Christina D Dutcher1, Sheila M Dowd2, Alyson K Zalta2,3, Daniel J Taylor4, David Rosenfield5, Alexander Perrone1, Michael W Otto6, Mark H Pollack2, Stefan G Hofmann6, Jasper A J Smits1. 1. Department of Psychology, Institute for Mental Health Research, The University of Texas at Austin, Austin, Texas, USA. 2. Department of Psychiatry and Behavioral Sciences, Rush University Medical Center, Chicago, Illinois, USA. 3. Department of Psychological Science, University of California, Irvine, California, USA. 4. Department of Psychology, University of Arizona, Tucson, Arizona, USA. 5. Department of Psychology, Southern Methodist University, Dallas, Texas, USA. 6. Department of Psychological and Brain Sciences, Boston University, Boston, Massachusetts, USA.
Abstract
INTRODUCTION: Poor sleep is prevalent among individuals with social anxiety disorder (SAD) and may negatively affect exposure therapy outcomes. Poor sleep may impair memory and learning, and thus compromise fear extinction learning thought to take place in exposure therapy. We examined poor sleep as a predictor of exposure therapy outcomes for SAD and the moderating role of d-cycloserine (DCS) on this relationship. METHODS: Participants were 152 individuals with a primary diagnosis of SAD. As part of a randomized clinical trial evaluating the efficacy of DCS for enhancing the effects of exposure therapy, they completed self-report baseline measure of sleep quality, and self-report sleep diaries assessing sleep duration (total sleep time [TST]) and sleep quality the nights before and after treatment sessions. RESULTS: Poorer baseline sleep quality was significantly associated with slower improvement over time and worse symptom outcomes at the end of treatment and follow-up after controlling for baseline symptoms of depression and social anxiety. Greater TST the night before treatment predicted lower SAD symptoms at the next session, after controlling for symptoms at the previous session. There was no relation between prior or subsequent night sleep quality on symptoms at the next session. No associations were moderated by DCS. CONCLUSIONS: We replicated and extended findings indicating that poor sleep quality is associated with poorer exposure therapy outcomes for SAD. Assessing for sleep difficulties before treatment initiation and incorporating sleep interventions into treatment may enhance exposure therapy outcomes for SAD.
INTRODUCTION: Poor sleep is prevalent among individuals with social anxiety disorder (SAD) and may negatively affect exposure therapy outcomes. Poor sleep may impair memory and learning, and thus compromise fear extinction learning thought to take place in exposure therapy. We examined poor sleep as a predictor of exposure therapy outcomes for SAD and the moderating role of d-cycloserine (DCS) on this relationship. METHODS: Participants were 152 individuals with a primary diagnosis of SAD. As part of a randomized clinical trial evaluating the efficacy of DCS for enhancing the effects of exposure therapy, they completed self-report baseline measure of sleep quality, and self-report sleep diaries assessing sleep duration (total sleep time [TST]) and sleep quality the nights before and after treatment sessions. RESULTS: Poorer baseline sleep quality was significantly associated with slower improvement over time and worse symptom outcomes at the end of treatment and follow-up after controlling for baseline symptoms of depression and social anxiety. Greater TST the night before treatment predicted lower SAD symptoms at the next session, after controlling for symptoms at the previous session. There was no relation between prior or subsequent night sleep quality on symptoms at the next session. No associations were moderated by DCS. CONCLUSIONS: We replicated and extended findings indicating that poor sleep quality is associated with poorer exposure therapy outcomes for SAD. Assessing for sleep difficulties before treatment initiation and incorporating sleep interventions into treatment may enhance exposure therapy outcomes for SAD.
Authors: Edward F Pace-Schott; Ryan M Bottary; Se-Yun Kim; Peter L Rosencrans; Shilpa Vijayakumar; Scott P Orr; Natasha B Lasko; Elizabeth M Goetter; Amanda W Baker; Matt T Bianchi; Karen Gannon; Susanne S Hoeppner; Stefan G Hofmann; Naomi M Simon Journal: Psychiatry Res Date: 2018-10-09 Impact factor: 3.222