Abstract
Introduction
Many people with psychotic disorders experience symptoms of post-traumatic stress disorder (PTSD). In recent years, several trauma-focused therapies (TFTs), including cognitive restructuring (CR), prolonged exposure (PE), and eye movement desensitization and reprocessing (EMDR) have been studied and found to be safe and effective in reducing PTSD symptoms in individuals with psychosis. However, studies were conducted in different countries, with varying inclusion criteria, therapy duration, control groups, and trial outcomes. RE.PROCESS will be the first study to compare the impact of CR, PE, and EMDR with a waiting list control condition within the same context.
Methods and analysis
This is the protocol of a pragmatic, single-blind, multicentre, superiority randomized controlled trial, in which CR, PE, and EMDR are compared to a waiting list control condition for TFT (WL) in a naturalistic treatment setting. Inclusion criteria are as follows: age ≥ 16 years; meeting full DSM-5 diagnostic criteria for PTSD on the Clinician-Administered PTSD Scale for DSM-5 (CAPS-5), with a total CAPS score ≥ 23; and a psychotic disorder in the schizophrenia spectrum confirmed by the Structured Clinical Interview for DSM-5 (SCID-5). Participants (N=200) will be randomly allocated to 16 sessions of one of the TFTs or WL, in addition to receiving treatment as usual (TAU) for psychosis. The primary objective is to compare the effects of CR, PE, and EMDR to WL on researcher-rated severity of PTSD symptoms over time from baseline to 6-month follow-up. Secondary objectives are to examine these effects at the separate time-points (i.e., mid-treatment, post-treatment, and at 6-month follow-up) and to test the effects for clinician-rated presence of PTSD diagnosis, and self-rated severity of (complex) PTSD symptoms.
Discussion
This is the first RCT to directly compare the effects of CR, PE, and EMDR within the same context to TAU on PTSD symptoms in individuals with psychosis and PTSD. Secondary effects on clinical and functional outcomes will be investigated both directly after therapy and long term.
Trial registration
ISRCTN ISRCTN56150327. Registered 18 June 2019.
Similar content being viewed by others
Introduction
Exposure to traumatic events is highly prevalent in individuals with psychotic disorders [1]. Experiencing childhood trauma increases the likelihood of developing psychotic symptoms [2, 3] and is associated with persistence of psychosis [4]. Individuals with severe mental illnesses are also at increased risk of revictimization [5, 6]. In individuals with psychosis, post-traumatic stress disorder (PTSD) is a common comorbidity (12.4-16.0%) [7, 8]. PTSD and psychosis symptoms tend to fuel each other, with symptoms interacting and overlapping [9,10,11,12].
Several studies have shown trauma-focused therapy (TFT) to be feasible and effective in reducing PTSD symptoms in individuals with psychosis, with more equivocal findings regarding their effects on psychotic symptoms [13]. Three TFTs targeting PTSD have been studied in psychosis with rigorous designs: cognitive restructuring (CR), prolonged exposure (PE), and eye movement desensitization and reprocessing therapy (EMDR). The 16-session CR intervention [14] was found to reduce PTSD symptoms in severe mental illnesses in two separate randomized controlled trials (RCT) in the USA [15, 16], in which a minority of participants had a psychosis diagnosis (15% and 33% respectively). A UK study with participants with psychosis found that while CR did significantly reduce PTSD symptoms, there were also significant reductions for the TAU group [17].
Pilot studies have reported positive effects of PE [18, 19] and EMDR [19, 20] on PTSD symptoms in psychosis samples. A Dutch RCT confirmed these results, comparing the effects of eight sessions of either PE or EMDR to waiting list for TFT (WL) [21, 22]. Both PE and EMDR were associated with a significant decrease of PTSD symptoms, and post-treatment effects were generally maintained at 12-month follow-up [23]. However, since most participants experienced multiple severe childhood traumatic events, the programme length of eight sessions was found to be too brief to address all the intrusive memories for many participants in the study.
Therefore, more treatment sessions could enhance the effects of these interventions, as observed in previous TFT studies [24, 25]. Providing additional sessions would also allow for targeting psychosis-related traumatic events when PTSD symptoms have resolved sufficiently. Psychotic experiences can be linked to traumatic events, often reflected in the content or the appraisal of the psychotic experiences (for example: hearing the voice of a perpetrator or interpreting shadowy figures as a replay of past persecution) suggesting that trauma processing can be beneficial. By targeting psychosis-related traumatic events, we aim to address a broader concept of post-traumatic reactions that includes psychosis [26].
Although CR, PE, and EMDR have similarities, they are based on different theoretical backgrounds and employ different therapeutic techniques [27]. Moreover, the context in which these therapies were tested differed greatly. The studies were executed in different countries, adopted slightly different inclusion and exclusion criteria, focused on targeting psychosis outcomes to varying degrees, and tested different dosages of therapy. Also, expertise of therapists may have differed and factors such as TAU for psychosis or PTSD differ amongst countries, influencing study results. Comparing all three TFTs to WL within the same context will provide more insight into their relative effects, working mechanisms, and acceptability.
Aims and objectives
This trial aims to test the effects of CR, PE, and EMDR in a sample of participants with psychosis and PTSD. The primary objective is to compare the effects of CR, PE, and EMDR to WL on researcher-rated severity of PTSD symptoms (CAPS-5 total score) over time from baseline to 6-month follow-up. Secondary objectives are to examine these effects for researcher-rated severity of PTSD symptoms at the separate time-points (i.e. mid-treatment, post-treatment, and at 6-month follow-up) and to test the effects (over time and at each time-point) for clinician-rated presence of PTSD diagnosis, and self-rated severity of (complex) PTSD symptoms.
Methods and design
Trial design
This study is a pragmatic, single-blind multicentre superiority randomized controlled trial with four arms: CR, PE, EMDR, and WL. Therapy in all three active arms will be delivered over 16 sessions by the same group of trained therapists working in routine mental health services to eliminate therapist effects and align as much as possible with the routine clinical reality. All groups receive TAU for psychosis and will be assessed at baseline (T0), mid-treatment (T1) at 7 weeks, post-treatment (T2) at 3 months, and at 6-month follow-up (T3). Participants in the WL condition receive therapy of choice after T3. The CR, PE, and EMDR conditions will also be assessed at 12-month (T4) and 24-month follow-up (T5). Up to the 6-month assessment, social functioning, adversities, and revictimization outcomes will be monitored weekly using smartphone questionnaires to enhance the ecological validity of these measurements. The Consolidated Standards of Reporting Trials (CONSORT) diagram depicting the eligibility and assessment stages is presented in Fig. 1.
