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Review

A commentary on the efficacy of olanzapine for the treatment of schizophrenia: the past, present, and future

Leslie Citrome1 Department of Psychiatry and Behavioral Sciences, New York Medical College, Valhalla, NY, USACorrespondence[email protected]
ORCID Iconhttps://orcid.org/0000-0002-6098-9266
ORCID Icon,
Joseph P McEvoy2 Department of Psychiatry and Health Behavior, Medical College of Georgia, Augusta University, Augusta, GA, USA
,
Mark S Todtenkopf3 Alkermes, Inc., Waltham, MA, USAORCID Iconhttps://orcid.org/0000-0003-4764-7816
ORCID Icon,
David McDonnell4 Alkermes Pharma Ireland Ltd., Dublin, Ireland
&
Peter J Weiden3 Alkermes, Inc., Waltham, MA, USAORCID Iconhttps://orcid.org/0000-0001-5583-5871
ORCID Icon
Pages 2559-2569 | Published online: 05 Sep 2019

Abstract

Olanzapine is a second-generation atypical antipsychotic with proven efficacy for the treatment of schizophrenia. Approved in 1996, olanzapine is one of the most studied antipsychotics, resulting in a considerable amount of clinical data across diverse patient populations. Despite the fact that olanzapine is associated with a known risk of metabolic side effects, including weight gain, many clinicians continue to prescribe olanzapine for the treatment of schizophrenia with the expectation of additional therapeutic antipsychotic efficacy relative to other first-line atypical antipsychotics. The goal of this narrative is to revisit the role of oral olanzapine in the management of patients with schizophrenia, including those with recently diagnosed schizophrenia (“first-episode”), those with an established schizophrenia diagnosis who experience acute exacerbations, those receiving long-term antipsychotic treatment as a maintenance intervention, and those with suboptimal response to antipsychotic treatment, including treatment resistance. Collectively, data from published literature support the favorable efficacy of olanzapine compared with other first- and second-generation antipsychotics, including lower rates of treatment discontinuation and clinically meaningful improvements in the symptoms of schizophrenia. The development of antipsychotic medications with the favorable efficacy of olanzapine, but with reduced weight gain, could address a major unmet need in the treatment of schizophrenia.

Introduction

Olanzapine is an atypical antipsychotic first approved by the US Food and Drug Administration (FDA) in September 1996 for the treatment of schizophrenia.Citation1,Citation2 The availability of olanzapine and the atypical class in general provided psychiatrists with treatment options with reduced risk of motoric adverse effects.Citation3 Several meta-analyses have been published establishing the efficacy and minimal extrapyramidal adverse effects with olanzapine compared to typical and some atypical antipsychotics in the treatment of schizophrenia.Citation4Citation6 However, due to the risk of metabolic dysregulation and weight gain, most guidelines have positioned olanzapine as a second-choice therapy for the treatment of schizophrenia.Citation7Citation11 This is similar to clozapine, which, despite its established efficacy for treatment-resistant symptoms, is positioned last because of safety concerns.Citation11,Citation12 Many experienced clinicians are of the opinion that olanzapine offers a distinctly favorable efficacy profile among the currently available antipsychotic medications,Citation4Citation6,Citation13 and therefore continue to prescribe the drug for patients with schizophrenia. This narrative review revisits the role of oral olanzapine in the management of adults with schizophrenia, examining evidence supporting the additional efficacy of olanzapine from the published literature since its initial approval.

