| Literature DB >> 29865055 |
Walter Gulisano1, Daniele Maugeri1, Marian A Baltrons2,3, Mauro Fà2, Arianna Amato4, Agostino Palmeri1, Luciano D'Adamio5, Claudio Grassi6, D P Devanand2,7, Lawrence S Honig2,8, Daniela Puzzo1, Ottavio Arancio9,2.
Abstract
The "Amyloid Cascade Hypothesis" has dominated the Alzheimer's disease (AD) field in the last 25 years. It posits that the increase of amyloid-β (Aβ) is the key event in AD that triggers tau pathology followed by neuronal death and eventually, the disease. However, therapeutic approaches aimed at decreasing Aβ levels have so far failed, and tau-based clinical trials have not yet produced positive findings. This begs the question of whether the hypothesis is correct. Here we have examined literature on the role of Aβ and tau in synaptic dysfunction, memory loss, and seeding and spreading of AD, highlighting important parallelisms between the two proteins in all of these phenomena. We discuss novel findings showing binding of both Aβ and tau oligomers to amyloid-β protein precursor (AβPP), and the requirement for the presence of this protein for both Aβ and tau to enter neurons and induce abnormal synaptic function and memory. Most importantly, we propose a novel view of AD pathogenesis in which extracellular oligomers of Aβ and tau act in parallel and upstream of AβPP. Such a view will call for a reconsideration of therapeutic approaches directed against Aβ and tau, paving the way to an increased interest toward AβPP, both for understanding the pathogenesis of the disease and elaborating new therapeutic strategies.Entities:
Keywords: Amyloid-β peptide; amyloid-β protein precursor; oligomers; synaptic dysfunction; tau
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Year: 2018 PMID: 29865055 DOI: 10.3233/JAD-179935
Source DB: PubMed Journal: J Alzheimers Dis ISSN: 1387-2877 Impact factor: 4.472