specialspack said:Serotonin syndrome is due to an excess of serotoninin the interneuronal space. Excess tryptophan can cause it, but the most common cause is the combination of drugs which block the removal of serotonin from the interneuronal space.
So when you said:
Nope.. if you take a non-selective or MAO-A inhibitor with MDMA, the serotonin will be massively released, and then not broken down -> serotonin syndrome. It won't affect your comedown (if you survive) - the serotonin will all have been released from your neurons and (eventually) depleted. MDMA blocks the re-uptake too, so non will be re-uptaken into the cells.
Again, no. 1. There will still be a post-E serotonin dip as you have excreted a large amount of serotonin by taking MDMA, which has not been re-uptaken.
2. The theory of neurotoxicity caused by the uptake of dopamine into the serotonin neurons has been pretty much discarded - http://thedea.org/neurotoxicity.html#m you're half right though - l-deprynl (selective MAO-B inhibitor at low doses) provides neuroprotection - http://mdma.net/depsave.htm but I'm not sure what the suggested mechanism is now?
That's why I thought you might not really know what you were talking about... MDMA with any strong non-selective or MAO-A inhibitor is potentially fatal, and would provide non of the benefits you suggest. MAO-B inhibitors may provide some neuroprotection, but won't enhance the effects (or at least, the anecdotal evidence seems to be mixed at best).*
As for the meth/4-mar, I really have no idea...
*All this is simply my amateur understanding, if anyone wants to correct anything I've said which is incorrect, please do so.
Well if you inhibit MAO, then you don't need to release as much serotonin as the levels would be naturally higher, and so depletion wouldn't be as significant. Also the serotonin wouldn't be oxidized during/after the E.
