Bristol-Myers Squibb and Otsuka Pharmaceutical Co, Ltd. may have provided support for some of these clinical trials. Please review the enclosed disclosures.
Major Depressive Disorder (MDD) in Adults – Adjunctive Therapy to an Antidepressant
ABILIFY is indicated for use as an adjunctive therapy to antidepressants for the acute treatment of Major Depressive Disorder in adults. Click here for dosing information.
CNS Spectrum. 2009 Apr; 14 (4): 197-206.
Berman RM, Fava M, Thase ME, et al.
Close summary
A randomized, double-blind, placebo-controlled study
evaluating the efficacy and safety of adjunctive ABILIFY compared to
adjunctive placebo in adult patients diagnosed with Major Depressive Disorder
who had an inadequate response to prior antidepressant therapy
(1 to 3 courses)
in the current episode and an inadequate response to 8 weeks of prospective
treatment with an antidepressant therapy. The primary endpoint was the mean
change from baseline in the Montgomery-Åsberg Depression Rating Scale
(MADRS) Total Score at endpoint (Week 6). The mean change in MADRS Total Score
was significantly greater in patients on adjunctive ABILIFY compared to
adjunctive placebo (P < 0.001) at endpoint. Adverse
events (incidence ≥ 5% of patients in the adjunctive ABILIFY group and at
least twice the rate of adjunctive placebo) included akathisia (18.2% for
ABILIFY + ADT, 3.5% for placebo + ADT), restlessness (12.5% for ABILIFY +
ADT, 3.5% for placebo + ADT), somnolence (5.7% for ABILIFY + ADT, 0.6% for
placebo + ADT), and vision blurred (7.4% for ABILIFY + ADT, 1.7% for placebo
+ ADT).
Journal of Clinical Psychopharmacology. 2008 Apr; 28 (2): 156-165.
Marcus RN, McQuade RD, Carson WH, et al.
Close summary
A randomized, double-blind, placebo-controlled study
evaluating the efficacy and safety of adjunctive ABILIFY compared to
adjunctive placebo in adult patients diagnosed with Major Depressive Disorder
who had an inadequate response to prior antidepressant therapy
(1 to 3 courses) in the current episode and an inadequate response to 8 weeks
of prospective treatment with an antidepressant therapy. The primary endpoint
was the mean change from baseline in the Montgomery-Åsberg Depression
Rating Scale (MADRS) Total Score at endpoint (Week 6). The mean change in MADRS
Total Score was significantly greater in patients on adjunctive ABILIFY
compared to adjunctive placebo (P < 0.001) at endpoint.
Adverse events (incidence ≥ 5% in the Adjunctive ABILIFY group and at least
twice that of adjunctive placebo) included akathisia (25.9% for ABILIFY + ADT,
4.2% for placebo + ADT), fatigue (10.1% for ABILIFY + ADT, 3.7% for placebo +
ADT), restlessness (9.5% for ABILIFY + ADT, 0.5% for placebo + ADT), insomnia
(7.4% for ABILIFY + ADT, 1.6% for placebo + ADT), tremor (6.3% for ABILIFY +
ADT, 2.6% for placebo + ADT), and constipation (5.3% for ABILIFY + ADT, 2.6%
for placebo + ADT).
Journal of Clinical Psychiatry. 2007 Jun; 68(6): 843-53.
Berman RM, Marcus RN, Swanink R, et al.
Close summary
A randomized, double-blind, placebo-controlled study
evaluating the efficacy and safety of adjunctive ABILIFY compared to
adjunctive placebo in adult patients diagnosed with Major Depressive Disorder
which had an inadequate response to prior antidepressant therapy
(1 to 3 courses) in the current episode and an inadequate response to 8
weeks of prospective treatment with an antidepressant therapy. The primary
endpoint was the change from baseline in the Montgomery-Åsberg
Depression Rating Scale (MADRS) Total Score at endpoint (week 6). The mean
change in MADRS Total Score was significantly greater in patients on
adjunctive ABILIFY compared to adjunctive placebo (P <
.001) at endpoint. Adverse events (incidence ≥ 5% in the adjunctive
ABILIFY group and at least twice the rate of adjunctive placebo) included
akathisia (23.1% for ABILIFY + ADT, 4.5% for placebo + ADT), restlessness
(14.3% for ABILIFY + ADT, 3.4% for placebo + ADT), upper respiratory tract
infection (8.2% for ABILIFY + ADT, 4.0% for placebo + ADT), insomnia (7.7%
for ABILIFY + ADT, 2.3% for placebo + ADT), and vision blurred (6.6% for
ABILIFY + ADT, 1.7% for placebo + ADT).
