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5. Artemether-lumefantrine dosing for malaria treatment in young children and pregnant women: A pharmacokinetic-pharmacodynamic meta-analysis

Author

Beeson, JG, Kloprogge, F, Workman, L, Borrmann, S, Tekete, M, Lefevre, G, Hamed, K, Piola, P, Ursing, J, Kofoed, PE, Martensson, A, Ngasala, B, Bjorkman, A, Ashton, M, Hietala, SF, Aweeka, F, Parikh, S, Mwai, L, Davis, TME, Karunajeewa, H, Salman, S, Checchi, F, Fogg, C, Newton, PN, Mayxay, M, Deloron, P, Faucher, JF, Nosten, F, Ashley, EA, McGready, R, van Vugt, M, Proux, S, Price, RN, Karbwang, J, Ezzet, F, Bakshi, R, Stepniewska, K, White, NJ, Guerin, PJ, Barnes, K, Tarning, J, Beeson, JG, Kloprogge, F, Workman, L, Borrmann, S, Tekete, M, Lefevre, G, Hamed, K, Piola, P, Ursing, J, Kofoed, PE, Martensson, A, Ngasala, B, Bjorkman, A, Ashton, M, Hietala, SF, Aweeka, F, Parikh, S, Mwai, L, Davis, TME, Karunajeewa, H, Salman, S, Checchi, F, Fogg, C, Newton, PN, Mayxay, M, Deloron, P, Faucher, JF, Nosten, F, Ashley, EA, McGready, R, van Vugt, M, Proux, S, Price, RN, Karbwang, J, Ezzet, F, Bakshi, R, Stepniewska, K, White, NJ, Guerin, PJ, Barnes, K, and Tarning, J

Abstract

BACKGROUND: The fixed dose combination of artemether-lumefantrine (AL) is the most widely used treatment for uncomplicated Plasmodium falciparum malaria. Relatively lower cure rates and lumefantrine levels have been reported in young children and in pregnant women during their second and third trimester. The aim of this study was to investigate the pharmacokinetic and pharmacodynamic properties of lumefantrine and the pharmacokinetic properties of its metabolite, desbutyl-lumefantrine, in order to inform optimal dosing regimens in all patient populations. METHODS AND FINDINGS: A search in PubMed, Embase, ClinicalTrials.gov, Google Scholar, conference proceedings, and the WorldWide Antimalarial Resistance Network (WWARN) pharmacology database identified 31 relevant clinical studies published between 1 January 1990 and 31 December 2012, with 4,546 patients in whom lumefantrine concentrations were measured. Under the auspices of WWARN, relevant individual concentration-time data, clinical covariates, and outcome data from 4,122 patients were made available and pooled for the meta-analysis. The developed lumefantrine population pharmacokinetic model was used for dose optimisation through in silico simulations. Venous plasma lumefantrine concentrations 7 days after starting standard AL treatment were 24.2% and 13.4% lower in children weighing <15 kg and 15-25 kg, respectively, and 20.2% lower in pregnant women compared with non-pregnant adults. Lumefantrine exposure decreased with increasing pre-treatment parasitaemia, and the dose limitation on absorption of lumefantrine was substantial. Simulations using the lumefantrine pharmacokinetic model suggest that, in young children and pregnant women beyond the first trimester, lengthening the dose regimen (twice daily for 5 days) and, to a lesser extent, intensifying the frequency of dosing (3 times daily for 3 days) would be more efficacious than using higher individual doses in the current standard treatment regimen (twice

