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Salvinorin Analogues; Beyond Salvinorin A Options
 
Infundibulum
#1 Posted : 5/22/2009 3:36:24 PM

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Salvinorin A is the active principle in the leaves of the psychotropic mint Salvia divinorum. Salvinorin A is a pharmacologically interesting compound; it is a kappa opioid receptor (KOR) agonist and as such it exerts its effects in a different way compared to the other classical psychedelics that act primarily on serotonin receptors. More intriguing though, it is possibly the first non-nitrogen containing molecule with psychedelic properties. It is not an alkaloid but a diterpene. Despite its unique psychedelic properties and remarkable potency, there have been limited (but thankfully insightful) investigations on its mechanism of action, metabolism and pharmacokinetics.

Here I summarise some important aspect on Salvinorins structure and how their structure affects their action. I also discuss the metabolism of Salvinorin A and how it may be affected by pharmacologican intervention. I also present data on some Salvinorin analogues and finally, I speculate on possible future directions on this very promising field of psychedelic substrances.


Salvinorins: What makes them active or inactive?

As mentioned above, Salvinorin A is a potent KOR agonist. Salvinorin B on the other hand is a very weak KOR agonist and is thought not to have psychedelic qualities. Salvinorin A and B are remarkably similar in structure (see Figure 1). Their difference is the addition of an acetate ester group (shown in red) on the carbon position 2. Technically speaking, Salvinorin A is the acetate ester of Salvinorin B. It has been demonstrated using molecular modeling on receptor-ligand interaction of Salvinorin A and KOR that this acetate ester is critical for their stabilisation of their interaction. Salvinorin B on the other hand lacks this group and it is a very weak KOR agonist.

The dramatic increase in potency brought by by the addition of the acetate ester on the Salvinorin molecule opens up new horizons and creates many questions. To the author's interest lie the putative metabolism of Salvinorin A in the body as well as the potential to synthesize novel analogues of Salvinorin B so as to create active Salvinorins with altered properties.


Uptake and clearance of Salvinorin A.

Salvinorin A is active either by smoking or absorption from the cavity of the mouth. In either case, it produces a short-lived experience which ranges from 5-10 min (when smoked) to almost an hour (when leaves are chewed). Both of these common methods of administration aim at the delivery of Salvinorin from the lungs (smoked) or the mouth cavity (chewed) to the blood from where it can reach the brain and exert its actions.

Salvinorin A is reported to be not orally active. The latter statement is partially true however and Salvinorin has been reported to be orally active but much larger quantities reaching 20-25 times more than smoked need to be ingested.

So, what makes Salvinorin A inactive when taken orally? Or likewise, which mechanism is responsible for the end of the experience after smoking or chewing Salvia leaves? A very recent publication showed that Salvinorin A is rapidly degraded in the blood (see attached abstract from Tsujikawa et al). This group showed that Salvinorin A is degraded to its deacetylated inactive form (which is Salvinorin B) by a group of enzymes called esterases. Using pharmacological intervention using esterase inhibitors they found that sodium fluoride, phenylmethylsulfonyl fluoride and bis-p-nitrophenyl phosphate (all of them are esterase inhibitors) increased markedly the stability of Salvinorin A. A few more experiments showed that the most likely enzyme responsible for the deacetylation of Salvinorin A is a carboxylesterase.

The same group also identified another degradation product of Salvinorin A in the blood. This by-product had a lactone-open ring and this is most likely due to the action of a lactonase enzyme. The degradation pathways of Salvinorin A are summarised in Figure 2.

Degradation of Salvinorin A to B and/or destruction of its lactone ring has also been suggested to be the likely mechanism that marks the end of its action on the body. The (not mutually exclusive) KOR receptor desensitisation, also known as tolerance building, is another plausible mechanism that may account for the end of Salvinorin A's effects. There are not enough data to support the latter however. On the contrary, synthetic Salvinorin analogues that have the ability to bind and activate the KOR receptor but cannot be hydrolysed by carboxylesterases have longer-lasting action. This suggests that deacetylation of Salvinorin a to B is the prime mechanism that limits its action.


