Authors: I. Gardoki-Souto, O. Martín de la Torre, B. Hogg, D Redolar-Ripoll, L. Martínez Sadurní, M. Fontana-McNally, J. M. Blanch, W. Lupo, V. Pérez, J. Radua, B. L. Amann, A. Valiente-Gómez, A. Moreno-Alcázar
Categories: Study Protocol, Eye Movement Desensitization and Reprocessing, Fibromyalgia, Multifocal transcranial current stimulation, Pain, Psychological trauma, Randomized controlled trial
Source: Trials
Fibromyalgia (FM) is a generalized, widespread chronic pain disorder affecting 2.7% of the general population. In recent years, different studies have observed a strong association between FM and psychological trauma. Therefore, a trauma-focused psychotherapy, such as Eye Movement Desensitization and Reprocessing (EMDR), combined with a non-invasive brain stimulation technique, such as multifocal transcranial current stimulation (MtCS), could be an innovative adjunctive treatment option. This double-blind randomized controlled trial (RCT) analyzes if EMDR therapy is effective in the reduction of pain symptoms in FM patients, and if its potential is boosted with the addition of MtCS.
Ninety-six patients with FM and a history of traumatic events will be randomly allocated to the treatment as usual (TAU) condition, EMDR + active-MtCS condition, or EMDR + sham-MtCS condition. Therapists and patients will be kept blind to MtCS conditions, and raters will be kept blind to both EMDR and MtCS. All patients will be evaluated at baseline, post-treatment, and follow-up at 6 months after post-treatment. Evaluations will assess the following sociodemographic data, pain, psychological trauma, sleep disturbance, anxiety and affective symptoms, wellbeing, self-care, emotional regulation, self-esteem, and cognitive functioning.
This study will provide evidence of whether EMDR therapy is effective in reducing pain symptoms in FM patients, and whether the effect of EMDR can be enhanced by MtCS.
This trial was registered at ClinicalTrials.gov on 2 August 2019, NCT04084795.
The online version contains supplementary material available at 10.1186/s13063-024-08708-3.
Keywords: Fibromyalgia, Eye Movement Desensitization and Reprocessing, Multifocal transcranial current stimulation, Psychological trauma, Pain, Randomized controlled trial
Fibromyalgia (FM) is a chronic pain (CP) disorder characterized by generalized and widespread pain, sleep disturbance, fatigue, cognitive dysfunction, and affective symptoms. The average prevalence of FM worldwide is 2.7%, affecting mainly female patients [1]. Although the etiology of FM remains unknown, it is currently conceptualized as a disorder involving the sensitization of the central nervous system (CNS) and impairments in endogenous pain inhibitory mechanisms, with genetic, hormonal, and immunological factors playing a role [2]. Different risk factors associated with FM onset have been highlighted, including the presence of traumatic experiences such as sexual and physical abuse, chronic stress, and adverse lifetime events [3–5]. In fact, posttraumatic stress disorder (PTSD) is considered an important and frequently present comorbidity in patients suffering from FM [6, 7], although it is often not given priority as a treatment objective. While the mechanism which links adverse events to FM development is not fully understood, evidence shows that allodynia and hyperalgesia can be stress-induced [8], and psychological trauma is thought to lead to dysregulation of the hypothalamic–pituitary–adrenal (HPA) axis, linked to the aberrant cortisol secretion and epigenetic mechanisms [3, 4]. Therefore, psychological therapies focused on adaptive processing of traumatic experiences may improve both somatic and psychological symptoms and could be an innovative treatment option for FM.
