Introduction
PTSD is a stress-related disorder that may develop following exposure to a traumatic event such as a terrorist attack, car crash or being the victim of violence. The core symptoms of PTSD include re-experiencing the traumatic event, a persistent heightened sense of threat, avoidance of reminders of the traumatic event and negative alterations in cognition and mood associated with the traumatic event (DSM-5; American Psychiatric Association, 2013). PTSD can significantly impact a person’s quality of life, functioning, and wellbeing. Therefore, it is important to provide effective and accessible treatment for people with PTSD. In England, one of the main sources of treatment for PTSD is the NHS Talking Therapies programme (formerly known as Improving Access to Psychological Therapies, IAPT). This programme was launched in 2008 and aims to provide evidence-based psychological therapies for common mental health problems, such as depression and anxiety disorders, including PTSD. For a full review of IAPT, see Clark (Reference Clark2018).
Individuals with PTSD should routinely be offered 8–12 sessions of NICE-recommended evidence-based therapy, such as trauma-focused cognitive behaviour therapy (TF-CBT) or eye movement desensitisation reprocessing (EMDR) (National Institute of Clinical Excellence, 2018). These approaches have shown good effectiveness (Bisson et al., Reference Bisson, Roberts, Andrew, Cooper and Lewis2013; Cusack et al., Reference Cusack, Jonas, Forneris, Wines, Sonis, Middleton, Feltner, Brownley, Olmsted, Greenblatt, Weil and Gaynes2016). However, standard NICE-recommended interventions may be less effective in more complex PTSD presentations (Cloitre, Reference Cloitre2021).
There has been considerable controversy over the recent clinical distinction of complex PTSD (CPTSD) (Resick et al., Reference Resick, Bovin, Calloway, Dick, King, Mitchell, Suvak, Wells, Stirman and Wolf2012). Although it is not a formal diagnostic category within the Diagnostic and Statistical Manual of Mental Disorders (DSM-5; American Psychiatric Association, 2013), the label is recognised by trauma experts (e.g. Cloitre et al., Reference Cloitre, Garvert, Brewin, Bryant and Maercker2013; Herman, Reference Herman1992; van der Kolk et al., Reference van der Kolk, Roth, Pelcovitz, Sunday and Spinazzola2005) and has recently been classified as a distinctive diagnosis within the 11th edition of the International Classification of Diseases (ICD-11) (World Health Organization, 2018). CPTSD is characterised by the core symptoms of PTSD, accompanied by enduring disturbances in the domains of emotion regulation, self, and interpersonal relationships (Cloitre et al., Reference Cloitre, Garvert, Brewin, Bryant and Maercker2013; ICD-11; World Health Organization, 2018).
The ICD-11 distinction has gained purchase within the psychological community (Hyland et al., Reference Hyland, Shevlin, Elklit, Murphy, Vallières, Garvert and Cloitre2017; Nickerson et al., Reference Nickerson, Cloitre, Bryant, Schnyder, Morina and Schick2016). Evidence supports the discriminative validity of PTSD and CPTSD diagnoses (Brewin et al., Reference Brewin, Cloitre, Hyland, Shevlin, Maercker, Bryant, Humayun, Jones, Kagee, Rousseau, Somasundaram, Suzuki, Wessely, van Ommeren and Reed2017), demonstrating its clinical relevance. Although there are no specific guidelines for treatment of CPTSD in the UK, NICE acknowledges complexity and recommends extended sessions if clinically indicated (National Institute of Clinical Excellence, 2018).
Whilst in harmony with NICE and NHS core values, routinely offering additional sessions to treat this challenging presentation can significantly increase wait times for therapy. This places pressure on IAPT services to deliver therapy within a timely manner and creates burden for those waiting for individual TF-CBT or EMDR. Longer wait times have also been associated with symptom deterioration (Hoppen et al., Reference Hoppen, Lindemann and Morina2022; Jayawickreme et al., Reference Jayawickreme, Cahill, Riggs, Rauch, Resick, Rothbaum and Foa2017) and poorer patient outcomes (Clark, Reference Clark2018). The pressure also has implications for IAPT targets. For example, 75% of IAPT service users should access treatment within 6 weeks, and 95% of people should access treatment within 18 weeks of referral (IAPT Manual; National Collaborating Centre for Mental Health, 2018); thus, systematically extended waiting times due to complexity can lead to service failures of the IAPT targets (Scott, Reference Scott2018).