Salvia divinorum analogues

There have been research groups that have managed to synthesise analogues of Salvinorin A. The interest in synthesizing synthetic analogues is manifold; analogues can be much more potent, more longer-lasting, more specific, more stable and they can have different qualities (e.g. they can block KOR instead of activating it). For a not exhaustive list of Salvinorin analogues see the attached paper from Beguin et al.

The most interesting Salvinorinn analogues are the ones that have substitution on the C2 carbon of Salvinorin B, i.e. the substitutions that confer binding of Salvinorins on the KOR receptor and/or remove the carboxyesterase-sensitive acetate ester. The compounds 2-Methoxymethyl-Salvinorin B, N-methylpropionamide Salvinorin B and N-methylacetamide Salvinorin B (Fig 3) are the most promising and their properties, differences and structures will be discussed below:

2-Methoxymethyl-Salvinorin B (MOM)

This compound is similar to Salvinorin A but has a methoxymethyl ether group instead of an acetate ester bond. It is reported to have a 3-fold higher affinity on the human KOR receptor compared to Salvinorin A and is therefore more potent than Salvinorin A. Intraperitoneal injection of this compound in mice and rats has shown 5- to 6-fold duration of the experience. The much longer lasting effects are thought to be a result of the inability of carboxylesterases to degrade MOM to the inactive Salvinorin B. There have not been reports of its effects in humans. For more information see the paper from Wang et al attached below.

N-methylpropionamide Salvinorin B (MPA)]


Synthesis of this compound involves conversion of Salvinorin B to its derivative n-methyl amine and then forming an amide bond this n-methyl amine derivative and proprionic acid. The result is actually a Salvinorin analogue that also contains a nitrogen atom, which technically speaking makes it an alkaloid. In contrast to MOM, MPA is not more potent than Salvinorin, it is however 10 times longer active than Salvinorin A. Again, its much longer-lasting action is thought to be due to the inability of the carboxylesterases to attack the molecule. There have not been tests of this compound in humans.

N-methylacetamide Salvinorin B (MNA)

Almost just like MPA, MNA is the amide formed by the reaction of an n-methyl amine derivative of Salvinorin B and acetic acid. Its action is very similar in many respects to MPA; it is no more potent than Salvinorin A and it lasts around 6 times as much as Salvinorin A. The most interesting fact about this compound is that contrary to MOM and MPA, it is orally active (at least in rats). Again, there have not been tests of this compound in humans. For more information on both MPA and MNA see the paper from Beguin et al, attached below.

The fact that MNA is orally active whereas MOM and MPA are not is intriguing. There is at least another enzyme that metabolises Salvinorins. Lactonase has been shown to degrade Salvinorins (Tsujikawa et al) in the blood. I speculate that a lactonase enzyme also degrades Salvinorins in the digestive tract. In this respect, MNA may be a very poor substrate or even inhibitor of this enzyme.


The Future of Psychedelic Research on Salvinorins.

The researrch on Salvinorin analogues is still in its infancy and there are still many uncharted areas. Research groups have managed to alter the chemical structure of Salvinorins found in S.divinorum to create compounds that are more potent, longer lasting and with expanded administration routes compared to Salvinorin A. This can be thought analogous to the development of LSD from lysergic derivatives of ergot alkaloids. It is very unfortunate that no reports can be found on the use of these novel Salvinorin analogues in humans. I feel that some day people will approach these (and future) compound and will be able to appreciate whether these compounds have different/better/worse/more insightful/less insightful etc. qualities than Salvinorin A.

More importantly though, Salvinorin analogues are (and will continue to to be) useful tools in the investigation of the mechanism of action and metabolism of Salvinorin A. Should we reach the equivalent level of understanding we currently have for the MAO system and psychedelic tryptamines, we may be able to prepare plant or pharmacological admixtures to the current S.divinorum preparations so as to control or direct the effects of Salvinorin A. In theory therefore, we could get to control the qualities of the Salvinorin A experience (e.g. make it more/less visual, more/less weird, more recreational, more insightful etc). Even the possibility of orally administering S.divinorum is open if in theory it is combined with certain esterases.



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jamie
#2 Posted : 5/23/2009 6:05:50 PM

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wow..good post man! I REALLY like salvia and have been getting into the possability of one day experimenting with other salvinorin A analogues...would be cool to see them available somewhere for research or something..
Long live the unwoke.
 
