Temporal Order of Alzheimer’s Disease-Related Cognitive Marker Changes in BLSA and WRAP Longitudinal Studies

Bilgel, Murat; Koscik, Rebecca L.; An, Yang; Prince, Jerry L.; Resnick, Susan M.; Johnson, Sterling C.; Jedynak, Bruno

doi:10.3233/jad-170448

Cited by 18 publications

(11 citation statements)

References 62 publications

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“…Data from the core WRAP protocol and from a subset of WRAP's linked studies are accessible to qualified researchers via an online request form and data use agreement which can be linked from the Global Alzheimer's Association Interactive Network web site ( www.gaain.org ). Recent examples of data-sharing collaborations include a study that found consistency in patterns of cognitive aging progression scores across the Baltimore Longitudinal Study on Aging and WRAP [98] , a meta-analysis of APOE and sex on dementia incidence [99] , and a study involving predictive algorithms for MCI in a consortium of five preclinical AD or adult children cohorts [100] .…”

Section: Review Of Select Study Findings and New Resultsmentioning

confidence: 99%

The Wisconsin Registry for Alzheimer's Prevention: A review of findings and current directions

Johnson

Koscik

Jonaitis

et al. 2017

Alz & Dem Diag Ass & Dis Mo

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197

218

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The Wisconsin Registry for Alzheimer's Prevention is a longitudinal observational cohort study enriched with persons with a parental history (PH) of probable Alzheimer's disease (AD) dementia. Since late 2001, Wisconsin Registry for Alzheimer's Prevention has enrolled 1561 people at a mean baseline age of 54 years. Participants return for a second visit 4 years after baseline, and subsequent visits occur every 2 years. Eighty-one percent (1270) of participants remain active in the study at a current mean age of 64 and 9 years of follow-up. Serially assessed cognition, self-reported medical and lifestyle histories (e.g., diet, physical and cognitive activity, sleep, and mood), laboratory tests, genetics, and linked studies comprising molecular imaging, structural imaging, and cerebrospinal fluid data have yielded many important findings. In this cohort, PH of probable AD is associated with 46% apolipoprotein E ( APOE ) ε4 positivity, more than twice the rate of 22% among persons without PH. Subclinical or worse cognitive decline relative to internal normative data has been observed in 17.6% of the cohort. Twenty-eight percent exhibit amyloid and/or tau positivity. Biomarker elevations, but not APOE or PH status, are associated with cognitive decline. Salutary health and lifestyle factors are associated with better cognition and brain structure and lower AD pathophysiologic burden. Of paramount importance is establishing the amyloid and tau AD endophenotypes to which cognitive outcomes can be linked. Such data will provide new knowledge on the early temporal course of AD pathophysiology and inform the design of secondary prevention clinical trials.

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Section: Review Of Select Study Findings and New Resultsmentioning

confidence: 99%

The Wisconsin Registry for Alzheimer's Prevention: A review of findings and current directions

Johnson

Koscik

Jonaitis

et al. 2017

Alz & Dem Diag Ass & Dis Mo

Self Cite

197

218

View full text Add to dashboard Cite

show abstract

“…Sensitivity analyses excluding APOE showed slightly older ages of divergence, suggesting that, as expected, APOE ε4 allele carriers experience earlier cognitive decline. Our findings are consistent with prior work 1 , 15 , 16 , 17 , 18 , 21 , 40 , 41 , 42 , 43 in early- and late-onset AD, suggesting that cognitive and physiologic changes associated with AD begin at least 15 years before diagnosis—the mean age of dementia diagnosis for White UK residents is 82 years. 44 Our study advances understanding of the natural history of late-onset AD by showing that, in a generally healthy, community-dwelling sample, those at high genetic risk of developing AD in late life performed worse on several cognitive measures in midlife.…”

Section: Discussionmentioning

confidence: 99%

“…Although episodic memory changes are generally considered leading indicators of AD, 15 , 16 , 17 , 18 , 19 , 20 subtle changes in other domains, such as semantic memory, processing speed, and executive functioning, may occur at the same age or earlier. 20 , 21 , 22 , 23 The potential for symptoms to manifest in any of multiple cognitive domains can be evaluated in parallel using a hypothesis-free approach to rapidly screen numerous possible indicators of disease based on phenotypes associated with a GRS.…”

Section: Introductionmentioning

confidence: 99%

Association of Genetic Variants Linked to Late-Onset Alzheimer Disease With Cognitive Test Performance by Midlife

et al. 2022

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Key Points Question At what age do individuals with higher genetic risk of Alzheimer disease first show cognitive differences from individuals with lower genetic risk, and which of 32 cognitive measures show the earliest difference? Findings In this cross-sectional study of 405 050 individuals, higher genetic risk of Alzheimer disease significantly modified the association of age with 13 of 32 cognitive measures. Best-fitting models suggested that higher genetic risk of Alzheimer disease was associated with changes in cognitive scores of individuals older than 56 years for all 13 measures and older than 47 years for 9 measures. Meaning These findings suggest that by early midlife, subtle differences in cognitive measures may emerge among individuals with higher genetic risk of Alzheimer disease.

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“…However, this is a challenging goal given that there is no scientific consensus regarding the definition of healthy aging. Several studies have approached this problem by including age and other demographic variables as covariates in addition to a disease stage variable [11,31,32] or by regressing out their effects before model fitting [5,33,34], whereas others have not included covariates to characterize trajectories that explain the natural history of AD dementia, including biological and cognitive changes that occur due to aging in addition to AD [4,[6][7][8][9]13,15]. We formulated our goal with this study as the characterization of the natural history of AD dementia, including biological and cognitive changes that occur due to aging in addition to AD pathology, and therefore did not include an adjustment for age or any other demographic variables.…”

Section: Discussionmentioning

confidence: 99%

Predicting time to dementia using a quantitative template of disease progression

Bilgel

Jedynak

2019

Alz & Dem Diag Ass & Dis Mo

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Introduction Characterization of longitudinal trajectories of biomarkers implicated in sporadic Alzheimer's disease (AD) in decades before clinical diagnosis is important for disease prevention and monitoring. Methods We used a multivariate Bayesian model to temporally align 1369 Alzheimer's disease Neuroimaging Initiative participants based on the similarity of their longitudinal biomarker measures and estimated a quantitative template of the temporal evolution of cerebrospinal fluid A , p- , and t-tau and hippocampal volume, brain glucose metabolism, and cognitive measurements. We computed biomarker trajectories as a function of time to AD dementia and predicted AD dementia onset age in a disjoint sample. Results Quantitative template showed early changes in verbal memory, cerebrospinal fluid Aβ 1–42 and p-tau 181p , and hippocampal volume. Mean error in predicted AD dementia onset age was years. Discussion Our method provides a quantitative approach for characterizing the natural history of AD starting at preclinical stages despite the lack of individual-level longitudinal data spanning the entire disease timeline.

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Temporal Order of Alzheimer’s Disease-Related Cognitive Marker Changes in BLSA and WRAP Longitudinal Studies

Cited by 18 publications

References 62 publications

The Wisconsin Registry for Alzheimer's Prevention: A review of findings and current directions

The Wisconsin Registry for Alzheimer's Prevention: A review of findings and current directions

Association of Genetic Variants Linked to Late-Onset Alzheimer Disease With Cognitive Test Performance by Midlife

Predicting time to dementia using a quantitative template of disease progression

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