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首页> 外文期刊>Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation >Simultaneous Modeling of Disease Status and Clinical Phenotypes To Increase Power in Genome-Wide Association Studies
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Simultaneous Modeling of Disease Status and Clinical Phenotypes To Increase Power in Genome-Wide Association Studies

机译:同时建立疾病状况和临床表型的模型,以提高全基因组关联研究的能力

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摘要

Genome-wide association studies have identified thousands of variants implicated in dozens of complex diseases. Most studies collect individuals with and without disease and search for variants with different frequencies between the groups. For many of these studies, additional disease traits are also collected. Jointly modeling clinical phenotype and disease status is a promising way to increase power to detect true associations between genetics and disease. In particular, this approach increases the potential for discovering genetic variants that are associated with both a clinical phenotype and a disease. Standard multivariate techniques fail to effectively solve this problem, because their case–control status is discrete and not continuous. Standard approaches to estimate model parameters are biased due to the ascertainment in case–control studies. We present a novel method that resolves both of these issues for simultaneous association testing of genetic variants that have both case status and a clinical covariate. We demonstrate the utility of our method using both simulated data and the Northern Finland Birth Cohort data.
机译:全基因组关联研究已经确定了与数十种复杂疾病有关的数千种变异。大多数研究都收集有或没有疾病的个体,并寻找群体之间频率不同的变异。对于许多这些研究,还收集了其他疾病特征。对临床表型和疾病状态进行联合建模是增加检测基因与疾病之间真正关联的能力的有前途的方法。特别是,这种方法增加了发现与临床表型和疾病相关的遗传变异的可能性。标准的多变量技术无法有效解决此问题,因为它们的案例控制状态是离散的而不是连续的。由于病例对照研究的确定性,估计模型参数的标准方法存在偏差。我们提出了一种新颖的方法,可以同时解决具有病例状态和临床协变量的遗传变异的关联测试,解决了这两个问题。我们使用模拟数据和北芬兰出生队列数据演示了我们方法的实用性。

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