AI Article Synopsis

  • The study investigates whether the negative effects of the APOE4 gene are limited to Alzheimer's disease or affect cognition more broadly.
  • The analysis included various neuropsychological measures and brain imaging data, focusing on individuals categorized by their APOE4 status and amyloid-PET results.
  • Results showed that amyloid positivity heavily influenced cognitive performance, with APOE4 impacting cognition primarily in those who were amyloid-positive, suggesting a complex interaction that could drive cognitive impairment through neurodegeneration in the hippocampus.

Article Abstract

Whether the deleterious effects of APOE4 are restricted to the Alzheimer's disease (AD) spectrum or cause cognitive impairment irrespectively of the development of AD is still a matter of debate, and the focus of this study. Our analyses included APOE4 genotype, neuropsychological variables, amyloid-βeta (Aβ) and Tau markers, FDG-PET values, and hippocampal volumetry data derived from the healthy controls sample of the ADNI database. We formed 4 groups of equal size (n = 30) based on APOE4 carriage and amyloid-PET status. Baseline and follow-up (i.e., 48 months post-baseline) results indicated that Aβ-positivity was the most important factor to explain poorer cognitive performance, while APOE4 only exerted a significant effect in Aβ-positive subjects. Additionally, multiple regression analyses evidenced that, within the Aβ-positive sample, hippocampal volumetry explained most of the variability in cognitive performance for APOE4 carriers. These findings represent a strong support for the so-called preclinical/prodromal hypothesis, which states that the reported differences in cognitive performance between healthy carriers and non-carriers are mainly due to the APOE4's capability to increase the risk of AD. Moreover, our results reinforce the notion that a synergistic interaction of Aβ and APOE4 elicits a neurodegenerative process in the hippocampus that might be the main cause of impaired cognitive performance.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8811053PMC
http://dx.doi.org/10.1007/s11357-021-00450-xDOI Listing

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