Evaluation of a calibrated 18F-FDG PET score as a biomarker for progression in alzheimer disease and mild cognitive impairment

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Abstract

Increasingly, clinical trials are being planned in patients with mild cognitive impairment (MCI) to prevent or delay the onset of dementia in Alzheimer disease (AD) by disease-modifying intervention. Inclusion of imaging techniques as biomarkers for patient selection and assessment of outcome is expected to increase trial efficacy. PET using 18F-FDG provides objective information about the impairment of synaptic function and could, with appropriate standardization, qualify as a biomarker. Methods: We evaluated a predefined quantitative measure (PET score) that is extracted automatically from 18F-FDG PET scans using a sample of controls (n = 44), patients with MCI (n = 94), and patients with mild AD (n = 40) from the Alzheimer Disease Neuroimaging Initiative (ADNI). Subjects received 4 scans and clinical assessments over 2 y. Results: PET scores provide much higher test - retest reliability than standard neuropsychologic test scores (Alzheimer's Disease Assessment Scale - Cognitive [ADAS-cog] and Mini-Mental State Examination) and superior signal strength for measuring progression. At the same time, they are related linearly to ADAS-cog scores, thus providing a valid measure of cognitive impairment. In addition, PET scores at study entry in MCI patients significantly predict clinical progression to dementia with a higher accuracy than Mini-Mental State Examination and ADAS-cog. Conclusion: 18F-FDG PET scores are a valid imaging biomarker to monitor the progression of MCI to AD. Their superior test - retest reliability and signal strength will allow the reduction in the number of subjects needed or shortening of study duration substantially. Copyright © 2011 by the Society of Nuclear Medicine, Inc.

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Herholz, K., Westwood, S., Haense, C., & Dunn, G. (2011). Evaluation of a calibrated 18F-FDG PET score as a biomarker for progression in alzheimer disease and mild cognitive impairment. Journal of Nuclear Medicine, 52(8), 1218–1226. https://doi.org/10.2967/jnumed.111.090902

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