Glutamate is the main excitatory neurotransmitter in the brain. 60-70% of all connections in the brain use glutamate to transfer messages. Glutamate functions to contribute to neural information transfer, ‘rewiring’ of the brain and behavioural state changes.
Glutamte acts upon 4 types of receptor, NMDA, AMPA, Kainate and metabotropic. The main receptors being targeted at the moment for medical conditions are the NMDA and the AMPA, there is evidence to suggest that agonists for either could increase cognitive performance.
The NMDA receptor is a rich new source for future pharmacology. Pscyodelic drugs such as ketamine “special K”, Phencyclidine “angel dust” block this receptor to cause their effect. Just like the receptor GABA (you may know from benzodiazepines (Valium), picamilon, alcohol and the debatable nootropic phenibut which all work here) NMDA (an ion channel) allows electrical charge to enter cells, however it works oppositely instead of inhibiting, causing relaxation, it excites).
NMDA are so called because of their specific activation of N-methyl-D-aspartic acid or NMDA. The amino acid glycine also needs to be present to activate it, it binds at a different site to glutamate. As mentioned the endogenous (already in the body) agonist glutamate activates this receptor. Another endogenously present amino acid, aspartic acid also binds but to a lesser affinity. NMDA was developed as a hybrid, between these two and is unique because it shows selectivity to this receptor over the other 3 (AMPA, Kainate mGlu). NMDA is used as an experimental tool only.
Therefore we have two sites to activate the receptor plus there are another couple of areas on the receptor where we can modulate it, and increase activation.
Agonists at the Glutamate (NMDA) site
L- aspartate
Quinolinate
Homocysterate
Agonists at glycine
D-serine
ACPL
L-alanine
Positive modulators
Polyamin, spermin and spermide like compounds
Magnesium
As mentioned above ketamine like drugs cause a psychotic like state which resembles Schizophrenia. Long term administration leads to pathology in the brain indistinguishable from the disease. Anti schizophrenic drugs are tested on animals treated with such drugs to give them the symptoms. There belief that NMDA together with dopamine are implicated and therefore pharmaceutical companies are developing agonists like the ones mentioned above to activate the receptor. Presently glycine, D-serine, D-alanine and D-cyclosine are being evaluated in clinical trials for what is known as the “negative symptoms” of schizophrenia (withdrawal, flatness, ahedonia (lacking pleasure or interest in previously enjoyed activities), avolition (lacking drive) and most importantly for cognition attention deficit disorder). These symptoms persist in schizophrenic patients after standard therapy which mostly works on the positive (delusions, hallucination, disordered thinking).
I believe that a cognitive enhancing drug is going to come from the AMPA receptor. It is very similar to the NMDA receptor, being activated again by Glutamate. It Modulate rewiring of the brain, more strongly and quicker and is thought to be the receptor which allows us to store our memories by strengthening signal paths. The racetams are thought to act at this receptor, Aniracetam has been shown to alter response at this receptor. One class of agent being tested here for Alzheimer’s is the ampakines, with CX-717 and CX-516.
Besides schizophrenia and Alzheimer’s, drugs targeting this group of receptors are being developed for other conditions including
Epilepsy- Tamapanel, an AMPA antagonists
Parkinsons disease – Ifenprodil – NMDA antagonist
Anxiety – LY354740- metabotropic receptor mGlu5 antagonist
Adiction – ifenprodil
Edited by paul, 11 January 2007 - 12:32 AM.
