Tau Protein Disrupts Nucleocytoplasmic Transport in Alzheimer’s Disease

Bahareh Eftekharzadeh,Sarah L Devos,Julia Schiantarelli,Susanne Wegmann,Jeannie Chew,Bianca T Corjuc,Michael Deture,Eckhard Mandelkow,Leonard Petrucelli,Svetlana Vidensky,Larisa E Kapinos,J Gavin Daigle,Casey Cook,Rachel E Bennett,Katharina Tepper,Yari Carlomagno,Jeffrey D Rothstein,Simon Dujardin,Jonathan C Grima,Fred H Gage,Bradley T Hyman,Xavier Salvatella,Roderick Y H Lim ,Charles Vanderburg ,André Cestonaro Do Amaral ,Jérôme Mertens ,Juan C Troncoso ,José Emilio Caballero González ,Sean Miller ,Alyssa N Coyne

doi:10.1016/j.neuron.2018.07.039

Abstract

Tau is the major constituent of neurofibrillary tangles in Alzheimer's disease (AD), but the mechanism underlying tau-associated neural damage remains unclear. Here, we show that tau can directly interact with nucleoporins of the nuclear pore complex (NPC) and affect their structural and functional integrity. Pathological tau impairs nuclear import and export in tau-overexpressing transgenic mice and in human AD brain tissue. Furthermore, the nucleoporin Nup98 accumulates in the cell bodies of some tangle-bearing neurons and can facilitate tau aggregation invitro. These data support the hypothesis that tau can directly interact with NPC components, leading to their mislocalization and consequent disruption of NPC function. This raises the possibility that NPC dysfunction contributes to tau-induced neurotoxicity in AD and tauopathies.

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