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源自阿尔茨海默病的纤维状和寡聚体tau蛋白均支持tau蛋白在体内的播种和传播。

Tau seeding and spreading in vivo is supported by both AD-derived fibrillar and oligomeric tau.

作者信息

Mate de Gerando Anastasie, Welikovitch Lindsay A, Khasnavis Anita, Commins Caitlin, Glynn Calina, Chun Joshua E, Perbet Romain, Hyman Bradley T

出版信息

bioRxiv. 2023 May 26:2023.03.28.534418. doi: 10.1101/2023.03.28.534418.

DOI:10.1101/2023.03.28.534418
PMID:37034629
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10081282/
Abstract

Insoluble fibrillar tau, the primary constituent of neurofibrillary tangles, has traditionally been thought to be the biologically active, toxic form of tau mediating neurodegeneration in Alzheimer's disease. More recent studies have implicated soluble oligomeric tau species, referred to as high molecular weight (HMW) due to its properties on size exclusion chromatography, in tau propagation across neural systems. These two forms of tau have never been directly compared. We prepared sarkosyl insoluble and HMW tau from the frontal cortex of Alzheimer patients and compared their properties using a variety of biophysical and bioactivity assays. Sarkosyl insoluble fibrillar tau is comprised of abundant paired helical filaments (PHF) as quantified by electron microscopy (EM), and is more resistant to proteinase K, compared to HMW tau which is mostly in an oligomeric form. Sarkosyl insoluble and HMW tau are nearly equivalent in potency in a HEK cell bioactivity assay for seeding aggregates and their injection reveals similar local uptake into hippocampal neurons in PS19 Tau transgenic mice. However, the HMW preparation appears to be far more potent in inducing a glial response including Clec7a-positive rod-microglia in the absence of neurodegeneration or synapse loss and promotes more rapid propagation of misfolded tau to distal, anatomically connected regions, such as entorhinal and perirhinal cortices. These data suggest that soluble HMW tau has similar properties to fibrillar sarkosyl insoluble tau with regard to tau seeding potential but may be equal or even more bioactive with respect to propagation across neural systems and activation of glial responses, both relevant tau-related Alzheimer phenotypes.

摘要

不溶性纤维状tau蛋白是神经原纤维缠结的主要成分,传统上一直被认为是介导阿尔茨海默病神经退行性变的具有生物活性的毒性tau蛋白形式。最近的研究表明,可溶性寡聚tau蛋白物种,由于其在尺寸排阻色谱上的特性而被称为高分子量(HMW),在tau蛋白跨神经系统传播中起作用。这两种形式的tau蛋白从未被直接比较过。我们从阿尔茨海默病患者的额叶皮质制备了 Sarkosyl 不溶性和 HMW tau蛋白,并使用各种生物物理和生物活性测定方法比较了它们的特性。通过电子显微镜(EM)定量,Sarkosyl 不溶性纤维状tau蛋白由大量双螺旋丝(PHF)组成,与主要呈寡聚形式的HMW tau蛋白相比,对蛋白酶K更具抗性。在用于接种聚集体的HEK细胞生物活性测定中,Sarkosyl不溶性和HMW tau蛋白的效力几乎相同,并且它们的注射显示在PS19 Tau转基因小鼠的海马神经元中具有相似的局部摄取。然而,在没有神经退行性变或突触丧失的情况下,HMW制剂在诱导包括Clec7a阳性杆状小胶质细胞在内的神经胶质反应方面似乎更有效,并促进错误折叠的tau蛋白更快地传播到远端、解剖学上相连的区域,如内嗅皮质和鼻周皮质。这些数据表明,可溶性HMW tau蛋白在tau蛋白播种潜力方面与纤维状Sarkosyl不溶性tau蛋白具有相似的特性,但在跨神经系统传播和神经胶质反应激活方面可能具有同等甚至更高的生物活性,这两种都是与tau蛋白相关的阿尔茨海默病表型。

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