4.4 Article

Baseline psychophysiological and cortisol reactivity as a predictor of PTSD treatment outcome in virtual reality exposure therapy

Journal

BEHAVIOUR RESEARCH AND THERAPY
Volume 82, Issue -, Pages 28-37

Publisher

PERGAMON-ELSEVIER SCIENCE LTD
DOI: 10.1016/j.brat.2016.05.002

Keywords

Acoustic startle; Posttraumatic stress disorder; Virtual reality; Psychophysiology; Exposure therapy; Cortisol

Funding

  1. Department of Defense Clinical Trial Grant [W81XWH-10-1-1045]
  2. NIMH [U19 MH-069056, R01 MH-70880, R01 MH-094757]
  3. Brain and Behavior Research Foundation (NARSAD) Distinguished Investigator Grant (Optimal Dose of Early Intervention to Prevent PTSD)
  4. McCormick Foundation (BraveHeart: MLB's Welcome Back Veterans Southeast Initiative)
  5. Genentech
  6. Posit Science Corporation
  7. National Institute on Drug Abuse

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Baseline cue-dependent physiological reactivity may serve as an objective measure of posttraumatic stress disorder (PTSD) symptoms. Additionally, prior animal model and psychological studies would suggest that subjects with greatest symptoms at baseline may have the greatest violation of expectancy to danger when undergoing exposure based psychotherapy; thus treatment approaches which enhanced the learning under these conditions would be optimal for those with maximal baseline cue-dependent reactivity. However methods to study this hypothesis objectively are lacking. Virtual reality (VR) methodologies have been successfully employed as an enhanced form of imaginal prolonged exposure therapy for the treatment of PTSD. Our goal was to examine the predictive nature of initial psychophysiological (e.g., startle, skin conductance, heart rate) and stress hormone responses (e.g., cortisol) during presentation of VR-based combat-related stimuli on PTSD treatment outcome. Combat veterans with PTSD underwent 6 weeks of VR exposure therapy combined with either D-cycloserine (DCS), alprazolam (ALP), or placebo (PBO). In the DCS group, startle response to VR scenes prior to initiation of treatment accounted for 76% of the variance in CAPS change scores, p < 0.001, in that higher responses predicted greater changes in symptom severity over time. Additionally, baseline cortisol reactivity was inversely associated with treatment response in the ALP group, p = 0.04. We propose that baseline cue-activated physiological measures will be sensitive to predicting patients' level of response to exposure therapy, in particular in the presence of enhancement (e.g., DCS). Published by Elsevier Ltd.

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