Bipolar Disorder Clinical Trial
Official title:
Escitalopram in Bipolar Depression: a Placebo-controlled Study of Acute and Maintenance Treatment
Funding: An investigator-initiated trial funded by H. Lundbeck AS.
Study design: Prospective, randomised, placebo-controlled parallel-group multicenter study.
Aim: To investigate efficacy and side effects (especially mood switches) of escitalopram,a
selective serotonin reuptake inhibitor, in the acute and maintenance treatment of bipolar
depression.
Hypotheses:
1. Escitalopram, given in addition to mood stabilising medications, is significantly more
efficacious, measured by response and remission rates than placebo in bipolar
depression (the acute phase study).
2. Continuation therapy with escitalopram gives significantly longer mean time to
depressive relapse and fewer depressive relapses compared to placebo (the continuation
study).
3. The incidence of "mood switching" (defined as development of mixed episodes, mania, or
hypomania according to DSM-IV criteria) do not differ significantly between
escitalopram and placebo in either the acute or the continuation phases.
Patients: In- and outpatients receiving care in the specialised psychiatric services of
Western Norway. The population is intended to be representative of the patients treated for
bipolar depression in ordinary specialist care. Patients must have a MADRS score of at least
20 at baseline. Patients with ongoing substance abuse or dependence, organic mental illness,
and non-affective psychotic symptoms are excluded.
Medication: Escitalopram 10-20 mg daily or placebo in addition to mood stabilisers. The dose
of mood stabilisers must have been constant for the last six weeks prior to randomisation.
Method: Phase 1 is a eight-week acute treatment trial with six clinical assessments.
Patients treated with escitalopram who have not responded after eight weeks (defined by at
least 50% reduction of MADRS score compared to baseline) leave the study. Placebo
non-responders are treated openly with escitalopram and repeat phase 1. Responders are
re-randomised to 32 weeks of maintenance treatment (phase 2). Phase 2 has nine clinical
assessments. Patients who develop hypomania, mania or depressive episodes (defined as
episodes meeting DSM-IV criteria for Major Depressive Episode with MADRS scores of at least
20 points) leave the study in this phase. Patients leaving the study prematurely will be
offered alternative treatment.
Aims
The study has two main aims:
1. To compare the efficacy and the risk of "mood switching" of escitalopram and placebo in
the acute phase treatment of bipolar depression in patients already taking mood
stabilising medication.
2. To compare the efficacy of escitalopram and placebo in continuation phase therapy for
bipolar depression using a placebo-controlled discontinuation design. The study will
compare the occurrence of syndromal and subsyndromal relapses, mixed states, mania,
hypomania, and "rapid cycling" in a seven months' maintenance study following response
to acute phase treatment.
Hypotheses
1. Escitalopram, given in addition to mood stabilising medications, is significantly more
efficacious, measured by response and remission rates than placebo in bipolar
depression (the acute phase study).
2. Continuation therapy with escitalopram gives significantly longer mean time to
depressive relapse and fewer depressive relapses compared to placebo (the continuation
study).
3. The incidence of "mood switching" (defined as development of mixed episodes, mania, or
hypomania according to DSM-IV criteria do not differ significantly between escitalopram
and placebo in either the acute or the continuation phases.
Design This is a multi-center RCT with parallel-group design. The study compares the
efficacy of placebo and escitalopram, given as add-on to mood stabilising medications in
patients with bipolar depression without non-affective psychotic symptoms according to
DSM-IV, and with a baseline MADRS score of ≥ 20 points.
The study has two phases. The acute phase study lasts for eight weeks and compares the
efficacy of escitalopram and placebo on depressive symptoms in bipolar depression. Response
is defined as at least 50% improvement on the MADRS compared to the baseline score.
Responders to escitalopram are re-randomised to escitalopram or placebo for the continuation
phase while placebo responders continue taking placebo for the continuation phase. Patients
on escitalopram who do not respond in the acute phase leave the study, whereas placebo
non-responders are treated openly with escitalopram and repeat phase 1. Responders to this
open-label treatment are then re-randomised double blind to escitalopram or placebo for the
continuation study.
The continuation phase study lasts for 32 weeks. Patients who responded to placebo in the
acute phase continue placebo and their usual mood stabilising medication for the remainder
of the study. Those who responded to escitalopram are re-randomised to continue taking
placebo or escitalopram in unchanged doses. Patients who develop new mood episodes
(DSM-IV-defined major depressive episode, mania, hypomania, or mixed episodes) or MADRS
score ≥ 20 points leave the study.
Method Screening includes sociodemographic variables, medical and psychiatric history,
diagnosis made on the basis of clinical interview and verified by the MINI, symptom
intensity measured by the MADRS,), results of medical examination and laboratory tests (ECG,
height, weight, blood pressure and blood tests). Sociodemographic variables include age,
gender, previous and concomitant disorders, course and treatment of mental disorders,
bipolar disorder type (I or II), age of onset and history of psychotropic medication use.
Study procedure As soon as the blood samples are analysed, eligible patients can be
randomised. They are rated on the MADRS, Clinical Global Impressions (CGI), Inventory of
Depressive Symptoms - Self Report (IDS-SR), Medical Outcomes Study Short Form 12 (SF-12),
Global Assessment of Functioning (GAF) and Sheehan Disability Inventory (SDI) at the
baseline visit. Study medication is dispensed. The patients will return to further visits as
shown below. Patients will receive study medication for a maximum of 40 weeks. Adverse
events and concomitant medications are recorded.
Assessments
The following assessments will be carried out::
1. MADRS, GAF, IDS-RS, and CGI-I at week 1, 2, 4, 6, 8, 9, 10, 12, 16, 20, 24, 28, 34 and
40
2. SDI and QLDS at week 8 and 40
3. Diagnostic criteria for Mania and Hypomania at week 1, 2, 4, 6, 8, 9, 10, 12, 16, 20,
24, 28, 34 and 40
4. Diagnostic criteria for Major Depressive Episode at week 8, 9, 10, 12, 16, 20, 24, 28,
34 and 40
For the acute study, response and remission rates as assessed by the MADRS are the primary
outcome measures. CGI-Improvement and IDS-SR are secondary outcome measures. In the
continuation study, primary outcome measures include emergence of major depressive episodes
and mania/hypomania, while time spent at different depressive symptom levels as assessed by
the DSM-IV diagnostic criteria are secondary outcome measures.
Definitions Response: at least a 50% reduction of the baseline MADRS score at the end of
phase 1 if the patient has completed at least four weeks of the study. CGI-I 1 or 2 at the
end of phase 1.
Remission: MADRS score of 12 or less at the end of the acute phase if the patient has
completed at least four weeks of the study.
New episode: A patient who has previously responded to treatment meets the DSM-IV criteria
for Major Depressive Episode. The patient must score at least 15 points on the MADRS and
have a CGI-S score of 3 or more during this episode.
Mania and hypomania: by DSM-IV criteria.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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