Plain Language Summary
Antipsychotic choice for individuals with schizophrenia or bipolar I disorder (BD-I) requires balancing efficacy with tolerability. For example, while olanzapine is highly efficacious, it is associated with weight gain and/or changes in how the body regulates glucose and lipids. Since the body's natural opioid system is involved in regulating weight and metabolism, combining samidorphan with olanzapine is a potential strategy to address olanzapine-associated weight and metabolic side effects. We summarize clinical data for OLZ/SAM, a combination of olanzapine and the opioid receptor-blocking compound samidorphan, recently approved in the United States for the treatment of adults with schizophrenia or BD-I. In pharmacokinetic studies, plasma concentrations of olanzapine were similar when administered as OLZ/SAM or as the branded product, Zyprexa, with dose-proportional increases in concentration with increasing doses. Adjunctive OLZ/SAM did not affect lithium or valproate pharmacokinetics. Samidorphan's pharmacokinetic profile supports once-daily dosing in combination with olanzapine as OLZ/SAM. In clinical studies, OLZ/SAM provided similar antipsychotic efficacy as olanzapine in patients with schizophrenia, with sustained symptom control during long-term treatment. OLZ/SAM treatment resulted in significantly less weight gain versus olanzapine; weight remained stable with long-term treatment. The safety profile of OLZ/SAM was generally consistent with that of olanzapine, except for less weight gain. Owing to samidorphan's opioid antagonist effects, OLZ/SAM is contraindicated in patients using opioids or undergoing acute opioid withdrawal. Lastly, because antipsychotic-associated weight gain is independent of disease state, OLZ/SAM provides a new treatment option for patients with either schizophrenia or BD-I that balances efficacy with a reduced risk of weight gain.
Introduction
Schizophrenia and bipolar I disorder (BD-I) are chronic, complex psychiatric illnesses associated with substantial functional impairment and disability,1–3 high rates of comorbid conditions,4,5 and a high risk of suicide.6,7 Both are associated with lower life expectancy, attributable in part to causes such as suicide, but also to higher rates of cardiovascular comorbidities.5,8,9 While antipsychotics are the cornerstone of treatment in schizophrenia, and second-generation antipsychotics are commonly prescribed in the treatment of BD-I either as monotherapy or in combination with mood stabilizers,10,11 they are often accompanied by adverse side effects12 that may contribute to suboptimal adherence and/or treatment discontinuation or to emergent cardiometabolic comorbidities.13,14 Despite a number of available antipsychotics, there remains a need for effective therapies with acceptable tolerability profiles that support long-term use.15–17
Based on data from clinical trials,18,19 real-world settings,20–22 meta-analyses,23,24 and pooled analyses,25 olanzapine is one of the most effective antipsychotics for the treatment of schizophrenia.26,27 Olanzapine also effectively treats manic or mixed episodes associated with BD-I and reduces relapse risk during maintenance treatment.28–30 While olanzapine's efficacy is well established,18,23,28,29,31 the clinical utility of olanzapine has been hampered by the risk of substantial weight gain and metabolic effects,32–38 such as elevations in blood glucose and lipid concentrations, waist circumference increases, and development of metabolic syndrome.36,37,39 Approximately 80% of patients gain at least 5 kg with long-term olanzapine treatment,40 and this weight gain can continue over several months or even years.40–43 In studies lasting at least 48 weeks, 64% of patients taking olanzapine gained at least 7% of their baseline body weight, and 12% gained at least 25% of their baseline body weight.40 Increases in waist circumference, reflecting central fat accumulation, are associated with higher cardiometabolic and mortality risks.44,45 Consistent with weight gain and/or increases in waist circumference, long-term olanzapine use increases the risk of developing diabetes or hyperlipidemia,46–49 as well as cardiovascular disease.45
The endogenous opioid receptor system is involved in the regulation of weight gain and metabolism.50–55 Opioid receptors exist in both the central nervous system and in the periphery (eg, the pancreas, muscle, and liver),56–58 making the opioid system a potential therapeutic target for addressing antipsychotic-associated weight gain. A combination of olanzapine and the opioid receptor antagonist samidorphan (OLZ/SAM; Lybalvi, Alkermes, Inc.) was recently approved by the US Food and Drug Administration (FDA) for the treatment of adults with schizophrenia or BD-I.59 OLZ/SAM provides the antipsychotic efficacy of olanzapine, but with less weight gain.60–62 OLZ/SAM is being developed to include 5-, 10-, 15-, or 20-mg doses of olanzapine (similar to dose ranges approved for adults with schizophrenia or BD-I)40 with a fixed 10-mg dose of samidorphan in a single tablet.
