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. 2011 Apr;134(Pt 4):1077-88.
doi: 10.1093/brain/awr044. Epub 2011 Mar 22.

Spatial patterns of brain amyloid-beta burden and atrophy rate associations in mild cognitive impairment

Collaborators, Affiliations

Spatial patterns of brain amyloid-beta burden and atrophy rate associations in mild cognitive impairment

Duygu Tosun et al. Brain. 2011 Apr.

Abstract

Amyloid-β accumulation in the brain is thought to be one of the earliest events in Alzheimer's disease, possibly leading to synaptic dysfunction, neurodegeneration and cognitive/functional decline. The earliest detectable changes seen with neuroimaging appear to be amyloid-β accumulation detected by (11)C-labelled Pittsburgh compound B positron emission tomography imaging. However, some individuals tolerate high brain amyloid-β loads without developing symptoms, while others progressively decline, suggesting that events in the brain downstream from amyloid-β deposition, such as regional brain atrophy rates, play an important role. The main purpose of this study was to understand the relationship between the regional distributions of increased amyloid-β and the regional distribution of increased brain atrophy rates in patients with mild cognitive impairment. To simultaneously capture the spatial distributions of amyloid-β and brain atrophy rates, we employed the statistical concept of parallel independent component analysis, an effective method for joint analysis of multimodal imaging data. Parallel independent component analysis identified significant relationships between two patterns of amyloid-β deposition and atrophy rates: (i) increased amyloid-β burden in the left precuneus/cuneus and medial-temporal regions was associated with increased brain atrophy rates in the left medial-temporal and parietal regions; and (ii) in contrast, increased amyloid-β burden in bilateral precuneus/cuneus and parietal regions was associated with increased brain atrophy rates in the right medial temporal regions. The spatial distribution of increased amyloid-β and the associated spatial distribution of increased brain atrophy rates embrace a characteristic pattern of brain structures known for a high vulnerability to Alzheimer's disease pathology, encouraging for the use of (11)C-labelled Pittsburgh compound B positron emission tomography measures as early indicators of Alzheimer's disease. These results may begin to shed light on the mechanisms by which amyloid-β deposition leads to neurodegeneration and cognitive decline and the development of a more specific Alzheimer's disease-specific imaging signature for diagnosis and use of this knowledge in the development of new anti-therapies for Alzheimer's disease.

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Figures

Figure 1
Figure 1
Data mapping of baseline PiB-standardized uptake value ratio (PiB-SUVR) and 1-year brain atrophy rates (Jac-map) for spatial statistical analysis in the unbiased large deformation (ULD) template image space. MCI = mild cognitive impairment.
Figure 2
Figure 2
First parallel independent component analysis component pair. SUVR = standardized uptake value ratio.
Figure 3
Figure 3
Second parallel independent component analysis component pair. SUVR = standardized uptake value ratio.

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