Distinct regulation of Tau Monomer and aggregate uptake and intracellular 
accumulation in human neurons

Marvian, A.T.; Strauss, T.; Tang, Q.; Tuck, B.J.; Keeling, S.; Rüdiger, D.; Mirzazadeh Dizaji, N.; Mohammad-Beigi, H.; Nuscher, B.; Chakraborty, Pijush; Sutherland, D.S.; McEwan, W.A.; Köglsperger, T.; Zahler, S.; Zweckstetter, Markus; Lichtenthaler, S.F.; Wurst, W.; Schwarz, S.; Höglinger, G.

doi:10.1186/s13024-024-00786-w

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Distinct regulation of Tau Monomer and aggregate uptake and intracellular accumulation in human neurons

Marvian, A., Strauss, T., Tang, Q., Tuck, B., Keeling, S., Rüdiger, D., et al. (2024). Distinct regulation of Tau Monomer and aggregate uptake and intracellular accumulation in human neurons. Molecular Neurodegeneration, 19: 100. doi:10.1186/s13024-024-00786-w.

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Datensatz-Permalink: https://hdl.handle.net/21.11116/0000-0010-62AE-C Versions-Permalink: https://hdl.handle.net/21.11116/0000-0010-62AF-B

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Urheber:
Marvian, A.T., Autor
Strauss, T., Autor
Tang, Q., Autor
Tuck, B.J., Autor
Keeling, S., Autor
Rüdiger, D., Autor
Mirzazadeh Dizaji, N., Autor
Mohammad-Beigi, H., Autor
Nuscher, B., Autor
Chakraborty, Pijush¹, Autor
Sutherland, D.S., Autor
McEwan, W.A., Autor
Köglsperger, T., Autor
Zahler, S., Autor
Zweckstetter, Markus^{1, 2}, Autor
Lichtenthaler, S.F., Autor
Wurst, W., Autor
Schwarz, S., Autor
Höglinger, G., Autor

Affiliations:
1Department of NMR Based Structural Biology, Max Planck Institute for Multidisciplinary Sciences, Max Planck Society, ou_3350124
2Research Group of Protein Structure Determination using NMR, Max Planck Institute for Multidisciplinary Sciences, Max Planck Society, ou_3350128

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Zusammenfassung: Background:
The prion-like spreading of Tau pathology is the leading cause of disease progression in various tauopathies. A critical step in propagating pathologic Tau in the brain is the transport from the extracellular environment and accumulation inside naïve neurons. Current research indicates that human neurons internalize both the physiological extracellular Tau (eTau) monomers and the pathological eTau aggregates. However, similarities or differences in neuronal transport mechanisms between Tau species remain elusive.

Method:
Monomers, oligomers, and fibrils of recombinant 2N4R Tau were produced and characterized by biochemical and biophysical methods. A neuronal eTau uptake and accumulation assay was developed for human induced pluripotent stem cell-derived neurons (iPSCNs) and Lund human mesencephalic cells (LUHMES)-derived neurons. Mechanisms of uptake and cellular accumulation of eTau species were studied by using small molecule inhibitors of endocytic mechanisms and siRNAs targeting Tau uptake mediators.

Results:
Extracellular Tau aggregates accumulated more than monomers in human neurons, mainly due to the higher efficiency of small fibrillar and soluble oligomeric aggregates in intraneuronal accumulation. A competition assay revealed a distinction in the neuronal accumulation between physiological eTau Monomers and pathology-relevant aggregates, suggesting differential transport mechanisms. Blocking heparan sulfate proteoglycans (HSPGs) with heparin only inhibited the accumulation of eTau aggregates, whereas monomers’ uptake remained unaltered. At the molecular level, the downregulation of genes involved in HSPG synthesis exclusively blocked neuronal accumulation of eTau aggregates but not monomers, suggesting its role in the transport of pathologic Tau. Moreover, the knockdown of LRP1, as a receptor of Tau, mainly reduced the accumulation of monomeric form, confirming its involvement in Tau’s physiological transport.

Conclusion:
These data propose that despite the similarity in the cellular mechanism, the uptake and accumulation of eTau Monomers and aggregates in human neurons are regulated by different molecular mediators. Thus, they address the possibility of targeting the pathological spreading of Tau aggregates without disturbing the probable physiological or non-pathogenic transport of Tau Monomers.

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Sprache(n): eng - English

Datum: Online veröffentlicht: 2024-12-31

Publikationsstatus: Online veröffentlicht

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Art der Begutachtung: Expertenbegutachtung

Identifikatoren: DOI: 10.1186/s13024-024-00786-w

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Projektname : IMPRiND

Grant ID : 116060

Förderprogramm : Horizon 2020 (H2020)

Förderorganisation : European Commission (EC)

Projektname : LLPS-NMR

Grant ID : 787679

Förderprogramm : Horizon 2020 (H2020)

Förderorganisation : European Commission (EC)

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Titel: Molecular Neurodegeneration

Kurztitel : Mol Neurodegeneration

Genre der Quelle: Zeitschrift

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Ort, Verlag, Ausgabe: BioMedCentral

Seiten: - Band / Heft: 19 Artikelnummer: 100 Start- / Endseite: - Identifikator: Anderer: ISSN
CoNE: https://pure.mpg.de/cone/journals/resource/1750-1326