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An Efficient Survival Multifactor Dimensionality Reduction Method for Detecting Gene-Gene Interactions of Lung Cancer Onset Age

机译:一种有效的存活多因素维度降低方法,用于检测肺癌发作年龄的基因 - 基因相互作用

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This study addresses the computational burden often encountered when analyzing gene-gene interactions in relation to time-to-event data, such as patient survival time or time-to-cancer relapse. The goal is to develop a method called Efficient Survival MDR (ES-MDR) that handles survival data by using Martingale Residuals to replace the survival outcome and uses the computationally efficient Quantitative MDR (QMDR) to identify significant interaction models. To demonstrate the strength of ES-MDR, two simulations are designed to evaluate the testing score's null distribution and to study the success rate of the method. Additionally, ES-MDR is applied on real data with 14,935cases and 12,787 controls of European descent from the OncoArray Consortium that examined the relationship between genetic variants and lung cancer susceptibility. Martingale Residuals, which replace onset age of lung cancer, is treated as the survival outcome, cases are considered event at diagnosis age, and controls are considered censored at interview age. Froman exhaustive search over all one-way and two-way interaction models, we identified a strong association with chr17_41196821_INDEL_T_Dfrom BRCA1 gene and exm1568790_Afrom CBR1 gene as the top SNP-SNP interaction with lung cancer susceptibility at age-of-onset.
机译:本研究解决了在分析与患者存活时间或癌症时间或癌症复发时的基因 - 基因相互作用时经常遇到的计算负担。目标是开发一种称为有效的生存MDR(ES-MDR)的方法,该方法通过使用Martingale残差来处理生存数据以取代生存结果,并使用计算有效的定量MDR(QMDR)来识别重要的交互模型。为了展示ES-MDR的强度,设计了两种模拟来评估测试得分的空分布,并研究方法的成功率。此外,ES-MDR适用于具有14,935个Case的实际数据和12,787个欧洲血管联盟的控制,欧洲血管联盟进行了检查,检测了遗传变异和肺癌易感性之间的关系。鞅残留物替代肺癌的发作年龄,被视为生存结果,案件被认为是诊断年龄的事件,并考虑在访谈年龄进行审查。从所有单向和双向交互模型的穷举搜索,我们确定了与CHR17_41196821_INCEL_T_DFROM BRCA1基因和EXM1568790_AFROM CBR1基因的强烈关联,因为顶部SNP-SNP与肺癌易感性在发作时期的相互作用。

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