RF1NS110437
Project Grant
Overview
Grant Description
Structure of Amyloid Fibrils in Human Neurodegenerative Diseases and Aging - Project Summary/Abstract
Recently, significant progress in understanding tauopathies and how tau aggregates lead to neurodegeneration has been made by the description of the atomic structures of tau filaments from human brain. We have established that the morphology of tau filaments comprising of all six tau isoforms (3R+4R TAU) in diseases associated with extracellular amyloid deposition is identical, regardless of the amino acid sequence of the amyloid subunit.
To gain further understanding on how different amyloids elicit a tau response comprising of 3R+4R TAU with a common fold (AD fold), we characterized the structures of filaments of human extracellular amyloid-SS (ASS) in Alzheimer disease (AD) and prion protein amyloid (APRP) in prion diseases. In addition, we characterized the structures of a-synuclein filaments in diffuse Lewy body disease, Parkinson disease, and multiple system atrophy, and TMEM106B filaments in several neurodegenerative diseases and aging.
The studies proposed in this MPI application are a logical continuation of this groundbreaking work. These studies are in response to PAR-22-208 “Structural Biology of Alzheimer's Disease Related Dementias (ADRDS) Proteinopathies” (R01). The main goals of this application are to continue to characterize, from brain tissue, the structure of filaments at high atomic-level resolution for future use in PET ligand development and other related purposes, with special emphasis on mutations/genotypes and sporadic versus familial forms of disease, different ages of onset (e.g. early vs. late onset), and presence of co-pathologies.
In addition, we propose to characterize fibrils derived from in vivo sources such as relevant animal models and biologically relevant in vitro systems, and to synthesize, identify, and characterize amyloid-specific ligands. In order to achieve our goals, our proposal has three specific aims.
The first aim is to perform cryo-EM studies on a large cohort of EOAD individuals with different APOE genotypes and age at onset, and familial EOAD individuals with different clinical, genetic, and neuropathologic features. In addition, we will determine for the first time the structure of filaments in individuals with Down syndrome, familial British and Danish dementia, and the structure and identity of Biondi bodies.
Second, we will generate a cryo-EM map and determine the corresponding atomic models of filaments extracted from the brain of murine models and generate high-resolution 3D images of the amyloid structures.
Lastly, we will characterize by cryo-EM the structure of recombinant tau and synthetic peptides homologous to ASS, ABRI, and ADAN and compare our results with the peptides isolated from human and animal models. We will also synthesize, identify, and characterize amyloid-specific ligands.
Recently, significant progress in understanding tauopathies and how tau aggregates lead to neurodegeneration has been made by the description of the atomic structures of tau filaments from human brain. We have established that the morphology of tau filaments comprising of all six tau isoforms (3R+4R TAU) in diseases associated with extracellular amyloid deposition is identical, regardless of the amino acid sequence of the amyloid subunit.
To gain further understanding on how different amyloids elicit a tau response comprising of 3R+4R TAU with a common fold (AD fold), we characterized the structures of filaments of human extracellular amyloid-SS (ASS) in Alzheimer disease (AD) and prion protein amyloid (APRP) in prion diseases. In addition, we characterized the structures of a-synuclein filaments in diffuse Lewy body disease, Parkinson disease, and multiple system atrophy, and TMEM106B filaments in several neurodegenerative diseases and aging.
The studies proposed in this MPI application are a logical continuation of this groundbreaking work. These studies are in response to PAR-22-208 “Structural Biology of Alzheimer's Disease Related Dementias (ADRDS) Proteinopathies” (R01). The main goals of this application are to continue to characterize, from brain tissue, the structure of filaments at high atomic-level resolution for future use in PET ligand development and other related purposes, with special emphasis on mutations/genotypes and sporadic versus familial forms of disease, different ages of onset (e.g. early vs. late onset), and presence of co-pathologies.
In addition, we propose to characterize fibrils derived from in vivo sources such as relevant animal models and biologically relevant in vitro systems, and to synthesize, identify, and characterize amyloid-specific ligands. In order to achieve our goals, our proposal has three specific aims.
The first aim is to perform cryo-EM studies on a large cohort of EOAD individuals with different APOE genotypes and age at onset, and familial EOAD individuals with different clinical, genetic, and neuropathologic features. In addition, we will determine for the first time the structure of filaments in individuals with Down syndrome, familial British and Danish dementia, and the structure and identity of Biondi bodies.
Second, we will generate a cryo-EM map and determine the corresponding atomic models of filaments extracted from the brain of murine models and generate high-resolution 3D images of the amyloid structures.
Lastly, we will characterize by cryo-EM the structure of recombinant tau and synthetic peptides homologous to ASS, ABRI, and ADAN and compare our results with the peptides isolated from human and animal models. We will also synthesize, identify, and characterize amyloid-specific ligands.
Awardee
Funding Goals
NOT APPLICABLE
Grant Program (CFDA)
Funding Agency
Place of Performance
Indianapolis,
Indiana
462022915
United States
Geographic Scope
Single Zip Code
Related Opportunity
Analysis Notes
Amendment Since initial award the total obligations have increased 3% from $3,924,261 to $4,038,617.
Trustees Of Indiana University was awarded
Structure of Amyloid Fibrils in Neurodegenerative Diseases & Aging
Project Grant RF1NS110437
worth $4,038,617
from National Institute on Aging in September 2018 with work to be completed primarily in Indianapolis Indiana United States.
The grant
has a duration of 8 years and
was awarded through assistance program 93.866 Aging Research.
The Project Grant was awarded through grant opportunity Structural Biology of Alzheimer's Disease Related Dementias (ADRDs) Proteinopathies (R01 Clinical Trial Not Allowed).
Status
(Ongoing)
Last Modified 6/20/24
Period of Performance
9/30/18
Start Date
8/31/26
End Date
Funding Split
$4.0M
Federal Obligation
$0.0
Non-Federal Obligation
$4.0M
Total Obligated
Activity Timeline
Subgrant Awards
Disclosed subgrants for RF1NS110437
Transaction History
Modifications to RF1NS110437
Additional Detail
Award ID FAIN
RF1NS110437
SAI Number
RF1NS110437-2210071527
Award ID URI
SAI UNAVAILABLE
Awardee Classifications
Public/State Controlled Institution Of Higher Education
Awarding Office
75NQ00 NIH NATIONAL INSTITUTE OF NEUROLOGICAL DISORDERS AND STROKE
Funding Office
75NN00 NIH NATIONAL INSITUTE ON AGING
Awardee UEI
SHHBRBAPSM35
Awardee CAGE
434D9
Performance District
IN-07
Senators
Todd Young
Mike Braun
Mike Braun
Budget Funding
| Federal Account | Budget Subfunction | Object Class | Total | Percentage |
|---|---|---|---|---|
| National Institute on Aging, National Institutes of Health, Health and Human Services (075-0843) | Health research and training | Grants, subsidies, and contributions (41.0) | $3,924,261 | 100% |
Modified: 6/20/24