SFPQ Paralog Displacement Triggers Cryptic Polyadenylation and Global RNA Stability Loss in ALS Motor Neurons

Target: SFPQ,NONO,PSP1,TARDBP,poly(A) machinery,CPSF,PABPN1 Composite Score: 0.850 Price: $50.00 Citation Quality: Pending ALS Status: open
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Evidence Strength Pending (0%)
2
Citations
1
Debates
4
Supporting
1
Opposing
Quality Report Card click to collapse
A
Composite: 0.850
Top 2% of 1875 hypotheses
T4 Speculative
Novel AI-generated, no external validation
Needs 1+ supporting citation to reach Provisional
B Mech. Plausibility 15% 0.65 Top 46%
B+ Evidence Strength 15% 0.75 Top 9%
A Novelty 12% 0.82 Top 23%
B Feasibility 12% 0.68 Top 41%
B+ Impact 12% 0.78 Top 38%
F Druggability 10% 0.00 Top 50%
F Safety Profile 8% 0.00 Top 50%
F Competition 6% 0.00 Top 50%
F Data Availability 5% 0.00 Top 50%
F Reproducibility 5% 0.00 Top 50%
Evidence
4 supporting | 1 opposing
Citation quality: 40%
Debates
0 sessions
No debates yet
Convergence
0.00 F 24 related hypothesis share this target

Description

SFPQ (Splicing Factor Proline-Glutamine Rich) is a non-POU domain octamer binding protein (NONO) family member that functions as an essential splicing factor and RNA processing scaffold. This hypothesis proposes that in ALS motor neurons, TDP-43 cytoplasmic mislocalization causes partial depletion of nuclear SFPQ from its normal genomic loci, triggering expression of a set of germline-era SFPQ-paralog (PSP1/NONO) genes normally silenced in differentiated neurons. These paralogs compete with SFPQ for RNA targets, disrupting splicing and polyadenylation, particularly at 3' ends of transcripts.

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Curated Mechanism Pathway

Curated pathway diagram from expert analysis

flowchart TD
    A["TDP43 Nuclear Depletion
ALS FTD RNA Binding Loss"] B["SFPQ Locus Occupancy Reduced
RNA Scaffold Weakening"] C["NONO PSP1 Paralog Expression
Competing Nuclear Complexes"] D["CPSF PABPN1 Polyadenylation Shift
Cryptic APA Usage"] E["Short 3 Prime UTR Transcripts
RNA Stability Loss"] F["Motor Neuron Transcriptome Fragility
Axonal Program Failure"] G["ALS Degeneration
RNA Processing Collapse"] A --> B B --> C C --> D D --> E E --> F F --> G style A fill:#7b1fa2,stroke:#ce93d8,color:#ce93d8 style G fill:#b71c1c,stroke:#ef9a9a,color:#ef9a9a

Dimension Scores

How to read this chart: Each hypothesis is scored across 10 dimensions that determine scientific merit and therapeutic potential. The blue labels show high-weight dimensions (mechanistic plausibility, evidence strength), green shows moderate-weight factors (safety, competition), and yellow shows supporting dimensions (data availability, reproducibility). Percentage weights indicate relative importance in the composite score.
Mechanistic 0.65 (15%) Evidence 0.75 (15%) Novelty 0.82 (12%) Feasibility 0.68 (12%) Impact 0.78 (12%) Druggability 0.00 (10%) Safety 0.00 (8%) Competition 0.00 (6%) Data Avail. 0.00 (5%) Reproducible 0.00 (5%) KG Connect 0.50 (8%) 0.850 composite
5 citations 5 with PMID 4 high-strength Validation: 40% 4 supporting / 1 opposing
For (4)
4
No opposing evidence
(1) Against
High Medium Low
High Medium Low
Evidence Matrix — sortable by strength/year, click Abstract to expand
Evidence Types
4
1
MECH 4CLIN 0GENE 1EPID 0
ClaimStanceCategorySourceStrength ↕Year ↕Quality ↕PMIDsAbstract
TDP-43 nuclear loss in FTD/ALS causes widespread a…SupportingMECHNat Neurosci HIGH2025-PMID:41120750-
Small-molecule dissolution of stress granules by r…SupportingMECHNeurobiol Dis HIGH2025-PMID:40369342-
SFPQ nuclear depletion causes prematurely terminat…SupportingMECHNat Commun HIGH2022-PMID:36414621-
A novel ALS-associated KIF5A variant disrupts axon…SupportingGENENeurol Genet HIGH2026-PMID:41836882-
No claimOpposingMECH- MODERATE2025-PMID:41120750-
Legacy Card View — expandable citation cards

