The amyloid cascade and Alzheimer's disease therapeutics: theory versus observation.

Lab Invest

Department of Biology and Brain Health Consortium, College of Sciences, The University of Texas at San Antonio, San Antonio, TX, USA.

Published: July 2019

AI Article Synopsis

  • - The discovery of APP mutations linked to early onset Alzheimer's disease and the role of amyloid-β in forming plaques led to the amyloid cascade hypothesis, which suggests a connection between amyloid-β accumulation and Alzheimer's pathology.
  • - Down syndrome supports this hypothesis due to the presence of an extra APP gene copy and the development of Alzheimer's-like symptoms by middle age.
  • - Despite promising initial findings, Aβ-targeted clinical trials have faced setbacks, raising questions about their effectiveness; while some clearance of Aβ has occurred, it hasn’t significantly improved cognitive outcomes, indicating that tackling amyloid-β alone may not sufficiently modify the disease.

Article Abstract

The identification of amyloid-β precursor protein (APP) pathogenic mutations in familial early onset Alzheimer's disease (AD), along with knowledge that amyloid-β (Aβ) was the principle protein component of senile plaques, led to the establishment of the amyloid cascade hypothesis. Down syndrome substantiated the hypothesis, given an extra copy of the APP gene and invariable AD pathology hallmarks that occur by middle age. An abundance of support for the amyloid cascade hypothesis followed. Prion-like protein misfolding and non-Mendelian transmission of neurotoxicity are among recent areas of investigation. Aβ-targeted clinical trials have been disappointing, with negative results attributed to inadequacies in patient selection, challenges in pharmacology, and incomplete knowledge of the most appropriate target. There is evidence, however, that proof of concept has been achieved, i.e., clearance of Aβ during life, but with no significant changes in cognitive trajectory in AD. Whether the time, effort, and expense of Aβ-targeted therapy will prove valuable will be determined over time, as Aβ-centered clinical trials continue to dominate therapeutic strategies. It seems reasonable to hypothesize that the amyloid cascade is intimately involved in AD, in parallel with disease pathogenesis, but that removal of toxic Aβ is insufficient for an effective disease modification.

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Source
http://dx.doi.org/10.1038/s41374-019-0231-zDOI Listing

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