Your search keyword '"C, Dubruc"' showing total 67 results

1. The pharmacokinetics of idraparinux, a long-acting indirect factor Xa inhibitor: population pharmacokinetic analysis from Phase III clinical trials

Author

M. Trellu, C. Veyrat-Follet, N. Vivier, G. J. Sanderink, and C. Dubruc

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, medicine.drug_mechanism_of_action, Metabolic Clearance Rate, Idraparinux, Population, Factor Xa Inhibitor, Oligosaccharides, Renal function, Phases of clinical research, Pharmacology, Gastroenterology, Young Adult, chemistry.chemical_compound, Pharmacokinetics, Internal medicine, Atrial Fibrillation, Secondary Prevention, Humans, Medicine, Single-Blind Method, Renal Insufficiency, Child, education, Aged, Aged, 80 and over, Venous Thrombosis, Volume of distribution, education.field_of_study, Creatinine, business.industry, Hematology, Middle Aged, chemistry, Child, Preschool, Female, Pulmonary Embolism, business, Factor Xa Inhibitors, Half-Life

Abstract

Summary. Background: Idraparinux, a long-acting synthetic pentasaccharide, is a specific antithrombin-dependent inhibitor of activated factor X that has been investigated in the treatment and prevention of thromboembolic events. Objectives: To characterize the population pharmacokinetic profile of idraparinux in patients enrolled in van Gogh and Amadeus Phase III clinical trials. Patients and methods: Idraparinux was administered once-weekly subcutaneously at a dose of 2.5 mg, or 2.5 mg (first dose) and then 1.5 mg for patients with severe renal insufficiency (creatinine clearance

Published

2009

2. New metabolic and pharmacokinetic characteristics of thiocolchicoside and its active metabolite in healthy humans

Author

P Lluel, J P Thénot, A Filali-Ansary, M. Trellu, D Françon, C Dubruc, and R Adam

Subjects

Adult, Male, Muscle Relaxation, Metabolite, Administration, Oral, Biological Availability, Pharmacology, urologic and male genital diseases, Intestinal absorption, Rats, Sprague-Dawley, chemistry.chemical_compound, Pharmacokinetics, Oral administration, medicine, Animals, Humans, Pharmacology (medical), Chromatography, High Pressure Liquid, Active metabolite, Cross-Over Studies, female genital diseases and pregnancy complications, Rats, Bioavailability, Muscle relaxation, Intestinal Absorption, chemistry, Thiocolchicoside, Area Under Curve, Colchicine, Half-Life, medicine.drug

Abstract

Thiocolchicoside (TCC) has been prescribed for several years as a muscle relaxant drug, but its pharmacokinetic (PK) profile and metabolism still remain largely unknown. Therefore, we re-investigated its metabolism and PK, and we assessed the muscle relaxant properties of its metabolites. After oral administration of 8 mg (a therapeutic dose) of 14C-labelled TCC to healthy volunteers, we found no detectable TCC in plasma, urine or faeces. On the other hand, the aglycone derivative obtained after de-glycosylation of TCC (M2) was observed and, in addition, we identified, as the major circulating metabolic entity, 3-O-glucuronidated aglycone (M1) obtained after glucuro-conjugation of M2. One hour after oral administration, M1 plus M2 accounted for more than 75% of the circulating total radioactivity. The pharmacological activity of these metabolites was assessed using a rat model, the muscle relaxant activity of M1 was similar to that of TCC whereas M2 was devoid of any activity. Subsequently, to investigate the PK profile of TCC in human PK studies, we developed and validated a specific bioanalytical method that combines liquid chromatography and ultraviolet detection to assay both active entities. After oral administration, TCC was not quantifiable with an lower limit of quantification set at 1 ng/mL, whereas its active metabolite M1 was detected. M1 appeared rapidly in plasma (tmax=1 h) and was eliminated with an apparent terminal half-life of 7.3 h. In contrast, after intramuscular administration both active entities (TCC and M1) were present; TCC was rapidly absorbed (tmax=0.4 h) and eliminated with an apparent terminal half-life of 1.5 h. M1 concentration peaked at 5 h and this metabolite was eliminated with an apparent terminal half-life of 8.6 h. As TCC and M1 present an equipotent pharmacological activity, the relative oral pharmacological bioavailability of TCC vs. intramuscular administration was calculated and represented 25%. Therefore, to correctly investigate the PK and bioequivalence of TCC, the biological samples obtained must be assayed with a bioanalytical method able to specifically analyse TCC and its active metabolite M1.

Published

2004

3. Study of cardiac repolarization in healthy volunteers performed with mizolastine, a new H 1 ‐receptor antagonist

Author

Henri Caplain, C. Dubruc, C L'héritier, N Lilienthal, C Deschamps, P Rosenzweig, and S Chaufour

Subjects

Adult, Male, Blood Pressure, Torsades de pointes, Placebo, QT interval, Electrocardiography, Double-Blind Method, Heart Rate, medicine, Humans, Repolarization, Pharmacology (medical), Terfenadine, Pharmacology, Cross-Over Studies, business.industry, Headache, Heart, medicine.disease, Crossover study, Astemizole, Area Under Curve, Anesthesia, Electrocardiography, Ambulatory, Histamine H1 Antagonists, Original Article, Benzimidazoles, Sleep Stages, business, Mizolastine, medicine.drug

Abstract

Aims The occurence of serious dysrhythmias, such as torsades de pointes, with terfenadine and astemizole had led to a reexamination of the potential effect of H1 antihistamines on cardiac repolarization. Mizolastine is a potent, selective, nonsedating peripherally acting H1-receptor antagonist which is registered for rhinitis and urticaria at a recommended dose of 10 mg once daily. The present study was carried out to investigate the effects of therapeutic and supratherapeutic doses of mizolastine, on ventricular repolarization in healthy volunteers. Methods Twenty-four healthy young volunteers participated in a double-blind, placebo-controlled, randomised study with three parallel groups. Each group consisted of 2 way cross-over 7 day treatment periods where mizolastine (10, 20 or 40 mg) and placebo were randomly administered. On day 1 and day 7, 12-lead ECG recordings were performed prior and 0.5, 1, 2, 3, 4, 6, 8, 12, 16, and 20 h after dosing and from day 2 to day 6, before dosing and 1, 2, 3, and 4 h after. Results Whatever the analysis used (raw data, changes from baseline, incidence of individual out-of-range values) no significant differences were observed at any dose level vs placebo, on any of ECG parameters (HR, PR, QRS, QT, and QTc). In particular, no effect of mizolastine vs placebo was shown on QT and QTc although 95% CIs were wide. The only subject who exhibited a QTc≥450 ms received placebo for 7 days. Conclusions This study found no evidence of an effect of mizolastine up to 40 mg (four times the therapeutic dose) on ventricular repolarization in healthy volunteers.

Published

1999

4. Pharmacokinetics and pharmacodynamics of zolpidem following repeated doses in hemodialyzed uraemic patients

Author

I. Etienne, Dhib M, P. Danjou, P. Rosenzweig, C. Dubruc, JP Fillastre, S Geffroy-Josse, and G. Bianchetti

Subjects

Adult, Male, Zolpidem, Pyridines, medicine.drug_class, medicine.medical_treatment, Biological Availability, Hypnotic, Pharmacokinetics, Renal Dialysis, Oral administration, medicine, Humans, Hypnotics and Sedatives, Pharmacology (medical), Chromatography, High Pressure Liquid, Aged, Uremia, Pharmacology, Sleep disorder, business.industry, musculoskeletal, neural, and ocular physiology, Middle Aged, medicine.disease, Spectrometry, Fluorescence, Repeated doses, Creatinine, Anesthesia, Sedative, Female, Hemodialysis, Arousal, Sleep, business, psychological phenomena and processes, medicine.drug

Abstract

Zolpidem, an imidazopyridine derivative, is a chemically novel, non-benzodiazepine hypnotic agent. Many uraemic patients complain of sleep disorders and ask for hypnotic medication which is well tolerated both clinically and biologically in such patients. We studied the pharmacokinetics and pharmacodynamics of zolpidem in 12 end-stage renal patients regularly treated by hemodialysis three times a week. Zolpidem (10 mg) was given orally for 14 or 21 days. Pharmacokinetic and pharmacodynamic evaluations were repeated at the end of the study on day 14 or day 21. Cmax, Tmax, t1/2 and the area under the curve were not modified in hemodialyzed patients. After daytime dosing, zolpidem induced the same level of sleepiness after the first and last dose and was well tolerated as a hypnotic agent after the night-time dosing. From these results, it can be said that zolpidem may be administered safely to patients with severe renal impairment without any modification of the dosage regimen.

Published

1993

5. The pharmacokinetic and pharmacodynamic effects of SL65.1498, a GABA-A alpha2,3 selective agonist, in comparison with lorazepam in healthy volunteers

Author

C Dubruc, Adam F. Cohen, Kari L. Franson, JB Fau, SL de Haas, Jma van Gerven, and Jaj Schmitt

Subjects

Agonist, Adult, Male, Indoles, Eye Movements, medicine.drug_class, Pharmacology, Neuropsychological Tests, Lorazepam, Partial agonist, Anxiolytic, Hypnotic, Young Adult, Cognition, Double-Blind Method, Memory, medicine, Saccades, Humans, Pharmacology (medical), Attention, Pyrroles, GABA-A Receptor Agonists, Receptor, GABA Modulators, GABA Agonists, Postural Balance, Cross-Over Studies, GABAA receptor, Receptors, GABA-A, Pursuit, Smooth, Psychiatry and Mental health, Pharmacodynamics, Female, Psychology, medicine.drug

Abstract

Abstract Benzodiazepines are effective short-term treatments for anxiety disorders, but their use is limited by undesirable side effects related to Central Nervous System impairment and tolerance development. SL65.1498 is a new compound that acts in vitro as a full agonist at the γ-aminobutyric acidA 2 and 3 receptor and as a partial agonist at the 1 and 5 receptor subtypes. It is thought that the compound could be anxiolytic by its activation at the alpha2 and alpha3 receptor subtypes, without causing unfavourable side effects, which are believed to be mediated by the alpha1 and alpha5 subtypes. This study was a double-blind, five-way cross-over study to investigate the effects of three doses of SL65.1498 in comparison with placebo and lorazepam 2 mg in healthy volunteers. The objective was to select a dose level (expected to be therapeutically active), free of any significant deleterious effect. Psychomotor and cognitive effects were measured using a validated battery of measurements, including eye movements, body sway, memory tests, reaction-time assessments, and visual analogue scales. The highest dose of SL65.1498 showed slight effects on saccadic peak velocity and smooth pursuit performance, although to a much lesser extent than lorazepam. In contrast to lorazepam, none of the SL65.1498 doses affected body sway, visual analogue scale alertness, attention, or memory tests. This study showed that the three doses of SL65.1498 were well tolerated and induced no impairments on memory, sedation, psychomotor, and cognitive functions.

