Abstract

The career goal of the K01 candidate is to become an independent investigator conducting research that contributes to the prevention of Alzheimer's disease (AD) dementia through elucidating disease mechanisms and deriving individual risk profiles during the preclinical stage of the disease. The environment at Massachusetts General Hospital and Harvard Medical School is ideal for the candidate's training and proposed research, providing state-of-the-art imaging facilities and a world-renowned community of AD researchers and clinicians. During this K award, the candidate will extend her expertise in multimodal neuroimaging by receiving training in Tau PET imaging, and acquire expertise in genetic analyses to pursue a novel research path. The research plan proposed herein examines the influence of known genetic risk factors, specifically the APOE4 genotype and 21 non-APOE loci associated with clinical AD in large GWAS analyses, on the relationship between AD biomarkers and cognitive decline in clinically normal older individuals (CN). An understanding of genetic risk factors within CN is especially relevant given the ability to select CN with biomarker evidence of elevated A? (preclinical AD). Although longitudinal studies have converged to reveal that CN with preclinical AD are at heightened risk of subsequent clinical impairment, heterogeneity in decline exists within this group, such that some of these individuals remain clinically normal for an extended period of time. Identification of genetic risk factors that influence the time between initial A? accumulation and the onset of clinical symptoms will greatly enhance our understanding of preclinical AD and improve our ability to identify individuals most at- risk for cognitive decline. Although some of the effects of known genetic risk factors for AD dementia are undoubtedly mediated by elevated A?, we hypothesize that these factors also influence the AD trajectory by interacting with A? to accelerate downstream effects such as the accumulation of neocortical Tau, neurodegeneration, and cognitive decline. Thus, for an equivalent level of A? burden, an individual with high genetic risk may show greater neurodegeneration than an individual with low genetic risk. This line of research should provide insight into why some A?+ individuals are able to remain clinically normal for longer periods of time whereas other A?+ individuals rapidly progress to clinical impairment. We will investigate these hypotheses in a large sample of 1777 CN combined across the Harvard Aging Brain Study (N=277), the Anti- Amyloid in Asymptomatic AD Study (A4, N=1000) and Longitudinal Evaluation of Amyloid Risk and Neurodegeneration Study (LEARN, N=500). All CN will complete amyloid PET, structural MRI, genotyping data, and longitudinal neuropsychological testing, and a large subset will additionally complete Tau PET imaging (N=827). Because disease-modifying strategies are most likely to be successful during the preclinical stage, elucidating AD disease mechanisms and deriving individual risk profiles during the preclinical stage will have tremendous impact on the prevention of AD.

Public Health Relevance

This application uses a multimodal neuroimaging approach to investigate the influence of known genetic risk factors on the Alzheimer's disease (AD) cascade. We will determine whether genetic risk factors accelerate the progression along this cascade in preclinical AD, which will enhance our ability to identify individuals most at- risk for cognitive decline who may benefit the most from disease-modifying treatments.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Scientist Development Award - Research & Training (K01)
Project #
5K01AG051718-04
Application #
9681395
Study Section
Neuroscience of Aging Review Committee (NIA)
Program Officer
Miller, Marilyn
Project Start
2017-02-16
Project End
2021-03-31
Budget Start
2019-04-01
Budget End
2020-03-31
Support Year
4
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Stanford University
Department
Neurology
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Tan, Chin Hong; Fan, Chun Chieh; Mormino, Elizabeth C et al. (2018) Polygenic hazard score: an enrichment marker for Alzheimer's associated amyloid and tau deposition. Acta Neuropathol 135:85-93
Schultz, Aaron P; Chhatwal, Jasmeer P; Hedden, Trey et al. (2017) Phases of Hyperconnectivity and Hypoconnectivity in the Default Mode and Salience Networks Track with Amyloid and Tau in Clinically Normal Individuals. J Neurosci 37:4323-4331
Lim, Yen Ying; Mormino, Elizabeth C; Alzheimer's Disease Neuroimaging Initiative (2017) APOE genotype and early ?-amyloid accumulation in older adults without dementia. Neurology 89:1028-1034
Papp, Kathryn V; Rentz, Dorene M; Orlovsky, Irina et al. (2017) Optimizing the preclinical Alzheimer's cognitive composite with semantic processing: The PACC5. Alzheimers Dement (N Y) 3:668-677
Buckley, Rachel F; Hanseeuw, Bernard; Schultz, Aaron P et al. (2017) Region-Specific Association of Subjective Cognitive Decline With Tauopathy Independent of Global ?-Amyloid Burden. JAMA Neurol 74:1455-1463
Mormino, Elizabeth C; Papp, Kathryn V; Rentz, Dorene M et al. (2017) Early and late change on the preclinical Alzheimer's cognitive composite in clinically normal older individuals with elevated amyloid ?. Alzheimers Dement 13:1004-1012
Mormino, Elizabeth C; Papp, Kathryn V; Rentz, Dorene M et al. (2016) Heterogeneity in Suspected Non-Alzheimer Disease Pathophysiology Among Clinically Normal Older Individuals. JAMA Neurol 73:1185-1191
Mormino, Elizabeth C; Sperling, Reisa A; Holmes, Avram J et al. (2016) Polygenic risk of Alzheimer disease is associated with early- and late-life processes. Neurology 87:481-8
Zhang, Xiuming; Mormino, Elizabeth C; Sun, Nanbo et al. (2016) Bayesian model reveals latent atrophy factors with dissociable cognitive trajectories in Alzheimer's disease. Proc Natl Acad Sci U S A 113:E6535-E6544