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N&PD Moderators: Skorpio | someguyontheinternet
Acid, dragonflies and the 5HT2A receptor
- Thread starter fastandbulbous
- Start date
fastandbulbous
Bluelight Crew
I had to limit my gallery. If you PM me with an e-mail address, I'll send you the associated diagrams/figures
Let's refresh the good old thread.
Is anybody out there who heard about furano-tryptamines?
Things like shulgin's inactive MDO-tryptamines with only one oxygen, either on 4- or the 5-position. From the 5-position there are two regioisomers possible: one tying the 5-membered ring from 5 to 4 and one from 5 to 6.
Is it possible that they are active or can one assume them inactive, when the MDO's are inactive?
Is anybody out there who heard about furano-tryptamines?
Things like shulgin's inactive MDO-tryptamines with only one oxygen, either on 4- or the 5-position. From the 5-position there are two regioisomers possible: one tying the 5-membered ring from 5 to 4 and one from 5 to 6.
Is it possible that they are active or can one assume them inactive, when the MDO's are inactive?
LuxEtVeritas
Bluelighter
^ The MDO-Trypts are not inactive that I am aware, though certainly have scant testing
notably 4,5-MDO-DIPT was in TiHKaL assay noted at 25mg after a 3hr post-consumption lull by this " I was reminded very much of LSD"
notably 4,5-MDO-DIPT was in TiHKaL assay noted at 25mg after a 3hr post-consumption lull by this " I was reminded very much of LSD"
fastandbulbous
Bluelight Crew
Original figures/diagrams restored to article
LuxEtVeritas
Bluelighter
fastandbulbous said:
looking at figure 4 what would one hypothesize a b-methoxy-DOM would be dosed at?
perhaps 2-fold as potent? (bMeO-2CD is 2-fold as potent as 2CD in the figure)
this also goes back to my speculation in a recent thread that concerned potential more potent 'bk-MDMA' type structures to thwart UK laws to look at a beta-methoxy-MDMA (bMeO-MDMA or Methoxylone [first coined here and possibly first 'suppositioned', LOL] )
oh and nice on having those diagrams back..thanks Fnb!
IGNVS
Bluelighter
I didn't mean to rule out that the above molecule will be active. What I meant to say is: there's only one way to find out if it is active as predicted: make it and test it. Since 3-chloropropionyl chloride is commercially available it would be an easy task to make this compound.
Another idea not related to this structure is to use the same rigid pyrrolidinylmethyl sidechain in PEAs which has proven to bring maximum potency to tryptamines:
The 4-OH-indole derivative is the most potent 'tryptamine', in rat drug discrimination equipotent with DOI and about 1/10 of LSD. It would be interesting to know how the activity of PEAs responds to this modification.
did you ever find out more about this?
fastandbulbous
Bluelight Crew
Going back to the issue of how altering the alkyl substitution of the amide group of LSD causes a big drop in potency, is there any info as to the activity of the amide of 2,5-dimethylpyrrolidine. It's that the azetadine amide (2,4-dimethylazetidine) is as active as LSD although I'm uncertain it has the same subjective feel as LSD (should be able to report back on that one sometime soon hopefully). The positioning of the carbon atoms should be similar to the 'gull wing' shape that the diethylamide assumes when bound to the receptor (hence why the azetidine derivative retains activity)
Beenhead
Bluelight Crew
^^ Where are you getting information on the shape of the 5ht2a? I have searched the protein data banks and found nothing.
Actually, a protein sequence would kick ass, so I could just draw it! I promise Ill post any pictures I draw of this receptor here!
Actually, a protein sequence would kick ass, so I could just draw it! I promise Ill post any pictures I draw of this receptor here!
Hammilton
Bluelighter
- Joined
- Sep 2, 2008
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- 3,435
Unfortunately the AA sequence won't be very useful without knowing how it's "folded."
This said, there are some models of the receptor around. I know Longimanus and Erny were working on one (or rather two, I'm pretty sure they did so independently) and I'm pretty sure Nichols has one but I don't think it's been published.
