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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Cerebellar circuitry is activated during convulsive episodes in the tottering (tg/tg) mutant mouse.
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Cerebellar circuitry is activated during convulsive episodes in the tottering (tg/tg) mutant mouse.

机译:在蹒跚(tg / tg)突变小鼠的惊厥发作期间,小脑电路被激活。

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Tottering (tg) is an autosomal recessive mutation of the calcium channel alpha1A subunit in the mouse that results in epileptic spike and wave discharges, mild ataxia and paroxysmal episodes of involuntary spasms of the limbs, trunk and face. These convulsions have been especially difficult to characterize because of their unpredictable occurrence and lack of electroencephalographic correlates. However, it is, in fact, possible to induce these convulsions, making this facet of the tottering phenotype amenable to controlled experimentation for the first time. Here, the neuroanatomical basis of the convulsions in tottering mice has been identified using in situ hybridization for c-fos messenger RNA to chart abnormal neuronal activity. Convulsion-induced c-fos messenger RNA expression was most prominent in the cerebellum of convulsing tottering mice. Additionally, cerebral cortex and principal cerebellar relay nuclei were also activated during a convulsion. The c-fos activation in the cerebellum temporally preceded expression in cerebral cortex, suggesting that cerebral cortex is not driving the expression of convulsions. These results suggest that the cerebellum, a region not classically associated with paroxysmal events, is important in the generation and/or maintenance of the intermittent convulsions in tottering mutant mice.
机译:Tottering(tg)是小鼠钙通道alpha1A亚基的常染色体隐性突变,可导致癫痫发作和波状放电,轻度共济失调和四肢,躯干和面部非自愿性痉挛发作。这些惊厥由于难以预测的发生和缺乏脑电图相关性而特别难以表征。然而,实际上,有可能诱发这些惊厥,使the杂表型的这一方面首次适合于受控实验。在这里,已经使用c-fos信使RNA的原位杂交技术绘制了异常的神经元活动,从而确定了蹒跚小鼠的惊厥的神经解剖学基础。惊厥诱导的c-fos信使RNA表达在惊厥的小脑小脑中最为突出。另外,惊厥期间大脑皮层和主要小脑中继核也被激活。小脑中c-fos的激活在时间上先于大脑皮层的表达,这表明大脑皮层并未驱动惊厥的表达。这些结果表明,小脑,与阵发性事件经典不相关的区域,在蹒跚突变小鼠中间歇性惊厥的产生和/或维持中很重要。

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