🧪
hypothesis

P2X7R PET Imaging for NLRP3 Inflammasome-Associated Priming

Hypothesis

P2X7R PET Imaging for NLRP3 Inflammasome-Associated Priming

P2X7R PET Imaging for NLRP3 Inflammasome-Associated Priming starts from the claim that modulating P2RX7/NLRP3 within the disease context of biomarkers can redirect a disease-relevant process.
🧬 P2RX7/NLRP3🩺 biomarkers🎯 Composite 56%💱 $0.54▼4.1%proposed
🔬 Microglial Biology🧠 Neurodegeneration🔥 Neuroinflammation
EvidencePending (0%)📖 0 cit🗣 1 debates 3 support 3 oppose
✓ All Quality Gates Passed
Mechanistic 0.52 (15%) Evidence 0.45 (15%) Novelty 0.68 (12%) Feasibility 0.35 (12%) Impact 0.78 (12%) Druggability 0.82 (10%) Safety 0.55 (8%) Competition 0.72 (6%) Data Avail. 0.38 (5%) Reproducible 0.40 (5%) KG Connect 0.50 (8%) 0.563 composite
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Composite56%

🧪 Overview

Mechanistic Overview


P2X7R PET Imaging for NLRP3 Inflammasome-Associated Priming starts from the claim that modulating P2RX7/NLRP3 within the disease context of biomarkers can redirect a disease-relevant process. The original description reads: "## Mechanistic Overview P2X7R PET Imaging for NLRP3 Inflammasome-Associated Priming starts from the claim that modulating P2RX7/NLRP3 within the disease context of biomarkers can redirect a disease-relevant process. The original description reads: "## Mechanistic Overview P2X7R PET Imaging for NLRP3 Inflammasome-Associated Priming starts from the claim that P2X7 receptor PET identifies NLRP3 inflammasome-engaged primed microglia by targeting the 'licensing' step required for full microglial activation. First-in-human tracer demonstrated brain penetration but is not yet qualified for clinical biomarker use. Fundamental limitations include non-microglial P2X7R expression and uncertain mechanistic specificity. Framed more explicitly, the hypothesis centers P2RX7/NLRP3 within the broader disease setting of biomarkers. The row currently records status `proposed`, origin `debate_synthesizer`, and mechanism category `unspecified`.

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🧬 Mechanism

🧬 Curated Mechanism Pathway

Curated pathway from expert analysis

flowchart TD
    A["Amyloid-beta/Tau<br/>Priming Signal"]
    B["Lysosomal Damage<br/>Cathepsin B Release"]
    C["NLRP3 Sensor<br/>NEK7 Binding"]
    D["ASC Speck Formation<br/>PYD Domain Oligomerization"]
    E["Pro-Caspase-1<br/>CARD Domain Recruitment"]
    F["Active Caspase-1<br/>Cleavage Activation"]
    G["IL-1B/IL-18 Secretion<br/>Pro-inflammatory"]
    H["Pyroptosis<br/>Gasdermin D Pore"]
    I["Feed-Forward Loop<br/>Sustained SASP Inflammasome"]
    A --> C
    B --> C
    C --> D
    D --> E
    E --> F
    F --> G
    F --> H
    G --> I
    I -.->|"amplifies"| C
    style A fill:#b71c1c,stroke:#ef9a9a,color:#ef9a9a
    style H fill:#b71c1c,stroke:#ef9a9a,color:#ef9a9a
    style I fill:#b71c1c,stroke:#ef9a9a,color:#ef9a9a

⚖️ Evidence

⚖️ Evidence Matrix3 supports3 contradicts
Supports
P2X7R deletion or blockade prevents microglial priming in mouse models
PMID:28465143
Supports
P2X7R expression correlates with disease severity in MS and ALS
PMID:30181108
Supports
First-in-human P2X7R PET tracer demonstrated brain penetration
PMID:31771992
Contradicts
Tracer brain penetration is necessary but insufficient; specific-to-nonspecific binding ratio not established
Contradicts
P2X7R expressed on neurons, astrocytes, oligodendrocytes, and peripheral cells; microglial attribution fails without validation
Contradicts
P2X7R-NLRP3-priming axis may be context-specific; not universally accepted
📖 Linked Papers

No linked papers recorded for this hypothesis yet.

