Efficacy and Safety of Vortioxetine and Duloxetine 60 mg Compared Placebo for the Treatment of Major Depressive Disorder: A Systematic Review and Meta-Analysis ()
1. Introduction
Major depressive disorder (MDD) is a serious public health problem affecting the lives of millions in the worldwide and leading causes of disability and disease [1] . This disease causes disorder in social, mental and physical functions of patients [2] . It is estimated that depressive disorder will have the first place disease burden in developing countries in the 2020. According to reports of the World Health Organization (WHO), about 350 million people worldwide suffer from major depressive illness [3] . Major depressive disorders are common mental health conditions which are thought to be caused by an imbalance in serotonin (5-HT) and nor epinephrine in addition to multiple situational, cognitive, and medical factors [4] . Patients with major depressive disorder often have such symptoms or signs: low pleasure usual activities, depressed mood, changes in sleeping or eating, fatigue, suicidal thoughts and difficulty concentrating [5] . Antidepressants play important role in the treatment of patients with depression and can often cause adverse effects [6] . In patients with major depression disorder, these diseases are reported: Parkinson’s disease, rheumatic arthritis, asthma, cancer, backs problems, chronic obstructive pulmonary disease (COPD), migraine, stroke, heart disease, diabetes mellitus, epilepsy, multiple sclerosis, and inflammatory bowel disease [7] . Vortioxetine, an antidepressant for the treatment of major depressive disorder, was approved by the Food and Drug Administration (FDA) in 2013. Vortioxetine is a selective serotonin reuptake inhibitor (SSRI) that binds to the presynaptic serotonin reuptake site, increasing the level of serotonin (5-HT) in the neuronal synapse and selectively binding to a variety of other serotonin receptors. It selectively binds to and acts as an antagonist of 5-HT3, 5-HT1D and 5-HT7 receptors, as a partial agonist to 5-HT1B receptors, and as an agonist of 5-HT1A receptor [8] . Duloxetine 60 mg, is an antidepressant which was approved for the treatment of major depressive disorder in 2004, and inhibits the neuronal uptake of serotonin and nor epinephrine, with a negligible affinity for other neuronal receptors, and this dual inhibition mechanism is believed to underlie its therapeutic effects [9] . In this study, Meeker et al., results showed Vortioxetine was significantly more effective than placebo for acute treatment of major depressive disorder (MDD). Although treatment effect estimates varied substantially between studies, a dose effect was not observed. Vortioxetine doesn’t appear to be more effective, and is potentially less effective than an SNRI [10] . This study aimed to evaluate the efficacy and safety of Vortioxetine and Duloxetine 60 mg compared to placebo for the treatment of major depressive disorder.
2. Methods
2.1. Search Strategy
The aim of this paper was to evaluate the efficacy and safety of Vortioxetine and Duloxetine 60 mg compared placebo for the treatment of major depressive disorder.
In this systematic and meta-analysis, we searched the Cochrane library, Pub Med, CRD, Scopus, Central Register of Controlled Trials to January 2015. We also searched ClinicalTrials.gov, International depressive disorder Conference and the Anxiety Disorders and Depression Conference. Our searches will not be limited by language, publication status or setting. The findings (data collection, summary and analysis of the identification) of this systematic review are reported according this systematic review and the results will be presented as a PRISMA [11] , which are shown in Figure 1.
2.2. Inclusion Criteria
We used randomized clinical trials (RTC) to investigate the efficacy and safety Vortioxetine and Duloxetine 60 mg compared to placebo (Vortioxetine and Duloxetine 60 mg and placebo in a three-arm study). Adult pa-
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Figure 1. Flowchart of included studies in meta-analysis.
tients of both genders man and women with a primary diagnosis of major depressive disorder according to the diagnostic and statistical manual of mental disorder 4 the Ed ? Text revision criteria were invluded [12] . Studies were excluded if the main outcome was prevention of relapse or if treatment outcomes based on rating scales of major depressive disorder were not available.
2.3. Data Extraction
In order to extract the data, two reviewers independently identified the “main outcome measure” and extracted data for each trial using a standard recording approach. First, screening the titles and abstracts of RCTs. Secondly, review author will independently full text of all trials. Compares the contents of each review author’s list, and conflicts were resolved by discussion. We collected data on treatment details, study procedures, participant characteristics, efficacy measures and adverse events (AEs). These data included arms (Vortioxetine, Duloxetine 60 mg, and placebo), size sample, age, sex, and duration of treatment, baseline MADRS and doses and study location. Outcome data related to the characteristics of the individual trial and the reported results were extracted for each trial. In the study, we assessed Montgomery Åsberg Depression Rating Scale (MADRS), and adverse effects contain diarrhea, dry mouth, dizziness, fatigue, headache and nausea included in meta-analysis..
