Aripiprazole: Complete Drug Monograph

Pharmacokinetic Profile

Half-Life

75 h (parent); 94 h (active metabolite)

Metabolism

Hepatic (CYP2D6, CYP3A4)

Protein Binding

>99% (albumin)

Bioavailability

87% (oral)

Volume of Distribution

404 L (4.9 L/kg)

Clinical Information

Drug Class

Atypical Antipsychotic (D2 Partial Agonist)

Available Doses

2, 5, 10, 15, 20, 30 mg tablets; 1 mg/mL solution; 9.75 mg/1.3 mL IM

Route

Oral, Intramuscular

Renal Adjustment

None required

Hepatic Adjustment

None required

Pregnancy

Category C; neonatal EPS risk with 3rd trimester use

Lactation

Present in breast milk; may reduce milk supply

Schedule / Legal Status

Not a controlled substance

Generic Available

Yes

Black Box Warning

Yes (dementia mortality; suicidality in youth)

Indications

Indication	Approved Population	Therapy Type	Status
Schizophrenia	Adults and adolescents ≥13 years	Monotherapy	FDA Approved
Bipolar I disorder — acute manic/mixed episodes	Adults and pediatric patients ≥10 years	Monotherapy or adjunctive to lithium/valproate	FDA Approved
Major depressive disorder	Adults	Adjunctive to antidepressants	FDA Approved
Irritability associated with autistic disorder	Pediatric patients 6–17 years	Monotherapy	FDA Approved
Tourette’s disorder	Pediatric patients 6–18 years	Monotherapy	FDA Approved
Agitation in schizophrenia or bipolar mania	Adults (IM formulation)	Acute IM injection	FDA Approved

Aripiprazole was first approved in 2002 and remains one of the most broadly indicated atypical antipsychotics. Its unique pharmacological profile as a dopamine D2 partial agonist distinguishes it from older second-generation agents that function primarily as D2 antagonists. The drug is available in multiple formulations including oral tablets, orally disintegrating tablets, oral solution, acute intramuscular injection, and long-acting injectable preparations (Abilify Maintena, Abilify Asimtufii, Aristada).

Off-Label Uses

Anxiety disorders — Open-label data suggest potential benefit, particularly as augmentation to SSRI therapy. Evidence quality: Low.

Treatment-resistant depression — Used as augmentation beyond the standard adjunctive MDD indication; some clinicians use doses above the approved 15 mg ceiling. Evidence quality: Moderate.

Psychosis in dementia — Occasionally used when non-pharmacological approaches fail, although the FDA boxed warning specifically advises against this use due to increased mortality. Evidence quality: Moderate (efficacy) / High (risk).

Antipsychotic-induced tardive dyskinesia — Case reports and small series suggest improvement after switching to aripiprazole. Evidence quality: Very low.

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Schizophrenia — acute episode or new diagnosis	10–15 mg/day	10–15 mg/day	30 mg/day	Doses above 15 mg have not shown superior efficacy (FDA PI) Steady state reached in ~14 days
Schizophrenia — relapse prevention	15 mg/day	15 mg/day	30 mg/day	Demonstrated efficacy in maintenance trials; reassess periodically
Bipolar I mania — monotherapy	15 mg/day	15 mg/day	30 mg/day	May increase based on clinical response
Bipolar I mania — adjunct to lithium or valproate	10–15 mg/day	15 mg/day	30 mg/day	Monitor lithium/valproate levels concurrently
MDD — adjunctive to antidepressant	2–5 mg/day	5–10 mg/day	15 mg/day	Titrate by ≤5 mg at ≥1-week intervals Lower doses than schizophrenia
Acute agitation (IM) — schizophrenia or bipolar mania	9.75 mg IM	N/A	30 mg/day IM	Range 5.25–15 mg per injection; wait ≥2 h between doses Switch to oral as soon as possible

Pediatric Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Schizophrenia — adolescent (13–17 years)	2 mg/day	10 mg/day	30 mg/day	Titrate: 2 mg → 5 mg (day 3) → 10 mg (day 5); 30 mg not more effective than 10 mg
Bipolar I mania — pediatric (10–17 years)	2 mg/day	10 mg/day	30 mg/day	Same titration schedule as schizophrenia; monotherapy or adjunctive
Autism-related irritability (6–17 years)	2 mg/day	5–10 mg/day	15 mg/day	Increase by ≤5 mg at ≥1-week intervals
Tourette’s disorder — body weight <50 kg (6–18 years)	2 mg/day	5 mg/day	10 mg/day	Target 5 mg after 2 days; may increase to 10 mg at ≥1-week intervals
Tourette’s disorder — body weight ≥50 kg (6–18 years)	2 mg/day	10 mg/day	20 mg/day	2 mg × 2 days → 5 mg × 5 days → 10 mg target on day 8

