Epigenetic SPI1 Reprogramming Therapy

Target: SPI1 Composite Score: 0.455 Price: $0.52▲5.8% Citation Quality: Pending neuroinflammation Status: active

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Evidence Strength Pending (0%)

Citations

Debates

Supporting

Opposing

Quality Report Card click to collapse

Composite: 0.455

Top 72% of 1800 hypotheses

T4 Speculative

Novel AI-generated, no external validation

Needs 1+ supporting citation to reach Provisional

C+ Mech. Plausibility 15% 0.50 Top 75%

C+ Evidence Strength 15% 0.50 Top 56%

C+ Novelty 12% 0.50 Top 82%

C+ Feasibility 12% 0.50 Top 64%

F Impact 12% 0.00 Top 50%

C+ Druggability 10% 0.50 Top 59%

C+ Safety Profile 8% 0.50 Top 56%

C+ Competition 6% 0.50 Top 76%

C+ Data Availability 5% 0.50 Top 69%

C+ Reproducibility 5% 0.50 Top 62%

Evidence

5 supporting | 0 opposing

Citation quality: 0%

Debates

1 session A+

Avg quality: 0.93

Convergence

0.00 F 5 related hypothesis share this target

From Analysis:

How does SPI1 transcriptionally regulate C1QA and C1QC expression in atherosclerotic contexts?

The authors identify SPI1 as a potential transcription factor regulating the hub genes but provide no mechanistic details of this regulatory relationship. Given SPI1's role in microglial activation and neuroinflammation, this regulatory circuit may be relevant to cerebrovascular disease and neurodegeneration. Gap type: unexplained_observation Source paper: An integrative analysis of single-cell and bulk transcriptome and bidirectional mendelian randomization analysis identified C1Q as a novel stimulated risk gene for Atherosclerosis. (2023, Front Immunol, PMID:38179058)

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Description

Chronic vascular inflammation epigenetically reprograms SPI1 chromatin accessibility, maintaining persistent neuroinflammatory gene expression even after vascular insult resolution. Targeted epigenetic editing to reset SPI1 binding landscapes could reverse pathological microglial activation states.

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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.

5 citations 5 with PMID 5 medium Validation: 0% 5 supporting / 0 opposing

✓ For (5)

No opposing evidence

(0) Against ✗

High Medium Low

Evidence Matrix — sortable by strength/year, click Abstract to expand

Evidence Types

MECH 5CLIN 0GENE 0EPID 0

Claim	Stance	Category	Source	Strength ↕	Year ↕	Quality ↕	PMIDs	Abstract
Microglial phagocytosis in Alzheimer disease.	Supporting	MECH	Nat Rev Neurol	MEDIUM	2026	-	PMID:41315858	-
Adult-onset CNS myelin sulfatide deficiency is suf…	Supporting	MECH	Mol Neurodegene…	MEDIUM	2021	-	PMID:34526055	-
Spi1 aggravates neuropathic pain by modulating Cle…	Supporting	MECH	J Headache Pain	MEDIUM	2025	-	PMID:40640733	-
Pu.1/Spi1 dosage controls the turnover and mainten…	Supporting	MECH	Elife	MEDIUM	2025	-	PMID:40673490	-
Iterative transcription factor screening enables r…	Supporting	MECH	Nat Commun	MEDIUM	2025	-	PMID:40494892	-

Legacy Card View — expandable citation cards

✓ Supporting Evidence 5

Microglial phagocytosis in Alzheimer disease. MEDIUM

Nat Rev Neurol · 2026 · PMID:41315858

Adult-onset CNS myelin sulfatide deficiency is sufficient to cause Alzheimer's disease-like neuroinflammation … MEDIUM▼

Adult-onset CNS myelin sulfatide deficiency is sufficient to cause Alzheimer's disease-like neuroinflammation and cognitive impairment.

