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Literature DB >> 26931569

The Tau/A152T mutation, a risk factor for frontotemporal-spectrum disorders, leads to NR2B receptor-mediated excitotoxicity.

Jochen Martin Decker¹, Lars Krüger¹, Astrid Sydow², Frank Ja Dennissen¹, Zuzana Siskova¹, Eckhard Mandelkow³, Eva-Maria Mandelkow⁴.

Abstract

We report on a novel transgenic mouse model expressing human full-length Tau with the Tau mutation A152T (hTau(AT)), a risk factor for FTD-spectrum disorders including PSP and CBD Brain neurons reveal pathological Tau conformation, hyperphosphorylation, mis-sorting, aggregation, neuronal degeneration, and progressive loss, most prominently in area CA3 of the hippocampus. The mossy fiber pathway shows enhanced basal synaptic transmission without changes in short- or long-term plasticity. In organotypic hippocampal slices, extracellular glutamate increases early above control levels, followed by a rise in neurotoxicity. These changes are normalized by inhibiting neurotransmitter release or by blocking voltage-gated sodium channels. CA3 neurons show elevated intracellular calcium during rest and after activity induction which is sensitive to NR2B antagonizing drugs, demonstrating a pivotal role of extrasynaptic NMDA receptors. Slices show pronounced epileptiform activity and axonal sprouting of mossy fibers. Excitotoxic neuronal death is ameliorated by ceftriaxone, which stimulates astrocytic glutamate uptake via the transporter EAAT2/GLT1. In summary, hTau(AT) causes excitotoxicity mediated by NR2B-containing NMDA receptors due to enhanced extracellular glutamate.

Entities: Chemical Disease Gene Mutation Species

Keywords: CA3; NR2B; Tau; excitotoxicity; frontotemporal‐spectrum disorders

Mesh：

Substances：

Year: 2016 PMID： 26931569 PMCID： PMC4818782 DOI： 10.15252/embr.201541439

Source DB: PubMed Journal: EMBO Rep ISSN： 1469-221X Impact factor: 8.807

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