Initial discovery and preclinical data

Olanzapine was first discovered while searching for a chemical analog of clozapine that would not require hematological monitoring. While investigating a series of thiophene isosteres on 1 of the phenyl rings in clozapine, a thienobenzodiazepine analog (olanzapine) was discovered.Citation1,Citation14,Citation15 The receptor binding affinities for olanzapine were determined using in vitro assaysCitation16 and confirmed by in vivo functional assays.Citation17 Olanzapine has high binding affinity for D1, D2, D4, 5HT2A, 5HT2C, 5HT3, α-1 adrenergic, histaminergic, and muscarinic receptors, which mirrors that of clozapine.Citation16 In functional studies, olanzapine was a potent antagonist at 5HT and D2 receptors, suggesting it might be useful as an antipsychotic agent.Citation17 In animal models, olanzapine produced antagonism of apomorphine-induced climbing and conditioned avoidance responding in rats, suggesting dopaminergic effects; antagonism of 5-hydroxytryptophan-induced head twitching and blockade of oxotremorine-induced tremor in mice indicate serotonergic and anticholinergic activity, respectively.Citation18 In addition, although not binding directly, research has indicated that olanzapine modulates N-methyl-d-aspartate (NMDA) receptors.Citation19,Citation20 These preclinical studies provided strong evidence that olanzapine could potentially be an effective antipsychotic drug with less drug-induced motoric activation associated with the existing antipsychotics at the time (see Safety section).Citation18,Citation21 The clinical pharmacokinetic profile of olanzapine supported once-daily oral administration, starting with a dose of 5–10 mg, with a target dose of 10 mg/day, and a maximum dose of 20 mg/day.Citation1 Taken together, the preclinical and pharmacokinetic data helped to support the full clinical development and eventual approval of olanzapine for the treatment of schizophrenia.Citation2

The approval of olanzapine in schizophrenia was initially based on data from short-term controlled trials (6 weeks).Citation22 A longer-term maintenance trial (up to 8 months) of adults who met DSM-III-R/DSM-IV criteria for schizophrenia was later conducted.Citation1 Since its approval over 2 decades ago, olanzapine has been one of the most investigated drugs in its class, leading to the generation of a considerable amount of clinical data on its efficacy and safety in patients with schizophrenia and other indications.Citation1,Citation3,Citation23

Assessment of antipsychotic effects

Schizophrenia is a chronic disease with a diverse psychopathology and multiple phases of illness.Citation11,Citation24 Consequently, numerous factors must be considered when assessing the benefits of a given treatment over short- and long-term periods.Citation11,Citation25 A number of scales and instruments are used in clinical trials of schizophrenia to assess treatment efficacy; these have been reviewed in detail elsewhere.Citation26Citation29 Improvements in the psychopathologic symptoms of schizophreniaCitation26 are commonly assessed using the 18-item Brief Psychiatric Rating Scale (BPRS),Citation30 the Clinical Global Impression (CGI) scale,Citation29,Citation31 or the 30-item Positive and Negative Syndrome Scale (PANSS).Citation32 Another well-recognized measure of treatment effectiveness that takes into consideration not only efficacy and tolerability but also patient experience is all-cause discontinuation.Citation33Citation35 The effect of antipsychotic treatment on hostility, given its close relationship to aggression and nonadherence to treatment,Citation36 has also been extensively studied,Citation37 commonly by examining treatment-associated changes to the hostility item of the PANSSCitation32 or BPRSCitation30 as a proxy measure of aggression.

Here, we summarize key evidence for the efficacy of olanzapine across various stages of treatment in patients with schizophrenia ().

Table 1 Selected first-episode, acute, chronic/maintenance, and treatment-resistant schizophrenia trials assessing efficacy of olanzapine

First-episode schizophrenia

Patients presenting with a first psychotic episode require prompt administration of an effective antipsychotic medication to minimize the duration of untreated psychosis.Citation11 The first episode of psychosis can be polymorphic and may evolve into a variety of conditions other than schizophrenia, with associated prognostic implications. Regardless of the eventual diagnosis, early intervention during a psychotic episode may prevent future deterioration and progression toward chronicity.Citation11

