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Simple and efficient analysis of disease association with missing genotype data.

机译:简单有效地分析缺少基因型数据的疾病。

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Missing genotype data arise in association studies when the single-nucleotide polymorphisms (SNPs) on the genotyping platform are not assayed successfully, when the SNPs of interest are not on the platform, or when total sequence variation is determined only on a small fraction of individuals. We present a simple and flexible likelihood framework to study SNP-disease associations with such missing genotype data. Our likelihood makes full use of all available data in case-control studies and reference panels (e.g., the HapMap), and it properly accounts for the biased nature of the case-control sampling as well as the uncertainty in inferring unknown variants. The corresponding maximum-likelihood estimators for genetic effects and gene-environment interactions are unbiased and statistically efficient. We developed fast and stable numerical algorithms to calculate the maximum-likelihood estimators and their variances, and we implemented these algorithms in a freely available computer program. Simulation studies demonstrated that the new approach is more powerful than existing methods while providing accurate control of the type I error. An application to a case-control study on rheumatoid arthritis revealed several loci that deserve further investigations.
机译:当基因分型平台上的单核苷酸多态性(SNP)未能成功检测,目标SNP不在平台上或仅在一小部分个体中确定总序列变异时,关联研究中就会缺少基因型数据。我们提出了一个简单而灵活的可能性框架来研究具有此类缺失基因型数据的SNP疾病关联。我们的可能性充分利用了病例对照研究和参考面板(例如HapMap)中的所有可用数据,并且适当地考虑了病例对照抽样的偏倚性质以及推断未知变异的不确定性。遗传效应和基因-环境相互作用的相应最大似然估计是无偏的,并且在统计上是有效的。我们开发了快速而稳定的数值算法来计算最大似然估计值及其方差,并在免费的计算机程序中实现了这些算法。仿真研究表明,新方法比现有方法更强大,同时可以精确控制I型错误。在风湿性关节炎病例对照研究中的一项应用发现了几个位点,值得进一步研究。

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