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. 2017 Aug 1;140(8):2112-2119.
doi: 10.1093/brain/awx137.

Cerebral quantitative susceptibility mapping predicts amyloid-β-related cognitive decline

Scott Ayton  1 Amir Fazlollahi  2   3 Pierrick Bourgeat  2   3 Parnesh Raniga  2 Amanda Ng  4 Yen Ying Lim  1 Ibrahima Diouf  1   2 Shawna Farquharson  1   4 Jurgen Fripp  2   3 David Ames  5   6 James Doecke  2   3 Patricia Desmond  7 Roger Ordidge  4 Colin L Masters  1   3 Christopher C Rowe  1   8 Paul Maruff  1   9 Victor L Villemagne  1   8 Australian Imaging Biomarkers and Lifestyle (AIBL) Research GroupOlivier Salvado  2   3 Ashley I Bush  1   3
Affiliations

Cerebral quantitative susceptibility mapping predicts amyloid-β-related cognitive decline

Scott Ayton et al. Brain. .

Abstract

See Derry and Kent (doi:10.1093/awx167) for a scientific commentary on this article.The large variance in cognitive deterioration in subjects who test positive for amyloid-β by positron emission tomography indicates that convergent pathologies, such as iron accumulation, might combine with amyloid-β to accelerate Alzheimer's disease progression. Here, we applied quantitative susceptibility mapping, a relatively new magnetic resonance imaging method sensitive to tissue iron, to assess the relationship between iron, amyloid-β load, and cognitive decline in 117 subjects who underwent baseline magnetic resonance imaging and amyloid-β positron emission tomography from the Australian Imaging, Biomarkers and Lifestyle study (AIBL). Cognitive function data were collected every 18 months for up to 6 years from 100 volunteers who were either cognitively normal (n = 64) or diagnosed with mild cognitive impairment (n = 17) or Alzheimer's disease (n = 19). Among participants with amyloid pathology (n = 45), higher hippocampal quantitative susceptibility mapping levels predicted accelerated deterioration in composite cognition tests for episodic memory [β(standard error) = -0.169 (0.034), P = 9.2 × 10-7], executive function [β(standard error) = -0.139 (0.048), P = 0.004), and attention [β(standard error) = -0.074 (0.029), P = 0.012]. Deteriorating performance in a composite of language tests was predicted by higher quantitative susceptibility mapping levels in temporal lobe [β(standard error) = -0.104 (0.05), P = 0.036] and frontal lobe [β(standard error) = -0.154 (0.055), P = 0.006]. These findings indicate that brain iron might combine with amyloid-β to accelerate clinical progression and that quantitative susceptibility mapping could be used in combination with amyloid-β positron emission tomography to stratify individuals at risk of decline.

Keywords: Alzheimer’s; MRI; Quantitative Susceptibility Mapping; cognitive decline; iron.

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