Several studies have provided evidence of olanzapine’s efficacy in first-episode schizophrenia patients.Citation38Citation41 Notably, patients treated with olanzapine were less likely to discontinue treatment compared with other antipsychotics. In the large-scale European First-Episode Schizophrenia Trial (EUFEST), olanzapine had the lowest rate of all-cause discontinuation () at 1 year (33%) compared with haloperidol (72%), quetiapine (53%), ziprasidone (45%), and amisulpride (40%).Citation40 In a separate trial, nearly 2 times as many patients remained on olanzapine (23%) compared with haloperidol (12%) at 2 years.Citation39 In both studies, treatment with olanzapine was associated with a more favorable efficacy profile, as evidenced by considerably lower rates of discontinuation due to lack of efficacy (14–19% vs 25–48%) during treatment with olanzapine compared with other antipsychotics.Citation39,Citation40 A post hoc analysis examining all-cause discontinuation rates from EUFEST found that treatment with olanzapine was associated with a number needed to treat (NNT) of 4 compared with haloperidol (indicating that 4 patients have to be treated with olanzapine instead of haloperidol to prevent 1 treatment discontinuation). For comparison, the NNT for quetiapine compared with haloperidol was 9.Citation42

Figure 1 Time to all-cause discontinuation of antipsychotics across studies. Time to all-cause discontinuation is consistently longer with olanzapine compared with other first- and second-generation antipsychotics. CATIE: From New England Journal of Medicine. Lieberman et al. Effectiveness of antipsychotic drugs in patients with chronic schizophrenia. Volume 353, page 1219. Copyright ©2005 Massachusetts Medical Society. Reprinted with permission from Massachusetts Medical Society.Citation56 EUFEST: Reprinted from The Lancet, Volume 371, Kahn et al. Effectiveness of antipsychotic drugs in first-episode schizophrenia and schizophreniform disorder: an open randomised clinical trial, Pages 1085-1097, Copyright 2008, with permission from Elsevier.Citation40 Kinon et al, 2006: Kinon et al, Differential rates of treatment discontinuation in clinical trials as a measure of treatment effectiveness for olanzapine and comparator atypical antipsychotics for schizophrenia. Journal of Clinical Psychopharmacology. 2006;26(6):632–637.Citation35 SOHO: Reprinted from European Neuropsychopharmacology. Volume 17. Haro et al. Three-year antipsychotic effectiveness in the outpatient care of schizophrenia: observational versus randomized studies results. Pages 235–244. Copyright 2007, with permission from Elsevier.Citation59

Figure 1 Time to all-cause discontinuation of antipsychotics across studies. Time to all-cause discontinuation is consistently longer with olanzapine compared with other first- and second-generation antipsychotics. CATIE: From New England Journal of Medicine. Lieberman et al. Effectiveness of antipsychotic drugs in patients with chronic schizophrenia. Volume 353, page 1219. Copyright ©2005 Massachusetts Medical Society. Reprinted with permission from Massachusetts Medical Society.Citation56 EUFEST: Reprinted from The Lancet, Volume 371, Kahn et al. Effectiveness of antipsychotic drugs in first-episode schizophrenia and schizophreniform disorder: an open randomised clinical trial, Pages 1085-1097, Copyright 2008, with permission from Elsevier.Citation40 Kinon et al, 2006: Kinon et al, Differential rates of treatment discontinuation in clinical trials as a measure of treatment effectiveness for olanzapine and comparator atypical antipsychotics for schizophrenia. Journal of Clinical Psychopharmacology. 2006;26(6):632–637.Citation35 SOHO: Reprinted from European Neuropsychopharmacology. Volume 17. Haro et al. Three-year antipsychotic effectiveness in the outpatient care of schizophrenia: observational versus randomized studies results. Pages 235–244. Copyright 2007, with permission from Elsevier.Citation59

Substantial improvements in several other efficacy-related outcome measures have also been observed. Greater improvements in total BPRS score have been reported with olanzapine compared with haloperidol, with patients over 2 times more likely to achieve clinical response (defined as ≥40% improvement from baseline in BPRS total score) with olanzapine (67% vs 29%, respectively; NNT=3).Citation38 Significantly greater reductions in PANSS positive subscale scores have also been reported with olanzapine following 1 year of follow-up compared with quetiapine.Citation41 In the EUFEST study, olanzapine provided numerical but not statistically significant differences in PANSS score reductions versus haloperidol; however, remission rates significantly favored olanzapine (57% vs 44%; NNT=8).Citation39 Furthermore, in patients with first-episode schizophrenia, olanzapine was associated with a significantly greater reduction of hostility at 1 and 3 months compared with haloperidol, quetiapine, and amisulpride during the first 3 months of treatment.Citation37