Overview of Clinical Trials
The effects of OLZ/SAM on weight gain and body composition have been previously characterized in preclinical studies in rats and nonhuman primates.63 In this narrative review, we summarize the clinical data for OLZ/SAM and describe its overall efficacy and safety profile.
The clinical development program of OLZ/SAM includes 18 studies: 10 Phase 1,64–72 two Phase 2,60,73 three randomized, double-blind Phase 3 (Study A307; NCT03187769),61,62 and three open-label, long-term, phase 3 safety extension studies (Study A308; NCT03201757)74,75 (Supplemental Table 1). These studies provided information on the pharmacokinetics,64–69 safety,70,74,75 and efficacy (both antipsychotic efficacy as well as mitigation of weight gain relative to olanzapine [ie, weight efficacy])60–62 of OLZ/SAM.
Pharmacology and Mode of Action of Samidorphan
The body's endogenous opioid system is involved in the regulation of weight and metabolism.50–55 Samidorphan is an opioid receptor antagonist that binds to and blocks opioid receptors.76,77 The exact mechanism(s) by which samidorphan mitigates olanzapine-associated weight gain is unknown. Samidorphan has unique binding properties, functional activity, and pharmacokinetic attributes that differentiate it from other opioid antagonists.77–79 It is thought that in the central nervous system, opioid receptor blockade may reduce the rewarding effects of stimuli in systems where aberrant opioid signaling may contribute to motivational dysregulation, such as in behavioral addiction (eg, binge-eating or gambling).80–82 In the periphery, blockade or genetic ablation of opioid receptors alters fat accumulation and glucose utilization, as well as glucose homeostasis.63,83–85 Therefore, the weight-mitigating properties of samidorphan in combination with olanzapine may be mediated through opioid receptor blockade in both central and peripheral compartments.
Pharmacokinetics and Pharmacodynamics
The pharmacokinetics of oral olanzapine and samidorphan have been extensively characterized alone and in combination.64–67,71,79,86,87 Samidorphan has an oral bioavailability of 69% and a half-life of approximately 7 to 10 hours,79,87 making it suitable for once-daily dosing in combination with olanzapine. Combining olanzapine with samidorphan did not affect the pharmacokinetics of either drug.66,71 After once-daily dosing of OLZ/SAM at doses of 10/10 mg to 20/10 mg, steady-state olanzapine exposures increased dose proportionally.66 In addition, consuming a high-fat, high-calorie meal prior to taking OLZ/SAM had no clinically relevant effects on the pharmacokinetics of olanzapine or samidorphan; therefore, OLZ/SAM can be taken with or without food.67
The olanzapine component of OLZ/SAM was bioequivalent to branded olanzapine oral tablets (Zyprexa, Eli Lilly and Company; Supplemental Figure 1A).64 Furthermore, coadministration of OLZ/SAM with lithium or valproate had no clinically significant effect on systemic exposures of lithium or valproate (Supplemental Figures 1B and C).68
Drug-drug interactions known to be important for olanzapine should be considered important for OLZ/SAM as well.40 In addition, coadministration of OLZ/SAM with rifampin, a strong inducer of cytochrome P450 [CYP]3A4 and an inducer of uridine 5′-diphospho-glucuronosyltransferase [UGT] enzymes, decreased the total systemic exposure of olanzapine and samidorphan by 48% and 73%, respectively.65 This effect is consistent with the known metabolic pathways for olanzapine (primarily via UGT-mediated direct glucuronidation and CYP-mediated oxidation)88,89 and for samidorphan (predominately mediated by CYP3A4).79 Therefore, concomitant use of OLZ/SAM with strong CYP3A4 inducers, such as rifampin, is not recommended.59
Subjects with severe renal impairment had up to a 2.3-fold increase in the total systemic exposure of olanzapine and samidorphan, while subjects with moderate hepatic impairment had up to 1.7-fold increases in total systemic exposure of olanzapine and samidorphan.69 No dose adjustment is needed for OLZ/SAM in patients with hepatic or renal impairment, but OLZ/SAM is not recommended for patients with end-stage renal disease.59
Based on a thorough QT study conducted in patients with schizophrenia, OLZ/SAM, at doses up to a supratherapeutic dose of 30/30 mg, had no clinically relevant effect on electrocardiogram parameters, including QT interval.70 Because no formal QT study had been conducted previously with olanzapine, this study fills an important information gap and provides further clinical context for the safety of OLZ/SAM treatment. Supplemental Table 1 summarizes these data, as well as data from other pharmacokinetic and pharmacodynamic studies.
