The main purpose of this study is to determine whether the antidepressant response of escitalopram 30mg/day or escitalopram 20mg/day + pindolol, a beta blocker, is different (faster) compared to a standard dose of escitalopram 20mg/day.
Antidepressant drug therapy is the primary therapeutic treatment option in moderate to severe Major Depressive Disorder. However, clinically significant antidepressant response needs sustained treatment during weeks to months. Indeed, in the largest effectiveness study conducted to date (STAR\*D study) involving nearly 3000 depressed outpatients, only about one third of those who ultimately responded did so after 6 weeks of drug treatment and for most patients longer treatment periods were necessary. This delay implies prolonged suffering for the patients and their families. By its antagonist action on the serotonin 1A receptor pindolol is hypothesized to reduce the down-regulation mechanisms of antidepressants. It is therefore expected that addition of pindolol to escitalopram will shorten the therapeutic response. Clinical and preclinical data indicate that escitalopram at 30 mg/day might be more effective and perhaps be associated with a faster onset of action than 20mg. For this purpose the speed of action will be compared between three blindly randomized samples: * escitalopram 20mg per day + placebo * escitalopram 30mg per day + placebo * escitalopram 20mg per day + pindolol 15mg per day (two doses of 7.5mg during 14 days). Subjects will be followed for 6 weeks. The dose of 15mg pindolol per day (during 14 days) is based on the optimal occupancy of the serotonin 1A receptor. At inclusion all subjects will be assessed by a trained psychiatrist using the SCID I mood disorder part which is based on DSM IV criteria, and by means of the French version of the MINI. Severity of depression will be assessed using the MADRS clinician rated and self-report questionnaire, and the French version of the QIDS. Each week subjects will be assessed using the two versions of the Montgomery-Asberg Depression Rating Scale (MADRS) and the HCL-32 a self-report questionnaire assessing hypomania. It is planned to include 135 patients during the three years of the study duration resulting in 45 subjects in each group.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
QUADRUPLE
Enrollment
18
escitalopram p.o., once daily, day 1-2: 10mg, days 3-42: 20mg pindolol p.o., twice daily 7.5 mg days 1-14, once daily 7.5 mg days 15-17
escitalopram p.o., once daily. days 1-2: 10 mg, days 3-4: 20 mg, days 5-42: 30 mg
escitalopram 20 mg, p.o., once daily. Days 1-2: 10mg, days 3-42: 20 mg
Centre de Thérapies Breves (CTB), Secteur Jonction
Geneva, Switzerland
MADRS score change between baseline and 2 weeks of treatment
Differences in MADRS score changes (baseline-day 14) between treatment groups
Time frame: day 14
Response/remission (MADRS) at 6 weeks
% of patients with a given treatment which meet response/remssion criteria after 6 weeks of treatment, based on MADRS
Time frame: day 42
Adverse events
Frequence of adverse events in treatment groups
Time frame: See primary outcome measure
Correlation of drug level of pindolol and/or escitalopram and clinical outcome (primary outcome) between treatment groups
Time frame: Day 10
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