Eye Movement Desensitization and Reprocessing (EMDR) is an integrative psychotherapeutic approach developed by Francine Shapiro at the end of the 1980s. While there is ongoing debate regarding the evidence for EMDR in treating PTSD [9], an individual data participant meta-analysis by the same group found no significant differences between EMDR and other trauma-focused interventions, such as trauma-focused cognitive behavioral psychotherapy [10]. Moreover, It has been recognized by the World Health Organization as a first-line therapeutic tool for PTSD [11] due to its efficacy in reducing clinical symptoms, evidenced in several meta-analyses in both adults [12–16] and children and adolescents [17, 18]. EMDR has shown its clinical applicability in the treatment of other pathologies, such as addictions [19], depression [20], anxiety [21], and CP [22]. In this last case, to date seven randomized controlled trials (RCT) have investigated the efficacy of EMDR in different conditions of CP: chronic pain [23], migraine headaches [24], chronic back pain [25], pain due to rheumatoid arthritis [26], acute pain after abdominal surgery [27], and pain due to FM or diffuse chronic pain [28]. These studies showed EMDR significantly reduced pain levels in comparison with TAU [23, 25–27] and in comparison with other treatment options, for example, standard pharmacology [24], guided imagery [26], or eclectic therapy [28]. Additionally, some systematic reviews also show positive outcomes for EMDR in non-PTSD conditions. Scelles and Bulnes [29] reported overall positive outcomes for EMDR in most cases (addictions, somatoform disorders, sexual dysfunction, eating disorders, personality disorders, mood disorders, pain, neurodegenerative disorders, sleep, etc.) and even being successful in usually difficult or unproductive cases (e.g., dementia or aphasia). Regarding pain specifically, Tesarz et al. [30]’s results suggest that EMDR may be a promising treatment line for chronic pain conditions with controlled trials demonstrating significant improvements in pain intensity, disability, depressive, and anxiety symptoms. However, the studies on this topic are few and contain methodological biases, such as a lack of active control subjects, variability in PTSD and depression diagnoses, and the high associated comorbidity.
Given the complex etiology of FM, combining psychotherapy with other treatment options might increase the effectiveness of the treatment and maximize therapeutic success. Due to the key role that CNS sensitivity plays in FM, pioneering non-invasive brain stimulation (NIBS) techniques, such as multifocal transcranial current stimulation (MtCS), are increasingly being investigated, as these can modify neural activities related to pain. This neurophysiological technique represents a promising intervention option, given its capacity to modulate cerebral excitability in a safe, not invasive, and painless manner [31]. The principal mechanism of action of MtCS is a subthreshold modulation of neuronal membrane potentials, modifying cortical excitability and activity dependent on the current direction of flow through the target neurons [32]. Based on this, MtCS modulates spontaneous neuronal activity without generating activity changes in resting neuronal networks [33], its effects depending on the previous state of physiological basal activity of the region of interest [34].
There is increasing evidence which shows that, in addition to psychotherapeutic and pharmacologic interventions, MtCS is useful in treating FM and CP in terms of inducing pain relief and improving quality of life [35–49]. Interestingly, MtCS can also increase the therapeutic potential of other therapies when used in conjunction with them [50]. In this regard, a recent review has shown that the combination of MtCS with Cognitive Therapies, such as Cognitive Control Therapy (CCT), increases its benefits when used for treating depressive disorders [50].
Taking into account the information presented above, we hypothesize that the combination of a trauma-focused therapy, such as EMDR, combined with MtCS targeted in the left dorsolateral prefrontal cortex (lDLPFC) could be a useful therapeutic option [51] for the treatment of patients with FM. The main reasons for selecting the lDLPFC are as (1) this region is critical in the regulation of the limbic system, implicated in emotion, which is hyperactivated in traumatized patients [52]; (2) it has been seen to be relatively hypoactivated in patients with depression [52–54], anxiety disorders [53, 54] and PTSD [55]; (3) there is a proved efficacy of lDLPFC MtCS in the treatment of resistant and non-resistant depression [50, 55], which suggests that FM patients will also benefit due to their comorbidities; (4) the lDLPFC also plays a central role in executive functions [56], and MtCS has the potential to improve cognitive functions associated with cortical plasticity, such as therapy-related learning processing [57].
