Major Depression Clinical Trial
Official title:
Secondary Prevention of Depression Applying an Experimental Attentional Bias Modification Procedure
| NCT number | NCT02658682 |
| Other study ID # | NFR-229135 |
| Secondary ID | |
| Status | Completed |
| Phase | N/A |
| First received | |
| Last updated | |
| Start date | January 2015 |
| Est. completion date | December 2017 |
| Verified date | April 2019 |
| Source | University of Oslo |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
Depression (Major Depressive Disorder; MDD) has been dubbed "the common cold among the mental
illnesses" and it is also a highly recurrent disorder. Secondary prevention has been
identified as a key goal in the long-term management of depression. High recurrence rate
suggests that there are specific vulnerability factors that increase people's risk for
developing repeated episodes of the disorder. Preventive strategies should identify and
ameliorate these factors to reduce the individual's risk of subsequent episodes. Biased
attention for emotional stimuli is central to the cognitive model where increased sensitivity
to negative cues is believed to fuel the negative thoughts and feelings in depression and
play a key role in maintaining the illness. Selective biases in attention can be modified by
a simple computerized technique; The Attention Bias Modification Task (ABM). This project
aims to investigate whether ABM can reduce surrogate and clinical markers of relapse in a
large group highly vulnerable to depressive episodes. The effects of ABM, immediately after
the two weeks intervention, on three key risk factors for depression will be studied:
Residual symptoms, cortisol awakening response and emotion regulation strategies. The
participants will be followed up after 1 month, 6 months and 12 months. The hypothesis that
ABM will reduce subsequent episodes of low mood over the following 12 months in this group in
a manner predicted by early changes in these risk factors will be investigated. It will also
be tested if such effects in the lab may be dependent on candidate genes which affect
serotonin reuptake and which have been implicated in malleability and emotional learning.
Effects on underlying neural correlates of emotion regulation will be studied in an fMRI
experiment in a sub-sample and which will also be stratified by serotonin transporter
genotype (see also NCT02931487). The predictive value of meta cognitions related to
rumination and the possible mediating effects of automatic thoughts and perceived stress will
also be investigated in a sub group (see also NCT02648165).
The characterization of the cognitive, genetic and neural mechanisms underlying the ABM
effect will have key implications for future treatment development and combination with other
treatment modalities like pharmacotherapy.
| Status | Completed |
| Enrollment | 350 |
| Est. completion date | December 2017 |
| Est. primary completion date | October 2016 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years to 65 Years |
| Eligibility |
Inclusion Criteria: - Nondepressed subjects (based on the MINI structured interview) with a history of major depression Exclusion Criteria: - Current or past neurological illness, bipolar disorder, psychosis or drug addiction. |
| Country | Name | City | State |
|---|---|---|---|
| Norway | Sørlandet Hospital, Department of Psychiatry | Arendal | Aust-Agder |
| Norway | University of Oslo, Department of Psychology | Oslo |
| Lead Sponsor | Collaborator |
|---|---|
| University of Oslo | Diakonhjemmet Hospital, Sorlandet Hospital HF, University of Oxford |
Norway,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Other | Automatic thoughts | Automatic Thought Questionnaire (ATQ) | At baseline, immediately after ABM intervention (average one day), 1 month after intervention, 6 months after intervention and 12 months after intervention | |
| Other | Changes in perceived stress | Perceived Stress Scale (PSS). | At baseline, immediately after ABM intervention (average one day), , 1 month after intervention, 6 months after intervention and 12 months after intervention | |
| Other | Meta cognitions | Positive and Negative Beliefs about Rumination scale (PBRS and NBRS) | At baseline and 12 months after intervention | |
| Other | 5-HTTLPR+A>G polymorphic variation divided by the triallelic functional "high expressive" versus "low expressive" genotype will moderat the effect of ABM on residual symptoms compared to neutral ABM placebo condition | Immediately after ABM intervention. | ||
| Other | Brain Derived Neurotrophic Factor (BDNF) val66met polymorphic variation linked to Brian Derived Neurotrophic Factor (BDNF) variation will moderate the effect of ABM on residual symptoms compared to neutral ABM placebo condition | Immediately after ABM intervention. | ||
| Other | A serotonergic cumulative Genetic score, including (5-HHTLPR, HTR1A 8rs6295) and HTR 2A (rs 6311) polymorphisms will moderate the effects of ABM on residual symptoms compared to neutral placebo condition | Immediately after ABM intervention. | ||
| Other | Change in residual symptoms of depression. Self report | Beck Depression Inventory | One month after intervention, 6 months after intervention and 12 months after intervention | |
| Other | Change in residual symptoms of depression. Clinical rating | Hamilton Depression Rating Scale | One month after intervention, 6 month after intervention and 12 month after intervention | |
| Other | Primary outcome measures will be modified by the degree of attentional change during the ABM intervention. | Immediately after the ABM intervention | ||
| Other | Primary outcome measures will be modified by executive functioning | At baseline | ||
| Primary | Change in residual symptoms of depression. Self report. | Beck Depression Inventory | At baseline and immediately after ABM intervention (during first week after ABM). | |
| Primary | Change in residual symptoms of depression. Clinician rating | Hamilton Depression Rating Scale | At baseline and immediately after ABM intervention (during first week after ABM). | |
| Secondary | Recurrence of major depressive episodes | Measured by the MINI structured interview | Will be measured 12 month after baseline | |
| Secondary | Changes in Emotion Regulation | Emotion Regulation Questionnaire (ERQ). | At baseline. | |
| Secondary | Changes in Rumination | The Rumination Response Scale | At baseline and 12 months after intervention | |
| Secondary | Changes in cortisol response. | Cortisol samples from saliva measured by diural variation (6 samples). | At baseline, immediately after ABM intervention and one month after intervention. | |
| Secondary | Changes in symptoms of anxiety | Beck Anxiety Inventory | At baseline, immediately after ABM intervention (during first week after ABM intervention), 1 month after intervention, 6 months after intervention and 12 months after intervention |
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