Recall that Memantine (alzheimer's drug) is a NMDA Receptor Antagonist that helps prevent excitotoxcity by Blocking Ca2+ entry. That's how I remember this.
So, for some reason, neurotransmitters is something I've ALWAYS struggled with... probably because I wasn't taught it well so never really learned it, just learned enough for whatever exam. I just found this boo through NCBI and its FANTASTIC! It's from 2001 so might be old, but it was great. You can search through the book and find the chapters. I pretty much just went through all of the neurotransmitter chapter. https://www.ncbi.nlm.nih.gov/books/NBK10799/
My main take-aways:
Glutamate = major excitatory neurotransmitter. Two types of receptors:
1) metabotropic, most of which are presynaptic Gi which leads to decreased NMDA receptor activity and risk of exocitotixicity, or postsynaptic Gq receptors that lead to increase Na+, K+, and decreased glutamate causes depolarization and increased Mg++ displacement and NMDA receptor activity and risk of exocitotxicity, and
2) ionotropic channels including NMDA and AMPA/kainate channels, which all allow nonspecific cation influx, but only NMDA allows Ca++ influx (and only in a voltage dependent manner after sufficient depolarization has displaced the inhibitor Mg++ ion in the channel).
GABA and glycine = inhibitory neurotransmitters.
1) GABA-A and GABA-C = ionotropic channels that lead to eflux of Cl-, and despite this causing depolarization, the neuron still stays below resting potential. GABA-A binding site for barbiturates, steroids, GABA, and picrotoxin = inside pore of channel. GABA-A binding site of benzodiazepines = outside of pore of channel.
2) Glycine channel is a very similar Cl- eflux channel.
3) GABA-B is a metabotropic channel that activates Gi leading to decreased cAMP which activates efflux K+ channels and inhibits Ca++ influx channels leading to hyperpolarization.
Biogenic amines = catecholamines dopamine (coordination of body movement, reward, motivation, reinforcement), norepinephrine (sleep, wakefulness, attention, feeding behavior, epinephrine (lowest concentration in CNS), plus serotonin (sleep, wakefulness, depression, anxiety, nausea) and histamine (arousal, attention, allergy, tissue damage, and may influence blood brain flow). Obviously, all of this is in addition to adrenergic neurotransmission and flight, fright, and fight response.
ATP and other purines = excitatory transmission, co-released with other small-molecule neurotransmitters. Adenosine isn't classically considered a neurotransmitter because it isn't stored/released in Ca++ dependent manner, but derived from ATP before having an excitatory potential.
Acetylcholine = major neurotransmitter involved in neurotransmission via muscarin and nicotinic receptors.
Peptide neurotransmitters = commonly released as propeptide larger precursors that are cleaved by specific enzymes that were in the same neurotransmitter vesicle upon release. Five types = brain/gut peptides, opioid peptides, pituitary peptids, hypothalamic releasing hormones, and those not classified. Examples = precursor that gives rise to substance P (hippocampus, neocortex, and GIT and released from small diameter PNS C fibers that transmit pain and temperature information, powerful hypotensive, inhibited by opioid peptides), neurokinin A, neuropeptide K, and neuropeptide gamma, and opioid peptides including plant alkaloids (like morphine), synthetic opioid derivatives, and endorphins, dynorphins, and enkephalins. In general opioid peptides are depressants (i.e. analgesia mechanism), involved in complex behaviors (sexual attraction, aggressive/submissive behaviors), and implicated (though not definitive) in psychiatric disorders.
Overall, neurotransmitters = type types: small-molecule transmitters and neuropeptides, where small-molecules transmitters are faster and mediate rapid synaptic transmission (i.e. androgen SNS fight/flight/fright quick response), where as neuropeptides (along with biologic amines and some small molecule transmitters) are slower and mediate gradual, prolonged neurotransmission.
Some pictures: http://tmedweb.tulane.edu/pharmwiki/doku.php/overview_of_cns_neurotransmitters, https://www.semanticscholar.org/paper/Targeting-GABAB-receptors-for-anti-abuse-drug-Phillips-Reed/a049643bb25c8631e0267a40182e6d310d1f31fb/figure/0, and https://www.bluelight.org/xf/threads/difference-between-gaba-a-and-gaba-b.733916/#lg=_xfUid-1-1562540128&slide=0
NMDA receptors in this case are being used for long term potentiation within the brain and out of all of there choices only this receptor uses Ca+
I picked NMDA because it’s stimulatory, but is there any deeper reason for this?
all the others a noncompetitive since they have specificity(specific ligands), NMDA is the only nonselective(hence competitive receptor), has a ligand site and ca , na and mg...hence competitive