Amphetamine: Difference between revisions

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Psychological: Moderate^[3]Amphetamine Medical: Oral, intravenous^[4]
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Amphetamine^{[note 2]} (contracted from alpha-methylphenethylamine) is a central nervous system (CNS) stimulant that is used in the treatment of attention deficit hyperactivity disorder (ADHD), narcolepsy, and obesity; it is also used to treat binge eating disorder in the form of its inactive prodrug lisdexamfetamine. Amphetamine was discovered as a chemical in 1887 by Lazăr Edeleanu, and then as a drug in the late 1920s. It exists as two enantiomers:^{[note 3]} levoamphetamine and dextroamphetamine. Amphetamine properly refers to a specific chemical, the racemic free base, which is equal parts of the two enantiomers in their pure amine forms. The term is frequently used informally to refer to any combination of the enantiomers, or to either of them alone. Historically, it has been used to treat nasal congestion and depression. Amphetamine is also used as an athletic performance enhancer and cognitive enhancer, and recreationally as an aphrodisiac and euphoriant. It is a prescription drug in many countries, and unauthorized possession and distribution of amphetamine are often tightly controlled due to the significant health risks associated with recreational use.^{[sources 1]}

The first amphetamine pharmaceutical was Benzedrine, a brand which was used to treat a variety of conditions. Pharmaceutical amphetamine is prescribed as racemic amphetamine, Adderall,^{[note 4]} dextroamphetamine, or the inactive prodrug lisdexamfetamine. Amphetamine increases monoamine and excitatory neurotransmission in the brain, with its most pronounced effects targeting the norepinephrine and dopamine neurotransmitter systems.^{[sources 2]}

At therapeutic doses, amphetamine causes emotional and cognitive effects such as euphoria, change in desire for sex, increased wakefulness, and improved cognitive control. It induces physical effects such as improved reaction time, fatigue resistance, decreased appetite, elevated heart rate, and increased muscle strength. Larger doses of amphetamine may impair cognitive function and induce rapid muscle breakdown. Addiction is a serious risk with heavy recreational amphetamine use, but is unlikely to occur from long-term medical use at therapeutic doses. Very high doses can result in psychosis (e.g., hallucinations, delusions and paranoia) which rarely occurs at therapeutic doses even during long-term use. Recreational doses are generally much larger than prescribed therapeutic doses and carry a far greater risk of serious side effects.^{[sources 3]}

Amphetamine belongs to the phenethylamine class. It is also the parent compound of its own structural class, the substituted amphetamines,^{[note 5]} which includes prominent substances such as bupropion, cathinone, MDMA, and methamphetamine. As a member of the phenethylamine class, amphetamine is also chemically related to the naturally occurring trace amine neuromodulators, specifically phenethylamine and N-methylphenethylamine, both of which are produced within the human body. Phenethylamine is the parent compound of amphetamine, while N-methylphenethylamine is a positional isomer of amphetamine that differs only in the placement of the methyl group.^{[sources 4]}

Uses

Medical

Amphetamine is used to treat attention deficit hyperactivity disorder (ADHD), narcolepsy, obesity, and, in the form of lisdexamfetamine, binge eating disorder.^[3]^[20]^[21] It is sometimes prescribed off-label for its past medical indications, particularly for depression and chronic pain.^[3]^[38]

ADHD

Long-term amphetamine exposure at sufficiently high doses in some animal species is known to produce abnormal dopamine system development or nerve damage,^[39]^[40] but, in humans with ADHD, long-term use of pharmaceutical amphetamines at therapeutic doses appears to improve brain development and nerve growth.^[41]^[42]^[43] Reviews of magnetic resonance imaging (MRI) studies suggest that long-term treatment with amphetamine decreases abnormalities in brain structure and function found in subjects with ADHD, and improves function in several parts of the brain, such as the right caudate nucleus of the basal ganglia.^[41]^[42]^[43]

Reviews of clinical stimulant research have established the safety and effectiveness of long-term continuous amphetamine use for the treatment of ADHD.^[30]^[44]^[45] Randomized controlled trials of continuous stimulant therapy for the treatment of ADHD spanning 2 years have demonstrated treatment effectiveness and safety.^[30]^[44] Two reviews have indicated that long-term continuous stimulant therapy for ADHD is effective for reducing the core symptoms of ADHD (i.e., hyperactivity, inattention, and impulsivity), enhancing quality of life and academic achievement, and producing improvements in a large number of functional outcomes^{[note 6]} across 9 categories of outcomes related to academics, antisocial behavior, driving, non-medicinal drug use, obesity, occupation, self-esteem, service use (i.e., academic, occupational, health, financial, and legal services), and social function.^[30]^[45] Additionally, a 2024 meta-analytic systematic review reported moderate improvements in quality of life when amphetamine treatment is used for ADHD.^[47] One review highlighted a nine-month randomized controlled trial of amphetamine treatment for ADHD in children that found an average increase of 4.5 IQ points, continued increases in attention, and continued decreases in disruptive behaviors and hyperactivity.^[44] Another review indicated that, based upon the longest follow-up studies conducted to date, lifetime stimulant therapy that begins during childhood is continuously effective for controlling ADHD symptoms and reduces the risk of developing a substance use disorder as an adult.^[30]

Models of ADHD suggest that it is associated with functional impairments in some of the brain's neurotransmitter systems;^[48] these functional impairments involve impaired dopamine neurotransmission in the mesocorticolimbic projection and norepinephrine neurotransmission in the noradrenergic projections from the locus coeruleus to the prefrontal cortex.^[48] Stimulants like methylphenidate and amphetamine are effective in treating ADHD because they increase neurotransmitter activity in these systems.^[11]^[48]^[49] Approximately 80% of those who use these stimulants see improvements in ADHD symptoms.^[50] Children with ADHD who use stimulant medications generally have better relationships with peers and family members, perform better in school, are less distractible and impulsive, and have longer attention spans.^[51]^[52] The Cochrane reviews^{[note 7]} on the treatment of ADHD in children, adolescents, and adults with pharmaceutical amphetamines stated that short-term studies have demonstrated that these drugs decrease the severity of symptoms, but they have higher discontinuation rates than non-stimulant medications due to their adverse side effects.^[54]^[55] However, a 2025 meta-analytic systematic review of 113 randomized controlled trials found that stimulant medications were the only intervention with robust short-term efficacy, and were associated with lower all-cause treatment discontinuation rates than non-stimulant medications (e.g., atomoxetine).^{[note 8]}^[56] A Cochrane review on the treatment of ADHD in children with tic disorders such as Tourette syndrome indicated that stimulants in general do not make tics worse, but high doses of dextroamphetamine could exacerbate tics in some individuals.^[57]

Binge eating disorder

Binge eating disorder (BED) is characterized by recurrent and persistent episodes of compulsive binge eating.^[58] These episodes are often accompanied by marked distress and a feeling of loss of control over eating.^[58] The pathophysiology of BED is not fully understood, but it is believed to involve dysfunctional dopaminergic reward circuitry along the cortico-striatal-thalamic-cortical loop.^[59]^[60] As of July 2024, lisdexamfetamine is the only USFDA- and TGA-approved pharmacotherapy for BED.^[21]^[61] Evidence suggests that lisdexamfetamine's treatment efficacy in BED is underpinned at least in part by a psychopathological overlap between BED and ADHD, with the latter conceptualized as a cognitive control disorder that also benefits from treatment with lisdexamfetamine.^[59]^[60]

Diagram of TAAR1 organ-specific expression and function

This diagram illustrates how TAAR1 activation induces incretin-like effects through the release of gastrointestinal hormones and influences food intake, blood glucose levels, and insulin release.^[62] TAAR1 expression in the periphery is indicated with "x".^[62]

Lisdexamfetamine's therapeutic effects for BED primarily involve direct action in the central nervous system after conversion to its pharmacologically active metabolite, dextroamphetamine.^[61] Centrally, dextroamphetamine increases neurotransmitter activity of dopamine and norepinephrine in prefrontal cortical regions that regulate cognitive control of behavior.^[59]^[61] Similar to its therapeutic effect in ADHD, dextroamphetamine enhances cognitive control and may reduce impulsivity in patients with BED by enhancing the cognitive processes responsible for overriding prepotent feeding responses that precede binge eating episodes.^[59]^[63]^[64] In addition, dextroamphetamine's actions outside of the central nervous system may also contribute to its treatment effects in BED. Peripherally, dextroamphetamine triggers lipolysis through noradrenergic signaling in adipose fat cells, leading to the release of triglycerides into blood plasma to be utilized as a fuel substrate.^[60]^[65] Dextroamphetamine also activates TAAR1 in peripheral organs along the gastrointestinal tract that are involved in the regulation of food intake and body weight.^[62] Together, these actions confer an anorexigenic effect that promotes satiety in response to feeding and may decrease binge eating as a secondary effect.^[64]^[62] While lisdexamfetamine's anorexigenic effects contribute to its efficacy in BED, evidence indicates that the enhancement of cognitive control is necessary and sufficient for addressing the disorder's underlying psychopathology.^[59]^[66] This view is supported by the failure of anti-obesity medications and other appetite suppressants to significantly reduce BED symptom severity, despite their capacity to induce weight loss.^[66]

Medical reviews of randomized controlled trials have demonstrated that lisdexamfetamine, at doses between 50–70 mg, is safe and effective for the treatment of moderate-to-severe BED in adults.^{[sources 5]} These reviews suggest that lisdexamfetamine is persistently effective at treating BED and is associated with significant reductions in the number of binge eating days and binge eating episodes per week.^{[sources 5]} Furthermore, a meta-analytic systematic review highlighted an open-label, 12-month extension safety and tolerability study that reported lisdexamfetamine remained effective at reducing the number of binge eating days for the duration of the study.^[64] In addition, both a review and a meta-analytic systematic review found lisdexamfetamine to be superior to placebo in several secondary outcome measures, including persistent binge eating cessation, reduction of obsessive-compulsive related binge eating symptoms, reduction of body-weight, and reduction of triglycerides.^[60]^[64] Lisdexamfetamine, like all pharmaceutical amphetamines, has direct appetite suppressant effects that may be therapeutically useful in both BED and its comorbidities.^[21]^[64] Based on reviews of neuroimaging studies involving BED-diagnosed participants, therapeautic neuroplasticity in dopaminergic and noradrenergic pathways from long-term use of lisdexamfetamine may be implicated in lasting improvements in the regulation of eating behaviors that are observed.^[21]^[61]^[64]

Narcolepsy

Narcolepsy is a chronic sleep-wake disorder that is associated with excessive daytime sleepiness, cataplexy, and sleep paralysis.^[68] Patients with narcolepsy are diagnosed as either type 1 or type 2, with only the former presenting cataplexy symptoms.^[69] Type 1 narcolepsy results from the loss of approximately 70,000 orexin-releasing neurons in the lateral hypothalamus, leading to significantly reduced cerebrospinal orexin levels;^[70]^[71] this reduction is a diagnostic biomarker for type 1 narcolepsy.^[69] Lateral hypothalamic orexin neurons innervate every component of the ascending reticular activating system (ARAS), which includes noradrenergic, dopaminergic, histaminergic, and serotonergic nuclei that promote wakefulness.^[71]^[72]

Amphetamine’s therapeutic mode of action in narcolepsy primarily involves increasing monoamine neurotransmitter activity in the ARAS.^[70]^[73]^[74] This includes noradrenergic neurons in the locus coeruleus, dopaminergic neurons in the ventral tegmental area, histaminergic neurons in the tuberomammillary nucleus, and serotonergic neurons in the dorsal raphe nucleus.^[72]^[74] Dextroamphetamine, the more dopaminergic enantiomer of amphetamine, is particularly effective at promoting wakefulness because dopamine release has the greatest influence on cortical activation and cognitive arousal, relative to other monoamines.^[70] In contrast, levoamphetamine may have a greater effect on cataplexy, a symptom more sensitive to the effects of norepinephrine and serotonin.^[70] Noradrenergic and serotonergic nuclei in the ARAS are involved in the regulation of the REM sleep cycle and function as "REM-off" cells, with amphetamine's effect on norepinephrine and serotonin contributing to the suppression of REM sleep and a possible reduction of cataplexy at high doses.^[70]^[69]^[72]

The American Academy of Sleep Medicine (AASM) 2021 clinical practice guideline conditionally recommends dextroamphetamine for the treatment of both type 1 and type 2 narcolepsy.^[75] Treatment with pharmaceutical amphetamines is generally less preferred relative to other stimulants (e.g., modafinil) and is considered a third-line treatment option.^[33]^[76]^[77] Medical reviews indicate that amphetamine is safe and effective for the treatment of narcolepsy.^[70]^[33]^[75] Amphetamine appears to be most effective at improving symptoms associated with hypersomnolence, with three reviews finding clinically significant reductions in daytime sleepiness in patients with narcolepsy.^[70]^[33]^[75] Additionally, these reviews suggest that amphetamine may dose-dependently improve cataplexy symptoms.^[70]^[33]^[75] However, the quality of evidence for these findings is low and is consequently reflected in the AASM's conditional recommendation for dextroamphetamine as a treatment option for narcolepsy.^[75]

Enhancing performance

Cognitive performance

In 2015, a systematic review and a meta-analysis of high quality clinical trials found that, when used at low (therapeutic) doses, amphetamine produces modest yet unambiguous improvements in cognition, including working memory, long-term episodic memory, inhibitory control, and some aspects of attention, in normal healthy adults;^[78]^[79] these cognition-enhancing effects of amphetamine are known to be partially mediated through the indirect activation of both dopamine D₁ receptor and α₂-adrenergic receptor in the prefrontal cortex.^[11]^[78] A systematic review from 2014 found that low doses of amphetamine also improve memory consolidation, in turn leading to improved recall of information.^[80] Therapeutic doses of amphetamine also enhance cortical network efficiency, an effect which mediates improvements in working memory in all individuals.^[11]^[81] Amphetamine and other ADHD stimulants also improve task saliency (motivation to perform a task) and increase arousal (wakefulness), in turn promoting goal-directed behavior.^[11]^[82]^[83] Stimulants such as amphetamine can improve performance on difficult and boring tasks and are used by some students as a study and test-taking aid.^[11]^[83]^[84] Based upon studies of self-reported illicit stimulant use, 5–35% of college students use diverted ADHD stimulants, which are primarily used for enhancement of academic performance rather than as recreational drugs.^[85]^[86]^[87] However, high amphetamine doses that are above the therapeutic range can interfere with working memory and other aspects of cognitive control.^[11]^[83]

Physical performance

Amphetamine is used by some athletes for its psychological and athletic performance-enhancing effects, such as increased endurance and alertness;^[12]^[26] however, non-medical amphetamine use is prohibited at sporting events that are regulated by collegiate, national, and international anti-doping agencies.^[88]^[89] In healthy people at oral therapeutic doses, amphetamine has been shown to increase muscle strength, acceleration, athletic performance in anaerobic conditions, and endurance (i.e., it delays the onset of fatigue), while improving reaction time.^[12]^[90]^[91] Amphetamine improves endurance and reaction time primarily through reuptake inhibition and release of dopamine in the central nervous system.^[90]^[91]^[92] Amphetamine and other dopaminergic drugs also increase power output at fixed levels of perceived exertion by overriding a "safety switch", allowing the core temperature limit to increase in order to access a reserve capacity that is normally off-limits.^[91]^[93]^[94] At therapeutic doses, the adverse effects of amphetamine do not impede athletic performance;^[12]^[90] however, at much higher doses, amphetamine can induce effects that severely impair performance, such as rapid muscle breakdown and elevated body temperature.^[13]^[90]

Recreational

Amphetamine, specifically the more dopaminergic dextrorotatory enantiomer (dextroamphetamine), is also used recreationally as a euphoriant and aphrodisiac, and like other amphetamines; is used as a club drug for its energetic and euphoric high. Dextroamphetamine (d-amphetamine) is considered to have a high potential for misuse in a recreational manner since individuals typically report feeling euphoric, more alert, and more energetic after taking the drug.^[95]^[96]^[97] A notable part of the 1960s mod subculture in the UK was recreational amphetamine use, which was used to fuel all-night dances at clubs like Manchester's Twisted Wheel. Newspaper reports described dancers emerging from clubs at 5 a.m. with dilated pupils.^[98] Mods used the drug for stimulation and alertness, which they viewed as different from the intoxication caused by alcohol and other drugs.^[98] Dr. Andrew Wilson argues that for a significant minority, "amphetamines symbolised the smart, on-the-ball, cool image" and that they sought "stimulation not intoxication [...] greater awareness, not escape" and "confidence and articulacy" rather than the "drunken rowdiness of previous generations."^[98] Dextroamphetamine's dopaminergic (rewarding) properties affect the mesocorticolimbic circuit; a group of neural structures responsible for incentive salience (i.e., "wanting"; desire or craving for a reward and motivation), positive reinforcement and positively-valenced emotions, particularly ones involving pleasure.^[99] Large recreational doses of dextroamphetamine may produce symptoms of dextroamphetamine overdose.^[97] Recreational users sometimes open dexedrine capsules and crush the contents in order to insufflate (snort) it or subsequently dissolve it in water and inject it.^[97] Immediate-release formulations have higher potential for abuse via insufflation (snorting) or intravenous injection due to a more favorable pharmacokinetic profile and easy crushability (especially tablets).^[100]^[101] Injection into the bloodstream can be dangerous because insoluble fillers within the tablets can block small blood vessels.^[97] Chronic overuse of dextroamphetamine can lead to severe drug dependence, resulting in withdrawal symptoms when drug use stops.^[97]

Contraindications

Script error: No such module "Labelled list hatnote". According to the International Programme on Chemical Safety (IPCS) and the U.S. Food and Drug Administration (FDA),^{[note 9]} amphetamine is contraindicated in people with a history of drug abuse,^{[note 10]} cardiovascular disease, severe agitation, or severe anxiety.^[20]^[13]^[103] It is also contraindicated in individuals with advanced arteriosclerosis (hardening of the arteries), glaucoma (increased eye pressure), hyperthyroidism (excessive production of thyroid hormone), or moderate to severe hypertension.^[20]^[13]^[103] These agencies indicate that people who have experienced allergic reactions to other stimulants or who are taking monoamine oxidase inhibitors (MAOIs) should not take amphetamine,^[20]^[13]^[103] although safe concurrent use of amphetamine and monoamine oxidase inhibitors has been documented.^[104]^[105] These agencies also state that anyone with anorexia nervosa, bipolar disorder, depression, hypertension, liver or kidney problems, mania, psychosis, Raynaud's phenomenon, seizures, thyroid problems, tics, or Tourette syndrome should monitor their symptoms while taking amphetamine.^[13]^[103] Evidence from human studies indicates that therapeutic amphetamine use does not cause developmental abnormalities in the fetus or newborns (i.e., it is not a human teratogen), but amphetamine abuse does pose risks to the fetus.^[103] Amphetamine has also been shown to pass into breast milk, so the IPCS and the FDA advise mothers to avoid breastfeeding when using it.^[13]^[103] Due to the potential for reversible growth impairments,^{[note 11]} the FDA advises monitoring the height and weight of children and adolescents prescribed an amphetamine pharmaceutical.^[13]

Adverse effects

The adverse side effects of amphetamine are many and varied, and the amount of amphetamine used is the primary factor in determining the likelihood and severity of adverse effects.^[13]^[26] Amphetamine products such as Adderall, Dexedrine, and their generic equivalents are currently approved by the U.S. FDA for long-term therapeutic use.^[22]^[13] Recreational use of amphetamine generally involves much larger doses, which have a greater risk of serious adverse drug effects than dosages used for therapeutic purposes.^[26]

Physical

Cardiovascular side effects can include hypertension or hypotension from a vasovagal response, Raynaud's phenomenon (reduced blood flow to the hands and feet), and tachycardia (increased heart rate).^[13]^[26]^[106] Sexual side effects in males may include erectile dysfunction, frequent erections, or prolonged erections.^[13] Gastrointestinal side effects may include abdominal pain, constipation, diarrhea, and nausea.^[3]^[13]^[107] Other potential physical side effects include appetite loss, blurred vision, dry mouth, excessive grinding of the teeth, nosebleed, profuse sweating, rhinitis medicamentosa (drug-induced nasal congestion), reduced seizure threshold, tics (a type of movement disorder), and weight loss.^{[sources 6]} Dangerous physical side effects are rare at typical pharmaceutical doses.^[26]

Amphetamine stimulates the medullary respiratory centers, producing faster and deeper breaths.^[26] In a normal person at therapeutic doses, this effect is usually not noticeable, but when respiration is already compromised, it may be evident.^[26] Amphetamine also induces contraction in the urinary bladder sphincter, the muscle which controls urination, which can result in difficulty urinating.^[26] This effect can be useful in treating bed wetting and loss of bladder control.^[26] The effects of amphetamine on the gastrointestinal tract are unpredictable.^[26] If intestinal activity is high, amphetamine may reduce gastrointestinal motility (the rate at which content moves through the digestive system);^[26] however, amphetamine may increase motility when the smooth muscle of the tract is relaxed.^[26] Amphetamine also has a slight analgesic effect and can enhance the pain relieving effects of opioids.^[3]^[26]

FDA-commissioned studies from 2011 indicate that in children, young adults, and adults there is no association between serious adverse cardiovascular events (sudden death, heart attack, and stroke) and the medical use of amphetamine or other ADHD stimulants.^{[sources 7]} However, amphetamine pharmaceuticals are contraindicated in individuals with cardiovascular disease.^{[sources 8]}

Psychological

At normal therapeutic doses, the most common psychological side effects of amphetamine include increased alertness, apprehension, concentration, initiative, self-confidence and sociability, mood swings (elated mood followed by mildly depressed mood), insomnia or wakefulness, and decreased sense of fatigue.^[13]^[26] Less common side effects include anxiety, change in libido, grandiosity, irritability, repetitive or obsessive behaviors, and restlessness;^{[sources 9]} these effects depend on the user's personality and current mental state.^[26] Amphetamine psychosis (e.g., delusions and paranoia) can occur in heavy users.^[13]^[27]^[28] Although very rare, this psychosis can also occur at therapeutic doses during long-term therapy.^[13]^[28]^[29] According to the FDA, "there is no systematic evidence" that stimulants produce aggressive behavior or hostility.^[13]

