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ALS-Associated G3BP1 Mutations Shift Phase Separation Equilibrium Toward Aberrant Condensate Stabilization

Target: G3BP1 Composite Score: 0.610 Price: $0.61 Citation Quality: Pending neurodegeneration Status: proposed
☰ Compare⚔ Duel⚛ Collideinteract with this hypothesis
✓ All Quality Gates Passed
Quality Report Card click to collapse
B
Composite: 0.610
Top 55% of 1166 hypotheses
T4 Speculative
Novel AI-generated, no external validation
Needs 1+ supporting citation to reach Provisional
B Mech. Plausibility 15% 0.62 Top 56%
B+ Evidence Strength 15% 0.70 Top 30%
B Novelty 12% 0.65 Top 69%
C+ Feasibility 12% 0.55 Top 53%
B+ Impact 12% 0.72 Top 39%
C Druggability 10% 0.40 Top 78%
C Safety Profile 8% 0.45 Top 74%
B+ Competition 6% 0.70 Top 41%
C+ Data Availability 5% 0.58 Top 59%
B Reproducibility 5% 0.65 Top 38%
Evidence
4 supporting | 3 opposing
Citation quality: 0%
Debates
1 session B
Avg quality: 0.69
Convergence
0.00 F 13 related hypothesis share this target

From Analysis:

How do disease-associated mutations in G3BP1 or its binding partners alter stress granule dynamics?

The study establishes G3BP1's role as a tunable switch for stress granule assembly, but doesn't address how neurodegeneration-linked mutations might dysregulate this process. Understanding mutation effects could explain disease mechanisms and guide therapeutic strategies. Gap type: open_question Source paper: G3BP1 Is a Tunable Switch that Triggers Phase Separation to Assemble Stress Granules. (2020, Cell, PMID:32302571)

→ View full analysis & debate transcript

Hypotheses from Same Analysis (6)

These hypotheses emerged from the same multi-agent debate that produced this hypothesis.

Ataxin-2 Polyglutamine Expansions Hijack G3BP1 to Form Toxic, Irreversible Stress Granule Complexes
Score: 0.700 | Target: ATXN2
G3BP1 Haploinsufficiency Reveals a Therapeutic Window for SG-Targeting Interventions
Score: 0.590 | Target: G3BP1
Dysregulated G3BP1 Signaling Impairs Local Translation in Neuronal Processes, Contributing to Synaptic Dysfunction
Score: 0.580 | Target: G3BP1
G3BP1-TDP-43 Cross-Seeding Drives Co-Aggregation That Prion-Spreads Across Neural Circuits
Score: 0.490 | Target: TARDBP
FUS Mutations Impede G3BP1's Chaperone Function, Exposing Neurotoxic Stress Granule Intermediates
Score: 0.430 | Target: FUS
Small-Molecule Modulation of G3BP1 Condensate Dynamics via PRMT1 Methylation as a Therapeutic Strategy
Score: 0.400 | Target: G3BP1, PRMT1

→ View full analysis & all 7 hypotheses

Description

Disease-linked missense mutations in G3BP1's intrinsically disordered region alter valency and net charge, increasing liquid-liquid phase separation propensity while reducing dynamic exchange rates. This creates solid-like stress granules that fail to dissolve, causing persistent RNA sequestration and translational arrest in motor neurons. Represents the most direct mechanistic link between patient-derived mutations and the tunable switch function established in the source paper.

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3D Protein Structure

PDB: Open in RCSB AlphaFold model

Interactive 3D viewer powered by RCSB PDB / Mol*. Use mouse to rotate, scroll to zoom.