Not surprisingly, long waits for treatment access are a national concern. To minimise suffering, some IAPT services have taken the initiative to offer psychoeducational group-based programmes delivering stabilisation and symptom management skills to those waiting for individual trauma therapy (Cole, Reference Cole2019).
Literature suggests that interventions aiming at initially stabilising patients with more complex presentations could be beneficial (Bohus et al., Reference Bohus, Dyer, Priebe, Krüger, Kleindienst, Schmahl, Niedtfeld and Steil2013; Cloitre et al., Reference Cloitre, Koenen, Cohen and Han2002; Courtois and Ford, Reference Courtois and Ford2012; Ford and Courtois, Reference Ford and Courtois2020; Herman, Reference Herman1992). Courtois et al. (Reference Courtois, Ford, Green, Alexander, Briere, Herman, Lanius, Anne Pearlman, Stolbach, Spinazzola, van der Kolk and van der Hart2012) argue that prior to trauma-focused therapy, individuals with CPTSD should acquire strategies to manage PTSD symptoms alongside information about the nature and effects of trauma (psychoeducation) to increase patient safety and improve emotion regulation. Evidence for better treatment outcomes of phase-based interventions that use a stabilisation phase with skills-based strategies prior to trauma-focused therapy is scarce and equivocal to date, with some evidence for its beneficial effect (Coventry et al., Reference Coventry, Meader, Melton, Temple, Dale, Wright, Cloitre, Karatzias, Bisson, Roberts, Brown, Barbui, Churchill, Lovell, McMillan and Gilbody2020; Eichfeld et al., Reference Eichfeld, Farrell, Mattheß, Bumke, Sodemann, Ean, Phoeun, Direzkia, Firmansyah, Sumampouw and Mattheß2019) but others challenging the need for it (Bicanic et al., Reference Bicanic, de Jongh and Broeke2015; Melegkovits et al., Reference Melegkovits, Blumberg, Dixon, Ehntholt, Gillard, Kayal, Kember, Ottisova, Walsh, Wood, Gafoor, Brewin, Billings, Robertson and Bloomfield2023) suggesting that TF–CBT was effective with or without a preceding stabilisation phase and warning that such interventions may delay individuals from receiving individual evidence-based interventions (De Jongh et al., Reference De Jongh, Resick, Zoellner, van Minnen, Lee, Monson, Foa, Wheeler, ten Broeke, Feeny, Rauch, Chard, Mueser, Sloan, van der Gaag, Rothbaum, Neuner, de Roos, Hehenkamp and Bicanic2016). However, in a context of high demand and extended waiting times, attending a stabilisation group whilst waiting for individual treatment could prevent symptom deterioration, reduce burden and potentially prepare patients for the individual trauma-focused therapies they are to receive. For example, at the time of this study, the average wait time for trauma-focused therapy at Plymouth Options was over 18 months.
The present study, therefore, investigated the feasibility and acceptability of a 5-week trauma-focused stabilisation group informed by Cloitre and colleagues (2012) for individuals with PTSD and complex presentations who were on the waitlist for individual PTSD therapy. Second, the study investigated whether the group prevented symptom deterioration and was associated with clinical benefits in PTSD, depression and anxiety symptoms.
Method
Design
The current study involved a mixed methods design exploring quantitative and qualitative data using a pre–post-case series design and summative content analysis (Berg et al., Reference Berg, Bruce and Lune2017).
Participants
Participants were recruited from Plymouth Options IAPT service trauma waitlist via an opt-in letter. Of 120 invited participants, 58 agreed to join the group. Thirty-eight participants completed all five sessions in the group.
All participants had undergone a standard IAPT assessment, including risk assessment and fulfilling PTSD criteria with a clinically significant IES-R score (>33). At assessment, a full trauma history was taken, including an assessment for a history of symptoms of disturbances in self-organisation. Those service users who met the proposed ICD-11 criteria for CPTSD were given the label ‘Complex PTSD’. Full patient characteristics can be viewed in Table 1. Participants were required to be over 18 and have sufficient knowledge of the English language to enable participation without the use of an interpreter. Participants in a state of psychological or suicide crisis, actively abusing alcohol or substances, were excluded from the programme due to the remit of IAPT service provision.