CYP450 Dose Adjustments

Clinical Scenario	Starting Dose	Maximum Dose	Notes
Known CYP2D6 poor metabolizer	Half of usual dose	Half of usual max	Reduced clearance prolongs exposure
Co-prescribed strong CYP3A4 or CYP2D6 inhibitor	Half of usual dose	Half of usual max	Restore original dose when inhibitor withdrawn
CYP2D6 poor metabolizer + strong CYP3A4 inhibitor	Quarter of usual dose	Quarter of usual max	Double impairment of clearance
Co-prescribed strong CYP3A4 inducer (e.g., carbamazepine)	Double usual dose	Double usual max	Increase over 1–2 weeks; reduce back over 1–2 weeks when inducer stopped

Clinical Pearl: Dosing

For the MDD adjunctive indication, aripiprazole doses are substantially lower (2–15 mg) than those used in schizophrenia (10–30 mg). This reflects the partial agonist pharmacology: in hyperdopaminergic states (psychosis), higher occupancy is needed for functional antagonism, while in hypodopaminergic states (depression), modest D2 partial agonism at lower doses can augment monoaminergic transmission.

Pharmacology

Mechanism of Action

Aripiprazole is classified as a third-generation antipsychotic due to its distinctive receptor profile. Unlike traditional antipsychotics that block dopamine D2 receptors outright, aripiprazole functions as a high-affinity partial agonist at D2 and D3 receptors. In conditions of dopaminergic excess (such as the mesolimbic pathway in psychosis), aripiprazole competes with dopamine and attenuates signalling. In regions of dopaminergic deficit (such as the mesocortical pathway), it provides modest agonist tone that may address negative symptoms and cognitive impairment. Additionally, aripiprazole acts as a partial agonist at serotonin 5-HT1A receptors, an antagonist at 5-HT2A receptors, and has moderate affinity for histamine H1 and adrenergic alpha-1 receptors. This balanced receptor engagement accounts for its relatively favourable metabolic and extrapyramidal side-effect profile compared with many other antipsychotics.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Bioavailability 87%; Tmax 3–5 h (oral), 1 h (IM); food does not affect extent of absorption	Can be administered without regard to meals; IM provides faster peak levels for acute agitation
Distribution	Vd = 404 L (4.9 L/kg); >99% protein-bound (albumin); crosses blood-brain barrier	Extensive tissue distribution; high D2 occupancy (>90%) at clinical doses persists for days after discontinuation
Metabolism	Hepatic via CYP3A4 and CYP2D6; active metabolite dehydro-aripiprazole (~40% of parent exposure)	CYP2D6 poor metabolizers have ~60% reduced clearance; requires dose reduction. No direct glucuronidation; smoking does not affect levels
Elimination	t½ = 75 h (parent), 94 h (dehydro-aripiprazole); steady state by day 14; excretion ~60% faeces, ~25% urine (minimal unchanged drug)	Long half-life means missed doses have less immediate impact but also means adverse effects persist after discontinuation; no renal or hepatic dose adjustment needed

Side Effects

≥10% Very Common

Adverse Effect	Incidence	Clinical Note
Nausea	15%	Most common GI complaint; usually transient and dose-related; onset often in first 1–2 weeks
Headache	12–27%	Rates vary by indication and trial; placebo rates are also high (15–25%), so drug-attributable headache is modest; typically mild and self-limiting
Insomnia	18%	Activating profile of D2 partial agonism; morning dosing may help; distinct from sedating antipsychotics
Akathisia	12%	Dose-related inner restlessness; higher in bipolar mania (~15%) than schizophrenia (~8%); frequently limits tolerability
Anxiety	17%	May overlap with akathisia; careful clinical assessment needed to differentiate from underlying disorder
Restlessness	12%	Related to akathisia spectrum; may present as subjective motor discomfort
Constipation	11%	Less prominent than with highly anticholinergic antipsychotics; dietary and hydration measures usually sufficient
Dizziness	10%	Related to alpha-1 antagonism; advise caution with position changes particularly during initiation