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 0.62 (15%) Evidence 0.70 (15%) Novelty 0.65 (12%) Feasibility 0.55 (12%) Impact 0.72 (12%) Druggability 0.40 (10%) Safety 0.45 (8%) Competition 0.70 (6%) Data Avail. 0.58 (5%) Reproducible 0.65 (5%) 0.610 composite
7 citations 7 with PMID Validation: 0% 4 supporting / 3 opposing
For (4)
No supporting evidence
No opposing evidence
(3) Against
High Medium Low
High Medium Low
Evidence Matrix — sortable by strength/year, click Abstract to expand
Evidence Types
2
5
MECH 2CLIN 0GENE 5EPID 0
ClaimStanceCategorySourceStrength ↕Year ↕Quality ↕PMIDsAbstract
G3BP1 mutations identified in ALS patientsSupportingGENE----PMID:30030428-
G3BP1 mutations identified in ALS patientsSupportingGENE----PMID:29686387-
Stress granule persistence documented in ALS/FTD p…SupportingMECH----PMID:28061422-
G3BP1 central scaffold role established for SG ass…SupportingMECH----PMID:32302571-
ALS-linked G3BP1 variants are extremely rare (<…OpposingGENE----PMID:29486656-
Mutation validation problem: rare does not equal p…OpposingGENE----PMID:29686387-
Directionality of effect not established; loss-of-…OpposingGENE----PMID:32302571-
Legacy Card View — expandable citation cards

Supporting Evidence 4

G3BP1 mutations identified in ALS patients
PMID:30030428
G3BP1 mutations identified in ALS patients
PMID:29686387
Stress granule persistence documented in ALS/FTD post-mortem tissue
PMID:28061422
G3BP1 central scaffold role established for SG assembly
PMID:32302571

Opposing Evidence 3

ALS-linked G3BP1 variants are extremely rare (<1% of cases); TDP-43 pathology can occur independently of G3BP1…
ALS-linked G3BP1 variants are extremely rare (<1% of cases); TDP-43 pathology can occur independently of G3BP1 mutation
PMID:29486656
Mutation validation problem: rare does not equal pathogenic without functional studies
PMID:29686387
Directionality of effect not established; loss-of-function could also be disease-associated
PMID:32302571
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 | 2026-04-22 | View Analysis
🧬 Theorist Proposes novel mechanisms and generates creative hypotheses

Mechanistic and Therapeutic Hypotheses: G3BP1 Mutations in Neurodegeneration

Hypothesis 1: ALS-Associated G3BP1 Mutations Shift Phase Separation Equilibrium Toward Aberrant Condensate Stabilization

Mechanism: Disease-linked missense mutations (e.g., G3BP1-G56E, Q305E) in the intrinsically disordered region alter the valency and net charge of G3BP1, increasing its propensity for liquid-liquid phase separation (LLPS) while reducing the dynamic exchange rate within condensates. This creates "solid-like" stress granules that fail to dissolve, leading to persistent RNA sequestration

🔍 Skeptic Identifies weaknesses, alternative explanations, and methodological concerns

Critical Evaluation of G3BP1 Neurodegeneration Hypotheses

I'm a rigorous scientific Skeptic. My job is to identify weaknesses, not to build confidence. What follows is a systematic critique of each hypothesis.

Hypothesis 1: ALS-Associated G3BP1 Mutations Shift Phase Separation Equilibrium

1. Mutation-validation problem. The cited PMIDs (30030428, 29686387) report identification of rare variants through whole-exome sequencing, but rare does not equal pathogenic. Without functional validation in model systems, these could be passenger mutations or polymorphisms i

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

Domain Expert Assessment: G3BP1 Neurodegeneration Hypotheses

Executive Summary

Following integration of the Skeptic's mechanistic critiques with drug discovery feasibility analysis, three hypotheses warrant serious translational consideration (H1, H2, H3), while H7 offers a differentiated synaptic biology angle, and H6 describes a therapeutic modality rather than mechanism. H4 and H5 have insufficient mechanistic foundations to support drug discovery investment at this stage.

Prioritization Framework

| Hypothesis | Mechanistic Validity | Druggability | Clinical Feasibility

Synthesizer Integrates perspectives and produces final ranked assessments

{
"ranked_hypotheses": [
{
"title": "ALS-Associated G3BP1 Mutations Shift Phase Separation Equilibrium Toward Aberrant Condensate Stabilization",
"description": "Disease-linked missense mutations in G3BP1's intrinsically disordered region alter valency and net charge, increasing liquid-liquid phase separation propensity while reducing dynamic exchange rates. This creates solid-like stress granules that fail to dissolve, causing persistent RNA sequestration and translational arrest in motor neurons. Represents the most direct mechanistic link between patient-derived mutations

Price History

0.600.610.62 0.63 0.59 2026-04-222026-04-222026-04-22 Market PriceScoreevidencedebate 1 events
7d Trend
Stable
7d Momentum
▲ 0.0%
Volatility
Low
0.0000
Events (7d)
1

