Clinical Trial Details
— Status: Enrolling by invitation
Administrative data
| NCT number |
NCT06251908 |
| Other study ID # |
p-2023-14655 |
| Secondary ID |
|
| Status |
Enrolling by invitation |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
February 12, 2024 |
| Est. completion date |
December 24, 2025 |
Study information
| Verified date |
February 2024 |
| Source |
Mental Health Services in the Capital Region, Denmark |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Health institutes call for psychosocial interventions and recovery-oriented approaches as
supplement to pharmacological treatment for mental health disorders. Participatory art
interventions have been suggested to be promising in promoting recovery by stimulating
connectedness, hope, renegotiation of identity, participatory meaning-making and empowerment.
In spite of promising findings, the evidence base is still thin. We have developed
Rewritalize (REWR), a manualised, recovery-oriented fifteen-session participatory creative
writing group intervention, led by a professional author and attended by a mental health
professional. Participants are introduced to literary forms, write spontaneously on those
forms, share their texts and engage in reflective discussions about them. It is designed to
provide a holding and non-stigmatising environment, structure and continuity, and to promote
self-expression, playful experimentation, agency, recognition, participatory meaning-making,
renegotiation of identity and social engagement.
The aim of the present project is to evaluate REWR for persons with schizophrenia spectrum
disorders. This study is a randomised controlled clinical trial focusing on clinical and
personal recovery.
This study is an investigator-initiated, randomised, two-arm, single-blinded, multi-center,
waiting list trial. Participants (n=266) with schizophrenia spectrum disorders (age: 18-35)
will be recruited at six psychiatric centres in region Zealand and randomised to active
(creative writing group + treatment as usual) or control (waiting list + treatment as usual)
condition. Assessments will be collected pre- and post-intervention and six months after end
of intervention. The primary outcome measure will be the questionnaire of the process of
recovery administered at the end of the intervention. Secondary outcome measures comprise
measures of recovery, self-efficacy and mentalising assessed at the end of the intervention
and six months after the the intervention ends. The post-intervention measures will be
compared between active and control groups by means of independent sample t-tests.
Description:
Objective: The primary objective is to determine if REWR in addition to standard mental
healthcare is more effective than standard mental healthcare alone for promoting personal
recovery in a sample of individuals living with schizophrenia spectrum disorders. The
secondary objective is to investigate if REWR in addition to standard mental healthcare is
more effective than standard mental healthcare alone in promoting a. mentalising, b.
self-efficacy, c. clinical recovery in a sample of individuals living with schizophrenia
spectrum disorders.
Hypotheses: The main hypothesis is that people living with a schizophrenia spectrum disorder
who participate in REWR as an add-on to standard mental healthcare, as compared to those that
receive standard mental healthcare alone, will show a greater improvement in personal
recovery, measured by the Questionnaire for the process of recovery (QPR) immediately after
the end of the intervention (approximately 4.5 months post-baseline). Secondary hypotheses
include that those who receive REWR in addition to standard mental healthcare will show a
greater improvement in personal recovery, as well as mentalising, self-efficacy, clinical
recovery and wellbeing immediately after the end of the intervention (approximately 4.5
months post-baseline), as well as six months later (approximately 10.5 months post-baseline).
Ethical considerations: Information about the studies is presented to all potential
participants both verbally and in written form so they can make an informed decision about
their participation before signing the informed consent forms. Research assistants will make
clear to the candidates that participation is voluntary, and that withdrawal can occur at any
time without consequence for treatment possibilities. Decisions regarding participation will
not influence clinical care in any way. At the information meeting and in the informed
consent form it will thus be made clear that the intervention is voluntary and safe, and that
participants at any time can stop their participation in the project and withdraw their
consent without any consequences for the standard treatment they receive. If the participants
wish to withdraw from the experiment during the course, there are three options: 1) They
withdraw from the intervention but not from the study, therefore they will participate in the
data collection at the follow-ups. 2) They withdraw from both the intervention and the study,
but data from the baseline measures can be used in the research project. 3) They withdraw
from both the intervention and the study, and their data will be deleted.
The study will be conducted in agreement with the Declaration of Helsinki. The Regional
ethical committee for the Capital Region has decided that the study is not required to seek
approval under their legislation, which covers human participation in medical trials. We will
adhere to all other ethical standards guiding good practice in research. The study has been
registered with the Danish Data Protection Agency (p-2023-14655), and we will comply with all
regulations regarding data security, and make sure that all technical solutions comply with
GDPR regulations. The study will be registered at clinicaltrials.gov. If any modifications
are made to the data collection or data analyses, these protocol amendments will be reported
to the Danish Data Protection Agency and to clinicaltrials.gov.
