNF-α. AP-1 binding sites were found in LT-α and LT-β promoter regions, and jun mRNA expression corresponded to LT-α and LT-β levels. TNF-α promoter activity was decreased due to the co-transfection of LT-α and LT-β., Conclusion: LT-α and LT-β controls the 24-hour rhythm in TNF-α levels after the onset of RA in order to suppress TNF-α promoter activity.

Published

2014

23. Mycophenolic acid glucuronide is transported by multidrug resistance-associated protein 2 and this transport is not inhibited by cyclosporine, tacrolimus or sirolimus.

Author

Patel CG, Ogasawara K, and Akhlaghi F

Subjects

Adenosine Triphosphate pharmacology, Animals, Biological Transport drug effects, Cell Membrane drug effects, Cell Membrane metabolism, Cell Membrane Permeability drug effects, Diffusion, Dogs, Epithelial Cells drug effects, Epithelial Cells metabolism, Humans, Madin Darby Canine Kidney Cells, Multidrug Resistance-Associated Protein 2, Mycophenolic Acid metabolism, Transport Vesicles drug effects, Transport Vesicles metabolism, Cyclosporine pharmacology, Glucuronides metabolism, Multidrug Resistance-Associated Proteins metabolism, Mycophenolic Acid analogs & derivatives, Sirolimus pharmacology, Tacrolimus pharmacology

Abstract

1. The purpose of this study was to investigate the contribution of MRP2 to the efflux of mycophenolic acid (MPA), and its phenyl glucuronide (MPAG) and acyl glucuronide (AcMPAG) metabolites, using Madin-Darby canine kidney II cells stably transfected with human MRP2 gene (MDCKII/MRP2 cells). 2. Compared to parental MDCKII cells, MPAG was significantly translocated from basolateral (BL) to apical (AP) side in MDCKII/MRP2 cells, indicating MPAG is a substrate for MRP2. AcMPAG is highly translocated from BL to AP side in both cells, suggesting that AcMPAG is actively secreted possibly through an efflux transporter other than MRP2. Appreciable translocation of MPA was not observed in MDCKII/MRP2 cells. 3. Furthermore, using MRP2-expressing Sf9 membrane vesicles, the Michaelis-Menten constant (Km) value for MRP2-mediated MPAG transport was calculated at 224.2 ± 42.7 µM. In the vesicle system, cyclosporine, tacrolimus and sirolimus did not inhibit the uptake of MPAG via MRP2. 4. These findings indicate that only MPAG not MPA and AcMPAG is a substrate for MRP2 and that the interaction between MPAG and concomitantly administered immunosuppressive agents does not occur at MRP2 level.

Published

2013

24. Influence of capsaicin on fluctuation of digoxin pharmacokinetics in lipopolysaccharide-treated rats.

Author

Kato R, Higashitani A, Irie T, Kusukawa Y, Yamamoto Y, Nakagawa M, Urashima Y, Nagata M, Hayashi T, Ijiri Y, and Tanaka K

Subjects

Administration, Oral, Animals, Blotting, Western, Capsaicin administration & dosage, Cytochrome P-450 CYP3A, DNA metabolism, Digoxin administration & dosage, Electrophoretic Mobility Shift Assay, Gene Expression Regulation drug effects, Injections, Intravenous, Lipopolysaccharides administration & dosage, Liver drug effects, Liver enzymology, Male, Pregnane X Receptor, Protein Binding drug effects, RNA, Messenger genetics, RNA, Messenger metabolism, Rats, Rats, Wistar, Real-Time Polymerase Chain Reaction, Receptors, Steroid metabolism, Capsaicin pharmacology, Digoxin pharmacokinetics, Lipopolysaccharides pharmacology

Abstract

In the present study, we investigated the influence of Cap on digoxin pharmacokinetics in lipopolysaccharide (LPS)-treated rats. After the oral administration of digoxin (0.1 mg/kg), the area under the plasma concentration-time curve (AUC) of digoxin increased significantly until day 3 after LPS treatment. In the LPS + Cap group, the recovery period of AUC was shortened to 3 days. On days 5 and 7, the maximum plasma concentrations decreased significantly as compared to the control group. The bioavailability of digoxin in LPS group was higher than that in the LPS + Cap group. The hepatic cytochrome P450 (CYP) 3A2 content decreased significantly until day 5 after LPS administration, but it returned to the control level until 5 days in the LPS + Cap group. Hepatic CYP3A2 mRNA expression of LPS group decreased significantly until day 3, but it returned to the control level on day 3 and increased significantly until day 7 in the LPS + Cap group. The DNA-binding activity of pregnane X receptor (PXR) was increased on days 3-7 in the Cap and LPS + Cap group. Cap decreased the absorption of digoxin by inducing CYP3A2 mRNA expression via indirect activation of PXR in LPS-treated rats.