Published
2018

6. Clinical pharmacokinetics and pharmacodynamics and pharmacodynamics of artemether-lumefantrine

Author

White, NJ, van Vugt, M, and Ezzet, F

Abstract

The combination of artemether and lumefantrine (benflumetol) is a new and very well tolerated oral antimalarial drug effective even against multidrug-resistant falciparum malaria. The artemether component is absorbed rapidly and biotransformed to dihydroartemisinin, and both are eliminated with terminal half-lives of around 1 hour. These are very active antimalarials which give a rapid reduction in parasite biomass and consequent rapid resolution of symptoms. The lumefantrine component is absorbed variably in malaria, and is eliminated more slowly (half-life of 3 to 6 days). Absorption is very dependent on coadministration with fat, and so improves markedly with recovery from malaria. Thus artemether clears most of the infection, and the lumefantrine concentrations that remain at the end of the 3- to 5-day treatment course are responsible for eliminating the residual 100 to 10 000 parasites. The area under the curve of plasma lumefantrine concentrations versus time, or its correlate the plasma concentration on day 7. has proved an important determinant of therapeutic response. Characterisation of these pharmacokinetic-pharmacodynamic relationships provided the basis for dosage optimisation, an approach that could be applied to other antimalarial drugs.

Published
2016

15. Clinical pharmacokinetics and pharmacodynamics and pharmacodynamics of artemether-lumefantrine.

Author

White, N J, van Vugt, M, and Ezzet, F

Subjects
PROTOZOA physiology, ANIMAL experimentation, ANTIMALARIALS, COMBINATION drug therapy, CLINICAL trials, COMPARATIVE studies, DRUG resistance, DRUG resistance in microorganisms, DRUG-food interactions, ETHANOLAMINES, HYDROCARBONS, MALARIA, RESEARCH methodology, MEDICAL cooperation, RESEARCH, RESEARCH funding, EVALUATION research, PHARMACODYNAMICS
Abstract

The combination of artemether and lumefantrine (benflumetol) is a new and very well tolerated oral antimalarial drug effective even against multidrug-resistant falciparum malaria. The artemether component is absorbed rapidly and biotransformed to dihydroartemisinin, and both are eliminated with terminal half-lives of around 1 hour. These are very active antimalarials which give a rapid reduction in parasite biomass and consequent rapid resolution of symptoms. The lumefantrine component is absorbed variably in malaria, and is eliminated more slowly (half-life of 3 to 6 days). Absorption is very dependent on coadministration with fat, and so improves markedly with recovery from malaria. Thus artemether clears most of the infection, and the lumefantrine concentrations that remain at the end of the 3- to 5-day treatment course are responsible for eliminating the residual 100 to 10 000 parasites. The area under the curve of plasma lumefantrine concentrations versus time, or its correlate the plasma concentration on day 7. has proved an important determinant of therapeutic response. Characterisation of these pharmacokinetic-pharmacodynamic relationships provided the basis for dosage optimisation, an approach that could be applied to other antimalarial drugs. [ABSTRACT FROM AUTHOR]

Published
1999
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16. Clinical Pharmacokinetics and Pharmacodynamics of Artemether-Lumefantrine.

Author

White, N.J., van Vugt, M., and Ezzet, F.

Subjects
ANTIMALARIALS, PHARMACOKINETICS, PHARMACODYNAMICS
Abstract

The combination of artemether and lumefantrine (benflumetol) is a new and very well tolerated oral antimalarial drug effective even against multidrug-resistant falciparum malaria. The artemether component is absorbed rapidly and biotransformed to dihydroartemisinin, and both are eliminated with terminal half-lives of around 1 hour. These are very active antimalarials which give a rapid reduction in parasite biomass and consequent rapid resolution of symptoms. The lumefantrine component is absorbed variably in malaria, and is eliminated more slowly (half-life of 3 to 6 days). Absorption is very dependent on coadministration with fat, and so improves markedly with recovery from malaria. Thus artemether clears most of the infection, and the lumefantrine concentrations that remain at the end of the 3- to 5-day treatment course are responsible for eliminating the residual 100 to 10 000 parasites. The area under the curve of plasma lumefantrine concentrations versus time, or its correlate the plasma concentration on day 7, has proved an important determinant of therapeutic response. Characterisation of these pharmacokinetic-pharmacodynamic relationships provided the basis for dosage optimisation, an approach that could be applied to other antimalarial drugs. [ABSTRACT FROM AUTHOR]

Published
1999
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19. Artemether-lumefantrine dosing for malaria treatment in young children and pregnant women: A pharmacokinetic-pharmacodynamic meta-analysis.

