Amphetamine: Difference between revisions
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Revision as of 15:20, 24 May 2011
Put Overweight Americans(Lazy Type II Diabetics in particular) on Amphetimines so the rest of the world can Eat!
Clinical data | |
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Other names | alpha-methylbenzeneethanamine, alpha-methylphenethylamine, beta-phenyl-isopropylamine |
Routes of administration | Oral, Intravenous, Vaporization, Insufflation, Rectal, Sublingual |
ATC code | |
Legal status | |
Legal status |
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Pharmacokinetic data | |
Bioavailability | nasal 75%; rectal 95–99%; intravenous 100% |
Protein binding | 15–40% |
Metabolism | Hepatic (CYP2D6)[2] |
Elimination half-life | 12h average for d-isomer, 13h for l-isomer |
Excretion | Renal; significant portion unaltered |
Identifiers | |
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CAS Number | |
PubChem CID | |
DrugBank | |
ChemSpider | |
UNII | |
KEGG | |
ChEMBL | |
CompTox Dashboard (EPA) | |
ECHA InfoCard | 100.005.543 |
Chemical and physical data | |
Formula | C9H13N |
Molar mass | 135.2084 g·mol−1 |
3D model (JSmol) | |
Melting point | 285 to 281 °C (545 to 538 °F) |
Solubility in water | 50–100 mg/mL (16C°) mg/mL (20 °C) |
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(what is this?) (verify) |
Amphetamine (USAN) or amfetamine (INN) is a psychostimulant drug of the phenethylamine class which produces increased wakefulness and focus in association with decreased fatigue and appetite.
Brand names of medications that contain, or metabolize into, amphetamine include Adderall, Dexedrine, Dextrostat, Desoxyn,[3] ProCentra, and Vyvanse, as well as Benzedrine in the past.
The drug is also used recreationally and as a performance enhancer. Recreational users of amphetamine have coined numerous street names for amphetamine, such as "speed". The European Monitoring Centre for Drugs and Drug Addiction reports the typical retail price of diluted amphetamine in Europe varied between €3 and €15 ($4 to $21.55 USD) a gram in half of the reporting countries. Street amphetamine is typically about 10% pure.[4] The name amphetamine is derived from its chemical name alpha-methyl phenethylamine.
Effects
Physical effects
Physical effects of dextroamphetamine can include hyperactivity, dilated pupils, blood shot eyes, flushing, restlessness, dry mouth, bruxism, headache, tachycardia, bradycardia, tachypnea, hypertension, hypotension, fever, diaphoresis, diarrhea, constipation, blurred vision, aphasia, dizziness, twitching, insomnia, numbness, palpitations, arrhythmias, tremors, dry and/or itchy skin, acne, pallor, convulsions, and with chronic and/or high doses, seizure, stroke, coma, heart attack and death can occur.[6][7][8][9][10] There is also significant research which highlights the possible neurotoxic effects of amphetamine on the dopaminergic system, even in clinical doses.[11]
Psychological effects
Psychological effects can include euphoria, anxiety, increased libido, alertness, concentration, energy, self-esteem, self-confidence, sociability, irritability, aggression, psychosomatic disorders, psychomotor agitation, grandiosity, excessive feelings of power and superiority, repetitive and obsessive behaviors, paranoia, and with chronic and/or high doses, amphetamine psychosis can occur.[12][13]
Withdrawal effects
Withdrawal symptoms of amphetamine primarily consist of mental fatigue, mental depression and increased appetite. Symptoms may last for days with occasional use and weeks or months with chronic use, with severity dependent on the length of time and the amount of amphetamine used. Withdrawal symptoms may also include anxiety, agitation, excessive sleep, vivid or lucid dreams, deep REM sleep and suicidal ideation.[14][15][16]
Side effects
Contraindications
Amphetamine elevates cardiac output and blood pressure making it dangerous for use by patients with a history of heart disease or hypertension. Amphetamine can cause a life-threatening complication in patients taking MAOI antidepressants. The use of amphetamine and amphetamine-like drugs is contraindicated in patients with narrow-angle glaucoma or anatomically narrow angles. Like other sympathomimetic amines, amphetamine can induce transient mydriasis. In patients with narrow angles, pupillary dilation can provoke an acute attack of angle-closure glaucoma. These agents should also be avoided in patients with other forms of glaucoma, as mydriasis may occasionally increase intraocular pressure.[17]
Amphetamine has been shown to pass through into breast milk. Because of this, mothers taking amphetamine are advised to avoid breastfeeding during their course of treatment.[18]
Dependence and addiction
Tolerance is developed rapidly in amphetamine abuse; therefore, periods of extended use require increasing amounts of the drug in order to achieve the same effect.[19]
Overdose
An amphetamine overdose is rarely fatal but can lead to a number of different symptoms, including psychosis, chest pain, and hypertension.
