Depression Clinical Trial
Official title:
Rumination Focused Cognitive Behavioral Therapy for Major Depression and Recurrent Depression and Relapse Prevention -a Pragmatic RCT Study in a Danish Psychiatric Outpatient Service
Group based cognitive behavioural therapy (CBT) is an effective treatment of depression,
however, one third of patients do not respond satisfactorily (McDermut, Miller, & Brown,
2001), and relapse rates around 30% have been reported from several studies (Butler,
Chapman, Forman, & Beck, 2006).
The present study compares group based CBT with rumination focused CBT for depression with
respect to outcome and relapse.
Rumination has been evidenced as a crucial vulnerability to depression (Smith & Alloy,
2009), predicting the onset, severity and duration of future depression (Nolen-Hoeksema,
2000). Depressed individuals show a negative bias in the perception of facial emotion, in
the acute phase as well as in remission (Bouhuys, Geerts, & Gordijn, 1999), and display
difficulties in disengaging from negative stimuli (Koster, De Raedt, Goeleven, Franck, &
Crombez, 2005). In addition the present study investigate rumination and perceptual
attention bias as potential key mechanisms underlying depression.
128 depressed patients will be recruited and randomised for group based CBT or group based
rumination focused CBT. Patients are assessed subsequently during treatment and at 6 month
follow-up regarding depression, rumination, worry, negative perceptual bias, attention
control. Results are expected at spring 2016.
Background and rationale
The aim of the present study is to compare the effectiveness of rumination-focused cognitive
behavior therapy vs. cognitive behavior therapy for treatment of depression.
Understanding the mechanisms involved in effective cognitive behavioural therapy is a key
focus of clinical research (Watkins, 2009). The study will investigate possible underlying
mechanisms of rumination and thereby provide insights about the information processing and
symptoms of depression.
Rumination, a process of recurrent negative thinking and dwelling on negative affect, is a
common residual symptom (Kim, Yu, Lee, & Kim, 2012; Riso et al., 2003). Rumination has been
evidenced as a crucial vulnerability to depression (Smith & Alloy, 2009), predicting the
onset, severity and duration of future depression (Nolen-Hoeksema, 2000).
Such knowledge indicates that rumination is a key factor involved in the initiation and
maintenance of depressive symptoms. Individuals that display high levels of rumination even
if not currently presenting depressive symptoms may therefore have an increased risk for
developing future depression. Consequently, if involved in the pathogenesis of depression,
rumination may constitute an active ingredient of psychological intervention. Hence,
interventions explicitly targeting rumination may improve the efficiency of CBT for
recurrent and chronic depression (Watkins, 2009). However, few studies have tested
interventions targeting rumination, with the exception of Watkins (2007; 2011).
Cognitive theories argue that information processing bias influences the aetiology and
maintenance of depression. On tests of cognitive performance, particularly attention and
memory has been repeatedly reported affected in depression (Goeleven, De Raedt, Baert, &
Koster, 2006). Depressed individuals show a negative bias in the perception of facial
emotion, in the acute phase as well as in remission (Bouhuys, Geerts, & Gordijn, 1999), and
display difficulties in disengaging from negative stimuli (Koster, De Raedt, Goeleven,
Franck, & Crombez, 2005).
It is suggested in the literature that depressed people are not able to gain control over
the emotional influence of negative stimuli due to dysfunctional inhibition of negative
stimuli (Donaldson, Lam, & Mathews, 2007). This idea is substantiated by the strong
relationship between rumination and depression suggesting that impaired inhibitory function
may be an underlying mechanism of rumination.
However, experimental paradigms used to study attention has, apart from Donaldson and
colleagues (2007), not been applied to rumination or other self-report measures assessing
attention and attentional control in clinical samples. The present study investigates the
relationship between clinical features of depression such as the self-reported tendency to
ruminate in response to negative affect, as well as the experience of attentional control
and actual performance on cognitive tests assessing attentional control. Furthermore by
combining clinical self-report with test performance, the study addresses potentially
underlying mechanisms of rumination. Understanding the mechanisms involved in effective
cognitive behavioural therapy is thus a key focus of clinical research (Watkins, 2009).
RFCBT will be compared to CBT for depression. Cognitive Behavioural Therapy (CBT) is
recommended for the treatment of depression by the National Institute for Health and
Clinical Excellence (NICE) in UK. Group CBT is an effective treatment of depression,
however, one third of patients do not respond satisfactorily (McDermut, Miller, & Brown,
2001), and relapse rates around 30% have been reported from several studies (Butler,
Chapman, Forman, & Beck, 2006). Residual symptoms following treatment is a common problem,
as 30-50% of remitted patients present residual symptoms by the end of treatment (Kennedy &
Paykel, 2004). These patients display more depressive symptoms, have a lower level of social
functioning and utilize more health care services (Cornwall & Scott, 1997) compared to fully
remitted patients.
