Hubbry Logo
AripiprazoleAripiprazoleMain
Open search
Aripiprazole
Community hub
Aripiprazole
logo
8 pages, 0 posts
0 subscribers
Be the first to start a discussion here.
Be the first to start a discussion here.
Contribute something
Aripiprazole
Aripiprazole
Aripiprazole
View on Wikipedia
from Wikipedia

Aripiprazole
Structural formula of aripiprazole
Ball-and-stick model of the aripiprazole molecule
Clinical data
Pronunciation/ˌɛrɪˈpɪprəzl/
AIR-ih-PIP-rə-zohl
Abilify /əˈbɪlɪf/
ə-BIL-if-eye
Trade namesAbilify, others
Other namesOPC-14597; OPC14597; OPC-31; OPC31; RDC-3317
AHFS/Drugs.comMonograph
MedlinePlusa603012
License data
Pregnancy
category
Routes of
administration		By mouth, intramuscular
Drug classAtypical antipsychotic
ATC code
Legal status
Legal status
Pharmacokinetic data
Bioavailability87%[7][12][13]
Protein binding>99%[7][12][13]
MetabolismLiver (mostly via CYP3A4 and 2D6[7][12][13])
MetabolitesDehydroaripiprazole
Elimination half-life75 hours (active metabolite is 94 hours)[7][12][13]
ExcretionKidney (27%; <1% unchanged)
feces (60%; 18% unchanged)[7][12][13]
Identifiers
  • 7-{4-[4-(2,3-Dichlorophenyl)piperazin-1-yl]butoxy}-3,4-dihydroquinolin-2(1H)-one
CAS Number
PubChem CID
IUPHAR/BPS
DrugBank
ChemSpider
UNII
KEGG
ChEBI
ChEMBL
CompTox Dashboard (EPA)
ECHA InfoCard100.112.532 Edit this at Wikidata
Chemical and physical data
FormulaC23H27Cl2N3O2
Molar mass448.39 g·mol−1
3D model (JSmol)
  • Clc4cccc(N3CCN(CCCCOc2ccc1c(NC(=O)CC1)c2)CC3)c4Cl
  • InChI=1S/C23H27Cl2N3O2/c24-19-4-3-5-21(23(19)25)28-13-11-27(12-14-28)10-1-2-15-30-18-8-6-17-7-9-22(29)26-20(17)16-18/h3-6,8,16H,1-2,7,9-15H2,(H,26,29) checkY
  • Key:CEUORZQYGODEFX-UHFFFAOYSA-N checkY
  (verify)
Aribit (Aripiprazole) tablets

Aripiprazole, sold under the brand name Abilify, Aripiprex, Ariply among others, is an atypical antipsychotic[14] primarily used in the treatment of schizophrenia, bipolar disorder, and irritability associated with autism spectrum disorder;[14] other uses include as an add-on treatment for major depressive disorder and tic disorders.[14] Aripiprazole is taken by mouth or via injection into a muscle.[14]

Common side effects include restlessness, insomnia, transient weight gain, nausea, vomiting, constipation, dizziness, and mild sedation.[14] Serious side effects may include neuroleptic malignant syndrome, tardive dyskinesia, and anaphylaxis.[14] It is not recommended for older people with dementia-related psychosis due to an increased risk of death.[14] In pregnancy, there is evidence of possible harm to the fetus.[14][15] It is not recommended in women who are breastfeeding.[14] It has not been very well studied in people younger than 18 years old.[14]

Aripiprazole was approved for medical use in the United States in 2002.[14] It is available as a generic medication.[16] In 2023, it was the 95th most commonly prescribed medication in the United States, with more than 7 million prescriptions.[17][18] It is on the World Health Organization's List of Essential Medicines.[19]

Medical uses

[edit]

Aripiprazole is primarily used for the treatment of schizophrenia or bipolar disorder.[13][14][7]

Schizophrenia

[edit]

The 2016 National Institute for Health and Care Excellence (NICE) guidance for treating psychosis and schizophrenia in children and young people recommended aripiprazole as a second-line treatment after risperidone for people between 15 and 17 who are having an acute exacerbation or recurrence of psychosis or schizophrenia.[20] A 2014 NICE review of the depot formulation of the drug found that it might have a role in treatment as an alternative to other depot formulations of second-generation antipsychotics for people who have trouble taking medication as directed or who prefer it.[21]

A 2014 Cochrane review comparing aripiprazole and other atypical antipsychotics found that it is difficult to determine differences as data quality is poor.[22] A 2011 Cochrane review comparing aripiprazole with placebo concluded that high dropout rates in clinical trials, and a lack of outcome data regarding general functioning, behavior, mortality, economic outcomes, or cognitive functioning make it difficult to definitively conclude that aripiprazole is useful for the prevention of relapse.[23] This review found only low-quality evidence of effectiveness in treating schizophrenia.[23]

A 2013 review placed aripiprazole in the middle range of 15 antipsychotics for effectiveness, approximately as effective as haloperidol and quetiapine[24] and slightly more effective than ziprasidone, chlorpromazine, and asenapine, with better tolerability compared to the other antipsychotic drugs (4th best for reducing weight gain, 5th best for reducing extrapyramidal symptoms, the best for reducing prolactin levels, 2nd best for prolongated QTc interval, and 5th best for sedative symptoms). The authors concluded that for acute psychotic episodes, aripiprazole results in benefits in some aspects of the condition.[25]

In 2013 the World Federation of Societies for Biological Psychiatry recommended aripiprazole for the treatment of acute exacerbations of schizophrenia as a Grade 1 recommendation and evidence level A.[26]

The British Association for Psychopharmacology similarly recommends that all persons presenting with psychosis receive treatment with an antipsychotic and that such treatment should continue for at least 1–2 years, as "There is no doubt that antipsychotic discontinuation is strongly associated with relapse during this period". The guideline further notes that "Established schizophrenia requires continued maintenance with doses of antipsychotic medication within the recommended range (Evidence level A)".[27]

The British Association for Psychopharmacology[27] and the World Federation of Societies for Biological Psychiatry suggest that there is little difference in effectiveness between antipsychotics in the prevention of relapse, and recommend that the specific choice of antipsychotic be chosen based on each person's preference and side effect profile. The latter group recommends switching to aripiprazole when excessive weight gain is encountered during treatment with other antipsychotics.[26]

Bipolar disorder

[edit]

Aripiprazole is effective for the treatment of acute manic episodes of bipolar disorder in adults, children, and adolescents.[28][29] Used as maintenance therapy, it is useful for the prevention of manic episodes but is not useful for bipolar depression.[30][31] Thus, it is often used in combination with an additional mood stabilizer; however, co-administration with a mood stabilizer increases the risk of extrapyramidal side effects.[32] In September 2014, aripiprazole had a UK marketing authorization for up to twelve weeks of treatment for moderate to severe manic episodes in bipolar I disorder in young people aged thirteen and older. Aripiprazole in low doses of 2.5 mg can cause mania in those with Bipolar disorder.[33][34][35]

Depression

[edit]

Aripiprazole is an effective add-on treatment for major depressive disorder; however, there is a greater rate of side effects such as weight gain and movement disorders.[36][37][38] The overall benefit is small to moderate and its use appears to neither improve quality of life nor functioning.[36] Aripiprazole may interact with some antidepressants, especially selective serotonin reuptake inhibitors (SSRIs) that are metabolized by CYP2D6. There are known interactions with fluoxetine and paroxetine[39] and it appears lesser interactions with sertraline, escitalopram, citalopram and fluvoxamine. CYP2D6 inhibitors increase aripiprazole concentrations to 2–3 times their normal level.[40] When strong CYP2D6 SSRIs (such as fluoxetine, paroxetine) are co-administered, the FDA recommends dose monitoring, although it is not clear the SSRI dose should be lowered.[7][41][42][43]

Autism

[edit]

Short-term data (8 weeks) shows reduced irritability, hyperactivity, inappropriate speech, and stereotypy, but no change in lethargic behaviours.[44] Adverse effects include weight gain, sleepiness, drooling, and tremors.[44] It is suggested that children and adolescents need to be monitored regularly while taking this medication to evaluate if this treatment option is still effective after long-term use and note if side effects are worsening. Further studies are needed to understand if this drug is helpful for children after long-term use.[44]

Tic disorders

[edit]

Aripiprazole is approved for the treatment of Tourette syndrome and other tic disorders.[45][46][47] There is evidence supporting that it is effective, safe, and well-tolerated for this use per systematic reviews and meta-analyses.[48][49][50][51]

Obsessive-compulsive disorder

[edit]

A 2014 systematic review and meta-analysis concluded that add-on therapy with low-dose aripiprazole is an effective treatment for obsessive-compulsive disorder (OCD) that does not improve with selective serotonin reuptake inhibitors (SSRIs) alone.[52] The conclusion was based on the results of two relatively small, short-term trials, each of which demonstrated improvements in symptoms.[52][53][54][55] However, aripiprazole is cautiously recommended by a 2017 review on antipsychotics for OCD.[56] Aripiprazole is not currently approved for the treatment of OCD and is instead used off-label for this indication.[45] Depending on the dose, aripiprazole can increase impulse control issues in a small percentage of people. The FDA Drug Safety Communication warned about this side effect.[57]

Available forms

[edit]
See also: Aripiprazole lauroxil

Aripiprazole is available in the form of oral tablets, orally disintegrating tablets, oral solutions, oral films, and as injectables for intramuscular administration.[58][failed verification] It is also available in the form of aripiprazole lauroxil, a lipophilic ester prodrug of aripiprazole for use as a long-acting injectable.[58][failed verification]

Contraindications

[edit]

Contraindications to aripiprazole include known hypersensitivity to aripiprazole, among others.[14]

Adverse effects

[edit]
See also: List of adverse effects of aripiprazole

In elderly with dementia-related psychosis who are treated with antipsychotics, there is an increased risk of death.[59] In children, adolescents, and young adults treated with antidepressants there is an increased risk of suicidal thoughts or behavior.[7]

In adults, side effects with greater than 10% incidence include weight gain, mania, headache, akathisia, insomnia, delirium, and gastrointestinal effects like nausea, constipation, and lightheadedness.[7][12][13][40][60] Side effects in children are similar, and include sleepiness, increased appetite, and stuffy nose.[40] A strong desire to gamble, binge eat, shop, and engage in sexual activity may also occur rarely.[61][62] These urges can be uncontrollable.[61]

Uncontrolled movement such as restlessness, tremors, and muscle rigidity may occur.[40]

Discontinuation

[edit]

The British National Formulary recommends a gradual withdrawal when discontinuing antipsychotics to avoid acute withdrawal syndrome or rapid relapse.[63] Symptoms of withdrawal commonly include nausea, vomiting, and loss of appetite.[64] Other symptoms may include restlessness, increased sweating, and trouble sleeping.[64] Less commonly there may be a feeling of the world spinning, numbness, or muscle pains.[64] Symptoms generally resolve after a short period of time.[64]

There is tentative evidence that discontinuation of antipsychotics can result in psychosis as a part of a withdrawal syndrome.[65] It may also result in reoccurrence of the condition that is being treated.[66] Rarely tardive dyskinesia can occur when the medication is stopped.[64]

Overdose

[edit]

Children or adults who ingested acute overdoses have usually manifested central nervous system depression ranging from mild sedation to coma; serum concentrations of aripiprazole and dehydroaripiprazole in these people were elevated by up to 3–4 fold over normal therapeutic levels; as of 2008, no deaths had been recorded.[67][68]

Interactions

[edit]

Aripiprazole is a substrate of CYP2D6 and CYP3A4. Coadministration with medications that inhibit (e.g. paroxetine, fluoxetine) or induce (e.g. carbamazepine) these metabolic enzymes are known to increase and decrease, respectively, plasma levels of aripiprazole.[69][7]

Precautions should be taken in people with an established diagnosis of diabetes mellitus who are started on atypical antipsychotics along with other medications that affect blood sugar levels and should be monitored regularly for worsening of glucose control. The liquid form (oral solution) of this medication may contain up to 15 grams of sugar per dose.[14]

