Amphetamine Syntheses Methods

Amphetamine Syntheses Methods

General information741KQUpZCJ.png

Amphetamine (also known as alpha-methylphenethylamine, amfetamine, and speed) is a classical stimulant substance of the phenethylamine class. It is the parent compound of the substituted amphetamines, a diverse group that includes methamphetamine, MDMA, cathinone, and bupropion. The mechanism of action involves promoting release of the neurotransmitters dopamine and norepinephrine.

Amphetamine, a substance discovered over 100 years ago, is one of the most restricted controlled drugs. It was previously used for a large variety of conditions and this changed until this point where its use is highly restricted. Amphetamine, with the chemical formula alpha-methylphenethylamine, was discovered in 1910 and first synthesized by 1927. After being proven to reduce drug-induced anesthesia and produce arousal and insomnia, amphetamine racemic mix was registered by Smith, Kline and French in 1935. Amphetamine structure presents one chiral center and it exists in the form of dextro- and levo-isomers. The first product of Smith, Kline and French was approved by the FDA on 1976.

2nq5bnpztb-jpg.6577edzp6bc5hs-jpg.6578

In the 1930s, it was sold over-the-counter under the name "Benzedrine" as a decongestant. It became widely used to treat a range of ailments such as alcohol hangover, narcolepsy, depression, and obesity. During World War II, amphetamine was used to promote wakefulness in the soldiers. This use derived into a large overproduction of amphetamine and all the surplus after the war finalized ended up in the black market, producing the initiation of the abuse. Due to issues with addiction and abuse, it was eventually listed as a controlled substance under the United Nations 1971 "Convention on Psychotropic Substances".

pe4qjwnh7a-jpeg.6582

Amphetamine is now primarily a prescription drug used to treat attention deficit hyperactivity disorder (ADHD), narcolepsy, and obesity. Additionally, it sees widespread illicit use as a performance enhancing agent and recreational substance.

 Physical properties

  • Formula C9H13N
  • Molar mass 135.210 g/mol
  • Density 0.936 g/cm3 at 25 °C
  • Melting point 11.3 °C (52.3 °F)
  • Boiling point 200-203 °C (397 °F) at 760 mmHg

Chemical properties

The free base of amphetamine is a colorless volatile oily liquid with a characteristic "fishy" odor and acrid, burning taste, poorly soluble in water, readily soluble in organic solvents, boiling point 200-203 °C.

tld6is4hjv-png.6579

Synthesis ways

There are list of most popular amphetamine synthesis ways. All of them have own advantages and disadvantages. Most popular non-selective synthesis is P2NP reduction, which can be carried out with aluminium (Al) amalgam. Also, it is possible to reduce by NaBH4, LAH or hydrogen gas with catalyst (PtO2 or Pd/C) and excess pressure. P2NP can be synthesized by simple condensation of nitroethane with benzaldehyde.

rucao4f7fm-png.6590

 

P2NP Al/Hg reduction

P2NP NaBH4 reduction

One of the most common methods of clandestine amphetamine production is the Leuckart reaction, which consists of the condensation of phenylacetone (phenyl-2-propanone, P2P) with formamide or ammonium formate in the presence of formic acid and subsequent acid hydrolysis of the resulting N-formylamphetamine.

qeak52xyzt-png.6589

 

A mphetamine can also be prepared by reductive amination of phenylacetone (P2P) in the presence of a metal catalyst. The reaction proceeds with the formation of an intermediate imine. Examples of a reaction are: Heterogeneous catalytic reduction of phenylacetone with ammonia. The catalyst may be palladium on carbon, platinum oxide or Raney nickel. Restoration with aluminum, zinc or magnesium amalgams.

vfrijahpjm-png.6594

 

If necessary, the amphetamine stereoisomers dextroamphetamine and levoamphetamine can be separated using tartaric acid. In addition, a method has been published for the stereoselective synthesis of dextroamphetamine, which consists in the reductive amination of phenylacetone with S-α-methylbenzylamine. The imine, which was obtained, is reduced with Pd/C or Raney nickel and recrystallized as the hydrochloride. The N-benzyl group is then hydrogenolyzed in the presence of palladium on charcoal to form high optical purity dextroamphetamine.

