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Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Häuser W, Urrútia G, Tort S, Üçeyler N, Walitt B This is a reprint of a Cochrane review, prepared and maintained by The Cochrane Collaboration and published in The Cochrane Library 2013, Issue 4 http://www.thecochranelibrary.com Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. TABLE OF CONTENTS HEADER . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . ABSTRACT . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . PLAIN LANGUAGE SUMMARY . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . SUMMARY OF FINDINGS FOR THE MAIN COMPARISON . . . . . . . . . . . . . . . . . . . BACKGROUND . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . OBJECTIVES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . METHODS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . RESULTS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Figure 1. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Figure 2. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Figure 3. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Figure 4. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Figure 5. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Figure 6. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . DISCUSSION . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . AUTHORS’ CONCLUSIONS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . ACKNOWLEDGEMENTS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . REFERENCES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . CHARACTERISTICS OF STUDIES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . DATA AND ANALYSES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Analysis 1.1. Comparison 1 SNRI versus placebo final treatment, Outcome 1 Pain. . . . . . . . . . . . . Analysis 1.2. Comparison 1 SNRI versus placebo final treatment, Outcome 2 30% pain reduction. . . . . . . Analysis 1.3. Comparison 1 SNRI versus placebo final treatment, Outcome 3 50% pain reduction. . . . . . . Analysis 1.4. Comparison 1 SNRI versus placebo final treatment, Outcome 4 Fatigue. . . . . . . . . . . . Analysis 1.5. Comparison 1 SNRI versus placebo final treatment, Outcome 5 Sleep problems. . . . . . . . . Analysis 1.6. Comparison 1 SNRI versus placebo final treatment, Outcome 6 Depression. . . . . . . . . . . Analysis 1.7. Comparison 1 SNRI versus placebo final treatment, Outcome 7 Anxiety. . . . . . . . . . . . Analysis 1.8. Comparison 1 SNRI versus placebo final treatment, Outcome 8 Disease-related quality of life. . . . Analysis 1.9. Comparison 1 SNRI versus placebo final treatment, Outcome 9 Disability. . . . . . . . . . . Analysis 1.10. Comparison 1 SNRI versus placebo final treatment, Outcome 10 Cognitive disturbances. . . . . . Analysis 1.11. Comparison 1 SNRI versus placebo final treatment, Outcome 11 Participant-perceived improvement. Analysis 1.12. Comparison 1 SNRI versus placebo final treatment, Outcome 12 Tenderness. . . . . . . . . . Analysis 1.13. Comparison 1 SNRI versus placebo final treatment, Outcome 13 Withdrawal due to adverse events. . Analysis 1.14. Comparison 1 SNRI versus placebo final treatment, Outcome 14 Serious adverse events. . . . . . Analysis 2.1. Comparison 2 Active drug baseline and final treatment, Outcome 1 Pain. . . . . . . . . . . . Analysis 2.2. Comparison 2 Active drug baseline and final treatment, Outcome 2 Quality of life. . . . . . . . Analysis 3.1. Comparison 3 Placebo baseline and final treatment, Outcome 1 Pain. . . . . . . . . . . . . Analysis 3.2. Comparison 3 Placebo baseline and final treatment, Outcome 2 Quality of life. . . . . . . . . . ADDITIONAL TABLES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . APPENDICES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . WHAT’S NEW . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . CONTRIBUTIONS OF AUTHORS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . DECLARATIONS OF INTEREST . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . SOURCES OF SUPPORT . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . DIFFERENCES BETWEEN PROTOCOL AND REVIEW . . . . . . . . . . . . . . . . . . . . . INDEX TERMS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 1 1 2 3 7 7 8 10 11 13 14 16 17 18 20 21 22 22 26 48 50 51 52 53 54 55 56 57 58 59 60 61 62 63 64 65 66 67 67 68 71 71 72 72 72 72 i [Intervention Review] Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Winfried Häuser1 , Gerard Urrútia2 , Sera Tort3 , Nurcan Üçeyler4, Brian Walitt5 1 Department of Psychosomatic Medicine and Psychotherapy, Technische Universität München, München, Germany. 2 Iberoamerican Cochrane Centre - IIB Sant Pau, CIBER Epidemiología y Salud Pública (CIBERESP), Spain, Barcelona, Spain. 3 Iberoamerican Cochrane Centre, Institute of Biomedical Research (IIB Sant Pau), Barcelona, Spain. 4 Department of Neurology, University of Würzburg, Würzburg, Germany. 5 Georgetown University Medical Center, Washington Hospital Center, Washington, DC, USA Contact address: Winfried Häuser, Department of Psychosomatic Medicine and Psychotherapy, Technische Universität München, Langerstr. 3, München, D-81675, Germany. [email protected]. Editorial group: Cochrane Musculoskeletal Group. Publication status and date: Edited (no change to conclusions), published in Issue 4, 2013. Review content assessed as up-to-date: 27 December 2012. Citation: Häuser W, Urrútia G, Tort S, Üçeyler N, Walitt B. Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome. Cochrane Database of Systematic Reviews 2013, Issue 1. Art. No.: CD010292. DOI: 10.1002/14651858.CD010292. Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. ABSTRACT Background Fibromyalgia syndrome (FMS) is a clinically well-defined chronic condition of unknown etiology characterized by chronic widespread pain that often co-exists with sleep disturbances, cognitive dysfunction and fatigue. Patients often report high disability levels and poor quality of life (QOL). Drug therapy focuses on reducing key symptoms and improving quality of life. Objectives To assess the benefits and harms of serotonin and noradrenaline reuptake inhibitors (SNRIs) compared with placebo for treating FMS symptoms in adults. Search methods We searched the Cochrane Central Register of Controlled Trials (CENTRAL), (The Cochrane Library 2012, Issue 9), MEDLINE (1966 to September 2012), EMBASE (1980 to September 2012), www.clinicalstudyresults.org (U.S.-marketed pharmaceuticals) (to September 2012) and www.clinicaltrials.gov (to September 2012) for published and ongoing trials and examined the reference lists of reviewed articles. Selection criteria We selected randomized, controlled trials of any formulation of SNRIs against placebo for the treatment of FMS in adults. Data collection and analysis Two review authors independently extracted the data from the included studies, and assessed the risks of bias of the studies. Discrepancies were resolved by discussion. Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 1 Main results Ten studies were included with a total of 6038 participants. Five studies investigated duloxetine against placebo, and five investigated milnacipran against placebo. A total of 3611 participants were included into duloxetine or milnacipran groups and 2427 participants into placebo groups. The studies had a low risk of bias in general. Duloxetine and milnacipran had a small incremental effect over placebo in reducing pain (standardized mean difference (SMD) -0.23; 95% confidence interval (CI) -0.29 to -0.18; 6.1% relative improvement). One-hundred and ninety-two participants per 1000 on placebo reported an at least 50% pain reduction compared to 280 per 1000 on SNRIs (Risk ratio (RR) 1.49, 95% CI 1.35 to 1.64; number needed to treat to benefit (NNTB) 11, 95% CI 9 to 15). Duloxetine and milnacipran did not reduce fatigue substantially (SMD -0.14; 95% CI -0.19 to -0.08; 2.5% relative improvement; NNTB 17, 95% CI 12 to 29), and did not improve QOL substantially (SMD -0.20; 95% CI -0.25 to -0.14; 4.6% relative improvement; NNTB 12, 95% CI 9 to 17) compared to placebo. There were no statistically significant differences between either duloxetine or milnacipran and placebo in reducing sleep problems (SMD -0.07; 95% CI -0.16 to 0.03; 2.5% relative improvement). One-hundred and seven participants per 1000 on placebo dropped out due to adverse events compared to 196 per 1000 on SNRIs. The dropout rate due to adverse events in the duloxetine and milnacipran groups was statistically significantly higher than in placebo groups (RR 1.83, 95% CI 1.53 to 2.18; number needed to treat to harm (NNTH) 11, 95% CI 9 to 13). There was no statistically significant difference in serious adverse events between either duloxetine or milnacipran and placebo (RR 0.78, 95% CI 0.55 to 1.12). Authors’ conclusions The SNRIs duloxetine and milnacipran provided a small incremental benefit over placebo in reducing pain. The superiority of duloxetine and milnacipran over placebo in reducing fatigue and limitations of QOL was not substantial. Duloxetine and milnacipran were not superior to placebo in reducing sleep problems. The dropout rates due to adverse events were higher for duloxetine and milnacipran than for placebo. The most frequently reported symptoms leading to stopping medication were nausea, dry mouth, constipation, headache, somnolence/dizziness and insomnia. Rare complications of both drugs may include suicidality, liver damage, abnormal bleeding, elevated blood pressure and urinary hesitation. PLAIN LANGUAGE SUMMARY Serotonin and noradrenaline reuptake inhibitors for fibromyalgia Researchers in the Cochrane Collaboration conducted a review of research about the effects of serotonin and noradrenaline reuptake inhibitors (SNRIs) on fibromyalgia syndrome (FMS). After searching for all relevant studies, they found 10 studies with up to 6038 people. Their findings are summarized below. Adults with FMS, who took the SNRIs duloxetine or milnacipran rather than a fake medication (placebo), were likely to have : - reduced pain, - slightly improved quality of life and reduced fatigue, - no improvement for sleep problems, - more drug-induced side effects and a greater likelihood of stopping medication. Serious side effects such as liver damage and suicidality were very rare. There was no difference between the SNRIs duloxetine or milnacipran and fake medication for these serious side effects. What is fibromyalgia syndrome and what are serotonin and noradrenaline reuptake inhibitors? People with FMS suffer from chronic widespread pain, sleep problems and fatigue. There is no cure for FMS at present, so the treatments aim to relieve the symptoms and to improve quality of life. Serotonin and noradrenaline are chemicals which are produced by the human body, involved in the regulation of pain, sleep and mood. Low concentrations of serotonin have been reported in people with FMS. SNRIs are antidepressants that increase the concentration of serotonin and noradrenaline in the brain. The SNRIs duloxetine and milnacipran had been approved by the US Food and Drug Administration but not by the European Medicines Agency for the management of FMS. The US and European Regulatory Authorities differed in their judgment of the efficacy Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 2 and safety of both drugs. Therefore it is important to know for people with FMS and healthcare providers on the effects of SNRIs on FMS. Best estimate of what happens to people with FMS when they take duloxetine or milnacipran after an average of 18 weeks Pain: Pain was reduced by 50% in: - 29 out of 100 people taking duloxetine or milnacipran - 19 out of 100 people taking placebo. - Therefore, 10 more people in every 100 benefited from duloxetine or milnacipran than benefited from placebo (10% absolute improvement). Sleep problems and fatigue: People taking duloxetine or milnacipran reported a slight reduction in fatigue and the same amount of sleep problems as people taking placebo. Disease-related quality of life (QOL): - People taking duloxetine or milnacipran scored their quality of life as 14 (on a scale of 0 to100), - People taking placebo scored theirs as 10. - This means that people taking duloxetine or milnacipran rated their quality of life four points higher than people taking placebo. Stopping treatment due to the side effects: - 20 people out of 100 taking duloxetine or milnacipran stopped medication due to side effects. - 11 people out of 100 taking fake medication stopped medication due to side effects. - This means that 9 more people out of 100 stopped taking duloxetin or milnacipran than stopped taking fake medication because of side effects. Serious adverse events: There were no differences between duloxetine or milnacipran and fake medication in the number of serious adverse events. We often do not have precise information about side effects and complications. This is particularly true for rare but serious side effects. Possible side effects may include nausea, dry mouth, headache, constipation and hyperhidrosis. Rare complications may include suicidality, liver damage, abnormal bleeding, elevated blood pressure and urinary hesitation. Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 3 Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 4 286 per 1000 (261 to 317) Fatigue Baseline mean 69.4 (SD The mean fatigue in the (20-100 scale) 12.3)2 intervention groups was 0.14 standard deviations Higher scores indicate lower higher fatigue levels (0.19 to 0.08 lower) 192 per 1000 Moderate risk population 5656 (9 studies) 5994 (10 studies) RR 1.49 (1.35 to 1.64) No of Participants (studies) 50% pain reduction SNRI versus placebo Control Relative effect (95% CI) 6038 (10 studies) Corresponding risk Assumed risk Illustrative comparative risks* (95% CI) Pain (0-100 scale) Baseline mean 64.4 (SD The mean pain in the inHigher scores indicate 17.0)1 tervention groups was 0.23 standard deviations higher pain levels lower (0.29 to 0.18 lower) Outcomes Patient or population: Participants with FMS Settings: Study centres in North America and Europe Intervention: SNRI versus placebo SNRI versus placebo final treatment FMS S U M M A R Y O F F I N D I N G S F O R T H E M A I N C O M P A R I S O N [Explanation] ⊕⊕⊕⊕ high ⊕⊕⊕⊕ high ⊕⊕⊕⊕ high Quality of the evidence (GRADE) SMD -0.14 (-0.19 to -0. 08) Absolute improvement 1. 7% Absolute risk difference 10% (95% CI 7 to 13) Relative per cent change 50% (95% CI 37 to 66) NNTB 11 (95% CI 9 to 15) SMD -0.23 (95% CI -0,29 to -0.18) 3.9 % (95% CI 3.1 to 4, 9%) fewer points on the scale (absolute improvement) 6.1 % (95% CI 4.8 to 7. 7%) relative improvement NNTB 11 (95% CI 9 to 15) Comments Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 5 Serious adverse events Moderate risk population 196 per 1000 (166 to 230) RR 0.78 (0.55 to 1.12) 5845 (9 studies) 6179 (10 studies) Withdrawal due to ad- Moderate risk population verse events 107 per 1000 5987 (10 studies) Disease-related quality Baseline mean 57.9 (SD The mean health-related of life 14.1)7 quality of life in the inter(0-100 scale) vention groups was Higher scores indicate 0.19 standard deviations higher burden of disease lower (lower quality of life) (0.24 to 0.14 lower) RR 1.83 (1.53 to 2.18) 4081 (6 studies) Sleep problems Baseline mean 68.0 (23. The mean sleep in the in(0-100 scale) 8)3 tervention groups was Higher scores indicate 0.07 standard deviations higher sleep problem lower levels (0.16 lower to 0.03 higher) ⊕⊕⊕ moderate8 ⊕⊕⊕⊕ high ⊕⊕⊕⊕ high ⊕⊕ low4,5,6 Absolute risk difference 0% (95% CI -1 to 0) Relative percent change 22 % Absolute risk difference 9% (95% CI 6 to 12) Relative percent change 83 % (95% CI 53 to 118) NNTH 11 (95% CI 9 to 13) SMD -0.20 (95% CI -0.25 to -0.14) Absolute improvement 2. 7% (95% CI 2.0% to 3.4%) fewer points on the scale Relative improvement 4. 6% (95% CI 1.0 % to 5.8%) NNTB 12 (95% CI 9 to 17) (95% CI 1.0% to 2.3%) fewer points on the scale Relative improvement 2. 5% SMD -0.07 (95% CI -0.16 (95% CI 1.4% to 3.4%) to 0.03) NNTB 17 (95% 12 to 29) Absolute improvement 1. 7% (95% CI 0.7% to 3. 8%) fewer points on the scale Relative improvement 2. 5% (95% CI 1.1% to 5.6%) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 6 19 per 1000 (13 to 27) 2 Arnold 2010b N = 509 participants; Patient Electronic Diary 24 hour pain (0-100) Clauw 2008: N = 401 participants; MFI NRS 20-100 scale 3 Mease 2009a: N = 223 participants; MOS Sleep problem index NRS 0-100 scale 4,5 Not all studies reported the sleep outcomes 6 95% CI included no effect 7 Arnold 2010b; N = 509 participants; FIQ VAS 0-100 scale 8 Serious adverse events not reported by one study Abbreviations FIQ = Fibromyalgia Impact Questionnaire MFI = Multidimensional Fatigue Inventory MOS-Sleep problem index = Medical Outcome Study - Sleep problem index NRS = Numerical rating scale VAS = Visual analogue scale 1 GRADE Working Group grades of evidence High quality: further research is very unlikely to change our confidence in the estimate of effect. Moderate quality: further research is likely to have an important impact on our confidence in the estimate of effect and may change the estimate. Low quality: further research is very likely to have an important impact on our confidence in the estimate of effect and is likely to change the estimate. Very low quality: we are very uncertain about the estimate. *The corresponding risk (and its 95% confidence interval) is based on the assumed risk in the comparison group and the relative effect of the intervention (and its 95% CI). Abbreviations CI = Confidence interval FMS = fibromyalgia syndrome GRADE = Grading of Recommendations, Assessment, Development and Evaluation in clinical guidelines NNTH = Number Needed to Treat for an additional Harmful outcome NNTB = Number Needed to Treat for an additional Beneficial outcome RR = risk ratio SMD = standardized mean difference SNRI = serotonin and noradrenaline reuptake inhibitors 24 per 1000 (95% CI 45% improvement to 12% worsening) BACKGROUND nervous system. Serotonin and noradrenaline are implicated in the mediation of endogenous pain inhibitory mechanisms. Description of the condition The key symptoms of fibromyalgia syndrome (FMS) are chronic, widespread pain associated with cognitive dysfunction, sleep disturbances and physical fatigue (Häuser 2008; Wolfe 2010). Correspondingly, patients often report high disability levels and poor quality of life, along with extensive use of medical care (Hawley 1991; Sauer 2011; Winkelmann 2011; Wolfe 1997). Lacking a specific laboratory test, diagnosis is established by a history of the key symptoms and the exclusion of somatic diseases that could explain the key symptoms (Häuser 2009; Wolfe 2010). For the clinical diagnosis the American College of Rheumatology (ACR) 1990 classification (Wolfe 1990), the ACR 2010 preliminary diagnostic criteria (Wolfe 2010), and the modified ACR 2010 preliminary diagnostic criteria (survey criteria) can be used (Häuser 2012; Wolfe 2011a). Previously other standardized criteria were used to diagnose FMS (Smythe 1981; Yunus 1981; Yunus 1982; Yunus 1984). The prevalence of FMS in adults in the USA was estimated to be five million (Lawrence 2008). The estimated overall prevalence of FMS was 2.9% in the general population of five European countries (Branco 2010b). The definite etiology (cause) of this syndrome remains unknown. A systematic review of studies of candidate genes demonstrated that 5-HT2A receptor 102T/C polymorphism (multiple forms) conferred susceptibility to FMS (Lee 2010), while a systematic review of case-control studies found an association between physical and sexual abuse and FMS (Häuser 2010a). For patients with rheumatoid arthritis (RA), social disadvantage, psychological distress and RA severity predicted future development of FMS (Wolfe 2011). Several factors are associated with the pathophysiology of FMS, but the causal relationship is unclear. This includes alterations of central pain pathways, hyporeactivity (low activity) of the hypothalamus-pituitary-adrenal axis, increased systemic