Antipsychotics like aripiprazole and stimulant medications, such as amphetamine, are traditionally thought to have opposing effects because both drugs affect dopaminergic neurons. However, both stimulants and antipsychotics lead to increases in synaptic dopamine levels.[70] In antipsychotics, this is caused by the inhibition of dopamine autoreceptors as well as the effects of antipsychotics on non-dopaminergic receptors, while in amphetamine this is caused by non-competitive inhibition of dopamine reuptake and agonism of intracellular TAAR1. Therefore, aripiprazole may interact with amphetamine to synergistically increase postsynaptic levels of dopamine. This interaction frequently occurs in the setting of comorbid attention deficit hyperactivity disorder (ADHD) (for which stimulants are commonly prescribed) and off-label treatment of aggression with antipsychotics. Aripiprazole has been reported to provide some benefit in improving cognitive functioning in people with ADHD without other psychiatric comorbidities, though the results have been disputed. The combination of antipsychotics like aripiprazole with stimulants should not be considered an absolute contraindication.[71]

Pharmacology

[edit]

Pharmacodynamics

[edit]
See also: Atypical antipsychotic § Pharmacodynamics, and Antipsychotic § Comparison of medications
Aripiprazole[72][73][74]
Site Ki (nM) IA (%) Action Ref
SERTTooltip Serotonin transporter 900–1260 Reuptake inhibitor [75][73]
NETTooltip Norepinephrine transporter 1340–2840 Reuptake inhibitor [73]
DATTooltip Dopamine transporter 2560–3880 Reuptake inhibitor [73]
5-HT1A 1.7–6.4 68% Partial agonist / functional full agonist [73][76][75]
5-HT1B 570–1090 ND [73]
5-HT1D 57–79 ND [73]
5-HT1E 3000 – >10,000 ND [73]
5-HT2A 6.7–39 0–52% Partial agonist / functional full agonist [77][75][73][76]
5-HT2B 0.25–0.47 Inverse agonist [73]
5-HT2C 11–197 82% Partial agonist / functional full agonist [75][73][76]
5-HT3 520–740 ND [73]
5-HT5A 960–1520 87% Near-full Agonist [73]
5-HT6 475–665 Antagonist [75][73][76]
5-HT7 6.6–14 58% Partial agonist / functional full agonist [73][76][75]
α1A 25.7 Antagonist [73][76]
α1B 35 Antagonist [73]
α2A 74.3 Antagonist [73][76]
α2B 103 ND [73][76]
α2C 38 Antagonist [73][76]
β1 141 Agonist [73]
β2 163 Agonist [73]
D1 1290–2630 Agonist [75][73]
D2 2.2–4.4 ~60% Partial agonist / functional antagonist [73]
D2 0.65–0.83 ~58% Partial agonist / functional full agonist
D3 4.3–15.1 ~40% Partial agonist / functional antagonist [75][73]
D4 417–603 ~30% Partial agonist / functional full agonist [75][73]
D5 1240–3940 Agonist [75][73]
H1 22.5–27.7 Neutral Antagonist [73][76][75]
H2 >10,000 ND [73]
H3 60–388 ND [73]
H4 >10,000 ND [73]
M1 6,780 ND [73]
M2 3,510 ND [73]
M3 4,680 ND [73][76]
M4 1,520 ND [73]
M5 2,330 ND [73]
GABAA Orthostatic
Negative allosteric modulator
NMDA
(PCP1) 		1.824 Uncompetitive channel blocker /
Antagonist 		[73]
NMDA
(PCP2) 		1.824 Uncompetitive channel blocker /
Antagonist 		[73]
Values are Ki (nM). The smaller the value, the more strongly the drug binds to the site. All data are for human cloned proteins, except 5-HT3 (rat), D4 (human/rat), H3 (guinea pig), and NMDA/PCP (rat).[73] IA = Intrinsic Activity

Aripiprazole's mechanism of action is different from those of the other FDA-approved atypical antipsychotics (e.g., clozapine, olanzapine, quetiapine, ziprasidone, and risperidone).[78][79][80][81] It shows differential engagement at the dopamine receptor (D2[73]) and acts as a partial agonist of this receptor. It is also a partial agonist of the serotonin 5-HT1A receptor. In addition, it is a weak partial agonist of the serotonin 5-HT2A, 5-HT2B, and 5-HT2C receptors.[82][83][84][85]

It appears to show predominantly partial agonistic activity on postsynaptic dopamine D2 receptors and partial agonist activity on presynaptic dopamine D2 receptors,[86] D3,[73][87][88] and partially D4[73][79] and is a partial activator of serotonin (5-HT1A,[73][89][90] 5-HT2A,[73] 5-HT2B,[73] 5-HT6, and 5-HT7).[73][81] It also shows lower effect on histamine (H1), as well as the serotonin transporter.[73][79] Aripiprazole acts by modulating neurotransmission overactivity of dopamine, which is thought to mitigate schizophrenia symptoms.[91]

As a pharmacologically unique antipsychotic with pronounced functional selectivity, characterization of this dopamine D2 partial agonist (with an intrinsic activity of ~50%)[92] as being similar to a full agonist but at a reduced level of activity presents a misleading oversimplification of its actions; for example, among other effects, aripiprazole has been shown, in vitro, to bind to and/or induce receptor conformations (i.e., facilitate receptor shapes) in such a way as to not only prevent receptor internalization (and, thus, lower receptor density) but even to lower the rate of receptor internalization below that of neurons not in the presence of agonists (including dopamine) or antagonists.[93] It is often the nature of partial agonists, including aripiprazole, to display a stabilizing effect (such as on mood in this case) with agonistic activity when there are low levels of endogenous neurotransmitters (such as dopamine) and antagonistic activity in the presence of high levels of agonists associated with events such as mania, psychosis, and drug use. In addition to aripiprazole's partial agonism and functional selectivity characteristics, its effectiveness may be mediated by its very high dopamine D2 receptor occupancy (approximately 31%, 44%, 75%, 80%, and 95% at daily dosages of 0.5 mg, 2 mg, 10 mg, 30 mg and 40 mg respectively)[94][95] Aripiprazole has been characterized as possessing predominantly partial agonist activity on postsynaptic D2 receptors and partial agonist activity on presynaptic D2 receptors;[86] however, while this explanation intuitively explains the drug's efficacy as an antipsychotic, as the degree of agonism is a function of more than a drug's inherent properties as well as in vitro demonstration of aripiprazole's partial agonism in cells expressing postsynaptic (D2L) receptors, it was noted that "It is unlikely that the differential actions of aripiprazole as an agonist, antagonist, or partial agonist were entirely due to differences in relative D2 receptor expression since aripiprazole was an antagonist in cells with the highest level of expression (4.6 pmol/mg) and a partial agonist in cells with an intermediate level of expression (0.5–1 pmol/mg). Instead, the current data are most parsimoniously explained by the "functional selectivity" hypothesis of Lawler et al. (1999)".[96] Aripiprazole is also a partial agonist of the D3 receptor.[73] In healthy human volunteers, D2 and D3 receptor occupancy levels are high, with average levels ranging between approximately 75% at 2 mg/day to approximately 95% at 40 mg/day.[87][88] Most atypical antipsychotics bind preferentially to extrastriatal receptors, but aripiprazole appears to be less preferential in this regard, as binding rates are high throughout the brain.[97]

Aripiprazole is also a partial agonist of the postsynaptic serotonin 5-HT1A receptor (intrinsic activity = 68%).[73][89][90] a PET scan study of 12 patients receiving doses ranging from 10 to 30 mg found 5-HT1A receptor occupancy to be only 16% compared to ~90% for D2.[90] It is a very weak partial agonist of the Postsynaptic 5-HT2A receptor (intrinsic activity = 12.7%).[73] The drug differs from other atypical antipsychotics in having higher affinity for the D2 receptor than for the 5-HT2A receptor.[90] At the 5-HT2B receptor, aripiprazole has both great binding affinity and acts as a potent inverse agonist, "Aripiprazole decreased PI hydrolysis from a basal level of 61% down to a low of 30% at 1000 nM, with an EC50 of 11 nM".[73] Unlike other antipsychotics, aripiprazole is a high-efficacy partial agonist of the postsynaptic 5-HT2C receptor (intrinsic activity = 82%) this property may underlie the minimal weight gain seen in the course of therapy, however if used while taking antidepressants it will become a functional antagonist and increase weight gain.[98] At the presynaptic 5-HT7 receptor, aripiprazole is a very weak partial agonist with barely measurable intrinsic activity, and hence is a functional antagonist of this receptor.[73][81] Aripiprazole also shows lower but likely clinically insignificant affinity for a number of other sites such as the serotonin transporter, while it has negligible affinity for the muscarinic acetylcholine receptors[73][79]

Since the actions of aripiprazole differ markedly across receptor systems aripiprazole was sometimes an antagonist (e.g., at 5-HT6), sometimes an inverse agonist (e.g., 5-HT2B), sometimes a partial agonist (e.g., D2S, D3S, D4S, D2L). Aripiprazole was frequently found to be a partial agonist or full agonist, with an intrinsic activity that could be low (5-HT2A, 5-HT7), intermediate (D2L, 5-HT1A), or high (5-HT2C). This mixture of agonist actions at D2-dopamine receptors is consistent with the hypothesis that aripiprazole has "functionally selective" actions.[99] The "functional-selectivity" hypothesis proposes that a mixture of agonist/partial agonist/antagonist actions are likely. According to this hypothesis, agonists may induce structural changes in receptor conformations that are differentially "sensed" by the local complement of G proteins to induce a variety of functional actions depending upon the precise cellular milieu. The diverse actions of aripiprazole at D2-dopamine receptors are clearly cell-type specific (e.g., agonism, antagonism, partial agonism), and are most parsimoniously explained by the "functional selectivity" hypothesis.[73]

Since 5-HT2C receptors have been implicated in the control of depression, obsessive–compulsive disorder (OCD), and appetite, postsynaptic partial agonism at the 5-HT2C receptor might be associated with therapeutic potential in obsessive-compulsive disorder, obesity, and depression. 5-HT2C agonism has been demonstrated to induce anorexia via enhancement of serotonergic neurotransmission via activation of postsynaptic 5-HT2C receptors; it is conceivable that the 5-HT2C partial agonist actions of aripiprazole may, thus, be partly responsible for the minimal weight gain associated with this compound in clinical trials. In terms of potential action as an antiobsessional agent, it is worthwhile noting that a variety of 5-HT2A/5-HT2C agonists have shown promise as antiobsessional agents, yet many of these compounds are hallucinogenic. Aripiprazole has a favorable pharmacological profile in being a 5-HT2C partial agonist. Based on this profile, one can predict that aripiprazole may have antiobsessional and anorectic actions in humans.[73]

Wood and Reavill's (2007) review of published and unpublished data proposed that, at therapeutically relevant doses, aripiprazole may act essentially as a selective partial agonist of the D2 receptor without significantly affecting the majority of serotonin receptors.[86] A positron emission tomography imaging study found that 10 to 30 mg/day aripiprazole resulted in 85 to 95% occupancy of the D2 receptor in various brain areas (putamen, caudate, ventral striatum) versus 54 to 60% occupancy of the 5-HT2A receptor and only 16% occupancy of the 5-HT1A receptor.[100][90] It has been suggested that the low occupancy of the 5-HT1A receptor by aripiprazole may have been an erroneous measurement however.[101]

Aripiprazole acts by modulating neurotransmission overactivity on the dopaminergic mesolimbic pathway, which is thought to be a cause of positive schizophrenia symptoms.[91] Due to its partial agonist activity on D2L receptors, aripiprazole may also increase dopaminergic activity to optimal levels in the mesocortical pathways where it is reduced.[91]

Pharmacokinetics

[edit]

Aripiprazole displays linear kinetics and has an elimination half-life of approximately 75 hours. Steady-state plasma concentrations are achieved in about 14 days. Cmax (maximum plasma concentration) is achieved 3–5 hours after oral dosing. Bioavailability of the oral tablets is about 90% and the drug undergoes extensive hepatic metabolization (dehydrogenation, hydroxylation, and N-dealkylation), principally by the enzymes CYP2D6 and CYP3A4. Its only known active metabolite is dehydro-aripiprazole, which typically accumulates to approximately 40% of the aripiprazole concentration. The parenteral drug is excreted only in traces, and its metabolites, active or not, are excreted via feces and urine.[79][7]

