TREM2 Function in Alzheimer's Disease — From Risk Variant to Therapeutic Target
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experiment665 wordssynced 2026-04-02
TREM2 Function in Alzheimer's Disease
Overview
This experiment addresses the critical AD knowledge gap: "What is the function of TREM2 variants in AD risk?" (ranked #13 in AD Knowledge Gaps with 30 points). TREM2 R47H increases AD risk 3x, making it a major genetic risk factor.
Supports microglial survival — prevents cell death
Modulates inflammatory response — balances pro/anti-inflammatory states
Enhances metabolic fitness — supports mitochondrial function
The R47H variant reduces ligand binding (lipids, Aβ) by ~40%, impairing these functions.
Study Design
Component 1: Mechanistic Studies
Approach: Multi-omics characterization of TREM2 function
| Model | N | Analysis | |-------|---|----------| | TREM2 knock-in mice | Variable | RNA-seq, ATAC-seq | | iPSC microglia (R47H vs WT) | 20 | Single-cell RNA-seq | | Human postmortem brain | 60 | Spatial transcriptomics |
Component 2: TREM2 Agonist Trials
Phase 1b/2a Trial Design:
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TREM2 Function in Alzheimer's Disease
Overview
This experiment addresses the critical AD knowledge gap: "What is the function of TREM2 variants in AD risk?" (ranked #13 in AD Knowledge Gaps with 30 points). TREM2 R47H increases AD risk 3x, making it a major genetic risk factor.
| System | Use | Strength | |--------|-----|----------| | Human iPSC microglia | Primary model | Patient-specific | | TREM2 R47H knock-in mice | In vivo | Genetic model | | Postmortem brain tissue | Validation | Human relevance | | Cerebral organoids with microglia | Development | 3D model |
Feasibility Assessment
| Factor | Assessment | |--------|------------| | Technical Feasibility | High — TREM2 antibodies in development | | Recruitment Feasibility | Moderate — genetic testing required | | Cost Estimate | $25-35M over 4 years | | Timeline | 48 months | | Cross-Disease Value | High — applicable to ALS, PD |