Amphetamine has also been shown to produce a conditioned place preference in humans taking therapeutic doses,^[54]^[114] meaning that individuals acquire a preference for spending time in places where they have previously used amphetamine.^[114]^[115]

Reinforcement disorders

Addiction

Template:Addiction glossary Template:Glossary infobox Template:Psychostimulant addiction Addiction is a serious risk with heavy recreational amphetamine use, but is unlikely to occur from long-term medical use at therapeutic doses;^[31]^[32]^[33] in fact, lifetime stimulant therapy for ADHD that begins during childhood reduces the risk of developing substance use disorders as an adult.^[30] Template:If pagename Pathological overactivation of the mesolimbic pathway, a dopamine pathway that connects the ventral tegmental area to the nucleus accumbens, plays a central role in amphetamine addiction.^[116]^[117] Individuals who frequently self-administer high doses of amphetamine have a high risk of developing an amphetamine addiction, since chronic use at high doses gradually increases the level of accumbal ΔFosB, a "molecular switch" and "master control protein" for addiction.^[118]^[119]^[120] Once nucleus accumbens ΔFosB is sufficiently overexpressed, it begins to increase the severity of addictive behavior (i.e., compulsive drug-seeking) with further increases in its expression.^[119]^[121] While there are currently no effective drugs for treating amphetamine addiction, regularly engaging in sustained aerobic exercise appears to reduce the risk of developing such an addiction.^[122]^[123] Exercise therapy improves clinical treatment outcomes and may be used as an adjunct therapy with behavioral therapies for addiction.^[122]^[124]^{[sources 10]}

Biomolecular mechanisms

Chronic use of amphetamine at excessive doses causes alterations in gene expression in the mesocorticolimbic projection, which arise through transcriptional and epigenetic mechanisms.^[120]^[125]^[126] The most important transcription factors^{[note 12]} that produce these alterations are Delta FBJ murine osteosarcoma viral oncogene homolog B (ΔFosB), cAMP response element binding protein (CREB), and nuclear factor-kappa B (NF-κB).^[120] ΔFosB is the most significant biomolecular mechanism in addiction because ΔFosB overexpression (i.e., an abnormally high level of gene expression which produces a pronounced gene-related phenotype) in the D1-type medium spiny neurons in the nucleus accumbens is necessary and sufficient^{[note 13]} for many of the neural adaptations and regulates multiple behavioral effects (e.g., reward sensitization and escalating drug self-administration) involved in addiction.^[118]^[119]^[120] Once ΔFosB is sufficiently overexpressed, it induces an addictive state that becomes increasingly more severe with further increases in ΔFosB expression.^[118]^[119] It has been implicated in addictions to alcohol, cannabinoids, cocaine, methylphenidate, nicotine, opioids, phencyclidine, propofol, and substituted amphetamines, among others.^{[sources 11]}

ΔJunD, a transcription factor, and G9a, a histone methyltransferase enzyme, both oppose the function of ΔFosB and inhibit increases in its expression.^[118]^[120]^[130] Sufficiently overexpressing ΔJunD in the nucleus accumbens with viral vectors can completely block many of the neural and behavioral alterations seen in chronic drug abuse (i.e., the alterations mediated by ΔFosB).^[120] Similarly, accumbal G9a hyperexpression results in markedly increased histone 3 lysine residue 9 dimethylation (H3K9me2) and blocks the induction of ΔFosB-mediated neural and behavioral plasticity by chronic drug use,^{[sources 12]} which occurs via H3K9me2-mediated repression of transcription factors for ΔFosB and H3K9me2-mediated repression of various ΔFosB transcriptional targets (e.g., CDK5).^[120]^[130]^[131] ΔFosB also plays an important role in regulating behavioral responses to natural rewards, such as palatable food, sex, and exercise.^[121]^[120]^[134] Since both natural rewards and addictive drugs induce the expression of ΔFosB (i.e., they cause the brain to produce more of it), chronic acquisition of these rewards can result in a similar pathological state of addiction.^[121]^[120] Consequently, ΔFosB is the most significant factor involved in both amphetamine addiction and amphetamine-induced sexual addictions, which are compulsive sexual behaviors that result from excessive sexual activity and amphetamine use.^[121]^[135]^[136] These sexual addictions are associated with a dopamine dysregulation syndrome which occurs in some patients taking dopaminergic drugs.^[121]^[134]

The effects of amphetamine on gene regulation are both dose- and route-dependent.^[126] Most of the research on gene regulation and addiction is based upon animal studies with intravenous amphetamine administration at very high doses.^[126] The few studies that have used equivalent (weight-adjusted) human therapeutic doses and oral administration show that these changes, if they occur, are relatively minor.^[126] This suggests that medical use of amphetamine does not significantly affect gene regulation.^[126]

Pharmacological treatments

Script error: No such module "labelled list hatnote". since December 2019,^[update]Template:Dated maintenance category (articles)Script error: No such module "Check for unknown parameters". there is no effective pharmacotherapy for amphetamine addiction.^[137]^[138]^[139] Reviews from 2015 and 2016 indicated that TAAR1-selective agonists have significant therapeutic potential as a treatment for psychostimulant addictions;^[25]^[140] however, since February 2016,^[update]Template:Dated maintenance category (articles)Script error: No such module "Check for unknown parameters". the only compounds which are known to function as TAAR1-selective agonists are experimental drugs.^[25]^[140] Amphetamine addiction is largely mediated through increased activation of dopamine receptors and co-localized NMDA receptors^{[note 14]} in the nucleus accumbens;^[117] magnesium ions inhibit NMDA receptors by blocking the receptor calcium channel.^[117]^[141] One review suggested that, based upon animal testing, pathological (addiction-inducing) psychostimulant use significantly reduces the level of intracellular magnesium throughout the brain.^[117] Supplemental magnesium^{[note 15]} treatment has been shown to reduce amphetamine self-administration (i.e., doses given to oneself) in humans, but it is not an effective monotherapy for amphetamine addiction.^[117]

A systematic review and meta-analysis from 2019 assessed the efficacy of 17 different pharmacotherapies used in randomized controlled trials (RCTs) for amphetamine and methamphetamine addiction;^[138] it found only low-strength evidence that methylphenidate might reduce amphetamine or methamphetamine self-administration.^[138] There was low- to moderate-strength evidence of no benefit for most of the other medications used in RCTs, which included antidepressants (bupropion, mirtazapine, sertraline), antipsychotics (aripiprazole), anticonvulsants (topiramate, baclofen, gabapentin), naltrexone, varenicline, citicoline, ondansetron, prometa, riluzole, atomoxetine, dextroamphetamine, and modafinil.^[138]

Behavioral treatments

A 2018 systematic review and network meta-analysis of 50 trials involving 12 different psychosocial interventions for amphetamine, methamphetamine, or cocaine addiction found that combination therapy with both contingency management and community reinforcement approach had the highest efficacy (i.e., abstinence rate) and acceptability (i.e., lowest dropout rate).^[142] Other treatment modalities examined in the analysis included monotherapy with contingency management or community reinforcement approach, cognitive behavioral therapy, 12-step programs, non-contingent reward-based therapies, psychodynamic therapy, and other combination therapies involving these.^[142]

Additionally, research on the neurobiological effects of physical exercise suggests that daily aerobic exercise, especially endurance exercise (e.g., marathon running), prevents the development of drug addiction and is an effective adjunct therapy (i.e., a supplemental treatment) for amphetamine addiction.^{[sources 10]} Exercise leads to better treatment outcomes when used as an adjunct treatment, particularly for psychostimulant addictions.^[122]^[124]^[143] In particular, aerobic exercise decreases psychostimulant self-administration, reduces the reinstatement (i.e., relapse) of drug-seeking, and induces increased dopamine receptor D₂ (DRD2) density in the striatum.^[121]^[143] This is the opposite of pathological stimulant use, which induces decreased striatal DRD2 density.^[121] One review noted that exercise may also prevent the development of a drug addiction by altering ΔFosB or c-Fos immunoreactivity in the striatum or other parts of the reward system.^[123] Template:FOSB addiction table

Dependence and withdrawal

Drug tolerance develops rapidly in amphetamine abuse (i.e., recreational amphetamine use), so periods of extended abuse require increasingly larger doses of the drug in order to achieve the same effect.^[144]^[145] According to a Cochrane review on withdrawal in individuals who compulsively use amphetamine and methamphetamine, "when chronic heavy users abruptly discontinue amphetamine use, many report a time-limited withdrawal syndrome that occurs within 24 hours of their last dose."^[146] This review noted that withdrawal symptoms in chronic, high-dose users are frequent, occurring in roughly 88% of cases, and persist for 3–4 weeks with a marked "crash" phase occurring during the first week.^[146] Amphetamine withdrawal symptoms can include anxiety, drug craving, depressed mood, fatigue, increased appetite, increased movement or decreased movement, lack of motivation, sleeplessness or sleepiness, and lucid dreams.^[146] The review indicated that the severity of withdrawal symptoms is positively correlated with the age of the individual and the extent of their dependence.^[146]

According to a 2025 review, the discontinuation of amphetamine at therapeutic doses does not typically result in withdrawal symptoms.^[147] Discontinuation may unmask or cause a rebound of ADHD symptoms due to the cessation of treatment-related drug effects.^[147] In cases where mild withdrawal symptoms do occur, they can be avoided by tapering the dose.^[3] Unlike amphetamine abuse, where drug tolerance necessitates escalating doses to achieve the same effect, tolerance to clinically relevant doses of amphetamine plateaus after the initial titration period, and "drug holidays" (i.e., temporary treatment discontinuation) are not required to prevent the development of tolerance.^[147]

Overdose

An amphetamine overdose can lead to many different symptoms, but is rarely fatal with appropriate care.^[3]^[103]^[148] The severity of overdose symptoms increases with dosage and decreases with drug tolerance to amphetamine.^[26]^[103] Tolerant individuals have been known to take as much as 5 grams of amphetamine in a day, which is roughly 100 times the maximum daily therapeutic dose.^[103] Symptoms of a moderate and extremely large overdose are listed below; fatal amphetamine poisoning usually also involves convulsions and coma.^[13]^[26] In 2013, overdose on amphetamine, methamphetamine, and other compounds implicated in an "amphetamine use disorder" resulted in an estimated 3,788 deaths worldwide (3,425–4,145 deaths, 95% confidence).^{[note 16]}^[149]

Overdose symptoms by system
System	Minor or moderate overdose^[13]^[26]^[103]	Severe overdose^{[sources 13]}
Cardiovascular	Abnormal heartbeat High or low blood pressure	Cardiogenic shock (heart not pumping enough blood) Cerebral hemorrhage (bleeding in the brain) Circulatory collapse (partial or complete failure of the circulatory system)
Central nervous system	Confusion Abnormally fast reflexes Severe agitation Tremor (involuntary muscle twitching)	Acute amphetamine psychosis (e.g., delusions and paranoia) Compulsive and repetitive movement Serotonin syndrome (excessive serotonergic nerve activity) Sympathomimetic toxidrome (excessive adrenergic nerve activity)
Musculoskeletal	Muscle pain	Rhabdomyolysis (rapid muscle breakdown)
Respiratory	Rapid breathing	Pulmonary edema (fluid accumulation in the lungs) Pulmonary hypertension (high blood pressure in the arteries of the lung) Respiratory alkalosis (reduced blood CO₂)
Urinary	Painful urination Urinary retention (inability to urinate)	No urine production Kidney failure
Other	Elevated body temperature Mydriasis (dilated pupils)	Elevated or low blood potassium Hyperpyrexia (extremely elevated core body temperature) Metabolic acidosis (excessively acidic bodily fluids)

Toxicity

In rodents and primates, sufficiently high doses of amphetamine cause dopaminergic neurotoxicity, or damage to dopamine neurons, which is characterized by dopamine terminal degeneration and reduced transporter and receptor function.^[151]^[152] There is no evidence that amphetamine is directly neurotoxic in humans.^[153]^[154] However, large doses of amphetamine may indirectly cause dopaminergic neurotoxicity as a result of hyperpyrexia, the excessive formation of reactive oxygen species, and increased autoxidation of dopamine.^{[sources 14]} Animal models of neurotoxicity from high-dose amphetamine exposure indicate that the occurrence of hyperpyrexia (i.e., core body temperature ≥ 40 °C) is necessary for the development of amphetamine-induced neurotoxicity.^[152] Prolonged elevations of brain temperature above 40 °C likely promote the development of amphetamine-induced neurotoxicity in laboratory animals by facilitating the production of reactive oxygen species, disrupting cellular protein function, and transiently increasing blood–brain barrier permeability.^[152]

Psychosis

Script error: No such module "Labelled list hatnote". An amphetamine overdose can result in a stimulant psychosis that may involve a variety of symptoms, such as delusions and paranoia.^[27]^[28] A Cochrane review on treatment for amphetamine, dextroamphetamine, and methamphetamine psychosis states that about 5–15% of users fail to recover completely.^[27]^[157] According to the same review, there is at least one trial that shows antipsychotic medications effectively resolve the symptoms of acute amphetamine psychosis.^[27] Psychosis rarely arises from therapeutic use.^[13]^[28]^[29]

Drug interactionsScript error: No such module "anchor".

Script error: No such module "Labelled list hatnote". Many types of substances are known to interact with amphetamine, resulting in altered drug action or metabolism of amphetamine, the interacting substance, or both.^[13] Inhibitors of enzymes that metabolize amphetamine (e.g., CYP2D6 and FMO3) will prolong its elimination half-life, meaning that its effects will last longer.^[158]^[13] Amphetamine also interacts with MAOIs, particularly monoamine oxidase A inhibitors, since both MAOIs and amphetamine increase plasma catecholamines (i.e., norepinephrine and dopamine);^[13] therefore, concurrent use of both is dangerous.^[13] Amphetamine modulates the activity of most psychoactive drugs. In particular, amphetamine may decrease the effects of sedatives and depressants and increase the effects of stimulants and antidepressants.^[13] Amphetamine may also decrease the effects of antihypertensives and antipsychotics due to its effects on blood pressure and dopamine respectively.^[13] Zinc supplementation may reduce the minimum effective dose of amphetamine when it is used for the treatment of ADHD.^{[note 17]}^[163] Norepinephrine reuptake inhibitors (NRIs) like atomoxetine prevent norepinephrine release induced by amphetamines and have been found to reduce the stimulant, euphoriant, and sympathomimetic effects of dextroamphetamine in humans.^[164]^[165]^[166]

In general, there is no significant interaction when consuming amphetamine with food, but the pH of gastrointestinal content and urine affects the absorption and excretion of amphetamine, respectively.^[13] Acidic substances reduce the absorption of amphetamine and increase urinary excretion, and alkaline substances do the opposite.^[13] Due to the effect pH has on absorption, amphetamine also interacts with gastric acid reducers such as proton pump inhibitors and H₂ antihistamines, which increase gastrointestinal pH (i.e., make it less acidic).^[13]

Pharmacology

Pharmacodynamics

Script error: No such module "For". Template:Amphetamine pharmacodynamics Amphetamine exerts its behavioral effects by altering the use of monoamines as neuronal signals in the brain, primarily in catecholamine neurons in the reward and executive function pathways of the brain.^[24]^[49] The concentrations of the main neurotransmitters involved in reward circuitry and executive functioning, dopamine and norepinephrine, increase dramatically in a dose-dependent manner by amphetamine because of its effects on monoamine transporters.^[24]^[49]^[167] The reinforcing and motivational salience-promoting effects of amphetamine are due mostly to enhanced dopaminergic activity in the mesolimbic pathway.^[11] 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.^[4]

Amphetamine potentiates monoaminergic neurotransmission by entering the presynaptic neuron both as a substrate for monoamine transporters (DAT, NET, and, SERT) and by passive diffusion across the neuronal membrane.^[168]^[169] Transporter-mediated uptake competes with reabsorption of endogenous neurotransmitters from the synaptic cleft and produces competitive reuptake inhibition as a consequence.^[168] Once inside the neuronal cytosol, amphetamine initiates intracellular signaling cascades that activate protein kinase C (PKC), leading to phosphorylation of DAT, NET, and SERT.^[169] PKC-dependent phosphorylation of monoamine transporters can either reverse their direction to induce efflux of cytosolic neurotransmitters into the synaptic cleft, or trigger the withdrawal of transporters into the presynaptic neuron (internalization), thereby ceasing their reuptake function in a non-competitive manner.^[169]^[170] Amphetamine also causes a rise in intracellular calcium, an effect associated with transporter phosphorylation through a Ca²⁺/calmodulin-dependent protein kinase II alpha (CaMKIIα) signaling cascade.^[169] Unlike PKC, CaMKIIα-mediated transporter phosphorylation appears to reverse the direction of DAT and NET without triggering internalization.^[169]^[171]

Amphetamine has been identified as a full agonist of trace amine-associated receptor 1 (TAAR1), a G_s-coupled and G_q-coupled G protein-coupled receptor (GPCR) discovered in 2001, which is important for regulation of brain monoamines.^[24] Several reviews have linked amphetamine’s agonism at TAAR1 to modulation of monoamine transporter function and subsequent neurotransmitter efflux and reuptake inhibition at monoaminergic synapses.^{[sources 15]} Activation of TAAR1 increases cAMPTooltip cyclic adenosine monophosphate production via adenylyl cyclase activation, which triggers protein kinase A (PKA)- and PKC-mediated transporter phosphorylation.^[24]^[172]^[175] Monoamine autoreceptors (e.g., D₂ short, presynaptic α₂, and presynaptic 5-HT_1A) have the opposite effect of TAAR1, and together these receptors provide a regulatory system for monoamines.^[24]^[25]^[176] Notably, amphetamine and trace amines possess high binding affinities for TAAR1, but not for monoamine autoreceptors.^[24]^[25] Although TAAR1 is implicated in amphetamine-induced transporter phosphorylation, the magnitude of TAAR1-mediated monoamine release in humans remains unclear.^{[sources 15]}^[176] Findings from studies using TAAR1 gene knockout models suggest that, despite facilitating monoamine release through reverse transport, TAAR1 activation may paradoxically attenuate amphetamine’s psychostimulant effects in part by opening G protein-coupled inwardly rectifying potassium channels, an action that reduces neuronal firing.^[24]^[176]

Amphetamine is also a substrate for the vesicular monoamine transporters VMAT1 and VMAT2.^[177]^[178] Under normal conditions, VMAT2 transports cytosolic monoamines into synaptic vesicles for storage and later exocytotic release. When amphetamine accumulates in the presynaptic terminal, it collapses the vesicular pH gradient and releases vesicular monoamines into the neuronal cytosol.^[177]^[178] These displaced monoamines expand the cytosolic pool available for reverse transport, thereby increasing the capacity for monoamine efflux beyond that achieved by amphetamine-mediated transporter phosphorylation alone.^[171]^[178] Although VMAT2 is recognized as a major target in amphetamine-induced monoamine release at higher doses, some reviews have challenged its relevance at therapeutic doses.^[168]^[171]^[178]

In addition to membrane and vesicular monoamine transporters, amphetamine also inhibits SLC1A1, SLC22A3, and SLC22A5.^{[sources 16]} SLC1A1 is excitatory amino acid transporter 3 (EAAT3), a glutamate transporter located in neurons, SLC22A3 is an extraneuronal monoamine transporter that is present in astrocytes, and SLC22A5 is a high-affinity carnitine transporter.^{[sources 16]} Amphetamine is known to strongly induce cocaine- and amphetamine-regulated transcript (CART) gene expression,^[7]^[185] a neuropeptide involved in feeding behavior, stress, and reward, which induces observable increases in neuronal development and survival in vitro.^[7]^[186]^[187] The CART receptor has yet to be identified, but there is significant evidence that CART binds to a unique G_i/G_o-coupled GPCR.^[187]^[188] Amphetamine also inhibits monoamine oxidases at very high doses, resulting in less monoamine and trace amine metabolism and consequently higher concentrations of synaptic monoamines.^[6]^[189] In humans, the only post-synaptic receptor at which amphetamine is known to bind is the 5-HT1A receptor, where it acts as an agonist with low micromolar affinity.^[190]^[191]

The full profile of amphetamine's short-term drug effects in humans is mostly derived through increased cellular communication or neurotransmission of dopamine,^[24] serotonin,^[24] norepinephrine,^[24] epinephrine,^[167] histamine,^[167] CART peptides,^[7]^[185] endogenous opioids,^[192]^[193]^[194] adrenocorticotropic hormone,^[195]^[196] corticosteroids,^[195]^[196] and glutamate,^[179]^[181] which it affects through interactions with CART, 5-HT1A, EAAT3, TAAR1, VMAT1, VMAT2, and possibly other biological targets.^{[sources 17]} Amphetamine also activates seven human carbonic anhydrase enzymes, several of which are expressed in the human brain.^[197]

Dextroamphetamine displays higher binding affinity for DAT than levoamphetamine, whereas both enantiomers share comparable affinity at NET;^[168] Consequently, dextroamphetamine produces greater CNS stimulation than levoamphetamine, roughly three to four times more, but levoamphetamine has slightly stronger cardiovascular and peripheral effects.^[168]^[26] Dextroamphetamine is also a more potent agonist of TAAR1 than levoamphetamine.^[198]

Dopamine

In certain brain regions, amphetamine increases the concentration of dopamine in the synaptic cleft by modulating DAT through several overlapping processes.^[171]^[169]^[172] Amphetamine can enter the presynaptic neuron either through DAT or by diffusing across the neuronal membrane directly.^[24]^[169] As a consequence of DAT uptake, amphetamine produces competitive reuptake inhibition at the transporter.^[24]^[4] Upon entering the presynaptic neuron, amphetamine provokes the release of Ca²⁺ from endoplasmic reticulum stores, an effect that raises intracellular calcium to levels sufficient for downstream kinase-dependent signalling.^[170]^[171] Subsequently, amphetamine initiates kinase-dependent signaling cascades that activate both protein kinase A (PKA) and protein kinase C (PKC).^[169]^[172] Phosphorylation of DAT by either kinase induces transporter internalization (non-competitive reuptake inhibition), but PKC-mediated phosphorylation alone induces the reversal of dopamine transport through DAT (i.e., dopamine efflux).^[169]^[170]