Pharmacokinetics of long-acting injectable antipsychotics
Medication Brand name Class Vehicle Dosage Tmax t1/2 single t1/2 multiple logPc Ref
Aripiprazole lauroxil Aristada Atypical Watera 441–1064 mg/4–8 weeks 24–35 days ? 54–57 days 7.9–10.0
Aripiprazole monohydrate Abilify Maintena Atypical Watera 300–400 mg/4 weeks 7 days ? 30–47 days 4.9–5.2
Bromperidol decanoate Impromen Decanoas Typical Sesame oil 40–300 mg/4 weeks 3–9 days ? 21–25 days 7.9 [102]
Clopentixol decanoate Sordinol Depot Typical Viscoleob 50–600 mg/1–4 weeks 4–7 days ? 19 days 9.0 [103]
Flupentixol decanoate Depixol Typical Viscoleob 10–200 mg/2–4 weeks 4–10 days 8 days 17 days 7.2–9.2 [103][104]
Fluphenazine decanoate Prolixin Decanoate Typical Sesame oil 12.5–100 mg/2–5 weeks 1–2 days 1–10 days 14–100 days 7.2–9.0 [105][106][107]
Fluphenazine enanthate Prolixin Enanthate Typical Sesame oil 12.5–100 mg/1–4 weeks 2–3 days 4 days ? 6.4–7.4 [106]
Fluspirilene Imap, Redeptin Typical Watera 2–12 mg/1 week 1–8 days 7 days ? 5.2–5.8 [108]
Haloperidol decanoate Haldol Decanoate Typical Sesame oil 20–400 mg/2–4 weeks 3–9 days 18–21 days 7.2–7.9 [109][110]
Olanzapine pamoate Zyprexa Relprevv Atypical Watera 150–405 mg/2–4 weeks 7 days ? 30 days
Oxyprothepin decanoate Meclopin Typical ? ? ? ? ? 8.5–8.7
Paliperidone palmitate Invega Sustenna Atypical Watera 39–819 mg/4–12 weeks 13–33 days 25–139 days ? 8.1–10.1
Perphenazine decanoate Trilafon Dekanoat Typical Sesame oil 50–200 mg/2–4 weeks ? ? 27 days 8.9
Perphenazine enanthate Trilafon Enanthate Typical Sesame oil 25–200 mg/2 weeks 2–3 days ? 4–7 days 6.4–7.2 [111]
Pipotiazine palmitate Piportil Longum Typical Viscoleob 25–400 mg/4 weeks 9–10 days ? 14–21 days 8.5–11.6 [104]
Pipotiazine undecylenate Piportil Medium Typical Sesame oil 100–200 mg/2 weeks ? ? ? 8.4
Risperidone Risperdal Consta Atypical Microspheres 12.5–75 mg/2 weeks 21 days ? 3–6 days
Zuclopentixol acetate Clopixol Acuphase Typical Viscoleob 50–200 mg/1–3 days 1–2 days 1–2 days 4.7–4.9
Zuclopentixol decanoate Clopixol Depot Typical Viscoleob 50–800 mg/2–4 weeks 4–9 days ? 11–21 days 7.5–9.0
Note: All by intramuscular injection. Footnotes: a = Microcrystalline or nanocrystalline aqueous suspension. b = Low-viscosity vegetable oil (specifically fractionated coconut oil with medium-chain triglycerides). c = Predicted, from PubChem and DrugBank. Sources: Main: See template.

Chemistry

[edit]

Aripiprazole belongs to the chemical class of drugs called 2,3-dichlorophenylpiperazines and is chemically related to cariprazine, nefazodone, etoperidone, and trazodone.[112][113] It is unusual in having twelve known crystalline polymorphs.[114][115]

Analogues

[edit]

Analogues of aripiprazole with higher-efficacy serotonin 5-HT2A receptor partial agonism and with psychedelic- and antidepressant-like effects have been developed.[82]

History

[edit]
Abilify (aripiprazole) 10 mg tablets (TR)

Aripiprazole was discovered in 1988 by scientists at the Japanese firm Otsuka Pharmaceutical and was called OPC-14597.[45][116][117][118][119][120] It was first published in 1995.[116][121] Otsuka initially developed the drug, and partnered with Bristol-Myers Squibb (BMS) in 1999 to complete development, obtain approvals, and market aripiprazole.[122]

It was approved by the US Food and Drug Administration (FDA) for schizophrenia in November 2002, and by the European Medicines Agency in June 2004;[123] for acute manic and mixed episodes associated with bipolar disorder on 1 October 2004; as an adjunct for major depressive disorder on 20 November 2007;[124] and to treat irritability in children with autism on 20 November 2009.[125] Likewise it was approved for use as a treatment for schizophrenia by the Therapeutic Goods Administration (TGA) of Australia in May 2003.[40]

Aripiprazole has been approved by the FDA for the treatment of both acute manic and mixed episodes, in people older than ten years.[126]

In 2006, the FDA required manufacturers to add a black box warning to the label, warning that older people who were given the drug for dementia-related psychosis were at greater risk of death.[127]

In 2007, aripiprazole was approved by the FDA for the treatment of unipolar depression when used adjunctively with an antidepressant medication.[7] That same year, BMS settled a case with the US government in which it paid $515 million; the case covered several drugs but the focus was on BMS's off-label marketing of aripiprazole for children and older people with dementia.[128]

In 2011 Otsuka and Lundbeck signed a collaboration to develop a depot formulation of aripiprazole.[129]

As of 2013, Abilify had annual sales of US$7 billion.[130] In 2013 BMS returned marketing rights to Otsuka, but kept manufacturing the drug.[131] Also in 2013, Otsuka and Lundbeck received US and European marketing approval for an injectable depot formulation of aripiprazole.[132][133]

Otsuka's US patent on aripiprazole expired on 20 October 2014, but due to a pediatric extension, a generic did not become available until 20 April 2015.[126] Barr Laboratories (now Teva Pharmaceuticals) initiated a patent challenge under the Hatch-Waxman Act in March 2007.[134] On 15 November 2010, this challenge was rejected by the U.S. District Court in New Jersey.[135]

Otsuka's European patent EP0367141 which would have expired on 26 October 2009, was extended by a Supplementary Protection Certificate (SPC) to 26 October 2014.,[136] The UK Intellectual Property Office decided[137] on 4 March 2015 that the SPC could not be further extended by six months under Regulation (EC) No 1901/2006. Even if the decision is successfully appealed, protection in Europe will not extend beyond 26 April 2015.

From April 2013 to March 2014, sales of Abilify amounted to almost $6.9 billion.[138]

In April 2015, the FDA announced the first generic versions.[139][140] In October 2015, aripiprazole lauroxil, a prodrug of aripiprazole that is administered via intramuscular injection once every four to six weeks for the treatment of schizophrenia, was approved by the FDA.[141][142]

In 2016, BMS settled cases with 42 US states that had charged BMS with off-label marketing to older people with dementia; BMS agreed to pay $19.5 million.[127][143]

In November 2017, the FDA approved Abilify Mycite, a digital pill containing a sensor intended to record when its consumer takes their medication.[144][145]

A long-acting injectable version of aripiprazole was approved by the FDA for the treatment of bipolar disorder 1 and schizophrenia in April 2023.[8][146][147]

In 2024, the European Commission approved the 2 month long-acting injectable formulation of aripiprazole for the maintenance treatment of schizophrenia.[148] This came after the 1 month long-acting injectable formulation lost drug exclusivity status in the US and Europe (the market is now open to generics).[149]

Society and culture

[edit]
[edit]
Regulatory administration (country)[150][151][152] Schizophrenia Acute mania Bipolar maintenance Major depressive disorder (as an adjunct) Irritability in autism
Food and Drug Administration (US)[7] Yes Yes Yes (as an adjunct to lithium/valproate) Yes Yes (children and adolescents)
Therapeutic Goods Administration (AU) Yes Yes (as an adjunct to lithium/valproate) Yes No No
Medicines and Healthcare products Regulatory Agency (UK) Yes Yes Yes (to prevent mania) No No
European Medicines Agency (EU)[11] Yes No Yes No No

Classification

[edit]

Aripiprazole has been described as the prototypical third-generation antipsychotic, as opposed to first-generation (typical) antipsychotics like haloperidol and second-generation (atypical) antipsychotics like clozapine.[153] It has received this classification due to its partial agonism of dopamine receptors, and is the first of its kind in this regard among antipsychotics, which before aripiprazole acted only as dopamine receptor antagonists.[153] The introduction of aripiprazole has led to a paradigm shift from a dopamine antagonist-based approach to a dopamine agonist-based approach for antipsychotic drug development.[153][118]

Brand names

[edit]

Brand names of aripiprazole include Abilify, Aristada (as aripiprazole lauroxil), Arip MT, Explemed, Abilify Maintena, Abilify Asimtufii and Arivitae, among others.[154]

Research

[edit]

Attention deficit hyperactivity disorder

[edit]

Aripiprazole was under development for the treatment of attention-deficit hyperactivity disorder (ADHD), but development for this indication was discontinued.[45] A 2017 meta review found only preliminary evidence (studies with small sample sizes and methodological problems) for aripiprazole in the treatment of ADHD.[155] A 2013 systematic review of aripiprazole for ADHD similarly reported that there is insufficient evidence of effectiveness to support aripiprazole as a treatment for the condition.[156] Although all 6 non-controlled open-label studies in the review reported effectiveness, two small randomized controlled trials found that aripiprazole did not significantly decrease ADHD symptoms.[156] A high rate of adverse effects with aripiprazole such as weight gain, sedation, and headache was noted.[156] Most research on aripiprazole for ADHD is in children and adolescents.[156][155] Evidence on aripiprazole specifically for adult ADHD appears to be limited to a single case report.[157][158]

Substance dependence

[edit]

Aripiprazole has been studied for the treatment of amphetamine dependence and other substance use disorders, but more research is needed to support aripiprazole for these potential uses.[159][160][161][162] Available evidence of aripiprazole for amphetamine dependence is mixed.[159][160][161][162] Some studies have reported attenuation of the effects of amphetamines by aripiprazole, whereas other studies have reported both enhancement of the effects of amphetamines and increased use of amphetamines by aripiprazole.[159][160][161][162] As such, aripiprazole may not only be ineffective but potentially harmful for treatment of amphetamine dependence, and caution is warranted with regard to its use for such purposes.[159][160][161][162]

References

[edit]

Further reading

[edit]
[edit]
Revisions and contributorsEdit on WikipediaRead on Wikipedia

Aripiprazole

View on Grokipedia
from Grokipedia
Aripiprazole is a third-generation medication that functions as a at D2 and serotonin 5-HT1A receptors while acting as an antagonist at 5-HT2A receptors, thereby stabilizing and serotonergic with a lower risk of extrapyramidal side effects compared to earlier antipsychotics. It is approved by the U.S. (FDA) for the treatment of in adults and adolescents aged 13 years and older, acute manic or mixed episodes associated with (as monotherapy or adjunctive therapy), irritability associated with autistic disorder in pediatric patients, and as an adjunctive treatment for in adults. Additional indications include maintenance treatment of and treatment of Tourette's disorder in pediatric patients (aged 6 to 18 years). Developed by Otsuka Pharmaceutical Co., Ltd., aripiprazole represents the first D2 receptor approved for and was initially granted FDA approval on November 15, 2002, under the brand name Abilify for oral tablet formulation. Chemically known as 7-[4-[4-(2,3-dichlorophenyl)piperazin-1-yl]butoxy]-3,4-dihydro-2(1H)-quinolinone with the molecular formula C23H27Cl2N3O2, aripiprazole is available in various formulations including oral tablets (2–30 mg), orally disintegrating tablets, oral solution, oral film, and long-acting injectable suspensions for intramuscular use (300–400 mg every 4 weeks or 720–960 mg every 2 months). Its pharmacokinetic profile features high bioavailability (87%), extensive protein binding (>99%), and a of approximately 75 hours, primarily metabolized by enzymes and CYP3A4. This unique receptor profile contributes to its efficacy in reducing positive and negative symptoms of while potentially improving cognitive function and minimizing metabolic adverse effects like and , distinguishing it from second-generation antipsychotics. Common adverse effects include , headache, , , and , with a warning for increased risk of in children, adolescents, and young adults, as well as elevated mortality in elderly patients with -related . Rare but serious risks encompass , , and seizures. Off-label applications have explored its utility in treating agitation in , , and , supported by its favorable tolerability profile in clinical studies.

