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Grants > Tracking Immune Cells in Alzheimer's Disease Brains Updated On: Ene. 20, 2025
Alzheimer's Disease Research Grant

Tracking Immune Cells in Alzheimer's Disease Brains

a headshot of Dr. Gate

Principal Investigator

David Gate, PhD

Northwestern University Feinberg School of Medicine

Chicago, IL, USA

About the Research Project

Program

Alzheimer's Disease Research

Award Type

Standard

Award Amount

$300,000

Active Dates

July 01, 2023 - June 30, 2026

Grant ID

A2023003S

Acknowledgement

Recipient of the Distinguished Investigator Award for Alzheimer’s Disease Research.

Goals

The project aim is to apply sophisticated techniques to brain samples from people with and without Alzheimer’s disease to compare their molecular and immune cell profiles.

Summary

For this project, David Gate, PhD, and his lab team will use postmortem tissue samples from people who had Alzheimer’s disease and people who did not. With sophisticated molecular tools, the researchers will compare differences between samples in terms of cell types, protein production, and the presence of misfolded proteins, which are implicated in Alzheimer’s disease. Taking an innovative approach with these tools, they will develop a snapshot in time of all of the proteins in production when the tissues were taken and flash frozen. The process also allows for proteins that are misfolded to be tagged and their locations to be captured using imaging.

This work will test the team’s hypothesis that specific immune cells called T cells will be found in the same places as misfolded tau and amyloid-beta, key proteins in Alzheimer’s disease. If the findings support their hypothesis, the presence of T cells will imply an immune system response to brain inflammation in Alzheimer’s disease, related to how the misfolded proteins attract the attention of T cells. Identifying such a link opens up new avenues for research into therapeutic targets.

Unique and Innovative

We will utilize an innovative proteogenomics approach new to the study of neurodegenerative disease. Our proteogenomics workflow will capture the whole transcriptome while simultaneously allowing for the labeling and imaging of pathogenic misfolded proteins.

Foreseeable Benefits

Successful completion of these aims will provide insight into the role of adaptive immunity in neuroinflammation associated with AD.