Acute exacerbation in patients with schizophrenia

Patients suffer a variety of positive psychotic symptoms during acute exacerbations of schizophrenia, including delusions, hallucinations, and thought disorder, which may be present along with other associated behaviors (such as agitation and aggression).Citation11 In addition, negative and affective symptoms may be the focus of intervention.Citation11 During exacerbations, the goal of treatment is to reduce the severity of psychosis and associated symptoms as quickly as possible, and to formulate short- and long-term treatment plans to prevent relapse and slow or limit disease progression.Citation11

The initial efficacy of olanzapine in acute schizophrenia was based on data from 4 pivotal, 6-week, double-blind trials in which reductions in BPRS total scores were significantly or numerically greater with olanzapine compared to placebo and haloperidol.Citation43Citation46 Subsequently, the efficacy of olanzapine in the treatment of acute exacerbations has been confirmed in several randomized, double-blind studies using the PANSS.Citation47Citation50 Similar to findings in first-episode schizophrenia patients,Citation37 olanzapine was also reported to be more effective than haloperidol in reducing aggressive behavior in a study that specifically enrolled physically assaultive patients with schizophrenia.Citation51

The efficacy of olanzapine in the treatment of acute exacerbations is supported by a meta-analysis involving direct and indirect comparisons of 212 randomized controlled studies of 15 first- and second-generation antipsychotics.Citation34 Olanzapine was among 4 antipsychotics (which also included clozapine, amisulpride, and risperidone) determined to be significantly more effective than other choices in the acute treatment of schizophrenia, based on improvements in PANSS or BPRS scores, and among 5 antipsychotics (also including amisulpride, clozapine, paliperidone, and risperidone) associated with significantly lower rates of all-cause discontinuation.Citation34 This latter finding is hypothesized to be related, at least in part, to the emergence of improved insight during olanzapine treatment and subsequent downstream effects.Citation52

Beyond acute treatment: long-term outcomes

Up to 50% of patients with schizophrenia do not adhere to treatment in the short term, and approximately 75% experience recurrent relapse and continued disability.Citation53 As such, long-term treatment of schizophrenia is focused on sustaining symptom remission, maintaining (or improving) the patient’s level of functioning and quality of life, and supporting patient adherence to recommended treatment over time.Citation11 The long-term effectiveness of olanzapine has been established across a number of long-term outcome domains, including relapse prevention (defined as preventing or delaying recurrence of acute exacerbations of the symptoms of schizophrenia, assessed by rates of hospitalization),Citation54 robustness of response (defined as the relative absence of active schizophrenia symptoms during long-term treatment, assessed by rates of remission),Citation55 and durability of therapy (defined as the relative duration of time the patient remains on any given antipsychotic, commonly assessed by all-cause discontinuation and subjective response).Citation56,Citation57

One of the initial studies assessing the long-term efficacy of olanzapine was an extension studyCitation58 for patients who responded well to treatment in olanzapine’s pivotal acute-phase trials.Citation43Citation46 Time to relapse, defined as hospitalization for psychopathology, was significantly lower for olanzapine than haloperidol, with a 1-year risk of relapse of 20% compared with 28% for haloperidol.Citation58 Data from 2 large studies comparing the efficacy of first- and second-generation antipsychotics, the Clinical Antipsychotic Trials of Intervention Effectiveness (CATIE)Citation56 study and the Schizophrenia Outpatient Health Outcomes (SOHO) study,Citation59 consistently found that olanzapine had lower rates of hospitalization for exacerbation of schizophrenia. Further, in the CATIE study, the rate of remission, based on the Andreasen Criteria,Citation55 was highest for olanzapine (12% vs 6–8% with other antipsychotics).Citation60 Olanzapine also had the highest rate of remission, based on CGI scores, in the SOHO study.Citation61