Adolescent Schizophrenia (Ages 13 to 17)
ABILIFY is indicated for acute and maintenance treatment of Schizophrenia in adolescents 13 to 17 years of age. Click here for dosing information.
American Journal of Psychiatry. 2008;16(11):1369-72.
Findling RL, Robb A, Nyilas M, et al.
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A multicenter, double-blind, placebo-controlled,
6-week study conducted to evaluate the efficacy and safety of oral ABILIFY
(10 mg/day or 30 mg/day) for the treatment of adolescents (13 to 17 years)
with Schizophrenia. The primary endpoint was the mean change from baseline
in the Positive and Negative Syndrome Scale (PANSS) Total Score. At endpoint
(Week 6), ABILIFY demonstrated statistically significantly greater improvement
on PANSS Total Score compared to placebo (P < 0.05).
Adverse events occurring at an incidence ≥5% for ABILIFY-treated patients and
greater than placebo included akathisia (ABILIFY 10 mg 5%; ABILIFY 30 mg 12%;
placebo 5%), extrapyramidal disorder (ABILIFY 10 mg 13%; ABILIFY 30 mg 22%;
placebo 5%), nausea (ABILIFY 10 mg 9%; ABILIFY
30 mg 10%; placebo 6%),
dizziness (ABILIFY 10 mg 7%; ABILIFY 30 mg 4%; placebo 3%), headache (ABILIFY
10 mg 16%; ABILIFY 30 mg 11%; placebo 10%), somnolence (ABILIFY 10 mg 11%;
ABILIFY 30 mg 22%; placebo 6%), tremor (ABILIFY 10 mg 2%; ABILIFY 30 mg 12%;
placebo 2%), and nasopharyngitis (ABILIFY 10 mg 5%; ABILIFY 30 mg 5%; placebo 4%).
Bipolar I Disorder, Manic and Mixed in Adults
ABILIFY is indicated for the treatment of manic or mixed episodes associated with Bipolar I Disorder either as monotherapy or adjunctive to lithium or valproate. Click here for dosing information.
American Journal of Psychiatry. 2003; 160: 1651-1658.
Keck PE Jr., Marcus RN, Tourkodimitris S, et al.
Close summary
A multicenter, double-blind, placebo-controlled,
3-week trial was conducted to evaluate the efficacy and safety of oral
ABILIFY (30 mg/day with the option to decrease to
15 mg/day) for the
treatment of adults with Bipolar I Disorder with acute manic or mixed
episodes. The primary endpoint was the Young Mania Rating Scale (Y-MRS)
at Week 3. ABILIFY demonstrated statistically significantly greater
improvement on Y-MRS Total Score compared to placebo, (P =
0.002) at endpoint. Adverse events occurring at an incidence of ≥10
for ABILIFY-treated patients and greater than placebo included headache
(ABILIFY 36%, placebo 31%), nausea (ABILIFY 23%, placebo 10%), dyspepsia
(ABILIFY 22%, placebo 10%), somnolence (ABILIFY 20%, placebo 5%), agitation
(ABILIFY 20%, placebo 19%), anxiety (ABILIFY 18%, placebo 10%), vomiting
(ABILIFY 16%, placebo 5%), insomnia (ABILIFY 15%, placebo 9%),
lightheadedness (ABILIFY 14%, placebo 8%), constipation (ABILIFY 13%,
placebo 6%), accidental injury (ABILIFY 12%, placebo 2%), diarrhea (ABILIFY
12%, placebo 9%), and akathisia (ABILIFY 11%, placebo 2%).
Journal of Psychopharmacology. 2006;20(4):536-46.
Sachs G, Sanchez R, Marcus R, et al.