🏥 Translation

🧬 3D Protein Structure — P2RX7

🧬 PDB 5U1L Click to expand

Experimental structure from RCSB PDB | Powered by Mol*

🧠 GTEx v10 Brain ExpressionJSON

Median TPM across 13 brain regions for P2RX7/NLRP3 from GTEx v10.

Spinal cord cervical c-119.6 Cerebellum10.7 Substantia nigra10.4 Cortex10.0 Hippocampus9.2 Cerebellar Hemisphere8.9 Frontal Cortex BA97.7 Amygdala6.2 Caudate basal ganglia5.8 Putamen basal ganglia5.4 Hypothalamus5.3 Anterior cingulate cortex BA244.8 Nucleus accumbens basal ganglia3.8median TPM (GTEx v10)

💉 Clinical Trials (1)

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Total Enrolled
Untitled TrialUnknown
Unknown·

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No DepMap CRISPR Chronos data found for P2RX7.

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💰 Estimated Development
Cost
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📊 Market Indicators

7d Trend
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🔮 Predictions

🔎 Predictions vs Observations2 predictions · 0 with recorded observations
PredictionPredictedObservedStatusConf
IF P2X7R PET imaging is performed in a cohort of individuals with early Alzheimer's disease and age-matched controls, THEN the standardized uptake value ratio (SUVR) in regions of known microglial accMean SUVR difference ≥ 0.25 between AD (n ≥ 40) and cognitively normal controls (n ≥ 40) in a priori defined regions of interest, with effect size Cohen's d ≥ 0— no observation —pending0.42
IF human induced pluripotent stem cell (iPSC)-derived microglia-like cells with NLRP3 inflammasome priming (48-hour pre-treatment with LPS 10 ng/mL) are imaged with [11C]P2X7R PET ligand in vitro, THERadioligand binding affinity (Bmax) ≥ 2.0-fold higher in LPS-primed microglia-like cells compared to vehicle-treated controls, with concurrent measurement of AS— no observation —pending0.38
🔮 Falsifiable Predictions (2)
pendingconf 42%
IF P2X7R PET imaging is performed in a cohort of individuals with early Alzheimer's disease and age-matched controls, THEN the standardized uptake value ratio (SUVR) in regions of known microglial accumulation (inferior temporal gyrus, entorhinal cortex) will be significantly elevated in AD patients
Predicted outcome: Mean SUVR difference ≥ 0.25 between AD (n ≥ 40) and cognitively normal controls (n ≥ 40) in a priori defined regions of interest, with effect size Coh
Falsification: No statistically significant SUVR difference (p > 0.05) between diagnostic groups, or SUVR elevations correlating equally strongly with peripheral blood monocyte P2X7R expression, indicating non-micro
pendingconf 38%
IF human induced pluripotent stem cell (iPSC)-derived microglia-like cells with NLRP3 inflammasome priming (48-hour pre-treatment with LPS 10 ng/mL) are imaged with [11C]P2X7R PET ligand in vitro, THEN radioligand binding will show ≥ 2.0-fold increase in primed versus non-primed cells within 6 month
Predicted outcome: Radioligand binding affinity (Bmax) ≥ 2.0-fold higher in LPS-primed microglia-like cells compared to vehicle-treated controls, with concurrent measure
Falsification: Primed cells showing ≥ 3-fold increase in NLRP3 mRNA/protein and caspase-1 activation fail to demonstrate > 1.2-fold increase in P2X7R radioligand binding, indicating insufficient mechanistic specific

📖 References (3)

  1. Genetic population data of three Y-STR genetic systems in Mexican-Mestizos from Monterrey, Nuevo León (Northeast, Mexico).
    ["Ramos-Gonz\u00e1lez et al.. Forensic science international. Genetics (2017)
    PubMed↗DOI↗
  2. Designing Emails Aimed at Increasing Family Physicians' Use of a Web-Based Audit and Feedback Tool to Improve Cancer Screening Rates: Cocreation Process.
    ["Bravo et al.. JMIR human factors (2018)
    PubMed↗DOI↗
  3. Impaired neural differentiation and glymphatic CSF flow in the Ccdc39 rat model of neonatal hydrocephalus: genetic interaction with L1cam.
    ["Emmert et al.. Disease models & mechanisms (2019)
    PubMed↗DOI↗
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