TAAR1 is a biomolecular target of amphetamine that can trigger the activation of PKA- and PKC-dependent pathways.^[24]^[169]^[172] TAAR1 agonism also activates Ras homolog A (RhoA) and its downstream effector, Rho-associated coiled-coil kinase (ROCK), which results in transient internalization of DAT and EAAT3;^{[note 18]}^[199]^[169] as intracellular cAMPTooltip cyclic adenosine monophosphate accumulates, PKA is activated and inhibits RhoA activity, thereby terminating ROCK-mediated transporter internalization.^[199]^[169] Importantly, TAAR1 has been demonstrated to also produce inhibitory effects on dopamine release that may attenuate amphetamine's psychostimulant effects.^[176] Through direct activation of G protein-coupled inwardly-rectifying potassium channels, TAAR1 reduces the firing rate of dopamine neurons, preventing a hyper-dopaminergic state.^[200]^[201]

Amphetamine's effect on intracellular calcium is associated with DAT phosphorylation through Ca²⁺/calmodulin-dependent protein kinase II alpha (CAMKIIα), in turn producing dopamine efflux.^[169]^[170]^[202] Notably, because conventional PKC isoforms can be activated by calcium ions, the rise in intracellular calcium can also promote PKC activation and subsequent DAT phosphorylation independent of TAAR1.^[171]

Effects of amphetamine on membrane transport proteins in dopamine neurons^{[note 19]}
Biological target of amphetamine	Initial effector / G-protein	Second messenger(s)	Secondary effector protein kinase	Phosphorylated transporter	Effect on transporter function	Effect on neurotransmission	Sources
Unidentified	Unidentified intracellular effector	IP₃-mediated intracellular Ca²⁺ release	CAMKIIαTooltip Calcium/calmodulin-dependent protein kinase II alpha	DATTooltip Dopamine transporter	Reverse transport of dopamine	Dopamine efflux into synaptic cleft	^[171]^[170]
TAAR1Tooltip Trace amine-associated receptor 1	G₁₃	RhoA–GTP	ROCK^†	DAT	Transporter internalization	Dopamine reuptake inhibition	^[169]^[203]^[199]
TAAR1Tooltip Trace amine-associated receptor 1	G₁₃	RhoA–GTP	ROCK^†	EAAT3Tooltip Excitatory amino acid transporter 3	Transporter internalization	Glutamate reuptake inhibition	^[169]^[176]^[199]
TAAR1Tooltip Trace amine-associated receptor 1	G_s	↑ cAMPTooltip cyclic adenosine monophosphate	PKATooltip Protein kinase A	DAT	Transporter internalization	Dopamine reuptake inhibition	^[24]^[169]^[172]
TAAR1Tooltip Trace amine-associated receptor 1	G_s	↑ Template:Abr	PKCTooltip Protein kinase C	DAT	Reverse transport of dopamine Transporter internalization	Dopamine efflux into synaptic cleft Dopamine reuptake inhibition	^[24]^[172]^[174]
Unidentified	Unidentified intracellular effector	IP₃/DAG pathway^‡	PKCTooltip Protein kinase C	DAT	Reverse transport of dopamine Transporter internalization	Dopamine efflux into synaptic cleft Dopamine reuptake inhibition	^[171]^[170]
†ROCK-mediated transporter internalization is transient due to the inactivation of RhoA (which activates ROCK) by PKA. ‡IP₃ binds to its receptors on the endoplasmic reticulum to release intracellular Ca²⁺ stores, and together with diacylglycerol activates conventional PKC isoforms.							^[169]^[170]^[199]

Amphetamine is also a substrate for the presynaptic vesicular monoamine transporter, VMAT2.^[177] Following amphetamine uptake at VMAT2, amphetamine induces the collapse of the vesicular pH gradient, which results in a dose-dependent release of dopamine molecules from synaptic vesicles into the cytosol via dopamine efflux through VMAT2.^[177]^[204] Subsequently, the cytosolic dopamine molecules are released from the presynaptic neuron into the synaptic cleft via reverse transport at DAT.^[177]^[204]

Norepinephrine

Similar to dopamine, amphetamine dose-dependently increases the level of synaptic norepinephrine, the direct precursor of epinephrine. Amphetamine is believed to affect norepinephrine analogously to dopamine.^[169]^[171]^[172] In other words, amphetamine induces competitive NET reuptake inhibition, non-competitive reuptake inhibition and efflux at phosphorylated NET via PKC activation, CAMKIIα-mediated NET efflux without internalization, and norepinephrine release from VMAT2.^[169]^[171]^[172]

Serotonin

Amphetamine exerts analogous, yet less pronounced, effects on serotonin as on dopamine and norepinephrine.^[24] Amphetamine affects serotonin via VMAT2 and is thought to phosphorylate SERT via a PKC-dependent signaling cascade.^[172] Like dopamine, amphetamine has low, micromolar affinity at the human 5-HT1A receptor.^[205]^[191]

Other neurotransmitters, peptides, hormones, and enzymes

Human carbonic anhydrase
activation potency
Enzyme	K_A (nMTooltip nanomolar)	Sources
hCA4	94	^[197]
hCA5A	810	^[197]^[206]
hCA5B	2560	^[197]
hCA7	910	^[197]^[206]
hCA12	640	^[197]
hCA13	24100	^[197]
hCA14	9150	^[197]

Acute amphetamine administration in humans increases endogenous opioid release in several brain structures in the reward system.^[192]^[193]^[194] Extracellular levels of glutamate, the primary excitatory neurotransmitter in the brain, have been shown to increase in the striatum following exposure to amphetamine.^[179] This increase in extracellular glutamate presumably occurs via the amphetamine-induced internalization of EAAT3, a glutamate reuptake transporter, in dopamine neurons.^[179]^[181] This internalization is mediated by RhoA activation and its downstream effector ROCK.^[169]^[207] Amphetamine also induces the selective release of histamine from mast cells and efflux from histaminergic neurons through VMAT2.^[167] Acute amphetamine administration can also increase adrenocorticotropic hormone and corticosteroid levels in blood plasma by stimulating the hypothalamic–pituitary–adrenal axis.^[20]^[195]^[196]

In December 2017, the first study assessing the interaction between amphetamine and human carbonic anhydrase enzymes was published;^[197] of the eleven carbonic anhydrase enzymes it examined, it found that amphetamine potently activates seven, four of which are highly expressed in the human brain, with low nanomolar through low micromolar activating effects.^[197] Based upon preclinical research, cerebral carbonic anhydrase activation has cognition-enhancing effects;^[208] but, based upon the clinical use of carbonic anhydrase inhibitors, carbonic anhydrase activation in other tissues may be associated with adverse effects, such as ocular activation exacerbating glaucoma.^[208]

Pharmacokinetics

The oral bioavailability of amphetamine varies with gastrointestinal pH;^[13] it is well absorbed from the gut, and bioavailability is typically 90%.^[209] Amphetamine is a weak base with a pK_a of 9.9;^[210] consequently, when the pH is basic, more of the drug is in its lipid soluble free base form, and more is absorbed through the lipid-rich cell membranes of the gut epithelium.^[210]^[13] Conversely, an acidic pH means the drug is predominantly in a water-soluble cationic (salt) form, and less is absorbed.^[210] Approximately 20% of amphetamine circulating in the bloodstream is bound to plasma proteins.^[7] Following absorption, amphetamine readily distributes into most tissues in the body, with high concentrations occurring in cerebrospinal fluid and brain tissue.^[211]

The half-lives of amphetamine enantiomers differ and vary with urine pH.^[210] At normal urine pH, the half-lives of dextroamphetamine and levoamphetamine are 9–11 hours and 11–14 hours, respectively.^[210] Highly acidic urine will reduce the enantiomer half-lives to 7 hours;^[211] highly alkaline urine will increase the half-lives up to 34 hours.^[211] The immediate-release and extended release variants of salts of both isomers reach peak plasma concentrations at 3 hours and 7 hours post-dose respectively.^[210] Amphetamine is eliminated via the kidneys, with 30–40% of the drug being excreted unchanged at normal urinary pH.^[210] When the urinary pH is basic, amphetamine is in its free base form, so less is excreted.^[210] When urine pH is abnormal, the urinary recovery of amphetamine may range from a low of 1% to a high of 75%, depending mostly upon whether urine is too basic or acidic, respectively.^[210] Following oral administration, amphetamine appears in urine within 3 hours.^[211] Roughly 90% of ingested amphetamine is eliminated 3 days after the last oral dose.^[211]Template:If pagename

CYP2D6, dopamine β-hydroxylase (DBH), flavin-containing monooxygenase 3 (FMO3), butyrate-CoA ligase (XM-ligase), and glycine N-acyltransferase (GLYAT) are the enzymes known to metabolize amphetamine or its metabolites in humans.^{[sources 18]} Amphetamine has a variety of excreted metabolic products, including 4-hydroxyamphetamine, 4-hydroxynorephedrine, 4-hydroxyphenylacetone, benzoic acid, hippuric acid, norephedrine, and phenylacetone.^[210]^[212] Among these metabolites, the active sympathomimetics are 4-hydroxyamphetamine,^[213] 4-hydroxynorephedrine,^[214] and norephedrine.^[215] The main metabolic pathways involve aromatic para-hydroxylation, aliphatic alpha- and beta-hydroxylation, N-oxidation, N-dealkylation, and deamination.^[210]^[216] The known metabolic pathways, detectable metabolites, and metabolizing enzymes in humans include the following: Template:Amphetamine pharmacokinetics

Pharmacomicrobiomics

The human metagenome (i.e., the genetic composition of an individual and all microorganisms that reside on or within the individual's body) varies considerably between individuals.^[217]^[218] Since the total number of microbial and viral cells in the human body (over 100 trillion) greatly outnumbers human cells (tens of trillions),^{[note 20]}^[217]^[219] there is considerable potential for interactions between drugs and an individual's microbiome, including: drugs altering the composition of the human microbiome, drug metabolism by microbial enzymes modifying the drug's pharmacokinetic profile, and microbial drug metabolism affecting a drug's clinical efficacy and toxicity profile.^[217]^[218]^[220] The field that studies these interactions is known as pharmacomicrobiomics.^[217]

Similar to most biomolecules and other orally administered xenobiotics (i.e., drugs), amphetamine is predicted to undergo promiscuous metabolism by human gastrointestinal microbiota (primarily bacteria) prior to absorption into the blood stream.^[220] The first amphetamine-metabolizing microbial enzyme, tyramine oxidase from a strain of E. coli commonly found in the human gut, was identified in 2019.^[220] This enzyme was found to metabolize amphetamine, tyramine, and phenethylamine with roughly the same binding affinity for all three compounds.^[220]

Related endogenous compounds

Script error: No such module "labelled list hatnote". Amphetamine has a very similar structure and function to the endogenous trace amines, which are naturally occurring neuromodulator molecules produced in the human body and brain.^[24]^[35]^[221] Among this group, the most closely related compounds are phenethylamine, the parent compound of amphetamine, and N-methylphenethylamine, a structural isomer of amphetamine (i.e., it has an identical molecular formula).^[24]^[35]^[222] In humans, phenethylamine is produced directly from L-phenylalanine by the aromatic amino acid decarboxylase (AADC) enzyme, which converts L-DOPA into dopamine as well.^[35]^[222] In turn, N-methylphenethylamine is metabolized from phenethylamine by phenylethanolamine N-methyltransferase, the same enzyme that metabolizes norepinephrine into epinephrine.^[35]^[222] Like amphetamine, both phenethylamine and N-methylphenethylamine regulate monoamine neurotransmission via TAAR1;^[24]^[221]^[222] unlike amphetamine, both of these substances are broken down by monoamine oxidase B, and therefore have a shorter half-life than amphetamine.^[35]^[222]

Chemistry

Template:Annotated image 4

Script error: No such module "Multiple image". Amphetamine is a methyl homolog of the mammalian neurotransmitter phenethylamine with the chemical formula Template:Chem2. The carbon atom adjacent to the primary amine is a stereogenic center, and amphetamine is composed of a racemic 1:1 mixture of two enantiomers.^[7] This racemic mixture can be separated into its optical isomers:^{[note 21]} levoamphetamine and dextroamphetamine.^[7] At room temperature, the pure free base of amphetamine is a mobile, colorless, and volatile liquid with a characteristically strong amine odor, and acrid, burning taste.^[223] Frequently prepared solid salts of amphetamine include amphetamine adipate,^[224] aspartate,^[13] hydrochloride,^[225] phosphate,^[226] saccharate,^[13] sulfate,^[13] and tannate.^[227] Dextroamphetamine sulfate is the most common enantiopure salt.^[36] Amphetamine is also the parent compound of its own structural class, which includes a number of psychoactive derivatives.^[34]^[7] In organic chemistry, amphetamine is an excellent chiral ligand for the stereoselective synthesis of 1,1'-bi-2-naphthol.^[228]

Substituted derivatives

Script error: No such module "Main list". The substituted derivatives of amphetamine, or "substituted amphetamines", are a broad range of chemicals that contain amphetamine as a "backbone";^[34]^[37]^[229] specifically, this chemical class includes derivative compounds that are formed by replacing one or more hydrogen atoms in the amphetamine core structure with substituents.^[34]^[37]^[230] The class includes amphetamine itself, stimulants like methamphetamine, serotonergic empathogens like MDMA, and decongestants like ephedrine, among other subgroups.^[34]^[37]^[229]

Synthesis

Script error: No such module "labelled list hatnote". Since the first preparation was reported in 1887,^[231] numerous synthetic routes to amphetamine have been developed.^[232]^[233] The most common route of both legal and illicit amphetamine synthesis employs a non-metal reduction known as the Leuckart reaction (method 1).^[36]^[234] In the first step, a reaction between phenylacetone and formamide, either using additional formic acid or formamide itself as a reducing agent, yields N-formylamphetamine. This intermediate is then hydrolyzed using hydrochloric acid, and subsequently basified, extracted with organic solvent, concentrated, and distilled to yield the free base. The free base is then dissolved in an organic solvent, sulfuric acid added, and amphetamine precipitates out as the sulfate salt.^[234]^[235]

A number of chiral resolutions have been developed to separate the two enantiomers of amphetamine.^[232] For example, racemic amphetamine can be treated with d-tartaric acid to form a diastereoisomeric salt which is fractionally crystallized to yield dextroamphetamine.^[236] Chiral resolution remains the most economical method for obtaining optically pure amphetamine on a large scale.^[237] In addition, several enantioselective syntheses of amphetamine have been developed. In one example, optically pure (R)-1-phenyl-ethanamine is condensed with phenylacetone to yield a chiral Schiff base. In the key step, this intermediate is reduced by catalytic hydrogenation with a transfer of chirality to the carbon atom alpha to the amino group. Cleavage of the benzylic amine bond by hydrogenation yields optically pure dextroamphetamine.^[237]

A large number of alternative synthetic routes to amphetamine have been developed based on classic organic reactions.^[232]^[233] One example is the Friedel–Crafts alkylation of benzene by allyl chloride to yield beta chloropropylbenzene which is then reacted with ammonia to produce racemic amphetamine (method 2).^[238] Another example employs the Ritter reaction (method 3). In this route, allylbenzene is reacted acetonitrile in sulfuric acid to yield an organosulfate which in turn is treated with sodium hydroxide to give amphetamine via an acetamide intermediate.^[239]^[240] A third route starts with ethyl 3-oxobutanoate which through a double alkylation with methyl iodide followed by benzyl chloride can be converted into 2-methyl-3-phenyl-propanoic acid. This synthetic intermediate can be transformed into amphetamine using either a Hofmann or Curtius rearrangement (method 4).^[241]

A significant number of amphetamine syntheses feature a reduction of a nitro, imine, oxime, or other nitrogen-containing functional groups.^[233] In one such example, a Knoevenagel condensation of benzaldehyde with nitroethane yields phenyl-2-nitropropene. The double bond and nitro group of this intermediate is reduced using either catalytic hydrogenation or by treatment with lithium aluminium hydride (method 5).^[234]^[242] Another method is the reaction of phenylacetone with ammonia, producing an imine intermediate that is reduced to the primary amine using hydrogen over a palladium catalyst or lithium aluminum hydride (method 6).^[234]

Amphetamine synthetic routes

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Detection in body fluids

Amphetamine is frequently measured in urine or blood as part of a drug test for sports, employment, poisoning diagnostics, and forensics.^{[sources 19]} Techniques such as immunoassay, which is the most common form of amphetamine test, may cross-react with a number of sympathomimetic drugs.^[246] Chromatographic methods specific for amphetamine are employed to prevent false positive results.^[247] Chiral separation techniques may be employed to help distinguish the source of the drug, whether prescription amphetamine, prescription amphetamine prodrugs, (e.g., selegiline), over-the-counter drug products that contain levomethamphetamine,^{[note 22]} or illicitly obtained substituted amphetamines.^[247]^[250]^[251] Several prescription drugs produce amphetamine as a metabolite, including benzphetamine, clobenzorex, famprofazone, fenproporex, lisdexamfetamine, mesocarb, methamphetamine, prenylamine, and selegiline, among others.^[4]^[252]^[253] These compounds may produce positive results for amphetamine on drug tests.^[252]^[253] Amphetamine is generally only detectable by a standard drug test for approximately 24 hours, although a high dose may be detectable for 2–4 days.^[246]

For the assays, a study noted that an enzyme multiplied immunoassay technique (EMIT) assay for amphetamine and methamphetamine may produce more false positives than liquid chromatography–tandem mass spectrometry.^[250] Gas chromatography–mass spectrometry (GC–MS) of amphetamine and methamphetamine with the derivatizing agent (S)-(−)-trifluoroacetylprolyl chloride allows for the detection of methamphetamine in urine.^[247] GC–MS of amphetamine and methamphetamine with the chiral derivatizing agent Mosher's acid chloride allows for the detection of both dextroamphetamine and dextromethamphetamine in urine.^[247] Hence, the latter method may be used on samples that test positive using other methods to help distinguish between the various sources of the drug.^[247]

History, society, and culture

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Amphetamine was first synthesized in 1887 in Germany by Romanian chemist Lazăr Edeleanu who named it phenylisopropylamine;^[231]^[254]^[255] its stimulant effects remained unknown until 1927, when it was independently resynthesized by Gordon Alles and reported to have sympathomimetic properties.^[255] Amphetamine had no medical use until late 1933, when Smith, Kline and French began selling it as an inhaler under the brand name Benzedrine as a decongestant.^[14] Benzedrine sulfate was introduced 3 years later and was used to treat a wide variety of medical conditions, including narcolepsy, obesity, low blood pressure, low libido, and chronic pain, among others.^[38]^[14] During World War II, amphetamine and methamphetamine were used extensively by both the Allied and Axis forces for their stimulant and performance-enhancing effects.^[231]^[256]^[257] As the addictive properties of the drug became known, governments began to place strict controls on the sale of amphetamine.^[231] For example, during the early 1970s in the United States, amphetamine became a schedule II controlled substance under the Controlled Substances Act.^[5] In spite of strict government controls, amphetamine has been used legally or illicitly by people from a variety of backgrounds, including authors,^[258] musicians,^[259] mathematicians,^[260] and athletes.^[12]

Amphetamine is illegally synthesized in clandestine labs and sold on the black market, primarily in European countries.^[261] Among European Union (EU) member states in 2018,^[update]Template:Dated maintenance category (articles)Script error: No such module "Check for unknown parameters". 11.9 million adults of ages 15–64 have used amphetamine or methamphetamine at least once in their lives and 1.7 million have used either in the last year.^[262] During 2012, approximately 5.9 metric tons of illicit amphetamine were seized within EU member states;^[263] the "street price" of illicit amphetamine within the EU ranged from €6–38 per gram during the same period.^[263] Outside Europe, the illicit market for amphetamine is much smaller than the market for methamphetamine and MDMA.^[261]

Legal status

As a result of the United Nations 1971 Convention on Psychotropic Substances, amphetamine became a schedule II controlled substance, as defined in the treaty, in all 183 state parties.^[15] Consequently, it is heavily regulated in most countries.^[264]^[265] Some countries, such as South Korea and Japan, have banned substituted amphetamines even for medical use.^[266]^[267] In other nations, such as Brazil (class A3),^[268] Canada (schedule I drug),^[269] the Netherlands (List I drug),^[270] the United States (schedule II drug),^[5] Australia (schedule 8),^[271] Thailand (category 1 narcotic),^[272] and United Kingdom (class B drug),^[273] amphetamine is in a restrictive national drug schedule that allows for its use as a medical treatment.^[261]^[16]

Pharmaceutical products

Several currently marketed amphetamine formulations contain both enantiomers, including those marketed under the brand names Adderall, Adderall XR, Mydayis,^{[note 1]} Adzenys ER, Adzenys XR-ODT, Dyanavel XR, Evekeo, and Evekeo ODT. Of those, Evekeo (including Evekeo ODT) is the only product containing only racemic amphetamine (as amphetamine sulfate), and is therefore the only one whose active moiety can be accurately referred to simply as "amphetamine".^[3]^[20]^[107] Dextroamphetamine, marketed under the brand names Dexedrine and Zenzedi, is the only enantiopure amphetamine product currently available. A prodrug form of dextroamphetamine, lisdexamfetamine, is also available and is marketed under the brand name Vyvanse. As it is a prodrug, lisdexamfetamine is structurally different from dextroamphetamine, and is inactive until it metabolizes into dextroamphetamine.^[22]^[274] The free base of racemic amphetamine was previously available as Benzedrine, Psychedrine, and Sympatedrine.^[4] Levoamphetamine was previously available as Cydril.^[4] Many current amphetamine pharmaceuticals are salts due to the comparatively high volatility of the free base.^[4]^[22]^[36] However, oral suspension and orally disintegrating tablet (ODT) dosage forms composed of the free base were introduced in 2015 and 2016, respectively.^[107]^[275]^[276] Some of the current brands and their generic equivalents are listed below.

