Search

Your search keyword '"GANDON J"' showing total 33 results
Start Over Author "GANDON J" Language english
33 results on '"GANDON J"'

11. Effects of Single and Multiple Doses of a New Reversible MAO-A Inhibitor, Befloxatone, on Psychomotor Performance and Memory in Healthy Subjects.

Author

Patat, A., Gandon, J. M., Durrieu, G., Coz, F. Le, Curet, O., Cimarosti, I., and Allain, H.

Subjects
*MOTOR ability, *MEMORY, *PLACEBOS, *SHORT-term memory, *VIGILANCE (Psychology), *ANTIDEPRESSANTS
Abstract

The effects on memory, psychomotor performance and mood of two dosage regimens of befloxatone, a new reversible and selective MAO-A inhibitor were assessed in a randomized, double-blind, cross-over, placebo-controlled study involving 12 healthy young male volunteers. Befloxatone and a placebo were orally administered as single (5 and 10 mg) and repeated doses (10 mg once daily and 5 mg twice daily) at one week wash-out intervals. Objective tests evaluated both memory (working memory, immediate and delayed free recall of a word list, dual coding and faces recognition) and vigilance (continuous performance task (CPT), and digit symbol substitution (DSST)). Subjective mood and sleep were assessed using visual analogue scales and the Leeds Sleep Evaluation Questionnaire. Statistical analysis was conducted using an ANOVA with pairwise comparisons using the Student Newman Keuls procedure. Both dosage regimens of befloxatone (10mg once daily or 5 mg twice daily) were free of any detrimental effect on vigilance (CPT) and information processing (DSST) and did not significantly disrupt short- and long-term memory (working memory, free recall of words, dual coding and laces recognition). In addition, no subjective sedation or sleep disturbances were recorded. In conclusion, this study gives no evidence to suggest that befloxatone, at a daily dose which shows potent MAO-A inhibition, has any sedative or amnestic properties likely to interfere with the activities of everyday-life in young subjects and therefore may be safely administered in depressed outpatients. [ABSTRACT FROM AUTHOR]

Published
1995
Full Text
View/download PDF

12. Use of zolpidem 10 mg as a benzodiazepine substitute in 84 patients with insomnia.

Author

Allain, H., Le Coz, F., Borderies, P., Schuck, S., De La Giclais, B., Patat, A., and Gandon, J. M.

Subjects
ZOLPIDEM, INSOMNIA, DRUG withdrawal symptoms, BENZODIAZEPINES, TRIAZOLAM, HYPNOTICS
Abstract

The antagonistic effects of zolpidem 10 mg on withdrawal symptoms caused by abrupt or gradual discontinuation (half-dose over 4 nights) of triazolam 0·25 mg in patients with chronic insomnia, who had been receiving regular treatment for over one month, were assessed in a randomized, double-blind, placebo-controlled clinical trial in general practice. Eighty-four patients were enrolled, mostly women (67·9%), with a mean age of 54·3±11·0 years. Twenty-one different general practitioners were solicitated for the recruitment. The subjects were randomized into four groups, and all received triazolam 0·25 mg during the run-in phase from day 1 (D1) to day 3 (D3). The following treatments were given from D4 to D7: triazolam 0·125 mg+zolpidem 10 mg (Group 1); zolpidem 10 mg (Group 2); placebo (Group 3); or triazolam 0·125 mg+placebo (Group 4). Groups 1 and 2 received zolpidem 10 mg from D7 to D24, while Groups 3 and 4 received placebo. Finally, all four groups received placebo (blind withdrawal phase) from D25 to D28. The following assessment criteria were used: clinical global impression (CGI) scale completed by the practitioner; patient questionnaire based on routine sleep criteria, wakefulness and daytime alertness. Secondary criteria were sleep diaries and visual analogue scales. Study drop-outs were reported and explained. The effectiveness/tolerance ratio was found to be statistically significant using the CGI (p <0·007) in favour of zolpidem 10 mg. There was no significant difference in patients subjective assessment between the groups except for nightmares (p <0·04) less frequent in patients receiving zolpidem. Zolpidem was found to be more effective than placebo at D21 (CGI) according to sleep diaries; the zolpidem group showed a statistically significant difference as compared to the three other concerning four sleep parameters: number of awakenings, anxiety, sleep duration, energy. Drop-out rates were significantly lower in the zolpidem group than in other ones (p <0·01). Abrupt and gradual triazolam withdrawal over 4 nights induced withdrawal symptoms. Equally no specific phenomena were observed at the end of the trial during the blind withdrawal phase. This study shows that zolpidem 10 mg improves sleep quality and reduces withdrawal symptoms after abrupt or gradual discontinuation of triazolam 0·25 mg in chronic patients with chronic insomnia. Copyright © 1998 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published
1998
Full Text
View/download PDF