Psychosis
Abuse of amphetamines can result in a stimulant psychosis that can present as a number of psychotic disorders (i.e. paranoia, hallucinations, delusions). The intensity and duration of symptoms may vary, but unlike true psychotic disorders (i.e. schizophrenia), stimulant psychoses are not considered to be permanent and will eventually resolve upon discontinuation of the drug's use.[citation needed]
Mechanism of action
Primary sites of action
Amphetamine exerts its behavioral effects by modulating several key neurotransmitters in the brain, including dopamine, serotonin, and norepinephrine. However, the activity of amphetamine throughout the brain appears to be specific;[20] certain receptors that respond to amphetamine in some regions of the brain tend not to do so in other regions. For instance, dopamine D2 receptors in the hippocampus, a region of the brain associated with forming new memories, appear to be unaffected by the presence of amphetamine.[20]
The major neural systems affected by amphetamine are largely implicated in the brain’s reward circuitry. Moreover, neurotransmitters involved in various reward pathways of the brain appear to be the primary targets of amphetamine.[21] One such neurotransmitter is dopamine, a chemical messenger heavily active in the mesolimbic and mesocortical reward pathways. Not surprisingly, the anatomical components of these pathways—including the striatum, the nucleus accumbens, and the ventral striatum—have been found to be primary sites of amphetamine action.[22][23]
The fact that amphetamine influences neurotransmitter activity specifically in regions implicated in reward provides insight into the behavioral consequences of the drug, such as the stereotyped onset of euphoria.[23] A better understanding of the specific mechanisms by which amphetamine operates may increase our ability to treat amphetamine addiction, as the brain’s reward circuitry has been widely implicated in addictions of many types.[24]
Endogenous amphetamines
Amphetamine has been found to have several endogenous analogues; that is, molecules of a similar structure found naturally in the brain.[25] l-Phenylalanine and β-Phenethylamine are two examples, which are formed in the peripheral nervous system as well as in the brain itself. These molecules are thought to modulate levels of excitement and alertness, among other related affective states.
Dopamine
The most widely studied neurotransmitter with regard to amphetamine action in the central nervous system is dopamine. All of the addictive drugs appear to enhance dopamine neurotransmission, including amphetamine and methamphetamine.[26] Studies have shown that in select regions, amphetamine increases the concentrations of dopamine in the synaptic cleft, thereby heightening the response of the post-synaptic neuron.[27] This specific action hints at the hedonic response to the drug as well as to the drug’s addictive quality.
The specific mechanisms by which amphetamine affects dopamine concentrations have been studied extensively. Currently, two major hypotheses have been proposed, which are not mutually exclusive. One theory emphasizes amphetamine’s actions on the vesicular level, increasing concentrations of dopamine in the cytosol of the pre-synaptic neuron.[25][28] The other focuses on the role of the dopamine transporter DAT, and proposes that amphetamine may interact with DAT to induce reverse transport of dopamine from the presynaptic neuron into the synaptic cleft.[21][29][30][31]
The former hypothesis is backed by studies from David Sulzer's lab at Columbia University demonstrating that injections of amphetamine result in rapid increases of cytosolic dopamine concentrations, while the drug decreases the number of dopamine molecules inside the synaptic vesicle.[32][33] Amphetamine is a substrate for a specific neuronal synaptic vesicle uptake transporter called VMAT2. When amphetamine is taken up by VMAT2, the vesicle releases dopamine molecules into the cytosol in exchange. The redistributed dopamine is then believed to interact with DAT to promote reverse transport.[25] Amphetamine and amphetamine derivatives are also weak bases that accept protons, and can collapse acidic pH gradients in the vesicles that would otherwise provide free energy for neurotransmitter accumulation: the "weak base hypothesis" of amphetamine action suggests that collapse of this free energy contributes to redistribution of dopamine from very high (molar) concentrations in the vesicles to the cytosol.[26][34] Calcium may be a key molecule involved in the interactions between amphetamine and VMATs.[28]
The increase of cytosolic dopamine appears to trigger neurotoxicity, as dopamine readily auto-oxidizes, so that amphetamine or methamphetamine's increase in cytosolic dopamine can lead to oxidative stress in the cytosol that in turn promotes autophagy-related degradation of dopamine axons and dendrites.[35]
The second hypothesis of amphetamine action on the plasma membrane dopamine transporter postulates a direct interaction between amphetamine and the DAT. The activity of DAT is believed to depend on specific phosphorylating kinases, such as protein kinase c, specifically PKC-β.[31] Upon phosphorylation, DAT undergoes a conformational change that results in the transportation of DAT-bound dopamine from the extracellular to the intracellular environment.[30] In the presence of amphetamine, however, DAT has been observed to function in reverse, spitting dopamine out of the presynaptic neuron and into the synaptic cleft.[29] Thus, beyond inhibiting reuptake of dopamine, amphetamine also stimulates the release of dopamine molecules into the synapse.[21]
In support of the above hypothesis, it has been found that PKC-β inhibitors eliminate the effects of amphetamine on extracellular dopamine concentrations in the striatum of rats.[31] This data suggests that the PKC-β kinase may represent a key point of interaction between amphetamine and the DAT transporter.