Published

2008

6. Pharmacokinetic and pharmacodynamic modeling of mizolastine in healthy volunteers with an indirect response model

Author

C, Deschamps, C, Dubruc, F, Mentre, and P, Rosenzweig

Subjects

Adult, Male, Urticaria, Coefficient of variation, Administration, Oral, Pharmacology, Placebo, Models, Biological, Placebos, Pharmacokinetics, Double-Blind Method, Oral administration, Predictive Value of Tests, medicine, Humans, Pharmacology (medical), Skin Tests, Cross-Over Studies, Dose-Response Relationship, Drug, Chemistry, Antagonist, Body Fluid Compartments, Crossover study, Pharmacodynamics, Histamine H1 Antagonists, Benzimidazoles, Mizolastine, medicine.drug, Histamine

Abstract

Objective The aim of this work was to model the pharmacokinetic and pharmacodynamic relationship of mizolastine, a new H1-receptor antagonist obtained from histamine-induced wheal and flare inhibition test. Methods Fifteen healthy volunteers participated in this double-blind crossover study and randomly received single doses of 5, 10, 15, and 20 mg of mizolastine and placebo at 1 week intervals. Simultaneous histamine tests and blood samples were performed before and at 9 different times up to 24 hours after each dosing. Pharmacokinetic and pharmacodynamic modeling were performed subject by subject for the 4 doses altogether by nonlinear regression. First, plasma concentrations were fit according to a two-compartment open model with zero order absorption and first order elimination. Then an indirect response model with inhibition of the formation rate was developed to describe the pharmacodynamic relationships between flare or wheal raw areas and plasma concentrations with the use of the pharmacokinetic parameters that were previously estimated. Results Mizolastine dose dependently inhibited the histamine-induced wheal and flare formation with a submaximum effect attained after 10 mg. The mean values of the pharmacodynamic parameters of apparent zero-order rate constant for the flare or wheal spontaneous appearance (kin), the first-order rate constant for the flare or wheal disappearance, the mizolastine concentration that produced 50% suppression of the maximum attainable inhibition of kin, and the maximum attainable inhibition of the effect production were 14.1 cm2/h (coefficient of variation [CV], 32%), 0.68 h−1 (CV, 24%), 21.1 ng/mL (CV, 77%), and 0.92 (CV, 8%), respectively, for the flare and 1.9 cm2/h (CV, 64%), 0.63 h−1 (CV, 39%), 43.9 ng/mL (CV, 68%), and 0.87 (CV, 12%), respectively, for the wheal inhibition. Conclusion Pharmacokinetic and pharmacodynamic relationships of mizolastine were reliably described with the use of an indirect pharmacodynamic model; this led to an accurate prediction of the pharmacodynamic activity of mizolastine. (Clin Pharmacol Ther 2000;68:647-57.) Clinical Pharmacology & Therapeutics (2000) 68, 647–657; doi: 10.1067/mcp.2000.112341

Published

2001

7. Clinical pharmacology of befloxatone: a brief review

Author

C. Dubruc, P Rosenzweig, I Zieleniuk, A Patat, O. Curet, E Legangneux, and G. Durrieu

Subjects

Adult, Monoamine Oxidase Inhibitors, medicine.drug_class, Tyramine, Pharmacology, law.invention, Methoxyhydroxyphenylglycol, Placebos, chemistry.chemical_compound, Cognition, Pharmacokinetics, law, medicine, Humans, Drug Interactions, Oxazoles, Aged, Monoamine oxidase inhibitor, Clinical pharmacology, Dose-Response Relationship, Drug, business.industry, Brain, Electroencephalography, Middle Aged, Psychiatry and Mental health, Clinical Psychology, chemistry, Anesthesia, Sedative, Pharmacodynamics, Befloxatone, Antidepressant, business, Psychomotor Performance

Abstract

Clinical pharmacology studies of befloxatone, a new selective reversible inhibitor of monoamine oxidase-A (MAO-A), have addressed safety, with special emphasis on tyramine interactions, and have also investigated pharmacokinetics (PK) and pharmacodynamics in terms of both MAO-A inhibition (using 3,4-dihydroxyphenylglycol, DHPG, as a pharmacological activity marker) and effects on psychomotor and cognitive function, in young and elderly healthy volunteers. Clinical and laboratory safety data were satisfactory in healthy volunteers given single doses of up to 160 mg or repeated doses of up to 80 mg/day for 7 days. Tyramine interaction studies showed that the expected potentiation of the tyramine pressor effect occurred with a safety margin that was so wide as to make dietary restrictions unnecessary with dosages of up to 20 mg once daily in clinical settings. Absorption was rapid ( t max =2 h), terminal halflife was about 11 h, and PK parameters increased linearly with the dose. Befloxatone induced a dose-dependent decrease in plasma DHPG levels from 2.5 mg upwards, and a 10-mg dose provided sub-maximal activity (80% DHPG decrease) of 24 h duration. No sedative or stimulant effects were detected using several batteries of psychometric tests. Befloxatone was devoid of deleterious effects on memory in young volunteers, and exhibited the EEG profile of a non-sedative antidepressant. In summary, available clinical pharmacology studies confirm that befloxatone is a safe and potent RIMA with no potential for inducing deleterious CNS effects.

Published

1999

8. Population pharmacokinetic analysis of mizolastine and validation from sparse data on patients using the nonparametric maximum likelihood method

Author

F, Mesnil, F, Mentré, C, Dubruc, J P, Thénot, and A, Mallet

Subjects

Likelihood Functions, Models, Statistical, Histamine H1 Antagonists, Humans, Reproducibility of Results, Benzimidazoles, Randomized Controlled Trials as Topic

Abstract

A population analysis of the kinetics of mizolastine was performed from concentrations on 449 allergic patients, using the nonparametric maximum likelihood method (NPML). A two-compartment open model with zero-order absorption was used to describe the kinetics of mizolastine after oral administration. A heteroscedastic variance model was assumed for the error. To explain the kinetic variability, eight covariates were introduced in the analysis: gender, pharmaceutical dosage form, age, body weight, serum creatinine concentration, creatinine renal clearance, plasma levels of hepatic transaminases ASAT and ALAT. Their relationships to the kinetic parameters were studied by means of the estimated distribution of each kinetic parameter conditional on different levels of each covariate. An important interindividual kinetic variability was found for all parameters. Moreover, several kinetic parameters among which the duration of absorption were found to be influenced by pharmaceutical dosage form and gender. Body weight and creatinine renal clearance were found to have a little influence on the oral clearance and the smallest disposition rate constant. This population analysis was validated on a separate group of 247 other patients. For each observed concentration of this sample, a predictive distribution was computed using the individual covariates. Predicted concentrations and standardized prediction errors were deduced. The mean and variance of the standardized prediction errors were, respectively, 0.21 and 2.79. Moreover, in the validation sample, the predicted cumulative distribution function of each observed concentration was computed. Empirical distribution of these values was not significantly different from a uniform distribution, as expected under the assumption that the population model estimated by NPML is adequate.

Published

1998

9. Lack of effect of mizolastine on the safety and pharmacokinetics of digoxin administered orally in repeated doses to healthy volunteers

Author

S, Chaufour, F, Le Coz, T, Denolle, C, Dubruc, I, Cimarosti, C, Deschamps, N, Ulliac, B, Delhotal-Landes, and P, Rosenzweig

Subjects

Adult, Male, Digoxin, Electrocardiography, Cross-Over Studies, Double-Blind Method, Area Under Curve, Histamine H1 Antagonists, Humans, Benzimidazoles, Blood Pressure, Drug Interactions, Anti-Arrhythmia Agents

Abstract

The effects of mizolatine, a new H1 receptor antagonist, on safety and pharmacokinetics of digoxin were studied in a double-blind placebo-controlled crossover study. After administration of digoxine alone (0.25 mg o.d. for 7 days), 12 healthy young male volunteers (23+/-2 years) received either placebo and digoxin (0.25 mg o.d.) or mizolastine (10 mg o.d.) and digoxin (0.25 mg o.d.) during 7 days. The assessment criteria consisted in hemodynamic and ECG parameters recordings and the pharmacokinetics of digoxin during the last day of coadministration (day 14). No difference between the 2 treatment groups was evidenced on ECG, hemodynamic, and clinical and laboratory safety parameters. No change in AUC and tmax was recorded. No clinically relevant effect of mizolastine on the digoxin pharmacokinetics was found. However, a statistically significant increase in digoxin Cmax (3.03+/-0.18 nmolxl(-1) vs 2.52+/-0.19 nmolxl(-1), p0.05) and Cmin (0.99+/-0.08 nmolxl(-1) vs 0.87+/-0.07 nmolxl(-1), p=0.05) occurred after the coadministration vs digoxin alone. It can be concluded that mizolastine and digoxin at therapeutic dosages can be safely coadministered.

Published

1998

10. Pharmacokinetic analysis of mizolastine in healthy young volunteers after single oral and intravenous doses: noncompartmental approach and compartmental modeling

Author

F, Mesnil, C, Dubruc, F, Mentre, S, Huet, A, Mallet, and J P, Thenot

Subjects

Adult, Adolescent, Injections, Intravenous, Histamine H1 Antagonists, Administration, Oral, Humans, Benzimidazoles, Body Fluid Compartments, Mathematical Computing, Models, Biological

Abstract

This paper presents the analysis of the kinetics of a new antihistamine, mizolastine, in 18 healthy volunteers, from concentrations measured after an intravenous infusion and two different oral administrations: tablet and capsule. Two approaches were used to analyze these data: (i) a noncompartmental approach implemented in PHARM-NCA; (ii) a compartmental modeling approach implemented in a new S-PLUS library, NLS2, which allows the estimation of variance parameters simultaneously with the kinetic parameters. For the compartmental modeling approach, two-compartment open models were used. According to the Akaike criterion, the best model describing the kinetics of mizolastine after oral administration was the zero-order absorption model. The kinetic parameters obtained with PHARM-NCA and NLS2 were similar. The estimated duration of absorption was greater for the tablets than for the capsules (with means equal to 1.13 hr and 0.84 hr respectively). After an intravenous infusion, the mean estimated clearance was 4.9 L/hr, the mean lambda 2-phase apparent volume of distribution was 89.6 L and the mean terminal half-life was 12.9 hr.

Published

1997

11. The psychomotor and cognitive effects of litoxetine in young and middle aged volunteers

Author

P. Rosenzweig, Alain Patat, C. Dubruc, C. Dunmore, D. B. Fairweather, Ian Hindmarch, and V.H. Curson

Subjects

Adult, Male, medicine.medical_specialty, medicine.drug_class, Sedation, Poison control, Administration, Oral, Flicker fusion threshold, Audiology, Choice Behavior, Flicker Fusion, Cognition, Double-Blind Method, Piperidines, Rating scale, Memory, medicine, Humans, Pharmacology (medical), Computer Simulation, Chromatography, High Pressure Liquid, Pharmacology, Analysis of Variance, Cross-Over Studies, business.industry, Middle Aged, Crossover study, Surgery, Tolerability, Sedative, Female, medicine.symptom, business, Sleep, Psychomotor Performance, Selective Serotonin Reuptake Inhibitors, Stroop effect, Research Article

Abstract

1. The effects of a range of doses of litoxetine (twice daily for 4 days), a novel specific serotonin re-uptake inhibitor, were evaluated in young and middle aged volunteers. 2. Psychometric testing was carried out at various time points on days 1 and 4 of each treatment period. The test battery consisted of critical flicker fusion (CFF), choice reaction time (CRT), compensatory tracking (CTT), Stroop and Sternberg memory scanning tests. Subjective feelings of sleep and sedation were measured by the Leeds Sleep Evaluation Questionnaire (LSEQ) and line analogue rating scales (LARS). 3. Pharmacokinetic profiles were determined from analyses of blood samples taken after the final dose on day 5. 4. Overall, there were few changes in any of the psychometric tests and although the higher doses of litoxetine improved CFF, these effects were weak in that differences could only be detected when the results were pooled against time. 5. The pharmacokinetic profile of litoxetine was very similar in both the young and middle aged subjects, and there was no difference regarding tolerability. 6. There is little evidence from this study to suggest that litoxetine has any intrinsic sedative activity which is likely to interfere with the performance of activities of everyday life.

