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

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

Author

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

Subjects

Administration, Oral, Adult, Humans, Injections, Intravenous, Male, Pharmacokinetics, Time Factors, Volunteers, Biological Availability, Diltiazem pharmacokinetics, Drug Delivery Systems

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

52. Flumazenil antagonizes the central effects of zolpidem, an imidazopyridine hypnotic.

Author

Patat A, Naef MM, van Gessel E, Forster A, Dubruc C, and Rosenzweig P

Subjects

Adult, Analysis of Variance, Cross-Over Studies, Double-Blind Method, Humans, Hypnotics and Sedatives blood, Male, Memory drug effects, Psychomotor Performance drug effects, Pyridines blood, Zolpidem, Flumazenil pharmacology, Hypnotics and Sedatives antagonists & inhibitors, Pyridines antagonists & inhibitors

Abstract

Zolpidem is a new imidazopyridine-hypnotic that selectively binds to the central omega 1-receptor subtype. A double-blind, randomized, three-way, crossover placebo-controlled study was carried out in nine healthy male volunteers to assess the possible antagonism of central nervous system--depressant effects of zolpidem by flumazenil. Subjects received zolpidem (0.21 mg/kg) or placebo, intravenously, followed 17 minutes later by flumazenil (0.04 mg/kg) or placebo. Vigilance and performance were assessed by a trained anesthetist with use of ciliary reflex, response to a verbal instruction, subjective sedation, a tracking task, and a free recall task. Zolpidem produced a clinically relevant hypnotic effect in five subjects and significantly impaired performance in all nine subjects up to 90 minutes after dosing. Flumazenil rapidly antagonized clinical sedation in the five subjects who were asleep and significantly reversed the performance decrement within 3 minutes, without any escape phenomenon. Flumazenil did not change zolpidem plasma concentrations, confirming the pharmacodynamic nature of the interaction. Flumazenil may thus be a safe and effective antidote in patients with zolpidem overdosage.

Published

1994

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

Author

Patat A, Gram LF, Dubruc C, Brohier S, Cabanis MJ, and Rosenzweig P

Subjects

Aged, Benzimidazoles adverse effects, Benzimidazoles pharmacokinetics, Female, Humans, Reaction Time drug effects, Aging, Benzimidazoles pharmacology, Memory drug effects, Psychomotor Performance drug effects

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.

Published

1994

54. EEG profile of intravenous zolpidem in healthy volunteers.

Author

Patat A, Trocherie S, Thebault JJ, Rosenzweig P, Dubruc C, Bianchetti G, Court LA, and Morselli PL

Subjects

Administration, Oral, Adult, Alpha Rhythm drug effects, Beta Rhythm drug effects, Cross-Over Studies, Delta Rhythm drug effects, Double-Blind Method, Humans, Hypnotics and Sedatives adverse effects, Hypnotics and Sedatives pharmacokinetics, Injections, Intravenous, Male, Pyridines adverse effects, Pyridines pharmacokinetics, Sleep Stages drug effects, Zolpidem, Electroencephalography drug effects, Hypnotics and Sedatives pharmacology, Pyridines pharmacology

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

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

Author

Patat A, Trocherie S, Thébault JJ, Rosenzweig P, Dubruc C, Bianchetti G, Morselli PL, and Court LA

Subjects

Administration, Oral, Adult, Analysis of Variance, Dose-Response Relationship, Drug, Double-Blind Method, Humans, Male, Piperidines administration & dosage, Piperidines pharmacokinetics, Selective Serotonin Reuptake Inhibitors administration & dosage, Selective Serotonin Reuptake Inhibitors pharmacokinetics, Brain drug effects, Electroencephalography drug effects, Piperidines pharmacology, Selective Serotonin Reuptake Inhibitors pharmacology

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

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

Author

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

Subjects

Adult, Aged, Arousal drug effects, Biological Availability, Chromatography, High Pressure Liquid, Creatinine urine, Female, Humans, Hypnotics and Sedatives administration & dosage, Male, Middle Aged, Pyridines administration & dosage, Sleep drug effects, Spectrometry, Fluorescence, Zolpidem, Hypnotics and Sedatives pharmacokinetics, Hypnotics and Sedatives pharmacology, Pyridines pharmacokinetics, Pyridines pharmacology, Renal Dialysis, Uremia metabolism

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

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

Author

Rosenzweig P, Thebault JJ, Caplain H, Dubruc C, Bianchetti G, Fuseau E, and Morselli PL