13. Therapeutic effect of mitoxantrone combined with methylprednisolone in multiple sclerosis: a randomised multicentre study of active disease using MRI and clinical criteria.

Author

Edan, G, Miller, D, Clanet, M, Confavreux, C, Lyon-Caen, O, Lubetzki, C, Brochet, B, Berry, I, Rolland, Y, Froment, J C, Cabanis, E, Iba-Zizen, M T, Gandon, J M, Lai, H M, Moseley, I, and Sabouraud, O

Subjects
MULTIPLE sclerosis diagnosis, AMENORRHEA, BALDNESS, IMMUNOMODULATORS, COMBINATION drug therapy, COMPARATIVE studies, LEUCOPENIA, LONGITUDINAL method, MAGNETIC resonance imaging, RESEARCH methodology, MEDICAL cooperation, MULTIPLE sclerosis, RESEARCH, EVALUATION research, RANDOMIZED controlled trials, MITOXANTRONE, METHYLPREDNISOLONE
Abstract

Objective: To evaluate the efficiency of mitoxantrone in multiple sclerosis.Methods: Forty two patients with confirmed multiple sclerosis, selected as having a very active disease on clinical and MRI criteria were randomised to receive either mitoxantrone (20 mg intravenously (IV) monthly) and methylprednisolone (1 g iv monthly) or methylprednisolone alone over six months. In the steroid alone group five patients dropped out due to severe exacerbation.Results: Blinded analysis of MRI data showed significantly more patients with no new enhancing lesions in the mitoxantrone group compared with the steroid alone group, (90% v 31%, P < 0.001). In the mitoxantrone group there was a month by month decrease almost to zero in the number of new enhancing lesions, and in the total number of enhancing lesions, whereas both remained high in the steroid alone group. The differences were significant for both indices at all months from 1-6. Unblinded clinical assessments showed a significant improvement in change in EDSS at months 2-6 in the mitoxantrone group, with a final mean improvement of more than one point (-1.1 v + 0.3; P < 0.001). There was a significant reduction in the number of relapses (7 v 31; P < 0.01), and an increase in the number of patients free of exacerbation (14 v 7; P < 0.05).Conclusion: In this selected group of patients with multiple sclerosis with very active disease, mitoxantrone combined with methylprednisolone was effective in improving both clinical and MRI indices of disease activity over a period of six months whereas methylprednisolone alone was not. Further double blinded long term studies are needed to properly evaluate the effect of mitoxantrone on progression in disability. [ABSTRACT FROM AUTHOR]

Published
1997

17. An in-vivo magnetic resonance imaging study of the olfactory bulbectomized rat model of depression.

Author

Wrynn AS, Mac Sweeney CP, Franconi F, Lemaire L, Pouliquen D, Herlidou S, Leonard BE, Gandon J, and de Certaines JD

Subjects
Amygdala physiology, Amygdala physiopathology, Animals, Brain physiology, Caudate Nucleus physiology, Caudate Nucleus physiopathology, Cerebral Cortex physiology, Cerebral Cortex physiopathology, Cerebral Ventricles physiology, Cerebral Ventricles physiopathology, Disease Models, Animal, Hippocampus physiology, Hippocampus physiopathology, Magnetic Resonance Imaging, Rats, Reference Values, Brain physiopathology, Depression physiopathology, Olfactory Bulb physiology
Abstract

The olfactory bulbectomized (OB) rat is a well-accepted animal model of depression. The present magnetic resonance imaging (MRI) investigation demonstrates alterations in signal intensities in cortical, hippocampal, caudate and amygdaloid regions in OB animals, but not in sham operated controls. Ventricular enlargement was also evident in OB animals. These alterations have implications with regard to the face and construct validity of this model.