Infundibulum
#3 Posted : 5/23/2009 7:42:34 PM

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Thanks, SWIM loves Salvinorin A (he usually smokes it pure) and he believes that Salvinorins andtheir analogues have a great potential. SWIM even think that some of the Salvinorin analogues may appeal more to people who do not usually like the effects of salvia/salvinorin A!

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soulfood
#4 Posted : 5/23/2009 8:21:47 PM

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I would be head over heels in love with a form of salvia that didn't have that feeling of irrational guilt I get from salvorin A.

Or perhaps a form of salvorin that could be smoked and had a more gradual and less weird onset.

Ooh possibilities!


Edit: Just realised reading back that it's actually "salvinorin" and all this time I've called it salvorin... yeh
 
Infundibulum
#5 Posted : 5/24/2009 4:10:43 PM

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Yeah, it is also sad that the current Salvinorin analogues have not been tested in humans. Or at least there are no testimonies of people who have tried them. Animal studies are useful for characterising their pharmacokinetics but SWIM believes that testing of these compounds on humans is imperative.

Even though theoretically Salvinorin A and all of its analogues exert their effects by binding and activating the KOR receptor there is no reason to assume that their experience is going to be qualitative the same!

SWIM believes that it is a matter of time (not too soon however!) before RC vendors start distributing them!

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jamie
#6 Posted : 5/25/2009 9:40:36 PM

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..It dissapointing how this amazing plant is for the most part, unapreciated within the mainsteam entheogenic community..you see ayahuasca conferances and tourism, churches popping up everywhere, lots of talk about ibogaine and peyote etc..but it's almost like noone wants to touch the sage..there are a few but for the most part I think people dont even know where to begin..it takes(or did for me anyway) lots of dedication to begin to figure out this plant(if possible) and what it is capable of/how you are capable of working with it..I have this feeling that her time here hasn't really even come yet..
Long live the unwoke.
 
'Coatl
#7 Posted : 5/28/2009 7:39:38 AM

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Very, very interesting!

Thank you for posting.

Quote:

There have been research groups that have managed to synthesise analogues of Salvinorin A. The interest in synthesizing synthetic analogues is manifold; analogues can be much more potent, more longer-lasting, more specific, more stable and they can have different qualities (e.g. they can block KOR instead of activating it). For a not exhaustive list of Salvinorin analogues see the attached paper from Beguin et al.


So they synthetically created natural organic compounds or modified inorganic analogs? Sorry, but this stuff is over my head, I'm not a chemistry girl, I may need some clarification if you don't mind. I'm doing my best to learn.

Basically I just wanna know if these "analogues" occur in Salvia divinorum or not.

Could you please link me to the full list of compounds that Salvia divinorum contains and it's analogues, please?

WARNING: DO NOT INGEST ANY BOTANICAL WHICH YOU HAVE NOT FULLY RESEARCHED AND CORRECTLY IDENTIFIED!!!

I am Teotzlcoatl, older cousin of Quetzalcoatl. My most famous physical incarnation was Nezahualcoyotl, but I have taken many forms since the dawn of the cosmos. In this realm I manifest as multiple entities at a single time. I am many, I am numbered. I am few, but more than one. I am a multifaceted being, a winged serpent with many heads. We are Teotzlcoatl.

"We Are The One's We've Been Waiting For" - Hopi Proverb
 
Infundibulum
#8 Posted : 5/28/2009 9:50:30 AM

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These novel analogues are synthetic (or semi-synthetic, whichever way you like). They are for Salvinorin A exactly what LSD is for LSA.

The precursors are provided by the plant. The novel modifications are the result of man's action.

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'Coatl
#9 Posted : 5/28/2009 5:26:54 PM

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Ok that is what I thought you meant.

There are other compounds present in Salvia divinorum besides Salvinorin A and Salvinorin B, correct? If so... can you give me a list of them?

WARNING: DO NOT INGEST ANY BOTANICAL WHICH YOU HAVE NOT FULLY RESEARCHED AND CORRECTLY IDENTIFIED!!!

I am Teotzlcoatl, older cousin of Quetzalcoatl. My most famous physical incarnation was Nezahualcoyotl, but I have taken many forms since the dawn of the cosmos. In this realm I manifest as multiple entities at a single time. I am many, I am numbered. I am few, but more than one. I am a multifaceted being, a winged serpent with many heads. We are Teotzlcoatl.