1–10% Common

Adverse Effect	Incidence	Clinical Note
Somnolence / Sedation	8%	More prominent in paediatric populations (up to 24% in autism trials); dose-related
Vomiting	8%	Typically occurs early in treatment and resolves; more common in children
Extrapyramidal symptoms (non-akathisia)	6%	Includes tremor, dystonia, and parkinsonian features; lower than many other antipsychotics
Tremor	5%	Fine postural tremor; generally mild; consider dose reduction if bothersome
Fatigue	6%	Distinguished from somnolence; may improve with time on treatment
Blurred vision	3%	Reported mainly in the MDD adjunctive trials; usually transient
Weight gain	2–5%	Mean gain +0.3 kg in short-term adult monotherapy trials (median 3–4 weeks); higher with longer exposure (~1.5 kg at 8 weeks); more pronounced in antipsychotic-naive youth; less than olanzapine or quetiapine
Dyspepsia	4%	Upper GI discomfort; taking with food may help
Musculoskeletal stiffness	4%	Part of EPS spectrum; usually responds to dose reduction

Serious Serious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Neuroleptic malignant syndrome (NMS)	Very rare	Days to weeks after initiation or dose change	Immediate discontinuation; ICU-level supportive care; monitor CK, renal function, temperature
Tardive dyskinesia	Rare (<1%)	Months to years of treatment	Consider discontinuation if clinically appropriate; may be irreversible; use AIMS for screening
Pathological gambling and compulsive behaviours	Rare	Variable; reported at any time during treatment	Dose reduction or discontinuation; proactively screen all patients; believed related to D3 agonism
Hyperglycaemia / new-onset diabetes	Uncommon (~1–2%)	Weeks to months	Monitor fasting glucose at baseline and periodically; risk lower than with olanzapine or clozapine
Cerebrovascular adverse events (elderly dementia patients)	Uncommon	Variable	Aripiprazole not approved for dementia-related psychosis; avoid use in this population
Seizures	Rare (0.1%)	Any time	Use with caution in patients with seizure history or conditions lowering seizure threshold
Leukopenia / Neutropenia / Agranulocytosis	Rare	First months of therapy	Monitor CBC in patients with pre-existing low WBC or drug-induced leukopenia history; discontinue if significant decline
Anaphylaxis / Angioedema	Very rare	Any time	Emergency treatment; permanent discontinuation; contraindicated in known hypersensitivity
Suicidal thoughts and behaviours (youth on adjunctive MDD therapy)	See boxed warning	Early weeks of treatment or dose changes	Close monitoring in all patients <25 years; family education; smallest prescription quantity

Discontinuation Discontinuation Rates

Adults (Schizophrenia Short-Term Trials)

11% vs 15% placebo

Top reasons: Lack of efficacy, akathisia, insomnia, agitation

Pediatric Patients

7–11% vs 7–17% placebo

Top reasons: Somnolence, EPS, weight gain, behavioural activation

Reason for Discontinuation	Incidence	Context
Akathisia	0.3–1.2%	Low discontinuation rate despite relatively high incidence; many patients tolerate with dose adjustment
EPS / Tremor	<1%	Rarely treatment-limiting; more common in children
Nausea / Vomiting	<1%	GI adverse effects usually self-limiting
Insomnia	<1%	Consider morning dosing before discontinuing

Managing Akathisia

Akathisia is the most clinically significant tolerability barrier with aripiprazole. Management strategies include dose reduction (often the first and most effective step), switching to evening dosing, or adding a short course of a beta-blocker (propranolol 20–80 mg/day) or benzodiazepine. When akathisia occurs with concomitant SSRI use, a pharmacokinetic interaction via CYP2D6 inhibition should be considered, and the aripiprazole dose may need halving.

Int

Drug Interactions

Aripiprazole is metabolised primarily by CYP2D6 and CYP3A4. It does not significantly inhibit or induce major CYP enzymes at clinical doses, so it is unlikely to alter the levels of co-administered medications. However, drugs that modulate CYP2D6 or CYP3A4 activity can substantially change aripiprazole exposure and require dose adjustment.