Medical uses

Schizophrenia

Aripiprazole received FDA approval on November 15, 2002, for the acute and maintenance treatment of in adults. In 2007, the FDA extended approval to adolescents aged 13-17 years for the same indications, based on clinical trials demonstrating and in this population. This is indicated for managing both positive and negative symptoms of through its activity at D2 receptors, which stabilizes . The recommended starting dose for adults is 10-15 mg orally once daily, with to a target of 15 mg/day and a maximum of 30 mg/day based on clinical response. Pivotal randomized, double-blind trials, such as the 2002 study by Kane et al., involved over 400 patients with acute and showed that aripiprazole at 15-30 mg/day produced significantly greater reductions in (PANSS) total scores compared to (mean change -17.4 vs. -7.2 at week 4; p<0.01), with improvements in both positive and negative symptom subscales. These findings established aripiprazole's superiority over in short-term symptom control, supporting its role in acute treatment. For maintenance therapy, aripiprazole 15 mg/day has demonstrated efficacy in preventing relapse in stabilized patients with chronic schizophrenia, as shown in a 26-week placebo-controlled trial where only 23% of aripiprazole-treated patients experienced relapse versus 57% on placebo (p<0.001), with sustained PANSS improvements. Long-term observational studies further indicate reduced hospitalization rates, with one analysis of over 1,000 patients switched to aripiprazole showing a 30% decrease in psychiatric hospitalizations over 12 months compared to prior oral antipsychotics. In first-episode schizophrenia, aripiprazole exhibits comparable overall efficacy to risperidone, as evidenced by a 52-week randomized trial in 198 patients where both drugs reduced PANSS scores similarly (approximately 50% improvement at 6 months), though aripiprazole showed advantages in negative symptom reduction. This supports its use as a first-line option in early-phase illness, potentially aiding long-term functional outcomes.

Bipolar disorder

Aripiprazole received FDA approval in September 2004 for the acute treatment of manic or mixed episodes associated with in adults. In February 2008, the FDA extended approval to include adolescents aged 10 to 17 years for the same indication, based on a 4-week placebo-controlled trial demonstrating significant improvements in manic symptoms. For maintenance therapy, oral aripiprazole was approved in March 2005 as monotherapy to prevent relapse in adults with following stabilization from an acute manic or mixed episode. In April 2023, the FDA approved Abilify Asimtufii, an extended-release injectable formulation administered every two months, for maintenance monotherapy in adults with , supported by data from a 52-week randomized withdrawal study showing delayed time to mood episode recurrence compared to placebo. For acute treatment of manic or mixed episodes, the recommended starting dose of oral aripiprazole is 15 mg once daily, which may be titrated to a target of 15 to 30 mg per day based on clinical response, with effects observed as early as day 2 and significant improvements in Young Mania Rating Scale (YMRS) total scores by week 1 in randomized, placebo-controlled trials. In three-week, double-blind studies involving adults with bipolar I disorder, aripiprazole at 15 or 30 mg/day led to mean YMRS reductions of approximately 8 to 10 points greater than placebo, with response rates (≥50% YMRS improvement) reaching 53% versus 30% for placebo. Similar efficacy was observed in pediatric patients aged 10 to 17, where both 10 mg and 30 mg doses significantly outperformed placebo on YMRS scores starting at week 1, with endpoint improvements of 20 to 23 points versus 11 points for placebo. In maintenance treatment, aripiprazole monotherapy at 15 to 30 mg/day has demonstrated superiority over placebo in preventing relapse, particularly manic recurrences, in a 26-week randomized, double-blind trial of recently manic patients with bipolar I disorder, where it delayed time to relapse (hazard ratio 0.59) and reduced the risk of manic episodes by about 50% compared to placebo. Over longer periods, such as 100 weeks, aripiprazole continued to show significant delays in manic relapse versus placebo (hazard ratio 0.35), though effects on depressive relapse were not significant. Compared to lithium, aripiprazole exhibited equivalent efficacy in preventing mood episode recurrences over 52 weeks in a double-blind study, with both reducing manic relapses by approximately 40% relative to baseline risk. This mood-stabilizing effect is attributed to aripiprazole's partial agonism at dopamine D2 receptors, which modulates dopaminergic activity without full blockade.

Major depressive disorder

Aripiprazole was approved by the U.S. Food and Drug Administration in 2007 as an adjunctive therapy to antidepressants for the treatment of major depressive disorder (MDD) in adults who have an inadequate response to antidepressant monotherapy. This approval was based on evidence from short-term, placebo-controlled trials demonstrating its ability to enhance antidepressant effects in treatment-resistant cases. In clinical practice, aripiprazole is typically added at doses of 2 to 15 mg per day to an existing antidepressant regimen, with a target dose of 5 to 10 mg/day and gradual titration to minimize side effects. Meta-analyses of randomized controlled trials have shown that this augmentation strategy yields significantly greater response rates compared to placebo, with relative risks around 1.5 and absolute improvements in response of approximately 12% to 15%, translating to number needed to treat values of 6 to 9 for response. Aripiprazole's partial agonism at serotonin 5-HT1A receptors may contribute to enhancing the antidepressant effects through modulation of serotonergic transmission. Key evidence comes from pivotal trials such as CN138-139 and CN138-163, which involved adults with MDD showing minimal improvement on antidepressants; these studies reported greater reductions in Montgomery-Åsberg Depression Rating Scale (MADRS) total scores with adjunctive aripiprazole (mean changes of -8.8 to -10.7 points) versus placebo (-6.1 to -7.6 points) over 6 weeks, alongside response rates of about 37% versus 23%. Similar findings were observed in the VAST-D trial, where aripiprazole augmentation led to higher remission rates (29%) compared to switching antidepressants (22%), without elevating the risk of manic symptoms beyond placebo levels (incidence <1% in both groups). These trials underscore improvements in core depressive symptoms while maintaining a low incidence of treatment-emergent mania. Aripiprazole is not approved for monotherapy in MDD due to insufficient evidence of efficacy in that context and the established benefits of combination therapy. Additionally, its use is limited by the potential for akathisia, which occurs in up to 25% of patients at higher doses and may lead to discontinuation.

Autism spectrum disorder

Aripiprazole is approved by the U.S. Food and Drug Administration for the treatment of irritability associated with autistic disorder in pediatric patients aged 6 to 17 years, based on data from two 8-week, randomized, double-blind, placebo-controlled trials. This approval, granted in November 2009, targets behavioral symptoms rather than the underlying neurodevelopmental condition. In clinical trials, aripiprazole was administered at doses of 2 to 15 mg per day, with titration starting at 2 mg/day and flexible dosing in one study (mean dose 8.2 mg/day) and fixed dosing (5, 10, or 15 mg/day) in another. Both studies used the Aberrant Behavior Checklist-Irritability (ABC-I) subscale as the primary efficacy measure, showing significant reductions in scores for aripiprazole compared to placebo (mean changes of -12.4 vs. -5.0 in the flexible-dose trial and -8.2 to -9.5 vs. -5.0 in fixed-dose groups). Response rates, defined as at least a 25% reduction in ABC-I score combined with a Clinical Global Impressions-Improvement score of much improved or very much improved, reached 52% with aripiprazole versus 14% with placebo in the flexible-dose study (Owen et al., 2009), and 49% to 56% versus 35% in fixed-dose arms (Marcus et al., 2009). The medication primarily addresses irritability-related behaviors, including aggression toward caregivers or others, deliberate self-injurious acts, and severe tantrums, as evidenced by improvements in these specific ABC-I items. It does not demonstrate efficacy against core autism spectrum disorder features, such as impairments in social communication or restricted/repetitive patterns of behavior. Aripiprazole's partial agonism at dopamine D2 receptors contributes to its stabilizing effect on hyperactivity and irritability in this population. For long-term use, a 52-week open-label extension study involving responders from the initial trials reported sustained improvements in irritability but highlighted the need for monitoring weight gain, with mean increases of 5.8 kg overall (higher in younger children at 7.2 kg for ages 6-11 versus 4.5 kg for 12-17). Clinicians should regularly assess growth parameters and metabolic changes in pediatric patients due to this risk.

Tourette syndrome and tic disorders

In 2014, the U.S. Food and Drug Administration (FDA) approved aripiprazole for the treatment of Tourette's disorder in pediatric patients aged 6 to 18 years, based on evidence from short-term clinical trials demonstrating tic reduction. The recommended starting dose is 2 mg per day, with gradual titration to a target of 5 to 10 mg per day depending on body weight (5 mg for patients under 50 kg and 10 mg for those 50 kg or more), and a maximum of 20 mg per day; dosing adjustments are made in 5 mg increments at intervals of no less than one week to optimize tic control while monitoring tolerability. Clinical studies, including open-label and randomized controlled trials, have shown aripiprazole's efficacy in reducing tic severity, with typical reductions of 40% to 60% in Yale Global Tic Severity Scale (YGTSS) total tic scores over 8 to 10 weeks. For instance, an open-label study by Yoo et al. reported a 52.8% mean reduction in YGTSS scores among 24 children and adolescents treated with doses averaging 11.7 mg per day, while a multicenter randomized trial by the same group in 61 patients demonstrated a 15-point absolute reduction (approximately 35% to 50% relative to baseline) compared to placebo. These improvements were observed in short- and medium-term durations, up to 10 weeks, supporting its role in managing chronic tic disorders. Compared to traditional antipsychotics like haloperidol, aripiprazole offers similar tic suppression (e.g., 54.3% YGTSS reduction versus 63.4% for haloperidol) but with a more favorable tolerability profile, including lower rates of extrapyramidal side effects such as dystonia and parkinsonism. Evidence from these trials indicates robust effects on both motor and vocal (phonic) tics, with some studies showing greater proportional reductions in vocal tics (up to 67%). Aripiprazole's mechanism involves partial agonism at dopamine D2 receptors, which stabilizes hyperdopaminergic activity in basal ganglia pathways implicated in tic generation.

Obsessive-compulsive disorder

Aripiprazole is used off-label as an adjunctive therapy to selective serotonin reuptake inhibitors (SSRIs) or serotonin-norepinephrine reuptake inhibitors (SNRIs) in patients with treatment-resistant obsessive-compulsive disorder (OCD). This approach targets individuals who have not achieved adequate symptom relief after adequate trials of first-line treatments, with evidence indicating moderate to large improvements in obsessive-compulsive symptoms. A meta-analysis of double-blind, randomized, placebo-controlled trials demonstrated that aripiprazole augmentation significantly reduces Yale-Brown Obsessive Compulsive Scale (Y-BOCS) scores, with a Hedges' g effect size of -1.35 (95% CI: -2.02 to -0.68), reflecting a large therapeutic benefit compared to placebo. Typical dosing for aripiprazole in this context ranges from 5 to 15 mg per day, added to ongoing regimens such as clomipramine or fluoxetine, with titration based on response and tolerability. Response rates, defined as at least a 35% reduction in Y-BOCS scores, reach up to 30% among non-responders to prior therapies, though rates vary across studies due to differences in patient severity and trial duration. Small randomized controlled trials (RCTs) have shown benefits for both obsessions and compulsions, particularly in severe cases, with significant Y-BOCS reductions observed after 8-12 weeks of augmentation. For instance, one pilot RCT reported a mean Y-BOCS decrease of 9.7 points in refractory patients, alongside improvements in global functioning. Aripiprazole's partial agonism at dopamine D2 receptors and antagonism at 5-HT2A receptors may contribute to enhancing SSRI effects in OCD by modulating serotonergic and dopaminergic pathways. However, it lacks approval for monotherapy in OCD due to insufficient evidence from large-scale trials, with available data limited to small open-label studies showing preliminary promise but not establishing efficacy or safety robustly. Current guidelines emphasize its role strictly as augmentation, with monitoring for metabolic side effects during use.

