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Placental epigenetic clocks: estimating gestational age using placental DNA methylation levels

机译:胎盘表观遗传钟:使用胎盘DNA甲基化水平估算胎龄

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摘要

The human pan-tissue epigenetic clock is widely used for estimating age across the entire lifespan, but it does not lend itself well to estimating gestational age (GA) based on placental DNAm methylation (DNAm) data. We replicate previous findings demonstrating a strong correlation between GA and genome-wide DNAm changes. Using substantially more DNAm arrays (n=1,102 in the training set) than a previous study, we present three new placental epigenetic clocks: 1) a robust placental clock (RPC) which is unaffected by common pregnancy complications (e.g., gestational diabetes, preeclampsia), and 2) a control placental clock (CPC) constructed using placental samples from pregnancies without known placental pathology, and 3) a refined RPC for uncomplicated term pregnancies. These placental clocks are highly accurate estimators of GA based on placental tissue; e.g., predicted GA based on RPC is highly correlated with actual GA (r>0.95 in test data, median error less than one week). We show that epigenetic clocks derived from cord blood or other tissues do not accurately estimate GA in placental samples. While fundamentally different from Horvath’s pan-tissue epigenetic clock, placental clocks closely track fetal age during development and may have interesting applications.
机译:人类全组织表观遗传时钟被广泛用于估计整个寿命中的年龄,但是它不能很好地根据胎盘DNAm甲基化(DNAm)数据来估计胎龄(GA)。我们重复以前的发现,证明GA和全基因组DNAm变化之间有很强的相关性。使用比以前的研究多得多的DNAm阵列(训练组中n = 1102),我们提出了三个新的胎盘表观遗传钟:1)坚固的胎盘钟(RPC),不受普通妊娠并发症(例如妊娠糖尿病,先兆子痫)的影响),以及2)使用胎盘样本(无已知胎盘病理学)构建的对照胎盘时钟(CPC),以及3)用于单纯妊娠足月的精制RPC。这些胎盘时钟是基于胎盘组织的GA的高精度估算器。例如,基于RPC的预测GA与实际GA高度相关(测试数据中r> 0.95,中值误差小于一周)。我们表明,源自脐带血或其他组织的表观遗传时钟不能准确估计胎盘样本中的GA。尽管胎盘钟与Horvath的全组织表观遗传钟完全不同,但胎盘钟可密切跟踪发育过程中的胎儿年龄,并可能具有有趣的用途。

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