Del Toro Juan, Martz Connor, Freilich Colin D, Rea-Sandin Gianna, Markon Kristian, Cole Steve, Krueger Robert F, Wilson Sylia
Department of Psychology, University of Minnesota-Twin Cities, Minneapolis.
Population Research Center, University of Texas-Austin, Austin.
JAMA Pediatr. 2024 Dec 1;178(12):1298-1306. doi: 10.1001/jamapediatrics.2024.3669.
Individuals exposed to discrimination may exhibit greater epigenetic age acceleration (ie, cellular indicators of premature aging) over time, but few studies have examined longitudinal changes in epigenetic age acceleration, the heterogeneity in these changes for diverse groups of youths, and contextual explanations (ie, discrimination) for differences by ethnicity or race.
To provide a descriptive illustration of changes in epigenetic age acceleration across childhood and adolescence among an ethnically and racially diverse sample of youths.
DESIGN, SETTING, AND PARTICIPANTS: This cohort study leveraged longitudinal data on a large sample of youths from low-income households in 20 large urban US cities who provided repeated assessments of saliva tissue samples at ages 9 and 15 years for DNA methylation analysis. Of 4898 youths from the Future of Families and Child Well-Being study, an ongoing study that oversampled children born to unmarried parents from 1998 to 2000, 2039 were included in the present analysis, as these youths had salivary DNA methylation data assayed and publicly available. Analyses were conducted from March 2023 to June 2024.
Racialized intrusive encounters with police (eg, stop and frisk and racial slurs).
Analyses were conducted to examine longitudinal changes in salivary epigenetic age acceleration over time, whether such changes varied across ethnically and racially diverse groups of youths, and whether police intrusion was associated with variation across ethnic and racial groups.
Among 2039 youths (mean [SD] age at baseline, 9.27 [0.38] years; 1023 [50%] male and 1016 [50%] female; 917 [45%] Black, 430 [21%] Hispanic or Latino, 351 [17%] White, and 341 [17%] other, including multiple races and self-identified other) with salivary epigenetic clocks at 9 and 15 years of age, longitudinal results showed that White youths exhibited less accelerated epigenetic aging over time than did Black and Hispanic or Latino youths and those reporting other or multiple races or ethnicities from ages 9 to 15 years, particularly in the Hannum (B, 1.54; 95% CI, 0.36-2.18), GrimAge (B, 1.31; 95% CI, 0.68-1.97), and DunedinPACE epigenetic clocks (B, 0.27; 95% CI, 0.11-0.44). Across these clocks and the PhenoAge clock, police intrusion was associated with Black youths' more accelerated epigenetic aging (Hannum: B, 0.11; 95% CI, 0.03-0.23; GrimAge: B, 0.09; 95% CI, 0.03-0.18; PhenoAge: B, 0.08; 95% CI, 0.02-0.18; DunedinPACE: B, 0.01; 95% CI, 0.01-0.03).
The transition from childhood to adolescence may represent a sensitive developmental period when racism can have long-term deleterious impacts on healthy human development across the life span. Future research should build on the present study and interrogate which social regularities and policies may be perpetuating discrimination against ethnically and racially minoritized adolescents.
随着时间推移,遭受歧视的个体可能表现出更大的表观遗传年龄加速(即过早衰老的细胞指标),但很少有研究考察表观遗传年龄加速的纵向变化、不同青年群体中这些变化的异质性,以及种族或民族差异的背景解释(即歧视)。
对不同种族和民族的青年样本在童年和青少年时期表观遗传年龄加速的变化进行描述性说明。
设计、背景和参与者:这项队列研究利用了来自美国20个大城市低收入家庭的大量青年的纵向数据,这些青年在9岁和15岁时提供了唾液组织样本的重复评估,用于DNA甲基化分析。在4898名来自“家庭与儿童福祉的未来”研究的青年中,该研究是一项正在进行的研究,对1998年至2000年未婚父母所生孩子进行了过度抽样,本分析纳入了2039名青年,因为这些青年有唾液DNA甲基化数据可供分析且已公开。分析于2023年3月至2024年6月进行。
与警察的种族化侵扰性接触(如拦截搜身和种族诋毁)。
进行分析以考察唾液表观遗传年龄加速随时间的纵向变化,这些变化在不同种族和民族的青年群体中是否存在差异,以及警察侵扰是否与不同种族和民族群体的差异相关。
在2039名9岁和15岁有唾液表观遗传时钟的青年中(基线时平均[标准差]年龄为9.27[0.38]岁;1023名[50%]为男性,1016名[50%]为女性;917名[45%]为黑人,430名[21%]为西班牙裔或拉丁裔,351名[17%]为白人,341名[17%]为其他,包括多种族和自我认定的其他种族),纵向结果显示,从9岁到15岁,白人青年表观遗传衰老加速程度低于黑人、西班牙裔或拉丁裔青年以及报告其他或多种种族或民族的青年,特别是在汉纳姆表观遗传时钟(B,1.54;95%置信区间,0.36 - 2.18)、GrimAge表观遗传时钟(B,1.31;95%置信区间,0.68 - 1.97)和达尼丁PACE表观遗传时钟(B,0.27;95%置信区间,0.11 - 0.44)方面。在这些表观遗传时钟和PhenoAge表观遗传时钟中,警察侵扰与黑人青年更快速的表观遗传衰老相关(汉纳姆表观遗传时钟:B,0.11;95%置信区间,0.03 - 0.23;GrimAge表观遗传时钟:B,0.09;95%置信区间,0.03 - 0.18;PhenoAge表观遗传时钟:B,0.08;95%置信区间,0.02 - 0.18;达尼丁PACE表观遗传时钟:B,0.01;95%置信区间,0.01 - 0.03)。
从童年到青少年的过渡可能是一个敏感的发育时期,此时种族主义可能对整个生命周期的健康人类发展产生长期有害影响。未来的研究应以本研究为基础,探究哪些社会规律和政策可能使对种族和民族少数群体青少年的歧视长期存在。