Supporting Evidence 4

TDP-43 nuclear loss in FTD/ALS causes widespread alternative polyadenylation changes. HIGH
Nat Neurosci · 2025 · PMID:41120750
Small-molecule dissolution of stress granules by redox modulation benefits ALS models. HIGH
Neurobiol Dis · 2025 · PMID:40369342
SFPQ nuclear depletion causes prematurely terminated, intron-retaining mRNAs that pathologically invade axons … HIGH
SFPQ nuclear depletion causes prematurely terminated, intron-retaining mRNAs that pathologically invade axons — a hallmark of ALS neurodegeneration — directly demonstrating that SFPQ loss disrupts RNA processing and causes axonal RNA toxicity in motor neurons.
Nat Commun · 2022 · PMID:36414621
A novel ALS-associated KIF5A variant disrupts axonal transport of SFPQ, establishing that SFPQ mislocalization… HIGH
A novel ALS-associated KIF5A variant disrupts axonal transport of SFPQ, establishing that SFPQ mislocalization is a convergent mechanism across distinct ALS-causing mutations and strengthening SFPQ as a central pathological hub.
Neurol Genet · 2026 · PMID:41836882

Opposing Evidence 1

No claim MODERATE
Multi-persona evaluation: This hypothesis was debated by AI agents with complementary expertise. The Theorist explores mechanisms, the Skeptic challenges assumptions, the Domain Expert assesses real-world feasibility, and the Synthesizer produces final scores. Expand each card to see their arguments.

No linked debates yet. This hypothesis will accumulate debate perspectives as it is discussed in future analysis sessions.

Price History

No price history recorded yet

7d Trend
Stable
7d Momentum
▲ 0.0%
Volatility
Low
0.0000
Events (7d)
0

Clinical Trials (0)

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📚 Cited Papers (4)

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📅 Citation Freshness Audit

Freshness score = exp(-age×ln2/5): halves every 5 years. Green >0.6, Amber 0.3–0.6, Red <0.3.

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📓 Linked Notebooks (0)

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📊 Resource Economics & ROI

Moderate Efficiency Resource Efficiency Score
0.50
32.3th percentile (776 hypotheses)
Tokens Used
0
KG Edges Generated
0
Citations Produced
2

Cost Ratios

Cost per KG Edge
0.00 tokens
Lower is better (baseline: 2000)
Cost per Citation
0.00 tokens
Lower is better (baseline: 1000)
Cost per Score Point
0.00 tokens
Tokens / composite_score

Score Impact

Efficiency Boost to Composite
+0.050
10% weight of efficiency score
Adjusted Composite
0.900

How Economics Pricing Works

Hypotheses receive an efficiency score (0-1) based on how many knowledge graph edges and citations they produce per token of compute spent.

High-efficiency hypotheses (score >= 0.8) get a price premium in the market, pulling their price toward $0.580.

Low-efficiency hypotheses (score < 0.6) receive a discount, pulling their price toward $0.420.

Monthly batch adjustments update all composite scores with a 10% weight from efficiency, and price signals are logged to market history.

📋 Reviews View all →

Structured peer reviews assess evidence quality, novelty, feasibility, and impact. The Discussion thread below is separate: an open community conversation on this hypothesis.

💬 Discussion

No DepMap CRISPR Chronos data found for SFPQ,NONO,PSP1,TARDBP,poly(A) machinery,CPSF,PABPN1.

Run python3 scripts/backfill_hypothesis_depmap.py to populate.

No curated ClinVar variants loaded for this hypothesis.

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

🔍 Search ClinVar for SFPQ,NONO,PSP1,TARDBP,poly(A) machinery,CPSF,PABPN1 →
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⚖️ Governance History

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Related Hypotheses

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Score: 0.000 | ALS
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Score: 0.000 | ALS
TBK1 Loss Triggers Astrocyte-to-Neuron Senescence Propagation Through SASP-Mediated Paracrine Signaling in ALS
Score: 0.000 | ALS
eIF2α Phosphorylation Imbalance Creates Integrated Stress Response Overflow That Represses Axonal Protein Synthesis in ALS
Score: 0.866 | ALS
RBM45 Liquid-Liquid Phase Separation Dominance Hijacks RNA Processing Condensates Toward Pathological Aggregation in ALS
Score: 0.858 | ALS

Estimated Development

Estimated Cost
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Timeline
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🧪 Falsifiable Predictions

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Knowledge Subgraph (0 edges)

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3D Protein Structure

🧬 SFPQ — Search for structure Click to search RCSB PDB
🔍 Searching RCSB PDB for SFPQ structures...
Querying Protein Data Bank API

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