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PIKfyve activity is required for lysosomal trafficking of tau aggregates and tau seeding

Alberto Carpinteiro Soares, Andreia Ferreira, Jonas Mariën, Charlotte Delay, Edward B. Lee, John Q. Trojanowski, Dieder Moechars, Wim Annaert, Louis De Muynck

2021Journal of Biological Chemistry41 citationsDOIOpen Access PDF

Abstract

Tauopathies, such as Alzheimer's disease (AD), are neurodegenerative disorders characterized by the deposition of hyperphosphorylated tau aggregates. Proteopathic tau seeds spread through the brain in a temporospatial pattern, indicative of transsynaptic propagation. It is hypothesized that reducing the uptake of tau seeds and subsequent induction of tau aggregation could be a potential approach for abrogating disease progression in AD. Here, we studied to what extent different endosomal routes play a role in the neuronal uptake of preformed tau seeds. Using pharmacological and genetic tools, we identified dynamin-1, actin, and Rac1 as key players. Furthermore, inhibition of PIKfyve, a protein downstream of Rac1, reduced both the trafficking of tau seeds into lysosomes and the induction of tau aggregation. Our work shows that tau aggregates are internalized by a specific endocytic mechanism and that their fate once internalized can be pharmacologically modulated to reduce tau seeding in neurons.

Topics & Concepts

Tau proteinCell biologyDynaminEndocytic cycleEndocytosisEndosomeNeurodegenerationChemistryBiologyNeuroscienceAlzheimer's diseaseBiochemistryCellDiseaseInternal medicineMedicineIntracellularAlzheimer's disease research and treatmentsCellular transport and secretionNeuroscience and Neuropharmacology Research
PIKfyve activity is required for lysosomal trafficking of tau aggregates and tau seeding | Litcius