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Trial registered on ANZCTR

Registration number

ACTRN12623001291673

Ethics application status

Approved

Date submitted

17/11/2023

Date registered

12/12/2023

Date last updated

1/06/2024

Date data sharing statement initially provided

12/12/2023

Type of registration

Prospectively registered

Titles & IDs

Public title

Assessing the Impact of Digital Cognitive Behavioural Therapy for Insomnia on Depression Symptoms and Processes in Young Adults.

Scientific title

Assessing the Impact of Digital Cognitive Behavioural Therapy for Insomnia on Depression Symptoms and Processes in Young Adults.

Secondary ID [1]

Nil

Universal Trial Number (UTN)

U1111-1300-1169

Trial acronym

Linked study record

Health condition

Health condition(s) or problem(s) studied:

Depression

Condition category

Condition code

Mental Health

Depression

Mental Health

Other mental health disorders

Intervention/exposure

Study type

Interventional

Description of intervention(s) / exposure

Digital Cognitive Behavioural Therapy for Insomnia (Digital CBTI).

Rationale: Digital CBTI (i.e., CBTI delivered in a digital format) is a well validated treatment for Insomnia. CBTI programs are known to effectively reduce symptoms of depression without directly targeting non-sleep symptoms. However, the mechanisms which underlie the association between improvement in insomnia and improvements in depression are not well understood. Many candidate mechanisms have been proposed (e.g., cognitive biases), yet, there is a lack of research which investigates these possible mechanisms, and data from treatment studies is greatly needed to investigate the causal role of these mechanisms in the association between insomnia and depression.

Type: Non-drug, online, interactive

Setting/location: Online, any location in Australia

Duration: 5 x 20 minute online sessions, delivered over 5 consecutive weeks

Protocol: This program is based on CBTI, the recommended treatment for insomnia (e.g. Qaseem et al., 2016, Ann Intern Med, DOI: 10.7326/M15-2175). It is based on a digitised version of a brief CBTI protocol described in a scientific article in the Australian Journal of General Practice (Sweetman et al., 2021, AJGP, doi: 10.31128/AJGP-04-20-5391).

Content: Each session will be administered online (computer or mobile phone). Each session will contain videos, text, and images. Participants will be asked to enter text-based, numerical (e.g. minutes of sleep duration) and multiple-choice data throughout the program. Participants will receive tailored therapy recommendations (e.g., prescribed time in bed) during each weekly session, determined by an in-built algorithm and participants' entered data (see Sweetman et al., 2021, Aus J General Practice for tailored therapy recommendations). Immediately after each session is completed, participants will receive an automated follow-up email with session-specific 'follow-up' information and tailored therapy recommendations including recommended bedtime window (approximate reading time: 15 minutes). Participants will receive another automated email one week later with a link to start each subsequent session. Videos are presented by researchers, psychologists, and sleep technicians, each with extensive experience (>8 years) in the management of insomnia.

Tailoring / personalisation: Therapy recommendations will be tailored to participant's insomnia symptoms at baseline and weekly changes in symptoms throughout the program. Bedtime Restriction Therapy (initial restriction of time in bed to consolidate sleep, and subsequent gradual extension of time in bed) is a core component of CBTI. Bedtime restriction recommendations will be tailored to the specific sleep/wake information that participants provide.

Primary therapeutic components: Psychoeducation about sleep, Bedtime restriction therapy, Stimulus Control Therapy, Relaxation Therapy, Cognitive Refocusing, Relapse Prevention.

Adherence assessment: Adherence will be defined as the number of participants commencing each of the 5 online sessions. This information is automatically collected through the online system.

Intervention code [1]

Treatment: Other

Intervention code [2]

Behaviour

Comparator / control treatment

Waitlist control for 8 weeks before commencing digital CBTI.

Participants in the waitlist condition will receive weekly emails with written information about insomnia and sleep health for the first 5 weeks of the trial. This includes information about;

- 'sleep hygiene' (healthy sleep behaviours)

- sleep myths and facts

- Information about caffeine and sleep

- depression and sleep

- chronic insomnia (symptoms, diagnosis, treatment options)

Each weekly information packet takes approximately 4 minutes to read and is sourced from the Sleep Health Foundation.

Control group

Active

Outcomes

Primary outcome [1]

Between-group change in self-reported depression symptoms on the Patient Health Questionnaire (PHQ-9).

Timepoint [1]

Between-group change in PHQ-9 scores from baseline to 8-week follow-up post-randomisation (primary timepoint).

Change in PHQ-9 scores from baseline to 16-week and 24-week follow-up.

Secondary outcome [1]

Between-group change in self-reported insomnia severity.

Timepoint [1]

Between-group change in ISI scores from baseline to 8-week follow-up post-randomisation.

Change in ISI from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [2]

Between-group change in self-reported anxiety symptoms on the Generalised Anxiety Disorder Questionnaire-7 (GAD-7).

