Schizophrenia Clinical Trial
Official title:
Psychological Interventions for Complex PTSD And Schizophrenia-Spectrum Disorder: PICASSO Trial
Psychosis is a highly distressing mental health condition, affecting up to 3% of the population. Conceptually, it has much in common with complex post-traumatic stress disorder (CPTSD), a recently introduced condition in ICD-11. Both involve negative self-esteem, impaired emotion regulation ability, interpersonal difficulties and intrusive trauma- related experiences (i.e. intrusive thoughts, flashbacks, nightmares). Both have been causally related to childhood trauma, such as abuse, neglect and loss. The current project will examine the feasibility of conducting an 'Umbrella trial' to test whether CPTSD is causally related to psychosis, and develop more effective trauma-focused psychological interventions for psychotic symptoms by treating underlying experiences of/reactions to trauma. An Umbrella trial involves running several individual randomised controlled trials concurrently. In this study, each trial will test whether psychological interventions designed to reduce different CPTSD symptoms cause improvements in psychotic symptoms. If the investigators can establish feasibility of this Umbrella trial, and if a definitive version shows that interventions for CPTSD also reduce psychosis, then this would be a breakthrough in both the conceptualisation and treatment of psychosis which will help transform the care of people with psychosis. Demonstrating the feasibility of our proposed methodology would also help to accelerate the development of interventions for other mental health problems.
BACKGROUND & RATIONALE FOR STUDY Psychosis, characterised by unusual experiences such as delusions and hallucinations, is commonly associated with a diagnosis of schizophrenia. It affects up to 3% of the population, and individuals with this condition often experience high levels of distress, a loss of ability to plan and work, and a loss of interpersonal relationships. People with psychosis die 15-20 years earlier than the general population, however existing treatments for psychosis have at best modest effects on symptoms and related distress. Consequently, many thousands of people are left with highly distressing symptoms that remain resistant to current treatment. Exposure to childhood trauma substantially increases the risk of developing psychosis. Post-traumatic stress disorder (PTSD) and psychosis frequently co-occur and PTSD is a known risk factor for later psychosis. However, strategies to treat PTSD in psychosis have had limited success. This may be because psychosis overlaps with a more complex condition than PTSD, namely Complex PTSD (CPTSD). CPTSD, now recognised in the 11th revision of the World Health Organisation's International Classification of Diseases (ICD-11), is defined as PTSD (i.e. intrusive thoughts, avoidance of reminders of the traumatic memory and hyperarousal) and co-occurring symptoms of affect dysregulation (AD), negative self-concept (NSC), and disturbed relationships (DR). These symptom domains, which are commonly referred to as Disturbances of Self-Organisation (DSO), are also highly prevalent in psychosis, and they appear to mediate the relationship between childhood adversity and psychotic symptoms. In a recent pilot study (n=85), 41% of people with psychosis endorsed symptoms of CPTSD, confirming that CPTSD and psychosis very frequently co-occur. Thus, psychological treatments that reduce CPTSD symptoms might represent a new direction in both the conceptualisation and treatment of psychosis. Although there is strong observational evidence that traumatic stress may cause psychosis via CPTSD symptoms, this relationship has not been tested experimentally. Furthermore, although there are existing psychological interventions for CPTSD symptoms, it is unknown whether they are effective at reducing psychotic symptoms. Based on an established effective therapy for complex traumatisation (Skills Training in Affective and Interpersonal Regulation; STAIR), the investigators have recently devised a treatment protocol for CPTSD (Enhanced STAIR for CPTSD - ESTAIR with three 6-session modules targeting individual DSO symptom clusters of CPTSD (AR, NSC & DR). The next stage of our research will focus on whether targeting DSO symptoms in people with psychosis can improve treatments for psychosis. The investigators will examine the feasibility of conducting an 'Umbrella trial' to test whether CPTSD symptoms are causally related to psychosis, and develop more effective trauma-focused psychological interventions for psychosis. This involves running three single-blind 'interventionist-causal' randomised controlled trials (IC-RCTs) concurrently, each testing whether an individual ESTAIR DSO module (addressing either AD, NSC or DR) causes improvements in psychotic symptoms. Recommended to accelerate the treatment of psychotic symptoms such as delusions, running these sophisticated trials concurrently can produce significant findings 10-15 years earlier compared to running each trial individually. If the feasibility of this Umbrella trial can be established, defined as successful recruitment and retention of participants with psychosis, the investigators will seek funding to conduct a definitive trial. AIMS and RESEARCH QUESTIONS Aim 1: Adapt an existing CPTSD modular intervention (ESTAIR) so that it can be used with people with psychosis (RQ 1) Aim 2: Test feasibility, acceptability, and safety of the CPSTD modular therapy in people with psychosis (RQ 2,3) Aim 3: Test recruitment rates, data quality and trial procedures for a definitive Umbrella (RQ 3,4) Research questions (RQ): RQ 1: Can an effective CPTSD