Measures
The Impact of Events Scale-Revised (IES-R; Weiss and Marmar, 1997)
The IES-R is an IAPT-recommended PTSD outcome measure. The questionnaire assesses respondents’ subjective level of trauma based on the DSM-5 diagnosis criteria using 22 items rated on a 0 (not at all) to 4 (extremely) scale concerning how distressing each item has been during the past week. The threshold for clinical significance is a score of ≥33, with a total score of 88 possible. High levels of internal consistency have been previously reported, with Cronbach’s alpha ranging from .79 to .94 (Creamer et al., Reference Creamer, Bell and Failla2003; Weiss and Marmar, Reference Weiss, Marmer, Wilson and Keane1997).
Patient Health Questionnaire-9 (PHQ-9; Kroenke and Spitzer, Reference Kroenke and Spitzer2002)
The PHQ-9 measures symptoms of depression based on the DSM-5 diagnostic criteria for depression. The questionnaire assesses how often the respondents had been disturbed by the nine listed items during the immediately preceding 2 weeks. The self-report measure is rated 0 (not at all) to 3 (nearly every day). The threshold for clinical significance is a score of ≥10, with a total score of 27 possible. The measure has been widely used within primary care and demonstrated good psychometric properties with Cronbach’s alpha of 0.89 (Kroenke et al., Reference Kroenke, Spitzer and Williams2001) and good criterion and construct validity of the PHQ–9 as a diagnostic and severity measure (Kroenke and Spitzer, Reference Kroenke and Spitzer2002).
Generalised Anxiety Disorder-7 (GAD-7; Spitzer et al., Reference Spitzer, Kroenke, Williams and Löwe2006)
The GAD-7 questionnaire assesses the severity of anxiety based on how often the respondents had been disturbed by the seven listed items during the immediately preceding 2 weeks. The self-report measure is rated 0 (not at all) to 3 (nearly every day). The threshold for clinical significance is a score of ≥8, with a total score of 21 possible. This questionnaire has demonstrated good internal consistency (Cronbach’s alpha=0.84) as well as test–retest reliability (Spitzer et al., Reference Spitzer, Kroenke, Williams and Löwe2006), criterion, construct, concurrent and convergent validity (Löwe et al., Reference Löwe, Decker, Müller, Brähler, Schellberg, Herzog and Herzberg2008; Ruiz et al., Reference Ruiz, Zamorano, García-Campayo, Pardo, Freire and Rejas2011; Spitzer et al., Reference Spitzer, Kroenke, Williams and Löwe2006).
Patient Experience Questionnaire (PEQ)
The PEQ was internally developed, informed by the IAPT Patient Experience Questionnaire (National Collaborating Centre for Mental Health, 2018) to ascertain participants’ satisfaction with the course and consisted of three distinct parts. Part 1 consisted of eight statements that measured the overall acceptability of the group on a 4-point scale from ‘strongly agree’ to ‘strongly disagree’. Part 2 considered the acceptability of each session and its associated components in detail via a session-by-session evaluation. Respondents were asked to rate the relevance of each component of the session on a 4-point scale from ‘very relevant’ to ‘not relevant’. Part 3 explored idiosyncratic feedback from group attendees. Respondents could reflect personally about what had been most helpful and least helpful about attending the group, what they would like more or less of in the group, and any other feedback.
Procedure
All participants were invited to complete the IAPT minimum dataset (MDS) on a session-by-session basis before the session commenced The IES-R was administered alongside the MDS at the first and last session only. The PEQ was administered at the end of the final session.
Intervention
The group intervention consisted of five face-to-face sessions focused on psychoeducation about the effects of trauma, including single-incident trauma, early life, or cumulative trauma and how this might relate to the individual’s symptoms, life course, worldview and relationships. Specific strategies taught included symptom management, emotion regulation skills, cognitive restructuring, and mindfulness. The group design was informed by ISTSS Expert Consensus Treatment Guidelines for Complex PTSD in Adults (Cloitre et al., 2012). Sessions were designed and structured to last two hours with a 15-minute midpoint break. Table 2 provides a summary of the content and format of the intervention.
The group took place weekly over five weeks at the same time and day of the week. It was facilitated by two qualified CBT and EMDR therapists. Each session consisted of psychoeducational information followed by several points of interactive group discussion. Each session also included voluntary experiential practice of a relevant stabilisation intervention introduced in the session. At the end of each session, time was allocated for reflections and questions. Each session was supplemented by a handbook, summarising the information introduced in the session with content-specific home practice activities. Time was also allocated at the start of each subsequent session to feed back on the group’s experiences of practising learned interventions.
