APP β-CTF triggers cell-autonomous synaptic toxicity independent of Aβ

bioRxiv Pub Date : 2024-07-16 DOI:10.1101/2024.07.11.603028
Mengxun Luo, Jia Zhou, Cailu Sun, Wanjia Chen, Chaoying Fu, Chenfang Si, Yaoyang Zhang, Yang Geng, Yelin Chen
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Abstract

Aβ is believed to play a significant role in synaptic degeneration observed in Alzheimer’s disease (AD) and is primarily investigated as a secreted peptide. However, the contribution of intracellular Aβ or other cleavage products of its precursor protein (APP) to synaptic loss remains uncertain. In this study, we conducted a systematic examination of their cell-autonomous impact using a sparse expression system. Here, these proteins/peptides were overexpressed in a single neuron, surrounded by thousands of untransfected neurons. Surprisingly, we found that APP induced dendritic spine loss only when co-expressed with BACE1. This effect was mediated by β-CTF, a β-cleavage product of APP, through an endosome-related pathway independent of Aβ. Neuronal expression of β-CTF in mouse brains resulted in defective synaptic transmission and cognitive impairments, even in the absence of amyloid plaques. These findings unveil a β-CTF-initiated mechanism driving synaptic toxicity irrespective of amyloid plaque formation and suggest a potential intervention by inhibiting the endosomal GTPase Rab5.
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APP β-CTF触发独立于Aβ的细胞自主突触毒性
据信,Aβ在阿尔茨海默病(AD)的突触退化中起着重要作用,目前主要作为一种分泌肽进行研究。然而,细胞内 Aβ 或其前体蛋白(APP)的其他裂解产物对突触丧失的贡献仍不确定。在本研究中,我们利用稀疏表达系统对它们对细胞自主性的影响进行了系统性研究。在这里,这些蛋白/肽被过量表达在单个神经元中,周围是成千上万个未转染的神经元。令人惊讶的是,我们发现只有当APP与BACE1共同表达时,APP才会诱导树突棘丧失。这种效应是由β-CTF介导的,β-CTF是APP的β-裂解产物,通过独立于Aβ的内含体相关途径产生。小鼠大脑神经元表达β-CTF会导致突触传递缺陷和认知障碍,即使没有淀粉样斑块也是如此。这些发现揭示了无论淀粉样斑块是否形成,β-CTF都会引发突触毒性的机制,并提出了通过抑制内体GTP酶Rab5进行干预的可能性。
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