Additional actions of amphetamine contribute to it's ability to release dopamine from neurons, including action as an inhibitor of monoamine oxidase, an enzyme responsible for dopamine breakdown in the cytosol; an ability to enhance dopamine synthesis apparently via actions on the enzyme tyrosine hydroxylase, which synthesizes the dopamine precursor L-DOPA; and some blockade of the DAT, an action that amphetamine shares with cocaine.[36] Due to the combination of these actions, amphetamine can release far more dopamine that can cocaine or other addictive drugs.[26][37]
Serotonin
Amphetamine has been found to exert similar effects on serotonin as on dopamine.[38] Like DAT, the serotonin transporter SERT can be induced to operate in reverse upon stimulation by amphetamine.[39] This mechanism is thought to rely on the actions of calcium ions, as well as on the proximity of certain transporter proteins.[39]
The interaction between amphetamine and serotonin is only apparent in particular regions of the brain, such as the mesocorticolimbic projection. Recent studies additionally postulate that amphetamine may indirectly alter the behavior of glutamatergic pathways extending from the ventral tegmental area to the prefrontal cortex.[38] Glutamatergic pathways are strongly correlated with increased excitability at the level of the synapse. Increased extracellular concentrations of serotonin may thus modulate the excitatory activity of glutamatergic neurons.[38]
The proposed ability of amphetamine to increase excitability of glutamatergic pathways may be of significance when considering serotonin-mediated addiction.[38] An additional behavioral consequence may be the stereotyped locomotor stimulation that occurs in response to amphetamine exposure.[27]
Other relevant neurotransmitters
Several other neurotransmitters have been linked to amphetamine activity. For instance, extracellular levels of glutamate, the primary excitatory neurotransmitter in the brain, have been shown to increase upon exposure to amphetamine. Consistent with other findings, this effect was found in the areas of the brain implicated in reward; namely, the nucleus accumbens, striatum, and prefrontal cortex. Additionally, several studies demonstrate increased levels of norepinephrine, a neurotransmitter related to adrenaline, in response to amphetamine. This is believed to occur via reuptake blockage as well as via interactions with the norepinephrine neuronal transport carrier.[40] The long-term effects of amphetamines use on neural development in children has not been well established.[41] Based on a study in rats, amphetamine use during adolescence may impair adult working memory.[42]
Pharmacology
Chemical properties
Amphetamine is a chiral compound. The racemic mixture can be divided into its optical isomers: levo- and dextro-amphetamine. Amphetamine is the parent compound of its own structural class, comprising a broad range of psychoactive derivatives, from empathogens, MDA (3,4-Methylenedioxyamphetamine) and MDMA (3,4-Methylenedioxy-N-methamphetamine) known as ecstasy, to the N-methylated form, methamphetamine known as 'meth', and to decongestants such as ephedrine (EPH) . Amphetamine is a homologue of phenethylamine.
At first, the medical drug came as the salt racemic-amphetamine sulfate (racemic-amphetamine contains both isomers in equal amounts). Attention disorders are often treated using Adderall or a generic equivalent, a formulation of mixed amphetamine and dextroamphetamine salts that contain
- 1/4 dextro-amphetamine saccharate
- 1/4 dextro-amphetamine sulfate
- 1/4 (racemic amphetamine) aspartate monohydrate
- 1/4 (racemic amphetamine) sulfate
Pharmacodynamics
Amphetamine has been shown to both diffuse through the cell membrane and travel via the dopamine transporter (DAT) to increase concentrations of dopamine in the neuronal terminal.
Amphetamine, both as d-amphetamine (dextroamphetamine) and l-amphetamine (or a racemic mixture of the two isomers), is believed to exert its effects by binding to the monoamine transporters and increasing extracellular levels of the biogenic amines dopamine, norepinephrine (noradrenaline) and serotonin. It is hypothesized that d-amphetamine acts primarily on the dopaminergic systems, while l-amphetamine is comparatively norepinephrinergic (noradrenergic). The primary reinforcing and behavioral-stimulant effects of amphetamine, however, are linked to enhanced dopaminergic activity, primarily in the mesolimbic dopamine system.
Amphetamine and other amphetamine-type stimulants principally act to release dopamine into the synaptic cleft. Amphetamine, unlike dopamine transporter inhibitor cocaine, acts as a substrate for DAT and slows reuptake by a secondary acting mechanism through the phosphorylation of dopamine transporters.[43] A primary action of amphetamine is mediated by vesicular monoamine transporters (VMATs); the transporters appear to provide a channel through which dopamine and other transmitters can exit the vesicle to the cytosol. According to the "weak base hypothesis" this is exacerbated by amphetamine acting to alkalinize the vesicle, which depletes the free energy favoring vesicle accummlation so that transmitter is redistributed to the cytosol. Together, these actions cause the release of dopamine, norepinephrine, and serotonin from monoamine vesicles, thereby increasing cytosolic concentrations of transmitter. This increase in concentration assists in the "reverse transport" of dopamine via the dopamine transporter (DAT) into the synapse.[44] In addition, amphetamine binds reversibly to the DATs and blocks the transporter's ability to clear DA from the synaptic space. Amphetamine also acts in this way with norepinephrine (noradrenaline) and to a lesser extent serotonin.
In addition, amphetamine binds to a group of receptors called Trace Amine Associated Receptors (TAAR).[45] TAAR are a newly discovered receptor system which seems to be affected by a range of amphetamine-like substances called trace amines.
