Efficacy of Bright Light Treatment, Fluoxetine, and the Combination in Patients With Nonseasonal Major Depressive Disorder: A Randomized Clinical Trial.

IMPORTANCE Bright light therapy is an evidence-based treatment for seasonal depression, but there is limited evidence for its efficacy in nonseasonal major depressive disorder (MDD). OBJECTIVE To determine the efficacy of light treatment, in monotherapy and in combination with fluoxetine hydrochloride, compared with a sham-placebo condition in adults with nonseasonal MDD. DESIGN, SETTING, AND PARTICIPANTS Randomized, double-blind, placebo- and sham-controlled, 8-week trial in adults (aged 19-60 years) with MDD of at least moderate severity in outpatient psychiatry clinics in academic medical centers. Data were collected from October 7, 2009, to March 11, 2014. Analysis was based on modified intent to treat (randomized patients with ≥1 follow-up rating). INTERVENTIONS Patients were randomly assigned to (1) light monotherapy (active 10,000-lux fluorescent white light box for 30 min/d in the early morning plus placebo pill); (2) antidepressant monotherapy (inactive negative ion generator for 30 min/d plus fluoxetine hydrochloride, 20 mg/d); (3) combination light and antidepressant; or (4) placebo (inactive negative ion generator plus placebo pill). MAIN OUTCOMES AND MEASURES Change score on the Montgomery-Åsberg Depression Rating Scale (MADRS) from baseline to the 8-week end point. Secondary outcomes included response (≥50% reduction in MADRS score) and remission (MADRS score ≤10 at end point). RESULTS A total of 122 patients were randomized (light monotherapy, 32; fluoxetine monotherapy, 31; combination therapy, 29; placebo, 30). The mean (SD) changes in MADRS score for the light, fluoxetine, combination, and placebo groups were 13.4 (7.5), 8.8 (9.9), 16.9 (9.2), and 6.5 (9.6), respectively. The combination (effect size [d] = 1.11; 95% CI, 0.54 to 1.64) and light monotherapy (d = 0.80; 95% CI, 0.28 to 1.31) were significantly superior to placebo in the MADRS change score, but fluoxetine monotherapy (d = 0.24; 95% CI, -0.27 to 0.74) was not superior to placebo. For the respective placebo, fluoxetine, light, and combination groups at the end point, response was achieved by 10 (33.3%), 9 (29.0%), 16 (50.0%), and 22 (75.9%) and remission was achieved by 9 (30.0%), 6 (19.4%), 14 (43.8%), and 17 (58.6%). Combination therapy was superior to placebo in MADRS response (β = 1.70; df = 1; P = .005) and remission (β = 1.33; df = 1; P = .02), with numbers needed to treat of 2.4 (95% CI, 1.6 to 5.8) and 3.5 (95% CI, 2.0 to 29.9), respectively. All treatments were generally well tolerated, with few significant differences in treatment-emergent adverse events. CONCLUSIONS AND RELEVANCE Bright light treatment, both as monotherapy and in combination with fluoxetine, was efficacious and well tolerated in the treatment of adults with nonseasonal MDD. The combination treatment had the most consistent effects. TRIAL REGISTRATION clinicaltrials.gov Identifier: NCT00958204.

[1]  M. Terman,et al.  Controlled trial of naturalistic dawn simulation and negative air ionization for seasonal affective disorder. , 2006, The American journal of psychiatry.

[2]  K. Martiny,et al.  Adjunctive Bright Light in Non‐Seasonal Major Depression , 2004, Acta psychiatrica Scandinavica. Supplementum.

[3]  G. Freedman,et al.  Burden of Depressive Disorders by Country, Sex, Age, and Year: Findings from the Global Burden of Disease Study 2010 , 2013, PLoS medicine.

[4]  Josephine Arendt,et al.  Human circadian rhythms: physiological and therapeutic relevance of light and melatonin , 2006, Annals of clinical biochemistry.

[5]  P. Bech,et al.  Adjunctive bright light in non‐seasonal major depression: results from clinician‐rated depression scales , 2005, Acta psychiatrica Scandinavica.

[6]  L. Berglund,et al.  Bright white light therapy in depression: A critical review of the evidence. , 2015, Journal of affective disorders.

[7]  R. Hamer,et al.  The efficacy of light therapy in the treatment of mood disorders: a review and meta-analysis of the evidence. , 2005, The American journal of psychiatry.

[8]  D. Kupfer,et al.  Acute and longer-term outcomes in depressed outpatients requiring one or several treatment steps: a STAR*D report. , 2006, The American journal of psychiatry.

[9]  S. Kasper,et al.  Effects of tryptophan depletion on drug-free patients with seasonal affective disorder during a stable response to bright light therapy. , 1997, Archives of general psychiatry.

[10]  M. Terman,et al.  Light Therapy for Seasonal and Nonseasonal Depression: Efficacy, Protocol, Safety, and Side Effects , 2005, CNS Spectrums.

[11]  R. Levitan,et al.  The chronobiology and neurobiology of winter seasonal affective disorder , 2007, Dialogues in clinical neuroscience.

[12]  J. Krystal,et al.  Effects of rapid tryptophan depletion in patients with seasonal affective disorder in remission after light therapy. , 1996, Archives of general psychiatry.

[13]  H. Fathy,et al.  Quality of Life: The Ultimate Outcome Measure of Interventions in Major Depressive Disorder , 2011, Harvard review of psychiatry.