Dosage forms and administration

Aripiprazole is available in several oral formulations to accommodate different patient needs and preferences. Oral tablets are supplied in strengths of 2 mg, 5 mg, 10 mg, 15 mg, 20 mg, and 30 mg, and may be administered once daily with or without food. Orally disintegrating tablets, designed for rapid dissolution on the tongue without water, are available in 10 mg and 15 mg strengths. An oral solution formulation at a concentration of 1 mg/mL allows for flexible dosing, particularly for patients who have difficulty swallowing tablets. Oral soluble films, which dissolve on or under the tongue without water, are available in 2 mg, 5 mg, and 10 mg strengths, with approvals including Opipza in July 2024 and Mezofy in April 2025 for the treatment of and other approved indications. For acute management, a short-acting intramuscular injection is available as a 7.5 mg/mL solution in a 9.75 mg/1.3 mL single-dose vial, administered via deep intramuscular injection into the deltoid or gluteal muscle. This formulation achieves rapid absorption, with peak plasma concentrations occurring within 1 to 3 hours. Long-acting injectable formulations provide options for maintenance therapy with extended dosing intervals. Abilify Maintena, an extended-release intramuscular suspension, is available in 300 mg and 400 mg strengths for monthly administration (every 26 days or longer) into the deltoid or gluteal muscle by a healthcare professional. Initiation requires establishing tolerability with oral aripiprazole, followed by 10 to 20 mg oral aripiprazole or the patient's current oral antipsychotic for 14 consecutive days after the first injection to ensure adequate plasma levels. Abilify Asimtufii, another extended-release intramuscular suspension approved by the FDA in 2023, is supplied in 720 mg and 960 mg pre-filled syringes for administration every 2 months (56 days) exclusively into the gluteal muscle. Similar to Maintena, initiation involves oral overlap for 14 days post-first injection. Aristada, a prodrug formulation of aripiprazole lauroxil, offers extended-release injectable suspensions in 441 mg, 662 mg, and 882 mg doses for monthly administration, or 882 mg every 6 or 8 weeks, via intramuscular injection into the deltoid (441 mg only) or gluteal muscle. Aristada Initio, a 675 mg single-dose initiation kit, is used with the first Aristada dose and a 30 mg oral aripiprazole tablet on the same day or up to 10 days later. Dosing adjustments are recommended for patients identified as CYP2D6 poor metabolizers, who exhibit approximately twice the plasma exposure of extensive metabolizers; in such cases, the oral dose or equivalent injectable dose should be reduced by 50%. This adjustment accounts for the pharmacokinetic profile where CYP2D6 contributes significantly to metabolism. In the European Union, a 960 mg two-month formulation of Abilify Maintena was approved in March 2024 for maintenance treatment of schizophrenia in adults previously stabilized on .

Safety profile

Contraindications

Aripiprazole is contraindicated in patients with a known hypersensitivity to the drug or any of its excipients, as reactions can range from pruritus and urticaria to anaphylaxis.

Warnings and precautions

Aripiprazole carries a black box warning for increased mortality in elderly patients with dementia-related psychosis, with studies showing a 1.6- to 1.7-fold higher risk of death compared to placebo, primarily due to cerebrovascular adverse events such as stroke; the drug is not approved for this indication. Another black box warning highlights the increased risk of suicidal thoughts and behaviors in children, adolescents, and young adults when aripiprazole is used as an adjunct to antidepressants for major depressive disorder, necessitating close monitoring, especially during initial treatment phases. Caution is advised when initiating aripiprazole in patients with known cardiovascular disease, including histories of myocardial infarction, ischemic heart disease, heart failure, or conduction abnormalities, due to the potential for orthostatic hypotension and, rarely, QT interval prolongation. Caution is advised in patients with untreated narrow-angle glaucoma due to rare case reports of acute angle-closure glaucoma potentially linked to pupillary dilation effects. No dosage adjustment is required for patients with severe hepatic impairment, but monitoring for potential liver function abnormalities is recommended.

Adverse effects

Aripiprazole is associated with a range of adverse effects, the most common of which occur during ongoing treatment and are generally mild to moderate in severity. In placebo-controlled clinical trials for adults with schizophrenia or bipolar mania, adverse effects reported in more than 10% of patients included akathisia (incidence 10-13%), headache (24-27%), nausea (11-15%), and insomnia (12-24%). Weight gain is also common, with mean increases of approximately 0.7-2.5 kg (1.5-5.5 lbs) observed in short-term trials and up to 2.1 kg (4.6 lbs) in longer-term maintenance studies for schizophrenia. Serious adverse effects are less frequent but can be severe. Neuroleptic malignant syndrome (NMS), a potentially life-threatening condition characterized by hyperpyrexia, muscle rigidity, and altered mental status, has been reported rarely with an estimated incidence below 0.1%. Tardive dyskinesia (TD), involving involuntary movements, is dose- and duration-dependent, with risks increasing after prolonged use, though aripiprazole's partial agonist profile at dopamine D2 receptors may confer a lower overall incidence compared to typical antipsychotics. Impulse control disorders, such as pathological gambling, compulsive shopping, binge eating, or hypersexuality, have been identified in postmarketing reports, prompting an FDA warning in 2016; these disorders are rare, with the FDA identifying 184 cases associated with aripiprazole use from 2002 to 2016, and typically resolve within days to weeks upon dose reduction or discontinuation. Metabolic changes represent another category of concern, including hyperglycemia and dyslipidemia, which may contribute to increased risk of diabetes or cardiovascular events. In clinical trials, shifts from normal to high fasting glucose occurred in about 3.8% of adults on aripiprazole, with similar patterns for lipid elevations. Extrapyramidal symptoms (EPS), such as parkinsonism or dystonia, occur at lower rates with aripiprazole (3-12% excluding ) than with typical antipsychotics (20-30%), attributable in part to its dopamine partial agonism. Aripiprazole has no potential for abuse, does not produce euphoria or reinforcing psychoactive effects, and lacks recreational value or street market presence, as evidenced by clinical and epidemiological data. In pediatric populations, adverse effects tend to be more pronounced. Clinical trials for schizophrenia in adolescents (13-17 years) reported somnolence in up to 24% and EPS in 18-25% of patients, higher than adult rates; similar elevations were noted in trials for bipolar mania and irritability associated with autism spectrum disorder. Weight gain in youth averaged 1.6-2.1 kg (3.5-4.6 lbs) over 4-6 weeks, underscoring the need for monitoring in this group.

Discontinuation effects

Discontinuation of can lead to withdrawal symptoms such as insomnia, nausea, anxiety, dizziness, lightheadedness, tremor, and irritability. These symptoms often emerge within 1 to 4 days of cessation and typically resolve within 1 to 2 weeks. The long elimination half-life of , approximately 75 hours, contributes to generally milder withdrawal effects compared to medications with shorter half-lives, such as selective serotonin reuptake inhibitors. Abrupt discontinuation poses a risk of rebound psychosis or mania, particularly in patients treated for schizophrenia or bipolar disorder. To mitigate these risks, clinical guidelines recommend gradual tapering, typically reducing the dose by 10% to 25% every 1 to 2 weeks over 1 to 4 weeks, with adjustments based on individual response; for example, decrements of 5 mg per week may be used for oral formulations. For long-acting injectable formulations, tapering involves prolonging inter-dose intervals or switching to oral equivalents, with close monitoring for relapse recommended for 3 to 6 months after the last dose. Observational studies on atypical antipsychotics, including , indicate that withdrawal symptoms occur in approximately 53% of cases with abrupt discontinuation, but rates are substantially lower—often mild and affecting 20% to 30% of patients—with proper gradual tapering.

Overdose and management

Symptoms and risks

Acute overdose of aripiprazole typically presents with central nervous system depression, manifesting primarily as somnolence in up to 63% of single-substance cases reported to poison centers. Other common symptoms include tremor, extrapyramidal symptoms (EPS) such as dystonia and akathisia, and tachycardia; in isolated overdoses, tachycardia occurs in approximately 39% of cases, while EPS such as dystonia are less common (around 5%). Nausea, vomiting (18%), and dizziness (36%) may also occur. Seizures and coma are rare but have been documented in pediatric cases at doses well below 100 times the therapeutic range, such as seizures after ~30 mg in a 3-year-old and coma after 195 mg in a toddler, often in the context of massive relative ingestions. Risk factors for severe outcomes include polypharmacy involving central nervous system depressants, which can exacerbate sedation and respiratory compromise. Pediatric overdoses pose a heightened risk of severity due to lower body weight, leading to higher relative exposures even at smaller absolute doses; for instance, ingestions as low as 10-195 mg in toddlers have resulted in prolonged lethargy and EPS. Aripiprazole exhibits low lethality, with an LD50 exceeding 700 mg/kg in rats following oral administration. Human case reports document recovery after ingestions up to 1080 mg without fatalities, and a 2024 retrospective cohort study of cases from 2013-2023 confirmed no fatalities in 44 isolated overdoses despite doses up to 450 mg, with all patients achieving full recovery. In monitoring overdose patients, electrocardiography is recommended to assess for QT prolongation (reported in 36% of isolated cases), though the risk remains minimal compared to other antipsychotics. Vital signs should be closely observed for hypotension, which occurs infrequently but can contribute to hemodynamic instability.

Treatment approaches

Management of aripiprazole overdose primarily involves supportive and symptomatic care, as no specific antidote exists. Decontamination measures are recommended only if ingestion occurred recently. Activated charcoal (50 g for adults or 1 g/kg for children) should be administered if the patient presents within 1-2 hours of ingestion, as it can reduce absorption by approximately 50%. Routine gastric lavage is not advised due to the drug's relatively low toxicity profile and the risks associated with the procedure. Supportive measures form the cornerstone of treatment, focusing on maintaining vital functions and addressing complications. Patients should receive continuous monitoring of vital signs, cardiac rhythm, and neurologic status, with admission to an intensive care unit (ICU) recommended for severe cases involving significant sedation, hemodynamic instability, or extrapyramidal symptoms (EPS). Hypotension, if present, typically responds to intravenous (IV) fluid boluses; vasopressors such as norepinephrine may be used if fluids are insufficient. Agitation or EPS, such as dystonia or tremors, can be managed with benzodiazepines (e.g., lorazepam or midazolam) or anticholinergics like benztropine (1-2 mg IV) or biperiden (2-5 mg IV). Flumazenil should be avoided, as it may precipitate seizures in the context of antipsychotic overdose. Enhanced elimination techniques, including hemodialysis, are ineffective due to aripiprazole's high protein binding (>99%) and large (4.9 L/kg). Most patients recover fully within 24-48 hours with appropriate supportive care, even after substantial ingestions (up to 1260 mg reported with no fatalities). However, with long-acting injectable formulations like or Abilify Maintena, effects may persist for weeks due to slow release from the injection site, necessitating prolonged monitoring potentially up to several weeks.

Drug interactions

Pharmacokinetic interactions

Aripiprazole undergoes extensive hepatic metabolism primarily via the cytochrome P450 enzymes CYP3A4 and CYP2D6, making it susceptible to pharmacokinetic interactions with drugs that induce or inhibit these enzymes. Strong inducers of CYP3A4, such as carbamazepine, accelerate aripiprazole metabolism, reducing its plasma concentrations by up to 70% and necessitating a dosage increase to approximately double the usual amount, typically up to 30-40 mg/day, to maintain therapeutic levels. Strong inhibitors of CYP3A4, such as ketoconazole or itraconazole, significantly increase aripiprazole exposure, requiring the dose to be halved (to approximately 5-10 mg/day). Conversely, strong inhibitors of CYP2D6, such as fluoxetine or paroxetine, impair aripiprazole clearance, elevating its exposure by approximately 110-140%, which requires halving the dose to 5-10 mg/day to avoid toxicity. When both a strong CYP3A4 and CYP2D6 inhibitor are coadministered, the dose should be reduced to one-quarter of the usual amount. Individuals with poor metabolizer phenotypes, occurring in 7-10% of Caucasians, exhibit approximately 80% higher aripiprazole exposure compared to extensive metabolizers due to reduced enzymatic activity, increasing the risk of adverse effects. Dosage adjustments, such as halving the standard dose, are recommended for known poor metabolizers, and pharmacogenetic testing for is advised in clinical guidelines like those from the Clinical Pharmacogenetics Implementation Consortium (CPIC) to guide personalized dosing. Food has minimal impact on aripiprazole's absorption; administration with a high-fat slightly increases C_max and AUC by less than 20% but does not warrant dosage adjustments, allowing intake with or without meals. Aripiprazole is highly bound to plasma proteins (approximately 99% to ), and while protein displacement interactions are rare, coadministration with highly protein-bound drugs like may require monitoring of effects due to isolated reports of elevated INR.