Published
2000
Full Text
View/download PDF

18. Detection and quantification of lysozyme in champagne wines.

Author

Marchal R, Chaboche D, Marchal-Delahaut L, Gerland C, Gandon JP, and Jeandet P

Subjects
Antigen-Antibody Reactions, Blotting, Western, Chromatography, High Pressure Liquid, Electrophoresis, Polyacrylamide Gel, Muramidase analysis, Wine analysis
Abstract

We describe here techniques to detect and quantify lysozyme in Pinot noir and Chardonnay Champagne wines. Using a dot-blot technique, lysozyme antibodies were able to recognize their antigens even when the concentration of lysozyme in wine was 75 mg/L. SDS-PAGE was the second technique used. After Coomassie Brilliant Blue (CBB) staining or antibody immunostaining was performed, the wine originating from the lysozyme-treated must gave only one band corresponding to the lysozyme. It is then possible to precisely determine the concentration of lysozyme in a must or a wine by densitometric measurement of this band. The control wine gave no band with the CBB staining, such as with the immunostaining. The quantification of lysozyme with HPLC is another useable technique because the lysozyme elution time is largely superior to that of all of the wine compounds. In wines, losses of lysozyme were higher when the enzyme was added at one time to the must (-34% for the Pinot noir and -37% for the Chardonnay) than when lysozyme is added in 2-fold both in the must and in the wine (around -26% for the two wines). The lowest diminution is observed when lysozyme was added to the wine only (-18%) in comparison to the addition to the must at 300 mg/L (-43%).

Published
2000
Full Text
View/download PDF

19. Aminotransferase levels and silymarin in de novo tacrine-treated patients with Alzheimer's disease.

Author

Allain H, Schück S, Lebreton S, Strenge-Hesse A, Braun W, Gandon JM, and Brissot P

Subjects
Aged, Chemical and Drug Induced Liver Injury, Cognition drug effects, Cognition Disorders diagnosis, Double-Blind Method, Humans, Neuropsychological Tests, Alzheimer Disease drug therapy, Cholinesterase Inhibitors pharmacology, Protective Agents pharmacology, Silymarin adverse effects, Silymarin blood, Tacrine antagonists & inhibitors, Tacrine blood, Transaminases blood, Transaminases drug effects
Abstract

Background: Silymarin is a well-known hepatoprotective agent. Tacrine, the first drug marketed for Alzheimer's disease (AD), induces an elevation of serum liver transaminase prohibiting an effective dosage in many patients. This 12-week randomised, double-blind, placebo-controlled study was undertaken to evaluate the ability of silymarin to antagonise or prevent the hepatotoxic effects of tacrine and to analyse its action on tacrine efficacy and tolerability., Methods: Outpatients suffering from mild-to-moderate dementia of the Alzheimer type were randomly assigned to two treatment groups: tacrine + silymarin and tacrine + placebo. The study was double-blind for silymarin and open for tacrine and was conducted in 22 French neurology and geriatric centres. Silymarin (420 mg/day) was given first (1 week) and tacrine was added at 40 mg/day for 6 weeks, then increased to 80 mg/day (6 weeks). Serum ALAT was the main evaluation criterion (> upper limit of normal, ULN). Serum ASAT as well as adverse side effects and cognitive performance assessed by MMSE and the Syndrome Kurtz test (SKT) were secondary evaluation criteria. Null hypotheses were evaluated with Fisher's exact test., Findings: 222 patients were recruited and received silymarin and tacrine (110 patients) or placebo and tacrine (112 patients). 28 patients dropped out; 217 were included in the intent-to-treat analysis. No statistical difference was observed between the two groups for serum ALAT (p = 0.39). Fewer patients had ALAT levels >5 ULN in the silymarin group (-33.3%). Side effects and notably gastrointestinal disorders were much less frequent in the silymarin group. Cognitive performance remained unchanged in both groups., Interpretation: Silymarin does not prevent tacrine-induced ALAT elevation but does reduce the rate of gastrointestinal and cholinergic side effects without any impact on cognitive status. As a consequence, silymarin (420 mg/day) could be co-administered with tacrine to improve tolerability in the initial phases of AD treatment.

