# Determining and Characterizing Substrates of Protein Degradation Impairments in Models of Alzheimer's Disease

> **NIH NIH F31** · NORTHWESTERN UNIVERSITY · 2020 · $45,520

## Abstract

Project Summary / Abstract
Alzheimer's disease (AD) is a debilitating disorder first recognized over a century ago. Since then, AD has been
extensively investigated; however, many questions remain concerning how molecular hallmarks translate to
clinical symptoms. Pathologically, AD is characterized by the misfolding and aggregation of proteins, particularly
amyloid beta 1-42 peptides (Aβ42) and hyperphosphorylated tau. Although Aβ42 accumulation is one of the
earliest pathological events, how increased levels of Aβ42 induce toxicity in neurons and contribute to synaptic
loss remains poorly understood. One hypothesis, as evidenced by the plaques and tangles found in AD patients'
brains, is that Aβ42 impairs protein degradation either by directly interacting with proteins or by sequestering or
hampering protein degradation machinery causing vulnerable proteins to persist in the brain. This project aims
to determine the specific proteins that have decreased degradation dynamics in models of AD-like pathology.
Proteins that persist for longer periods due to stunted degradation may potentially contribute to AD etiology
through loss-of-function mechanisms or by disrupting protein homeostasis balance, both of which may lead to
neuronal dysfunction. To investigate protein degradation dynamics in AD-like pathology, I am using pulse-chase
metabolic labeling in an in vivo paradigm with the recently developed APP knock-in mice. I will then analyze the
degradation rates of thousands of proteins using proteomic-based quantitative mass spectrometry. In these
experiments, proteins are labeled with “heavy” isotopes, then chased with “light” isotopes. I subsequently
measure degradation rates by monitoring the remaining “heavy” proteins. Proteins with decreased degradation
dynamics in the presence of Aβ42 may represent substrates of impaired protein degradation and may reveal
critical components in early AD pathology. Based on preliminary data, proteins with the most severe degradation
impairments were significantly enriched for proteins associated with the presynaptic active zone, especially
synaptic vesicle proteins. These proteins had impaired degradation in the cortex and hippocampus, but not the
cerebellum, a brain region where Aβ42 pathology is absent until late stages of the disease, further supporting an
Aβ42 dependent effect. These findings indicate that synaptic vesicle proteins may represent pioneering protein
networks that contribute to synaptic dysfunction in AD-like pathology. This project also aims to determine the
molecular mechanisms underlying the degradation impairment in synaptic vesicle proteins by investigating the
involvement of non-Aβ42 fragments of APP processing, as well as by investigating the role of tau. This proposal
represents a unique approach that has the potential to identify novel proteins or protein pathways that contribute
to AD etiology or early pathology, as well as determine potential mechanisms for how some proteins, which m...

## Key facts

- **NIH application ID:** 9812748
- **Project number:** 5F31AG059364-02
- **Recipient organization:** NORTHWESTERN UNIVERSITY
- **Principal Investigator:** Timothy John Hark
- **Activity code:** F31 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $45,520
- **Award type:** 5
- **Project period:** 2018-12-01 → 2020-11-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9812748

## Citation

> US National Institutes of Health, RePORTER application 9812748, Determining and Characterizing Substrates of Protein Degradation Impairments in Models of Alzheimer's Disease (5F31AG059364-02). Retrieved via AI Analytics 2026-05-24 from https://api.ai-analytics.org/grant/nih/9812748. Licensed CC0.

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