Published

2012

25. Changes in the pharmacokinetics of digoxin in polyuria in streptozotocin-induced diabetic mice and lithium carbonate-treated mice.

Author

Ikarashi N, Kagami M, Kobayashi Y, Ishii M, Toda T, Ochiai W, and Sugiyama K

Subjects

ATP Binding Cassette Transporter, Subfamily B genetics, ATP Binding Cassette Transporter, Subfamily B metabolism, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Animals, Antidepressive Agents adverse effects, Aquaporin 2 metabolism, Aquaporin 2 urine, Aquaporin 3 metabolism, Aquaporin 3 urine, Creatinine metabolism, Drug Interactions, Kidney drug effects, Kidney metabolism, Lithium Carbonate adverse effects, Male, Mice, Mice, Inbred ICR, Models, Biological, Polyuria chemically induced, RNA, Messenger metabolism, Streptozocin, Anti-Arrhythmia Agents pharmacokinetics, Antidepressive Agents pharmacology, Diabetes Mellitus, Experimental metabolism, Digoxin pharmacokinetics, Lithium Carbonate pharmacology, Polyuria metabolism

Abstract

In humans, digoxin is mainly eliminated through the kidneys unchanged, and renal clearance represents approximately 70% of the total clearance. In this study, we used the mouse models to examine digoxin pharmacokinetics in polyuria induced by diabetes mellitus and lithium carbonate (Li(2)CO(3)) administration, including mechanistic evaluation of the contribution of glomerular filtration, tubular secretion, and tubular reabsorption. After digoxin administration to streptozotocin (STZ)-induced diabetic mice, digoxin CL/F increased to approximately 2.2 times that in normal mice. After treatment with Li(2)CO(3) (0.2%) for 10 days, the CL/F increased approximately 1.1 times for normal mice and 1.6 times for STZ mice. Creatinine clearance (CLcr) and the renal mRNA expression levels of mdr1a did not differ significantly between the normal, STZ, and Li(2)CO(3)-treated mice. The urine volume of STZ mice was approximately 26 mL/day, 22 times that of normal mice. The urine volume of Li(2)CO(3)-treated mice increased approximately 7.3 times for normal mice and 2.3 times for STZ mice. These results suggest that the therapeutic effect of digoxin may be significantly reduced in the presence of polyuria either induced by diabetes mellitus or manifested as an adverse effect of Li(2)CO(3) in diabetic patients, along with increased urine volume.

Published

2011

26. Activation of CYP3A-mediated testosterone 6β-hydroxylation by tanshinone IIA and midazolam 1-hydroxylation by cryptotanshinone in human liver microsomes.

Author

Qiu F, Zhang R, Wang G, Gao C, Sun J, Jiang J, and Ma Y

Subjects

Abietanes chemistry, Enzyme Activation drug effects, Humans, Hydroxylation drug effects, Phenanthrenes chemistry, Abietanes pharmacology, Cytochrome P-450 CYP3A metabolism, Hydroxytestosterones metabolism, Microsomes, Liver drug effects, Microsomes, Liver enzymology, Midazolam pharmacology, Phenanthrenes pharmacology, Testosterone metabolism

Abstract

This study evaluated the in vitro activation of CYP3A-mediated midazolam 1-hydroxylation and testosterone 6β-hydroxylation by tanshinone I, tanshinone IIA, and cryptotanshinone. The abilities of tanshinones to activate CYP3A-mediated midazolam 1-hydroxylation and testosterone 6β-hydroxylation in human liver microsomes (HLMs) were tested. Substrate- and effector-dependent activation of CYP3A by tanshinones were both observed. Cryptotanshinone was shown to activate CYP3A-mediated midazolam 1-hydroxylation in a concentration-dependent manner. In contrast, tanshinone IIA and tanshinone I did not activate this hydroxylation reaction. In addition, tanshinone IIA activated CYP3A-mediated testosterone 6β-hydroxylation, whereas cryptotanshinone and tanshinone I did not. The results from our study enhance the understanding of CYP3A activation by tanshinone IIA and cryptotanshinone in HLMs. Additionally, these data allow for an accurate prediction of the magnitude and likelihood of Danshen-drug interactions.