"We Are The One's We've Been Waiting For" - Hopi Proverb
 
ComaProphet
#10 Posted : 5/31/2009 5:56:40 PM

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Awesome post man! Thank you.
Meditation to cure Depression.

What It Will Do for You

This meditation totally recharges you.
It is an antidote to depression. It builds a new system, gives you the capacity and caliber to deal with life, and gives you a direct relationship with your pranic body.
How to Do It
Sit with a straight spine in easy pose. Arms are extended straight out in front of you, parallel to the ground. Close your right hand into a fist. Wrap your left fingers around it. The bases of the palms touch. The thumbs are close together and are pulled straight up. The eyes are focused on the thumbs.
Now inhale for 5 seconds (do not hold the breath in); exhale for 5 seconds; hold the breath out for 15 seconds. Continue.
Start with 3 - 5 minutes and work up to 11 minutes. Build up the time slowly.
In time, you can work up to holding the breath out for 1 full minute.
 
SWIMfriend
#11 Posted : 5/31/2009 6:06:10 PM

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'Coatl wrote:
...So they synthetically created natural organic compounds or modified inorganic analogs?...


The first organic compound to be synthesized (urea) was made in the EARLY 1800's. There is ZERO difference between an organic molecule synthesized in a lab, or synthesized in a cell.
 
'Coatl
#12 Posted : 5/31/2009 6:58:26 PM

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I know that.

I was just asking what organic compounds occur in Salvia divinorum besides Salvinorin A and Salvinorin B.
WARNING: DO NOT INGEST ANY BOTANICAL WHICH YOU HAVE NOT FULLY RESEARCHED AND CORRECTLY IDENTIFIED!!!

I am Teotzlcoatl, older cousin of Quetzalcoatl. My most famous physical incarnation was Nezahualcoyotl, but I have taken many forms since the dawn of the cosmos. In this realm I manifest as multiple entities at a single time. I am many, I am numbered. I am few, but more than one. I am a multifaceted being, a winged serpent with many heads. We are Teotzlcoatl.

"We Are The One's We've Been Waiting For" - Hopi Proverb
 
jamie
#13 Posted : 5/31/2009 11:27:51 PM

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I doubt there is any other active molecule in salvia when fresh..if thats what you mean coatl..I have tried salvia many times fresh and dried and I did not notice any diff..its beautiful either way. Others seem to have diff experiences when fresh as compared to dry, s who knows?..maybe there is still unknown actives present.
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69ron
#14 Posted : 5/31/2009 11:33:56 PM

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For SWIM fresh leaves picked and used as a quid immediately are very different from dried ones, or leaves a few hours old. The difference for him is enough so that it feels like a different drug. SWIM had the so called "palatable clone", so maybe that made a difference.

I'm sure there's something active in the fresh leaves of the clone he had that decomposes within hours after picking the leaves. Even refrigerating them doesn’t preserve it. It’s likely oxidizing rapidly after being picked.
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jamie
#15 Posted : 6/1/2009 7:33:29 PM

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hmm, thats interesting...I have never taken a large dose right off of the plant..usually it does sit in the fridge for at least an hour or more...I have used very small quids right after the leaves were picked, and had really euphoric experiences..but never tested out a full dose that way. Looks like I need to experiment a bit this summer when I take cuttings..

how would you're swim say the experience differes from older leaf? Are the visual and tactile sensations different?..more light in the experience?
Long live the unwoke.
 
'Coatl
#16 Posted : 6/1/2009 7:46:11 PM

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I'm with 69ron! Using fresh leafs as a quid is like a whole different psychoactive compared to smoking!
WARNING: DO NOT INGEST ANY BOTANICAL WHICH YOU HAVE NOT FULLY RESEARCHED AND CORRECTLY IDENTIFIED!!!

I am Teotzlcoatl, older cousin of Quetzalcoatl. My most famous physical incarnation was Nezahualcoyotl, but I have taken many forms since the dawn of the cosmos. In this realm I manifest as multiple entities at a single time. I am many, I am numbered. I am few, but more than one. I am a multifaceted being, a winged serpent with many heads. We are Teotzlcoatl.

