Comparative characterization of 5XFAD and hAbeta SAA mouse models of familial AD
Abstract Background The failure of most clinical Alzheimer’s disease (AD) trials has been partially attributed to the lack of translatability of current AD mouse models to human patients. A recently developed model of familial AD (fAD), expressing Swedish, Arctic and Austrian mutations in App (hAbet...
Published in: | Alzheimer's & Dementia |
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Main Authors: | , , , , , , , , , , , , , |
Format: | Article in Journal/Newspaper |
Language: | English |
Published: |
Wiley
2022
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Subjects: | |
Online Access: | http://dx.doi.org/10.1002/alz.067648 https://onlinelibrary.wiley.com/doi/pdf/10.1002/alz.067648 |
Summary: | Abstract Background The failure of most clinical Alzheimer’s disease (AD) trials has been partially attributed to the lack of translatability of current AD mouse models to human patients. A recently developed model of familial AD (fAD), expressing Swedish, Arctic and Austrian mutations in App (hAbeta SAA ), has been shown to be a useful amyloidogenic model which recapitulates many aspects of human AD, including plaque distribution and microglial transcriptional changes. Our aim is to further characterize the hAbeta SAA model and compare it to the widely used 5xFAD transgenic model. Method Motion Sequencing (MoSeq) software was used to model the underlying structure of spontaneous behaviors recorded in an open field in hAbeta SAA and 5xFAD mice longitudinally from 10 to 18 months of age. Aged hAbeta SAA and 5xFAD brain tissue was used for spatial transcriptomic/proteomic profiling, performed by Nanostring’s GeoMx®, which allowed for quantification of gene and protein expression in plaque‐associated and non‐plaque‐associated regions of interest. A fluorophore‐conjugated amyloid antibody (Methoxy‐X04) was administered to cohorts of hAbeta SAA and 5xFAD prior to harvest at various ages. An additional fluorophore‐conjugated antibody (lectin Dylight®594) was administered to 19‐month‐old cohorts permitting visualization of cerebral amyloid angiopathy (CAA). Whole brains were sectioned/imaged using Serial Two‐Photon Tomography on the TissueCyte (TissueVision), creating indexed tissue sections and high‐resolution 3D models of each brain. Subsequent rounds of staining permitted characterization of disease‐associated microglia (DAM) and dystrophic neurites. An independent cohort was evaluated for EEG telemetry. Result MoSeq revealed divergent behaviors of 5xFAD and hAbeta SAA mice suggesting differences in behavioral phenotypes of these two models. Preliminary GeoMx data shows upregulation of DAM genes localized to plaques in hAbeta SAA homozygotes as identified by RNA‐seq; correlating 5xFAD data is in progress. Further ... |
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