Tau fragmentation, aggregation and clearance: the dual role of lysosomal processing

doi:10.1093/hmg/ddp367

Human Molecular Genetics Advance Access originally published online on August 4, 2009
Human Molecular Genetics 2009 18(21):4153-4170; doi:10.1093/hmg/ddp367

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Tau fragmentation, aggregation and clearance: the dual role of lysosomal processing

Yipeng Wang¹, Marta Martinez-Vicente², Ulrike Krüger¹, Susmita Kaushik², Esther Wong², Eva-Maria Mandelkow¹, Ana Maria Cuervo² and Eckhard Mandelkow¹^,*

¹ Max-Planck-Unit for Structural Molecular Biology, Notkestrasse 85, 22607 Hamburg, Germany ² Departments of Developmental and Molecular Biology and of Anatomy and Structural Biology, Marion Bessin Liver Research Center, Albert Einstein College of Medicine, Bronx, NY 10461, USA

^* To whom correspondence should be addressed. Fax: +49 4089716810; Email: mand{at}mpasmb.desy.de

Received May 14, 2009; Accepted July 29, 2009

Aggregation and cleavage are two hallmarks of Tau pathologyin Alzheimer disease (AD), and abnormal fragmentation of Tauis thought to contribute to the nucleation of Tau paired helicalfilaments. Clearance of the abnormally modified protein couldoccur by the ubiquitin–proteasome and autophagy–lysosomalpathways, the two major routes for protein degradation in cells.There is a debate on which of these pathways contributes toclearance of Tau protein and of the abnormal Tau aggregatesformed in AD. Here, we demonstrate in an inducible neuronalcell model of tauopathy that the autophagy–lysosomal systemcontributes to both Tau fragmentation into pro-aggregating formsand to clearance of Tau aggregates. Inhibition of macroautophagyenhances Tau aggregation and cytotoxicity. The Tau repeat domaincan be cleaved near the N terminus by a cytosolic protease togenerate the fragment F1. Additional cleavage near the C terminusby the lysosomal protease cathepsin L is required to generateTau fragments F2 and F3 that are highly amyloidogenic and capableof seeding the aggregation of Tau. We identify in this workthat components of a selective form of autophagy, chaperone-mediatedautophagy, are involved in the delivery of cytosolic Tau tolysosomes for this limited cleavage. However, F1 does not fullyenter the lysosome but remains associated with the lysosomalmembrane. Inefficient translocation of the Tau fragments acrossthe lysosomal membrane seems to promote formation of Tau oligomersat the surface of these organelles which may act as precursorsof aggregation and interfere with lysosomal functioning.

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