The intervention is not expected to have any serious side-effects. This is supported by the
pilot study and similar studies. The social setting can be associated with anxiety and
discomfort, at least initially, as known from previous group start-ups. A mental health care
professional will always be present in the group (the co-conductor, see REWRITALIZE under
Interventions) and this is expected to reduce participants' distress and to regulate
reactions including crisis following the group activity. Supportive sessions are offered by
the co-conductor if needed.
Participant Timeline: Clinical staff will inform potential candidates about the study and
arrange for a meeting with a research clinician. Research clinicians provide information
about the study, confirms the diagnosis with present state examination (PSE) and administers
a SCIP-D for assessment of cognitive impairment.
After informed consent forms have been signed (either at the same session or at a second
session depending on if the participant needs deliberation time), baseline measures will be
assessed. This includes clinician-rated PANSS-6 and GAF-F (see Outcome measures), two tasks
(TASIT and VISPT, see Outcome measures), and a link will be provided for the self-report
questionnaires. Participants may fill out the questionnaires either at home, or with the help
of a research assistant at site using the link. They will also be given the possibility to
fill out the questionnaires on paper at site. If a participant wants to do just half of the
tasks and interviews on the first session and then wants to come back another day to finish
the baseline assessment, this option will be given. The data collection, including
questionnaires, interviews and tasks, takes some time. The participants will be offered help
to fill in the questionnaires and complete the tasks. They will be given the opportunity for
breaks and reflection time in connection with the interviews.
When all baseline data have been collected, randomisation is performed. The creative writing
group will start when 8-10 participants have been allocated to the active condition.
Participants will be followed up immediately after the end of the intervention, corresponding
to approximately 4.5 months after baseline and six months later, approximately 10.5 months
after baseline. At the 4.5 months follow-up, all measures will be collected. At the 10.5
months follow-up, the questionnaire data will be collected. If additional funding is
received, the interview assessments (PANSS-6 and GAF-F) will be conducted also at the 10.5
months follow-up.
Assignment of interventions: After baseline data are obtained, the participants are randomly
allocated to either the control (standard mental healthcare) or active group (REWR + standard
mental healthcare) with a 1:1 allocation using the randomisation module in REDCap (Research
Electronic Data Capture). The randomisation sequence will be generated by a researcher at
Copenhagen Research Centre for Mental Health (CORE), who is not part of the present research
team, and will be entered into RedCap. The randomisation is stratified by sites. Varying
block sizes, unknown to the research team, are used. To ensure concealment, the randomisation
schedule is stored away from the research team and the block sizes are not disclosed. The
allocation of active or control condition is performed by one (unblinded) research assistant,
who informs firstly the participant about the result, secondly the co-conductor at the site
who keeps track of what participants have been allocated to active condition. Participants
randomised to the control group will be set on a waiting list and will be informed that they
will be offered to participate in a creative writing group within one year of the
randomisation.
Sample size and power calculations:The minimum sample size is calculated based on the ability
to detect a minimal but clinically significant difference between the active intervention
group and the control group in the primary personal recovery QPR measure. The minimal
clinically significant difference between the study groups has been estimated to 4 points.
The assumed standard deviation in the study population of 10, based on trials in similar
populations, hence corresponds to an effect size of Cohen's d=0.4. To achieve a statistical
power of 90 % at a significance level of 5 %, a total of 266 participants must be included in
this study to detect a difference; 133 in each group. Based on the needed participants, power
calculations for secondary outcomes were calculated and are shown in table 7. Because of the
relatively high drop-out rate in the pilot study (see appendix 2) and similar studies, we
will plan for a sample size of 150 participants in the active group and 150 participants in
the control group. This should hence allow for at least a 90% power of finding a minimally
clinically significant difference in the primary measure, i.e., the QPR measure of personal
recovery.
Data analyses:The primary outcome measure is personal recovery measured by QPR. To test the
research hypothesis, the differences between the active intervention group and the control
group will be analysed using independent-samples t-test. Effect sizes to judge clinical
relevance will be calculated by Cohen's d. All variables are continous and secondary measures
will be tested by the same means. The significance level is set to 0.05. Data analyses will
be based on the intention-to-treat principle. Data from all participants will be included in
the analysis. In accordance with the intention-to-treat principle, missing data from the
follow-up will be imputed using multiple imputation.
The prerequisite for the use of multiple imputations is that data are missing at random or
completely at random as opposed to non-ignorable nonresponse. This distinction is important
since multiple imputations are based on a statistical estimation of non-existent responses,
and the prerequisites for this estimation must be met for the analyses to be valid.
Significant prognostic characteristics of the non-follow-up participants will thus be
compared with those for whom follow-up data have been collected. Variables where there is a
difference between participants and non-participants will be included as co-variables in the
analyses of differences between active and control group to make these analyses valid. As a
supplementary analysis, we will carry out per-protocol where only cases with follow-up data
are included.
A detailed statistical analysis plan will be prepared before initiating analysis and uploaded
at clinicaltrials.gov.