Published

2010

27. Differences in the pharmacokinetics of Cyp3a substrates in TSOD and streptozotocin-induced diabetic mice.

Author

Kudo T, Toda T, Ushiki T, Ohi K, Ikarashi N, Ochiai W, and Sugiyama K

Subjects

Animals, Blotting, Western, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme System analysis, Humans, Insulin administration & dosage, Intestine, Small enzymology, Intestine, Small ultrastructure, Kinetics, Male, Mice, Mice, Inbred C57BL, Mice, Inbred ICR, Mice, Obese, Microsomes enzymology, Microsomes, Liver enzymology, Triazolam administration & dosage, Triazolam metabolism, Triazolam pharmacokinetics, Cytochrome P-450 Enzyme System metabolism, Diabetes Mellitus, Experimental enzymology, Diabetes Mellitus, Type 1 enzymology, Diabetes Mellitus, Type 2 enzymology

Abstract

The pharmacokinetics of drugs can change in diabetes mellitus and even among diabetics. They may differ between type I diabetes (T1DM) and type 2 diabetes (T2DM). As triazolam was administered orally to Tsumura, Suzuki, obese, diabetes (TSOD) mice and streptozotocin (STZ) mice, clearance per body (CL/F) in TSOD mice did not differ compared with Tsumura, Suzuki, non-obesity (TSNO) mice. In STZ mice, CL/F was greater than in control mice. Small intestinal cytochrome P450 (Cyp) 3a expression in TSOD mice was significantly lower than in TSNO mice. No significant difference existed in small intestinal Cyp3a expression between STZ mice and control mice. In insulin-treated mice, small intestinal Cyp3a expression was significantly lower than in control mice. These results suggested that the differences in changes in small intestinal Cyp3a expression between T1DM and T2DM may be due to differences in plasma insulin concentrations. This may be a factor in the difference in the drug pharmacokinetics between T2DM and T1DM patients.

Published

2010

28. Altered expression of CYP in TSOD mice: a model of type 2 diabetes and obesity.

Author

Kudo T, Shimada T, Toda T, Igeta S, Suzuki W, Ikarashi N, Ochiai W, Ito K, Aburada M, and Sugiyama K

Subjects

Animals, Cytochrome P-450 Enzyme System metabolism, Dexamethasone pharmacology, Diabetes Mellitus, Type 2 genetics, Disease Models, Animal, Gene Expression Regulation drug effects, Gluconeogenesis drug effects, Gluconeogenesis genetics, Isoenzymes genetics, Isoenzymes metabolism, Liver drug effects, Liver enzymology, Male, Mice, Obesity genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Receptors, Cytoplasmic and Nuclear genetics, Receptors, Cytoplasmic and Nuclear metabolism, Time Factors, Triazolam metabolism, Triazolam pharmacokinetics, Cytochrome P-450 Enzyme System genetics, Diabetes Mellitus, Type 2 complications, Diabetes Mellitus, Type 2 enzymology, Obesity complications, Obesity enzymology

Abstract

To investigate the pharmacokinetic characteristics in TSOD (Tsumura, Suzuki, obese, diabetes) mice, a model of type 2 diabetes and obesity, the expressions of major hepatic CYP enzymes in TSOD and TSNO (Tsumura, Suzuki, non-obesity; control) mice were compared. The 7-month-old TSOD mice, which represented severe obesity/diabetes-related pathophysiology, showed higher expressions of Cyp2c and Cyp3a compared with TSNO mice, while those of Cyp1a and Cyp2e were lower. Cyp3a metabolic activity was also higher in TSOD mice. In the 7-month-old liver, pregnane X receptor (PXR) (nuclear receptor) and peroxisome proliferator-activated receptor-gamma coactivator-1alpha (PGC-1alpha) (cofactor) mRNA expression were higher in TSOD mice, possibly playing a role in the altered expression of Cyp3a. This specifically altered CYP expression in TSOD mice suggests that the biotransformation of drugs metabolized by these CYP enzymes differs from that in normal animals. Based on these findings, further investigation on the relationship between altered CYP expression and pathophysiology may be useful in elucidating changes in pharmacokinetics in obese/diabetic patients.

Published

2009

29. Genetic polymorphisms of uptake (OATP1B1, 1B3) and efflux (MRP2, BCRP) transporters: implications for inter-individual differences in the pharmacokinetics and pharmacodynamics of statins and other clinically relevant drugs.