Although in two studies it was found that the application of MtCS on the lDLPFC was generally less effective in reducing pain in FM patients compared to the application of stimulation on the primary motor cortex [43, 49], other studies were able to demonstrate a short-term efficacy in terms of pain and life quality [38], pain and fatigue [41], and pain and improvement in executive attention and orientation [37]. In all the studies mentioned, the stimulation applied over lDLPFC was anodal.
Regarding the mechanisms underlying the effects of DLPFC/tDCS, while no studies have specifically explored them, it is plausible that the cognitive and affective effects of DLPFC stimulation could be induced through the connections with the limbic system (fronto-limbic network) [58]; while the effects on pain relief could be due to connectivity with the Diffuse Noxious Inhibitory Controls (DNIC) pathways that are involved in the inhibitory modulation of nociceptive input [59, 60].
Recently, multifocal transcranial current stimulation (MtCS) devices have been used to achieve more focal stimulation of specific cortical targets, because they use smaller electrodes compared to MtCS devices. Different methods have been designed to optimize the configuration of MtCS montage for stimulation of brain networks, represented by spatially extended cortical targets [61]. In this sense, MtCS could be more effective in modifying the functioning of the networks that are altered in patients with FM [58–60]. Previous studies with MtCS in FM have focused on the DLPFC; however, the effects of modulating the activity of this area with MtCS have not yet been explored.
The main objective of the study is to analyze whether EMDR therapy is effective in the reduction of pain symptoms in FM patients, and if its potential is boosted with the addition of MtCS. As secondary objectives, the study will analyze whether EMDR therapy is effective in reducing psychological trauma symptoms and comorbid symptoms of anxiety and depression, and in improving sleep quality and patient wellbeing, and if these effects are boosted by the addition of MtCS.
Within a double-blind randomized controlled design, patients will be randomized to (1) Waitlist Condition, 92) EMDR + active-MtCS (20 sessions), or (3) EMDR + sham-MtCS (20 sessions). All subjects will continue to receive their treatment as usual (TAU), regardless of the group to which they have been assigned during the study. If a participant does not attend 3 sessions consecutively, she will be withdrawn from the study. In this case, no follow-up will be carried out, all gathered data will be kept and used for pertinent analyses unless the patient rescinds their consent. If this is the case, all data will be erased. Psychotherapists and patients will be kept blind for MtCS treatment conditions until the end of the trial, and raters will be kept blind to both EMDR and MtCS conditions. It is not possible for patients to be blind to the EMDR condition due to its use of bilateral stimulation. The experimental condition assigned to the participants will only be revealed if the patient abandons the study. Otherwise, the blind condition will be maintained until the end of the study. All patients will be clinically evaluated at baseline, at post treatment and at 6 months from post treatment as follow-up.
Figure 1 shows a flow chart of the progress of the study.
