2016 Articles
Accelerating rates of cognitive decline and imaging markers associated with β-amyloid pathology
Objective: To estimate points along the spectrum of b-amyloid pathology at which rates of change of several measures of neuronal injury and cognitive decline begin to accelerate. Methods: In 460 patients with mild cognitive impairment (MCI), we estimated the points at which rates of florbetapir PET, fluorodeoxyglucose (FDG) PET, MRI, and cognitive and functional decline begin to accelerate with respect to baseline CSF Ab42. Points of initial acceleration in rates of decline were estimated using mixed-effects regression. Results: Rates of neuronal injury and cognitive and even functional decline accelerate substantially before the conventional threshold for amyloid positivity, with rates of florbetapir PET and FDG PET accelerating early. Temporal lobe atrophy rates also accelerate prior to the threshold, but not before the acceleration of cognitive and functional decline. Conclusions: A considerable proportion of patients with MCI would not meet inclusion criteria for a trial using the current threshold for amyloid positivity, even though on average, they are experiencing cognitive/functional decline associated with prethreshold levels of CSF Ab42. Future trials in early Alzheimer disease might consider revising the criteria regarding b-amyloid thresholds to include the range of amyloid associated with the first signs of accelerating rates of decline. Neurology® 2016;86:1887–1896
Files
- Insel and Mattsson - 2016 - Accelerating rates of cognitive decline and imagin.pdf application/pdf 1.11 MB Download File
Also Published In
More About This Work
- Academic Units
- Neurology
- Published Here
- February 11, 2022