Author

Ieiri I, Higuchi S, and Sugiyama Y

Subjects

ATP Binding Cassette Transporter, Subfamily G, Member 2, Animals, Humans, Intestinal Absorption genetics, Liver metabolism, Liver-Specific Organic Anion Transporter 1, Multidrug Resistance-Associated Protein 2, Solute Carrier Organic Anion Transporter Family Member 1B3, ATP-Binding Cassette Transporters genetics, Genetic Variation genetics, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacokinetics, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Multidrug Resistance-Associated Proteins genetics, Neoplasm Proteins genetics, Organic Anion Transporters genetics, Organic Anion Transporters, Sodium-Independent genetics, Polymorphism, Genetic genetics

Abstract

Recent pharmacogenomic/pharmacogenetic studies have disclosed important roles of drug transporters in the pharmacokinetic/pharmacodynamic (PK/PD) profiles of some clinically relevant drugs. It has concurrently been explained that variations in the drug transporter genes are associated with not only inter-individual but also inter-ethnic differences in PK/PD profiles of these drugs. This review focuses on two uptake and two efflux transporters. Organic anion transporting polypeptide (OATP) 1B1 and OATP1B3 are uptake transporters, specifically expressed in the liver, and considered important for drugs, particularly as their pharmacological target organ is the liver. Two ATP-binding cassette transporters, multi-drug resistance-associated protein 2 and breast cancer resistance protein, are efflux transporters, expressed in various human tissues, and considered particularly important for intestinal drug absorption and hepatic drug elimination. All 3-hydroxyl-3-methylglutaryl-CoA reductase inhibitors (statins) except fluvastatin are substrates for OATP1B1, but hepatobiliary (canalicular) efflux transporters differ among statins. In this review, we update the pharmacogenomic/pharmacogenetic properties of these transporters and their effects on PK/PD profiles of statins and other clinically relevant drugs. In addition, we describe a physiologically-based pharmacokinetic model for predicting the effects of changes in transporter activities on systemic and hepatic exposure to pravastatin.

Published

2009

30. Intestinal flora induces the expression of Cyp3a in the mouse liver.

Author

Toda T, Saito N, Ikarashi N, Ito K, Yamamoto M, Ishige A, Watanabe K, and Sugiyama K

Subjects

Animals, Bacteria chemistry, Blotting, Western, Chromatography, High Pressure Liquid, Constitutive Androstane Receptor, Cytochrome P-450 CYP3A, DNA Primers genetics, Germ-Free Life, Isoenzymes metabolism, Kinetics, Lithocholic Acid pharmacology, Male, Mice, Oligonucleotide Array Sequence Analysis, Pregnane X Receptor, Receptors, Cytoplasmic and Nuclear metabolism, Receptors, Steroid metabolism, Reverse Transcriptase Polymerase Chain Reaction, Specific Pathogen-Free Organisms, Transcription Factors metabolism, Cytochrome P-450 Enzyme System metabolism, Gene Expression Regulation, Enzymologic drug effects, Intestines microbiology, Liver metabolism, RNA, Messenger metabolism

Abstract

In order to determine the effects of intestinal flora on the expression of cytochrome P450 (CYP), the mRNA expression of CYP was compared between specific pathogen-free (SPF) and germ-free (GF) mice. Most of the major CYP isozymes showed higher expression in the livers of SPF mice compared with GF mice. Nuclear factors such as pregnane X receptor (PXR) and constitutive androstane receptor (CAR), as well as transporters and conjugation enzymes involved in the detoxification of lithocholic acid (LCA), also showed higher expression in SPF mice. The findings suggest that in the livers of SPF mice, LCA produced by intestinal flora increases the expression of CYPs via activation of PXR and CAR. Drugs such as antibiotics, some diseases and ageing, etc. are known to alter intestinal flora. The present findings suggest that such changes also affect CYP and are one of the factors responsible for individual differences in pharmacokinetics.