Published
1999
Full Text
View/download PDF

20. Effects of 50mg amisulpride on EEG, psychomotor and cognitive functions in healthy sleep-deprived subjects.

Author

Patat A, Rosenzweig P, Miget N, Allain H, and Gandon JM

Subjects
Adult, Amisulpride, Analysis of Variance, Antipsychotic Agents adverse effects, Antipsychotic Agents pharmacokinetics, Cognition physiology, Dose-Response Relationship, Drug, Double-Blind Method, Headache chemically induced, Humans, Male, Nausea chemically induced, Reaction Time drug effects, Sleep drug effects, Sulpiride adverse effects, Sulpiride pharmacokinetics, Sulpiride pharmacology, Treatment Outcome, Antipsychotic Agents pharmacology, Cognition drug effects, Electroencephalography drug effects, Psychomotor Performance drug effects, Sleep Deprivation, Sulpiride analogs & derivatives
Abstract

Amisulpride, a substituted benzamide, binds selectively to the dopamine D2- and D3-receptors. It has higher affinity for limbic compared to striatal dopamine receptors in vivo. At low doses, amisulpride facilitates dopamine transmission via a selective blockade of presynaptic D2- and D3-receptors. Amisulpride is an active antipsychotic compound effective at low doses for negative symptoms and at high doses for positive symptoms of schizophrenia. The CNS profile of multiple doses of a low dosage regimen of amisulpride (50 mg once daily for 4 days) was assessed in a randomised, double-blind, 3-way crossover, placebo-controlled study carried out in 12 young sleep-deprived (for 36 h) subjects, using EEG and various measures of psychomotor and cognitive functions. Caffeine slow release (600 mg) was used as a positive reference. Multiple doses of 50 mg amisulpride once daily were devoid of any detrimental effects on EEG and psychomotor performance and cognitive function after total sleep deprivation. In addition, 50mg amisulpride partially antagonized the deleterious effects of sleep deprivation on EEG and subjective sedation as shown by trends, and a significant increase in EEG relative beta power and a decrease in subjective sedation. These effects were more pronounced at the end of sleep deprivation, suggesting possible alerting effects of amisulpride at this dose level. Caffeine significantly antagonized the detrimental effects of sleep deprivation on vigilance (increase in EEG beta waves, speed of reaction, sustained attention and reduction in subjective sedation). In conclusion, the present results demonstrate that 50 mg amisulpride is devoid of detrimental effects on EEG, psychomotor and cognitive performance after sleep deprivation, a situation well-known to amplify such effects if they exist. Moreover, some data suggest possible alerting effects of this low dosage regimen of amisulpride.

Published
1999
Full Text
View/download PDF

21. Cognitive performance in elderly subjects after a single dose of befloxatone, a new reversible selective monoamine oxidase A inhibitor.

Author

Rosenzweig P, Patat A, Zieleniuk I, Cimarosti I, Allain H, and Gandon JM

Subjects
Aged, Aged, 80 and over, Cross-Over Studies, Depression drug therapy, Double-Blind Method, Female, Humans, Male, Reference Values, Amitriptyline pharmacology, Antidepressive Agents, Tricyclic pharmacology, Cognition drug effects, Monoamine Oxidase Inhibitors pharmacology, Oxazoles pharmacology, Psychomotor Performance drug effects
Abstract

