Journal
BRAIN
Volume 141, Issue -, Pages 1529-1544Publisher
OXFORD UNIV PRESS
DOI: 10.1093/brain/awy050
Keywords
event-based model; differential-equation model; disease progression; dominantly-inherited Alzheimer's disease; biomarker dynamics
Categories
Funding
- Dominantly Inherited Alzheimer Network (DIAN) - National Institute on Aging [UF1 AG032438]
- German Center for Neurodegenerative Diseases
- Medical Research Council (MRC) Dementias Platform UK [MR/L023784/2, MR/009076/2]
- National Institute for Health Research University College London Hospitals Biomedical Research Centre
- National Institute of Health
- Alzheimer's Association
- BrightFocus Foundation
- Cure Alzheimer's Fund
- European Union's Horizon research and innovation programme [666992]
- UK Engineering and Physical Sciences Research Council (EPSRC) [EP/M020533/1, EP/M006093/1, EP/J020990/01]
- European Commission
- Michael J Fox Foundation for Parkinson's Research
- Alzheimer's Research UK
- Weston Brain Institute
- EPSRC
- Alzheimer Society [AS-PG-15-025]
- Alzheimer's Research UK [ARUK-PG2014-1946]
- Medical Research Council UK [MR/M023664/1]
- UK Dementia Research Institute
- Janssen
- Eli Lilly
- Novartis
- Sanofi
- GlaxoSmithKline
- NIH [P50AG005681, P01AG003991, P01AG026276, UF01AG032438]
- MRC [G0801306, MR/M023664/1, MR/M009106/1, UKDRI-1001, G0401247, G0601846, G116/143, MR/L023784/2] Funding Source: UKRI
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Dominantly-inherited Alzheimer's disease is widely hoped to hold the key to developing interventions for sporadic late onset Alzheimer's disease. We use emerging techniques in generative data-driven disease progression modelling to characterize dominantly-inherited Alzheimer's disease progression with unprecedented resolution, and without relying upon familial estimates of years until symptom onset. We retrospectively analysed biomarker data from the sixth data freeze of the Dominantly Inherited Alzheimer Network observational study, including measures of amyloid proteins and neurofibrillary tangles in the brain, regional brain volumes and cortical thicknesses, brain glucose hypometabolism, and cognitive performance from the Mini-Mental State Examination (all adjusted for age, years of education, sex, and head size, as appropriate). Data included 338 participants with known mutation status (211 mutation carriers in three subtypes: 163 PSEN1, 17 PSEN2, and 31 APP) and a baseline visit (age 19-66; up to four visits each, 1.1 +/- 1.9 years in duration; spanning 30 years before, to 21 years after, parental age of symptom onset). We used an event-based model to estimate sequences of biomarker changes from baseline data across disease subtypes (mutation groups), and a differential equation model to estimate biomarker trajectories from longitudinal data (up to 66 mutation carriers, all subtypes combined). The two models concur that biomarker abnormality proceeds as follows: amyloid deposition in cortical then subcortical regions (similar to 24 +/- 11 years before onset); phosphorylated tau (17 +/- 8 years), tau and amyloid-beta changes in cerebrospinal fluid; neurodegeneration first in the putamen and nucleus accumbens (up to 6 +/- 2 years); then cognitive decline (7 +/- 6 years), cerebral hypometabolism (4 +/- 4 years), and further regional neurodegeneration. Our models predicted symptom onset more accurately than predictions that used familial estimates: root mean squared error of 1.35 years versus 5.54 years. The models reveal hidden detail on dominantly-inherited Alzheimer's disease progression, as well as providing data-driven systems for fine-grained patient staging and prediction of symptom onset with great potential utility in clinical trials.
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