Changes in brain transcripts related to alzheimer's disease in a model of HFE hemochromatosis are not consistent with increased alzheimer's disease risk

D.M. Johnstone; R.M. Graham; D. Trinder; C. Riveros; J.K. Olynyk; R.J. Scott; P. Moscato; E.A. Milward

doi:10.3233/JAD-2012-112183

Back

Changes in brain transcripts related to alzheimer's disease in a model of HFE hemochromatosis are not consistent with increased alzheimer's disease risk

Journal article

Open access

Peer reviewed

Changes in brain transcripts related to alzheimer's disease in a model of HFE hemochromatosis are not consistent with increased alzheimer's disease risk

D.M. Johnstone, R.M. Graham, D. Trinder, C. Riveros, J.K. Olynyk, R.J. Scott, P. Moscato and E.A. Milward

Journal of Alzheimer's disease : JAD, Vol.30(4), pp.791-803

2012

DOI: https://doi.org/10.3233/JAD-2012-112183

Files and links (2)

pdf

changes_in_brain_transcripts.pdf416.50 kBDownload View

Published (Version of Record) Open Access

url

Link to Published Version *Subscription may be requiredView

Abstract

Amyloid-beta protein precursor

gamma-secretase

hemochromatosis

HFE

iron

notch signaling

Iron abnormalities are observed in the brains of Alzheimer's disease (AD) patients, but it is unclear whether common disorders of systemic iron overload such as hemochromatosis alter risks of AD. We used microarrays and real-time reverse transcription-PCR to investigate changes in the brain transcriptome of adult Hfe-/- mice, a model of hemochromatosis, relative to age- and gender-matched wildtype controls. Classification by functional pathway analysis revealed transcript changes for various genes important in AD. There were decreases of up to 9-fold in transcripts for amyloid-β protein precursor, tau, apolipoprotein E, presenilin 1, and various other γ-secretase components, as well as Notch signaling pathway molecules. This included decreased transcripts for 'hairy and enhancer of split' Hes1 and Hes5, downstream targets of Notch canonical signaling. The reductions in Hes1 and Hes5 transcripts provide evidence that the changes in levels of transcripts for γ-secretase components and Notch signaling genes have functional consequences. The effects appeared relatively specific for AD in that few genes pertaining to other important neurodegenerative diseases, notably Parkinson's disease and Huntington's disease, or to inflammation, oxidative stress, or apoptosis, showed altered transcript levels. The observed effects on AD-related gene transcripts do not appear to be consistent with increased AD risk in HFE hemochromatosis and might, if anything, be predicted to protect against AD to some extent. As Hfe-/- mice did not have higher brain iron levels than wildtype controls, these studies highlight the need for further research in models of more severe hemochromatosis with brain iron loading.

Details

Title: Changes in brain transcripts related to alzheimer's disease in a model of HFE hemochromatosis are not consistent with increased alzheimer's disease risk
Authors/Creators: D.M. Johnstone (Author/Creator)
R.M. Graham (Author/Creator)
D. Trinder (Author/Creator)
C. Riveros (Author/Creator)
J.K. Olynyk (Author/Creator)
R.J. Scott (Author/Creator)
P. Moscato (Author/Creator)
E.A. Milward (Author/Creator)
Publication Details: Journal of Alzheimer's disease : JAD, Vol.30(4), pp.791-803
Publisher: IOS Press
Number of pages: 13
Identifiers: 991005540012907891
Murdoch Affiliation: Murdoch University
Language: English
Resource Type: Journal article

UN Sustainable Development Goals (SDGs)

This output has contributed to the advancement of the following goals:

Source: InCites

Metrics

419 File views/ downloads

80 Record Views

10 Times Cited - Web of Science

InCites Highlights

These are selected metrics from InCites Benchmarking & Analytics tool, related to this output

Collaboration types: Domestic collaboration
Citation topics: 1 Clinical & Life Sciences; 1.184 Physiology & Metals; 1.184.573 Iron Metabolism
Web Of Science research areas: Neurosciences
ESI research areas: Neuroscience & Behavior