The abuse potential of samidorphan has been assessed90 in a study with naltrexone, an opioid antagonist with no abuse potential,91 serving as a negative control. Samidorphan's score on a drug-liking visual analog scale was similar to both placebo and naltrexone, indicating that samidorphan has no abuse potential.90 Furthermore, at doses of 10 mg and 30 mg, samidorphan had significantly lower drug-liking scores compared with those of the positive controls, oxycontin and pentazocine, which are scheduled drugs with known abuse potential.
Efficacy and Safety Overview
The antipsychotic efficacy of OLZ/SAM was primarily evaluated in a pivotal phase 3 study in patients with an acute exacerbation of schizophrenia,61 while weight efficacy was primarily evaluated in a pivotal phase 3 study of stable outpatients with schizophrenia.62 Additional studies support the antipsychotic60,62 and weight mitigation60 efficacy of OLZ/SAM. The durability of antipsychotic and weight mitigation effects, as well as long-term effects on metabolic parameters, were derived from two 52-week, open-label, extension studies.74,75 These findings are summarized below; additional detailed descriptions can be found in Tables 1 and 2.
Table 3 presents a summary of adverse events (AEs) and other key safety observations. In addition to collecting safety information from different populations of patients with schizophrenia (ie, acutely ill inpatients and stable outpatients), OLZ/SAM safety information was also derived from a study in patients with schizophrenia and comorbid alcohol use disorder.73 In general, the AE profile for OLZ/SAM was similar to that of olanzapine, except for less weight gain. Because samidorphan is an opioid antagonist, concomitant use of opioids was exclusionary in the OLZ/SAM clinical trials, and OLZ/SAM is contraindicated in patients using opioids and in those undergoing acute opioid withdrawal.59
Specific Study Results Related to Antipsychotic Effects
The phase 3 ENLIGHTEN-1 study evaluated the antipsychotic efficacy of OLZ/SAM in patients experiencing an acute exacerbation of schizophrenia requiring inpatient treatment. Treatment with OLZ/SAM resulted in significant improvements in symptoms compared with placebo at week 4, as measured by changes in Positive and Negative Syndrome Scale (PANSS) total scores from baseline61 (Figure 1A, Table 2). Improvement in PANSS scores with OLZ/SAM relative to placebo was similar to that observed with olanzapine; Figure 1A, Table 2). Antipsychotic efficacy of OLZ/SAM relative to placebo was also supported by improvements in Clinical Global Impression-Severity (CGI-S) scores61 (Table 2). The inclusion of samidorphan in OLZ/SAM did not negatively impact the antipsychotic efficacy of olanzapine.59
The efficacy of OLZ/SAM in controlling symptoms of schizophrenia was further supported by findings from ENLIGHTEN-2,62 a pivotal study assessing weight gain as the primary endpoint. In that study, 24 weeks of treatment with either OLZ/SAM or olanzapine resulted in similar improvements in PANSS total and CGI-S scores (Figure 1B; Table 2). Details and key findings on these and other studies assessing antipsychotic effects of OLZ/SAM are provided in Table 2 and in Figure 1B and C. The long-term effects of OLZ/SAM are summarized below.