Objectives:
The aim of the present study to compare the effectiveness of rumination-focused CBT vs. CBT
for treatment of depression.
Trial design:
The design is a pragmatic block randomized controlled blinded trial comparing two types of
group based cognitive behavioural therapy for depression.
Study design:
The study takes place in a community psychiatric outpatient service in Hillerød, Denmark,
which receives 200-250 patients with depression per year. Patients that are referred for
treatment at the Psychiatric Outpatient Centre in Hillerød with a primary diagnosis of
depression, recurrent or chronic, are recruited to the study. We plan to recruit a total of
128 patients, 64 in each treatment type. Intake will take place from July 2013 until Marts
2015.
Therapists conducting the group therapies are trained and experienced cognitive behavioural
therapist with at least 4 years of experience with CBT. The therapist conduction the groups
with RFCBT are trained and supervised by professor Ed Watkins (affiliation).
Both interventions runs for 11 week with a 3 hours session once a week and will be delivered
by trained clinicians with at least two years of experience in CBT. Preceding the first
group session the participants will be given an individual session with a group therapist to
prepare for the groupbased treatment.
The psychiatrist conducting the initial evaluation of the patients invites the patients to
participate if the inclusion criteria are met. The patients will receive verbal and written
information about the project from the psychiatrist. If interested in participation the
patients will be contacted by the Ph.D. student to sign the informed consent and invited to
first assessment. After the assessment the patients are finally randomised by computer
method to receive one of the two treatment types.
Primary outcome:
Primary outcome is the post-treatment assessment of the Hamilton Rating Scale for Depression
(HRSD) Bech P, Kastrup M, Rafaelsen OJ. (1986).
Secondary outcomes:
Post-treatment measures of HAM-D-6 (Bech et al., 1975), Penn State Worry Questionnaire
(PSWQ; Meyer, Miller, Metzger, & Borkovec, 1990), Ruminative Response Scale of the Response
Style Questionnaire (RRS;(Nolen-Hoeksema & Morrow, 1991), Generalized Anxiety Disorder 7
(GAD-7; Spitzer, et al. 2006). Trail-making A and B (Strauss et al. 2006), Dot-probe task
-computerized test of cognitive control and emotional processing (Donaldson et al., 2007).
Sample size estimation:
Assuming similar mean changes in HRSD scores from pre-to-post intervention as found by
Watkins and colleagues [18] for RFCBT (M = 7.81) and by Paykel and colleagues [11] for CBT
(M = 3.52), and a conservative estimate of pooled standard deviation for change in HRSD of 6
(when SD= 3.60 for change in HRSD in RFCBT), we estimate a between-treatment effect size of
Cohen's d = 0.7. To detect a difference in effect size of 0.7 between RFCBT and CBT at a
two-tailed significance level of 5%, each treatment arm requires 44 patients each to obtain
90% statistical power [40]. Assuming a dropout rate of 20%, we will recruit 55 patients into
each treatment arm. With an average size of the therapy group of m = 8 in both treatment
arms, and an intraclass correlation of about ρ = 0.05, a design effect of 1 + (m - 1)ρ =
1.35 follows, so that we plan to recruit 8 groups in each treatment arm (128 patients in
total).
Statistical analysis:
The primary outcome is the post-treatment score on the HRSD, which is treated as a
continuous, normally distributed variable. The primary efficacy hypothesis will be tested
using a multilevel two-group comparison (RFCBT vs. CBT), with Group as a main effect,
Therapy Group as a random intercept, and the HRSD baseline score as a continuous covariate.
The test will be performed at the 5% two-tailed significance level.
The primary test for efficacy will be based on the intention-to-treat population, with all
randomized patients entering the analysis set, and multiple imputation of missing values in
the primary endpoint [42]. For the secondary outcomes, similar analyses will be used, taking
into consideration the scale of the variable (e.g., logistic regression for binary
outcomes).
Ethical considerations:
The patients will be informed about the research project and purpose of the project prior to
participation and asked for informed consent. There are no side effect due to the rumination
focused cognitive behavioral therapy. It is not possible to pay the patients for the
participating in the research project.
Participant can leave the treatment on request. If anyone involved in the trial get
knowledge of increased risk of suicide among participants relevant prevention will be
initiated.
The participant will be given treatment as usual, clinical management and medical treatment
if needed assessed by highly trained psychiatrist at PCN.
The project is approved by the Danish national ethical scientific committee and is
registered at The Danish Data Protection Agency by Region Hovedstaden Psychiatry (casenumber
H-1-2013-049).
;
Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Double Blind (Investigator, Outcomes Assessor), Primary Purpose: Treatment
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