intervention (ESTAIR) be adapted and used to help individuals with psychosis? RQ 2: What proportion of eligible individuals participate, engage, and complete the interventions as part of the Umbrella trial? RQ 3: What proportion of eligible individuals participate in, engage with and complete research assessments, and what data quality and completion rates can therefore be obtained? RQ 4: What sample size is required for a definitive trial? STUDY DESIGN Following consultation with NIHR EME, this study has been designed to ensure the investigators can successfully recruit and retain participants in a larger trial characterised by the same design parameters (e.g., allocation ratio, blind assessment, types of treatment and control offered, multiple sites). The proposed randomised pilot study is therefore a 20-month feasibility/pilot of a multi-site single (rater) blind Umbrella trial of psychological interventions to treat CPTSD symptoms in people diagnosed with non-affective psychosis (schizophrenia-spectrum disorders). It has been designed primarily to examine post-treatment (8 week) data retention rates for the planned primary outcome (PANSS; psychotic symptoms) in a future definitive trial. In this and the future study, participants will be randomly allocated to receive treatment as usual (TAU) plus a psychological intervention to improve (i) affect dysregulation (AD), (ii) negative self-concept (NSC), or (iii) disturbed relationships (DR), or TAU alone by way of control condition. To ensure recruitment from a large pool of participants from multiple sites, 50% of the sample will be recruited from the lead site (NHS Lothian) and 50% from NHS Greater Glasgow and Clyde. Each intervention group will be compared to its own control group (each will receive the same standardised procedure) to ensure participants in each trial are equivalent with respect to their presenting mechanism. Participants & setting: Adults (aged 18-65) diagnosed with schizophrenia-spectrum disorder, and presence of AD, NSC or DR (as a result of exposure to traumatic life events) will be recruited from inpatient and outpatient NHS mental health services across two Scottish sites; 50% from NHS Lothian; 50% from NHS Greater Glasgow and Clyde. Allocation and randomisation: Participants will be randomly assigned to one of the two-arm IC-RCTs based on whether they present with AD, NSC or DR (score ≥2 in each domain as assessed by the ITQ). Participants with multiple mechanisms will be randomly assigned. All participants will be randomised (1:1) to either treatment or control using Sealed Envelope online randomisation prior to the start of treatment session 1. Interventions and control: Each of the three ESTAIR DSO modules is structurally equivalent (6 sessions each over 8 weeks) and will be delivered by the same trained therapist. Each has been designed to reduce symptoms of a specific CPTSD symptom cluster (AD, NSC or DR). Participants allocated to intervention will receive one of the three 6-session modules, over an 8-week window.In the full trial it will be monitored whether TAU moderates outcomes by using an appropriate tool (i.e. Client Receipt Service Inventory; CSRI). Data collection & masking: Clinical research data will be gathered at baseline, post-intervention (week 8) and follow-up (week 12). RAs will be masked to group allocation to demonstrate to future funders this is achievable in an Umbrella trial. Blind-breaks will be recorded, and minimised using previously successful strategies (e.g., separate offices / diaries). Data Analysis: Blind analysis of outcome data according to a fully pre-registered plan will be conducted. Proportions, means, SDs, effect sizes and 95% CIs for all time points will be reported descriptively on both a strict intention-to-treat and per-protocol basis (≥50% attendance in treatment or control). Missing data due to attrition will be minimised by maintaining up to two phone contacts with participants between assessments. Progression criteria for a full trial: the investigators will progress if the recruitment target is achieved and post-intervention (8 week) PANSS data is acquired from ≥75% of those randomised (45). Research Team & Expert Advisory Group This project will receive strong support from: A) An Expert Advisory group: This will include an expert by experience with interest in research in trauma and psychosis B) An experienced multi-disciplinary research team: the team has been chosen to ensure it comprises clinical, academic and methodological experience and expertise in all relevant areas required for successful completion of the project. STUDY POPULATION NUMBER OF PARTICIPANTS NIHR guidance was used to calculate that 60 participants (2 per month per site over 15-months) will allow us to estimate a drop-out rate (i.e. data non-retention) of 15%, at week 8, to within a 95% confidence interval of +/- 10%. The proportion of people with schizophrenia-spectrum disorders who have at least one of our proposed causal mechanisms is estimated to be approximately 40%. IDENTIFYING AND RECRUITMENT OF PARTICIPANTS As per previous trials in the field of psychosis, local site leads will enable RAs to visit clinical services to present the trial, determine initial interest, and distribute information sheets. Referrers will seek consent from potential participants to be contacted by the researchers. Those consenting will be given a participant information sheet and any initial questions will be answered. They will be re-contacted after a minimum period. Those consenting will be assessed. Those eligible will enter the trial. Self referral will be accepted. A poster will be placed in NHS mental health services to advertise the study. If an individual self-refers, they