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突触淀粉样β寡聚体先于磷酸化tau蛋白出现,并可区分高病理学对照病例。

Synaptic Amyloid-β Oligomers Precede p-Tau and Differentiate High Pathology Control Cases.

作者信息

Bilousova Tina, Miller Carol A, Poon Wayne W, Vinters Harry V, Corrada Maria, Kawas Claudia, Hayden Eric Y, Teplow David B, Glabe Charles, Albay Ricardo, Cole Gregory M, Teng Edmond, Gylys Karen H

机构信息

University of California Los Angeles School of Nursing, Los Angeles, California; Mary S. Easton Center for Alzheimer's Research at the University of California Los Angeles, Los Angeles, California.

Departments of Pathology, Neurology, and the Program in Neuroscience, University of Southern California Keck School of Medicine, Los Angeles, California.

出版信息

Am J Pathol. 2016 Jan;186(1):185-98. doi: 10.1016/j.ajpath.2015.09.018.

DOI:10.1016/j.ajpath.2015.09.018
PMID:26718979
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4715217/
Abstract

Amyloid-β (Aβ) and hyperphosphorylated tau (p-tau) aggregates form the two discrete pathologies of Alzheimer disease (AD), and oligomeric assemblies of each protein are localized to synapses. To determine the sequence by which pathology appears in synapses, Aβ and p-tau were quantified across AD disease stages in parietal cortex. Nondemented cases with high levels of AD-related pathology were included to determine factors that confer protection from clinical symptoms. Flow cytometric analysis of synaptosome preparations was used to quantify Aβ and p-tau in large populations of individual synaptic terminals. Soluble Aβ oligomers were assayed by a single antibody sandwich enzyme-linked immunosorbent assay. Total in situ Aβ was elevated in patients with early- and late-stage AD dementia, but not in high pathology nondemented controls compared with age-matched normal controls. However, soluble Aβ oligomers were highest in early AD synapses, and this assay distinguished early AD cases from high pathology controls. Overall, synapse-associated p-tau did not increase until late-stage disease in human and transgenic rat cortex, and p-tau was elevated in individual Aβ-positive synaptosomes in early AD. These results suggest that soluble oligomers in surviving neocortical synaptic terminals are associated with dementia onset and suggest an amyloid cascade hypothesis in which oligomeric Aβ drives phosphorylated tau accumulation and synaptic spread. These results indicate that antiamyloid therapies will be less effective once p-tau pathology is developed.

摘要

淀粉样β蛋白(Aβ)和高度磷酸化的tau蛋白(p-tau)聚集体构成了阿尔茨海默病(AD)的两种不同病理特征,并且每种蛋白的寡聚体都定位于突触。为了确定病理特征在突触中出现的顺序,我们在顶叶皮质的AD疾病各阶段对Aβ和p-tau进行了定量分析。纳入了具有高水平AD相关病理特征的非痴呆病例,以确定能够预防临床症状的因素。利用对突触体标本的流式细胞术分析来定量大量单个突触终末中的Aβ和p-tau。可溶性Aβ寡聚体通过单抗体夹心酶联免疫吸附测定法进行检测。与年龄匹配的正常对照相比,早期和晚期AD痴呆患者原位Aβ总量升高,但高病理特征的非痴呆对照中未升高。然而,可溶性Aβ寡聚体在早期AD突触中含量最高,并且该检测方法能够将早期AD病例与高病理特征对照区分开来。总体而言,在人类和转基因大鼠皮质中,突触相关的p-tau直到疾病晚期才增加,并且在早期AD中,单个Aβ阳性突触体中的p-tau升高。这些结果表明,存活的新皮质突触终末中的可溶性寡聚体与痴呆症的发病有关,并提示了一种淀粉样蛋白级联假说,即寡聚体Aβ驱动磷酸化tau蛋白的积累和突触扩散。这些结果表明,一旦p-tau病理特征形成,抗淀粉样蛋白疗法的效果将降低。

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