Flowchart of the inclusion, allocation, assessments, and therapy. Note: T1 = mid-treatment, T2 = post-treatment, T3 = 6-month follow-up, T4 = 12-month follow-up, T5 = 24-month follow-up
Additional explorations
We plan on the following explorations: (A) examine the effects of the treatments on disruption of social functioning by PTSD symptoms, post-traumatic cognitions, dissociation, depression symptoms, paranoid ideation, presence and impact of auditory hallucinations, sexual functioning, social functioning, personal recovery, adversities, experienced resilience, and revictimization over time and at each time-point; (B) examine long-term effects of the treatments (12- and 24-month follow-up) on all variables; (C) determine the cost-effectiveness and cost-utility of the treatments compared to each other and to WL [28]; (D) test how participants’ expectancy of therapy effects, their perception of the therapist, therapeutic alliance, and treatment effects interact and change over time [29]; (E) test baseline predictors of treatment outcome given that experimental studies on predictors of treatment outcome are scarce [30, 31]; and (F) gain insights into the experience of participants receiving TFT, through qualitative interviews.
Study setting
Participants are recruited from psychosis outpatient services of multiple mental healthcare organizations in the Netherlands. A list of study sites can be obtained at the ISRCTN registry. All participants receive TAU for psychosis, which consists of care in multidisciplinary assertive outreach teams and usually includes antipsychotic medication, psychological therapies, and supportive counseling by psychologists, caseworkers, nurses, and psychiatrists.
Eligibility criteria
Inclusion criteria for participants are as follows: (A) aged ≥ 16 years; (B) a psychotic disorder in the schizophrenia spectrum, confirmed by the Structured Clinical Interview for DSM-5 (SCID-5); and (C) meeting DSM-5 symptom criteria for PTSD based on the Clinician-Administered PTSD Scale for DSM-5 (CAPS-5) with a total score ≥23.
Exclusion criteria are as follows: (A) changes in antipsychotic or antidepressant medication within 4 weeks before the eligibility assessment (to control for medication effects); (B) insufficient mastery of the Dutch language; (C) severe intellectual impairment, defined as an estimated IQ of 70 or less; and (D) not willing or able to learn to use a smartphone for weekly assessments.
Sample size
Sample size for longitudinal intention-to-treat (ITT) analyses with linear mixed models (LMM) was calculated [32] and based on data from previous RCTs [21, 33]. With alpha = 0.05, beta = 0.2, rho = 0.45, and 3 repeated follow-up assessments, and an additional 20% to compensate for dropout, this study needs 50 participants in each arm to detect at least medium effects of 0.5 against waiting list condition. The aim is therefore to randomize 200 participants.
Interventions
In each therapy arm, participants receive a maximum of 16 therapy sessions, delivered as two 75-min sessions per week. Baseline assessment data of traumatic experiences, PTSD, and psychosis are used to support the development of a case formulation and treatment plan. Treatment and recovery goals are set in a start-session before the beginning of therapy, with progress evaluated and future plans agreed on in an end-session after finishing therapy. All therapies are based on a collaborative therapeutic relationship and entail recognition of the trauma and its consequences, attention, and hope. Participants monitor their post-traumatic stress and psychosis symptoms weekly, and review these with their therapist.
Cognitive restructuring (CR) for PTSD
CR for PTSD supports people to learn how to manage or modify distressing thoughts. CR for PTDS is based on the cognitive model of PTSD which argues that PTSD symptoms develop and are maintained by unhelpful and inaccurate thoughts and beliefs related to traumatic events, which then manifest in a more global set of distressing and unhealthy beliefs pertaining to the self, others, and the world. The primary focus is on thoughts associated with PTSD symptoms, although thoughts related to any situation can be targeted (including those linked to psychosis), especially in earlier sessions, as the therapist teaches the CR skill to the client so they can move toward mastery. The first 3 sessions of CR teach an anxiety-management skill (breathing retraining) for managing arousal and provide information about PTSD, followed by 13 sessions of CR. Participants learn CR as a simplified, step-by-step self-management skill to deal with any negative feelings and situations. This involves identifying distressing thoughts, evaluating them, and then either modifying them by developing alternatives or making a detailed, systematic action plan to manage distressing them. In CR for PTSD, participants initially learn to cope with any distressing feelings and as their skills develop, shift to trauma-related thoughts and beliefs underlying PTSD symptoms. Home assignments to practice breathing retraining and CR skills are collaboratively set in each session [14].
Prolonged exposure (PE)
PE is a psychotherapy that aims to reduce PTSD symptom severity by systematically confronting the patient with safe but anxiety-provoking reminders of the trauma, including trauma-related memories (imaginal exposure, including homework of listening to audio recordings) and real-life trauma-related stimuli (in vivo exposure). PE aims to activate the trauma-related fear memory network and change trauma-related cognitions. In the first session, the therapist and the participant develop a case formulation that contains the most important intrusive trauma memories (based on intensity and frequency scores) and the most important avoidance behaviours to which patients are then exposed in the following sessions. PE therapy will be delivered using the Dutch protocol of van Minnen and Arntz [34], based on the protocol of Foa, Hembree, and Rothbaum [35].
EMDR therapy
EMDR is a psychotherapy that aims to process traumatic memories by simultaneously retrieving the traumatic memory and taxing the working memory. Eye movements will be applied as the default working memory taxation stimulus, with added memory taxation (tapping, spelling words, steps) when eye movements are not sufficient to tax a patient’s working memory [36,37,38] or not possible due to COVID-19 restrictions. In the first sessions, the therapist and the participant develop a case formulation that contains the most important traumatic experiences, a hierarchy of the most relevant intrusive trauma memories based on their subjective units of distress (SUD), with the memories with the highest SUD being targeted first. EMDR will be delivered according to the standard 8-phase protocol by Shapiro [39], using the Dutch translation [40].
Therapists
The therapists are trained in all three TFTs (PE, EMDR, and CR), with competence assessed before seeing trial cases. Therapists are frontline clinicians working within the participating institutions, delivering the trial therapies as part of routine care. All therapists are at least Masters level psychologists, with varying experience, training, and expertise in working with psychosis and PTSD. Case formulations and treatment plans are reviewed by an expert supervisor (AH, AM, CR, AJ, TS, PB, BV, TL). Therapists receive monthly group supervision and online on-demand supervision after each session. Therapists provide a fidelity checklist of each session to the supervisor, which the supervisor reviews and provides feedback on. In addition, in line with the CR for PTSD protocol, sessions were rated for competence at regular intervals by supervisors.
Treatment fidelity
Therapists provide a fidelity checklist of each session to the supervisor. All sessions are videotaped and reviewed in monthly supervision. A random selection of sessions will be rated for treatment fidelity for each TFT. After each session, the therapists fill in a fidelity checklist which is reviewed by a supervisor.
