Microglia in Huntington's Disease

cell · SciDEX wiki

Microglia in Huntington's Disease
Taxonomy ID
Cell Ontology (CL) [CL:0000129](https://www.ebi.ac.uk/ols4/ontologies/cl/classes/http%253A%252F%252Fpurl.obolibrary.org%252Fobo%252FCL_0000129)
Database ID
Cell Ontology [CL:0000129](https://www.ebi.ac.uk/ols4/ontologies/cl/classes/http%253A%252F%252Fpurl.obolibrary.org%252Fobo%252FCL_0000129)

Introduction

Microglia In Huntington’S Disease is a cell type relevant to neurodegenerative disease research. This page covers its role in brain function, involvement in disease processes, and significance for therapeutic strategies.

Pathway / Mechanism Diagram

graph TD
    A["HTT Gene: CAG Repeat Expansion"] --> B["Mutant Huntingtin (mHTT)"]
    B --> C["Polyglutamine Aggregation"]
    C --> D["Nuclear Inclusions"]
    B --> E["Transcriptional Dysregulation"]
    E --> F["BDNF Downregulation"]
    F --> G["Striatal Neuron Vulnerability"]
    B --> H["Mitochondrial Dysfunction"]
    H --> I["Energy Deficit"]
    B --> J["Impaired Autophagy"]
    J --> K["Toxic Protein Accumulation"]
    G --> L["Medium Spiny Neuron Death"]
    I --> L
    K --> L
    L --> M["Chorea and Motor Symptoms"]
    L --> N["Cognitive Decline"]
    L --> O["Psychiatric Symptoms"]
    style A fill:#ef5350,color:#e0e0e0
    style L fill:#ef5350,color:#e0e0e0
    style B fill:#5d4400,color:#e0e0e0

Overview

Huntington’s disease (HD) is characterized by selective neurodegeneration of striatal medium spiny neurons and cortical pyramidal neurons, driven by mutant huntingtin (mHTT) expansion. Microglia, the brain’s innate immune cells, play a complex role in HD pathogenesis, contributing to neuroinflammation while also attempting to clear pathological protein aggregates and cellular debris. 1(2019)2019

2(2020)2020

Multi-Taxonomy Classification

Taxonomy Database Cross-References

Morphology & Electrophysiology

  • Morphology: microglial cell (source: Cell Ontology)

    • Morphology can be inferred from Cell Ontology classification

PanglaoDB Marker Cross-References

  • Unknown (PanglaoDB):

Taxonomy & Classification

PanglaoDB Marker Cross-References

  • Unknown (PanglaoDB):

Molecular Markers

Microglial Markers

  • IBA1 (AIF1) - ionized calcium-binding adapter molecule 1

  • CD68 - lysosomal marker (activated microglia)

  • CD11b (ITGAM) - complement receptor 3

  • TREM2 - triggering receptor expressed on myeloid cells 2

  • TYROBP (DAP12) - adaptor protein for TREM2

  • CX3CR1 - fractalkine receptor

  • P2RY12 - purinergic receptor

Disease-Associated Markers

  • CD68 upregulation: Chronic activation

  • TREM2 expression: In HD microglia

  • HLA-DR: MHC class II (activated state)