Major Ketoconazole / Itraconazole

MechanismStrong CYP3A4 inhibition

EffectApproximately doubles aripiprazole AUC, increasing risk of dose-dependent side effects

ManagementReduce aripiprazole to half of usual dose; restore full dose when azole discontinued

FDA PI

Major Fluoxetine / Paroxetine

MechanismStrong CYP2D6 inhibition

EffectIncreased aripiprazole levels; higher risk of akathisia and EPS

ManagementReduce aripiprazole to half of usual dose; particularly relevant in adjunctive MDD treatment

FDA PI

Major Carbamazepine / Rifampin

MechanismStrong CYP3A4 induction

EffectSubstantially reduces aripiprazole plasma levels, risking therapeutic failure

ManagementDouble aripiprazole dose over 1–2 weeks; reduce back when inducer stopped

FDA PI

Major Quinidine

MechanismStrong CYP2D6 inhibition

EffectElevated aripiprazole exposure similar to CYP2D6 poor-metaboliser phenotype

ManagementReduce aripiprazole to half of usual dose

FDA PI

Moderate Benzodiazepines

MechanismAdditive CNS depression

EffectEnhanced sedation, orthostatic hypotension, and respiratory depression (IM co-administration)

ManagementMonitor closely when using both for acute agitation; avoid IV lorazepam within 1 h of IM aripiprazole

FDA PI

Moderate Antihypertensives

MechanismAdditive alpha-1 blockade / hypotensive effects

EffectIncreased risk of orthostatic hypotension and syncope

ManagementMonitor blood pressure; consider slower aripiprazole titration in patients on multiple antihypertensives

Lexicomp

Moderate Lithium / Valproate

MechanismNo significant pharmacokinetic interaction; pharmacodynamic overlap

EffectApproved combination for bipolar mania; additive sedation possible

ManagementNo dose adjustment needed; monitor for additive CNS effects and metabolic parameters

FDA PI

Minor Sertraline / Citalopram / Escitalopram

MechanismWeak-to-moderate CYP2D6 inhibition (sertraline); minimal CYP effect (citalopram/escitalopram)

EffectMild increase in aripiprazole exposure with sertraline; negligible with citalopram

ManagementNo routine dose adjustment; monitor for akathisia especially at higher aripiprazole doses

Lexicomp

Mon

Monitoring

Fasting Glucose & HbA1c Baseline, 12 weeks, then annually
Routine All atypical antipsychotics carry metabolic risk. Aripiprazole has a more favourable glucose profile than olanzapine or clozapine, but monitoring remains standard of care per APA/ADA consensus guidelines.
Lipid Panel Baseline, 12 weeks, then annually
Routine Fasting total cholesterol, LDL, HDL, and triglycerides. Aripiprazole-associated dyslipidaemia is less common than with other second-generation agents.
Body Weight & BMI Baseline, monthly for 3 months, then quarterly
Routine Track weight trajectory particularly in antipsychotic-naive patients and adolescents. Clinically significant gain (≥7% baseline) occurred in up to 33% of paediatric patients over 26 weeks.
Blood Pressure Baseline, then periodically
Routine Orthostatic measurements at initiation; aripiprazole can cause postural hypotension via alpha-1 blockade.
Extrapyramidal Symptoms Each visit
Routine Use AIMS for tardive dyskinesia screening at least every 6–12 months; use Barnes Akathisia Scale if restlessness symptoms reported.
Compulsive Behaviours Each visit
Routine Proactively ask about new gambling, shopping, eating, or sexual urges. Patients may not volunteer this information. Dose reduction or discontinuation required if identified.
CBC with Differential If signs of infection or pre-existing low WBC
Trigger-Based Frequent monitoring during first few months for patients with a history of drug-induced leukopenia. Discontinue if ANC falls significantly without other explanation.
Suicidality Assessment Weekly for first 4 weeks, then at dose changes
Trigger-Based Particularly important in patients <25 years receiving adjunctive aripiprazole for MDD per the boxed warning. Educate family and caregivers to report concerning behavioural changes.