9srapzicdz-png.6593

 

6rmcdyynki-png.6592

 

Analysis and purification

Toxic and dangerous substances are used in any synthesis way of amphetamine. There are two amphetamine purification methods "Product Washing" and more advanced method "Acid-base Extraction".

 Drug washing is an essential and final part of almost any synthesis. Sometimes repeated several times. The method is available to anyone, does not require skills, can significantly improve the quality of product and presentation. The method is Ideal for small quantities. Washing is indicated for residues of P2NP, alkalis, acids and so on. Washing will not remove contaminants (acetaminophen, caffeine, etc.) and mercury salts.

 The most accessible, and therefore easier, is to wash amphetamine with isopropyl alcohol (IPA). More difficult to use is anhydrous acetone. IPA does not contain water, and therefore it does not dissolve amph salt. The key to the process success is the lack of water. It is needing for avoiding amph from dissolution with pollutants because they will be thrown out.

 Acid-base extraction (ABE), as a purification method, allows you to get a high-quality drug. Method is good by reason of using available reagents, tools and instruments.

Amphetamine is cut unacceptably often by caffeine, starch, nootropics such as Cinnarizine and Piracetam, a-PVP, methamphetamine and other stimulants and pharmacy substances. There are several methods to check your amphetamine. The most popular and easiest way is Drugs testing reagents. You can read about other methods in Amphetamine assessment protocol.

 

There are pictures of different amphetamine samples after tests by reagents

5yus7iywpm-jpg.6588xwrscfkdee-jpg.65831mwlfuzcoh-jpg.658695co0hasqb-jpg.6584epgw2l6urc-jpg.6587vy1oe3f8kd-jpg.6585

 

Effects and dosage

Subjective effects include stimulation, focus enhancement, motivation enhancement, increased libido, appetite suppression, and euphoria. It is usually taken orally, but can also be insufflated, injected, or administered rectally. Lower doses tend to increase focus and productivity while higher doses tend to increase sociability, sexual desire, and euphoria.

 Amphetamine has high abuse potential. Chronic use (i.e. high dose, repeat administration) is associated with compulsive redosing, escalating tolerance, and psychological dependence. Additionally, abuse has been linked to a number of health conditions, especially cardiovascular issues such as high blood pressure and increased risk of stroke. It is highly advised to use harm reduction practices if using this substance.

Physical effects

Stimulation - Amphetamine is reported to be very energetic and stimulating. It can encourage physical activities such as dancing, socializing, running, or cleaning. The particular style of stimulation that amphetamine produces can be described as forced. This means that at higher dosages, it becomes difficult or impossible to keep still. Jaw clenching, involuntary bodily shakes, and vibrations become present, resulting in extreme shaking of the entire body, unsteadiness of the hands, and a general loss of fine motor control. This is replaced with mild fatigue and general exhaustion during the offset of the experience.

  •       Spontaneous bodily sensations - The "body high" of amphetamine can be described as a moderate euphoric tingling sensation that encompasses the entire body. This sensation maintains a consistent presence that steadily rises with the onset and hits its limit once the peak has been reached.
  •        Physical euphoria
  •        Abnormal heartbeat
  •        Increased heart rate
  •        Increased blood pressure- By about 30mmHg systolic and 20mmHg diastolic, from naive users taking 40mg d-AMP.
  •        Appetite suppression
  •        Bronchodilation
  •        Dehydration
  •        Dry mouth
  •        Frequent urination
  •        Difficulty urinating
  •        Increased bodily temperature
  •        Increased perspiration
  •        Mania - Amphetamine can produce mania in genetically predisposed individuals, such as those on the spectrum of bipolar disorder or schizophrenia. Higher doses and sleep deprivation appears to increase the risk.
  •        Nausea - This can be mitigated by eating before dosing and throughout the experience.
  •        Pupil dilation - This effect is experienced only at common to high dosages and is more prominent on the comedown.
  •        Reflex syncope
  •        Stamina enhancement
  •        Teeth grinding - Teeth grinding may be present at higher doses. However, it is less intense than that of MDMA.
  •       Temporary erectile dysfunction
  •        Vasoconstriction - Amphetamine use causes blood vessels to constrict resulting in not enough blood reaching some parts of the body. This can cause feelings of tingling or pain, a cold feeling, numbness, paleness, or skin color changes especially in the fingers and toes.