Fig. 1 SPIRIT checklist—Flow Schedule of enrollment, interventions and assessments. t1 = Baseline evaluation; 0 = randomization process; t2 = Post-treatment evaluation; t3 = Follow-up evaluation; t4 = Waitlist group participants receive treatment; VAS pain = Visual Analog Scale for pain; PCS = Pain Catastrophizing Scale; FIQ-R = Fibromyalgia Impact Questionnaire; BFI = Brief Fatigue Inventory; CTQ = Childhood Trauma Questionnaire; EGEP-5 = Evaluación General del Estrés Postraumático; TTE = Timeline of traumatic experiences; PCL-5 = Posttraumatic Stress Disorder Checklist, ITQ = The International Trauma Questionnaire; SUD = Subjective Units of Distress; CDS = Cambridge Depersonalization Scale; SDQ-20 = Somatoform Dissociation Questionnaire, MINI = MINI International Neuropsychiatric Scale; HADS = Hospital Anxiety and Depression Scale; AIS = Athens Insomnia Scale; SWLS = Satisfaction With Life Scale; ERSQ = Emotion Regulation Skills Questionnaire; RSE = Rosenberg Self-Esteem Scale; SCIP = Screen for cognitive impairment in psychiatry
This multicenter collaborative project will involve the participation of the Centre Fòrum Research Unit of the Hospital del Mar as the entity responsible for coordinating the study and carrying out the evaluations, the Rheumatology Department of Parc de Salut Mar for patient diagnosis and referral to the study, the Institut d'investigacions Biomèdiques August Pi i Sunyer (IDIBAPS) for randomization and data base management, and the Cognitive Neuro-Lab of Open University of Catalonia (UOC) for MtCS. External accredited EMDR psychotherapists, who have extensive experience and have received specific training for this study, will carry out the therapy, with supervision from the Centre Fòrum Research Unit (Barcelona, Spain). The study has been approved by the Ethics Committee of the IMIM, Parc de Salut Mar (2019/8772/I). All participants will sign the informed consent prior to enrollment in the baseline visit. Since this study involves a low-risk intervention, a Data Monitoring Committee will not be considered. However, AV (PI) and BA (co-PI) will be in charge of assessing the progress of the trial, data safety and, if needed, may access unblinded study information during the duration of the study in order to provide recommendations regarding study modification. Any deviation from the initial protocol will be communicated to the Ethics Committee through an official statement as well as to the Clinical Trials register.
The patient sample will consist of 96 females who have been diagnosed by the Rheumatology Department of the Hospital del Mar, Barcelona, Spain, through a clinical interview aligned with the 2016 American College of Rheumatology criteria for FM. According to the CDC [62], FM is twice as likely to happen to women than men. However, in a population-based cross-sectional study by Font Gayà et al. [63] evaluating the prevalence of fibromyalgia and associated factors in Spain, the distribution by sex prevalence was 4.49% in women (95% CI, 3.76–5.35); significantly higher than the 0.29% in men (95% CI, 0.14–0.60). Our own cross-sectional study about trauma prevalence in FM was offered to both sexes, but only female patients were finally referred and included [64]. As the distribution in the study’s country is so skewed towards the female population, we decided to include female patients only. Patients with this diagnosis will be referred from the Rheumatology Department, Anxiety Disorders Unit, Adult Mental Health Centers, and other departments of the Hospital del Mar. When a participant meets the study criteria, she will be informed about the study and asked whether she would like to participate. Once she accepts, the raters will contact her to schedule the baseline visit and then she will be randomized to one of the groups. Inclusion criteria will be as (1) aged between 18 and 70 years, (2) mean pain score of at least 4 on the visual analog scale for pain (VAS pain ≥ 4) in the two weeks preceding the clinical trial, (3) presence of one or more traumatic events causing current trauma-related symptoms (detection of at least one traumatic event using the EGEP-5 initial list of traumatic events), (4) current clinical symptoms of depression and/or anxiety (Hospital Anxiety and Depression Scale ≥ 8), (5) stable medication regime over the previous 2 weeks, and (6) met internationally-established MtCS safety criteria [65]. Exclusion criteria will be as (1) comorbid autoimmune or chronic inflammatory disease, (2) neurological or serious medical diseases, (3) bipolar disorder, schizoaffective disorder, or schizophrenia, (4) suicidal ideation, (5) previous EMDR therapy, (6) substance abuse/dependency within 1 month prior to participation (except for nicotine abuse/dependency), (7) pending FM-related litigation or disability, (8) metallic implants in the head, or (9) pregnancy.