In the long-term management of schizophrenia, it is important to understand the significance patients and providers place on the benefits and risks of different antipsychotics when making treatment decisions. Surveys have found that improvements in the positive symptoms of schizophrenia are ultimately more important to both healthcare providers and patients than avoiding adverse side effects of antipsychotics such as weight gain and extrapyramidal symptoms,Citation57,Citation62 although more severe adverse events may shift this opinion in the other direction. Likewise, in an analysis of data from 32 schizophrenia trials, discontinuation of medication was largely driven by lack of efficacy rather than intolerability.Citation63 Therefore, a key finding supportive of the distinctly favorable efficacy of olanzapine is its durability of treatment. As shown in , time to all-cause discontinuation is consistently longer for olanzapine compared with other antipsychotics.Citation35,Citation40,Citation56,Citation59 In CATIE, only 15% of patients treated with olanzapine discontinued treatment due to lack of efficacy, as compared with 24–28% of patients treated with other antipsychotics.Citation56 Further, a naturalistic study comparing olanzapine, risperidone, and haloperidol found better subjective response and compliance in patients treated with olanzapine compared with the other antipsychotics.Citation64 Collectively, these data suggest that patients taking olanzapine remain on treatment longer, despite the drug’s known side effects, than do patients taking other antipsychotics, potentially owing to olanzapine’s superior efficacy.

Furthermore, post hoc analysis of data from the CATIE study identified a significant difference in favor of olanzapine for hostility in schizophrenia,Citation36 consistent with the post hoc analysis of hostility in first-episode patients from the EUFEST study.Citation37

Suboptimal treatment response

Treatment resistance, commonly defined as little or no symptomatic response to at least 2 previous antipsychotics, occurs in approximately 10–30% of patients with schizophrenia.Citation11 This definition is used as the criteria for recommending treatment with clozapine.Citation65 It is also not uncommon for patients to experience partial response to a prescribed antipsychotic with a clinical status that lies somewhere between full responder and treatment resistance.Citation65,Citation66 The management of these patients is a major challenge and constitutes a serious public health concern given the associated social and economic burden.Citation67

The use of olanzapine in patients with treatment-resistant schizophrenia or suboptimal response has been evaluated in several studies.Citation68Citation74 In a study of patients with suboptimal treatment response randomized to olanzapine, clozapine, risperidone, or haloperidol, improvements in global psychopathology were significantly greater at week 14 with olanzapine compared with haloperidol.Citation69 In phase 2E of the CATIE study, which included patients who discontinued from phase 1 primarily due to lack of efficacy, no significant differences were found between clozapine and olanzapine with regard to all-cause discontinuation or improvements in PANSS total score at 3 months, with clozapine being superior to treatment with either quetiapine or risperidone.Citation70 Other studies in patients with treatment-resistant schizophrenia or suboptimal treatment response have also reported similar reductions with olanzapine and clozapine in PANSS total score, CGI severity score, and BPRS total score.Citation69,Citation71Citation73

In many of the aforementioned studies, olanzapine dosages above the maximum recommended dose of 20 mg/day were used in treatment-resistant patients.Citation13 This is not without controversy, as doses of 40 mg/day did not confer an advantage over lower doses in a large (N=599) randomized clinical trial of patients with suboptimal response to their current treatment (but who were not defined as treatment resistant).Citation75

