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Coverage tradeoffs and power estimation in the design of whole-genome sequencing experiments for detecting association.

机译:用于检测关联的全基因组测序实验设计中的权衡取舍和功率估计。

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Whole-genome sequencing (WGS) allows direct interrogation of previously undetected uncommon or rare variants, which potentially contribute to the missing heritability of human disease. However, cost of sequencing large numbers of samples limits its application in case-control association studies. Here, we describe theoretical and empirical design considerations for such sequencing studies, aimed at maximizing the power of detecting association under the constraint of study-wide cost. RESULTS: We consider two cost regimes. First, assuming cost is proportional to the total amount of base pairs to be sequenced across all samples, which is a practical model for whole-genome sequencing, we explored the tradeoff in terms of study power between increasing the number of subjects and increasing depth coverage. We demonstrate that the optimal power of detecting association is achieved at medium depth coverage under a wide range of realistic conditions for case-only sequencing designs. Second, if cost is fixed per sample, which is approximately the case in exome sequencing, we show that in a simple case+control sequencing study, the optimal design should include cases totaling 1/e of all subjects. AVAILABILITY: A web tool implementing the methods is available at http://www.cs.columbia.edu/~itsik/OPERA/.
机译:全基因组测序(WGS)可以直接询问以前未发现的罕见或罕见变体,这可能会导致人类疾病的遗传力缺失。但是,测序大量样品的成本限制了其在病例对照关联研究中的应用。在这里,我们描述了此类测序研究的理论和经验设计考虑,旨在最大程度地在整个研究成本的约束下检测关联。结果:我们考虑了两种成本制度。首先,假设成本与所有样本中要测序的碱基对的总量成正比,这是全基因组测序的实用模型,那么我们在增加研究对象数量和增加深度覆盖范围之间的研究能力方面进行了权衡。我们证明,仅在案例设计中,在广泛的实际条件下,在中等深度覆盖范围内实现了检测关联的最佳能力。其次,如果每个样品的成本是固定的(大约是外显子组测序的情况),我们表明在简单的病例+对照测序研究中,最佳设计应包括所有受试者总数的1 / e。可用性:可通过http://www.cs.columbia.edu/~itsik/OPERA/获得实现该方法的Web工具。

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