Published

1995

12. Pharmacokinetics and bioavailability of a sustained-release diltiazem formulation (Mono-Tildiem LP 300 mg) after repeated administration in healthy volunteers

Author

P. Rosenzweig, G. Bianchetti, C. Dubruc, G. Houin, and V. Sultana

Subjects

Adult, Male, Volunteers, Time Factors, Administration, Oral, Biological Availability, Pharmacology, Bioequivalence, Dosage form, Diltiazem, Drug Delivery Systems, Pharmacokinetics, Oral administration, Healthy volunteers, medicine, Humans, heterocyclic compounds, Pharmacology (medical), Absolute bioavailability, business.industry, General Medicine, musculoskeletal system, Bioavailability, Injections, Intravenous, cardiovascular system, business, circulatory and respiratory physiology, medicine.drug

Abstract

The usual dosage regimen of diltiazem (Tildiem) is 60 mg 3-4 times a day. A sustained-release formulation has been developed (Mono-Tildiem LP 300 mg) in order to allow a single daily administration. Two repeated dosing studies were performed in healthy volunteers. The absolute bioavailability of sustained-release diltiazem LP 300 mg was investigated using concomitant i.v. administration of 13C-labelled drug: absolute bioavailability of the "once a day" formulation was 35%. The second study compared sustained-release diltiazem LP 300 mg with the standard formulation of diltiazem. The results showed that the diltiazem plasma concentrations obtained after the LP formulation remained stable between 2 and 14 h after administration and were compatible with a once a day administration. Relative bioavailability of sustained-release diltiazem LP 300 mg was 79.3% compared with diltiazem. Therefore, a unitary dose of sustained-release diltiazem LP 300 mg was chosen as the dose equivalent to the daily dose administered with the standard diltiazem formulation.

Published

1995

13. Pharmacokinetic and bioavailability of diltiazem sustained-release: influence of food and time of administration

Author

JP Thénot, C. Dubruc, G. Bianchetti, G. Houin, and H. Bagheri

Subjects

Adult, Male, Time Factors, Cmax, Administration, Oral, Biological Availability, Pharmacology, Drug Administration Schedule, law.invention, Angina, Diltiazem, Eating, Randomized controlled trial, Pharmacokinetics, Oral administration, law, medicine, Humans, Pharmacology (medical), Cross-Over Studies, business.industry, medicine.disease, Crossover study, Bioavailability, Anesthesia, Delayed-Action Preparations, business, medicine.drug

Abstract

Diltiazem is a calcium channel blocking agent known to be effective in the treatment of angina pectoris, hypertension and supraventricular arrhythmias. To improve the conditions of diltiazem administration in the treatment of hypertensive patients, a sustained-release formulation (Mono-Tildiem LP 300 mg) allowing a single daily oral administration has been developed. The aim of the present study was to first evaluate the influence of food intake and second to evaluate those of the time of administration on the pharmacokinetic parameters and the bioavailability of this sustained-release formulation. The influence of these factors was investigated over two different open, randomized, cross-over studies in 12 healthy volunteers. Although a significant decrease in Tmax and an increase in Cmax occurred when diltiazem sustained-release was administered with food intake, AUC0-48, and therefore the fraction absorbed, were not modified either by concurrent food intake or by different times of administration. The minor modifications of pharmacokinetic parameters of diltiazem sustained release observed were unlikely to induce any clinical consequence.

Published

1995

14. EEG profile of intravenous zolpidem in healthy volunteers

Author

C. Dubruc, Thebault Jj, G Bianchetti, P Rosenzweig, A Patat, S. Trocherie, L A Court, and Paolo L. Morselli

Subjects

Adult, Male, Zolpidem, medicine.drug_class, Pyridines, Cmax, Administration, Oral, Pharmacology, Hypnotic, Route of administration, Pharmacokinetics, Double-Blind Method, Oral administration, medicine, Humans, Hypnotics and Sedatives, Volume of distribution, Cross-Over Studies, business.industry, Electroencephalography, Alpha Rhythm, Delta Rhythm, Anesthesia, Sedative, Injections, Intravenous, Sleep Stages, business, Beta Rhythm, medicine.drug

Abstract

Zolpidem is an imidazopyridine which binds specifically to the omega 1 receptor. Zolpidem demonstrated potent hypnotic activity at a dose of 10 mg. Pharmacodynamics and pharmacokinetics of zolpidem were studied after daytime administration in a randomised, double-blind, placebo-controlled, cross-over trial. Single doses of zolpidem (10 mg IV as a 3-min infusion and 20 mg orally) and placebo were firstly tested in 12 healthy young male volunteers. Two other doses (5 mg IV and orally) were then evaluated in 6 out of these 12 subjects. EEG (4 leads = Fp2-T4, Fp1-T3, T4-02 and T3-01), and Stanford Sleepiness Scale (SSS) were measured up to 5 h postdosing. Blood samples were also collected up to 24 h. The time course of the hypnotic activity of zolpidem, assessed by the score obtained on SSS, showed a similar profile whatever the route or the dose administered: slightly earlier onset after IV but sedative scores were reached at 30 min and the effect peaked between 1 and 1.5 h and lasted 4 h in both conditions. The EEG profile of zolpidem was characterised by a decrease of alpha activity and an increase in delta and in beta activity. The effect on beta activity was marked within the first hour and then disappeared. The time course of delta and alpha activities indicated a rapid onset (10 min after IV, 30 min after oral route) and a duration of 3-4 h. The amplitude of these relative EEG changes and their duration were independent of the route of administration and the dose administered. AUC and Cmax increased proportionally to the administered dose and elimination half life (2h), clearance and volume of distribution did not change according to the dose or the route of administration.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1994

15. EEG profile of litoxetine after single and repeated administration in healthy volunteers

Author

Paolo L. Morselli, Thebault Jj, S Trocherie, L A Court, Alain Patat, C. Dubruc, G Bianchetti, and P. Rosenzweig

Subjects

Adult, Male, Dose, Serotonin reuptake inhibitor, Cmax, Administration, Oral, Pharmacology, Litoxetine, Pharmacokinetics, Double-Blind Method, Piperidines, Oral administration, Medicine, Humans, Pharmacology (medical), Analysis of Variance, Dose-Response Relationship, Drug, business.industry, Brain, Electroencephalography, Dose–response relationship, Pharmacodynamics, business, Selective Serotonin Reuptake Inhibitors, Research Article

Abstract

1. Litoxetine is a selective serotonin reuptake inhibitor with antidepressant activity in animal models and in depressed patients. 2. This double-blind, cross-over, placebo-controlled study was carried out in 12 healthy young male volunteers. The aim was to assess the EEG profile of litoxetine in parallel with its pharmacokinetics after a single dose or multiple administrations for 4 days (6 doses) of two dosages (10 mg and 25 mg). Spectral analysis of four EEG leads (F4-T4, F3-T3, T4-02 and T3-01) was done up to 12 h post-dose. 3. In single or multiple doses, litoxetine induced EEG changes characterised by a dose-related increase in fast beta energies, mainly beta 2, without any changes in slow waves (delta and theta). A slight reduction in alpha activity occurred only after repeated doses. 4. EEG changes occurred after a single oral administration and lasted at least 12 h with litoxetine blood concentrations ranging from 4 to 10 ng ml-1. With repeated administrations, the pharmacodynamic steady-state was achieved as the increase in beta 2 energies was the same before and 12 h post-dose. These effects occurred with litoxetine blood concentrations ranging from 3 to 7 ng ml-1 with the 10 mg dosage and from 8 to 18 ng ml-1 with the 25 mg dosage. The EEG profile did not change after 4 days of repeated administration, indicating that tolerance did not develop. 5. Cmax and AUC showed proportionality between the administered dosages of 10 and 25 mg.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1994

16. Effects of mizolastine, a new antihistamine, on psychomotor performance and memory in elderly subjects

Author

Gram Lf, Cabanis Mj, Rosenzweig P, Brohier S, C. Dubruc, and Alain Patat

Subjects

Psychomotor learning, Aging, Dose, business.industry, medicine.medical_treatment, Poison control, Flicker fusion threshold, Placebo, Psychiatry and Mental health, Memory, Clemastine, Anesthesia, medicine, Reaction Time, Humans, Pharmacology (medical), Antihistamine, Benzimidazoles, Female, business, Psychomotor Performance, Mizolastine, medicine.drug, Aged

Abstract

The effects of a single 10 mg dose of the new H1 antihistamine mizolastine on psychomotor performance and memory in the elderly were assessed in a double-blind, cross-over, placebo-controlled study in 15 elderly female volunteers aged 66-77 years, using clemastine 2 mg as a positive control. Objective (critical flicker fusion, choice reaction time, digit symbol substitution, immediate and delayed free recall) and subjective (linear analogue rating scales) assessments were done on each test day before the dose, then 4 and 8 h post-dose. Plasma samples were also collected. A single oral dose of mizolastine within the range of recommended daily therapeutic dosages (10 mg) failed to induce subjective drowsiness and produced no detrimental effects on psychomotor performance or on short-term and long-term memory in the elderly subjects. In contrast, 2 mg clemastine induced significant impairments (decrease in critical flicker fusion, increase in recognition reaction time) in comparison with placebo and mizolastine, although it did not impair memory. The pharmacokinetic profile of mizolastine in the elderly study subjects was similar to that observed in healthy young volunteers. Therefore, it can be concluded that mizolastine 10 mg could be used safely in elderly out-patients as it preserves functions involved in activities of daily living. Language: en

Published

1994

17. Pharmacodynamics and pharmacokinetics of mizolastine (SL 85.0324), a new nonsedative H1 antihistamine

Author

P, Rosenzweig, J J, Thebault, H, Caplain, C, Dubruc, G, Bianchetti, E, Fuseau, and P L, Morselli

Subjects

Adult, Male, Double-Blind Method, Psychometrics, Histamine H1 Antagonists, Humans, Benzimidazoles, Sleep Stages

Abstract

The antihistaminic activity, clinical safety, and pharmacokinetics of mizolastine (SL 85.0324) were studied in a 5-way, double-blind crossover study of ten healthy volunteers with doses of 1 to 75 mg. Inhibition of the histamine-induced wheal and flare showed clear dose-dependent antihistaminic activity beginning from the 2-mg dose with a maximum attained between 10 and 20 mg. The onset of action was rapid (one hour) and the effect persisted for more than 24 hours after a 10-mg dose or more. Mizolastine was well tolerated at doses up to 75 mg; subjective and objective signs of transient sedative activity were not observed at doses below 30 mg. The pharmacokinetic profile (rapid absorption with Tmax congruent to 1 h and elimination T1/2 of about eight hours) parallels the pharmacodynamic activity. Within the considered dose range, the pharmacokinetics was linear with no saturation phenomena.