proinflammatory and reduced anti-inflammatory cytokine profiles, and disturbances in the dopaminergic and serotonergic systems (Sommer 2012). There is evidence that cardinal pain symptoms of fibromyalgia may be due to alterations in central processing of sensory input, along with aberrations in the endogenous inhibition of pain. Exposure to physical or psychosocial stressors as outlined above may contribute to dysfunctional pain processing (Bradley 2009). Since specific treatment aimed at altering the pathogenesis is not possible, drug therapy that focuses on symptom reduction is ubiquitously employed. How the intervention might work Dysfunction of serotonin and noradrenaline transmission, which mediates endogenous analgesic mechanisms via the descending inhibitory pain pathways in the central nervous system, may play a key role in the pathophysiology of FMS. Researchers found that levels of metabolites of biogenic amines key to descending inhibition were lower than normal in at least three FMS body fluid compartments (Legangneux 2001; Russell 1992). Imbalance or deficiency in serotonin and noradrenaline is also associated with other key symptoms of FMS such as fatigue and cognitive deficits (Bradley 2009). Treatment with SNRI increases transmission of these neurotransmitters and may improve disease states associated with serotonin and noradrenaline deficiencies such as pain, fatigue and cognitive deficits. Why it is important to do this review There is a transatlantic difference in the approval of SNRIs as a treatment for FMS by drug agencies (Briley 2010). The SNRIs duloxetine and milnacipran have been approved by the US Food and Drug Administration (FDA), but not by the European Medical Agencies (EMA), for the management of FMS. The FDA stated that the sponsors of the two drugs had provided adequate evidence of their benefits and harms to support their indication for the management of FMS (Food and Drug Administration 2009a; Food and Drug Administration 2009b).The EMA, however, denied clinically relevant effects for both drugs, on the basis of a lack of robust evidence of efficacy, and because the adverse effects profile was considered to outweigh the benefits (European Medicines Agency 2008; European Medicines Agency 2010). Meanwhile new randomized controlled trials with duloxetine (Arnold 2010a), and milnacipran (Arnold 2010b), were published that had not been evaluated by the FDA and EMA. With new data available, and in the light of the divergent appraisals of duloxetine and milnacipran by the FDA and EMA, we saw the need to evaluate the efficacy and safety of SNRIs according to recently established methodological standards of pain medicine (Moore 2010a), in order to assist FMS-patients and doctors in shared decision making on pharmacological treatment options. OBJECTIVES Description of the intervention Serotonin and noradrenaline (norepinephrine) reuptake inhibitors (SNRIs) act on noradrenergic and serotonergic neurons in the To assess the benefits and harms of serotonin and noradrenaline reuptake inhibitors (SNRIs) compared with placebo or other active drug(s) in the treatment of FMS. The outcomes of efficacy Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 7 (benefits) were derived from the key domains as defined by a consensus among experts and people with FMS (Mease 2009a). Safety (harms) was defined by the frequency of study withdrawals due to adverse events and of serious adverse events. METHODS Criteria for considering studies for this review (MFI), Fatigue Severity Scale (FSS), or other validated scales) over single item scales (e.g. Fibromyalgia Impact Questionnaire (FIQ) fatigue VAS, or other single item scales). 3. Self-reported sleep problems: we used the following preference: validated combined scale (e.g. Medical Outcomes Study (MOS) sleep scale, or other validated scales), over single item assessment (e.g. FIQ sleep VAS, or other single item scales). 4. Self-reported disease-related quality of life (QOL) measured by the total score of the Fibromyalgia Impact Questionnaire (FIQ). 5. Safety. 5.1 Withdrawals due to side effects. 5.2 Serious adverse events. Types of studies We selected all relevant double-blind randomized controlled trials (RCTs), with SNRIs and with a study duration of more than four weeks. Types of participants Adults (over 18 years) having a clinical diagnosis of FMS by any published, recognized and standardized criteria (Smythe 1981; Wolfe 1990; Wolfe 2010; Wolfe 2011a, Yunus 1981; Yunus 1982; Yunus 1984). Types of interventions We included trials comparing SNRIs with placebo or another active drug with proven efficacy to reduce FMS-symptoms. We allowed co-interventions, such as physical therapy or other drugs different from those being assessed in the trial. We considered the following SNRIs in this review: desvenlaxafine, duloxetine, milnacipran, venlaxafine Types of outcome measures We followed some suggestions of the OMERACT Fibromyalgia Working Group (Mease 2009b), the Initiative of Methods, Measurement and Pain Assessment in Clinical Trials (IMMPACT) (Dworkin 2009), and of best practice in the reporting of systematic reviews in chronic pain (Moore 2010a), for selecting outcome measures. Minor outcomes 1. Self-reported 30% pain reduction. 2. Self-reported depression: we used the following preference: validated combined scale (Beck Depression Inventory (BDI), or other validated scales), over single-item assessment (e.g. FIQ subscale for depression, or other single item scales). 3. Self-reported anxiety: we used the following preference: validated combined scale (Beck Anxiety Inventory (BAI), State Trait Anxiety Inventory (STAI), or other validated scales), over single item scale (FIQ anxiety VAS, or other single item scales). 4.Self-reported disability (impairment of physical function): we used the following preference: validated combined scale (Brief Pain Inventory (BPI) interference from pain, Short-Form Health Survey (SF-36) physical summary score, or other validated scales), over single item scale (FIQ physical impairment VAS, or other single item scales). 5. Self-reported sexual function: we used the following preference: validated combined scale (Arizona Sexual Experience Scale, or other validated scale), over single item scale. 6. Patient perceived global improvement (Patient Global Impression of Change (PGIC), or Clinical Global Impression (CGI) of severity). 7. Self-reported cognitive disturbances: validated combined scale (Multiple Ability Self-report Questionnaire (MASQ), or any other validated scale), over single item scale. 8. Tenderness: measurement of tender point pain threshold. Major outcomes Search methods for identification of studies 1. Self-reported pain: we used the following preference: a) electronic diaries over paper; b) 24-hour recall pain, weekly recall pain with visual analogue scale (VAS); c) paper VAS, paper numeric 11point ordinal scale (Numeric Rating Scale NRS), combined pain measures, pain drawings. 1.1 Self-reported pain. 1.2 Self-reported 50% pain reduction. 2. Self-reported fatigue: we used the following preference: validated combined scale (e.g. Multidimensional Fatigue Inventory We ran an electronic search in the Cochrane Central Register of Controlled Trials (CENTRAL) (The Cochrane Library 2012, Issue 9), MEDLINE accessed through PubMed (1966 to September 2012), and EMBASE accessed through OVID (1980 to September 2012). Furthermore we searched www.clinicalstudyresults.org ( U.S.-marketed pharmaceuticals) and www.clinicaltrials.gov (website of the US National Institute of Health) to 12 September 2012 for ongoing trials (See Appendix 1). We searched bibliographies from reviewed articles and we retrieved relevant articles. Our search Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 8 included all languages. We analyzed the reports of the approval of duloxetine and milnacipran for FMS of the FDA center for drug evaluation and research (Food and Drug Administration 2009a; Food and Drug Administration 2009b). We contacted content experts for unpublished and further possible studies. Data collection and analysis Selection of studies Two review authors (GU,ST) independently scrutinized all the titles and abstracts revealed by the searches and determined which fulfilled the selection criteria. A third review author (WH) verified that the selection had been properly realized. Data extraction and management Two review authors (NÜ, WH) extracted data independently onto a specially designed data extraction form. We would have resolved any disagreements by discussion with the third review author (GU), but this was not necessary. One author (WH) entered data into Review Manager (RevMan) and a second author (NÜ) checked them. Discrepancies were resolved by discussion. Assessment of risk of bias in included studies Two review authors (NÜ,WH) independently assessed the risk of bias of each included trial. We resolved disagreements by consensus and, if needed, referral to a third review author (ST). For each included study, we assessed risk of bias against key criteria: random sequence generation (selection bias); allocation concealment (selection bias); incomplete outcome data (attrition bias); selective outcome reporting (reporting bias); blinding of participants and personnel (performance bias); blinding of outcome assessment (detection bias) in accordance with methods recommended by The Cochrane Collaboration (Higgins 2011). Each of these criteria was explicitly judged as being of: low risk of bias, high risk of bias or unclear risk of bias (i.e. lack of information or uncertainty over the potential for bias). The quality of evidence was rated by the GRADE approach with GRADEprofiler (Guyatt 2011). large effect size (Cohen 1988). We considered values of g less than 0.2 to equate to a “not substantial” effect size. Differences in mean reductions of symptoms between active drug and placebo groups do not adequately describe the potential benefit of a drug treatment. The differences between treatment and placebo group reflect the incremental benefit of active treatment that contribute to treatment effect after subtracting out placebo, natural history and regression to the mean (Dworkin 2009). The differences between treatment and placebo group in FMS are limited by the magnitude of the response in the placebo group that accounts for approximately 50% of the treatment response in the active drug groups in FMS trials (Häuser 2011a). Therefore, we calculated the MD of the pain and QOL outcomes at baseline and at final treatment for active drug and placebo groups to give an impression of the potential of true drug and placebo. Pain outcomes were converted to a 0 to 10 scale. QOL outcomes (FIQ total score) were converted to a 0 to 100 scale. We calculated the mean baseline pain and QOL scores in the placebo group by using the generic inverse method. We used the following benchmarks: a) pain reduction: i) 20% to 30% decrease classed as minimally important; ii) 30% to 50% decrease classed as moderately important; iii) 50% or more decrease classed as substantial (Dworkin 2008); b) Health-Related Quality of Life (HRQOL) (FIQ total score): minimal clinically important difference defined as at least a 14% reduction (Bennett 2009). The numbers needed to treat for an additional beneficial outcome (NNTBs) for continuous variables (fatigue, sleep problems, HRQOL) were calculated using the Wells calculator software available at the Cochrane Musculoskeletal Group editorial office, which estimates, from the SMDs, the proportion of participants who will benefit from treatment. The estimation of responders is nearly independent of the minimally important difference (MIT) (Norman 2001). We used a MIT of 0.5 for calculation. Unit of analysis issues In trials where multiple SNRI-dosage arms were compared with one placebo group, for continuous outcomes we adjusted the number of participants in the placebo group according to the number of participants in the different SNRI-dosage arms. For dichotomous variables we pooled the different SNRI dosage arms and compared the pooled results with the placebo arm. Measures of treatment effect Dealing with missing data The effect measures of choice were risk ratio (RR) for dichotomous data and mean difference (MD) or standardized mean difference (SMD) (when different scales were used to measure outcomes) for continuous data. Uncertainty was expressed with 95% confidence intervals (CIs). We used Cohen’s categories to evaluate the magnitude of the effect size, calculated by SMD, with values for Hedges’ g as follows: 0.2 to 0.5 equating to a small effect size, 0.5 to 0.8 equating to a medium effect size, and more than 0.8 equating to a We used intention-to-treat (ITT) analysis data. The ITT population consisted of participants who were randomized, took the assigned study medication, and provided at least one post-baseline assessment. Wherever possible, we assigned zero improvement to missing participants. However, most studies in chronic pain report results, including responder results, using last observation carried forward. This has been questioned as being potentially biased, as withdrawal is an important outcome that makes last observation Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 9 carried forward unreliable. Last observation carried forward can lead to overestimation of efficacy, particularly in situations where adverse event withdrawal rates differ between active and control groups. At this time it is unclear what strategy can actually be used to deal with missing data inside studies (Moore 2012). We examined and reported imputation strategies clearly. Where means or SDs were missing, attempts were made to obtain these data through contacting trial authors. Where SDs were not available from trial authors, they were calculated from t-values, CIs or standard errors, where reported in articles (Higgins 2011). Where 30% and 50% pain reduction rates were not reported and not provided on request, they were calculated from means and SDs by a validated imputation method (Furukawa 2005). Assessment of heterogeneity We used the I2 statistic for heterogeneity. I2 statisitic values less than 25% indicate low heterogeneity; values of 25% to 50% indicate moderate heterogeneity, and values of 50% or over indicate substantial heterogeneity (Higgins 2011). A more detailed analysis of European versus non-European participants was not possible because the studies with mixed continent samples did not report how many participants were recruited from each continent. We decided to restrict the comparisons on the key domains of FMS (pain, fatigue, sleep) and adverse events in order not to inflate the number of comparisons. To test the hypotheses of a subgroup effect, a test of interaction with a predetermined two-tailed α value of 0.05 was used for subgroup analysis of studies with and without European participants (Altman 2003). The intended subgroup analyses with gender and pain were not conducted because individual patient data were not available. Sensitivity analysis The intended sensitivity analyses (different statistical models applied, presence of temporal differences, diagnostic criteria used in the trial, according to the presence/absence of any mental or psychiatric disorder, and according to the presence/absence of any concomitant systemic disease) were not conducted, because the studies did not differ in these characteristics. Assessment of reporting biases Publication bias was addressed by visual inspection of funnel plots and tests for funnel plot asymmetry (Begg 1994; Egger 1997), when there were at least 10 studies included in the meta-analysis (Higgins 2011). Outcome reporting bias was addressed by checking whether the means and SDs of all primary and secondary outcomes outlined in the methods section of the published studies had been reported, or provided on request. Data synthesis We undertook each meta-analysis using a random-effects model in RevMan. Subgroup analysis and investigation of heterogeneity We performed a subgroup analysis of duloxetine, and milnacipran, studies to test for potential differences in benefits and harms of these two drugs. We performed a subgroup analysis of studies with and without European participants to test for potential transatlantic differences between the efficacy and adverse events of SNRIs. RESULTS Description of studies See: Characteristics of included studies; Characteristics of excluded studies. We initially identified 3755 studies. We excluded 3735 references as they did not fulfill inclusion criteria related to the interventions evaluated in this review. We did not find head-to-head comparisons of SNRIs or of SNRIs with other drugs used for FMStreatment. We identified 20 studies potentially related to SNRIs, and the full text was obtained for each of them. We excluded 10 studies (Branco 2011; Chappell 2009; Dwight 1998; Gendreau 2005; Goldenberg 2010; Hsiao 2007; Mease 2010; Sayard 2003; Saxe 2012; Wyeth 2008). See the Characteristics of excluded studies table for further details about reasons for exclusion and Figure 1 for studies’ flow. Finally, we included 10 studies. See the Characteristics of included studies table for a full description of the studies. Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 10 Figure 1. Study flow diagram. Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 11 Included studies We included five studies comparing placebo with duloxetine ( Arnold 2004; Arnold 2005; Arnold 2010a; Chappell 2008; Russell 2008), and five studies comparing placebo with milnacipran ( Arnold 2010b; Branco 2010; Clauw 2008; Mease 2009a; Vitton 2004), in the analysis. mg/day, and in milnacipran trials was hydrocodone up to 60 mg/ day. Major outcomes Pain Study characteristics All studies were conducted in research centers. Five studies were conducted in the USA (Arnold 2004; Arnold 2005; Clauw 2008; Mease 2009a; Vitton 2004), two studies in the USA and Puerto Rico (Arnold 2010a; Russell 2008), one study each in the USA and Western Europe (Chappell 2008), in the USA and Canada (Arnold 2010b), and in Europe (Branco 2010). All studies had a parallel design. The median of the therapy phase of the studies was 17.5 weeks (range 12 to 27 weeks). A total of 3611 participants were included into true drug groups, and 2427 participants into placebo groups. The mean of participants in all true drug group arms was 366 (range 97 to 605), and in placebo groups was 241 (range 28 to 509). All studies used different measures for pain. We selected the predefined primary outcome variables of the studies for analysis. Pain was assessed in duloxetine studies by the Brief Pain Inventory (BPI) 24 average pain score, and in milnacipran trials by the patient electronic diary 24-hour recall pain. Fatigue Fatigue was assessed either by the single item of the FIQ (Arnold 2004; Arnold 2005; Vitton 2004), or by the Multidimensional Fatigue Inventory (MFI) in the other studies. The fatigue score of the FIQ was not reported by one study (Arnold 2005). Sleep disturbances Participant characteristics Participants were recruited in duloxetine trials by referral and advertisement in media, and in milnacipran trials by referral. All studies included participants over 18 years old. All studies excluded participants with somatic diseases including inflammatory rheumatic diseases. All duloxetine studies included participants with mental disorders, except for major depression (all studies) and general anxiety disorder (all but one study (Arnold 2010a)). All milnacipran studies excluded participants with severe mental disorders including major depression. One study did not report the number of participants screened (Chappell 2008). In nine studies 5740 of the 10,589 screened participants (54.2%) were randomized. Middle-aged white women prevailed in all studies: the median of the mean age was 49 years (range 47 to 51 years). The median of the percentage of women was 95% (range 92% to 100%). The median of the percentage of whites was 89.5% (range 77.5% to 97.5%). Sleep disturbances were assessed by the BPI sleep interference scale in the duloxetine studies, and by Medical Outcomes Study (MOS) in three milnacipran studies (Branco 2010; Clauw 2008; Mease 2009a). The Vitton 2004 study used the Jenkins Sleep Scale. Three duloxetine studies did not report the sleep outcomes (Arnold 2004; Arnold 2010a; Chappell 2008). One milnacipran study did not report on the assessment of sleep outcomes (Arnold 2010b). Quality of life All studies except one reported the FIQ-total score as a measure of disease-specific health-related quality of life (HRQOL) (Arnold 2010a). Cognitive disturbances (“fibro fog”) were assessed in three duloxetine studies by the mental fatigue subscale of the MFI (Arnold 2010a; Chappell 2008; Russell 2008), and in four milnacipran studies by the Multiple Ability Self-report Questionnaire (MASQ) (Arnold 2010b; Branco 2010; Clauw 2008; Mease 2009a). Interventions All studies, except for three (Arnold 2010a; Arnold 2010b; Vitton 2004), had fixed dosages. In five studies two dosages of SNRIs (duloxetine 60 and 120 mg/day and milnacipran 100 and 200 mg/day) were tested against placebo (Arnold 2005; Clauw 2008; Mease 2009a; Russell 2008; Vitton 2004). The other studies had a single SNRI-arm. The rescue medication in duloxetine trials was acetaminophen (paracetamol) up to 2 g/day and aspirin up to 325 Adverse events All studies used physical examination, electrocardiograms, and laboratory analysis for the assessment of adverse events. Four studies did not report details about how subjective adverse symptoms were assessed (Arnold 2004; Arnold 2005; Arnold 2010a; Arnold 2010b). Three studies reported the recording of spontaneously-reported adverse events (Chappell 2008; Russell 2008; Vitton 2004), Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 12 another two studies reported spontaneously-reported and investigator-observed adverse events (Clauw 2008; Mease 2009a), and one study reported both spontaneously-reported and observerassessed (use of non-leading questions) adverse events (Branco 2010). Minor outcomes Depression and anxiety Depression was assessed in all studies by the Beck Depression Inventory (BDI), except for the Arnold 2005 study that used the Hamilton Depression Rating Scale (HDRS), and Vitton 2004 that used the FIQ single item depression scale. Anxiety was assessed by the Beck Anxiety Inventory (BAI) in three studies (Arnold 2004; Arnold 2010a; Arnold 2010b), by the Stait-Trait Anxiety Inventory (STAI) in one study (Branco 2010), and by the FIQ single item scale in one study (Vitton 2004). The remaining studies did not assess anxiety. Disability We used the BPI average interference scale as a measure of disability for seven studies. The remaining three studies used three different measures for disability/physical function, namely subscale data of: Multidimensional Health Assessment Questionnaire (MDHAQ) (Clauw 2008); the Short Form Health Survey (SF-36) (Mease 2009a); and the FIQ (Vitton 2004). Sexual function Only two studies reported on the assessment of sexual function, however, one study did not report the data (Clauw 2008), and the other did not report the SDs (Mease 2009a). Patient perceived global improvement All studies but one (Vitton 2004) assessed global improvement using the patient global impression of change scale (PGIC). The data presented in one study (Branco 2010) were not suited for analysis. Cognitive disturbances Three studies used the cognitive function subscale of the Multiple Ability Self-report Questionnaire (MASQ) (Arnold 2010b; Clauw 2008; Mease 2009a), four studies used the mental fatigue subscale of the Multidimensional Fatigue Inventory (MFI) (Arnold 2010a; Branco 2010; Chappell 2008; Russell 2008) and three studies did not assess cognitive disturbances (Arnold 2004; Arnold 2005; Vitton 2004). Tender point pain threshold Tender point pain threshold measurements were only conducted in four duloxetine studies (Arnold 2004; Arnold 2005; Chappell 2008; Russell 2008). Risk of bias in included studies In general, the risk of bias of included studies was low (See Figure 2 and Figure 3 for risk of bias summary and graph). Detailed information regarding risk of bias assessments of every study are given in the Characteristics of included studies table. Figure 2. Risk of bias graph: review authors’ judgements about each risk of bias item presented as percentages across all included studies. Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 13 Figure 3. Risk of bias summary: review authors’ judgements about each risk of bias item for each included study. Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 14 Allocation Blinding anxiety outcomes. Clauw 2008 did not report 50% pain reduction rates and anxiety outcomes. Mease 2009a did not report the standard deviations of sexual dysfunction outcome. Most notably, the missing outcomes were not provided on request, therefore, a reporting bias for some outcomes (pain, anxiety, sleep problems, sexual dysfunction) in some studies cannot be excluded. Blinding of participants, personnel and outcome assessors were adequate in all studies. Effects of interventions Random sequence generation and allocation concealment were adequate in all studies. Incomplete outcome data All studies used ITT analysis. All studies except Vitton 2004 imputed missing data by baseline or last observation carried forward method. Most outcomes of the study of Vitton 2004 were based on observed cases analysis that were provided on request. See: Summary of findings for the main comparison Serotonin and noradrenaline reuptake inhibitors (SNRI) versus placebo for fibromyalgia syndrome (FMS) - results at final treatment All SNRIs versus placebo Pain Selective reporting Viusal inspection of funnel plots was not indicative for a publication bias. In Egger’s test the intercept of the effect size on pain was -1.16 (95% CI -0.08 to -2.23) with t equal to 2.30 (two-tailed P value 0.04). In Begg’s test Kendall’s tau without continuity correction was -0.40 and Z equalled 2.12 (two-tailed P value 0.03). Both tests were indicative for a publication bias. All studies with duloxetine and milnacipran had been registered for the application of an approval for FMS-management by regulatory agencies. We searched these databases, therefore, we do not assume a nonpublication of RCTs with both drugs in FMS. All studies except Vitton 2004 did not report completely on all outcomes assessed. Arnold 2004 did not report 30% pain reduction rates, sleep outcomes and serious adverse events. Arnold 2005 did not report anxiety outcomes. Arnold 2010a did not report sleep problem outcomes. Arnold 2010b did not report sleep problem and anxiety outcomes. Branco 2010 did not report 50% pain reduction rates. Chappell 2008 did not report sleep problem and Mean pain reduction All 10 studies, with 6038 participants, were entered into an analysis of the effects of SNRIs on pain reduction. The overall effect on pain was significant (P value < 0.001). The SMD was -0.23 (95% CI -0.29 to -0.18). According to Cohen’s categories the effect on pain of SNRIs compared to placebo was small. 50% pain reduction All 10 studies, with 5994 participants, were entered into an analysis of the RR of a 50% pain reduction. The response rates for two studies had to be calculated by an imputation method because the data had not been reported and were not provided on request (Branco 2010; Clauw 2008). The RR of a 50% pain reduction by SNRI versus placebo was significant (P value < 0.0001): the RR was 1.49 (95% CI 1.35 to 1.64) (see Figure 4). Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 15 Figure 4. Forest plot of comparison: 1 SNRI versus placebo final treatment, outcome: 1.3 50% pain reduction. Fatigue Nine studies, with 5656 participants, were entered into an analysis of the effects of SNRIs on fatigue reduction. The overall effect on fatigue was significant (P value < 0.001). SMD was -0.14 (95% CI -0.19 to -0.08). Based on Cohen’s categories, the effect on fatigue of SNRIs versus placebo was not substantial. Sleep problems Six studies, with 4081 participants, were entered into an analysis of the effects of SNRIs on reduction of sleep disturbances. The overall effect on sleep disturbances was not significant (P value = 0.15). Disease-related quality of life (QOL) Nine studies, with 5457 participants, were entered into an analysis of the effects of SNRIs on the total score of the FIQ. The overall effect on QOL was significant (P value < 0.001). SMD was -0.20 (0.25 to -0.14). Based on Cohen’s categories the effect on disability of SNRIs versus placebo was not substantial (see Figure 5). Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 16 Figure 5. Forest plot of comparison: 1 SNRI versus placebo final treatment, outcome: 1.8 Disease-related quality of life. Withdrawal due to adverse events All 10 studies, with 6179 participants, were entered into an analysis of withdrawals due to adverse events. 743 out of 3607 participants (20.6%) dropped out due to adverse events in true drug groups and 262 out of 2412 (10.9%) dropped out in placebo groups. The RR of dropping out due to adverse events was significant (P value < 0.001). The RR was 1.83 (95% CI 1.55 to 2.15). The number of participants needed to achieve an incremental harm by true drug was 11 (96% CI 9 to 13) (see Figure 6). Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 17 Figure 6. Forest plot of comparison: 1 SNRI versus placebo final treatment, outcome: 1.13 Withdrawal due to adverse events. Serious adverse events Nine studies, with 5845 participants, were entered into an analysis of withdrawals due to serious adverse events. The RR of dropping out due to serious adverse events was not significant (P value 0.15). The RR was 0.78 (95% CI 0.55 to 1.12). 30% pain reduction All 10 studies, with 6004 participants, were entered into an analysis of the risk ratio (RR) of a 30% pain reduction. The RR of a 30% pain reduction by SNRI versus placebo was significant (P value < 0.0001): the RR was 1.36 (95% CI 1.26 to 1.46). Anxiety Five studies, with 2713 participants, were entered into an analysis of the effects of SNRIs on anxiety reduction. The overall effect on anxiety was not significant (P value = 0.54). Disability Ten studies, with 5995 participants, were entered into an analysis of the effects of SNRIs on disability reduction. The overall effect on disability was significant (P value < 0.001). SMD was -0.22 (95% CI -0.28 to -0.16). Based on Cohen’s categories the effect on disability of SNRIs versus placebo was small. Depression Nine studies, with 5656 participants, were entered into an analysis of the effects of SNRIs on depression reduction. One study reported only the outcomes of one of three dosage groups (Russell 2008).The overall effect on depression was significant (P value < 0.001). SMD was -0.15 (95% CI -0.21 to -0.10). Based on Cohen’s categories, the effect on depression of SNRIs versus placebo was not substantial. Sexual function Two studies reported on the assessment of sexual function. A quantitative synthesis was not possible due to a lack of data reporting (Clauw 2008). In one study both milnacipran arms did not differ significantly from placebo in reducing sexual problems (Mease 2009a). Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 18 Patient perceived global improvement Placebo baseline and final treatment Eight studies, with 4551 participants, were entered into an analysis of the effects of SNRIs on patient perceived global improvement. The overall effect on patient perceived global improvement was significant (P value < 0.001). SMD was -0.27 (95% CI -0.33 to 0.21). Based on Cohen’s categories the effect on patient perceived global improvement of SNRIs versus placebo was small. Pain reduction number needed to treat for an additional beneficial outcome Cognitive disturbances Seven studies, with 5344 participants, were entered into an analysis of the effects of SNRIs on cognitive disturbances. The overall effect on “fibro fog” was significant (P value < 0.001). SMD was -0.15 (95% CI -0.21 to -0.10). Based on Cohen’s categories, the effect on cognitive disturbances of SNRIs versus placebo was not substantial. Tenderness Four studies, with 1364 participants, performed tender point pain threshold measurement. SNRIs were superior to placebo in raising the tender point pain threshold (P value < 0.001), suggesting less tenderness. SMD was -0.23 (95% CI -0.35 to -0.12). Based on Cohen’s categories the effect on tenderness of SNRIs versus placebo was small. SNRIs baseline and final treatment Pain reduction The outcomes were converted into a 0 to 10 scale, if necessary. Ten studies, with 6038 participants, were entered into an analysis of the mean difference of pain at final treatment and at baseline in true drug groups. The pooled mean pain score was 6.53 (95% CI 6.42 to 6.63). The mean difference (MD) was 2.04 (95% CI 1.86 to 2.21) of a 0 to 10 numeric scale. Based on benchmarks for interpreting changes in chronic pain trials (Dworkin 2008), SNRIs led to a moderately important (31.2%) pain reduction: 1423 out of 3617 participants (39.3%) reported an at least 30% pain reduction, and 1118 out of 3566 (31.4%) reported an at least 50% pain reduction. QOL The outcomes were converted into a 0 to 100 scale, if necessary. Nine studies, with 5457 participants, were entered into an analysis of the mean difference of QOL measured by the FIQ total score at final treatment and at baseline in true drug groups. The pooled mean QOL score was 58.42 (95% CI 45.70 to 64.45). The MD was 14.28 (95% CI 12.84 to 15.72). Based on a benchmark ( Bennett 2009), SNRIs led to a minimal clinically relevant (24.4%) change in the FIQ total score. The outcomes were converted into a 0-10 scale, if necessary. Ten studies, with 4716 participants, were entered into an analysis of the mean difference of pain at final treatment and at baseline in placebo groups. The pooled mean pain score was 6.55 ( 95% CI 6.49 to 6.60). The MD was 1.22 (95% CI 1.11 to 1.33) of a 010 numeric scale. Based on benchmarks for interpreting changes in chronic pain trials (Dworkin 2008), placebo led to a minimally important (18.6%) pain reduction: 717 out of 2387 participants (30.0%) reported an at least 30% pain reduction, and 475 out of 2382 (19.90%) reported an at least 50% pain reduction. The number needed to treat for an additional beneficial outcome (NNTB) to achieve an at least 30% pain reduction by true drug was 11 participants (95% CI 8 to 14). The NNTB to achieve an at least 50% pain reduction by true drug was nine participants (95% CI 7 to 11). QOL The outcomes were converted into a 0 to 100 scale, if necessary. Nine studies with 4262 participants were entered into an analysis of the mean difference of QOL measured by the FIQ total score at final treatment and at baseline in placebo drug groups. The pooled mean QOL score was 55.08 (95% CI 45.70 to 64.45). The MD was 10.06 (95% CI 8.32 to 11.79). Based on a benchmark (Bennett 2009), placebo led to a minimal clinically relevant (18.6%) change in the FIQ total score. Subgroup analysis We restricted the subgroup analyses to the main outcomes. Duloxetine and milnacipran Duloxetine was superior to milnacipran in reducing mean pain and mean sleep problems. The SMD for mean pain reduction in duloxetine groups was -0.32 (95% CI -0.41 to -0.22) and in milnacipran groups -0.20 (95% CI -0.26 to -0.13) (Chi² 4.3; P value 0.04) (see Analysis 1.1). The SMD for mean sleep problem reduction in duloxetine groups was -0.24 (95% CI -0.37 to 0.12), and in milnacipran groups was 0.02 (95% CI -0.05 to 0.10) (Chi² 12.8; P value 0.0003) (see Analysis 1.5).There were no significant differences between the two drugs in the other main outcomes (50% pain reduction, fatigue, QOL, withdrawal due to adverse events (see Analysis 1.3., Analysis 1.4, Analysis 1.8, Analysis 1.13)). Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 19 Studies with and without European participants The RR of a 50% pain reduction was higher in studies without European participants than with European participants (Z = 2.04; P value 0.05). There were no significant differences in the other outcomes (pain, fatigue, QOL, withdrawal due to adverse events) (see Additional Table 1). DISCUSSION Summary of main results The SNRIs duloxetine and milnacipran had a small incremental effect compared to the effect placebo had in reducing pain, disability and tenderness, and increasing patient-perceived global improvement. The incremental effect of duloxetine and milnacipran compared to the effect placebo had in reducing fatigue, depression, limitations of QOL and cognitive disturbances was not substantial. There were no significant differences between duloxetine or milnacipran and placebo in reducing sleep problems and anxiety. The drop out rate due to adverse events with duloxetine or milnacipran was significantly higher than with a placebo. There were no significant differences in the frequency of serious adverse events between duloxetine or milnacipran and placebo. Duloxetine and milnacipran led to a moderately important pain reduction, while placebo led to a minimally important pain reduction. Duloxetine was superior to milnacipran in reducing pain. Both SNRIs and placebo led to a clinically relevant improvement of a disease-specific quality of life score. Overall completeness and applicability of evidence We are sure that we did not miss to include a study with the SNRIs duloxetine and milnacipran, because all trials with these drugs had been registered within the application of an approval for FMS-management by regulatory agencies. We cannot rule out the possibility that negative study results with other SNRIs have not been published or have been missed by our search strategy. All statements regarding the efficacy and safety of SNRIs should be restricted to duloxetine and milnacipran only. We identified one study investigating desvenlaxafine was terminated prior to completion. The limited data available did not suggest any therapeutic effect, therefore, it would be inappropriate to suggest a class effect of SNRIs on FMS-symptoms. The applicability (external validity) of evidence is strongly limited for the following reasons: 1. The studies were performed in research centers and not in routine clinical care. It is known that the efficacy of drug therapies is higher in the context of RCTs than in routine clinical care (Routman 2010). 2. The exclusion criteria were strict. Participants were not allowed to take some defined concomitant medications for their FMS symptoms. This excluded a large number of participants who were unwilling, or unable, to come off medications, such as other antidepressants and anticonvulsants. For this reason, patient selection in the RCTs was biased towards recruiting participants with less severe symptoms than are seen in the community (Fuller-Thomson 2012). Participants with other medical disorders, such as inflammatory rheumatic diseases, were also excluded. The study results cannot be applied to patients with FMS complicated by other medical disorders. Also, the SNRI studies excluded most participants with psychiatric diagnoses. All except one of the studies with milnacipran excluded all potential participants with major mental disorders, while the studies with duloxetine excluded all participants with major mental disorders except for those with major depression and general anxiety disorder. The study results cannot be applied to patients with FMS and concomitant psychiatric disease, except for the duloxetine studies that suggest efficacy in FMS with major depression and general anxiety disorder. 