Fenethylline (Captagon) synthesis

cyb3r0

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I'm not an expert in chemistry just a hobbyist and I want to know the following ratios how much are they equivalent in grams

Theophylline 10 mmol
Sodium hydroxide 10–20 mmol
aliquat-336 0.6 mmol
1,2-dichloroethane 10–20 ml
And the other point here, do you leave it here at a certain temperature?
 

Eleusius_hive_reboot

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then WHAT DO YOU BOTHER US HERE AND SPAM THIS BEAUTIFUL THREAD ?
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stop acting as if you would even try to pull of this synthesis...how can i now???

you would pet ether confuse with ether...BOOM! so go elsewhere....back in the HIVE days we`d slaughtered such folks!
 

MadHatter

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A hobbyist should know how to google stuff. Otherwise it's impossible to be a hobbyist. Learn to google.
 

Field7

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Wow. I came from the UTFSE generation.
 

Mo0odi

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I mean in [method 1-2] there is a hydrochloric acid (hcl) alcohol solution.

My question here is how can I make this solution
 

41Dxflatline

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You literally just mix them together. I will simplify it for you, if you want a 4% solution get 100ml of your alchol and add 3.6ml of alcohol to it. assume 1% of concentration is 0.9 in 100ml and you will have no trouble.
 

Mo0odi

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Thank you
 

diogenes

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Patton, can 1,2 Dichloroethane be substituted with something else? This solvent is quite difficult to get, I have searched and couldn`t find it anywhere.
 

G.Patton

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Hello, it works in this reaction not as a solvent. You can't substitute it, unfortunately.
 

Mandooooo

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Captagon pill. How much does it contain mg of the active substance?
 

yuiopjkl

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Captagon tablet contain 50 mg of Fenethylline

But it no longer exists.All existing tablets contain amphetamine and some adulterants.
 

fayd

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fayd

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Hi buddy, I have the raw theophylline (and I'll make phenylnitropropene. I found an easy way). Can you explain to me how Captagon tablets are made from these materials? (I am a beginner and I want a video clip or a simplified explanation of making Captagon using theophylline and phenylnitropropene.
 

G.Patton

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Hello. Dear @fayd. If you continue spam by the same question under this topic, I'll ban you. It's not nice to behave like this. We won't make video about Captagon.
The synthesis is explained clearly. If you need to figure out some details or you don't understand something, you can ask me or here what exactly you need.

Do not spam!

P.S. I deleted previous 3 same messages.
 

fayd

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I apologize for that
 

Carlz

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Hi @fayd, do you mean you want Captagon powder in tablet form? This requires mechanical tablet compression, either by wet or dry granulation or direct compression, that is if you are planning to start your own business, but if you just want to know how to synthesize it here is @G.Patton the expert, explaining the whole process.
 

طهرانmobster

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Hello G.patton
Hello brother how are u
In Second mathod part 2
After extraction with dcm (aqueous phase) and dry organic phase with sodium sulfate and filtering
After this part i dont understand and i search alot before ask and take your time
Can explain to me please?
Thank you
 

loadingST

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Can someone clarify me did the fenetiline is a stronger stimulant than d-amph, or just the products of which it becomes metabolized the simple theophiline and amphetamine and just because it happens very slow it have that long lasting effect compared to amphetamine and and nice boost of the theophiline that gets metabolized too ? Is the theophiline MDA analogue tested and probably even unsheduled ?
 

G.Patton

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The physiological effects of fenethylline therefore seem to result from a combination of these two compounds, although it is not entirely clear how, and seems to involve a synergistic effect between amphetamine and theophylline produced following metabolism. The pharmacological actions of fenethylline before cleavage also remain poorly established, though it appears to act directly at several serotonin receptors. I assume it gives long lasting effect a little as well.

It's interesting question. I haven't met such compound in literature data. In theory, it's possible to make similarly.

