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Association between insomnia and cognitive performance, gray matter volume, and white matter microstructure in cognitively unimpaired adults

机译:认知未受损成人的失眠和认知性能,灰质体积和白质微观结构的关系

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Mounting evidence links poor sleep quality with a higher risk of late-life dementia. However, the structural and cognitive correlates of insomnia are still not well understood. The study aims were to characterize the cognitive performance and brain structural pattern of cognitively unimpaired adults at increased risk for Alzheimer’s disease (AD) with insomnia. This cross-sectional study included 1683 cognitively unimpaired middle/late-middle-aged adults from the ALFA (ALzheimer and FAmilies) study who underwent neuropsychological assessment, T1-weighted structural imaging (n?=?366), and diffusion-weighted imaging (n?=?334). The World Health Organization’s World Mental Health Survey Initiative version of the Composite International Diagnostic Interview was used to define the presence or absence of insomnia. Multivariable regression models were used to evaluate differences in cognitive performance between individuals with and without insomnia, as well as potential interactions between insomnia and the APOE genotype. Voxel-based morphometry and tract-based spatial statistics were used to assess between-group differences and potential interactions between insomnia and the APOE genotype in gray matter volume and white matter diffusion metrics. Insomnia was reported by 615 out of 1683 participants (36.5%), including 137 out of 366 (37.4%) with T1-weighted structural imaging available and 119 out of 334 (35.6%) with diffusion-weighted imaging. Individuals with insomnia (n?=?615) performed worse in executive function tests than non-insomniacs and displayed lower gray matter volume in left orbitofrontal and right middle temporal cortex, bilateral precuneus, posterior cingulate cortex and thalamus, higher gray matter volume in the left caudate nucleus, and widespread reduction of mean and axial diffusivity in right hemisphere white matter tracts. Insomnia interacted with the APOE genotype, with APOE-ε4 carriers displaying lower gray matter volumes when insomnia was present, but higher volumes when insomnia was not present, in several gray matter regions, including the left angular gyrus, the bilateral superior frontal gyri, the thalami, and the right hippocampus. Insomnia in cognitively unimpaired adults at increased risk for AD is associated to poorer performance in some executive functions and volume changes in cortical and subcortical gray matter, including key areas involved in Alzheimer’s disease, as well as decreased white matter diffusivity.
机译:安装证据将睡眠质量较差,具有更高的痴呆症风险较高。然而,失眠的结构和认知相关性仍然不太了解。该研究旨在表征认知未受吸入性成人的认知性能和脑结构模式,以增加阿尔茨海默病(AD)的失眠。该横断面研究包括1683项认知的中/晚期中/晚期中生成人来自Alfa(阿尔茨海默氏症和家族)研究,谁研究了神经心理学评估,T1加权结构成像(N?= 366)和扩散加权成像( n?=?334)。世界卫生组织的世界心理健康调查倡议版综合国际诊断访谈用于定义失眠症的存在或不存在。多变量回归模型用于评估具有和不具有失眠的个体之间的认知性能的差异,以及失眠与ApoE基因型之间的潜在相互作用。基于体素的形态学和基于传道的空间统计学用于评估灰质体积和白质量扩散度量的失眠和ApoE基因型之间的组差异和潜在相互作用。 1683名参与者(36.5%)中报告了失眠的615名(36.5%),其中366例(37.4%)中有137名(37.4%),可用T1加权结构成像,334个(35.6%),扩散加权成像。具有失眠症的个体(n?=Δ615)在执行功能测试中表现比非失眠症,并且在左眶内和右中间时颞皮质皮层,双侧前骑士,后刺皮层和丘脑中显示出较低的灰质体积,较高的灰质体积左侧核心核,并在右半球白质龟头中广泛减少平均值和轴向扩散性。失眠与apoe基因型相互作用,具有达到灰质物质的Apoe-ε4载体,当存在失眠时,但在几个灰质区域中没有出现失眠时,包括左角度的偏振子,双侧上额前gyri丘脑和右海马。在AD的增加风险上的认知未受审计的成年人的失眠与某些行政职能和皮质和皮质灰质的体积变化的性能有关,包括参与阿尔茨海默病的关键领域,以及减少白质扩散率。

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