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基于暴露的认知行为疗法对焦虑神经相关因素的早期影响。

Early effects of exposure-based cognitive behaviour therapy on the neural correlates of anxiety.

机构信息

Department of Psychiatry, University of Oxford, Oxford, UK.

Oxford Psychologists Ltd, Oxford, UK.

出版信息

Transl Psychiatry. 2018 Oct 19;8(1):225. doi: 10.1038/s41398-018-0277-5.

Abstract

Exposure-based cognitive-behaviour therapy (CBT) for anxiety disorders is an effective intervention, but the brain mechanisms driving recovery are largely unknown. In this experimental medicine study, we investigated to what degree CBT affects neural markers of anxiety at an early stage of treatment, to identify dynamic mechanistic changes which might be crucial in the process of recovery as opposed to those seen following full treatment completion. In a randomised controlled trial, unmedicated patients with panic disorder either received four weekly sessions of exposure-based CBT (N = 14) or were allocated to a waiting group (N = 14). Symptom severity was measured before and after the intervention. During functional magnetic resonance imaging (fMRI), patients performed an emotion regulation task, either viewing negative images naturally, or intentionally down-regulating negative affect using previously taught strategies. Four-session CBT led to marked reductions in symptoms and 71% of patients reached recovery status (versus 7% in the control group). This intervention normalised brain hyperactivation previously seen in panic disorder, particularly in areas linked to threat monitoring, fear memory, and maladaptive emotion regulation, such as amygdala, dorsomedial and dorsolateral prefrontal cortex, and temporal gyrus. Our findings suggest that optimal treatment doses for panic disorder might be much lower than previously thought. Furthermore, this is the first study to show that neural markers of anxiety change very early during CBT, highlighting potential neural mechanisms that might drive clinical recovery. Such knowledge is important for the development of more compact combination treatments targeting these mechanisms more effectively. (Neural Effects of Cognitive-behaviour Therapy in Panic Disorder; clinicaltrials.gov; NCT03251235).

摘要

基于暴露的认知行为疗法(CBT)治疗焦虑症是一种有效的干预措施,但驱动康复的大脑机制在很大程度上尚不清楚。在这项实验医学研究中,我们研究了 CBT 在治疗早期对焦虑的神经标记物有多大影响,以确定在恢复过程中至关重要的动态机制变化,而不是在完成完整治疗后看到的那些变化。在一项随机对照试验中,未经药物治疗的惊恐障碍患者要么接受每周 4 次的暴露性 CBT(N=14),要么被分配到等待组(N=14)。在干预前后测量症状严重程度。在功能磁共振成像(fMRI)期间,患者执行情绪调节任务,要么自然地观看负面图像,要么使用先前教授的策略有意地抑制负面情绪。四疗程 CBT 导致症状明显减轻,71%的患者达到康复状态(对照组为 7%)。这种干预措施使惊恐障碍中先前存在的大脑过度激活正常化,特别是在与威胁监测、恐惧记忆和适应不良情绪调节相关的区域,如杏仁核、背内侧和背外侧前额叶皮层以及颞叶。我们的发现表明,惊恐障碍的最佳治疗剂量可能比以前认为的要低得多。此外,这是第一项表明 CBT 期间焦虑的神经标记物很早就发生变化的研究,强调了可能驱动临床康复的潜在神经机制。这些知识对于开发更紧凑的联合治疗方法以更有效地针对这些机制非常重要。(惊恐障碍的认知行为治疗的神经效应;clinicaltrials.gov;NCT03251235)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3ec7/6195621/337023d00380/41398_2018_277_Fig1_HTML.jpg

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