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ID: h-gap-456a357b-m1
Hypothesis

age-linked CpG drift is the actionable driver in: Are DNA methylation changes in neurodegeneration causal drivers or protective consequences

The gap can be tested by treating age-linked CpG drift as an upstream driver rather than a passive correlate.
🧬 age-linked CpG drift🩺 neurodegeneration🎯 Composite 34%💱 $0.59▲5.5%active
EvidencePending (0%)📖 6 cit🗣 2 debates 6 support 1 oppose
✓ All Quality Gates Passed
🏆 ChallengeValidate epigenetic drift causality in neurodegeneration DNA methylation$500 →
☰ Compare⚔️ Duel⚛️ Collide
📄 Export LaTeX
📖 Export BibTeXinteract with this hypothesis
Composite34%

🧪 Overview

The gap can be tested by treating age-linked CpG drift as an upstream driver rather than a passive correlate. If true, perturbing locus-specific epigenome editing should shift cell-sorted methylomes before downstream neurodegeneration markers change.

🧬 Mechanism

🧬 Curated Mechanism Pathway

Curated pathway from expert analysis

flowchart TD
    A["Age-Linked CpG Drift<br/>Progressive Hypomethylation"]
    B["DNMT1 Maintenance Failure<br/>Replication-Linked Fidelity Loss"]
    C["Transposon Derepression<br/>LINE-1 and IAP Silencing Loss"]
    D["cGAS-STING Innate Sensing<br/>Cytosolic DNA Detection"]
    E["Heterochromatin Erosion<br/>H3K9me3 and H3K27me3 Loss"]
    F["SASP Cytokine Secretion<br/>Senescence-Associated Phenotype"]
    G["Glial Identity Drift<br/>Microglia and Astrocyte Dysregulation"]
    A --> B
    A --> C
    B --> E
    C --> D
    D --> F
    E --> G
    F --> G
    style A fill:#1a237e,stroke:#4fc3f7,color:#4fc3f7
    style D fill:#7b1fa2,stroke:#ce93d8,color:#ce93d8
    style F fill:#b71c1c,stroke:#ef9a9a,color:#ef9a9a
    style G fill:#b71c1c,stroke:#ef9a9a,color:#ef9a9a

⚖️ Evidence

⚖️ Evidence Matrix5 supports1 contradicts
Supports
TDP-43 Triggers Mitochondrial DNA Release via mPTP to Activate cGAS/STING in ALS.
Cell2020PMID:33031745medium
Supports
DNA Damage, Neurodegeneration, and Synaptic Plasticity.
Neural Plast2016PMID:27313899medium
Supports
Human endogenous retrovirus-K contributes to motor neuron disease.
Sci Transl Med2015PMID:26424568medium
Supports
Premature polyadenylation-mediated loss of stathmin-2 is a hallmark of TDP-43-dependent neurodegeneration.
Nat Neurosci2019PMID:30643298medium
Supports
WDR45 contributes to neurodegeneration through regulation of ER homeostasis and neuronal death.
Autophagy2020PMID:31204559medium
Contradicts
causal direction requires longitudinal perturbation
skeptic_round
📖 Linked Papers (17)Export BibTeX ↗
Figures
Figures
Figures available at source paper (no open-access XML found).
Figure 1
Figure 1
No caption available
Figure S1
Figure S1
Elevated NF-κB and Type I IFN Signaling Because of TDP-43 In Vitro , Related to Figure 1 (A) Doxycycline (Dox inducible wild-type (WT) or ALS mutant (Q331K) T...
No figures

🏥 Translation

🧬 3D Protein Structure — AGE-LINKED

No curated PDB or AlphaFold mapping for AGE-LINKED 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 age-linked CpG drift →

No DepMap CRISPR Chronos data found for age-linked CpG drift.

Run python3 scripts/backfill_hypothesis_depmap.py to populate.

🏆 Tournament

🏆 Arenas / Elo

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📊 Market Indicators

7d Trend
Stable
7d Momentum
▲ 0.0%
Volatility
High
0.2167
Events (7d)
1
Price History
▲5.5%

💾 Resource Usage

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

🔮 Predictions

🔎 Predictions vs Observations2 predictions · 0 with recorded observations
PredictionPredictedObservedStatusConf
IF CpG drift is upstream, THEN baseline drift burden in aging brain organoids will predict subsequent neuronal-loss markers at r >=0.30 over 60 days.CpG drift burden predicts later cleaved-caspase or synapse-loss module with r >=0.30.— no observation —pending0.51
IF age-linked CpG drift is causal in neurodegeneration, THEN epigenome editing of top drift CpGs in human neurons will shift stress-response and synaptic gene expression by >=20% within 14 days.Targeted CpG editing produces >=20% expression change in preregistered stress/synaptic modules versus scrambled guide controls.— no observation —pending0.55
🔮 Falsifiable Predictions (2)
pendingconf 55%
IF age-linked CpG drift is causal in neurodegeneration, THEN epigenome editing of top drift CpGs in human neurons will shift stress-response and synaptic gene expression by >=20% within 14 days.
Predicted outcome: Targeted CpG editing produces >=20% expression change in preregistered stress/synaptic modules versus scrambled guide controls.
Falsification: Expression module change is <5% despite >=25% methylation editing at target CpGs.
pendingconf 51%
IF CpG drift is upstream, THEN baseline drift burden in aging brain organoids will predict subsequent neuronal-loss markers at r >=0.30 over 60 days.
Predicted outcome: CpG drift burden predicts later cleaved-caspase or synapse-loss module with r >=0.30.
Falsification: Predictive correlation is |r| <0.10 or appears only after neuronal-loss markers are already elevated.
Metadatasource: v1_phase_c_backfill · origin_type: debate_synthesis
sourcev1_phase_c_backfill
origin_typedebate_synthesis
_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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