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Model-based clustering for identifying disease-associated SNPs in case-control genome-wide association studies

机译:基于模型的聚类,用于鉴定疾病相关的SNP,在病例控制基因组 - 范围内协会研究中

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Genome-wide association studies (GWASs) aim to detect genetic risk factors for complex human diseases by identifying disease-associated single-nucleotide polymorphisms (SNPs). The traditional SNP-wise approach along with multiple testing adjustment is over-conservative and lack of power in many GWASs. In this article, we proposed a model-based clustering method that transforms the challenging high-dimension-small-sample-size problem to low-dimension-large-sample-size problem and borrows information across SNPs by grouping SNPs into three clusters. We pre-specify the patterns of clusters by minor allele frequencies of SNPs between cases and controls, and enforce the patterns with prior distributions. In the simulation studies our proposed novel model outperforms traditional SNP-wise approach by showing better controls of false discovery rate (FDR) and higher sensitivity. We re-analyzed two real studies to identifying SNPs associated with severe bortezomib-induced peripheral neuropathy (BiPN) in patients with multiple myeloma (MM). The original analysis in the literature failed to identify SNPs after FDR adjustment. Our proposed method not only detected the reported SNPs after FDR adjustment but also discovered a novel BiPN-associated SNP rs4351714 that has been reported to be related to MM in another study.
机译:基因组 - 范围协会研究(GWASS)通过鉴定疾病相关的单核苷酸多态性(SNP)来检测复杂人类疾病的遗传危险因素。传统的SNP-WISE方法以及多种测试调整是过于保守的,并且在许多GWAS中缺乏电力。在本文中,我们提出了一种基于模型的聚类方法,通过将SNP分组到三个集群中,将挑战的高维 - 小样本问题转换为低维 - 大样本大小问题,并借用SNP的借款信息。我们通过案例和控制之间的SNP的次要等位基因频率预先指定群集模式,并强制使用现有分布。在仿真研究中,我们所提出的小说模型通过显示出更好的虚假发现率(FDR)和更高的灵敏度来优于传统的SNP-Wise方法。我们重新分析了两项实际研究,以鉴定患有多个骨髓瘤(MM)患者的严重硼珠诱导的周围神经病变(BIPN)相关的SNP。文献中的原始分析未能在FDR调整后识别SNP。我们所提出的方法不仅在FDR调整后检测到报告的SNP,而且发现了一种新的BIPN相关的SNP RS4351714,其据报道,在另一个研究中据报道与MM相关。

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