2.4. Quality Assessment
Quality assessment studies included the review by the Cochrane Collaboration “Risk of bias” [13] , which were shown in Table 1.
2.5. Quality of RCTs Included
The study quality was assessed with Jadad scores. This instrument was used to assess the quality of RCT [14] .
It includes three items as follows: randomization, blinding and dropouts. The score standards and the results of our included studies are shown in Table 2, respectively. We’re rated as providing good methodological quality based on a Jadad score of 1 - 5. So the total scores for all included articles indicated a high study quality.
2.6. Statistical Analysis
In the study, the Montgomery Åsberg Depression Rating Scale (MADRS) [15] were reported in studies and adverse effects of Vortioxetine and Duloxetine 60 mg compared to placebo were statistically combined using the Mantel-Haenszel random effects model. The effect sizes were expressed as SMD (Standardized Mean Differences) [16] . The assessment of adverse effects was also determined using the Mantel-Haenszel model [17] , and the results were expressed as the OR (Odds Ratio). The SMD and OR reported by 95% CI (confidence intervals) and P values. Heterogeneity across each effect size was evaluated by using the I2 and Chi-squared test statistic [18] . This measure evaluates how much of the variance among studies can be attributed to the actual differences among the studies rather than to chance. A magnitude of considerable heterogeneity is usually I2 = 75% - 100 % [19] . To assess the Publication bias by a funnel plot, Egger’s test [20] , and Begg’s [21] rank correlation test were used. All the statistical analyses were performed by using Review Manager (Rev Man 5.3) software and Stata 11 software.
3. Results
This study evaluated the efficacy, safety of Vortioxetine and Duloxetine 60 mg compared to placebo for treatment of major depressive disorder in patients. The literature search resulted in a total of 189 records after duplicates
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Table 1. Risk of bias graph of the included studies.
L = low risk of bias; U = unclear risk of bias; H = high risk of bias.
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Table 2. Jadad score quality assessment of the included studies in meta-analysis.
were removed. Of these, 176 were excluded because they did not meet inclusion criteria, and 12 candidate trials were assessed for eligibility. We identified five randomized clinical trials with a total of 3039 patients fulfilled the inclusion criteria for treatment MDD. Table 3 summarizes the characteristics and findings of the included studies. Randomized clinical trials ranged in size from 452 to 755 participants. All five trials were Vortioxetine, Duloxetine 60 mg and placebo in the three arms. Trials ranged studied more than one Vortioxetine dose ranging from 2.5 to 20 mg and Duloxetine 60 mg dose was 60 mg. According to jaded scores five included trials indicated a high study quality.
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Table 3. Characteristics of included studies.
VTX = Vortioxetine; DLX = Duloxetine 60 mg.
3.1. Efficacy Vortioxetine and Duloxetine 60 mg Compared to Placebo
Five trials [22] -[26] compared Vortioxetine to placebo for response using the MADRS scale. As shown in Figure 2(a), compared to placebo, response rates were not significant for Vortioxetine 2.5 mg (SMD = −1.11; 95% CI −2.34, 0.13; I2 = 98%), significant for Vortioxetine 5 mg (SMD = −2.61; 95% CI −5.22 to −0.00; I2 = 99.5%), significant for Vortioxetine 10 mg (SMD = −1.85; 95% CI −2.12 to −1.58; I2 = 0), no significant for Vortioxetine 15 mg (SMD = −4.42; 95% CI −9.74 to 0.90; I2 = 99.6%), significant for Vortioxetine 20 mg (SMD = −6.20; 95% CI −12.08 to −0.31; I2 = 99.5%), and significant for total Vortioxetine (SMD = −3.29; 95% CI −4.47 to −2.10; I2 = 99.3%). Heterogeneity was very high for most of the dose comparisons. Five trials compared Duloxetine 60 mg to placebo for response using the MADRS scale. As shown in Figure 2(b), compared to placebo, response rates were no significant for Duloxetine 60 mg 60 mg (SMD = −6.35; 95% CI −8.84, −3.87; I2 = 99.3%).
3.2. Safety Vortioxetine and Duloxetine 60 mg Compared to Placebo
Table 4 summarizes pooled adverse events (AEs) absolute Odds Ratio for each vortioxetine and Duloxetine 60 mg compared to placebo. The most frequently reported adverse events were diarrhea, dry mouth, dizziness, fatigue, headache and nausea. Results showed that vortioxetine 2.5, 5, 10, 15, 20 mg and overall compared to placebo have a significant effective for Nausea and no significant for diarrhea, dry mouth, dizziness, fatigue and headache. Results also showed that duloxetine 60 mg compared to placebo has a significant effective for dry mouth, dizziness, fatigue and nausea.