Safety

The safety profile of olanzapine has been reviewed extensively elsewhere.Citation3,Citation76Citation79 In brief, second-generation antipsychotics are generally better tolerated than are the first-generation antipsychotics with regard to antipsychotic-induced movement disorders.Citation33 However, many of these drugs are associated with clinically significant metabolic disturbances, including increased risk of diabetes, dyslipidemia, and weight gain.Citation80 Olanzapine has one of the highest risks for metabolic syndrome among the second-generation atypical antipsychotics, especially during long-term treatment and with the administration of high doses, in accordance with a report from professional associations of psychiatrists, endocrinologists, and diabetologists.Citation81 In particular, hypertriglyceridemia can represent a sensitive marker of insulin resistance, a condition that induces obesity, especially central obesity, a primary risk factor for metabolic syndrome.Citation82 In a recent animal model study, olanzapine exacerbated atherosclerosis by deregulating hepatic lipid metabolism and worsening hyperlipidemia and aortic inflammation.Citation83 Antagonistic effects of olanzapine at 5-HT2c, histaminergic H1, and muscarinic M3 receptors have been implicated in olanzapine-induced weight gain. Although a 2010 meta-analysisCitation84 reported significantly less weight gain when adjunctive metformin, fenfluramine, sibutramine, topiramate, and reboxetine versus placebo were added on to olanzapine therapy, and more recent studies support the efficacy of betahistine,Citation85Citation88 to date, data are insufficient to recommend the routine use of any of these medications to mitigate olanzapine-induced weight gain.Citation84,Citation85

Olanzapine’s adverse effects on glucose and lipid metabolism, weight, and body composition are of serious concern and require close monitoring.Citation77 In an analysis of 13 short-term, placebo-controlled olanzapine monotherapy studies (median exposure: 6 weeks), the average weight gain with olanzapine was 2.6 kg (5.7 lb) compared to a weight loss of 0.3 kg (0.6 lb) with placebo. The percentage of patients who gained at least 7% of their baseline weight was 22% with olanzapine versus 3% with placebo.Citation1 In long-term studies (at least 48 weeks), 64%, 32%, and 12% of patients gained 7%, 15%, or 25% or more of their baseline body weight, respectively.Citation1 Shifts from normal/borderline to abnormal plasma glucose or lipid variables have also been observed and are a concern.Citation77,Citation89 Several guidelines and publications have included strategies to help mitigate these side effects, such as with concomitant off-label use of metformin, as well as greater attention to promoting positive lifestyle modifications with respect to diet and exercise.Citation9,Citation80,Citation90Citation92 However, there are currently no FDA-approved treatments indicated to mitigate the metabolic dysregulation, including weight gain, associated with olanzapine or any other currently available atypical antipsychotics.

Despite these well-known adverse metabolic effects, olanzapine does have some safety advantages relative to other antipsychotics. Olanzapine is associated with a lower incidence of extrapyramidal symptoms than typical and some atypical antipsychotics,Citation93,Citation94 an important cause of noncompliance and treatment discontinuation.Citation95 Further, agranulocytosis, a potentially fatal adverse event that limits clozapine’s use,Citation96 was not reported in any of the more than 2000 patients receiving olanzapine in the 4 pivotal efficacy and safety trials.Citation43Citation46 Olanzapine also has generally little impact on prolactin compared with some typical and atypical antipsychotics.Citation33 A significantly lower proportion of patients had elevations in prolactin during treatment with olanzapine compared with haloperidol (18–35% vs 82%)Citation45 or with risperidone (51% vs 94%).Citation97 Although prolactin effects with olanzapine are likely dose related,Citation75 increases in prolactin associated with olanzapine were generally mild, transient, and of lesser magnitude than haloperidol and risperidone.Citation44Citation46,Citation97 Several studies have subsequently confirmed a favorable impact of olanzapine on prolactin levels.Citation98Citation100 As a result, patients taking olanzapine may be at reduced risk for complications of hyperprolactinemia, including gynecomastia, galactorrhea, menstrual irregularities, and sexual dysfunction, compared with other antipsychotics.Citation101 Lastly, olanzapine treatment was associated with a low incidence of seizures, 22/2500 (0.9%), during premarketing studies.Citation1 Based on this finding, the Epilepsy Foundation lists olanzapine as 1 of 3 antipsychotics recommended on the basis of both epileptogenesis and side effect profile.Citation102

