首页> 美国卫生研究院文献>The Journal of Neuroscience >Selective Loss of Thin Spines in Area 7a of the Primate Intraparietal Sulcus Predicts Age-Related Working Memory Impairment
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Selective Loss of Thin Spines in Area 7a of the Primate Intraparietal Sulcus Predicts Age-Related Working Memory Impairment

机译:灵长类动物腹内沟7a区细刺的选择性丢失预测了与年龄有关的工作记忆障碍

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摘要

Brodmann area 7a of the parietal cortex is active during working memory tasks in humans and nonhuman primates, but the composition and density of dendritic spines in area 7a and their relevance both to working memory and cognitive aging remain unexplored. Aged monkeys have impaired working memory, and we have previously shown that this age-induced cognitive impairment is partially mediated by a loss of thin spines in prefrontal cortex area 46, a critical area for working memory. Because area 46 is reciprocally connected with area 7a of the parietal cortex and 7a mediates visual attention integration, we hypothesized that thin spine density in area 7a would correlate with working memory performance as well. To investigate the synaptic profile of area 7a and its relevance to working memory and cognitive aging, we investigated differences in spine type and density in layer III pyramidal cells of area 7a in young and aged, male and female rhesus macaques (Macaca mulatta) that were cognitively assessed using the delayed response test of working memory. Area 7a shows age-related loss of thin spines, and thin spine density positively correlates with delayed response performance in aged monkeys. In contrast, these cells show no age-related changes in dendritic length or branching. These changes mirror age-related changes in area 46 but are distinct from other neocortical regions, such as V1. These findings support our hypothesis that cognitive aging is driven primarily by synaptic changes, and more specifically by changes in thin spines, in key association areas.>SIGNIFICANCE STATEMENT This study advances our understanding of cognitive aging by demonstrating the relevance of area 7a thin spines to working memory performance. This study is the first to look at cognitive aging in the intraparietal sulcus, and also the first to report spine or dendritic measures for area 7a in either young adult or aged nonhuman primates. These results contribute to the hypothesis that thin spines support working memory performance and confirm our prior observation that cognitive aging is driven by synaptic changes rather than changes in dendritic morphology or neuron death. Importantly, these data show that age-related working memory changes are not limited to disruptions of the prefrontal cortex but also include an association region heavily interconnected with prefrontal cortex.
机译:在人类和非人类灵长类动物的工作记忆任务中,顶叶皮层的Brodmann区域7a活跃,但是7a区域的树突棘的组成和密度以及它们与工作记忆和认知衰老的相关性仍未得到探索。年迈的猴子损害了工作记忆,我们以前已经表明,这种年龄引起的认知障碍部分由额叶前额叶皮层区域46(工作记忆的关键区域)中细刺的丧失部分介导。由于区域46与顶叶皮层区域7a相互连接,并且7a介导视觉注意力整合,因此我们假设区域7a中的薄脊柱密度也将与工作记忆性能相关。为了研究区域7a的突触分布及其与工作记忆和认知衰老的相关性,我们调查了年龄在7a左右的雄性和雌性猕猴(猕猴)中7a区域III层锥体细胞的脊柱类型和密度的差异。使用工作记忆的延迟反应测试进行认知评估。区域7a显示了与年龄相关的瘦脊椎丧失,而瘦脊椎密度与衰老的猴子的延迟反应表现成正相关。相反,这些细胞在树突长度或分支中没有显示出与年龄相关的变化。这些变化反映了区域46中与年龄相关的变化,但与其他新皮质区域(例如V1)不同。这些发现支持了我们的假设,即认知衰老主要是由关键关联区域中的突触变化驱动的,更具体地说是由细刺的变化驱动的。>意义声明:本研究通过证明其相关性,增进了我们对认知衰老的理解。区域7a细刺对工作记忆性能的影响。这项研究是第一个研究顶内沟认知老化的研究,也是第一个报告年轻人或年长的非人灵长类动物7a区脊柱或树突测量的研究。这些结果有助于假说细刺支持工作记忆性能,并证实我们先前的观察结果,即认知衰老是由突触变化而非树突形态或神经元死亡引起的。重要的是,这些数据表明与年龄有关的工作记忆变化不仅限于前额叶皮层的破坏,还包括与前额叶皮层紧密相连的关联区域。

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