Procedures
Recruitment, baseline assessment, and randomization
Trial therapists and their teams identify participants, screen for initial eligibility using patient records and routine outcome measures, and conduct Module B and C of the SCID-5 on psychotic symptoms to check whether a psychotic disorder is present [41], and then refer them to the study coordinator (SB). The participant receives both oral and written information about the study from the study coordinator or a research assistant and has at least 1-week time to decide upon participation. The participant is asked to sign informed consent and is assessed for inclusion criteria. After the baseline assessment, the participant is randomized to one of the 4 conditions. Randomization is stratified by trial therapist and conducted by an independent researcher via a randomization programme (http://www.randomizer.org). The allocation sequence is saved in a protected folder to which the research team has no access. The independent researcher informs the therapist of the allocation who in turn informs the participant.
Assessments
A researcher (SB) or research assistant from the VU/Parnassia, who is blind to the allocation of the participant, carries out the (planning of) the assessments (Fig. 2). They are supervised in administering the CAPS-5 interview by a clinical psychologist with extensive experience in administering the CAPS-5 (DB). Research assistants are trained to competence on the interview outcome measures (CAPS-5 and PSYRATS) before conducting any assessments. Research assistants write a clinical report on the CAPS-5 and PSYRATS of every assessment which is reviewed by SB to insure inter-rater reliability and minimize rater drift. In case of incidental unblinding, a different assessor performs the rest of the assessment. Participants are compensated for expenses (e.g. travel costs) with 20 Euro per assessment.
Schedule of enrolment, interventions, and assessments. Structured Clinical Interview for DSM-5 (SCID-5) [41] Module B and C on psychotic symptoms. Clinician Administered PTSD scale for DSM-5 (CAPS-5) [42]. Brief Version of the Alcohol, Smoking and Substance Involvement Screening Test (ASSIST) [43]. Trauma and Life Events (TALE) [44]. Psychosis Symptoms Rating Scale (PSYRATS) [45, 46]. Enriched Social Support Instrument (ESSI) [47]. The PTSD Checklist for the DSM-5 (PCL-5) [48, 49]. International Trauma Questionnaire (ITQ) [50]. Brief Version of the Posttraumatic Cognitions Inventory (PTCI-9) [51]. Trait State Dissociation Questionnaire – short version (TSDQ-s) [52]. Beck Depression Inventory II (BDI-II) [53]. Revised version of the Green et al Paranoid Thoughts Scale (R-GPTS) [54]. Auditory Hallucination Rating Scale (AHRS) [45, 46]. Voice Impact Scale (VIS). Arizona Sexual Experience Scale (ASEX) [55]. Sexual Autonomy Scale (SAS) [56]. Questionnaire about the Process of Recovery (QPR) [57]. Brief Resilience Scale (BRS) [58]. Treatment Inventory of Costs in Patients with psychiatric disorders (TIC-P) [59, 60]. EuroQol 5-dimensions (EQ-5D) [61]. Working Alliance Inventory – Short Form Revised (WAI-SR) [62]. Counselor Rating Form – Short (CRF-S) [63]
All weekly assessments are conducted using an online questionnaire application (RoQua). Participants receive a text message with a link through which they can access the assessment.
The therapist will provide the hardcopy questionnaires for the participant’s perception of the therapy and the therapeutic alliance during the introductory session, sessions 3, 8, and 16. To ensure anonymity/confidentiality, participants are asked to return the completed questionnaires in a sealed envelope and are informed that the therapist will not be able to review their answers.
A subgroup of approximately 15 participants [64] is invited to partake in qualitative interviews to assess their experience of the TFT 2 to 6 weeks after the post-treatment assessment. Purposive sampling will be applied to include participants from all treatment arms and treatment drop-outs.
Outcome measures
Outcome measures are shown in Fig. 2.
Demographics and baseline assessments
Demographic characteristics include age, sex, gender, country of birth (including that of parents), education, employment, living condition, relationship status, duration of PTSD, duration of psychosis, and duration of contact with mental healthcare. Substance use is assessed with the first two questions of the Alcohol, Smoking and Substance Involvement Screening Test (ASSIST) [43]. Social support is measured with the Enriched Social Support Instrument (ESSI), which is a 5-item measure of social support with good validity and reliability [47]. The Trauma and Life Event Checklist (TALE) is a 21-item checklist for traumatic experiences and life events in people with psychosis [44].
PTSD symptoms
The Dutch version of the Clinician-Administered PTSD Scale for DSM-5 (CAPS-5) is used to assess the severity of PTSD symptoms, the presence of PTSD diagnosis, and the influence of PTSD symptoms on social functioning. The CAPS is anchored to all reported criterion A events, as identified by the TALE. These can include traumatic events associated with the psychosis symptoms (e.g. a voice threatening to kill the participant). The CAPS-5 assesses the intensity and frequency of all PTSD symptoms and yields a continuous severity score. Symptoms with a severity score ≥2 are considered clinically significant. The CAPS-5 is the gold standard diagnostic interview for PTSD [42, 65]. The DSM-5 version has recently been validated and has good psychometric properties [66], also in Dutch translation [67].
The PTSD Checklist for the DSM-5 (PCL-5) is a 20-item self-report questionnaire on assessing all DSM-5 PTSD symptoms. The DSM-5 version demonstrated strong validity and reliability [48, 49].
The International Trauma Questionnaire (ITQ) is an 18-item self-report questionnaire that assesses the presence of complex PTSD as defined in the ICD-11 and the severity of these symptoms, including two items on how PTSD symptoms influence social functioning [68]. Results on psychometrics were encouraging [50].
The Brief version of the Posttraumatic Cognitions Inventory (PTCI-9) measures trauma-related cognitive distortions about the self, the world and self-blame. This 9-item version is based on the original PTCI [51] and was found to have strong psychometrics [69].
The Trait State Dissociation Questionnaire – short version (TSDQ-s) is a 15-item self-report questionnaire and consists of items from existing dissociation measures (including the Dissociative Experiences Scale [70] and the Peritraumatic Dissociation Scale [71]) and new items measuring aspects of dissociation which were not sufficiently represented in existing scales. The TSDQ-s has been shown to be psychometrically robust [52].
Other psychiatric symptomatology
The Beck Depression Inventory II (BDI-II) is a widely used 21-item self-report questionnaire for depression [53]. It provides a continuous score for the severity of depression symptoms and has excellent psychometric properties [72, 73].
The Revised Green et al. Paranoid Thought Scales (R-GPTS) is an 18-item self-report questionnaire that assesses ideas of persecution and social reference and was found to have excellent psychometric properties [54].
The psychotic symptoms rating scales (PSYRATS) is an 18-item clinical interview that assesses delusions and auditory hallucinations. The PSYRATS subscales have excellent inter-rater reliability and strong validity [45, 46]. We use a slightly augmented version which also captures type and content of delusions and hallucinations. At follow-up, assessments only the frequency, duration, and disruption items on auditory verbal hallucinations will be conducted.