Published

1992

18. Pharmacokinetic profile of a new modified-release formulation of zolpidem designed to improve sleep maintenance

Author

E. Weinling, E. Krupka, G. Bianchetti, C. Dubruc, S. McDougall, and F. Andreé

Subjects

Pharmacology, Zolpidem, Chemistry, musculoskeletal, neural, and ocular physiology, Significant difference, Cmax, Crossover study, Bioavailability, Pharmacokinetics, Anesthesia, Plasma concentration, medicine, Pharmacology (medical), Sleep maintenance, psychological phenomena and processes, medicine.drug

Abstract

Aims/Background To evaluate relative bioavailability and plasma pharmacokinetic (PK) profile of single oral doses of zolpidem modified-release (MR) formulations (10 mg and 12.5 mg) compared to standard zolpidem 10 mg. Methods 24 healthy, Caucasian, male volunteers (18–45 years old) received single oral doses of zolpidem MR 10 mg and 12.5 mg, or standard zolpidem 10 mg via a randomized, open-label, crossover study. Blood sample (n=18) were collected up to 16h postdose. PK parameters were determined by noncompartmental analysis: Cmax, tmax, t1/2z, AUC, MRT, and half-value duration (HVD). Comparisons between treatments were performed by ANOVA (α=0.05). Results The initial absorption phase of zolpidem MR formulations was as fast as that of standard zolpidem with no significant difference in tmax. With zolpidem MR 12.5 mg, Cmax values were moderately lower (ratio of 0.82) compared with standard zolpidem and plasma concentrations were maintained above those observed with standard zolpidem for a longer period of time, and particularly from 3 to 6h postdose. This was confirmed by an increase of the HVD from 2.3h for standard zolpidem to 4.6h for zolpidem MR 12.5 mg. The mean terminal half-life was similar with all 3 formulations. Conclusion These results show that this new zolpidem MR formulation provides the appropriate PK characteristics to extend plasma concentration into the middle of the night (3–6 h postdose), while retaining the same tmax and terminal half-life. Clinical Pharmacology & Therapeutics (2005) 77, P44–P44; doi: 10.1016/j.clpt.2004.12.062

Published

2005

19. Amisulpride: kinetics in patients with renal failure

Author

M. Canal, C. Dubruc, M. MacMahon, and J. Kwan

Subjects

Pharmacology, medicine.medical_specialty, business.industry, Kinetics, Urology, Psychiatry and Mental health, Neurology, Medicine, Pharmacology (medical), In patient, Neurology (clinical), Amisulpride, business, Biological Psychiatry, medicine.drug

Published

2000

20. Pharmacokinetics and safety of cicloprolol in uraemic patients [letter]

Author

P. Rosenzweig, J. P. Fillastre, M. Aparicio, C. Dubruc, C. Porquet, and P. L. Morselli

Subjects

Pharmacology, business.industry, medicine.disease, Uremia, Propanolamines, chemistry.chemical_compound, chemistry, Pharmacokinetics, Cicloprolol, Adrenergic beta-Agonists, medicine, Pharmacology (medical), business

Published

1991

21. PK-PD relationship of the effects of argatroban on haemostasis in healthy young volunteers

Author

C. Thuillez, D. Garrigou, J.P. Thenot, C. Dubruc, and L. Bergougnan

Subjects

Pharmacology, business.industry, Medicine, Pharmacology (medical), business, PK/PD models, Argatroban, medicine.drug

Published

1999

22. Clinical pharmacology profile of befloxatone

Author

C. Dubruc, O. Curet, G. Durrieu, P. Rosenzweig, and J.L. Pinquier

Subjects

Pharmacology, Clinical pharmacology, business.industry, law.invention, Psychiatry and Mental health, chemistry.chemical_compound, Neurology, chemistry, law, Befloxatone, Medicine, Pharmacology (medical), Neurology (clinical), business, Biological Psychiatry

Published

1996

23. Regional Cerebral Blood Flow during Bicuculline-Induced Seizures in the Newborn Piglet: Effect of Phenobarbital

Author

Monin P, C. Dubruc, Daval Jl, Paul Vert, P. L. Morselli, and Martine Clozel

Subjects

medicine.medical_specialty, Time Factors, Swine, Radioactive microsphere technique, medicine.medical_treatment, Hemodynamics, Blood Pressure, Bicuculline, Cerebral autoregulation, Potassium Chloride, Seizures, Internal medicine, medicine, Animals, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, Acidosis, Acid-Base Equilibrium, business.industry, Microspheres, Endocrinology, Anticonvulsant, Animals, Newborn, Cerebral blood flow, Cerebrovascular Circulation, Phenobarbital, Anesthesia, Blood Gas Analysis, medicine.symptom, business, circulatory and respiratory physiology, medicine.drug

Abstract

The changes in cerebral blood flow (CBF) during and after bicuculline-induced seizures were studied by the radioactive microsphere technique in 12 newborn, urethan-anesthetized piglets, 6 piglets pretreated with phenobarbital (10 mg/kg) and 6 without phenobarbital. The mean arterial blood pressure (MABP), PaO2, PaCO2 and the cerebral tissue pH (CtpH) were measured. CBF was increased during seizure, more in basal ganglia (98 and 106% in the control and phenobarbital group, respectively) than in brainstem, cerebellum and cortex. 15 min after seizure, CBF has returned to preseizure values. There was no significant difference at any time between the control and phenobarbital group. The increase in CBF was correlated with an increase in MABP (r = 0.753, p less than 0.01), suggesting a loss of cerebral autoregulation. CBF was significantly correlated with PaCO2 before and after seizure, but not during seizure. Finally, the increase in CBF was significantly correlated with an early increase in CtpH (r = 0.570, p less than 0.05), suggesting that brain acidosis is not involved in the pathogenesis of the increased CBF during seizures.

Published

1985

24. Determination of S-carboxymethyl-L-cysteine in plasma by high-performance liquid chromatography with column switching following precolumn derivatization

Author

A. Haddouche, J. P. Thenot, C. Dubruc, M.M. Badarani, and Ph. Hermann

Subjects

S-carboxymethyl-L-cysteine, Chromatography, Chemistry, Carbocysteine, General Chemistry, Reversed-phase chromatography, Plasma, High-performance liquid chromatography, Kinetics, Drug Stability, Chromatography detector, Carbocisteine, medicine, Humans, Indicators and Reagents, Cysteine, Chromatography column, Chromatography, High Pressure Liquid, o-Phthalaldehyde, medicine.drug, Precolumn derivatization

Published

1987

25. An improved method for the determination of S-Carboxymethyl-L-cysteine in biological fluids with precolumn derivatization and on-line clean-up

Author

A. Haddouche, C. Dubruc, G. Bianchetti, C. Colafranceschi, and P. Guinebault

Subjects

S-carboxymethyl-L-cysteine, Chromatography, Organic Chemistry, Clinical Biochemistry, Improved method, Biochemistry, High-performance liquid chromatography, Analytical Chemistry, Clean-up, chemistry.chemical_compound, Pharmacokinetics, chemistry, Biological fluids, Derivatization, Precolumn derivatization

Abstract

In order to follow levels of S-Carboxymethyl-L-cysteine in biological fluids for a period as long as three half-lives after drug administration during pharmacokinetic studies, an improved method for its determination had to be developed. Like the previous one, this method uses a protein precipitation step followed by an O-Phthalaldehyde derivatization step and then an HPLC on-line clean-up. This latter was obtained by means of a switching valve system, including a Nucleosil CN 5 μm (3 cm × 4.6 mm i.d.) precolumn and a Spherisorb ODS 5 μm (15 cm×4.6 mm i.d.) analytical column. The sensitivity limit was improved to 0.1 μg/ml in plasma samples and 0.2 μg/ml in urine samples.

Published

1988

26. Pharmacokinetics of lndomethacin in the Premature Infant

Author

C. Dubruc, G. Bianchetti, Marchal F, Paul Vert, P. L. Morselli, Monin P, and Marie-Jeanne Boutroy

Subjects

Drug, Plasma clearance, business.industry, media_common.quotation_subject, Therapeutic effect, Pharmacology, Rectal route, medicine.anatomical_structure, Pharmacokinetics, Ductus arteriosus, Plasma concentration, Medicine, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, business, Compartment (pharmacokinetics), media_common

Abstract

Indomethacin (I) pharmacokinetics was evaluated in 6 premature infants who received the drug for treatment of patent ductus arteriosus. Administered by oral or rectal route, I (0.2 mg/kg/24 h X 3) was promptly absorbed with peak plasma concentrations attained within 1 and 3 h. The elimination of I appeared to follow two compartment open model kinetics, with terminal plasma half-lives ranging from 30 to 90 h. Apparent plasma clearance values were between 0.076 and 0.335 ml/min/kg. Ductal closure was observed in 4 of the 6 infants. Data point to a possible relationship between therapeutic effects and I plasma concentrations.

Published

1980

27. Treatment of persistent fetal circulation syndrome of the newborn. Comparison of different doses of tolazoline

Author

P. L. Morselli, Paul Vert, P. Monin, and C. Dubruc

Subjects

medicine.medical_treatment, Blood Pressure, Persistent Fetal Circulation Syndrome, Persistent fetal circulation, Drug Administration Schedule, Bolus (medicine), Pharmacokinetics, medicine, Humans, Pharmacology (medical), Tolazoline, Pharmacology, Chemotherapy, business.industry, Pulmonary Gas Exchange, Infant, Newborn, Half-life, General Medicine, Plasma levels, Carbon Dioxide, medicine.disease, Oxygen, Kinetics, Anesthesia, business, medicine.drug, Half-Life

Abstract

The effects of two doses of tolazoline have been compared in 2 groups of newborns suffering from the persistent fetal circulation syndrome. The effects on PaO2 and AaDO2 were similar in the 2 groups who received either a bolus of 1 or 0.5 mg X kg-1 tolazoline, followed by a continuous infusion of 1 or 0.5 mg X kg-1 X h-1. The observed changes did not differ significantly from those previously observed in babies treated with 2 mg X kg-1. A rise in PaO2 and a reduction in AaDO2 were usually observed shortly after the bolus injection and at plasma levels between 1.5 and 4 micrograms X ml X -1. A progressive rise in plasma level over time occurred after 1 mg X kg-1 (and in the previous study of 2 mg) but not with 0.5 g/kg tolazoline. The elimination half-life of tolazoline in 6 patients was 5 to 13 h. The data suggest that continuous infusion of tolazoline is not necessarily required and that the dose of 0.5 mg/kg is more appropriate and safer than the higher doses usually proposed.

