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why & how are you measuring doses of DMT low enough to give leave you still functioning and not hanging out here:
Edited by ajnast4r, 21 May 2010 - 05:45 PM.
Posted 21 May 2010 - 05:43 PM
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Edited by ajnast4r, 21 May 2010 - 05:45 PM.
Posted 21 May 2010 - 05:55 PM
That isnt true, DMT is actually known for its lack of tolerance, altough tolerance barely (if ever) occurs to low doses of psychedelics.My only reserve with DMT, is as it binds to the receptors (LD) it creates a very dreary depressant feeling(in me), until 4.5 hours comes along and all the natural serotonin built-up comes to swarm the receptors and then I'm super-happy, and plus, DMT has that switch that protects daily usage, right? That melatonergic or tryptaminergic switch or whatever it is that prevents daily dosing, can't remember the specifics, but know daily tryptaminergics usually don't work. Could be wrong, but, there's a stop-switch mechanism on DMT I know.
Posted 21 May 2010 - 05:56 PM
lol, i'm took like 1/10th of my mimosa hostilis extract this morning, now took 2/10th, slowly going up...
why & how are you measuring doses of DMT low enough to give leave you still functioning and not hanging out here:
Posted 21 May 2010 - 09:50 PM
That isnt true, DMT is actually known for its lack of tolerance, altough tolerance barely (if ever) occurs to low doses of psychedelics.My only reserve with DMT, is as it binds to the receptors (LD) it creates a very dreary depressant feeling(in me), until 4.5 hours comes along and all the natural serotonin built-up comes to swarm the receptors and then I'm super-happy, and plus, DMT has that switch that protects daily usage, right? That melatonergic or tryptaminergic switch or whatever it is that prevents daily dosing, can't remember the specifics, but know daily tryptaminergics usually don't work. Could be wrong, but, there's a stop-switch mechanism on DMT I know.
Posted 25 May 2010 - 06:10 AM
Posted 25 May 2010 - 09:57 AM
1. Yes but i dont think that is a problem, quite the opposite.A few people here are clearly a lot better read in this area than I am, but here are some simplistic propositions that I have developed (ignoring downstream effects, nb):
1. 5HT2 agonism of some sort is a required feature of most of these substances.
2. Downregulation often occurs rapidly (ie, if someone is enough of a desperado to want to try for a second helping, the subsequent experience will be greatly attenuated). This presumably has implications for tolerance development.
3. Euphoria during the tryptamine experience is a bit of a hit and miss affair; however, day-after mood elevation seems to be better documented. PEAs, which started off as the topic of this thread, are obviously a completely different kettle of fish.
4. Some anti-depressants are specifically based upon 5HT2 antagonism, not agonism.
5. Kappa opioid antagonism can also result in an anti-depressant action. So, no get-out clause for salvinorin either.
Conclusion (highly simplistic, like I said): seeing things doesn't make anyone feel any better, but the aftermath might. Whether this has implications for chronic administration of stimulating PEAs is another matter.
Posted 25 May 2010 - 10:07 AM
These are DMT's affinities:That isnt true, DMT is actually known for its lack of tolerance, altough tolerance barely (if ever) occurs to low doses of psychedelics.My only reserve with DMT, is as it binds to the receptors (LD) it creates a very dreary depressant feeling(in me), until 4.5 hours comes along and all the natural serotonin built-up comes to swarm the receptors and then I'm super-happy, and plus, DMT has that switch that protects daily usage, right? That melatonergic or tryptaminergic switch or whatever it is that prevents daily dosing, can't remember the specifics, but know daily tryptaminergics usually don't work. Could be wrong, but, there's a stop-switch mechanism on DMT I know.
Possibly, but from my knowledge on DMT HD from my experiences in 2003; it has a mechanistic swithoff effect, and I commend you on your source! Mimosa Hostilis rootbark is probably the best source for it, but that is one I've LD'd and HD'd, and I'm telling you DMT has some negative perception qualities to it LD. (perhaps animal, or whoever can step in here and list the 5ht binding affinities?)
If it works for you though, nice bro, and if you ever decide to try the DOC path - I've got just the chickety to talk to, to help you on this quest.
