Self-Aggregating Tau Fragments Recapitulate Pathologic Phenotypes and Neurotoxicity of Alzheimer's Disease in Mice

Authors
Le, Ly Thi Huong LuuLee, JeeyoungIm, DongjoonPark, SunhaHwang, Kyoung-DooLee, Jung HoonJiang, YanxialeiLee, Yong-SeokSuh, Young HoKim, Hugh I.Lee, Min Jae
Issue Date
2023-10
Publisher
Wiley-VCH Verlag
Citation
Advanced Science, v.10, no.29
Abstract
In tauopathy conditions, such as Alzheimer's disease (AD), highly soluble and natively unfolded tau polymerizes into an insoluble filament; however, the mechanistic details of this process remain unclear. In the brains of AD patients, only a minor segment of tau forms & beta;-helix-stacked protofilaments, while its flanking regions form disordered fuzzy coats. Here, it is demonstrated that the tau AD nucleation core (tau-AC) sufficiently induced self-aggregation and recruited full-length tau to filaments. Unexpectedly, phospho-mimetic forms of tau-AC (at Ser324 or Ser356) show markedly reduced oligomerization and seeding propensities. Biophysical analysis reveal that the N-terminus of tau-AC facilitates the fibrillization kinetics as a nucleation motif, which becomes sterically shielded through phosphorylation-induced conformational changes in tau-AC. Tau-AC oligomers are efficiently internalized into cells via endocytosis and induced endogenous tau aggregation. In primary hippocampal neurons, tau-AC impaired axon initial segment plasticity upon chronic depolarization and is mislocalized to the somatodendritic compartments. Furthermore, it is observed significantly impaired memory retrieval in mice intrahippocampally injected with tau-AC fibrils, which corresponds to the neuropathological staining and neuronal loss in the brain. These findings identify tau-AC species as a key neuropathological driver in AD, suggesting novel strategies for therapeutic intervention.
Keywords
PAIRED HELICAL FILAMENT; POSTTRANSLATIONAL MODIFICATIONS; PROTEIN; TAUOPATHY; REQUIRES; NEURONS; CORE; aggregation; Alzheimer' s disease; axon initial segment; phosphorylation; tau
ISSN
2198-3844
URI
https://pubs.kist.re.kr/handle/201004/113228
DOI
10.1002/advs.202302035
Appears in Collections:
KIST Article > 2023
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