Background: Patients with depression often have cognitive and psychomotor performance impairments. Antidepressive treatments can correct these deficits, provided sedative and anticholinergic adverse effects do not add to the preexisting condition, particularly in elderly patients. Newly developed antidepressants therefore should be without deleterious effects on cognitive functions, including memory. Befloxatone is a new antidepressant with a potent, selective, competitive, and reversible inhibitory activity on the A isoform of monoamine oxidase (MAO-A)., Methods: The effects on cognition and psychomotor performance of single oral doses of befloxatone (10 mg) and amitriptyline (50 mg) were compared in a randomized, double-blind, placebo-controlled, three-way crossover design trial in 12 healthy elderly (65 to 85 years) volunteers. The performances of the subjects were evaluated by a comprehensive battery of validated psychometric tests that explored alertness, psychomotor performance, information processing, and memory. Subjective feelings on mood and sleep were rated on visual analog scales. MAO-A inhibition was estimated by multiple titrations of 3,4-dihydrophenylglycol (DHPG) in plasma., Results: Amitriptyline displayed the expected deleterious effects on performance tasks, critical flicker fusion threshold, digit symbol substitution, and body sway, and it deteriorated memory (immediate and delayed free recall of words). In contrast, befloxatone did not impair cognition or psychomotor performance but instead significantly improved the delayed free recall. Amitriptyline adversely affected subjective feelings of alertness and contentedness, but befloxatone permitted sustained alertness and did not alter other subjective feelings or sleep. Concurrently, a single dose of 10 mg befloxatone markedly decreased the DHPG concentration in plasma., Conclusion: Contrary to tricyclic antidepressants, whose deleterious effects are greater in elderly subjects, this study demonstrated the safety of befloxatone on cognition and psychomotor performance in elderly subjects.

Published
1998
Full Text
View/download PDF

22. Antidepressant-like effects of alnespirone (S 20499) in the learned helplessness test in rats.

Author

Mac Sweeney CP, Lesourd M, and Gandon JM

Subjects
Animals, Male, Rats, Rats, Wistar, Anti-Anxiety Agents therapeutic use, Depression drug therapy, Helplessness, Learned, Serotonin Receptor Agonists therapeutic use, Spiro Compounds therapeutic use
Abstract

The effects of the new chroman derivative, alnespirone (S 20499), which is a selective 5-HT1A receptor agonist, were investigated in an animal model of depression, the learned helplessness test. Rats previously submitted to a session of 60 inescapable electric foot shocks (learned helpless controls) exhibited a deficit in escape performance in three subsequent shuttle-box sessions. Alnespirone was administered twice daily via the oral route (2.5, 5, 10, 20 mg kg(-1) day(-1)). It was shown to protect against the elevation in escape failures caused by exposure to the uncontrollable aversive situation at 5 and 10 mg kg(-1) day(-1) p.o. (13+/-2 and 10+/-3 escape failures, respectively, vs. 9+/-2 escape failures in control rats). In addition, alnespirone had a tendency to elevate the number of intertrial crossings during the resting periods, depending on the dose and day on which the avoidance task was performed (15+/-2 intertrial crossings at the dose of 5 mg kg(-1) day(-1), vs. 5+/-2 intertrial crossings for the helpless control rats, on the second day). In comparison, imipramine (64 mg kg(-1) day(-1) p.o.) provided marked protection on all three days of the avoidance task and tended to increase the number of intertrial crossings during the resting periods on the second and the third days. It is concluded that alnespirone exerts antidepressant-like properties in the learned helplessness test in rats, in a manner similar to 8-OH-DPAT (8-hydroxy-2-(di-n-propylamino)tetralin), buspirone and ipsapirone, other 5-HT1A receptor agonists.

Published
1998
Full Text
View/download PDF

23. Absolute bioavailability and electroencephalographic effects of conventional and extended-release formulations of venlafaxine in healthy subjects.

Author

Patat A, Troy S, Burke J, Trocherie S, Danjou P, Le Coz F, Allain H, and Gandon JM

Subjects
Adult, Area Under Curve, Biological Availability, Cross-Over Studies, Cyclohexanols adverse effects, Cyclohexanols blood, Cyclohexanols pharmacology, Delayed-Action Preparations, Double-Blind Method, Humans, Male, Selective Serotonin Reuptake Inhibitors adverse effects, Selective Serotonin Reuptake Inhibitors blood, Selective Serotonin Reuptake Inhibitors pharmacology, Venlafaxine Hydrochloride, Cyclohexanols pharmacokinetics, Electroencephalography drug effects, Selective Serotonin Reuptake Inhibitors pharmacokinetics
Abstract