History
Amphetamine was first synthesized in 1887 by the Romanian chemist Lazăr Edeleanu in Berlin, Germany.[46] He named the compound phenylisopropylamine. It was one of a series of compounds related to the plant derivative ephedrine, which had been isolated from Ma-Huang that same year by Nagayoshi Nagai.[47] No pharmacological use was found for amphetamine until 1927, when pioneer psychopharmacologist Gordon Alles resynthesized and tested it on himself, in search of an artificial replacement for ephedrine. From 1933 or 1934 Smith, Kline and French began selling the volatile base form of the drug as an inhaler under the trade name Benzedrine, useful as a decongestant but readily usable for other purposes.[48] One of the first attempts at using amphetamine as a scientific study was done by M. H. Nathanson, a Los Angeles physician, in 1935. He studied the subjective effects of amphetamine in 55 hospital workers who were each given 20 mg of Benzedrine. The two most commonly reported drug effects were "a sense of well being and a feeling of exhilaration" and "lessened fatigue in reaction to work".[49] During World War II amphetamine was extensively used to combat fatigue and increase alertness in soldiers. After decades of reported abuse, the FDA banned Benzedrine inhalers, and limited amphetamine to prescription use in 1965, but non-medical use remained common. Amphetamine became a schedule II drug under the Controlled Substances Act in 1971.
The related compound methamphetamine was first synthesized from ephedrine in Japan in 1920 by chemist Akira Ogata, via reduction of ephedrine using red phosphorus and iodine. The pharmaceutical Pervitin was a tablet of 3 mg methamphetamine which was available in Germany from 1938 and widely used in the Wehrmacht, but by mid-1941 it became a controlled substance, partly because of the amount of time needed for a soldier to rest and recover after use and partly because of abuse. For the rest of the war, military doctors continued to issue the drug, but less frequently and with increasing discrimination.[50]
In 1997 and 1998,[51][52] researchers at Texas A&M University claimed to have found amphetamine and methamphetamine in the foliage of two Acacia species native to Texas, A. berlandieri and A. rigidula. Previously, both of these compounds had been thought to be human inventions. These findings have never been duplicated, and the analyses are believed by many biochemists to be the result of experimental error, and as such the validity of the report has come into question. Alexander Shulgin, one of the most experienced biochemical investigators and the discoverer of many new psychotropic substances, has tried to contact the Texas A&M researchers and verify their findings. The authors of the paper have not responded; natural amphetamine remains an unconfirmed discovery.[53]
Performance-enhancing use
Adderall, an amphetamine mixture, is used by some college and high-school students as a study and test-taking aid.[54] Amphetamine works by increasing energy levels, concentration, and motivation, thus allowing students to study for an extended period of time.
Amphetamine has been, and is still, used by militaries around the world. British troops used 72 million amphetamine tablets in the second world war[55] and the RAF used so many that "Methedrine won the Battle of Britain" according to one report.[56] American bomber pilots use amphetamine ("go pills") to stay awake during long missions. The Tarnak Farm incident, in which an American F-16 pilot killed several friendly Canadian soldiers on the ground, was blamed by the pilot on his use of amphetamine.[57] A nonjudicial hearing rejected the pilot's claim.[citation needed]
Amphetamine is also used by some professional,[58] collegiate[59] and high school[59] athletes for its strong stimulant effect. Energy levels are perceived to be dramatically increased and sustained, which is believed to allow for more vigorous and longer play. However, at least one study has found that this effect is not measurable.[60] The use of amphetamine during strenuous physical activity can be extremely dangerous, especially when combined with alcohol, and athletes have died as a result, for example, British cyclist Tom Simpson.
Amphetamine use has historically been especially common among Major League Baseball players and is usually known by the slang term "greenies".[61] In 2006, the MLB banned the use of amphetamine. The ban is enforced through periodic drug-testing. However, the MLB has received some criticism because the consequences for amphetamine use are dramatically less severe than for anabolic steroid use, with the first offense bringing only a warning and further testing.[62][63][64]
Amphetamine was formerly in widespread use by truck drivers[65] to combat symptoms of somnolence and to increase their concentration during driving, especially in the decades prior to the signing by former president Ronald Reagan of Executive Order 12564, which initiated mandatory random drug testing of all truck drivers and employees of other DOT-regulated industries. Although implementation of the order on the trucking industry was kept to a gradual rate in consideration of its projected effects on the national economy, in the decades following the order, amphetamine and other drug abuse by truck drivers has since dropped drastically. (See also Truck driver—Implementation of drug detection).