Author

Kloprogge F, Workman L, Borrmann S, Tékété M, Lefèvre G, Hamed K, Piola P, Ursing J, Kofoed PE, Mårtensson A, Ngasala B, Björkman A, Ashton M, Friberg Hietala S, Aweeka F, Parikh S, Mwai L, Davis TME, Karunajeewa H, Salman S, Checchi F, Fogg C, Newton PN, Mayxay M, Deloron P, Faucher JF, Nosten F, Ashley EA, McGready R, van Vugt M, Proux S, Price RN, Karbwang J, Ezzet F, Bakshi R, Stepniewska K, White NJ, Guerin PJ, Barnes KI, and Tarning J

Subjects
Antimalarials pharmacokinetics, Artemether, Lumefantrine Drug Combination pharmacokinetics, Child, Preschool, Dose-Response Relationship, Drug, Ethanolamines metabolism, Ethanolamines pharmacokinetics, Ethanolamines pharmacology, Female, Fluorenes metabolism, Fluorenes pharmacokinetics, Fluorenes pharmacology, Humans, Infant, Infant, Newborn, Malaria, Falciparum drug therapy, Male, Models, Chemical, Pregnancy, Antimalarials pharmacology, Antimalarials therapeutic use, Artemether, Lumefantrine Drug Combination pharmacology, Artemether, Lumefantrine Drug Combination therapeutic use
Abstract

Background: The fixed dose combination of artemether-lumefantrine (AL) is the most widely used treatment for uncomplicated Plasmodium falciparum malaria. Relatively lower cure rates and lumefantrine levels have been reported in young children and in pregnant women during their second and third trimester. The aim of this study was to investigate the pharmacokinetic and pharmacodynamic properties of lumefantrine and the pharmacokinetic properties of its metabolite, desbutyl-lumefantrine, in order to inform optimal dosing regimens in all patient populations., Methods and Findings: A search in PubMed, Embase, ClinicalTrials.gov, Google Scholar, conference proceedings, and the WorldWide Antimalarial Resistance Network (WWARN) pharmacology database identified 31 relevant clinical studies published between 1 January 1990 and 31 December 2012, with 4,546 patients in whom lumefantrine concentrations were measured. Under the auspices of WWARN, relevant individual concentration-time data, clinical covariates, and outcome data from 4,122 patients were made available and pooled for the meta-analysis. The developed lumefantrine population pharmacokinetic model was used for dose optimisation through in silico simulations. Venous plasma lumefantrine concentrations 7 days after starting standard AL treatment were 24.2% and 13.4% lower in children weighing <15 kg and 15-25 kg, respectively, and 20.2% lower in pregnant women compared with non-pregnant adults. Lumefantrine exposure decreased with increasing pre-treatment parasitaemia, and the dose limitation on absorption of lumefantrine was substantial. Simulations using the lumefantrine pharmacokinetic model suggest that, in young children and pregnant women beyond the first trimester, lengthening the dose regimen (twice daily for 5 days) and, to a lesser extent, intensifying the frequency of dosing (3 times daily for 3 days) would be more efficacious than using higher individual doses in the current standard treatment regimen (twice daily for 3 days). The model was developed using venous plasma data from patients receiving intact tablets with fat, and evaluations of alternative dosing regimens were consequently only representative for venous plasma after administration of intact tablets with fat. The absence of artemether-dihydroartemisinin data limited the prediction of parasite killing rates and recrudescent infections. Thus, the suggested optimised dosing schedule was based on the pharmacokinetic endpoint of lumefantrine plasma exposure at day 7., Conclusions: Our findings suggest that revised AL dosing regimens for young children and pregnant women would improve drug exposure but would require longer or more complex schedules. These dosing regimens should be evaluated in prospective clinical studies to determine whether they would improve cure rates, demonstrate adequate safety, and thereby prolong the useful therapeutic life of this valuable antimalarial treatment., Competing Interests: I have read the journal's policy and the authors of this manuscript have the following competing interests: KIB and NJW are members of the WHO Technical Expert Group (TEG) on Malaria Chemotherapy. KIB is also a member of the WHO TEG on Drug Resistance and Containment. KIB, NJW, JT and SP are members of the WHO Malaria Chemotherapy sub-group on dosage recommendations. GL, KH, FE and RB are employees of Novartis, the manufacturer of the drug that is the subject of this publication. EAA and NJW are members of the Editorial Board of PLOS Medicine. None of the authors declare any other conflict of interest.

