Mixed amphetamine salts

Mixed amphetamine salts (MAS) — marketed primarily as Adderall — is a 3:1 mixture of dextroamphetamine and levoamphetamine salts (dextroamphetamine sulfate, amphetamine sulfate, dextroamphetamine saccharate, and amphetamine aspartate). Amphetamine was first synthesized in 1887 by Lazăr Edeleanu, then developed as a medicine in the late 1920s. "Adderall" was approved by the FDA in 1996, and has since become one of the most popular medicines in the United States. Adderall/MAS is FDA-approved for attention-deficit hyperactivity disorder and narcolepsy. It is listed in Schedule II of the Controlled Substances Act, and so is tightly regulated in the United States as well as many other countries around the world.

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<indication ref="distractibility" author="MDElliottMD"> Impoved sustained attention by decreasing distractibility </indication>

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• Attention and focus👤 100% +83.5 (n=2)⚕️ ~80% +100.0 (n=1)Rate×

  Improved sustained attention, particularly on uninteresting things.
• Reduced impulsivity and hyperactivity👤 100% +33.0 (n=2)⚕️ ~50% +67.0 (n=1)Rate×
• Wakefulness👤 100% +83.5 (n=2)⚕️ ~80% +100.0 (n=1)Rate×
• Motivation and drive👤 100% +66.5 (n=2)⚕️ ~66% +100.0 (n=1)Rate×
• Mild euphoria👤 50% +100.0 (n=2)⚕️ ~66% +100.0 (n=1)Rate×
• Decreased appetite/Anorexia👤 100% +50.0 (n=2)⚕️ ~50% +33.0 (n=1)Rate×
• Dry mouth👤 50% -33.0 (n=2)⚕️ ~66% -33.0 (n=1)Rate×
• Elevated heart rate / blood pressure👤 50% +0.0 (n=2)⚕️ ~50% -33.0 (n=1)Rate×
• Jaw clenching / bruxism👤 50% -33.0 (n=2)⚕️ ~33% -33.0 (n=1)Rate×
• Insomnia👤 0% — (n=2)⚕️ ~5% -67.0 (n=1)Rate×

  (with proper am dosing)
• Irritability👤 50% -33.0 (n=2)⚕️ ~20% -67.0 (n=1)Rate×
• Anxiety👤 0% — (n=2)⚕️ ~20% -67.0 (n=1)Rate×
• Headache👤 0% — (n=2)⚕️ ~5% -67.0 (n=1)Rate×
• Weight loss👤 0% — (n=2)⚕️ ~20% +67.0 (n=1)Rate×
• Palpitations👤 0% — (n=2)⚕️ ~20% -67.0 (n=1)Rate×
• Stereotyped behaviors👤 50% -67.0 (n=2)⚕️ ~5% -67.0 (n=1)Rate×

  Repetitive movements, e.g. skin picking, muscle twitches, tics
• Serious cardiac event👤 0% — (n=2)⚕️ ~0% -100.0 (n=1)Rate×
• Agitation👤 0% — (n=2)⚕️ ~5% -67.0 (n=1)Rate×
• Psychosis👤 0% — (n=2)⚕️ ~5% -100.0 (n=1)Rate×
• Mania👤 0% — (n=2)⚕️ ~5% -100.0 (n=1)Rate×
• Dependence / misuse👤 0% — (n=2)⚕️ ~5% -67.0 (n=1)Rate×
• Tolerance👤 50% -33.0 (n=2)⚕️ ~5% -33.0 (n=1)Rate×
• Growth suppression👤 0% — (n=2)⚕️ ~0% -67.0 (n=1)Rate×

  (well documented effect with chronic use in children)
• Serotonin syndrome👤 0% — (n=2)⚕️ ~0% -100.0 (n=1)Rate×

  Especially in combination with MAOIs
• Peripheral vasculopathy👤 0% — (n=2)⚕️ ~5% -33.0 (n=1)Rate×

  Raynaud-like phenomenon, rare digital ischemia.
• Seizure/Epileptic fit👤 0% — (n=2)⚕️ ~0% -100.0 (n=1)Rate×
• Hyperthermia👤 0% — (n=2)⚕️ ~0% -67.0 (n=1)Rate×

  Risk in hot environments or with vigorous exercise.
• Withdrawal/Discontinuation Syndrome👤 50% -33.0 (n=2)⚕️ ~50% -67.0 (n=1)Rate×

  Low motivation, low mood, hypersomnia, increased appetite on abrupt discontinuation.
• Urinary Retention👤 50% -33.0 (n=2)⚕️ ~33% -33.0 (n=1)Rate×

  Difficult/slow urination

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Absorption

Excellent oral bioavailability — sources report ">75%" to "~90%". Food does not significantly affect total absorption but can delay peak concentration.

