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本文引用的文献

1
Anxiety Sensitivity as a Malleable Mechanistic Target for Prevention Interventions: A Meta-Analysis of the Efficacy of Brief Treatment Interventions.焦虑敏感性作为预防干预的可塑机制靶点:简短治疗干预效果的荟萃分析
Clin Psychol (New York). 2021 Dec;28(4):323-337. doi: 10.1037/cps0000038. Epub 2021 Oct 21.
2
Change in posttraumatic stress disorder-related thoughts during treatment: Do thoughts drive change when pills are involved?治疗过程中创伤后应激障碍相关思维的变化:药物治疗时思维是否会驱动变化?
J Trauma Stress. 2022 Apr;35(2):496-507. doi: 10.1002/jts.22762. Epub 2021 Dec 31.
3
A guide to guidelines for the treatment of posttraumatic stress disorder in adults: An update.成人创伤后应激障碍治疗指南:更新版。
Psychotherapy (Chic). 2019 Sep;56(3):359-373. doi: 10.1037/pst0000231.
4
Efficacy of Prolonged Exposure Therapy, Sertraline Hydrochloride, and Their Combination Among Combat Veterans With Posttraumatic Stress Disorder: A Randomized Clinical Trial. prolonged exposure therapy、盐酸舍曲林及其联合治疗对创伤后应激障碍退伍军人的疗效:一项随机临床试验。
JAMA Psychiatry. 2019 Feb 1;76(2):117-126. doi: 10.1001/jamapsychiatry.2018.3412.
5
Treatment choice among veterans with PTSD symptoms and substance-related problems: Examining the role of preparatory treatments in trauma-focused therapy.创伤后应激障碍症状和物质相关问题的退伍军人的治疗选择:审查创伤聚焦疗法中预备治疗的作用。
Psychol Serv. 2020 Nov;17(4):405-413. doi: 10.1037/ser0000313. Epub 2018 Nov 26.
6
Integrating biological treatment mechanisms into randomized clinical trials: Design of PROGrESS (PROlonGed ExpoSure and Sertraline Trial).将生物治疗机制纳入随机临床试验:PROGrESS(长期暴露与舍曲林试验)的设计。
Contemp Clin Trials. 2018 Jan;64:128-138. doi: 10.1016/j.cct.2017.10.013. Epub 2017 Oct 29.
7
Randomized Clinical Trial Investigating the Effects of an Anxiety Sensitivity Intervention on Posttraumatic Stress Symptoms: A Replication and Extension.一项关于焦虑敏感性干预对创伤后应激症状影响的随机临床试验:一项重复与扩展研究。
J Trauma Stress. 2017 Jun;30(3):296-303. doi: 10.1002/jts.22194. Epub 2017 Jun 6.
8
The Clinician-Administered PTSD Scale for DSM-5 (CAPS-5): Development and initial psychometric evaluation in military veterans.用于 DSM-5 的临床医生管理 PTSD 量表(CAPS-5):退伍军人中的开发和初步心理计量评估。
Psychol Assess. 2018 Mar;30(3):383-395. doi: 10.1037/pas0000486. Epub 2017 May 11.
9
Temporal Sequencing of Change in Posttraumatic Cognitions and PTSD Symptom Reduction During Prolonged Exposure Therapy.创伤后认知变化与延长暴露疗法中创伤后应激障碍症状减轻的时间顺序
Behav Ther. 2017 Mar;48(2):156-165. doi: 10.1016/j.beth.2016.02.008. Epub 2016 Mar 3.
10
Pre-treatment predictors of dropout from prolonged exposure therapy in patients with chronic posttraumatic stress disorder and comorbid substance use disorders.慢性创伤后应激障碍合并物质使用障碍患者长期暴露疗法脱落的预处理预测因素。
Behav Res Ther. 2017 Apr;91:43-50. doi: 10.1016/j.brat.2017.01.011. Epub 2017 Jan 25.

创伤后应激障碍治疗对焦虑敏感的影响:延长暴露、舍曲林及其联合治疗的影响。

The influence of posttraumatic stress disorder treatment on anxiety sensitivity: Impact of prolonged exposure, sertraline, and their combination.

机构信息

San Diego State University Research Foundation, San Diego, California, USA.

VA San Diego Healthcare System, San Diego, California, USA.

出版信息

J Trauma Stress. 2023 Feb;36(1):157-166. doi: 10.1002/jts.22894. Epub 2022 Nov 30.

DOI:10.1002/jts.22894
PMID:36451271
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9974893/
Abstract

Trauma-informed beliefs often decrease during posttraumatic stress disorder (PTSD) treatment. This may also extend to anxiety sensitivity (AS), defined as a fear of anxiety-related sensations and beliefs that anxiety is dangerous and/or intolerable. However, little is known about how AS changes during exposure-based and psychopharmacological PTSD treatments. Further, high AS may be a risk factor for diminished PTSD symptom improvement and increased treatment dropout. To better understand how AS impacts and is impacted by PTSD treatment, we conducted a secondary analysis of a randomized clinical trial with a sample of 223 veterans (87.0% male, 57.5% White) with PTSD from four U.S. sites. Veterans were randomized to receive prolonged exposure (PE) plus placebo (n = 74), sertraline plus enhanced medication management (n = 74), or PE plus sertraline (n = 75). Veterans answered questions about PTSD symptoms and AS at baseline and 6-, 12-, 24-, 36-, and 52-week follow-ups. High baseline AS was related to high levels of PTSD severity at 24 weeks across all conditions, β = .244, p = .013, but did not predict dropout from exposure-based, β = .077, p = .374, or psychopharmacological therapy, β = .009, p = .893. AS also significantly decreased across all three treatment arms, with no between-group differences; these reductions were maintained at the 52-week follow-up. These findings suggest that high AS is a risk factor for attenuated PTSD treatment response but also provide evidence that AS can be improved by both PE and an enhanced psychopharmacological intervention for PTSD.

摘要

创伤知情信念通常会在创伤后应激障碍(PTSD)治疗过程中减少。这也可能扩展到焦虑敏感性(AS),AS 被定义为对焦虑相关感觉的恐惧以及对焦虑是危险和/或无法忍受的信念。然而,人们对 AS 在基于暴露的和精神药理学 PTSD 治疗中如何变化知之甚少。此外,高 AS 可能是 PTSD 症状改善程度降低和治疗退出率增加的风险因素。为了更好地了解 AS 如何影响 PTSD 治疗以及如何受到 PTSD 治疗的影响,我们对一项有 223 名退伍军人(87.0%为男性,57.5%为白人)参与的随机临床试验进行了二次分析,这些退伍军人患有 PTSD,来自美国的四个地点。退伍军人被随机分配接受延长暴露(PE)加安慰剂(n = 74)、舍曲林加增强药物管理(n = 74)或 PE 加舍曲林(n = 75)治疗。退伍军人在基线和 6、12、24、36 和 52 周随访时回答 PTSD 症状和 AS 问题。在所有条件下,高基线 AS 与 24 周时 PTSD 严重程度高相关,β=0.244,p=0.013,但与暴露基础治疗(β=0.077,p=0.374)或精神药理学治疗(β=0.009,p=0.893)的退出无关。AS 也在所有三种治疗组中显著降低,组间无差异;这些减少在 52 周随访时仍保持。这些发现表明,高 AS 是 PTSD 治疗反应减弱的风险因素,但也有证据表明,PE 和增强的精神药理学 PTSD 干预都可以改善 AS。