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Complement receptor 4 mediates the clearance of extracellular tau fibrils by microglia

Authors
유창재Choi, Youngtae복유진Lin, Yuxi천무경Lee, Young‐HoKim, Jaekwang
Issue Date
May-2024
Publisher
Blackwell Publishing Inc.
Keywords
Alzheimer's disease; complement receptor 4; microglia; tau fibril; tauopathy
Citation
FEBS Journal
Journal Title
FEBS Journal
URI
http://scholarworks.bwise.kr/kbri/handle/2023.sw.kbri/1171
DOI
10.1111/febs.17150
ISSN
1742-464X
1742-4658
Abstract
<jats:p>Tauopathies exhibit a characteristic accumulation of misfolded tau aggregates in the brain. Tau pathology shows disease‐specific spatiotemporal propagation through intercellular transmission, which is closely correlated with the progression of clinical manifestations. Therefore, identifying molecular mechanisms that prevent tau propagation is critical for developing therapeutic strategies for tauopathies. The various innate immune receptors, such as complement receptor 3 (CR3) and complement receptor 4 (CR4), have been reported to play a critical role in the clearance of various extracellular toxic molecules by microglia. However, their role in tau clearance has not been studied yet. In the present study, we investigated the role of CR3 and CR4 in regulating extracellular tau clearance. We found that CR4 selectively binds to tau fibrils but not to tau monomers, whereas CR3 does not bind to either of them. Inhibiting CR4, but not CR3, significantly reduces the uptake of tau fibrils by BV2 cells and primary microglia. By contrast, inhibiting CR4 has no effect on the uptake of tau monomers by BV2 cells. Furthermore, inhibiting CR4 suppresses the clearance of extracellular tau fibrils, leading to more seed‐competent tau fibrils remaining in the extracellular space relative to control samples. We also provide evidence that the expression of CR4 is upregulated in the brains of human Alzheimer's disease patients and the PS19 mouse model of tauopathy. Taken together, our data strongly support that CR4 is a previously undescribed receptor for the clearance of tau fibrils in microglia and may represent a novel therapeutic target for tauopathy.</jats:p>
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