首页> 外文期刊>Epilepsy research >Pilocarpine-induced epileptogenesis in the rat: Impact of initial duration of status epilepticus on electrophysiological and neuropathological alterations.
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Pilocarpine-induced epileptogenesis in the rat: Impact of initial duration of status epilepticus on electrophysiological and neuropathological alterations.

机译:毛果芸香碱诱导的大鼠癫痫发生:癫痫持续状态的初始持续时间对电生理和神经病理改变的影响。

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This study characterized the electrophysiological and neuropathological changes in rat brains caused by pilocarpine (PILO)-induced status epilepticus (SE) of different duration. SE induced by PILO (375 mg/kg, i.p. adm.) were terminated with a bolus dose of diazepam (10 mg/kg, i.v. adm.) injected 7.5, 15, 30, 60 or 120 min after initiation of the secondary generalization of the SE. Three weeks later, the gain in body weight was significantly reduced in the rats exposed to PILO-induced SE lasting 30 min or more, when compared to controls. Spontaneous seizures were not detected in rats with PILO-induced SE of 7.5 min duration whereas 50 and 25% of the rats exposed to seizure durations of 30 and 120 min expressed motor seizures. Significant alterations reflecting hyperexcitability (increased number of population spikes (PSs)) and reduced paired-pulse inhibition were observed in recordings of hippocampal field potentials from rats with PILO-induced SE of at least 30 min duration. This was substantiated by brain lesions (necrosis in olfactory cortex, hippocampus, amygdala and thalamus) in all rats manifesting a SE of at least 30 min duration. Thus, the results of the present study demonstrate that rats exposed to PILO-induced SE of at least 30 min duration manifest an epileptogenic process, revealed 3 weeks later by several parameters. Among these, hippocampal field potentials appear to represent the most sensitive marker, potentially useful for pharmacological evaluation of drugs with putative antiepileptogenic properties.
机译:这项研究的特点是毛果芸香碱(PILO)引起的持续状态癫痫持续状态(SE)引起的大鼠脑电生理和神经病理学变化。 PILO(375 mg / kg,ip adm。)诱导的SE终止于大剂量的地西epa(10 mg / kg,iv adm。)的大剂量二次注射后7.5、15、30、60或120分钟注射SE。三周后,与对照组相比,暴露于PILO诱导的SE持续30分钟或更长时间的大鼠的体重增加显着降低。在PILO诱导的SE持续时间为7.5分钟的大鼠中未检测到自发性癫痫发作,而在发作持续时间为30和120分钟的大鼠中有50%和25%的患者表现出运动性癫痫发作。在PILO诱导的SE持续至少30分钟的大鼠的海马场电位记录中观察到了反映过度兴奋性的显着变化(种群尖峰(PSs)的数量增加)和成对脉冲抑制的降低。在所有表现出SE持续时间至少为30分钟的大鼠中,脑部病变(嗅觉皮层,海马,杏仁核和丘脑坏死)证实了这一点。因此,本研究的结果表明,暴露于PILO诱导的SE至少持续30分钟的大鼠表现出了致癫痫的过程,并在3周后通过多个参数显示出来。其中,海马场电位似乎代表了最敏感的标志物,潜在地可用于具有推定的抗癫痫药特性的药物的药理评估。

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