  • LPL (Lipoprotein Lipase): Lipid metabolism in disease

Anatomy and Distribution

Regional Distribution

  • Striatum: Highest microglial density, severe pathology

  • Cortex: Layer-specific activation

  • Hippocampus: Moderate involvement

  • White matter: Subcortical regions

Activation Patterns

  • Early activation: Pre-symptomatic stages

  • Progressive increase: With disease progression

  • Spatial correlation: With neurodegeneration

Pathology in HD

Microglial Activation

  • Morphological changes: Amoeboid morphology

  • Increased density: 2-3 fold in striatum

  • Cluster formation: Around degenerating neurons

  • Chronic activation: Sustained pro-inflammatory state

Interactions with Mutant Huntingtin

  • mHTT in microglia: Cell-autonomous dysfunction

  • Impaired phagocytosis: Reduced clearance

  • Cytokine dysregulation: Altered secretion

  • NLRP3 inflammasome: Enhanced activation

Mechanisms of Dysfunction

1. Mutant Huntingtin Effects

  • Cell-autonomous pathology: mHTT in microglia

  • Transcriptional dysregulation: Altered gene expression

  • Metabolic impairment: Mitochondrial dysfunction

  • Protein aggregation: mHTT inclusions

2. Inflammatory Cascade

  • Pro-inflammatory cytokines: TNF-α, IL-1β, IL-6

  • Chemokines: CCL2, CXCL10

  • Nitric oxide: ROS production

  • Prostaglandins: Cyclooxygenase products

3. Neuron-Microglia Interaction

  • CX3CL1/CX3CR1: Fractalkine signaling

  • CD47/SIRPα: Phagocytic checkpoint

  • Complement system: Synaptic pruning

  • TREM2/DAP12: Activation signaling

4. Metabolic Dysfunction

  • Energy impairment: Glycolysis defects

  • Mitochondrial dysfunction: Complex I-V deficits

  • Oxidative stress: ROS accumulation

Clinical Implications

Disease Progression

  • Correlation with severity: Microglial activation and clinical scores

  • Early marker: Pre-symptomatic activation

  • Therapeutic target: Disease modification

Symptoms Affected

  • Motor dysfunction: Contributes to chorea

  • Cognitive decline: Neuroinflammation role

  • Behavioral changes: Cytokine effects on mood

Therapeutic Implications

Anti-inflammatory Approaches

  • Minocycline: Inhibits microglial activation

  • Coenzyme Q10: Mitochondrial support

  • CX3CR1 antagonists: Reduce inflammation

Modulation Strategies

  • TREM2 modulation: Protective approaches

  • Cytokine inhibitors: TNF-α blockade

  • Phagocytosis enhancement: Improve clearance

Gene Therapy

  • HTT lowering: Reduces microglial pathology

  • Antisense oligonucleotides: mHTT reduction

  • CRISPR approaches: Future therapies

Background

The study of Microglia In Huntington’S Disease has evolved significantly over the past decades. Research in this area has revealed important insights into the underlying mechanisms of neurodegeneration and continues to drive therapeutic development.

Historical context and key discoveries in this field have shaped our current understanding and will continue to guide future research directions.

See Also

Cross-References

From the SciDEX Exchange — scored by multi-agent debate

Related Analyses:

Pathway Diagram

The following diagram shows the key molecular relationships involving Microglia in Huntington’s Disease discovered through SciDEX knowledge graph analysis:

graph TD
    ds_f2c28aed24a7["ds-f2c28aed24a7"] -->|"data in"| microglia["microglia"]
    ent_gene_28e2cb01["ent-gene-28e2cb01"] -->|"expressed in"| microglia["microglia"]
    Iba1["Iba1"] -->|"expressed in"| microglia["microglia"]
    anxiety["anxiety"] -->|"affects"| microglia["microglia"]
    aging["aging"] -->|"affects"| microglia["microglia"]
    Alzheimer_s_disease["Alzheimer's disease"] -->|"affects"| microglia["microglia"]
    NF_kB_signaling["NF-kB signaling"] -->|"active in"| microglia["microglia"]
    TNF["TNF"] -->|"secreted by"| microglia["microglia"]
    unfolded_protein_response["unfolded protein response"] -->|"active in"| microglia["microglia"]
    complement_cascade["complement cascade"] -->|"active in"| microglia["microglia"]
    TNF__["TNF-α"] -->|"secreted by"| microglia["microglia"]
    TREM2_APOE_pathway["TREM2-APOE pathway"] -->|"regulates"| microglia["microglia"]
    ULK1["ULK1"] -->|"expressed in"| microglia["microglia"]
    neuroinflammation["neuroinflammation"] -->|"affects"| microglia["microglia"]
    neurodegeneration["neurodegeneration"] -->|"affects"| microglia["microglia"]
    style ds_f2c28aed24a7 fill:#4fc3f7,stroke:#333,color:#000
    style microglia fill:#80deea,stroke:#333,color:#000
    style ent_gene_28e2cb01 fill:#ce93d8,stroke:#333,color:#000
    style Iba1 fill:#4fc3f7,stroke:#333,color:#000
    style anxiety fill:#ef5350,stroke:#333,color:#000
    style aging fill:#ef5350,stroke:#333,color:#000
    style Alzheimer_s_disease fill:#ef5350,stroke:#333,color:#000
    style NF_kB_signaling fill:#81c784,stroke:#333,color:#000
    style TNF fill:#4fc3f7,stroke:#333,color:#000
    style unfolded_protein_response fill:#81c784,stroke:#333,color:#000
    style complement_cascade fill:#81c784,stroke:#333,color:#000
    style TNF__ fill:#4fc3f7,stroke:#333,color:#000
    style TREM2_APOE_pathway fill:#81c784,stroke:#333,color:#000
    style ULK1 fill:#ce93d8,stroke:#333,color:#000
    style neuroinflammation fill:#ef5350,stroke:#333,color:#000
    style neurodegeneration fill:#ef5350,stroke:#333,color:#000

References

  1. (2019) Palpagama TH, et al 2019
  2. (2020) Bhattacharyya A, et al 2020

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