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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Reduction of pentylenetetrazole-induced seizure activity in awake rats by seizure-triggered trigeminal nerve stimulation.
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Reduction of pentylenetetrazole-induced seizure activity in awake rats by seizure-triggered trigeminal nerve stimulation.

机译:通过癫痫发作触发的三叉神经刺激,降低戊烯四唑诱导的清醒大鼠癫痫发作的活性。

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摘要

Stimulation of the vagus nerve has become an effective method for desynchronizing the highly coherent neural activity typically associated with epileptic seizures. This technique has been used in several animal models of seizures as well as in humans suffering from epilepsy. However, application of this technique has been limited to unilateral stimulation of the vagus nerve, typically delivered according to a fixed duty cycle, independently of whether ongoing seizure activity is present. Here, we report that stimulation of another cranial nerve, the trigeminal nerve, can also cause cortical and thalamic desynchronization, resulting in a reduction of seizure activity in awake rats. Furthermore, we demonstrate that providing this stimulation only when seizure activity begins results in more effective and safer seizure reduction per second of stimulation than with previous methods. Seizure activity induced by intraperitoneal injection of pentylenetetrazole was recorded from microwire electrodes in the thalamus and cortex of awake rats while the infraorbital branch of the trigeminal nerve was stimulated via a chronically implanted nerve cuff electrode. Continuous unilateral stimulation of the trigeminal nerve reduced electrographic seizure activity by up to 78%, and bilateral trigeminal stimulation was even more effective. Using a device that automatically detects seizure activity in real time on the basis of multichannel field potential signals, we demonstrated that seizure-triggered stimulation was more effective than the stimulation protocol involving a fixed duty cycle, in terms of the percent seizure reduction per second of stimulation. In contrast to vagus nerve stimulation studies, no substantial cardiovascular side effects were observed by unilateral or bilateral stimulation of the trigeminal nerve. These findings suggest that trigeminal nerve stimulation is safe in awake rats and should be evaluated as a therapy for human seizures. Furthermore, the results demonstrate that seizure-triggered trigeminal nerve stimulation is technically feasible and could be further developed, in conjunction with real-time seizure-predicting paradigms, to prevent seizures and reduce exposure to nerve stimulation.
机译:迷走神经的刺激已成为使与癫痫发作通常相关的高度连贯的神经活动失去同步的有效方法。这项技术已用于癫痫发作的几种动物模型以及患有癫痫的人类中。但是,该技术的应用仅限于对迷走神经的单侧刺激,通常根据固定的工作周期进行传递,而与是否存在持续的癫痫发作活动无关。在这里,我们报告说,另一头颅神经,即三叉神经的刺激,也可能引起皮层和丘脑失步,导致清醒大鼠的癫痫发作活动减少。此外,我们证明,仅当癫痫发作开始时才提供这种刺激,比以前的方法每秒更有效,更安全地减少癫痫发作。从清醒大鼠的丘脑和皮层中的微丝电极记录了腹膜内注射戊四氮诱导的癫痫发作活动,同时通过长期植入的神经袖带电极刺激三叉神经的眶下分支。连续单方面刺激三叉神经可将电图癫痫发作的活动降低多达78%,而双侧三叉神经刺激则更为有效。使用基于多通道场电势信号自动实时实时检测癫痫发作活动的设备,我们证明了癫痫发作刺激比涉及固定占空比的刺激方案更有效,即每秒减少癫痫发作的百分比刺激。与迷走神经刺激研究相反,单侧或双侧三叉神经刺激未观察到明显的心血管副作用。这些发现表明,三叉神经刺激在清醒的大鼠中是安全的,应评估为治疗癫痫的一种疗法。此外,结果表明,癫痫发作触发的三叉神经刺激在技术上是可行的,并且可以结合实时的癫痫发作预测范例进一步发展,以预防癫痫发作并减少对神经刺激的暴露。

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