Abstract

BackgroundThe daytime effects of insomnia pose a significant burden to patients and drive treatment seeking. In addition to subjective deficits, meta-analytic data show that patients experience reliable objective impairments across several cognitive domains. While Cognitive Behavioural Therapy for Insomnia (CBT-I) is an effective and scalable treatment, we know little about its impact upon cognitive function. Trials of CBT-I have typically used proxy measures for cognitive functioning, such as fatigue or work performance scales, and no study has assessed self-reported impairment in cognitive function as a primary outcome. Moreover, only a small number of studies have assessed objective cognitive performance, pre-to-post CBT-I, with mixed results. This study specifically aims to (1) investigate the impact of CBT-I on cognitive functioning, assessed through both self-reported impairment and objective performance measures, and (2) examine whether change in sleep mediates this impact.Methods/designWe propose a randomised controlled trial of 404 community participants meeting criteria for Insomnia Disorder. In the DISCO trial (Defining the Impact of improved Sleep on COgnitive function (DISCO)) participants will be randomised to digital automated CBT-I delivered by a web and/or mobile platform (in addition to treatment as usual (TAU)) or to a wait-list control (in addition to TAU). Online assessments will take place at 0 (baseline), 10 (post-treatment), and 24 (follow-up) weeks. At week 25, all participants allocated to the wait-list group will be offered digital CBT-I, at which point the controlled element of the trial will be complete. The primary outcome is self-reported cognitive impairment at post-treatment (10 weeks). Secondary outcomes include objective cognitive performance, insomnia severity, sleepiness, fatigue, and self-reported cognitive failures and emotional distress. All main analyses will be carried out on completion of follow-up assessments and will be based on the intention-to-treat principle. Further analyses will determine to what extent observed changes in self-reported cognitive impairment and objective cognitive performance are mediated by changes in sleep. The trial is supported by the National Institute for Health Research (NIHR) Oxford Biomedical Research Centre (BRC) based at Oxford University Hospitals NHS Trust and University of Oxford, and by the NIHR Oxford Health BRC.DiscussionThis study will be the first large-scale examination of the impact of digital CBT-I on self-reported cognitive impairment and objective cognitive performance.Trial registrationISRCTN, ID: ISRCTN89237370. Registered on 17 October 2016.

Highlights

  • The daytime effects of insomnia pose a significant burden to patients and drive treatment seeking

  • Insomnia disorder is defined as persistent difficulties with sleep initiation and/or maintenance, resulting in significant daytime impairment

  • Recent, wellcontrolled studies find evidence of insomnia-related impairments in switching of attention and working memory [8], and sustained attention and episodic memory [9]. These impairments are associated with global insomnia severity, sleep duration, and disturbed sleep continuity

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Summary

Introduction

The daytime effects of insomnia pose a significant burden to patients and drive treatment seeking. This study aims to (1) investigate the impact of CBT-I on cognitive functioning, assessed through both self-reported impairment and objective performance measures, and (2) examine whether change in sleep mediates this impact. With respect to cognitive function, meta-analytic data indicate that patients exhibit reliable impairments (of medium effect size) in tasks probing episodic memory, working memory, and problem solving [7]. Recent, wellcontrolled studies find evidence of insomnia-related impairments in switching of attention and working memory [8], and sustained attention and episodic memory [9]. These impairments are associated with global insomnia severity, sleep duration, and disturbed sleep continuity (from both sleep diaries and polysomnography). Neurocognitive findings are consistent with results from functional imaging studies, which reveal evidence of hypoactivation within fronto-striatal networks during task-related functional magnetic resonance imaging (fMRI) [10,11,12,13]

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