Published
2018
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20. Daily dosing of vismodegib to steady state does not prolong the QTc interval in healthy volunteers.

Author

Graham RA, Chang I, Jin JY, Wang B, Dufek MB, Ayache JA, Ezzet F, Zerivitz K, Low JA, and Dresser MJ

Subjects
Administration, Oral, Aged, Anilides adverse effects, Anilides pharmacokinetics, Antineoplastic Agents adverse effects, Antineoplastic Agents pharmacokinetics, Aza Compounds administration & dosage, Double-Blind Method, Drug Administration Schedule, Electrocardiography, Female, Fluoroquinolones, France, Heart Rate drug effects, Humans, Linear Models, Long QT Syndrome chemically induced, Long QT Syndrome physiopathology, Middle Aged, Models, Biological, Moxifloxacin, Pyridines adverse effects, Pyridines pharmacokinetics, Quinolines administration & dosage, Risk Assessment, Time Factors, Anilides administration & dosage, Antineoplastic Agents administration & dosage, Pyridines administration & dosage
Abstract

Introduction: Vismodegib was assessed as being of low risk for QT interval prolongation based on prior nonclinical and clinical experience. A dedicated study was conducted to further assess the potential for vismodegib to prolong the QTc interval., Methods and Results: Given the nonlinear pharmacokinetics of vismodegib, a thorough QTc study as is typically designed was not possible, and an innovative design was employed. This dedicated QTc study was powered to exclude a 20-millisecond change from the baseline QTc interval. The subjects were administered daily oral 150 mg of vismodegib for 7 days, or a single dose of 400 mg of moxifloxacin, with corresponding matching placebos. The upper limits of the 90% confidence intervals for the difference in ΔQTcF between vismodegib and placebo at steady state were <20 milliseconds at all timepoints with a maximum of 10 milliseconds at 12 hours postdose. Exposure-response analysis yielded an estimated slope equal to 0.11 ms/μM, which was not statistically significant. After a single dose of moxifloxacin was administered, the lower limits of the 90% confidence interval of the difference in ΔQTcF between moxifloxacin and placebo were >5 milliseconds from 1-12 hours postdose, thereby establishing assay sensitivity., Conclusions: There was no effect of vismodegib on the QTc interval when dosed daily at 150 mg to steady state.

Published
2013
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21. Armodafinil and modafinil in patients with excessive sleepiness associated with shift work disorder: a pharmacokinetic/pharmacodynamic model for predicting and comparing their concentration-effect relationships.

Author

Darwish M, Bond M, and Ezzet F

Subjects
Benzhydryl Compounds blood, Central Nervous System Stimulants blood, Double-Blind Method, Humans, Modafinil, Sleep Disorders, Circadian Rhythm blood, Sleep Disorders, Circadian Rhythm physiopathology, Wakefulness drug effects, Benzhydryl Compounds pharmacology, Central Nervous System Stimulants pharmacology, Models, Biological, Sleep Disorders, Circadian Rhythm drug therapy
Abstract