The main analysis will be the comparison between patients assigned to EMDR vs those not assigned to EMDR. The secondary analysis, only amongst patients assigned to EMDR, will be the comparison between patients assigned to active-MtCS vs patients assigned to sham-MtCS. Therefore, the individuals will not randomly be assigned to one of the three arms. Instead, the patients meeting the inclusion criteria will be randomized first to EMDR vs non-EMDR, and then those in the EMDR group to active-MtCS or sham-MtCS. For the sake of brevity, only the randomization to EMDR vs non-EMDR is described here, because the randomization to active-MtCS vs. sham-MtCS is identical. The variables used for the randomization will be age, educational level, and pain intensity score. The first two patients will be randomly allocated to EMDR with p = 2/3. For each subsequent patient, the following biased coin algorithm will be if a group includes at least two more patients than it would have to have to maintain the ratio 2 EMDR / 1 control, the patient will be randomly assigned to the other group with p = 0.6. Otherwise, there will be a simulation of the new patient as it was allocated to EMDR and calculate the between-group standardized difference in pain intensity variable, then simulate that the new patient is allocated to non-EMDR and recalculate the difference, and finally randomly allocate the patient to the group associated to the smallest difference with p = 0.6. This strategy decreases prognostic imbalances between groups because it decreases differences in potential co-founders, yet still includes randomization.
Once the randomization group has been obtained, the principal investigator (PI) of the study will inform the participants accordingly. If the participants have been assigned to the EMDR group, the coordinator will also contact the therapist responsible of the treatment.
EMDR therapy will consist of a maximum of 20 individual 60-min sessions of psychotherapy, principally using the EMDR protocol for FM [66]. This protocol begins by gathering information about all aspects of the patient related to FM (phase 1) and helps create a hierarchy of the targets that are going to be processed during the sessions (phase 2). The following phases (3 to 8) follow the same steps as the EMDR Standard protocol [67]. The protocol is briefly described
When a patient appears to suffer intense pain during the regular EMDR session, and the pain is threatening the patient’s processing, the CP protocol will be used. Here, the target chosen is the current pain referred to by the patient. The main differences between the FM and the Pain protocols are the in phase 3, the patient must describe the pain felt and draw a representation of it, as well as assigning it personal characteristics; after phase 6, when improvements in levels of pain occur, the patient alongside the therapist will build a positive resource in order to reinforce the positive progress. It will then be followed by phases 7 and 8 of the standard protocol mentioned. Below is a brief description of the CP
It is important to mention that this psychological intervention does not usually cause any risk to the health of the participants. However, due to remembering and reprocessing past traumatic experiences, it is possible that emotional discomfort will be felt during the evaluation and the therapeutic sessions. This discomfort usually disappears before the end of a session or, in exceptional cases, can also continue in the following day. If the discomfort continues, a new session with the patient should be immediately scheduled to assist her.
Would adverse effects other than those related to emotional discomfort from the therapeutic sessions occur, these shall be reported to the PI of the project. Additionally, if it is likely considered that EMDR was the cause, they will also be reported to the Ethics Committee department and relevant regulatory bodies, as required, indicating expectedness, seriousness, severity, and causality. However, as no problems that are detrimental to the participant are anticipated, no interim analyses or formal stopping rules have been planned.
Throughout the duration of the study, no participant may receive trauma-focused therapy sessions in parallel.
Multifocal transcranial current stimulation (MtCS) montage (F3 anodal; Fp1, F7, Fc5, AF3, Fc1, Fz return) will be used with the anode over the lDLPFC. This montage, guided by StarStim® computational modeling data (see Fig. 2), was planned with the intention of enhancing the activity of the lDLFPC. Active stimulation will consist of 2 mA MtCS for 20 min applied immediately before EMDR sessions. The same protocol and montage will be used for sham stimulation, but the protocol will be implemented by ramping down (slowly) the current immediately after the ramp up period, and by ramping up (slowly) the current right before the final ramp down portion of the session. This way, the subject will feel the ramp up and ramp down events, but will not receive a significant dose of stimulation. Thus, the patient will believe she is being stimulated normally, but there should not be any real effects, in order to control for placebo effects of the MtCS treatment. The device used will be the StarStim®, which is a wireless hybrid EEG/tCS 8-channel neurostimulator system. StarStim® is currently classified as an investigational device under US federal law.