Detection in body fluids
Amphetamine is frequently measured in urine as part of a drug abuse testing program, in plasma or serum to confirm a diagnosis of poisoning in hospitalized victims, or in whole blood to assist in the forensic investigation of a traffic or other criminal violation or a case of sudden death. Techniques such as immunoassay may cross-react with a number of sympathomimetics drugs, so chromatographic methods specific for amphetamine should be employed to prevent false positive results. Chiral techniques may be employed to help distinguish the source of the drug, whether obtained legally (via prescription) or illicitly, or possibly as a result of formation from a prodrug such as lisdexamfetamine or selegiline. Chiral separation is needed to assess the possible contribution of l-methamphetamine (Vicks Inhaler) toward a positive test result.[66][67][68]
Society and culture
From the 1960s onward, amphetamine has been popular with many youth subcultures in Britain (and other parts of the world) as a recreational drug. It has been commonly used by mods, skinheads, punks, goths, gangsters, and casuals in all night soul and ska dances, punk concerts, basement shows and fighting on the terraces by casuals. [citation needed]
The hippie counterculture was very critical of amphetamines due to the behaviors they cause; in an interview with the Los Angeles Free Press in 1965, beat writer Allen Ginsberg commented that "Speed is antisocial, paranoid making, it's a drag... all the nice gentle dope fiends are getting screwed up by the real horror monster Frankenstein speed freaks who are going round stealing and bad-mouthing everybody".[69]
In literature
The writers of the Beat Generation used amphetamine extensively, mainly under the Benzedrine brand name. Jack Kerouac was a particularly avid user of amphetamine, which was said to provide him with the stamina needed to work on his novels for extended periods of time.[70]
Scottish author Irvine Welsh often portrays drug use in his novels, though in one of his journalism works he comments on how drugs (including amphetamine) have become part of consumerism and how his novels Trainspotting and Porno reflect the changes in drug use and culture during the years that elapse between the two texts.[71]
Amphetamine is frequently mentioned in the work of American journalist Hunter S. Thompson. Speed appears not only amongst the inventory of drugs Thompson consumed for what could broadly be defined as recreational purposes, but also receives frequent, explicit mention as an essential component of his writing toolkit,[72] such as in his "Author's Note" in Fear and Loathing on the Campaign Trail '72.[73]
"One afternoon about three days ago [the publishers] showed up at my door with no warning, and loaded about forty pounds of supplies into the room: two cases of Mexican beer, four quarts of gin, a dozen grapefruits, and enough speed to alter the outcome of six Super Bowls. ... Meanwhile, [...] with the final chapter still unwritten and the presses scheduled to start rolling in twenty-four hours . . . . unless somebody shows up pretty soon with extremely powerful speed, there might not be a final chapter. About four fingers of king-hell Crank would do the trick, but I am not optimistic."
In mathematics
Famous mathematician Paul Erdős took amphetamine, and once won a bet from his friend Ron Graham, who bet him $500 that he could not stop taking the drug for a month.[74] Erdős won the bet, but complained during his abstinence that mathematics had been set back by a month: "Before, when I looked at a piece of blank paper my mind was filled with ideas. Now all I see is a blank piece of paper." After he won the bet, he promptly resumed his amphetamine habit.
In music
Many songs have been written about amphetamine, for example in the track entitled "St. Ides Heaven" from singer/songwriter, Elliott Smith's self-titled album. Semi Charmed Life by Third Eye Blind also references amphetamine. Another blatant example would be the song simply labelled "Amphetamine" by Alternative rock band Everclear, and the song "20 Dollar nose bleed" by the Pop-rock band Fall Out Boy. It has also influenced the aesthetics of many rock'n'roll bands (especially in the garage rock, mod R&B, death rock, punk/hardcore, gothic rock and extreme heavy metal genres). Hüsker Dü, Jesus and Mary Chain's and The Who were keen amphetamine users early in their existence. Land Speed Record is an allusion to Hüsker Dü's amphetamine use. [citation needed] Amphetamine was widely abused in the 1980s underground punk-rock scene. Pop-punk band NOFX have incorporated references to Amphetamines and other stimulants, the two most obvious being the song "Three on Speed" from the "Surfer" 8" LP (in reference to the three guys being on Amphetamine while recording the album), and earlier the album "The Longest Line" is in reference to a "line" of Amphetamine ready for insufflation. The Rolling Stones referenced the drug in their song "Can't You Hear Me Knocking" on the album Sticky Fingers ("Y'all got cocaine eyes / Yeah, ya got speed-freak jive now"). Lou Reed refers explicitly to the drug on his album Berlin, in the song "How Do You Think It Feels?". Reed's band The Velvet Underground, a creation of Andy Warhol's Factory Years, was fueled by amphetamines, as well as naming their second album White Light/White Heat after the drug and making reference to the song in "Sister Ray.".
Many rock'n'roll bands have named themselves after amphetamine and drug slang surrounding it. For example Mod revivalists, The Purple Hearts named themselves after the amphetamine tablets popular with mods during the 1960s, as did the Australian band of the same name during the mid-1960s. [citation needed] The Amphetameanies, a ska-punk band, are also named after amphetamine, but also imitate its effects. Dexy's Midnight Runners, of number one hit "Come On Eileen", are named after Dexedrine. Motörhead derived their name from the British slang for 'speed freak' and Motorhead's Lemmy Kilmister is a long-term user of speed.