3.3. Publication Bias
Publication bias for five studies was detected by drawing Egger’s funnel plot in the meta-analysis. Result showed significantly for publication bias (p = 0.000) (Figure 3).
4. Discussion
In this systematic review and meta-analysis, we include 5 studies in the meta-analysis. They include Vortioxetine, Duloxetine 60 mg and placebo. Results on relevant clinical efficacy and safety outcomes were included. Study quality was assessed and results were pooled by using random effect meta-analyses where applicable. A sensitivity analysis did not influence the results. The present meta- analysis demonstrated the superior efficacy of overall Vortioxetine compared placebo in MADRS for the treatment of major depressive disorder. The decrease in depression symptoms seems to be associated with Vortioxetine compared placebo. Results of meta- analysis demonstrated the of Duloxetine 60 mg compared placebo in MADRS. In the clinical studies analyzed, the common adverse effects of Vortioxetine compared to placebo, included diarrhea, dry mouth, dizziness, fatigue,
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Table 4. Pooled adverse events (AEs) in the included studies.
(a)
(b)
Figure 2. Forest plot of Standardized Mean Differences (SMD) and 95% confidence intervals (CIs) of change from baseline in the Montgomery-Åsberg Depression Rating Scale (MADRS Vortioxetine (a) and Duloxetine 60 mg (b) compared to placebo in the included studies.
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Figure 3. Egger’s funnel plot for publication bias.
headache and nausea. This meta-analysis showed that vortioxetine more easily induced nausea when compared with placebo, but there were no significant differences among the other five common side effects. Results also showed the common adverse effects of duloxetine 60 mg compared to placebo more commonly induced dry mouth, dizziness, fatigue and nausea. It seems that the effectiveness of the Vortioxetine and Duloxetine 60 mg in particular improves disease symptoms of major depressive disorder. Of course, the consequences of the improvement are measured in the Vortioxetine. The choice of vortioxetine or duloxetine 60 mg by a physician for the treatment of major depressive disorder and illness depends on the conditions and characteristics of the patient.
Considering the number of studies in this meta-analysis, we can say Vortioxetine drug is effective in the treatment of depression, but more studies to be done if in the future. And this drug, compared with other drugs that are currently used to treat depression, can be a better judgment about the effectiveness of the drug.
There are at least six limitations to this systematic review: 1. All included studies were supported by the Takeda company, Ltd., as part of a joint clinical development program with H. Lundbeck, which may have influenced the results; 2. Due to the limited number of the published and unpublished studies, we did not analyze the efficacy and safety of different doses of vortioxetine in the treatment of major depressive disorder; 3. The inclusion of patients was only during the acute phase (8 weeks), which did not enable us to analyze finding the long- term efficacy and safety of vortioxetine and douloxetine 60 mg in treating major depressive disorder; 4. All included studies in meta-analysis did not include the efficacy and adverse effects based on sex and we could not evaluate gender differences; 5. Primary meta-analyses had significant heterogeneity; this was resolved by subgroup studies by racial composition; 6. Additional large-scale and well-designed studies are needed to determine the optimal dose, the most appropriate treatment group, and the efficacy and safety of vortioxetine combined with other antidepressants in treatment of major depressive disorder. However, major depressive disorder (MDD) is frequently associated with heart diseases [27] , diabetes [28] , stroke, pregnancy, and the postpartum period [29] [30] . Vortioxetine should also benefit the physical state of these patients.
5. Conclusion
We find that Vortioxetine and Duloxetine 60 mg are significantly more effective than placebo for acute treatment of major depressive disorder (MDD). Vortioxetine also appears to be effective for treating symptoms of major depressive disorder. Some researchers’ suggestions concerning the place of vortioxetine treatment for adults with major depressive disorder are provided.
Acknowledgments
The authors are grateful to Dr. Hamidreza Dehghan, Dr. Korush Saki, Dr. Ehrampoush, Dr. Mosadegh, Dr. Dastgerdi, Dr. Maryam Saran and Meysam Behzadifar for their useful advice.
Authors’ Contributions
Masoud Behzadifar and Ali Akbari Sari are responsible for the study concept, design, and literature searching. Masoud Behzadifar and Mohammad Rastian are responsible for data analysis and interpretation. Abouzar Keshavarzi, Abed Tofighian and Mohammad Zobidi draft the paper. All authors participate in the analysis and interpretation of data and approve the final paper.
NOTES
*Corresponding author.