🧪
hypothesis

Cortical Layer 5 Pyramidal Neuron GluN2B-Mediated Hyperactivity Drives Tau Secretion Into Glymphatic Flow

Hypothesis

Cortical Layer 5 Pyramidal Neuron GluN2B-Mediated Hyperactivity Drives Tau Secretion Into Glymphatic Flow

Hyperactive GluN2B in L5 corticothalamic neurons increases extracellular glutamate, activating astrocytes and oligodendrocytes to release tau via exosome pathways.
🧬 GRIN2B (L5 pyramidal neurons); downstream: ADAM10/ADAM17🩺 neuroscience🎯 Composite 68%💱 $0.58▼13.4%proposed
EvidencePending (0%)📖 0 cit🗣 1 debates 3 support 2 oppose
✓ All Quality Gates Passed
Mechanistic 0.68 (15%) Evidence 0.70 (15%) Novelty 0.68 (12%) Feasibility 0.68 (12%) Impact 0.72 (12%) Druggability 0.65 (10%) Safety 0.70 (8%) Competition 0.65 (6%) Data Avail. 0.68 (5%) Reproducible 0.65 (5%) KG Connect 0.50 (8%) 0.679 composite
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arXiv PreprintNeurIPSNature MethodsPLOS ONE
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Composite68%

🧪 Overview

Hyperactive GluN2B in L5 corticothalamic neurons increases extracellular glutamate, activating astrocytes and oligodendrocytes to release tau via exosome pathways. Enhanced neuronal activity simultaneously increases interstitial flow, redirecting tau-seed-bearing exosomes into perivascular channels for clearance—or facilitating prion-like spreading. Links activity-dependent tau release to glymphatic routing.

🧬 Mechanism

🔗 Mechanism from KG for GRIN2B (L5 pyramidal neurons); downstream: ADAM10/ADAM17

Auto-built from this analysis's top knowledge-graph edges.

graph TD
    GluN2B["GluN2B"] -->|regulates| thalamic_burst_firing["thalamic burst firing"]
    slow_wave_oscillations["slow-wave oscillations"] -->|enhances| glymphatic_clearance["glymphatic_clearance"]
    tau_pathology["tau_pathology"] -.->|inhibits| glymphatic_clearance_effi["glymphatic clearance efficiency"]
    Trem2["Trem2"] -->|regulates| tau_phagocytosis["tau phagocytosis"]
    TREM2_deficiency["TREM2 deficiency"] -->|associated with| Tau_Clearance["Tau Clearance"]
    Cx3Cl1["Cx3Cl1"] -->|associated with| Cx3Cr1["Cx3Cr1"]
    Cx3Cr1_1["Cx3Cr1"] -->|regulates| tau_phagocytosis_2["tau phagocytosis"]
    Memantine["Memantine"] -->|enhances| CSF_tracer_clearance["CSF tracer clearance"]
    GluN2B_3["GluN2B"] -->|associated with| cortical_slow_wave_oscill["cortical slow-wave oscillations"]
    oxidative_stress["oxidative_stress"] -->|causes| AQP4_oxidation["AQP4 oxidation"]
    GLUTAMATE_EXCITOTOXICITY["GLUTAMATE EXCITOTOXICITY"] -->|enhances| Tau_Secretion["Tau Secretion"]
    sess_SRB_2026_04_28_h_var["sess_SRB-2026-04-28-h-var-e2b5a7e7db_task_9aae8fc5"] -->|causal extracted| processed["processed"]
    style GluN2B fill:#4fc3f7,stroke:#333,color:#000
    style thalamic_burst_firing fill:#4fc3f7,stroke:#333,color:#000
    style slow_wave_oscillations fill:#4fc3f7,stroke:#333,color:#000
    style glymphatic_clearance fill:#81c784,stroke:#333,color:#000
    style tau_pathology fill:#ef5350,stroke:#333,color:#000
    style glymphatic_clearance_effi fill:#4fc3f7,stroke:#333,color:#000
    style Trem2 fill:#4fc3f7,stroke:#333,color:#000
    style tau_phagocytosis fill:#4fc3f7,stroke:#333,color:#000
    style TREM2_deficiency fill:#4fc3f7,stroke:#333,color:#000
    style Tau_Clearance fill:#4fc3f7,stroke:#333,color:#000
    style Cx3Cl1 fill:#4fc3f7,stroke:#333,color:#000
    style Cx3Cr1 fill:#4fc3f7,stroke:#333,color:#000
    style Cx3Cr1_1 fill:#4fc3f7,stroke:#333,color:#000
    style tau_phagocytosis_2 fill:#4fc3f7,stroke:#333,color:#000
    style Memantine fill:#ce93d8,stroke:#333,color:#000
    style CSF_tracer_clearance fill:#ce93d8,stroke:#333,color:#000
    style GluN2B_3 fill:#4fc3f7,stroke:#333,color:#000
    style cortical_slow_wave_oscill fill:#4fc3f7,stroke:#333,color:#000
    style oxidative_stress fill:#4fc3f7,stroke:#333,color:#000
    style AQP4_oxidation fill:#4fc3f7,stroke:#333,color:#000
    style GLUTAMATE_EXCITOTOXICITY fill:#4fc3f7,stroke:#333,color:#000
    style Tau_Secretion fill:#4fc3f7,stroke:#333,color:#000
    style sess_SRB_2026_04_28_h_var fill:#4fc3f7,stroke:#333,color:#000
    style processed fill:#4fc3f7,stroke:#333,color:#000