The Voice Impact Scale (VIS) is a 24-item self-report questionnaire that assesses the impact of hearing voices. A publication concerning the psychometrics is pending.
Sexual functioning, disruption of social functioning, social functioning, and personal recovery
The 5-item Arizona Sexual Experience Scale (ASEX) is a 5-item self-report questionnaire that assesses sexual dysfunction. The ASEX has high validity and reliability, regardless of availability of a sexual partner and sexual orientation [55].
The Sexual Autonomy Scale (SAS) consists of three self-report items measuring the extent to which individuals feel their sexual behaviours are self-determined with good reliability [56].
Social functioning is assessed with two items adapted from the Time Use Survey on the number of minutes spend with others and spend on pleasant activities [74, 75].
The Questionnaire about the Process of Recovery (QPR) assesses personal recovery in 15 self-reported items and has good psychometric properties [57].
Adversities, resilience and revictimization
Adversities (e.g. self-harm or hospitalization) are measured using the 7-item TTIP Adverse Events Questionnaire (TAEQ) [76, 77]. Revictimization is assessed using eight interpersonal victimization items from the TALE [44]. Resilience is measured using the Brief Resilience Scale (BRS), a 6-item self-report questionnaire of resilience that has good psychometric properties [58].
Cost-effectiveness and cost-utility
The Treatment Inventory of Costs in Patients with psychiatric disorders (TiC-P) short version is an interview consisting of 17 items measuring the economic costs and benefits of therapy [59, 60]. It asks individuals for the number of contacts with healthcare providers and for productivity losses. The EuroQol (EQ-5D) is the World Health Organization measurement for health outcome that can be expressed in utilities. Utilities can be combined with cost-effectiveness data into quality-adjusted life years (QALYs) [61, 78].
Therapy-related measures
The Counselor Rating Form – Short (CRF-S) is a 12-item self-report questionnaire that assesses counselor’s amiability, expertness, and trustworthiness as perceived by the participant. The CRF-S has been shown to be psychometrically robust [63].
The Working Alliance Inventory – Short Form Revised (WAI-SR) is a 12-item self-report questionnaire that assesses the strength of the therapeutic alliance as perceived by the participant and has good psychometric properties [62].
Harm expectancies (e.g. being afraid to “lose control” during a session), burden expectancies, and credibility of the therapy as perceived by the participant are assessed with a 9-item questionnaire developed for the Treating Trauma in Psychosis trial [76].
Qualitative study
Experience of the TFT will be assessed with a semi-structured interview guided by a topic list constructed by the research team.
Therapy procedures
In PE and EMDR, when PCL-5 scores for sections B (reliving) and C (avoidance) are both 0 for at least two consecutive sessions and the intrusive trauma memories hierarchy contains no PTSD-related trauma memories with a SUD > 0, therapists can target psychosis-related traumatic memories. PE and EMDR therapies can be completed early after a shared decision-making process between participant and therapist when PTSD is in remission (using criteria above) and no psychosis-related trauma memories or imagery have a SUD > 0. In CR, participants are encouraged to complete all 16 sessions even if PTSD remits prior to this time, to support generalization of learning and planning for the future.
The participant and treatment team are asked not to start any other form of TFT, to refrain from CBT and changes in medications until the 6-month follow-up. However, in the case of an adverse event or an increase in (psychosis) symptoms that demands intervention, antipsychotics, sedatives, or CBT may be increased or provided without consequences for therapy and/or study participation.
Withdrawal of individual participants
Participants can leave the study at any time for any reason if they wish to do so without any consequences. The investigators can decide to withdraw a participant from the study for urgent medical reasons. When a participant withdraws from treatment and is still willing to partake in assessments, follow-up assessments will be conducted. There will be no replacement of individual participants after withdrawal.
Analysis
The primary and secondary outcomes will all be analysed on an intention-to-treat basis. We will perform completers (sensitivity) analyses to test the robustness of the outcomes. Both primary and secondary continuous outcomes will be analysed with linear mixed models (LMM) with baseline values included as covariates. Dichotomous primary and secondary outcomes will be analysed with Generalized Estimating Equations (GEE). The main outcome is the effect over time including all data points between baseline and 6-month follow-up. The effects at the different time-points will also be computed using interaction terms.
To test whether the effects of CR, PE, and EMDR on the primary and secondary outcomes endure in the long term, we will test the changes from 6-month follow-up to the 12-month and 24-month follow-up respectively. These within-group changes will be analysed with paired samples t-tests (continuous outcomes) and McNemar’s tests (dichotomous outcomes). Although not powered, we will also do an exploratory analysis for differences between CR, PE, and EMDR at these time-points with independent samples t-tests and chi-square tests for independence. The predictive value of the potential predictor variables will be tested with multiple linear regression analysis.
If a therapy is found to be effective compared to WL at 6 months, cost-effectiveness and cost-utility analyses will be performed in the same way as in the TTIP trial [28]. The incremental cost-effectiveness ratios (ICERs) are considered a single-point estimate of an underlying continuum. Acceptability curves are produced with bootstrap simulations and confidence intervals. The outcome will be costs in Euro’s per QALY and the costs in Euros per day without PTSD gained. If none of the therapies are effective, which is not expected, a cost-minimization calculation will be performed. For all TFTs, interaction between the participants’ perception of the therapy, view of the therapist, strength of the therapeutic alliance in different points of the therapy, and treatment effects will be studied using regression analysis and Spearman’s rho. Predictive value of the baseline variables will be investigated using regression analyses. Thematic analysis will be used to analyse themes in the interviews with regard to how participants have experienced the TFT [79, 80] consisting of data familiarization, initial coding, searching for themes, reviewing themes, defining and naming themes, and finally producing the report. Analysis will be performed in parallel with conducting the interviews.
Monitoring
The study was classified as imposing negligible added risk through research procedures on participants by the medical ethics committee of the VU University Medical Centre. Therefore, a trial management group was established in place of a data monitoring committee. No interim analyses will be performed. Serious adverse events (SAEs) are monitored by therapists and supervisors and will be reported to the medical ethics committee.
Ethics
This trial was set up in accordance with the SPIRIT checklist (Standard Protocol Items for Randomized Trials; Additional file 2) [81, 82]. The study protocol was approved by the Medical Ethics Committee of the VU University Medical Centre (METC number: 2019.046/ NL66431.029.19) and the trial was published in an online registry (ISRCTN56150327). METC and registry are notified of any protocol changes. The study is conducted according to the principles of the Declaration of Helsinki and in accordance with the Dutch Medical Research Involving Human Subjects Act (WMO). SAEs and a long-term increase of adverse events as a result of the interventions are not expected, since previous research has shown that treatment significantly reduces the odds of adverse events [77].
