Literature DB >> 30883669

Second-generation antidepressants for preventing seasonal affective disorder in adults.

Gerald Gartlehner1, Barbara Nussbaumer-Streit, Bradley N Gaynes, Catherine A Forneris, Laura C Morgan, Amy Greenblatt, Jörg Wipplinger, Linda J Lux, Megan G Van Noord, Dietmar Winkler.   

Abstract

BACKGROUND: Seasonal affective disorder (SAD) is a seasonal pattern of recurrent major depressive episodes that most commonly occurs during autumn or winter and remits in spring. The prevalence of SAD ranges from 1.5% to 9%, depending on latitude. The predictable seasonal aspect of SAD provides a promising opportunity for prevention. This review - one of four reviews on efficacy and safety of interventions to prevent SAD - focuses on second-generation antidepressants (SGAs).
OBJECTIVES: To assess the efficacy and safety of SGAs (in comparison with other SGAs, placebo, light therapy, melatonin or agomelatine, psychological therapies or lifestyle interventions) in preventing SAD and improving patient-centred outcomes among adults with a history of SAD. SEARCH
METHODS: We searched Ovid MEDLINE (1950- ), Embase (1974- ), PsycINFO (1967- ) and the Cochrane Central Register of Controlled Trials (CENTRAL) to 19 June 2018. An earlier search of these databases was conducted via the Cochrane Common Mental Disorders Controlled Trial Register (CCMD-CTR) (all years to 11 August 2015). Furthermore, we searched the Cumulative Index to Nursing and Allied Health Literature, Web of Science, the Cochrane Library, the Allied and Complementary Medicine Database and international trial registers (to 19 June 2018). We also conducted a grey literature search and handsearched the reference lists of included studies and pertinent review articles. SELECTION CRITERIA: For efficacy, we included randomised controlled trials (RCTs) on adults with a history of winter-type SAD who were free of symptoms at the beginning of the study. For adverse events, we planned to include non-randomised studies. Eligible studies compared a SGA versus another SGA, placebo, light therapy, psychological therapy, melatonin, agomelatine or lifestyle changes. We also intended to compare SGAs in combination with any of the comparator interventions versus placebo or the same comparator intervention as monotherapy. DATA COLLECTION AND ANALYSIS: Two review authors independently screened abstracts and full-text publications, extracted data and assessed risk of bias of included studies. When data were sufficient, we conducted random-effects (Mantel-Haenszel) meta-analyses. We assessed statistical heterogeneity by calculating the Chi2 statistic and the Cochran Q. We used the I2 statistic to estimate the magnitude of heterogeneity. We assessed publication bias by using funnel plots.We rated the strength of the evidence using the system developed by the GRADE Working Group. MAIN
RESULTS: We identified 3745 citations after de-duplication of search results and excluded 3619 records during title and abstract reviews. We assessed 126 full-text papers for inclusion in the review, of which four publications (on three RCTs) providing data from 1100 people met eligibility criteria for this review. All three RCTs had methodological limitations due to high attrition rates.Overall, moderate-quality evidence indicates that bupropion XL is an efficacious intervention for prevention of recurrence of depressive episodes in people with a history of SAD (risk ratio (RR) 0.56, 95% confidence interval (CI) 0.44 to 0.72; 3 RCTs, 1100 participants). However, bupropion XL leads to greater risk of headaches (moderate-quality evidence), insomnia and nausea (both low-quality evidence) when compared with placebo. Numbers needed to treat for additional beneficial outcomes (NNTBs) vary by baseline risks. For a population with a yearly recurrence rate of 30%, the NNTB is 8 (95% CI 6 to 12). For populations with yearly recurrence rates of 50% and 60%, NNTBs are 5 (95% CI 4 to 7) and 4 (95% CI 3 to 6), respectively.We could find no studies on other SGAs and no studies comparing SGAs with other interventions of interest, such as light therapy, psychological therapies, melatonin or agomelatine. AUTHORS'
CONCLUSIONS: Available evidence indicates that bupropion XL is an effective intervention for prevention of recurrence of SAD. Nevertheless, even in a high-risk population, three out of four people will not benefit from preventive treatment with bupropion XL and will be at risk for harm. Clinicians need to discuss with patients advantages and disadvantages of preventive SGA treatment, and might want to consider offering other potentially efficacious interventions, which might confer a lower risk of adverse events. Given the lack of comparative evidence, the decision for or against initiating preventive treatment of SAD and the treatment selected should be strongly based on patient preferences.Future researchers need to assess the effectiveness and risk of harms of SGAs other than bupropion for prevention of SAD. Investigators also need to compare benefits and harms of pharmacological and non-pharmacological interventions.