Armodafinil, the longer lasting R-isomer of racemic modafinil, improves wakefulness in patients with excessive sleepiness associated with shift work disorder (SWD). Pharmacokinetic studies suggest that armodafinil achieves higher plasma concentrations than modafinil late in a dose interval following equal oral doses. Pooled Multiple Sleep Latency Test (MSLT) data from 2 randomized, double-blind, placebo-controlled trials in 463 patients with SWD, 1 with armodafinil 150 mg/d and 1 with modafinil 200 mg/d (both administered around 2200 h before night shifts), were used to build a pharmacokinetic/pharmacodynamic model. Predicted plasma drug concentrations were obtained by developing and applying a population pharmacokinetic model using nonlinear mixed-effects modeling. Armodafinil 200 mg produced a plasma concentration above the EC(50) (4.6 µg/mL) for 9 hours, whereas modafinil 200 mg did not exceed the EC(50). Consequently, armodafinil produced greater increases in predicted placebo-subtracted MSLT times of 0.5-1 minute (up to 10 hours after dosing) compared with modafinil. On a milligram-to-milligram basis, armodafinil 200 mg consistently increased wakefulness more than modafinil 200 mg, including times late in the 8-hour shift.

Published
2012
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22. The use of biosimulation in the design of a novel multilevel weight loss maintenance program for overweight children.

Author

Wilfley DE, Van Buren DJ, Theim KR, Stein RI, Saelens BE, Ezzet F, Russian AC, Perri MG, and Epstein LH

Subjects
Child, Child Behavior, Female, Health Promotion methods, Humans, Life Style, Male, Overweight psychology, Psychology, Child, Recurrence, Risk Reduction Behavior, Social Support, Computer Simulation, Health Behavior, Overweight prevention & control, Overweight therapy, Weight Loss physiology
Abstract

Weight loss outcomes achieved through conventional behavior change interventions are prone to deterioration over time. Basic learning laboratory studies in the area of behavioral extinction and renewal and multilevel models of weight control offer clues as to why newly acquired weight loss skills are prone to relapse. According to these models, current clinic-based interventions may not be of sufficient duration or scope to allow for the practice of new skills across the multiple community contexts necessary to promote sustainable weight loss. Although longer, more intensive interventions with greater reach may hold the key to improving weight loss outcomes, it is difficult to test these assumptions in a time efficient and cost-effective manner. A research design tool that has been increasingly utilized in other fields (e.g., pharmaceuticals) is the use of biosimulation analyses. The present study describes our research team's use of computer simulation models to assist in designing a study to test a novel, comprehensive socio-environmental treatment approach to weight loss maintenance in children ages 7-12 years. Weight outcome data from the weight loss, weight maintenance, and follow-up phases of a recently completed randomized controlled trial (RCT) were used to describe the time course of a proposed, extended multilevel treatment program. Simulations were then conducted to project the expected changes in child percent overweight (POW) trajectories in the proposed study. A 12.9% decrease in POW at 30 months was estimated based upon the midway point between models of "best-case" and "worst-case" weight maintenance scenarios. Preliminary data and further analyses, including biosimulation projections, suggest that our socio-environmental approach to weight loss maintenance treatment is promising and warrants evaluation in a large-scale RCT. Biosimulation techniques may have utility in the design of future community-level interventions for the treatment and prevention of childhood overweight.

Published
2010
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23. Oral bioavailability of posaconazole in fasted healthy subjects: comparison between three regimens and basis for clinical dosage recommendations.

Author

Ezzet F, Wexler D, Courtney R, Krishna G, Lim J, and Laughlin M

Subjects
Administration, Oral, Adult, Biological Availability, Cross-Over Studies, Drug Administration Schedule, Humans, Male, Models, Biological, Triazoles adverse effects, Fasting metabolism, Triazoles administration & dosage, Triazoles pharmacokinetics
Abstract

