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创伤后应激的表观遗传学:NR3C1 甲基化与叙事暴露疗法治疗创伤后应激障碍症状变化的相关性。

Epigenetics of traumatic stress: The association of NR3C1 methylation and posttraumatic stress disorder symptom changes in response to narrative exposure therapy.

机构信息

Clinical Psychology and Psychotherapy, Bielefeld University, Universitätsstraße 25, 33615, Bielefeld, Germany.

vivo international e.V., P.O. box 5108, 78430, Konstanz, Germany.

出版信息

Transl Psychiatry. 2023 Jan 19;13(1):14. doi: 10.1038/s41398-023-02316-6.

Abstract

Epigenetic processes allow plasticity in gene regulation in response to significant environmental events. Accumulating evidence suggests that effective psychotherapy is accompanied by epigenetic changes, rendering DNA methylation a potential biomarker of therapy success. Due to the central role of glucocorticoid dynamics in stress regulation and the alteration of aversive memories, glucocorticoid receptors are likely involved in the molecular processes that are required to successfully treat Posttraumatic Stress Disorder (PTSD). This study aimed to investigate the relationship between methylation at the glucocorticoid receptor gene (NR3C1) and PTSD treatment success of evidence-based psychotherapy. A sample of N = 153 conflict survivors from Northern Uganda (98 females and 55 males) with PTSD were treated with Narrative Exposure Therapy (NET). Diagnostic interviews and saliva sampling took place at pretreatment and 4 and 10 months after treatment completion. We investigated potential associations between PTSD symptom development and methylation changes at 38 CpG sites spanning NR3C1 over the three times of measurement using the repeated measures correlation. After accounting for multiple comparisons, DNA methylation at CpG site cg25535999 remained negatively associated with PTSD symptoms. These results were followed up by mixed models as well as structural equation modelling. These analyses revealed that treatment responders had a significant cg25535999 methylation increase after treatment with NET. Furthermore, lower methylation at cg25535999 pretreatment predicted a higher symptom improvement. Our results suggest different epigenetic profile dynamics at NR3C1 cg25535999 in therapy responders compared to non-responders and underscore the central role of glucocorticoid signaling in trauma-focused therapy.

摘要

表观遗传过程允许基因调控在应对重大环境事件时具有可塑性。越来越多的证据表明,有效的心理治疗伴随着表观遗传变化,使 DNA 甲基化为治疗成功的潜在生物标志物。由于糖皮质激素动态在应激调节和厌恶记忆改变中的核心作用,糖皮质激素受体可能参与成功治疗创伤后应激障碍 (PTSD) 所需的分子过程。本研究旨在调查糖皮质激素受体基因 (NR3C1) 甲基化与基于证据的心理治疗 PTSD 治疗成功之间的关系。来自乌干达北部的 153 名冲突幸存者(98 名女性和 55 名男性)患有 PTSD,接受了叙事暴露疗法 (NET)。诊断访谈和唾液采样分别在治疗前和治疗完成后 4 个月和 10 个月进行。我们使用重复测量相关分析,研究了 38 个跨越 NR3C1 的 CpG 位点在三个测量时间点上 PTSD 症状发展与甲基化变化之间的潜在关联。在考虑了多次比较后,NR3C1 的 CpG 位点 cg25535999 的 DNA 甲基化与 PTSD 症状呈负相关。这些结果通过混合模型和结构方程模型进行了跟进。这些分析表明,NET 治疗后,治疗反应者 cg25535999 的甲基化有显著增加。此外,治疗前 cg25535999 的低甲基化预测了更高的症状改善。我们的结果表明,NR3C1 的 cg25535999 处的不同表观遗传谱动力学在治疗反应者与非反应者之间存在差异,并强调了糖皮质激素信号在创伤聚焦治疗中的核心作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/090c/9852425/8f04673650f0/41398_2023_2316_Fig1_HTML.jpg

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