astrocyte_dysfunction

Astrocyte Dysfunction

Astrocyte dysfunction refers to the pathological alteration of astrocytic functions that support neuronal activity, blood-brain barrier integrity, and synaptic regulation.

🧠 Physiological Roles of Astrocytes

  • Regulation of ion homeostasis (e.g., K⁺ buffering).
  • Uptake and recycling of neurotransmitters (especially glutamate via EAATs).
  • Modulation of neurovascular coupling through endfoot signaling.
  • Maintenance of blood-brain barrier (BBB) via interactions with endothelial cells.
  • Participation in synapse formation and pruning.

⚠️ Mechanisms of Dysfunction

  • Impaired glutamate clearance → excitotoxicity.
  • Calcium signaling deficits → disrupted astrocyte-neuron communication.
  • AQP4 mislocalization → defective water homeostasis and edema.
  • Reactive astrogliosis:
    1. Triggered by injury or inflammation.
    2. Can be protective or contribute to scarring and inhibition of regeneration.
  • Metabolic dysfunction: Impaired lactate shuttle and oxidative stress.

🧬 Associated Conditions

  • Neurodegenerative diseases:
    1. Alzheimer’s disease
    2. Parkinson’s disease
    3. Amyotrophic lateral sclerosis (ALS)
  • Cerebrovascular disease:
    1. Stroke → astrocyte-mediated ischemic damage.
  • Epilepsy:
    1. Hyperexcitable networks due to failed K⁺ and glutamate buffering.
  • Brain tumors:
    1. Astrocyte-tumor interactions contribute to invasion and microenvironment modulation.

🧪 Experimental Markers and Models

  • Markers:
    1. GFAP, S100β, AQP4, EAAT1/2
  • Models:
    1. Sorcs2 knockout → impaired calcium signaling and NVC.
    2. Conditional AQP4 deletion → defective water regulation.
    3. GFAP-overexpression mice → study of reactive astrogliosis.

🔗 Related Concepts

  • astrocyte_dysfunction.txt
  • Last modified: 2025/05/10 09:12
  • by administrador