I found a bit about the affinity for different sodium channel states that I was crudely referencing
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2857610/ -
"Eslicarbazepine binds avidly and blocks the inactivated voltage-gated sodium channel (VGSC). The VGSC is the major source of sodium entry when a neuron depolarizes, and consequently allows for the action potential to propagate. VGSCs have 3 states. In the deactivated or resting state, the VGSC is closed, but the channel is responsive to a depolarization signal. When the cell depolarizes, the VGSC opens to allow sodium ion entry. After the action potential, the VGSC enters an inactivated state, in which it is closed and not responsive to voltage changes.
15 Eslicarbazepine binds to the inactivated form of the VGSC and prevents its reversion to the receptive resting or deactivated form.
16,
17 This means that eslicarbazepine binds to more active neurons preferentially. This mechanism is shared by carbamazepine, oxcarbazepine, and other anticonvulsants.
17,
18 The affinity of eslicarbazepine to the inactivated form of the VGSC is similar to that of carbamazepine, but its affinity to the resting form of VGSC is some 3 times less.
12,
17 This suggests that eslicarbazepine is less likely to bind to normally active neurons, and therefore, less likely to cause adverse neurological consequences. Indeed when compared with either carbamazepine or oxcarbazepine, eslicarbazepine had less neurologic impairment in rats,
14 and was less toxic to cultured hippocampal neurons.
19"
So I guess the firing rates of neurons is important in determining what activity is suppressed. Interesting to think about because it makes sense that this would be a good class of drugs for bi-polar, in the sense that if you're manic it will antagonize the cells firing really fast, and if you're depressed it might start to exert more of an inhibitory effect on the GABA interneurons or what have you. I don't know what this means for cells that fire rhythmically. It seems like it would disorient that rhythm. Also, I wonder if sodium channels are somewhat equally expressed across all cell types or if there are certain cells that (through the wisdom of nature) have acquired an abundance of sodium channels (As I recall some degree of sodium channel dysfunction/dysregulation or something is involved in some mental illness).
I think retrograde transmission has to do with gaseous molecules like nitric oxide diffusing from post synaptic to pre synaptic (If I recall correctly somehow CB1 facilitates that). Also just thinking about volume transmission hurts my brain lol
Ho-Chi-Minh, mind if I ask if you were ever on sodium channel antagonists, and if yes did they help normalize you?
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But it is no measure of good health to be well adjusted to a profoundly sick society.