Data analysis
Feasibility and acceptability were determined from group uptake, retention (percentage of participants who completed at least three sessions) and participant feedback about the group from the PEQ. Results from parts 1 and 2 of the PEQ are presented graphically.
Textual data from each question were analysed and coded to identify common patterns of responses using content analysis (Erlingsson and Brysiewicz, Reference Erlingsson and Brysiewicz2017). Content analysis is typically applied to find response patterns in brief text such as the open-ended questions in part 3 of the PEQ.
We evaluated the clinical benefit of our intervention in multiple ways. Firstly, we analysed the pre-and post-treatment scores of attendees who completed the IES-R, PHQ-9 and GAD-7 measures. Those who did not complete the measures were excluded from the analysis (n=15). To determine meaningful changes at an individual level, we followed the recommendations of Morley and Dowzer (Reference Morley and Dowzer2014) by using the reliable change index (RCI) (Jacobson and Truax, Reference Jacobson and Truax1991) and clinically significant change methodology (CSC). We utilised Morley and Dowser’s (Reference Morley and Dowzer2014) Leeds RCI Excel application for RCI and CSC calculations. We calculated the cut-off scores for IES-R, PHQ-9 and GAD-7 using the method developed by Jacobson and Truax (Reference Jacobson and Truax1991) and Jacobson et al. (Reference Jacobson, Dobson, Truax, Addis, Koerner, Gollan, Gortner and Prince1996).
We retrieved the mean, standard deviation, and Cronbach’s alpha scores from Creamer et al. (Reference Creamer, Bell and Failla2003), Kroenke et al. (Reference Kroenke, Spitzer and Williams2001), and Jacobson and Truax (Reference Jacobson and Truax1991) for IES-R, PHQ-9 and GAD-7, respectively. We presented the results in a scatter plot that allows for visual analysis of pre- and post-treatment data points for each measure.
Second, we determined the effect size (Cohen’s d) and confidence intervals of the overall intent-to-treat (ITT) and per protocol (PP) symptom change using paired sample t-tests. For the ITT, missing values at the last session (IES-R) or post-intervention (PHQ-9, GAD-7) were replaced by the last observation carried forward method (Last Observation Carried Forward, 2010).
Third, we identified patients’ perceived benefits from the PEQ content analysis.
Results
Feasibility and acceptability
Recruitment and retention
The offer of attending the group whilst on the waitlist was taken up by nearly 50% of the patients waiting for individual therapy (58 out of 120). Reasons for not joining were declining a group format, care, and work commitments. As seen in Table 3, of the 58 assigned to the groups, six did not start for various reasons, including change of circumstances, illness and changing mind about the group. From the 52 who started the group, 45 (86%) completed at least 60% of the group (three or more sessions). Seven (14%) dropped out. Reasons for drop-out were destabilisation (no longer meeting IAPT service suitability and being referred to CMHT), offers of individual treatment, family illness and declining group format. This indicates that the stabilisation group was acceptable and feasible for around 37.5% of PTSD/CPTSD patients in this clinical service. Session attendance was high, with 38 (74%) of the completers attending all five sessions, suggesting that those who joined the group found it feasible and acceptable. Further quantitative ratings and qualitative feedback from the PEQ confirmed this.
Participant feedback about acceptability, feasibility and perceived benefit
As shown in Fig. 1, 97% of participants strongly agreed that they would recommend the course to other people, that the course was worthwhile and that the length and frequency of the sessions were just right; 80–90% of participants reflected that the group worked well together, and 86% indicated that the programme made them more confident in managing their trauma symptoms. Participants reflected on specific benefits of the course, such as:
‘The course has really helped me to accept the way that I am right now and given me hope for the future with the skills I’ve learned; thank you so much. It’s been a real help.’
‘I have gained strength and courage from attending and learning the coping mechanisms.’
Participants also found a sense of validation of their trauma experience through attending the group:
‘Attending the group helped me to realise that I am not alone in this … I found comfort in this.’
‘Learning about everything with everybody and being in a room where people understand what it’s like to go through this has been so helpful to me.’
Taken together, participant feedback indicated that the group was both acceptable and feasible to the participants and conferred individual benefits through learning in a group and being validated.