Pharmacodynamic interactions

Aripiprazole, acting as a at D2 receptors, can engage in pharmacodynamic interactions with other drugs that modulate similar systems, potentially leading to additive or antagonistic effects at the receptor level. Concomitant use of aripiprazole with (CNS) depressants, such as alcohol or benzodiazepines, may result in additive CNS depression, increasing the risk of , , and impaired psychomotor performance. For instance, alcohol can exacerbate the sedative effects of aripiprazole, and caution is advised to avoid concurrent consumption. Similarly, when aripiprazole is administered with parenteral benzodiazepines like , there is an elevated risk of excessive and , necessitating close monitoring of patients for these effects. Aripiprazole's antagonism at alpha-1 adrenergic receptors can potentiate the hypotensive effects of antihypertensives, such as beta-blockers or , leading to enhanced risk of . This interaction arises from overlapping mechanisms that impair vascular tone, and monitoring is recommended in patients on combined therapy. Co-administration of aripiprazole with agents may mask (EPS) induced by the , as anticholinergics like benztropine counteract blockade-related motor effects. However, this combination can also heighten the risk of side effects, including , due to the additive burden on gastrointestinal motility. Regarding cardiac effects, aripiprazole has a low propensity for prolongation, with clinical studies showing minimal changes (less than 10 ms on average). Nonetheless, when combined with other QT-prolonging drugs, such as , there is a cumulative risk of or other arrhythmias, warranting electrocardiographic monitoring in at-risk patients.

Pharmacology

Pharmacodynamics

Aripiprazole acts primarily as a partial agonist at D₂ and D₃ receptors (Ki values of 0.34 nM and 0.8 nM, respectively) and at the serotonin 5-HT₁A receptor (Ki = 1.7 nM), while functioning as an at the 5-HT₂A receptor (Ki = 3.4 nM). This receptor binding profile distinguishes aripiprazole from traditional antipsychotics, which are typically full antagonists at D₂ receptors, by allowing it to modulate and serotonergic in a context-dependent manner. The high affinity for these receptors enables aripiprazole to exert stabilizing effects on signaling, acting as an agonist in regions of low dopamine activity and as an antagonist in areas of high dopamine activity, such as the in or hypodopaminergic states associated with depression. This dopamine-stabilizing property arises from aripiprazole's partial agonism at D₂ receptors, where it exhibits an intrinsic activity of approximately 30-40%, meaning it activates the receptor to a lesser extent than full agonists like itself but more than pure antagonists. In hypodopaminergic conditions, such as those in the during depressive states, aripiprazole enhances transmission to restore balance; conversely, in hyperdopaminergic states like , it dampens excessive signaling to reduce symptoms. This functional selectivity at D₂ receptors contributes to a lower incidence of extrapyramidal side effects (EPS) compared to full D₂ antagonists, as it avoids complete blockade of pathways essential for . Downstream, aripiprazole's actions extend to modulation of (PFC) activity through enhanced and serotonin release in this region, mediated partly by its 5-HT₁A agonism and 5-HT₂A antagonism. This neurochemical stabilization in the PFC, along with effects in the and , underpins its therapeutic efficacy across a range of psychiatric disorders by improving executive function and emotional regulation without the typical disruptions seen with other antipsychotics. Furthermore, like other antipsychotics such as clozapine and haloperidol, aripiprazole reduces selective long-range correlations between deep layer 5 cortical neurons, an effect independent of dopaminergic profiles; this may correct excess synchrony or aberrant predictive signals in psychosis, restoring balance in the predictive hierarchy, where superficial layers transmit bottom-up prediction errors and deep layers convey top-down predictions.

Pharmacokinetics

Aripiprazole exhibits favorable absorption characteristics following , with an absolute of approximately 87% for the tablet formulation. Peak plasma concentrations (T_max) are typically achieved within 3 to 5 hours after dosing. The of aripiprazole are linear and dose-proportional over the therapeutic range with once-daily administration. Steady-state plasma concentrations are reached after about 14 days, reflecting the elimination of approximately 75 hours for the parent compound and 94 hours for its , dehydro-aripiprazole. Aripiprazole is extensively distributed throughout the body, with a steady-state volume of distribution of 4.9 L/kg following intravenous administration. The drug is highly bound to plasma proteins, with more than 99% binding, primarily to albumin. Metabolism occurs predominantly in the liver via cytochrome P450 enzymes, with CYP3A4 and CYP2D6 playing key roles in dehydrogenation, hydroxylation, and N-dealkylation pathways. The primary active metabolite, dehydro-aripiprazole, accounts for about 40% of the parent drug's area under the curve (AUC) and retains approximately 40% of its pharmacological activity. Elimination of aripiprazole and its metabolites is primarily fecal, with approximately 55% of the dose recovered in feces and 25% in urine; less than 1% is excreted unchanged in the urine. No dosage adjustments are necessary for patients with mild to moderate renal or hepatic impairment.

Chemistry

Chemical structure and properties

Aripiprazole has the empirical formula C23_{23}H27_{27}Cl2_{2}N3_{3}O2_{2} and a molecular weight of 448.4 g/mol. It is classified as an atypical antipsychotic in the quinolinone class, characterized by a 3,4-dihydroquinolin-2(1H)-one core linked through a butoxy chain to a piperazine ring substituted with a 2,3-dichlorophenyl group at the 4-position. The molecular structure imparts significant to aripiprazole, with a calculated logP value of 4.5, which influences its distribution and . Physically, it appears as a to off-white crystalline powder and exhibits low aqueous , being practically insoluble in (less than 0.3 µg/mL) but slightly soluble in organic solvents such as . serves as a close to aripiprazole, sharing the quinolinone-piperazine framework but incorporating a ring modification that enhances its affinity for the 5-HT1A_{1A} receptor. Aripiprazole is often categorized as a third-generation , distinguished by its partial agonism at D2_{2} receptors rather than full antagonism.

Synthesis and manufacturing

Aripiprazole is synthesized through a multi-step process originally developed by , beginning with 7-hydroxy-3,4-dihydro-2(1H)-quinolinone as the key starting material. The initial step involves O-alkylation of the phenolic hydroxy group with 1,4-dibromobutane (3 molar equivalents) in the presence of (1 molar equivalent) in N,N-dimethylformamide at 60°C for 4 hours, yielding the intermediate 7-(4-bromobutoxy)-3,4-dihydro-2(1H)-quinolinone after extraction with and recrystallization from . This intermediate is then treated with (2 molar equivalents) in under reflux for 30 minutes, followed by addition of 1-(2,3-dichlorophenyl) (1.5 molar equivalents) and triethylamine (2 molar equivalents), and further reflux for 4 hours to facilitate and form aripiprazole , which is purified by filtration, evaporation, extraction with , and recrystallization from . On an industrial scale, the process is multi-step and optimized for efficiency, achieving an overall yield of approximately 70-75%. Manufacturing adheres to (GMP) standards to ensure product quality and consistency. Impurity control is critical, with related substances limited to less than 0.1% in accordance with International Council for Harmonisation (ICH) Q3A(R2) guidelines for new drug substances. Genotoxic impurities arising from synthesis are monitored and reduced to acceptable levels through process controls and purification steps. The foundational patent for this synthesis, US Patent 5,006,528 issued to Otsuka in 1991, expired in 2014, facilitating the entry of generic manufacturers using similar or improved variants of the process.

History

Development and discovery

Aripiprazole was discovered by Otsuka Pharmaceutical in Japan during the 1980s as part of efforts to develop novel antipsychotics targeting schizophrenia, with the compound initially synthesized in 1988 under the code name OPC-31. This synthesis marked a significant milestone in the company's research on dopamine-modulating agents, building on earlier work with autoreceptor agonists like OPC-4392 from 1980. Key innovators at Otsuka drove the design of aripiprazole as a at dopamine D2 and serotonin 5-HT1A receptors, aiming to stabilize without the full receptor blockade associated with traditional antipsychotics, thereby reducing side effects like (EPS). This rationale emerged from observations that full D2 antagonists often exacerbated negative symptoms and motor issues in patients. In preclinical studies during the late and early , aripiprazole demonstrated balanced at presynaptic D2 autoreceptors and antagonism at postsynaptic sites in animal models, alongside strong 5-HT1A partial that contributed to its antidepressant-like effects. Notably, it exhibited low in and models, indicating reduced EPS liability compared to typical antipsychotics, while effectively inhibiting apomorphine-induced behaviors and synthesis . Phase I and II clinical trials in the confirmed aripiprazole's favorable safety profile, including minimal sedation and metabolic effects, in healthy volunteers and patients with . These early studies established preliminary efficacy against positive symptoms and paved the way for the (NDA) filing in in 1995.

Regulatory approvals and milestones

Aripiprazole, marketed under the brand name Abilify, received its initial approval from Japan's Ministry of Health, Labour and Welfare on January 17, 2006, for the treatment of in adults. It received its initial approval from the U.S. (FDA) on November 15, 2002, for the treatment of in adults. Subsequent expansions included approval on September 20, 2004, for the acute treatment of manic or mixed episodes associated with in adults, as monotherapy or adjunctive therapy with or . In 2007, the FDA approved aripiprazole as an adjunctive treatment to antidepressants for in adults. Further approvals came on November 20, 2009, for associated with autistic disorder in pediatric patients aged 6 to 17 years, and on December 12, 2014, for Tourette's disorder in pediatric patients aged 6 to 18 years. In the , the (EMA) granted marketing authorization for aripiprazole on June 4, 2004, initially for the treatment of in adults and for the prevention of relapse in patients with previously stabilized . Key expansions followed, including approval for moderate to severe manic episodes in in adolescents aged 13 to 17 years on February 6, 2013. The long-acting injectable formulation, Abilify Maintena, was approved by the EMA on November 15, 2013, for maintenance treatment of in adults. On March 27, 2024, the approved a once-every-two-months dosing regimen (720 mg or 960 mg) for Abilify Maintena in the maintenance treatment of in adults previously stabilized on oral aripiprazole. The FDA approved Abilify Maintena on February 28, 2013, for the maintenance treatment of in adults. This was followed by approval of Abilify Asimtufii, a ready-to-use extended-release injectable suspension, on April 27, 2023, for the treatment of in adults and maintenance monotherapy treatment of in adults. On April 15, 2025, the FDA approved Mezofy (aripiprazole oral soluble film) for the treatment of in adults. The primary U.S. patent for oral aripiprazole (U.S. Patent No. 5,006,528) expired on April 20, 2015, allowing generic entry; the first generic versions were approved by the FDA on , 2015. In a notable regulatory controversy, Bristol-Myers Squibb, a former marketing partner for Abilify, agreed to a $19.5 million settlement in December 2016 with 43 U.S. states and the District of Columbia over allegations of improper promotion of the drug for unapproved pediatric uses, including off-label marketing to children for conditions beyond FDA-approved indications.

Society and culture

Aripiprazole is classified as a prescription-only (Rx) worldwide, requiring a physician's prescription for dispensing in all major regulatory jurisdictions. In , it falls under of the Drugs and Cosmetics Rules, 1945, mandating sale only on the prescription of a registered medical practitioner, with specific requirements for record-keeping by pharmacists. In the , it is designated as a Prescription Only (POM) under the Human Medicines Regulations 2012, restricting supply to authorized prescriptions from qualified healthcare professionals. Aripiprazole is not controlled under the (1961), the (1971), or the United Nations Convention Against Illicit Traffic in Narcotic Drugs and Psychotropic Substances (1988). In the United States, the (DEA) does not schedule it, reflecting its lack of established abuse potential; clinical evaluations indicate it has not been systematically associated with tolerance, , or significant misuse risk. Pediatric approvals for aripiprazole vary by region and indication. In the , it is authorized for treatment in adolescents aged 15 years and older, with restrictions prohibiting use in those under 15 years for this condition due to insufficient and data in younger children. Post-marketing in the EU includes monitoring for suicidality, as the product information highlights an inherent risk in psychotic and mood disorders, with requirements for close observation of adolescents and young adults for worsening depression or emergence of suicidal thoughts. In the US, the approves it for in adolescents aged 13 to 17 years, accompanied by a black box warning for increased suicidality risk in pediatric patients based on pooled data. Recent regulatory developments in the have expanded generic availability of aripiprazole since the mid-2010s, following expiry, with multiple authorizations granted in the for bioequivalent versions such as Aripiprazole , Aripiprazole Accord, and Aripiprazole , enhancing access while maintaining the prescription-only status. In March 2024, the approved Abilify Maintena 960 mg, a once-every-two-months long-acting injectable formulation for maintenance treatment of in adults.