Summary

Two decades ago, the safety risks associated with olanzapine were not as well understood as they are today. Now, olanzapine is no longer the first choice of treatment for patients with schizophrenia. Even so, olanzapine remains widely used, lending indirect support to the hypothesis that olanzapine’s effectiveness differs from other antipsychotic treatment options. This commentary aims to highlight the significant body of data supporting the hypothesis that olanzapine may be more effective than other non-clozapine antipsychotics currently considered the first choice of treatment for schizophrenia. Although our focus was to highlight olanzapine’s unique efficacy qualities, we acknowledge that olanzapine’s efficacy is not a universal finding across all studies; however, for the purposes of the current commentary, it was not our intention to conduct an exhaustive meta-analysis. The relative efficacy seems to depend, in part, on the clinical situation in which it is used. Collectively, these data suggest that if efficacy alone were the only consideration, olanzapine may be a preferred first-line treatment option for patients with chronic schizophrenia requiring effective long-term treatment (ie, for prevention of relapse, robustness of response, and treatment persistence aspects) and in those with suboptimal responses during treatment with other antipsychotics. Despite the known risk for metabolic side effects, including weight gain, olanzapine continues to be prescribed due to the overall favorable drug profile. As with any treatment, selection of the most appropriate antipsychotic agent for patients with schizophrenia must be individualized and thoughtfully considered, taking into account both the benefits and risks associated with its use. Therefore, the development of interventions that offer the efficacy of olanzapine but reduce the weight gain and potential long-term complications associated with its use could address a major unmet need in the treatment of schizophrenia. These interventions could include agents with new mechanisms of action or single-pill combination products that contain both olanzapine and agent(s) that could potentially mitigate olanzapine’s propensity for weight gain to serve as potential alternatives in clinical situations in which olanzapine would have been considered.

Abbreviations

BPRS, Brief Psychiatric Rating Scale; CATIE, Clinical Antipsychotic Trials of Intervention Effectiveness; CGI, Clinical Global Impression; EUFEST, European First-Episode Schizophrenia Trial; FDA, US Food and Drug Administration; NNT, number needed to treat; PANSS, Positive and Negative Syndrome Scale; SOHO, Schizophrenia Outpatient Health Outcomes.

Disclosures

LC has, in the past 5 years, engaged in collaborative research with, or received consulting or speaking fees, from: Acadia, Alexza, Alkermes, Allergan, AstraZeneca, Avanir, Boehringer Ingelheim, Bristol-Myers Squibb, Eli Lilly, Forum, Genentech, Intra-Cellular Therapeutics, Janssen, Jazz, Lundbeck, Merck, Medivation, Mylan, Neurocrine, Novartis, Noven, Otsuka, Pfizer, Indivior/Reckitt Benckiser, Reviva, Shire, Sunovion, Takeda, Teva, Valeant, Vanda. In the past 12 months, consultant: Acadia, Alkermes, Allergan, Indivior, Intra-Cellular Therapeutics, Janssen, Lundbeck, Merck, Neurocrine, Noven, Osmotica, Otsuka, Pfizer, Shire, Sunovion, Takeda, Teva, Vanda. In the past 12 months, speaker: Acadia, Alkermes, Allergan, Janssen, Lundbeck, Merck, Neurocrine, Otsuka, Pfizer, Shire, Sunovion, Takeda, Teva. Stocks (small number of shares of common stock): Bristol-Myers Squibb, Eli Lilly, J & J, Merck, Pfizer purchased >10 years ago. Royalties: Wiley (Editor-in-Chief, International Journal of Clinical Practice), UpTo Date (reviewer), Springer Healthcare (book). JPM serves on advisory boards for Neurocrine and Alkermes. MST, DM, and PJW are full-time employees of Alkermes, Inc., and may own stock in the company.

Acknowledgments

This study was sponsored by Alkermes, Inc. Medical writing and editorial support was provided by Peloton Advantage, LLC, an OPEN Health company, Parsippany, NJ, and funded by Alkermes, Inc. Alkermes, Inc. is developing a combination product of olanzapine and samidorphan for the treatment of schizophrenia, and has funded the development of this manuscript.

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