Associations of amyloid-β oligomers and plaques with neuropathology in the App NL-G-F mouse. Academic Article uri icon

Overview

abstract

  • Amyloid-β pathology and neurofibrillary tangles lead to glial activation and neurodegeneration in Alzheimer's disease. In this study, we investigated the relationships between the levels of amyloid-β oligomers, amyloid-β plaques, glial activation and markers related to neurodegeneration in the App NL-G-F triple mutation mouse line and in a knock-in line homozygous for the common human amyloid precursor protein (App hu mouse). The relationships between neuropathological features were characterized with immunohistochemistry and imaging mass cytometry. Markers assessing human amyloid-β proteins, microglial and astrocytic activation and neuronal and synaptic densities were used in mice between 2.5 and 12 months of age. We found that amyloid-β oligomers were abundant in the brains of App hu mice in the absence of classical amyloid-β plaques. These brains showed morphological changes consistent with astrocyte activation but no evidence of microglial activation or synaptic or neuronal pathology. In contrast, both high levels of amyloid-β oligomers and numerous plaques accumulated in App NL-G-F mice in association with substantial astrocytic and microglial activation. The increase in amyloid-β oligomers over time was more strongly correlated with astrocytic than with microglia activation. Spatial analyses suggested that activated microglia were more closely associated with amyloid-β oligomers than with amyloid-β plaques in App NL-G-F mice, which also showed age-dependent decreases in neuronal and synaptic density markers. A comparative study of the two models highlighted the dependence of glial and neuronal pathology on the nature and aggregation state of the amyloid-β peptide. Astrocyte activation and neuronal pathology appeared to be more strongly associated with amyloid-β oligomers than with amyloid-β plaques, although amyloid-β plaques were associated with microglia activation.

authors

  • Tang, Jiabin
  • Huang, Helen
  • Muirhead, Robert C J
  • Zhou, Yue
  • Li, Junheng
  • DeFelice, John
  • Kopanitsa, Maksym V
  • Serneels, Lutgarde
  • Davey, Karen
  • Tilley, Bension S
  • Gentleman, Steve
  • Matthews, Paul M

publication date

  • June 25, 2024

Identity

PubMed Central ID

  • PMC11258573

Scopus Document Identifier

  • 85199249457

Digital Object Identifier (DOI)

  • 10.1093/braincomms/fcae218

PubMed ID

  • 39035420

Additional Document Info

volume

  • 6

issue

  • 4