Brand names and economics

Aripiprazole is primarily marketed under the brand name Abilify by Otsuka Pharmaceutical Co., Ltd., in collaboration with Bristol-Myers Squibb for certain regions. Extended-release injectable formulations include Abilify Maintena and Abilify Asimtufii, also from Otsuka, while Aristada (aripiprazole lauroxil) is marketed by Alkermes plc. These brands target schizophrenia and bipolar I disorder maintenance therapy. Abilify reached peak global sales of over $7 billion in , driven by its widespread use as an . The expiration in 2015 enabled generic entry, leading to a sharp decline in branded sales due to increased ; U.S. sales, for instance, fell from $2.3 billion in 2013 to $746 million in 2015. By 2020, global branded revenues had diminished to approximately $1 billion amid generic dominance. Abilify Maintena generated approximately $1.35 billion in global sales in 2023. In the U.S., generic aripiprazole is produced by manufacturers including , (now part of ), , , Hetero Labs, and , with monthly costs typically ranging from $10 to $50 for a 30-day supply of 15 mg tablets, compared to over $1,000 for branded Abilify without insurance. This cost differential has accelerated the shift to generics, enhancing accessibility for patients treating and . Among injectables, Aristada generated $328 million in net sales in 2023 and $346 million in , reflecting steady demand for long-acting options in maintenance therapy. Abilify Asimtufii, a once-every-two-months formulation, was launched in 2023 to further support adherence in the maintenance market for and . expirations for extended-release forms, including a dual expiry for Abilify Maintena in 2024-2025, are expected to introduce generic and pressure sales for these products; the U.S. FDA approved the first generic version of aripiprazole extended-release injectable suspension in , though it had not yet launched as of late 2025.

Research

Attention-deficit/hyperactivity disorder

Aripiprazole is employed off-label for managing attention-deficit/hyperactivity disorder (ADHD) symptoms, especially in patients with comorbid tics or . Small randomized controlled trials indicate modest improvements in (ADHD-RS) scores with aripiprazole treatment. A systematic review of clinical trials, including four RCTs and five open-label studies, reported significant reductions in ADHD symptoms in several investigations, though results varied. Despite these findings, aripiprazole lacks FDA approval for ADHD treatment. In dosing trials, aripiprazole administered at 2–10 mg/day as an adjunct to medications has demonstrated reductions in hyperactivity symptoms. For instance, a mean dose of 6.7 mg/day led to significant improvements in ADHD and functional outcomes in children. However, this approach is associated with an increased incidence of , a common extrapyramidal . The evidence for aripiprazole in ADHD remains limited by inconsistent results across studies, with controlled trials often failing to consistently support its efficacy compared to open-label designs. A review of off-label uses concluded there is insufficient evidence to recommend aripiprazole as monotherapy for ADHD.

Substance use disorders

Aripiprazole has been investigated as a potential treatment for dependence, primarily due to its partial at D2 receptors, which may stabilize activity and reduce reward-driven behaviors associated with craving. In a randomized, double-blind, -controlled trial conducted in 2013 involving 90 methamphetamine-dependent adults, participants received aripiprazole (10-15 mg/day) or for 12 weeks alongside weekly counseling. The study found no significant reduction in methamphetamine use, as evidenced by similar proportions of positive tests at endpoint (44% in the aripiprazole group versus 45% in ). Craving scores, measured via visual analog scale, decreased in both groups from baseline (mean 46) but showed no between-group difference, suggesting limited clinical benefit for sustained abstinence despite theoretical D2 stabilization effects. For alcohol use disorder, aripiprazole has been explored both alone and in combination with to enhance relapse prevention. A randomized, double-blind compared aripiprazole (15 mg/day) to (50 mg/day) in 71 patients with over 12 weeks, finding both agents similarly effective in reducing heavy drinking days and craving, with no significant differences in relapse rates or duration. An exploratory initiated in (NCT00667875) specifically tested adjunctive aripiprazole (up to 15 mg/day) added to (50 mg/day) in 40 alcohol-dependent individuals over 16 weeks, reporting good tolerability in a preliminary pilot but no published results indicating superior relapse reduction. A 2022 of novel agents for alcohol use disorder concluded that aripiprazole demonstrates comparable to in reducing drinking but lacks robust evidence for adjunctive benefits in preventing relapse when combined. Research on aripiprazole for use disorder has yielded mixed results, with some evidence of reduced cue-induced reactivity but no consistent impact on abstinence. A 2017 in 80 cocaine-dependent outpatients using ecological momentary assessment found that aripiprazole (15 mg/day) over 8 weeks did not increase abstinence rates or reduce use days compared to . A 2013 of 22 trials on antipsychotics for or psychostimulant dependence, including aripiprazole, reported no significant effects on cocaine-positive urines or retention relative to , though tolerability was comparable. However, a 2021 comprehensive of pharmacotherapies for use disorder highlighted adjunctive potential for aripiprazole in laboratory paradigms measuring cue-reactivity, where it attenuated subjective responses to cues in some participants, suggesting a role in managing triggers rather than overall dependence. This effect is attributed to its partial agonism at dopamine D2 receptors, which stabilizes dopaminergic activity and attenuates cocaine-seeking behaviors, as demonstrated in preclinical models. Despite these investigational efforts, aripiprazole's application in substance use disorders faces challenges, including higher dropout rates attributed to side effects such as , fatigue, and drowsiness, which were significantly more common than with in methamphetamine and trials. A 2025 systematic review across alcohol and use disorders confirmed no superiority of aripiprazole over for or reduced use, with elevated discontinuation in active treatment arms. Aripiprazole has not received regulatory approval for any indication, and ongoing research post-2024 includes preclinical studies demonstrating its ability to attenuate morphine-induced release in animal models of opioid dependence, alongside case reports exploring its role in comorbid opioid use and psychiatric conditions.

Emerging applications

Aripiprazole is under investigation for the treatment of agitation and associated with and other , where it has shown potential as an off-label option despite the lack of specific FDA approval for this indication. A multicenter, randomized, double-blind, placebo-controlled trial demonstrated that aripiprazole at 10 mg/day significantly improved psychotic symptoms, as measured by the Brief Psychiatric Rating Scale (BPRS) psychosis cluster score, and reduced agitation, as assessed by the Cohen-Mansfield Agitation Inventory (CMAI) total and subscale scores, in institutionalized patients with . Recent reviews continue to highlight its role in managing behavioral and psychological symptoms of , including agitation, though its use requires careful monitoring for increased mortality risk in elderly patients, as indicated by the FDA warning for antipsychotics in this population. In the context of post-traumatic stress disorder (PTSD), aripiprazole has been explored as an adjunctive therapy, particularly in military veterans with treatment-resistant symptoms. A pilot randomized, placebo-controlled trial involving U.S. military veterans with chronic PTSD who were resistant to antidepressants found that adjunctive aripiprazole led to improvements in overall PTSD symptoms, with notable reductions in hyperarousal, potentially mediated by its partial agonism at the 5-HT1A receptor. However, the 2024 clinical guidelines from the U.S. Department of Veterans Affairs and Department of Defense recommend against the adjunctive use of aripiprazole (along with other atypical antipsychotics) for PTSD due to lack of demonstrated benefit and potential risks such as weight gain and metabolic effects. Structural studies have provided insights into aripiprazole's binding mechanism at the D2 receptor, informing the design of next-generation partial agonists. A investigation into the molecular determinants of aripiprazole's intrinsic efficacy revealed key noncovalent interactions, including hydrogen bonding and hydrophobic contacts within the D2 receptor's orthosteric site, that contribute to its balanced partial agonism and reduced side effect profile compared to full antagonists. These findings underscore aripiprazole's pharmacodynamic versatility and have guided structural modifications in developing novel antipsychotics with improved selectivity and efficacy for conditions involving dysregulation. Early investigational data support aripiprazole's role in augmenting treatment for pediatric (GAD), though evidence remains preliminary and safety remains a concern. Ongoing monitoring for long-term safety is essential, given the limited randomized data in this population and the preference for non-antipsychotic options as first-line therapy.

