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载脂蛋白 E 对健康成年人脑白质微观结构的影响。

Effects of APOE on brain white matter microstructure in healthy adults.

机构信息

Department of Psychology, Center for the Study of Human Cognition, University of Oslo, Oslo, Norway.

出版信息

Neurology. 2012 Nov 6;79(19):1961-9. doi: 10.1212/WNL.0b013e3182735c9c. Epub 2012 Oct 24.

Abstract

OBJECTIVES

APOE is related to cholesterol transport and clearance and brain white matter (WM) properties involving myelin, of which cholesterol is a major component. Diffusion tensor imaging enables in vivo investigations of brain WM, and could increase our understanding of the pathways leading to Alzheimer disease. The main objective was to investigate the association between APOE and diffusion tensor imaging-derived indices of WM microstructure.

METHODS

Healthy participants were assessed on a range of neuropsychological measures, genotyped, and underwent MRI. A total of 203 volunteers (aged 21.1-69.9 years, mean = 47.6, SD = 14.9) with APOE genotypes ε2/ε3 (n = 30), ε3/ε3 (n = 113), and ε3/ε4 (n = 60) were included.

RESULTS

There were widespread increases in mean and radial diffusion in carriers of the ε3/ε4 alleles compared with ε3/ε3 with medium to strong effect sizes (Cohen's d = 0.77-0.79). No interactions between genotype and age were observed, indicating relatively stable differences from early adulthood. The results were independent of presence of dementia in close family. We also observed increased mean and radial diffusion and decreased fractional anisotropy in carriers of the ε2/ε3 alleles compared with ε3/ε3 carriers. No significant differences were found between ε2/ε3 and ε3/ε4.

CONCLUSIONS

APOE affects microstructural properties of the brain WM from early adulthood, but the specific allelic effects do not directly reflect the associated risk of developing Alzheimer disease. The role of APOE in cholesterol transport, the high density of cholesterol in myelin, and the specific effects on radial diffusivity support a putative functional role of APOE in modulating myelin-related processes in the brain.

摘要

目的

载脂蛋白 E(APOE)与胆固醇转运和清除以及涉及髓鞘的脑白质(WM)特性有关,其中胆固醇是髓鞘的主要成分。弥散张量成像可用于研究脑 WM 的活体,这可能会增加我们对导致阿尔茨海默病的途径的理解。主要目的是研究 APOE 与 WM 微观结构的弥散张量成像衍生指数之间的关联。

方法

对健康参与者进行一系列神经心理学评估、基因分型和 MRI 检查。共纳入 203 名志愿者(年龄 21.1-69.9 岁,均值=47.6,标准差=14.9),携带 APOE 基因型 ε2/ε3(n=30)、ε3/ε3(n=113)和 ε3/ε4(n=60)。

结果

与 ε3/ε3 携带者相比,携带 ε3/ε4 等位基因的个体的平均扩散和径向扩散均广泛增加,具有中到强的效应量(Cohen's d=0.77-0.79)。未观察到基因型和年龄之间的相互作用,这表明从成年早期开始就存在相对稳定的差异。研究结果与近亲中是否存在痴呆无关。与 ε3/ε3 携带者相比,携带 ε2/ε3 等位基因的个体的平均扩散和径向扩散增加,各向异性分数降低。ε2/ε3 和 ε3/ε4 之间没有显著差异。

结论

APOE 从成年早期开始影响脑 WM 的微观结构特性,但特定的等位基因效应并不直接反映发生阿尔茨海默病的相关风险。APOE 在胆固醇转运中的作用、髓鞘中胆固醇的高密度以及对径向扩散的特定影响,支持 APOE 在调节大脑中与髓鞘相关的过程中的潜在功能作用。

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