Yes, I agree with the poster that wondering how in the living fuck are you taking DMT and still able to function normally? IN HD limits you are a vegetable, same with MD, but LD I was able to walk around fine but I was in a negative mood - same thing Shulgin experienced. Still, best of luck!
DMT: 4.00 5ht7, 3.97 5ht1d, 3.91 5ht2b, 3.53 Alpha2B, 3.53 Alpha2C, 3.51 D1, 3.42 5ht2c, 3.28 5ht1e, 3.25 5ht6, 3.16 5ht5a, 3.13 Imidazoline1, 2.95 Alpha1B, 2.75 Alpha2A, 2.70 Alpha1A, 2.58 5ht2a, 2.37 SERT, 2.23 Sigma1; 0.00: 5ht1a, D4, D5, Beta1, D2, D3, DAT, NET, 5ht1b, Beta2, Sigma2, CB2, KOR, Ca+Channel, M1, M2, M3, M4, M5, H2, CB1; ND: H1, DOR, MOR, NMDA
Edited by medievil, 25 May 2010 - 10:08 AM.
Posted 11 March 2013 - 11:37 AM
Edited by medievil, 11 March 2013 - 11:40 AM.
Posted 11 March 2013 - 04:24 PM
Posted 11 March 2013 - 04:44 PM
Posted 11 March 2013 - 05:29 PM
Posted 11 March 2013 - 05:37 PM
Posted 11 March 2013 - 07:02 PM
Posted 11 March 2013 - 07:24 PM
Posted 12 March 2013 - 10:10 PM
Edited by SpawnMoreOverlords, 12 March 2013 - 10:34 PM.
Posted 13 March 2013 - 02:30 AM
Posted 13 March 2013 - 03:46 AM
Posted 13 March 2013 - 04:18 AM
Posted 13 March 2013 - 11:13 PM
Get ready for the "Broke my brain now you tell me how to fix it again" threads.
Edited by SpawnMoreOverlords, 13 March 2013 - 11:19 PM.
Posted 14 March 2013 - 12:59 AM
I would love to try Ayahuasca. I can get the ingredients and have a few recipes. Just seems such a pain in the ass to make. I've never been able to get hold of DMT :(
Posted 28 April 2014 - 04:42 AM
http://www.ncbi.nlm....pubmed/23638910
beta-phenethylamine--a phenylalanine derivative in brain--contributes to oxidative stress by inhibiting mitochondrial complexes and DT-diaphorase: an in silico study.
Mazumder MK1, Paul R, Borah A. AIM:
Till date, the mode of action of ?-PEA on neurons is not well illustrated. We tested the hypothesis that ?-PEA has the ability to cause oxidative stress by inhibiting the antioxidant enzyme DT-diaphorase and mitochondrial complexes (Complex-I and complex-III).
METHODS:
Using molecular docking as a tool, we here studied and compared the inhibitory capacity of beta-PEA on DT-diaphorase and mitochondrial complexes. Three-dimensional structures of mitochondrial complexes and DT-diaphorase and their ligands were downloaded from the respective data banks, and free energy of binding (docking scores) were determined.
RESULTS:
The present finding demonstrated for the first time that ?-PEA potentiates reactive oxygen species generation by inhibiting the antioxidant enzyme DT-diaphorase, in addition to the mitochondrial complex-I and complex-III.
CONCLUSION:
As lowering of cellular antioxidant molecules is evident in many neurodegenerative disorders, beta-PEA-induced lowering of DT-diaphorase activity may have the capability to cause neurodegeneration, which may be potentiated by its ability to inhibit mitochondrial complexes. Thus, beta-PEA due to its cumulative actions may be more potent in causing neurodegeneration as compared to other endogenous neurotoxins.
Posted 15 June 2015 - 03:09 AM
http://www.ncbi.nlm....pubmed/23638910
beta-phenethylamine--a phenylalanine derivative in brain--contributes to oxidative stress by inhibiting mitochondrial complexes and DT-diaphorase: an in silico study.