will only be included if they agree to the investigators contacting a mental health professional involved in their care, to obtain information for risk assessment purposes and to ensure participation is not contraindicated in some way. CONSENTING PARTICIPANTS Only include adults who have capacity to consent to research will be included. For potential participants entering the study through the clinician-referral recruitment pathway, their clinician will discuss the study with them, answer any questions, give them an information sheet and seek their verbal consent to pass on their details to the research team, and allow them to complete an initial risk assessment. A trained and supervised research assistant (RA) will then contact clinicians to gather contact details for potential participants and complete the risk assessment. The RA will then contact potential participants directly to discuss the study further and answer any questions. For potential participants entering the study through self-referral, the RA will obtain their explicit verbal consent to contact their keyworker/ care-coordinator to determine whether they meet inclusion criteria for the study and to complete an initial risk assessment. The RA will also ask the clinical care team if they have any concerns about the potential participant's capacity to consent to take part in research. Should participants meet inclusion criteria for the study and continue to express an interest in taking part, the RA will contact them to arrange an appointment. All potential participants will have as long as they wish to consider the information sheet prior to being contacted by the RA, with a minimum period of 48 hours. The information sheet will detail what participants are asked to do, how their information will be used and the possible risks and benefits of taking part in the study. PARTICIPANT WITHDRAWAL Participants are free to withdraw from the study at any point, without giving any reason and without their legal rights or usual care being affected. Investigators may also withdraw participants if they deem their continuation to be harmful. Advance consent will be sought from all participants to retain their existing data should they subsequently withdraw due to loss of contact or loss of capacity to consent to research, where they have not otherwise informed us they wish their data to be removed. See information below regarding Serious Adverse Events. STUDY SUSPENSION OR DISCONTINUATION The research would be stopped in the event of a number of SAEs which are deemed attributable to participation in PICASSO. All SAEs will be passed on to the independent Data Monitoring and Ethics Committee (DMEC) for review, who would have responsibility for advising the Chief Investigator and Sponsor as to whether they are attributable to study participation, setting the threshold for discontinuation and issuing advice to suspend or discontinue. After taking into account advice from the DMEC and consulting with the Chief Investigator, the Sponsor and Research Ethics Committee (REC) will make the final determination on whether the trial will continue or not. See Section 9 for more details. ADVERSE EVENTS PARTICIPANTS The interventions have been used previously with people with CPTSD, including in randomised controlled trials and no severe adverse events have been reported. However, the investigators wish to improve the recording and reporting of adverse effects of psychological interventions, and have therefore developed a robust protocol for assessing and managing any such risk, which will be completed at end of treatment and at follow-up by RAs masked to treatment condition. Using an approach adapted from the DEC:IDES trial serious adverse events will be defined as (i) death by suicide; (ii) suicide attempt; (iii) suicidal crisis without attempt ; (iv) severe symptom exacerbation (rating of ≥6 on the patient or researcher-rated Clinical Global Impression Scale (CGI) and CGI-Improvement scale). Non-severe adverse events will be defined as a score of ≥3 (agree 'quite a lot' or 'a lot') on any relevant item (e.g., subjectively worsening mental state, heightened stigma, increased medication use, increased conflict) on the patient-rated 27-item Adverse Events Questionnaire. This protocol, excluding the Adverse Events Questionnaire (which is designed to be completed after treatment), will also be completed by clinicians during the intervention (i.e., every session) to complete an assessment of severe adverse events. This will be primarily for clinical purposes, although scores will also be reported to the DMEC, the Sponsor, and in the final paper. As noted above, the DMEC will review each serious adverse event (SAEs) and provide an independent assessment to the Sponsor (Edinburgh Napier University) of whether or not it is likely to be attributable to the person's participation in PICASSO. The Sponsor will make the final decision as to whether the SAE was attributable to participation, and therefore whether it needs to be reported to the NHS REC. The research would be stopped in the event of a number of SAEs which are deemed attributable to participation in PICASSO. All SAEs will be passed on to the independent DMEC for review, who would have responsibility for advising the Chief Investigator and Sponsor as to whether they are attributable to study participation, setting the threshold for discontinuation and issuing advice to suspend or discontinue. After taking into account advice from the DMEC and consulting with the Chief Investigator, the Sponsor and REC will make the final determination on whether the trial will continue or not. See Section 9 for more details. ;
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