🧪
hypothesis

Gut butyrate deficiency impairs microglial amyloid clearance via HDAC2-mediated epigenetic dysregulation

Hypothesis

Gut butyrate deficiency impairs microglial amyloid clearance via HDAC2-mediated epigenetic dysregulation

Gut dysbiosis in Alzheimer's disease reduces butyrate-producing bacteria (Faecalibacterium prausnitzii, Roseburia intestinalis), causing systemic butyrate deficiency.
🧬 HDAC2🩺 alzheimers🎯 Composite 38%💱 $0.53▲9.6%proposed
neurodegeneration
EvidencePending (0%)📖 5 cit🗣 1 debates 5 support 1 oppose
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🧪 Overview

Gut dysbiosis in Alzheimer's disease reduces butyrate-producing bacteria (Faecalibacterium prausnitzii, Roseburia intestinalis), causing systemic butyrate deficiency. Butyrate normally acts as an endogenous histone deacetylase (HDAC) inhibitor; decreased butyrate allows HDAC2 to suppress histone acetylation at promoters of anti-inflammatory genes in microglia, impairing their ability to phagocytose and clear amyloid-beta plaques. This HDAC2-mediated epigenetic silencing reduces expression of genes encoding phagocytic receptors (TREM2, CR3) and lysosomal enzymes, creating a feed-forward loop where accumulated amyloid further disrupts gut barrier integrity and exacerbates dysbiosis. Oral supplementation with butyrate or butyrate-producing bacterial consortia would restore microglial epigenetic regulation and enhance amyloid clearance.

🧬 Mechanism

🧬 Curated Mechanism Pathway

Curated pathway from expert analysis

flowchart TD
    A["HDAC2 Activity<br/>Histone Deacetylase"]
    B["Microglial Epigenetic<br/>Regulation"]
    C["Phagocytosis<br/>Gene Expression"]
    D["Microglial Amyloid<br/>Clearance Capacity"]
    E["HDAC-Dependent<br/>Epigenetic Dysregulation"]
    F["HDAC2 as<br/>Microglial Reprogramming Target"]
    A --> B
    B --> C
    C --> D
    D --> E
    E --> F
    style A fill:#7b1fa2,stroke:#ce93d8,color:#ce93d8
    style F fill:#1b5e20,stroke:#a5d6a7,color:#a5d6a7

⚖️ Evidence

⚖️ Evidence Matrix5 supports0 contradicts
Supports
PubMed PMID 39276955
PubMedPMID:39276955medium
Supports
PubMed PMID 36833274
PubMedPMID:36833274medium
Supports
PubMed PMID 37642942
PubMedPMID:37642942medium
Supports
PubMed PMID 37328865
PubMedPMID:37328865medium
Supports
PubMed PMID 40451396
PubMedPMID:40451396medium
📖 Linked Papers

No linked papers recorded for this hypothesis yet.

🏥 Translation

🧬 3D Protein Structure — HDAC2

No curated PDB or AlphaFold mapping for HDAC2 yet. Search RCSB →

🧠 GTEx v10 Brain ExpressionJSON

Median TPM across 13 brain regions for HDAC2 from GTEx v10.

Cerebellar Hemisphere19.9 Cerebellum14.5median TPM (GTEx v10)

💉 Clinical Trials

No clinical trials data linked to this hypothesis yet.

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

🔍 Search ClinVar for HDAC2 →

No DepMap CRISPR Chronos data found for HDAC2.

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🔮 Predictions

🔎 Predictions vs Observations2 predictions · 0 with recorded observations
PredictionPredictedObservedStatusConf
IF adult 5xFAD mice with established amyloid pathology are given oral sodium butyrate supplementation (150 mg/kg/day) for 8 weeks, THEN hippocampal amyloid plaque burden will decrease by at least 25% Hippocampal amyloid plaque burden reduced by ≥25% (Thioflavin-S stereology or 11C-PiB PET SUVR) after 8 weeks of butyrate supplementation— no observation —pending0.65
IF butyrate supplementation restores microglial phagocytic capacity, THEN butyrate-treated 5xFAD mice will show at least 2-fold increase in TREM2 and CR3 gene expression and enhanced in vivo amyloid pTREM2 and CR3 mRNA expression ≥2-fold higher; in vivo phagocytosis assay shows ≥2-fold increased amyloid internalization by microglia in butyrate-treated mice— no observation —pending0.55
🔮 Falsifiable Predictions (2)
pendingconf 65%
IF adult 5xFAD mice with established amyloid pathology are given oral sodium butyrate supplementation (150 mg/kg/day) for 8 weeks, THEN hippocampal amyloid plaque burden will decrease by at least 25% compared to vehicle-treated controls, as quantified by Thioflavin-S or 11C-PiB PET imaging.
Predicted outcome: Hippocampal amyloid plaque burden reduced by ≥25% (Thioflavin-S stereology or 11C-PiB PET SUVR) after 8 weeks of butyrate supplementation
Falsification: No significant difference in amyloid plaque load between butyrate and vehicle groups (p > 0.05), indicating butyrate supplementation does not reduce amyloid burden
pendingconf 55%
IF butyrate supplementation restores microglial phagocytic capacity, THEN butyrate-treated 5xFAD mice will show at least 2-fold increase in TREM2 and CR3 gene expression and enhanced in vivo amyloid phagocytosis rate compared to vehicle controls.
Predicted outcome: TREM2 and CR3 mRNA expression ≥2-fold higher; in vivo phagocytosis assay shows ≥2-fold increased amyloid internalization by microglia in butyrate-trea
Falsification: TREM2/CR3 expression unchanged or decreased despite butyrate treatment, or no increase in amyloid phagocytosis rate, indicating HDAC2 is not mediating butyrate's effects on microglial gene expression
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