# APOE Genotype Mediated Effects on Alzheimer Disease Risk and Mechanisms

> **NIH NIH U01** · BOSTON UNIVERSITY MEDICAL CAMPUS · 2024 · $810,698

## Abstract

ABSTRACT
The APOE ɛ2 and ɛ4 alleles are by far the strongest and most well-established common genetic risk factors for
Alzheimer disease (AD). The deleterious effect of ɛ4 on AD risk is dependent on dose, age, sex, and ethnicity,
but the protective effect of ɛ2 is is less well studied. We will build upon our previous work aimed at identifying
mechanisms underlying the associations of AD with the ɛ2 and ɛ4 alleles in multiple population groups. Recently,
we identified a highly significant association of AD with PPP2CB among ɛ2 carriers. PPP2CB encodes the
catalytic subunit of protein phosphatase 2A, which is known to dephosphorylate tau protein. Complement C4A
and C4B were the most significantly differentially expressed genes in brain tissue from AD cases and controls
with the ɛ2/ɛ3 genotype, and we showed that levels of C4b and PPP2CB proteins are significantly correlated.
We also identified a novel genome-wide significant association of AD with MGMT that is specific to women
lacking ɛ4 (ε4-). Omics analyses of brain-derived data showed significant association of (1) MGMT AD risk alleles
with increased MGMT methylation (2) MGMT methylation with MGMT expression and worse AD-related
pathology in ε4- women. This proposed project will identify new ε2- and ε4-mediated AD associations using a
greatly enlarged multi-ethnic Alzheimer Disease Genetics Consortium GWAS sample and GWAS datasets from
European AD genetics consortia which include more than 240,000 subjects. Next, we will identify functional
variants in the identified loci in large whole genome whole exome sequencing datasets from diverse populations
assembled by the Alzheimer Disease Sequencing Project. We will calculate ethnicity-specific AD polygenic risk
scores (PRS) for APOE genotype subgroups and evaluate the moderating effect of each PRS score on AD risk
associated with ɛ2 and ɛ4. In a second aim, we will perform proteomic studies in plasma from 2,813 Framingham
Heart Study participants to identify proteins whose expression is associated with AD status and measures of
cognitive performance in the total sample and APOE genotype groups. We will then investigate methylation and
transcriptome profiles in the APOE related loci in 1,391 blood and 952 brain samples from European and African
ancestry subjects. APOE genotype-dependent omics signatures derived from these analyses will be validated
by testing their association with AD-related neuropathological traits and other proteins measured in brain by
multiplex immunofluorescence. Finally, in a third aim we will determine mechanisms through which genes
identified by GWAS confer protection against AD pathophysiology using a novel human iPSC-derived human
3D spheroid model of AD that allows testing of multiple brain cell types. We will generate the model by growing
induced neurons, astrocytes and microglia separately in 2D cultures, and then combining them in 3D cultures
where the integrated neurodegenerative process ensues. We will selectively t...

## Key facts

- **NIH application ID:** 10879309
- **Project number:** 1U01AG082665-01A1
- **Recipient organization:** BOSTON UNIVERSITY MEDICAL CAMPUS
- **Principal Investigator:** Lindsay A. Farrer
- **Activity code:** U01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $810,698
- **Award type:** 1
- **Project period:** 2024-09-15 → 2029-06-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10879309

## Citation

> US National Institutes of Health, RePORTER application 10879309, APOE Genotype Mediated Effects on Alzheimer Disease Risk and Mechanisms (1U01AG082665-01A1). Retrieved via AI Analytics 2026-05-24 from https://api.ai-analytics.org/grant/nih/10879309. Licensed CC0.

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