Venlafaxine is currently marketed for treatment of depressive disorders as a conventional tablet formulation with a twice or three times daily dosage regimen. The absolute bioavailability of the conventional (CF) and extended-release (XR) formulations and their effects on electroencephalograms (EEG) and on a visual analog scale (VAS) for nausea were assessed in a randomized, double-blind, four-way crossover, placebo-controlled study of 16 healthy young men who were given either a single oral dose of 50 mg of CF venlafaxine, 75 mg of XR venlafaxine, or an intravenous dose of 10 mg of venlafaxine, or a placebo at 1-week intervals. The absolute bioavailability of venlafaxine was between 40% and 45% and was similar for both the CF and XR formulations. Venlafaxine produced central effects of a desipramine-like antidepressant. Regardless of formulation tested, the main EEG changes were an increase in fast beta (20-30 Hz) energy, which was more pronounced over the frontotemporal regions and extended within the full beta range (16-40 Hz). Maximum effect was reached at 6 hours for the CF and reached a plateau from 10 to 24 hours for the XR formulation. A dose-proportional increase in central activity, expressed as area under the effect curve (AUE) of the beta band, was observed between the CF (50 mg) and XR (75 mg) formulations. Compared with the CF tablet, the XR formulation also produced a much less intense maximum effect and a decrease of 63% in the AUE of nausea normalized by dose. The XR formulation has the same absolute bioavailability and the same central activity as assessed by EEG, but produced less intensive nausea than CF venlafaxine. The present findings suggest that a once-daily dosage regimen should be sufficient. This was confirmed by several clinical trials in depressive patients.

Published
1998
Full Text
View/download PDF

24. Drugs used in Alzheimer's disease and neuroplasticity.

Author

Allain H, Bentue-Ferrer D, Gandon JM, Le Doze F, and Belliard S

Subjects
Cholinesterase Inhibitors therapeutic use, Clinical Trials as Topic, Humans, Neuronal Plasticity drug effects, Tacrine therapeutic use, Alzheimer Disease drug therapy
Abstract

Drugs indicated for use in Alzheimer's disease (AD) must clinically improve the cognitive symptomatology of the disorder, although nonexclusively. From a neurochemical standpoint, these drugs must oppose the multiple processes recognized as stigmata of AD. In these two ways, so-called AD drugs may be considered substances modifying cerebral plasticity. Long-term evaluation of anticholinesterases and of tacrine, in particular, provides arguments in support of this initially purely biologic, theoretical approach. This concept of neuroplasticity applied to dementia may modify the traditional pharmaceutical drug development programs.

Published
1997
Full Text
View/download PDF

25. Systemic and regional hemodynamic and biological effects of a new kappa-opioid agonist, niravoline, in healthy volunteers.

Author

Bellissant E, Denolle T, Sinnassamy P, Bichet DG, Giudicelli JF, Lecoz F, Gandon JM, and Allain H

Subjects
Adult, Atrial Natriuretic Factor blood, Humans, Kinetics, Male, Osmolar Concentration, Renin blood, Benzeneacetamides, Blood Pressure drug effects, Hemodynamics drug effects, Pyrrolidines pharmacology, Receptors, Opioid, kappa agonists
Abstract

We noninvasively investigated the effects of a single 30-min i.v. infusion of a 2-mg dose of niravoline, a new selective kappa-opioid agonist, on systemic and regional (brachial artery) hemodynamics, on plasma levels of the main hormones regulating the cardiovascular system, on diuresis and on plasma and urinary osmolalities and electrolytes. This was a placebo-controlled, randomized, double-blind, crossover study performed in 12 healthy volunteers. Compared with placebo, niravoline induced a significant, early and potent diuresis, which peaked within 2 hr (urine output increased 2.4-fold) and lasted for 4 hr. Niravoline significantly decreased, between 0 and 2 hr, urine osmolality (-71%) and sodium (-38%) and potassium (-29%) excretion and significantly increased plasma osmolality and natremia, without changing kalemia. Niravoline induced a slight, but significant, increase in blood pressure (+8% at 0.5 hr), which disappeared within 2 hr. Because heart rate, stroke volume and cardiac output were not modified, this effect was due to an increase in total peripheral resistance (+22% at 0.5 hr). Niravoline did not modify brachial artery diameter and flow and corresponding vascular resistance. Niravoline tended to decrease plasma vasopressin levels and urinary excretion and significantly increased plasma levels of norepinephrine (+44% at 0.5 hr), active renin (+22% at 1.25 hr), aldosterone (+52% at 1.25 hr) and atrial natriuretic factor (+20% at 2 hr). We conclude that niravoline induces a potent aquaretic effect associated with antinatriuresis and antikaliuresis. These main effects are accompanied by a stimulation of the sympathetic and reninangiotensin systems and a slight and transient increase in blood pressure.