Specific Study Results Related to Effects on Weight, Waist Circumference, and Metabolic Parameters
The 24-week phase 3 ENLIGHTEN-2 study primarily assessed the weight profile of OLZ/SAM versus olanzapine in stable outpatients with schizophrenia (Table 1).62 Patients treated with OLZ/SAM gained significantly less weight than those treated with olanzapine (Table 2).62 Figure 2A depicts the mean percent body weight changes in this study, which were similar to the findings observed in a phase 2 dose-finding study (Figure 2B).60 In the 24-week study, the least squares (LS) mean percent weight change from baseline to the end of treatment was 4.2% with OLZ/SAM versus 6.6% with olanzapine, yielding an LS mean difference of −2.4%.62 In the phase 2 study, the LS mean percent change from baseline in weight at week 12 was 2.6% with OLZ/SAM versus 4.1% with olanzapine, yielding an LS mean difference between groups of −1.5%.60 In both studies, patients treated with olanzapine and OLZ/SAM had similar weight gain for the first 4 to 6 weeks. With OLZ/SAM, weight gain stabilized thereafter, whereas patients who received olanzapine continued to gain weight throughout the remainder of the treatment period.60,62 In ENLIGHTEN-2, this resulted in an alteration of the weight gain trajectory (eg, the distribution curve of weight gain was shifted for OLZ/SAM compared with olanzapine, indicating that fewer patients gained weight across a wide range of percent weight gain cutoffs; Figure 2C).
In addition to assessing differences in mean percent weight gain, the ENLIGHTEN-2 study assessed the proportion of patients gaining at least 10% of their body weight as a coprimary endpoint. The risk of gaining 10% or more of body weight from baseline was reduced by 50% with OLZ/SAM compared with olanzapine. In psychiatric practice, a weight gain of 7% or more is considered to be clinically significant.92,93 As with the 10% weight gain threshold, the odds of gaining 7% body weight or more from baseline at week 24 was also reduced by 50% for OLZ/SAM compared with olanzapine (Table 2; Figure 2C). Based on a number needed to treat (NNT) analysis of the proportion of patients with clinically significant weight gain at week 24, the NNT for OLZ/SAM versus olanzapine was 7 and 8 for the ≥7% and ≥10% weight gain thresholds, respectively (Table 2). Generally, NNTs less than 10 denote a clinically meaningful effect size, and the lower the NNT value, the better the treatment response.94,95
OLZ/SAM was also associated with smaller increases in waist circumference compared with olanzapine (Table 2; Figure 3A),62 which occurred as early as week 1. As with the distribution curve for weight gain, the distribution curve for waist circumference increases was also shifted. Fewer patients had waist circumference increases across a range of cutoff values in comparison to olanzapine. The risk of experiencing a 5-cm increase in waist circumference was 50% lower for patients treated with OLZ/SAM versus olanzapine (Table 2; Figure 3B). This is clinically significant, as a 5-cm or greater increase in waist circumference is associated with an increased risk of all-cause mortality and cardiovascular disease.44 The NNT for the proportion of patients with a waist circumference increase of ≥5 cm in the OLZ/SAM group versus the olanzapine group was 6 (Table 2).
Changes in metabolic laboratory parameters in patients treated with olanzapine or OLZ/SAM in ENLIGHTEN-2 were generally small and were similar between groups (Figure 4A and B). In addition, there were little differences between the two treatment groups in metabolic parameter changes considered to be of potential clinical significance, based on commonly used thresholds (Supplemental Table 2). In the context of metabolic laboratory parameters, sustained shifts are more clinically relevant than single excursions resulting from visit-to-visit variability or inconsistencies in fasting status. Across the fasting lipid and glycemic parameters, the incidence of sustained shifts was substantially lower than the incidence of anytime shifts and was similar for both groups (Supplemental Table 2).
Adverse Events in Phase 3 Efficacy Trials
The AE profile of OLZ/SAM was consistent with the known AE profile of olanzapine. In ENLIGHTEN 1, adverse events that occurred at least twice the rate of placebo with OLZ/SAM included increased weight, somnolence, dry mouth, and headache; these were similar in type and frequency to those reported in the olanzapine group (Table 3).61 In ENLIGHTEN-2, the most commonly reported AEs (in ≥10% of patients) associated with treatment were increased weight, somnolence, dry mouth, and increased appetite (Table 3).62 In both studies, rates of serious AEs and AEs leading to discontinuation were low and were similar between groups (Table 3).
