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Detection of Fetomaternal Genotype Associations in Early-Onset Disorders: Evaluation of Different Methods and Their Application to Childhood Leukemia

机译:早期疾病中Fetomaternal基因型关联的检测:不同方法的评估及其在儿童白血病中的应用

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摘要

Several designs and analytical approaches have been proposed to dissect offspring from maternal genetic contributions to early-onset diseases. However, lack of parental controls halts the direct verification of the assumption of mating symmetry (MS) required to assess maternally-mediated effects. In this study, we used simulations to investigate the performance of existing methods under mating asymmetry (MA) when parents of controls are missing. Our results show that the log-linear, likelihood-based framework using a case-triad/case-control hybrid design provides valid tests for maternal genetic effects even under MA. Using this approach, we examined fetomaternal associations between 29 SNPs in 12 cell-cycle genes and childhood pre-B acute lymphoblastic leukemia (ALL). We identified putative fetomaternal effects at loci CDKN2A rs36228834 (P = .017) and CDKN2B rs36229158 (P = .022) that modulate the risk of childhood ALL. These data further corroborate the importance of the mother's genotype on the susceptibility to early-onset diseases.
机译:已经提出了几种设计和分析方法来剖析后代与母体遗传因素对早期疾病的关系。但是,由于缺乏父母控制,因此无法直接验证评估母体介导效应所需的交配对称性(MS)假设。在这项研究中,我们使用模拟方法来研究缺少对照父母时在交配不对称性(MA)下现有方法的性能。我们的结果表明,使用病例三元组/病例对照混合设计的对数线性,基于可能性的框架即使在MA情况下也能提供有效的孕产妇遗传效应测试。使用这种方法,我们检查了12个细胞周期基因中29个SNP与儿童前B型急性淋巴细胞白血病(ALL)之间的母系关联。我们在基因座CDKN2A rs36228834(P = .017)和CDKN2B rs36229158(P = .022)处确定了可能的fetomaternal效应,这些效应调节了儿童ALL的风险。这些数据进一步证实了母亲的基因型对早期发病的敏感性的重要性。

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