3. The majority of the participants were middle-aged women. The authors of the duloxetine-studies provided a pooled subgroup analysis that demonstrated the efficacy of duloxetine in male participants (Russell 2008). A similar analysis was not available for milnacipran. Both pharmaceutical companies (Eli-Lilly and Pierre Fabre/Forest Laboratories) did not present a subgroup analysis of participants over 65 years of age. The results of these drugs cannot be applied to children and adolescents with FMS, because they were excluded from the trials. The substantial placebo effect seen across all of the SNRI trials is worth noting here. The improvement seen with placebo is considered to be a clinically significant amount. If a similar improvement in pain were seen with a new drug that was tested against placebo, the results would be used to justify its use in FMS. Furthermore, the high degree of placebo effect seen with SNRIs was observed in all FMS drug trials (Häuser 2011a). Quality of the evidence All of the reviewed studies had been sponsored by pharmaceutical companies. Although the original data of half of the studies analyzed in this review had been presented to the EMA and the FDA, a meta-analysis of all studies conducted by an independent statistical unit had not been performed until now. The quality of evidence of this review is based on the data presented in peer reviewed journals and some additional details that were provided on request by the pharmaceutical companies or principal investigators. However, not all data requested were provided. A selective non-reporting of some negative study results on pain, sleep and anxiety, as well as non-reporting of serious adverse events is possible. Despite these limitations, the overall quality of evidence was high for most primary outcomes in the majority of studies (see Summary of findings for the main comparison). Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 20 Potential biases in the review process We searched for unpublished studies with SNRIs other than duloxetine and milnacipran for FMS, but we are not certain that we identified all other studies that might have been performed but not published. We did identify one study that tested desvenlaxafine but it was terminated prior to completion. Efficacy outcomes were analyzed using last observation carried forward to impute missing data. This procedure may lead to an overestimation of efficacy (Moore 2012). The use of the baseline observation carried forward method has been recommended for analysis (Moore 2010a). In addition, the 50% pain reduction rates of two studies with milnacipran were not reported, or provided, on request (Branco 2010; Clauw 2008). We calculated these values by an established imputation method (Furukawa 2005). The influence of allowed co-interventions (e.g. rescue medication) on positive effects and adverse events was unclear because type and dosage of co-interventions were not clearly reported or controlled for. Agreements and disagreements with other studies or reviews We cannot share the conclusion of some reviews that the efficacy of duloxetine and milnacipran in the management of FMS has been proven (Arnold 2010c; Kyle 2010; Ormseth 2010; Ursini 2010). Neither drug has a benefit on all key symptoms of FMS. We confirm the results of a previous analysis, that duloxetine and milnacipran are superior to placebo in the reduction of pain and limitations of QOL (Häuser 2011b), but not in the reduction of fatigue and sleep disturbances. Our results do confirm the conclusions of the aforementioned reviews, that tolerability and safety of both drugs is limited, because a substantial number of participants dropped out of trials due to adverse events. The most frequent adverse events in both drugs were nausea, dry mouth, headache, constipation and hyperhidrosis (increased perspiration) (Häuser 2010b). The lack of difference in serious adverse events between true drug and placebo demonstrated that both drugs are rather safe. The subgroup analyses demonstrated that duloxetine is superior to milnacipran in mean pain reduction, confirming the conclusions of previous analyses performed with adjusted indirect comparisons that did not include all studies available (Häuser 2010b; Häuser 2011b). This review could not confirm the results of a previous analysis (Häuser 2011b), that milnacipran is superior to duloxetine in reducing fatigue, and that duloxetine is superior to milnacipran in reducing sleep disturbances and limitations of QOL. In the light of current regulatory differences regarding the use of SNRIs in FMS in the USA and Europe, it seems relevant to comment on whether the data support either of these positions. It is our view that the trial data show that the benefits of SNRIs (NNTB = 9 for an incremental 50% pain reduction) are nearly counterbalanced by the risk of side effects (number needed to treat for an additional harmful outcome (NNTH) = 11 for an incremental drop out rate due to adverse events). The data do not provide clear support for either of the regulatory positions over the other. If duloxetine or milnacipran are being considered for the treatment of FMS, a frank discussion between the physician and patient about the potential benefits and harms of both drugs should occur. The contraindications (concomitant use of monoaminooxydase inhibitors, uncontrolled narrow-angle glaucoma, substantial alcohol use or evidence of chronic liver damage) and warnings (suicidality, hepatotoxicity, serotonin syndrome, abnormal bleeding, discontinuation syndrome, elevated blood pressure, urinary hesitation and retention) should also be kept in mind (Häuser 2010b). The recommended dosages are duloxetine 60 mg/day, and milnacipran 100 mg/day. Häuser 2010b observed that higher dosages are not more efficacious, but are associated with more adverse events. Monotherapy of FMS with duloxetine and milnacipran should be discouraged. Current best practices in FMS guidelines recommend using a combination of pharmacological therapy with aerobic exercise and psychological therapies. Although the combination of SNRIs with non-pharmacological treatment options has not been tested in randomized controlled trials, this dearth of data should not be used as a reason to avoid combination therapy. This is especially true for symptoms where duloxetine and milnacipran are ineffective, but other therapies are effective, e.g. aerobic exercise for fatigue (Häuser 2010c), and cognitive-behavioral therapies for depression (Bernardy 2010). AUTHORS’ CONCLUSIONS Implications for practice Of the SNRIs currently available, only duloxetine and milnacipran have been sufficiently studied for the management of FMS.The potential benefit of duloxetine and milnacipran to reduce pain is counterbalanced by their potential harms: 22% of participants reported a substantial (at least 50%) pain reduction at post-treatment; 21% discontinued medication due to adverse events. Both drugs did not reduce sleep problems. Their incremental benefit over placebo to reduce fatigue was not substantial. Both drugs have been approved for treatment of FMS in USA, but not in Europe. Duloxetine is approved in most European countries for major depression. Its efficacy in pain reduction has been shown for FMS-patients with and without major depression (Arnold 2005; Russell 2008). In contrast, there are no data available to show whether milnacipran is effective in FMS-patients with major depression. Therefore, duloxetine can be regarded to be the first drug option for FMS-patients with major depression. Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 21 Lastly, it should be noted that the positive effects of duloxetine and milnacipran on FMS-symptoms has been proven for only six months in placebo-controlled trials, therefore, a trial of omission can be considered with responders after these time intervals. Implications for research The main research directions that would help in the future include: Available studies with SNRIs in FMS Analysis of all studies investigating duloxetine and milnacipran in FMS at the level of individual patient data could provide important information, e.g. whether or not a clinically important pain response delivers large functional and quality of life benefits (Moore 2010b). Moreover, a re-analysis of the data using baseline observation carried forward, and responder analysis where discontinuation is classified as non-response, would allow a determination of the true efficacy of duloxetine and milnacipran in FMS. These analyses should be performed by a research team not affiliated with the manufacturers of the drugs. Future studies with SNRIs in FMS 1. Duloxetine and milnacipran are effective in a minority of patients. Clinical effectiveness trials with SNRIs are necessary; they should provide information on the proportion of patients with a moderate or substantial response, with tolerable adverse events, and with willingness to continue therapy (Moore 2010c). 2. The significance of the two SNRIs duloxetine and milnacipran compared to established therapies such as aerobic exercise, amitriptyline and cognitive-behavioral therapies in the management of FMS still needs to be determined. 3. Clinical studies in FMS should be conducted with patient samples representative of clinical practice including participants with comorbid anxiety, affective disorders and inflammatory rheumatic diseases. Moreover, studies should include participants with different durations of disease and levels of severity all over the world. Subgroup analyses for male participants and seniors should also be conducted. 4. The assessment strategies of adverse events in RCTs should be standardized by regulatory agencies. Potential effects of cointerventions on outcomes should be controlled for. 5. The definition of subgroups (e.g. FMS with and without major depression) and the development of more tailored therapies are major tasks of future research. ACKNOWLEDGEMENTS None. REFERENCES References to studies included in this review blind, placebo-controlled trial. Arthritis and Rheumatism 2010;62(9):2745–56. Arnold 2004 {published and unpublished data} Arnold LM, Lu Y, Crofford LJ, Wohlreich M, Detke MJ, Iyengar S, et al.A double-blind, multicenter trial comparing duloxetine with placebo in the treatment of fibromyalgia patients with or without major depressive disorder. Arthritis and Rheumatism 2004;50(9):2974–84. Branco 2010 {published data only} Branco JC, Zachrisson O, Perrot S, Mainguy Y, Multinational Coordinator Study Group. A European multicenter randomized double-blind placebo-controlled monotherapy clinical trial of milnacipran in treatment of fibromyalgia. 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Published by John Wiley & Sons, Ltd. 26 CHARACTERISTICS OF STUDIES Characteristics of included studies [ordered by study ID] Arnold 2004 Methods Study setting: multicenter study with 18 outpatient research centres in USA Study design: parallel Duration therapy: 12 weeks Follow-up: not described Analysis: ITT; LOCF; mixed-effects model: the model included the fixed, categorical effects of treatment, investigator, visit, and interaction of treatment with visit, as well as the continuous, fixed covariates of baseline and interaction of baseline with visit Participants Participants: 207 (89% female, 87% white, mean age 49 years) Inclusion criteria: ACR 1990 criteria; score ≥ 4 on the pain intensity item of the FIQ; age ≥ 18 years; with and without major depressive disorder (MDD) Exclusion criteria: pain from traumatic injury or structural or regional rheumatic disease; rheumatoid arthritis, inflammatory arthritis, or autoimmune disease; unstable medical or psychiatric illness; current dysthymia, which is more resistant to treatment than major depression, or primary psychiatric disorder other than MDD; substance abuse in the last year; history of psychosis; pregnancy or breast feeding; unacceptable contraception in those of childbearing potential; involvement in disability reviews that might compromise treatment response; use of an investigational drug within 30 days; prior participation in a study of duloxetine; severe allergic reactions to multiple medications; intolerance to 3 psychoactive drugs or 1 SSRI; and failure to respond to 2 adequate regimens of 2 different classes of antidepressants for depression or fibromyalgia. Concomitant medication exclusions included use of medications or herbal agents with CNS activity (antidepressants required a 7-day washout prior to visit 2 except for monoamine oxidase inhibitors, which required a 14-day washout, and fluoxetine, which required a 30-day washout); regular use of analgesics with the exception of acetaminophen up to 2 g/day and aspirin up to 325 mg/day; chronic use of sedatives, antiemetics, or antispasmodics; episodic use of anticoagulants; 3 months stable therapy with antihypertensives, hormones, antiarrhythmics, antidiarrheals, antihistamines, cough/cold preparations (excluding dextromethorphan), or laxatives; and initiation of or change in unconventional or alternative therapies Interventions Active drug: DLX 120 mg (n = 104) for 12 weeks. Titration from 20 mg/day to 60 mg twice a day during first 2 weeks of the therapy phase, as follows: 20 mg every day for 5 days, 20 mg twice a day for at least 3 days, 40 mg twice a day for at least 2 days, and 60 mg twice a day for the remainder of the study Placebo (n = 103) for 12 weeks Rescue and/or allowed medication: acetaminophen (paracetamol) up to 2 g/day and aspirin up to 325 mg/day Outcomes Pain: Brief Pain Inventory (BPI) average pain severity (NRS 0-10) Fatigue: FIQ single item (VAS 0-10) Sleep: BPI (NRS 0-10): not reported Depression: BDI -II total score (NRS 0-63) Anxiety: Beck Anxiety Inventory total score (NRS 0-63) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 27 Arnold 2004 (Continued) Disability: BPI interference from pain (NRS 0-10) Sexual function: not assessed Quality of life: FIQ total score (0-80) Cognitive disturbances: not assessed Global perceived improvement: Patient Global Impression of Change PGIC (1-7) Tenderness: mean tender point threshold (kg/cm²) Adverse events (AEs): physical examination, electrocardiograms (EKGs ,ECGs), and laboratory analysis. Details of assessment of adverse symptoms not reported Notes Safety: 90.4% of the DLX and 74.8% of the placebo group reported at least 1 adverse event (AE) (P < 0.01). DLX-treated subjects reported insomnia, dry mouth, and constipation significantly more frequently than did placebo-treated subjects. Most treatmentemergent AEs were of mild or moderate severity. There were no significant treatment group differences in the percentage of severe treatment-emergent AEs (details not reported). No deaths were reported These mean differences in laboratory test were within normal reference ranges and were not considered clinically relevant. No subject experienced elevated corrected QT intervals during the study Risk of bias Bias Authors’ judgement Support for judgement Random sequence generation (selection Low risk bias) Computer-generated random sequence using an interactive response system Allocation concealment (selection bias) Low risk Central independent unit (details reported on request) Incomplete outcome data (attrition bias) All outcomes Low risk Imputation using last observation carried forward for efficacy data. ITT analysis Selective reporting (reporting bias) High risk Outcomes: sleep problems, 30% pain reduction and serious AEs not reported Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar, details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 28 Arnold 2005 Methods Study setting: multicenter study with 21 outpatient research centres in USA Study design: parallel Duration therapy: 12 weeks Follow-up: not described Analysis: ITT; LOCF; primary analysis: changes from baseline to endpoint on the BPI average pain severity score, other efficacy measures were analysed by an analysis of covariance (ANCOVA) model with the terms of treatment, investigator, and baseline score. Secondary analysis: longitudinal changes from baseline on continuous efficacy measures analysed with a mixed-effects model for analysis of repeated measures. The model included the fixed, categorical effects of treatment, investigator, visit, and treatment-byvisit interaction, as well as the continuous, fixed covariates of baseline and baseline-byvisit interaction Participants Participants: 354 (100% females, 90% white, mean age 49.6 years) Inclusion criteria: ACR 1990 criteria; score ≥ 4 on the pain intensity item of the FIQ; age ≥ 18 years; with and without MDD Exclusion criteria: pain from traumatic injury or structural or regional rheumatic disease; rheumatoid arthritis, inflammatory arthritis, or autoimmune disease; unstable medical or psychiatric illness; current primary psychiatric diagnosis other than MDD, a primary anxiety disorder within the past year (specific phobias allowed); substance abuse within the past year; serious suicide risk; pregnancy or breast-feeding; women who, in the opinion of the investigator, were treatment refractory or may have had an involvement in disability reviews that might compromise treatment response; severe allergic reactions to multiple medications; or prior participation in a study of DLX. Concomitant medication exclusions included use of medications or herbal agents with CNS activity; regular use of analgesics with the exception of acetaminophen up to 2 g/day and aspirin for cardiac prophylaxis up to 325 mg/day; chronic use of sedatives, antiemetics, or antispasmodics; and initiation of or change in unconventional or alternative therapies Interventions Active drugs DLX 60 mg/day (118) participants DLX 120 mg/day (116 participants): forced titration from 60 mg/d to 120 mg/d within 3 days Placebo (120 participants) Rescue and or allowed medication: acetaminophen up to 2 g/day and aspirin up to 325 mg/day Outcomes Pain: (BPI average pain severity (NRS 0-10) Fatigue: FIQ (VAS 0-10): not reported Sleep: BPI sleep interference (NRS 0-10) Depression: Hamilton Depression Rating Scale HDRS (NRS 0-52) Anxiety: FIQ (VAS 0-10): not reported Disability: BPI interference from pain (NRS 0-10) Sexual function: not assessed Quality of life: FIQ total score (0-80) Cognitive disturbances: not assessed Global perceived improvement: PGIC (1-7) Tenderness: mean tender point threshold (kg/cm²) AEs: physical examination, electrocardiograms (EKGs/ECGs), and laboratory analysis. Details of assessment of adverse symptoms not reported Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 29 Arnold 2005 (Continued) Notes Safety: 92.4% of the participants in the DLX 60 mg group and 90.5% of the participants in the DLX 120 mg group reported at least 1 AE compared to placebo group (79.2%). Participants in the DLX 60 mg and 120 mg groups reported nausea, dry mouth, constipation, decreased appetite and anorexia significantly more frequently than did placebotreated participants. Diarrhea and nasopharyngitis were reported more frequently by participants treated with DLX 60 mg than did placebo treated participants. Somnolence, increased sweating, feeling jittery, and nervousness were reported significantly more frequently by participants on DLX 120 mg compared with placebo-treated participants. There were no significant treatment group differences in the percentage of serious treatment-emergent AEs (1 blood creatine phosphokinase and 1 hepatic enzyme increase each in DLX groups). No deaths were reported Mean increases of alkaline phosphatase and a mean decrease in chloride, mean increase of weight, systolic and diastolic heart pressure in both DLX-groups over placebo were significant, but not considered clinically relevant Risk of bias Bias Authors’ judgement Support for judgement Random sequence generation (selection Low risk bias) Computer-generated random sequence using an interactive response system (details reported on request) Allocation concealment (selection bias) Low risk Central independent unit (details reported on request) Incomplete outcome data (attrition bias) All outcomes Low risk Imputation using last observation carried forward for efficacy data. ITT analysis Selective reporting (reporting bias) Unclear risk Outcome of anxiety not reported Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar, details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 30 Arnold 2010a Methods Study setting: multicenter study with 48 outpatient research centres in USA and Puerto Rico Study design: parallel Duration therapy: 24 weeks Follow-up: not described Analysis: ITT; LOCF; a restricted maximum likelihood-based MMRM analysis