# Project 3: Models of neurodegenerative aggregate formation

> **NIH NIH P01** · UNIV OF ARKANSAS FOR MED SCIS · 2020 · $239,722

## Abstract

Abstract
Protein aggregation is a hallmark of diverse neurodegenerative diseases, including Alzheimer, Huntington and
Parkinson Diseases (AD, HD and PD) which will be studied in this Program Project, but little is known about
the role of aggregates in neurotoxicity or clinical manifestations. Different brain regions are affected in each
disease, underlying their distinctive pathologies, and different diagnostic proteins are detected immunologically
for each (presumably reflecting distinct proteins that initiate or feed aggregates due to their high abundance or
post-synthetic modifications in the vulnerable tissue). Increasingly, however, proteins “characteristic” of one
neuropathy have been detected in other disease aggregates, leading us to the hypothesis that a common
aggregation mechanism is involved. To learn what features cause proteins to coalesce with the “seed proteins”
(i. e., the mutated and/or misfolded protein that initiates aggregation), we propose a systematic proteomic
comparison of aggregates purified from affected tissue of each disease, using unaffected tissue from patients
and corresponding areas of normal brain as controls. Our preliminary proteomic analyses show that immuno-
affinity for tau or Aβ allows isolation of two distinctive types of aggregates, which nevertheless share many
proteins in common. Aggregates derived from AD vs. age-matched-control (AMC) hippocampus differ strikingly
in protein composition, whether they bind tau or Aβ antibodies. These results are supported by images
showing co-localization of proteins by immunohistochemical and proximity-ligation methods, and by C. elegans
models of AD in which orthologs of identified AD-aggregate proteins contribute functionally to aggregation and
associated traits. In Aim 1, proteomic analyses of proteins (and their most common modifications) from AD,
PD, HD and AMC tissues will enable us to seek features common to two or three diseases or unique to each.
We will also seek “leading indicators” of AD, in individuals at highest risk (based on ApoE4 alleles, age or
Down Syndrome) and in 3xTg-AD mice prior to overt AD pathology. We will then analyze aggregates from
various cell and worm models, to prioritize these based on their similarity to the disease aggregates they
mimic. In Aim 2, we will identify cross-linked peptides from aggregates, defining protein:protein contacts that
Project 1 will attempt to confirm by immuno-stain colocalization, and by proximity-ligation PCR. These results
will guide molecular-dynamic modeling of aggregate formation, in which we can assess the energies (‒ΔE and
‒ΔG) driving and stabilizing protein accretion, and test the effects of mutating putative contact residues. Key
aggregate proteins seen in multiple diseases (Aim 1) will be tested for functional roles and pathways
employed, using RNAi in neuroblastoma cells (SY5Y-APP) and worm models. NSAID-derived compounds from
Core D will be screened in Aim 3 for protection of SY5Y-APP cells from ...

## Key facts

- **NIH application ID:** 9964622
- **Project number:** 5P01AG012411-21
- **Recipient organization:** UNIV OF ARKANSAS FOR MED SCIS
- **Principal Investigator:** Robert Joseph Shmookler Reis
- **Activity code:** P01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $239,722
- **Award type:** 5
- **Project period:** 1997-08-01 → 2023-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9964622

## Citation

> US National Institutes of Health, RePORTER application 9964622, Project 3: Models of neurodegenerative aggregate formation (5P01AG012411-21). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/9964622. Licensed CC0.

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