Abstract

With growing emphasis on primary and secondary prevention as long-term goals in Alzheimer's disease (AD) research, there is growing need to identify the initiating pathological cascades in asymptomatic older individuals so that preventive intervention targets can be identified to minimize underlying damage before cognitive symptoms become irreversible. Biomarkers are also urgently needed that measure the dynamic changes in those processes which contribute to progressive dementia through the long and variable course of disease, and ideally, which are widely available, affordable, and non-invasive. Multiple processes are likely to contribute to these cascades, and our knowledge of which processes combine with amyloid and neurofibrillary tangles to lead to AD is incomplete. Hence, effective primary and secondary prevention will require assessment of a broad array of biomarkers to uncover processes contributing to AD. Genetics, proteomics and neuroimaging have become increasingly important tools to identify underlying pathological processes for AD, and over the past several years, we have been advantaged by talented young investigators who are making great strides in identifying new techniques and targets for further investigation. Emory ADRC leadership and investigators have realized that gaining maximum scientific leverage for both local and national (NACC) investigators requires a Core to focus on standardized specimen collection and analysis to help move the work forward. The Biomarker Core will provide state of the art biomarkers for the ADRC and in addition, foster innovative research focusing on discovery of new intervention targets, biomarkers and pathogenic mechanisms with attention to inter-individual and racial differences in the following ways: (1) establish an ethnoracially diverse biomarker collection in the Emory ADRC cohort; (2) perform assays for established CSF AD biomarkers; (3) support network-wide neuroimaging initiatives and evaluate promising exploratory sequences; and (4) establish standard genetic profiles for the UDS cohort and explore potential gene expression and epigenomic changes relevant to AD. The Biomarker Core will work to optimize interdisciplinary research by providing a framework for standardized neuroimaging, proteomic and genomic measurements for a subset of our Emory ADRC Clinical Core cohort. The Biomarker Core will also enhance the Center's overall mission to work collaboratively to advance high impact AD research, care, and education, including support of NACC, ADCS, ADGC, ADNI, and other federal, state, and community centers, programs and agencies by making data and specimens available through NACC and NCRAD. By increasing the phenotyping data available to further distinguish our study population, we anticipate further illuminating the trajectory and variables that differentiate normal aging from the onset, progression, and clinical manifestation of AD.

Public Health Relevance

The Biomarker Core will help the Emory ADRC implement state of the art biological markers and pathological processes for Alzheimer's disease, including amyloid and tau measures in CSF, mass spectrometry based novel protein biomarkers emerging from AMP-AD, harmonized MRI protocols, and advanced genetic data and analytics. The Core will extend access to these services and foster discoveries that will accelerate development of new candidate biomarkers. Current and future biomarkers will play a key role in the field's progress in slowing and preventing the disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Specialized Center (P50)
Project #
3P50AG025688-15S1
Application #
9705590
Study Section
Special Emphasis Panel (ZAG1)
Program Officer
Silverberg, Nina B
Project Start
2005-04-01
Project End
2021-04-30
Budget Start
2019-05-01
Budget End
2021-04-30
Support Year
15
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Emory University
Department
Neurology
Type
Schools of Medicine
DUNS #
066469933
City
Atlanta
State
GA
Country
United States
Zip Code
30322

  Publications

Barnes, Josephine; Bartlett, Jonathan W; Wolk, David A et al. (2018) Disease Course Varies According to Age and Symptom Length in Alzheimer's Disease. J Alzheimers Dis 64:631-642
Schaffert, Jeff; LoBue, Christian; White, Charles L et al. (2018) Traumatic brain injury history is associated with an earlier age of dementia onset in autopsy-confirmed Alzheimer's disease. Neuropsychology 32:410-416
Kotlar, Alex V; Trevino, Cristina E; Zwick, Michael E et al. (2018) Bystro: rapid online variant annotation and natural-language filtering at whole-genome scale. Genome Biol 19:14
Walker, Lary C (2018) Prion-like mechanisms in Alzheimer disease. Handb Clin Neurol 153:303-319
Burke, Shanna L; Maramaldi, Peter; Cadet, Tamara et al. (2018) Decreasing hazards of Alzheimer's disease with the use of antidepressants: mitigating the risk of depression and apolipoprotein E. Int J Geriatr Psychiatry 33:200-211
Davis, Jeremy J (2018) Performance validity in older adults: Observed versus predicted false positive rates in relation to number of tests administered. J Clin Exp Neuropsychol 40:1013-1021
Jucker, Mathias; Walker, Lary C (2018) Propagation and spread of pathogenic protein assemblies in neurodegenerative diseases. Nat Neurosci 21:1341-1349
Rangaraju, Srikant; Dammer, Eric B; Raza, Syed Ali et al. (2018) Identification and therapeutic modulation of a pro-inflammatory subset of disease-associated-microglia in Alzheimer's disease. Mol Neurodegener 13:24
Qian, Winnie; Fischer, Corinne E; Schweizer, Tom A et al. (2018) Association Between Psychosis Phenotype and APOE Genotype on the Clinical Profiles of Alzheimer's Disease. Curr Alzheimer Res 15:187-194
Lin, Ming; Gong, Pinghua; Yang, Tao et al. (2018) Big Data Analytical Approaches to the NACC Dataset: Aiding Preclinical Trial Enrichment. Alzheimer Dis Assoc Disord 32:18-27

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