Enhancing prolonged exposure therapy for PTSD among veterans with oxytocin: Design of a multisite randomized controlled trial

Enhancing prolonged exposure therapy for PTSD among veterans with oxytocin: Design of a multisite randomized controlled trial

Posttraumatic stress disorder (PTSD) is the most highly prevalent mental health disorder among U.S. military Veterans. Prolonged Exposure (PE) therapy is one of the most widely used evidence-based treatments for PTSD, but there is substantial room for improvement in outcomes and retention rates. Acc...

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Veröffentlicht in:Contemporary clinical trials 2020-08, Vol.95, p.106074-106074, Article 106074
Hauptverfasser: Flanagan, Julianne C., Mitchell, Jennifer M., Baker, Nathaniel L., Woolley, Joshua, Wangelin, Bethany, Back, Sudie E., McQuaid, John R., Neylan, Thomas C., Wolfe, William R., Brady, Kathleen T.
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Oxytocin
Prolonged exposure therapy
Psychophysiology
PTSD
Veteran
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container_start_page 106074
container_title Contemporary clinical trials
container_volume 95
creator Flanagan, Julianne C.
Mitchell, Jennifer M.
Baker, Nathaniel L.
Woolley, Joshua
Wangelin, Bethany
Back, Sudie E.
McQuaid, John R.
Neylan, Thomas C.
Wolfe, William R.
Brady, Kathleen T.
description Posttraumatic stress disorder (PTSD) is the most highly prevalent mental health disorder among U.S. military Veterans. Prolonged Exposure (PE) therapy is one of the most widely used evidence-based treatments for PTSD, but there is substantial room for improvement in outcomes and retention rates. Accumulating data suggest that oxytocin offers a promising pharmacological approach towards achieving this goal. Therefore, the primary objective of this two-site Phase II study is to examine the ability of oxytocin (vs. placebo) administration combined with PE therapy to (1) reduce PTSD symptom severity, (2) accelerate the rate of PTSD symptom improvement, and (3) improve PE adherence and retention rates. To accomplish these objectives, we will employ a randomized, double-blind, placebo-controlled trial and use standardized, repeated dependent measures of change at five time points (baseline, mid-treatment, end of treatment, and 3 and 6 month follow-up). Intranasal oxytocin (40 IU) will be administered directly prior to each PE therapy session. Findings from this study will provide critical new information regarding the efficacy of oxytocin to augment psychosocial treatment for PTSD, as well as information regarding the physiological mechanisms underlying PTSD and positive treatment response. ClinicalTrials.gov Identifier: NCT04228289
doi_str_mv 10.1016/j.cct.2020.106074
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subjects Oxytocin
Prolonged exposure therapy
Psychophysiology
PTSD
Veteran
title Enhancing prolonged exposure therapy for PTSD among veterans with oxytocin: Design of a multisite randomized controlled trial
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