"We Are The One's We've Been Waiting For" - Hopi Proverb
 
69ron
#17 Posted : 6/1/2009 8:40:56 PM

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fractal enchantment wrote:
hmm, thats interesting...I have never taken a large dose right off of the plant..usually it does sit in the fridge for at least an hour or more...I have used very small quids right after the leaves were picked, and had really euphoric experiences..but never tested out a full dose that way. Looks like I need to experiment a bit this summer when I take cuttings..

how would you're swim say the experience differes from older leaf? Are the visual and tactile sensations different?..more light in the experience?


It's almost like a mushroom trip when fresh leaves are used as a quid. Also VERY EUPHORIC. It's almost a completely different experience. I've heard that apparently the strain of Salvia makes a difference too. SWIM used the so called “palatable clone” grown in his house and used the leaves right off the plant without letting them sit even for a few minutes. The fresher the better. They lose their mushroom-like effects rapidly and become sort of unpleasant after a while, but are still “active”, just not enjoyable for SWIM.
You may remember me as 69Ron. I was suspended years ago for selling bunk products under false pretenses. I try to sneak back from time to time under different names, but unfortunately, the moderators of the DMT-Nexus are infinitely smarter than I am.

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burnt
#18 Posted : 6/1/2009 9:22:45 PM

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There are many reasons why smoking salvia can be different then chewing it. One is metabolism of the active substance. When you eat stuff it usually goes into your liver and can potentially be converted. Conversions can also happen in the gut. Two is what active substances are actually being injested which will differ depending how its taken.

Also its very likely that salvia contains other diterpenoids similar to salvinorin A and B just because of the way these molecules are biosynthesized. Infact there can be really no doubt that other diterpenoids with a similar skeleton are in the plant. However they are most likely present in low amounts so either they are not discussed or no one has isolated them. They could also be unstable intermediates.

SWIM has an interesting paper about separating salvinorin A using centrifugal partition chromatography. CPC is an awesome technique for natural products isolation. Salvinorins are now interesting to medicinal chemistry because of there selectivity on the K-opiod receptor and contain no nitrogen. Some claim they may be useful for alzheimers although there are other potenials here too.

SWIM never chewed salvia but has smoked it a few times. SWIM never enjoyed smoking it on its own. It was always unpleasant. But using it with LSD and other dissociatives was very enjoyable and intense.
 
69ron
#19 Posted : 6/1/2009 9:45:25 PM

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Well, the fresh leaves from the “palatable clone” SWIM had lost their mushroom-like effects within a few hours after being picked, so how would one go about testing for such unstable compounds? It seems to me that by the time you grind the leaves and do an extraction for testing, these unstable compounds would likely be lost.

These unstable compounds are likely oxidizing rapidly, much the way an apple or avocado does after being pealed and left out in the air.
You may remember me as 69Ron. I was suspended years ago for selling bunk products under false pretenses. I try to sneak back from time to time under different names, but unfortunately, the moderators of the DMT-Nexus are infinitely smarter than I am.

If you see me at the waterpark, please say hello. I'll be the delusional 50 something in the American flag Speedo, oiling up his monster guns while responding to imaginary requests for selfies from invisible teenage girls.
 
'Coatl
#20 Posted : 6/2/2009 12:58:42 AM

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Quote:
Also its very likely that salvia contains other diterpenoids similar to salvinorin A and B just because of the way these molecules are biosynthesized. Infact there can be really no doubt that other diterpenoids with a similar skeleton are in the plant.


THAT is what I am interested in... does anybody have a FULL list of the compounds in Salvia divinorum?
WARNING: DO NOT INGEST ANY BOTANICAL WHICH YOU HAVE NOT FULLY RESEARCHED AND CORRECTLY IDENTIFIED!!!

I am Teotzlcoatl, older cousin of Quetzalcoatl. My most famous physical incarnation was Nezahualcoyotl, but I have taken many forms since the dawn of the cosmos. In this realm I manifest as multiple entities at a single time. I am many, I am numbered. I am few, but more than one. I am a multifaceted being, a winged serpent with many heads. We are Teotzlcoatl.

"We Are The One's We've Been Waiting For" - Hopi Proverb
 
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