Close summary
A multicenter, double-blind, placebo-controlled,
3-week trial was conducted to evaluate the efficacy and safety of oral
ABILIFY (30 mg/day with the option to decrease to
15 mg/day) for the
treatment of adults with Bipolar I Disorder with acute manic or mixed
episode. The primary endpoint was the Young Mania Rating Scale (Y-MRS)
at Week 3. ABILIFY demonstrated statistically significantly greater
improvement on Y-MRS Total Score compared to placebo (P
≤ 0.001) at endpoint. Adverse events occurring at an
incidence of ≥10% for ABILIFY-treated patients and greater than placebo
included headache (ABILIFY 25%, placebo 24.8%), nausea (ABILIFY 21.3%,
placebo 15.8%), somnolence (ABILIFY 19.9%, placebo 10.5%), akathisia
(ABILIFY 17.6%, placebo 4.5%,), dyspepsia (ABILIFY 15.4%, placebo 6.8%,),
agitation (ABILIFY 14.7%, placebo 14.3%), constipation (ABILIFY 11.8%,
placebo 5.3%), vomiting (ABILIFY 11%, placebo 7.5%), anxiety (ABILIFY 10.3%,
placebo 8.3%) and extremity pain (ABILIFY 10.3%, placebo 5.3%).
Journal of Clinical Psychiatry. 2006;67: 626-637.
Keck PE Jr., Calabrese JR, McQuade RD, et al.
Close summary
A double-blind, randomized, placebo-controlled 26-week
study conducted to evaluate the efficacy and safety of oral ABILIFY
(15 mg/day or 30 mg/day) in adults with a recent manic or mixed episode
associated with Bipolar I Disorder. Patients were stabilized (YMRS ≤10 and
MADRS ≤13) on ABILIFY monotherapy for 6 consecutive weeks and then
randomized to either aripiprazole or placebo and observed for manic, mixed,
or depressive relapse. Treatment with ABILIFY significantly decreased time
to manic relapse compared to placebo. Adverse events occurring at an
incidence of ≥10% for ABILIFY-treated patients and greater than placebo
included anxiety (ABILIFY 16.9%, placebo 14.5%) nervousness (ABILIFY
10.4%, placebo 6%).
Agitation Associated With Bipolar Mania in Adults
ABILIFY injection is indicated for the acute treatment of agitation associated with Bipolar Disorder, manic or mixed in adults. Click here for dosing information.
Journal of Clinical Psychopharmacology. 2007;27 27:176-6.
Zimbroff DL, Marcus RN, Manos G, et al.
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A 24-hour, randomized, double-blind, placebo-controlled study conducted to evaluate the efficacy and safety of intramuscular (IM) ABILIFY injection (9.75 mg and 15 mg) for the treatment of acute agitation in hospitalized patients with Bipolar I Disorder who were experiencing an acute mixed or manic episode. Study was not designed for any comparison between ABILIFY Injection and lorazepam. ABILIFY injection was observed to be significantly more effective than placebo for the treatment of acute agitation as measured by the change in the Positive and Negative Syndrome Scale (PANSS)-Excited Component (PEC) scores at endpoint (2 hours). Adverse events reported during IM treatment (at least 5% of patients in any treatment group) included headache (ABILIFY IM 9.75 mg 14.7%; ABILIFY IM 15 mg 17.3%; placebo 12.5%), insomnia (ABILIFY IM 9.75 mg 10.7%; ABILIFY IM 15 mg 6.7%; placebo 8.3%), dizziness (ABILIFY IM 9.75 mg 2.7%; ABILIFY IM 15 mg 12.0%; placebo 5.6%), nausea (ABILIFY IM 9.75 mg 10.7%; ABILIFY IM 15 mg 18.7%; placebo 5.6%), somnolence (ABILIFY IM 9.75 mg 8.0%; ABILIFY IM 15 mg 8.0%; placebo 5.6%), sedation (ABILIFY IM 9.75 mg 4.0%; ABILIFY IM 15 mg 5.3%; placebo 1.4%), vomiting (ABILIFY IM 9.75 mg 4.0%; ABILIFY IM 15 mg 6.7%; placebo 1.4%).
Journal of Clinical Psychiatry. 2003; 64(9):1048-1056.
Pigott TA, Carson WH, Saha AR, et al.