Amphetamine pharmaceuticals
Brand name	United States Adopted Name	(D:L) ratio	Dosage form	Marketing start date	Sources
Adderall	–	3:1 (salts)	tablet	1996	^[4]^[22]
Adderall XR	–	3:1 (salts)	capsule	2001	^[4]^[22]
Mydayis	–	3:1 (salts)	capsule	2017	^[277]^[278]
Adzenys ER	amphetamine	3:1 (base)	suspension	2017	^[279]
Adzenys XR-ODT	amphetamine	3:1 (base)	ODT	2016	^[276]^[280]
Dyanavel XR	amphetamine	3.2:1 (base)	suspension	2015	^[107]^[275]
Evekeo	amphetamine sulfate	1:1 (salts)	tablet	2012	^[20]^[281]
Evekeo ODT	amphetamine sulfate	1:1 (salts)	ODT	2019	^[282]
Dexedrine	dextroamphetamine sulfate	1:0 (salts)	capsule	1976	^[4]^[22]
Zenzedi	dextroamphetamine sulfate	1:0 (salts)	tablet	2013	^[22]^[283]
Vyvanse	lisdexamfetamine dimesylate	1:0 (prodrug)	capsule	2007	^[4]^[274]^[284]
Vyvanse	lisdexamfetamine dimesylate	1:0 (prodrug)	tablet	2007	^[4]^[274]^[284]
Xelstrym	dextroamphetamine	1:0 (base)	patch	2022	^[285]

Template:Amphetamine base in marketed amphetamine medications

Notes

↑ ^a ^b Adderall and other mixed amphetamine salts products such as Mydayis are not racemic amphetamine – they are a mixture composed of equal parts racemate and dextroamphetamine.
See Mixed amphetamine salts for more information about the mixture, and this section for information about the various mixtures of amphetamine enantiomers marketed.
↑ Synonyms and alternate spellings include: 1-phenylpropan-2-amine (IUPAC name), α-methylphenethylamine, amfetamine (International Nonproprietary Name [INN]), β-phenylisopropylamine, thyramine, and speed.^[6]^[7]^[8]
↑ Enantiomers are molecules that are mirror images of one another; they are structurally identical, but of the opposite orientation.^[9]
Levoamphetamine and dextroamphetamine are also known as L-amph or levamfetamine (INN) and D-amph or dexamfetamine (INN) respectively.^[6]
↑ The brand name Adderall is used throughout this article to refer to the amphetamine four-salt mixture it contains (dextroamphetamine sulfate 25%, dextroamphetamine saccharate 25%, amphetamine sulfate 25%, and amphetamine aspartate 25%). The nonproprietary name, which lists all four active constituent chemicals, is excessively lengthy.^[22]
↑ The term "amphetamines" also refers to a chemical class, but, unlike the class of substituted amphetamines,^[34] the "amphetamines" class does not have a standardized definition in academic literature.^[1] One of the more restrictive definitions of this class includes only the racemate and enantiomers of amphetamine and methamphetamine.^[1] The most general definition of the class encompasses a broad range of pharmacologically and structurally related compounds.^[1]
Due to confusion that may arise from use of the plural form, this article will only use the terms "amphetamine" and "amphetamines" to refer to racemic amphetamine, levoamphetamine, and dextroamphetamine and reserve the term "substituted amphetamines" for its structural class.
↑ The ADHD-related outcome domains with the greatest proportion of significantly improved outcomes from long-term continuous stimulant therapy include academics (≈55% of academic outcomes improved), driving (100% of driving outcomes improved), non-medical drug use (47% of addiction-related outcomes improved), obesity (≈65% of obesity-related outcomes improved), self-esteem (50% of self-esteem outcomes improved), and social function (67% of social function outcomes improved).^[45]

The largest effect sizes for outcome improvements from long-term stimulant therapy occur in the domains involving academics (e.g., grade point average, achievement test scores, length of education, and education level), self-esteem (e.g., self-esteem questionnaire assessments, number of suicide attempts, and suicide rates), and social function (e.g., peer nomination scores, social skills, and quality of peer, family, and romantic relationships).^[45]

Long-term combination therapy for ADHD (i.e., treatment with both a stimulant and behavioral therapy) produces even larger effect sizes for outcome improvements and improves a larger proportion of outcomes across each domain compared to long-term stimulant therapy alone.^[45] These findings were further supported by a 2025 review of interventions for adolescents, which concluded that medications and cognitive-behavioral treatments (CBT) provide complementary benefits. Medications demonstrated strong short-term efficacy on core symptoms, while CBT contributed modest to strong, and sometimes long-lasting, improvements in functional impairments and executive skills when used as part of combination therapy.^[46]
↑ Cochrane reviews are high quality meta-analytic systematic reviews of randomized controlled trials.^[53]
↑ In contrast to the Cochrane reviews that observed higher treatment discontinuation from adverse effects alone, this figure represents any cause of discontinuation (e.g., insufficient perceived treatment benefit).^[56]
↑ The statements supported by the USFDA come from prescribing information, which is the copyrighted intellectual property of the manufacturer and approved by the USFDA. USFDA contraindications are not necessarily intended to limit medical practice but limit claims by pharmaceutical companies.^[102]
↑ According to one review, amphetamine can be prescribed to individuals with a history of abuse provided that appropriate medication controls are employed, such as requiring daily pick-ups of the medication from the prescribing physician.^[4]
↑ In individuals who experience sub-normal height and weight gains, a rebound to normal levels is expected to occur if stimulant therapy is briefly interrupted.^[30]^[44]^[106] The average reduction in final adult height from 3 years of continuous stimulant therapy is 2 cm.^[106]
↑ Transcription factors are proteins that increase or decrease the expression of specific genes.^[127]
↑ In simpler terms, this necessary and sufficient relationship means that ΔFosB overexpression in the nucleus accumbens and addiction-related behavioral and neural adaptations always occur together and never occur alone.
↑ NMDA receptors are voltage-dependent ligand-gated ion channels that requires simultaneous binding of glutamate and a co-agonist ([[D-serine|Template:Smallcaps all-serine]] or glycine) to open the ion channel.^[141]
↑ The review indicated that magnesium L-aspartate and magnesium chloride produce significant changes in addictive behavior;^[117] other forms of magnesium were not mentioned.
↑ The 95% confidence interval indicates that there is a 95% probability that the true number of deaths lies between 3,425 and 4,145.
↑ The human dopamine transporter (hDAT) contains a high-affinity, extracellular, and allosteric Zn²⁺ (zinc ion) binding site which, upon zinc binding, inhibits dopamine reuptake, inhibits amphetamine-induced hDAT internalization, and amplifies amphetamine-induced dopamine efflux.^[159]^[160]^[161]^[162] The human serotonin transporter and norepinephrine transporter do not contain zinc binding sites.^[161]
↑ Mesolimbic dopamine neurons co-express the glutamate transporter EAAT3 alongside DAT, permitting amphetamine-induced EAAT3 internalization to influence glutamatergic signaling in the mesolimbic pathway.^[179]^[169]
↑ Amphetamine interacts with its receptor protein target(s), TAAR1 and an as-yet-unidentified biomolecular target, which initiates signaling cascades that generate second messengers and activate protein kinases. The activated kinases then phosphorylate their respective transporter(s), which in turn causes a conformational change in transporter protein, thereby altering its function and affecting dopaminergic/glutamatergic neurotransmission at dopaminergic synapses.^[169]^[170]
↑ There is substantial variation in microbiome composition and microbial concentrations by anatomical site.^[217]^[218] Fluid from the human colon – which contains the highest concentration of microbes of any anatomical site – contains approximately one trillion (10^12) bacterial cells/ml.^[217]
↑ Enantiomers are molecules that are mirror images of one another; they are structurally identical, but of the opposite orientation.^[9]
↑ The active ingredient in some OTC inhalers in the United States is listed as levmetamfetamine, the INN and USAN of levomethamphetamine.^[248]^[249]

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Reference notes

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References

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Figure 3: Treatment benefit by treatment type and outcome group
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External links

Script error: No such module "citation/CS1".
CID 5826 from PubChem Template:EditAtWikidata Template:WikidataCheck – Dextroamphetamine
CID 32893 from PubChem Template:EditAtWikidata Template:WikidataCheck – Levoamphetamine
Comparative Toxicogenomics Database entry: Amphetamine
Comparative Toxicogenomics Database entry: CARTPT

Template:Amphetamine Template:ADHD pharmacotherapies Template:TAAR ligands Template:Monoamine releasing agents Script error: No such module "Navbox". Template:Drug use Template:Chemical classes of psychoactive drugs Template:Portal bar Template:Authority control

Template:Top icon

[AdderallDiff-5] Adderall and other mixed amphetamine salts products such as Mydayis are not racemic amphetamine – they are a mixture composed of equal parts racemate and dextroamphetamine.
See Mixed amphetamine salts for more information about the mixture, and this section for information about the various mixtures of amphetamine enantiomers marketed.

[10] Synonyms and alternate spellings include: 1-phenylpropan-2-amine (IUPAC name), α-methylphenethylamine, amfetamine (International Nonproprietary Name [INN]), β-phenylisopropylamine, thyramine, and speed.^[6]^[7]^[8]

[12] Enantiomers are molecules that are mirror images of one another; they are structurally identical, but of the opposite orientation.^[9]
Levoamphetamine and dextroamphetamine are also known as L-amph or levamfetamine (INN) and D-amph or dexamfetamine (INN) respectively.^[6]

[UseOfAdderallName-27] The brand name Adderall is used throughout this article to refer to the amphetamine four-salt mixture it contains (dextroamphetamine sulfate 25%, dextroamphetamine saccharate 25%, amphetamine sulfate 25%, and amphetamine aspartate 25%). The nonproprietary name, which lists all four active constituent chemicals, is excessively lengthy.^[22]

[42] The term "amphetamines" also refers to a chemical class, but, unlike the class of substituted amphetamines,^[34] the "amphetamines" class does not have a standardized definition in academic literature.^[1] One of the more restrictive definitions of this class includes only the racemate and enantiomers of amphetamine and methamphetamine.^[1] The most general definition of the class encompasses a broad range of pharmacologically and structurally related compounds.^[1]
Due to confusion that may arise from use of the plural form, this article will only use the terms "amphetamine" and "amphetamines" to refer to racemic amphetamine, levoamphetamine, and dextroamphetamine and reserve the term "substituted amphetamines" for its structural class.

[56] The ADHD-related outcome domains with the greatest proportion of significantly improved outcomes from long-term continuous stimulant therapy include academics (≈55% of academic outcomes improved), driving (100% of driving outcomes improved), non-medical drug use (47% of addiction-related outcomes improved), obesity (≈65% of obesity-related outcomes improved), self-esteem (50% of self-esteem outcomes improved), and social function (67% of social function outcomes improved).^[45]

The largest effect sizes for outcome improvements from long-term stimulant therapy occur in the domains involving academics (e.g., grade point average, achievement test scores, length of education, and education level), self-esteem (e.g., self-esteem questionnaire assessments, number of suicide attempts, and suicide rates), and social function (e.g., peer nomination scores, social skills, and quality of peer, family, and romantic relationships).^[45]

Long-term combination therapy for ADHD (i.e., treatment with both a stimulant and behavioral therapy) produces even larger effect sizes for outcome improvements and improves a larger proportion of outcomes across each domain compared to long-term stimulant therapy alone.^[45] These findings were further supported by a 2025 review of interventions for adolescents, which concluded that medications and cognitive-behavioral treatments (CBT) provide complementary benefits. Medications demonstrated strong short-term efficacy on core symptoms, while CBT contributed modest to strong, and sometimes long-lasting, improvements in functional impairments and executive skills when used as part of combination therapy.^[46]

[64] Cochrane reviews are high quality meta-analytic systematic reviews of randomized controlled trials.^[53]

[all-cause_discontinuation-68] In contrast to the Cochrane reviews that observed higher treatment discontinuation from adverse effects alone, this figure represents any cause of discontinuation (e.g., insufficient perceived treatment benefit).^[56]

[116] The statements supported by the USFDA come from prescribing information, which is the copyrighted intellectual property of the manufacturer and approved by the USFDA. USFDA contraindications are not necessarily intended to limit medical practice but limit claims by pharmaceutical companies.^[102]

[117] According to one review, amphetamine can be prescribed to individuals with a history of abuse provided that appropriate medication controls are employed, such as requiring daily pick-ups of the medication from the prescribing physician.^[4]

[122] In individuals who experience sub-normal height and weight gains, a rebound to normal levels is expected to occur if stimulant therapy is briefly interrupted.^[30]^[44]^[106] The average reduction in final adult height from 3 years of continuous stimulant therapy is 2 cm.^[106]

[149] Transcription factors are proteins that increase or decrease the expression of specific genes.^[127]

[150] In simpler terms, this necessary and sufficient relationship means that ΔFosB overexpression in the nucleus accumbens and addiction-related behavioral and neural adaptations always occur together and never occur alone.

[167] NMDA receptors are voltage-dependent ligand-gated ion channels that requires simultaneous binding of glutamate and a co-agonist ([[D-serine|Template:Smallcaps all-serine]] or glycine) to open the ion channel.^[141]

[168] The review indicated that magnesium L-aspartate and magnesium chloride produce significant changes in addictive behavior;^[117] other forms of magnesium were not mentioned.

[176] The 95% confidence interval indicates that there is a 95% probability that the true number of deaths lies between 3,425 and 4,145.

[zinc-193] The human dopamine transporter (hDAT) contains a high-affinity, extracellular, and allosteric Zn²⁺ (zinc ion) binding site which, upon zinc binding, inhibits dopamine reuptake, inhibits amphetamine-induced hDAT internalization, and amplifies amphetamine-induced dopamine efflux.^[159]^[160]^[161]^[162] The human serotonin transporter and norepinephrine transporter do not contain zinc binding sites.^[161]

[mesolimbic_EAAT3-233] Mesolimbic dopamine neurons co-express the glutamate transporter EAAT3 alongside DAT, permitting amphetamine-induced EAAT3 internalization to influence glutamatergic signaling in the mesolimbic pathway.^[179]^[169]

[DAT_table-238] Amphetamine interacts with its receptor protein target(s), TAAR1 and an as-yet-unidentified biomolecular target, which initiates signaling cascades that generate second messengers and activate protein kinases. The activated kinases then phosphorylate their respective transporter(s), which in turn causes a conformational change in transporter protein, thereby altering its function and affecting dopaminergic/glutamatergic neurotransmission at dopaminergic synapses.^[169]^[170]

[256] There is substantial variation in microbiome composition and microbial concentrations by anatomical site.^[217]^[218] Fluid from the human colon – which contains the highest concentration of microbes of any anatomical site – contains approximately one trillion (10^12) bacterial cells/ml.^[217]

[261] Enantiomers are molecules that are mirror images of one another; they are structurally identical, but of the opposite orientation.^[9]

[OTC_levmetamfetamine-290] The active ingredient in some OTC inhalers in the United States is listed as levmetamfetamine, the INN and USAN of levomethamphetamine.^[248]^[249]

[25] [4]^[10]^[1]^[11]^[12]^[13]^[14]^[15]^[16]^[17]^[18]^[19]^[20]^[21]

[31] [4]^[23]^[11]^[14]^[20]^[24]^[25]

[40] [23]^[11]^[12]^[13]^[17]^[26]^[27]^[28]^[29]^[30]^[31]^[32]^[33]

[46] [35]^[36]^[37]

[BED_efficacy-80] [60]^[21]^[64]^[61]^[67]

[125] [3]^[13]^[26]^[106]^[107]^[108]

[130] [109]^[110]^[111]^[112]

[131] [13]^[103]^[109]^[111]

[133] [17]^[13]^[26]^[113]

[Exercise_therapy-145] [121]^[122]^[123]^[124]^[143]

[153] [119]^[121]^[120]^[128]^[129]

[158] [120]^[131]^[132]^[133]

[179] [8]^[13]^[26]^[148]^[150]

[186] [39]^[152]^[155]^[156]

[TAAR1_phosphorylation-206] [24]^[169]^[172]^[173]^[174]

[Reuptake_inhibition-217] [167]^[179]^[180]^[181]^[182]^[183]^[184]

[230] [24]^[167]^[180]^[181]^[185]^[190]

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[285] [12]^[243]^[244]^[245]

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Figure 3: Treatment benefit by treatment type and outcome group