Clinical benefit
PTSD symptom severity and recovery
Reliable and clinical change
As can be seen in Fig. 2a, out of the sample size of 38, 73% (n=27) of those patients that attended the group reliably improved, with two participants meeting the clinically significant change criterion indicating recovery from active symptoms of PTSD (IES-R<33). Nine participants placed within the corridor of uncertainty, indicating no significant change in rated symptoms of PTSD. Two participants deteriorated, suggesting symptoms of PTSD worsened whilst attending the group. From the results pre-test mean score of 63.5, IES-R can be compared with post-test mean IES-R score of 51.2, suggesting an average score decrease of 12.3 (SD=11.0).
Effect size for per-protocol (PP) and intent-to-treat (ITT) analyses
Paired sample t-test revealed a significant mean pre-to-post reduction of PTSD severity, t 37=6.90, p<.001, Cohen’s d=1.05, 95% CI [0.66, 1.45], suggesting a large treatment effect. In more conservative ITT analyses with all group starters, there was also a significant mean pre-to-post reduction of PTSD severity of 9.73 (SD=10.97) on the IES-R from 63.73 to 54.00, t 47=6.15, p<.001, Cohen’s d=0.77, 95% CI [0.47, 1.07]. This describes a medium to large treatment effect.
Follow-up PTSD Symptom Change According to the Clinician-Administered IES-R can be found in the Supplementary material.
Depression symptom severity and recovery
Reliable and clinical change
As can be seen in Fig. 2b, out of the sample size of 38, 73% (n=27) of those patients that attended the group placed within the corridor of uncertainty, indicating no significant change in rated symptoms of depression. Five participants deteriorated, suggesting symptoms of depression worsened whilst attending the group. Six participants’ symptoms of depression reliably improved whilst attending the group.
Effect size for PP and ITT analyses
Paired sample t-test revealed that there was no significant mean pre-to-post deterioration of depression severity of –0.54 (SD=5.32) on the PHQ-9 from 15.88 to 16.41, t 40=–0.64, p=.261, Cohen’s d=–0.09, 95% CI [–0.39, 0.20] suggesting a small treatment effect. Similarly, ITT analyses revealed no significant mean pre-to-post deterioration of depression severity of –0.43 (SD=4.76) on the PHQ-9 from 16.59 to 17.02, t 50=–0.64, p=.261, Cohen’s d=–0.08, 95% CI [–0.32, 0.16].
Overall, the aim of the intervention, to prevent a deterioration of depression symptoms, was accomplished in 73% of group patients.
Anxiety symptom severity and recovery
Reliable and clinical change
Similar results were also found from the case series analysis of pre-and post-treatment scores of the GAD-7. As shown in Fig. 2c, out of the sample size of 38, 70% (n=25) of patients that attended the group placed within the corridor of uncertainty indicated no significant change in rated anxiety symptoms. Four participants deteriorated, suggesting symptoms of anxiety worsened whilst attending the group and nine participants’ symptoms of anxiety reliably improved whilst attending the group.
Effect size for PP and ITT analyses
Paired sample t-test revealed that there was no significant mean pre-to-post deterioration of anxiety severity of 0.54 (SD=3.46) on the GAD-7 from 15.49 to 14.95, t 40=0.99, p=.163, Cohen’s d=0.12, 95% CI [–0.12, 0.35] suggesting a small treatment effect. Similarly, ITT analysis revealed no significant mean pre-to-post reduction of anxiety severity of 0.43 (SD=3.10) on the GAD-7 from 15.53 to 15.10, t 50=0.99, p=.163, Cohen’s d=0.10, 95% CI [–0.10, 0.29]. This describes a small treatment effect.
Overall, the aim of the intervention to prevent a deterioration of anxiety symptoms was accomplished in 70% of group participants.
Discussion
The primary aim of this study was to ascertain whether a psychoeducational group-based programme delivering stabilisation and symptom management skills to those waiting for individual trauma therapy was acceptable to service users expected to have a long wait for therapy. The study also sought to investigate the preliminary clinical benefit of this new group using a mixed-method design. Overall, we found the stabilisation group to be feasible and acceptable. We found evidence of marginal symptom deterioration and, interestingly, for PTSD, we found medium to large effects for symptom reductions.
Feasibility and acceptability of the group
Participants’ experiences and our ability to recruit and retain them suggest good feasibility and acceptability of the stabilisation group. Most participants reported that they found the psychoeducational programme applicable, helpful, easy to understand and the right length, suggesting that participants were satisfied with the overall structure and content of the course. These findings are consistent with Dorrepaal and colleagues (Dorrepaal et al., Reference Dorrepaal, Thomaes, Smit, van Balkom, van Dyck, Veltman and Draijer2010), who also found the delivery of a group-based stabilisation course for PTSD clinically beneficial.
