Functional spreading of hyperexcitability induced by human and synthetic intracellular Aβ oligomers

Eduardo J. Fernandez-Perez
Braulio Muñoz
Denisse A. Bascuñan
Christian Peters
Nicolas O. Riffo-Lepe
Maria P. Espinoza
Peter J. Morgan
Caroline Filippi
Romain Bourboulou
Urmi Sengupta
Rakez Kayed
Jérôme Epsztein
Luis G. Aguayo

4 evaluations Published on Oct 17, 2020

This article on Sciety

Abstract

Background

Intracellular amyloid-beta oligomers (iAβo) accumulation and neuronal hyperexcitability are two crucial events at early stages of Alzheimer’s disease (AD). However, to date, no mechanism linking them has been reported.

Methods

Here, the effects of human AD brain-derived (h-iAβo) and synthetic (iAβo) peptides on synaptic currents and action potential (AP) firing were investigated in hippocampal neuronsin vitro, ex vivoandin vivo.

Results

Starting from 500 pM, iAβo rapidly increased the frequency of synaptic currents and higher concentrations potentiated the AMPA receptor-mediated current. Both effects were PKC-dependent. Parallel recordings of synaptic currents and nitric oxide (NO)-related fluorescence changes indicated that the increased frequency, related to pre-synaptic release, was dependent on a NO-mediated retrograde signaling. Moreover, increased synchronization in NO production was also observed in neurons neighboring those dialyzed with iAβo, indicating that iAβo can increase network excitability at a distance. Current-clamp recordings suggested that iAβo increased neuronal excitability via AMPA-driven synaptic activity without altering membrane intrinsic properties.

Conclusion

These results strongly indicate that iAβo causes functional spreading of hyperexcitability through a synaptic-driven mechanism and offer an important neuropathological significance to intracellular species in the initial stages of AD, which include brain hyperexcitability and seizures.

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