LTP and memory impairment caused by extracellular Aβ and Tau oligomers is APP-dependent

Puzzo, Daniela; Piacentini, Roberto; Fa', Mauro; Gulisano, Walter; Li Puma, Domenica D; Staniszewski, Agnes; Zhang, Hong; Tropea, Maria Rosaria; Cocco, Sara; Palmeri, Agostino; Fraser, Paul; D'Adamio, Luciano; Grassi, Claudio; Arancio, Ottavio

doi:10.7554/eLife.26991

The concurrent application of subtoxic doses of soluble oligomeric forms of human amyloid-beta (oAβ) and Tau (oTau) proteins impairs memory and its electrophysiological surrogate long-term potentiation (LTP), effects that may be mediated by intra-neuronal oligomers uptake. Intrigued by these findings, we investigated whether oAβ and oTau share a common mechanism when they impair memory and LTP in mice. We found that as already shown for oAβ, also oTau can bind to amyloid precursor protein (APP). Moreover, efficient intra-neuronal uptake of oAβ and oTau requires expression of APP. Finally, the toxic effect of both extracellular oAβ and oTau on memory and LTP is dependent upon APP since APP-KO mice were resistant to oAβ- and oTau-induced defects in spatial/associative memory and LTP. Thus, APP might serve as a common therapeutic target against Alzheimer's Disease (AD) and a host of other neurodegenerative diseases characterized by abnormal levels of Aβ and/or Tau.

Titolo:	LTP and memory impairment caused by extracellular Aβ and Tau oligomers is APP-dependent
Autori interni:	PUZZO, DANIELA (Primo) Piacentini, Roberto Fa', Mauro GULISANO, WALTER Li Puma, Domenica D Staniszewski, Agnes Zhang, Hong Tropea, Maria Rosaria Cocco, Sara PALMERI, Agostino Fraser, Paul D'Adamio, Luciano Grassi, Claudio Arancio, Ottavio mostra contributor esterni nascondi contributor esterni
Data di pubblicazione:	2017
Rivista:	ELIFE
Abstract:	The concurrent application of subtoxic doses of soluble oligomeric forms of human amyloid-beta (oAβ) and Tau (oTau) proteins impairs memory and its electrophysiological surrogate long-term potentiation (LTP), effects that may be mediated by intra-neuronal oligomers uptake. Intrigued by these findings, we investigated whether oAβ and oTau share a common mechanism when they impair memory and LTP in mice. We found that as already shown for oAβ, also oTau can bind to amyloid precursor protein (APP). Moreover, efficient intra-neuronal uptake of oAβ and oTau requires expression of APP. Finally, the toxic effect of both extracellular oAβ and oTau on memory and LTP is dependent upon APP since APP-KO mice were resistant to oAβ- and oTau-induced defects in spatial/associative memory and LTP. Thus, APP might serve as a common therapeutic target against Alzheimer's Disease (AD) and a host of other neurodegenerative diseases characterized by abnormal levels of Aβ and/or Tau.
Handle:	http://hdl.handle.net/20.500.11769/301137
Appare nelle tipologie:	1.1 Articolo in rivista

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