Visual effect

  • The visual effects of amphetamine are inconsistent and occur only mildly noticeable at higher doses. They are somewhat comparable to deliriant visuals and occur more readily in darker areas.

Distortions

  • Drifting - This effect is usually subtle and barely noticeable and only occurs at higher dosages or when combined with cannabis. Commonly this consists of level 1-2 drifting.

  • Brightness alteration - Amphetamine can make spaces seem brighter as a result of its pupil dilating effects.
  • Tracers - This effect is imperceptible with low dosages. It's most pronounced with bigger dosages and especially when someone becomes sleep deprived, what on the other hand can be easily provoked by other effects of this substantion.    Transformations - This effect occurs very rarely, and typically only when the user has taken high doses, is coming down, or has been awake for unusually long periods. They are usually very mild when they do occur.

Hallucinatory states

  • Transformations - This effect occurs very rarely, and typically only when the user has taken high doses, is coming down, or has been awake for unusually long periods. They are usually very mild when they do occur.

  • Geometry - This effect is reported by some users of amphetamine and related substances, typically at heavier doses when one is attempting to sleep. It can be described in its variations as simplistic, algorithmic, synthetic, dimly lit, multicolored, glossy, sharp edges, zoomed out, smooth, angular, immersive, and progressive. It typically occurs at level 3 however may progress to 4 and 5 when combined with substances like cannabis or DXM.

Cognitive effects

  •        Analysis enhancement
  •        Cognitive euphoria
  •        Compulsive redosing
  •        Ego inflation
  •        Emotion suppression - This effect is typically most intense at light and common doses, and is more commonly reported from medical usage rather than recreational.
  •        Focus enhancement - This effect is most effective at low to moderate doses as anything higher will usually impair concentration.
  •        Increased libido - While amphetamine use can cause feelings of sexual enhancement, the constricting of blood vessels may make it difficult to get or maintain an erection.
  •        Increased music appreciation
  •        Irritability - This is more likely to occur at higher doses.
  •        Memory enhancement
  •        Motivation enhancement
  •        Psychosis - This effect only occurs in either predisposed individuals, or after chronic, high frequency use, or due to sleep deprivation.
  •        Suggestibility suppression
  •        Thought acceleration
  •        Thought organization
  •        Time distortion - This can be described as the experience of time speeding up and passing much quicker than it usually would when sober.
  •        Wakefulness

After effects

The effects which occur during the offset of a stimulant experience generally feel negative and uncomfortable in comparison to the effects which occurred during its peak. This is often referred to as a "comedown" and occurs because of neurotransmitter depletion. Its effects commonly include:

  •        Anxiety - Anxiety can reach severe levels during the comedown in some users.
  •        Appetite suppression
  •        Cognitive fatigue
  •        Depression
  •        Increased heart rate - While blood concentration of amphetamine and most subjective effects are highest about 3 hours after administration, heart rate peaks much later at 10 hours after administration.
  •        Irritability
  •        Motivation suppression
  •        Restless legs
  •        Sleep paralysis - Some users note sleep paralysis after consuming amphetamine.
  •        Dream suppression
  •        Thought deceleration
  •        Wakefulness - The insomnia following a repeated series of amphetamine doses can last for longer than a day in some users.
  •        Motivation suppression - Experiences can range from mild demotivation to extreme states of disinterest. This effect is more prominent at common and heavy doses.