I think you're referring to the part where FnB mentions the shape of the dimethylazetidine derivative. He's not talking about the shape of the receptor, but rather the conformation of the LSD derivative. This is at least something we can look at fairly easily with MM2 minimization using something like Chembiodraw 3D.
This said, there are some models of the receptor around. I know Longimanus and Erny were working on one (or rather two, I'm pretty sure they did so independently) and I'm pretty sure Nichols has one but I don't think it's been published.
I think you're referring to the part where FnB mentions the shape of the dimethylazetidine derivative. He's not talking about the shape of the receptor, but rather the conformation of the LSD derivative. This is at least something we can look at fairly easily with MM2 minimization using something like Chembiodraw 3D.
IGNVS
Bluelighter
we can look at fairly easily with MM2 minimization using something like Chembiodraw 3D.
can we? (pix plz )
can we? (pix plz )
Beenhead
Bluelight Crew
I realize what he is talking about, but How do you know the shape that the molecule will make with out knowing the shape of the active site. Are you saying the active site has been mapped?
Well I can throw up a pic of LSD with a MM2, but how do you know its conformation in the receptor? I have CHem 3d, so Ill draw it and put it up...
Well I can throw up a pic of LSD with a MM2, but how do you know its conformation in the receptor? I have CHem 3d, so Ill draw it and put it up...
Beenhead
Bluelight Crew
These were all minimized with the MM2 function, though I think Gaussian or Mopac would of been better. The azetidine just looks so much smaller compared to even the pyrrol. Seems like any type of dipole/dipole or vander waals force going on is not going to be nearly as strong at that distance. No?
EDIT:
So it seems from this article that these rings are too small and distort the shape of the receptor, dropping affinity,a nd potentcy. Its amazing that LSD fits JUUUUST right to create the perfect fit..
Last edited:
Hammilton
Bluelighter
- Joined
- Sep 2, 2008
- Messages
- 3,435
Because the compound prefers the energy minimized state (for obvious reasons), it will assume this state most often. For a drug that's so exceptionally potent, one can only assume that it's binding in a conformation equal to or very close to the minimized state.
And like I said, there are models available of the active site. It's hard to say how accurate they are, though.
/navarone/
Bluelighter
Greetings everyone.
Unfortunately i'm really in a rush but after reading the post from F&B about %-HT receptor affinity, i couldn't keep myself from sketching a new molecule.
Its a hybrid between LSD-25 and Fully aromatic iodo-DragonFLY with an extra double bond on the cyclohexane ring to give the molecule a more planar structure.
I'll post a bitmap image right away:
5-ht receptor activity arent't my forte but any opinion would be greaty apreciated.
Unfortunately i'm really in a rush but after reading the post from F&B about %-HT receptor affinity, i couldn't keep myself from sketching a new molecule.
Its a hybrid between LSD-25 and Fully aromatic iodo-DragonFLY with an extra double bond on the cyclohexane ring to give the molecule a more planar structure.
I'll post a bitmap image right away:
5-ht receptor activity arent't my forte but any opinion would be greaty apreciated.
/navarone/
Bluelighter
Some interesting information about LSD receptor affinity that i easey found on th net.
BTW could someone explain to me the meaning of that black line at the bottom of the graph?
Plus, could anyone share their opinion on the activity of the theoretical LSD-IodoDragonFLY hybrid I posted above?
Thanks
BTW could someone explain to me the meaning of that black line at the bottom of the graph?
Plus, could anyone share their opinion on the activity of the theoretical LSD-IodoDragonFLY hybrid I posted above?
Thanks
^ where is the chart from? the looks like a 10 nM cut off, why 10nM I don't know, but it is used I guess as a guide to which receptors it would interact with at I guess a typical physiological concentration.
IMHO the hybrid dragonfly ergoline is just an abomination, it fits neither the known SAR of ergolines at 5ht2a nor the SAR of the phenethylamine/ dragonflys. it is it doesn't fit the rule of 5 either. a waste of time.
IMHO the hybrid dragonfly ergoline is just an abomination, it fits neither the known SAR of ergolines at 5ht2a nor the SAR of the phenethylamine/ dragonflys. it is it doesn't fit the rule of 5 either. a waste of time.