utilized on longitudinal changes from baseline for continuous efficacy measures.The model included the fixed categorical effects of treatment, investigator, visit, and treatment-byvisit interaction, as well as the continuous, fixed covariates of baseline score and baseline score-by-visit interaction. LOCF changes from baseline to endpoint were analyzed using an analysis of covariance (ANCOVA) model with the terms of treatment, investigator, and baseline scores. Continuous baseline measures were evaluated using fixedeffects (treatment, investigator) analysis of variance (ANOVA), and categorical baseline measures were evaluated using Fisher’s exact test. Continuous safety measures were analyzed using MMRM, ANOVA, or ANCOVA as described above, and categorical safety measures were analyzed using Fisher’s exact test. Rank-transformed laboratory analytes were analyzed using the ANOVA model to assess treatment differences. Participants Participants: 530 (93% female, 77% white, mean age 50 years) Inclusion criteria: ACR 1990 criteria; score ≥ 4 on the pain intensity item of the FIQ; age ≥ 18 years; with and without MDD/generalized anxiety disorder (GAD) Exclusion criteria: current or diagnosed within the past year with any primary psychiatric disorder other than MDD or GAD defined by DSM-IV; clinically judged to be at serious risk of suicide; had any unstable medical illness likely to require intervention or hospitalization; pain symptoms unrelated to FM that could interfere with interpretation of outcome measures; regional pain syndromes; multiple surgeries or failed back syndrome; a confirmed current or previous diagnosis of rheumatoid arthritis, inflammatory arthritis, or other autoimmune disease; severe liver disease; pregnant or breast-feeding; or history of substance abuse within the past year. Participants were also excluded if they had been treated with an adequate trial of DLX and did not respond or could not tolerate DLX; were judged by the opinion of the investigator to be treatment-refractory in FM; or whose treatment response might be compromised by disability compensation issues Interventions Active drug:DLX flexible 60-120 mg/day (263 participants): DLX was initiated at 30 mg and escalated to 60 mg after 1 week. At week 4 and week 8 visits, DLX dose was automatically escalated via IVRS by 30 mg daily for those participants who had < 50% reduction from baseline in their BPI 24-hour pain score and the investigator had endorsed a dose increase. If the patient could not tolerate the dose increase, it was reduced to the pre-escalation dose via IVRS Placebo (267 participants) Rescue and/or allowed medication: acetaminophen up to 2 g/day and aspirin up to 325mg/day Outcomes Pain: BPI 24-h average pain severity (NRS 0-10) Fatigue: MFI general fatigue (NRS 4-20) Sleep: bothered by sleep difficulties (NRS 0-10): data extracted from figure Depression: BDI total score (NRS 0-63) Anxiety: BAI total score (NRS 0-63) Disability: BPI pain interference pain (NRS 0-10) Sexual function: not assessed Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 31 Arnold 2010a (Continued) Quality of life: FIQ not used Cognitive disturbances: MFI mental fatigue (NRS 4-20) Global perceived improvement: PGIC (NRS 1-7) Tenderness: not assessed AEs: physical examination, EKGs, and laboratory analysis. Details of assessment of adverse symptoms not reported Notes Safety: significantly more participants in the DLX group than in the placebo group reported at least 1 AE (82.9% vs 71.5%). Participants in the DLX group reported significantly more nausea, headache, constipation,dry mouth, dizziness, diarrhea, hyperhidrosis, hot flush, vomiting, feeling jittery and middle insomnia. Occurrence of constipation and hyperhydrosis were severe and significantly greater with DLX treatment. There were no significant treatment group differences in the rate of serious AEs (SAEs) (1 suicidal ideation in placebo group) Mean increases in some laboratory tests, mean increase of weight, systolic and diastolic heart pressure in DLX group over placebo were significant, but not considered clinically relevant Risk of bias Bias Authors’ judgement Support for judgement Random sequence generation (selection Low risk bias) Computer-generated random sequence using an interactive response system Allocation concealment (selection bias) Low risk Central independent unit (details reported on request) Incomplete outcome data (attrition bias) All outcomes Low risk Imputation using last observation carried forward for efficacy data. ITT analysis Selective reporting (reporting bias) Unclear risk Outcome of sleep not reported Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar-details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 32 Arnold 2010b Methods Study setting: multicenter study with 68 outpatient research centres in USA and Canada Study design: parallel Duration therapy: 18-20 weeks Follow-up: not described Statistical analysis: ITT, BOCF and LOCF (LOCF data reported);data were analyzed at each post-baseline visit using an analysis of covariance (ANCOVA) model, with treatment group and study center as factors and the baseline value as a covariate, except for PGIC, which were analyzed using analysis of variance (ANOVA) Participants Participants: 1025 participants (95% women, 91% white, mean age 49 years) Inclusion criteria: 1990 ACR criteria, 18-70 years, raw score of ≥ 4 on the FIQ Exclusion criteria: previous exposure to milnacipran (MLN); treatment with an investigational drug within 30 days of screening; BDI score > 25 at screening or randomization; current major depressive episode as determined by MINI; significant risk of suicide according to investigator’s judgment or results of the MINI or BDI; lifetime history of psychosis, hypomania, or mania; substance abuse; other severe psychiatric illness as determined by investigator judgment; history of behavior that would, in the investigator’s judgment, prohibit compliance for the duration of the study; active or pending disability claim, workman’s compensation claim, or litigation; pregnancy or breastfeeding; unacceptable contraception; active or unstable medical illness; prostate enlargement or other genitourinary disorder Interventions Active drug: MLN flexible up to 100 mg/day (516 participants): MLN 12.5 mg on days 1-3; MLN 25 mg (12.5 mg twice daily) for 4 days; MLN 50 mg (25 mg twice daily) for 7 days; MLN 75 mg (37.5 mg twice daily) for 7 days; and MLN 100 mg (50 mg twice daily) for 7 days. If side effects developed, the dose of milnacipran could be temporarily reduced Placebo (509 participants) Rescue and allowed medication: tramadol or hydrocodone between randomisation and week 4 (end of dose escalation). Permitted analgesic medications were acetaminophen, aspirin, and NSAIDs Outcomes Pain: PED 24-h recall pain score (VAS 0-100) Fatigue: MFI total (NRS 20-100) Sleep: BPI sleep interference: not reported Depression: BDI total score (NRS 0-63) Anxiety: BAI total score (NRS 0-63) Disability: BPI pain interference pain (NRS 0-10) Sexual function: not assessed Quality of life: FIQ total score (VAS 0-100) Cognitive disturbances: MASQ cognitive function (NRS 38-190) Global perceived improvement: PGIC (NRS 1-7) Tenderness: not assessed AEs: physical examination, EKGs, and laboratory analysis. Details of assessment of adverse symptoms not reported Notes Safety: AEs reported in 75.0% in the placebo group and 84.1% in MLN group (P < 0. 001). Nausea, constipation, hot flush, dizziness, hyperhidrosis, palpitations, tachycardia and hypertension more frequent in MLN than in placebo. Proportion of participants Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 33 Arnold 2010b (Continued) experiencing SAEs was comparable across treatment groups. No deaths reported during study Mean increases in some laboratory tests, mean increase of weight, systolic and diastolic heart pressure in DLX group over placebo were significant, but not considered clinically relevant Risk of bias Bias Authors’ judgement Support for judgement Random sequence generation (selection Low risk bias) Computer-generated random sequence using an interactive response system Allocation concealment (selection bias) Low risk Central independent unit Incomplete outcome data (attrition bias) All outcomes Low risk Imputation using last observation carried forward for efficacy data. ITT analysis Selective reporting (reporting bias) Unclear risk Outcomes of sleep and anxiety not reported Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar, details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Branco 2010 Methods Study setting: multicenter study with 89 outpatient research centres in 13 European countries Study design: parallel Duration therapy: 17 weeks Follow-up: not described Analysis: ITT; LOCF; change from baseline in FIQ score was analyzed using a covariance analysis (ANCOVA) model with baseline FIQ score as a covariate and country and treatment as fixed factors. Changes from baseline in other secondary efficacy assessments were similarly analyzed using ANCOVA Participants Participants: 884 (94% female, % white not reported and not provided on request, mean age 49 years) Inclusion criteria: 1990 ACR criteria; raw score ≥ 3 on physical function component of FIQ; baseline VAS pain intensity rating between 40-90 (0-100 scale) Exclusion criteria: severe psychiatric illness including generalized anxiety disorder or current major depressive episode (assessed by MINI, BDI27 score > 25), alcohol/substance abuse; significant cardiovascular, respiratory, rheumatoid, rheumatic, hepatic, renal, or other medical condition; systemic infection; epilepsy; active cancer; severe sleep Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 34 Branco 2010 (Continued) apnea; unstable endocrine disease; active peptic ulcer or inflammatory bowel disease; prostatic enlargement or other genitourinary disorders (in male participants); pregnancy or breastfeeding; and history or behavior that would prohibit compliance for the duration of the study Interventions Active drug: MLN 200 mg/day (430 participants): 25 mg once daily (evening dose, days 1 and 2); 25 mg twice daily (days 3-7); 50 mg (days 8-14); 50 mg (morning dose) and 100 mg (evening dose, days 15-21); and 100 mg (days 22-28). Participants then entered the 12-week stable-dose treatment period, followed by a 9-day down-titration phase and a 2-week follow-up phase without treatment Placebo (446 participants) Rescue or allowed medication: not reported Outcomes Pain: PED 24-h recall pain score (VAS 0-100); 50% response rates not reported and not provided on request; calculated by imputation method Fatigue: MFI total (NRS 20-100) Sleep: MOS-Sleep Index II (NRS 0-100) Depression: BDI total score (NRS 0-63) Anxiety: State-Trait Anxiety Inventory (NRS 20-80) Disability: BPI pain interference pain (NRS 0-10) Sexual function: not assessed Quality of life: FIQ total score (VAS 0-100) Cognitive disturbances: MASQ cognitive function (NRS 38-190) Global perceived improvement: PGIC: details insufficiently reported Tenderness: not assessed AEs: physical examination, EKGs, and laboratory analysis. AEs were assessed throughout the study based on spontaneous reporting by participants, investigators’ use of nonleading questions, and clinical evaluation Notes Safety: a total of 331 (74.2%) placebo-treated participants and 363 (84.2%) milnacipran-treated participants experienced at least 1 treatment-emergent AE (P < 0.01) . Nausea, hyperhidrosis, constipation, palpitations, hot flush and tachycardia occurred significantly more frequent in MLN group than in placebo group. Potentially clinically significant increases in supine systolic BP (≥ 180 mmHg with ≥ 20 mmHg increase from baseline), diastolic BP (≥ 105 mmHg with ≥ 15 mmHg increase from baseline), and heart rate (≥ 120 bpm with ≥ 15 bpm increase from baseline) observed in 0.9%, 3.5%, and 1.4%, respectively, of participants treated with milnacipran, compared with 1.1%, 2.0%, and 0.2%, respectively, for placebo-treated participants. No deaths were reported during the study Risk of bias Bias Authors’ judgement Random sequence generation (selection Low risk bias) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. Support for judgement Computer-generated random sequence using an interactive response system (details provided on request) 35 Branco 2010 (Continued) Allocation concealment (selection bias) Low risk Central independent unit (details provided on request) Incomplete outcome data (attrition bias) All outcomes Low risk Imputation using last observation carried forward for efficacy data. ITT analysis Selective reporting (reporting bias) High risk 50% pain reduction not reported and not provided on request; The FDA report on MLN stated that a female participant committed suicide and that this death was possibly related to MLN Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar-details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Chappell 2008 Methods Study setting: multicenter study with 36 outpatient research centres in Western Europe (Germany, Spain, Sweden, UK) and USA Study design: parallel Duration therapy: 27 weeks Follow-up: not described Analysis: ITT; LOCF; an analysis-of-covariance (ANCOVA) model was the primary analytic method used to analyzed continuous efficacy variables, overall and within subgroups, where the model contained the main effects of treatment and investigator, with the baseline score as a covariate. The treatment-by-investigator interaction was tested using a separate ANCOVA. Some efficacy variables measured repeatedly over time were analyzed using a likelihood-based MMRM approach, to better understand the time profile of response. The model included the fixed categorical effects of treatment, investigator, visit, and treatment-by-visit interaction, as well as the continuous fixed covariates of baseline score and baseline score-by-visit interaction Participants Participants: 330 (93% women, 91% white, mean age 50 years) Inclusion criteria: ACR 1990 criteria; age ≥ 18 years; with and without MDD Exclusion criteria: current or previous treatment with DLX; any current primary Axis I diagnosis other than MDD; pain symptoms related to traumatic injury, structural rheumatic disease, or regional rheumatic disease (such as osteoarthritis, bursitis, tendonitis); regional pain syndrome; multiple surgeries or failed back syndrome; confirmed current or previous diagnosis of rheumatoid arthritis, inflammatory arthritis, infectious arthritis, or an autoimmune disease; and serious medical illness Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 36 Chappell 2008 (Continued) Interventions Active drug: DLX 60 mg/day or 120 mg/day (162 participants): participants randomly assigned to the DLX 60 mg treatment group underwent a titration in which they received DLX 30 mg for 1 week before receiving DLX 60 mg for 12 weeks. At visit 8 (week 13) participants who did not have 50% reduction in the BPI-Modified Short Form average pain scorewere blindly escalated to 120 mg. Those that could not tolerate this dose were allowed to return to the 60 mg dose. Participants were allowed to increase their dose to 120 mg at any time between visits 8 and 10 (weeks 13 and 23), based upon whether they had 50% reduction in their BPI average pain score. If at any time between visits 9 and 11 (weeks 18 and 27) participants had tolerability issues with the higher dose (120 mg), they were allowed to go back to the lower dose (60 mg) Placebo (168 participants) Rescue or allowed medication: not reported Outcomes Pain: BPI 24-h average pain severity (NRS 0-10) Fatigue: MFI general fatigue (NRS 4-20) Sleep: BPI sleep interference (NRS 0-10): not reported Depression: BDI-II total score (NRS 0-63) Anxiety: FIQ anxiety (VAS 0-10): not reported Disability: BPI pain interference (NRS 0-10) Sexual function: not assessed Quality of life: FIQ total score (VAS 0-80) Cognitive disturbances: MFI mental fatigue (NRS 4-20) Global perceived improvement: PGIC (NRS 1-7) Tenderness: mean tender point threshold (kg/cm²) AEs: physical examination, EKGs, and laboratory analysis. AEs were assessed throughout the study based on spontaneous reporting by participants Notes Safety: Significantly more participants with DLX reported at least 1 AE compared to placebo (89.5% vs 81.5%; P 0.04). AEs that occurred in 5% of DLX-treated and twice the rate of placebo-treated participants included nausea, headache, dry mouth, diarrhoea, constipation, hyperhidrosis, arthralgia, somnolence, dyspepsia, sleep disorder. No significant difference between treatment groups was observed in the percentage of participants with at least 1 SAE. There were no deaths Mean increases of alkaline phosphatase, alanine transaminase and a mean decrease in chloride, mean increase of weight, systolic and diastolic heart pressure in both DLXgroups over placebo were significant, but not considered clinically relevant Risk of bias Bias Authors’ judgement Support for judgement Random sequence generation (selection Low risk bias) Computer-generated random sequence stratified by major depression status within each study centre Allocation concealment (selection bias) Central independent unit (details reported on request) Low risk Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 37 Chappell 2008 (Continued) Incomplete outcome data (attrition bias) All outcomes Low risk Imputation using last observation carried forward for efficacy data. ITT analysis Selective reporting (reporting bias) Unclear risk Outcomes of sleep and anxiety not reported Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar, details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Clauw 2008 Methods Study setting: multicenter study with 86 outpatient research centres in USA Study design: parallel Duration therapy: 15 weeks Follow-up: not described Analysis: ITT; BOCF for primary endpoints, LOCF for secondary endpoints; ANCOVA with baseline values as covariates Participants Participants: 1196 (96% female, 93% white, mean age 50 years) Inclusion criteria: 1990 ACR criteria; raw score ≥ 4 on the physical function component of the FIQ; baseline VAS pain intensity rating between ≥ 40 (0 to 100 scale) Exclusion criteria: severe psychiatric illness including generalized anxiety disorder or current major depressive episode (assessed by MINI), BDI27 score > 25; alcohol/substance abuse; significant cardiovascular, respiratory, rheumatoid, rheumatic, hepatic, renal, or other medical condition; systemic infection; epilepsy; active cancer; severe sleep apnea; unstable endocrine disease; active peptic ulcer or inflammatory bowel disease; prostatic enlargement or other genitourinary disorders (in male participants); pregnancy or breastfeeding; and history or behavior that would prohibit compliance for the duration of the study Interventions Active drugs MLN 100 mg/day (399 participants): dose escalation within 3 weeks MLN 200 mg/day (396 participants): dose escalation within 3 weeks Placebo (401 participants) Rescue medication: hydrocodone up to 60 mg/day Outcomes Pain: PED 24-h recall pain score (VAS 0-100); 50% response rates not reported and not provided on request; calculated by imputation method Fatigue: MFI total (NRS 20-100) Sleep: MOS-Sleep Index II (NRS 0-100) Depression: BDI total score (NRS 0-63) Anxiety: FIQ anxiety (VAS 0-10): not reported Disability: MDHAQ disability subscale score Sexual function: Arizona sexual experience scale: not reported Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 38 Clauw 2008 (Continued) Quality of life: FIQ total score (VAS 0-100) Cognitive disturbances: MASQ cognitive function (NRS 38-190) Global perceived improvement: PGIC (NRS 1-7) Tenderness: not assessed AEs: physical examination, EKGs, and laboratory analysis. AEs were assessed throughout the study based on spontaneous reporting by participants and investigators’ observation Notes Safety: 89.7% of the participants in the MLN 100 mg group, 87.4% in the MLN 20 mg group and 79.1% in the placebo group reported at least 1 AE (P < 0.001). AEs occurring in ≥ 5% in either MLN group and with an incidence ≥ 2 