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@@ Line 16: / Line 16: @@
 | width2 = 300
-<!-- Clinical data -->
+<!-- Clinical data -->| pronounce = {{IPAc-en|audio=En-us-amphetamine.ogg|æ|m|ˈ|f|ɛ|t|ə|m|iː|n}}
-| pronounce = {{IPAc-en|audio=En-us-amphetamine.ogg|æ|m|ˈ|f|ɛ|t|ə|m|iː|n}}
 | tradename = Evekeo, [[Adderall]],{{#tag:ref|Adderall and other mixed amphetamine salts products such as Mydayis are not [[Racemic mixture|racemic]] amphetamine – they are a mixture composed of equal parts racemate and [[dextroamphetamine]].<br />
 ''See [[Mixed amphetamine salts]] for more information about the mixture, and [[#Pharmaceutical products|this section]] for information about the various mixtures of amphetamine [[enantiomer]]s marketed.''|name=AdderallDiff|group=note}} [[#Pharmaceutical products|others]]
@@ Line 33: / Line 32: @@
 | ATC_supplemental = {{ATC|N06|BA02}} {{ATC|N06|BA12}}
-<!-- Legal status -->
+<!-- Legal status -->| legal_AU = Schedule 8
-| legal_AU = Schedule 8
 | legal_BR = A3
 | legal_BR_comment =
@@ Line 43: / Line 41: @@
 | legal_US = [[List of Schedule II controlled substances (U.S.)|Schedule II]]<ref name=":USAS2">{{Cite web | vauthors = Ingersoll J |date=7 July 1971 |title=Amphetamine, Methamphetamine, and Optical Isomers |url=https://archives.federalregister.gov/issue_slice/1971/7/7/12730-12734.pdf |url-status=live |archive-url= https://archive.today/20241127164332/https://archives.federalregister.gov/issue_slice/1971/7/7/12730-12734.pdf |archive-date=27 November 2024 |access-date=27 November 2024 |website=[[Federal Register]]|publisher=[[Bureau of Narcotics and Dangerous Drugs]]}}</ref>
 | legal_UN = Psychotropic Schedule II
-| legal_status =
+| legal_status = <!-- Physiological data -->
-<!-- Physiological data -->
 | target_tissues =
 | receptors = [[Trace amine-associated receptor 1|TAAR1]], [[VMAT2]], [[5HT1A]]
-<!-- Pharmacokinetic data -->
+<!-- Pharmacokinetic data -->| bioavailability = Oral: {{nowrap|~90%}}<ref name="Antunes_2022" />
-| bioavailability = Oral: {{nowrap|~90%}}<ref name="handbook2022" />
 | protein_bound = {{nowrap|20%}}<ref name="Drugbank-amph" />
 | metabolism = [[CYP2D6]],<ref name="FDA Pharmacokinetics" /> [[Dopamine β-hydroxylase|DBH]],<ref name="Substituted amphetamines, FMO, and DBH" /><ref name="DBH amph primary" /> [[Flavin-containing monooxygenase 3|FMO3]]<ref name="Substituted amphetamines, FMO, and DBH" /><ref name="FMO" /><ref name="FMO3-Primary" />
@@ Line 59: / Line 54: @@
 | excretion = Primarily [[renal]];<br />[[pH]]-dependent {{nowrap|range: 1–75%}}<ref name="FDA Pharmacokinetics" />
-<!-- Identifiers -->
+<!-- Identifiers -->| IUPAC_name = <div class="center">(''RS'')-1-phenylpropan-2-amine</div>
-| IUPAC_name = <div class="center">(''RS'')-1-phenylpropan-2-amine</div>
 | synonyms = α-methylphenethylamine
 | CAS_number_Ref = {{cascite|correct|CAS}}
@@ Line 79: / Line 73: @@
 | ChEMBL = 405
 | NIAID_ChemDB = 018564
-| PDB_ligand =
+| PDB_ligand = <!-- Chemical and physical data -->
-<!-- Chemical and physical data -->
 | C = 9
 | H = 13
@@ Line 220: / Line 212: @@
 ====Dependence and withdrawal====
 [[Drug tolerance]] develops rapidly in amphetamine abuse (i.e., recreational amphetamine use), so periods of extended abuse require increasingly larger doses of the drug in order to achieve the same effect.<ref name="Cochrane 2013 treatments">{{cite journal | vauthors = Perez-Mana C, Castells X, Torrens M, Capella D, Farre M | title = Efficacy of psychostimulant drugs for amphetamine abuse or dependence | journal =Cochrane Database of Systematic Reviews| volume = 2013 | issue = 9 | pages = CD009695 | date = September 2013 | pmid = 23996457 | doi = 10.1002/14651858.CD009695.pub2 | pmc = 11521360 }}</ref><ref>{{cite web| title = Amphetamines: Drug Use and Abuse | website = Merck Manual Home Edition | publisher = Merck | url = http://www.merckmanuals.com/home/special_subjects/drug_use_and_abuse/amphetamines.html | access-date = 28 February 2007 | archive-url = https://web.archive.org/web/20070217053619/http://www.merck.com/mmhe/sec07/ch108/ch108g.html |date=February 2003 | archive-date = 17 February 2007}}</ref>
-According to a Cochrane review on [[drug withdrawal|withdrawal]] in individuals who compulsively use amphetamine and methamphetamine, "when chronic heavy users abruptly discontinue amphetamine use, many report a time-limited withdrawal syndrome that occurs within 24&nbsp;hours of their last dose."<ref name="Cochrane Withdrawal">{{cite journal |vauthors=Shoptaw SJ, Kao U, Heinzerling K, Ling W | title = Treatment for amphetamine withdrawal | journal =Cochrane Database of Systematic Reviews| issue = 2 | pages = CD003021 | date = April 2009 | volume = 2009 | pmid = 19370579 | doi = 10.1002/14651858.CD003021.pub2 | veditors = Shoptaw SJ | quote = The prevalence of this withdrawal syndrome is extremely common (Cantwell 1998; Gossop 1982) with 87.6% of 647 individuals with amphetamine dependence reporting six or more signs of amphetamine withdrawal listed in the DSM when the drug is not available (Schuckit 1999)&nbsp;... The severity of withdrawal symptoms is greater in amphetamine dependent individuals who are older and who have more extensive amphetamine use disorders (McGregor 2005). Withdrawal symptoms typically present within 24&nbsp;hours of the last use of amphetamine, with a withdrawal syndrome involving two general phases that can last 3 weeks or more. The first phase of this syndrome is the initial "crash" that resolves within about a week (Gossop 1982;McGregor 2005)&nbsp;... | pmc = 7138250}}</ref> This review noted that withdrawal symptoms in chronic, high-dose users are frequent, occurring in roughly 88% of cases, and persist for {{nowrap|3–4}}&nbsp;weeks with a marked "crash" phase occurring during the first week.<ref name="Cochrane Withdrawal" /> Amphetamine withdrawal symptoms can include anxiety, [[Craving (withdrawal)|drug craving]], [[Dysphoria|depressed mood]], [[Fatigue (medical)|fatigue]], [[hyperphagia|increased appetite]], increased movement or [[psychomotor retardation|decreased movement]], lack of motivation, sleeplessness or sleepiness, and [[lucid dream]]s.<ref name="Cochrane Withdrawal" /> The review indicated that the severity of withdrawal symptoms is positively correlated with the age of the individual and the extent of their dependence.<ref name="Cochrane Withdrawal" /> Mild withdrawal symptoms from the discontinuation of amphetamine treatment at therapeutic doses can be avoided by tapering the dose.<ref name="Stahl's Essential Psychopharmacology" />
+According to a Cochrane review on [[drug withdrawal|withdrawal]] in individuals who compulsively use amphetamine and methamphetamine, "when chronic heavy users abruptly discontinue amphetamine use, many report a time-limited withdrawal syndrome that occurs within 24&nbsp;hours of their last dose."<ref name="Cochrane Withdrawal">{{cite journal |vauthors=Shoptaw SJ, Kao U, Heinzerling K, Ling W | title = Treatment for amphetamine withdrawal | journal =Cochrane Database of Systematic Reviews| issue = 2 | pages = CD003021 | date = April 2009 | volume = 2009 | pmid = 19370579 | doi = 10.1002/14651858.CD003021.pub2 | veditors = Shoptaw SJ | quote = The prevalence of this withdrawal syndrome is extremely common (Cantwell 1998; Gossop 1982) with 87.6% of 647 individuals with amphetamine dependence reporting six or more signs of amphetamine withdrawal listed in the DSM when the drug is not available (Schuckit 1999)&nbsp;... The severity of withdrawal symptoms is greater in amphetamine dependent individuals who are older and who have more extensive amphetamine use disorders (McGregor 2005). Withdrawal symptoms typically present within 24&nbsp;hours of the last use of amphetamine, with a withdrawal syndrome involving two general phases that can last 3 weeks or more. The first phase of this syndrome is the initial "crash" that resolves within about a week (Gossop 1982;McGregor 2005)&nbsp;... | pmc = 7138250}}</ref> This review noted that withdrawal symptoms in chronic, high-dose users are frequent, occurring in roughly 88% of cases, and persist for {{nowrap|3–4}}&nbsp;weeks with a marked "crash" phase occurring during the first week.<ref name="Cochrane Withdrawal" /> Amphetamine withdrawal symptoms can include anxiety, [[Craving (withdrawal)|drug craving]], [[Dysphoria|depressed mood]], [[Fatigue (medical)|fatigue]], [[hyperphagia|increased appetite]], increased movement or [[psychomotor retardation|decreased movement]], lack of motivation, sleeplessness or sleepiness, and [[lucid dream]]s.<ref name="Cochrane Withdrawal" /> The review indicated that the severity of withdrawal symptoms is positively correlated with the age of the individual and the extent of their dependence.<ref name="Cochrane Withdrawal" />
+According to a 2025 review, the discontinuation of amphetamine at therapeutic doses does not typically result in withdrawal symptoms.<ref name="2025_Leaver">{{Cite journal | vauthors = Leaver L |date=2025-06-03 |title=Medical management of ADHD in adults: part 2 |url=https://pubmed.ncbi.nlm.nih.gov/40461172 |journal=Drug and Therapeutics Bulletin |volume=63 |issue=6 |pages=85–93 |doi=10.1136/dtb.2025.000019 |pmid=40461172 |quote=Tolerance to stimulants is rare (<3%) at least after the initial dose titration period. If there are repeated requests for increasing doses, this might suggest non- medical use, or that treatment goals may not reflect what ADHD medication can achieve. Drug ‘holidays’ are not necessary to avoid the risk of tolerance (but may be helpful to assess or mitigate adverse effects, or to establish continuing need for treatment).&nbsp;...</br> There are many SPCs for different stimulants mention the possibility of withdrawal symptoms. In practice, many patients experience periods without medication but do not suffer withdrawal symptoms. Discontinuation may unmask symptoms of ADHD, but small trials of discontinuing therapeutic doses of methylphenidate and lisdexamfetamine have not found withdrawal symptoms. |doi-access=free}}</ref> Discontinuation may unmask or cause a rebound of ADHD symptoms due to the cessation of treatment-related drug effects.<ref name="2025_Leaver" /> In cases where mild withdrawal symptoms do occur, they can be avoided by tapering the dose.<ref name="Stahl's Essential Psychopharmacology" /> Unlike amphetamine abuse, where drug tolerance necessitates escalating doses to achieve the same effect, tolerance to clinically relevant doses of amphetamine plateaus after the initial titration period, and "drug holidays" (i.e., temporary treatment discontinuation) are not required to prevent the development of tolerance.<ref name="2025_Leaver" />
 ==Overdose==
@@ Line 304: / Line 298: @@
 Amphetamine exerts its behavioral effects by altering the use of [[monoamines]] as neuronal signals in the brain, primarily in [[catecholamine]] neurons in the reward and executive function pathways of the brain.<ref name="Miller" /><ref name="cognition enhancers" /> The concentrations of the main neurotransmitters involved in reward circuitry and executive functioning, dopamine and norepinephrine, increase dramatically in a dose-dependent manner by amphetamine because of its effects on [[monoamine transporter]]s.<ref name="Miller" /><ref name="cognition enhancers" /><ref name="E Weihe" /> The [[reinforcement|reinforcing]] and [[motivational salience]]-promoting effects of amphetamine are due mostly to enhanced dopaminergic activity in the [[mesolimbic pathway]].<ref name="Malenka_2009" /> 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]].<ref name="Amph Uses" />
-Amphetamine potentiates monoaminergic neurotransmission by entering the presynaptic neuron both as a substrate for monoamine transporters ([[Dopamine transporter|DAT]], [[Norepinephrine|NET]], and, [[Serotonin transporter|SERT]]) and by passive diffusion across the [[neuronal membrane]].<ref name="Stahl2021">{{Cite book |title=Stahl's essential psychopharmacology: neuroscientific basis and practical applications |vauthors=Stahl SM |publisher=Cambridge University Press |year=2021 |isbn=9781108975292 |edition=5th |location=Cambridge |pages=471-73 |quote=Unlike methylphenidate and reuptake blocking drugs used for depression, amphetamine is a competitive inhibitor and pseudosubstrate for NETs and DATs (Figure 11-32, top left), binding at the same site that the monoamines bind to the transporters, thus inhibiting NE and DA reuptake. At the doses of amphetamine used for the treatment of ADHD, the clinical differences between the actions of amphetamine versus methylphenidate can be relatively small. However, at the high doses of amphetamine used by stimulant addicts, additional pharmacological actions of amphetamine are triggered.&nbsp;...<br /> Once there in sufficient quantities, such as occurs at doses taken for abuse, amphetamine is also a competitive inhibitor of the vesicular transporter (VMAT2) for both DA and NE. Once amphetamine hitch-hikes another ride into synaptic vesicles, it displaces DA there, causing a flood of DA release. As DA accumulates in the cytoplasm of the presynaptic neuron, it causes the DATs to reverse directions, spilling intracellular DA into the synapse, and also opening presynaptic channels to further release DA in a flood into the synapse. These pharmacological actions of high-dose amphetamine are not linked to therapeutic action in ADHD but to reinforcement, reward, and euphoria in amphetamine abuse. &nbsp;...<br /> The D-isomer of amphetamine is more potent than the L-isomer for DAT binding, but D- and L- amphetamine isomers are more equally potent in their actions on NET binding. Thus, D-amphetamine preparations will have relatively more action on DATs at lower therapeutic doses utilized for the treatment of ADHD.}}</ref><ref name="handbook2022_DAT">{{Cite book |title=Handbook of Substance Misuse and Addictions |vauthors=Tendilla-Beltran H, Arroyo-García LE, Flores G |publisher=Springer International Publishing |year=2022 |isbn=978-3-030-92391-4 |veditors=Patel VB, Preedy VR |location=Cham |pages=2176-2177 |chapter=Chapter 102: Amphetamine and the Biology of Neuronal Morphology |doi=10.1007/978-3-030-92392-1 |quote=At low concentrations, amphetamines (extracellular) and dopamine (intracellular) are interchanged as described by the exchange diffusion model&nbsp;... Amphetamines can also increase dopaminergic transmission by channel-like transport which involves second-messenger signaling. Amphetamines increase PKC activity, which increase DAT N-terminus domain phosphorylation, and consequently DAT activity, which, because of the amphetamines, will release dopamine from the presynaptic terminal.&nbsp; PKC and CaMKIIα-mediated reverse transport have also been demonstrated in NET&nbsp;...<br /> Also, amphetamines can indirectly enhance monoaminergic neurotransmission through the stimulation of trace amine-associated receptor 1 (TAAR1) (Underhill et al. 2021). TAAR1 is an intracellular G protein-coupled receptor (GPCR), which has activity that promotes the endocytosis of both DAT and the excitatory amino acid transporter 3 (EAAT3). DAT endocytosis, together with the aforementioned mechanisms, contributes to the enhancement of the dopaminergic neurotransmission.&nbsp;... <br /> It is important to note that amphetamines also stimulate protein kinase A (PKA) activity, which in turn inhibits RhoA activity and consequently reduces DAT internalization.}}</ref> Transporter-mediated uptake competes with reabsorption of [[endogenous]] neurotransmitters from the synaptic cleft and produces competitive [[Reuptake inhibitor|reuptake inhibition]] as a consequence.<ref name="Stahl2021" /> Once inside the neuronal [[cytosol]], amphetamine initiates intracellular [[Biochemical cascade|signaling cascades]] that activate [[protein kinase C]] (PKC), leading to [[phosphorylation]] of DAT, NET, and SERT.<ref name="handbook2022_DAT" /> PKC-dependent phosphorylation of monoamine transporters can either reverse their direction to induce efflux of cytosolic neurotransmitters into the synaptic cleft, or trigger the withdrawal of transporters into the presynaptic neuron ([[Endocytosis|internalization]]), thereby ceasing their reuptake function in a non-competitive manner.<ref name="handbook2022_DAT" /><ref name="Kinase-dependent transporter regulation review">{{cite journal |vauthors=Bermingham DP, Blakely RD |date=October 2016 |title=Kinase-dependent Regulation of Monoamine Neurotransmitter Transporters |journal=Pharmacol. Rev. |volume=68 |issue=4 |pages=888–953 |doi=10.1124/pr.115.012260 |pmc=5050440 |pmid=27591044 |quote=<!--RhoA signaling--> The Amara laboratory recently provided evidence that AMPH triggered DAT endocytosis is clathrin-independent and requires the small GTPase Rho (Wheeler et al., 2015)...<!--CAMKII signaling--> Whereas little support for CaMKII regulation of DA uptake exists, substantial evidence supports a role for the kinase in DAT-dependent DA efflux triggered by AMPH... Importantly, AMPH treatment of DAT transfected cells produced a rise in intracellular Ca2+ that could be blocked by thapsigargin or cocaine, supporting a model whereby AMPH is first transported into cells where it can then produce release of endoplasmic reticulum Ca2+ stores. Subsequently, AMPH was shown to activate CaMKII in DAT transfected cells (Wei et al., 2007).&nbsp;... At present, information is lacking as to the site(s) that support CaMKII phosphorylation of DAT in vivo ... The current model... DAT by phosphorylating one or more Ser residues in the transporter N terminus. This phosphorylation is then thought to facilitate conformational changes that place the transporter in a “DA efflux-willing” conformation.}}</ref> Amphetamine also causes a rise in [[Calcium in biology|intracellular calcium]], an effect associated with transporter phosphorylation through a [[Ca2+/calmodulin-dependent protein kinase II alpha|Ca²⁺/calmodulin-dependent protein kinase II alpha]] (CaMKIIα) signaling cascade.<ref name="handbook2022_DAT" /> Unlike PKC, CaMKIIα-mediated transporter phosphorylation appears to reverse the direction of DAT and NET without triggering internalization.<ref name="handbook2022_DAT" /><ref name="2020_Reith">{{cite journal |vauthors=Reith ME, Gnegy ME |date=2020 |title=Molecular Mechanisms of Amphetamines |journal=Handbook of Experimental Pharmacology |volume=258 |pages=265–297 |doi=10.1007/164_2019_251 |pmid=31286212 |quote=At lower doses, amphetamine preferentially releases a newly synthesized pool of DA. Administration of the tyrosine hydroxylase inhibitor α-methyl-para-tyrosine (AMPT) simultaneously with amphetamine blocks the DA-releasing effect of amphetamine (Smith 1963; Weissman et al. 1966; Chiueh and Moore 1975; Butcher et al. 1988).&nbsp;...<br /> Undoubtedly vesicles contribute strongly to the maximal DA released by amphetamine, although VMAT2 is not absolutely required for amphetamine to release DA from nerve terminals (Pifl et al. 1995; Fon et al. 1997; Wang et al. 1997; Patel et al. 2003).&nbsp;...<br /> However, the study in rat PC12 cells and hDAT-HEK293 cells demonstrated some involvement of extracellular Ca2+ (effect of nisoxetine or removal of extracellular Ca2+) and as well as of Ca2+ stores in the endoplasmic reticulum (blockade by thapsigargin) (Gnegy et al. 2004).&nbsp;...<br /> The increase in intracellular Ca2+ stimulated by amphetamine activates two major modulators of amphetamine action: protein kinase C (PKC) and Ca2+ and calmodulin-stimulated protein kinase II (CaMKII).}}</ref>