Contraindications & Cautions

Absolute Contraindications

Known hypersensitivity to aripiprazole — reactions have ranged from urticaria to anaphylaxis (FDA PI)

Relative Contraindications (Specialist Input Recommended)

Dementia-related psychosis in elderly patients — increased mortality risk; not an approved indication; prescribing requires exceptional clinical justification and documented informed consent
Known CYP2D6 poor metaboliser receiving concomitant strong CYP3A4 inhibitor — markedly reduced clearance may lead to toxicity even at standard doses; requires quarter-dose or alternative agent
Active pathological gambling or history of impulse-control disorders — aripiprazole’s D3 agonism may exacerbate compulsive behaviours; weigh alternatives carefully

Use with Caution

Cardiovascular or cerebrovascular disease — orthostatic hypotension risk
History of seizures or conditions that lower the seizure threshold
Conditions predisposing to aspiration — dysphagia reported with all antipsychotics
Diabetes or risk factors for diabetes — monitor glucose even though aripiprazole has a relatively favourable metabolic profile
Patients at risk for falls — somnolence, motor instability, and orthostatic hypotension increase fall risk
Extreme heat exposure — antipsychotics can impair thermoregulation

FDA Boxed Warning Increased Mortality in Elderly Patients with Dementia-Related Psychosis

Elderly patients with dementia-related psychosis treated with antipsychotic drugs are at an increased risk of death. Analyses of 17 placebo-controlled trials (modal duration 10 weeks) in this population showed a death rate of 4.5% in drug-treated patients versus 2.6% in placebo-treated patients. Aripiprazole is not approved for dementia-related psychosis.

FDA Boxed Warning Suicidal Thoughts and Behaviours in Youth

Antidepressants (including aripiprazole when used adjunctively for MDD) increased the risk of suicidal thinking and behaviour in children, adolescents, and young adults (18–24 years) in short-term studies. All patients started on antidepressant therapy should be monitored closely for clinical worsening, suicidality, and unusual behavioural changes, particularly during the initial months or at dose adjustments.

Patient Counselling

Purpose of Therapy

Aripiprazole works by rebalancing dopamine activity in the brain. Depending on the condition being treated, it may reduce hallucinations and disordered thinking (schizophrenia), stabilise mood and reduce manic episodes (bipolar disorder), enhance the effectiveness of an antidepressant (depression), or reduce irritability and behavioural outbursts (autism, Tourette’s). The full benefit typically emerges over 2–4 weeks, although some improvement may be noticed within the first week.

How to Take

Take aripiprazole once daily at the same time each day, with or without food. If a dose is missed, take it as soon as remembered unless it is almost time for the next dose. Do not stop the medication suddenly without consulting a prescriber, as abrupt discontinuation may lead to withdrawal-like symptoms. The orally disintegrating tablet should be placed on the tongue and allowed to dissolve; it can be taken without water.

Akathisia (Inner Restlessness)

Tell patient Some patients experience a feeling of needing to keep moving or an inability to sit still. This is a recognised side effect and not a worsening of the psychiatric condition. It is most likely to occur in the first 1–2 weeks and often improves with dose adjustment.

Call prescriber If restlessness is severe, persistent, or causing significant distress. Do not stop the medication without guidance.

Insomnia & Activation

Tell patient Unlike many antipsychotics, aripiprazole can be activating rather than sedating. If sleep difficulties occur, morning dosing is preferred. Practising good sleep hygiene and avoiding caffeine in the afternoon may help.

Call prescriber If insomnia persists for more than 2 weeks or if agitation, racing thoughts, or increased energy suggest a mood change.

Gambling & Compulsive Urges

Tell patient Aripiprazole has been associated with new or intensified urges to gamble, shop excessively, binge eat, or engage in other compulsive behaviours. These urges may be hard to resist and may not feel medication-related.

Call prescriber Immediately if any new compulsive urges develop. The prescriber may reduce the dose or switch to an alternative medication.

Dizziness & Falls

Tell patient The medication can cause lightheadedness, especially when standing up quickly. Rise slowly from sitting or lying positions, particularly during the first few days of treatment. Stay well hydrated.

Call prescriber If fainting occurs or if dizziness is persistent and interferes with daily activities.

Weight & Metabolic Health

Tell patient While aripiprazole generally causes less weight gain than many other antipsychotics, some patients may gain weight. Maintaining a balanced diet and regular physical activity is important. Blood sugar and cholesterol will be monitored periodically.

Call prescriber If experiencing increased thirst, frequent urination, or unexplained weight gain of more than 3 kg.

Mood Changes & Suicidality (MDD Indication)

Tell patient When used alongside an antidepressant, there is a small increased risk of worsening depression or suicidal thoughts, particularly in young adults. Family members should be aware of warning signs including withdrawal, agitation, or talking about self-harm.

Call prescriber Immediately if new or worsening thoughts of self-harm, panic attacks, or marked behavioural changes emerge.