In film
This article contains a list of miscellaneous information. (December 2010) |
Producer David O. Selznick was an amphetamine user, and would often dictate long and rambling memos under the influence of amphetamine to his directors.[75] The documentary Shadowing The Third Man relates that Selznick introduced The Third Man director Carol Reed to the use of amphetamine, which allowed Reed to bring the picture in below budget and on schedule by filming nearly 22 hours at a time.[76]
Garrett Scott's documentary Cul-de-Sac: A Suburban War Story has a brief history of the manufacture and spread of amphetamine, and of its effects.[77]
In the film Requiem for a Dream, Ellen Burstyn portrays Sara Goldfarb, an elderly widow who becomes addicted to weight-loss amphetamine pills. After suffering from amphetamine psychosis, she is hospitalized against her will, undergoes electro-convulsive therapy, and later on was confined at a mental asylum.[78]
The title of the 2009 movie Amphetamine plays on the double meaning of the word in Chinese - besides the name for the drug it also means 'isn't this his fate?' which figuratively ties to the movie's plot. The word is transliterated as 安 非 他 命 - "ān fēi tā mìng" - and as commonly happens with transliteration of non-Chinese terms each character has independent meaning as an individual unrelated word.
In the 1972 film Ciao! Manhattan, Edie Sedgwick portrays Susan Superstar, a fictional version of herself, who discusses her addiction with drugs, mainly amphetamines. In one particular scene, she talks about the exhilaration of her drug addiction in the infamous "Speed Monologue".[79]
In the 2005 Oscar winner Walk the Line Joaquin Phoenix portrays John Cash, an uprising star in the music industry. He becomes addicted to amphetamines and eventually gets caught trying to cross borders with them.
In the film Empire Records Liv Tyler's character admits to having an amphetamine addiction.
Legal status
- In the United Kingdom, amphetamines are regarded as Class B drugs. The maximum penalty for unauthorized possession is five years in prison and an unlimited fine. The maximum penalty for illegal supply is 14 years in prison and an unlimited fine. Methamphetamine has recently been reclassified to Class A, penalties for possession of which are more severe (7 years in prison and an unlimited fine).[80]
- In the Netherlands, amphetamine and methamphetamine are List I drugs of the Opium Law, but the dextro isomer of amphetamine is indicated for ADD/ADHD and narcolepsy and available for prescription as 5 and 10 mg generic tablets, and 5 and 10 mg gel capsules.
- In the United States, amphetamine and methamphetamine are Schedule II drugs, classified as CNS (central nervous system) stimulants.[81] A Schedule II drug is classified as one that has a high potential for abuse, has a currently-accepted medical use and is used under severe restrictions, and has a high possibility of severe psychological and physiological dependence.
- In Canada, possession of amphetamines is a criminal offence under Schedule III of the Controlled Drugs and Substances Act, with a maximum penalty for repeat offenders of fines of up to $2,000, imprisonment for up to one year, or both.[82]
Internationally, amphetamine is a Schedule II drug under the Convention on Psychotropic Substances.[83]
Prodrugs
A number of substances have been shown to produce amphetamine and/or methamphetamine as metabolites, including amfecloral, amphetaminil, benzphetamine, clobenzorex, dimethylamphetamine, ethylamphetamine, famprofazone, fencamine, fenethylline, fenproporex, furfenorex, lisdexamfetamine, mefenorex, mesocarb, prenylamine, propylamphetamine, and selegiline, among others.[84][85] These compounds may produce positive results for amphetamine on drug tests.[84][85]
Derivatives
Amphetamine derivatives are a class of potent drugs that act by increasing levels of dopamine and norepinephrine in the brain, inducing euphoria.[86][87][88] The class includes prescription CNS drugs commonly used to treat attention-deficit hyperactivity disorder (ADHD). It is also used to treat symptoms of traumatic brain injury (TBI) and the daytime drowsiness symptoms of narcolepsy, postural orthostatic tachycardia syndrome (POTS) and chronic fatigue syndrome (CFS).
References and notes
- ^ "FDA-sourced list of all drugs with black box warnings (Use Download Full Results and View Query links.)". nctr-crs.fda.gov. FDA. Retrieved 22 Oct 2023.
- ^ Miranda-G E, Sordo M, Salazar AM (2007). "Determination of amphetaminoe, methamphetamine, and hydroxyamphetamine derivatives in urine by gas chromatography-mass spectrometry and its relation to CYP2D6 phenotype of drug users". J Anal Toxicol. 31 (1): 31–6. PMID 17389081.
{{cite journal}}
: CS1 maint: multiple names: authors list (link) - ^ Drug Test FAQ | Craig Medical Distribution, Inc.
- ^ European Monitoring Centre for Drugs and Drug Addiction (2008). Annual report: the state of the drugs problem in Europe (PDF). Luxembourg: Office for Official Publications of the European Communities. p. 48. ISBN 978-92-9168-324-6.
- ^ Nutt, D; King, LA; Saulsbury, W; Blakemore, C (2007). "Development of a rational scale to assess the harm of drugs of potential misuse". Lancet. 369 (9566): 1047–53. doi:10.1016/S0140-6736(07)60464-4. PMID 17382831.