Long-Term Treatment Effects
The long-term effects of OLZ/SAM on safety, tolerability, and symptoms of schizophrenia were investigated in two open-label, phase 3, 52-week extension studies, ENLIGHTEN-1-EXT and ENLIGHTEN-2-EXT74,75 that enrolled patients who completed the respective antecedent phase 3 studies.61,62
Long-term tolerability was evidenced by low rates of AEs that led to treatment discontinuation: in both extension studies, the rate of discontinuation due to an AE was ≤6%.74,75 Additionally, neither extension study reported any clinically meaningful changes over time in hematology, biochemistry, vital signs, or electrocardiogram parameters. The incidence of extrapyramidal symptoms and suicidality was low in both long-term extension studies (Table 3).
Importantly, OLZ/SAM was effective in controlling symptoms of schizophrenia over 52 weeks of treatment (Table 2; Figure 5A and B), as evidenced by sustained improvements in PANSS and CGI-S scores over time. However, in contrast to what has been described with long-term olanzapine treatment, weight remained stable during open-label OLZ/SAM treatment in both long-term extension studies (Figure 5C and D).74,75 The observed long-term changes in weight were consistent with weight changes observed with other second-generation antipsychotics, although comparisons to other antipsychotics must be interpreted cautiously owing to different study objectives, designs, and analyses, and to the lack of comparators in these studies.96–99 Waist circumference also remained stable during long-term OLZ/SAM treatment.75
In general, long-term changes in metabolic laboratory parameter values were small and remained stable (Supplemental Table 3).74,75 In addition, there was little change in glycosylated hemoglobin (hemoglobin A1c) values, suggesting that glycemic control was maintained with long-term OLZ/SAM treatment.74,75
Results from numerous long-term treatment studies have indicated that patients discontinue olanzapine less frequently, or take longer to do so, compared with most other antipsychotics, and this is attributed to its efficacy in treating and controlling symptoms.18–20 In the OLZ/SAM extension studies, the effectiveness of OLZ/SAM in controlling symptoms of schizophrenia was supported by the low rates of all-cause discontinuation, with nearly two thirds of patients (66.1% in ENLIGHTEN-1-EXT; 63.0% in ENLIGHTEN-2-EXT) completing the respective treatment periods.74,75 This completion rate is higher than what is typically observed in similar 1-year extension studies with other antipsychotics (ie, brexpiprazole, cariprazine, and lurasidone), which average less than a 50% completion rate.96–100 Time to all-cause discontinuation is presented graphically for each extension study in Figure 5E and F.
Results from the long-term extension studies should be considered in light of some limitations: (1) these were single-arm, open-label studies (ie, randomization was lost at study entry) without comparators, (2) the interpretation of long-term data may be impacted by missing data due to patient discontinuations over the long study duration, and (3) the studies may have selected for patients who responded favorably to OLZ/SAM treatment in the preceding studies.
Other Populations
The efficacy, safety, and tolerability of OLZ/SAM compared with olanzapine have also been examined in patients with schizophrenia and comorbid alcohol use disorder.73,101 In this study, while treatment with OLZ/SAM or olanzapine resulted in similar times to a composite endpoint of worsening illness and there was no added benefit of OLZ/SAM compared with olanzapine with regard to drinking behaviors, patients in both treatment groups had reduced alcohol use and improved psychiatric symptoms. Overall, OLZ/SAM treatment for up to 9 months was generally well tolerated in this patient population (safety data are summarized in Table 3). In addition, treatment with OLZ/SAM resulted in similar effectiveness to olanzapine in controlling symptoms of schizophrenia, based on changes in PANSS total scores over 60 weeks (Figure 1D).73
Evidence for the Use of OLZ/SAM in Bipolar I Disorder
OLZ/SAM is approved in the United States for treatment of manic or mixed episodes in BD-I, as monotherapy or as an adjunct to lithium or valproate, as well as for maintenance monotherapy in BD-I. The efficacy of OLZ/SAM in the treatment of adult patients with BD-I has been established based on adequate and well-controlled studies of orally administered olanzapine.40 Additionally, the olanzapine component of OLZ/SAM was shown to be bioequivalent to olanzapine in the branded product, Zyprexa.64 Furthermore, treatment with OLZ/SAM had no clinically significant effect on lithium or valproate pharmacokinetics.68 In schizophrenia patients, samidorphan did not negatively affect the efficacy of olanzapine when administered as OLZ/SAM.59 Finally, OLZ/SAM consistently mitigated olanzapine-associated weight gain across a range of species/populations (eg, rodents, non-human primates, healthy individuals, and patients with schizophrenia),60,62,71 and antipsychotic-associated weight gain and metabolic dysregulation occur independently of disease.102–104
