| Literature DB >> 25899416 |
Sander C J Verfaillie1, Sofie M Adriaanse, Maja A A Binnewijzend, Marije R Benedictus, Rik Ossenkoppele, Mike P Wattjes, Yolande A L Pijnenburg, Wiesje M van der Flier, Adriaan A Lammertsma, Joost P A Kuijer, Ronald Boellaard, Philip Scheltens, Bart N M van Berckel, Frederik Barkhof.
Abstract
OBJECTIVES: Alzheimer's disease (AD) and frontotemporal (FTD) dementia can be differentiated using [(18)F]-2-deoxy-2-fluoro-D-glucose (FDG)-PET. Since cerebral blood flow (CBF) is related to glucose metabolism, our aim was to investigate the extent of overlap of abnormalities between AD and FTD.Entities:
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Year: 2015 PMID: 25899416 PMCID: PMC4562004 DOI: 10.1007/s00330-015-3696-1
Source DB: PubMed Journal: Eur Radiol ISSN: 0938-7994 Impact factor: 5.315
Demographic and clinical data
| Patient group | AD | FTD | Controls | Test-statistic ( |
|---|---|---|---|---|
| Age in years (SD) | 64 (8) | 61 (8) | 56 (10) | F(37,2) = 1.9, |
| Gender | 61 % male | 42 % male | 90 % male | χ2(2) = 5.5, |
| MMSE (SD) | 24 (4) | 24 (4) | 27 (3) | F(37,2) = 2.6, |
| Median years of complaints (interquartile range)* | 2.0 (1.9) | 2.3 (1.9) | n.a. | U = 101.5, |
| Scan interval in months (SD) | 2.1 (1) | 2.2 (2) | 1.9 (2) | F(37,2) = .8, |
| FDG SUV normalization variables | ||||
| Body | ||||
| Weight in kg (SD) | 78 (11) | 75 (15) | 86 (17) | F(37,2) = 2.2, |
| Length in cm (SD) | 176 (9) | 169 (10) | 175 (9) | F(37,2) = 1.5, |
| Injected dose in MBq (SD) | 190 (8) | 187 (8) | 188 (7) | F(37,2) = .97, |
Abbreviations: cm centimetre, kg kilogram, MBq megabecquerel, SD standard deviation, SUV standardized uptake value
*Obtained through interviews with relatives of patients
Fig. 1Transversal FDG and ASL images of an FTD (first and second rows, MMSE 26) and an AD (third and fourth rows, MMSE 17) patient with early-onset disease. Both transversal planes show predominantly prefrontal abnormalities in FTD and parietal abnormalities in AD. Red colour reflects normal metabolism and perfusion
Fig. 2Functional brain abnormalities of AD and FTD compared to controls projected onto a MNI glass brain. Predominantly parietal, precuneus aberrant function is visible in AD compared to controls, while FTD compared to controls shows mostly prefrontal abnormalities with both FDG and ASL. For illustrative purposes, images were thresholded at p < 0.005
Fig. 3Panel A shows FDG and ASL regional mean z-scores of AD (left) and FTD (right) compared to controls. Panel B shows AD < FTD (left) and FTD < AD (right) perfusion and metabolism abnormalities
Fig. 4Positive correlations between FDG SUV and ASL derived CBF in (A) medial prefrontal cortex (right, r = .74, p < 0.001) and (B) inferior parietal lobule (left, r = .61, p < 0.001) across groups
Fig. 5ROC curves for FDG and ASL in AD and FTD. A) Precuneus function for ASL and FDG in discriminating AD from FTD. B) mPFC function in discriminating FTD from AD. Ratios were taken between the mPFC and precuneus and entered into ROC analyses as ‘ratio ROI’