Participants highlighted the beneficial contribution of the group format of the stabilisation intervention. For example, participants reflected that ‘hearing from others’ helped normalise their emotions and trauma-related symptoms. In addition, several participants reflected that the group format provided peer support and a sense of no longer feeling ‘alone’. Similar findings have been demonstrated in other studies (Dorrepaal et al., Reference Dorrepaal, Thomaes, Smit, van Balkom, Veltman, Hoogendoorn and Draijer2012; Krupnick et al., Reference Krupnick, Green, Stockton, Miranda, Krause and Mete2008) and are consistent with high levels of patient satisfaction and perceived benefit from attending group therapy for PTSD (Mott et al., Reference Mott, Sutherland, Williams, Lanier, Ready and Teng2013; Sloan et al., Reference Sloan, Gallagher, Feinstein, Gayle Beck and Keane2013).
However, not all PTSD patients find group interventions acceptable (Kracen et al., Reference Kracen, Mastnak, Loaiza and Matthieu2013), which is reflected in an uptake rate of about 50% from our waitlist individuals. This suggests that many PTSD patients we approached potentially preferred one-to-one interventions, although we have not explicitly assessed this in our study. In previous research, barriers to group format have included concerns about expressing emotions within a group setting, stigmatisation by the group, general disliking of the group composition and concerns about group participation (Kracen et al., Reference Kracen, Mastnak, Loaiza and Matthieu2013)
Additionally, our study’s treatment drop-out rate of 35% was higher than for average PTSD therapies (Lewis et al., Reference Lewis, Roberts, Gibson and Bisson2020). However, many of our participants (69%) had high symptom severity and complex presentations, which has been acknowledged as a contributor to higher drop-out (Dorrepaal et al., Reference Dorrepaal, Thomaes, Smit, van Balkom, Veltman, Hoogendoorn and Draijer2012; Gene-Cos et al., Reference Gene-Cos, Fisher, Ogden and Cantrell2016; McDonagh et al., Reference McDonagh, McHugo, Sengupta, Demment, Schnurr, Friedman, Ford, Mueser, Founder and Descamps2005; Vogel et al., Reference Vogel, Braungardt, Kaul and Schneider2017). Given that stabilisation is hypothesised to improve treatment drop-out (Lewis et al., Reference Lewis, Roberts, Gibson and Bisson2020) and given that services such as Plymouth Options deliver recovery-orientated psychological therapy, further improvement of uptake and attrition is important for this population and warrants further research. This study’s participants provided suggestions on how to make the groups more accessible and inclusive. Recommendations included small group sizes and suitable timings for those in work and involving families in the psychoeducation. This feedback highlights the importance of working closely with service users to address barriers to attending our group-based course.
Preliminary clinical benefit
Our stabilisation group for waitlist individuals was aimed at reducing the burden for patients with more complex PTSD presentations by preventing symptom deterioration whilst they waited for NICE-recommended individual trauma-focused treatments.
In line with our hypotheses, there was minimal deterioration in depression (PHQ-9) and anxiety (GAD-7). This aligns with previous research where a 10-week psychoeducational programme aimed at survivors of complex sexual abuse found no changes in participants’ rated symptoms of depression and anxiety (Karatzias et al., Reference Karatzias, Ferguson, Chouliara, Gullone, Cosgrove and Douglas2014).
Interestingly, we found a statistically reliable reduction in PTSD symptoms with a medium effect for intent-to-treat and a large effect for per-protocol analyses. This suggests that the programme went beyond the stabilisation of post-traumatic stress for the majority of patients. This contrasts earlier research into stabilisation treatments for PTSD, which found that evidence for stabilisation treatment is weak (De Jongh et al., Reference De Jongh, Resick, Zoellner, van Minnen, Lee, Monson, Foa, Wheeler, ten Broeke, Feeny, Rauch, Chard, Mueser, Sloan, van der Gaag, Rothbaum, Neuner, de Roos, Hehenkamp and Bicanic2016; Melegkovits et al., Reference Melegkovits, Blumberg, Dixon, Ehntholt, Gillard, Kayal, Kember, Ottisova, Walsh, Wood, Gafoor, Brewin, Billings, Robertson and Bloomfield2023). Other research has proposed that attending stabilisation programmes facilitated increased knowledge and understanding of PTSD, which can be accompanied by a significant reduction in trauma-related symptoms (Cloitre et al., Reference Cloitre, Koenen, Cohen and Han2002; Dorrepaal et al., Reference Dorrepaal, Thomaes, Smit, van Balkom, van Dyck, Veltman and Draijer2010).
