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A synapsin Ⅰ cleavage fragment contributes to synaptic dysfunction in Alzheimer's disease

Lanxia Meng, Li Zou, Min Xiong, Jiehui Chen, Xingyu Zhang, Ting Yu, Yiming Li, Congcong Liu, Guiqin Chen, Zhihao Wang, Keqiang Ye, Zhentao Zhang

2022Aging Cell40 citationsDOIOpen Access PDF

Abstract

Synaptic dysfunction is a key feature of Alzheimer's disease (AD). However, the molecular mechanisms underlying synaptic dysfunction remain unclear. Here, we show that synapsin Ⅰ, one of the most important synaptic proteins, is fragmented by the cysteine proteinase asparagine endopeptidase (AEP). AEP cleaves synapsin at N82 in the brains of AD patients and generates the C-terminal synapsin Ⅰ (83-705) fragment. This fragment is abnormally distributed in neurons and induces synaptic dysfunction. Overexpression of AEP in the hippocampus of wild-type mice results in the production of the synapsin Ⅰ (83-705) fragment and induces synaptic dysfunction and cognitive deficits. Moreover, overexpression of the AEP-generated synapsin Ⅰ (83-705) fragment in the hippocampus of tau P301S transgenic mice and wild-type mice promotes synaptic dysfunction and cognitive deficits. These findings suggest a novel mechanism of synaptic dysfunction in AD.

Topics & Concepts

SynapsinSynapsin IBiologyNeuroscienceHippocampusSynaptic plasticitySynaptophysinCalpainSynaptic fatigueExcitatory postsynaptic potentialBiochemistryImmunologySynaptic vesicleReceptorInhibitory postsynaptic potentialEnzymeImmunohistochemistryMembraneVesiclePeptidase Inhibition and AnalysisAlzheimer's disease research and treatmentsCellular transport and secretion