Clinical Perspectives
Most second-generation antipsychotics used in the context of serious mental illness are associated with weight gain,14 which may lead to detrimental effects in patients, including lower self-esteem and the potential for negative outcomes when patients do not fill prescriptions or take their medication.105–108 Additionally, excess weight gain may exacerbate cardiometabolic risk factors,45,109 especially in people with serious mental illness, including those with schizophrenia or BD-I.110,111 This is partially attributable to the rising prevalence of obesity in the general population, and in patients with schizophrenia and BD-I in particular.112–114 Additionally, patients with serious mental illness have an increased prevalence of risk factors for cardiovascular disease relative to the general population, which contributes to excess early mortality in these patients.115–117
Up until now, there have not been any FDA-approved agents that address the specific issue of antipsychotic-induced weight gain. Several potential strategies have been investigated to reduce or mitigate antipsychotic-associated weight gain, including both nonpharmacologic and pharmacologic interventions. With some exceptions, studies of pharmacologic options have mostly assessed weight reduction in patients who have already experienced weight gain, rather than investigating the prevention of antipsychotic-associated weight gain from the outset.118
An example of an "off-label" pharmacologic intervention that has been extensively studied is adjunctive metformin. In a meta-analysis of 32 randomized studies evaluating 15 pharmacologic agents for minimizing or attenuating antipsychotic-associated weight gain, metformin outperformed other agents versus placebo.119 In the 7 trials (lasting 6 to 16 weeks) informing that analysis, metformin treatment was associated with a weight loss of −2.94 kg versus placebo in patients who had already experienced antipsychotic-associated weight gain.119 However, this meta-analysis did not detect a weight change difference versus placebo when metformin was initiated concomitantly with antipsychotics.119 In an updated systematic review and meta-analysis on this topic that included 10 metformin studies,118 a mean 3.17-kg reduction in weight versus placebo was observed across studies. However, 3 of the 4 studies that investigated the prevention of antipsychotic-associated weight gain with metformin were negative,120–122 while one was positive in patients who completed the study.123
For other pharmacologic interventions that have been assessed for minimizing antipsychotic-associated weight, there is inadequate evidence of effect, no clinical benefit, or an AE profile that offsets any potential benefits for reducing existing antipsychotic-associated weight gain.124 Current guidelines suggest that the use of such agents should be considered in the context of limited long-term data and the potential for AEs.11 Because OLZ/SAM is a single tablet, concerns regarding adding medications onto an existing regimen to reduce weight (eg, AEs, drug-drug interaction effects, and pill burden) may be avoided.
Appropriate antipsychotic selection for an individual patient requires that clinicians consider the benefits and risks of the treatment, as well as bearing in mind an individual patient's characteristics and treatment goals. For patients who may benefit from the established efficacy of olanzapine, clinicians have to balance choosing this highly effective therapy for their patient while risking other safety concerns, including the risk of significant weight gain and its associated long-term health consequences.32,33 OLZ/SAM may be an option in this regard, as it provides similar efficacy compared with olanzapine but with significantly less weight gain. The weight-mitigating effects of OLZ/SAM relative to olanzapine have been replicated in at least 2 studies and is supported by long-term data extending over 1 year.41,125,126 For certain patients who are at greater risk of antipsychotic-associated weight gain, including those with a lower body mass index41,125,126 and those with less prior exposure to antipsychotics (eg, patients early in illness), OLZ/SAM may also be useful.127,128 However, it should be noted that, because OLZ/SAM contains the opioid antagonist samidorphan, it should not be used in patients using opioids or in those undergoing acute opioid withdrawal.59
One ongoing OLZ/SAM study will provide additional long-term safety and tolerability data (NCT03201757). Another ongoing study (NCT03187769; ENLIGHTEN-Early) is assessing treatment effects of OLZ/SAM in patients early in their disease course with schizophrenia, schizophreniform disorder, or BD-I.
