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体外受精与新生儿双胞胎的全基因组及IGF2/H19甲基化变异的关联。

Association of in vitro fertilization with global and IGF2/H19 methylation variation in newborn twins.

作者信息

Loke Y J, Galati J C, Saffery R, Craig J M

机构信息

1Early Life Epigenetics Group,Murdoch Childrens Research Institute (MCRI),Royal Children's Hospital,Parkville,VIC,Australia.

2Clinical Epidemiology and Biostatistics Unit,MCRI,Royal Children's Hospital,Parkville,VIC,Australia.

出版信息

J Dev Orig Health Dis. 2015 Apr;6(2):115-24. doi: 10.1017/S2040174415000161.

Abstract

In vitro fertilization (IVF) and its subset intracytoplasmic sperm injection (ICSI), are widely used medical treatments for conception. There has been controversy over whether IVF is associated with adverse short- and long-term health outcomes of offspring. As with other prenatal factors, epigenetic change is thought to be a molecular mediator of any in utero programming effects. Most studies focused on DNA methylation at gene-specific and genomic level, with only a few on associations between DNA methylation and IVF. Using buccal epithelium from 208 twin pairs from the Peri/Postnatal Epigenetic Twin Study (PETS), we investigated associations between IVF and DNA methylation on a global level, using the proxies of Alu and LINE-1 interspersed repeats in addition to two locus-specific regulatory regions within IGF2/H19, controlling for 13 potentially confounding factors. Using multiple correction testing, we found strong evidence that IVF-conceived twins have lower DNA methylation in Alu, and weak evidence of lower methylation in one of the two IGF2/H19 regulatory regions and LINE-1, compared with naturally conceived twins. Weak evidence of a relationship between ICSI and DNA methylation within IGF2/H19 regulatory region was found, suggesting that one or more of the processes associated with IVF/ICSI may contribute to these methylation differences. Lower within- and between-pair DNA methylation variation was also found in IVF-conceived twins for LINE-1, Alu and one IGF2/H19 regulatory region. Although larger sample sizes are needed, our results provide additional insight to the possible influence of IVF and ICSI on DNA methylation. To our knowledge, this is the largest study to date investigating the association of IVF and DNA methylation.

摘要

体外受精(IVF)及其分支卵胞浆内单精子注射(ICSI)是广泛应用于受孕的医学治疗方法。关于IVF是否与后代的短期和长期不良健康后果相关一直存在争议。与其他产前因素一样,表观遗传变化被认为是任何子宫内编程效应的分子介导因素。大多数研究集中在基因特异性和基因组水平的DNA甲基化,只有少数研究关注DNA甲基化与IVF之间的关联。我们利用围产期/产后表观遗传双胞胎研究(PETS)中208对双胞胎的颊黏膜上皮,除了IGF2/H19内的两个位点特异性调控区域外,还使用Alu和LINE-1散布重复序列作为代理,在全球范围内研究IVF与DNA甲基化之间的关联,并控制13个潜在的混杂因素。通过多重校正测试,我们发现有力证据表明,与自然受孕的双胞胎相比,IVF受孕的双胞胎Alu中的DNA甲基化水平较低,并且在IGF2/H19的两个调控区域之一和LINE-1中甲基化水平较低的证据较弱。发现ICSI与IGF2/H19调控区域内的DNA甲基化之间存在微弱的关系证据,这表明与IVF/ICSI相关的一个或多个过程可能导致这些甲基化差异。在IVF受孕的双胞胎中,LINE-1、Alu和一个IGF2/H19调控区域的配对内和配对间DNA甲基化变异也较低。尽管需要更大的样本量,但我们的结果为IVF和ICSI对DNA甲基化的可能影响提供了更多见解。据我们所知,这是迄今为止调查IVF与DNA甲基化关联的最大规模研究。

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