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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT03852706
Other study ID # 206789
Secondary ID 25911
Status Terminated
Phase N/A
First received
Last updated
Start date March 1, 2019
Est. completion date March 25, 2022

Study information

Verified date March 2022
Source University of Dublin, Trinity College
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This study's primary objective is to perform a randomized controlled pilot study to assess the feasibility of using EEG-based neurofeedback to reduce the severity of treatment-resistant auditory verbal hallucinations ('hearing voices') in patients diagnosed with schizophrenia. Patients will be randomized to receive either EEG-based neurofeedback or treatment-as-usual.


Description:

Auditory verbal hallucinations (AVH) are experienced by up to 80% of patients diagnosed with schizophrenia, where they can cause significant occupational and social impairment. Current treatments are incompletely effective. Around 25-30% of AVH are refractory to antipsychotic drugs, and cognitive behavioural therapy only shows a small-medium effect size. Initially promising studies of neurostimulation have shown smaller effect sizes as better controlled trials have been conducted. There is hence the need for innovative new treatments. One potential option is neurofeedback training. The primary objective of study is to perform a randomized, controlled, rater-blinded pilot trial (n=40) of EEG neurofeedback for AVH in patients with treatment-resistant schizophrenia, to assess trial process, which will then inform a future definitive trial. The secondary objective is to calculate a 95% confidence interval that will allow interpretation of statistical difference between neurofeedback and treatment-as-usual groups to assess neurofeedback for reducing auditory verbal hallucinations. Participants will be randomly allocated to either a neurofeedback (plus treatment-as-usual) or treatment-as-usual alone condition. Neurofeedback will employ Z-score based LORETA (Low Resolution Brain Electromagnetic Tomography). After a baseline assessment, twenty sessions of personalized neurofeedback training will be delivered over a period of approximately four months. This is the first registered trial of EEG neurofeedback for hallucinations. The primary focus of the pilot trial is on feasibility. However, a 95% confidence interval will be determined for the difference on PSYRATS-AH and AHRS scores between neurofeedback and treatment-as-usual to help inform a future definitive trial.


Recruitment information / eligibility

Status Terminated
Enrollment 4
Est. completion date March 25, 2022
Est. primary completion date March 25, 2022
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: - Are = 18 years old - Have a clinical diagnosis of a schizophrenia-spectrum disorder - Have been experiencing auditory verbal hallucinations for at least one year - Score 2 or more on the frequency item of the auditory hallucinations subscale of the Psychotic Symptom Ratings Scale (PSYRATS-AH; Haddock et al., 1999) at time of initial assessment (representing voices occurring at least once a day) - Are deemed refractory to antipsychotic treatment (defined as still hearing voices despite 4-6 weeks of treatment with two different antipsychotics) - Have been on a stable dose of antipsychotic medication for the three months prior to study enrolment - Are right-handed, as determined by the Edinburgh Handedness Inventory (Oldfield, 1971) - Are able to provide written, informed consent. Exclusion Criteria: - Having a diagnosed substance abuse disorder - Prior head injury with loss of consciousness for more than five minutes - At immediate risk of harm to self or others.

Study Design


Related Conditions & MeSH terms


Intervention

Other:
LORETA
Twenty sessions of neurofeedback training using LORETA in combination with z-scores.
Treatment as usual
Treatment-as-usual

Locations

Country Name City State
Ireland Tallaght University Hospital / St. James' Hospital Dublin

Sponsors (2)

Lead Sponsor Collaborator
University of Dublin, Trinity College Actualise

Country where clinical trial is conducted

Ireland, 

Outcome

Type Measure Description Time frame Safety issue
Primary Recruitment rate We will measure how many patients were recruited into the trial per calendar month of active recruitment. 24 months
Primary Willingness of participants to be randomised. We will measure the proportion of patients who were entered in the trial but refused randomisation. 24 months
Primary Willingness of participants to complete assessments We will measure the proportion of participants who were entered into the trial and completed all baseline assessment measures. 24 months
Primary Drop-out rate: LORETA condition We will measure the proportion of patients who were entered into the trial, randomised to the neurofeedback condition, and dropped out of the study. 24 months
Primary Success of blinding of raters We will measure the proportion of blind raters who were correctly able to guess the group allocation of participants, and assess if this was greater than chance. 24 months
Primary Rates of adverse psychiatric events We will assess the proportion of patients entered into the trial who experienced adverse psychiatric events reported. 24 months
Primary Drop-out rate: Controls We will measure the proportion of patients who were entered into the trial, randomised to the control condition, and dropped out of the study. 24 months
Secondary Auditory Hallucination Subscale of the Psychotic Symptom Ratings Scale (PSYRATS-AH) The Auditory Hallucination Subscale of the Psychotic Symptom Ratings Scale (PSYRATS-AH; Haddock et al., 1999) is an 11-item measure of the severity of auditory verbal hallucinations. Total scores can range from 0 to 44 with higher scores indicating greater severity of auditory verbal hallucinations. The PSYRATS-AH has been found to have a four-factor structure (Woodward et al., 2014). These are Emotion (range 0-20), Physical (range 0-12), Cognitive (range 0-8) and Loudness (range 0-4). Higher scores on each of these subscales represents more severe auditory verbal hallucinations. We will assess between group differences in both the total and four factor scores of the PSYRATS-AH at end of therapy. End of intervention (~4 months)
Secondary Auditory Hallucinations Rating Scale (AHRS) The Auditory Hallucinations Rating Scale (AHRS; Hoffman et al., 2003) is a seven-item structured clinical interview, which assesses the severity of auditory verbal hallucinations in the past week. Its items assess frequency, reality, loudness, number, length, attentional salience (how demanding of attention the voice is) and distress level. Items are rated on unique scales. Total scores on this measure can range from 0 - 41 . Higher scores represent more severe auditory verbal hallucinations. End of intervention (~4 months)
Secondary Delusions Subscale of the Psychotic Symptom Ratings (PSYRATS-D). Delusions will be assessed by the Delusions Subscale of the Psychotic Symptom Ratings Scale (PSYRATS-D; Haddock et al., 1999). This is a 6-item structured clinical interview. Total scores can range from 0-24, with higher scores representing more severe delusions. It has been found to have two factors (Woodward et al., 2014), namely Distress (distress amount, distress intensity) and Frequency (preoccupation amount, preoccupation duration, conviction, disruption). Total scores on these factors can range from 0-8 and 0-16 respectively, with higher scores representing more severe delusions. Both total PSYRATS-D and factor scores will be employed. End of intervention (~4 months)
Secondary Hospital Anxiety and Depression scale The Hospital Anxiety and Depression scale (HADS; Zigmund & Snaith, 1983) is a 16-item self-report measure of both anxiety and depression. Eight items assess depression and eight items assess anxiety. Depression scores can range from 0-24 with higher scores representing higher levels of depression. Anxiety scores can range from 0-24 with higher scores representing higher levels of anxiety. End of intervention (~4 months)
Secondary Quality of Life Enjoyment and Satisfaction Questionnaire Quality of life will be assessed by the short-form of the self-report Quality of Life Enjoyment and Satisfaction Questionnaire (QLESQ; Endicott et al., 1993). Total scores on 16-item measure can range from 14 to 70, with higher scores representing greater quality of life. End of intervention (~4 months)
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