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Year:  2019        PMID: 30883669      PMCID: PMC6422318          DOI: 10.1002/14651858.CD011268.pub3

Source DB:  PubMed          Journal:  Cochrane Database Syst Rev        ISSN: 1361-6137


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2.  GRADE guidelines: 1. Introduction-GRADE evidence profiles and summary of findings tables.

Authors:  Gordon Guyatt; Andrew D Oxman; Elie A Akl; Regina Kunz; Gunn Vist; Jan Brozek; Susan Norris; Yngve Falck-Ytter; Paul Glasziou; Hans DeBeer; Roman Jaeschke; David Rind; Joerg Meerpohl; Philipp Dahm; Holger J Schünemann
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Review 3.  Update on the biology of seasonal affective disorder.

Authors:  Chang-Ho Sohn; Raymond W Lam
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Review 4.  Interactions of the serotonin and circadian systems: nature and nurture in rhythms and blues.

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Journal:  Neuroscience       Date:  2011-09-21       Impact factor: 3.590

Review 5.  Bupropion: pharmacology and therapeutic applications.

Authors:  Kevin F Foley; Kevin P DeSanty; Richard E Kast
Journal:  Expert Rev Neurother       Date:  2006-09       Impact factor: 4.618

Review 6.  Controlling for drug dose in systematic review and meta-analysis: a case study of the effect of antidepressant dose.

Authors:  Richard A Hansen; Charity G Moore; Stacie B Dusetzina; Brian I Leinwand; Gerald Gartlehner; Bradley N Gaynes
Journal:  Med Decis Making       Date:  2009-01-13       Impact factor: 2.583

7.  Prevalence of seasonal affective disorder at four latitudes.

Authors:  L N Rosen; S D Targum; M Terman; M J Bryant; H Hoffman; S F Kasper; J R Hamovit; J P Docherty; B Welch; N E Rosenthal
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Review 8.  Light therapy for preventing seasonal affective disorder.

Authors:  Barbara Nussbaumer; Angela Kaminski-Hartenthaler; Catherine A Forneris; Laura C Morgan; Jeffrey H Sonis; Bradley N Gaynes; Amy Greenblatt; Jörg Wipplinger; Linda J Lux; Dietmar Winkler; Megan G Van Noord; Julia Hofmann; Gerald Gartlehner
Journal:  Cochrane Database Syst Rev       Date:  2015-11-08

9.  Relapse prevention by citalopram in SAD patients responding to 1 week of light therapy. A placebo-controlled study.

Authors:  K Martiny; M Lunde; C Simonsen; L Clemmensen; D L Poulsen; K Solstad; P Bech
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10.  Preferred reporting items for systematic reviews and meta-analyses: the PRISMA statement.

Authors:  David Moher; Alessandro Liberati; Jennifer Tetzlaff; Douglas G Altman
Journal:  PLoS Med       Date:  2009-07-21       Impact factor: 11.069

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2.  Melatonin and agomelatine for preventing seasonal affective disorder.

Authors:  Barbara Nussbaumer-Streit; Amy Greenblatt; Angela Kaminski-Hartenthaler; Megan G Van Noord; Catherine A Forneris; Laura C Morgan; Bradley N Gaynes; Jörg Wipplinger; Linda J Lux; Dietmar Winkler; Gerald Gartlehner
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3.  Psychological therapies for preventing seasonal affective disorder.

Authors:  Catherine A Forneris; Barbara Nussbaumer-Streit; Laura C Morgan; Amy Greenblatt; Megan G Van Noord; Bradley N Gaynes; Jörg Wipplinger; Linda J Lux; Dietmar Winkler; Gerald Gartlehner
Journal:  Cochrane Database Syst Rev       Date:  2019-05-24
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