# Project 1: Differential Roles of ApoE Isoforms in Neural Network Dysfunction of Alzheimer's Disease

> **NIH NIH P01** · J. DAVID GLADSTONE INSTITUTES · 2021 · $942,704

## Abstract

PROJECT 1 – SUMMARY
The complexity and multifactorial nature of Alzheimer’s disease (AD) pose unique challenges for mechanistic
studies and developing therapies. Although the three major pathogenic factors of AD—amyloid-beta peptides,
tau, and apolipoprotein E4 (apoE4)—have been extensively studied as independent entities in AD pathogenesis,
efforts to target individual AD-related pathways, such as Ab production or clearance, have largely failed in human
trials. Emerging evidence strongly suggests that AD is a consequence of age-dependent neural network
dysfunction in brain regions that mostly affect cognition, likely through the interactive effects of multiple
pathogenic factors. Thus, there is a pressing need to identify novel mechanisms and therapeutic targets, at a
neural network level and in the context of interactions between multiple pathogenic factors—the focus of this
proposal.
 APOE4, which encodes one of the three major isoforms of apoE in humans, is the major genetic risk factor for
AD and lowers the age of onset in a gene dose-dependent manner. In most clinical studies, APOE4 carriers
account for 60–75% of AD cases, highlighting the importance of APOE4 in AD pathogenesis. On the other hand,
many clinical and population studies show that APOE2, encoding the rarest apoE isoform, is a strongly protective
genetic factor in AD. A pathological hallmark of AD is the formation of neurofibrillary tangles (NFTs) consisting
of hyperphosphorylated, insoluble tau, containing both 3R and 4R tau isoforms. In cell cultures and mouse
models, apoE isoforms have tau-dependent differential effects, and tau has apoE isoform-dependent effects,
suggesting interactive roles in AD pathogenesis. However, almost all of these studies of apoE isoforms and tau
drew conclusions based either on mouse tau, which is present almost exclusively as 4R tau, or on mutant human
tau, which is associated with frontotemporal dementia but not AD. In Project 1, we propose to determine cell-
type-specific, differential roles of apoE isoforms in age-dependent neural network dysfunction and behavioral
deficits, in the context of wildtype (WT) human tau (both 3R and 4R tau isoforms), in novel mouse models of AD.
 In Aim 1, we will determine differential roles of apoE isoforms in neural network dysfunction and behavioral
deficits, using apoE-isoform-floxed knock-in (APOEfE2/fE2 [fE2], APOEfE3/fE3 [fE3], and APOEfE4/fE4 [fE4]) mice
expressing WT human tau (MAPT knock-in or TAUWT) at different ages. In Aim 2, we will determine cell-type-
specific, differential roles of apoE isoforms in neural network dysfunction and behavioral deficits, using
fE2/TAUWT, fE3/TAUWT, and fE4/TAUWT mice expressing cell-type-specific Cre recombinase (neuron-specific
Cresyn1, astrocyte-specific CreGFAP, and microglia-specific CreCx3cr1) in order to delete the APOE allele in a cell-
type-specific manner. The studies in this project, together with those of the three other projects of this program
project gran...

## Key facts

- **NIH application ID:** 10271126
- **Project number:** 1P01AG073082-01
- **Recipient organization:** J. DAVID GLADSTONE INSTITUTES
- **Principal Investigator:** YADONG HUANG
- **Activity code:** P01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2021
- **Award amount:** $942,704
- **Award type:** 1
- **Project period:** 2021-08-15 → 2026-07-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10271126

## Citation

> US National Institutes of Health, RePORTER application 10271126, Project 1: Differential Roles of ApoE Isoforms in Neural Network Dysfunction of Alzheimer's Disease (1P01AG073082-01). Retrieved via AI Analytics 2026-05-21 from https://api.ai-analytics.org/grant/nih/10271126. Licensed CC0.

---

*[NIH grants dataset](/datasets/nih-grants) · CC0 1.0*