Mol Neurodegener · 2021 · PMID:34526055

Spi1 aggravates neuropathic pain by modulating Clec7a-mediated neuroinflammation and microglial phagocytosis. MEDIUM

J Headache Pain · 2025 · PMID:40640733

Pu.1/Spi1 dosage controls the turnover and maintenance of microglia in zebrafish and mammals. MEDIUM

Elife · 2025 · PMID:40673490

Iterative transcription factor screening enables rapid generation of microglia-like cells from human iPSC. MEDIUM

Nat Commun · 2025 · PMID:40494892

✗ Opposing Evidence 0

No evidence recorded

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.

Gap Analysis | 4 rounds | 2026-04-09 | View Analysis

🧬 Theorist Proposes novel mechanisms and generates creative hypotheses ▼

Based on the literature describing SPI1's role as a transcription factor regulating hub genes in atherosclerosis and neuroinflammation, I'll generate novel therapeutic hypotheses that bridge vascular and neurological pathology:

Hypothesis 1: SPI1-C1Q Transcriptional Circuit Drives Cerebrovascular Neuroinflammation

Description: SPI1 directly regulates C1Q expression in brain microglia, creating a feed-forward loop that amplifies neuroinflammation in cerebrovascular disease. Selective inhibition of SPI1 binding to C1Q promoter regions could break this pathological circuit while preservin

🔍 Skeptic Identifies weaknesses, alternative explanations, and methodological concerns ▼

I'll provide a rigorous critique of each hypothesis based on the evidence presented and known biological principles. Let me evaluate these systematically:

Hypothesis 1: SPI1-C1Q Transcriptional Circuit Drives Cerebrovascular Neuroinflammation

Confidence: 0.75 → Revised: 0.35

Critical Weaknesses:

Speculative Direct Regulation: No evidence provided that SPI1 directly binds C1Q promoter regions in brain microglia

Feed-Forward Loop Assumption: The proposed "feed-forward loop" mechanism lacks supporting data - C1Q doesn't necessarily regulate SPI1 expression

**Tissue C

🎯 Domain Expert Assesses practical feasibility, druggability, and clinical translation ▼

Now let me check for specific information about complement C1q therapies and look up more details about ANX005, which appears to be a C1q inhibitor in clinical development.

⚖ Synthesizer Integrates perspectives and produces final ranked assessments ▼

Based on the comprehensive debate between the Theorist, Skeptic, and Expert assessments, I'll synthesize the evidence and provide scored rankings for the seven SPI1-targeted therapeutic hypotheses.

Price History

7d Trend

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Stable

7d Momentum

▲ 7.2%

Volatility

High

0.0530

Events (7d)

Clinical Trials (0)

No clinical trials data available

📚 Cited Papers (5)

Adult-onset CNS myelin sulfatide deficiency is sufficient to cause Alzheimer's disease-like neuroinflammation and cognitive impairment.

Molecular neurodegeneration (2021) · PMID:34526055

No extracted figures yet

Paper:40494892

No extracted figures yet

Paper:40640733

No extracted figures yet

Paper:40673490

No extracted figures yet

Microglial phagocytosis in Alzheimer disease.

Nature reviews. Neurology (2026) · PMID:41315858

No extracted figures yet

📅 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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📙 Related Wiki Pages (0)

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📓 Linked Notebooks (1)

📓 How does SPI1 transcriptionally regulate C1QA and C1QC expression in atherosclerotic contexts? — Analysis Notebook

CI-generated notebook stub for analysis SDA-2026-04-08-gap-pubmed-20260406-062122-bfac06c8. The authors identify SPI1 as a potential transcription factor regulating the hub genes but provide no mechan …

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📊 Resource Economics & ROI

Moderate Efficiency Resource Efficiency Score

0.50

32.3th percentile (776 hypotheses)

Tokens Used

KG Edges Generated

Citations Produced

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

0.505

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 SPI1.

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⚖️ Governance History

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