Ref

Sources

Regulatory (PI / SmPC)

Otsuka America Pharmaceutical, Inc. ABILIFY (aripiprazole) Prescribing Information. Revised January 2025. FDA Label Primary source for all dosing, indications, contraindications, adverse reaction incidence data, and drug interaction guidance used in this monograph.
Otsuka America Pharmaceutical, Inc. ABILIFY MAINTENA (aripiprazole) Prescribing Information. 2023. FDA Label Reference for long-acting injectable formulation safety and dosing data.
OPIPZA (aripiprazole) Oral Film Prescribing Information. 2025. FDA Label Most recently approved formulation; adverse reaction data from pooled aripiprazole clinical trial database.

Key Clinical Trials

Potkin SG, Saha AR, Kujawa MJ, et al. Aripiprazole, an antipsychotic with a novel mechanism of action, and risperidone vs. placebo in patients with schizophrenia and schizoaffective disorder. Arch Gen Psychiatry. 2003;60(7):681-690. doi:10.1001/archpsyc.60.7.681 Pivotal RCT establishing efficacy versus placebo with comparative data against risperidone including EPS rates.
Vieta E, Bourin M, Sanchez R, et al. Effectiveness of aripiprazole v. haloperidol in acute bipolar mania: double-blind, randomised, comparative 12-week trial. Br J Psychiatry. 2005;187:235-242. doi:10.1192/bjp.187.3.235 Head-to-head trial demonstrating comparable antimanic efficacy with superior EPS tolerability profile.
Berman RM, Marcus RN, Swanink R, et al. The efficacy and safety of aripiprazole as adjunctive therapy in major depressive disorder: a multicenter, randomized, double-blind, placebo-controlled study. J Clin Psychiatry. 2007;68(6):843-853. doi:10.4088/jcp.v68n0604 Key trial supporting the adjunctive MDD indication with dose-response and akathisia incidence data.

Guidelines

American Psychiatric Association. Practice guideline for the treatment of patients with schizophrenia, 3rd edition. Am J Psychiatry. 2021;178(suppl). doi:10.1176/appi.books.9780890424841 Current APA guideline positioning aripiprazole among first-line oral antipsychotic options for schizophrenia.
American Diabetes Association, American Psychiatric Association, American Association of Clinical Endocrinologists, North American Association for the Study of Obesity. Consensus development conference on antipsychotic drugs and obesity and diabetes. Diabetes Care. 2004;27(2):596-601. doi:10.2337/diacare.27.2.596 Establishes metabolic monitoring standards for all atypical antipsychotics including aripiprazole.

Mechanistic / Basic Science

Burris KD, Molski TF, Xu C, et al. Aripiprazole, a novel antipsychotic, is a high-affinity partial agonist at human dopamine D2 receptors. J Pharmacol Exp Ther. 2002;302(1):381-389. doi:10.1124/jpet.102.033175 Foundational study characterising the D2 partial agonist mechanism that underpins aripiprazole’s unique pharmacology.
Grunder G, Carlsson A, Wong DF. Mechanism of new antipsychotic medications: occupancy is not just antagonism. Arch Gen Psychiatry. 2003;60(10):974-977. doi:10.1001/archpsyc.60.10.974 Conceptual framework for understanding dopamine partial agonism and functional selectivity in antipsychotic action.

Pharmacokinetics / Special Populations

Boulton DW, Kollia G, Mallikaarjun S, et al. Pharmacokinetics and tolerability of intramuscular, oral and intravenous aripiprazole in healthy subjects and in patients with schizophrenia. Clin Pharmacokinet. 2008;47(7):475-485. doi:10.2165/00003088-200847070-00006 Comprehensive PK characterisation across formulations including IM bioavailability and Tmax data.
Kim JR, Sohn S, Yoon YR, et al. Population pharmacokinetic modelling of aripiprazole and its active metabolite, dehydroaripiprazole, in psychiatric patients. Br J Clin Pharmacol. 2008;66(6):802-810. doi:10.1111/j.1365-2125.2008.03223.x Population PK model confirming CYP2D6 genotype impact on clearance with metabolite kinetics in real-world psychiatric populations.
Grunder G, Fellows C, Carlsson A, et al. Brain and plasma pharmacokinetics of aripiprazole in patients with schizophrenia. Am J Psychiatry. 2008;165(8):988-995. doi:10.1176/appi.ajp.2008.07101574 PET study demonstrating high D2/D3 receptor occupancy across brain regions at clinical doses with slow dissociation.