Data management, data security, and quality control
The handling of personal data complies with the European General Data Protection Regulation (GDPR). Data are handled confidentially and data files are coded and separated from name, date of birth, and address data. Only the principal investigators have the key to this code and access to the source data. The CASTOR trial management software is used for this trial. Raw data will be kept for 5 years according to Dutch guidelines. A data management plan can be found at the Department of Psychosis research and Innovation, Parnassia Psychiatric Institute, The Hague, The Netherlands.
RoQua is hosted in data centres of the University of Groningen and operates in compliance with the NEN-ISO/IEC 27001 standard and the GDPR.
Dissemination
The results of this study will be published in peer-reviewed journals and presented at national and international scientific conferences. Our international project team has the experience and network to ensure effective dissemination of the results to the national and international scientific community and into clinical practice. The sponsor will have no influence on the publication of the results.
Discussion
The RE.PROCESS trial will be the first study to directly compare the effects of three types of TFT (CR, PE and EMDR) to TAU on PTSD symptoms in individuals with psychosis and PTSD. It is, in part, a replication study, aiming to validate the findings of previous RCTs on the effectiveness of PE, EMDR, and CR in people with psychosis [15,16,17, 21]. By targeting psychosis-related traumatic events in therapy when PTSD symptoms have sufficiently resolved, this study aims to address a broader concept of post-traumatic reactions that include psychosis. Secondary effects on clinical and functional outcomes, as well as cost-effectiveness, will be investigated providing a comprehensive investigation of the potential benefits of these therapies both directly after therapy and long term.
This study also aims to identify possibilities and challenges in implementing these therapies in routine clinical practice, although this is not a full implementation trial [83]. Additional benefits of the trial are that the therapists will be trained in all three TFTs and will deliver therapy as part of their clinical role in routine care. They will therefore be well placed to disseminate the TFTs, if found to be effective, in their services following completion of the trial.
Trial status
Protocol version number and date: 1.13, 27 September 2022
Date of first enrolment: June 24, 2019 (current sample size: 103)
Date recruitment is expected to be completed: December 31, 2023
Expected date of study completion: December 31, 2025
Recruitment status: Recruiting
Availability of data and materials
The investigators will permit trial-related monitoring and audits by providing the Sponsor and METC direct access to source data and other documents as required.
An anonymized version of the main outcome data and the corresponding statistical code will be available from the trial team on reasonable request after publication of the main results paper.
Abbreviations
- ASEX:
-
Arizona Sexual Experience Scale
- ASSIST:
-
Alcohol, Smoking and Substance Involvement Screening Test
- BDI-II:
-
Beck Depression Inventory II
- BRS:
-
Brief Resilience Scale
- CAPS-5:
-
Clinician-Administered PTSD Scale for DSM-5
- CBT:
-
Cognitive behaviour therapy
- CR:
-
Cognitive restructuring
- CRF-s:
-
Counselor Rating Form – Short
- DSM-5:
-
Diagnostic and Statistical Manual of Mental Disorders-5th Edition
- EMDR:
-
Eye Movement Desensitization and Reprocessing
- EQ-5d:
-
EuroQol
- ESSI:
-
Enriched Social Support Instrument
- GDPR:
-
European General Data Protection Regulation
- GEE:
-
Generalized Estimating Equations
- ICERs:
-
Incremental cost-effectiveness ratios
- ITQ:
-
International Trauma Questionnaire
- ITT:
-
Intention-to-treat
- LMM:
-
Linear mixed models
- METC:
-
Medical Ethics Committee
- PCL-5:
-
PTSD Checklist for DSM-5
- PE:
-
Prolonged exposure
- PSYRATS:
-
Psychosis Symptom Rating Scales
- PTCI:
-
Posttraumatic Cognitions Inventory
- PTSD:
-
Post-traumatic stress disorder
- QALYs:
-
Quality-adjusted life years
- QPR:
-
Questionnaire about the Process of Recovery
- RCT:
-
Randomized controlled trial
- R-GPTS:
-
Revised Green et al. Paranoid Thought Scales
- SAE:
-
Serious adverse event
- SAS:
-
Sexual Autonomy Scale
- SCID-5:
-
Structured Clinical Interview for DSM-5
- SPIRIT:
-
Standard Protocol Items for Randomized Trials
- SUD:
-
Subjective Units of Distress
- TAEQ TTIP:
-
Adverse Events Questionnaire
- TALE:
-
Trauma And Life Events Checklist
- TAU:
-
Treatment as usual
- TDSQ-s:
-
Trait State Dissociation Questionnaire – short version
- TFT:
-
Trauma-focused treatment
- TiC-P:
-
Treatment Inventory of Costs in Patients with psychiatric disorders
- VIS:
-
Voice Impact Scale
- VU:
-
Vrije Universiteit Amsterdam
- WAI-SR:
-
Working Alliance Inventory – Short Form Revised
- WL:
-
Waiting list control group
- WMO:
-
Dutch Medical Research Involving Human Subjects Act
References
Matheson SL, Shepherd AM, Pinchbeck RM, Laurens KR, Carr VJ. Childhood adversity in schizophrenia: a systematic meta-analysis. Psychol Med. 2013;43(2):225–38.
Varese F, Smeets F, Drukker M, Lieverse R, Lataster T, Viechtbauer W, et al. Childhood adversities increase the risk of psychosis: a meta-analysis of patient-control, prospective- and cross-sectional cohort studies. Schizophr Bull. 2012;38(4):661–71.
Bjorkenstam E, Burstrom B, Vinnerljung B, Kosidou K. Childhood adversity and psychiatric disorder in young adulthood: an analysis of 107,704 Swedes. J Psychiatr Res. 2016;77:67–75.
Trotta A, Murray RM, Fisher HL. The impact of childhood adversity on the persistence of psychotic symptoms: a systematic review and meta-analysis. Psychol Med. 2015;45(12):2481–98.
Maniglio R. Significance, nature, and direction of the association between child sexual abuse and conduct disorder: a systematic review. Trauma Violence Abuse. 2015;16(3):241–57.
Kamperman AM, Henrichs J, Bogaerts S, Lesaffre EM, Wierdsma AI, Ghauharali RR, et al. Criminal victimisation in people with severe mental illness: a multi-site prevalence and incidence survey in the Netherlands. PLoS One. 2014;9(3):e91029.
Achim AM, Maziade M, Raymond E, Olivier D, Merette C, Roy MA. How prevalent are anxiety disorders in schizophrenia? A meta-analysis and critical review on a significant association. Schizophr Bull. 2011;37(4):811–21.
de Bont PA, van den Berg DP, van der Vleugel BM, de Roos C, de Jongh A, van der Gaag M, et al. Predictive validity of the Trauma Screening Questionnaire in detecting post-traumatic stress disorder in patients with psychotic disorders. Br J Psychiatry. 2015;206(5):408–16.