⚖️ Evidence

⚖️ Evidence Matrix3 supports2 contradicts
Supports
Activity-dependent tau release is NMDAR-dependent
PMID:28609677
Supports
Glymphatic clearance inversely correlates with wakefulness
PMID:22641029
Supports
L5 neurons project to both thalamus and pia, positioning as integration points
PMID:N/A
Contradicts
Activity-dependent tau release studies mostly in vitro; trans-synaptic spreading uses different mechanisms
PMID:N/A
Contradicts
Glymphatic routing of exosomes not directly demonstrated
PMID:N/A
📖 Linked Papers

No linked papers recorded for this hypothesis yet.

🏥 Translation

🧬 3D Protein Structure — GRIN2B

🧬 PDB 7EU8 Click to expand

Experimental structure from RCSB PDB | Powered by Mol*

💉 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 GRIN2B (L5 pyramidal neurons); downstream: ADAM10 →

No DepMap CRISPR Chronos data found for GRIN2B (L5 pyramidal neurons); downstream: ADAM10.

Run python3 scripts/backfill_hypothesis_depmap.py to populate.

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💾 Resource Usage

No resource usage or linked notebooks recorded for this hypothesis yet.

🔮 Predictions

🔎 Predictions vs Observations2 predictions · 0 with recorded observations
PredictionPredictedObservedStatusConf
IF we genetically ablate ADAM10/ADAM17 in astrocytes using Aldh1l1-Cre;Adam10/17 flox mice crossed with rTg4510 tauopathy mice, THEN astrocyte-derived exosome tau content will decrease by ≥50% and gly≥50% decrease in astrocyte exosome tau content, ≥30% improvement in glymphatic clearance rate, with no compensatory changes in neuronal firing properties— no observation —pending0.58
IF we selectively inhibit GluN2B-containing NMDA receptors in L5 corticothalamic pyramidal neurons using ifenprodil (10 mg/kg, i.p., 2 weeks) in 6-month-old 5xFAD mice, THEN extracellular tau concentr≥40% reduction in extracellular tau concentration and ≥40% reduction in tau seeding activity in perivascular fluid within 2 weeks of continuous GluN2B inhibitio— no observation —pending0.65
🔮 Falsifiable Predictions (2)
pendingconf 65%
IF we selectively inhibit GluN2B-containing NMDA receptors in L5 corticothalamic pyramidal neurons using ifenprodil (10 mg/kg, i.p., 2 weeks) in 6-month-old 5xFAD mice, THEN extracellular tau concentration in interstitial fluid (measured via microdialysis) will decrease by ≥40% and perivascular tau
Predicted outcome: ≥40% reduction in extracellular tau concentration and ≥40% reduction in tau seeding activity in perivascular fluid within 2 weeks of continuous GluN2B
Falsification: No significant change (<20%) in interstitial or perivascular tau levels, or paradoxically increased tau after GluN2B inhibition, indicating GluN2B is not the primary driver
pendingconf 58%
IF we genetically ablate ADAM10/ADAM17 in astrocytes using Aldh1l1-Cre;Adam10/17 flox mice crossed with rTg4510 tauopathy mice, THEN astrocyte-derived exosome tau content will decrease by ≥50% and glymphatic clearance efficiency (MRI Gd-DTPA perivascular flux) will increase by ≥30%, while neuronal a
Predicted outcome: ≥50% decrease in astrocyte exosome tau content, ≥30% improvement in glymphatic clearance rate, with no compensatory changes in neuronal firing propert
Falsification: No change in astrocyte exosome tau despite ADAM10/17 deletion, indicating these proteases are not required for activity-dependent tau release; or impaired rather than enhanced glymphatic clearance
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