Fig. 2 Multifocal transcranial Current Stimulation (MtCS) montage
In the case of patients who have been prescribed medication with effects on the nervous system, such as antidepressants, anxiolytic drugs, anticonvulsants, or atypical antipsychotics, an individualized follow-up of the clinical outcomes will be carried out to ensure that there is no interaction with the brain stimulation [31]. Although the application of MtCS is painless, in the event that a participant, due to her medical condition, feels marked pain or very significant discomfort due to the application of the stimulation and asks to stop the stimulation, this decision will be respected and the participant will receive EMDR treatment only. Again, if other different adverse effects than those mentioned above occur, they will be reported to the PI, and, in the event they are considered to be related to MtCS, also to the Ethics Committee department and relevant regulatory bodies as required, indicating the expectedness, seriousness, severity, and causality of the adverse effect. However, as has been mentioned previously, no problems that are detrimental to the participant are anticipated, meaning no interim analyses or formal stopping rules have been planned.
During the time of the study, no participant may receive MtCS sessions in parallel.
The patients allocated to this condition will follow their usual treatment without receiving any other additional therapy. Treatment as usual consists of regular visits with the rheumatologist, psychiatrist, and general practitioners, who are responsible for prescribing and monitoring the pharmacological treatment, principally in form of analgesics such as non-steroidal anti-inflammatory drugs, opioids, paracetamol, and/or gabapentin, but also antidepressant drugs and anxiolytics/hypnotics. Health psychoeducation by the nursing service and therapeutic physical exercise are also included in the waitlist condition.
Demographic and clinical variables will be collected through a clinical interview using the medical history of the patients and a specific Case Report Form (CRF) designed for the study which will include age, educational level, personal and family history, drug use, current pharmacological treatment, and previous psychological treatment. We will also use the MINI International Neuropsychiatric Interview [68], Spanish validation [69] to explore the principal psychiatric disorders from Axis I of DSM-IV and CIE-10.
Pain intensity will be assessed using the following
Psychological trauma and trauma-related symptoms will be evaluated using the following
Anxiety and depression will be assessed using the following
Quality of sleep will be assessed using the following
Wellbeing will be assessed using the following
Self-care will be assessed using the following
Emotional regulation will be assessed using the following
Self-esteem will be assessed using the following
Cognitive functioning will be assessed using the following
All patients will be clinically evaluated at baseline/enrollment (t1), post treatment (t2), and follow-up evaluation at 6 months from post-treatment (t3) (see Tables 1, 2, and 3). Personal participant data will be numerically coded and kept in a database in the Centre Forum Research Unit, who will be responsible for data maintenance and safety. Only the researchers involved in this trial will have access to this data. The database will contain the information of both the participants who finish the study as well as those who drop out, along with the corresponding causes for not completing the study. The Centre Forum Research Unit will be responsible for creating and maintaining the database.
The main tests of the study will consist of assessing whether patients assigned to EMDR show different levels in the pain intensity variable using a standard formula for two-tailed t-tests. The total sample size required to detect large to very large effect size differences (Cohen’s d ≥ 1) between three groups with a significance level of 0.05 and statistical power of 80% is 28. Assuming 15% dropouts, we will aim to randomize 96 patients, meaning 32 per group.
The distribution of the sociodemographic and clinical variables between groups at baseline will be summarized by descriptive statistics. We will use t-tests to compare pain levels at post-treatment and follow up between groups (Waitlist vs EMDR; active-MtCS vs sham-MtCS). In order to avoid regression toward the mean and confusion effects, baseline levels of pain will be added as covariates, as well as age, depression and anxiety severity and number of years of education. Due to the sample size no further analysis is expected. The statistical software used for the analysis will be R. For the principal statistical analysis an intention to treat (ITT) analysis will be used, and multiple imputation for losses at follow-up. The dataset analyses during the current study will be available from the corresponding author on reasonable request.