Close summary
A 26-week, randomized, placebo-controlled study conducted to evaluate the efficacy and safety of oral ABILIFY (15 mg/day) in preventing relapse in patients with schizophrenia who were stabilized on other antipsychotic medications for 3 months or longer and were discontinued from these other medications and given ABILIFY or placebo and observed for relapse. ABILIFY significantly delayed the time to relapse and demonstrated significant reduction in risk of relapse compared to placebo. Adverse events (≥5% and greater than placebo) observed in subjects receiving ABILIFY included insomnia (ABILIFY 42.5%, placebo 39.9%), tremor (ABILIFY 8.5%, placebo 1.3%), akathisia (ABILIFY 7.8%, placebo 6.5%), vomiting (ABILIFY 5.9%, placebo 3.3%), and nausea (ABILIFY 5.2%, placebo 3.3%).
Agitation Associated With Schizophrenia in Adults
ABILIFY injection is indicated for the acute treatment of agitation associated with Schizophrenia in adults. Click here for dosing information.
Journal of Clinical Psychiatry. 2007; 68(1):111-119.
Tran-Johnson TK, Sack DA, Marcus RN, et al.
Close summary
A 24-hour, randomized, double-blind, placebo-controlled study conducted to evaluate the efficacy and safety of intramuscular (IM) ABILIFY Injection (in a range of doses) or IM haloperidol compared with placebo for the treatment of acute agitation in hospitalized patients primarily with schizophrenia. ABILIFY was observed to be significantly more effective than placebo for the treatment of acute agitation, as measured by the change in the Positive and Negative Syndrome Scale (PANSS)-Excited Component (PEC) score, at 2 hours (ABILIFY Injection IM 5.25 mg, 9.75 mg and 15 mg). Adverse events reported during ABILIFY Injection IM treatment (at least 5% of patients in any treatment group) included tachycardia (ABILIFY IM 5.25 mg 3.2%; ABILIFY IM 9.75 mg 7.1%; ABILIFY IM 15 mg 0%; placebo 1.6%), vomiting (ABILIFY IM 5.25 mg 0%; ABILIFY IM 9.75 mg 3.6%; ABILIFY IM 15 mg 5.2%; placebo 1.6%), nausea (ABILIFY IM 5.25 mg 9.7%; ABILIFY IM 9.75 mg 10.7%; ABILIFY IM 15 mg 3.4%; placebo 3.3%), dizziness (ABILIFY IM 5.25 mg 11.3%; ABILIFY IM 9.75 mg 7.1%; ABILIFY IM 15 mg 12.1%; placebo 6.6%), headache (ABILIFY IM 5.25 mg 17.7%; ABILIFY IM 9.75 mg 10.7%; ABILIFY IM 15 mg 13.8%; placebo 1.6%), somnolence (ABILIFY IM 5.25 mg 8.1%; ABILIFY IM 9.75 mg 5.4%; ABILIFY IM 15 mg 10.3%; placebo 4.9%), akathisia (ABILIFY IM 5.25 mg 3.2%; ABILIFY IM 9.75 mg 5.4%; ABILIFY IM 15 mg 0%; placebo 0%), agitation (ABILIFY IM 5.25 mg 0%; ABILIFY IM 9.75 mg 3.6%; ABILIFY IM 15 mg 5.2%; placebo 1.6%).
Psychopharmacology. 2006:188:281-292.
Andrezina R, Josiassen RC, Marcus RN, et al.
Close summary
A 24-hour, randomized, double-blind, placebo-controlled study conducted to evaluate the efficacy and safety of intramuscular (IM) ABILIFY Injection (9.75 mg) or IM haloperidol compared with placebo for the treatment of acute agitation in hospitalized patients primarily with schizophrenia. ABILIFY was observed to be significantly more effective than placebo for the treatment of acute agitation, as measured by the change in the Positive and Negative Syndrome Scale (PANSS)-Excited Component (PEC) score, at 2 hours (study endpoint). Adverse events reported during IM treatment (at least 5% of patients in any treatment group) included headache (ABILIFY IM 7.4%, placebo 6.9%), dizziness (ABILIFY IM 6.3%, placebo 2.3%), nausea (ABILIFY IM 5.7%, placebo 1.2%), insomnia (ABILIFY IM 5.7%, placebo 9.2%), and agitation (ABILIFY IM 4%, placebo 5.8%).
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