Comparative analysis of brain-derived tau oligomer interactomes in Alzheimer's disease, non-demented with Alzheimer's neuropathology, and primary age-related tauopathy: Implications for neurodegeneration and cognitive resilience.

IF 3.4 3区医学 Q2 NEUROSCIENCES

Journal of Alzheimer's Disease Pub Date : 2025-06-27 DOI:10.1177/13872877251352382

Danielle Jamison, Shrinath Kadamangudi, Batbayar Tumurbaatar, Wen-Ru Zhang, Lee Palmer, Steve Kunkel, Rakez Kayed, Agenor Limon, Giulio Taglialatela

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引用次数: 0

Abstract

BackgroundIn Alzheimer's disease (AD), soluble tau oligomers are central to neurodegeneration and cognitive decline. Resilient individuals, such as those with non-demented Alzheimer's neuropathology (NDAN) or primary age-related tauopathy (PART), offer critical insights into protective mechanisms against tau-mediated neurodegeneration. NDAN individuals exhibit AD neuropathology without cognitive impairment or neurodegeneration, while PART, characterized by hippocampal- and entorhinal-restricted tau pathology, manifests with minimal-to-no amnestic changes. Brain-derived tau oligomers (BDTO) from these cohorts provide a unique platform to explore molecular pathways underlying both vulnerability and resilience to tau pathology.ObjectiveTo identify vulnerability- and resilience-associated pathways by comparing BDTO interactomes across AD, NDAN, and PART.MethodsBDTO were isolated from AD (n = 4; 2M, 2F), NDAN (n = 4; 2M, 2F), and PART (n = 4; 1M, 3F) hippocampal autopsy specimens using co-immunoprecipitation. Proteins were identified via liquid chromatography-tandem mass spectrometry, and non-specific interactors were filtered using SAINTq. Interactome networks and enrichment analyses were performed using Metascape. Findings were cross-referenced with the Neuropro database and existing literature on tangle-associated proteins. Key interactors were validated through reverse co-immunoprecipitation.ResultsA total of 203 proteins were identified, including eight novel interactors not previously linked to AD. All interactomes were enriched in proteins related to tau physiology and lysosomal degradation. NDAN and PART interactomes showed unique enrichment in proteins involved in cellular responses to reactive oxygen species.ConclusionsOne vulnerability-associated and 18 resilience-associated pathways that may mitigate tau-mediated neurodegeneration were identified, laying the groundwork for novel diagnostic and therapeutic strategies targeting pathological tau oligomers.

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脑源性tau寡聚物相互作用组在阿尔茨海默病、非痴呆性阿尔茨海默病神经病理学和原发性年龄相关tau病中的比较分析：对神经变性和认知弹性的影响。

在阿尔茨海默病（AD）中，可溶性tau低聚物是神经变性和认知能力下降的核心。弹性个体，如那些患有非痴呆性阿尔茨海默氏神经病理学（NDAN）或原发性年龄相关性牛头病（PART）的个体，为研究tau介导的神经退行性变的保护机制提供了重要见解。NDAN个体表现为AD神经病理，无认知障碍或神经退行性变，而PART以海马和内源性受限tau蛋白病理为特征，表现为最小至无遗忘改变。来自这些群体的脑源性tau寡聚物（BDTO）提供了一个独特的平台来探索tau病理脆弱性和恢复力背后的分子途径。目的通过比较AD、NDAN和PART的BDTO相互作用组，确定脆弱性和弹性相关途径。方法从AD中分离sbdto (n = 4；2M, 2F), NDAN (n = 4；2M, 2F), PART (n = 4；1M, 3F)海马解剖标本共免疫沉淀。通过液相色谱-串联质谱法鉴定蛋白质，使用SAINTq过滤非特异性相互作用物。相互作用组网络和富集分析使用metscape进行。研究结果与Neuropro数据库和现有的缠结相关蛋白文献进行了交叉参考。通过反向共免疫沉淀验证关键相互作用物。结果共鉴定出203个蛋白，包括8个以前未与AD关联的新相互作用蛋白。所有相互作用组都富含与tau生理和溶酶体降解相关的蛋白质。NDAN和PART相互作用组在参与细胞对活性氧反应的蛋白质中显示出独特的富集。结论发现了1种易感性相关通路和18种弹性相关通路，可减轻tau介导的神经退行性变，为针对病理性tau寡聚物的新诊断和治疗策略奠定了基础。

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来源期刊

Journal of Alzheimer's Disease 医学-神经科学

CiteScore

6.40

自引率

7.50%

发文量

1327

审稿时长

2 months

期刊介绍： The Journal of Alzheimer''s Disease (JAD) is an international multidisciplinary journal to facilitate progress in understanding the etiology, pathogenesis, epidemiology, genetics, behavior, treatment and psychology of Alzheimer''s disease. The journal publishes research reports, reviews, short communications, hypotheses, ethics reviews, book reviews, and letters-to-the-editor. The journal is dedicated to providing an open forum for original research that will expedite our fundamental understanding of Alzheimer''s disease.