It is important to note that the intervention was aimed at stabilisation only. Although two participants entered ‘recovery’ on the IES-R, it is expected that ‘recovery’ would usually be achieved through one-to-one trauma-focused intervention. This is congruent with findings from several meta-analyses, demonstrating that the largest reductions in trauma symptoms are achieved through individual trauma-focused interventions that include detailed trauma processing (Bisson et al., Reference Bisson, Roberts, Andrew, Cooper and Lewis2013; Ehring et al., Reference Ehring, Welboren, Morina, Wicherts, Freitag and Emmelkamp2014; Watts et al., Reference Watts, Schnurr, Mayo, Young-Xu, Weeks and Friedman2013). In addition, the findings of Bicanic et al. (Reference Bicanic, de Jongh and Broeke2015) and Melegkovits et al. (Reference Melegkovits, Blumberg, Dixon, Ehntholt, Gillard, Kayal, Kember, Ottisova, Walsh, Wood, Gafoor, Brewin, Billings, Robertson and Bloomfield2023) suggested that stabilisation cannot be viewed as a stand-alone intervention that replaces the core components of reprocessing the trauma memory.
Our findings of clinically beneficial symptom reduction could indicate that some trauma-focused elements of the group, such as psychoeducation, affect regulation skills, reclaiming life and the role of thought suppression in PTSD, facilitated an effect beyond stabilisation. These elements are key components of NICE-recommended PTSD treatments. Although the effect size consideration warrants some caution due to the small and self-selecting participant sample, trauma-focused symptom management, as facilitated in the group, could have enabled participants to reduce some cognitive and emotional avoidance, allowed individuals to reappraise and process aspects of their trauma memory in a more adaptive way and to start challenging some unhelpful threat appraisals. In line with the cognitive model of PTSD (Ehlers and Clark, Reference Ehlers and Clark2000), the group’s trauma focus could have addressed some of the maintenance factors of PTSD in our sample. The results that 75% of participants who completed the programme reported that they felt more confident in their ability to manage their symptoms of PTSD by using the course interventions supports this conclusion. Whilst these results are promising, caution should be used when interpreting them, given the naturalistic nature of this study and that there is no control group for comparison.
Finally, during the intervention, we observed reliable symptom deterioration of depression, anxiety and PTSD in a small subsample. Only 36% of randomised control trials for trauma-focused treatments for PTSD reported adverse effects or specifically analyse symptom deterioration, but a recent meta-analysis revealed that trauma-focused treatments are generally safe (Hoppen et al., Reference Hoppen, Lindemann and Morina2022). Data for stabilisation treatments’ adverse effects or symptom deterioration are even scarcer. Melegkovits et al., (Reference Melegkovits, Blumberg, Dixon, Ehntholt, Gillard, Kayal, Kember, Ottisova, Walsh, Wood, Gafoor, Brewin, Billings, Robertson and Bloomfield2023) reported 11% and 8% of patients showed deterioration in PTSD and depression, respectively, during the stabilisation phase compared with about 3% and 2% during the trauma-focused phase. Waitlist deterioration in PTSD symptoms has been described in 8–11% (Jayawickreme et al., Reference Jayawickreme, Cahill, Riggs, Rauch, Resick, Rothbaum and Foa2017; Hoppen et al., Reference Hoppen, Lindemann and Morina2022). Deterioration rates in our study ranged between 4% for PTSD and 9 and 11% for anxiety and depression and were thus smaller than empirically observed waitlist for PTSD and comparable to other stabilisation (Melegkovits et al., Reference Melegkovits, Blumberg, Dixon, Ehntholt, Gillard, Kayal, Kember, Ottisova, Walsh, Wood, Gafoor, Brewin, Billings, Robertson and Bloomfield2023) or waitlist findings for depression (Jayawickreme et al., Reference Jayawickreme, Cahill, Riggs, Rauch, Resick, Rothbaum and Foa2017; Hoppen et al., Reference Hoppen, Lindemann and Morina2022). Although we can cautiously conclude that our group waitlist intervention is almost as safe as trauma-focused therapy and safer than previous stabilisation or waitlist for PTSD symptoms, the importance of understanding mechanisms of symptom deterioration in health interventions has recently been emphasised (Bonell et al., Reference Bonell, Jamal, Melendez-Torres and Cummins2015). Further research evaluating this group needs to study adverse effects, deterioration, and engagement in evidence-based treatments to establish cost–benefit analyses.
