Publication: Genetik Absans Epilepsili Wag Rij Sıçanlarda Genel Anasteziklerin Etkisi
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Amaç: Deneysel çalışmalarda kullanılan basit ve güvenli bir anestezi yöntemini belirlemek amacıyla genetik absans epilepsili (WAG\Rij) sıçanlarda ketamin, ketamin/ksilazin, üretan, kloral hidrat, pentobarbital, izofluran, deksmedetomidin ve deksmedetomidin/ketaminin epileptiform aktivite üzerine olan etkisi araştırıldı. Materyal ve Metot: Bu çalışmada 170-190 g ağırlığında 63 erkek Albino WAG/Rij sıçan kullanıldı. Elektrofizyolojik kayıt almak için sıçanların kafatasına tripolar elektrotlar yerleştirildi. Deneyin ilk iki saatinde ECoG aktiviteleri her bir hayvan için kontrol olarak kaydedildi ve ardından anestezik maddeler uygulandı. İnhalasyon yoluyla uygulanan izofluran dışındaki tüm anestezik maddeler intraperitoneal olarak uygulandı. Elektrofizyolojik aktivite PowerLab very kazanım sistemiyle online olarak kaydedildive daha sonar offline olarak analiz edildi. Bulgular: Ketamin (90 mg/kg), ketamin/ksilazin (90/10 mg/kg), üretan (1,25 g/kg), kloral hidrat (175 mg/kg), pentobarbital (50-90 mg/kg), izofluran (indüksiyon %5, muhafaza %3-4), deksmedetomidin (0,5-1 mg/kg) ve deksmedetomidin/ketamin (50/90 mg/kg) uygulamaları, toplam DDD sayısını, toplam spike sayısını, ve SWD süresini önemli ölçüde azalttı (p<0,05). Pentobarbital (50-90 mg/kg), izofluran (%5 indüksiyon, %3-4 muhafaza), deksmedetomidin (0,5-1 mg/kg) ve deksmedetomidin/ketamin (50/90 mg/kg) gruplarında ortalama SWD süresi değişmedi (p>0,05). Deksmedetomidin (0,5-1 mg/kg) ve deksmedetomidin/ketamin (50/90 mg/kg) grupları (50/90 mg/kg) dışındaki (p>0,05) tüm gruplarda ilk 20 dakikada toplam DDD sayısında önemli bir azalma görüldü (P<0,001). Sonuç: Mevcut veriler, deksmedetomidin ve deksmedetomidin/ketamin grubu dışında kullanılan tüm anestetik maddelerin, uygulamadan hemen sonra epileptiform aktiviteyi önemli ölçüde azalttığını ortaya çıkardı, bu nedenle, anesteziklerle birlikte yapılacak elektrofizyolojik çalışmalarda deksmedetomidin ve deksmedetomidin/ketamin kullanımını öneriyoruz. Anahtar Sözcükler: Anestezi, Deksmedetomidin, Epilepsy, Ketaminin, WAG\Rij.
Aim: To establish a simple and safe method of anesthesia that used in experimental studies. so we examined the effect of ketamine, ketamine/xylazine, urethane, chloral hydrate, pentobarbital, isoflurane, dexmedetomidine, and dexmedetomidine/ketamine on epileptiform activity in genetic absence epilepsy (WAG\Rij) rats. Material and Method: In this study, 63 male of Albino WAG/Rij rats weighing (170-190 g) were used. Tripolar electrodes were inserted into the skull of the rats. In the first two hours of the experiment, ECoG activities were recorded as a control for each animal, then the anesthetic substances were administered. All the anesthetic substances were administered intraperitoneally except isoflurane which administered by inhalation. Electrophysiological activity was recorded online by PowerLab data acquisition system and then offline analyzed. Results: The administration of ketamine (90 mg/kg), ketamine/xylazine (90/10 mg/kg), urethane (1.25 g/kg), chloral hydrate (175 mg/kg), pentobarbital (50-90 mg/kg), isoflurane (induction 5%, maintaining 3-4%), dexmedetomidine (0.5-1 mg/kg), and dexmedetomidine/ketamine (50/90 mg/kg), significantly decreased the total number of SWD, the total number of spikes, and the SWD duration (p<0,05). The mean duration of SWD was not affected in pentobarbital (50-90 mg/kg), isoflurane (induction 5%, maintaining 3-4%), dexmedetomidine (0.5-1 mg/kg), and Dexmedetomidine/ketamine (50/90 mg/kg) groups (p>0.05). Time scale showed a significant decrease in the total number of SWD in the first 20 minutes (P<0.001) for all groups except dexmedetomidine (0.5-1 mg/kg), and dexmedetomidine/ketamine (50/90 mg/kg) groups (p>0.05). Conclusion: The current data revealed that all the anesthetics substances which we used were significantly reduced the epileptiform activity immediately after the administration, except dexmedetomidine and dexmedetomidine/ketamine group, so we recommend to use dexmedetomidine and Dexmedetomidine/ketamine in electrophysiological studies accompanied with anesthetics. Keywords: Anesthesia, Dexmedetomidine, Epilepsy, Ketamine, WAG\Rij, Rat.
Aim: To establish a simple and safe method of anesthesia that used in experimental studies. so we examined the effect of ketamine, ketamine/xylazine, urethane, chloral hydrate, pentobarbital, isoflurane, dexmedetomidine, and dexmedetomidine/ketamine on epileptiform activity in genetic absence epilepsy (WAG\Rij) rats. Material and Method: In this study, 63 male of Albino WAG/Rij rats weighing (170-190 g) were used. Tripolar electrodes were inserted into the skull of the rats. In the first two hours of the experiment, ECoG activities were recorded as a control for each animal, then the anesthetic substances were administered. All the anesthetic substances were administered intraperitoneally except isoflurane which administered by inhalation. Electrophysiological activity was recorded online by PowerLab data acquisition system and then offline analyzed. Results: The administration of ketamine (90 mg/kg), ketamine/xylazine (90/10 mg/kg), urethane (1.25 g/kg), chloral hydrate (175 mg/kg), pentobarbital (50-90 mg/kg), isoflurane (induction 5%, maintaining 3-4%), dexmedetomidine (0.5-1 mg/kg), and dexmedetomidine/ketamine (50/90 mg/kg), significantly decreased the total number of SWD, the total number of spikes, and the SWD duration (p<0,05). The mean duration of SWD was not affected in pentobarbital (50-90 mg/kg), isoflurane (induction 5%, maintaining 3-4%), dexmedetomidine (0.5-1 mg/kg), and Dexmedetomidine/ketamine (50/90 mg/kg) groups (p>0.05). Time scale showed a significant decrease in the total number of SWD in the first 20 minutes (P<0.001) for all groups except dexmedetomidine (0.5-1 mg/kg), and dexmedetomidine/ketamine (50/90 mg/kg) groups (p>0.05). Conclusion: The current data revealed that all the anesthetics substances which we used were significantly reduced the epileptiform activity immediately after the administration, except dexmedetomidine and dexmedetomidine/ketamine group, so we recommend to use dexmedetomidine and Dexmedetomidine/ketamine in electrophysiological studies accompanied with anesthetics. Keywords: Anesthesia, Dexmedetomidine, Epilepsy, Ketamine, WAG\Rij, Rat.
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