Published

1987

28. Clonazepam pharmacokinetics and therapeutic efficacy in neonatal seizures

Author

C. Dubruc, M. J. Boutroy, Paul Vert, L. Sola, J P Thénot, M. André, P. L. Morselli, and G. Bianchetti

Subjects

Adult, Male, medicine.medical_treatment, Clonazepam, Pharmacokinetics, Seizures, Convulsion, medicine, Humans, Pharmacology (medical), Adverse effect, Infusions, Intravenous, Pharmacology, business.industry, Therapeutic effect, Infant, Newborn, Gestational age, General Medicine, Kinetics, Anticonvulsant, Anesthesia, Phenobarbital, Female, medicine.symptom, business, medicine.drug, Half-Life

Abstract

Eighteen newborns (gestational age 28 to 42 weeks and post-natal age 0.5 to 44 days) suffering from convulsions not controlled by phenobarbital were treated with clonazepam 0.1 mg/kg (8 cases) or 0.2 mg/kg (10 cases) administered by slow intravenous infusion. The plasma half-lives in these ‘phenobarbital pretreated neonates’ were of the same order of magnitude as those reported in adults (20–43 h). Post-natal age did affect clearance, which was 50–70% less than in adults and older children. At the end of the infusion period, plasma clonazepam ranged from 28 to 117 ng/ml in the 0.1 mg/kg group and from 99 to 380 ng/ml in the 0.2 mg/kg group. In the former an immediate therapeutic response was observed in 7 out of 8 cases, and in the latter a significant and somehow delayed effect on convulsion was present only in 6 cases. The data suggest that optimal therapeutic response might already have been achieved with the 0.1 mg/kg dose. Higher doses and toxic concentrations of clonazepam may be detrimental to complete control of seizures and may expose the newborn to an unnecessary risk of adverse events.

Published

1986

29. High-performance liquid chromatographic determination of zolpidem, a new sleep inducer, in biological fluids with fluorimetric detection

Author

P. Guinebault, P. Hermann, C. Dubruc, and J.P. Thénot

Subjects

Quality Control, Zolpidem, Chromatography, medicine.drug_class, Chemistry, Pyridines, Fluorescence spectrometry, General Chemistry, Hydrogen-Ion Concentration, High-performance liquid chromatography, Sleep in non-human animals, Biological fluid, Hypnotic, Spectrometry, Fluorescence, Biological fluids, medicine, Solvents, Humans, Hypnotics and Sedatives, Inducer, Indicators and Reagents, medicine.drug

Published

1986

30. Pharmacokinetics of indomethacin in the premature infant

Author

G, Bianchetti, P, Monin, F, Marchal, C, Dubruc, M J, Boutroy, P L, Morselli, and P, Vert

Subjects

Male, Kinetics, Creatinine, Indomethacin, Infant, Newborn, Prostaglandins, Humans, Female, Ductus Arteriosus, Patent, Infant, Premature, Half-Life

Abstract

Indomethacin (I) pharmacokinetics was evaluated in 6 premature infants who received the drug for treatment of patent ductus arteriosus. Administered by oral or rectal route, I (0.2 mg/kg/24 h X 3) was promptly absorbed with peak plasma concentrations attained within 1 and 3 h. The elimination of I appeared to follow two compartment open model kinetics, with terminal plasma half-lives ranging from 30 to 90 h. Apparent plasma clearance values were between 0.076 and 0.335 ml/min/kg. Ductal closure was observed in 4 of the 6 infants. Data point to a possible relationship between therapeutic effects and I plasma concentrations.

Published

1980

31. Determination of vincamine in human plasma using automated high-performance liquid chromatography

Author

C. Dubruc, G. Bianchetti, and H. Caqueret

Subjects

Chromatography, Coefficient of variation, Organic Chemistry, Vincamine, General Medicine, Phosphate, Biochemistry, High-performance liquid chromatography, Analytical Chemistry, Solvent, chemistry.chemical_compound, chemistry, Potassium phosphate, Human plasma, Phase (matter), medicine, Humans, Vinca Alkaloids, Chromatography, High Pressure Liquid, medicine.drug

Abstract

A specific and sensitive high-performance liquid chromatographic method for the quantitative determination of vincamine at therapeutic concentrations in plasma is described. The column was packed with Spherisorb ODS 5 μm, and the mobile phase was acetonitrile—potassium phosphate (0.02 M , pH 2.3) (50:50) with a flow-rate of 10 ml/min. Detection was at 230 nm. Using automated large-volume injection of a non-eluting solvent (0.02 M potassium phosphate) the method was capable of the analysis of a large number of samples daily. The coefficient of variation of the procedure was 4.8% at a plasma vincamine concentration of 10 ng/ml.

Published

1981

32. To nurse when receiving acebutolol: is it dangerous for the neonate?

Author

P. L. Morselli, C. Dubruc, Paul Vert, M. J. Boutroy, and G. Bianchetti

Subjects

Drug, medicine.medical_specialty, media_common.quotation_subject, Physiology, Renal function, Breast milk, Acebutolol, Pharmacokinetics, Pregnancy, Internal medicine, medicine, Humans, Pharmacology (medical), Prospective Studies, Active metabolite, media_common, Pharmacology, Milk, Human, business.industry, Postpartum Period, Infant, Newborn, General Medicine, Endocrinology, Breast Feeding, Diacetolol, Hypertension, Female, business, Breast feeding, medicine.drug

Abstract

The concentrations of acebutolol and of its main active metabolite diacetolol in milk and plasma were studied in 7 hypertensive mothers treated with acebutolol, a cardioselective beta-adrenoceptor blocking agent. Clinical monitoring on their newborn babies was also done, as well as measurement of plasma level of the drug in them. The ratio between milk and plasma concentrations ranged from 1.9 to 9.2 for acebutolol and from 2.3 to 24.7 for diacetolol, and in any given milk sample, the diacetolol concentration was always higher than that of acebutolol. In a newborn infant, plasma concentrations of the two transplacentally acquired substances was raised when breast feeding started and remained high. Clinical signs of pharmacological beta-blockade were observed. Evaluation of the iatrogenic risk shows that pharmacologically active amounts of acebutolol might be received by a neonate if the daily maternal dosage exceeds 400 mg/day and/or renal function in the mother is impaired.

Published

1986

33. Effect of seizures on brain phenobarbital concentration in newborn piglets

Author

P. L. Morselli, M Clozel, Paul Vert, C. Dubruc, and P. Monin

Subjects

medicine.medical_specialty, Swine, medicine.medical_treatment, Seizures, Internal medicine, Convulsion, PH partition, Medicine, Animals, Pentylenetetrazol, Acidosis, business.industry, Brain, Bicuculline, Carbon Dioxide, Hydrogen-Ion Concentration, Oxygen, Blood pressure, Endocrinology, Anticonvulsant, Neurology, Animals, Newborn, Anesthesia, Phenobarbital, Neurology (clinical), medicine.symptom, business, medicine.drug

Abstract

Phenobarbital (PB) brain and blood concentrations were measured together with brain and blood pH in newborn piglets before and at the end of seizure activity induced by pentylenetetrazol or bicuculline. Seizures induced a significant elevation of arterial blood pressure and profound changes in the blood gases and in the acid-base balance, with a marked reduction in brain tissue pH. Despite an intense brain acidosis, however, and a significant rise in blood/brain [H+] gradient, phenobarbital brain concentrations were not reduced during seizures but, on the contrary, were increased in 7 of 11 piglets. These data suggest that contrary to the pH partition hypothesis, brain uptake of PB is concomitantly increased during seizures and brain acidosis.

Published

1987

34. A mechanism-based model for the population pharmacokinetics of free and bound aflibercept in healthy subjects.

Author

Thai HT, Veyrat-Follet C, Vivier N, Dubruc C, Sanderink G, Mentré F, and Comets E

Subjects

Clinical Trials as Topic, Humans, Male, Models, Biological, Protein Binding, Receptors, Vascular Endothelial Growth Factor, Vascular Endothelial Growth Factor A metabolism, Recombinant Fusion Proteins pharmacokinetics

Abstract

Aim: Aflibercept (VEGF-Trap), a novel anti-angiogenic agent that binds to VEGF, has been investigated for the treatment of cancer. The aim of this study was to develop a mechanism-based pharmacokinetic (PK) model for aflibercept to characterize its binding to VEGF and its PK properties in healthy subjects., Methods: Data from two phase I clinical studies with aflibercept administered as a single intravenous infusion were included in the analysis. Free and bound aflibercept concentration-time data were analysed using a nonlinear mixed-effects modelling approach with MONOLIX 3.1., Results: The best structural model involved two compartments for free aflibercept and one for bound aflibercept, with a Michaelis-Menten type binding of free aflibercept to VEGF from the peripheral compartment. The typical estimated clearances for free and bound aflibercept were 0.88 l day(-1) and 0.14 l day(-1), respectively. The central volume of distribution of free aflibercept was 4.94 l. The maximum binding capacity was 0.99 mg day(-1) and the concentration of aflibercept corresponding to half of maximum binding capacity was 2.91 µg ml(-1). Interindividual variability of model parameters was moderate, ranging from 13.6% (V(max) ) to 49.8% (Q)., Conclusion: The present PK model for aflibercept adequately characterizes the underlying mechanism of disposition of aflibercept and its nonlinear binding to VEGF., (© 2011 sanofi-aventis RSD. British Journal of Clinical Pharmacology © 2011 The British Pharmacological Society.)

Published

2011

35. The pharmacokinetic and pharmacodynamic effects of SL65.1498, a GABA-A alpha2,3 selective agonist, in comparison with lorazepam in healthy volunteers.

Author

de Haas SL, Franson KL, Schmitt JA, Cohen AF, Fau JB, Dubruc C, and van Gerven JM

Subjects

Adult, Attention drug effects, Cognition drug effects, Cross-Over Studies, Double-Blind Method, Eye Movements drug effects, Female, GABA Agonists adverse effects, GABA Modulators adverse effects, Humans, Indoles adverse effects, Lorazepam adverse effects, Male, Memory drug effects, Neuropsychological Tests, Postural Balance drug effects, Pursuit, Smooth drug effects, Pyrroles adverse effects, Receptors, GABA-A, Saccades drug effects, Young Adult, GABA Agonists pharmacokinetics, GABA Agonists pharmacology, GABA Modulators pharmacokinetics, GABA Modulators pharmacology, GABA-A Receptor Agonists, Indoles pharmacokinetics, Indoles pharmacology, Lorazepam pharmacokinetics, Lorazepam pharmacology, Pyrroles pharmacokinetics, Pyrroles pharmacology

Abstract

Benzodiazepines are effective short-term treatments for anxiety disorders, but their use is limited by undesirable side effects related to Central Nervous System impairment and tolerance development. SL65.1498 is a new compound that acts in vitro as a full agonist at the gamma-aminobutyric acid(A) 2 and 3 receptor and as a partial agonist at the 1 and 5 receptor subtypes. It is thought that the compound could be anxiolytic by its activation at the alpha2 and alpha3 receptor subtypes, without causing unfavourable side effects, which are believed to be mediated by the alpha1 and alpha5 subtypes. This study was a double-blind, five-way cross-over study to investigate the effects of three doses of SL65.1498 in comparison with placebo and lorazepam 2 mg in healthy volunteers. The objective was to select a dose level (expected to be therapeutically active), free of any significant deleterious effect. Psychomotor and cognitive effects were measured using a validated battery of measurements, including eye movements, body sway, memory tests, reaction-time assessments, and visual analogue scales. The highest dose of SL65.1498 showed slight effects on saccadic peak velocity and smooth pursuit performance, although to a much lesser extent than lorazepam. In contrast to lorazepam, none of the SL65.1498 doses affected body sway, visual analogue scale alertness, attention, or memory tests. This study showed that the three doses of SL65.1498 were well tolerated and induced no impairments on memory, sedation, psychomotor, and cognitive functions.