 

b2j4z7wr5k-png.6576

Pharmacology

Amphetamine exerts its behavioural effects by increasing the signaling activity of neurotransmitters norepinephrine and dopamine in the reward and executive function pathways of the brain. The reinforcing and motivational effects of amphetamine are mostly due to enhanced dopaminergic activity in the mesolimbic pathway.

The euphoric and locomotor-stimulating effects of amphetamine are dependent upon the magnitude and speed by which it increases synaptic dopamine and norepinephrine concentrations in the striatum.

It is a potent full agonist of the trace amine-associated receptor 1 (TAAR1) and interacts with vesicular monoamine transporter 2 (VMAT2). Combined action on TAAR1 and VMAT2 results in increased concentrations of dopamine and norepinephrine in the synapses, which stimulates neuronal activity.

Dextroamphetamine is a more potent agonist of TAAR1 than levoamphetamine. Consequently, dextroamphetamine produces greater CNS stimulation than levoamphetamine, roughly three to four times more, but levoamphetamine has slightly stronger cardiovascular and peripheral effects.

The exact bioavailability of amphetamine is not known, but it is believed to be over 75% by mouth, and higher by injection or intranasal administration. Its absorption and excretion may be pH dependent. As it is a weak base hence the more basic the environment the more of the drug is found in a lipid-soluble form and the absorption through lipid-rich cell membranes is highly favored. The peak response of amphetamine occurs 1-3 hours after oral administration and approximately 15 minutes after injection. Complete amphetamine absorption is usually done after 4-6 hours. The basic form is more readily absorbed in the intestine and less readily removed by the kidneys, potentially increasing its half life. It is removed by the kidneys via excretion and a small amount is removed by hepatic enzymes.

Bibliography

  1. BlueDex

    Aluminum Galinstan amalgam

    The Aluminum and galinstan can be heated up to form an aluminum galinstan amalgam.
  2. Amphetamine synthesis

    Amphetamine synthesis

    Amphetamine synthesis via NaBH4 reductive amination from P2NP. https://bbgate.com/threads/one-pot-amphetamine-synthesis-from-p2np-with-nabh4-cucl2-1kg-scale.70/
  3. 1-Phenyl-2-nitropropene synthesis

    1-Phenyl-2-nitropropene synthesis

    Benzaldehyde and nitroethane Henry condensation. https://bbgate.com/threads/1-phenyl-2-nitropropene-p2np-video-synthesis-from-benzaldehyde-and-nitroethane-henry-reaction.52/
  4. GaDjo

    where to buy laboratory glassware and equipment ?

    Question 
    Good morning all I would like to estimate the cost of a lab of 4-MMC and/or amphetamine. For that, I have to look for laboratory glassware. I've tried looking in existing threads, but can't find any advice on where to buy it. So, do you have a site to advise me to buy my first pieces? I'm in...
  5. KokosDreams

    Largest ever European haul of amphetamine precursor BMK seized

    The Criminal Department of CBI Polish Police, Unit Gdansk, has seized Europe's largest ever haul of the amphetamine precursor, BMK, in Warsaw. This was the result of a long-term investigation conducted by the Polish CBI of Gdansk since 2013. The seizure consisted of 346 blue jerry cans, each...
  6. Power

    What is the “paste” part of amphetamine

    Question 
    I’m looking for ways to purify amphetamine paste but what is the paste is it actual amphetamine or should I look for a way to remove the amphetamine paste its hard to dose paste because well purity is unknown most advertised as 74 percent but seems to be a lie most of the time because I can...
  7. Alphamethylphenethylamine (amphetamine) synthesis

    Alphamethylphenethylamine (amphetamine) synthesis

    479Mb (.mp4) 1-Phenyl-2-nitropropene (P2NP) reduction to α-methylphenylethylamine by aluminium amalgam. https://bbgate.com/threads/amphetamine-synthesis-from-p2np-via-al-hg-video.196/
  8. KokosDreams

