Intraneuronal Aβ accumulation causes tau hyperphosphorylation via endolysosomal leakage

IF 13 1区医学 Q1 CLINICAL NEUROLOGY

Alzheimer's & Dementia Pub Date : 2025-03-27 DOI:10.1002/alz.70091

Yang Gao, Lisha Wang, Tosca Doeswijk, Bengt Winblad, Sophia Schedin-Weiss, Lars O. Tjernberg

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引用次数: 0

Abstract

INTRODUCTION

Alzheimer's disease (AD) is characterized by amyloid beta (Aβ) peptide plaques and intracellular neurofibrillary tangles formed by hyperphosphorylated tau. Many attempts have been made to clarify the link between Aβ and tau in the pathogenesis, but conclusive data describing a pathway for this connection are still lacking.

METHODS

We developed a neuronal model of Aβ-induced toxicity and studied downstream effects of intraneuronal Aβ42 accumulation on tau hyperphosphorylation using confocal microscopy and live cell imaging.

RESULTS

Aβ42 added to the medium was endocytosed into neurons, inducing the formation of endolysosomal protofibrils and endolysosomal leakage, which in turn promoted tau hyperphosphorylation. Asparaginyl endopeptidase (AEP) was released from the disrupted lysosomes, and inhibition of this peptidase activity reduced tau hyperphosphorylation.

DISCUSSION

The data suggest a mechanism of AD in which Aβ42 accumulates and aggregates gradually in neurons over time, leading to endolysosomal leakage and release of AEP, which subsequently triggers tau hyperphosphorylation.

Highlights

Aβ42 endocytosis leads to its endolysosomal accumulation in neurons over time.
Aβ42 polymerizes into protofibrils and causes endolysosomal leakage.
Tau hyperphosphorylation is induced by endolysosomal asparagine endopeptidase leakage.
Tau hyperphosphorylation is inhibited by an asparagine endopeptidase inhibitor.

Abstract Image

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阿尔茨海默病（AD）的特征是淀粉样 beta（Aβ）肽斑块和由高磷酸化 tau 形成的细胞内神经纤维缠结。人们曾多次尝试阐明 Aβ 和 tau 在发病机制中的联系，但仍缺乏描述这种联系途径的确凿数据。方法我们建立了 Aβ 诱导毒性的神经元模型，并使用共聚焦显微镜和活细胞成像技术研究了神经元内 Aβ42 积累对 tau 过度磷酸化的下游影响。结果添加到培养基中的 Aβ42 被内吞到神经元中，诱导形成内溶酶体原纤维和内溶酶体渗漏，进而促进 tau 过度磷酸化。天冬酰胺酰内肽酶（AEP）从被破坏的溶酶体中释放出来，抑制这种肽酶的活性可减少 tau 的过度磷酸化。讨论这些数据提示了一种 AD 的发病机制，即 Aβ42 在神经元中随着时间的推移逐渐累积和聚集，导致溶酶体内漏和 AEP 的释放，进而引发 tau 过度磷酸化。 Aβ42 内吞导致其在神经元内溶酶体中逐渐积累。 Aβ42 聚合成原纤维并导致内溶酶体渗漏。内溶酶体天冬酰胺内肽酶渗漏会诱导 Tau 过度磷酸化。天冬酰胺内肽酶抑制剂可抑制 Tau 过度磷酸化。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Alzheimer's & Dementia 医学-临床神经学

CiteScore

14.50

自引率

5.00%

发文量

299

审稿时长

3 months

期刊介绍： Alzheimer's & Dementia is a peer-reviewed journal that aims to bridge knowledge gaps in dementia research by covering the entire spectrum, from basic science to clinical trials to social and behavioral investigations. It provides a platform for rapid communication of new findings and ideas, optimal translation of research into practical applications, increasing knowledge across diverse disciplines for early detection, diagnosis, and intervention, and identifying promising new research directions. In July 2008, Alzheimer's & Dementia was accepted for indexing by MEDLINE, recognizing its scientific merit and contribution to Alzheimer's research.