This scientific paper presents the first protocol of a double-blind RCT to investigate whether EMDR is effective in the treatment of FM and its comorbid symptoms, and if its potential is boosted with the addition of MtCS. Patients with FM can be a great clinical challenge for healthcare professionals, due to their high comorbidities and unexplained symptoms [102, 103]. The etiology of FM is poorly understood [104], consequently leading to an erroneous interpretation of the disorder and its manifestations, resulting in a pattern of excessive and non-beneficial therapy [105]. Patients usually feel frustrated about their treatment options [106] and dissatisfied with the support 38% of FM patients in Spain state that the public health system is the entity which gives them the least support, despite 72% of the FM patients only visiting doctors within this system. This lack of satisfaction with current diagnostic and treatment options could explain why 87% of FM patients prioritize scientific research as the means to a painless future [107]. It is the duty of researchers and clinicians to study precipitators and susceptible populations to build beneficial therapy protocols [4], and thus it is imperative to recognize the evidence showing the importance of the psychological trauma as a trigger in the development, maintenance, and chronification of FM, and provide suitable therapeutic options to address this.
This protocol is innovative in combining the EMDR approach for treating psychological trauma and reducing pain levels with MtCS. This approach should also help treat comorbidity, which, according to the results of recently published works, may also improve FM symptoms [105, 108–110]. The stress-related antecedents of FM include early-life traumas, PTSD, depression, anxiety, and major life stress [111]. Therefore, since traumatic events can predispose individuals to FM, mood, and anxiety disorders and influence mental and physical health [107, 110], the interventions appearing in this protocol seem beneficial.
Although there are several studies showing high comorbidity between FM and PTSD [4], very few studies have been carried out testing interventions targeting trauma-related comorbidity, and those which exist are of low quality [4], due to factors such as a lack of control subjects, variability in PTSD and depression diagnoses, and the high associated comorbidity [6]. Thus, this study will be a useful addition to the extant literature, and it will shed light on the possibility of developing a larger RCT using a new psychotherapeutic approach for the treatment of FM.
Some limitations of our trial have been taken into account. Firstly, the lack of control regarding drug treatment is a potential source of bias. To partly overcome this limitation, the current medication regimen should not be changed, as far as possible once patients have been included in the study. Secondly, this study only includes females. Further studies would be needed to see if the findings of this study can be replicated in the much lower proportion of male FM patients. Thirdly, this is an exploratory and pragmatic trial with a relatively moderate size, meaning findings will later need to be replicated in a larger sample. Finally, another possible limitation could be the scalability of the MtCS treatment.
In September 25th, 2019, we initiated a pilot study with the objective of enlisting 45 participants to be randomly assigned to one of three (1) EMDR + tDCS active (n = 15), (2) EMDR + tDCS sham (n = 15), or (3) TAU (n = 15). Unfortunately, the onset of the COVID-19 pandemic led to the suspension of the trial, as the intervention could not be administered remotely. Subsequently, AVG and BA secured funding for a randomized controlled trial (RCT) which allowed the previous pilot study to expanded to a full study, increasing the cohort to 96 patients. Additionally, author MFM was added as her involvement in this manuscript has been significant due to her current and future dedication to the project, which will be the main paper of her PhD. As for the change in outcomes (self-care, emotional regulation, self-esteem, and cognitive functioning), while reflecting on the population this study is targeting and other potential troubles they encounter, MFM and AMA hypothesized that the intervention should help in alleviating patient’s troubles in these areas. Therefore, evaluating these new outcomes is relevant in order to identify if EMDR therapy + MtDCS is an effective treatment for said aspects of general mental health.