Mazumder MK1, Paul R, Borah A. AIM:
Till date, the mode of action of ?-PEA on neurons is not well illustrated. We tested the hypothesis that ?-PEA has the ability to cause oxidative stress by inhibiting the antioxidant enzyme DT-diaphorase and mitochondrial complexes (Complex-I and complex-III).
METHODS:
Using molecular docking as a tool, we here studied and compared the inhibitory capacity of beta-PEA on DT-diaphorase and mitochondrial complexes. Three-dimensional structures of mitochondrial complexes and DT-diaphorase and their ligands were downloaded from the respective data banks, and free energy of binding (docking scores) were determined.
RESULTS:
The present finding demonstrated for the first time that ?-PEA potentiates reactive oxygen species generation by inhibiting the antioxidant enzyme DT-diaphorase, in addition to the mitochondrial complex-I and complex-III.
CONCLUSION:
As lowering of cellular antioxidant molecules is evident in many neurodegenerative disorders, beta-PEA-induced lowering of DT-diaphorase activity may have the capability to cause neurodegeneration, which may be potentiated by its ability to inhibit mitochondrial complexes. Thus, beta-PEA due to its cumulative actions may be more potent in causing neurodegeneration as compared to other endogenous neurotoxins.
Oh yes. reactive oxygen species. this is stuff like molecular degeneration such as when mitochondria's electric transport chain is doing its thing such as metabolizing a hydoxal lipid for energy source and as a result a by product is created such as peroxide (H2O2). Now this peroxide is a free radical that has to be dealt with. more likely, it'll be dealt with by the mito's process of hydrolyzation. But for some reason, if the mito is to taxed out or its due to having some age on you, this hydrolyzation isn't gonna take place either at all or as effiencently as it should. What's gonna happen is this H2O2 will be food for reactive oxygen species to grow! The study I quoted above is saying that more than likely PEA interferes with things like H2O2 free radicals being dealt with, thus potentiating reactive oxygen species development. If this is the case, I will tell you that trimethylglycine (betaine) will help with peroxidation by products and another supplement by the name of PQQ will help combat against reactive oxygen species through the process of reducing Glutathione (when I say reducing, it doesn't mean diminish, its more of a meaning of restoring a already defeated/useless antioxidant that at one time was usefull before it was rendered of its benefits) so Glutathione may do its job by kicking some reactive oxygen species butt. So there you have it; on account of this articles study of PEA causing neurodegenerative disorders due to those bastard reactive oxygen species, just take ya one or both of the supplements I mentioned. Thats all.
Posted 15 June 2015 - 10:34 AM
Found this, its according to them far safer than amphetamines:
β-phenylethylamine, a small molecule with a large impact
PEA has been suggested as a ‘safe’ alternative to drugs, such as amphetamine or methylphenidate, which are accompanied by many undesirable side effects
http://www.ncbi.nlm....les/PMC3904499/
I just didnt know how problematic are the effects on the mitochondria.
Posted 15 June 2015 - 09:34 PM
PEA alone should be fairly inactive when taken orally because it is broken down quickly which is probably similar to taking DMT orally.
There should be hardly any effect from it. Is your article talking about endogenous phenetylamine?
Back to my microdose experiences which are from a while ago:
2C-D - I really really doubt this makes you smart. The only reason people think that is because a test person in Shulgin's book reported "I felt I could learn faster" or something to that effect.
What is possible with microdosing many psychedelics is in my oppinion getting into a flow state easier. With 2C-D this happens to be 5mg whereas a normal dose would be closer to 30mg (which makes you too altered for work) and getting a full trip with this is really hard dosage wise I would look elsewhere for that.
Some people mentioned using it as pre-workout on bluelight. I would say this makes running easier and the urge to stop excercise is reduced. So it can feel mildly stimulating and keep you in the flow easier (running trance or how you want to call it)
Posted 15 June 2015 - 09:47 PM
It looks to me that the supplemental form is discussed. Its brocken down to something active (opioids or something).
However it worked to me without any mao inhibitors: I was horny as fuck, anxious, high bloodpressure/vasoconstriction and pushed
but the effect decreased after a while if I remember correctly. Got depressed in the meantime and since then, it doesnt work at all.
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