Department of Psychiatry, Faculty of Medicine and Health Sciences Stellenbosch University, Cape Town, South Africa.
Gender and Health Research Unit, South African Medical Research Council, Cape Town, South Africa.
Transl Psychiatry. 2021 Nov 19;11(1):594. doi: 10.1038/s41398-021-01608-z.
Rape is associated with a high risk for posttraumatic stress disorder (PTSD). DNA methylation changes may confer risk or protection for PTSD following rape by regulating the expression of genes implicated in pathways affected by PTSD. We aimed to: (1) identify epigenome-wide differences in methylation profiles between rape-exposed women with and without PTSD at 3-months post-rape, in a demographically and ethnically similar group, drawn from a low-income setting; (2) validate and replicate the findings of the epigenome-wide analysis in selected genes (BRSK2 and ADCYAP1); and (3) investigate baseline and longitudinal changes in BRSK2 and ADCYAP1 methylation over six months in relation to change in PTSD symptom scores over 6 months, in the combined discovery/validation and replication samples (n = 96). Rape-exposed women (n = 852) were recruited from rape clinics in the Rape Impact Cohort Evaluation (RICE) umbrella study. Epigenome-wide differentially methylated CpG sites between rape-exposed women with (n = 24) and without (n = 24) PTSD at 3-months post-rape were investigated using the Illumina EPIC BeadChip in a discovery cohort (n = 48). Validation (n = 47) and replication (n = 49) of BRSK2 and ADCYAP1 methylation findings were investigated using EpiTYPER technology. Longitudinal change in BRSK2 and ADCYAP1 was also investigated using EpiTYPER technology in the combined sample (n = 96). In the discovery sample, after adjustment for multiple comparisons, one differentially methylated CpG site (chr10: 61385771/ cg01700569, p = 0.049) and thirty-four differentially methylated regions were associated with PTSD status at 3-months post-rape. Decreased BRSK2 and ADCYAP1 methylation at 3-months and 6-months post-rape were associated with increased PTSD scores at the same time points, but these findings did not remain significant in adjusted models. In conclusion, decreased methylation of BRSK2 may result in abnormal neuronal polarization, synaptic development, vesicle formation, and disrupted neurotransmission in individuals with PTSD. PTSD symptoms may also be mediated by differential methylation of the ADCYAP1 gene which is involved in stress regulation. Replication of these findings is required to determine whether ADCYAP1 and BRSK2 are biomarkers of PTSD and potential therapeutic targets.
强奸与创伤后应激障碍(PTSD)的高风险相关。DNA 甲基化变化可能通过调节 PTSD 相关途径中受影响的基因的表达,为强奸后 PTSD 的风险或保护提供依据。我们旨在:(1)在一个来自低收入环境、人口统计学和种族相似的群体中,在强奸后 3 个月,确定暴露于强奸的女性中 PTSD 与无 PTSD 之间甲基化谱的全基因组差异;(2)验证和复制在选定基因(BRSK2 和 ADCYAP1)中全基因组分析的发现;(3)在发现/验证和复制样本(n=96)中,在 6 个月内调查 BRSK2 和 ADCYAP1 甲基化的基线和纵向变化与 6 个月内 PTSD 症状评分的变化之间的关系。从强奸影响队列评估(RICE)伞式研究中的强奸诊所招募了暴露于强奸的女性(n=852)。在发现队列(n=48)中使用 Illumina EPIC BeadChip 研究了强奸后 3 个月有(n=24)和无(n=24)PTSD 的暴露于强奸的女性之间全基因组差异甲基化 CpG 位点。使用 EpiTYPER 技术验证(n=47)和复制(n=49)BRSK2 和 ADCYAP1 甲基化发现。在合并样本(n=96)中还使用 EpiTYPER 技术研究了 BRSK2 和 ADCYAP1 的纵向变化。在发现样本中,经过多次比较调整后,一个差异甲基化 CpG 位点(chr10: 61385771/cg01700569,p=0.049)和 34 个差异甲基化区域与强奸后 3 个月的 PTSD 状态相关。强奸后 3 个月和 6 个月时 BRSK2 和 ADCYAP1 甲基化减少与同一时间点 PTSD 评分增加相关,但在调整模型中这些发现并不显著。总之,BRSK2 甲基化减少可能导致 PTSD 个体中神经元极化、突触发育、囊泡形成和神经传递中断异常。ADCYAP1 基因参与应激调节,其差异甲基化也可能介导 PTSD 症状。需要对这些发现进行复制,以确定 ADCYAP1 和 BRSK2 是否是 PTSD 的生物标志物和潜在的治疗靶点。
