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BETASEQ: a powerful novel method to control type-I error inflation in partially sequenced data for rare variant association testing

机译:BETASEQ:一种功能强大的新颖方法,用于控制部分序列数据中的I型错误填充,以进行稀有变异关联测试

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摘要

Despite its great capability to detect rare variant associations, next-generation sequencing is still prohibitively expensive when applied to large samples. In case-control studies, it is thus appealing to sequence only a subset of cases to discover variants and genotype the identified variants in controls and the remaining cases under the reasonable assumption that causal variants are usually enriched among cases. However, this approach leads to inflated type-I error if analyzed naively for rare variant association. Several methods have been proposed in recent literature to control type-I error at the cost of either excluding some sequenced cases or correcting the genotypes of discovered rare variants. All of these approaches thus suffer from certain extent of information loss and thus are underpowered. We propose a novel method (BETASEQ), which corrects inflation of type-I error by supplementing pseudo-variants while keeps the original sequence and genotype data intact. Extensive simulations and real data analysis demonstrate that, in most practical situations, BETASEQ leads to higher testing powers than existing approaches with guaranteed (controlled or conservative) type-I error.
机译:尽管其强大的检测稀有变异关联的能力,但将下一代测序应用于大型样品时仍然昂贵。因此,在病例对照研究中,仅对病例的子集进行测序以发现变体并在对照和其余病例中进行基因型分型是很有吸引力的,而合理的假设是因果变体通常在病例之间得到了丰富。但是,如果天真地分析罕见变体关联,此方法会导致I型错误膨胀。在最近的文献中已经提出了几种方法来控制I型错误,其代价是排除一些测序病例或校正发现的稀有变体的基因型。因此,所有这些方法都会遭受一定程度的信息丢失,因此功能不足。我们提出了一种新颖的方法(BETASEQ),该方法通过补充伪变量来纠正I型错误的膨胀,同时保持原始序列和基因型数据的完整性。大量的仿真和真实数据分析表明,在大多数实际情况下,BETASEQ都比具有保证的(受控或保守)I型错误的现有方法产生更高的测试能力。

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