Cognitive behavioural therapy for insomnia (CBTi) as a treatment for tinnitus-related insomnia: protocol for a randomised controlled trial

The insomnia literature offers the most useful definitions [24, 29], measures [24, 32, 33] and criteria for improvement [32, 34, 35], so far absent from the tinnitus literature. This will guide the definitions, measures and inclusion criteria used in this study.

Because tinnitus-related insomnia is common and associated with severe distress, it is important to test the most effective treatment. As yet, evidence for standard audiologically based care (ABC) for tinnitus-related insomnia does not exist, and whilst evidence for CBTi in a variety of health conditions is strong, it has not been tested in tinnitus. Robust testing will require a randomised controlled design. Because treatment intensity is different (CBTi involves six sessions, ABC rarely more than two) a third treatment arm involving six sessions of a supportive sleep group (SSG) will balance the CBTi contact time. Because tinnitus and insomnia are chronic conditions, a follow-up period of at least 6 months is required.

Participants will be adults with chronic distressing tinnitus and related insomnia. They will be randomly allocated to receive CBTi, ABC or SSG.

Participants are eligible if they report:

Participants will be excluded if they report:

Participants taking hypnotic or psychotropic medication at the point of consent will be asked to keep this stable for the duration of the trial and not to engage in additional psychotherapy.

The intention is to recruit 102 participants with distressing tinnitus and related insomnia from June 2017 to April 2019, which had been completed at the time of the proof-review of this article (November 2019). Participants will be identified from usual referral routes to the psychology service, where they will be informed of the trial as one option for care. To achieve adequate enrolment, the study will be advertised online via tinnitus charities, in print and web-based media outlets, across the hospital, and through regular briefings of local clinicians.

Participants responding to advertisements will complete basic eligibility screening with a clinical psychologist or research assistant using standardised measures of insomnia (ISI), tinnitus severity (Mini-TQ) and potential organic sleep disorders. If organic sleep disorder is indicated, a consultant in sleep medicine will manage queries, and onward referral will be advised as appropriate. If eligible, the GP will be informed and will have 3 weeks to ‘opt out’ of further care. Eligible individuals will be invited to attend a 1-hour full eligibility assessment with a clinical psychologist. Participants who are referred to the study by a clinician will complete eligibility criteria and the full assessment in the same appointment. If full eligibility is met, full informed consent will be collected by the clinical psychologist conducting the interview. The participants will receive sleep diary training and opt into Actiwatch (Philips Respironics, Murrysville, PA, USA) random allocation (one per group). They will be placed on a waiting list for randomisation, which will occur 3 weeks prior to intervention commencement. If eligibility is not met, alternative treatment or onward referral will be offered.

Treatment will be group-based, with group sizes including six participants, on average. Treatment will be delivered in cohorts, with three groups, one for each arm of the study, running in parallel. Randomisation will be done using a customised computer algorithm for each cohort separately. The study requires individual randomisation with stratification for gender. Within each cohort, stratification will be used to ensure groups are comparable in gender composition. Because group size will be small per cohort, it was decided that stratification for age was not appropriate to run per cohort. Instead, age differences will be checked post-randomisation per group to ensure there are no significant group differences in age in each cohort.

Randomisation of consented participants will take place 3 weeks prior to the commencement of intervention. Age, gender and participant number will be provided to an independent party, who will use a computer-based random number sequence generation to allocate group. Allocation information will be returned to the research assistant, who will then notify participants of their group allocation (group 1, 2 or 3). Participants will only be informed of the treatment associated with their group number when they arrive at the first session. It is not possible to blind participants or therapists to allocation; however, participants will be blind to the content of the other therapies. Statistical analysis will be conducted by an independent statistician who will be blind to group (i.e., provided with group number, not group type).

All interventions will take place in the same place, on the same day, at different times. The same two clinical psychologists will conduct all treatments together. They both have significant experience, skills and knowledge of working with chronic tinnitus, insomnia, group therapy, supportive interventions and CBTi. Treatment sessions will be 120 minutes in duration, and follow-up sessions will be 90 minutes in duration. There are three intervention options:

Treatment fidelity will be assessed by a clinical psychologist not involved in treatment. A random selection of treatment sessions will be recorded and assessed using a fidelity checklist. The two treating clinicians will discuss each session to assess fidelity independently of this, and breaches will be reported.

Participants will be recruited from August 2017 to April 2019, which had been completed at the time of proof-review of this article (November 2019). Screening will be followed by full psychological assessment. Outcome measures will be reported at baseline (3 weeks post-randomisation) and at 10 weeks (post-treatment), 14 weeks (1 month follow-up) and 34 weeks (6-month follow-up) post-randomisation. Figure 1 shows the Consolidated Standards of Reporting Trials (CONSORT) flow diagram for the study.

The rationale for the repeated measures will be indicated to encourage follow-up. Completed measures will be checked so that missing items can be minimised. Participants who do not attend all sessions will be contacted and asked to complete and return outcome measures. Participants who request to end participation in the trial will be invited to an individual follow-up session and offered further treatment outside of the trial if required.

