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ID: h-0455aa58e4
Hypothesis

Rare TREM2-TYROBP pathway variants complement standard PRS by identifying microglial-mediated LOAD risk

We hypothesize that rare loss-of-function variants in microglial-expressed genes within the TREM2-TYROBP signaling cascade (PLCG2, TREM2, INPP5D, APOC2) capture a distinct late-onset Alzheimer's disease etiological subtype characterized .
🧬 PLCG2🩺 late-onset-alzheimers🎯 Composite 38%💱 $0.53▲9.6%proposed
neurodegeneration
EvidencePending (0%)📖 5 cit🗣 1 debates 5 support 2 oppose
✓ All Quality Gates Passed
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Composite38%

🧪 Overview

We hypothesize that rare loss-of-function variants in microglial-expressed genes within the TREM2-TYROBP signaling cascade (PLCG2, TREM2, INPP5D, APOC2) capture a distinct late-onset Alzheimer's disease etiological subtype characterized by dysregulated microglial lipid sensing and enhanced synaptic pruning that is not captured by standard AD polygenic risk scores. This rare variant burden identifies individuals with enhanced microglial-driven neurodegeneration who fall below PRS risk thresholds, representing a 'microglial subtype' that may respond differently to immunomodulatory therapies. Testable prediction: combining rare variant burden scores from microglial regulatory genes with standard AD PRS will improve area under the ROC curve by >0.05 in independent cohorts and reclassify ~15-20% of cases currently missed by PRS alone.

🧬 Mechanism

🧬 Curated Mechanism Pathway

Curated pathway from expert analysis

flowchart TD
    A["PLCG2 Variant<br/>Gain of Function"]
    B["TREM2-TYROBP<br/>Signaling Cascade"]
    C["PLCgamma2<br/>Phospholipase Activation"]
    D["Microglial<br/>Calcium Signaling"]
    E["Phagocytic Activity<br/>Enhanced"]
    F["PLCG2 as Modifier of<br/>TREM2 Pathogenesis"]
    A --> B
    B --> C
    C --> D
    D --> E
    E --> F
    style A fill:#1a237e,stroke:#4fc3f7,color:#4fc3f7
    style F fill:#1b5e20,stroke:#a5d6a7,color:#a5d6a7

⚖️ Evidence

⚖️ Evidence Matrix5 supports2 contradicts
Supports
Human and mouse single-nucleus transcriptomics reveal TREM2-dependent and TREM2-independent cellular responses in Alzheimer's disease.
Nat Med2020PMID:31932797medium
Supports
TREM2, microglia, and Alzheimer's disease.
Mech Ageing Dev2021PMID:33516818medium
Supports
Anti-human TREM2 induces microglia proliferation and reduces pathology in an Alzheimer's disease model.
J Exp Med2020PMID:32579671medium
Supports
A Unique Microglia Type Associated with Restricting Development of Alzheimer's Disease.
Cell2017PMID:28602351medium
Supports
TREM2 dependent and independent functions of microglia in Alzheimer's disease.
Mol Neurodegener2022PMID:36564824medium
Contradicts
PLCG2 is expressed and functionally relevant in neurons and astrocytes in addition to microglia; non-microglial PLCG2 downregulation impairs synaptic function independently, complicating the assignment of TREM2-TYROBP pathway rare variants to a purely microglial mechanism
Contradicts
The protective PLCG2 P522R variant has a moderate effect size (HR ~0.68) and the incremental improvement in LOAD prediction from rare TREM2-TYROBP pathway variants over standard APOE+common-variant PRS is modest; large sequencing studies show these rare variants explain <1% of additional LOAD variance
📖 Linked Papers

No linked papers recorded for this hypothesis yet.

🏥 Translation

🧬 3D Protein Structure — PLCG2

No curated PDB or AlphaFold mapping for PLCG2 yet. Search RCSB →

💉 Clinical Trials

No clinical trials data linked to this hypothesis yet.

No curated ClinVar variants loaded for this hypothesis.

Run scripts/backfill_clinvar_variants.py to fetch P/LP/VUS variants.

🔍 Search ClinVar for PLCG2 →

No DepMap CRISPR Chronos data found for PLCG2.

Run python3 scripts/backfill_hypothesis_depmap.py to populate.

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📊 Market Indicators

7d Trend
Stable
7d Momentum
▲ 0.0%
Volatility
High
0.3519
Events (7d)
0
Price History
▲9.6%

💾 Resource Usage

LLM Tokens
48,732
$0.1462
Total Cost
$0.1462

🔮 Predictions

🔎 Predictions vs Observations2 predictions · 0 with recorded observations
PredictionPredictedObservedStatusConf
IF individuals are stratified by rare loss-of-function variant burden (MAF <1%) in PLCG2, TREM2, INPP5D, and APOC2 THEN combining a rare variant burden score with standard AD polygenic risk scores wilAUC improvement >0.05 when rare variant burden is added to standard PRS; reclassification of 15-20% of LOAD cases currently classified as low-risk by PRS alone— no observation —pending0.72
IF human iPSC-derived microglia or mouse models carrying rare PLCG2/TREM2/INPP5D loss-of-function variants are exposed to amyloid-beta oligomers THEN these cells will demonstrate enhanced synaptic pru≥30% increase in complement-mediated synaptic engulfment (C1q/C3d colocalization with synaptic markers) in microglia harboring rare loss-of-function variants fo— no observation —pending0.65
🔮 Falsifiable Predictions (2)
pendingconf 72%
IF individuals are stratified by rare loss-of-function variant burden (MAF <1%) in PLCG2, TREM2, INPP5D, and APOC2 THEN combining a rare variant burden score with standard AD polygenic risk scores will improve area under the ROC curve by >0.05 in independent late-onset Alzheimer's disease cohorts co
Predicted outcome: AUC improvement >0.05 when rare variant burden is added to standard PRS; reclassification of 15-20% of LOAD cases currently classified as low-risk by
Falsification: AUC improvement ≤0.03 in independent cohorts OR reclassification rate <10% when rare variant burden is added to PRS, indicating rare variants in this pathway do not capture distinct LOAD risk beyond s
pendingconf 65%
IF human iPSC-derived microglia or mouse models carrying rare PLCG2/TREM2/INPP5D loss-of-function variants are exposed to amyloid-beta oligomers THEN these cells will demonstrate enhanced synaptic pruning activity (measured by complement co-localization or PSD95/C3 ratio reduction) compared to isoge
Predicted outcome: ≥30% increase in complement-mediated synaptic engulfment (C1q/C3d colocalization with synaptic markers) in microglia harboring rare loss-of-function v
Falsification: No significant difference in synaptic pruning markers between variant-carrying and wild-type microglia (<10% change), indicating the proposed microglial dysfunction mechanism is not supported
Metadatasource: v1_phase_c_backfill · origin_type: audit_hypothesis_generator
sourcev1_phase_c_backfill
origin_typeaudit_hypothesis_generator
_schema_version1
📊 Evidence Profile
Evidence Balance
+0%
Certainty
0%
Debates
0
Incoming
0
Outgoing
0
0 supporting 0 contradicting 0 neutral
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