NMDA Receptor Antagonists & Clinical Applications
Glutamate, the NMDA Channel & its Blockers — Ketamine, Memantine, Amantadine, N₂O & Rapid-acting Antidepressants
Past RGUHS · 3
RGUHSJun '24
RGUHSNov '21
RGUHSMay '10
Introduction
- NMDA receptor antagonists inhibit the N-methyl-D-aspartate subtype of the ionotropic glutamate receptor — the substrate of slow excitatory transmission, synaptic plasticity (LTP) and glutamate-mediated excitotoxicity.
- The class is therapeutically heterogeneous; only two agents are in mainstream use — ketamine (anaesthesia, analgesia, depression) and memantine (Alzheimer's) — with amantadine, nitrous oxide (N2O), dextromethorphan and the prototype drug-of-abuse phencyclidine (PCP) as additional channel-blocking members.
- Unifying lesson: broad NMDA blockade has been therapeutically disappointing because glutamate is ubiquitous — flooding the brain with an antagonist causes dissociation/hallucination before benefit. The successful agents block the channel with kinetics that let physiological signalling escape (memantine) or exploit the dissociative state itself (ketamine).
- The topic spans three therapeutic contexts united by one receptor: (1) dissociative anaesthesia (ketamine, N2O); (2) neurodegeneration/excitotoxicity (memantine in AD, amantadine in PD/dyskinesia); (3) rapid-acting antidepressants (esketamine, dextromethorphan-bupropion).
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Nmda Receptor Antagonists
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