Background and Objective: Posaconazole is a potent, extended-spectrum triazole antifungal agent currently in clinical development for the treatment of invasive fungal infections. This study was conducted to compare the bioavailability and resulting serum concentrations of posaconazole 800 mg following administration of three different dose regimens to fasting adults., Study Design: This was a randomised, open-label, three-way crossover study., Methods: Subjects fasted 12 hours before and 48 hours after the administration of posaconazole oral suspension (800 mg) given as a single dose (regimen A), 400 mg every 12 hours (regimen B) or 200 mg every 6 hours (regimen C). Plasma posaconazole concentrations were determined for 48 hours after the initial dose and subjects completed a 1-week washout period between treatment regimens. A one-compartment oral model with first-order rate of absorption and first-order rate of elimination was fitted to the plasma concentration-time data. Differences in exposure were investigated by allowing the bioavailability fraction to vary among regimens., Study Participants: A total of 18 healthy men were enrolled in and completed the study., Main Outcome Measures and Results: Posaconazole relative bioavailability was estimated to be significantly different among regimens (p < 0.0001) and increased with the number of doses, such that regimen B/regimen A = 1.98 +/- 0.35, representing a 98% increase, and regimen C/regimen A = 3.20 +/- 0.69, or a 220% increase. With use of the one-compartment model, the population steady-state values for area under the concentration-time curve over 24 hours were predicted to be 3900, 7700 and 12 400 microg.h/L, with average plasma concentrations of 162, 320 and 517 microg/L for regimens A, B and C, respectively., Conclusion: These data suggest that divided daily dose administration (every 12 or 6 hours) significantly increases posaconazole exposure under fasted conditions.

Published
2005
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24. Pharmacodynamics of a new triazole, posaconazole, in a murine model of disseminated candidiasis.

Author

Andes D, Marchillo K, Conklin R, Krishna G, Ezzet F, Cacciapuoti A, and Loebenberg D

Subjects
Animals, Area Under Curve, Candida albicans drug effects, Candidiasis microbiology, Colony Count, Microbial, Dose-Response Relationship, Drug, Female, Mice, Mice, Inbred ICR, Microbial Sensitivity Tests, Neutropenia chemically induced, Neutropenia complications, Antifungal Agents pharmacokinetics, Antifungal Agents therapeutic use, Candidiasis drug therapy, Triazoles pharmacokinetics, Triazoles therapeutic use
Abstract

Previous in vivo studies have characterized the pharmacodynamic characteristics of two triazole compounds, fluconazole and ravuconazole. These investigations demonstrated that the 24-h area under the concentration-time curve (AUC)/MIC ratio is the critical pharmacokinetic-pharmacodynamic (PK-PD) parameter associated with treatment efficacy. Further analysis demonstrated that a free-drug triazole 24-h AUC/MIC ratio of 20 to 25 was predictive of treatment success in both experimental models and clinical trials. We used a neutropenic murine model of disseminated Candida albicans infection to similarly characterize the time course activity of the new triazole, posaconazole. The PK-PD parameters (percent time above MIC, AUC/MIC ratio, and peak serum drug level/MIC ratio) were correlated with in vivo efficacy, as measured by organism number in kidney cultures after 48 h of therapy. Kinetics and protein binding following oral posaconazole dosing were performed in neutropenic infected mice. Peak levels and AUC from 0 h to infinity values were nonlinear over the 16-fold dose range studied. Serum drug elimination half-life ranged from 12.0 to 17.7 h. Protein binding was 99%. Single dose postantifungal effect studies demonstrated prolonged suppression of organism regrowth after serum posaconazole levels had fallen below the MIC. Treatment efficacy with the four dosing intervals studied was similar, supporting the AUC/MIC ratio as the PK-PD parameter predictive of efficacy. Nonlinear regression analysis also suggested that the AUC/MIC ratio was strongly predictive of treatment outcomes (AUC/MIC ratio R(2) = 83%; peak serum drug/MIC ratio R(2) = 85%; time that serum levels of posaconazole remained above the MIC R(2) = 65%). Similar studies were conducted with 11 additional C. albicans isolates with various posaconazole susceptibilities (MIC, 0.015 to 0.12 micro g/ml) to determine if a similar 24-h AUC/MIC ratio was associated with efficacy. The posaconazole free-drug AUC/MIC ratios were similar for all of the organisms studied (6.12 to 26.7, mean +/- SD = 16.9 +/- 7.8, P value, 0.42). These free-drug AUC/MIC ratios are similar to those observed for other triazoles in this model.

Published
2004
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25. Population pharmacokinetic analysis of pegylated interferon alfa-2b and interferon alfa-2b in patients with chronic hepatitis C.