- ^ Erowid Amphetamines Vault | Effects
- ^ Amphetamine; Facts | Alcoholism and Drug Addiction Research Foundation, Toronto Canada
- ^ Amphetamines | Better Health Channel
- ^ Dextroamphetamine (Oral Route) | MayoClinic.com
- ^ Vitiello B (2008). "Understanding the risk of using medications for attention deficit hyperactivity disorder with respect to physical growth and cardiovascular function". Child Adolesc Psychiatr Clin N Am. 17 (2): 459–74, xi. doi:10.1016/j.chc.2007.11.010. PMC 2408826. PMID 18295156.
- ^ Ricaurte GA, Mechan AO, Yuan J; et al. (2005). "Amphetamine treatment similar to that used in the treatment of adult attention-deficit/hyperactivity disorder damages dopaminergic nerve endings in the striatum of adult nonhuman primates" (PDF). J. Pharmacol. Exp. Ther. 315 (1): 91–8. doi:10.1124/jpet.105.087916. PMID 16014752. Retrieved 28 March 2011.
{{cite journal}}
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(help); Unknown parameter|month=
ignored (help)CS1 maint: multiple names: authors list (link) - ^ Erowid Amphetamines Vault: Effects
- ^ Amphetamines | Merck Sharp & Dohme Corp.
- ^ Symptoms of Amphetamine withdrawal | WrongDiagnosis.com
- ^ eMedTV | Dextroamphetamine Withdrawals
- ^ Drug Abuse Help | Dexedrine Information
- ^ Amphetamine Disease Interactions - Drugs.com
- ^ "ADDERALL XR capsule" (PDF). 2005. Retrieved 2009-07-24.
{{cite web}}
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missing|last=
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value (help) - ^ "Amphetamines: Drug Use and Abuse: Merck Manual Home Edition". Merck. Archived from the original on February 17, 2007. Retrieved February 28, 2007.
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instead. - ^ a b Kuczenski R, Segal DS (1997). "Effects of methylphenidate on extracellular dopamine, serotonin, and norepinephrine: comparison with amphetamine". J. Neurochem. 68 (5): 2032–7. doi:10.1046/j.1471-4159.1997.68052032.x. PMID 9109529.
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ignored (help)CS1 maint: multiple names: authors list (link) - ^ a b c "A mechanism for amphetamine-induced dopamine overload". PLoS Biology. 2 (3): e87. 2004. doi:10.1371/journal.pbio.0020087. PMC 368179.
{{cite journal}}
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|pmid=7751968
instead. - ^ Attention: This template ({{cite pmid}}) is deprecated. To cite the publication identified by PMID 19409267, please use {{cite journal}} with
|pmid=19409267
instead. - ^ Attention: This template ({{cite pmid}}) is deprecated. To cite the publication identified by PMID 2268433, please use {{cite journal}} with
|pmid=2268433
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|pmid=12388602
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|pmid=15955613
instead. - ^ Attention: This template ({{cite pmid}}) is deprecated. To cite the publication identified by PMID 11487614, please use {{cite journal}} with
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instead. - ^ a b c d Jones S, Kauer JA (1999). "Amphetamine depresses excitatory synaptic transmission via serotonin receptors in the ventral tegmental area". J. Neurosci. 19 (22): 9780–7. PMID 10559387.
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- ^ "Amphetamine use in adolescence may impair adult working memory". Retrieved 2009-10-22.
- ^ WikiAnswers google cached page: 'Does Namenda memantine work in preventing tolerance to adderall ADD amphetamine type drugs?'
- ^ Sulzer D, Sonders MS, Poulsen NW, Galli A (2005). "Mechanisms of neurotransmitter release by amphetamines: a review". Prog. Neurobiol. 75 (6): 406–33. doi:10.1016/j.pneurobio.2005.04.003. PMID 15955613.
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- ^ Rasmussen, Nicolas (2008). "Ch. 4". On Speed: The Many Lives of Amphetamine. New York, New York: New York University Press. ISBN 0-8147-7601-9.
- ^ Clement B.A., Goff C.M., Forbes T.D.A. (1998). "Toxic amines and alkaloids from Acacia rigidula". Phytochemistry. 49 (5): 1377–1380. doi:10.1016/S0031-9422(97)01022-4.
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: CS1 maint: multiple names: authors list (link) - ^ Ask Dr. Shulgin Online: Acacias and Natural Amphetamine
- ^ Twohey, Megan (2006-03-25). "Pills become an addictive study aid". JS Online. Archived from the original on 2007-08-15. Retrieved 2007-12-02.
- ^ De Mondenard, Dr Jean-Pierre: Dopage, l'imposture des performances, Chiron, France, 2000
- ^ Grant, D.N.W.; Air Force, UK, 1944
- ^ "Air force rushes to defend amphetamine use". The Age. January 18, 2003. Retrieved 26 January 2009.
- ^ Yesalis, Charles E.; Bahrke, Michael (2005-12). "Anabolic Steroid and Stimulant Use in North American Sport between 1850 and 1980". Sport in History. 25 (3): 434–451. doi:10.1080/17460260500396251. Retrieved 2007-12-02.
