Glutamate Transporter Neurons represent a critical component in maintaining synaptic homeostasis and preventing excitotoxic neurodegeneration. The excitatory amino acid transporters (EAATs) are responsible for clearing glutamate from the synaptic cleft, preventing excessive activation of NMDA and AMPA receptors that can lead to calcium influx and neuronal death.
| Property |
Value |
| Category |
Synaptic Transmission |
| Location |
Neuronal and glial membranes |
| Transporters |
EAAT1-5 (GLAST, GLT-1, EAAC1, EAAT4, EAAT5) |
| Function |
Glutamate clearance from synaptic cleft |
| Primary Role |
Prevent excitotoxicity |
¶ EAAT Function and Distribution
- Distribution: Predominantly in astrocytes, Bergmann glia in cerebellum
- Function: High-affinity glutamate uptake
- Expression: Cerebellum, retina, inner ear
- Distribution: Astrocytic processes ensheathing synapses (70% of CNS glutamate uptake)
- Function: Primary glutamate transporter in forebrain
- Significance: Major therapeutic target for neurodegeneration
- Distribution: Neuronal cell bodies and dendrites
- Function: Glutamate transport in neurons
- Role: Cysteine uptake for glutathione synthesis
- Distribution: Cerebellar Purkinje cells, retina
- Function: Modulates synaptic plasticity
- Distribution: Retina
- Function: Photoreceptor and bipolar cell function
The EAAT transporters work by coupling glutamate uptake to sodium and potassium gradients:
- Sodium gradient: 3 Na+ ions transported inward with glutamate
- Potassium gradient: 1 K+ ion transported outward
- Electrogenic: Net positive charge moved into cell
- Coupling: Requires intact Na+/K+ ATPase function
This mechanism allows for concentrative glutamate uptake against 10,000-fold concentration gradients.
- GLT-1 loss: Up to 95% reduction in GLT-1 expression in ALS spinal cord
- Astrocytic dysfunction: Failure of glutamate clearance precedes motor neuron death
- Excitotoxicity hypothesis: Excessive glutamate stimulation leads to motor neuron degeneration
- Riluzole: FDA-approved EAAT enhancer, modestly extends survival
- Gene therapy approaches: AAV-mediated GLT-1 delivery showing promise in preclinical models
- Ceftriaxone: Beta-lactam antibiotic upregulates GLT-1, tested in clinical trials
- EAAT dysfunction: Impaired glutamate transport in AD hippocampus
- Amyloid-beta effects: Direct downregulation of EAAT2 expression
- Tau pathology: Affects EAAT trafficking to synaptic membranes
- Calcium dysregulation: Excitotoxicity cascade from impaired clearance
- Therapeutic targeting: EAAT2 agonists under investigation
- Substrate-specific changes: Variable EAAT expression in PD substantia nigra
- Excitotoxic contribution: Mechanism in dopaminergic neuron loss
- Neuroprotection strategies: EAAT upregulation approaches
- MPTP model: Demonstrates EAAT dysfunction in toxin-induced Parkinsonism
- EAAT2 reduction: Decreased expression in HD striatum
- Excitotoxic mechanisms: Contributing to selective striatal neuron vulnerability
- Riluzole trials: Investigated for HD treatment
- Riluzole: Primary FDA-approved EAAT enhancer
- Ceftriaxone: Antibiotic upregulates GLT-1 expression via NF-κB
- Beta-lactams: Screen identified multiple GLT-1 upregulators
- AAV-GLT-1: Viral vector delivery of EAAT2
- Gene editing: CRISPR approaches to enhance EAAT expression
- Astrocyte transplantation: Replace dysfunctional astrocytes
- Stem cell approaches: Generate EAAT-expressing cells