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视运动整合缺陷在家族性和散发性临床前阿尔茨海默病中很常见。

Visuomotor integration deficits are common to familial and sporadic preclinical Alzheimer's disease.

作者信息

Lu Kirsty, Nicholas Jennifer M, Weston Philip S J, Stout Julie C, O'Regan Alison M, James Sarah-Naomi, Buchanan Sarah M, Lane Christopher A, Parker Thomas D, Keuss Sarah E, Keshavan Ashvini, Murray-Smith Heidi, Cash David M, Sudre Carole H, Malone Ian B, Coath William, Wong Andrew, Richards Marcus, Henley Susie M D, Fox Nick C, Schott Jonathan M, Crutch Sebastian J

机构信息

Dementia Research Centre, UCL Queen Square Institute of Neurology, University College London, London, WC1N 3BG, UK.

Department of Medical Statistics, London School of Hygiene and Tropical Medicine, London, WC1E 7HT, UK.

出版信息

Brain Commun. 2021 Jan 25;3(1):fcab003. doi: 10.1093/braincomms/fcab003. eCollection 2021.

Abstract

We investigated whether subtle visuomotor deficits were detectable in familial and sporadic preclinical Alzheimer's disease. A circle-tracing task-with direct and indirect visual feedback, and dual-task subtraction-was completed by 31 individuals at 50% risk of familial Alzheimer's disease (19 presymptomatic mutation carriers; 12 non-carriers) and 390 cognitively normal older adults (members of the British 1946 Birth Cohort, all born during the same week; age range at assessment = 69-71 years), who also underwent β-amyloid-PET/MRI to derive amyloid status (positive/negative), whole-brain volume and white matter hyperintensity volume. We compared preclinical Alzheimer's groups against controls cross-sectionally (mutation carriers versus non-carriers; amyloid-positive versus amyloid-negative) on speed and accuracy of circle-tracing and subtraction. Mutation carriers (mean 7 years before expected onset) and amyloid-positive older adults traced disproportionately less accurately than controls when visual feedback was indirect, and were slower at dual-task subtraction. In the older adults, the same pattern of associations was found when considering amyloid burden as a continuous variable (Standardized Uptake Value Ratio). The effect of amyloid was independent of white matter hyperintensity and brain volumes, which themselves were associated with different aspects of performance: greater white matter hyperintensity volume was also associated with disproportionately poorer tracing accuracy when visual feedback was indirect, whereas larger brain volume was associated with faster tracing and faster subtraction. Mutation carriers also showed evidence of poorer tracing accuracy when visual feedback was direct. This study provides the first evidence of visuomotor integration deficits common to familial and sporadic preclinical Alzheimer's disease, which may precede the onset of clinical symptoms by several years.

摘要

我们研究了在家族性和散发性临床前阿尔茨海默病中是否能检测到细微的视觉运动缺陷。31名有50%家族性阿尔茨海默病风险的个体(19名症状前突变携带者;12名非携带者)和390名认知正常的老年人(英国1946年出生队列的成员,均在同一周出生;评估时年龄范围 = 69 - 71岁)完成了一项圆圈追踪任务——有直接和间接视觉反馈以及双任务减法。这些人还接受了β淀粉样蛋白PET/MRI检查以确定淀粉样蛋白状态(阳性/阴性)、全脑体积和白质高信号体积。我们将临床前阿尔茨海默病组与对照组在圆圈追踪和减法的速度及准确性方面进行了横断面比较(突变携带者与非携带者;淀粉样蛋白阳性与淀粉样蛋白阴性)。当视觉反馈为间接时,突变携带者(平均预期发病前7年)和淀粉样蛋白阳性的老年人追踪的准确性明显低于对照组,并且在双任务减法中速度较慢。在老年人中,将淀粉样蛋白负担视为连续变量(标准化摄取值比率)时也发现了相同的关联模式。淀粉样蛋白的影响独立于白质高信号和脑体积,而白质高信号和脑体积本身与表现的不同方面相关:更大的白质高信号体积在视觉反馈为间接时也与追踪准确性明显较差相关,而更大的脑体积与更快的追踪和更快的减法相关。当视觉反馈为直接时,突变携带者也显示出追踪准确性较差的证据。这项研究首次提供了家族性和散发性临床前阿尔茨海默病共有的视觉运动整合缺陷的证据,这些缺陷可能在临床症状出现前数年就已存在。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c82c/7882207/865623886c16/fcab003f4.jpg

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