cocaine analog(s?) from arecoline

fidelis

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writeup by beagle and rhodium, taken from the vespiary. check the link 4 references!!


Introduction

This is one of the most promising area of research on cocaine analogs that I've come across. In the article [1], the authors were attempting to come up with an equivalent of methadone for cocaine addicts. That is, a substance that would have some of the effects of cocaine without all the euphoria (Coke-Lite®, I guess it will be called [fidelis note: i think it would b funny if they called it diet coke lol]). The research was based on some work done in 1973 (by Clarke [2]) in which a series of similar compounds was made and found not to cause stimulation in mice (i.e. no fun). However, in this study, the compounds were found to be up to 30 times the potency of cocaine in blocking dopamine transport or binding of cocaine to its receptor. So the results are rather confusing. Possibly the researchers have actually found a lead in their search for coke-adone, or maybe they have found a series of ridiculously easy to synthesize highly potent coke analogs. Either way, interesting work. Currently they are shooting up monkeys to see if they like it or not, but it may be years before they publish their work. Maybe someone out there could help them out. I always say, never send a monkey to do a man's work.

In Clarke's 1973 paper [2], a series of structurally reduced cocaine analogs are synthesized in which 2 carbons and an ester group have been removed from the tropane skeleton, giving 4-phenyl-piperidines with an ester group at the 3-position. The most active compound in their series is about 30 times the potency of cocaine (in blocking dopamine uptake). The synthesis is much easier than any other active cocaine analog, and starts from non-exotic reagents.

The main starting material used by the authors is Arecoline (3,4-unsaturated N-methyl-piperidine-3-carboxylic acid methyl ester), the active principle of the popular red betel nut. Treatment of this alpha,beta-unsaturated ester with the Grignard reagent 4-Chlorophenylmagnesium Bromide gave rise to four products, easily grouped into two racemic forms of each cis- and trans-isomer. The racemic cis-isomer is twice as potent as cocaine, while the racemic trans-isomer is only half as strong.

The authors start with arecoline (the active compound in betel nut: N-methyl-piperidine- 3-carboxylic acid methyl ester with a double bond between the 3 and 4 positions). Reaction of this with a 4-chlorophenylmagnesium bromide Grignard reagent gives a mixture of a total of four discrete entities: A cis- and trans-mixture in a 3:1 ratio, each constisting of a of two isomers, each isomer also being racemic, all which the which the authors resolve through fractional crystallization as their dibenzoyl tartaric acids, but this is not strictly necessary since each of the isomers are active. Arecoline Hydrobromide is a fairly cheap commercial starting material, $80/50g from Aldrich. Also, I think that it is used in veterinary medicine.

GAM0bK3irO


Synthetic Outline
The Arecoline freebase was prepared by treating the Arecoline Hydrobromide of commerce with concentrated aqueous sodium bicarbonate, followed by extraction with methylene chloride, thorough drying of the extracts over anhydrous Magnesium Sulfate, followed by suction filtration and evaporation of the solvent in vacuo. The freebase was then used as is in the next step.

To a solution of 166ml of 1M 4-chlorophenylmagnesium bromide in 700ml ether was added 12.9g of arecoline freebase in 300ml ether at -10°C. The mix was stirred at -10°C for 30 min, poured onto ice and treated with 200ml of 10% HCl. The aqueous layer was separated, washed with 200ml ether, cooled in an ice bath, and 100ml of saturated sodium bicarb. solution added. The solution was extracted with 2x100ml of ether, washed with brine, dried, and concentrated in vacuo. The crude mixture was crystallized from EtOAc/hexane to give racemic cis-isomer as a white solid (5g, 22%). Additional cis-isomer (Total: 12.4g, 56%, mp 98-99°C), as well as 2.0g (18%) of the trans-isomer was obtained by flash chromatography of the mother liquor.
 

Osmosis Vanderwaal

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I meant to respond to this last week but I started fact checking myself and my facts checked out but I got distracted. I have spent some time on this subject. Betel nuts are perfectly legal in the US, they sell them in many places.
The chemical in your post, I reconstructed it in kingdraw, so I could get a name for it, which I did. And look it up. Which I did. It is an isomer of nocaine. In other news, if you use a different grignard, the product is paroxetine, IE Paxil. When I was looking at how to synthesize Grignard reagents, it sounded pretty difficult. Also I didn't find any for sale that didn't require a dea#.. if you can get some, I'll buy the betel nut.
All of the arecoline based analogs of cocaine can be read about in the super awesome "cocaine analogs" book by .Signed? It's in the library here and it's a masterpiece
 
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CryoThio

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Not a chemist.

This might be good for home chemist use, for making a stimulant that is possibly Uncontrolled and while needing grignard conditions, and grignard reagents, could be a viable way to get some stimulants.

Large scale, I don't think so.

Large scale grignards probably need a real chemist/chemical engineer to plan out, and it seems not very "dense" of a reaction.

To get 129 or so grams (the synthesis mentioned scaled up 10x) one needs about a 20L flask, as you don't generally fill flasks more than halfway as a good practice.

The same amount of space could a whooole lot more of say p2p in the same amount of space. One thread from the vespiary claims about 250 grams of mdp2p could be reacted with about 3000ml of solvents, etc.

So one needs 20L for 129 grams, while say mdp2p on can fit about 833 grams of mdp2p.

Not that ideal large scale.
 
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