Conclusions
OLZ/SAM provides the established efficacy of olanzapine while mitigating olanzapine-associated weight gain through opioid receptor blockade. Studies to date have characterized the pharmacokinetics, safety, and efficacy (both antipsychotic and weight efficacy) of OLZ/SAM. Clinical pharmacokinetic data indicate the feasibility of once-daily dosing with OLZ/SAM and provide support for the use of OLZ/SAM in BD-I based on bioequivalence of OLZ/SAM to olanzapine and the lack of clinically significant effects of adjunctive OLZ/SAM on lithium or valproate pharmacokinetics. The antipsychotic and weight gain mitigation efficacy of OLZ/SAM was observed in multiple studies; these effects were durable and were maintained during open-label treatment. Overall, data from more than 1600 patients in studies of differing designs, durations, and treatment populations indicate an AE profile for OLZ/SAM that is similar to that of olanzapine, with the exception of less weight gain. Taken together, these data support the recent approval of OLZ/SAM as a clinically useful option for patients with schizophrenia or BD-I and its suitability for long-term treatment.
Abbreviations
1° EP, prespecified primary endpoint; 2° EP, prespecified secondary endpoint; AE, adverse event; ANCOVA, analysis of covariance; AUC∞, area under the plasma concentration-time curve from time 0 to infinity; BD-I, bipolar I disorder; CGI-S, Clinical Global Impression-Severity; Cmax, maximum plasma concentration; CYP, cytochrome P450 enzyme; ENLIGHTEN-1-EXT, 52-week extension study of ENLIGHTEN-1; ENLIGHTEN-2-EXT, 52-week extension study of ENLIGHTEN-2; HbA1c, hemoglobin A1c; HDL, high-density lipoprotein; LDL, low-density lipoprotein; LS, least squares; MMRM, mixed-model repeated measures; NA, not assessed; NNT, number needed to treat; OL, open-label; OLZ/SAM, a combination of olanzapine and samidorphan; PANSS, Positive and Negative Syndrome Scale; PK, pharmacokinetics; QT(c), (corrected) QT interval; R, DB, C, randomized, double-blind, controlled (placebo and/or active comparator) trial; SAE, serious adverse event; UGT, uridine 5′-diphospho-glucuronosyltransferase; WHO, World Health Organization.
Acknowledgments
Medical writing and editorial support were provided by Gina Daniel, PhD, and John H. Simmons, MD, of Peloton Advantage, LLC, an OPEN Health company, and funded by Alkermes, Inc.
Author Contributions
All authors made a significant contribution to the work reported, whether that is in the conception, study design, execution, acquisition of data, analysis and interpretation, or in all these areas; took part in drafting, revising or critically reviewing the article; gave final approval of the version to be published; have agreed on the journal to which the article has been submitted; and agree to be accountable for all aspects of the work.
Disclosure
These studies were sponsored by Alkermes, Inc. L. Citrome reports being a Consultant for AbbVie/Allergan, Acadia, Adamas, Alkermes, Angelini, Astellas, Avanir, Axsome, BioXcel, Boehringer Ingelheim, Cadent Therapeutics, Eisai, Impel, Intra-Cellular Therapies, Janssen, Karuna, Lundbeck, Lyndra, Medavante-ProPhase, Merck, Neurocrine, Novartis, Noven, Otsuka, Ovid, Relmada, Reviva, Sage, Sunovion, Teva, and University of Arizona and providing one-off ad hoc consulting for individuals/entities conducting marketing, commercial, or scientific scoping research; being a Speaker for AbbVie/Allergan, Acadia, Alkermes, Angelini, Eisai, Intra-Cellular Therapies, Janssen, Lundbeck, Neurocrine, Noven, Otsuka, Sage, Sunovion, Takeda, Teva, and CME activities organized by medical education companies such as Medscape, NACCME, NEI, Vindico, and Universities and Professional Organizations/Societies; owning stock (small number of shares of common stock) at Bristol-Myers Squibb, Eli Lilly, J & J, Merck, and Pfizer purchased >10 years ago; and receiving royalties from Wiley (Editor-in-Chief, International Journal of Clinical Practice, through end of 2019), UpToDate (reviewer), Springer Healthcare (book), and Elsevier (Topic Editor, Psychiatry, Clinical Therapeutics).