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(help) - ^ a b National Collegiate Athletic Association (2006-01), NCAA Study of Substance Use Habits of College Student-Athletes (PDF), National Collegiate Athletic Association, pp. 2–4, 11–13, retrieved 2007-12-02
{{citation}}
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(help) - ^ Margaria, R; Aghemo, P.; Rovelli, E. (1964-07-01). "The effect of some drugs on the maximal capacity of athletic performance in man". European Journal of Applied Physiology. 20 (4): 281–287. doi:10.1007/BF00697020. PMID 14252788.
- ^ Frias, Carlos (2006-04-02). "Baseball and amphetamines". Palm Beach Post. Retrieved 2007-12-02.
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This study has provided the first objective data regarding the use of potentially abusive drugs by tractor-trailer drivers... Prescription stimulants, such as amphetamine, methamphetamine, and phentermine were found in 5 percent of the [317] drivers [who participated in the study], often in combination with similar but less potent stimulants, such as phenylpropanolamine. Nonprescription stimulants were detected in 12 percent of the drivers, about half of whom gave no medical explanation for their presence... One limitation of these findings is that 12 percent of the randomly selected drivers refused to participate in the study or provided insufficient urine and blood for testing; the distribution of drugs among these 42 drivers is unknown... Finally, the results apply to tractor-trailer drivers operating on a major east-west interstate route in Tennessee. Drug incidence among other truck-driver populations are unknown and may be higher or lower than reported here. (64)
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suggested) (help) - ^ Verstraete AG, Heyden FV (2005). "Comparison of the sensitivity and specificity of six immunoassays for the detection of amphetamines in urine". J Anal Toxicol. 29 (5): 359–64. PMID 16105261.
- ^ Paul BD, Jemionek J, Lesser D, Jacobs A, Searles DA (2004). "Enantiomeric separation and quantitation of (+/-)-amphetamine, (+/-)-methamphetamine, (+/-)-MDA, (+/-)-MDMA, and (+/-)-MDEA in urine specimens by GC-EI-MS after derivatization with (R)-(-)- or (S)-(+)-alpha-methoxy-alpha-(trifluoromethy)phenylacetyl chloride (MTPA)". J Anal Toxicol. 28 (6): 449–55. PMID 15516295.
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ignored (help)CS1 maint: multiple names: authors list (link) - ^ R. Baselt, Disposition of Toxic Drugs and Chemicals in Man, 8th edition, Biomedical Publications, Foster City, CA, 2008, pp. 83-86.
- ^ Brecher, Edward M. (1972). "How speed was popularized". The Consumers Union Report on Licit and Illicit Drugs. Schaffer Drug Library. Retrieved 1 June 2010.
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- ^ Welsh, Irvine (2006-08-10). "Drug Cultures in Trainspotting and Porno". irvinewelsh.net. Retrieved 2008-10-13.
- ^ Carr, David (29 June 2008). "Fear and Loathing on a Documentary Screen". New York Times. pp. AR7. Retrieved 18 March 2009.
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(help) - ^ Thompson, Hunter S. (1973). Fear and Loathing on the Campaign Trail '72. New York: Warner Books. pp. 15–16, 21. ISBN 0-446-31364-5.
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- ^ Cul-de-Sac, http://www.imdb.com/title/tt0317273/
- ^ Resurrection (1980) - IMDb
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- ^ a b Musshoff F (2000). "Illegal or legitimate use? Precursor compounds to amphetamine and methamphetamine". Drug Metabolism Reviews. 32 (1): 15–44. doi:10.1081/DMR-100100562. PMID 10711406.
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ignored (help) - ^ a b Cody JT (2002). "Precursor medications as a source of methamphetamine and/or amphetamine positive drug testing results". Journal of Occupational and Environmental Medicine / American College of Occupational and Environmental Medicine. 44 (5): 435–50. PMID 12024689.
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ignored (help) - ^ Drevets, W; et al. (2001). "Amphetamine-Induced Dopamine Release in Human Ventral Striatum Correlates with Euphoria" (PDF). Psychiatry. 49: 81–96. Retrieved 23 May 2009.
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(help) - ^ Rang and Dale, Pharmacology
- ^ Schep LJ, Slaughter RJ, Beasley DM (2010). "The clinical toxicology of metamfetamine". Clinical Toxicology (Philadelphia, Pa.). 48 (7): 675–94. doi:10.3109/15563650.2010.516752. ISSN 1556-3650. PMID 20849327.
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External links
- CID 5826 from PubChem (D-form—dextroamphetamine)
- CID 3007 from PubChem (L-form and D, L-forms)
- CID 32893 from PubChem (L-form—Levamphetamine or L-amphetamine)
- List of 504 Compounds Similar to Amphetamine (PubChem)
- EMCDDA drugs profile: Amphetamine (2007)
- Drugs.com - Amphetamine
- Asia & Pacific Amphetamine-Type Stimulants Information Centre
- U.S. National Library of Medicine: Drug Information Portal - Amphetamine
- Articles with trivia sections from December 2010
- Amphetamines
- Anorectics
- Bronchodilators
- German inventions
- Monoamine oxidase inhibitors
- Dopamine agonists
- Norepinephrine-dopamine reuptake inhibitors
- Serotonin receptor agonists
- Drugs acting on the nervous system
- Drugs acting on the cardiovascular system
- Euphoriants
- Youth culture in the United Kingdom