Mueser KT, Rosenberg SD, Goodman LA, Trumbetta SL. Trauma PTSD and the course of severe mental illness: an interactive model. Schizophr Res. 2002;53:123–43.
Alsawy S, Wood L, Taylor PJ, Morrison AP. Psychotic experiences and PTSD: exploring associations in a population survey. Psychol Med. 2015;45(13):2849–59.
Hamner MB, Frueh BC, Ulmer HG. Psychotic features in chronic posttraumatic stress disorder and schizophrenia: comparative severity. J Nerv Ment Dis. 2000;188(4):217–21.
OConghaile A, DeLisi LE. Distinguishing schizophrenia from posttraumatic stress disorder with psychosis. Curr Opin Psychiatry. 2015;28(3):249–55.
Brand RM, McEnery C, Rossell S, Bendall S, Thomas N. Do trauma-focussed psychological interventions have an effect on psychotic symptoms? A systematic review and meta-analysis. Schizophr Res. 2018;195:13–22.
Mueser KT, Rosenberg SD, Jankowski MK, Hamblen JL, Monica D. A cognitive-behavioral treatment program for posttraumatic stress disorder in persons with severe mental illness. Am J Psychiatr Rehabil. 2004;7:107–46.
Mueser KT, Rosenberg SD, Xie H, Jankowski MK, Bolton EE, Lu W, et al. A randomized controlled trial of cognitive-behavioral treatment for posttraumatic stress disorder in severe mental illness. J Consult Clin Psychol. 2008;76(2):259–71.
Mueser KT, Gottlieb JD, Xie H, Lu W, Yanos PT, Rosenberg SD, et al. Evaluation of cognitive restructuring for post-traumatic stress disorder in people with severe mental illness. Br J Psychiatry. 2015;206(6):501–8.
Steel C, Hardy A, Smith B, Wykes T, Rose S, Enright S, et al. Cognitive-behaviour therapy for post-traumatic stress in schizophrenia. A randomized controlled trial. Psychol Med. 2017;47(1):43–51.
Frueh BC, Grubaugh AL, Cusack KJ, Kimble MO, Elhai JD, Knapp RG. Exposure-based cognitive-behavioral treatment of PTSD in adults with schizophrenia or schizoaffective disorder: a pilot study. J Anxiety Disord. 2009;23(5):665–75.
de Bont PA, van Minnen A, de Jongh A. Treating PTSD in patients with psychosis: a within-group controlled feasibility study examining the efficacy and safety of evidence-based PE and EMDR protocols. Behav Ther. 2013;44(4):717–30.
van den Berg DP, van der Gaag M. Treating trauma in psychosis with EMDR: a pilot study. J Behav Ther Exp Psychiatry. 2012;43(1):664–71.
van den Berg DP, de Bont PA, van der Vleugel BM, de Roos C, de Jongh A, Van Minnen A, et al. Prolonged exposure vs eye movement desensitization and reprocessing vs waiting list for posttraumatic stress disorder in patients with a psychotic disorder: a randomized clinical trial. JAMA Psychiatry. 2015;72(3):259–67.
de Bont PA, van den Berg DP, van der Vleugel BM, de Roos C, de Jongh A, van der Gaag M, et al. Prolonged exposure and EMDR for PTSD v. a PTSD waiting-list condition: effects on symptoms of psychosis, depression and social functioning in patients with chronic psychotic disorders. Psychol Med. 2016;46(11):2411–21.
van den Berg D, de Bont P, van der Vleugel BM, de Roos C, de Jongh A, van Minnen A, et al. Long-term outcomes of trauma-focused treatment in psychosis. Br J Psychiatry. 2018;212(3):180–2.
Foa EB, Hembree EA, Cahill SP, Rauch SA, Riggs DS, Feeny NC, et al. Randomized trial of prolonged exposure for posttraumatic stress disorder with and without cognitive restructuring: outcome at academic and community clinics. J Consult Clin Psychol. 2005;73(5):953–64.
van den Berg DPG, van der Vleugel BM, de Bont PAJM, Staring ABP, Kraan T, Ising H, et al. Predicting trauma-focused treatment outcome in psychosis. Schizophr Res. 2016;176(2-3):239–44.
Hardy A. Pathways from trauma to psychotic experiences: a theoretically informed model of posttraumatic stress in psychosis. Front Psychol. 2017;8:697.
Schnyder U, Ehlers A, Elbert T, Foa EB, Gersons BP, Resick PA, et al. Psychotherapies for PTSD: what do they have in common? Eur J Psychotraumatol. 2015;6:28186.
de Bont PAJM, van der Vleugel BM, van den Berg DPG, de Roos C, Lokkerbol J, Smit F, et al. Health-economic benefits of treating trauma in psychosis. Eur J Psychotraumatol. 2019;10(1):1565032.
Waller G, Evans J, Stringer H. The therapeutic alliance in the early part of cognitive-behavioral therapy for the eating disorders. Int J Eat Disord. 2012;45(1):63–9.
Lecomte T, Spidel A, Leclerc C, MacEwan GW, Greaves C, Bentall RP. Predictors and profiles of treatment non-adherence and engagement in services problems in early psychosis. Schizophr Res. 2008;102(1-3):295–302.
Hardy A, O’Driscoll C, Steel C, van der Gaag M, van den Berg D. A network analysis of post-traumatic stress and psychosis symptoms. Psychol Med. 2020;51(14):1–8.
Liu G, Liang KY. Sample size calculations for studies with correlated observations. Biometrics. 1997;53(3):937–47.
Seow LSE, Ong C, Mahesh MV, Sagayadevan V, Shafie S, Chong SA, et al. A systematic review on comorbid post-traumatic stress disorder in schizophrenia. Schizophr Res. 2016;176(2-3):441–51.
Van Minnen A, Arntz A. Protocollaire behandeling van patiënten met een posttraumatische stressstoornis (PTSS). Imaginaire exposure en exposure in vivo. In: Keijsers G, Van Minnen A, Verbraak M, editors. Protocollaire behandelingen voor volwassenen met psychische klachten, vol. 1. Amsterdam: Boom; 2017. p. 311–69.
Foa EB, Hembree EA, Rothbaum BO. Prolonged exposure therapy for PTSD. 1st ed. Oxford: Oxford University Press; 2007.
van Veen SC, van Schie K, Wijngaards-de Meij LD, Littel M, Engelhard IM, van den Hout MA. Speed matters: relationship between speed of eye movements and modification of aversive autobiographical memories. Front Psychiatry. 2015;6:45.
van den Hout MA, Engelhard IM. How does EMDR work? J Exp Psychopathol. 2012;3(5):724–38.
