Bipolar Disorder Clinical Trial
Official title:
Effect of Action-Based Cognitive Remediation on Cognition and Frontal Lobe Activity in Patients With Bipolar Disorder in Remission (PRETEC-ABC)
PRETEC-ABC aims to assess the effect of a new form of cognitive remediation, Action-Based Cognitive Remediation (ABCR), in patients with bipolar disorder in remission on cognition, and to assess the neural assays for treatment effects with the purpose of identifying a neural biomarker for pro-cognitive effect. It is hypothesized (i) that ABCR vs. a control treatment has a beneficial effect on cognition in remitted patients with bipolar disorder remission. It is hypothesized (ii) that this treatment-associated improvement of cognition translates into better functional capacity at a six months follow-up assessment (secondary outcome). Finally, as an exploratory measure, it is hypothesized that ABCR will produce an early change in frontal activity and that this activity will correlate with ABCR-associated improvements in cognitive function.
The trial will include outpatients with BD in full or partial remission (a score ≤14 on the
Hamilton Depression Rating Scale (HDRS) and Young Mania Rating Scale (YMRS). Recruitment will
be carried out through the ongoing Bipolar Illness Onset (BIO) study, the Copenhagen
Affective Disorder Clinic, Psychiatric Centre Copenhagen, Rigshospitalet, other mental health
centres, consultant psychiatrists in the Capital Region of Denmark, and through
advertisements on relevant websites.
Participants will undergo an eligibility assessment followed by randomisation. When 4 - 6
participants have been randomised to either the ABCR or the control group, the baseline
assessments are carried out. The baseline assessment is completed over two days, 1 - 3 days
apart. A fMRI scan is carried out on day 1 encompassing spatial and verbal working memory
N-back tasks, a picture encoding task, a resting state and a structural scan. On day 2, a
blood sample is drawn in the morning, followed by administration of a comprehensive
neuropsychological test battery. Participants fill in questionnaires concerning subjective
cognitive complaints, psychosocial functioning and quality of life and functional capacity is
assessed using a clinician-rated interview and a performance based assessment. Sleep quantity
and quality in the past three days is assessed. After two weeks of ABCR or control treatment,
functional MRI, neuropsychological testing an assessment of mood and subjective cognition are
repeated. These assessments, as well as assessments of functional capacity and quality of
life, are repeated within two weeks after treatment completion and six months after treatment
completion.
Block randomisation is carried out by Pharma Consulting Group, stratified by gender and age
(patients < or ≥ 35 years).
Power calculation was also carried out by Pharma Consulting Group based on findings from a
previous RCT in our group assessing the effect of 8 weeks of EPO treatment on the same
cognitive composite score. In PreTEC-ABC, a clinically relevant difference between the ABCR
and the control groups following 10 weeks of treatment is assumed to be 0.4 SD (corresponding
to a medium effect size) on the primary outcome, with a mean change in the cognitive
composite score of 0.5 SD. Assuming a 10% drop-out rate, we will recruit up to N=58 in order
to achieve complete datasets for N=52 participants.
Data will be analysed using mixed models using intention-to-treat (ITT) analyses.
Functional MRI-data will be pre-processed and analysed with the FMRIB Expert Analysis Tool
(FEAT) and the "randomize" algorithm implemented in FMRIB Software Library (FSL). Functional
MRI data will be analysed using a Region of interest (ROI) analysis to assess differences
between the ABCR and control group in neural activity in the dlPFC and the hippocampi after 2
weeks. Exploratory whole-brain analyses will be conducted to investigate any effects in other
brain regions. Any differences in neural activity will be correlated with potential changes
in the cognitive composite score at weeks 2 and post-treatment. If there is a significant
correlation with cognition at post-treatment, multiple regression analysis will be carried
out, adjusting for mood and demographic characteristics, to assess whether early change in
neural activity is predictive of pro-cognitive effects.
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