The investigators want to thank to the EMDR therapists (TC, AA, MC, and KC) for their future implications in the present project and to the Spanish EMDR Association for the training support. AMA wants to thank to “Secretaria d′Universitats i Recerca del Departament d′Economia i Coneixement (2017 SGR 46 to “Unitat de Recerca del Centre Fòrum”), Generalitat de Catalunya (Government of Catalonia)” for the recognition as an emerging research group. VP wants to thank unrestricted research funding from “Secretaria d′Universitats i Recerca del Departament d′Economia i Coneixement (2017 SGR 134 to “Mental Health Research Group”), Generalitat de Catalunya (Government of Catalonia)”. He also acknowledges the continuous support by the CIBERSAM (Centro de Investigación Biomédica en Red de Salud Mental), Madrid, Spain. AVG wants to thank to Instituto Carlos III for supporting her research thanks to the Juan Rodés Research Contract (JR19/00001) in the period between 2020 and 2024. None of the acknowledged funders have played a part in the study design; collection, management, analysis, and interpretation of data; writing of the report; or in the decision of submitting the report for publication.
AMA and BLA had the idea of the project. IGS, VP, WL, BLA, and AMA contributed to the design of the study. AVG will be the coordinator of the study. OMT and DRR will apply MtCS stimulation to the patients. JR will carry out the randomization and all statistical analysis. IGS, BH, LMS, and MFM will blindly evaluate the participants. IGS wrote the first draft of the manuscript with the supervision of AMA and BLA. IGS, OMT, BH, DRR, AVG, LMS, MFM, JMB, WL, VP, JR, BLA, and AMA contributed to the revisions and modifications of the manuscript and all have approved the final version. No professional writers have been involved in the manuscript.
This work has been supported by a grant for AVG and BLA from the Plan Nacional de I + D + i and co-funded by the Instituto de Salud CarlosIII-Subdirección General de Evaluación y Fomento de la Investigación, Plan Nacional 2024–2026 with the following Research Project (PI23/00072).
Personal data of the participant will be numerically coded and kept in a database at the Centre Forum Research Unit. Only the researchers involved in the trial will have access to this data, however, the dataset analysis of the current study will be available from the corresponding author upon reasonable request. When the study finishes and results are obtained, we will send a copy of the article in Spanish to all, together with a plain language summary, as well as providing individual feedback about progress during the study if any participant requests it. The results of the study will also be published in peer review journals, and national and international conferences. The datasets analyzed during the current study will be available from the corresponding author on reasonable request.
The study has been approved by the Ethics Committee of the Parc de Salut Mar (2019/8772/I) and re-approved with all changes for the new study by the same Ethics Committe in April 10th 2024. All participants will sign the informed consent prior to enrollment in the baseline visit. The informed consent will be available from the corresponding author upon request. Details of the design of the trial can be also gathered from Supplementary Material (Standard Protocol Items: Recommendations for Interventional Trials [SPIRIT] Checklist and Schedule of enrolment, interventions and assessments [SPIRIT] Flow diagram). The trial is registered at ClinicalTrials.gov, NCT04084795 (2nd of August of 2019).
Not applicable.
BLA was the Research Committee Chair of EMDR Europe between 2017 and 2021 and has been invited as speaker to various national and international congresses of EMDR. AVG is member of the Research Committee of EMDR Europe since May 2023 until now. AMA is member of the Research Committee of the Spanish EMDR Organization since September 2023 until now. The other authors declare they have no competing interests.
Personal data of the participant will be numerically coded and kept in a database at the Centre Forum Research Unit. Only the researchers involved in the trial will have access to this data, however, the dataset analysis of the current study will be available from the corresponding author upon reasonable request. When the study finishes and results are obtained, we will send a copy of the article in Spanish to all, together with a plain language summary, as well as providing individual feedback about progress during the study if any participant requests it. The results of the study will also be published in peer review journals, and national and international conferences. The datasets analyzed during the current study will be available from the corresponding author on reasonable request.