Differential impact of prenatal PTSD symptoms and preconception trauma exposure on placental NR3C1 and FKBP5 methylation.

IF 2.6 4区 心理学 Q2 BEHAVIORAL SCIENCES
Laura R Stroud, Nancy C Jao, L G Ward, Sharon Y Lee, Carmen J Marsit
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引用次数: 0

Abstract

Perinatal stress is associated with altered placental methylation, which plays a critical role in fetal development and infant outcomes. This proof-of-concept pilot study investigated the impact of lifetime trauma exposure and perinatal PTSD symptoms on epigenetic regulation of placenta glucocorticoid signaling genes (NR3C1 and FKBP5). Lifetime trauma exposure and PTSD symptoms during pregnancy were assessed in a racially/ethnically diverse sample of pregnant women (N = 198). Participants were categorized into three groups: (1) No Trauma (-T); (2) Trauma, No Symptoms (T - S); and (3) Trauma and Symptoms (T + S). Placental tissue was analyzed via bisulfite pyrosequencing for degree of methylation at the NR3C1 promoter and FKBP5 regulatory regions. Analyses of covariance were used to test group differences in percentages of NR3C1 and FKBP5 methylation overall and at each CpG site. We found a significant impact of PTSD symptoms on placental NR3C1 methylation. Compared to the -T group, the T + S group had greater NR3C1 methylation overall and at CpG6, CpG8, CpG9, and CpG13, but lower methylation at CpG5. The T + S group had significantly higher NR3C1 methylation overall and at CpG8 compared to the T - S group. There were no differences between the T - S group and - T group. Additionally, no group differences emerged for FKBP5 methylation. Pregnant trauma survivors with PTSD symptoms exhibited differential patterns of placental NR3C1 methylation compared to trauma survivors without PTSD symptoms and pregnant women unexposed to trauma. Results highlight the critical importance of interventions to address the mental health of pregnant trauma survivors.

产前创伤后应激障碍症状和孕前创伤暴露对胎盘 NR3C1 和 FKBP5 甲基化的不同影响。
围产期压力与胎盘甲基化的改变有关,而胎盘甲基化在胎儿发育和婴儿结局中起着至关重要的作用。这项概念验证试验研究调查了终生创伤暴露和围产期创伤后应激障碍症状对胎盘糖皮质激素信号基因(NR3C1和FKBP5)表观遗传调控的影响。研究人员对不同种族/族裔的孕妇样本(N = 198)进行了孕期终生创伤暴露和创伤后应激障碍症状的评估。参与者被分为三组:(1) 无创伤 (-T);(2) 有创伤、无症状 (T - S);(3) 有创伤和症状 (T + S)。胎盘组织通过亚硫酸氢盐热测序分析 NR3C1 启动子和 FKBP5 调控区的甲基化程度。我们使用协方差分析来检验 NR3C1 和 FKBP5 整体甲基化百分比以及各 CpG 位点甲基化百分比的组间差异。我们发现创伤后应激障碍症状对胎盘 NR3C1 甲基化有明显影响。与 -T 组相比,T + S 组的 NR3C1 甲基化程度总体较高,CpG6、CpG8、CpG9 和 CpG13 的甲基化程度也较高,但 CpG5 的甲基化程度较低。与 T - S 组相比,T + S 组的总体 NR3C1 甲基化程度和 CpG8 的甲基化程度明显更高。T - S 组和 - T 组之间没有差异。此外,FKBP5 甲基化也没有出现组间差异。与没有创伤后应激障碍症状的创伤幸存者和未受过创伤的孕妇相比,有创伤后应激障碍症状的创伤幸存者的胎盘 NR3C1 甲基化表现出不同的模式。研究结果凸显了干预创伤幸存者孕妇心理健康的重要性。
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来源期刊
CiteScore
5.60
自引率
0.00%
发文量
25
审稿时长
6-12 weeks
期刊介绍: The journal Stress aims to provide scientists involved in stress research with the possibility of reading a more integrated view of the field. Peer reviewed papers, invited reviews and short communications will deal with interdisciplinary aspects of stress in terms of: the mechanisms of stressful stimulation, including within and between individuals; the physiological and behavioural responses to stress, and their regulation, in both the short and long term; adaptive mechanisms, coping strategies and the pathological consequences of stress. Stress will publish the latest developments in physiology, neurobiology, molecular biology, genetics research, immunology, and behavioural studies as they impact on the understanding of stress and its adverse consequences and their amelioration. Specific approaches may include transgenic/knockout animals, developmental/programming studies, electrophysiology, histochemistry, neurochemistry, neuropharmacology, neuroanatomy, neuroimaging, endocrinology, autonomic physiology, immunology, chronic pain, ethological and other behavioural studies and clinical measures.
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