Homeostatic normalization of alpha brain rhythms within the default-mode network and reduced symptoms in post-traumatic stress disorder following a randomized controlled trial of electroencephalogram neurofeedback

Author:

Nicholson Andrew A1234ORCID,Densmore Maria56,Frewen Paul A57ORCID,Neufeld Richard W J587,Théberge Jean87469ORCID,Jetly Rakesh10,Lanius Ruth A586,Ros Tomas1112ORCID

Affiliation:

1. School of Psychology, University of Ottawa , Ottawa , Canada

2. Atlas Institute for Veterans and Families, Royal Ottawa Hospital , Ottawa , Canada

3. The University of Ottawa’s Institute of Mental Health Research, Royal Ottawa Hospital , Ottawa , Canada

4. Department of Medical Biophysics, Western University , London , Canada

5. Department of Neuroscience, Western University , London , Canada

6. Imaging, Lawson Health Research Institute , London , Canada

7. Department of Psychology, Western University , London , Canada

8. Department of Psychiatry, Western University , London , Canada

9. Department of Diagnostic Imaging, St. Joseph’s Healthcare , London , Canada

10. Defence Research and Development Canada , Toronto , Canada

11. Departments of Neuroscience and Psychiatry, University of Geneva; Campus Biotech , Geneva , Switzerland

12. Centre for Biomedical Imaging (CIBM) , Geneva , Switzerland

Abstract

AbstractCollective research has identified a key electroencephalogram signature in patients with post-traumatic stress disorder, consisting of abnormally reduced alpha (8–12 Hz) rhythms. We conducted a 20-session, double-blind, randomized controlled trial of alpha desynchronizing neurofeedback in patients with post-traumatic stress disorder over 20 weeks. Our objective was to provide mechanistic evidence underlying potential clinical improvements by examining changes in aberrant post-traumatic stress disorder brain rhythms (namely, alpha oscillations) as a function of neurofeedback treatment. We randomly assigned participants with a primary diagnosis of post-traumatic stress disorder (n = 38) to either an experimental group (n = 20) or a sham-control group (n = 18). A multichannel electroencephalogram cap was used to record whole-scalp resting-state activity pre- and post-neurofeedback treatment, for both the experimental and sham-control post-traumatic stress disorder groups. We first observed significantly reduced relative alpha source power at baseline in patients with post-traumatic stress disorder as compared to an age/sex-matched group of neurotypical healthy controls (n = 32), primarily within regions of the anterior default mode network. Post-treatment, we found that only post-traumatic stress disorder patients in the experimental neurofeedback group demonstrated significant alpha resynchronization within areas that displayed abnormally low alpha power at baseline. In parallel, we observed significantly decreased post-traumatic stress disorder severity scores in the experimental neurofeedback group only, when comparing baseline to post-treatment (Cohen’s d = 0.77) and three-month follow-up scores (Cohen’s d = 0.75), with a remission rate of 60.0% at the three-month follow-up. Overall, our results indicate that neurofeedback training can rescue pathologically reduced alpha rhythmicity, a functional biomarker that has repeatedly been linked to symptoms of hyperarousal and cortical disinhibition in post-traumatic stress disorder. This randomized controlled trial provides long-term evidence suggesting that the ‘alpha rebound effect’ (i.e. homeostatic alpha resynchronization) occurs within key regions of the default mode network previously implicated in post-traumatic stress disorder.

Funder

Canadian Institute for Veteran Health Research

ANS Research

European Union’s Horizon 2020 research and innovation

Banting Research Foundation

Publisher

Oxford University Press (OUP)

Subject

Neurology,Cellular and Molecular Neuroscience,Biological Psychiatry,Psychiatry and Mental health

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