R01AG089497
Project Grant
Overview
Grant Description
A proteomic comparison of sporadic early-onset, late-onset, and autosomal dominant Alzheimer's disease - Project summary
Alzheimer’s disease (AD) is commonly considered a disease exclusive to the elderly.
While aging is the largest risk factor for the development of AD, approximately 5 to 10 percent of AD develops in people younger than age 65.
In most early-onset AD cases there is no clearly identifiable genetic mutation that causes the disease, and therefore such cases have been termed sporadic early-onset AD (SEOAD).
Compared to late-onset AD (LOAD) or autosomal dominant forms of AD (ADAD), little is known about the pathophysiology of SEOAD.
In contrast to LOAD and ADAD, SEOAD more often presents with clinical syndromes that affect visual-spatial, language, executive and behavioral cognitive domains, and on average has a more rapidly progressive course compared to LOAD.
Whether the underlying pathophysiology and biological pathway alterations, and biofluid biomarkers that reflect these changes, are the same in SEOAD as those in LOAD and ADAD is unknown.
Our previous brain proteomic studies on LOAD through the Accelerating Medicines Partnership for AD (AMP-AD) have revealed many different pathological changes in LOAD beyond amyloid-β and tau dyshomeostasis.
The goal of this project is to apply a similar proteomic approach to SEOAD to advance our understanding of SEOAD pathophysiology and how it is similar or distinct from LOAD and ADAD pathophysiology.
We hypothesize that SEOAD will have more severe changes in mitochondrial, proteostasis, complement, and RNA-associated protein pathways compared to LOAD and ADAD.
We will leverage a multi-platform discovery proteomic approach to analyze SEOAD and LOAD cerebrospinal fluid (CSF) and plasma to determine whether differences in EOAD brain pathophysiology can be observed in biofluids, and how these changes are related between CSF and plasma compartments.
From our cross-tissue proteomic data we will assess which brain-linked biomarkers in SEOAD are most predictive of cognitive decline.
These studies will significantly increase our understanding of the protein network changes that characterize SEOAD and how they are similar or unique to those observed in LOAD and ADAD.
Such knowledge will be critical to ensuring that therapies and biomarkers developed for LOAD are applicable to those with early-onset forms of AD.
Alzheimer’s disease (AD) is commonly considered a disease exclusive to the elderly.
While aging is the largest risk factor for the development of AD, approximately 5 to 10 percent of AD develops in people younger than age 65.
In most early-onset AD cases there is no clearly identifiable genetic mutation that causes the disease, and therefore such cases have been termed sporadic early-onset AD (SEOAD).
Compared to late-onset AD (LOAD) or autosomal dominant forms of AD (ADAD), little is known about the pathophysiology of SEOAD.
In contrast to LOAD and ADAD, SEOAD more often presents with clinical syndromes that affect visual-spatial, language, executive and behavioral cognitive domains, and on average has a more rapidly progressive course compared to LOAD.
Whether the underlying pathophysiology and biological pathway alterations, and biofluid biomarkers that reflect these changes, are the same in SEOAD as those in LOAD and ADAD is unknown.
Our previous brain proteomic studies on LOAD through the Accelerating Medicines Partnership for AD (AMP-AD) have revealed many different pathological changes in LOAD beyond amyloid-β and tau dyshomeostasis.
The goal of this project is to apply a similar proteomic approach to SEOAD to advance our understanding of SEOAD pathophysiology and how it is similar or distinct from LOAD and ADAD pathophysiology.
We hypothesize that SEOAD will have more severe changes in mitochondrial, proteostasis, complement, and RNA-associated protein pathways compared to LOAD and ADAD.
We will leverage a multi-platform discovery proteomic approach to analyze SEOAD and LOAD cerebrospinal fluid (CSF) and plasma to determine whether differences in EOAD brain pathophysiology can be observed in biofluids, and how these changes are related between CSF and plasma compartments.
From our cross-tissue proteomic data we will assess which brain-linked biomarkers in SEOAD are most predictive of cognitive decline.
These studies will significantly increase our understanding of the protein network changes that characterize SEOAD and how they are similar or unique to those observed in LOAD and ADAD.
Such knowledge will be critical to ensuring that therapies and biomarkers developed for LOAD are applicable to those with early-onset forms of AD.