+Amphetamine potentiates monoaminergic neurotransmission by entering the presynaptic neuron both as a substrate for monoamine transporters ([[Dopamine transporter|DAT]], [[Norepinephrine|NET]], and, [[Serotonin transporter|SERT]]) and by passive diffusion across the [[neuronal membrane]].<ref name="Stahl2021">{{Cite book |title=Stahl's essential psychopharmacology: neuroscientific basis and practical applications |vauthors=Stahl SM |publisher=Cambridge University Press |year=2021 |isbn=9781108975292 |edition=5th |location=Cambridge |pages=471-73 |quote=Unlike methylphenidate and reuptake blocking drugs used for depression, amphetamine is a competitive inhibitor and pseudosubstrate for NETs and DATs (Figure 11-32, top left), binding at the same site that the monoamines bind to the transporters, thus inhibiting NE and DA reuptake. At the doses of amphetamine used for the treatment of ADHD, the clinical differences between the actions of amphetamine versus methylphenidate can be relatively small. However, at the high doses of amphetamine used by stimulant addicts, additional pharmacological actions of amphetamine are triggered.&nbsp;...<br /> Once there in sufficient quantities, such as occurs at doses taken for abuse, amphetamine is also a competitive inhibitor of the vesicular transporter (VMAT2) for both DA and NE. Once amphetamine hitch-hikes another ride into synaptic vesicles, it displaces DA there, causing a flood of DA release. As DA accumulates in the cytoplasm of the presynaptic neuron, it causes the DATs to reverse directions, spilling intracellular DA into the synapse, and also opening presynaptic channels to further release DA in a flood into the synapse. These pharmacological actions of high-dose amphetamine are not linked to therapeutic action in ADHD but to reinforcement, reward, and euphoria in amphetamine abuse. &nbsp;...<br /> The D-isomer of amphetamine is more potent than the L-isomer for DAT binding, but D- and L- amphetamine isomers are more equally potent in their actions on NET binding. Thus, D-amphetamine preparations will have relatively more action on DATs at lower therapeutic doses utilized for the treatment of ADHD.}}</ref><ref name="handbook2022_DAT">{{Cite book |title=Handbook of Substance Misuse and Addictions |vauthors=Tendilla-Beltran H, Arroyo-García LE, Flores G |publisher=Springer International Publishing |year=2022 |isbn=978-3-030-92391-4 |veditors=Patel VB, Preedy VR |location=Cham |pages=2176-2177 |chapter=Chapter 102: Amphetamine and the Biology of Neuronal Morphology |doi=10.1007/978-3-030-92392-1_115 |quote=At low concentrations, amphetamines (extracellular) and dopamine (intracellular) are interchanged as described by the exchange diffusion model&nbsp;... Amphetamines can also increase dopaminergic transmission by channel-like transport which involves second-messenger signaling. Amphetamines increase PKC activity, which increase DAT N-terminus domain phosphorylation, and consequently DAT activity, which, because of the amphetamines, will release dopamine from the presynaptic terminal.&nbsp; PKC and CaMKIIα-mediated reverse transport have also been demonstrated in NET&nbsp;...<br /> Also, amphetamines can indirectly enhance monoaminergic neurotransmission through the stimulation of trace amine-associated receptor 1 (TAAR1) (Underhill et al. 2021). TAAR1 is an intracellular G protein-coupled receptor (GPCR), which has activity that promotes the endocytosis of both DAT and the excitatory amino acid transporter 3 (EAAT3). DAT endocytosis, together with the aforementioned mechanisms, contributes to the enhancement of the dopaminergic neurotransmission.&nbsp;... <br /> It is important to note that amphetamines also stimulate protein kinase A (PKA) activity, which in turn inhibits RhoA activity and consequently reduces DAT internalization.}}</ref> Transporter-mediated uptake competes with reabsorption of [[endogenous]] neurotransmitters from the synaptic cleft and produces competitive [[Reuptake inhibitor|reuptake inhibition]] as a consequence.<ref name="Stahl2021" /> Once inside the neuronal [[cytosol]], amphetamine initiates intracellular [[Biochemical cascade|signaling cascades]] that activate [[protein kinase C]] (PKC), leading to [[phosphorylation]] of DAT, NET, and SERT.<ref name="handbook2022_DAT" /> PKC-dependent phosphorylation of monoamine transporters can either reverse their direction to induce efflux of cytosolic neurotransmitters into the synaptic cleft, or trigger the withdrawal of transporters into the presynaptic neuron ([[Endocytosis|internalization]]), thereby ceasing their reuptake function in a non-competitive manner.<ref name="handbook2022_DAT" /><ref name="Kinase-dependent transporter regulation review">{{cite journal |vauthors=Bermingham DP, Blakely RD |date=October 2016 |title=Kinase-dependent Regulation of Monoamine Neurotransmitter Transporters |journal=Pharmacol. Rev. |volume=68 |issue=4 |pages=888–953 |doi=10.1124/pr.115.012260 |pmc=5050440 |pmid=27591044 |quote=<!--RhoA signaling--> The Amara laboratory recently provided evidence that AMPH triggered DAT endocytosis is clathrin-independent and requires the small GTPase Rho (Wheeler et al., 2015)...<!--CAMKII signaling--> Whereas little support for CaMKII regulation of DA uptake exists, substantial evidence supports a role for the kinase in DAT-dependent DA efflux triggered by AMPH... Importantly, AMPH treatment of DAT transfected cells produced a rise in intracellular Ca2+ that could be blocked by thapsigargin or cocaine, supporting a model whereby AMPH is first transported into cells where it can then produce release of endoplasmic reticulum Ca2+ stores. Subsequently, AMPH was shown to activate CaMKII in DAT transfected cells (Wei et al., 2007).&nbsp;... At present, information is lacking as to the site(s) that support CaMKII phosphorylation of DAT in vivo ... The current model... DAT by phosphorylating one or more Ser residues in the transporter N terminus. This phosphorylation is then thought to facilitate conformational changes that place the transporter in a “DA efflux-willing” conformation.}}</ref> Amphetamine also causes a rise in [[Calcium in biology|intracellular calcium]], an effect associated with transporter phosphorylation through a [[Ca2+/calmodulin-dependent protein kinase II alpha|Ca²⁺/calmodulin-dependent protein kinase II alpha]] (CaMKIIα) signaling cascade.<ref name="handbook2022_DAT" /> Unlike PKC, CaMKIIα-mediated transporter phosphorylation appears to reverse the direction of DAT and NET without triggering internalization.<ref name="handbook2022_DAT" /><ref name="2020_Reith">{{cite journal |vauthors=Reith ME, Gnegy ME |date=2020 |title=Molecular Mechanisms of Amphetamines |journal=Handbook of Experimental Pharmacology |volume=258 |pages=265–297 |doi=10.1007/164_2019_251 |pmid=31286212 |quote=At lower doses, amphetamine preferentially releases a newly synthesized pool of DA. Administration of the tyrosine hydroxylase inhibitor α-methyl-para-tyrosine (AMPT) simultaneously with amphetamine blocks the DA-releasing effect of amphetamine (Smith 1963; Weissman et al. 1966; Chiueh and Moore 1975; Butcher et al. 1988).&nbsp;...<br /> Undoubtedly vesicles contribute strongly to the maximal DA released by amphetamine, although VMAT2 is not absolutely required for amphetamine to release DA from nerve terminals (Pifl et al. 1995; Fon et al. 1997; Wang et al. 1997; Patel et al. 2003).&nbsp;...<br /> However, the study in rat PC12 cells and hDAT-HEK293 cells demonstrated some involvement of extracellular Ca2+ (effect of nisoxetine or removal of extracellular Ca2+) and as well as of Ca2+ stores in the endoplasmic reticulum (blockade by thapsigargin) (Gnegy et al. 2004).&nbsp;...<br /> The increase in intracellular Ca2+ stimulated by amphetamine activates two major modulators of amphetamine action: protein kinase C (PKC) and Ca2+ and calmodulin-stimulated protein kinase II (CaMKII).}}</ref>
-Amphetamine has been identified as a [[full agonist]] of [[TAAR1|trace amine-associated receptor 1]] (TAAR1), a {{nowrap|[[Gs alpha subunit|G<sub>s</sub>-coupled]]}} and {{nowrap|[[Gq alpha subunit|G<sub>q</sub>-coupled]]}} [[G protein-coupled receptor]] (GPCR) discovered in 2001, which is important for regulation of brain monoamines.<ref name="Miller" /> Several reviews have linked amphetamine’s agonism at TAAR1 to modulation of monoamine transporter function and subsequent neurotransmitter efflux and reuptake inhibition at monoaminergic synapses.{{#tag:ref|<ref name="Miller" /><ref name="handbook2022_DAT" /><ref name="2022 T1 LDX">{{Cite journal |vauthors=Quintero J, Gutiérrez-Casares JR, Álamo C |date=11 August 2022 |title=Molecular Characterisation of the Mechanism of Action of Stimulant Drugs Lisdexamfetamine and Methylphenidate on ADHD Neurobiology: A Review |url=https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9588136/ |journal=Neurology and Therapy |volume=11 |issue=4 |pages=1489–1517 |doi=10.1007/s40120-022-00392-2 |issn= |pmc=9588136 |pmid=35951288 |quote=The active form of the drug has a central nervous system stimulating activity by the primary inhibition of DAT, NET, trace amine-associated receptor 1 (TAAR1) and vesicular monoamine transporter 2 (SLC18A2), among other targets, therefore regulating the reuptake and release of catecholamines (primarily NE and DA) on the synaptic cleft.&nbsp;...<br /> LDX can also promote the increase of DA in the synaptic cleft by activating protein TAAR1, which produces the efflux of monoamine NTs, mainly DA, from storage sites on presynaptic neurons. TAAR1 activation leads to intracellular cAMP signalling that results in PKA and PKC phosphorylation and activation. This PKC activation decreases DAT1, NET1 and SERT cell surface expression, intensifying the direct blockage of monoamine transporters by LDX and improving the neurotransmission imbalance in ADHD. |doi-access=free}}</ref><ref>{{Cite journal |vauthors=Garey JD, Lusskin SI, Scialli AR |year=2020 |title=Teratogen update: Amphetamines |url=https://pubmed.ncbi.nlm.nih.gov/32755038 |journal=Birth Defects Research |volume=112 |issue=15 |pages=1171–1182 |doi=10.1002/bdr2.1774 |pmid=32755038 |quote=According to a systematic review of the literature on CNS actions of amphetamine by Faraone (2018), the primary pharmacologic effect of amphetamine is to increase central dopamine and norepinephrine activity. The trace amine-associated receptor 1 (TAAR1) is a G-coupled receptor expressed in the monoaminergic regions of the brain (Lam et al., 2018). When activated by appropriate ligands including methamphetamine, dopaminergic function is modulated (Miner, Elmore, Baumann, Phillips, & Janowsky, 2017).&nbsp;...<br /> It has long been assumed that amphetamines are indirectly acting sympathomimetic amines, with responses being due to the release of norepinephrine from sympathetic neurons (Broadley, 2010). With the discovery of TAAR in blood vessels and evidence that amphetamine binds to these receptors, it has been suggested that the vasoconstrictor effect may be due in part to this additional mechanism (Broadley, Fehler, Ford, & Kidd, 2013).}}</ref><ref name="TAAR1_cAMP2025">{{Cite journal |vauthors=Dalvi S, Bhatt LK |year=2025 |title=Trace amine-associated receptor 1 (TAAR1): an emerging therapeutic target for neurodegenerative, neurodevelopmental, and neurotraumatic disorders |url=https://pubmed.ncbi.nlm.nih.gov/39738834 |journal=Naunyn-Schmiedeberg's Archives of Pharmacology |volume=398 |issue=5 |pages=5057–5075 |doi=10.1007/s00210-024-03757-6 |pmid=39738834 |quote=The mechanism of efflux of monoamines in the synapse is due to the activation of TAAR1 by TAs or drugs belonging to the amphetamine class which increases the level of cAMP (cyclic adenosine monophosphate) followed by an increase in the level of PKA (protein kinase A) and PKC (protein kinase C) phosphorylation. This reverses the monoamine transport by reversing the direction of monoamine transporters.}}</ref>|group="sources"|name="TAAR1 phosphorylation"}} Activation of {{abbr|TAAR1|trace amine-associated receptor 1}} increases {{abbrlink|cAMP|cyclic adenosine monophosphate}} production via [[adenylyl cyclase]] activation, which triggers [[protein kinase A]] (PKA)- and PKC-mediated transporter phosphorylation.<ref name="Miller" /><ref name="2022 T1 LDX" /><ref name="pmid114599292">{{cite journal |vauthors=Borowsky B, Adham N, Jones KA, Raddatz R, Artymyshyn R, Ogozalek KL, Durkin MM, Lakhlani PP, Bonini JA, Pathirana S, Boyle N, Pu X, Kouranova E, Lichtblau H, Ochoa FY, Branchek TA, Gerald C |date=July 2001 |title=Trace amines: identification of a family of mammalian G protein-coupled receptors |journal=Proceedings of the National Academy of Sciences |volume=98 |issue=16 |pages=8966–8971 |bibcode=2001PNAS...98.8966B |doi=10.1073/pnas.151105198 |pmc=55357 |pmid=11459929 |doi-access=free |title-link=doi}}</ref> Monoamine [[autoreceptors]] (e.g., [[D2sh|D<sub>2</sub> short]], [[Alpha-2 adrenergic receptor|presynaptic α<sub>2</sub>]], and [[5-HT1A#Autoreceptors|presynaptic 5-HT<sub>1A</sub>]]) have the opposite effect of TAAR1, and together these receptors provide a regulatory system for monoamines.<ref name="Miller" /><ref name="Miller+Grandy 2016" /><ref name="handbook2022_TAAR1">{{Cite book |title=Handbook of Substance Misuse and Addictions |vauthors=Liu J |publisher=Springer International Publishing |year=2022 |isbn=978-3-030-92391-4 |veditors=Patel VB, Preedy VR |location=Cham |page= |pages=560-565 |chapter=Chapter 28: Trace Amine-Associated Receptor 1 and Its Links to Addictions |doi=10.1007/978-3-030-92392-1 |quote=The study further showed that amphetamine (AMPH) activated TAAR1 by interacting with G13 and GS α-subunits to increase RhoA and PKA activity, respectively (Underhill et al. 2021).&nbsp;...<br />  Using microdialysis showed that TAAR1 knockout mice showed higher AMPH-triggered dopamine, norepinephrine, and serotonin levels in the striatum (Lindemann et al. 2008; Wolinsky et al. 2007). As mentioned above, the psychostimulants amphetamines are TAAR1 agonists. These studies may suggest that amphetamines activate TAAR1 in WT animals to attenuate the behavioral responses to amphetamines.}}</ref> Notably, amphetamine and [[Trace amine|trace amines]] possess high binding affinities for TAAR1, but not for monoamine autoreceptors.<ref name="Miller" /><ref name="Miller+Grandy 2016" /> Although TAAR1 is implicated in amphetamine-induced transporter phosphorylation, the [[Magnitude (mathematics)|magnitude]] of TAAR1-mediated monoamine release in humans remains unclear.<ref name="TAAR1 phosphorylation" group="sources" /><ref name="handbook2022_TAAR1" /> Findings from studies using TAAR1 [[gene knockout]] models suggest that, despite facilitating monoamine release through [[reverse transport]], TAAR1 activation may paradoxically attenuate amphetamine’s psychostimulant effects in part by opening [[G protein-coupled inwardly rectifying potassium channels]], an action that reduces [[neuronal firing]].<ref name="Miller" /><ref name="handbook2022_TAAR1" />
+Amphetamine has been identified as a [[full agonist]] of [[TAAR1|trace amine-associated receptor 1]] (TAAR1), a {{nowrap|[[Gs alpha subunit|G<sub>s</sub>-coupled]]}} and {{nowrap|[[Gq alpha subunit|G<sub>q</sub>-coupled]]}} [[G protein-coupled receptor]] (GPCR) discovered in 2001, which is important for regulation of brain monoamines.<ref name="Miller" /> Several reviews have linked amphetamine’s agonism at TAAR1 to modulation of monoamine transporter function and subsequent neurotransmitter efflux and reuptake inhibition at monoaminergic synapses.{{#tag:ref|<ref name="Miller" /><ref name="handbook2022_DAT" /><ref name="2022 T1 LDX">{{Cite journal |vauthors=Quintero J, Gutiérrez-Casares JR, Álamo C |date=11 August 2022 |title=Molecular Characterisation of the Mechanism of Action of Stimulant Drugs Lisdexamfetamine and Methylphenidate on ADHD Neurobiology: A Review |url=https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9588136/ |journal=Neurology and Therapy |volume=11 |issue=4 |pages=1489–1517 |doi=10.1007/s40120-022-00392-2 |issn= |pmc=9588136 |pmid=35951288 |quote=The active form of the drug has a central nervous system stimulating activity by the primary inhibition of DAT, NET, trace amine-associated receptor 1 (TAAR1) and vesicular monoamine transporter 2 (SLC18A2), among other targets, therefore regulating the reuptake and release of catecholamines (primarily NE and DA) on the synaptic cleft.&nbsp;...<br /> LDX can also promote the increase of DA in the synaptic cleft by activating protein TAAR1, which produces the efflux of monoamine NTs, mainly DA, from storage sites on presynaptic neurons. TAAR1 activation leads to intracellular cAMP signalling that results in PKA and PKC phosphorylation and activation. This PKC activation decreases DAT1, NET1 and SERT cell surface expression, intensifying the direct blockage of monoamine transporters by LDX and improving the neurotransmission imbalance in ADHD. |doi-access=free}}</ref><ref>{{Cite journal |vauthors=Garey JD, Lusskin SI, Scialli AR |year=2020 |title=Teratogen update: Amphetamines |url=https://pubmed.ncbi.nlm.nih.gov/32755038 |journal=Birth Defects Research |volume=112 |issue=15 |pages=1171–1182 |doi=10.1002/bdr2.1774 |pmid=32755038 |quote=According to a systematic review of the literature on CNS actions of amphetamine by Faraone (2018), the primary pharmacologic effect of amphetamine is to increase central dopamine and norepinephrine activity. The trace amine-associated receptor 1 (TAAR1) is a G-coupled receptor expressed in the monoaminergic regions of the brain (Lam et al., 2018). When activated by appropriate ligands including methamphetamine, dopaminergic function is modulated (Miner, Elmore, Baumann, Phillips, & Janowsky, 2017).&nbsp;...<br /> It has long been assumed that amphetamines are indirectly acting sympathomimetic amines, with responses being due to the release of norepinephrine from sympathetic neurons (Broadley, 2010). With the discovery of TAAR in blood vessels and evidence that amphetamine binds to these receptors, it has been suggested that the vasoconstrictor effect may be due in part to this additional mechanism (Broadley, Fehler, Ford, & Kidd, 2013).}}</ref><ref name="TAAR1_cAMP2025">{{Cite journal |vauthors=Dalvi S, Bhatt LK |year=2025 |title=Trace amine-associated receptor 1 (TAAR1): an emerging therapeutic target for neurodegenerative, neurodevelopmental, and neurotraumatic disorders |url=https://pubmed.ncbi.nlm.nih.gov/39738834 |journal=Naunyn-Schmiedeberg's Archives of Pharmacology |volume=398 |issue=5 |pages=5057–5075 |doi=10.1007/s00210-024-03757-6 |pmid=39738834 |quote=The mechanism of efflux of monoamines in the synapse is due to the activation of TAAR1 by TAs or drugs belonging to the amphetamine class which increases the level of cAMP (cyclic adenosine monophosphate) followed by an increase in the level of PKA (protein kinase A) and PKC (protein kinase C) phosphorylation. This reverses the monoamine transport by reversing the direction of monoamine transporters.}}</ref>|group="sources"|name="TAAR1 phosphorylation"}} Activation of {{abbr|TAAR1|trace amine-associated receptor 1}} increases {{abbrlink|cAMP|cyclic adenosine monophosphate}} production via [[adenylyl cyclase]] activation, which triggers [[protein kinase A]] (PKA)- and PKC-mediated transporter phosphorylation.<ref name="Miller" /><ref name="2022 T1 LDX" /><ref name="pmid114599292">{{cite journal |vauthors=Borowsky B, Adham N, Jones KA, Raddatz R, Artymyshyn R, Ogozalek KL, Durkin MM, Lakhlani PP, Bonini JA, Pathirana S, Boyle N, Pu X, Kouranova E, Lichtblau H, Ochoa FY, Branchek TA, Gerald C |date=July 2001 |title=Trace amines: identification of a family of mammalian G protein-coupled receptors |journal=Proceedings of the National Academy of Sciences |volume=98 |issue=16 |pages=8966–8971 |bibcode=2001PNAS...98.8966B |doi=10.1073/pnas.151105198 |pmc=55357 |pmid=11459929 |doi-access=free |title-link=doi}}</ref> Monoamine [[autoreceptors]] (e.g., [[D2sh|D<sub>2</sub> short]], [[Alpha-2 adrenergic receptor|presynaptic α<sub>2</sub>]], and [[5-HT1A#Autoreceptors|presynaptic 5-HT<sub>1A</sub>]]) have the opposite effect of TAAR1, and together these receptors provide a regulatory system for monoamines.<ref name="Miller" /><ref name="Miller+Grandy 2016" /><ref name="handbook2022_TAAR1">{{Cite book |title=Handbook of Substance Misuse and Addictions |vauthors=Liu J |publisher=Springer International Publishing |year=2022 |isbn=978-3-030-92391-4 |veditors=Patel VB, Preedy VR |location=Cham |pages=560-565 |chapter=Chapter 28: Trace Amine-Associated Receptor 1 and Its Links to Addictions |doi=10.1007/978-3-030-92392-1_32 |quote=The study further showed that amphetamine (AMPH) activated TAAR1 by interacting with G13 and GS α-subunits to increase RhoA and PKA activity, respectively (Underhill et al. 2021).&nbsp;...<br />  Using microdialysis showed that TAAR1 knockout mice showed higher AMPH-triggered dopamine, norepinephrine, and serotonin levels in the striatum (Lindemann et al. 2008; Wolinsky et al. 2007). As mentioned above, the psychostimulants amphetamines are TAAR1 agonists. These studies may suggest that amphetamines activate TAAR1 in WT animals to attenuate the behavioral responses to amphetamines.}}</ref> Notably, amphetamine and [[Trace amine|trace amines]] possess high binding affinities for TAAR1, but not for monoamine autoreceptors.<ref name="Miller" /><ref name="Miller+Grandy 2016" /> Although TAAR1 is implicated in amphetamine-induced transporter phosphorylation, the [[Magnitude (mathematics)|magnitude]] of TAAR1-mediated monoamine release in humans remains unclear.<ref name="TAAR1 phosphorylation" group="sources" /><ref name="handbook2022_TAAR1" /> Findings from studies using TAAR1 [[gene knockout]] models suggest that, despite facilitating monoamine release through [[reverse transport]], TAAR1 activation may paradoxically attenuate amphetamine’s psychostimulant effects in part by opening [[G protein-coupled inwardly rectifying potassium channels]], an action that reduces [[neuronal firing]].<ref name="Miller" /><ref name="handbook2022_TAAR1" />
 Amphetamine is also a substrate for the vesicular monoamine transporters [[VMAT1]] and [[Vesicular monoamine transporter 2|VMAT2]].<ref name="Amphetamine VMAT2 pH gradient">{{cite journal | vauthors = Sulzer D, Cragg SJ, Rice ME | title = Striatal dopamine neurotransmission: regulation of release and uptake | journal =Basal Ganglia| volume = 6 | issue = 3 | pages = 123–148 | date = August 2016 | pmid = 27141430 | pmc = 4850498 | doi = 10.1016/j.baga.2016.02.001 | quote = Despite the challenges in determining synaptic vesicle pH, the proton gradient across the vesicle membrane is of fundamental importance for its function. Exposure of isolated catecholamine vesicles to protonophores collapses the pH gradient and rapidly redistributes transmitter from inside to outside the vesicle.&nbsp;... Amphetamine and its derivatives like methamphetamine are weak base compounds that are the only widely used class of drugs known to elicit transmitter release by a non-exocytic mechanism. As substrates for both DAT and VMAT, amphetamines can be taken up to the cytosol and then sequestered in vesicles, where they act to collapse the vesicular pH gradient.}}</ref><ref name="VMAT2ADHD">{{Cite journal |vauthors=Warlick Iv H, Tocci D, Prashar S, Boldt E, Khalil A, Arora S, Matthews T, Wahid T, Fernandez R, Ram D, Leon L, Arain A, Rey J, Davis K |year=2024 |title=Role of vesicular monoamine transporter-2 for treating attention deficit hyperactivity disorder: a review |url=https://pubmed.ncbi.nlm.nih.gov/39302436/ |journal=Psychopharmacology |volume=241 |issue=11 |pages=2191–2203 |doi=10.1007/s00213-024-06686-7 |pmid=39302436 |quote=Current psychopharmacology research shows that at high doses (non-therapeutic ranges), VMAT-2 can be “inhibited” by amphetamines, causing VMAT-2 vesicles to release the classical monoamines DA and NE into the axoplasm; however, this model is no longer broadly accepted. For instance, Stahl (2014) reported that VMAT-2 is not affected by amphetamines at therapeutic doses but is affected at higher doses.}}</ref> Under normal conditions, VMAT2 transports cytosolic monoamines into synaptic vesicles for storage and later [[Exocytosis|exocytotic]] release. When amphetamine accumulates in the presynaptic terminal, it collapses the vesicular pH gradient and releases vesicular monoamines into the neuronal cytosol.<ref name="Amphetamine VMAT2 pH gradient" /><ref name="VMAT2ADHD" /> These displaced monoamines expand the cytosolic pool available for reverse transport, thereby increasing the capacity for monoamine efflux beyond that achieved by amphetamine-mediated transporter phosphorylation alone.<ref name="2020_Reith" /><ref name="VMAT2ADHD" /> Although VMAT2 is recognized as a major target in amphetamine-induced monoamine release at higher doses, some reviews have challenged its relevance at therapeutic doses.<ref name="Stahl2021" /><ref name="2020_Reith" /><ref name="VMAT2ADHD" />
