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Phase-amplitude coupling and epileptogenesis in an animal model of mesial temporal lobe epilepsy

机译:间隙颞叶癫痫动物模型中的相位振缩耦合和癫痫凋亡

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Polyrhythmic coupling of oscillatory components in electrophysiological signals results from the interactions between neuronal sub-populations within and between cell assemblies. Since the mechanisms underlying epileptic disorders should affect such interactions, abnormal level of cross-frequency coupling is expected to provide a signal marker of epileptogenesis. We measured phase-amplitude coupling (PAC), a form of cross-frequency coupling between neural oscillations, in a rodent model of mesial temporal lobe epilepsy. Sprague-Dawley rats (n = 4, 250-300 g) were injected with pilocarpine (380 mg/kg, i.p) to induce a status epilepticus (SE) that was stopped after 1 h with diazepam (5 mg/kg, s.c.) and ketamine (50 mg/kg, s.c.). Control animals (n = 6) did not receive any injection or treatment. Three days after SE, all animals were implanted with bipolar electrodes in the hippocampal CA3 subfield, entorhinal cortex, dentate gyrus and subiculum. Continuous video/EEG recordings were performed 24/7 at a sampling rate of 2 kHz, over 15 consecutive days. Pilocarpine-treated animals showed interictal spikes (5.25 (+/- 2.5) per minute) and seizures (n = 32) that appeared 7 (+/- 0.8) days after SE. We found that CA3 was the seizure onset zone in most epileptic animals, with stronger ongoing PAC coupling between seizures than in controls (Kruskal-Wallis test: chi(2) (1,36) = 46.3, Bonferroni corrected, p 0.001). Strong PAC in CA3 occurred between the phase of slow-wave oscillations ( 1 Hz) and the amplitude of faster rhythms (50-180 Hz), with the strongest bouts of high-frequency activity occurring preferentially on the ascending phase of the slow wave. We also identified that cross-frequency coupling in CA3 (rho = 0.44, p 0.001) and subiculum (rho = 0.41, p 0.001) was positively correlated with the daily number of seizures. Overall, our study demonstrates that cross-frequency coupling may represent a signal marker in epilepsy and suggests that this methodology could be transferred to clinical scalp MEG and EEG recordings.
机译:电生理信号中的振荡组分的多性半音偶联是由细胞组件内和细胞组件内和之间的神经元亚群之间的相互作用。由于癫痫病症的机制应该影响这种相互作用,因此预期横频耦合的异常水平提供癫痫发生的信号标志物。我们测量相位振荡(PAC),神经振荡之间的横频耦合的形式,在薄膜颞叶癫痫的啮齿动物模型中。 Sprague-Dawley大鼠(n = 4,250-300g)注射含柳甘油(380mg / kg,IP),以诱导1小时后停止的状态癫痫(SE)(5 mg / kg,sc)和氯胺酮(50 mg / kg,sc)。对照动物(n = 6)未接受任何注射或治疗。 SE后三天,所有动物植入海马CA3子场中的双极电极,Entorlinal皮质,齿状回形图和次粒子。连续视频/ EEG记录以2 kHz的采样率为24/7,连续15天。汲昆宾治疗的动物显示液晶钉(每分钟5.25(+/- 2.5))和癫痫发作(n = 32),其在SE之后出现7(+/- 0.8)天。我们发现CA3是大多数癫痫动物中的癫痫发作区域,癫痫发作均具有较强的持续的PAC偶联而不是对照组(Kruskal-Wallis试验:Chi(2)(1,36)= 46.3,Bonferroni校正,P <0.001) 。 CA3中的强PAC发生在慢波振荡(& 1 Hz)的阶段和更快的节奏(50-180 Hz)的幅度之间发生,最优先发生最强的高频活动对缓慢的升序发生海浪。我们还鉴定了Ca3中的横频耦合(rho = 0.44,p <0.001)和亚奇(rho = 0.41,p <0.001)与每日癫痫发作呈正相关。总体而言,我们的研究表明,交叉频率耦合可以代表癫痫中的信号标记,并表明该方法可以转移到临床头皮MEG和EEG记录。

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