Prenatal exposure to genocide accelerates epigenetic aging in third- and fourth-generation clocks among young adults in Rwanda.

IF 5.4 Q1 MEDICINE, RESEARCH & EXPERIMENTAL
Glorieuse Uwizeye, Luisa M Rivera, Hannah G Stolrow, Brock C Christensen, Julienne N Rutherford, Zaneta M Thayer
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Abstract

Background: Prenatal exposure genocide-related to trauma has been previously associated with increased morbidity. Whether the prenatal exposure to genocide and rape also impacts various aspects of biological regulation, including patterns of DNA methylation, remains unknown. The purpose of this study was to evaluate whether prenatal exposure to genocide-related trauma, including conception through rape, is associated with accelerated epigenetic aging, a molecular indicator of biological aging.

Methods: We used a cross-sectional dataset to evaluate whether prenatal exposure to genocide or genocidal rape, among individuals conceived during the 1994 genocide against Tutsi in Rwanda were associated with differences in age acceleration in a range of clocks (first generation: Horvath and Hannum; second generation: PhenoAge; third generation: GrimAge and DunedinPace; and fourth generation: YingDamAge and YingAdaptAge), while taking into account exposure to adverse childhood experiences (ACEs). Participants were 24 years old during the time of data collection, and we enrolled 46 female and 45 male participants. Control participants were those of Rwandan descent who did not live in Rwanda during the genocide.

Results: We show that there are no differences in age acceleration observed with first- or second-generation age clocks. However, age acceleration was associated with prenatal exposure to extreme stress for all other clocks, with the greatest acceleration observed in the genocidal rape conception group. For the YingDamAge clock, acceleration effects were strengthened after the inclusion of ACEs.

Conclusions: Our findings suggest that prenatal trauma exposure is associated with epigenetic age acceleration. Third and fourth-generation clocks may more accurately capture these relationships.

在卢旺达,产前暴露于种族灭绝会加速第三代和第四代年轻人的表观遗传衰老。
背景:产前暴露与创伤相关的种族灭绝先前与发病率增加有关。产前暴露于种族灭绝和强奸是否也会影响生物调节的各个方面,包括DNA甲基化模式,目前尚不清楚。这项研究的目的是评估产前暴露于种族灭绝相关的创伤,包括通过强奸怀孕,是否与加速表观遗传衰老有关,表观遗传衰老是生物衰老的一种分子指标。方法:我们使用一个横断面数据集来评估在1994年卢旺达对图西族的种族灭绝期间怀孕的个体中,产前暴露于种族灭绝或种族灭绝强奸是否与一系列时钟的年龄加速差异有关(第一代:Horvath和Hannum;第二代:PhenoAge;第三代:格里马奇和邓尼迪佩斯;第四代:YingDamAge和YingAdaptAge),同时考虑不良童年经历(ace)。参与者在数据收集时年龄为24岁,我们招募了46名女性和45名男性参与者。对照组的参与者是在种族灭绝期间不在卢旺达居住的卢旺达后裔。结果:我们表明,在年龄加速观察到的第一代和第二代时钟没有差异。然而,年龄加速与产前暴露于所有其他时钟的极端压力有关,在种族灭绝强奸怀孕组中观察到的加速最大。对于YingDamAge时钟,在加入ace后加速效果得到了加强。结论:我们的研究结果表明,产前创伤暴露与表观遗传年龄加速有关。第三代和第四代时钟可能更准确地捕捉到这些关系。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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