Matthijsen SJMA, Brouwers T, van Roozendaal C, Vuister T, de Jongh A. The effect of EMDR versus EMDR 2.0 on emotionality and vividness of aversive memories in a non-clinical sample. Eur J Psychotraumatol. 2021;12(1):1–11.
Shapiro F. Eye movement desensitization and reprocessing: basic principles, protocols, and procedures. New York: Guildford Press; 2001.
De Jongh A, ten Broeke E. Handboek EMDR: een geprotocolleerde behandelmethode voor de gevolgen van psychotrauma. Amsterdam: Harcourt; 2003.
First MB, Williams JB, Karg RS, Spitzer RL. Structured clinical interview for DSM-5—Research version (SCID-5 for DSM-5, research version; SCID-5-RV). Arlington: American Psychiatric Association; 2015.
Blake DD, Weathers FW, Nagy LM, Kaloupek DG, Gusman FD, Charney DS, et al. The development of a Clinician-Administered PTSD Scale. J Trauma Stress. 1995;8(1):75–90.
Group WAW. The Alcohol Smoking and Substance Involvement Screening Test (ASSIST): development, reliability and feasibility. Addiction. 2002;97:1183–94.
Carr S, Hardy A, Fornells-Ambrojo M. The Trauma and Life Events (TALE) checklist: development of a tool for improving routine screening in people with psychosis. Eur J Psychotraumatol. 2018;9(1):1512265.
Haddock G, McCarron J, Tarrier N, Faragher EB. Scales to measure dimensions of hallucinations and delusions: the psychotic symptom rating scales (PSYRATS). Psychol Med. 1999;29(4):879–89.
Drake R, Haddock G, Tarrier N, Bentall R, Lewis S. The Psychotic Symptom Rating Scales (PSYRATS): their usefulness and properties in first episode psychosis. Schizophr Res. 2007;89(1-3):119–22.
Mitchell PH, Powell L, Blumenthal J, Norten J, Ironson G, Pitula CR, et al. A short social support measure for patients recovering from myocardial infarction: the ENRICHED Social Support Inventory. J Cardiopulm Rehabil Prev. 2003;23(6):389–403.
Blevins CA, Weathers FW, Davis MT, Witte TK, Domino JL. The Posttraumatic Stress Disorder Checklist for DSM-5 (PCL-5): development and initial psychometric evaluation. J Trauma Stress. 2015;28(6):489–98.
McDonald SD, Calhoun PS. The diagnostic accuracy of the PTSD checklist: a critical review. Clin Psychol Rev. 2010;30(8):976–87.
Cloitre M, Shevlin M, Brewin CR, Bisson JI, Roberts NP, Maercker A, et al. The International Trauma Questionnaire: development of a self-report measure of ICD-11 PTSD and complex PTSD. Acta Psychiatr Scand. 2018;138(6):536–46.
Foa EB, Ehlers A, Clark DM, Tolin DF, Orsillo SM. The Posttraumatic Cognitions Inventory (PTCI): development and validation. Psychol Assess. 1999;11:303–14.
Murray J, Ehlers A, Mayou RA. Dissociation and post-traumatic stress disorder: two prospective studies of road traffic accident survivors. Br J Psychiatry. 2002;180:363–8.
Beck AT, Steer RA, Brown GK. Manual for the Beck Depresion Inventory-II. San Antonio: Psychological Corporation; 1996.
Freeman D, Loe BS, Kingdon D, Startup H, Molodynski A, Rosebrock L, et al. The revised Green et al., Paranoid Thoughts Scale (R-GPTS): psychometric properties, severity ranges, and clinical cut-offs. Psychol Med. 2019;51(2):244–53.
McGahuey CA, Gelenberg AJ, Laukes CA, Moreno FA, Delgado PL, McKnight KM, et al. The Arizona Sexual Experience Scale (ASEX): reliability and validity. J Sex Marital Ther. 2000;26(1):25–40.
Sanchez DT, Crocker J, Boike KR. Doing gender in the bedroom: investing in gender norms and the sexual experience. Pers Soc Psychol Bull. 2005;31(10):1445–55.
Neil ST, Kilbride M, Pitt L, Nothard S, Welford M, Sellwood W, et al. The questionnaire about the process of recovery (QPR): a measurement tool developed in collaboration with service users. Psychosis. 2009;1(2):145–55.
Smith BW, Dalen J, Wiggins K, Tooley E, Christopher P, Bernard J. The brief resilience scale: assessing the ability to bounce back. Int J Behav Med. 2008;15(3):194–200.
Hakkaart-van Roijen L, Van Straten A, Donker M, Tiemens B. Manual Trimbos/iMTA questionnaire for Costs associated with Psychiatric illness (TiC-P): Institute for Medical Technology Assessment; 2002.
Bouwmans C, De Jong K, Timman R, Zijlstra-Vlasveld M, Van der Feltz-Cornelis C, Tan Swan S, et al. Feasibility, reliability and validity of a questionnaire on healthcare consumption and productivity loss in patients with a psychiatric disorder (TiC-P). BMC Health Serv Res. 2013;13:217.
Konig HH, Roick C, Angermeyer MC. Validity of the EQ-5D in assessing and valuing health status in patients with schizophrenic, schizotypal or delusional disorders. Eur Psychiatry. 2007;22(3):177–87.
Paap D, Dijkstra PU. Working Alliance Inventory-Short Form Revised. J Physiother. 2017;63(2):118.
Corrigan JD, Schmidt LD. Development and validation of revisions in the counselor rating form. J Couns Psychol. 1983;30(1):64–75.
Hennink M, Kaiser BN. Sample sizes for saturation in qualitative research: a systematic review of empirical tests. Soc Sci Med. 2022;292:114523.
Weathers FW, Keane TM, Davidson JR. Clinician-administered PTSD scale: a review of the first ten years of research. Depress Anxiety. 2001;13(3):132–56.
Weathers FW, Bovin MJ, Lee DJ, Sloan DM, Schnurr PP, Kaloupek DG, et al. The Clinician-Administered PTSD Scale for DSM-5 (CAPS-5): development and initial psychometric evaluation in military veterans. Psychol Assess. 2018;30(3):383–95.
Boeschoten MA, Van der Aa N, Bakker A, Ter Heide FJJ, Hoofwijk MC, Jongedijk RA, et al. Development and evaluation of the Dutch Clinician-Administered PTSD Scale for DSM-5 (CAPS-5). Eur J Psychotraumatol. 2018;9(1):1546085.
Hyland P, Shevlin M, Brewin CR, Cloitre M, Downes AJ, Jumbe S, et al. Validation of post-traumatic stress disorder (PTSD) and complex PTSD using the International Trauma Questionnaire. Acta Psychiatr Scand. 2017;136(3):313–22.