Timepoint [2]

Between-group change in GAD-7 scores from baseline to 8-week follow-up post-randomisation.

Change in GAD-7 scores from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [3]

Between-group change in self-reported approach-related behaviour on the Behavioural Inhibition System and Behavioural Activation System Scales (BIS/BAS)

Timepoint [3]

Between-group change in BAS scores from baseline to 8-week follow-up post-randomisation.

Change in BAS scores from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [4]

Between-group change in self-reported emotion regulation ability on the Perth Emotion Regulation Competency Inventory (PERCI)

Timepoint [4]

Between-group change in PERCI scores from baseline to 8-week follow-up post-randomisation.

Change in PERCI scores from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [5]

Between-group change in self-reported emotion reactivity on the Perth Emotional Reactivity Scale Short-Form (PERS-S).

Timepoint [5]

Between-group change in PERS-S scores from baseline to 8-week follow-up post-randomisation.

Change in PERS-S scores from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [6]

Between-group change in self-reported emotion expressivity on the Emotional Expressivity Scale (EES).

Timepoint [6]

Between-group change in EES scores from baseline to 8-week follow-up post-randomisation.

Change in EES scores from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [7]

Between-group change in self-reported repetitive negative thinking on the Persistent and Intrusive Negative Thoughts Scale (PINTS).

Timepoint [7]

Between-group change in PINTS scores from baseline to 8-week follow-up post-randomisation.

Change in PINTS scores from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [8]

Between-group change in self-reported friendship, isolation, negative and positive attitudes to solitude on the Perth A-Loneness Scale (PALs).

Timepoint [8]

Between-group change in PALs scores from baseline to 8-week follow-up post-randomisation.

Change in PALs scores from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [9]

Between-group change in emotion recognition on a computerised version of the Penn Emotion Recognition-40 test.

Timepoint [9]

Between-group change in the Penn Emotion Recognition-40 test from baseline to 8-week follow-up post-randomisation.

Change in the Penn Emotion Recognition-40 test from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [10]

Between-group change in executive functioning on a computerised version of the Wisconsin Card Sorting Task (WCST)

Timepoint [10]

Between-group change on the WCST from baseline to 8-week follow-up post-randomisation.

Change on the WCST from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [11]

Between-group change in working memory on a computerised version of the Digit Span Backwards Task (DSB)

Timepoint [11]

Between-group change on the DSB from baseline to 8-week follow-up post-randomisation.

Change on the DSB from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [12]

Between-group change in attentional control on a computerised version of the Anti-saccade Task (AS Task)

Timepoint [12]

Between-group change on the AS Task from baseline to 8-week follow-up post-randomisation.

Change on the AS Task from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [13]

Between-group change in sleep-related and depression-related attention bias on a computerised Dual-Probe Attention-Bias task.

Timepoint [13]

Between-group change on the Dual-Probe Attention-Bias Task from baseline to 8-week follow-up post-randomisation.

Change on the Dual-Probe Attention-Bias Task from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [14]

Between-group change in sleep-related and depression-related interpretation bias on an Ambiguous Scenarios Test.

Timepoint [14]

Between-group change on an Ambiguous Scenarios Test from baseline to 8-week follow-up post-randomisation.

Change on an Ambiguous Scenarios Test from baseline to 16-week and 24-week follow-up. post-randomisation

Secondary outcome [15]

Change in daytime sleepiness.

Timepoint [15]

Between-group change in ESS from baseline to 8-week follow-up post-randomisation.

Change in ESS from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [16]

Change in fatigue.

Timepoint [16]

Between-group change FFS from baseline to 8-week follow-up post-randomisation.

Change in FFS from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [17]

Change in Dysfunctional Beliefs about Sleep

Timepoint [17]

Between-group change in DBAS-16 scores from baseline to 8-week follow-up post-randomisation.

Change in DBAS-16 scores from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [18]

Change in self-reported sleep.

Timepoint [18]

Between-group change in Sleep Diary metrics from baseline to 8-week follow-up post-randomisation.

Change in Sleep Diary metrics from baseline to 16-week and 24-week follow-up post-randomisation.

Secondary outcome [19]

Between-group change in self-reported withdrawal-related behaviour on the Behavioural Inhibition System and Behavioural Activation System Scales (BIS/BAS)

Timepoint [19]

Between-group change in BIS scores from baseline to 8-week follow-up post-randomisation.

Change in BIS scores from baseline to 16-week and 24-week follow-up post-randomisation.

Eligibility

Key inclusion criteria

Young adults aged 18 – 24 years.

PHQ-9 score of 10 or above (i.e., moderate depression symptoms)

Reliable access to computer, tablet or smartphone, with internet access

Basic English language comprehension as required for digital CBTI program

Minimum age

18 Years

Maximum age

24 Years

Sex

Both males and females

Can healthy volunteers participate?

