%0 Conference Paper
%A Wisch, Julie K
%A McKay, Nicole S
%A Zammit, Matthew D
%A Christian, Bradley T
%A Schultz, Stephanie A
%A Millar, Peter R
%A Barthélemy, Nicolas R
%A Ryan, Natalie S
%A Renton, Alan E
%A Vermunt, Lisa
%A Joseph-Mathurin, Nelly
%A Shirzadi, Zahra
%A Strain, Jeremy F
%A Chrem, Patricio
%A Daniels, Alisha
%A Chhatwal, Jasmeer P
%A Cruchaga, Carlos
%A Ibanez, Laura
%A Jucker, Mathias
%A Day, Gregory S
%A Lee, Jae-Hong
%A Levin, Johannes
%A Llibre-Guerra, Jorge J
%A Aguillon, David
%A Roh, Jee Hoon
%A Supnet-Bell, Charlene
%A Xiong, Chengjie
%A Schindler, Suzanne E
%A Wang, Guoqiao
%A Li, Yan
%A Koeppe, Robert
%A Jack, Clifford R
%A Morris, John C
%A McDade, Eric
%A Bateman, Randall J
%A Benzinger, Tammie L S
%A Ances, Beau
%A Betthauser, Tobey J
%A Gordon, Brian A
%T Validation of Amyloid Chronicity in Autosomal Dominant Alzheimer Disease
%J Alzheimer's and dementia
%V 21
%N Suppl 2
%@ 1552-5260
%M DZNE-2025-01463
%P e103008
%D 2025
%X Alzheimer Disease (AD) pathology evolves over decades, and understanding this progression is critical to the understanding of the disease and timing therapeutic interventions. Since individuals with Autosomal Dominant AD (ADAD) develop symptoms around the same age as their parent, it is possible to predict symptom onset and stage individuals by their estimated years to symptom onset (EYO). This approach does not generalize to other forms of AD, thus there is a pressing need for the timecourse of ADAD to be defined in broadly relevant terms. The objective of this project is to validate the Sampled Iterative Local Approximation (SILA) algorithm in a cohort with a known disease timecourse. SILA generates an estimate of time from amyloid positivity (Atime) based on longitudinal PET data.We evaluated Atime in a longitudinal ADAD sample (N = 316) with PET PiB data in three ways. First, we compared predicted age at amyloid positive (A+) to observed age at A+ for individuals who became A+ during enrollment. Next, using linear regression, we compared estimated age at A+ to estimated age at symptom onset (EYO=0). Finally, we used generalized additive models to compare the amount of variance in concurrent cognitive performance explained both Atime and EYO.We observed a mean average error of 1.15 years between actual age at A+ (N = 26) and the SILA-predicted Atime. Across all participants, SILA-estimated age at A+ explained 39
%B Alzheimer’s Association International Conference
%C 27 Jul 2025 - 31 Jul 2025, Toronto (Canada)
Y2 27 Jul 2025 - 31 Jul 2025
M2 Toronto, Canada
%K Humans
%K Alzheimer Disease: diagnostic imaging
%K Alzheimer Disease: diagnosis
%K Alzheimer Disease: metabolism
%K Positron-Emission Tomography
%K Male
%K Female
%K Biomarkers: metabolism
%K Longitudinal Studies
%K Aged
%K Disease Progression
%K Middle Aged
%K Algorithms
%K Amyloid beta-Peptides: metabolism
%K Brain: diagnostic imaging
%K Brain: metabolism
%K Biomarkers (NLM Chemicals)
%K Amyloid beta-Peptides (NLM Chemicals)
%F PUB:(DE-HGF)1 ; PUB:(DE-HGF)16
%9 AbstractJournal Article
%$ pmid:41451762
%2 pmc:PMC12741810
%R 10.1002/alz70856_103008
%U https://pub.dzne.de/record/283056