times as high as in placebo group were constipation, hot flush, dizziness, palpitations, hyperhidrosis, hypertension, vomiting, increased heart rate and migraine. No significant differences in potentially clinically relevant increase in supine heart rate or systolic blood pressure were found between MLN and placebo groups Risk of bias Bias Authors’ judgement Support for judgement Random sequence generation (selection Low risk bias) Computer-generated random sequence using an interactive response system (details provided on request) Allocation concealment (selection bias) Low risk Central independent unit (details provided on request) Incomplete outcome data (attrition bias) All outcomes Low risk Imputation using baseline and last observation carried forward for efficacy data. ITT analysis Selective reporting (reporting bias) High risk Anxiety scores and number of 50% pain reduction not reported and not provided on request Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar, details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 39 Mease 2009a Methods Study setting: multicenter study with 59 outpatient research centres in USA Study design: parallel Duration therapy: 27 weeks Follow-up: not described Analysis: ITT; BOCF for primary endpoints, LOCF for secondary endpoints; changes from baseline in paper-based VAS assessments of pain, as well as other secondary efficacy assessments, were summarized by treatment group and visit. These data were analyzed at each post-baseline visit using an ANCOVA model, with treatment group and study centre as factors and the baseline value as a covariate Participants Participants: 888 (95% female, 94% white, mean age 49 years) Inclusion criteria: 1990 ACR criteria; baseline VAS pain intensity rating between ≥ 50 (0 to 100 scale) Exclusion criteria: severe psychiatric illness; current major depressive episode (as assessed by MINI); significant risk of suicide according to the investigator’s judgment; alcohol or other drug abuse; a history of significant cardiovascular, respiratory, endocrine, genitourinary, liver, or kidney disease; autoimmune disease; systemic infection; cancer or current chemotherapy; significant sleep apnea; active peptic ulcer or inflammatory bowel disease Interventions Active drugs MLN 100 mg/day (224 participants): dose-escalation period lasted 3 weeks MLN 200 mg/day (441 participants):dose-escalation period lasted 3 weeks Placebo (223 participants) Rescue medication: hydrocodone up to 60 mg/day Outcomes Pain: PED 24-h recall pain score (VAS 0-100); missing means and SDs provided on request Fatigue: MFI total (NRS 20-100); missing SDs reported on request Sleep: MOS-Sleep Index I (NRS 0-100); missing SDs provided on request Depression: BDI total score (NRS 0-63): missing means and SDs provided on request Anxiety: FIQ (VAS 0-10): not reported Disability: SF-36 physical function (0-50): missing means and SDs provided on request Sexual function: Arizona sexual experience scale (NRS 5-30); missing means and SDs provided on request Quality of life: FIQ total score (VAS 0-100): missing SDs provided on request Cognitive disturbances: MASQ cognitive function (NRS 38-190) Global perceived improvement: PGIC (NRS 1-7): only OC cases reported and analyzed Tenderness: not assessed AEs: physical examination, EKGs, and laboratory analysis. AEs were assessed throughout the study based on spontaneous reporting by participants and investigators’ observation Notes Safety: the incidence of treatment-emergent AEs was 85.2% among placebo participants and 90.7% and 83.9% among participants on MLN 200 mg/day and 100 mg/day, respectively. AEs occurred in at least 5% of participants in either MLN treatment group, and at an incidence of 2 times that of placebo participants, and included: constipation, hyperhidrosis, hot flush, vomiting, increased heart rate, dry mouth, palpitations, and hypertension 3 participants had SAEs that were judged to be possibly or probably related to study Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 40 Mease 2009a (Continued) medication, including 1 case each of chest discomfort, exercise-induced intermittent rapid heart rate and chest pain, and nausea. Cardiac assessments in the first 2 cases revealed no evidence of coronary ischemia and neither patient experienced long-term sequelae. The frequency of potentially clinically significant changes in supine systolic (≥ 180 mmHg with an increase of ≥ 20 mmHg from baseline) or diastolic blood pressure (≥ 110 mmHg with an increase of ≥ 15 mmHg from baseline) was comparable among MLN-treated and placebo-treated participants Risk of bias Bias Authors’ judgement Support for judgement Random sequence generation (selection Low risk bias) Computer-generated random sequence using an interactive response system (details provided on request) Allocation concealment (selection bias) Low risk Central independent unit (details provided on request) Incomplete outcome data (attrition bias) All outcomes Low risk Imputation using last observation carried forward for efficacy data. ITT analysis Selective reporting (reporting bias) Unclear risk Standard deviations of outcome “sexual dysfunction” not reported and not provided on request Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar-details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 41 Russell 2008 Methods Study setting: multicenter study with 38 outpatient research centres in USA and Puerto Rico Study design: parallel Duration: 26 weeks Follow up: not described Analysis: ITT; LOCF; for continuous efficacy variables, with the exception of the PGI-I scores, treatment group differences in change from baseline to endpoint were examined using an analysis of covariance (ANCOVA) model with treatment and investigator as main effects and the baseline score as the covariate. To assess the robustness of the coprimary endpoints, a similar ANCOVA analysis in which the baseline observation was carried forward (BOCF) for all participants who discontinued early was implemented post hoc for the BPI average pain score. Similarly, for the PGI-I, mean scores at endpoint were reassessed with all discontinued participants assigned an endpoint PGI-I score of 4, corresponding to “no change” Participants Participants: 520 (95% women, 84% white, mean age 51 years) Inclusion criteria: ACR 1990 criteria; score ≥ 4 on the pain intensity item of the FIQ; age ≥ 18 years; with and without MDD Exclusion criteria: any current primary psychiatric diagnosis other than MDD; pain symptoms unrelated to fibromyalgia that could interfere with interpretation of outcome measures; regional pain syndromes; multiple surgeries or failed back syndrome; a confirmed current or previous diagnosis of rheumatoid arthritis, inflammatory arthritis, or other autoimmune disease; unstable medical or psychiatric disorders; severe liver disease; current pregnancy or breast-feeding; or a history of substance abuse within the past year. Participants who were judged by the investigator to be treatment-refractory or whose response might be compromised by disability compensation issues in the opinion of the investigator were also excluded Interventions Active drugs DLX 20/60 mg/day (79 participants): blindly increased to 60 mg/day after 3 months on study drug when participants entered the second half of the 6-month trial DLX 60 mg/day (150 participants): started at 30 mg/day for 1 week, then titrated to 60 mg/day DLX 120 mg/day (147 participants): started at 30 mg/day for 1 week, then titrated to 60 mg/day for 1 week, and then to 120 mg/day Placebo (144 participants) Rescue and/or allowed medication: acetaminophen up to 2 g/day and aspirin up to 325 mg/day Outcomes Pain: BPI average pain severity (NRS 0-10) Fatigue: MFI general fatigue (NRS 4-20) Sleep: BPI sleep interference (NRS 0-10): not reported Depression: BDI-II total score (NRS 0-63): incompletety reported Anxiety: FIQ anxiety (VAS 0-10): not reported Disability: BPI pain interference pain (NRS 0-10) Sexual function: not assessed Quality of life: FIQ score (VAS 0-80) Cognitive disturbances: MFI mental fatigue (NRS 4-20) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 42 Russell 2008 (Continued) Global perceived improvement: PGIC (NRS 1-7) Tenderness: mean tender point threshold (kg/cm²) AEs: physical examination, EKGs, and laboratory analysis. AEs were assessed throughout the study based on spontaneous reporting by participants Notes Safety: the rates of participants in DLX and placebo groups experiencing at least 1 AE were not reported. 15 treatment-emergent AEs occurred in at least 1 of the DLX groups at a frequency greater than 5% and twice the rate of the placebo group. There were no statistically significant differences in SAEs between treatment groups. In the opinion of the investigator, the serious adverse event of suicidal ideation was possibly causally related to the study drug, but not to the protocol procedures Risk of bias Bias Authors’ judgement Support for judgement Random sequence generation (selection Low risk bias) Randomisation: computer-generated random sequence using an interactive response system Allocation concealment (selection bias) Low risk Central independent unit (details reported on request) Incomplete outcome data (attrition bias) All outcomes Low risk Imputation using last observation carried forward for efficacy data. ITT analysis Selective reporting (reporting bias) High risk Outcomes of sleep, anxiety and depression not reported; depression scores only reported in ClinicalStudyResults.org for 20/ 60 mg DLX Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar, details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 43 Vitton 2004 Methods Study setting: multicenter study with 12 outpatient research centres in USA Study design: parallel Duration therapy: 12 weeks Follow-up: not described Analysis: ITT; LOCF; ANOVA Participants Participants: 125 (97% female, 84% white, mean age 47 years) Inclusion criteria: 1990 ACR criteria; 18-70 years Exclusion criteria: severe psychiatric illness excluding depression; significant risk of suicide according to the investigator’s judgement; alcohol or other drug abuse; a history of significant cardiovascular, respiratory, endocrine, genitourinary, liver or kidney disease; autoimmune disease; systemic infection; cancer or current chemotherapy; significant sleep apnea; life expectancy < 1 year; active peptic ulcer or inflammatory bowel disease Interventions Active drugs MLN flexible dosage up to 200 mg/day, dose escalation within 3 weeks 46 participants: once a day 51 participants: twice a day Placebo (28 participants) The study used a flexible dosing titration design, where participants on active treatment initially received 25 mg of MLN in 1 dose of 25 mg or 2 doses of 12.5 mg a day during week 1. Participants who tolerated this dose were stepped up to a daily dose of 50 mg for week 2, 100 mg for week 3 and 200 mg for week 4, or matching placebo Rescue medication: hydrocodone up to 60 mg/day Outcomes Pain: PED 24-h recall pain score (VAS 0-100) Fatigue: FIQ VAS 0-10. Data provided on request. OC analysis Sleep: Jenkins Sleep Survey total score (NRS). Data provided on request.OC analysis Depression: FIQ VAS 0-10. Data provided on request. OC analysis Anxiety: FIQ VAS 0-10. Data provided on request. OC analysis Disability: FIQ VAS 0-10. Data provided on request. OC analysis Sexual function: Not assessed Quality of life: FIQ total score (VAS 0-80). Data provided on request. OC-Analysis Cognitive disturbances: not assessed Global perceived improvement: not assessed Tenderness: not assessed AEs: physical examination, EKGs, and laboratory analysis. AEs were assessed throughout the study based on spontaneous reporting by participants Notes Safety: no data on at least 1 AE in MLN and placebo group reported. No SAE or death reported. Headache, nausea, constipation and dizziness more frequent in MLN than in placebo Risk of bias Bias Authors’ judgement Random sequence generation (selection Low risk bias) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. Support for judgement Computer-generated random sequence (details provided on request) 44 Vitton 2004 (Continued) Allocation concealment (selection bias) Low risk Central independent unit (details provided on request) Incomplete outcome data (attrition bias) All outcomes High risk OC analysis Selective reporting (reporting bias) Low risk All outcomes reported or provided on request Blinding of participants and personnel Low risk (performance bias) All outcomes Double blind (number and appearance of placebo capsules similar, details reported on request) Blinding of outcome assessment (detection Low risk bias) All outcomes Independent data imputation and statistical analysis (details reported on request) Abbreviations ≥ = greater than or equal to < = less than ACR = American College of Rheumatology AE = adverse event BAI = Beck Anxiety Inventory BDI = Beck Depression Inventory BOCF = basis observation carried forward (statistical method) BP = blood pressure BPI = Brief Pain Inventory bpm = beats per minute CNS = central nervous system DLX = duloxetine DSM-IV = Diagnostic and Statistical Manual of Mental Disorders, 4th edition ECG = EKG = electrocardiogram EKG = ECG = electrocardiogram FIQ = Fibromyalgia Impact Questionnaire FM = fibromyalgia GAD = generalized anxiety disorder HDRS = Hamilton Depression Rating Scale IVRS = Interactive Voice Respone System ITT = intention-to-treat analysis LOCF = last observation carried forward (statistical method) MASQ = Multiple Ability Self-report Questionnaire MDD = major depressive disorder MDHAQ = Multi-Dimensional Health Assessment Questionnaire MFI = Multidimensional Fatigue Inventory MINI = Mini International Neuropsychiatric Interview MLN = milnacipran MMRM = mixed-effects model repeated measures MOS = Medical Outcomes Study Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 45 NRS = Numerical rating scale NSAID = non-steroidal anti-inflammatory drug OC = observed cases PED = patient electronic diary PGIC = Patient Global Impression of Change Inventory QT = The Q-T interval represents the time for both ventricular depolarization and repolarization to occur, and therefore roughly estimates the duration of an average ventricular action potential in the ECG. SAE = serious adverse effect SSR = Society of Skeletal Radiology VAS = visual analogue scale Characteristics of excluded studies [ordered by study ID] Study Reason for exclusion Branco 2011 1-year extension study, double-blind, randomized, not placebo controlled, of 3 doses of MLN (468 participants) Chappell 2009 8-week open-label period followed by a 52-week, double-blind, that were not placebo-controlled, randomized to 1 or 2 doses of DLX (350 participants) Dwight 1998 8-week open trial with venlaxafine in 15 FMS-participants Gendreau 2005 Double publication (see Vitton 2004) Goldenberg 2010 6-month extension study, double-blind, randomized, not placebo-controlled, of 2 doses of MLN (449 participants) Hsiao 2007 Case report of 1 patient with FM comorbid with premenstrual dysphoric disorder with a low dose of venlafaxine Mease 2010 6-month extension phases without placebo-control of 2 randomized controlled trials with DLX (492 participants) Saxe 2012 2-week randomized, placebo-controlled withdrawal design. Participants who had originally received MLN 100mg/day for 12 weeks were re-randomized to continue MLN (n=178) or switch directly to placebo (n=178); participants originally receiving placebo continued with placebo (n=359) Sayard 2003 12-week open trial with venlaxafine in 15 FMS-patients Wyeth 2008 Randomized placebo-controlled trial with 696 FMS-patients on 4 fixed oral doses of desvenlaxafine sustained release (DVS SR) (50 mg, 100 mg, 150 mg and 200 mg). Interim data analysis indicated that none of the 4 DVS SR treatment groups showed separation from placebo, and that there was a high placebo response rate. Consequently, the study was discontinued because of the failure of DVS to meet the predefined efficacy criteria (pain reduction, health-related quality of life (FIQ-total score) and PGIC score). Discontinuation rates because of side effects were twice as high in desvenlaxafine 100 mg,150 mg and 200 mg groups than in placebo. Details (Means, SDs, absolute numbers) not reported Abbreviations DLX = duloxetine Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 46 FM = fibromyalgia FMS = fibromyalgia syndrome MLN = milnacipran PGIC = Patient Global Impression of Change Inventory SD = standard deviation Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 47 DATA AND ANALYSES Comparison 1. SNRI versus placebo final treatment Outcome or subgroup title 1 Pain 1.1 Duloxetine 1.2 MIlncipran 2 30% pain reduction 2.1 Duloxetine 2.2 Milnacipran 3 50% pain reduction 3.1 Duloxetine 3.2 Milnacipran 4 Fatigue 4.1 Duloxetine 4.2 Milnacpran 5 Sleep problems 5.1 Duloxetine 5.2 Milnacipran 6 Depression 6.1 Duloxetine 6.2 Milnacipran 7 Anxiety 7.1 Duloxetine 7.2 Milnacipran 8 Disease-related quality of life 8.1 Duloxetine 8.2 Milnacipran 9 Disability 9.1 Duloxetine 9.2 Milnacipran 10 Cognitive disturbances 10.1 Duloxetine 10.2 Milnacipran 11 Participant-perceived improvement 11.1 Duloxetine 11.2 Milnacipran 12 Tenderness 12.1 Duloxetine 12.2 Milnacipran 13 Withdrawal due to adverse events 13.1 Duloxetine 13.2 Milnacipran 14 Serious adverse events 14.1 Duloxetine No. of studies No. of participants Statistical method Effect size 10 5 5 10 5 5 10 5 5 9 4 5 6 2 4 10 5 5 5 2 3 9 4 5 10 5 5 7 3 4 8 6012 1925 4087 6004 1894 4110 5994 1884 4110 5656 1568 4088 4081 996 3085 5658 1570 4088 2713 709 2004 5457 1380 4077 5995 1908 4087 5344 1360 3984 4551 Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) -0.23 [-0.29, -0.18] -0.32 [-0.41, -0.22] -0.20 [-0.26, -0.13] 1.36 [1.26, 1.46] 1.33 [1.18, 1.51] 1.38 [1.25, 1.51] 1.49 [1.35, 1.64] 1.59 [1.35, 1.88] 1.44 [1.28, 1.62] -0.14 [-0.19, -0.08] -0.12 [-0.23, -0.02] -0.14 [-0.21, -0.08] -0.07 [-0.16, 0.03] -0.24 [-0.37, -0.12] 0.02 [-0.05, 0.10] -0.15 [-0.21, -0.10] -0.26 [-0.37, -0.16] -0.11 [-0.17, -0.04] -0.03 [-0.15, 0.08] -0.05 [-0.22, 0.13] -0.04 [-0.23, 0.14] -0.20 [-0.25, -0.14] -0.27 [-0.39, -0.15] -0.18 [-0.24, -0.11] -0.22 [-0.28, -0.16] -0.33 [-0.43, -0.24] -0.16 [-0.23, -0.10] -0.15 [-0.21, -0.10] -0.27 [-0.38, -0.16] -0.11 [-0.18, -0.05] -0.27 [-0.33, -0.21] 5 3 4 4 0 10 1903 2648 1364 1364 0 6059 Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Std. Mean Difference (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) -0.29 [-0.39, -0.20] -0.25 [-0.33, -0.17] -0.23 [-0.35, -0.12] -0.23 [-0.35, -0.12] 0.0 [0.0, 0.0] 1.83 [1.53, 2.18] 5 5 9 4 1941 4118 5845 1734 Risk Ratio (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) Risk Ratio (IV, Random, 95% CI) 1.65 [1.30, 2.09] 2.00 [1.47, 2.73] 0.78 [0.55, 1.12] 0.63 [0.34, 1.16] Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 48 14.2 Milnacipran 5 4111 Risk Ratio (IV, Random, 95% CI) 0.88 [0.57, 1.37] Comparison 2. Active drug baseline and final treatment Outcome or subgroup title 1 Pain 2 Quality of life No. of studies No. of participants 10 9 6908 6699 Statistical method Mean Difference (IV, Random, 95% CI) Mean Difference (IV, Random, 95% CI) Effect size 2.04 [1.86, 2.21] 15.89 [14.45, 17.34] Comparison 3. Placebo baseline and final treatment Outcome or subgroup title 1 Pain 2 Quality of life No. of studies No. of participants 10 9 4716 4262 Statistical method Mean Difference (IV, Random, 95% CI) Mean Difference (IV, Random, 95% CI) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. Effect size 1.22 [1.11, 1.33] 11.41 [10.31, 12.51] 49 Analysis 1.1. Comparison 1 SNRI versus placebo final treatment, Outcome 1 Pain. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 1 Pain Study or subgroup Favours SNRIs Std. Mean Difference Favours Placebo Weight IV,Random,95% CI Std. Mean Difference N Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2004 100 -1.83 (2.4) 102 -0.94 (2.3) 3.6 % -0.38 [ -0.66, -0.10 ] Arnold 2005 116 -2.39 (2.4) 59 -1.16 (2.3) 2.8 % -0.52 [ -0.84, -0.20 ] Arnold 2005 114 -2.4 (2.4) 59 -1.16 (2.3) 2.8 % -0.52 [ -0.84, -0.20 ] Arnold 2010a 263 -2.3 (2.7) 267 -1.5 (2.8) 9.6 % -0.29 [ -0.46, -0.12 ] Chappell 2008 158 -1.62 (2.5) 167 -1.13 (2.5) 5.9 % -0.20 [ -0.41, 0.02 ] Russell 2008 79 -2 (2.5) 30 -1.43 (2.5) 1.6 % -0.23 [ -0.65, 0.20 ] Russell 2008 150 -1.98 (2.6) 58 -1.43 (2.5) 3.1 % -0.21 [ -0.52, 0.09 ] Russell 2008 147 -2.26 (2.5) 56 -1.43 (2.5) 2.9 % -0.33 [ -0.64, -0.02 ] 1 Duloxetine Subtotal (95% CI) 1127 32.3 % -0.32 [ -0.41, -0.22 ] 798 Heterogeneity: Tau2 = 0.0; Chi2 = 5.20, df = 7 (P = 0.64); I2 =0.0% Test for overall effect: Z = 6.62 (P < 0.00001) 2 MIlncipran Arnold 2010b 516 -17.7 (27.9) 509 -10.76 (29.3) 18.7 % -0.24 [ -0.37, -0.12 ] Branco 2010 430 -16.5 (24.5) 446 -11.97 (24.1) 16.0 % -0.19 [ -0.32, -0.05 ] Clauw 2008 396 -17.4 (21.9) 200 -13 (20) 9.7 % -0.21 [ -0.38, -0.04 ] Clauw 2008 399 -15.7 (22) 201 -13 (20) 9.8 % -0.13 [ -0.30, 0.04 ] Mease 2009a 223 53.2 (24.6) 75 56.2 (23.9) 4.1 % -0.12 [ -0.38, 0.14 ] Mease 2009a 441 52.2 (24.4) 148 56.2 (23.9) 8.1 % -0.16 [ -0.35, 0.02 ] Vitton 2004 42 -2.3 (2.7) 13 -0.8 (2.7) 0.7 % -0.55 [ -1.18, 0.08 ] Vitton 2004 37 -1.9 (2.9) 11 -0.8 (2.7) 0.6 % -0.38 [ -1.06, 0.30 ] Subtotal (95% CI) 2484 1603 67.7 % -0.20 [ -0.26, -0.13 ] 2401 100.0 % -0.23 [ -0.29, -0.18 ] Heterogeneity: Tau2 = 0.0; Chi2 = 3.12, df = 7 (P = 0.87); I2 =0.0% Test for overall effect: Z = 5.92 (P < 0.00001) Total (95% CI) 3611 Heterogeneity: Tau2 = 0.0; Chi2 = 12.63, df = 15 (P = 0.63); I2 =0.0% Test for overall effect: Z = 8.64 (P < 0.00001) Test for subgroup differences: Chi2 = 4.32, df = 1 (P = 0.04), I2 =77% -2 -1 0 Favours SNRIs Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 1 2 Favours Placebo 50 Analysis 1.2. Comparison 1 SNRI versus placebo final treatment, Outcome 2 30% pain reduction. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 2 30% pain reduction Study or subgroup SNRIs Placebo n/N n/N Risk Ratio Weight Arnold 2004 34/101 32/103 3.5 % 1.08 [ 0.73, 1.61 ] Arnold 2005 125/230 39/118 6.9 % 1.64 [ 1.24, 2.18 ] Arnold 2010a 119/249 85/248 11.8 % 1.39 [ 1.12, 1.73 ] Chappell 2008 60/158 55/167 6.4 % 1.15 [ 0.86, 1.55 ] 183/376 54/144 10.0 % 1.30 [ 1.03, 1.64 ] 1114 780 38.6 % 1.33 [ 1.18, 1.51 ] IV,Random,95% CI Risk Ratio IV,Random,95% CI 1 Duloxetine Russell 2008 Subtotal (95% CI) Total events: 521 (SNRIs), 265 (Placebo) Heterogeneity: Tau2 = 0.00; Chi2 = 4.31, df = 4 (P = 0.37); I2 =7% Test for overall effect: Z = 4.52 (P < 0.00001) 2 Milnacipran Arnold 2010b 230/516 156/509 20.9 % 1.45 [ 1.24, 1.71 ] Branco 2010 166/430 134/446 16.1 % 1.28 [ 1.07, 1.55 ] Clauw 2008 307/795 115/401 17.5 % 1.35 [ 1.13, 1.61 ] Mease 2009a 171/665 41/223 5.9 % 1.40 [ 1.03, 1.90 ] 36/97 6/28 1.0 % 1.73 [ 0.81, 3.69 ] 2503 1607 61.4 % 1.38 [ 1.25, 1.51 ] 100.0 % 1.36 [ 1.26, 1.46 ] Vitton 2004 Subtotal (95% CI) Total events: 910 (SNRIs), 452 (Placebo) Heterogeneity: Tau2 = 0.0; Chi2 = 1.40, df = 4 (P = 0.84); I2 =0.0% Test for overall effect: Z = 6.60 (P < 0.00001) Total (95% CI) 3617 2387 Total events: 1431 (SNRIs), 717 (Placebo) Heterogeneity: Tau2 = 0.0; Chi2 = 5.86, df = 9 (P = 0.75); I2 =0.0% Test for overall effect: Z = 8.12 (P < 0.00001) Test for subgroup differences: Chi2 = 0.15, df = 1 (P = 0.70), I2 =0.0% 0.01 0.1 Favours placebo 1 10 100 Favours SNRIs Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 51 Analysis 1.3. Comparison 1 SNRI versus placebo final treatment, Outcome 3 50% pain reduction. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 3 50% pain reduction Study or subgroup SNRIs Placebo n/N n/N Risk Ratio Weight Arnold 2004 29/104 17/103 3.3 % 1.69 [ 0.99, 2.88 ] Arnold 2005 95/230 27/118 6.9 % 1.81 [ 1.25, 2.60 ] Arnold 2010a 83/249 52/248 10.4 % 1.59 [ 1.18, 2.14 ] Chappell 2008 37/158 30/167 5.0 % 1.30 [ 0.85, 2.00 ] 126/368 30/139 7.7 % 1.59 [ 1.12, 2.24 ] 1109 775 33.2 % 1.59 [ 1.35, 1.88 ] IV,Random,95% CI Risk Ratio IV,Random,95% CI 1 Duloxetine Russell 2008 Subtotal (95% CI) Total events: 370 (SNRIs), 156 (Placebo) Heterogeneity: Tau2 = 0.0; Chi2 = 1.33, df = 4 (P = 0.86); I2 =0.0% Test for overall effect: Z = 5.47 (P < 0.00001) 2 Milnacipran Arnold 2010b 143/516 92/509 17.2 % 1.53 [ 1.22, 1.93 ] Branco 2010 112/430 88/446 15.3 % 1.32 [ 1.03, 1.69 ] Clauw 2008 224/795 75/401 17.1 % 1.51 [ 1.19, 1.90 ] Mease 2009a 241/665 58/223 15.6 % 1.39 [ 1.09, 1.78 ] 27/97 6/28 1.5 % 1.30 [ 0.60, 2.83 ] 2503 1607 66.8 % 1.44 [ 1.28, 1.62 ] 100.0 % 1.49 [ 1.35, 1.64 ] Vitton 2004 Subtotal (95% CI) Total events: 747 (SNRIs), 319 (Placebo) Heterogeneity: Tau2 = 0.0; Chi2 = 1.04, df = 4 (P = 0.90); I2 =0.0% Test for overall effect: Z = 6.04 (P < 0.00001) Total (95% CI) 3612 2382 Total events: 1117 (SNRIs), 475 (Placebo) Heterogeneity: Tau2 = 0.0; Chi2 = 3.36, df = 9 (P = 0.95); I2 =0.0% Test for overall effect: Z = 8.09 (P < 0.00001) Test for subgroup differences: Chi2 = 0.98, df = 1 (P = 0.32), I2 =0.0% 0.5 0.7 Favours placebo 1 1.5 2 Favours SNRIs Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 52 Analysis 1.4. Comparison 1 SNRI versus placebo final treatment, Outcome 4 Fatigue. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 4 Fatigue Study or subgroup SNRIs Std. Mean Difference Placebo Weight IV,Random,95% CI Std. Mean Difference N Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2004 101 -1.3 (2.9) 103 -0.88 (2.9) 3.9 % -0.14 [ -0.42, 0.13 ] Arnold 2010a 263 -2.2 (3.2) 267 -1.4 (3.3) 10.2 % -0.25 [ -0.42, -0.07 ] Chappell 2008 152 -0.33 (3.7) 162 -0.37 (3.7) 6.1 % 0.01 [ -0.21, 0.23 ] Russell 2008 147 -2.12 (4) 56 -1.69 (4.1) 3.1 % -0.11 [ -0.41, 0.20 ] Russell 2008 79 -1.79 (3.9) 30 -1.69 (4.1) 1.7 % -0.03 [ -0.45, 0.40 ] Russell 2008 150 -1.83 (4) 58 -1.69 (4.1) 3.2 % -0.03 [ -0.34, 0.27 ] 28.3 % -0.12 [ -0.23, -0.02 ] 1 Duloxetine Subtotal (95% CI) 892 676 Heterogeneity: Tau2 = 0.0; Chi2 = 3.95, df = 5 (P = 0.56); I2 =0.0% Test for overall effect: Z = 2.36 (P = 0.018) 2 Milnacpran Arnold 2010b 516 -4.31 (17.5) 509 -2.61 (17.4) 19.8 % -0.10 [ -0.22, 0.03 ] Branco 2010 430 -5.94 (15.1) 446 -3.53 (14.8) 16.9 % -0.16 [ -0.29, -0.03 ] Clauw 2008 399 -5.4 (11.9) 201 -3.8 (12) 10.3 % -0.13 [ -0.30, 0.04 ] Clauw 2008 396 -5.4 (11.9) 200 -3.8 (12) 10.3 % -0.13 [ -0.30, 0.04 ] Mease 2009a 224 -5 (12.8) 75 -3.4 (12.1) 4.4 % -0.13 [ -0.39, 0.14 ] Mease 2009a 441 -5.8 (14) 148 -3.4 (12.1) 8.6 % -0.18 [ -0.36, 0.01 ] Vitton 2004 42 -2 (2.6) 13 -0.7 (2.8) 0.8 % -0.48 [ -1.11, 0.14 ] Vitton 2004 37 -2.4 (2.6) 11 -0.7 (2.8) 0.6 % -0.63 [ -1.32, 0.05 ] 71.7 % -0.14 [ -0.21, -0.08 ] 100.0 % -0.14 [ -0.19, -0.08 ] Subtotal (95% CI) 2485 1603 Heterogeneity: Tau2 = 0.0; Chi2 = 3.85, df = 7 (P = 0.80); I2 =0.0% Test for overall effect: Z = 4.35 (P = 0.000014) Total (95% CI) 3377 2279 Heterogeneity: Tau2 = 0.0; Chi2 = 7.91, df = 13 (P = 0.85); I2 =0.0% Test for overall effect: Z = 4.94 (P < 0.00001) Test for subgroup differences: Chi2 = 0.10, df = 1 (P = 0.75), I2 =0.0% -2 -1 Favours SNRIs 0 1 2 Favours placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 53 Analysis 1.5. Comparison 1 SNRI versus placebo final treatment, Outcome 5 Sleep problems. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 5 Sleep problems Study or subgroup SNRIs Std. Mean Difference Placebo Weight IV,Random,95% CI Std. Mean Difference N Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2005 114 -2.69 (3.1) 118 -1.71 (2.7) 8.7 % -0.34 [ -0.60, -0.08 ] Arnold 2005 116 -2.67 (3.1) 118 -1.71 (3) 8.7 % -0.31 [ -0.57, -0.06 ] Arnold 2010a 263 -2 (2.9) 267 -1.5 (2.9) 13.6 % -0.17 [ -0.34, 0.00 ] 31.0 % -0.24 [ -0.37, -0.12 ] 1 Duloxetine Subtotal (95% CI) 493 503 Heterogeneity: Tau2 = 0.0; Chi2 = 1.45, df = 2 (P = 0.48); I2 =0.0% Test for overall effect: Z = 3.82 (P = 0.00013) 2 Milnacipran Branco 2010 430 -6.9 (20.1) 446 -7.4 (19.6) 16.5 % 0.03 [ -0.11, 0.16 ] Clauw 2008 396 -2.3 (23.1) 200 -3 (22) 13.7 % 0.03 [ -0.14, 0.20 ] Clauw 2008 399 -1.7 (21.9) 201 -3 (22) 13.7 % 0.06 [ -0.11, 0.23 ] Mease 2009a 224 -0.1 (20.2) 148 0.1 (20.6) 11.2 % -0.01 [ -0.22, 0.20 ] Mease 2009a 441 1.7 (22.2) 75 0.1 (20.6) 9.3 % 0.07 [ -0.17, 0.32 ] Vitton 2004 51 -1.3 (2.6) 15 -0.5 (2.9) 2.4 % -0.30 [ -0.87, 0.28 ] Vitton 2004 46 -1.3 (3.6) 13 -0.5 (2.9) 2.2 % -0.23 [ -0.84, 0.39 ] 69.0 % 0.02 [ -0.05, 0.10 ] 100.0 % -0.07 [ -0.16, 0.03 ] Subtotal (95% CI) 1987 1098 Heterogeneity: Tau2 = 0.0; Chi2 = 2.24, df = 6 (P = 0.90); I2 =0.0% Test for overall effect: Z = 0.61 (P = 0.54) Total (95% CI) 2480 1601 Heterogeneity: Tau2 = 0.01; Chi2 = 16.50, df = 9 (P = 0.06); I2 =45% Test for overall effect: Z = 1.44 (P = 0.15) Test for subgroup differences: Chi2 = 12.80, df = 1 (P = 0.00), I2 =92% -2 -1 Favours SNRIs 0 1 2 Favours placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 54 Analysis 1.6. Comparison 1 SNRI versus placebo final treatment, Outcome 6 Depression. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 6 Depression Study or subgroup SNRIs Std. Mean Difference Placebo Weight IV,Random,95% CI Std. Mean Difference N Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2004 88 -3.32 (8) 89 -1.02 (7.7) 3.4 % -0.29 [ -0.59, 0.00 ] Arnold 2005 110 -2.79 (4.7) 54 -2.24 (4.7) 2.8 % -0.12 [ -0.44, 0.21 ] Arnold 2005 111 -3.79 (4.6) 55 -2.24 (4.7) 2.8 % -0.33 [ -0.66, -0.01 ] Arnold 2010a 263 -5.5 (8.1) 267 -3.6 (8.2) 10.1 % -0.23 [ -0.40, -0.06 ] Chappell 2008 154 -3.42 (7.7) 164 -1.45 (7.8) 6.1 % -0.25 [ -0.47, -0.03 ] 76 -7.26 (7) 139 -3.91 (8.9) 3.7 % -0.40 [ -0.69, -0.12 ] 28.8 % -0.26 [ -0.37, -0.16 ] 1 Duloxetine Russell 2008 Subtotal (95% CI) 802 768 Heterogeneity: Tau2 = 0.0; Chi2 = 2.06, df = 5 (P = 0.84); I2 =0.0% Test for overall effect: Z = 5.12 (P < 0.00001) 2 Milnacipran Arnold 2010b 516 -2.12 (7) 509 -1.24 (7) 19.7 % -0.13 [ -0.25, 0.00 ] Branco 2010 430 -0.74 (7.5) 446 -0.29 (7.2) 16.8 % -0.06 [ -0.19, 0.07 ] Clauw 2008 399 -3 (8) 201 -2.3 (8) 10.3 % -0.09 [ -0.26, 0.08 ] Clauw 2008 396 -3.6 (8) 200 -2.3 (8) 10.2 % -0.16 [ -0.33, 0.01 ] Mease 2009a 224 -2.8 (7.8) 75 -2.3 (8.3) 4.3 % -0.06 [ -0.32, 0.20 ] Mease 2009a 441 -3 (8.9) 148 -2.3 (8.3) 8.5 % -0.08 [ -0.27, 0.11 ] Vitton 2004 37 -1.7 (2.9) 11 -0.6 (2.7) 0.6 % -0.38 [ -1.06, 0.30 ] Vitton 2004 42 -1.5 (2.9) 13 -0.6 (2.7) 0.8 % -0.31 [ -0.94, 0.31 ] 71.2 % -0.11 [ -0.17, -0.04 ] 100.0 % -0.15 [ -0.21, -0.10 ] Subtotal (95% CI) 2485 1603 Heterogeneity: Tau2 = 0.0; Chi2 = 2.22, df = 7 (P = 0.95); I2 =0.0% Test for overall effect: Z = 3.20 (P = 0.0014) Total (95% CI) 3287 2371 Heterogeneity: Tau2 = 0.0; Chi2 = 11.05, df = 13 (P = 0.61); I2 =0.0% Test for overall effect: Z = 5.45 (P < 0.00001) Test for subgroup differences: Chi2 = 6.77, df = 1 (P = 0.01), I2 =85% -4 -2 Favours SNRIs 0 2 4 Favours placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 55 Analysis 1.7. Comparison 1 SNRI versus placebo final treatment, Outcome 7 Anxiety. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 7 Anxiety Study or subgroup SNRIs Std. Mean Difference Placebo Weight IV,Random,95% CI Std. Mean Difference N Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2004 93 -2.6 (6.7) 86 -1.39 (6.4) 12.0 % -0.18 [ -0.48, 0.11 ] Arnold 2010a 263 -3.1 (8.1) 267 -3.2 (8.2) 23.2 % 0.01 [ -0.16, 0.18 ] 35.2 % -0.05 [ -0.22, 0.13 ] 1 Duloxetine Subtotal (95% CI) 356 353 Heterogeneity: Tau2 = 0.00; Chi2 = 1.28, df = 1 (P = 0.26); I2 =22% Test for overall effect: Z = 0.53 (P = 0.60) 2 Milnacipran Arnold 2010b 516 -0.7 (9) 509 -1.7 (9) 30.1 % 0.11 [ -0.01, 0.23 ] Branco 2010 430 -0.96 (11.2) 446 0.01 (11) 28.5 % -0.09 [ -0.22, 0.05 ] Vitton 2004 42 -1.6 (3.1) 13 -0.5 (3.4) 3.4 % -0.34 [ -0.97, 0.28 ] Vitton 2004 37 -1.8 (2.9) 11 -0.5 (3.4) 2.9 % -0.42 [ -1.10, 0.25 ] 64.8 % -0.04 [ -0.23, 0.14 ] 100.0 % -0.03 [ -0.15, 0.08 ] Subtotal (95% CI) 1025 979 Heterogeneity: Tau2 = 0.02; Chi2 = 7.46, df = 3 (P = 0.06); I2 =60% Test for overall effect: Z = 0.45 (P = 0.65) Total (95% CI) 1381 1332 Heterogeneity: Tau2 = 0.01; Chi2 = 8.96, df = 5 (P = 0.11); I2 =44% Test for overall effect: Z = 0.57 (P = 0.57) Test for subgroup differences: Chi2 = 0.00, df = 1 (P = 0.97), I2 =0.0% -4 -2 Favours SNRIs 0 2 4 Favours placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 56 Analysis 1.8. Comparison 1 SNRI versus placebo final treatment, Outcome 8 Disease-related quality of life. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 8 Disease-related quality of life Study or subgroup Favours SNRIs Std. Mean Difference Favours Placebo N Weight IV,Random,95% CI Std. Mean Difference Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2004 101 -13.46 (18.3) 102 -7.93 (17.5) 4.1 % -0.31 [ -0.58, -0.03 ] Arnold 2005 114 -16.72 (16.6) 58 -8.35 (16.4) 3.1 % -0.50 [ -0.82, -0.18 ] Arnold 2005 112 -16.81 (16.6) 57 -8.35 (16.4) 3.0 % -0.51 [ -0.83, -0.19 ] Chappell 2008 153 -7.96 (17) 163 -5.81 (16.5) 6.5 % -0.13 [ -0.35, 0.09 ] Russell 2008 147 -13.86 (17) 56 -10.42 (17.5) 3.3 % -0.20 [ -0.51, 0.11 ] Russell 2008 150 -12.28 (17.6) 58 -10.42 (17.5) 3.4 % -0.11 [ -0.41, 0.20 ] Russell 2008 79 -14.77 (16.7) 30 -10.42 (17.5) 1.8 % -0.26 [ -0.68, 0.17 ] 1 Duloxetine Subtotal (95% CI) 856 524 25.2 % -0.27 [ -0.39, -0.15 ] Heterogeneity: Tau2 = 0.00; Chi2 = 7.13, df = 6 (P = 0.31); I2 =16% Test for overall effect: Z = 4.28 (P = 0.000019) 2 Milnacipran Arnold 2010b 516 -12.34 (24.8) 509 -7.12 (24.4) 21.0 % -0.21 [ -0.33, -0.09 ] Branco 2010 430 -14.18 (21.4) 446 -11.18 (20.9) 18.0 % -0.14 [ -0.27, -0.01 ] Clauw 2008 396 -15.4 (19.9) 200 -12 (20) 10.9 % -0.17 [ -0.34, 0.00 ] Clauw 2008 399 -16.6 (20) 201 -12 (20) 10.9 % -0.23 [ -0.40, -0.06 ] Mease 2009a 441 -16.7 (21.6) 75 -15 (20.5) 5.3 % -0.08 [ -0.32, 0.17 ] Mease 2009a 224 -17.7 (22.5) 148 -15 (20.5) 7.3 % -0.12 [ -0.33, 0.08 ] Vitton 2004 37 -10.5 (14.5) 11 -5.4 (13.4) 0.7 % -0.35 [ -1.03, 0.33 ] Vitton 2004 33 -10.3 (14.1) 11 -5.4 (13.4) 0.7 % -0.35 [ -1.03, 0.34 ] Subtotal (95% CI) 2476 1601 74.8 % -0.18 [ -0.24, -0.11 ] 2125 100.0 % -0.20 [ -0.25, -0.14 ] Heterogeneity: Tau2 = 0.0; Chi2 = 2.31, df = 7 (P = 0.94); I2 =0.0% Test for overall effect: Z = 5.31 (P < 0.00001) Total (95% CI) 3332 Heterogeneity: Tau2 = 0.0; Chi2 = 11.22, df = 14 (P = 0.67); I2 =0.0% Test for overall effect: Z = 6.91 (P < 0.00001) Test for subgroup differences: Chi2 = 1.72, df = 1 (P = 0.19), I2 =42% -2 -1 0 Favours SNRIs Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 1 2 Favours Placebo 57 Analysis 1.9. Comparison 1 SNRI versus placebo final treatment, Outcome 9 Disability. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 9 Disability Study or subgroup SNRIs Std. Mean Difference Placebo Weight IV,Random,95% CI Std. Mean Difference N Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2004 101 -2.01 (2.6) 102 -0.95 (2.7) 3.9 % -0.40 [ -0.68, -0.12 ] Arnold 2005 116 -2.57 (2.4) 59 -1.43 (2.3) 3.0 % -0.48 [ -0.80, -0.16 ] Arnold 2005 114 -2.58 (2.3) 59 -1.43 (2.3) 3.0 % -0.50 [ -0.82, -0.18 ] Arnold 2010a 263 -2.6 (3.2) 267 -1.7 (3.3) 9.7 % -0.28 [ -0.45, -0.11 ] Chappell 2008 158 -1.69 (2.5) 167 -1.03 (2.5) 6.1 % -0.26 [ -0.48, -0.04 ] Russell 2008 77 -2.34 (2.4) 29 -1.37 (2.4) 1.6 % -0.40 [ -0.83, 0.03 ] Russell 2008 144 -1.98 (2.6) 56 -1.37 (2.4) 3.1 % -0.24 [ -0.55, 0.07 ] Russell 2008 142 -2.27 (2.5) 54 -1.37 (2.4) 3.0 % -0.36 [ -0.68, -0.05 ] 33.5 % -0.33 [ -0.43, -0.24 ] 1 Duloxetine Subtotal (95% CI) 1115 793 Heterogeneity: Tau2 = 0.0; Chi2 = 3.35, df = 7 (P = 0.85); I2 =0.0% Test for overall effect: Z = 7.00 (P < 0.00001) 2 Milnacipran Arnold 2010b 516 -1.49 (3.2) 509 -0.91 (2.9) 17.5 % -0.19 [ -0.31, -0.07 ] Branco 2010 430 -1.26 (2.3) 446 -0.93 (2.3) 15.3 % -0.14 [ -0.28, -0.01 ] Clauw 2008 396 -2.6 (6) 200 -1.5 (6) 9.8 % -0.18 [ -0.35, -0.01 ] Clauw 2008 399 -2.4 (6) 201 -1.5 (6) 9.8 % -0.15 [ -0.32, 0.02 ] Mease 2009a 223 -2.99 (8.46) 74 -2.43 (7.74) 4.3 % -0.07 [ -0.33, 0.20 ] Mease 2009a 441 -3.34 (8.42) 148 -2.43 (7.74) 8.3 % -0.11 [ -0.30, 0.08 ] Vitton 2004 43 -3.2 (6.2) 13 0.1 (7.5) 0.8 % -0.50 [ -1.13, 0.13 ] Vitton 2004 37 -3.5 (5.9) 11 0.1 (7.5) 0.7 % -0.56 [ -1.25, 0.12 ] 66.5 % -0.16 [ -0.23, -0.10 ] 100.0 % -0.22 [ -0.28, -0.16 ] Subtotal (95% CI) 2485 1602 Heterogeneity: Tau2 = 0.0; Chi2 = 3.59, df = 7 (P = 0.83); I2 =0.0% Test for overall effect: Z = 4.92 (P < 0.00001) Total (95% CI) 3600 2395 Heterogeneity: Tau2 = 0.00; Chi2 = 15.82, df = 15 (P = 0.39); I2 =5% Test for overall effect: Z = 7.76 (P < 0.00001) Test for subgroup differences: Chi2 = 8.89, df = 1 (P = 0.00), I2 =89% -4 -2 Favours SNRIs 0 2 4 Favours placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 58 Analysis 1.10. Comparison 1 SNRI versus placebo final treatment, Outcome 10 Cognitive disturbances. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 10 Cognitive disturbances Study or subgroup SNRIs Std. Mean Difference Placebo Weight IV,Random,95% CI Std. Mean Difference N Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2010a 263 -2 (3.2) 263 -1.1 (3.3) 10.7 % -0.28 [ -0.45, -0.10 ] Chappell 2008 153 -0.99 (4.1) 161 -0.03 (3.9) 6.4 % -0.24 [ -0.46, -0.02 ] Russell 2008 79 -2.37 (3.9) 30 -1.14 (4.1) 1.8 % -0.31 [ -0.73, 0.11 ] Russell 2008 147 -2.37 (4) 56 -1.14 (4.1) 3.3 % -0.30 [ -0.61, 0.00 ] Russell 2008 150 -2.29 (4.2) 58 -1.14 (4.1) 3.4 % -0.27 [ -0.58, 0.03 ] 25.6 % -0.27 [ -0.38, -0.16 ] 1 Duloxetine Subtotal (95% CI) 792 568 Heterogeneity: Tau2 = 0.0; Chi2 = 0.16, df = 4 (P = 1.00); I2 =0.0% Test for overall effect: Z = 4.81 (P < 0.00001) 2 Milnacipran Arnold 2010b 516 -3.89 (17.5) 509 -2.36 (17.4) 21.0 % -0.09 [ -0.21, 0.03 ] Branco 2010 430 -5.88 (20.8) 446 -3.53 (20.3) 17.9 % -0.11 [ -0.25, 0.02 ] Clauw 2008 399 -3.3 (12) 201 -2.5 (12) 11.0 % -0.07 [ -0.24, 0.10 ] Clauw 2008 395 -3.8 (11.9) 200 -2.5 (12) 10.9 % -0.11 [ -0.28, 0.06 ] Mease 2009a 224 -1.56 (11.5) 75 0.16 (12.93) 4.6 % -0.14 [ -0.41, 0.12 ] Mease 2009a 441 -2.68 (13.5) 148 0.16 (12.93) 9.1 % -0.21 [ -0.40, -0.03 ] 74.4 % -0.11 [ -0.18, -0.05 ] 100.0 % -0.15 [ -0.21, -0.10 ] Subtotal (95% CI) 2405 1579 Heterogeneity: Tau2 = 0.0; Chi2 = 1.60, df = 5 (P = 0.90); I2 =0.0% Test for overall effect: Z = 3.40 (P = 0.00069) Total (95% CI) 3197 2147 Heterogeneity: Tau2 = 0.0; Chi2 = 7.70, df = 10 (P = 0.66); I2 =0.0% Test for overall effect: Z = 5.36 (P < 0.00001) Test for subgroup differences: Chi2 = 5.94, df = 1 (P = 0.01), I2 =83% -4 -2 Favours SNRIs 0 2 4 Favours placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 59 Analysis 1.11. Comparison 1 SNRI versus placebo final treatment, Outcome 11 Participant-perceived improvement. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 11 Participant-perceived improvement Study or subgroup SNRIs Std. Mean Difference Placebo Weight IV,Random,95% CI Std. Mean Difference N Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2004 95 3.02 (1.7) 99 3.53 (1.7) 4.6 % -0.30 [ -0.58, -0.02 ] Arnold 2005 111 3.06 (1.8) 55 3.71 (1.6) 3.5 % -0.37 [ -0.70, -0.05 ] Arnold 2005 114 3.11 (1.9) 56 3.71 (1.6) 3.6 % -0.33 [ -0.65, -0.01 ] Arnold 2010a 263 2.8 (1.8) 267 3.4 (1.6) 12.5 % -0.35 [ -0.52, -0.18 ] Chappell 2008 158 3.4 (1.6) 165 3.7 (1.5) 7.7 % -0.19 [ -0.41, 0.03 ] Russell 2008 150 3.08 (1.6) 58 3.37 (1.6) 4.0 % -0.18 [ -0.48, 0.12 ] Russell 2008 147 2.93 (1.6) 56 3.37 (1.6) 3.9 % -0.27 [ -0.58, 0.03 ] Russell 2008 79 2.79 (1.5) 30 3.37 (1.6) 2.1 % -0.38 [ -0.80, 0.05 ] 41.8 % -0.29 [ -0.39, -0.20 ] 1 Duloxetine Subtotal (95% CI) 1117 786 Heterogeneity: Tau2 = 0.0; Chi2 = 2.23, df = 7 (P = 0.95); I2 =0.0% Test for overall effect: Z = 6.14 (P < 0.00001) 2 Milnacipran Arnold 2010b 516 3.06 (1.8) 509 3.53 (1.8) 24.4 % -0.26 [ -0.38, -0.14 ] Clauw 2008 393 3.1 (2) 199 3.5 (2) 12.6 % -0.20 [ -0.37, -0.03 ] Clauw 2008 386 3 (2) 198 3.5 (2) 12.5 % -0.25 [ -0.42, -0.08 ] Mease 2009a 115 2.78 (1.8) 43 3.07 (1.6) 3.0 % -0.17 [ -0.52, 0.19 ] Mease 2009a 204 2.52 (1.7) 85 3.07 (1.6) 5.7 % -0.33 [ -0.58, -0.07 ] 58.2 % -0.25 [ -0.33, -0.17 ] 100.0 % -0.27 [ -0.33, -0.21 ] Subtotal (95% CI) 1614 1034 Heterogeneity: Tau2 = 0.0; Chi2 = 0.94, df = 4 (P = 0.92); I2 =0.0% Test for overall effect: Z = 6.08 (P < 0.00001) Total (95% CI) 2731 1820 Heterogeneity: Tau2 = 0.0; Chi2 = 3.74, df = 12 (P = 0.99); I2 =0.0% Test for overall effect: Z = 8.61 (P < 0.00001) Test for subgroup differences: Chi2 = 0.57, df = 1 (P = 0.45), I2 =0.0% -4 -2 Favours SNRIs 0 2 4 Favours Placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 60 Analysis 1.12. Comparison 1 SNRI versus placebo final treatment, Outcome 12 Tenderness. