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首页> 外文期刊>Epilepsy & behavior: E&B >Seizure elements and seizure element transitions during tonic-clonic seizure activity in the synapsin I/II double knockout mouse: a neuroethological description.
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Seizure elements and seizure element transitions during tonic-clonic seizure activity in the synapsin I/II double knockout mouse: a neuroethological description.

机译:突触素I / II双敲除小鼠的强直-阵挛性癫痫发作活动中的癫痫发作元素和癫痫发作元素转变:神经伦理学描述。

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摘要

Inactivation of genes for the synaptic terminal proteins synapsin I and synapsin II leads to development of epileptic seizures in mice (Syn-DKO mice) in which no other behavioral abnormalities or any gross anatomical brain deformities have been reported. In humans, mutated synapsin I is associated with epilepsy. Thus, the Syn-DKO mouse might model human seizure development. Here we describe a neuroethological analysis of behavioral elements and relationships between these elements during seizures in Syn-DKO mice. The seizure elements belong to one of three clusters each characterized by specific patterns of activity: truncus-dominated elements, myoclonic elements, and running-fit activity. The first two clusters, constituting the majority of seizural activity, evolve quite differently during ongoing seizure activity. Whereas truncus-dominated elements unfold in a strict sequence, the myoclonic elements wax and wane more independently, once myoclonic activity has started. These differences may point to neurobiological mechanisms relevant to both rodent and human epilepsies.
机译:突触末端蛋白synapsin I和synapsin II的基因失活导致小鼠(Syn-DKO小鼠)癫痫性癫痫发作的发展,其中没有其他行为异常或任何严重的大脑解剖畸形的报道。在人类中,突触蛋白I突变与癫痫有关。因此,Syn-DKO小鼠可能模拟人类癫痫发作的发展。在这里,我们描述了在Syn-DKO小鼠癫痫发作期间行为元素以及这些元素之间的关系的神经伦理学分析。癫痫发作元素属于三个集群之一,每个集群均以特定的活动模式为特征:截头肌为主的元素,肌阵挛元素和跑步健身活动。前两个簇构成了主要的癫痫发作活动,在持续的癫痫发作过程中其演化差异很大。截骨占主导地位的元素以严格的顺序展开,而肌阵挛活性一旦开始,肌阵挛元素就会更加独立地蜡和衰弱。这些差异可能表明与啮齿动物和人类癫痫有关的神经生物学机制。

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