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tau免疫反应性海马颗粒和淀粉样体的积累表明衰老过程中反应性胶质细胞参与tau蛋白致病机制。

The Accumulation of Tau-Immunoreactive Hippocampal Granules and Corpora Amylacea Implicates Reactive Glia in Tau Pathogenesis during Aging.

作者信息

Wander Connor M, Tseng Jui-Heng, Song Sheng, Al Housseiny Heba A, Tart Dalton S, Ajit Aditi, Ian Shih Yen-Yu, Lobrovich Rebecca, Song Juan, Meeker Rick B, Irwin David J, Cohen Todd J

机构信息

Department of Pharmacology, University of North Carolina, Chapel Hill, NC 27599, USA.

Department of Neurology, University of North Carolina, Chapel Hill, NC 27599, USA.

出版信息

iScience. 2020 Jul 24;23(7):101255. doi: 10.1016/j.isci.2020.101255. Epub 2020 Jun 10.

Abstract

The microtubule-associated tau protein forms pathological inclusions that accumulate in an age-dependent manner in tauopathies including Alzheimer's disease (AD). Since age is the major risk factor for AD, we examined endogenous tau species that evolve during aging in physiological and diseased conditions. In aged mouse brain, we found tau-immunoreactive clusters embedded within structures that are reminiscent of periodic acid-Schiff (PAS) granules. We showed that PAS granules harbor distinct tau species that are more prominent in 3xTg-AD mice. Epitope profiling revealed hypo-phosphorylated rather than hyper-phosphorylated tau commonly observed in tauopathies. High-resolution imaging and 3D reconstruction suggest a link between tau clusters, reactive astrocytes, and microglia, indicating that early tau accumulation may promote neuroinflammation during aging. Using postmortem human brain, we identified tau as a component of corpora amylacea (CA), age-related structures that are functionally analogous to PAS granules. Overall, our study supports neuroimmune dysfunction as a precipitating event in tau pathogenesis.

摘要

与微管相关的tau蛋白形成病理性包涵体,这些包涵体在包括阿尔茨海默病(AD)在内的tau蛋白病中以年龄依赖性方式积累。由于年龄是AD的主要风险因素,我们研究了在生理和疾病条件下衰老过程中演变的内源性tau蛋白种类。在老年小鼠大脑中,我们发现tau免疫反应性簇嵌入类似于过碘酸希夫(PAS)颗粒的结构中。我们表明,PAS颗粒含有不同的tau蛋白种类,在3xTg-AD小鼠中更为突出。表位分析显示,tau蛋白病中常见的是低磷酸化而非高磷酸化的tau蛋白。高分辨率成像和三维重建表明tau蛋白簇、反应性星形胶质细胞和小胶质细胞之间存在联系,表明tau蛋白的早期积累可能在衰老过程中促进神经炎症。利用死后的人脑,我们确定tau蛋白是老年淀粉样体(CA)的一个组成部分,CA是与年龄相关的结构,在功能上类似于PAS颗粒。总体而言,我们的研究支持神经免疫功能障碍是tau蛋白发病机制中的一个促发事件。

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