| Literature DB >> 34655982 |
Erica Barini1, Gudrun Plotzky2, Yulia Mordashova3, Jonas Hoppe2, Esther Rodriguez-Correa2, Sonja Julier2, Florie LePrieult4, Ina Mairhofer4, Mario Mezler4, Sandra Biesinger2, Miroslav Cik2, Marcus W Meinhardt2, Ebru Ercan-Herbst5, Dagmar E Ehrnhoefer6, Andreas Striebinger2, Karen Bodie7, Corinna Klein2, Laura Gasparini1, Kerstin Schlegel8.
Abstract
In Alzheimer disease, Tau pathology is thought to propagate from cell to cell throughout interconnected brain areas. However, the forms of Tau released into the brain interstitial fluid (ISF) in vivo during the development of Tauopathy and their pathological relevance remain unclear. Combining in vivo microdialysis and biochemical analysis, we find that in Tau transgenic mice, human Tau (hTau) present in brain ISF is truncated and comprises at least 10 distinct fragments spanning the entire Tau protein. The fragmentation pattern is similar across different Tau transgenic models, pathological stages and brain areas. ISF hTau concentration decreases during Tauopathy progression, while its phosphorylation increases. ISF from mice with established Tauopathy induces Tau aggregation in HEK293-Tau biosensor cells. Notably, immunodepletion of ISF phosphorylated Tau, but not Tau fragments, significantly reduces its ability to seed Tau aggregation and only a fraction of Tau, separated by ultracentrifugation, is seeding-competent. These results indicate that ISF seeding competence is driven by a small subset of Tau, which potentially contribute to the propagation of Tau pathology.Entities:
Keywords: Interstitial fluid; Microdialysis; Tau aggregates; Tau phosphorylation; Transneuronal propagation
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Year: 2021 PMID: 34655982 DOI: 10.1016/j.neurobiolaging.2021.09.013
Source DB: PubMed Journal: Neurobiol Aging ISSN: 0197-4580 Impact factor: 4.673