Genetic Risk for Alzheimer Disease and Plasma Tau Are Associated With Accelerated Parietal Cortex Thickness Change in Middle-Aged Adults.

IF 3 3区医学 Q2 CLINICAL NEUROLOGY Neurology-Genetics Pub Date : 2023-02-01 DOI:10.1212/NXG.0000000000200053

Jasmeet Pannu Hayes, Meghan E Pierce, Emma Brown, David Salat, Mark W Logue, Julie Constantinescu, Kate Valerio, Mark W Miller, Richard Sherva, Bertrand Russell Huber, William Milberg, Regina McGlinchey

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Abstract

Background and objectives: Neuroimaging and biomarker studies in Alzheimer disease (AD) have shown well-characterized patterns of cortical thinning and altered biomarker concentrations of tau and β-amyloid (Aβ). However, earlier identification of AD has great potential to advance clinical care and determine candidates for drug trials. The extent to which AD risk markers relate to cortical thinning patterns in midlife is unknown. The first objective of this study was to examine cortical thickness change associated with genetic risk for AD among middle-aged military veterans. The second objective was to determine the relationship between plasma tau and Aβ and change in brain cortical thickness among veterans stratified by genetic risk for AD.

Methods: Participants consisted of post-9/11 veterans (N = 155) who were consecutively enrolled in the Translational Research Center for TBI and Stress Disorders prospective longitudinal cohort and were assessed for mild traumatic brain injury (TBI) and posttraumatic disorder (PTSD). Genome-wide polygenic risk scores (PRSs) for AD were calculated using summary results from the International Genomics of Alzheimer's Disease Project. T-tau and Aβ40 and Aβ42 plasma assays were run using Simoa technology. Whole-brain MRI cortical thickness change estimates were obtained using the longitudinal stream of FreeSurfer. Follow-up moderation analyses examined the AD PRS × plasma interaction on change in cortical thickness in AD-vulnerable regions.

Results: Higher AD PRS, signifying greater genetic risk for AD, was associated with accelerated cortical thickness change in a right hemisphere inferior parietal cortex cluster that included the supramarginal gyrus, angular gyrus, and intraparietal sulcus. Higher tau, but not Aβ42/40 ratio, was associated with greater cortical thickness change among those with higher AD PRS. Mild TBI and PTSD were not associated with cortical thickness change.

Discussion: Plasma tau, particularly when combined with genetic stratification for AD risk, can be a useful indicator of brain change in midlife. Accelerated inferior parietal cortex changes in midlife may be an important factor to consider as a marker of AD-related brain alterations.

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阿尔茨海默病的遗传风险和血浆 Tau 与中年人顶叶皮层厚度的加速变化有关。

背景和目的：阿尔茨海默病（AD）的神经影像学和生物标志物研究显示，皮质变薄、tau 和β-淀粉样蛋白（Aβ）生物标志物浓度改变的模式特征明显。然而，尽早发现注意力缺失症对于促进临床治疗和确定药物试验候选者具有巨大潜力。注意力缺失症风险标志物与中年皮质变薄模式的相关程度尚不清楚。本研究的第一个目的是研究中年退伍军人皮质厚度变化与注意力缺失症遗传风险的相关性。第二个目的是确定血浆 tau 和 Aβ 与根据 AD 遗传风险分层的退伍军人大脑皮质厚度变化之间的关系：参与者包括连续加入创伤性脑损伤和应激障碍转化研究中心（TBI and Stress Disorders Translational Research Center）前瞻性纵向队列的 9/11 后退伍军人（N = 155），他们接受了轻度创伤性脑损伤（TBI）和创伤后应激障碍（PTSD）的评估。利用国际阿尔茨海默病基因组学项目的汇总结果计算了AD的全基因组多基因风险评分（PRS）。使用Simoa技术进行T-tau、Aβ40和Aβ42血浆检测。利用FreeSurfer的纵向流获得了全脑核磁共振成像皮层厚度变化估计值。后续调节分析检验了 AD PRS × 血浆对 AD 易感区域皮层厚度变化的交互作用：结果：AD PRS越高，表明AD遗传风险越大，这与右半球顶叶下皮层群皮层厚度的加速变化有关，该皮层群包括边上回、角回和顶内沟。在AD PRS较高的人群中，较高的tau（而非Aβ42/40比值）与较大的皮层厚度变化相关。轻度创伤性脑损伤和创伤后应激障碍与皮质厚度变化无关：讨论：血浆tau，尤其是与AD风险遗传分层相结合时，可作为中年大脑变化的有用指标。中年时下顶叶皮层的加速变化可能是作为与AD相关的脑部改变标志的一个重要考虑因素。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Neurology-Genetics Medicine-Neurology (clinical)

CiteScore

6.30

自引率

3.20%

发文量

107

审稿时长

15 weeks

期刊介绍： Neurology: Genetics is an online open access journal publishing peer-reviewed reports in the field of neurogenetics. Original articles in all areas of neurogenetics will be published including rare and common genetic variation, genotype-phenotype correlations, outlier phenotypes as a result of mutations in known disease-genes, and genetic variations with a putative link to diseases. This will include studies reporting on genetic disease risk and pharmacogenomics. In addition, Neurology: Genetics will publish results of gene-based clinical trials (viral, ASO, etc.). Genetically engineered model systems are not a primary focus of Neurology: Genetics, but studies using model systems for treatment trials are welcome, including well-powered studies reporting negative results.