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首页> 外文期刊>Biological psychiatry >SCN1A affects brain structure and the neural activity of the aging brain
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SCN1A affects brain structure and the neural activity of the aging brain

机译:SCN1A影响大脑结构和衰老大脑的神经活动

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Background: The aging of the human brain is accompanied by changes in cortical structure as well as functional activity and variable degrees of cognitive decline. One-third of the observable inter-individual differences in cognitive decline are thought to be heritable. SCN1A encodes the sodium channel α subunit and is considered to be a susceptibility gene for several neurological disorders with prominent cognitive deficits. In a recent genome-wide association study the C allele of the SCN1A variant rs10930201 was observed to be significantly associated with poor short-term memory performance. rs10930201 was further observed to be related to differences in neural activity during a working memory task. Methods: The aim of the present study was to explore whether SCN1A modifies the vulnerability to aging processes of the human brain. Therefore we assessed the interacting effects of the SCN1A vulnerability allele rs10930201 and age in terms of brain activity and brain morphology in 62 healthy volunteers between 21 and 82 years of age. Results: In C allele carriers, activity in the right inferior frontal cortex and the posterior cingulate cortex increased with age. Moreover, exploratory analysis revealed regional effects of rs10930201 on brain structure, indicating reduced gray matter densities in the frontal and insular regions in the C allele carriers. Conclusions: Collectively, the present results suggest that the SCN1A polymorphism has modulatory effects on brain morphology and vulnerability to age-related alterations in brain activity of cortical regions that subserve working memory.
机译:背景:人脑的衰老伴随着皮质结构的改变,功能活动和不同程度的认知能力下降。认知能力下降中可观察到的个体间差异的三分之一被认为是可遗传的。 SCN1A编码钠通道α亚基,被认为是几种具有明显认知缺陷的神经系统疾病的易感基因。在最近的全基因组关联研究中,观察到SCN1A变体rs10930201的C等位基因与不良的短期记忆表现显着相关。进一步观察到rs10930201与工作记忆任务期间神经活动的差异有关。方法:本研究的目的是探讨SCN1A是否能改善人脑衰老过程的脆弱性。因此,我们评估了62名21至82岁健康志愿者的SCN1A易感性等位基因rs10930201和年龄之间的相互作用,以大脑活动和大脑形态为依据。结果:在C等位基因携带者中,右下额叶皮层和后扣带回皮层的活性随年龄增加。此外,探索性分析显示rs10930201对脑结构的区域影响,表明C等位基因携带者的额叶和岛状区域灰质密度降低。结论:总的来说,目前的结果表明,SCN1A基因多态性对大脑形态具有调节作用,并且容易受到年龄相关的皮质区域大脑活动变化的影响,从而有助于工作记忆。

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