Key exclusion criteria

Psychiatric condition (Bipolar disorder, schizophrenia)

Epilepsy

Currently pregnant

Moderate daytime sleepiness (Epworth Sleepiness Scale score equal to or more than 16)

People who are commercial drivers or operate heavy machinery for work

People with a cognitive impairment

Shift workers

Previous diagnosis of a narcolepsy or REM sleep disorder

Previous sleepiness-related motor-vehicle accident

In all cases where individuals are excluded from the study, an appropriate onward referral will be made.

Study design

Purpose of the study

Treatment

Allocation to intervention

Randomised controlled trial

Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)

Allocation is not concealed

Methods used to generate the sequence in which subjects will be randomised (sequence generation)

Computer generated block randomisation, with block sizes of 2 and 4.

Masking / blinding

Open (masking not used)

Who is / are masked / blinded?

Intervention assignment

Parallel

Other design features

Phase

Not Applicable

Type of endpoint/s

Statistical methods / analysis

To detect small-to-moderate (f=0.175) between group effects between the two groups from pre-treatment to the 8 week follow-up, a minimum of 196 participants need to be recruited. Therefore, approximately 200 participants will be recruited.

Recruitment

Recruitment status

Recruiting

Date of first participant enrolment

Anticipated

1/02/2024

Actual

6/03/2024

Date of last participant enrolment

Anticipated

1/02/2029

Actual

Date of last data collection

Anticipated

1/08/2029

Actual

Sample size

Target

200

Accrual to date

Final

Recruitment in Australia

Recruitment state(s)

Funding & Sponsors

Funding source category [1]

University

Name [1]

University of Western Australia

Address [1]

35 Stirling Highway Crawley WA 6009

Country [1]

Australia

Primary sponsor type

University

Name

University of Western Australia

Address

35 Stirling Highway Crawley WA 6009

Country

Australia

Secondary sponsor category [1]

None

Name [1]

Address [1]

Country [1]

Ethics approval

Ethics application status

Approved

Ethics committee name [1]

UWA Human Research Ethics Committee

Ethics committee address [1]

35 Stirling Highway Crawley WA 6009

Ethics committee country [1]

Australia

Date submitted for ethics approval [1]

30/03/2023

Approval date [1]

11/07/2023

Ethics approval number [1]

2023/ET000230

Summary

Brief summary

Depression and insomnia are important and related public health problems for young people. The recommended treatment for insomnia is Cognitive Behavioural Therapy for insomnia (CBTI). CBTI programs are known to effectively reduce symptoms of depression without directly targeting non-sleep symptoms. However, the mechanisms which underlie the association between insomnia and depression are not well understood. Many candidate mechanisms have been proposed (e.g., cognitive biases), yet, there is a lack of research which investigates these possible mechanisms, and data from treatment studies is greatly needed to investigate the causal role of these mechanisms in the association between insomnia and depression.  

This randomised controlled trial aims to investigate what psychological mechanisms explain how digital cognitive behavioural therapy for insomnia improves depression in young people. 

It is hypothesised that the group who receive the brief CBTI program will display greater improvement in symptoms of depression and insomnia, and a greater change in mechanisms thought to underlie the association between depression and insomnia symptoms, compared to the group that receive education (waitlist control).

Trial website

Trial related presentations / publications

Public notes

Contacts

Principal investigator

Name

Dr Cele Richardson

Address

University of Western Australia, 35 Stirling Highway Crawley WA 6009

Country

Australia

Phone

+61 8 6488 3141

Fax

[email protected]

Contact person for public queries

Name

Cele Richardson

Address

University of Western Australia, 35 Stirling Highway Crawley WA 6009

Country

Australia

Phone

+61 8 6488 3141

Fax

[email protected]

Contact person for scientific queries

Name

Cele Richardson

Address

University of Western Australia 35 Stirling Highway Crawley WA 6009

Country

Australia

Phone

+61 8 6488 3141

Fax

[email protected]

Data sharing statement

Will individual participant data (IPD) for this trial be available (including data dictionaries)?

Yes

What data in particular will be shared?

Data will be shared after de-identification only. Participant data of published results and other available data will be shared upon reasonable request.

When will data be available (start and end dates)?

Data will be made available following publication of outcomes, and will remain available as long as data is stored (in compliance with retention policies).

Available to whom?

Only research who provide a methodologically sound proposal will have access to the data.

Available for what types of analyses?

Methodologically sound projects and meta-analysis

How or where can data be obtained?

By contacting the principle investigator at [email protected]

What supporting documents are/will be available?

No Supporting Document Provided

Results publications and other study-related documents

Documents added manually

No documents have been uploaded by study researchers.

Documents added automatically

No additional documents have been identified.

Trial Review

Documents added manually

Documents added automatically