Dreier J P, Zhang C L, Heinemann U
Department of Neurology, Charité, Humboldt-University, Berlin, Germany.
Acta Neurol Scand. 1998 Sep;98(3):154-60. doi: 10.1111/j.1600-0404.1998.tb07286.x.
It was shown previously that low-Mg2+-induced epileptiform activity in rat entorhinal cortex slices changes with time from a pattern of serial seizure-like events (SLEs) to a state of continuously recurring epileptiform activity. Valproic acid blocked the early SLEs but not the late activity. It was proposed that the late activity is a model for pharmacoresistant status epilepticus since it was also refractory to phenytoin, carbamazepine, phenobarbital, and midazolam. In the present study, it is demonstrated that phenytoin (50 microM, n=6), phenobarbital (150 microM, n=7), and midazolam (50 microM, n=5) were able to block the early SLEs but not the late activity at the same concentrations. Carbamazepine (50 microM) reduced the duration of the SLEs from 21 +/-5 s to 4+/-3 s (P<0.01), the interictal interval from 123+/-27 s to 27+/-19 s (P<0.01), the SLE-associated rise of [K+]o from 7.7+/-0.5 mM to 5.7+/-0.8 mM (n=4, P<0.05), and the spread of the SLE between entorhinal cortex and neocortex from 4.0+/-0.6 s to 0.8+/-0.1 s (n=4, P<0.05). Lower concentrations of phenytoin (5 and 10 microM, n=5), carbamazepine (10 microM, n =6), and phenobarbital (50 microM, n = 4) had no effect. In conclusion, the hypothesis is supported that low-Mg2+-induced epileptiform activity in rat entorhinal cortex is an in vitro model for the transition from pharmacosensitive to pharmacoresistant status epilepticus.
先前的研究表明,低镁离子诱导的大鼠内嗅皮质切片癫痫样活动随时间从一系列癫痫样事件(SLEs)模式转变为持续反复出现的癫痫样活动状态。丙戊酸可阻断早期的SLEs,但对后期活动无效。有人提出,后期活动是药物难治性癫痫持续状态的模型,因为它对苯妥英钠、卡马西平、苯巴比妥和咪达唑仑也具有耐药性。在本研究中,结果表明,苯妥英钠(50μM,n = 6)、苯巴比妥(150μM,n = 7)和咪达唑仑(50μM,n = 5)在相同浓度下能够阻断早期的SLEs,但对后期活动无效。卡马西平(50μM)可将SLEs的持续时间从21±5秒缩短至4±3秒(P<0.01),发作间期从123±27秒缩短至27±19秒(P<0.01),SLEs相关的细胞外钾离子浓度升高从7.7±0.5 mM降至5.7±0.8 mM(n = 4,P<0.05),SLEs在内嗅皮质和新皮质之间的传播时间从4.0±0.6秒缩短至0.8±0.1秒(n = 4,P<0.05)。较低浓度的苯妥英钠(5和10μM,n = 5)、卡马西平(10μM,n = 6)和苯巴比妥(50μM,n = 4)则无此作用。总之,低镁离子诱导的大鼠内嗅皮质癫痫样活动是从药物敏感型癫痫持续状态转变为药物难治型癫痫持续状态的体外模型这一假说得到了支持。