Probably, @Paracelsus have any thoughts about this.
 

loadingST

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If its confirmed the fenetiline acts on serotonine receptors, it for shure have additional effects of the fenetiline produced, thats very intrested topic, im gona research this, i cant wait @Paracelsus to clear it up this topic more if he can haha
 

Paracelsus

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It is really interesting question. I will try to answer, but in general @G.Patton has already said everything :)

Fenethylline is a mutual prodrug – the molecule is cleaved (likely by hepatic enzymes) to yield amphetamine and theophylline in a roughly 2:1 ratio by dose. Importantly, only a small fraction of the potential amphetamine content is actually released in the body – suggesting fenethylline is not completely broken down into amphetamine. The pharmacodynamics, however, align more with the parent compound and combined metabolites than with just that small amphetamine release. This indicates fenethylline’s intact form and its metabolites collectively determine its effects, rather than it acting purely as a slow amphetamine “prodrug.” Once in circulation, fenethylline (being more lipophilic than amphetamine) crosses the blood–brain barrier efficiently. As it metabolizes, amphetamine and theophylline are released gradually. Amphetamine stimulates dopamine/norepinephrine release, while theophylline blocks adenosine receptors, producing wakefulness and alertness.

The metabolic breakdown of fenethylline leads to a different time-course of effects compared to taking d-amphetamine alone. Because fenethylline’s active ingredients are generated in vivo, the stimulant effect can be more sustained and smoother. Amphetamine from fenethylline is released over time and penetrates the brain slightly later than an equivalent dose of pre-formed amphetamine. This delayed arrival to the brain may dampen the immediate “rush” (reducing acute euphoria and addiction potential) while still providing robust stimulation. Meanwhile, theophylline’s presence provides an immediate mild stimulant boost (since theophylline starts working as soon as it’s liberated, akin to a caffeine jolt) and continues to act for several hours. Notably, amphetamine can inhibit the metabolism of theophylline by competing for CYP2D6. This means theophylline stays in the system longer when both are present, further prolonging the stimulant effect. Indeed, reports state Captagon’s effects last longer than typical amphetamine’s. One source notes fenethylline’s half-life is roughly 12 hours, on par with or a bit longer than dextroamphetamine’s.

In practical terms, fenethylline’s metabolism prolongs its action and shapes its strength. The user may experience a rapid onset of alertness (due to quick CNS absorption and theophylline’s action) and a sustained stimulant effect as amphetamine steadily exerts its influence. The synergy can make the perceived strength quite high and long-lasting – for example, soldiers taking Captagon report being able to stay awake, alert, and confident for long periods. By contrast, d-amphetamine (especially immediate-release) tends to have a more defined peak and then taper, unless redosed or in extended-release form.

The metabolism effectively turns fenethylline into a “two-stage” stimulant: an initial caffeine-like kick followed by a delayed amphetamine boost, yielding a longer, arguably smoother stimulant experience than a single dose of d-amphetamine alone.

There is no strong evidence of direct serotonergic activity for Captagon at the moment. In research by Wenthur et al. (2017) Fenethylline was tested at a concentration of 10 μM against a panel of 31 CNS targets. Among these targets was the serotonin receptor subtype 5-HT2B, where fenethylline showed only a modest interaction (23% inhibition), which indicates very weak or negligible serotonergic activity. Usually, significant serotonergic effects would require much higher affinity (greater inhibition percentage or lower IC50 values). The study explicitly states that fenethylline’s distinctive psychoactive properties are not attributed directly to the parent compound's activity at standard CNS receptors but rather emerge due to the synergistic actions of its metabolites—primarily amphetamine and theophylline.

Based on my research, there is no evidence that a theophylline–MDA analogue has been synthesized or studied. No patents, journal articles, or official reports describe making this specific compound, suggesting it remains a theoretical or clandestine concept rather than a documented chemical. Combined in one molecule, the released MDA would produce mood-elevating and psychoactive effects while theophylline would add a caffeine-like stimulation. It is possible these two could also act synergistically (similar to amphetamine/theophylline). The net effect might be a somewhat prolonged entactogenic stimulant experience, potentially smoother in onset/offset than MDA alone (due to gradual metabolism). Without actual studies, this profile remains speculative. Importantly, MDA is a more serotonergic agent than amphetamine, so a theophylline–MDA drug might carry more risk of entactogenic side effects (e.g. serotonin release, neurotoxicity) alongside stimulation.

Here is some Captagon related papers:
 
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