Published

2009

36. The pharmacokinetics of idraparinux, a long-acting indirect factor Xa inhibitor: population pharmacokinetic analysis from Phase III clinical trials.

Author

Veyrat-Follet C, Vivier N, Trellu M, Dubruc C, and Sanderink GJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Atrial Fibrillation, Child, Child, Preschool, Factor Xa Inhibitors, Female, Half-Life, Humans, Male, Metabolic Clearance Rate, Middle Aged, Pharmacokinetics, Pulmonary Embolism prevention & control, Renal Insufficiency complications, Secondary Prevention, Single-Blind Method, Venous Thrombosis prevention & control, Young Adult, Oligosaccharides pharmacokinetics, Pulmonary Embolism drug therapy, Renal Insufficiency drug therapy, Venous Thrombosis drug therapy

Abstract

Background: Idraparinux, a long-acting synthetic pentasaccharide, is a specific antithrombin-dependent inhibitor of activated factor X that has been investigated in the treatment and prevention of thromboembolic events., Objectives: To characterize the population pharmacokinetic profile of idraparinux in patients enrolled in van Gogh and Amadeus Phase III clinical trials., Patients and Methods: Idraparinux was administered once-weekly subcutaneously at a dose of 2.5 mg, or 2.5 mg (first dose) and then 1.5 mg for patients with severe renal insufficiency (creatinine clearance<30 mL min(-1)). A population pharmacokinetic model was developed using data from 704 patients with acute deep-vein thrombosis or pulmonary embolism, 1310 patients suffering from atrial fibrillation, and 40 healthy subjects. Potential covariates analyzed included demographics (age, sex, weight and ethnicity), and serum creatinine and creatinine clearance determinations., Results: A three-compartment model best described idraparinux pharmacokinetics, with interindividual variability on clearance, central volume of distribution, and absorption rate constant; residual variability was low. Typical clearance, central volume of distribution, absorption rate constant and volume of distribution at steady-state were 0.0255 L h(-1), 3.36 L, 1.37 h and 30.8 L, respectively. Peak concentration was reached at 2.5 h. The terminal half-life was 66.3 days and time to steady-state was 35 weeks. At steady-state, exposures were similar for patients without and with severe renal impairment receiving adjusted-dose. Creatinine clearance was the most important covariate affecting idraparinux clearance. The particular characteristics of idraparinux--rapid onset of action and long-acting anticoagulant effect--offer interesting clinical perspectives currently under investigation with idrabiotaparinux, the reversible biotinylated form of idraparinux.

Published

2009

37. Pharmacokinetic profile of a new modified release formulation of zolpidem designed to improve sleep maintenance.

Author

Weinling E, McDougall S, Andre F, Bianchetti G, and Dubruc C

Subjects

Administration, Oral, Adult, Biological Availability, Cross-Over Studies, Delayed-Action Preparations, Half-Life, Humans, Hypnotics and Sedatives administration & dosage, Hypnotics and Sedatives adverse effects, Hypnotics and Sedatives blood, Infusions, Intravenous, Male, Middle Aged, Models, Biological, Pyridines administration & dosage, Pyridines adverse effects, Pyridines blood, Reference Values, Zolpidem, Hypnotics and Sedatives pharmacokinetics, Pyridines pharmacokinetics, Sleep drug effects

Abstract

The aim of this study was to compare the relative bioavailability and the pharmacokinetic profile of a single oral dose of a zolpidem modified-release (MR) 12.5-mg formulation with those of the standard 10-mg zolpidem immediate-release (IR) formulation. Absolute bioavailabilities of oral formulations were evaluated using intravenously (i.v.) administered zolpidem as a reference. Twenty-four healthy, Caucasian, male volunteers (18-45 years old) received single doses of three oral formulations (zolpidem-MR 12.5 mg, zolpidem-IR 10 mg and an experimental form) and zolpidem i.v. infusion (8 mg) in a randomized, open-label, crossover trial. Blood samples (18 time-points) were collected up to 16 h post-dose after oral administration and up to 12 h post-dose after i.v. administration. Pharmacokinetic parameters were determined by non-compartmental analysis, allowing comparisons between treatments based on estimated ratios and differences, with 90% confidence intervals. The initial absorption phase of the zolpidem-MR formulation was as fast as that of zolpidem-IR with no significant difference in t(max). With zolpidem-MR 12.5 mg, C(max) was moderately lower than with zolpidem-IR (ratio of 0.82), and plasma zolpidem concentrations were maintained above those observed with zolpidem-IR for a longer period of time, particularly from 3 to 6 h post-dose. This was confirmed by an increase in half-value duration (HVD) from 2.3 h with zolpidem-IR to 4.6 h with zolpidem-MR 12.5 mg. The mean terminal half-life was similar between formulations. Zolpidem-MR 12.5 mg provides the appropriate pharmacokinetic characteristics to extend plasma zolpidem concentrations into the middle of the night (3-6 h post-dose), while retaining the same t(max) and terminal half-life.

Published

2006

38. New metabolic and pharmacokinetic characteristics of thiocolchicoside and its active metabolite in healthy humans.

Author

Trellu M, Filali-Ansary A, Françon D, Adam R, Lluel P, Dubruc C, and Thénot JP

Subjects

Administration, Oral, Adult, Animals, Area Under Curve, Biological Availability, Chromatography, High Pressure Liquid, Colchicine blood, Colchicine pharmacokinetics, Cross-Over Studies, Half-Life, Humans, Intestinal Absorption, Male, Rats, Rats, Sprague-Dawley, Colchicine analogs & derivatives, Colchicine metabolism, Muscle Relaxation drug effects

Abstract

Thiocolchicoside (TCC) has been prescribed for several years as a muscle relaxant drug, but its pharmacokinetic (PK) profile and metabolism still remain largely unknown. Therefore, we re-investigated its metabolism and PK, and we assessed the muscle relaxant properties of its metabolites. After oral administration of 8 mg (a therapeutic dose) of 14C-labelled TCC to healthy volunteers, we found no detectable TCC in plasma, urine or faeces. On the other hand, the aglycone derivative obtained after de-glycosylation of TCC (M2) was observed and, in addition, we identified, as the major circulating metabolic entity, 3-O-glucuronidated aglycone (M1) obtained after glucuro-conjugation of M2. One hour after oral administration, M1 plus M2 accounted for more than 75% of the circulating total radioactivity. The pharmacological activity of these metabolites was assessed using a rat model, the muscle relaxant activity of M1 was similar to that of TCC whereas M2 was devoid of any activity. Subsequently, to investigate the PK profile of TCC in human PK studies, we developed and validated a specific bioanalytical method that combines liquid chromatography and ultraviolet detection to assay both active entities. After oral administration, TCC was not quantifiable with an lower limit of quantification set at 1 ng/mL, whereas its active metabolite M1 was detected. M1 appeared rapidly in plasma (tmax=1 h) and was eliminated with an apparent terminal half-life of 7.3 h. In contrast, after intramuscular administration both active entities (TCC and M1) were present; TCC was rapidly absorbed (tmax=0.4 h) and eliminated with an apparent terminal half-life of 1.5 h. M1 concentration peaked at 5 h and this metabolite was eliminated with an apparent terminal half-life of 8.6 h. As TCC and M1 present an equipotent pharmacological activity, the relative oral pharmacological bioavailability of TCC vs. intramuscular administration was calculated and represented 25%. Therefore, to correctly investigate the PK and bioequivalence of TCC, the biological samples obtained must be assayed with a bioanalytical method able to specifically analyse TCC and its active metabolite M1.

Published

2004

39. Population pharmacokinetic analysis and optimization of the experimental design for mizolastine solution in children.

Author

Mentré F, Dubruc C, and Thénot JP

Subjects

Adult, Benzimidazoles administration & dosage, Child, Child, Preschool, Drug Administration Schedule, Female, Histamine H1 Antagonists administration & dosage, Humans, Least-Squares Analysis, Male, Nonlinear Dynamics, Solutions, Benzimidazoles pharmacokinetics, Histamine H1 Antagonists pharmacokinetics, Models, Chemical, Research Design statistics & numerical data

Abstract

Mizolastine is a second generation antihistamine agent approved in Europe for the treatment of allergic rhinitis and skin conditions for which Sanofi-Synthélabo is developing a pediatric solution. Our objective was to design the population pharmacokinetic (PK) study of mizolastine pediatric solution in children. A bioavailability study of this solution compared to the marketed tablet was performed in 18 young volunteers. These PK data were analyzed by nonlinear regression using a two-compartment open model with zero-order absorption. From the estimated parameters, we designed population PK studies in two groups of children: 6 to 12 years and 2 to 6 years, respectively. To compare several population designs and to derive the optimal ones, we used the determinant of the Fisher information matrix of the population characteristics using a first-order expansion of the model. We have evaluated a "reference" population design with 10 samples (from 0.25 to 36 hr after drug intake) per child in 6 children, which could not be implemented in practice for ethical reasons. We then derived optimal population designs with 1, 2, 3, 4, or 5 samples per child and a total of 60 samples. Finally, the designs that were implemented in the population PK study were "compromise" population designs with 60 samples; one defined for 20 children 6 to 12 years old, and one with 24 children 2 to 6 years. In the older group, the population design involved 8 children with a catheter from which 6 samples at time 0.25, 0.5, 0.75, 2, 3, and 6 hr after drug intake are collected, and 12 children with only one sample at time 8, 12, 24, or 36 hr. In the younger group, the population design involved 15 children with a catheter who are divided in three groups with four samples at different times from 0.25 to 6 hr after drug intake, and 12 children with only one sample at time 8, 12, 18, or 24 hr. The expected average increase of variances of these designs compared to the reference design were 1.6 and 1.8 for the older and younger group, respectively, which was decided to be acceptable. Better population designs would have involved three groups of children with five samples per child but could not be implemented in practice. The data of the PK study in children 6 to 12 years were available and were analyzed using NONMEM. A total of 53 concentrations were obtained in 18 children. The same two-compartment model with zero-order absorption was used. The interindividual variability in children was small. The estimated population parameters in children 6 to 12 years, were 0.28 L/kg for Vc/F, 0.10 L/hr per kg for CL/F, 0.53 hr-1 for lambda 1, 0.076 hr-1 for lambda 2, and 0.49 hr for Tabs. These values were close to the median values observed in young volunteers when standardized to 70 kg; notably, CL/F in L/hr per kg was similar, so that a dose of 0.15 mg/kg o.d. for mizolastine pediatric solution should give an equivalent area under the curve to a 10 mg o.d. tablet in adults.