Author

Jen JF, Glue P, Ezzet F, Chung C, Gupta SK, Jacobs S, and Hajian G

Subjects
Adolescent, Adult, Aged, Algorithms, Antiviral Agents adverse effects, Antiviral Agents therapeutic use, Blood Platelets metabolism, Chronic Disease, Female, Hepatitis C drug therapy, Humans, Interferon alpha-2, Logistic Models, Male, Middle Aged, Models, Biological, Neutrophils metabolism, Population, Recombinant Proteins, Antiviral Agents pharmacokinetics, Hepatitis C metabolism, Interferon-alpha adverse effects, Interferon-alpha pharmacokinetics, Interferon-alpha therapeutic use, Polyethylene Glycols
Abstract

Background: This study quantified pharmacokinetic changes in pegylated and nonpegylated interferon alfa-2b during 48 weeks of treatment and the influences of covariates on the basis of sparsely sampled serum concentrations and activity values. Possible relationships between pharmacokinetic and pharmacodynamic variables were investigated., Methods: Patients with chronic hepatitis C were enrolled in a clinical trial that compared the efficacy of pegylated interferon alfa-2b with interferon alfa-2b. Single blood samples were obtained from each patient at weeks 4, 12, 24, 36, and 48. Three pharmacostatistical models were developed for 2 immunoassays and 1 bioassay., Results: Apparent clearance values of pegylated interferon alfa-2b and interferon alfa-2b at the end of treatment declined 33.7% and 80.0%, respectively, from their week 4 values. Bioactivity increased 41% to 58% at week 48 for different treatment groups. Changes were greatest in the first weeks of administration and diminished during the subsequent months. Body weight had a modest positive effect on clearance values and activity. Within each dose level, no significant associations were observed between pharmacokinetic variables and any pharmacodynamic variables (hepatitis C virus--RNA responses or changes in neutrophils and platelets)., Conclusions: This analysis confirms earlier observations of progressive pharmacokinetic changes in the patients with hepatitis C during 48 weeks of treatment. The absence of a relationship between toxicity or efficacy variables and interferon concentration or activity (within a dose level) suggests that clinical management of patients (eg, for efficacy or to manage toxicity) should be based on clinically derived dosing guidelines rather than on serum concentration or activity criteria.

Published
2001
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26. Population pharmacokinetics and therapeutic response of CGP 56697 (artemether + benflumetol) in malaria patients.

Author

Ezzet F, Mull R, and Karbwang J

Subjects
Adolescent, Adult, Antimalarials pharmacology, Antimalarials therapeutic use, Artemether, Artemether, Lumefantrine Drug Combination, Double-Blind Method, Drug Combinations, Ethanolamines pharmacokinetics, Female, Fluorenes pharmacology, Fluorenes therapeutic use, Humans, Lumefantrine, Malaria drug therapy, Male, Middle Aged, Sesquiterpenes pharmacology, Sesquiterpenes therapeutic use, Treatment Outcome, Antimalarials pharmacokinetics, Artemisinins, Fluorenes pharmacokinetics, Malaria metabolism, Sesquiterpenes pharmacokinetics
Abstract