Published

2009

31. Drug transporters and renal drug disposition in the newborn.

Author

De Gregori S, De Gregori M, Ranzani GN, Borghesi A, Regazzi M, and Stronati M

Subjects

Animals, Animals, Newborn, Glomerular Filtration Rate, Humans, Kidney Tubules embryology, Mice, Rats, Infant, Newborn metabolism, Kidney Tubules growth & development, Kidney Tubules metabolism, Membrane Transport Proteins metabolism, Pharmaceutical Preparations metabolism

Abstract

The individual response to a drug in terms of drug efficacy and toxicity is highly variable; this represents a major problem in clinical practice. Potential causes for such variability include pathogenesis and severity of the disease being treated, drug interactions, patient age, nutritional status, renal and liver function and concomitant illness. Inherited differences in drug metabolism and genetic polymorphism of targets of drug therapy can have even greater influence on the efficacy and toxicity of medications. We will discuss the role of drug transporters (organic anion transporting polypeptides and Pgp), drug-related gene polymorphisms and pathologies, renal function and drug metabolism in a very special patient population, the newborn. Reliable predictions of drug pharmacokinetics in the newborn, derived from an understanding of the transport mechanisms, should allow therapeutic agents to be used more safely in this special population.

Published

2009

32. Two-year follow-up of the pharmacokinetics of immunosuppressive drugs in a neonate who underwent heart transplantation.

Author

Regazzi M, Perotti G, Pellegrini C, Molinaro MD, Tzialla C, Cabano R, D'Armini AM, Stronati M, and Viganò M

Subjects

Drug Therapy, Combination, Humans, Hypoplastic Left Heart Syndrome drug therapy, Hypoplastic Left Heart Syndrome metabolism, Infant, Infant, Newborn, Male, Metabolic Clearance Rate, Mycophenolic Acid analogs & derivatives, Mycophenolic Acid therapeutic use, Cyclosporine pharmacokinetics, Heart Transplantation, Hypoplastic Left Heart Syndrome surgery, Immunosuppressive Agents pharmacokinetics, Tacrolimus pharmacokinetics

Abstract

The pharmacokinetic properties of immunosuppressive drugs are quite different in newborns than in adults and few studies describe the pharmacokinetics of these drugs in pediatric heart transplant recipients. We report on the two-year follow up of a neonate who underwent heart transplantation for Hypoplastic Left Heart Syndrome on day of life 9. Two different immunosuppressive regimens were used: cyclosporine, azathioprine and prednisone in the early postoperative period, followed by the routine tacrolimus and mycophenolate mofetil combination plus prednisone from post-transplant day 22. Our findings demonstrate marked variability in immunosuppressive pharmacokinetic profiles early post-transplant. Frequent monitoring of drug levels is required to ensure that they remain within the therapeutic range. After the first 2-3 months post-transplant, changes in immunosuppressive drug levels are less marked and correlate more with the administered dosage.

Published

2009

33. Pharmacokinetic model and simulations of dose conversion from immediate- to extended-release tramadol.

Author

Murthy BP, Skee DM, Danyluk AP, Brett V, Vorsanger GJ, and Moskovitz BL

Subjects

Analgesics, Opioid administration & dosage, Analgesics, Opioid blood, Area Under Curve, Clinical Trials, Phase I as Topic statistics & numerical data, Delayed-Action Preparations, Humans, Monte Carlo Method, Randomized Controlled Trials as Topic statistics & numerical data, Tramadol administration & dosage, Tramadol blood, Analgesics, Opioid pharmacokinetics, Computer Simulation, Models, Chemical, Tramadol pharmacokinetics

Abstract

Objective: Extended-release tramadol (tramadol ER) is a once-daily formulation of tramadol approved in the United States for moderate to moderately severe chronic pain in adults. This modeling and simulation analysis was conducted to support dosing recommendations for switching patients receiving immediate-release tramadol (tramadol IR) to tramadol ER., Research Design and Methods: Monte Carlo simulations based on steady-state data from three Phase 1 studies predicted minimum plasma concentration (C(min)), maximum plasma concentration (C(max)), and area under the plasma-concentration-versus-time curve (AUC)., Main Outcome Measures: Pharmacokinetic parameters were compared between 100-mg daily increments of tramadol ER every 24 h (Q24H) and corresponding 25-mg increments of tramadol IR every 6 h (Q6H), such as tramadol ER 200 mg Q24H versus tramadol IR 200, 225, 250, and 275 mg daily., Results: Tramadol ER and IR were predicted to provide similar exposure (AUC) at a total daily dose of 100, 200, or 300 mg. Estimated exposure was comparable between tramadol IR 125-, 225-, and 325-mg and tramadol ER 100-, 200-, and 300-mg, respectively. Estimated exposure was 30-41% lower with tramadol ER 100 mg versus tramadol IR 150 and 175 mg daily, 15-26% lower with tramadol ER 200 mg versus tramadol IR 250 and 275 mg daily, and 8-19% lower with tramadol ER 300 mg versus tramadol IR 350 and 375 mg daily., Conclusions: This pharmacokinetic analysis supports switching patients from a total daily dose of tramadol IR 200 or 300 mg directly to tramadol ER 200 and 300 mg once daily, respectively. Patients who take other doses of tramadol IR may switch to the next lower 100-mg increment of tramadol ER (e.g., from tramadol IR 225, 250, or 275 mg daily in divided doses to tramadol ER 200 mg once daily). Confirmation of these findings would require clinical studies comparing the systemic exposure of tramadol upon switching from the IR to the ER formulation.