Wells SY, Morland LA, Torres EM, Kloezeman K, Mackintosh MA, Aarons GA. The development of a brief version of the Posttraumatic Cognitions Inventory (PTCI-9). Assessment. 2019;26(2):193–208.
Bernstein EM, Putnam FW. Development, reliability, and validity of a dissociation scale. J Nerv Ment Dis. 1986;174(12):727–35.
Marmar CR, Weiss DS, Schlenger WE, Fairbank JA, Jordan BK, Kulka RA, et al. Peritraumatic dissociation and posttraumatic stress in male Vietnam theater veterans. Am J Psychiatry. 1994;151(6):902–7.
Beck AT, Steer RA, Ball R, Ranieri W. Comparison of Beck Depression Inventories -IA and -II in psychiatric outpatients. J Pers Assess. 1996;67(3):588–97.
Dozios DJ, Dobson KS, Ahnberg JL. Psychometric evaluation of the Beck Depression Inventory-II. Psychol Assess. 1998;10(2):83–8. https://doi.org/10.1037/1040-3590.10.2.83.
Fowler D, Hodgekins J, Painter M, Reilly T, Crane C, Macmillan I, et al. Cognitive behaviour therapy for improving social recovery in psychosis: a report from the ISREP MRC Trial Platform Study (Improving Social Recovery in Early Psychosis). Psychol Med. 2009;39(10):1627–36.
Short S. Review of the UK 2000 time use survey. London: Office for National Statistics; 2006.
de Bont PA, van den Berg DP, van der Vleugel BM, de Roos C, Mulder CL, Becker ES, et al. A multi-site single blind clinical study to compare the effects of prolonged exposure, eye movement desensitization and reprocessing and waiting list on patients with a current diagnosis of psychosis and co morbid post traumatic stress disorder: study protocol for the randomized controlled trial Treating Trauma in Psychosis. Trials. 2013;14:151.
van den Berg DP, de Bont PA, van der Vleugel BM, de Roos C, de Jongh A, van Minnen A, et al. Trauma-focused treatment in PTSD patients with psychosis: symptom exacerbation, adverse events, and revictimization. Schizophr Bull. 2016;42(3):693–702.
Brazier J. Is the EQ-5D fit for purpose in mental health? Br J Psychiatry. 2010;197(5):348–9.
Braun V, Clarke V. Using thematic analysis in psychology. Qual Res Psychol. 2006;3:77–101.
Braun V, Clarke V. Successful qualitative research: a practical guide for beginners. London: Sage; 2003.
Chan AW, Tetzlaff JM, Altman DG, Laupacis A, Gotzsche PC, Krleza-Jeric K, et al. SPIRIT 2013 statement: defining standard protocol items for clinical trials. Ann Intern Med. 2013;158(3):200–7.
Chan AW, Tetzlaff JM, Gotzsche PC, Altman DG, Mann H, Berlin JA, et al. SPIRIT 2013 explanation and elaboration: guidance for protocols of clinical trials. BMJ. 2013;346:e7586.
Skivington K, Matthews L, Simpson SA, Craig P, Baird J, Blazeby JM, et al. A new framework for developing and evaluating complex interventions: update of Medical Research Council guidance. BMJ. 2021;374:n2061.
Acknowledgements
The authors wish to thank the funder, the participating mental health institutions, the therapists, the research assistants, the independent specialists, advisors and all others who aid in bringing this study to a successful end.
Sponsor contact information
Trial Sponsor: Vrije Universiteit Amsterdam, the Netherlands
Contact name: Prof. Dr. Annemieke van Straten
Address: Van der Boechorstraat 7, 1081BT Amsterdam
Email: a.van.straten@vu.nl
Role of the sponsor and funder
This trial was designed by the research team. Neither the funder nor the sponsor will have a role in data collection, management, analysis, or interpretation; nor in the writing of the final report or decision to submit the report. The views expressed in this publication are those of the authors and not necessarily those of Stichting tot Steun VCVGZ or Vrije Universiteit Amsterdam.
Contact information
Contact for public and scientific queries: re.process@vu.nl, TL (Tineke.vander.linden@vu.nl), SB (s.r.burger@vu.nl)
Corresponding author: Simone Burger, room MF-B543, Van der Boechorstraat 7 1081 BT Amsterdam, s.r.burger@vu.nl
Funding
This work is supported by Stichting tot Steun VCVGZ (Foundation for VCVGZ Support), the Netherlands, grant number 241.
Stichting tot Steun VCVGZ
Toernooiveld 300, 6525 EC Nijmegen
T: 024-3512120
Author information
Authors and Affiliations
Contributions
DB (principal investigator) and MvdG received the funding for this study. DB, AH, and MvdG developed the concept and design of the study. DB, TL, CZ, and SB coordinate and monitor the study (data and therapy coordination). DB, MvdG, AH, AM, and MM supervise the PhD students. AH, AJ, CR, AM, TS, BV, PB, and TL supervise the therapists. KM and JG advise the trial team on the execution and fidelity of CR. TL, SB, and DB will carry out the statistical analyses. All authors will have access to the final trial data and contribute to writing manuscripts. All authors have contributed to and read and approved the final version of the protocol. All contributors will author the main outcome papers.
Corresponding author
Ethics declarations
Ethics approval and consent to participate
This protocol was approved by the Medical Ethics Committee of the VU University Medical Centre in Amsterdam, the Netherlands (METC number: 2019.046/ NL66431.029.19) on March 27th of 2019. Written informed consent will be gained from each participant before any study procedures are initiated.
Consent for publication
Please see Additional file 1 for the consent form.
Competing interests
AH, TS, MvdG, and DB receive income for published books on psychotic disorders and for the training of postdoctoral professionals in the treatment of psychotic disorders. JG and KM receive incomes for training of postdoctoral professionals in Cognitive Restructuring. AJ receives incomes for published books on EMDR therapy and for the training of postdoctoral professional in this method. AM receives income for published book chapters on PTSD and for the training of postdoctoral professionals in Prolonged Exposure. CR receives income for the training of postdoctoral professionals in EMDR therapy.
Additional information
Publisher’s Note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
Supplementary Information
Additional file 1.
Model Consent Form.
Additional file 2.
SPIRIT Checklist for Trials.
Rights and permissions
Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated in a credit line to the data.
About this article
Cite this article
Burger, S.R., van der Linden, T., Hardy, A. et al. Trauma-focused therapies for post-traumatic stress in psychosis: study protocol for the RE.PROCESS randomized controlled trial. Trials 23, 851 (2022). https://doi.org/10.1186/s13063-022-06808-6
Received:
Accepted:
Published:
DOI: https://doi.org/10.1186/s13063-022-06808-6