Published

2001

40. Pharmacokinetic and pharmacodynamic modeling of mizolastine in healthy volunteers with an indirect response model.

Author

Deschamps C, Dubruc C, Mentre F, and Rosenzweig P

Subjects

Administration, Oral, Adult, Benzimidazoles adverse effects, Body Fluid Compartments, Cross-Over Studies, Dose-Response Relationship, Drug, Double-Blind Method, Histamine, Histamine H1 Antagonists adverse effects, Humans, Male, Placebos, Predictive Value of Tests, Skin Tests, Urticaria chemically induced, Urticaria prevention & control, Benzimidazoles pharmacokinetics, Benzimidazoles pharmacology, Histamine H1 Antagonists pharmacokinetics, Histamine H1 Antagonists pharmacology, Models, Biological

Abstract

Objective: The aim of this work was to model the pharmacokinetic and pharmacodynamic relationship of mizolastine, a new H1-receptor antagonist obtained from histamine-induced wheal and flare inhibition test., Methods: Fifteen healthy volunteers participated in this double-blind crossover study and randomly received single doses of 5, 10, 15, and 20 mg of mizolastine and placebo at 1 week intervals. Simultaneous histamine tests and blood samples were performed before and at 9 different times up to 24 hours after each dosing. Pharmacokinetic and pharmacodynamic modeling were performed subject by subject for the 4 doses altogether by nonlinear regression. First, plasma concentrations were fit according to a two-compartment open model with zero order absorption and first order elimination. Then an indirect response model with inhibition of the formation rate was developed to describe the pharmacodynamic relationships between flare or wheal raw areas and plasma concentrations with the use of the pharmacokinetic parameters that were previously estimated., Results: Mizolastine dose dependently inhibited the histamine-induced wheal and flare formation with a submaximum effect attained after 10 mg. The mean values of the pharmacodynamic parameters of apparent zero-order rate constant for the flare or wheal spontaneous appearance (k(in)), the first-order rate constant for the flare or wheal disappearance, the mizolastine concentration that produced 50% suppression of the maximum attainable inhibition of k(in), and the maximum attainable inhibition of the effect production were 14.1 cm2/h (coefficient of variation [CV], 32%), 0.68 h(-1) (CV, 24%), 21.1 ng/mL (CV, 77%), and 0.92 (CV, 8%), respectively, for the flare and 1.9 cm2/h (CV, 64%), 0.63 h-1 (CV, 39%), 43.9 ng/mL (CV, 68%), and 0.87 (CV, 12%), respectively, for the wheal inhibition., Conclusion: Pharmacokinetic and pharmacodynamic relationships of mizolastine were reliably described with the use of an indirect pharmacodynamic model; this led to an accurate prediction of the pharmacodynamic activity of mizolastine.

Published

2000

41. Study of cardiac repolarization in healthy volunteers performed with mizolastine, a new H1-receptor antagonist.

Author

Chaufour S, Caplain H, Lilienthal N, L'héritier C, Deschamps C, Dubruc C, and Rosenzweig P

Subjects

Adult, Area Under Curve, Benzimidazoles adverse effects, Benzimidazoles pharmacokinetics, Blood Pressure drug effects, Cross-Over Studies, Double-Blind Method, Electrocardiography drug effects, Electrocardiography, Ambulatory, Headache chemically induced, Heart physiology, Heart Rate drug effects, Histamine H1 Antagonists adverse effects, Histamine H1 Antagonists pharmacokinetics, Humans, Male, Sleep Stages drug effects, Benzimidazoles pharmacology, Heart drug effects, Histamine H1 Antagonists pharmacology

Abstract

Aims: The occurrence of serious dysrhythmias, such as torsades de pointes, with terfenadine and astemizole had led to a reexamination of the potential effect of H1 antihistamines on cardiac repolarization. Mizolastine is a potent, selective, nonsedating peripherally acting H1-receptor antagonist which is registered for rhinitis and urticaria at a recommended dose of 10 mg once daily. The present study was carried out to investigate the effects of therapeutic and supratherapeutic doses of mizolastine, on ventricular repolarization in healthy volunteers., Methods: Twenty-four healthy young volunteers participated in a double-blind, placebo-controlled, randomised study with three parallel groups. Each group consisted of 2 way cross-over 7 day treatment periods where mizolastine (10, 20 or 40 mg) and placebo were randomly administered. On day 1 and day 7, 12-lead ECG recordings were performed prior and 0.5, 1, 2, 3, 4, 6, 8, 12, 16, and 20 h after dosing and from day 2 to day 6, before dosing and 1, 2, 3, and 4 h after., Results: Whatever the analysis used (raw data, changes from baseline, incidence of individual out-of-range values) no significant differences were observed at any dose level vs placebo, on any of ECG parameters (HR, PR, QRS, QT, and QTc). In particular, no effect of mizolastine vs placebo was shown on QT and QTc although 95% CIs were wide. The only subject who exhibited a QTc>/=450 ms received placebo for 7 days., Conclusions: This study found no evidence of an effect of mizolastine up to 40 mg (four times the therapeutic dose) on ventricular repolarization in healthy volunteers.

Published

1999

42. Clinical pharmacology of befloxatone: a brief review.

Author

Rosenzweig P, Patat A, Curet O, Durrieu G, Dubruc C, Zieleniuk I, and Legangneux E

Subjects

Adult, Aged, Brain drug effects, Brain physiology, Cognition drug effects, Cognition physiology, Dose-Response Relationship, Drug, Drug Interactions, Electroencephalography, Humans, Methoxyhydroxyphenylglycol analogs & derivatives, Methoxyhydroxyphenylglycol blood, Methoxyhydroxyphenylglycol metabolism, Middle Aged, Monoamine Oxidase Inhibitors pharmacokinetics, Oxazoles pharmacokinetics, Placebos, Psychomotor Performance drug effects, Psychomotor Performance physiology, Tyramine adverse effects, Tyramine pharmacology, Monoamine Oxidase Inhibitors adverse effects, Monoamine Oxidase Inhibitors pharmacology, Oxazoles adverse effects, Oxazoles pharmacology

Abstract

Clinical pharmacology studies of befloxatone, a new selective reversible inhibitor of monoamine oxidase-A (MAO-A), have addressed safety, with special emphasis on tyramine interactions, and have also investigated pharmacokinetics (PK) and pharmacodynamics in terms of both MAO-A inhibition (using 3,4-dihydroxyphenylglycol, DHPG, as a pharmacological activity marker) and effects on psychomotor and cognitive function, in young and elderly healthy volunteers. Clinical and laboratory safety data were satisfactory in healthy volunteers given single doses of up to 160 mg or repeated doses of up to 80 mg/day for 7 days. Tyramine interaction studies showed that the expected potentiation of the tyramine pressor effect occurred with a safety margin that was so wide as to make dietary restrictions unnecessary with dosages of up to 20 mg once daily in clinical settings. Absorption was rapid (tmax = 2 h), terminal halflife was about 11 h, and PK parameters increased linearly with the dose. Befloxatone induced a dose-dependent decrease in plasma DHPG levels from 2.5 mg upwards, and a 10-mg dose provided sub-maximal activity (80% DHPG decrease) of 24 h duration. No sedative or stimulant effects were detected using several batteries of psychometric tests. Befloxatone was devoid of deleterious effects on memory in young volunteers, and exhibited the EEG profile of a non-sedative antidepressant. In summary, available clinical pharmacology studies confirm that befloxatone is a safe and potent RIMA with no potential for inducing deleterious CNS effects.

Published

1998

43. Lack of effect of mizolastine on the safety and pharmacokinetics of digoxin administered orally in repeated doses to healthy volunteers.

Author

Chaufour S, Le Coz F, Denolle T, Dubruc C, Cimarosti I, Deschamps C, Ulliac N, Delhotal-Landes B, and Rosenzweig P

Subjects

Adult, Anti-Arrhythmia Agents administration & dosage, Area Under Curve, Benzimidazoles administration & dosage, Blood Pressure drug effects, Cross-Over Studies, Digoxin administration & dosage, Double-Blind Method, Drug Interactions, Electrocardiography drug effects, Histamine H1 Antagonists administration & dosage, Humans, Male, Anti-Arrhythmia Agents pharmacokinetics, Benzimidazoles pharmacology, Digoxin pharmacokinetics, Histamine H1 Antagonists pharmacology

Abstract

The effects of mizolatine, a new H1 receptor antagonist, on safety and pharmacokinetics of digoxin were studied in a double-blind placebo-controlled crossover study. After administration of digoxine alone (0.25 mg o.d. for 7 days), 12 healthy young male volunteers (23+/-2 years) received either placebo and digoxin (0.25 mg o.d.) or mizolastine (10 mg o.d.) and digoxin (0.25 mg o.d.) during 7 days. The assessment criteria consisted in hemodynamic and ECG parameters recordings and the pharmacokinetics of digoxin during the last day of coadministration (day 14). No difference between the 2 treatment groups was evidenced on ECG, hemodynamic, and clinical and laboratory safety parameters. No change in AUC and tmax was recorded. No clinically relevant effect of mizolastine on the digoxin pharmacokinetics was found. However, a statistically significant increase in digoxin Cmax (3.03+/-0.18 nmolxl(-1) vs 2.52+/-0.19 nmolxl(-1), p < 0.05) and Cmin (0.99+/-0.08 nmolxl(-1) vs 0.87+/-0.07 nmolxl(-1), p=0.05) occurred after the coadministration vs digoxin alone. It can be concluded that mizolastine and digoxin at therapeutic dosages can be safely coadministered.

Published

1998

44. Population pharmacokinetic analysis of mizolastine and validation from sparse data on patients using the nonparametric maximum likelihood method.

Author

Mesnil F, Mentré F, Dubruc C, Thénot JP, and Mallet A

Subjects

Humans, Likelihood Functions, Models, Statistical, Randomized Controlled Trials as Topic, Reproducibility of Results, Benzimidazoles pharmacokinetics, Histamine H1 Antagonists pharmacokinetics

Abstract

A population analysis of the kinetics of mizolastine was performed from concentrations on 449 allergic patients, using the nonparametric maximum likelihood method (NPML). A two-compartment open model with zero-order absorption was used to describe the kinetics of mizolastine after oral administration. A heteroscedastic variance model was assumed for the error. To explain the kinetic variability, eight covariates were introduced in the analysis: gender, pharmaceutical dosage form, age, body weight, serum creatinine concentration, creatinine renal clearance, plasma levels of hepatic transaminases ASAT and ALAT. Their relationships to the kinetic parameters were studied by means of the estimated distribution of each kinetic parameter conditional on different levels of each covariate. An important interindividual kinetic variability was found for all parameters. Moreover, several kinetic parameters among which the duration of absorption were found to be influenced by pharmaceutical dosage form and gender. Body weight and creatinine renal clearance were found to have a little influence on the oral clearance and the smallest disposition rate constant. This population analysis was validated on a separate group of 247 other patients. For each observed concentration of this sample, a predictive distribution was computed using the individual covariates. Predicted concentrations and standardized prediction errors were deduced. The mean and variance of the standardized prediction errors were, respectively, 0.21 and 2.79. Moreover, in the validation sample, the predicted cumulative distribution function of each observed concentration was computed. Empirical distribution of these values was not significantly different from a uniform distribution, as expected under the assumption that the population model estimated by NPML is adequate.

Published

1998

45. Pharmacokinetic analysis of mizolastine in healthy young volunteers after single oral and intravenous doses: noncompartmental approach and compartmental modeling.

