老年人大脑中与阿尔茨海默病样神经退行性变相关的区域性脑白质高信号与纵向变化的关联。

Association of Regional White Matter Hyperintensities With Longitudinal Alzheimer-Like Pattern of Neurodegeneration in Older Adults.

机构信息

Taub Institute for Research on Alzheimer's Disease and the Aging Brain, Vagelos College of Physicians and Surgeons, Columbia University, New York, New York.

Department of Psychiatry, Vagelos College of Physicians and Surgeons, Columbia University, New York, New York.

出版信息

JAMA Netw Open. 2021 Oct 1;4(10):e2125166. doi: 10.1001/jamanetworkopen.2021.25166.

DOI:10.1001/jamanetworkopen.2021.25166

PMID:34609497

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8493439/

Abstract

IMPORTANCE

Small vessel cerebrovascular disease, visualized as white matter hyperintensities (WMH), is associated with cognitive decline and risk of clinical Alzheimer disease (AD). One way in which small vessel cerebrovascular disease could contribute to AD is through the promotion of neurodegeneration; the effect of small vessel cerebrovascular disease on neurodegeneration may differ across racial and ethnic groups.

OBJECTIVE

To examine whether WMH volume is associated with cortical thinning over time and subsequent memory functioning and whether the association between WMH volume and cortical thinning differs among racial and ethnic groups.

DESIGN, SETTING, AND PARTICIPANTS: This longitudinal community-based cohort study included older adults from northern Manhattan who were participants in the Washington Heights-Inwood Columbia Aging Project. Participants underwent two 3T magnetic resonance imaging (MRI) scans a mean of 4 years apart. Data were collected from March 2011 to January 2020.

EXPOSURES

Total and regional WMH volumes.

MAIN OUTCOMES AND MEASURES

The association of total and regional WMH volumes with cortical thinning over time was tested using general linear models in a vertexwise analysis. Cortical thinning was measured vertexwise by symmetrized percent change between 2 time points. The association of changes in cortical thickness with memory and whether this association differed by race and ethnicity was also analyzed. Delayed memory was a secondary outcome.

RESULTS

In 303 participants (mean [SD] age, 73.16 [5.19] years, 181 [60%] women, 96 [32%] non-Hispanic White, 113 [37%] Non-Hispanic Black, 94 [31%] Hispanic), baseline WMH volumes were associated with cortical thinning in medial temporal and frontal/parietal regions. Specifically, total WMH volume was associated with cortical thinning in the right caudal middle frontal cortex (P = .001) and paracentral cortex (P = .04), whereas parietal WMH volume was associated with atrophy in the left entorhinal cortex (P = .03) and right rostral middle frontal (P < .001), paracentral (P < .001), and pars triangularis (P = .02) cortices. Thinning of the right caudal middle frontal and left entorhinal cortices was related to lower scores on a memory test administered closest to the second MRI visit (right caudal middle frontal cortex: standardized β = 0.129; unstandardized b = 0.335; 95% CI, 0.055 to 0.616; P = .01; left entorhinal cortex: β = 0.119; b = 0.290; 95% CI, 0.018 to 0.563; P = .03). The association of total WMH with thinning in the right caudal middle frontal and right paracentral cortex was greater in non-Hispanic Black participants compared with White participants (right caudal middle frontal cortex: β = -0.222; b = -0.059; 95% CI, -0.114 to -0.004; P = .03; right paracentral cortex: β = -0.346; b = -0.155; 95% CI, -0.244 to -0.066; P = .001). The association of parietal WMH with cortical thinning of the right rostral middle frontal, right pars triangularis, and right paracentral cortices was also stronger among non-Hispanic Black participants compared with White participants (right rostral middle frontal cortex: β = -0.252; b = -0.202; 95% CI, -0.349 to -0.055; P = .007; right pars triangularis cortex: β = -0.327; b = -0.253; 95% CI, -0.393 to -0.113; P < .001; right paracentral cortex: β = -0.263; b = -0.337; 95% CI, -0.567 to -0.107; P = .004).

CONCLUSIONS AND RELEVANCE

In this study, small vessel cerebrovascular disease, operationalized as WMH, was associated with subsequent cortical atrophy in regions that overlap with typical AD neurodegeneration patterns, particularly among non-Hispanic Black older adults. Cerebrovascular disease may affect risk and progression of AD by promoting neurodegeneration and subsequent memory decline.

摘要

重要性

小血管脑血管疾病，表现为白质高信号（WMH），与认知能力下降和临床阿尔茨海默病（AD）风险相关。小血管脑血管疾病可能通过促进神经退行性变来导致 AD 的一种方式；小血管脑血管疾病对神经退行性变的影响可能因种族和民族群体而异。

目的

检查 WMH 体积是否与皮质变薄随时间的变化相关，以及与皮质变薄相关的后续记忆功能，以及 WMH 体积与皮质变薄之间的关联是否因种族和民族群体而异。

设计、地点和参与者：这是一项基于社区的纵向队列研究，参与者来自曼哈顿北部的老年人，他们是华盛顿高地-因伍德哥伦比亚老龄化项目的参与者。参与者在平均 4 年的时间里接受了两次 3T 磁共振成像（MRI）扫描。数据收集时间为 2011 年 3 月至 2020 年 1 月。

暴露

总 WMH 体积和区域 WMH 体积。

主要结果和测量

使用顶点分析中的一般线性模型测试总 WMH 体积和区域 WMH 体积与随时间的皮质变薄之间的关联。通过在两个时间点之间的对称百分比变化来测量皮质变薄的顶点。还分析了皮质厚度变化与记忆的关系，以及这种关系是否因种族和民族而异。延迟记忆是次要结果。

结果

在 303 名参与者（平均[标准差]年龄 73.16[5.19]岁，181 名[60%]女性，96 名[32%]非西班牙裔白人，113 名[37%]非西班牙裔黑人，94 名[31%]西班牙裔）中，基线 WMH 体积与内侧颞叶和额顶/顶叶区域的皮质变薄相关。具体来说，总 WMH 体积与右侧尾状中额皮质（P = .001）和旁中央皮质（P = .04）的皮质变薄相关，而顶叶 WMH 体积与左侧内嗅皮质（P = .03）和右侧额极中额（P < .001）、旁中央（P < .001）和三角部（P = .02）皮质的萎缩相关。右侧尾状中额皮质和左侧内嗅皮质的变薄与第二次 MRI 检查最接近时的记忆测试得分较低相关（右侧尾状中额皮质：标准化β=0.129；未标准化 b=0.335；95%置信区间，0.055 至 0.616；P=0.01；左侧内嗅皮质：β=0.119；b=0.290；95%置信区间，0.018 至 0.563；P=0.03）。与白人参与者相比，非西班牙裔黑人参与者中总 WMH 与右侧尾状中额和右侧旁中央皮质变薄的关联更强（右侧尾状中额皮质：β=−0.222；b=−0.059；95%置信区间，−0.114 至−0.004；P=0.03；右侧旁中央皮质：β=−0.346；b=−0.155；95%置信区间，−0.244 至−0.066；P=0.001）。与白人参与者相比，非西班牙裔黑人参与者中顶叶 WMH 与右侧额极中额、右侧三角部和右侧旁中央皮质变薄的关联也更强（右侧额极中额皮质：β=−0.252；b=−0.202；95%置信区间，−0.349 至−0.055；P=0.007；右侧三角部皮质：β=−0.327；b=−0.253；95%置信区间，−0.393 至−0.113；P< .001；右侧旁中央皮质：β=−0.263；b=−0.337；95%置信区间，−0.567 至−0.107；P=0.004）。