Subjects

Adult, Benzimidazoles adverse effects, Benzimidazoles pharmacokinetics, Double-Blind Method, Histamine H1 Antagonists adverse effects, Histamine H1 Antagonists pharmacokinetics, Humans, Male, Psychometrics, Sleep Stages, Benzimidazoles pharmacology, Histamine H1 Antagonists pharmacology

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

58. Pharmacokinetics and safety of cicloprolol in uraemic patients.

Author

Fillastre JP, Aparicio M, Porquet C, Dubruc C, Rosenzweig P, and Morselli PL

Subjects

Adrenergic beta-Agonists adverse effects, Adrenergic beta-Agonists therapeutic use, Angina Pectoris complications, Angina Pectoris drug therapy, Angina Pectoris metabolism, Half-Life, Hemodynamics drug effects, Humans, Propanolamines adverse effects, Propanolamines therapeutic use, Uremia complications, Adrenergic beta-Agonists pharmacokinetics, Propanolamines pharmacokinetics, Uremia metabolism

Published

1991

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

Author

Dubruc C, Caqueret H, and Bianchetti G

Subjects

Humans, Chromatography, High Pressure Liquid methods, Vinca Alkaloids blood, Vincamine blood

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 micrometer, 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

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

Author

Guinebault P, Dubruc C, Hermann P, and Thénot JP

Subjects

Humans, Hydrogen-Ion Concentration, Hypnotics and Sedatives blood, Indicators and Reagents, Quality Control, Solvents, Spectrometry, Fluorescence, Zolpidem, Hypnotics and Sedatives analysis, Pyridines analysis

Published

1986

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

Author

Monin P, Clozel M, Morselli PL, Dubruc C, and Vert P

Subjects

Animals, Animals, Newborn, Brain physiopathology, Carbon Dioxide metabolism, Hydrogen-Ion Concentration, Oxygen metabolism, Seizures physiopathology, Swine metabolism, Brain metabolism, Phenobarbital metabolism, Seizures metabolism

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

62. Pharmacokinetics of indomethacin in the premature infant.

Author

Bianchetti G, Monin P, Marchal F, Dubruc C, Boutroy MJ, Morselli PL, and Vert P

Subjects

Creatinine blood, Ductus Arteriosus, Patent drug therapy, Female, Half-Life, Humans, Indomethacin therapeutic use, Infant, Newborn, Kinetics, Male, Prostaglandins biosynthesis, Indomethacin metabolism, Infant, Premature

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

63. Regional cerebral blood flow during bicuculline-induced seizures in the newborn piglet: effect of phenobarbital.

Author

Clozel M, Daval JL, Monin P, Dubruc C, Morselli PL, and Vert P

Subjects

Acid-Base Equilibrium, Animals, Blood Gas Analysis, Blood Pressure drug effects, Microspheres, Potassium Chloride pharmacology, Seizures chemically induced, Swine, Time Factors, Animals, Newborn physiology, Bicuculline pharmacology, Cerebrovascular Circulation drug effects, Phenobarbital pharmacology, Seizures physiopathology

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

64. Clonazepam pharmacokinetics and therapeutic efficacy in neonatal seizures.

Author

André M, Boutroy MJ, Dubruc C, Thenot JP, Bianchetti G, Sola L, Vert P, and Morselli PL

Subjects

Adult, Clonazepam administration & dosage, Clonazepam metabolism, Female, Half-Life, Humans, Infant, Newborn, Infusions, Intravenous, Kinetics, Male, Seizures congenital, Clonazepam therapeutic use, Seizures drug therapy

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

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

Author

Monin P, Dubruc C, Vert P, and Morselli PL

Subjects

Blood Pressure drug effects, Carbon Dioxide blood, Drug Administration Schedule, Half-Life, Humans, Infant, Newborn, Kinetics, Oxygen blood, Persistent Fetal Circulation Syndrome blood, Pulmonary Gas Exchange drug effects, Tolazoline blood, Tolazoline therapeutic use, Persistent Fetal Circulation Syndrome drug therapy, Tolazoline administration & dosage

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

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

Author

Boutroy MJ, Bianchetti G, Dubruc C, Vert P, and Morselli PL

Subjects

Acebutolol analogs & derivatives, Acebutolol blood, Acebutolol therapeutic use, Breast Feeding, Female, Humans, Hypertension drug therapy, Postpartum Period, Pregnancy, Prospective Studies, Acebutolol metabolism, Infant, Newborn blood, Milk, Human analysis

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

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

Author

Dubruc C, Hermann P, Haddouche A, Badarani MM, and Thénot JP

Subjects

Chromatography, High Pressure Liquid, Drug Stability, Humans, Indicators and Reagents, Kinetics, o-Phthalaldehyde analysis, Carbocysteine blood, Cysteine analogs & derivatives

Published

1987