Published
1996

26. 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
Full Text
View/download PDF

27. Procedural memory and Parkinson's disease.

Author

Allain H, Lieury A, Quemener V, Thomas V, Reymann JM, and Gandon JM

Subjects
Adult, Age Distribution, Aged, Cognition, Humans, Memory, Memory Disorders psychology, Middle Aged, Models, Psychological, Parkinson Disease psychology, Reading, Task Performance and Analysis, Memory Disorders diagnosis, Parkinson Disease diagnosis
Abstract

A detailed analysis of the mnestic deficits associated with Parkinson's disease (PD) contributes to explaining the cognitive disorders and their well documented consequences. This study was designed to show that, in PD declarative as well as procedural memory is severely impaired. Three tests designed to explore this aspect of mnestic functioning were proposed to a group of 16 parkinsonian patients whose motoricity was controlled: inverted reading, braille reading, sound form association. The results obtained, compared with those of young and aged controls, show that PD is associated with marked deficits in both declarative and procedural memory. Declarative memory impairment was similar to that observed in the control population (healthy elderly subjects, age-matched with the PD patients) but more marked in PD subjects. The procedural memory deficit was linked with age and pathology. Procedural memory involves a variety of processing modules dedicated to the type of information (visual, auditive, tactile codes). The deficits observed were more like a loss of automatism than procedural impairment stricto sensu ('knowing how'). It would be worth pursuing research by studying akinesia and motor disorders from the angle of automatic memory impairment.

Published
1995
Full Text
View/download PDF

28. Explicit and procedural memory in Parkinson's disease.

Author

Allain H, Lieury A, Thomas V, Reymann JM, Gandon JM, and Belliard S

Subjects
Adult, Aged, Automatism, Humans, Learning, Middle Aged, Parkinson Disease physiopathology, Memory, Parkinson Disease psychology
Abstract

One of the aims of cognitive psychology is to breakdown complex tasks into their most basic components. The components of explicit (declarative) and implicit (procedural) memory were thus analyzed in undemented, non-depressed Parkinsonian patients under anti-Parkinsonian treatment, and compared with young and elderly healthy subjects. Three series of experiments were conducted in 61 patients in total. Statistically significant results revealed an impairment of explicit memory (verbal recall of words and drawings) with preserved recall of faces, in Parkinsonians. Implicit memory was also deficient, only in association tests (sound-form; arithmetical alphabet) and maze tests. Braille reading tests and Toronto tower tests did not discriminate between Parkinsonians and elderly subjects. Lastly, analyzing learning and automation revealed a dysfunctioning in Parkinsonian patients. All these data indicate a dysregulation of the cortical-sub-cortical systems, not essentially pre-frontal, and not necessarily dopaminergic. Cognitively, it appears that procedural and implicit memories should be dissociated conceptually.

Published
1995
Full Text
View/download PDF

29. Comparative study of the effects of zopiclone (7.5 mg), zolpidem, flunitrazepam and a placebo on nocturnal cognitive performance in healthy subjects, in relation to pharmacokinetics.

Author

Allain H, Patat A, Lieury A, Le Coz F, Janus C, Menard G, and Gandon J

Abstract

The effect of zopiclone (7.5 mg) on attention, vigilance and memory components was evaluated during a nocturnal period in comparison to a placebo, to zolpidem (10 mg) and to flunitrazepam (1 mg) in a double blind, randomized study, after administration of a single dose in 16 young healthy volunteers. It appears that there is a clear effect on attention and vigilance; this effect is apparent during the kinetic phase of the absorption of the medication. The effect on memory is transient and is absent four hours after the ingestion of the drug. The objective results are not strictly consistent with the chronology of the subjective parameters (Leeds scale - Visual Analogue Scale). The three hypnotics under comparison do not fundamentally differ except in their kinetic/pharmacodynamic effect relationship. One important fact, taking the parameters as a whole, is that there is no objective "residual" effect.