Clinical Trials (0)

No clinical trials data available

📚 Cited Papers (5)

Paper:28061422
No extracted figures yet
Paper:29486656
No extracted figures yet
Paper:29686387
No extracted figures yet
Paper:30030428
No extracted figures yet
G3BP1 Is a Tunable Switch that Triggers Phase Separation to Assemble Stress Granules.
Cell (2020) · PMID:32302571
No extracted figures yet

📓 Linked Notebooks (2)

📓 How do disease-associated mutations in G3BP1 or its binding partners alter stress granule dynamics? - Notebook
Analysis notebook for: How do disease-associated mutations in G3BP1 or its binding partners alter stress granule dynamics?
📓 How do disease-associated mutations in G3BP1 or its binding partners alter stress granule dynamics? — Analysis Notebook
CI-generated notebook stub for analysis SDA-2026-04-06-gap-pubmed-20260406-041428-e14e6524. The study establishes G3BP1's role as a tunable switch for stress granule assembly, but doesn't address how …
→ Browse all notebooks

⚔ Arena Performance

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KG Entities (35)

ALSALS riskASO-mediated Ataxin-2 knockdownAberrant SG sequestration of eIF4G/eIF3Ataxin-2 expansionsAtaxin-2 polyglutamine expansions (>34 rAtaxin-2-G3BP1 complexesAutophagy clearance evasionCognitive declineDetergent-resistant aggregatesG3BP1G3BP1 complex formationG3BP1 dynamicsG3BP1 dysfunctionG3BP1 material propertiesG3BP1 mutationsG3BP1-TDP-43 hybrid aggregatesLocal translation in neuronal processesNMJ denervationRNA sequestration

Related Hypotheses

Ubiquitin-Mediated Liquid-to-Solid Transition Prevention
Score: 0.730 | neurodegeneration
Phase-Separated Organelle Targeting
Score: 0.729 | neurodegeneration
Autophagic Receptor Sequestration via K63-Ub 'Signalone' Recognition
Score: 0.720 | neurodegeneration
Stress Granule Phase Separation Modulators
Score: 0.720 | neurodegeneration
RNA Granule Nucleation Site Modulation
Score: 0.662 | neurodegeneration

Estimated Development

Estimated Cost
$0
Timeline
0 months

🧪 Falsifiable Predictions

No explicit predictions recorded yet. Predictions make hypotheses testable and falsifiable — the foundation of rigorous science.

Knowledge Subgraph (22 edges)

associated with (1)

G3BP1 mutations ALS

causes (12)

G3BP1 mutations Stress granule persistence
Stress granule persistence RNA sequestration
RNA sequestration Translational arrest
Ataxin-2 polyglutamine expansions (>34 repeats) G3BP1 complex formation
Ataxin-2-G3BP1 complexes RNA-binding protein sequestration
...and 7 more

indicates (1)

G3BP1 dynamics Stress granule dysfunction

inhibits (1)

ASO-mediated Ataxin-2 knockdown Toxic Ataxin-2-G3BP1 complexes

modulates (1)

TDP-43 G3BP1 material properties

produced (1)

sess_SDA-2026-04-06-gap-pubmed-20260406-041428-e14e6524_task_9aae8fc5 SDA-2026-04-06-gap-pubmed-20260406-041428-e14e6524

regulates (3)

G3BP1 Stress granule assembly
G3BP1 Local translation in neuronal processes
eIF4G Synaptic proteostasis

risk factor for (1)

Ataxin-2 expansions ALS risk

templates (1)