Published

2007

34. Genetic polymorphisms of drug transporters: pharmacokinetic and pharmacodynamic consequences in pharmacotherapy.

Author

Ieiri I, Takane H, Hirota T, Otsubo K, and Higuchi S

Subjects

ATP-Binding Cassette Transporters metabolism, Animals, Drug Therapy, Humans, Organic Anion Transporters metabolism, Organic Cation Transport Proteins metabolism, Pharmacogenetics, Pharmacokinetics, Polymorphism, Genetic, ATP-Binding Cassette Transporters genetics, Organic Anion Transporters genetics, Organic Cation Transport Proteins genetics

Abstract

There has been increasing appreciation of the role of drug transporters in pharmacokinetic and pharmacodynamic consequences in pharmacotherapy. The clinical relevance of drug transporters depends on the localisation in human tissues (i.e., vectorial movement), the therapeutic index of the substrates and inherent interindividual variability. With regard to variability, polymorphisms of drug transporter genes have recently been reported to be associated with alterations in the pharmacokinetics and pharmacodynamics of clinically useful drugs. A growing number of preclinical and clinical studies have demonstrated that the application of genetic information may be useful in individualised pharmacotherapy for numerous diseases. However, the reported effects of variants in certain drug transporter genes have been inconsistent and, in some cases, conflicting among studies. Furthermore, the incidence of almost all known variants in transporter genes tends to be racially dependent. These observations suggest the necessity of considering interethnic variability before extrapolating pharmacokinetic data obtained in one ethic group to another, especially in the early phase of drug development. This review focuses on the impact of genetic variations in the function of drug transporters (ABC, organic anion and cation transporters) and the implications of these variations for pharmacotherapy from pharmacokinetic and pharmacodynamic viewpoints.

Published

2006

35. Drug interactions in the management of HIV infection.

Author

Robertson SM, Penzak SR, and Pau AK

Subjects

Anti-HIV Agents therapeutic use, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme Inhibitors, Cytochrome P-450 Enzyme System metabolism, Disease Management, HIV Infections drug therapy, HIV Protease Inhibitors therapeutic use, HIV-1 drug effects, Humans, Anti-HIV Agents pharmacokinetics, Drug Interactions physiology, HIV Infections enzymology, HIV Protease Inhibitors pharmacokinetics, HIV-1 enzymology

Abstract

The availability of antiretroviral therapy has significantly reduced the morbidity and mortality of HIV infection. In addition, improved treatment of opportunistic infections and comorbidities common to patients with HIV is further prolonging the lives of patients. Improvement in the treatment of HIV has led to a significant increase in the number of medications which caregivers are able to utilise to manage HIV/AIDS. Antiretroviral medications, as well as many of the drugs used in the management of opportunistic infections and primary care (e.g., macrolide antibiotics, azole antifungals, cholesterol-lowering medications), are particularly prone to drug interactions. The interpretation of clinically significant interactions is complicated by the rate at which new information on drug metabolism and transport is becoming available. Management of drug interactions in HIV is further confounded by conflicting study results and differences between documented and theoretical inter-actions. The mechanisms and significance of interactions involving antiretrovirals, drugs used for opportunistic infections, and other medications commonly used in HIV patients will be reviewed.