Aims: To investigate the pharmacokinetic and pharmacodynamic properties of artemether and benflumetol in a fixed combination tablet (CGP 56697) and to offer an explanation for the lower than expected cure rate in a Thai clinical trial., Methods: Two hundred and sixty patients were enrolled into a randomized, double-blind, parallel group, dose-finding trial. CGP 56697 was given orally, either as: A, 4 x 4 tablets over 48 h; B, 4 x 2 tablets over 48 h or C, 3 x 4 tablets over 24 h. Each tablet contained artemether 20 mg amd benflumetol 120 mg. The pharmacokinetics were determined using a population-based approach combining full profiles (42 patients) and sparse data (218 patients). Parasite clearance time and 28 day cure rate were correlated with the derived pharmacokinetic parameters., Results: The median absorption half-life of benflumetol was 5.3 h, with a tmax of 10 h and terminal elimination half-life of 4.5 days. For artemether (and its metabolite, dihydroartemisinin), the corresponding values were 1.9 (1.9) h, 1.8 (1.2) h, and 0.84 (0.43) h. The variability in bioavailability of artemether and dihydroartemisinin was large both between doses and between patients, but was less pronounced for benflumetol. Compared with the first dose, benflumetol bioavailability was estimated to increase three-fold by the third and fourth doses. Higher artemether or dihydroartemisinin AUC was found to decrease parasite clearance time. Higher benflumetol AUC was found to significantly increase the chance of cure., Conclusions: Using a population-based approach it was confirmed that the pharmacokinetic and pharmacodynamic properties of benflumetol and artemether differ markedly. Benflumetol AUC is associated with cure and the effect of benflumetol when coadministered with artemether is to prevent recrudescence. The mode of action of benflumetol is consistent with its longer elimination half-life. A short course of low-dose artemether, which is rapidly absorbed and has a short elimination half-life, produced effective parasite clearance. The complementary pharmacokinetic and pharmacodynamic properties of benflumetol and artemether was the main rationale for developing a fixed-dose combination. While the 4 x 4 dose regimen is very effective in most endemic areas, the poorer absorption (2.5 fold lower than in China) and the more resistant parasites in Thailand require higher doses of this drug.

Published
1998
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27. A random effects model for ordinal responses from a crossover trial.

Author

Ezzet F and Whitehead J

Subjects
Data Interpretation, Statistical, Mathematical Computing, Probability, Random Allocation, Clinical Trials as Topic methods, Models, Statistical
Abstract

Crossover studies have been successfully conducted in the case of continuous responses. Existing procedures of analysis for ordinal responses, on the other hand, are rarely satisfactory unless strict, usually unrealistic, assumptions are made. In this paper we investigate a random effects model and show that the model is simple and general. Interpretation of parameters is easy, though with a complicated fitting procedure.

Published
1991
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28. Long-term follow-up of asymptomatic carotid bruits.

Author

Dorazio RA, Ezzet F, and Nesbitt NJ

Subjects
Adult, Aged, Auscultation, Cerebrovascular Disorders epidemiology, Female, Follow-Up Studies, Humans, Ischemic Attack, Transient epidemiology, Male, Middle Aged, Time Factors, Carotid Artery Diseases diagnosis
Abstract

Ninety-seven patients with asymptomatic carotid bruits were followed up 5 to 13 years or until the occurrence of transient ischemic attacks, stroke or death. In 11% of the patients transient ischemic attacks developed and in 19%, strokes. Symptoms that developed in more than half of the patients did so within 2 years and 90% within 6 years of detection of the bruit. Seventeen of 18 strokes occurred without antecedent transient ischemic attacks. Fifty-three of the patients underwent 94 major noncarotid operations with no postoperative strokes. Death occurred in 37% of the patients during the follow-up period, and 90% of the deaths were due to cardiac problems or stroke.

Published
1980
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29. Horseshoe and pelvic kidneys associated with abdominal aortic aneurysms.

Author

Ezzet F, Dorazio R, and Herzberg R

Subjects
Aged, Aorta, Abdominal surgery, Aortic Aneurysm surgery, Female, Humans, Kidney surgery, Male, Middle Aged, Aortic Aneurysm complications, Kidney abnormalities
Abstract

Preoperative recognitiion of horseshoe or pelvic kidney with abdominal aortic aneurysm greatly facilitates proper operative care of such patients. Operative management of three reported patients varied significantly, depending on complicated and anomalous blood supply to the kidney.

Published
1977
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30. Arterial complications of the thoracic outlet syndrome.

Author

Dorazio RA and Ezzet F

Subjects
Adult, Aged, Aneurysm surgery, Arm blood supply, Female, Humans, Male, Methods, Nerve Compression Syndromes surgery, Thromboembolism surgery, Aneurysm etiology, Brachial Artery, Brachial Plexus, Nerve Compression Syndromes complications, Subclavian Artery, Thromboembolism etiology
Published
1979
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