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Methods for detection of parent-of-origin effects in genetic studies of case-parents triads.

机译:在个案父母三联体的遗传研究中检测原产地效应的方法。

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摘要

When affected probands and their biological parents are genotyped at a candidate gene or a marker, the resulting case-parents-triad data enable powerful tests for linkage in the presence of association. When linkage disequilibrium has been detected in such a study, the investigator may wish to look further for possible parent-of-origin effects. If, for example, the transmission/disequilibrium test restricted to fathers is statistically significant, whereas that restricted to mothers is not, the investigator might interpret this as evidence for nonexpression of the maternally derived disease gene-that is, imprinting. This report reviews existing methods for detection of parent-of-origin effects, showing that each can be invalid under certain scenarios. Two new methods are proposed, based on application of likelihood-based inference after stratification on both the parental mating type and the inherited number of copies of the allele under study. If there are no maternal genetic effects expressed prenatally during gestation, the parental-asymmetry test is powerful and provides valid estimation of a parent-of-origin parameter. For diseases for which there could be maternal effects on risk, the parent-of-origin likelihood-ratio test provides a robust alternative. Simulations based on an admixed population demonstrate good operating characteristics for these procedures, under diverse scenarios.
机译:当在候选基因或标记处对受影响的先证者及其生物学亲本进行基因分型时,所产生的病例-父母-三元组数据可以在存在关联的情况下进行强大的链接测试。当在这项研究中检测到连锁不平衡时,研究者可能希望进一步寻找可能的起源母体效应。例如,如果仅限于父亲的传播/不平衡测试在统计上是有意义的,而仅限于母亲的传播/不平衡测试没有统计学意义,则研究人员可能会将其解释为母亲表达的疾病基因未表达的证据,即印记。该报告回顾了检测原产地效应的现有方法,表明每种方法在某些情况下可能是无效的。在对父母的交配类型和所研究的等位基因的遗传拷贝数进行分层之后,应用基于可能性的推理,提出了两种新方法。如果在妊娠期间未在产前表达母亲遗传效应,则父母不对称性测试功能强大,可以有效评估父母的原产地参数。对于可能对母亲造成风险影响的疾病,产地父母似然比检验提供了可靠的选择。在各种情况下,基于混合总体的模拟显示了这些程序的良好操作特性。

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