Limitations and strengths
This study had some important limitations. First, the overall sample size was small, and only limited statistical analyses were possible. It is important to note that this analysis only considered those who completed the intervention, so we must exercise caution when interpreting the results. Second, as the experimental design did not include a control group, it is impossible to say for certain that participant improvement was solely attributable to the intervention. Reports about improved PTSD symptom management support interpreting our findings but do not ecologically validate them. Similarly, no controls were established for external factors such as medication, social, employment or personal factors, which may have contributed to the patient’s improvement.
Third, only those participants who completed the programme were able to fill out the PEQ, as this was administered at the final session. In addition, no other party was available to participate in the content analysis coding, highlighting potential reliability biases regarding coding themes and common responses. A qualitative semi-structured interview approach of a sample of all invited to participate in the programme may have been more effective in allowing a broad range of emerging themes to be explored relating to the acceptability of the intervention and to understanding what aspects of the treatment contributed to its beneficial effects or prevented them.
With regard to measurement tools, the International Trauma Questionnaire (Cloitre et al., Reference Cloitre, Shevlin, Brewin, Bisson, Roberts, Maercker, Karatzias and Hyland2018) was not yet published when the study started. It would have been an excellent clinical measure to have used alongside the other routine outcome measures as it is the only validated measure for the assessment of ICD-11 CPTSD.
Despite these limitations, the study is the first published evaluation of group stabilisation intervention delivered within an IAPT setting to service users waiting for individual therapy. Furthermore, given the study’s naturalistic design, the findings have high external validity and are applicable to NHS primary-care settings and relevant for clinical service provision.
Conclusions and recommendations for future research
The present study provides preliminary evidence for the acceptability and clinical benefit of attending a stabilisation group whilst waiting for one-to-one trauma work. This is particularly beneficial for IAPT services receiving extremely high referrals of complex presentations of PTSD where waits for treatment may be lengthy. Future research should follow up patients of the stabilisation group to explore whether they continued to benefit in their recovery journey. The group delivery also required IAPT resources in the form of therapist time. Thus, future research should include a cost–benefit analysis.
Supplementary material
The supplementary material for this article can be found at https://doi.org/10.1017/S1352465823000486
Data availability statement
The full data set is available on request from the corresponding author.
Acknowledgements
We would like to thank our colleagues Justine Hall and Michael Geldard for their patience and support with the development and running of Plymouth Options Overcoming and Processing Trauma Course. We would also like to thank Plymouth Options for embracing change and endorsing the commissioning of the programme, as well as supporting its evaluation. Finally, we would like to express our sincere thanks to Dr Ian Frampton for his guidance and support during this project.
Author contribution
Michelle Wells: Conceptualization (lead), Data curation (lead), Formal analysis (lead), Funding acquisition (lead), Investigation (lead), Methodology (lead), Project administration (lead), Writing – original draft (lead), Writing – review & editing (equal); Anke Karl: Conceptualization (supporting), Data curation (supporting), Formal analysis (supporting), Methodology (supporting), Writing – review & editing (equal); Rachel Handley: Conceptualization (supporting), Formal analysis (supporting), Methodology (supporting), Writing – review & editing (supporting).
Financial support
This research was undertaken as part of a MSc and was partially supported by Livewell Southwest Professional Training Department and by Ministry of Defence Enhanced Learning Credits, CAN No. 303421.
Competing interests
The authors declare none.
Ethical standard
The study was brought to the Trust’s local R&D Committee and was approved as a service evaluation, not requiring full NHS ethical approval in accordance with the NHS National Research Ethics Service guidance (National Health Service Research Authority, 2011). The University of Exeter granted ethical approval for the evaluation. A data-sharing agreement was established between the Trust and the University of Exeter to ensure strict data anonymity and protection prior to evaluation. No personally identifiable information is contained within this study. All participants gave informed consent to participate and for the findings of the service evaluation to be published. All authors have abided by the Ethical Principles of Psychologists and Code of Conduct set out by the BABCP and BPS. All participants were informed that they could withdraw from the group at any time without affecting their care, treatment, or place on the waitlist.
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