Elbasheir Aziz, Katrinli Seyma, Kearney Breanne E, Lanius Ruth A, Harnett Nathaniel G, Carter Sierra E, Ely Timothy D, Bradley Bekh, Gillespie Charles F, Stevens Jennifer S, Lori Adriana, van Rooij Sanne J H, Powers Abigail, Jovanovic Tanja, Smith Alicia K, Fani Negar
Department of Psychiatry and Behavioral Sciences, Emory University School of Medicine, Atlanta, Georgia.
Department of Neuroscience, Schulich School of Medicine and Dentistry, Western University, London, Ontario, Canada.
JAMA Netw Open. 2024 Jun 3;7(6):e2416588. doi: 10.1001/jamanetworkopen.2024.16588.
Racial discrimination increases the risk of adverse brain health outcomes, potentially via neuroplastic changes in emotion processing networks. The involvement of deep brain regions (brainstem and midbrain) in these responses is unknown. Potential associations of racial discrimination with alterations in deep brain functional connectivity and accelerated epigenetic aging, a process that substantially increases vulnerability to health problems, are also unknown.
To examine associations of racial discrimination with brainstem and midbrain resting-state functional connectivity (RSFC) and DNA methylation age acceleration (DMAA) among Black women in the US.
DESIGN, SETTING, AND PARTICIPANTS: This cohort study was conducted between January 1, 2012, and February 28, 2015, and included a community-based sample of Black women (aged ≥18 years) recruited as part of the Grady Trauma Project. Self-reported racial discrimination was examined in association with seed-to-voxel brain connectivity, including the locus coeruleus (LC), periaqueductal gray (PAG), and superior colliculus (SC); an index of DMAA (Horvath clock) was also evaluated. Posttraumatic stress disorder (PTSD), trauma exposure, and age were used as covariates in statistical models to isolate racial discrimination-related variance. Data analysis was conducted between January 10 and October 30, 2023.
Varying levels of racial discrimination exposure, other trauma exposure, and posttraumatic stress disorder (PTSD).
Racial discrimination frequency was assessed with the Experiences of Discrimination Scale, other trauma exposure was evaluated with the Traumatic Events Inventory, and current PTSD was evaluated with the PTSD Symptom Scale. Seed-to-voxel functional connectivity analyses were conducted with LC, PAG, and SC seeds. To assess DMAA, the Methylation EPIC BeadChip assay (Illumina) was conducted with whole-blood samples from a subset of 49 participants.
This study included 90 Black women, with a mean (SD) age of 38.5 (11.3) years. Greater racial discrimination was associated with greater left LC RSFC to the bilateral precuneus (a region within the default mode network implicated in rumination and reliving of past events; cluster size k = 228; t85 = 4.78; P < .001, false discovery rate-corrected). Significant indirect effects were observed for the left LC-precuneus RSFC on the association between racial discrimination and DMAA (β [SE] = 0.45 [0.16]; 95% CI, 0.12-0.77).
In this study, more frequent racial discrimination was associated with proportionately greater RSFC of the LC to the precuneus, and these connectivity alterations were associated with DMAA. These findings suggest that racial discrimination contributes to accelerated biological aging via altered connectivity between the LC and default mode network, increasing vulnerability for brain health problems.
种族歧视会增加不良脑健康结局的风险,可能是通过情绪处理网络中的神经可塑性变化。目前尚不清楚深部脑区(脑干和中脑)是否参与这些反应。种族歧视与深部脑功能连接改变以及加速表观遗传衰老(这一过程会大幅增加健康问题的易感性)之间的潜在关联也尚不清楚。
研究美国黑人女性中种族歧视与脑干和中脑静息态功能连接(RSFC)以及DNA甲基化年龄加速(DMAA)之间的关联。
设计、背景和参与者:这项队列研究于2012年1月1日至2015年2月28日进行,纳入了作为格雷迪创伤项目一部分招募的社区黑人女性样本(年龄≥18岁)。研究了自我报告的种族歧视与种子点到体素的脑连接性之间的关系,包括蓝斑(LC)、导水管周围灰质(PAG)和上丘(SC);还评估了DMAA指数(霍瓦斯时钟)。创伤后应激障碍(PTSD)、创伤暴露和年龄在统计模型中用作协变量,以分离与种族歧视相关的方差。数据分析于2023年1月10日至10月30日进行。
不同程度的种族歧视暴露、其他创伤暴露和创伤后应激障碍(PTSD)。
使用歧视经历量表评估种族歧视频率,使用创伤事件量表评估其他创伤暴露,使用PTSD症状量表评估当前的PTSD。采用LC、PAG和SC种子点进行种子点到体素的功能连接分析。为了评估DMAA,对49名参与者子集的全血样本进行了甲基化EPIC芯片检测(Illumina)。
本研究纳入了90名黑人女性,平均(标准差)年龄为38.5(11.3)岁。种族歧视程度越高,左侧LC与双侧楔前叶的RSFC越强(楔前叶是默认模式网络中的一个区域,与对过去事件的沉思和回忆有关;聚类大小k = 228;t85 = 4.78;P <.001,经错误发现率校正)。观察到左侧LC - 楔前叶RSFC在种族歧视与DMAA之间的关联中存在显著的间接效应(β [标准误] = 0.45 [0.16];95%可信区间,0.12 - 0.77)。
在本研究中,更频繁的种族歧视与LC与楔前叶成比例更强的RSFC相关,并且这些连接性改变与DMAA相关。这些发现表明,种族歧视通过改变LC与默认模式网络之间的连接性导致生物衰老加速,增加了脑健康问题的易感性。