-In addition to [[Membrane transport protein|membrane]] and [[Vesicular monoamine transporter|vesicular monoamine transporters]], amphetamine also inhibits [[SLC1A1]], [[SLC22A3]], and [[SLC22A5]].{{#tag:ref|<ref name="E Weihe" /><ref name="EAAT3">{{cite journal |vauthors=Underhill SM, Wheeler DS, Li M, Watts SD, Ingram SL, Amara SG | title = Amphetamine modulates excitatory neurotransmission through endocytosis of the glutamate transporter EAAT3 in dopamine neurons | journal =Neuron| volume = 83 | issue = 2 | pages = 404–416 | date = July 2014 | pmid = 25033183 | pmc = 4159050 | doi = 10.1016/j.neuron.2014.05.043 | quote = AMPH also increases intracellular calcium (Gnegy et al., 2004) that is associated with calmodulin/CamKII activation (Wei et al., 2007) and modulation and trafficking of the DAT (Fog et al., 2006; Sakrikar et al., 2012).&nbsp;... For example, AMPH increases extracellular glutamate in various brain regions including the striatum, VTA and NAc (Del Arco et al., 1999; Kim et al., 1981; Mora and Porras, 1993; Xue et al., 1996), but it has not been established whether this change can be explained by increased synaptic release or by reduced clearance of glutamate.&nbsp;... DHK-sensitive, EAAT2 uptake was not altered by AMPH (Figure 1A). The remaining glutamate transport in these midbrain cultures is likely mediated by EAAT3 and this component was significantly decreased by AMPH}}</ref><ref name="IUPHAR VMATs">{{cite web|title=SLC18 family of vesicular amine transporters|url=http://www.guidetopharmacology.org/GRAC/FamilyDisplayForward?familyId=193|website=IUPHAR database|publisher=International Union of Basic and Clinical Pharmacology|access-date=13 November 2015}}</ref><ref name="SLC1A1">{{cite web | title=SLC1A1 solute carrier family 1 (neuronal/epithelial high affinity glutamate transporter, system Xag), member 1 [ Homo sapiens (human) ] | url=https://www.ncbi.nlm.nih.gov/gene/6505 | website=NCBI Gene | publisher=United States National Library of Medicine&nbsp;– National Center for Biotechnology Information | access-date=11 November 2014 | quote = Amphetamine modulates excitatory neurotransmission through endocytosis of the glutamate transporter EAAT3 in dopamine neurons.&nbsp;... internalization of EAAT3 triggered by amphetamine increases glutamatergic signaling and thus contributes to the effects of amphetamine on neurotransmission.}}</ref><ref name="SLC22A3">{{cite journal |vauthors=Zhu HJ, Appel DI, Gründemann D, Markowitz JS | title = Interaction of organic cation transporter 3 (SLC22A3) and amphetamine | journal =Journal of Neurochemistry| volume = 114 | issue = 1 | pages = 142–149 |date=July 2010 | pmid = 20402963 | pmc = 3775896 | doi = 10.1111/j.1471-4159.2010.06738.x}}</ref><ref name="SLC22A5">{{cite journal |vauthors=Rytting E, Audus KL | s2cid = 31465243 | title = Novel organic cation transporter 2-mediated carnitine uptake in placental choriocarcinoma (BeWo) cells | journal =Journal of Pharmacology and Experimental Therapeutics| volume = 312 | issue = 1 | pages = 192–198 |date=January 2005 | pmid = 15316089 | doi = 10.1124/jpet.104.072363}}</ref><ref name="pmid13677912">{{cite journal |vauthors=Inazu M, Takeda H, Matsumiya T | title = [The role of glial monoamine transporters in the central nervous system] | language = ja | journal =Nihon Shinkei Seishin Yakurigaku Zasshi | volume = 23 | issue = 4 | pages = 171–178 |date=August 2003 | pmid = 13677912}}</ref>|group="sources"|name="Reuptake inhibition"}} SLC1A1 is [[excitatory amino acid transporter 3]] (EAAT3), a glutamate transporter located in neurons, SLC22A3 is an extraneuronal monoamine transporter that is present in [[astrocyte]]s, and SLC22A5 is a high-affinity [[carnitine]] transporter.<ref name="Reuptake inhibition" group="sources" /> Amphetamine is known to strongly induce [[cocaine- and amphetamine-regulated transcript]] (CART) [[gene expression]],<ref name="Drugbank-amph" /><ref name="CART NAcc">{{cite journal |vauthors=Vicentic A, Jones DC | title = The CART (cocaine- and amphetamine-regulated transcript) system in appetite and drug addiction | journal =Journal of Pharmacology and Experimental Therapeutics| volume = 320 | issue = 2 | pages = 499–506 |date=February 2007 | pmid = 16840648 | doi = 10.1124/jpet.105.091512 | s2cid = 14212763 | quote = The physiological importance of CART was further substantiated in numerous human studies demonstrating a role of CART in both feeding and psychostimulant addiction.&nbsp;... Colocalization studies also support a role for CART in the actions of psychostimulants.&nbsp;... CART and DA receptor transcripts colocalize (Beaudry et al., 2004). Second, dopaminergic nerve terminals in the NAc synapse on CART-containing neurons (Koylu et al., 1999), hence providing the proximity required for neurotransmitter signaling. These studies suggest that DA plays a role in regulating CART gene expression possibly via the activation of CREB.}}</ref> a [[neuropeptide]] involved in feeding behavior, stress, and reward, which induces observable increases in neuronal development and survival ''[[in vitro]]''.<ref name="Drugbank-amph" /><ref name="CART functions">{{cite journal |vauthors=Zhang M, Han L, Xu Y | title = Roles of cocaine- and amphetamine-regulated transcript in the central nervous system | journal =Clinical and Experimental Pharmacology and Physiology| volume = 39 | issue = 6 | pages = 586–592 |date=June 2012 | pmid = 22077697 | doi = 10.1111/j.1440-1681.2011.05642.x | s2cid = 25134612 | quote = Recently, it was demonstrated that CART, as a neurotrophic peptide, had a cerebroprotective against focal ischaemic stroke and inhibited the neurotoxicity of β-amyloid protein, which focused attention on the role of CART in the central nervous system (CNS) and neurological diseases.&nbsp;... The literature indicates that there are many factors, such as regulation of the immunological system and protection against energy failure, that may be involved in the cerebroprotection afforded by CART}}</ref><ref name="CART">{{cite journal |vauthors=Rogge G, Jones D, Hubert GW, Lin Y, Kuhar MJ |title=CART peptides: regulators of body weight, reward and other functions |journal=Nature Reviews Neuroscience |volume=9 |issue=10 |pages=747–758 |date=October 2008 |pmid=18802445 |pmc=4418456 |doi=10.1038/nrn2493 |quote=Several studies on CART (cocaine- and amphetamine-regulated transcript)-peptide-induced cell signalling have demonstrated that CART peptides activate at least three signalling mechanisms. First, CART 55–102 inhibited voltage-gated L-type Ca2+ channels&nbsp;...}}</ref> The CART receptor has yet to be identified, but there is significant evidence that CART binds to a unique {{nowrap|[[Gi alpha subunit|G<sub>i</sub>/G<sub>o</sub>-coupled]]}} {{abbr|GPCR|G protein-coupled receptor}}.<ref name="CART" /><ref name="pmid21855138">{{cite journal |vauthors=Lin Y, Hall RA, Kuhar MJ |title=CART peptide stimulation of G protein-mediated signaling in differentiated PC12 cells: identification of PACAP 6–38 as a CART receptor antagonist |journal=Neuropeptides |volume=45 |issue=5 |pages=351–358 |date=October 2011 |pmid=21855138 |pmc=3170513 |doi=10.1016/j.npep.2011.07.006}}</ref> Amphetamine also inhibits [[monoamine oxidase]]s at very high doses, resulting in less monoamine and trace amine metabolism and consequently higher concentrations of synaptic monoamines.<ref name="PubChem Header">{{cite encyclopedia |title=Amphetamine |section-url=https://pubchem.ncbi.nlm.nih.gov/summary/summary.cgi?cid=3007 |publisher=United States National Library of Medicine&nbsp;– National Center for Biotechnology Information. PubChem Compound Database |access-date=17 April 2015 |date=11 April 2015 |section=Compound Summary}}</ref><ref name="BRENDA MAO Homo sapiens">{{cite encyclopedia |title=Monoamine oxidase (Homo sapiens)|url=http://www.brenda-enzymes.info/enzyme.php?ecno=1.4.3.4&Suchword=&organism%5B%5D=Homo+sapiens&show_tm=0 |publisher=Technische Universität Braunschweig. BRENDA |access-date=4 May 2014 |date=1 January 2014}}</ref> In humans, the only post-synaptic receptor at which amphetamine is known to bind is the [[5-HT1A receptor|{{nowrap|5-HT1A}} receptor]], where it acts as an agonist with low [[micromolar]] affinity.<ref name="5HT1A secondary">{{cite encyclopedia |title=Amphetamine |publisher=University of Alberta: T3DB |url=http://www.t3db.ca/toxins/T3D2706 |access-date=24 February 2015 |section=Targets}}</ref><ref name="5HT1A Primary">{{cite journal |vauthors=Toll L, Berzetei-Gurske IP, Polgar WE, Brandt SR, Adapa ID, Rodriguez L, Schwartz RW, Haggart D, O'Brien A, White A, Kennedy JM, Craymer K, Farrington L, Auh JS |date=March 1998 |title=Standard binding and functional assays related to medications development division testing for potential cocaine and opiate narcotic treatment medications |journal=NIDA Research Monograph |volume=178 |pages=440–466 |pmid=9686407}}</ref>
+In addition to [[Membrane transport protein|membrane]] and [[Vesicular monoamine transporter|vesicular monoamine transporters]], amphetamine also inhibits [[SLC1A1]], [[SLC22A3]], and [[SLC22A5]].{{#tag:ref|<ref name="E Weihe" /><ref name="EAAT3">{{cite journal |vauthors=Underhill SM, Wheeler DS, Li M, Watts SD, Ingram SL, Amara SG | title = Amphetamine modulates excitatory neurotransmission through endocytosis of the glutamate transporter EAAT3 in dopamine neurons | journal =Neuron| volume = 83 | issue = 2 | pages = 404–416 | date = July 2014 | pmid = 25033183 | pmc = 4159050 | doi = 10.1016/j.neuron.2014.05.043 | quote = AMPH also increases intracellular calcium (Gnegy et al., 2004) that is associated with calmodulin/CamKII activation (Wei et al., 2007) and modulation and trafficking of the DAT (Fog et al., 2006; Sakrikar et al., 2012).&nbsp;... For example, AMPH increases extracellular glutamate in various brain regions including the striatum, VTA and NAc (Del Arco et al., 1999; Kim et al., 1981; Mora and Porras, 1993; Xue et al., 1996), but it has not been established whether this change can be explained by increased synaptic release or by reduced clearance of glutamate.&nbsp;... DHK-sensitive, EAAT2 uptake was not altered by AMPH (Figure 1A). The remaining glutamate transport in these midbrain cultures is likely mediated by EAAT3 and this component was significantly decreased by AMPH}}</ref><ref name="IUPHAR VMATs">{{cite web|title=SLC18 family of vesicular amine transporters|url=http://www.guidetopharmacology.org/GRAC/FamilyDisplayForward?familyId=193|website=IUPHAR database|publisher=International Union of Basic and Clinical Pharmacology|access-date=13 November 2015}}</ref><ref name="SLC1A1">{{cite web | title=SLC1A1 solute carrier family 1 (neuronal/epithelial high affinity glutamate transporter, system Xag), member 1 [ Homo sapiens (human) ] | url=https://www.ncbi.nlm.nih.gov/gene/6505 | website=NCBI Gene | publisher=United States National Library of Medicine&nbsp;– National Center for Biotechnology Information | access-date=11 November 2014 | quote = Amphetamine modulates excitatory neurotransmission through endocytosis of the glutamate transporter EAAT3 in dopamine neurons.&nbsp;... internalization of EAAT3 triggered by amphetamine increases glutamatergic signaling and thus contributes to the effects of amphetamine on neurotransmission.}}</ref><ref name="SLC22A3">{{cite journal |vauthors=Zhu HJ, Appel DI, Gründemann D, Markowitz JS | title = Interaction of organic cation transporter 3 (SLC22A3) and amphetamine | journal =Journal of Neurochemistry| volume = 114 | issue = 1 | pages = 142–149 |date=July 2010 | pmid = 20402963 | pmc = 3775896 | doi = 10.1111/j.1471-4159.2010.06738.x}}</ref><ref name="SLC22A5">{{cite journal |vauthors=Rytting E, Audus KL | s2cid = 31465243 | title = Novel organic cation transporter 2-mediated carnitine uptake in placental choriocarcinoma (BeWo) cells | journal =Journal of Pharmacology and Experimental Therapeutics| volume = 312 | issue = 1 | pages = 192–198 |date=January 2005 | pmid = 15316089 | doi = 10.1124/jpet.104.072363}}</ref><ref name="pmid13677912">{{cite journal |vauthors=Inazu M, Takeda H, Matsumiya T | title = [The role of glial monoamine transporters in the central nervous system] | language = ja | journal =Nihon Shinkei Seishin Yakurigaku Zasshi | volume = 23 | issue = 4 | pages = 171–178 |date=August 2003 | pmid = 13677912}}</ref>|group="sources"|name="Reuptake inhibition"}} SLC1A1 is [[excitatory amino acid transporter 3]] (EAAT3), a glutamate transporter located in neurons, SLC22A3 is an extraneuronal monoamine transporter that is present in [[astrocyte]]s, and SLC22A5 is a high-affinity [[carnitine]] transporter.<ref name="Reuptake inhibition" group="sources" /> Amphetamine is known to strongly induce [[cocaine- and amphetamine-regulated transcript]] (CART) [[gene expression]],<ref name="Drugbank-amph" /><ref name="CART NAcc">{{cite journal |vauthors=Vicentic A, Jones DC | title = The CART (cocaine- and amphetamine-regulated transcript) system in appetite and drug addiction | journal =Journal of Pharmacology and Experimental Therapeutics| volume = 320 | issue = 2 | pages = 499–506 |date=February 2007 | pmid = 16840648 | doi = 10.1124/jpet.105.091512 | s2cid = 14212763 | quote = The physiological importance of CART was further substantiated in numerous human studies demonstrating a role of CART in both feeding and psychostimulant addiction.&nbsp;... Colocalization studies also support a role for CART in the actions of psychostimulants.&nbsp;... CART and DA receptor transcripts colocalize (Beaudry et al., 2004). Second, dopaminergic nerve terminals in the NAc synapse on CART-containing neurons (Koylu et al., 1999), hence providing the proximity required for neurotransmitter signaling. These studies suggest that DA plays a role in regulating CART gene expression possibly via the activation of CREB.}}</ref> a [[neuropeptide]] involved in feeding behavior, stress, and reward, which induces observable increases in neuronal development and survival ''[[in vitro]]''.<ref name="Drugbank-amph" /><ref name="CART functions">{{cite journal |vauthors=Zhang M, Han L, Xu Y | title = Roles of cocaine- and amphetamine-regulated transcript in the central nervous system | journal =Clinical and Experimental Pharmacology and Physiology| volume = 39 | issue = 6 | pages = 586–592 |date=June 2012 | pmid = 22077697 | doi = 10.1111/j.1440-1681.2011.05642.x | s2cid = 25134612 | quote = Recently, it was demonstrated that CART, as a neurotrophic peptide, had a cerebroprotective against focal ischaemic stroke and inhibited the neurotoxicity of β-amyloid protein, which focused attention on the role of CART in the central nervous system (CNS) and neurological diseases.&nbsp;... The literature indicates that there are many factors, such as regulation of the immunological system and protection against energy failure, that may be involved in the cerebroprotection afforded by CART}}</ref><ref name="CART">{{cite journal |vauthors=Rogge G, Jones D, Hubert GW, Lin Y, Kuhar MJ |title=CART peptides: regulators of body weight, reward and other functions |journal=Nature Reviews Neuroscience |volume=9 |issue=10 |pages=747–758 |date=October 2008 |pmid=18802445 |pmc=4418456 |doi=10.1038/nrn2493 |quote=Several studies on CART (cocaine- and amphetamine-regulated transcript)-peptide-induced cell signalling have demonstrated that CART peptides activate at least three signalling mechanisms. First, CART 55–102 inhibited voltage-gated L-type Ca2+ channels&nbsp;...}}</ref> The CART receptor has yet to be identified, but there is significant evidence that CART binds to a unique {{nowrap|[[Gi alpha subunit|G<sub>i</sub>/G<sub>o</sub>-coupled]]}} {{abbr|GPCR|G protein-coupled receptor}}.<ref name="CART" /><ref name="pmid21855138">{{cite journal |vauthors=Lin Y, Hall RA, Kuhar MJ |title=CART peptide stimulation of G protein-mediated signaling in differentiated PC12 cells: identification of PACAP 6–38 as a CART receptor antagonist |journal=Neuropeptides |volume=45 |issue=5 |pages=351–358 |date=October 2011 |pmid=21855138 |pmc=3170513 |doi=10.1016/j.npep.2011.07.006}}</ref> Amphetamine also inhibits [[monoamine oxidase]]s at very high doses, resulting in less monoamine and trace amine metabolism and consequently higher concentrations of synaptic monoamines.<ref name="PubChem Header">{{cite encyclopedia |title=Amphetamine |section-url=https://pubchem.ncbi.nlm.nih.gov/summary/summary.cgi?cid=3007 |publisher=United States National Library of Medicine&nbsp;– National Center for Biotechnology Information. PubChem Compound Database |access-date=17 April 2015 |date=11 April 2015 |section=Compound Summary}}</ref><ref name="BRENDA MAO Homo sapiens">{{cite encyclopedia |title=Monoamine oxidase (Homo sapiens)|url=http://www.brenda-enzymes.info/enzyme.php?ecno=1.4.3.4&Suchword=&organism%5B%5D=Homo+sapiens&show_tm=0 |publisher=Technische Universität Braunschweig. BRENDA |access-date=4 May 2014 |date=1 January 2014}}</ref> In humans, the only post-synaptic receptor at which amphetamine is known to bind is the [[5-HT1A receptor|{{nowrap|5-HT1A}} receptor]], where it acts as an agonist with low [[micromolar]] affinity.<ref name="5HT1A secondary">{{cite encyclopedia |title=Amphetamine |publisher=University of Alberta T3DB |url=http://www.t3db.ca/toxins/T3D2706 |access-date=24 February 2015 |section=Targets}}</ref><ref name="5HT1A Primary">{{cite journal |vauthors=Toll L, Berzetei-Gurske IP, Polgar WE, Brandt SR, Adapa ID, Rodriguez L, Schwartz RW, Haggart D, O'Brien A, White A, Kennedy JM, Craymer K, Farrington L, Auh JS |date=March 1998 |title=Standard binding and functional assays related to medications development division testing for potential cocaine and opiate narcotic treatment medications |journal=NIDA Research Monograph |volume=178 |pages=440–466 |pmid=9686407}}</ref>
 The full profile of amphetamine's short-term drug effects in humans is mostly derived through increased cellular communication or [[neurotransmission]] of [[dopamine]],<ref name="Miller">{{cite journal | vauthors = Miller GM |title=The emerging role of trace amine-associated receptor 1 in the functional regulation of monoamine transporters and dopaminergic activity | journal =Journal of Neurochemistry |volume=116 |issue=2 |pages=164–176 |date=January 2011 |pmid=21073468 |pmc=3005101 |doi=10.1111/j.1471-4159.2010.07109.x}}</ref> [[serotonin]],<ref name="Miller" /> [[norepinephrine]],<ref name="Miller" /> [[epinephrine]],<ref name="E Weihe">{{cite journal |vauthors=Eiden LE, Weihe E |title=VMAT2: a dynamic regulator of brain monoaminergic neuronal function interacting with drugs of abuse | journal =Annals of the New York Academy of Sciences| volume = 1216 |issue = 1 | pages = 86–98 | date=January 2011 | pmid = 21272013 | pmc=4183197 | doi = 10.1111/j.1749-6632.2010.05906.x | quote = VMAT2 is the CNS vesicular transporter for not only the biogenic amines DA, NE, EPI, 5-HT, and HIS, but likely also for the trace amines TYR, PEA, and thyronamine (THYR)&nbsp;... [Trace aminergic] neurons in mammalian CNS would be identifiable as neurons expressing VMAT2 for storage, and the biosynthetic enzyme aromatic amino acid decarboxylase (AADC).&nbsp;... AMPH release of DA from synapses requires both an action at VMAT2 to release DA to the cytoplasm and a concerted release of DA from the cytoplasm via "reverse transport" through DAT.| bibcode = <!-- No --> }}</ref> [[histamine]],<ref name="E Weihe" /> [[cocaine and amphetamine regulated transcript|CART peptides]],<ref name="Drugbank-amph" /><ref name="CART NAcc" /> [[endogenous opioid]]s,<ref name="Amphetamine-induced endogenous opioid release review">{{cite journal | vauthors = Finnema SJ, Scheinin M, Shahid M, Lehto J, Borroni E, Bang-Andersen B, Sallinen J, Wong E, Farde L, Halldin C, Grimwood S | title = Application of cross-species PET imaging to assess neurotransmitter release in brain | journal =Psychopharmacology| volume = 232 | issue = 21–22 | pages = 4129–4157 | date = November 2015 | pmid = 25921033 | pmc = 4600473 | doi = 10.1007/s00213-015-3938-6 | quote = More recently, Colasanti and colleagues reported that a pharmacologically induced elevation in endogenous opioid release reduced [<sup>11</sup>C]carfentanil binding in several regions of the human brain, including the basal ganglia, frontal cortex, and thalamus (Colasanti et al. 2012). Oral administration of d-amphetamine, 0.5&nbsp;mg/kg, 3&nbsp;h before [<sup>11</sup>C]carfentanil injection, reduced BPND values by 2–10%. The results were confirmed in another group of subjects (Mick et al. 2014). However, Guterstam and colleagues observed no change in [<sup>11</sup>C]carfentanil binding when d-amphetamine, 0.3&nbsp;mg/kg, was administered intravenously directly before injection of [<sup>11</sup>C]carfentanil (Guterstam et al. 2013). It has been hypothesized that this discrepancy may be related to delayed increases in extracellular opioid peptide concentrations following amphetamine-evoked monoamine release (Colasanti et al. 2012; Mick et al. 2014).}}</ref><ref name="Opioids">{{cite journal | vauthors = Loseth GE, Ellingsen DM, Leknes S | title = State-dependent μ-opioid modulation of social motivation | journal =Frontiers in Behavioral Neuroscience| volume = 8 | pages = 430 | date = December 2014 | pmid = 25565999 | pmc = 4264475 | doi = 10.3389/fnbeh.2014.00430 | quote = Similar MOR activation patterns were reported during positive mood induced by an amusing video clip (Koepp et al., 2009) and following amphetamine administration in humans (Colasanti et al., 2012). | doi-access = free | title-link = doi }}</ref><ref name="Opioids cited primary source">{{cite journal | vauthors = Colasanti A, Searle GE, Long CJ, Hill SP, Reiley RR, Quelch D, Erritzoe D, Tziortzi AC, Reed LJ, Lingford-Hughes AR, Waldman AD, Schruers KR, Matthews PM, Gunn RN, Nutt DJ, Rabiner EA | title = Endogenous opioid release in the human brain reward system induced by acute amphetamine administration | journal =Biological Psychiatry| volume = 72 | issue = 5 | pages = 371–377 | date = September 2012 | pmid = 22386378 | doi = 10.1016/j.biopsych.2012.01.027| s2cid = 18555036 }}</ref> [[adrenocorticotropic hormone]],<ref name="Human amph effects" /><ref name="Primary: Human HPA axis" /> [[corticosteroid]]s,<ref name="Human amph effects" /><ref name="Primary: Human HPA axis" /> and [[glutamate]],<ref name="EAAT3" /><ref name="SLC1A1" /> which it affects through interactions with {{abbr|CART|cocaine- and amphetamine-regulated transcript}}, {{nowrap|{{abbr|5-HT1A|serotonin receptor 1A}}}}, {{abbr|EAAT3|excitatory amino acid transporter 3}}, {{abbr|TAAR1|trace amine-associated receptor 1}}, {{abbr|VMAT1|vesicular monoamine transporter 1}}, {{abbr|VMAT2|vesicular monoamine transporter 2}}, and possibly other [[biological target]]s.{{#tag:ref|<ref name="Miller" /><ref name="E Weihe" /><ref name="IUPHAR VMATs" /><ref name="SLC1A1" /><ref name="CART NAcc" /><ref name="5HT1A secondary" />|group="sources"}} Amphetamine also activates seven human [[carbonic anhydrase]] enzymes, several of which are expressed in the human brain.<ref name="Amphetamine-induced activation of 7 hCA isoforms" />