G3BP1 TDP-43 amyloidogenesis

Mechanism Pathway for G3BP1

Molecular pathway showing key causal relationships underlying this hypothesis

graph TD
    G3BP1["G3BP1"] -->|regulates| Stress_granule_assembly["Stress granule assembly"]
    G3BP1_mutations["G3BP1 mutations"] -->|causes| Stress_granule_persistenc["Stress granule persistence"]
    G3BP1_mutations_1["G3BP1 mutations"] -->|associated with| ALS["ALS"]
    Ataxin_2_polyglutamine_ex["Ataxin-2 polyglutamine expansions (>34 repeats)"] -->|causes| G3BP1_complex_formation["G3BP1 complex formation"]
    Ataxin_2_G3BP1_complexes["Ataxin-2-G3BP1 complexes"] -->|causes| RNA_binding_protein_seque["RNA-binding protein sequestration"]
    Ataxin_2_G3BP1_complexes_2["Ataxin-2-G3BP1 complexes"] -->|causes| Detergent_resistant_aggre["Detergent-resistant aggregates"]
    ASO_mediated_Ataxin_2_kno["ASO-mediated Ataxin-2 knockdown"] -.->|inhibits| Toxic_Ataxin_2_G3BP1_comp["Toxic Ataxin-2-G3BP1 complexes"]
    G3BP1_3["G3BP1"] -->|regulates| Local_translation_in_neur["Local translation in neuronal processes"]
    G3BP1_dysfunction["G3BP1 dysfunction"] -->|causes| Synaptic_translation_dysr["Synaptic translation dysregulation"]
    G3BP1_dysfunction_4["G3BP1 dysfunction"] -->|causes| NMJ_denervation["NMJ denervation"]
    G3BP1_dysfunction_5["G3BP1 dysfunction"] -->|causes| Cognitive_decline["Cognitive decline"]
    TDP_43["TDP-43"] -->|modulates| G3BP1_material_properties["G3BP1 material properties"]
    G3BP1_6["G3BP1"] -->|templates| TDP_43_amyloidogenesis["TDP-43 amyloidogenesis"]
    G3BP1_TDP_43_hybrid_aggre["G3BP1-TDP-43 hybrid aggregates"] -->|causes| Autophagy_clearance_evasi["Autophagy clearance evasion"]
    G3BP1_dynamics["G3BP1 dynamics"] -->|indicates| Stress_granule_dysfunctio["Stress granule dysfunction"]
    style G3BP1 fill:#ce93d8,stroke:#333,color:#000
    style Stress_granule_assembly fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_mutations fill:#ce93d8,stroke:#333,color:#000
    style Stress_granule_persistenc fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_mutations_1 fill:#ce93d8,stroke:#333,color:#000
    style ALS fill:#ef5350,stroke:#333,color:#000
    style Ataxin_2_polyglutamine_ex fill:#ce93d8,stroke:#333,color:#000
    style G3BP1_complex_formation fill:#4fc3f7,stroke:#333,color:#000
    style Ataxin_2_G3BP1_complexes fill:#4fc3f7,stroke:#333,color:#000
    style RNA_binding_protein_seque fill:#4fc3f7,stroke:#333,color:#000
    style Ataxin_2_G3BP1_complexes_2 fill:#4fc3f7,stroke:#333,color:#000
    style Detergent_resistant_aggre fill:#4fc3f7,stroke:#333,color:#000
    style ASO_mediated_Ataxin_2_kno fill:#4fc3f7,stroke:#333,color:#000
    style Toxic_Ataxin_2_G3BP1_comp fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_3 fill:#4fc3f7,stroke:#333,color:#000
    style Local_translation_in_neur fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_dysfunction fill:#ce93d8,stroke:#333,color:#000
    style Synaptic_translation_dysr fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_dysfunction_4 fill:#ce93d8,stroke:#333,color:#000
    style NMJ_denervation fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_dysfunction_5 fill:#ce93d8,stroke:#333,color:#000
    style Cognitive_decline fill:#4fc3f7,stroke:#333,color:#000
    style TDP_43 fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_material_properties fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_6 fill:#4fc3f7,stroke:#333,color:#000
    style TDP_43_amyloidogenesis fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_TDP_43_hybrid_aggre fill:#4fc3f7,stroke:#333,color:#000
    style Autophagy_clearance_evasi fill:#4fc3f7,stroke:#333,color:#000
    style G3BP1_dynamics fill:#4fc3f7,stroke:#333,color:#000
    style Stress_granule_dysfunctio fill:#4fc3f7,stroke:#333,color:#000

3D Protein Structure

🧬 G3BP1 — PDB 4FCJ Click to expand 3D viewer

Experimental structure from RCSB PDB | Powered by Mol* | Rotate: click+drag | Zoom: scroll | Reset: right-click

Source Analysis

How do disease-associated mutations in G3BP1 or its binding partners alter stress granule dynamics?

neurodegeneration | 2026-04-06 | archived

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