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ε4状态与血管负担对伴有和不伴有神经认知功能减退的老年人白质微结构完整性的交互作用。

Interactive effects of ɛ4 status and vascular burden on white matter microstructural integrity in aging with and without neurocognitive decline.

作者信息

Konwar Srijan, Manca Riccardo, De Marco Matteo, Soininen Hilkka, Venneri Annalena

机构信息

Department of Life Sciences, Brunel University London, Uxbridge, UK.

Department of Medicine and Surgery, University of Parma, Parma, Italy.

出版信息

J Alzheimers Dis. 2025 Apr;104(3):902-918. doi: 10.1177/13872877251320660. Epub 2025 Mar 25.

DOI:10.1177/13872877251320660
PMID:40129408
Abstract

BackgroundCarrying the Apolipoprotein () ε4 allele lowers age of onset and increases Alzheimer's disease (AD) risk. Neuropathological findings suggest a mixed etiology in many AD patients, and vascular pathology is common.ObjectiveThis study tested the interactive effect of status and multiple vascular comorbidities on white matter (WM) microstructure in aging and early AD.Methods195 participants from the VPH-DARE@IT dataset were stratified in low/high vascular burden based on the Framingham Risk Score (BMI version). Tract-based spatial statistics was used for WM analyses.ResultsThere was a main effect of , with ɛ4 carriers having higher fractional anisotropy (FA) and lower axial diffusivity (AxD), mean diffusivity (MD), and radial diffusivity (RD) than non-carriers. There was a main effect of vascular burden with lower FA and higher AxD, MD, and RD in the high-burden than the low-burden group. A significant interaction between genotype and vascular burden was also found for all diffusion indices. comparisons revealed lower left hemisphere WM integrity when comparing the low risk group (i.e., non-carriers low burden) to intermediate risk groups (i.e., non-carriers high burden or ɛ4 carriers low burden). The contrasts between the two intermediate risk groups showed altered WM integrity bilaterally. Only the non-carriers high burden showed greater alterations in WM integrity when compared with the high risk group (i.e., ɛ4 carriers high burden) mainly in right hemisphere tracts.ConclusionsThese findings indicate an interactive effect of a risk gene and vascular comorbidities on WM integrity in aging and early AD.

摘要

背景

携带载脂蛋白()ε4等位基因会降低发病年龄并增加患阿尔茨海默病(AD)的风险。神经病理学研究结果表明,许多AD患者病因复杂,血管病理学较为常见。

目的

本研究测试了状态和多种血管合并症对衰老和早期AD患者白质(WM)微观结构的交互作用。

方法

根据弗雷明汉风险评分(BMI版本),将VPH-DARE@IT数据集中的195名参与者分为低/高血管负担组。采用基于体素的空间统计学方法进行WM分析。

结果

存在主要效应,ε4携带者的分数各向异性(FA)较高,轴向扩散率(AxD)、平均扩散率(MD)和径向扩散率(RD)低于非携带者。血管负担存在主要效应,高负担组的FA较低,AxD、MD和RD较高。在所有扩散指数上,还发现了基因型与血管负担之间的显著交互作用。比较显示,低风险组(即非携带者低负担)与中度风险组(即非携带者高负担或ε4携带者低负担)相比,左半球WM完整性较低。两个中度风险组之间的对比显示双侧WM完整性改变。与高风险组(即ε4携带者高负担)相比,只有非携带者高负担组在WM完整性方面有更大改变,主要在右半球脑区。

结论

这些发现表明风险基因和血管合并症对衰老和早期AD患者WM完整性存在交互作用。

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