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Gap Junction Dysfunction Validation in Parkinson's Disease
Experiment Overview
Hypothesis: [Connexin](/proteins/gja1-protein) and [pannexin](/proteins/panx1-protein) channel dysfunction drives [dopaminergic neurodegeneration](/diseases/parkinsons-disease) through impaired cellular communication, [calcium dysregulation](/mechanisms/calcium-dysregulation-alzheimers), and [neuroinflammation](/mechanisms/neuroinflammation).
Primary Objective: Validate that connexin hemichannel dysfunction is a disease-modifying mechanism in PD.
Study Design
Phase 1: In Vitro Validation (6 months)
...
Experiment Overview
Hypothesis: [Connexin](/proteins/gja1-protein) and [pannexin](/proteins/panx1-protein) channel dysfunction drives [dopaminergic neurodegeneration](/diseases/parkinsons-disease) through impaired cellular communication, [calcium dysregulation](/mechanisms/calcium-dysregulation-alzheimers), and [neuroinflammation](/mechanisms/neuroinflammation).
Primary Objective: Validate that connexin hemichannel dysfunction is a disease-modifying mechanism in PD.
Study Design
Phase 1: In Vitro Validation (6 months)
1.1 Human iPSC-Derived Dopaminergic Neurons
Model: iPSC-derived dopaminergic neurons from:
- Healthy controls (n=3 lines)
- PD patients with SNCA triplication (n=2 lines)
- PD patients with LRRK2 G2019S (n=2 lines)
- Cx36 gap junction coupling ( dye transfer assay)
- Cell viability (MTS assay) under basal and stress conditions
- Calcium dynamics (Fluo-4 AM imaging)
- α-Synuclein aggregation (pSer129 immunostaining)
- Vehicle control
- α-Synuclein pre-formed fibrils (10 μg/mL, 24h)
- Carbenoxolone (100 μM, Cx hemichannel blocker)
- Gap26 (100 μM, Cx43 specific blocker)
1.2 Astrocyte-Neuron Co-Culture
Model: Primary rat astrocytes + human iPSC neurons in transwell system
Endpoints:
- Cx43 expression and localization (confocal microscopy)
- Lactate transport (Seahorse metabolic assay)
- K+ buffering capacity (ion-selective microelectrodes)
- Neuronal survival under metabolic stress
Phase 2: Animal Model Validation (12 months)
2.1 MPTP Mouse Model
Design: C57BL/6 mice, 8 weeks old, n=12/group
| Group | Treatment | Dose | Duration |
|-------|-----------|------|----------|
| 1 | Vehicle | - | 4 weeks |
| 2 | MPTP | 30 mg/kg | 4 weeks |
| 3 | MPTP + Carbenoxolone | 50 mg/kg | 4 weeks |
| 4 | MPTP + Gap26 | 3 mg/kg | 4 weeks |
| 5 | Probenecid | 50 mg/kg | 4 weeks |
Endpoints:
- Behavioral: Rotarod, cylinder test, gait analysis
- Histological: TH+ neuron count in SNc, striatal dopamine
- Molecular: Cx43, PANX1 expression (Western blot)
- Inflammation: Iba1+ microglial density, IL-1β levels
2.2 α-Synuclein Preformed Fibril Model
Design: C57BL/6 mice, unilateral striatal PFF injection, n=10/group
Endpoints:
- pSer129 α-synuclein pathology (15, 30, 60 days)
- Cx43 hemichannel activity (ethidium bromide uptake)
- Optogenetic assessment of circuit function
Phase 3: Clinical Biomarker Study (18 months)
3.1 CSF Biomarker Cohort
Cohort:
- Early PD (n=50, H&Y 1-2)
- Advanced PD (n=50, H&Y 3-4)
- Healthy controls (n=30)
- Extracellular ATP (luminex assay)
- IL-1β, IL-18 (ELISA)
- Neurofilament light chain (NfL)
- α-Synuclein seeding (RT-QuIC)
- UPDRS motor scores
- Disease duration
- MoCA cognitive scores
Statistical Analysis
Power Calculation
For Phase 2 (animal study):
- α = 0.05, power = 0.80
- Expected effect size (Cohen's d) = 1.2
- n = 10 per group provides adequate power
Primary Endpoints
| Endpoint | Analysis |
|----------|----------|
| TH+ neuron count | One-way ANOVA + Tukey post-hoc |
| Behavioral scores | Repeated measures ANOVA |
| Biomarker levels | Linear mixed effects model |
| Correlation analysis | Pearson/Spearman as appropriate |
Risks and Mitigations
| Risk | Mitigation |
|------|------------|
| Limited BBB penetration of blockers | Use multiple compounds with different properties |
| Species differences | Validate in human iPSC models |
| Off-target effects | Use isoform-selective compounds where available |
| Biomarker variability | Standardized collection protocols, multi-analyte panels |
Expected Outcomes
Budget Estimate
| Phase | Duration | Estimated Cost |
|-------|----------|----------------|
| Phase 1 (in vitro) | 6 months | $150,000 |
| Phase 2 (animal) | 12 months | $400,000 |
| Phase 3 (clinical) | 18 months | $350,000 |
| Total | 36 months | $900,000 |
Timeline
Month: 1---6---12---18---24---30---36
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P1: [=====]
References
▸Metadataorigin_type: v1_polymorphic_backfill
| slug | experiments-gap-junction-dysfunction-parkinsons |
| kg_node_id | None |
| entity_type | experiment |
| origin_type | v1_polymorphic_backfill |
| source_table | wiki_pages |
| wiki_page_id | wp-1e9293bbfef4 |
| __merged_from | {'merged_at': '2026-05-13', 'unprefixed_id': 'experiments-gap-junction-dysfunction-parkinsons'} |
| _schema_version | 1 |
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