Awardee
Funding Goals
TO ENCOURAGE BIOMEDICAL, SOCIAL, AND BEHAVIORAL RESEARCH AND RESEARCH TRAINING DIRECTED TOWARD GREATER UNDERSTANDING OF THE AGING PROCESS AND THE DISEASES, SPECIAL PROBLEMS, AND NEEDS OF PEOPLE AS THEY AGE. THE NATIONAL INSTITUTE ON AGING HAS ESTABLISHED PROGRAMS TO PURSUE THESE GOALS. THE DIVISION OF AGING BIOLOGY EMPHASIZES UNDERSTANDING THE BASIC BIOLOGICAL PROCESSES OF AGING. THE DIVISION OF GERIATRICS AND CLINICAL GERONTOLOGY SUPPORTS RESEARCH TO IMPROVE THE ABILITIES OF HEALTH CARE PRACTITIONERS TO RESPOND TO THE DISEASES AND OTHER CLINICAL PROBLEMS OF OLDER PEOPLE. THE DIVISION OF BEHAVIORAL AND SOCIAL RESEARCH SUPPORTS RESEARCH THAT WILL LEAD TO GREATER UNDERSTANDING OF THE SOCIAL, CULTURAL, ECONOMIC AND PSYCHOLOGICAL FACTORS THAT AFFECT BOTH THE PROCESS OF GROWING OLD AND THE PLACE OF OLDER PEOPLE IN SOCIETY. THE DIVISION OF NEUROSCIENCE FOSTERS RESEARCH CONCERNED WITH THE AGE-RELATED CHANGES IN THE NERVOUS SYSTEM AS WELL AS THE RELATED SENSORY, PERCEPTUAL, AND COGNITIVE PROCESSES ASSOCIATED WITH AGING AND HAS A SPECIAL EMPHASIS ON ALZHEIMER'S DISEASE. SMALL BUSINESS INNOVATION RESEARCH (SBIR) PROGRAM: TO EXPAND AND IMPROVE THE SBIR PROGRAM, TO INCREASE PRIVATE SECTOR COMMERCIALIZATION OF INNOVATIONS DERIVED FROM FEDERAL RESEARCH AND DEVELOPMENT, TO INCREASE SMALL BUSINESS PARTICIPATION IN FEDERAL RESEARCH AND DEVELOPMENT, AND TO FOSTER AND ENCOURAGE PARTICIPATION OF SOCIALLY AND ECONOMICALLY DISADVANTAGED SMALL BUSINESS CONCERNS AND WOMEN-OWNED SMALL BUSINESS CONCERNS IN TECHNOLOGICAL INNOVATION. SMALL BUSINESS TECHNOLOGY TRANSFER (STTR) PROGRAM: TO STIMULATE AND FOSTER SCIENTIFIC AND TECHNOLOGICAL INNOVATION THROUGH COOPERATIVE RESEARCH DEVELOPMENT CARRIED OUT BETWEEN SMALL BUSINESS CONCERNS AND RESEARCH INSTITUTIONS, TO FOSTER TECHNOLOGY TRANSFER BETWEEN SMALL BUSINESS CONCERNS AND RESEARCH INSTITUTIONS, TO INCREASE PRIVATE SECTOR COMMERCIALIZATION OF INNOVATIONS DERIVED FROM FEDERAL RESEARCH AND DEVELOPMENT, AND TO FOSTER AND ENCOURAGE PARTICIPATION OF SOCIALLY AND ECONOMICALLY DISADVANTAGED SMALL BUSINESS CONCERNS AND WOMEN-OWNED SMALL BUSINESS CONCERNS IN TECHNOLOGICAL INNOVATION.
Grant Program (CFDA)
Awarding / Funding Agency
Place of Performance
Atlanta,
Georgia
303221047
United States
Geographic Scope
Single Zip Code
Related Opportunity
Analysis Notes
Amendment Since initial award the total obligations have increased 105% from $2,840,883 to $5,825,826.
Emory University was awarded
Proteomic Comparison of SEOAD, LOAD, and ADAD in Alzheimer's
Project Grant R01AG089497
worth $5,825,826
from National Institute on Aging in September 2024 with work to be completed primarily in Atlanta Georgia United States.
The grant
has a duration of 4 years 10 months and
was awarded through assistance program 93.866 Aging Research.
The Project Grant was awarded through grant opportunity Research on Current Topics in Alzheimer's Disease and Its Related Dementias (R01 Clinical Trial Optional).
Status
(Ongoing)
Last Modified 8/20/25
Period of Performance
9/30/24
Start Date
7/31/29
End Date
Funding Split
$5.8M
Federal Obligation
$0.0
Non-Federal Obligation
$5.8M
Total Obligated
Activity Timeline
Transaction History
Modifications to R01AG089497
Additional Detail
Award ID FAIN
R01AG089497
SAI Number
R01AG089497-3962478248
Award ID URI
SAI UNAVAILABLE
Awardee Classifications
Private Institution Of Higher Education
Awarding Office
75NN00 NIH National Insitute on Aging
Funding Office
75NN00 NIH National Insitute on Aging
Awardee UEI
S352L5PJLMP8
Awardee CAGE
2K291
Performance District
GA-05
Senators
Jon Ossoff
Raphael Warnock
Raphael Warnock
Modified: 8/20/25