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ABCA7 Lipid Transport and Microglial Phagocytosis AD Causal Chain

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ABCA7 Lipid Transport and Microglial Phagocytosis AD Causal Chain

Overview

ABCA7 (ATP-Binding Cassette Transporter A7) is a major Alzheimer's disease (AD) risk gene identified through genome-wide association studies (GWAS)[@kim2015][@holstege2017]. The ABCA7 protein plays a critical role in lipid transport, particularly in the regulation of apolipoprotein E (APOE) lipidation and microglial function. Loss-of-function variants in ABCA7 approximately double AD risk, making it one of the strongest genetic modifiers of AD pathogenesis[@kim2015]. This causal chain traces the molecular pathway from ABCA7 genetic variants through lipid homeostasis disruption and impaired microglial phagocytosis to amyloid-beta accumulation and AD progression.

ABCA7 Genetic Architecture

GWAS-Identified Risk Variants

Common variants in the ABCA7 locus have been consistently associated with AD risk in multiple GWAS meta-analyses:

| Variant | Risk Allele | Odds Ratio | Population |
|---------|-------------|------------|-------------|
| rs3764650 | G | 1.23 | European |
| rs4149268 | A | 1.15 | European |
| rs2279796 | T | 1.18 | European |
| rs5986736 | G | 1.21 | European |

The rs3764650 variant, located in a splice donor site, creates a cryptic splice site leading to truncated ABCA7 protein with reduced function[@kim2015]. This variant is one of the most significant AD risk alleles outside the APOE locus.

Rare Loss-of-Function Variants


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