References

  1. https://pubchem.ncbi.nlm.nih.gov/compound/Aripiprazole
  2. https://www.ncbi.nlm.nih.gov/books/NBK547739/
  3. https://dailymed.nlm.nih.gov/dailymed/lookup.cfm?setid=178f09f0-e08e-452b-b817-717c5c49e110
  4. https://www.accessdata.fda.gov/drugsatfda_docs/nda/2002/21-436_abilify.cfm
  5. https://pmc.ncbi.nlm.nih.gov/articles/PMC8340839/
  6. https://www.fda.gov/drugs/novel-drug-approvals-fda/novel-drug-approvals-2023
  7. https://www.drugs.com/history/mezofy.html
  8. https://pmc.ncbi.nlm.nih.gov/articles/PMC5495458/
  9. https://www.accessdata.fda.gov/drugsatfda_docs/nda/2002/21-436_abilify_approv.pdf
  10. https://www.accessdata.fda.gov/drugsatfda_docs/label/2020/021436s044s045%2C021713s035s036%2C021729s027s028%2C021866s029s030lbl.pdf
  11. https://www.accessdata.fda.gov/drugsatfda_docs/label/2014/021436s038%2C021713s030%2C021729s022%2C021866s023lbl.pdf
  12. https://pubmed.ncbi.nlm.nih.gov/12363115/
  13. https://pubmed.ncbi.nlm.nih.gov/14628980/
  14. https://www.tandfonline.com/doi/full/10.3111/13696998.2014.979936
  15. https://academicworks.medicine.hofstra.edu/cgi/viewcontent.cgi?article=1898&context=publications
  16. https://pubmed.ncbi.nlm.nih.gov/26338693/
  17. https://www.accessdata.fda.gov/drugsatfda_docs/nda/2004/021436orig1s002.pdf
  18. https://news.bms.com/news/details/2008/US-Food-and-Drug-Administration-Approves-ABILIFY-aripiprazole-for-the-Acute-Treatment-of-Manic-and-Mixed-Episodes-Associated-with-Bipolar-I-Disorder-in-Pediatric-Patients-10-to-17-Years-of-Age/default.aspx
  19. https://www.accessdata.fda.gov/drugsatfda_docs/appletter/2005/21436s005%2C008%2C21713s003ltr.pdf
  20. https://www.accessdata.fda.gov/drugsatfda_docs/label/2023/217006s000lbl.pdf
  21. https://pubmed.ncbi.nlm.nih.gov/18835043/
  22. https://pubmed.ncbi.nlm.nih.gov/19906348/
  23. https://pubmed.ncbi.nlm.nih.gov/17960961/
  24. https://www.sciencedirect.com/science/article/abs/pii/S0165032711007609
  25. https://pmc.ncbi.nlm.nih.gov/articles/PMC3269345/
  26. https://pubmed.ncbi.nlm.nih.gov/21254788/
  27. https://www.dovepress.com/efficacy-acceptability-and-safety-of-adjunctive-aripiprazole-in-treatm-peer-reviewed-fulltext-article-NDT
  28. https://pmc.ncbi.nlm.nih.gov/articles/PMC4543152/
  29. https://pmc.ncbi.nlm.nih.gov/articles/PMC3466032/
  30. https://jamanetwork.com/journals/jama/fullarticle/2643308
  31. https://pmc.ncbi.nlm.nih.gov/articles/PMC2805571/
  32. https://www.accessdata.fda.gov/drugsatfda_docs/nda/2009/021436Orig1s027.pdf
  33. https://news.bms.com/news/details/2009/US-Food-and-Drug-Administration-Approves-ABILIFY-aripiprazole-for-the-Treatment-of-Irritability-Associated-with-Autistic-Disorder-in-Pediatric-Patients-Ages-6-to-17-Years/default.aspx
  34. https://publications.aap.org/pediatrics/article/124/6/1533/72227/Aripiprazole-in-the-Treatment-of-Irritability-in
  35. https://pubmed.ncbi.nlm.nih.gov/19797985/
  36. https://pmc.ncbi.nlm.nih.gov/articles/PMC8143447/
  37. https://www.sciencedirect.com/science/article/abs/pii/S0890856709602598
  38. https://pubmed.ncbi.nlm.nih.gov/21813076/
  39. https://www.accessdata.fda.gov/scripts/opdlisting/oopd/detailedIndex.cfm?cfgridkey=207905
  40. https://pmc.ncbi.nlm.nih.gov/articles/PMC5683285/
  41. https://pubmed.ncbi.nlm.nih.gov/24021518/
  42. https://pmc.ncbi.nlm.nih.gov/articles/PMC1324961/
  43. https://pubmed.ncbi.nlm.nih.gov/25939614/
  44. https://pmc.ncbi.nlm.nih.gov/articles/PMC3115673/
  45. https://pubmed.ncbi.nlm.nih.gov/19629012/
  46. https://pubmed.ncbi.nlm.nih.gov/15669888/
  47. https://journals.lww.com/indianjpsychiatry/fulltext/2019/61001/antipsychotic_augmentation_in_the_treatment_of.8.aspx
  48. https://www.accessdata.fda.gov/drugsatfda_docs/nda/2024/216655Orig1s000MultidisciplineR.pdf
  49. https://www.accessdata.fda.gov/drugsatfda_docs/appletter/2025/211448Orig1s000ltr.pdf
  50. https://pmc.ncbi.nlm.nih.gov/articles/PMC556368/
  51. https://pmc.ncbi.nlm.nih.gov/articles/PMC11062306/
  52. https://pubmed.ncbi.nlm.nih.gov/29189543/
  53. https://www.drugs.com/dosage/aripiprazole.html
  54. https://www.fda.gov/drugs/drug-safety-and-availability/fda-drug-safety-communication-fda-warns-about-new-impulse-control-problems-associated-mental-health
  55. https://www.medicalnewstoday.com/articles/drugs-abilify-withdrawal-symptoms
  56. https://pmc.ncbi.nlm.nih.gov/articles/PMC3719459/
  57. https://www.scirp.org/journal/paperinformation?paperid=141533
  58. https://pubmed.ncbi.nlm.nih.gov/14686220/
  59. https://shanghaiarchivesofpsychiatry.org/abilify-withdrawal/
  60. https://www.researchgate.net/publication/7008372_Does_antipsychotic_withdrawal_provoke_psychosis_Review_of_the_literature_on_rapid_onset_psychosis_supersenstivity_psychosis_and_withdrawal-related_relapse
  61. https://pmc.ncbi.nlm.nih.gov/articles/PMC8266572/
  62. https://pmc.ncbi.nlm.nih.gov/articles/PMC10501077/
  63. https://bmcpsychiatry.biomedcentral.com/articles/10.1186/s12888-024-05699-y
  64. https://pmc.ncbi.nlm.nih.gov/articles/PMC7552943/
  65. https://www.sciencedirect.com/science/article/pii/S2352853222000165
  66. https://pubmed.ncbi.nlm.nih.gov/28881461/
  67. https://onlinelibrary.wiley.com/doi/10.1155/2024/8883047
  68. https://www.researchgate.net/publication/395020485_Aripiprazole_overdose_in_Hong_Kong_A_10-year_retrospective_cohort
  69. https://pubmed.ncbi.nlm.nih.gov/23348561/
  70. https://pubmed.ncbi.nlm.nih.gov/18418794/
  71. https://pmc.ncbi.nlm.nih.gov/articles/PMC2759317/
  72. https://pubmed.ncbi.nlm.nih.gov/15902794/
  73. https://pmc.ncbi.nlm.nih.gov/articles/PMC8885235/
  74. https://www.pharmatutor.org/articles/toxicological-aspects-of-aripiprazole-new-antipsychotic-drug-review-article
  75. https://onlinelibrary.wiley.com/doi/10.1002/hkj2.70035
  76. https://www.tandfonline.com/doi/full/10.1080/15563650701665142
  77. https://pmc.ncbi.nlm.nih.gov/articles/PMC11319046/
  78. https://www.ema.europa.eu/en/documents/product-information/abilify-maintena-epar-product-information_en.pdf
  79. https://www.ncbi.nlm.nih.gov/books/NBK385288/
  80. https://pmc.ncbi.nlm.nih.gov/articles/PMC3249179/
  81. https://dailymed.nlm.nih.gov/dailymed/getFile.cfm?setid=11202c0a-7401-41c9-b1e7-d93739fcd36f&type=pdf
  82. https://go.drugbank.com/drugs/DB01238
  83. https://medlineplus.gov/druginfo/meds/a603012.html
  84. https://gpsych.bmj.com/content/33/4/e100235
  85. https://www.cambridge.org/core/books/antipsychotics-and-their-side-effects/anticholinergic-effects/C67891945598FF98A7D8471E1E1CA34A
  86. https://pubmed.ncbi.nlm.nih.gov/25524787/
  87. https://www.uspharmacist.com/article/qtc-prolongation-with-antidepressants-and-antipsychotics
  88. https://www.accessdata.fda.gov/drugsatfda_docs/label/2003/21436se1-001_abilify_lbl.pdf
  89. https://pmc.ncbi.nlm.nih.gov/articles/PMC4602118/
  90. https://pubmed.ncbi.nlm.nih.gov/12065741/
  91. https://pmc.ncbi.nlm.nih.gov/articles/PMC8450743/
  92. https://pmc.ncbi.nlm.nih.gov/articles/PMC9889418/
  93. https://pubmed.ncbi.nlm.nih.gov/11775041/
  94. https://pmc.ncbi.nlm.nih.gov/articles/PMC4819596/
  95. https://pubmed.ncbi.nlm.nih.gov/17265076/
  96. https://pmc.ncbi.nlm.nih.gov/articles/PMC5725548/
  97. https://elifesciences.org/articles/86805
  98. https://www.accessdata.fda.gov/drugsatfda_docs/label/2022/021436s048lbledit.pdf
  99. https://pmc.ncbi.nlm.nih.gov/articles/PMC10046771/
  100. https://pmc.ncbi.nlm.nih.gov/articles/PMC2958217/
  101. https://patents.google.com/patent/US5006528A/en
  102. https://data.epo.org/publication-server/rest/v1.0/publication-dates/20100818/patents/EP1480953NWB2/document.html
  103. https://www.ema.europa.eu/en/documents/assessment-report/aripiprazole-pharmathen-epar-public-assessment-report_en.pdf
  104. https://www.accessdata.fda.gov/drugsatfda_docs/nda/2017/207202Orig1s000MedR.pdf
  105. https://www.accessdata.fda.gov/drugsatfda_docs/appletter/2014/021436Orig1s038,021713Orig1s030,021729Orig1s022,021866Orig1s023ltr.pdf
  106. https://www.ema.europa.eu/en/medicines/human/EPAR/abilify
  107. https://www.otsuka.co.jp/en/company/newsreleases/2013/20130206_1.html
  108. https://www.ema.europa.eu/en/medicines/human/EPAR/abilify-maintena
  109. https://www.otsuka.co.jp/en/company/newsreleases/2024/20240327_1.html
  110. https://www.accessdata.fda.gov/drugsatfda_docs/nda/2013/202971s000TOC.cfm
  111. https://otsuka-us.com/news/fda-approves-otsuka-and-lundbecks-abilify-asimtufiir-aripiprazole-first-once-every-two-months
  112. https://www.accessdata.fda.gov/drugsatfda_docs/appletter/2015/202101Orig1s000ltr.pdf
  113. https://oag.ca.gov/news/press-releases/attorney-general-kamala-d-harris-42-other-attorneys-general-announce-195-million
  114. https://www.mayoclinic.org/drugs-supplements/aripiprazole-oral-route/description/drg-20066890
  115. https://tajpharmaindia.com/portfolio-item/aripiprazole-tablets-ip-2mg/
  116. https://bnf.nice.org.uk/drugs/aripiprazole/medicinal-forms/
  117. https://dailymed.nlm.nih.gov/dailymed/drugInfo.cfm?setid=f87dbfe4-5417-47c9-a97f-d246cfc10023
  118. https://www.unodc.org/documents/commissions/CND/Scheduling_Resource_Material/Scheduling_Control_Regimes.pdf
  119. https://www.ema.europa.eu/en/documents/product-information/abilify-epar-product-information_en.pdf
  120. https://www.ema.europa.eu/en/medicines/human/EPAR/aripiprazole-zentiva
  121. https://www.ema.europa.eu/en/medicines/human/EPAR/aripiprazole-accord
  122. https://www.ema.europa.eu/en/medicines/human/EPAR/aripiprazole-sandoz
  123. https://www.pharmiweb.com/press-release/2024-03-27/abilify-maintena-960-mg-aripiprazole-approved-in-the-eu-as-the-first-once-every-two-months-long-acting-injectable-for-the-maintenance-treatment-of
  124. https://www.drugs.com/aripiprazole.html
  125. https://reference.medscape.com/drug/abilify-maintena-aristada-aripiprazole-342983
  126. https://www.aristada.com/
  127. https://www.drugpatentwatch.com/p/drug-sales/drugname/ABILIFY
  128. https://www.biopharmadive.com/news/bristol-myers-hit-with-marketing-fine-for-abilify/432130/
  129. https://www.pharmaceutical-technology.com/analyst-comment/otsukas-abilify-maintena-dual-drug-expiry-signals-sales-decline/
  130. https://xtalks.com/top-20-best-selling-neurology-drugs-to-watch-in-2024-3931/
  131. https://www.tevausa.com/news-and-media/press-releases/teva-launches-generic-abilify-tablets-in-the-united-states/
  132. https://www.drugpatentwatch.com/p/generic-api/ARIPIPRAZOLE
  133. https://www.goodrx.com/aripiprazole
  134. https://www.talkspace.com/blog/abilify-cost-insurance/
  135. https://investor.alkermes.com/static-files/3ecedd18-3cfc-4a7d-a384-ad6266e734ef
  136. https://investor.alkermes.com/static-files/2dc67144-9b40-4e3f-8718-b9889df0bdf1
  137. https://www.globaldata.com/media/pharma/otsukas-new-formulations-offset-abilify-maintena-dual-patent-expiry-impact-says-globaldata/
  138. https://www.fda.gov/drugs/drug-and-biologic-approval-and-ind-activity-reports/2024-first-generic-drug-approvals
  139. https://www.drugs.com/availability/generic-abilify-maintena.html
  140. https://psychopharmacologyinstitute.com/publication/aripiprazole-indications-fda-approved-and-off-label-uses-2120/
  141. https://pubmed.ncbi.nlm.nih.gov/18759644/
  142. https://pubmed.ncbi.nlm.nih.gov/24141455/
  143. https://www.nami.org/about-mental-illness/treatments/mental-health-medications/types-of-medication/aripiprazole-abilify/
  144. https://nsj.org.sa/content/nsj/18/4/323.full.pdf
  145. https://pubmed.ncbi.nlm.nih.gov/23186131/
  146. https://pmc.ncbi.nlm.nih.gov/articles/PMC3602333/
  147. https://pubmed.ncbi.nlm.nih.gov/18515460/
  148. https://clinicaltrials.gov/study/NCT00667875
  149. https://link.springer.com/article/10.1007/s40265-021-01670-3
  150. https://pmc.ncbi.nlm.nih.gov/articles/PMC5233586/
  151. https://www.psychiatrist.com/jcp/antipsychotics-cocaine-psychostimulant-dependence/
  152. https://jamanetwork.com/journals/jamanetworkopen/fullarticle/2779686
  153. https://pmc.ncbi.nlm.nih.gov/articles/PMC3121303/
  154. https://journals.lww.com/journaladdictionmedicine/fulltext/2025/09000/aripiprazole_is_not_effective_for_abstinence_or.6.aspx
  155. https://www.sciencedirect.com/science/article/abs/pii/S0028390823001363
  156. https://www.cureus.com/articles/269218-aripiprazole-provoking-gambling-disorder-in-a-patient-with-opioid-use-disorder-a-case-report
  157. https://www.researchgate.net/publication/5871265_Aripiprazole_for_the_Treatment_of_Psychoses_in_Institutionalized_Patients_With_Alzheimer_Dementia_A_Multicenter_Randomized_Double-Blind_Placebo-Controlled_Assessment_of_Three_Fixed_Doses
  158. https://pubmed.ncbi.nlm.nih.gov/34761857/
  159. https://pubmed.ncbi.nlm.nih.gov/35145438/
  160. https://pubmed.ncbi.nlm.nih.gov/25647451/
  161. https://www.healthquality.va.gov/guidelines/MH/ptsd/PTSD-in-Annals-2024.pdf
  162. https://pmc.ncbi.nlm.nih.gov/articles/PMC7365685/
  163. https://www.orpdl.org/durm/meetings/meetingdocs/2024_02_01/archives/2024_02_01_Antipsyc_DUE_6-17yo.pdf
Add your contribution
Related Hubs
Contribute something
User Avatar
No comments yet.