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首页> 外文期刊>Brain research >Acute seizure-suppressing effect of vagus nerve stimulation in the amygdala kindled rat.
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Acute seizure-suppressing effect of vagus nerve stimulation in the amygdala kindled rat.

机译:迷走神经刺激对杏仁核点燃大鼠的急性癫痫发作抑制作用。

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PURPOSE: Vagus nerve stimulation (VNS) is a moderately effective anti-epileptic treatment. Clinically relevant animal models that are suitable to study the mechanism of action of VNS are not available. The aim of the current study was to develop a clinically relevant animal model for VNS-treated epilepsy that can be used to study the mechanism of action of VNS. METHODS: The anticonvulsive effect of VNS was studied in fully kindled rats by measuring behavioral and electrophysiological parameters. Afferent vagus nerve activation was confirmed by quantifying nNOS immunoreactive cells in the nucleus of the solitary tract (NTS). RESULTS: VNS rats had more nNOS immunoreactive cells/mm(2) in the NTS than shams. VNS induced a >25% decrease in stage 5 duration (S5D) in 32% of rats. Prior to VNS this type of responders suffered from seizures with a longer total seizure duration (TSD) than non-responders. In 21% of rats VNS resulted in a >25% decrease in TSD. This type of responders had a shorter TSD prior to VNS than non-responders. In 29% of rats VNS resulted in >200% increase in stage 5 latency (S5L). This type of responders had higher kindling rates than non-responders. CONCLUSION: The VNS-treated kindled rat is a clinically relevant animal model because it is a chronic epilepsy model that responds to VNS with effects that are comparable to the effects of VNS in epilepsy patients. In addition, this study demonstrates that VNS-treated kindled rats can be used to study the mode of action of VNS using immunohistochemical techniques.
机译:目的:迷走神经刺激(VNS)是一种中度有效的抗癫痫药。没有适合研究VNS作用机制的临床相关动物模型。本研究的目的是为VNS治疗的癫痫建立一种临床相关的动物模型,该模型可用于研究VNS的作用机理。方法:通过测量行为和电生理参数,对完全点燃的大鼠研究VNS的抗惊厥作用。通过定量孤立道(NTS)核中的nNOS免疫反应性细胞,证实了传入迷走神经的激活。结果:VNS大鼠在NTS中的nNOS免疫反应性细胞/ mm(2)多于假性。 VNS导致32%的大鼠的5期持续时间(S5D)降低> 25%。在使用VNS之前,这类反应者的癫痫发作总发作持续时间(TSD)比无反应者长。在21%的大鼠中,VNS导致TSD降低> 25%。这种类型的响应者在VNS之前的TSD短于非响应者。在29%的大鼠中,VNS导致5期潜伏期(S5L)的增加> 200%。这种类型的响应者的点燃率要高于非响应者。结论:经VNS处理的点燃的大鼠是临床相关的动物模型,因为它是一种慢性癫痫模型,可对VNS做出反应,其作用可与VNS对癫痫患者的作用相媲美。此外,这项研究表明,可以使用VNS处理的点燃大鼠使用免疫组织化学技术来研究VNS的作用方式。

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