    Saudi Arabia seizes record 47 million amphetamine pills hidden in flour shipment

    Some 47 million amphetamine pills hidden in a flour shipment were seized by Saudi Arabia's authorities. Authorities in Saudi Arabia have confiscated 47 million amphetamine pills which were hidden in a flour shipment, in an operation described as the biggest one-time drug smuggling attempt in...
  9. KokosDreams

    Question regarding amphetamine synthesis via P2NP + NabH4/CuCL2

    Hey folks, going through my notes (read below) I am wondering about three main questions right now: My questions now are: What PH do I need to bring the reaction to before adding DCM? Is it necessary to extract the aqueous phase with IPA or can I just extract with DCM and distill after...
  10. C

    Smelly amphetamine in Europe

    European amphetamine smells very very different from amphetamine in North America I find. I talked to a few people and was told that in Europe (except in the Netherlands) they take the amphetamine oil and instead of puryfing and crysallizing it they add caffeine and all sorts of different...
  11. Dragovich

    Methamphetamine From Amphetamine Sytnthesis Report (With Success and Final Photos)

    Hello everyone again after a long time. Today I will briefly describe my success in synthesis and what steps I followed. I'm sorry I won't keep long. I don't know what the chemicals you have and the materials you have, but since I live in Turkey, the poorest country in Europe, I pushed the...
  12. C

    Need a little help with something

    Question 
    Hey guys, since in my country I can buy only one medicine without a prescription that contains pseudoephedrine, it contains also ibuprofen. Is there a way to separate pseudoephedrine from ibuprofen?
  13. KokosDreams

    Recrystalization of P2NP

    Question 
    Hey folks, as I am ordering my first P2NP soon I am looking for advice for the following subject: Recrystalization of P2NP I have read some things about this process in the forum and understood that it is recommended not only proof the quality of the P2NP but also to improve it's quality if...
  14. KokosDreams

    EU Supplier for Mercury (II) Nitrate CAS 10045-94-0 for Amphetamine Freebase Synthesis

    Looking for a vendor 
    Dear Breaking Bad Community, I am Koko, I have been active on the DN since a few weeks. Since 4-5 months I am on the mission to understand the synthesis of Amphetamine Freebase. Mainly I am looking for 2 synthesis methods: 1. Manufacture Amphetamine Freebase from P2NP & Mercury (II) Nitrate...
  15. BHBlueberry

    Few basic but most important amphet-amine facts

    Hello. Maybe someone will save his life or health, knowing these rather new facts observed in my own laboratua. 1. Amphet-amine does not work always the same even if taken from one bath (cooking) - Your body will sometimes get full of this substance. I know, it's hard to accept but most...
  16. M

    Amphetamine bulk supply

    Looking for a vendor 
    Hello After failed attempts of synthesis, Im looking for a bulk supplier of amphetamine. Large quantities required, central europe, write me.
  17. meribel

    Synthesis and sell

    Question 
    Good evening to all, first of all, thank you to the contributors for the vastness of the resources found here. I have 2 questions : I would like to start synthesizing methamphetamine and amphetamine and I would like to know if there are alternatives to products that are not easily found such...
  18. chemden

    Methods to synthesis Amphetamine

    I'm looking for a method to synthesize amphetamine in my laboratory. I have a chemistry degree, but almost no experience. This is why I don't know which synthesis method to choose. It would be helpful if some of you that have experience in this field could describe or refer to synthesis...
  19. M

    neutralization of amphetamine free base to amphetamine sulfate. questions and answers that may be bothering you.

    Hello everyone . the thread was created due to the fact that I have a few unanswered questions. questions : 1.should amphetamine free base (oil) be mixed with a solvent toluene / dcm etc before neutralization? if so, in what proportions? 20-30% of the oil volume will be OK? 2. in what ratio...
  20. BMKOILEY123

    EASIEST WAY TO CONVERT BMK TO AMPH.

    Hey folks, one question.... I have been buying BMK oil from holland for a while, which is mixed 1:1 with isopropanol and then carefully precipitated with concentrated sulfuric acid to amphetamine sulfate. I have now tested bmk oil from another supplier and tried to convert it to amphetamine...
Top