@@ Line 317: / Line 311: @@
 ====Dopamine====
-In certain brain regions, amphetamine increases the concentration of dopamine in the [[synaptic cleft]] by modulating {{abbr|DAT|dopamine transporter}} through several overlapping processes.<ref name="2020_Reith" /><ref name="handbook2022_DAT">{{Cite book |title=Handbook of Substance Misuse and Addictions |vauthors=Tendilla-Beltran H, Arroyo-García LE, Flores G |publisher=Springer International Publishing |year=2022 |isbn=978-3-030-92391-4 |veditors=Patel VB, Preedy VR |location=Cham |pages=2176-2177 |chapter=Chapter 102: Amphetamine and the Biology of Neuronal Morphology |doi=10.1007/978-3-030-92392-1 |quote=At low concentrations, amphetamines (extracellular) and dopamine (intracellular) are interchanged as described by the exchange diffusion model&nbsp;... Amphetamines can also increase dopaminergic transmission by channel-like transport which involves second-messenger signaling. Amphetamines increase PKC activity, which increase DAT N-terminus domain phosphorylation, and consequently DAT activity, which, because of the amphetamines, will release dopamine from the presynaptic terminal.&nbsp; PKC and CaMKIIα-mediated reverse transport have also been demonstrated in NET&nbsp;...<br /> Also, amphetamines can indirectly enhance monoaminergic neurotransmission through the stimulation of trace amine-associated receptor 1 (TAAR1) (Underhill et al. 2021). TAAR1 is an intracellular G protein-coupled receptor (GPCR), which has activity that promotes the endocytosis of both DAT and the excitatory amino acid transporter 3 (EAAT3). DAT endocytosis, together with the aforementioned mechanisms, contributes to the enhancement of the dopaminergic neurotransmission.&nbsp;... <br /> It is important to note that amphetamines also stimulate protein kinase A (PKA) activity, which in turn inhibits RhoA activity and consequently reduces DAT internalization.}}</ref><ref name="2022 T1 LDX" /> Amphetamine can enter the [[presynaptic neuron]] either through {{abbr|DAT|dopamine transporter}} or by diffusing across the neuronal membrane directly.<ref name="Miller" /><ref name="handbook2022_DAT" /> As a consequence of DAT uptake, amphetamine produces competitive reuptake inhibition at the transporter.<ref name="Miller" /><ref name="Amph Uses" /> Upon entering the presynaptic neuron, amphetamine provokes the release of [[Ca²⁺]] from [[endoplasmic reticulum]] stores, an effect that raises intracellular calcium to levels sufficient for downstream kinase-dependent signalling.<ref name="Kinase-dependent transporter regulation review" /><ref name="2020_Reith" /> Subsequently, amphetamine initiates kinase-dependent signaling cascades that activate both [[protein kinase A]] (PKA) and [[protein kinase C]] (PKC).<ref name="handbook2022_DAT" /><ref name="2022 T1 LDX" /> Phosphorylation of DAT by either kinase induces transporter [[Endocytosis|internalization]] ({{nowrap|non-competitive}} reuptake inhibition), but {{nowrap|PKC-mediated}} phosphorylation alone induces the [[Reverse transport|reversal of dopamine transport]] through DAT (i.e., dopamine [[wiktionary:efflux|efflux]]).<ref name="handbook2022_DAT" /><ref name="Kinase-dependent transporter regulation review" />
+In certain brain regions, amphetamine increases the concentration of dopamine in the [[synaptic cleft]] by modulating {{abbr|DAT|dopamine transporter}} through several overlapping processes.<ref name="2020_Reith" /><ref name="handbook2022_DAT">{{Cite book |title=Handbook of Substance Misuse and Addictions |vauthors=Tendilla-Beltran H, Arroyo-García LE, Flores G |publisher=Springer International Publishing |year=2022 |isbn=978-3-030-92391-4 |veditors=Patel VB, Preedy VR |location=Cham |pages=2176-2177 |chapter=Chapter 102: Amphetamine and the Biology of Neuronal Morphology |doi=10.1007/978-3-030-92392-1_115 |quote=At low concentrations, amphetamines (extracellular) and dopamine (intracellular) are interchanged as described by the exchange diffusion model&nbsp;... Amphetamines can also increase dopaminergic transmission by channel-like transport which involves second-messenger signaling. Amphetamines increase PKC activity, which increase DAT N-terminus domain phosphorylation, and consequently DAT activity, which, because of the amphetamines, will release dopamine from the presynaptic terminal.&nbsp; PKC and CaMKIIα-mediated reverse transport have also been demonstrated in NET&nbsp;...<br /> Also, amphetamines can indirectly enhance monoaminergic neurotransmission through the stimulation of trace amine-associated receptor 1 (TAAR1) (Underhill et al. 2021). TAAR1 is an intracellular G protein-coupled receptor (GPCR), which has activity that promotes the endocytosis of both DAT and the excitatory amino acid transporter 3 (EAAT3). DAT endocytosis, together with the aforementioned mechanisms, contributes to the enhancement of the dopaminergic neurotransmission.&nbsp;... <br /> It is important to note that amphetamines also stimulate protein kinase A (PKA) activity, which in turn inhibits RhoA activity and consequently reduces DAT internalization.}}</ref><ref name="2022 T1 LDX" /> Amphetamine can enter the [[presynaptic neuron]] either through {{abbr|DAT|dopamine transporter}} or by diffusing across the neuronal membrane directly.<ref name="Miller" /><ref name="handbook2022_DAT" /> As a consequence of DAT uptake, amphetamine produces competitive reuptake inhibition at the transporter.<ref name="Miller" /><ref name="Amph Uses" /> Upon entering the presynaptic neuron, amphetamine provokes the release of [[Ca²⁺]] from [[endoplasmic reticulum]] stores, an effect that raises intracellular calcium to levels sufficient for downstream kinase-dependent signalling.<ref name="Kinase-dependent transporter regulation review" /><ref name="2020_Reith" /> Subsequently, amphetamine initiates kinase-dependent signaling cascades that activate both [[protein kinase A]] (PKA) and [[protein kinase C]] (PKC).<ref name="handbook2022_DAT" /><ref name="2022 T1 LDX" /> Phosphorylation of DAT by either kinase induces transporter [[Endocytosis|internalization]] ({{nowrap|non-competitive}} reuptake inhibition), but {{nowrap|PKC-mediated}} phosphorylation alone induces the [[Reverse transport|reversal of dopamine transport]] through DAT (i.e., dopamine [[wiktionary:efflux|efflux]]).<ref name="handbook2022_DAT" /><ref name="Kinase-dependent transporter regulation review" />
 {{abbr|TAAR1|trace amine associated receptor 1}} is a [[biomolecular target]] of amphetamine that can trigger the activation of PKA- and PKC-dependent pathways.<ref name="Miller" /><ref name="handbook2022_DAT" /><ref name="2022 T1 LDX" /> TAAR1 agonism also activates [[Transforming protein RhoA|Ras homolog A]] (RhoA) and its downstream effector, [[Rho-associated coiled-coil kinase]] (ROCK), which results in transient internalization of DAT and [[Excitatory amino acid transporter 3|EAAT3]];{{#tag:ref|Mesolimbic dopamine neurons co-express the glutamate transporter EAAT3 alongside DAT, permitting amphetamine-induced EAAT3 internalization to influence glutamatergic signaling in the [[mesolimbic pathway]].<ref name="EAAT3" /><ref name="handbook2022_DAT" />|name="mesolimbic EAAT3"|group="note"}}<ref name="Amphetamine signaling through ROCKs" /><ref name="handbook2022_DAT" /> as intracellular {{abbrlink|cAMP|cyclic adenosine monophosphate}} accumulates, PKA is activated and inhibits RhoA activity, thereby terminating ROCK-mediated transporter internalization.<ref name="Amphetamine signaling through ROCKs">{{cite journal | vauthors = Saunders C, Galli A | title = Insights in how amphetamine ROCKs (Rho-associated containing kinase) membrane protein trafficking | journal = Proc. Natl. Acad. Sci. U.S.A. | volume = 112 | issue = 51 | pages = 15538–15539 | date = December 2015 | pmid = 26607447 | pmc = 4697384 | doi = 10.1073/pnas.1520960112 | quote = In this elegant and thorough study (7), Amara and her collaborators identify multiple novel targets for intracellular AMPH. They demonstrate that cytoplasmic AMPH stimulates a secondary pathway of cAMP production, which leads to Rho inactivation by PKA-dependent phosphorylation.&nbsp;... ROCK inhibition blocks the effects of AMPH pretreatment on DA uptake, supporting previous studies suggesting a role for ROCK in AMPH’s behavioral effects... These results further support the idea that direct activation of cytoplasmic signaling cascades by AMPH might contribute to the behavioral effects of acute AMPH exposure.}}</ref><ref name="handbook2022_DAT" /> Importantly, TAAR1 has been demonstrated to also produce inhibitory effects on dopamine release that may attenuate amphetamine's psychostimulant effects.<ref name="handbook2022_TAAR1" /> Through direct activation of [[G protein-coupled inwardly-rectifying potassium channel|G protein-coupled inwardly-rectifying potassium channels]], {{abbr|TAAR1|trace amine associated receptor 1}} reduces the [[Action potential|firing rate]] of dopamine neurons, preventing a hyper-dopaminergic state.<ref name="GIRK">{{cite journal |vauthors=Ledonne A, Berretta N, Davoli A, Rizzo GR, Bernardi G, Mercuri NB | title = Electrophysiological effects of trace amines on mesencephalic dopaminergic neurons | journal =Frontiers in Systems Neuroscience| volume = 5 | pages = 56 | date = July 2011 | pmid = 21772817 | pmc = 3131148 | doi = 10.3389/fnsys.2011.00056 | quote = Three important new aspects of TAs action have recently emerged: (a) inhibition of firing due to increased release of dopamine; (b) reduction of D2 and GABAB receptor-mediated inhibitory responses (excitatory effects due to disinhibition); and (c) a direct TA1 receptor-mediated activation of GIRK channels which produce cell membrane hyperpolarization. | doi-access = free | title-link = doi }}</ref><ref name="Genatlas TAAR1">{{cite web | url = http://genatlas.medecine.univ-paris5.fr/fiche.php?symbol=TAAR1 | title = TAAR1 | date = 28 January 2012 | website = GenAtlas | publisher = University of Paris | access-date = 29 May 2014 | quote={{•}} tonically activates inwardly rectifying K(+) channels, which reduces the basal firing frequency of dopamine (DA) neurons of the ventral tegmental area (VTA) }}</ref>
@@ Line 398: / Line 392: @@
 ====Serotonin====
-Amphetamine exerts analogous, yet less pronounced, effects on serotonin as on dopamine and norepinephrine.<ref name="Miller" /> Amphetamine affects serotonin via {{abbr|VMAT2|vesicular monoamine transporter 2}} and is thought to phosphorylate {{abbr|SERT|serotonin transporter}} via a PKC-dependent signaling cascade.<ref name="2022 T1 LDX" /> Like dopamine, amphetamine has low, micromolar affinity at the human [[5-HT1A receptor]].<ref name="5HT1A secondary2">{{cite encyclopedia |title=Amphetamine |publisher=University of Alberta: T3DB |url=http://www.t3db.ca/toxins/T3D2706 |access-date=24 February 2015 |section=Targets}}</ref><ref name="5HT1A Primary" />
+Amphetamine exerts analogous, yet less pronounced, effects on serotonin as on dopamine and norepinephrine.<ref name="Miller" /> Amphetamine affects serotonin via {{abbr|VMAT2|vesicular monoamine transporter 2}} and is thought to phosphorylate {{abbr|SERT|serotonin transporter}} via a PKC-dependent signaling cascade.<ref name="2022 T1 LDX" /> Like dopamine, amphetamine has low, micromolar affinity at the human [[5-HT1A receptor]].<ref name="5HT1A secondary2">{{cite encyclopedia |title=Amphetamine |publisher=University of Alberta T3DB |url=http://www.t3db.ca/toxins/T3D2706 |access-date=24 February 2015 |section=Targets}}</ref><ref name="5HT1A Primary" />
 ====Other neurotransmitters, peptides, hormones, and enzymes====
@@ Line 428: / Line 422: @@
 ===Pharmacokinetics===
-The oral [[bioavailability]] of amphetamine varies with gastrointestinal pH;<ref name="FDA" /> it is well [[Absorption (pharmacology)|absorbed]] from the gut, and bioavailability is typically 90%.<ref name="handbook2022">{{Cite book |title=Handbook of Substance Misuse and Addictions |publisher=Springer International Publishing |year=2022 |isbn=978-3-030-92391-4 |veditors=Patel VB, Preedy VR |location=Cham |page=2006 |doi=10.1007/978-3-030-92392-1 |quote=Amphetamine is usually consumed via inhalation or orally, either in the form of a racemic mixture (levoamphetamine and dextroamphetamine) or dextroamphetamine alone (Childress et al. 2019). In general, all amphetamines have high bioavailability when consumed orally, and in the specific case of amphetamine, 90% of the consumed dose is absorbed in the gastrointestinal tract, with no significant differences in the rate and extent of absorption between the two enantiomers (Carvalho et al. 2012; Childress et al. 2019). The onset of action occurs approximately 30 to 45 minutes after consumption, depending on the ingested dose and on the degree of purity or on the concomitant consumption of certain foods (European Monitoring Centre for Drugs and Drug Addiction 2021a; Steingard et al. 2019). It is described that those substances that promote acidification of the gastrointestinal tract cause a decrease in amphetamine absorption, while gastrointestinal alkalinization may be related to an increase in the compound’s absorption (Markowitz and Patrick 2017).}}</ref> Amphetamine is a weak base with a [[Acid dissociation constant|p''K''<sub>a</sub>]] of 9.9;<ref name="FDA Pharmacokinetics" /> consequently, when the pH is basic, more of the drug is in its [[lipid]] soluble [[free base]] form, and more is absorbed through the lipid-rich [[cell membranes]] of the gut [[epithelium]].<ref name="FDA Pharmacokinetics" /><ref name="FDA" /> Conversely, an acidic pH means the drug is predominantly in a water-soluble [[cation]]ic (salt) form, and less is absorbed.<ref name="FDA Pharmacokinetics" /> Approximately {{nowrap|20%}} of amphetamine circulating in the bloodstream is bound to [[plasma protein]]s.<ref name="Drugbank-amph">{{cite DrugBank|drug=Amphetamine|id=DB00182}}</ref> Following absorption, amphetamine readily [[Distribution (pharmacology)|distributes]] into most tissues in the body, with high concentrations occurring in [[cerebrospinal fluid]] and [[human brain|brain]] tissue.<ref name="HSDB Toxnet October 2017 Full archived record">{{cite encyclopedia |title=Amphetamine |section=Metabolism/Pharmacokinetics |url=http://toxnet.nlm.nih.gov/cgi-bin/sis/search/r?dbs+hsdb:@term+@rn+@rel+300-62-9 |publisher=Hazardous Substances Data Bank. United States National Library of Medicine&nbsp;– Toxicology Data Network |access-date=2 October 2017 |archive-url=https://web.archive.org/web/20171002194327/https://toxnet.nlm.nih.gov/cgi-bin/sis/search2/cgi-bin/sis/search2/f?.%2Ftemp%2F~mdjW95%3A1%3AFULL |archive-date=2 October 2017 |quote=Duration of effect varies depending on agent and urine pH. Excretion is enhanced in more acidic urine. Half-life is 7 to 34&nbsp;hours and is, in part, dependent on urine pH (half-life is longer with alkaline urine).&nbsp;... Amphetamines are distributed into most body tissues with high concentrations occurring in the brain and CSF. Amphetamine appears in the urine within about 3&nbsp;hours following oral administration.&nbsp;... Three days after a dose of (+ or -)-amphetamine, human subjects had excreted 91% of the (14)C in the urine}}</ref>
+The oral [[bioavailability]] of amphetamine varies with gastrointestinal pH;<ref name="FDA" /> it is well [[Absorption (pharmacology)|absorbed]] from the gut, and bioavailability is typically 90%.<ref name="Antunes_2022">{{cite book | vauthors = Antunes M, Marques H, Rosado T, Soares S, Gonçalves J, Barroso M, Gallardo E, Simão AY | veditors = Patel VB, Preedy VR | chapter = Amphetamine in Biological Specimens: Impact and Implications for Public Health | title = Handbook of Substance Misuse and Addictions | pages = 2003–2027 (2006) | date = 2022 | doi = 10.1007/978-3-030-92392-1_104 | publisher = Springer International Publishing | publication-place = Cham | isbn = 978-3-030-92391-4 | chapter-url = https://www.researchgate.net/profile/Tiago-Rosado/publication/358977284_Amphetamine_in_biological_specimens_impact_and_implications_for_public_health/links/63fc955757495059454aaae6/Amphetamine-in-biological-specimens-impact-and-implications-for-public-health.pdf | quote = Amphetamine is usually consumed via inhalation or orally, either in the form of a racemic mixture (levoamphetamine and dextroamphetamine) or dextroamphetamine alone (Childress et al. 2019). In general, all amphetamines have high bioavailability when consumed orally, and in the specific case of amphetamine, 90% of the consumed dose is absorbed in the gastrointestinal tract, with no significant differences in the rate and extent of absorption between the two enantiomers (Carvalho et al. 2012; Childress et al. 2019). The onset of action occurs approximately 30 to 45 minutes after consumption, depending on the ingested dose and on the degree of purity or on the concomitant consumption of certain foods (European Monitoring Centre for Drugs and Drug Addiction 2021a; Steingard et al. 2019). It is described that those substances that promote acidification of the gastrointestinal tract cause a decrease in amphetamine absorption, while gastrointestinal alkalinization may be related to an increase in the compound’s absorption (Markowitz and Patrick 2017). }}</ref> Amphetamine is a weak base with a [[Acid dissociation constant|p''K''<sub>a</sub>]] of 9.9;<ref name="FDA Pharmacokinetics" /> consequently, when the pH is basic, more of the drug is in its [[lipid]] soluble [[free base]] form, and more is absorbed through the lipid-rich [[cell membranes]] of the gut [[epithelium]].<ref name="FDA Pharmacokinetics" /><ref name="FDA" /> Conversely, an acidic pH means the drug is predominantly in a water-soluble [[cation]]ic (salt) form, and less is absorbed.<ref name="FDA Pharmacokinetics" /> Approximately {{nowrap|20%}} of amphetamine circulating in the bloodstream is bound to [[plasma protein]]s.<ref name="Drugbank-amph">{{cite DrugBank|drug=Amphetamine|id=DB00182}}</ref> Following absorption, amphetamine readily [[Distribution (pharmacology)|distributes]] into most tissues in the body, with high concentrations occurring in [[cerebrospinal fluid]] and [[human brain|brain]] tissue.<ref name="HSDB Toxnet October 2017 Full archived record">{{cite encyclopedia |title=Amphetamine |section=Metabolism/Pharmacokinetics |url=http://toxnet.nlm.nih.gov/cgi-bin/sis/search/r?dbs+hsdb:@term+@rn+@rel+300-62-9 |publisher=Hazardous Substances Data Bank. United States National Library of Medicine&nbsp;– Toxicology Data Network |access-date=2 October 2017 |archive-url=https://web.archive.org/web/20171002194327/https://toxnet.nlm.nih.gov/cgi-bin/sis/search2/cgi-bin/sis/search2/f?.%2Ftemp%2F~mdjW95%3A1%3AFULL |archive-date=2 October 2017 |quote=Duration of effect varies depending on agent and urine pH. Excretion is enhanced in more acidic urine. Half-life is 7 to 34&nbsp;hours and is, in part, dependent on urine pH (half-life is longer with alkaline urine).&nbsp;... Amphetamines are distributed into most body tissues with high concentrations occurring in the brain and CSF. Amphetamine appears in the urine within about 3&nbsp;hours following oral administration.&nbsp;... Three days after a dose of (+ or -)-amphetamine, human subjects had excreted 91% of the (14)C in the urine}}</ref>
 The [[Biological half-life|half-lives]] of amphetamine enantiomers differ and vary with urine pH.<ref name="FDA Pharmacokinetics" /> At normal urine pH, the half-lives of dextroamphetamine and levoamphetamine are {{nowrap|9–11}}&nbsp;hours and {{nowrap|11–14}}&nbsp;hours, respectively.<ref name="FDA Pharmacokinetics" /> Highly acidic urine will reduce the enantiomer half-lives to 7&nbsp;hours;<ref name="HSDB Toxnet October 2017 Full archived record" /> highly alkaline urine will increase the half-lives up to 34&nbsp;hours.<ref name="HSDB Toxnet October 2017 Full archived record" /> The immediate-release and extended release variants of salts of both isomers reach [[Cmax (pharmacology)|peak plasma concentrations]] at 3&nbsp;hours and 7&nbsp;hours post-dose respectively.<ref name="FDA Pharmacokinetics" /> Amphetamine is [[Elimination (pharmacology)|eliminated]] via the [[kidney]]s, with {{nowrap|30–40%}} of the drug being excreted unchanged at normal urinary pH.<ref name="FDA Pharmacokinetics" /> When the urinary pH is basic, amphetamine is in its free base form, so less is excreted.<ref name="FDA Pharmacokinetics" /> When urine pH is abnormal, the urinary recovery of amphetamine may range from a low of 1% to a high of 75%, depending mostly upon whether urine is too basic or acidic, respectively.<ref name="FDA Pharmacokinetics" /> Following oral administration, amphetamine appears in urine within 3&nbsp;hours.<ref name="HSDB Toxnet October 2017 Full archived record" /> Roughly 90% of ingested amphetamine is eliminated 3&nbsp;days after the last oral dose.<ref name="HSDB Toxnet October 2017 Full archived record" />{{if pagename|Adderall=|Dextroamphetamine=|other=&nbsp;

Amphetamine: Difference between revisions

Revision as of 19:16, 17 June 2025

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