Published
1995
Full Text
View/download PDF

30. Monoamine oxidase inhibitors, cognitive functions and neurodegenerative diseases.

Author

Delumeau JC, Bentué-Ferrer D, Gandon JM, Amrein R, Belliard S, and Allain H

Subjects
Alzheimer Disease psychology, Animals, Brain metabolism, Humans, Monoamine Oxidase metabolism, Parkinson Disease psychology, Alzheimer Disease drug therapy, Cognition drug effects, Monoamine Oxidase Inhibitors therapeutic use, Parkinson Disease drug therapy
Abstract

Recent data obtained in animals and in humans suggest that both MAO-A and MAO-B inhibitors present cognitive enhancing properties of possible interest in the treatment of cognitive disorders. In addition, the rational for using selegiline as a neuroprotector in Parkinson's disease may also be applicable in Alzheimer's disease in which a dramatic increase in the MAO-B activity has been reported. It seems then worthwhile to investigate the neuroprotective effect of MAOIs in humans and to assess, furthermore, the real therapeutical benefit of their cognitive enhancing properties.

Published
1994
Full Text
View/download PDF

31. Effect of two doses of ginkgo biloba extract (EGb 761) on the dual-coding test in elderly subjects.

Author

Allain H, Raoul P, Lieury A, LeCoz F, Gandon JM, and d'Arbigny P

Subjects
Aged, Aged, 80 and over, Dose-Response Relationship, Drug, Double-Blind Method, Female, Ginkgo biloba, Humans, Male, Mental Recall drug effects, Middle Aged, Reaction Time drug effects, Memory Disorders drug therapy, Plant Extracts therapeutic use
Abstract

The subjects of this double-blind study were 18 elderly men and women (mean age, 69.3 years) with slight age-related memory impairment. In a crossover-study design, each subject received placebo or an extract of Ginkgo biloba (EGb 761) (320 mg or 600 mg) 1 hour before performing a dual-coding test that measures the speed of information processing; the test consists of several coding series of drawings and words presented at decreasing times of 1920, 960, 480, 240, and 120 ms. The dual-coding phenomenon (a break point between coding verbal material and images) was demonstrated in all the tests. After placebo, the break point was observed at 960 ms and dual coding beginning at 1920 ms. After each dose of the ginkgo extract, the break point (at 480 ms) and dual coding (at 960 ms) were significantly shifted toward a shorter presentation time, indicating an improvement in the speed of information processing.

Published
1993

32. Comparison of three regimens of Parlodel-SRO in levodopa-treated parkinsonians: a randomized double-blind crossover study.

Author

Allain H, Le Coz F, Goulley F, Brunet-Bourgin F, Loria Y, Bentue-Ferrer D, Decombe R, Reymann JM, Chaumet-Riffaud P, and Gandon JM

Subjects
Adult, Aged, Aged, 80 and over, Behavior drug effects, Bromocriptine adverse effects, Bromocriptine therapeutic use, Delayed-Action Preparations, Double-Blind Method, Female, Humans, Male, Middle Aged, Parkinson Disease metabolism, Parkinson Disease psychology, Bromocriptine administration & dosage, Levodopa therapeutic use, Parkinson Disease drug therapy
Abstract

Parlodel-SRO is a newly developed slow-release formulation of bromocriptine, which prevents initial plasma peak--a known source of adverse events--and extends the half-life of the compound, an interesting feature for the management of motor symptoms in Parkinsonians. This study was designed to determine the best daily administration schedule for 30 mg Parlodel-SRO in 18 parkinsonians previously treated with levodopa and standard Bromocriptine (Br). The 30 mg dose was replaced from one day to the next, in a randomized, double-blind latin square design trial. Three consecutive 7-day courses were implemented, during which a total daily dose of 30 mg P-SRO was administered in one dose, two intakes (b.i.d.) and three intakes, (t.i.d.) respectively. The b.i.d. schedule produced the best improvement in UPDRS scores, especially as to postural stability, walking, bradykinesia; it also provided greater pharmacological stability throughout the assessment day. Adverse event analysis was not in favor of a single daily dose. It appeared that P-SRO administered in two 15 mg intakes (morning and evening) produces the best benefit-risk ratio in Parkinsonians who were already being treated with levodopa.

Published
1991

Catalog

Books, media, physical & digital resources
See catalog results