# Decoding Selective Vulnerability: Effectors and Regulators of Tau Lesion Spread in Alzheimer's Disease

> **NIH NIH F30** · OHIO STATE UNIVERSITY · 2024 · $44,879

## Abstract

Abstract
Alzheimer’s Disease (AD) is the most common cause of dementia and a major cause of morbidity in the United
States, yet there remains no disease-modifying therapy as the mechanism of disease is incompletely
understood. AD is defined by the accumulation of two protein lesions in the brain, amyloid-β plaques and
neurofibrillary tangles. Neurofibrillary tangles, which are composed of aggregated tau protein, are a better marker
of disease progression than amyloid-β, correlating with neuron loss and cognitive decline. Notably, tau tangles
spread through the brain in a stereotypical fashion defined by Braak staging, starting in the locus coeruleus and
spreading along networked synapses. This suggests that misfolded tau is propagated across the synapse,
templating normal tau to become misfolded as well and generate new lesions. However, some regions never
develop tau lesions despite parallel synaptic exposure to the locus coeruleus, suggesting selective vulnerability
of different regions to tau lesions. Although some cases of AD are due to dominant single gene mutations, the
vast majority of AD cases are sporadic with no clear genetic cause. One approach to such complexity is to study
the gene expression response to disease in order to capture functional interactions between genes. Most
transcriptomic studies have limited their analysis to the disease response in affected areas of the brain,
comparing diseased individuals to normal controls. In contrast, our analysis incorporates the selective
vulnerability of specific brain regions to developing tau lesions, comparing a lesion-affected area of the brain
(prefrontal cortex) to a lesion-protected area (cerebellum) in both diseased and control individuals. According to
the premise that both regions receive the same anterograde tau insult, but differential expression uniquely
protects the cerebellum, this comparison will highlight the drivers of neuroprotection in areas that never develop
lesions. This approach has yielded a list of candidate drivers of disease neuroprotection, notably enriching for
chaperone proteins that regulate protein folding. Our analysis also identified several transcription factors (TF)
candidates, such as the core clock regulator BHLHE40. This aligns with observations of several circadian
phenotypes observed in AD, such as the increased risk of AD among patients with sleep disorders and vice
versa. This proposal aims to test our candidate driver genes through several approaches. Aim 1 will test the
identified chaperone proteins for functional inhibition of tau misfolding in both a biochemical model of induced
recombinant tau fibrillization and in vitro with a cellular biosensor of tau aggregation. Aim 2 will test TF candidates
for modulation of tau aggregate accumulation in vitro with a cellular biosensor of tau aggregation. Finally, Aim 3
will test how a circadian TF, BHLHE40, modulates tau spreading in a mouse model of misfolded tau seed
injection. Together these aims wi...

## Key facts

- **NIH application ID:** 10899770
- **Project number:** 5F30AG072804-03
- **Recipient organization:** OHIO STATE UNIVERSITY
- **Principal Investigator:** Christopher Anthony Ayoub
- **Activity code:** F30 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $44,879
- **Award type:** 5
- **Project period:** 2022-09-01 → 2025-05-04

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10899770

## Citation

> US National Institutes of Health, RePORTER application 10899770, Decoding Selective Vulnerability: Effectors and Regulators of Tau Lesion Spread in Alzheimer's Disease (5F30AG072804-03). Retrieved via AI Analytics 2026-05-24 from https://api.ai-analytics.org/grant/nih/10899770. Licensed CC0.

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