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Genome wide study of maternal and parent-of-origin effects on the etiology of orofacial clefts

机译:基因组对母亲和父母的父母和父母母亲对orofacial leftts病因的影响

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摘要

We performed a genome wide association analysis of maternally-mediated genetic effects and parent-of-origin effects on risk of orofacial clefting using over 2,000 case-parent triads collected through an international cleft consortium. We used log-linear regression models to test individual SNPs. For SNPs with a p-value <10−5 for maternal genotypic effects, we also applied a haplotype-based method, TRIMM, to extract potential information from clusters of correlated SNPs. None of the SNPs were significant at the genome wide level. Our results suggest neither maternal genome nor parent of origin effects play major roles in the etiology of orofacial clefting in our sample. This finding is consistent with previous genetic studies and recent population-based cohort studies in Norway and Denmark, which showed no apparent difference between mother-to-offspring and father-to-offspring recurrence of clefting. We, however, cannot completely rule out maternal genome or parent of origin effects as risk factors because very small effects might not be detectable with our sample size, they may influence risk through interactions with environmental exposures or may act through a more complex network of interacting genes. Thus the most promising SNPs identified by this study may still be worth further investigation.
机译:我们对母动介导的遗传效果和父母起源的基因组关联分析进行了血液介导的遗传效应和原产地对orofacial Cleding的风险的影响,使用通过国际裂缝联盟收集的2,000个案例母体三国组织。我们使用了对数线性回归模型来测试单个SNP。对于具有p值<10 -5的SNP进行母体基因型效应,我们还应用了基于单倍型的方法Trimm,以从相关的SNP的簇中提取潜在信息。没有一个SNP在基因组广泛水平上显着。我们的结果表明,母体基因组和父母的原始效应都不在我们样本中的orofacial Clepting的病因中发挥重要作用。这一发现与挪威和丹麦的先前基于遗传学研究和最近的人口队列研究一致,在母亲到后代和父亲到后代复发之间没有明显差异。然而,我们不能完全排除母体基因组或父母的原始效应作为风险因素,因为我们的样本大小可能无法检测到非常小的效果,它们可能通过与环境暴露的相互作用影响风险,或者可以通过更复杂的交互网络行动基因。因此,本研究确定的最有前途的SNP可能仍然值得进一步调查。

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