Historique
Article de Périodique
Changes in seizure threshold and aggression during chronic treatment with three anticonvulsants and on drug withdrawal (1990)
(Modifications du seuil d'apparition des convulsions et de l'agressivité au cours d'un traitement chronique par trois anti convulsivants et au cours du sevrage)
Auteur(s) :
FILE, S. E. ;
WILKS, L. J.
Année
1990
Page(s) :
237-242
Langue(s) :
Anglais
Refs biblio. :
22
Domaine :
Drogues illicites / Illicit drugs
Discipline :
PRO (Produits, mode d'action, méthode de dépistage / Substances, action mode, screening methods)
Résumé :
FRANÇAIS :
Etude portant sur la durée des effets anticonvulsivants et les manifestations de sevrage de 3 molécules (phenobarbital, phenitoine et lorazepam) chez la souris mâle dont les convulsions sont induites par le pentylenetetrazole. Les effets anticonvulsivants du phenobarbital persistent pendant 3 semaines de traitement. Les effets sur le comportement dépendaient du moment de la mesure, les effets sur la socialisation dépendaient de la dose utilisée. Le sevrage a entrainé une diminution de la socialisation pendant 48 heures. Pour la phenitoine, l'action anticonvulsivante apparaissait au bout de 7 jours et persistait 21 jours. Les diminutions observées de la socialisation et de l'agressivité s'épuisaient au bout de 7 et 14 jours. Le sevrage n'a pas eu d'effet comportemental. Le lorazepam a diminué le seuil des crises pendant 14 jours seulement sans effet au sevrage. Pour les 3 molécules les seuils de crise ont été diminués pendant 48 heures au moins.
ENGLISH:
Sodium phenobarbitone (20 and 70 mg/kg) had a significant anticonvulsant action against pentylenetetrazole-induced seizures, which persisted for 21 days of treatment. On drug withdrawal there was a significant decrease in seizure threshold below control level 24–48 h after the last dose of 70 mg/kg. Phenytoin (40 mg/kg) had a significant anticonvulsant action after 7 days of treatment and this persisted for 21 days of treatment. On drug withdrawal there was a significant decrease in seizure threshold 48 h after the last dose. Lorazepam (0.1 mg/kg) had a significant anticonvulsant action, but the group tested after 21 days of treatment did not differ from the controls, indicating that tolerance had developed to this effect; on drug withdrawal there was a decrease in seizure threshold from 24 to 72 h. The only drug to increase aggressive behaviour was sodium phenobarbitone (70 mg/kg); this reached significance after 14 and 21 days of treatment and occurred 8 h after drug administration; 0.5 h after drug administration phenobarbitone (70 mg/kg) abolished aggressive behaviour. After 7 days of treatment phenobarbitone (70 mg/kg) increased social behaviour 0.5 h after administration and this was still increased after 21 days of treatment. On drug withdrawal, there were no changes in aggressive behaviour, but there were significant decreases in social behaviour 24 and 48 h after phenobarbitone (70 mg/kg) withdrawal and 24, 48 and 72 h after lorazepam (0.1 mg/kg) withdrawal.
Etude portant sur la durée des effets anticonvulsivants et les manifestations de sevrage de 3 molécules (phenobarbital, phenitoine et lorazepam) chez la souris mâle dont les convulsions sont induites par le pentylenetetrazole. Les effets anticonvulsivants du phenobarbital persistent pendant 3 semaines de traitement. Les effets sur le comportement dépendaient du moment de la mesure, les effets sur la socialisation dépendaient de la dose utilisée. Le sevrage a entrainé une diminution de la socialisation pendant 48 heures. Pour la phenitoine, l'action anticonvulsivante apparaissait au bout de 7 jours et persistait 21 jours. Les diminutions observées de la socialisation et de l'agressivité s'épuisaient au bout de 7 et 14 jours. Le sevrage n'a pas eu d'effet comportemental. Le lorazepam a diminué le seuil des crises pendant 14 jours seulement sans effet au sevrage. Pour les 3 molécules les seuils de crise ont été diminués pendant 48 heures au moins.
ENGLISH:
Sodium phenobarbitone (20 and 70 mg/kg) had a significant anticonvulsant action against pentylenetetrazole-induced seizures, which persisted for 21 days of treatment. On drug withdrawal there was a significant decrease in seizure threshold below control level 24–48 h after the last dose of 70 mg/kg. Phenytoin (40 mg/kg) had a significant anticonvulsant action after 7 days of treatment and this persisted for 21 days of treatment. On drug withdrawal there was a significant decrease in seizure threshold 48 h after the last dose. Lorazepam (0.1 mg/kg) had a significant anticonvulsant action, but the group tested after 21 days of treatment did not differ from the controls, indicating that tolerance had developed to this effect; on drug withdrawal there was a decrease in seizure threshold from 24 to 72 h. The only drug to increase aggressive behaviour was sodium phenobarbitone (70 mg/kg); this reached significance after 14 and 21 days of treatment and occurred 8 h after drug administration; 0.5 h after drug administration phenobarbitone (70 mg/kg) abolished aggressive behaviour. After 7 days of treatment phenobarbitone (70 mg/kg) increased social behaviour 0.5 h after administration and this was still increased after 21 days of treatment. On drug withdrawal, there were no changes in aggressive behaviour, but there were significant decreases in social behaviour 24 and 48 h after phenobarbitone (70 mg/kg) withdrawal and 24, 48 and 72 h after lorazepam (0.1 mg/kg) withdrawal.
Affiliation :
UMSD Div. Pharmacol., Psychopharmacol. Res. Unit, Univ. London, Guy's Hosp., London SE1 9RT
Royaume-Uni. United Kingdom.
Royaume-Uni. United Kingdom.