Published

2005

36. Pharmacokinetic and mass balance study of unlabelled and (14)C-labelled emedastine difumarate in healthy volunteers.

Author

Brunner M, Kletter K, Assandri A, Ermanno Corrado M, Eichler HG, and Müller M

Subjects

Adult, Area Under Curve, Carbon Radioisotopes, Female, Humans, Kidney metabolism, Male, Models, Chemical, Time Factors, Benzimidazoles pharmacokinetics, Histamine H1 Antagonists pharmacokinetics

Abstract

1. In a mass balance study, six healthy male volunteers received a single oral dose of 4 mg (14)C-labelled emedastine difumarate. The pharmacokinetics of the total radioactivity and unchanged drug were assessed over 48 h. Urinary and faecal excretion were measured over 120 h. Additionally, urinary metabolites were investigated. 2. In a single- and multiple-dose pharmacokinetic study, nine male and nine female healthy volunteers received 2 mg oral emedastine difumarate b.i.d. or 4 mg o.d. for 7 consecutive days. The plasma pharmacokinetics were assessed on day 1 and at steady-state. 3. The mass balance study demonstrated almost complete gastrointestinal absorption of the administered dose. A total of 94.2% of the radioactivity was eliminated via the kidneys. Unchanged emedastine in the urine accounted for <5% of dose. 5-Hydroxy, 6-hydroxy and N-oxide metabolites previously identified in the Japanese were present in Caucasian subjects. 4. AUC after single and multiple dosing were dose-proportional. On day 7, no statistical difference in AUC(0-24) could be detected between the two regimens, with AUC = 70.6 +/- 36.1 and 71.7 +/- 52.3 ng h ml(-1), respectively. There were no gender differences in the pharmacokinetics of emedastine. 5. The results corroborate the use of emedastine in a Caucasian population and support the extrapolation of safety and efficacy data from Asians to Caucasians.

Published

2002

37. Transfer of drospirenone to breast milk after a single oral administration of 3 mg drospirenone + 30 microg ethinylestradiol to healthy lactating women.

Author

Blode H, Foidart JM, and Heithecker R

Subjects

Adult, Androstenes administration & dosage, Androstenes analysis, Area Under Curve, Ethinyl Estradiol administration & dosage, Female, Humans, Infant, Newborn, Milk, Human drug effects, No-Observed-Adverse-Effect Level, Progesterone Congeners pharmacokinetics, Radioimmunoassay, Androstenes pharmacokinetics, Contraceptives, Oral, Combined pharmacokinetics, Contraceptives, Oral, Hormonal pharmacokinetics, Ethinyl Estradiol pharmacokinetics, Lactation metabolism, Milk, Human metabolism

Abstract

Drospirenone (DRSP) is a synthetic progestogen which has been developed in combination with ethinylestradiol (EE) for use as an oral contraceptive (Yasmin, Schering AG, Berlin, Germany). The pharmacokinetic characteristics of DRSP were evaluated in serum and breast milk from lactating women who received a single oral dose of 3 mg DRSP + 30 microg EE, to determine the fraction of the dose of DRSP which transfers to breast milk. Nine healthy, lactating women were included into the present study and pharmacokinetic data were obtained from six participants. The maximum DRSP concentrations (data given as mean +/- standard deviation) were reached on average 2.5+/-1.2 and 2.8+/-1.3 h in serum and breast milk, respectively after oral administration of 3 mg DRSP + 30 microg EE, and amounted on average to 30.8+/-14.4 and 13.5+/-11.7 ng DRSP/ml in serum and breast milk. The mean breast milk versus serum concentration ratios of DRSP increased from 0.16 to 0.57 within 2 h after dosing and decreased to 0.16 after 24 h. The average ratio of AUC0-48 h, values in breast milk versus serum was 0.23+/-0.09. The mean DRSP concentration in breast milk over the 24-h period after dosing was 3.7+/-1.9 ng/ml. The amount of DRSP measured to be transferred into breast milk in the six women participating in the present study was, on average, 635 ng (range 256.2-1357.9 ng) within 24 h, corresponding to about 0.02% of the maternal dose. Based on the average concentration of the drug in breast milk over 24 h and assuming a daily ingestion of approximately 800 ml breast milk, the daily dose that reaches an infant via breast milk is estimated to be approximately 3 microg DRSP. The subjective and objective tolerances of 3 mg DRSP + 30 microg EE were good, with no adverse events reported.

Published

2001

38. A 1-year pharmacokinetic investigation of a novel oral contraceptive containing drospirenone in healthy female volunteers.