Three screening measures will be used:

The primary outcome will be reduction of insomnia (ISI) and improvement in subjective sleep (diary) from 3 to 10 weeks, 14 weeks and 34 weeks post-randomisation. Daily sleep diaries will be completed by participants at home; questionnaire data will be completed independently in the treatment session and collected by the trial therapists.

Following treatment, participants will indicate the usefulness and relevance of treatment on 11-point Likert scales (0 to 10). They will be asked to provide qualitative feedback regarding their experiences and views of treatment.

A diagrammatic representation of the trial process (enrolment, intervention and assessment) is shown in the Standard Protocol Items: Recommendations for Interventions (SPIRIT) diagram (Fig. 2). For the full SPIRIT checklist, please see supplementary material Additional file 1.

We calculated the sample size required to test the primary hypothesis on the basis of a recent meta-analysis of 14 randomised controlled trials comparing CBTi with control groups in the treatment of primary insomnia [22]. Here, between-group comparisons reported effect sizes on subjective sleep variables (Cohen’s d) as ranging from medium (d = 0.44) to large (d = 1.09) across a range of control groups (including no intervention, placebo control, waiting list, treatment as usual and information controls). Similarly, medium to large effect sizes were seen on self-rating measures. When looking at treating insomnia in the context of a chronic health condition such as pain, similar moderate to large effect sizes are reported [27]. These findings have led us to base a power analysis on an assumed effect size of 0.8.

Estimation of potential loss to follow-up was set at 10%, based on rates reported by Okajima et al. [22], as ranging from 0% to 33% and as 8% from a clinical evaluation of CBTi within a tinnitus clinic [31]. We assumed a cluster design with six patients per group, and we assumed a within-group correlation of 7%, estimated from a previous study [31]. Correlation between measures was estimated as 25% on the basis of a small pilot study. It is likely that the true correlation will be higher, so this estimate has a conservative effect on required sample size. Assuming a significance level of 5% and 80% power, the number of participants needed to detect a statistically significant difference between the CBTi and ABC groups on the primary measures of interest was 34 per group (102 across all three groups).

The three groups will be compared at baseline on outcome measures and demographic information. Data will be reported as mean (SD) on continuous variables, (primary and secondary outcomes), and as percentage (number) for categorical data (demographic data, change in use of sound enrichment, medication, naps, caffeine, alcohol). A logistic model will be used to assess predictors of missing data and to examine all baseline characteristics and demographic variables.

The primary hypothesis to be tested is that CBTi will lead to a significantly greater reduction in insomnia in patients with tinnitus than usual care (ABC) from pre- to post-treatment and at follow-up, based on the primary outcomes of total ISI and 2-week average of SE and TST from a daily diary.

The ISI and sleep diary data will be analysed using linear mixed models, accounting for repeated measures on participants and the cluster structure of the trial. Post hoc comparisons of independent groups will allow multiple comparisons by using adjusted P values. We will also conduct an analysis to indicate the number needed to treat based on reliable change in the ISI.

Analysis will be based on modified intention to treat (excluding those who contribute no data). For data missing at random, multiple imputation will be used. To minimise missing data, the research assistant will follow up on missing data after questionnaire completion.

As for the primary analysis, a linear mixed model will be used to investigate differences in outcome between the three groups at additional time points (1-month and 6-month follow-up) and on all secondary outcome measures described above. In addition, correlational analyses will be used as a quality control to check for the level of association between actigraphy and sleep diary data, including TST, TWT, SOL and SE.

Regression analyses will be conducted to assess whether changes in the primary outcome measure (ISI, TST, SE) are associated with changes in sleep beliefs (DBAS-16) score.

Satisfaction will be assessed via a single three-group analysis of variance on treatment usefulness and relevance. Written responses will be analysed using thematic analysis. Treatment adherence will be assessed on the basis of attendance rates. Categorical outcomes, including adverse events and non-adherence, will be recorded, reported and compared with Fisher’s exact test.

Additional sensitivity analysis will be conducted as follows: outliers (analyses with and without outliers), non-compliance (a per-protocol analysis), baseline imbalance (analyses with and without adjustment for baseline characteristics, if imbalanced), and impact of distributional assumptions (analysis plan will assume a normal distribution for continuous outcomes, and this will be tested for goodness of fit in the analysis). In addition, sensitivity analyses will be conducted using other suitable distribution under further statistical advice.

The trial was retrospectively registered with ClinicalTrials.gov on 29 December 2017 (NCT03386123↗). Recruitment began in June 2017 and continued until April 2019. Before submitting the protocol, 78 of 102 participants (76%) had been consented and randomised, at the time of proof-review of this paper, 100% of participants had been consented and randomised. Current protocol version 5 is dated November 2018.

The datasets that will be generated and/or analysed during the current study will be held by the research team within UCLH. They will not be publicly available, owing to the ethical agreement obtained for this study and to maintain individual privacy.