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 12 Tenderness Study or subgroup SNRIs Std. Mean Difference Placebo Weight IV,Random,95% CI Std. Mean Difference N Mean(SD) N Mean(SD) IV,Random,95% CI Arnold 2004 104 -0.29 (0.7) 103 0.04 (0.7) 16.6 % -0.47 [ -0.75, -0.19 ] Arnold 2005 111 -0.22 (0.8) 55 -0.06 (0.8) 12.1 % -0.20 [ -0.52, 0.12 ] Arnold 2005 110 -0.39 (0.8) 54 -0.06 (0.8) 11.7 % -0.41 [ -0.74, -0.08 ] Chappell 2008 148 -0.4 (1.1) 159 -0.2 (1) 25.2 % -0.19 [ -0.41, 0.03 ] Russell 2008 150 -0.52 (1.1) 58 -0.42 (1.1) 13.8 % -0.09 [ -0.39, 0.21 ] Russell 2008 79 -0.54 (1.1) 30 -0.42 (1.1) 7.2 % -0.11 [ -0.53, 0.31 ] Russell 2008 147 -0.54 (1.1) 56 -0.42 (1.1) 13.4 % -0.11 [ -0.42, 0.20 ] 100.0 % -0.23 [ -0.35, -0.12 ] 0 0.0 % 0.0 [ 0.0, 0.0 ] 515 100.0 % -0.23 [ -0.35, -0.12 ] 1 Duloxetine Subtotal (95% CI) 849 515 Heterogeneity: Tau2 = 0.0; Chi2 = 5.93, df = 6 (P = 0.43); I2 =0.0% Test for overall effect: Z = 4.06 (P = 0.000050) 2 Milnacipran Subtotal (95% CI) 0 Heterogeneity: not applicable Test for overall effect: not applicable Total (95% CI) 849 Heterogeneity: Tau2 = 0.0; Chi2 = 5.93, df = 6 (P = 0.43); I2 =0.0% Test for overall effect: Z = 4.06 (P = 0.000050) Test for subgroup differences: Not applicable -100 -50 SNRIs 0 50 100 Placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 61 Analysis 1.13. Comparison 1 SNRI versus placebo final treatment, Outcome 13 Withdrawal due to adverse events. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 13 Withdrawal due to adverse events Study or subgroup SNRIs Placebo n/N n/N Risk Ratio Weight Arnold 2004 18/104 11/103 5.3 % 1.62 [ 0.81, 3.26 ] Arnold 2005 52/234 14/120 7.8 % 1.90 [ 1.10, 3.29 ] Arnold 2010a 41/263 24/267 9.6 % 1.73 [ 1.08, 2.79 ] Chappell 2008 30/162 19/168 8.1 % 1.64 [ 0.96, 2.79 ] Russell 2008 62/376 17/144 8.9 % 1.40 [ 0.85, 2.31 ] 1139 802 39.7 % 1.65 [ 1.30, 2.09 ] IV,Random,95% CI Risk Ratio IV,Random,95% CI 1 Duloxetine Subtotal (95% CI) Total events: 203 (SNRIs), 85 (Placebo) Heterogeneity: Tau2 = 0.0; Chi2 = 0.73, df = 4 (P = 0.95); I2 =0.0% Test for overall effect: Z = 4.07 (P = 0.000046) 2 Milnacipran Arnold 2010b 92/516 71/509 17.6 % 1.28 [ 0.96, 1.70 ] Branco 2010 96/435 44/449 15.1 % 2.25 [ 1.62, 3.14 ] Clauw 2008 172/795 38/401 15.1 % 2.28 [ 1.64, 3.18 ] Mease 2009a 163/665 23/223 11.7 % 2.38 [ 1.58, 3.58 ] 17/97 1/28 0.8 % 4.91 [ 0.68, 35.28 ] 2508 1610 60.3 % 2.00 [ 1.47, 2.73 ] 100.0 % 1.83 [ 1.53, 2.18 ] Vitton 2004 Subtotal (95% CI) Total events: 540 (SNRIs), 177 (Placebo) Heterogeneity: Tau2 = 0.07; Chi2 = 11.70, df = 4 (P = 0.02); I2 =66% Test for overall effect: Z = 4.37 (P = 0.000013) Total (95% CI) 3647 2412 Total events: 743 (SNRIs), 262 (Placebo) Heterogeneity: Tau2 = 0.02; Chi2 = 13.32, df = 9 (P = 0.15); I2 =32% Test for overall effect: Z = 6.75 (P < 0.00001) Test for subgroup differences: Chi2 = 0.94, df = 1 (P = 0.33), I2 =0.0% 0.05 0.2 Favours SNRIs 1 5 20 Favours Placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 62 Analysis 1.14. Comparison 1 SNRI versus placebo final treatment, Outcome 14 Serious adverse events. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 1 SNRI versus placebo final treatment Outcome: 14 Serious adverse events Study or subgroup SNRIs Placebo n/N n/N Risk Ratio Weight Arnold 2005 2/234 0/120 1.4 % 2.57 [ 0.12, 53.20 ] Arnold 2010a 1/267 6/263 2.9 % 0.16 [ 0.02, 1.35 ] Chappell 2008 4/162 4/168 6.8 % 1.04 [ 0.26, 4.08 ] 17/376 11/144 23.7 % 0.59 [ 0.28, 1.23 ] 1039 695 34.7 % 0.63 [ 0.34, 1.16 ] IV,Random,95% CI Risk Ratio IV,Random,95% CI 1 Duloxetine Russell 2008 Subtotal (95% CI) Total events: 24 (SNRIs), 21 (Placebo) Heterogeneity: Tau2 = 0.0; Chi2 = 2.93, df = 3 (P = 0.40); I2 =0.0% Test for overall effect: Z = 1.49 (P = 0.14) 2 Milnacipran Arnold 2010b 8/516 6/509 11.5 % 1.32 [ 0.46, 3.76 ] Branco 2010 14/431 16/446 25.6 % 0.91 [ 0.45, 1.83 ] Clauw 2008 9/795 6/401 12.1 % 0.76 [ 0.27, 2.11 ] Mease 2009a 14/665 6/223 14.3 % 0.78 [ 0.30, 2.01 ] 1/97 1/28 1.7 % 0.29 [ 0.02, 4.47 ] 2504 1607 65.3 % 0.88 [ 0.57, 1.37 ] 100.0 % 0.78 [ 0.55, 1.12 ] Vitton 2004 Subtotal (95% CI) Total events: 46 (SNRIs), 35 (Placebo) Heterogeneity: Tau2 = 0.0; Chi2 = 1.35, df = 4 (P = 0.85); I2 =0.0% Test for overall effect: Z = 0.57 (P = 0.57) Total (95% CI) 3543 2302 Total events: 70 (SNRIs), 56 (Placebo) Heterogeneity: Tau2 = 0.0; Chi2 = 5.03, df = 8 (P = 0.75); I2 =0.0% Test for overall effect: Z = 1.34 (P = 0.18) Test for subgroup differences: Chi2 = 0.76, df = 1 (P = 0.38), I2 =0.0% 0.5 0.7 Favours SNRIs 1 1.5 2 Favours Placebo Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 63 Analysis 2.1. Comparison 2 Active drug baseline and final treatment, Outcome 1 Pain. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 2 Active drug baseline and final treatment Outcome: 1 Pain Study or subgroup Baseline Mean Difference Final treatment Weight N Mean(SD) N Mean(SD) Arnold 2004 103 6.1 (1.7) 103 4.3 (2.4) 5.2 % 1.80 [ 1.23, 2.37 ] Arnold 2005 118 6.4 (1.4) 116 4 (2.4) 5.9 % 2.40 [ 1.90, 2.90 ] Arnold 2005 116 6.4 (1.6) 114 4 (2.4) 5.6 % 2.40 [ 1.87, 2.93 ] Arnold 2010a 263 6.5 (1.6) 263 4.2 (2.7) 7.5 % 2.30 [ 1.92, 2.68 ] Arnold 2010b 516 6.3 (1.3) 516 4.5 (2.8) 9.1 % 1.80 [ 1.53, 2.07 ] Branco 2010 430 6.6 (1.3) 430 4.9 (2.5) 9.1 % 1.70 [ 1.43, 1.97 ] Chappell 2008 162 6.6 (1.5) 158 5 (2.5) 6.5 % 1.60 [ 1.15, 2.05 ] Clauw 2008 399 6.5 (1.4) 399 4.9 (2) 9.5 % 1.60 [ 1.36, 1.84 ] Clauw 2008 396 6.5 (1.4) 396 4.7 (2.2) 9.3 % 1.80 [ 1.54, 2.06 ] Mease 2009a 224 6.6 (1.2) 115 4.3 (3.3) 4.7 % 2.30 [ 1.68, 2.92 ] Mease 2009a 441 6.8 (1.2) 204 4.3 (3.7) 5.7 % 2.50 [ 1.98, 3.02 ] Russell 2008 150 6.5 (1.4) 150 4 (2.6) 6.3 % 2.50 [ 2.03, 2.97 ] Russell 2008 79 6.8 (1.6) 79 4.6 (2.5) 4.4 % 2.20 [ 1.55, 2.85 ] Russell 2008 147 6.4 (1.6) 147 4.1 (2.5) 6.2 % 2.30 [ 1.82, 2.78 ] Vitton 2004 49 6.9 (1.9) 42 4.6 (2.7) 2.5 % 2.30 [ 1.33, 3.27 ] Vitton 2004 46 7 (1.7) 37 5.1 (2.9) 2.2 % 1.90 [ 0.84, 2.96 ] 100.0 % 2.04 [ 1.86, 2.21 ] Total (95% CI) 3639 IV,Random,95% CI Mean Difference IV,Random,95% CI 3269 Heterogeneity: Tau2 = 0.07; Chi2 = 39.37, df = 15 (P = 0.00056); I2 =62% Test for overall effect: Z = 22.77 (P < 0.00001) Test for subgroup differences: Not applicable -2 -1 0 Baseline Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 1 2 Final treatment 64 Analysis 2.2. Comparison 2 Active drug baseline and final treatment, Outcome 2 Quality of life. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 2 Active drug baseline and final treatment Outcome: 2 Quality of life Study or subgroup Baseline Mean Difference Final treatment Weight N Mean(SD) N Mean(SD) Arnold 2004 104 60.9 (18.8) 102 44 (22.9) 4.3 % 16.90 [ 11.17, 22.63 ] Arnold 2005 118 64.3 (15.3) 114 43.4 (23.6) 5.0 % 20.90 [ 15.76, 26.04 ] Arnold 2005 116 65.6 (15.9) 112 44.6 (20.8) 5.4 % 21.00 [ 16.18, 25.82 ] Arnold 2010b 516 56.7 (12.7) 516 44.4 (24.8) 9.7 % 12.30 [ 9.90, 14.70 ] Branco 2010 430 56.7 (11.9) 430 42.5 (21.3) 9.9 % 14.20 [ 11.89, 16.51 ] Chappell 2008 162 62 (14.1) 153 52 (21.3) 6.5 % 10.00 [ 5.99, 14.01 ] Clauw 2008 396 64.5 (13.8) 396 47.1 (22) 9.4 % 17.40 [ 14.84, 19.96 ] Clauw 2008 399 64.6 (13.5) 399 48.8 (22) 9.4 % 15.80 [ 13.27, 18.33 ] Mease 2009a 441 64.3 (14.4) 441 47.6 (22.6) 9.5 % 16.70 [ 14.20, 19.20 ] Mease 2009a 223 65.1 (13.7) 223 47.4 (22.2) 7.6 % 17.70 [ 14.28, 21.12 ] Russell 2008 79 67.5 (14.3) 79 49 (20.9) 4.4 % 18.50 [ 12.92, 24.08 ] Russell 2008 150 64.6 (14.8) 150 49.3 (22) 6.2 % 15.30 [ 11.06, 19.54 ] Russell 2008 147 64.6 (17.6) 147 47.3 (17.3) 6.6 % 17.30 [ 13.31, 21.29 ] Vitton 2004 42 49.9 (13) 33 37 (17.6) 3.1 % 12.90 [ 5.72, 20.08 ] Vitton 2004 44 50.6 (14.3) 37 37.5 (18.1) 3.1 % 13.10 [ 5.90, 20.30 ] 100.0 % 15.89 [ 14.45, 17.34 ] Total (95% CI) 3367 IV,Random,95% CI Mean Difference IV,Random,95% CI 3332 Heterogeneity: Tau2 = 4.10; Chi2 = 32.12, df = 14 (P = 0.004); I2 =56% Test for overall effect: Z = 21.57 (P < 0.00001) Test for subgroup differences: Not applicable -20 -10 Baseline 0 10 20 Final treatment Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 65 Analysis 3.1. Comparison 3 Placebo baseline and final treatment, Outcome 1 Pain. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 3 Placebo baseline and final treatment Outcome: 1 Pain Study or subgroup Baseline Mean Difference Final treatment Weight N Mean(SD) N Mean(SD) Arnold 2004 104 6.1 (1.8) 102 5.2 (2.3) 4.0 % 0.90 [ 0.34, 1.46 ] Arnold 2005 120 6.5 (1.5) 118 5.3 (2.3) 5.3 % 1.20 [ 0.71, 1.69 ] Arnold 2010a 267 6.5 (1.6) 267 5 (2.8) 8.6 % 1.50 [ 1.11, 1.89 ] Arnold 2010b 509 6.4 (1.3) 509 5.3 (2.9) 16.9 % 1.10 [ 0.82, 1.38 ] Branco 2010 446 6.6 (1.3) 446 5.3 (2.4) 20.0 % 1.30 [ 1.05, 1.55 ] Chappell 2008 168 6.4 (1.5) 167 5.3 (2.5) 6.6 % 1.10 [ 0.66, 1.54 ] Clauw 2008 401 6.6 (1.3) 401 5.3 (2) 23.6 % 1.30 [ 1.07, 1.53 ] Mease 2009a 223 6.8 (1.2) 128 5.9 (2.1) 8.2 % 0.90 [ 0.50, 1.30 ] Russell 2008 144 6.6 (1.7) 144 5.2 (2.2) 6.2 % 1.40 [ 0.95, 1.85 ] Vitton 2004 28 6.7 (2.2) 24 5.9 (2.7) 0.7 % 0.80 [ -0.55, 2.15 ] 100.0 % 1.22 [ 1.11, 1.33 ] Total (95% CI) 2410 IV,Random,95% CI Mean Difference IV,Random,95% CI 2306 Heterogeneity: Tau2 = 0.0; Chi2 = 8.57, df = 9 (P = 0.48); I2 =0.0% Test for overall effect: Z = 21.08 (P < 0.00001) Test for subgroup differences: Not applicable -4 -2 0 Baseline Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 2 4 Final treatment 66 Analysis 3.2. Comparison 3 Placebo baseline and final treatment, Outcome 2 Quality of life. Review: Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome Comparison: 3 Placebo baseline and final treatment Outcome: 2 Quality of life Study or subgroup Baseline Mean Difference Final treatment Mean Difference Weight N Mean(SD) N Mean(SD) Arnold 2004 101 62.8 (16.6) 101 52.9 (21.9) 4.2 % 9.90 [ 4.54, 15.26 ] Arnold 2005 120 66.4 (15.5) 115 55.9 (20.5) 5.5 % 10.50 [ 5.84, 15.16 ] Arnold 2010b 509 57.9 (12.7) 509 45.6 (24.8) 19.8 % 12.30 [ 9.88, 14.72 ] Branco 2010 446 57 (11.8) 446 45.8 (20.9) 23.2 % 11.20 [ 8.97, 13.43 ] Chappell 2008 168 63.3 (15.6) 163 56 (20.6) 7.7 % 7.30 [ 3.35, 11.25 ] Clauw 2008 401 62.5 (14.1) 401 50.5 (14.1) 29.7 % 12.00 [ 10.05, 13.95 ] Mease 2009a 223 64.7 (13.4) 223 48.8 (59.8) 1.9 % 15.90 [ 7.86, 23.94 ] Russell 2008 144 66.3 (14) 144 53.3 (21.9) 6.6 % 13.00 [ 8.75, 17.25 ] Vitton 2004 26 51.6 (16) 22 44.8 (16.8) 1.4 % 6.80 [ -2.53, 16.13 ] 100.0 % 11.41 [ 10.31, 12.51 ] Total (95% CI) 2138 IV,Random,95% CI IV,Random,95% CI 2124 Heterogeneity: Tau2 = 0.07; Chi2 = 8.20, df = 8 (P = 0.41); I2 =2% Test for overall effect: Z = 20.27 (P < 0.00001) Test for subgroup differences: Not applicable -20 -10 Baseline 0 10 20 Final treatment ADDITIONAL TABLES Table 1. Subgroup analysis: Efficacy and safety of SNRIs in studies with and without European participants Outcome title Number of participants Effect size Test for SMD (95% CI) or overall RR (95% CI) effect P value Heterogeneity I²(%); Pain Test of interaction: effect estimate and P value Z = 1.0; P = 0.32 Without European 4837 participants -0.25 (-0.31 to -0. < 0.001 19) 0 With European par- 1201 ticipants -0.19 (-0-30 to -0. < 0.001 08) 0 Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 67 Table 1. Subgroup analysis: Efficacy and safety of SNRIs in studies with and without European participants Fatigue (Continued) Z = 0.57; P = 0.57 Without European 4466 participants -0.14 (-0.21 to -0. < 0.001 08) 0 With European par- 1190 ticipants -0.10 (-0.2 to -0.06) < 0.001 41 Disease-related quality of life Z = 1.0; P = 0.32 Without European 4795 participants -0.21 (-0.27 to -0. < 0.001 15) 0 With European par- 1192 ticipants -0.14 (-0.25 to -0. < 0.001 02) 0 RR 50% pain reduction Z = 2.0; P = 0.045 Without European 4774 participants 1.56 (1.40 to 1.74) < 0.001 0 With European par- 1201 ticipants 1.32 (1.06 to 1.63) < 0.001 0 Withdrawal due to adverse events Z = 0.82; P = 0.41 Without European 4965 participants 1.78 (1.47 to 2.17) < 0.001 0 With European par- 1214 ticipants 2.06 (1.55 to 2.73) < 0.001 0 Abbreviations CI= confidence interval RR = risk ratio SMD: standardized mean difference Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 68 APPENDICES Appendix 1. Search strategies and hits retrieved RCTs in FMS (updated search September 11, 2012) DATABASE (ACCESS) and date of search Search Strategy and hits retrieved MEDLINE (PubMed) 11 September 2012 #1“Fibromyalgia”[MeSH] OR fibromyalgi*[ti] OR fibrositis[ti] 6070 #2 (randomized controlled trial[pt] OR controlled clinical trial[pt] OR randomized[tiab] OR placebo[tiab] OR drug therapy[sh] OR randomly[tiab] OR trial[tiab] OR groups[tiab]) NOT (animals[mh] NOT (humans[mh] AND animals[mh])) 2600091 #3 Search cymbalta OR savella OR ixel OR pristiq OR effexor OR desvenlafaxine OR duloxetine OR milnacipran OR venlafaxine 4353 #4 Search ((#1) AND #2) AND #3 Filters: Publication date from 2010/10/01 to 2012/09/10 42 CENTRAL (The Cochrane Library) 2012, Issue 9 #1MeSH descriptor Fibromyalgia explode all trees 510 #2 (fibromyalgi$):ti,ab,kw or (fibrositis):ti,ab,kw 62 #3 (#1 OR #2), from 2010 to 2012 107 #4 (cymbalta):ti,ab,kw or (savella):ti,ab,kw or (ixel):ti,ab,kw or (pristiq):ti,ab, kw or (effexor):ti,ab,kw 17 #5 (desvenlaxafine):ti,ab,kw or (duloxetine):ti,ab,kw or (milnacipran):ti,ab,kw or (venlaxafine):ti,ab,kw 454 #6 (#4 OR #5), from 2010 to 2012 77 #7 (#3 AND #6) 17 EMBASE via SCOPUS 11 September 2012 1 (TITLE-ABS-KEY(random) OR TITLE-ABS-KEY(placebo) OR TITLEABS-KEY(double-blind)) AND DOCTYPE(ar) AND PUBYEAR > 2009 97115 2 (TITLE-ABS-KEY(expfibromyalgia/) OR TITLE-ABS-KEY(fibrositis) OR TITLE-ABS-KEY(fibromyalgia)) AND DOCTYPE(ar) AND PUBYEAR > 2009 1265 3 (TITLE-ABS-KEY(cymbalta) OR TITLE-ABS-KEY(savella) OR TITLEABS-KEY(ixel) OR TITLE-ABS-KEY(pristiq) OR TITLE-ABS-KEY(effexor) OR TITLE-ABS-KEY(desvenlaxafine) OR TITLE-ABS-KEY(duloxetine) OR TITLE-ABS-KEY(venlaxafine) OR TITLE-ABS-KEY(milnacipran)) AND DOCTYPE(ar) AND PUBYEAR > 2009 1051 4 ((TITLE-ABS-KEY(expfibromyalgia/) OR TITLE-ABS-KEY(fibrositis) OR TITLE-ABS-KEY(fibromyalgia)) AND DOCTYPE(ar) AND PUBYEAR > 2009) AND ((TITLE-ABS-KEY(random) OR TITLE-ABS-KEY(placebo) OR TITLE-ABS-KEY(double-blind)) AND DOCTYPE(ar) AND PUBYEAR > 2009) AND ((TITLE-ABS-KEY(cymbalta) OR TITLE-ABS-KEY(savella) OR TITLE-ABS-KEY(ixel) OR TITLE-ABS-KEY(pristiq) OR TITLE-ABS-KEY (effexor) OR TITLE-ABS-KEY(desvenlaxafine) OR TITLE-ABS-KEY(duloxetine) OR TITLE-ABS-KEY(venlaxafine) OR TITLE-ABS-KEY(milnacipran) ) AND DOCTYPE(ar) AND PUBYEAR > 2009) 50 Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 69 (Continued) ClinicalTrials.gov 11 September 2012 1 fibromyalgia 401 2 fibromyalgia and desvenlaxafine 4 3 fibromyalgia and duloxetine 25 4 fibromyalgia and milnacipran 27 5 fibromyalgia and venlaxafine 0 RCTs in FMS (updated search November 2010) DATABASE (ACCESS) and date of search Search Strategy and hits retrieved MEDLINE (PubMed) 4 November.2010 #1“Fibromyalgia”[MeSH] OR fibromyalgi*[ti] OR fibrositis[ti] 5248 #2 (randomized controlled trial[pt] OR controlled clinical trial[pt] OR randomized[tiab] OR placebo[tiab] OR drug therapy[sh] OR randomly[tiab] OR trial[tiab] OR groups[tiab]) NOT (animals[mh] NOT (humans[mh] AND animals[mh])) 2309479 #3 #1 AND #2 1682 #4 (#2) AND #1 Limits: Publication Date from 2009 312 CENTRAL (The Cochrane Library) 2010, Issue 10 #1MeSH descriptor Fibromyalgia explode all trees 449 #2 fibromyalgi* 755 #3 fibrositis 50 #4 #1 OR #2 OR #3 774 #5 (#1 OR #2 OR #3), from 2009 to 2010 137 (69 in clinical trials) EMBASE (Ovid) 4 November.2010 1 exp Fibromyalgia/ 8833 2 fibromyalgia.ti,ab. 6702 3 exp Fibromyalgia/ 8833 4 fibrositis.ti. 271 5 1 or 2 or 3 or 4 9482 6 random:.tw. or placebo:.mp. or double-blind:.mp. 776985 7 5 and 6 1417 8 limit 7 to yr=“2009 -Current” 405 ClinicalStudyResults.org 31 December 2010 1 fibromyalgia 19 2 fibromyalgia and cymbalta 4 3 fibromyalgia and savella or ixel: no search possible 4 fibromyalgia and pristiq 4 5 fibromyalgia and effexor 0 ClinicalTrials.gov 31 December 2010 1 fibromyalgia 326 2 fibromyalgia and desvenlaxafine 4 3 fibromyalgia and duloxetine 20 4 fibromyalgia and milnacipran 20 5 fibromyalgia and venlaxafine 0 RCTs in FMS (initial search February 2009) Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 70 DATABASE (ACCESS) and date of search Search Strategy and hits retrieved MEDLINE (PubMed) 9 February 2009 #1“Fibromyalgia”[MeSH] OR fibromyalgi*[ti] OR fibrositis[ti] 4433 #2 (randomized controlled trial[pt] OR controlled clinical trial[pt] OR randomized[tiab] OR placebo[tiab] OR drug therapy[sh] OR randomly[tiab] OR trial[tiab] OR groups[tiab]) AND humans [mh] 1912816 #3 #1 AND #2 1316 CENTRAL (The Cochrane Library) 2009, Issue 1 #1MeSH descriptor Fibromyalgia explode all trees 315 #2 fibromyalgi* 512 #3 fibrositis 36 #4 #1 OR #2 OR #3 526 EMBASE (Ovid) 9 February 2009 1 exp Fibromyalgia/ 5537 2 fibromyalgia.ti,ab. 4304 3 exp Fibromyalgia/ 354 4 fibrositis.ti. 122 5 1 or 2 or 3 or 4 6046 6 random:.tw. or placebo:.mp. or double-blind:.mp. 514373 7 5 and 6 886 WHAT’S NEW Last assessed as up-to-date: 27 December 2012. Date Event Description 21 March 2013 Amended Minor edits in summary of findings table 14 January 2013 Amended Revisions to risk of bias tables 23 October 2012 Amended The protocol ’Antidepressants and centrally active agents for fibromyalgia syndrome’ published in 2006 (Nishishinya 2006) has been split into several systematic reviews that will be/have been published as: - Anticonvulsants for fibromyalgia syndrome - Monoamine oxidase inhibitors (MAOIs) for fobromyalgia syndrome - Non-steroidal anti-inflammatory drugs (NSAIDs), analgesics and opioid agents for fibromyalgia syndrome - Sedatives and hypnotic agents for fibromyalgia syndrome - Selective serotonin reuptake inhibitors (SNRIs) for fibromyalgia syndrome - Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome - Tricyclic agents for fibromyalgia syndrome Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 71 CONTRIBUTIONS OF AUTHORS WH: topic conception and methodological aspects; protocol revision; systematic review study selection, data extraction, data analysis, interpretation of findings and author of review. NÜ: systematic review study selection, data extraction, data analysis, data extraction, interpretation of findings; review final proof. ST:topic conception and methodological aspects; protocol review and revision; search of literature; systematic review dispute resolution for methodological quality; review final proof. GU: topic conception and methodological aspects; protocol review and revision; search of literature; review final proof. BW: protocol review and revision; interpretation of findings; review final proof. DECLARATIONS OF INTEREST WH received one consulting fee from Daiichi Sankyo. NÜ received consultancy honoraria by Grünenthal GmbH and travel grants by Pfizer, Astellas, Grünenthal GmbH, and CSL Behring. BW received a consulting fee from Jazz Pharmaceuticals and was a site investigator for a milnacipran trial. ST and GU have no conflicts of interest to declare. SOURCES OF SUPPORT Internal sources • New Source of support, Not specified. None External sources • New Source of support, Not specified. None DIFFERENCES BETWEEN PROTOCOL AND REVIEW The protocol ’Antidepressants and centrally active agents for fibromyalgia syndrome’ has been split into several systematic reviews (Nishishinya 2006). We have added an additional comparison, namely cognitive disturbances, and the calculation of intra-group effect sizes (baseline and final treatment) of true drug and placebo on pain and QOL. A random-effects model was used for all analysis irrespective of the amount of heterogeneity. The GRADE approach was used for the grading of evidence. INDEX TERMS Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 72 Medical Subject Headings (MeSH) Adrenergic Uptake Inhibitors [∗ therapeutic use]; Cyclopropanes [∗ therapeutic use]; Fibromyalgia [∗ drug therapy]; Norepinephrine [∗ metabolism]; Quality of Life; Serotonin Uptake Inhibitors [∗ therapeutic use]; Syndrome; Thiophenes [∗ therapeutic use] MeSH check words Adult; Humans Serotonin and noradrenaline reuptake inhibitors (SNRIs) for fibromyalgia syndrome (Review) Copyright © 2013 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd. 73