C. Graham, A. Simmons, M.S. Todtenkopf, H. Cummings, and L. Sun are employees of Alkermes, Inc. Y. Jiang, B. Silverman, and L. DiPetrillo were employees of Alkermes, Inc., at the time of these studies. D. McDonnell is an employee of Alkermes Pharma Ireland Ltd. Dr Mark S. Todtenkopf has patents 8778960 (Methods for treating antipsychotic-induced weight gain; the other patents are for the same indication and are a part of a subset/family), 16/899708 (pending), 17/071166, and 17/071236. The authors report no other conflicts of interest in this work.
You have requested "on-the-fly" machine translation of selected content from our databases. This functionality is provided solely for your convenience and is in no way intended to replace human translation. Show full disclaimer
Neither ProQuest nor its licensors make any representations or warranties with respect to the translations. The translations are automatically generated "AS IS" and "AS AVAILABLE" and are not retained in our systems. PROQUEST AND ITS LICENSORS SPECIFICALLY DISCLAIM ANY AND ALL EXPRESS OR IMPLIED WARRANTIES, INCLUDING WITHOUT LIMITATION, ANY WARRANTIES FOR AVAILABILITY, ACCURACY, TIMELINESS, COMPLETENESS, NON-INFRINGMENT, MERCHANTABILITY OR FITNESS FOR A PARTICULAR PURPOSE. Your use of the translations is subject to all use restrictions contained in your Electronic Products License Agreement and by using the translation functionality you agree to forgo any and all claims against ProQuest or its licensors for your use of the translation functionality and any output derived there from. Hide full disclaimer
© 2021. This work is licensed under https://creativecommons.org/licenses/by-nc/3.0/ (the “License”). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.
Abstract
Olanzapine effectively treats schizophrenia and bipolar I disorder (BD-I); however, its use is limited by the risk of significant weight gain and metabolic effects. OLZ/SAM, a combination of olanzapine and samidorphan, was recently approved in the United States for the treatment of adults with schizophrenia or BD-I. OLZ/SAM provides the efficacy of olanzapine while mitigating olanzapine-associated weight gain through opioid-receptor blockade. Here, we summarize OLZ/SAM clinical data characterizing pharmacokinetics, antipsychotic efficacy, weight mitigation efficacy, safety, and long-term treatment effects. In an acute exacerbation of schizophrenia, OLZ/SAM and olanzapine provided similar symptom improvements versus placebo at week 4. In stable outpatients with schizophrenia, OLZ/SAM treatment resulted in significantly less weight gain, reducing the risk for clinically significant weight gain and waist circumference increases of ≥ 5 cm by half, compared with olanzapine at week 24. Based on open-label extension studies, OLZ/SAM is safe and well tolerated for up to 3.5 years of treatment, while maintaining schizophrenia symptom control and stabilizing weight. The olanzapine component of OLZ/SAM was bioequivalent to branded olanzapine (Zyprexa); adjunctive OLZ/SAM had no clinically significant effects on lithium or valproate pharmacokinetics. Additionally, OLZ/SAM had no clinically relevant effect on electrocardiogram parameters in a dedicated thorough QT study. Overall, safety and tolerability findings from clinical studies with OLZ/SAM indicate a similar safety profile to that of olanzapine, with the exception of less weight gain. As OLZ/SAM contains the opioid antagonist samidorphan, it is contraindicated in patients using opioids and in those undergoing acute opioid withdrawal. Clinical trial results from more than 1600 subjects support the use of OLZ/SAM as a new treatment option for patients with schizophrenia or BD-I.
You have requested "on-the-fly" machine translation of selected content from our databases. This functionality is provided solely for your convenience and is in no way intended to replace human translation. Show full disclaimer
Neither ProQuest nor its licensors make any representations or warranties with respect to the translations. The translations are automatically generated "AS IS" and "AS AVAILABLE" and are not retained in our systems. PROQUEST AND ITS LICENSORS SPECIFICALLY DISCLAIM ANY AND ALL EXPRESS OR IMPLIED WARRANTIES, INCLUDING WITHOUT LIMITATION, ANY WARRANTIES FOR AVAILABILITY, ACCURACY, TIMELINESS, COMPLETENESS, NON-INFRINGMENT, MERCHANTABILITY OR FITNESS FOR A PARTICULAR PURPOSE. Your use of the translations is subject to all use restrictions contained in your Electronic Products License Agreement and by using the translation functionality you agree to forgo any and all claims against ProQuest or its licensors for your use of the translation functionality and any output derived there from. Hide full disclaimer