脑血管疾病与唐氏综合征成人阿尔茨海默氏症血浆生物标志物浓度有关。

IF 4.1 Q1 CLINICAL NEUROLOGY
Brain communications Pub Date : 2024-09-25 eCollection Date: 2024-01-01 DOI:10.1093/braincomms/fcae331
Natalie C Edwards, Patrick J Lao, Mohamad J Alshikho, Olivia M Ericsson, Batool Rizvi, Melissa E Petersen, Sid O'Bryant, Lisi Flores Aguilar, Sabrina Simoes, Mark Mapstone, Dana L Tudorascu, Shorena Janelidze, Oskar Hansson, Benjamin L Handen, Bradley T Christian, Joseph H Lee, Florence Lai, H Diana Rosas, Shahid Zaman, Ira T Lott, Michael A Yassa, José Gutierrez, Donna M Wilcock, Elizabeth Head, Adam M Brickman
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引用次数: 0

摘要

到 40 岁时,90% 以上的成年唐氏综合征患者会出现阿尔茨海默病的病理变化,而且大多数会发展为痴呆症。尽管唐氏综合征患者几乎没有全身性血管风险因素,但他们的脑血管疾病标志物升高,与阿尔茨海默病的临床进展相一致,这表明脑血管疾病可能是由炎症因素介导的。本研究探讨了小血管脑血管疾病导致阿尔茨海默病相关病理生理学和唐氏综合征成人神经退行性变的途径。本研究共纳入了 185 名来自阿尔茨海默氏症生物标志物联盟-唐氏综合征(Alzheimer's Biomarkers Consortium-Down Syndrome)的参与者[平均(标清)年龄 = 45.2 (9.3)岁],他们都有可用的核磁共振成像和血浆生物标志物数据。白质高密度(WMH)体积由 T2 加权流体增强反转复原 MRI 扫描得出,血浆中淀粉样 beta 42/40、磷酸化 tau 217、星形胶质细胞增多症(胶质纤维酸性蛋白)和神经变性(神经丝蛋白轻链)的生物标记物浓度由超敏免疫测定法测定。我们研究了不同阿尔茨海默病诊断组的 WMH、淀粉样 beta 42/40、磷酸化 tau 217 和胶质纤维酸性蛋白与年龄残留神经丝轻链的二元关系。一系列中介和路径分析研究了将 WMH 与阿尔茨海默病病理生理学联系起来的统计路径,这些路径促进了总样本和按临床诊断分层的各组的神经变性。在整个样本中,WMH通过胶质纤维酸性蛋白对磷酸化tau 217浓度产生直接和间接的双向影响,而磷酸化tau 217浓度与神经丝轻链浓度相关。在认知功能稳定的参与者中,WMH通过胶质纤维酸性蛋白直接或间接地与磷酸化tau 217浓度相关,而在轻度认知障碍患者中,WMH对磷酸化tau 217和神经丝轻链浓度有直接影响。在确诊为痴呆症的患者中,WMH与生物标志物浓度没有关联。这项横断面研究的结果表明,在唐氏综合征患者中,脑血管疾病会在阿尔茨海默病的无症状阶段通过增加星形胶质细胞增多和tau病理生理学促进神经变性,但未来的研究需要通过纵向数据来证实这些关联。这项研究加入了新兴文献的行列,这些文献认为脑血管疾病及其与神经炎症的相互作用是唐氏综合征成人阿尔茨海默病的核心病理特征。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cerebrovascular disease is associated with Alzheimer's plasma biomarker concentrations in adults with Down syndrome.

By age 40 years, over 90% of adults with Down syndrome have Alzheimer's disease pathology and most progress to dementia. Despite having few systemic vascular risk factors, individuals with Down syndrome have elevated cerebrovascular disease markers that track with the clinical progression of Alzheimer's disease, suggesting a role of cerebrovascular disease that is hypothesized to be mediated by inflammatory factors. This study examined the pathways through which small vessel cerebrovascular disease contributes to Alzheimer's disease-related pathophysiology and neurodegeneration in adults with Down syndrome. One hundred eighty-five participants from the Alzheimer's Biomarkers Consortium-Down Syndrome [mean (SD) age = 45.2 (9.3) years] with available MRI and plasma biomarker data were included in this study. White matter hyperintensity (WMH) volumes were derived from T2-weighted fluid-attenuated inversion recovery MRI scans, and plasma biomarker concentrations of amyloid beta 42/40, phosphorylated tau 217, astrocytosis (glial fibrillary acidic protein) and neurodegeneration (neurofilament light chain) were measured with ultrasensitive immunoassays. We examined the bivariate relationships of WMH, amyloid beta 42/40, phosphorylated tau 217 and glial fibrillary acidic protein with age-residualized neurofilament light chain across Alzheimer's disease diagnostic groups. A series of mediation and path analyses examined statistical pathways linking WMH and Alzheimer's disease pathophysiology to promote neurodegeneration in the total sample and groups stratified by clinical diagnosis. There was a direct and indirect bidirectional effect through the glial fibrillary acidic protein of WMH on phosphorylated tau 217 concentration, which was associated with neurofilament light chain concentration in the entire sample. Amongst cognitively stable participants, WMH was directly and indirectly, through glial fibrillary acidic protein, associated with phosphorylated tau 217 concentration, and in those with mild cognitive impairment, there was a direct effect of WMH on phosphorylated tau 217 and neurofilament light chain concentrations. There were no associations of WMH with biomarker concentrations among those diagnosed with dementia. The findings from this cross-sectional study suggest that among individuals with Down syndrome, cerebrovascular disease promotes neurodegeneration by increasing astrocytosis and tau pathophysiology in the presymptomatic phases of Alzheimer's disease, but future studies will need to confirm these associations with longitudinal data. This work joins an emerging literature that implicates cerebrovascular disease and its interface with neuroinflammation as a core pathological feature of Alzheimer's disease in adults with Down syndrome.

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