首页> 外文期刊>Journal of Pharmacological and Toxicological Methods >EEG in the FEAB model: measurement of electroencephalographical burst suppression and seizure liability in safety pharmacology.
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EEG in the FEAB model: measurement of electroencephalographical burst suppression and seizure liability in safety pharmacology.

机译:FEAB模型中的EEG:安全性药理学中脑电图猝发抑制和癫痫发作易感性的测量。

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INTRODUCTION: The purpose of this study was to explore the integration of electroencephalographical (EEG) measurements into the fentanyl/etomidate-anaesthetised Beagle (FEAB) model in order to detect burst suppression and/or seizure development caused by compounds, prior to new molecular entity (NME) declaration. Detecting such unfavourable side effects prevents their being found in conscious animals at a later stage of safety evaluation. In addition, this has the advantage of performing safety studies on the three vital organ systems (cardiovascular system, respiratory system and central nervous system) within one and the same animal model. METHODS: Dogs were anaesthetized and instrumented according to the FEAB model requirements, and in addition three needle electrodes were placed on the cranium and a one lead EEG signal was measured. The raw signal was analysed by the Narcotrend(R) (MonitorTechnik, Bad Bramstedt, Germany) for depth of anaesthesia registration, visually analysed for burst suppression ratio calculation after different anaesthetics (pentobarbital and etomidate), and spiking and seizure activity were quantified after intravenous administration of different proconvulsant agents: pentylenetetrazole (PTZ), bicuculline (BCC), bupropion (BUP) and pilocarpine (PIL). RESULTS: High doses of pentobarbital (60 mg/kg over 10 min) and etomidate (6 mg/kg over 10 min) induced dose-dependent burst suppression of 98 +/- 2% and 61 +/- 16%, respectively. Infusions of PTZ (1.5mg/kg/min), BCC (0.0625 mg/kg/min), BUP (0.5mg/kg/min) and PIL (5mg/kg/min) induced dose-dependent spiking and seizures: the thresholds were 34 +/- 2, 0.15 +/- 0.03, 10.0 +/- 1 and 144 +/- 9 mg/kg, respectively. In PTZ-treated dogs, spiking and seizures could be abolished with diazepam (2mg/kg i.v.) or with propofol (4 mg/kg i.v.). DISCUSSION: The present study showed that a one lead EEG can be used reliably in the FEAB model to estimate the depth of anaesthesia, and to detect burst suppression and seizure risk in safety pharmacology studies.
机译:简介:这项研究的目的是探索将脑电图(EEG)测量值整合到芬太尼/依托咪酯麻醉的Beagle(FEAB)模型中,以便在新的分子实体之前检测化合物引起的猝发抑制和/或癫痫发作发展(NME)声明。检测到这种不利的副作用会阻止在安全评估的后期阶段在有意识的动物中发现它们。此外,这具有在一个动物模型中对三个重要器官系统(心血管系统,呼吸系统和中枢神经系统)进行安全性研究的优势。方法:根据FEAB模型的要求对狗进行麻醉和检测,并在颅骨上放置三个针状电极,并测量一个铅脑电信号。由Narcotrend(MonitorTechnik,Bad Bramstedt,德国)分析原始信号的麻醉深度,目测分析不同麻醉药(戊巴比妥和依托咪酯)后的猝发抑制率计算,并在静脉注射后定量加标和癫痫发作活动服用不同的惊厥药:戊四氮(PTZ),双瓜氨酸(BCC),安非他酮(BUP)和毛果芸香碱(PIL)。结果:高剂量的戊巴比妥(10分钟内60 mg / kg)和依托咪酯(10分钟内6 mg / kg)分别引起98 +/- 2%和61 +/- 16%的剂量依赖性猝发抑制。输注PTZ(1.5mg / kg / min),BCC(0.0625 mg / kg / min),BUP(0.5mg / kg / min)和PIL(5mg / kg / min)会引起剂量依赖性的发作和癫痫发作:阈值分别为34 +/- 2、0.15 +/- 0.03、10.0 +/- 1和144 +/- 9 mg / kg。在用PTZ治疗的狗中,地西epa(2mg / kg静脉内)或异丙酚(4mg / kg静脉内)可以消除尖峰和癫痫发作。讨论:本研究表明,一种先导脑电图可在FEAB模型中可靠地用于估计麻醉深度,并在安全药理学研究中检测猝发抑制和癫痫发作风险。

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