Falker Clemens, Hartmann Alexander, Guett Inga, Dohler Frank, Altmeppen Hermann, Betzel Christian, Schubert Robin, Thurm Dana, Wegwitz Florian, Joshi Pooja, Verderio Claudia, Krasemann Susanne, Glatzel Markus
Institute of Neuropathology, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.
Laboratory of Structural Biology of Infection and Inflammation, Institute of Biochemistry and Molecular Biology, University of Hamburg, Hamburg, Germany.
J Neurochem. 2016 Apr;137(1):88-100. doi: 10.1111/jnc.13514. Epub 2016 Mar 2.
Alzheimer's disease is a common neurodegenerative, progressive, and fatal disorder. Generation and deposition of amyloid beta (Aβ) peptides associate with its pathogenesis and small soluble Aβ oligomers show the most pronounced neurotoxic effects and correlate with disease initiation and progression. Recent findings showed that Aβ oligomers bind to the cellular prion protein (PrP(C) ) eliciting neurotoxic effects. The role of exosomes, small extracellular vesicles of endosomal origin, in Alzheimer's disease is only poorly understood. Besides serving as disease biomarkers they may promote Aβ plaque formation, decrease Aβ-mediated synaptotoxicity, and enhance Aβ clearance. Here, we explore how exosomal PrP(C) connects to protective functions attributed to exosomes in Alzheimer's disease. To achieve this, we generated a mouse neuroblastoma PrP(C) knockout cell line using transcription activator-like effector nucleases. Using these, as well as SH-SY5Y human neuroblastoma cells, we show that PrP(C) is highly enriched on exosomes and that exosomes bind amyloid beta via PrP(C) . Exosomes showed highest binding affinity for dimeric, pentameric, and oligomeric Aβ species. Thioflavin T assays revealed that exosomal PrP(C) accelerates fibrillization of amyloid beta, thereby reducing neurotoxic effects imparted by oligomeric Aβ. Our study provides further evidence for a protective role of exosomes in Aβ-mediated neurodegeneration and highlights the importance of exosomal PrP(C) in molecular mechanisms of Alzheimer's disease. We show that the prion protein (PrP(C) ) on exosomes captures neurotoxic species of amyloid beta (Aβ) promoting its fibrillization. Our study provides evidence for a protective role of exosomes in Alzheimer`s disease and suggests that, depending on its membrane topology, PrP(C) holds a dual function: when expressed at the neuronal surface it acts as receptor for Aβ leading to neurotoxic signaling, whereas it detoxifies Aβ when present on exosomes. This provides further support for key roles of PrP(C) in Alzheimer's disease.
阿尔茨海默病是一种常见的神经退行性、进行性和致命性疾病。淀粉样β(Aβ)肽的产生和沉积与其发病机制相关,小的可溶性Aβ寡聚体表现出最显著的神经毒性作用,并与疾病的起始和进展相关。最近的研究发现表明,Aβ寡聚体与细胞朊蛋白(PrP(C))结合,引发神经毒性作用。外泌体是内体来源的小细胞外囊泡,其在阿尔茨海默病中的作用仍知之甚少。除了作为疾病生物标志物外,它们可能促进Aβ斑块形成,降低Aβ介导的突触毒性,并增强Aβ清除。在这里,我们探讨外泌体PrP(C)如何与阿尔茨海默病中外泌体的保护功能相关联。为了实现这一目标,我们使用转录激活样效应核酸酶生成了一种小鼠神经母细胞瘤PrP(C)敲除细胞系。利用这些细胞系以及SH-SY5Y人神经母细胞瘤细胞,我们表明PrP(C)在外泌体上高度富集,并且外泌体通过PrP(C)与淀粉样β结合。外泌体对二聚体、五聚体和寡聚体Aβ物种表现出最高的结合亲和力。硫黄素T分析表明,外泌体PrP(C)加速淀粉样β的纤维化,从而降低寡聚体Aβ所带来的神经毒性作用。我们的研究为外泌体在Aβ介导的神经退行性变中的保护作用提供了进一步的证据,并突出了外泌体PrP(C)在阿尔茨海默病分子机制中的重要性。我们表明,外泌体上的朊蛋白(PrP(C))捕获淀粉样β(Aβ)的神经毒性物种,促进其纤维化。我们的研究为外泌体在阿尔茨海默病中的保护作用提供了证据,并表明,根据其膜拓扑结构,PrP(C)具有双重功能:当在神经元表面表达时,它作为Aβ的受体,导致神经毒性信号传导,而当存在于外泌体上时,它使Aβ解毒。这为PrP(C)在阿尔茨海默病中的关键作用提供了进一步的支持。
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