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DNA Methylation in Newborns and Maternal Smoking in Pregnancy: Genome-wide Consortium Meta-analysis

机译:新生儿和孕妇吸烟中的DNA甲基化:全基因组财团Meta分析

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Epigenetic modifications, including DNA methylation, represent a potential mechanism for environmental impacts on human disease. Maternal smoking in pregnancy remains an important public health problem that impacts child health in a myriad of ways and has potential lifelong consequences. The mechanisms are largely unknown, but epigenetics most likely plays a role. We formed the Pregnancy And Childhood Epigenetics (PACE) consortium and meta-analyzed, across 13 cohorts (n = 6,685), the association between maternal smoking in pregnancy and newborn blood DNA methylation at over 450,000 CpG sites (CpGs) by using the Illumina 450K BeadChip. Over 6,000 CpGs were differentially methylated in relation to maternal smoking at genome-wide statistical significance (false discovery rate, 5%), including 2,965 CpGs corresponding to 2,017 genes not previously related to smoking and methylation in either newborns or adults. Several genes are relevant to diseases that can be caused by maternal smoking (e.g., orofacial clefts and asthma) or adult smoking (e.g., certain cancers). A number of differentially methylated CpGs were associated with gene expression. We observed enrichment in pathways and processes critical to development. In older children (5 cohorts, n = 3,187), 100% of CpGs gave at least nominal levels of significance, far more than expected by chance (p value < 2.2 x 10(-16)). Results were robust to different normalization methods used across studies and cell type adjustment. In this large scale meta-analysis of methylation data, we identified numerous loci involved in response to maternal smoking in pregnancy with persistence into later childhood and provide insights into mechanisms underlying effects of this important exposure.
机译:表观遗传修饰,包括DNA甲基化,代表了环境对人类疾病影响的潜在机制。怀孕期间的孕妇吸烟仍然是一个重要的公共健康问题,它以多种方式影响着儿童的健康,并可能导致终身后果。机理尚不清楚,但表观遗传学最有可能发挥作用。我们成立了妊娠和儿童表观遗传学(PACE)联盟,并通过使用Illumina 450K对13个队列(n = 6685)中的孕妇吸烟与超过450,000 CpG位点(CpGs)的新生儿血液DNA甲基化之间的关联进行了荟萃分析。 BeadChip。在全基因组统计显着性上,超过6,000种CpGs与孕妇吸烟相关地甲基化差异(错误发现率,5%),包括2,965个CpGs,它们对应于2,017个先前与新生儿或成年人中的吸烟和甲基化无关的基因。几种基因与孕妇吸烟(例如口面部裂口和哮喘)或成人吸烟(例如某些癌症)可能引起的疾病有关。许多差异甲基化的CpG与基因表达有关。我们观察到了对发展至关重要的途径和过程的丰富化。在年龄较大的儿童(5个队列,n = 3,187)中,100%的CpG至少具有名义上的显着水平,远高于偶然的预期(p值<2.2 x 10(-16))。结果对于研究和细胞类型调整中使用的不同归一化方法均很可靠。在这项大规模的甲基化数据荟萃分析中,我们确定了许多与孕妇吸烟相关的基因座,并持续到儿童期,并提供了对该重要暴露影响的潜在机制的见解。

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