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穹窿深部脑刺激可挽救雷特综合征小鼠的海马记忆。

Forniceal deep brain stimulation rescues hippocampal memory in Rett syndrome mice.

作者信息

Hao Shuang, Tang Bin, Wu Zhenyu, Ure Kerstin, Sun Yaling, Tao Huifang, Gao Yan, Patel Akash J, Curry Daniel J, Samaco Rodney C, Zoghbi Huda Y, Tang Jianrong

机构信息

Jan and Dan Duncan Neurological Research Institute, Texas Children's Hospital, Houston, Texas 77030, USA.

Department of Pediatrics, Baylor College of Medicine, Houston, Texas 77030, USA.

出版信息

Nature. 2015 Oct 15;526(7573):430-4. doi: 10.1038/nature15694.

DOI:10.1038/nature15694
PMID:26469053
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4828032/
Abstract

Deep brain stimulation (DBS) has improved the prospects for many individuals with diseases affecting motor control, and recently it has shown promise for improving cognitive function as well. Several studies in individuals with Alzheimer disease and in amnesic rats have demonstrated that DBS targeted to the fimbria-fornix, the region that appears to regulate hippocampal activity, can mitigate defects in hippocampus-dependent memory. Despite these promising results, DBS has not been tested for its ability to improve cognition in any childhood intellectual disability disorder. Such disorders are a pressing concern: they affect as much as 3% of the population and involve hundreds of different genes. We proposed that stimulating the neural circuits that underlie learning and memory might provide a more promising route to treating these otherwise intractable disorders than seeking to adjust levels of one molecule at a time. We therefore studied the effects of forniceal DBS in a well-characterized mouse model of Rett syndrome (RTT), which is a leading cause of intellectual disability in females. Caused by mutations that impair the function of MeCP2 (ref. 6), RTT appears by the second year of life in humans, causing profound impairment in cognitive, motor and social skills, along with an array of neurological features. RTT mice, which reproduce the broad phenotype of this disorder, also show clear deficits in hippocampus-dependent learning and memory and hippocampal synaptic plasticity. Here we show that forniceal DBS in RTT mice rescues contextual fear memory as well as spatial learning and memory. In parallel, forniceal DBS restores in vivo hippocampal long-term potentiation and hippocampal neurogenesis. These results indicate that forniceal DBS might mitigate cognitive dysfunction in RTT.

摘要

深部脑刺激(DBS)改善了许多患有影响运动控制疾病的个体的前景,最近它在改善认知功能方面也显示出了前景。对患有阿尔茨海默病的个体和失忆大鼠的多项研究表明,针对穹窿-海马伞(似乎调节海马体活动的区域)进行DBS,可以减轻海马体依赖性记忆的缺陷。尽管有这些令人鼓舞的结果,但DBS尚未在任何儿童智力残疾障碍中测试其改善认知的能力。此类障碍是一个紧迫的问题:它们影响多达3%的人口,涉及数百种不同的基因。我们提出,刺激学习和记忆背后的神经回路,可能比一次调整一种分子的水平,为治疗这些原本难以治疗的疾病提供一条更有前景的途径。因此,我们在一种特征明确的雷特综合征(RTT)小鼠模型中研究了穹窿DBS的效果,雷特综合征是女性智力残疾的主要原因。由损害MeCP2功能的突变引起(参考文献6),RTT在人类生命的第二年出现,导致认知、运动和社交技能的严重损害,以及一系列神经学特征。RTT小鼠再现了这种疾病的广泛表型,在海马体依赖性学习和记忆以及海马体突触可塑性方面也表现出明显的缺陷。在这里,我们表明,对RTT小鼠进行穹窿DBS可挽救情境恐惧记忆以及空间学习和记忆。同时,穹窿DBS可恢复体内海马体长期增强和海马体神经发生。这些结果表明,穹窿DBS可能减轻RTT中的认知功能障碍。

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Epigenetic Regulation and Neurodevelopmental Disorders: From MeCP2 to the TCF20/PHF14 Complex.表观遗传调控与神经发育障碍:从MeCP2到TCF20/PHF14复合物

本文引用的文献

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Deep brain stimulation for cognitive disorders.用于认知障碍的深部脑刺激
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