[14]  Julian M Somers,et al.  Prevalence and Incidence Studies of Mood Disorders: A Systematic Review of the Literature , 2004, Canadian journal of psychiatry. Revue canadienne de psychiatrie.

[15]  P. Cuijpers,et al.  Excess mortality in depression: a meta-analysis of community studies. , 2002, Journal of affective disorders.

[16]  Anne Germain,et al.  Circadian rhythm disturbances in depression , 2008, Human psychopharmacology.

[17]  Jacob Cohen,et al.  A power primer. , 1992, Psychological bulletin.

[18]  M. Hamilton,et al.  Development of a rating scale for primary depressive illness. , 1967, The British journal of social and clinical psychology.

[19]  Fluoxetine versus other types of pharmacotherapy for depression , 2013 .

[20]  S. Patten,et al.  Canadian Network for Mood and Anxiety Treatments (CANMAT) clinical guidelines for the management of major depressive disorder in adults. Introduction. , 2009, Journal of affective disorders.

[21]  C. Beasley,et al.  Fluoxetine: relationships among dose, response, adverse events, and plasma concentrations in the treatment of depression. , 1990, Psychopharmacology bulletin.

[22]  C. Eastman,et al.  Bright Light Therapy for Winter Depression—Is Phase Advancing Beneficial? , 2004, Chronobiology international.

[23]  Raymond W Lam,et al.  A controlled trial of the Litebook light-emitting diode (LED) light therapy device for treatment of Seasonal Affective Disorder (SAD) , 2007, BMC psychiatry.

[24]  Raymond W Lam,et al.  The Can-SAD study: a randomized controlled trial of the effectiveness of light therapy and fluoxetine in patients with winter seasonal affective disorder. , 2006, The American journal of psychiatry.

[25]  M A Young,et al.  Bright light treatment of winter depression: a placebo-controlled trial. , 1998, Archives of general psychiatry.

[26]  Z. Segal,et al.  Canadian Network for Mood and Anxiety Treatments (CANMAT) clinical guidelines for the management of major depressive disorder in adults. II. Psychotherapy alone or in combination with antidepressant medication. , 2009, Journal of affective disorders.

[27]  M. Hotopf,et al.  Fluoxetine versus other types of pharmacotherapy for depression. , 2005, The Cochrane database of systematic reviews.

[28]  K. Kobak,et al.  Development and reliability of a structured interview guide for the Montgomery-Åsberg Depression Rating Scale (SIGMA) , 2008, British Journal of Psychiatry.

[29]  C. McClung,et al.  Circadian rhythms and mood regulation: Insights from pre-clinical models , 2011, European Neuropsychopharmacology.

[30]  J. Stewart,et al.  Controlled trial of bright light and negative air ions for chronic depression , 2005, Psychological Medicine.

[31]  Altamura Ac,et al.  The evidence for 20mg a day of fluoxetine as the optimal dose in the treatment of depression. , 1988 .

[32]  T. Borkovec,et al.  Credibility of analogue therapy rationales , 1972 .

[33]  J. Markowitz,et al.  The 16-Item quick inventory of depressive symptomatology (QIDS), clinician rating (QIDS-C), and self-report (QIDS-SR): a psychometric evaluation in patients with chronic major depression , 2003, Biological Psychiatry.

[34]  A. Neumeister Tryptophan depletion, serotonin, and depression: where do we stand? , 2003, Psychopharmacology bulletin.

[35]  S. Kasper,et al.  Effects of tryptophan depletion vs catecholamine depletion in patients with seasonal affective disorder in remission with light therapy. , 1998, Archives of general psychiatry.

[36]  Raymond W Lam,et al.  Seasonal affective disorder: a clinical update. , 2007, Annals of clinical psychiatry : official journal of the American Academy of Clinical Psychiatrists.

[37]  Lorena Hsu,et al.  Prevalence and Incidence Studies of Anxiety Disorders: A Systematic Review of the Literature , 2004, Canadian journal of psychiatry. Revue canadienne de psychiatrie.

[38]  Christian Even,et al.  Efficacy of light therapy in nonseasonal depression: a systematic review. , 2008, Journal of affective disorders.

[39]  R. Lam,et al.  Update on the Biology of Seasonal Affective Disorder , 2005, CNS Spectrums.

[40]  S. Patten,et al.  Canadian Network for Mood and Anxiety Treatments (CANMAT) clinical guidelines for the management of major depressive disorder in adults. III. Pharmacotherapy. , 2009, Journal of affective disorders.

[41]  M. Åsberg,et al.  A New Depression Scale Designed to be Sensitive to Change , 1979, British Journal of Psychiatry.

[42]  Ronald C Kessler,et al.  The economic burden of adults with major depressive disorder in the United States (2005 and 2010). , 2015, The Journal of clinical psychiatry.

[43]  Janet B W Williams,et al.  Diagnostic and Statistical Manual of Mental Disorders , 2013 .

[44]  D. Sheehan,et al.  The Mini-International Neuropsychiatric Interview (M.I.N.I.): the development and validation of a structured diagnostic psychiatric interview for DSM-IV and ICD-10. , 1998, The Journal of clinical psychiatry.

[45]  D. Kripke,et al.  Light therapy for non-seasonal depression. , 2004, The Cochrane database of systematic reviews.

[46]  C. Eastman What the placebo literature can tell us about light therapy for SAD. , 1990, Psychopharmacology bulletin.

[47]  J. Emens,et al.  The circadian basis of winter depression. , 2006, Proceedings of the National Academy of Sciences of the United States of America.