Author

Blode H, Wuttke W, Loock W, Röll G, and Heithecker R

Subjects

Adult, Androstenes blood, Area Under Curve, Carrier Proteins blood, Contraceptives, Oral, Synthetic blood, Female, Humans, Progesterone Congeners blood, Reference Values, Androstenes pharmacokinetics, Contraceptives, Oral, Synthetic pharmacokinetics, Progesterone Congeners pharmacokinetics, Sex Hormone-Binding Globulin metabolism

Abstract

Drospirenone is a novel synthetic progestogen with a pharmacological profile similar to that of natural progesterone. It has been developed in combination with ethinylestradiol for use as an oral contraceptive (EE/DRSP, Yasmin, Schering AG, Berlin, Germany). The pharmacokinetic characteristics of drospirenone and ethinylestradiol have been assessed in healthy female volunteers over a 1-year period. During each of the 13 treatment cycles, volunteers received the combined active ingredients for 21 days, followed by a 7-day, tablet-free interval. The concentrations of the serum proteins, sex hormone binding globulin (SHBG) and corticoid binding globulin (CBG), were determined at intervals after the cessation of treatment (day 21) at the end of cycles 1, 6, 9 and 13. Drospirenone and ethinylestradiol were found to be absorbed rapidly and to reach a peak concentration in serum 1.5-2.0 h after dosing. Serum concentrations ofdrospirenone declined, with mean terminal half-lives of 30.8-32.5 h. Accumulation of both drospirenone and ethinylestradiol was observed within a treatment cycle, with a mean accumulation ratio of 3.0 for drospirenone and 2.1 for ethinylestradiol. In addition, serum drospirenone concentrations increased between treatment cycles 1 and 6, but remained steady thereafter, as reflected in the AUC values determined at the end of treatment cycles 1, 6, 9 and 13. Serum SHBG and CBG concentrations declined in a biphasic manner after cessation of treatment at the end of cycle 13, and physiological steady-state concentrations were reached within 4-6 weeks. In conclusion, drospirenone was absorbed at a similar rate as other synthetic progestogens contained in various oral contraceptives, as indicated by similar tmax values. The terminal half-life of drospirenone was intermediate between those of 19-nortestosterone derivatives like desogestrel, levonorgestrel or gestodene and C21-progestogens like cyproterone acetate. Both active ingredients of the new contraceptive EE/DRSP showed accumulation within a treatment cycle, which is also the case with other synthetic progestogen/ethinylestradiol combinations. Similar to other oral contraceptives, a reversible induction of serum SHBG and CBG concentrations was observed under EE/DRSP treatment.

Published

2000

39. Establishing the dose response curve for metabolic control with troglitazone, an insulin action enhancer, in type 2 diabetes patients.

Author

Young MA, Eckland DJ, Eastmond R, and Lettis S

Subjects

Adult, Aged, Aged, 80 and over, Blood Glucose analysis, Chromans pharmacokinetics, Diabetes Mellitus, Type 2 blood, Dose-Response Relationship, Drug, Double-Blind Method, Fatty Acids, Nonesterified blood, Glycated Hemoglobin analysis, Humans, Hypoglycemic Agents pharmacokinetics, Insulin blood, Middle Aged, Thiazoles pharmacokinetics, Triglycerides blood, Troglitazone, Chromans administration & dosage, Diabetes Mellitus, Type 2 drug therapy, Hypoglycemic Agents administration & dosage, Thiazoles administration & dosage, Thiazolidinediones

Abstract

Troglitazone is a novel once-daily oral antidiabetic agent for the treatment of type 2 diabetes patients. Here, we report the overall dose response characteristics of troglitazone, with respect to effects on metabolic control, using a pharmacodynamic model. Data from week 12 from two previously reported double-blind, randomized, parallel-group, placebo-controlled, dose-ranging multicentre studies examining once-daily doses of 10, 30, 100, 200, 400, 600 and 800 mg of troglitazone were combined for the analyses. The pharmacodynamic relationships for relevant parameters of metabolic control were modelled using a nonlinear regression modelling programme. The troglitazone dose-concentration relationship was linear over 10-800 mg. Using an inhibitory sigmoid Emax model, ED50 values of approximately 100 mg and 200 mg were found for fasting serum glucose and triglycerides, respectively. The 200 mg dose for HbA1c showed an inconsistent reduction compared with placebo between the two studies; this illustrates the difficulties associated with comparing results from different assay techniques. Insulin and nonesterified fatty acid reductions compared with placebo were not consistent between studies, and no pharmacodynamic modelling was possible. No changes in body weight were observed at any dose. Troglitazone was as well tolerated as placebo across the dose range investigated. This pharmacodynamic analysis has established that 200-600 mg once daily can be considered the therapeutic dose range of troglitazone that significantly improves metabolic control in type 2 diabetes patients.

Published

1998