Distribution

Volume of distribution ~4 L/kg; plasma protein binding less than 20%. Crosses the blood–brain barrier and placenta.

Metabolism

Amphetamine is oxidized to 4-hydroxyamphetamine, α-hydroxyamphetamine, or norephedrine. Norephedrine and 4-hydroxyamphetamine are active metabolites and are further metabolized to 4-hydroxy-norephedrine. Deamination of α-hydroxyamphetamine yields phenylacetone, which is metabolized to benzoic acid and conjugated to its glucuronide and hippuric acid. CYP2D6 is crucial for amphetamine metabolism; genetic polymorphism causes significant inter-patient variability in clearance. Amphetamine itself inhibits monoamine oxidase (MAO), and both CYP1A2 and CYP3A4 contribute to its metabolism.^[2]

Elimination

Primarily renal — ~30–40% recovered as unchanged amphetamine, the rest as metabolites. Due to its pK_a of 9.9, urinary elimination is highly pH-dependent: alkaline urine reduces ionization and decreases renal clearance, while acidic urine and high flow rates accelerate clearance via active tubular secretion. Half-life: D-enantiomer 9 h (children 6–12 y), 11 h (adolescents 13–17 y), 10 h (adults); L-enantiomer 11 h, 13–14 h, 13 h respectively.

Amphetamine purportedly works via several converging mechanisms at monoaminergic terminals:

• Trace amine-associated receptor 1 (TAAR1) agonism — activates TAAR1 in monoaminergic neurons, triggering PKA/PKC signaling that phosphorylates the dopamine and norepinephrine transporters (DAT, NET), causing them to internalize and reverse direction.
• VMAT2 substrate — enters the presynaptic terminal, displaces dopamine and norepinephrine from vesicles into the cytoplasm.
• Reverse transport via DAT/NET — the elevated cytoplasmic monoamine pool is then ejected into the synaptic cleft via the now-reversed transporters. This is the primary mechanism of action — release, not reuptake inhibition.
• Weak reuptake inhibition at DAT and NET (secondary to release).
• MAO inhibition at higher concentrations, slowing presynaptic catabolism of monoamines.
• Serotonergic effects at high or supratherapeutic doses (relevant to overdose and serotonin syndrome risk).

The net result is a robust increase in synaptic dopamine and norepinephrine in prefrontal cortex, striatum, and nucleus accumbens — underlying both therapeutic (attention, executive function, wakefulness) and reinforcing (euphoria, abuse liability) effects.

Minimal in practice. Caution with other psychostimulants, including caffeine. metabolized by 2D6, so relevant caution applies.

Category C. Crosses the placenta. Prenatal amphetamine exposure has been associated with low birth weight, premature delivery, and neonatal withdrawal (agitation, dysphoria, lassitude). Long-term neurodevelopmental outcomes from prescribed therapeutic exposure are less clear and likely modest, but illicit-dose exposure is associated with significant developmental impact. Decision should be individualized; many patients defer ADHD treatment during pregnancy. Excreted in breast milk in clinically significant amounts — breastfeeding generally discouraged.

• Baseline: cardiovascular history, weight/height, mental health history (especially for psychosis/bipolar/substance use risk), (optional) blood pressure, (optional) heart rate,
• At each visit: efficacy, side effects, general well-being
• Periodically reassess continued need; consider drug holidays to assess ongoing benefit
• Sleep quality (insomnia is dose-limiting)

  Patient counseling

• Take first thing in the morning to minimize insomnia; avoid (late) afternoon dosing.
• Do not crush, chew, or split Adderall XR or Mydayis capsules — disrupts the controlled-release mechanism. (Capsules may be opened and sprinkled on applesauce if needed.)
• Take with or without food; high-acid beverages (orange juice, vitamin C) may reduce absorption.
• Stay well-hydrated, especially in heat or during exercise.
• Eat regular meals despite appetite suppression.
• Report any chest pain, palpitations, severe agitation, hallucinations, or signs of poor circulation in extremities.
• Sudden discontinuation can cause a fatigue/depression "crash" — plan for it.
• Take caution: make increase bowel motility and increase risk of expelled fecal content.

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