Author

Mesnil F, Dubruc C, Mentre F, Huet S, Mallet A, and Thenot JP

Subjects

Administration, Oral, Adolescent, Adult, Benzimidazoles administration & dosage, Body Fluid Compartments, Histamine H1 Antagonists administration & dosage, Humans, Injections, Intravenous, Mathematical Computing, Benzimidazoles pharmacokinetics, Histamine H1 Antagonists pharmacokinetics, Models, Biological

Abstract

This paper presents the analysis of the kinetics of a new antihistamine, mizolastine, in 18 healthy volunteers, from concentrations measured after an intravenous infusion and two different oral administrations: tablet and capsule. Two approaches were used to analyze these data: (i) a noncompartmental approach implemented in PHARM-NCA; (ii) a compartmental modeling approach implemented in a new S-PLUS library, NLS2, which allows the estimation of variance parameters simultaneously with the kinetic parameters. For the compartmental modeling approach, two-compartment open models were used. According to the Akaike criterion, the best model describing the kinetics of mizolastine after oral administration was the zero-order absorption model. The kinetic parameters obtained with PHARM-NCA and NLS2 were similar. The estimated duration of absorption was greater for the tablets than for the capsules (with means equal to 1.13 hr and 0.84 hr respectively). After an intravenous infusion, the mean estimated clearance was 4.9 L/hr, the mean lambda 2-phase apparent volume of distribution was 89.6 L and the mean terminal half-life was 12.9 hr.

Published

1997

46. Pharmacodynamics and pharmacokinetics of two dose regimens of befloxatone, a new reversible and selective monoamine oxidase inhibitor, at steady state in healthy volunteers.

Author

Patat A, le Coz F, Dubruc C, Gandon JM, Durrieu G, Cimarosti I, Jezequel S, Curet O, Zieleniuk I, Allain H, and Rosenzweig P

Subjects

Adult, Cross-Over Studies, Double-Blind Method, Drug Administration Schedule, Humans, Male, Metabolic Clearance Rate, Methoxyhydroxyphenylglycol blood, Monoamine Oxidase Inhibitors administration & dosage, Oxazoles administration & dosage, Methoxyhydroxyphenylglycol analogs & derivatives, Monoamine Oxidase Inhibitors pharmacokinetics, Monoamine Oxidase Inhibitors pharmacology, Oxazoles pharmacokinetics, Oxazoles pharmacology

Abstract

The pharmacodynamic equipotency of 2 dose regimens (5 mg twice daily versus 10 mg once daily) of befloxatone, a new reversible and selective monoamine oxidase A (MAO-A) inhibitor, after single and multiple doses for 6 days was examined in a randomized, double-blind, three-way crossover, placebo-controlled trial of 12 healthy volunteers. Plasma levels of the deaminated metabolite 3-4 dihydroxyphenylglycol (DHPG), as measured by high-performance liquid chromatography (HPLC) with coulometric electrochemical detection, were used as an index of MAO inhibition. A single dose of befloxatone produced a significant dose-related reduction in plasma DHPG levels, as shown by the decrease in the 24-hour area under the concentration-time curve (AUC0-24) of DHPG, which peaked 2 hours after administration and persisted over 24 hours. Both dose regimens provided equipotent extent and duration of MAO-A inhibition at steady state, suggesting a once daily dosage should be sufficient for most patients. The pharmacokinetic bioavailability at steady state of both dose regimens was also similar. The concentration-time effect curve after a single dose revealed a hysteresis corresponding to the delay necessary to elicit MAO inhibition and/or elimination of DHPG. The relationship between plasma levels of DHPG and/or elimination of plasma concentrations of DHPG and befloxatone after a single dose can be modeled using the Emax model with a mean EC50 of 4.75 ng/mL, and suggests the presence of a maximal response from the single dose. This model permits prediction of steady-state levels of DHPG.

Published

1996

47. Inhibition of histamine-induced skin wheal and flare after 5 days of mizolastine.

Author

Pinquier JL, Caplain H, Cabanis MJ, Dubruc C, Stalla-Bourdillon A, and Rosenzweig P

Subjects

Adult, Benzimidazoles adverse effects, Benzimidazoles pharmacokinetics, Cross-Over Studies, Dermatitis, Allergic Contact etiology, Dose-Response Relationship, Drug, Double-Blind Method, Drug Administration Schedule, Histamine immunology, Histamine H1 Antagonists adverse effects, Histamine H1 Antagonists pharmacokinetics, Humans, Injections, Intradermal, Male, Placebos, Skin Tests, Benzimidazoles therapeutic use, Dermatitis, Allergic Contact prevention & control, Histamine H1 Antagonists therapeutic use

Abstract

Mizolastine is a new, nonsedating antihistamine providing satisfactory symptomatic relief in allergic rhinitis and urticaria. The purpose of this study was to use inhibition of wheal and flare formation after 2-mu g intradermal histamine injections as a measure of the antihistamine effect of repeated doses of mizolastine. Eight volunteers were enrolled in this four-arm, double-blind, cross-over, randomized study. Three dose levels of once-daily mizolastine (5 mg, 10 mg, and 15 mg) were compared with placebo during 5-day dose periods. Histamine tests were performed before drug intake on days 1 and 5, and then 2, 3, 4, 6, 8, 10, 12, 14, and 24 hours after drug intake on day 5. All 3 doses of mizolastine were more effective than placebo in suppressing wheal and flare reactions, and the antihistamine activity was highest at both the 10- and 15-mg dose levels. The effect on the flare reaction appeared within 1 hour, reached a maximum effect 4 hours after administration, and persisted for as long as 24 hours. The relative changes in wheal and flare areas were correlated with mizolastine trough plasma levels on day 5. Safety was satisfactory in all groups. This study confirms that mizolastine is a rapid and potent antihistamine; and its long-lasting effectiveness indicates that a once-daily regimen is acceptable for clinical use.

Published

1996

48. Plasma and skin suction-blister-fluid pharmacokinetics and time course of the effects of oral mizolastine.

Author

Chosidow O, Dubruc C, Danjou P, Fuseau E, Espagne E, Bianchetti G, Thenot JP, Herson S, Rosenzweig P, and Revuz J

Subjects

Administration, Oral, Adult, Benzimidazoles blood, Histamine, Histamine H1 Antagonists blood, Humans, Hypersensitivity, Male, Benzimidazoles pharmacokinetics, Blister metabolism, Body Water metabolism, Histamine H1 Antagonists pharmacokinetics

Abstract

Objective: To investigate plasma and skin suction-blister-fluid pharmacokinetics of oral mizolastine in order to determine whether the drug concentration in the fluid of suction-induced skin blisters could better predict the antihistamine activity than the plasma concentration., Setting: Department of Internal Medicine, Université Paris 6., Subjects: Ten healthy male volunteers., Methods: The volunteers (mean age 26.8 years, mean weight 75.8 kg) received a single 10-mg oral dose of mizolastine at 1000 hours. The pharmacokinetic study included 11 plasma and 9 blister fluid samples and blister epidermal-roof specimens. Mizolastine was assayed by high-performance liquid chromatography (HPLC). Each volunteer also received nine intradermal injections of 5 micrograms histamine. Antihistamine activity was assessed as the post-treatment percentages of changes in the histamine-induced relative wheal and flare areas versus baseline., Results: Mizolastine mean Cmax (SD) and median tmax were, respectively, 380 ng.ml-1 and 0.8 h in plasma, and 21.8 ng.ml-1 and 10 h in blister fluid. Mizolastine could not be quantified in the epidermis. The maximal histamine-induced relative flare inhibition was 72.5% and was attained at the median time of 3 h post-dosing and therefore was delayed by 2.2 h with respect to the plasma tmax. Mean relative wheal inhibition, although lower, showed the same time profile. A direct relationship could not be found between drug concentrations in blister fluid and antihistamine activity. Simulated concentrations in the peripheral compartment better explain the maximum inhibition effect on flare, observed 3 h post-dosing, with a flatter hysteresis loop obtained when plotting relative flare inhibition versus plasma or blister-fluid drug concentrations., Conclusion: The mizolastine concentrations in the skin suction-blister fluid were not predictive of the antihistamine activity.

Published

1996

49. The psychomotor and cognitive effects of litoxetine in young and middle aged volunteers.

Author

Fairweather DB, Patat A, Rosenzweig P, Curson VH, Dunmore C, Dubruc C, and Hindmarch I

Subjects

Administration, Oral, Adult, Analysis of Variance, Choice Behavior drug effects, Chromatography, High Pressure Liquid, Computer Simulation, Cross-Over Studies, Double-Blind Method, Female, Flicker Fusion drug effects, Humans, Male, Memory drug effects, Middle Aged, Piperidines administration & dosage, Piperidines blood, Piperidines pharmacokinetics, Selective Serotonin Reuptake Inhibitors administration & dosage, Selective Serotonin Reuptake Inhibitors blood, Selective Serotonin Reuptake Inhibitors pharmacokinetics, Sleep drug effects, Cognition drug effects, Piperidines pharmacology, Psychomotor Performance drug effects, Selective Serotonin Reuptake Inhibitors pharmacology

Abstract

1. The effects of a range of doses of litoxetine (twice daily for 4 days), a novel specific serotonin re-uptake inhibitor, were evaluated in young and middle aged volunteers. 2. Psychometric testing was carried out at various time points on days 1 and 4 of each treatment period. The test battery consisted of critical flicker fusion (CFF), choice reaction time (CRT), compensatory tracking (CTT), Stroop and Sternberg memory scanning tests. Subjective feelings of sleep and sedation were measured by the Leeds Sleep Evaluation Questionnaire (LSEQ) and line analogue rating scales (LARS). 3. Pharmacokinetic profiles were determined from analyses of blood samples taken after the final dose on day 5. 4. Overall, there were few changes in any of the psychometric tests and although the higher doses of litoxetine improved CFF, these effects were weak in that differences could only be detected when the results were pooled against time. 5. The pharmacokinetic profile of litoxetine was very similar in both the young and middle aged subjects, and there was no difference regarding tolerability. 6. There is little evidence from this study to suggest that litoxetine has any intrinsic sedative activity which is likely to interfere with the performance of activities of everyday life.

Published

1995

50. Pharmacokinetic and bioavailability of diltiazem sustained-release: influence of food and time of administration.

Author

Bianchetti G, Bagheri H, Houin G, Dubruc C, and Thénot JP

Subjects

Administration, Oral, Adult, Biological Availability, Cross-Over Studies, Delayed-Action Preparations, Drug Administration Schedule, Humans, Male, Time Factors, Diltiazem administration & dosage, Diltiazem pharmacokinetics, Eating

Abstract

Diltiazem is a calcium channel blocking agent known to be effective in the treatment of angina pectoris, hypertension and supraventricular arrhythmias. To improve the conditions of diltiazem administration in the treatment of hypertensive patients, a sustained-release formulation (Mono-Tildiem LP 300 mg) allowing a single daily oral administration has been developed. The aim of the present study was to first evaluate the influence of food intake and second to evaluate those of the time of administration on the pharmacokinetic parameters and the bioavailability of this sustained-release formulation. The influence of these factors was investigated over two different open, randomized, cross-over studies in 12 healthy volunteers. Although a significant decrease in Tmax and an increase in Cmax occurred when diltiazem sustained-release was administered with food intake, AUC0-48, and therefore the fraction absorbed, were not modified either by concurrent food intake or by different times of administration. The minor modifications of pharmacokinetic parameters of diltiazem sustained release observed were unlikely to induce any clinical consequence.

Published

1995