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母体心脏代谢因素和遗传背景影响胎盘的表观遗传衰老。

Maternal cardiometabolic factors and genetic ancestry influence epigenetic aging of the placenta.

机构信息

Epidemiology Branch, Division of Intramural Population Health Research, Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, MD, USA.

Laboratory of Epidemiology and Population Sciences, National Institute on Aging, National Institutes of Health, Baltimore, MD, USA.

出版信息

J Dev Orig Health Dis. 2021 Feb;12(1):34-41. doi: 10.1017/S2040174419000801. Epub 2020 Jan 17.

Abstract

Disruption of physiological aging of the placenta can lead to pregnancy complications and increased risk for cardiometabolic diseases during childhood and adulthood. Maternal metabolic and genetic factors need to operate in concert with placental development for optimal pregnancy outcome. However, it is unknown whether maternal cardiometabolic status and genetic ancestry contribute to differences in placental epigenetic age acceleration (PAA). We investigated whether maternal prepregnancy obesity, gestational weight gain (GWG), blood pressure, and genetic ancestry influence PAA. Among 301 pregnant women from 4 race/ethnic groups who provided placenta samples at delivery as part of the National Institute of Child Health and Human Development Fetal Growth Studies, placental DNA methylation age was estimated using 62 CpGs known to predict placental aging. PAA was defined to be the difference between placental DNA methylation age and gestational age at birth. Percentage of genetic ancestries was estimated using genotype data. We found that a 1 kg/week increase in GWG was associated with up to 1.71 (95% CI: -3.11, -0.32) week lower PAA. Offspring Native American ancestry and African ancestry were associated, respectively, with higher and lower PAA among Hispanics, and maternal East Asian ancestry was associated with lower PAA among Asians (p < 0.05). Among mothers with a male offspring, blood pressure was associated with lower PAA across all three trimesters (p < 0.05), prepregnancy obesity compared to normal weight was associated with 1.24 (95% CI: -2.24, -0.25) week lower PAA. In summary, we observed that maternal cardiometabolic factors and genetic ancestry influence placental epigenetic aging and some of these influences may be male offspring-specific.

摘要

胎盘生理衰老的破坏可导致妊娠并发症,并增加儿童和成年期患心脏代谢疾病的风险。母体代谢和遗传因素需要与胎盘发育协同作用,以实现最佳妊娠结局。然而,尚不清楚母体心脏代谢状况和遗传背景是否会导致胎盘表观遗传年龄加速(PAA)的差异。我们研究了母体孕前肥胖、孕期体重增加(GWG)、血压和遗传背景是否会影响 PAA。在作为国家儿童健康与人类发展研究所胎儿生长研究的一部分,在分娩时提供胎盘样本的 4 个种族/民族的 301 名孕妇中,使用已知可预测胎盘老化的 62 个 CpG 来估计胎盘 DNA 甲基化年龄。PAA 定义为胎盘 DNA 甲基化年龄与出生时的胎龄之间的差异。使用基因型数据估计遗传背景的百分比。我们发现,GWG 每周增加 1 公斤与 PAA 降低多达 1.71 周(95%CI:-3.11,-0.32)相关。非裔美国人后裔和非洲裔美国人后裔与西班牙裔中的 PAA 分别较高和较低相关,而东亚裔母亲与亚洲人中的 PAA 较低相关(p<0.05)。在有男性后代的母亲中,血压与所有三个孕期的 PAA 较低相关(p<0.05),与正常体重相比,孕前肥胖与 PAA 降低 1.24 周(95%CI:-2.24,-0.25)相关。总之,我们观察到母体心脏代谢因素和遗传背景会影响胎盘的表观遗传衰老,其中一些影响可能是针对男性后代的。

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