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Information fusion of CNVs and SNPs on gene-gene interactions for molecular subtypes of lymphoma

机译:CNVS和SNP对淋巴瘤分子亚型基因基因相互作用的信息融合

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Although genome-wide association studies report many disease-associated loci involved in pathogenesis, current identified variants only explain a little part of the heritability underlying complex diseases. To explore the other missing part of heritability, data-mining methods are proposed and developed to detect disease-associated interactions between variants. Recently, some studies have revealed the linkage disequilibrium between chromosome structure variations and disease-associated loci. We are motivated to employ a fusion approach that incorporates the information of copy number variations (CNVs) for identifying interactions between single nucleotide polymorphisms (SNPs). The CNV profiles are first used for clustering analysis of disease subtypes, and then the SNP-SNP interactions are examined by the multifactor dimensionality reduction (MDR) method. We applied the fusion approach in analyzing 214 lymphoma cases. The results showed that the interactions identified by the fusion approach were more significantly associated with lymphoma than those identified only by MDR without incorporating CNV information. Therefore, we conclude that information fusion of CNVs and SNPs provides a proper strategy for detecting gene-gene interactions in disease association studies.
机译:虽然基因组关联研究报告了许多涉及发病机制的疾病相关基因座,但目前鉴定的变体仅解释了遗传性的一部分遗传性疾病。为了探讨其他缺少的可遗传性部分,提出了数据采矿方法,并开发出来检测变种之间的疾病相关的相互作用。最近,一些研究揭示了染色体结构变化和病情相关基因座之间的连锁不平衡。我们的动力是使用一种融合方法,该融合方法包括拷贝数变异(CNV)的信息,用于鉴定单个核苷酸多态性(SNP)之间的相互作用。 CNV型材首先用于疾病亚型的聚类分析,然后通过多重吸收的维度减少(MDR)方法检查SNP-SNP相互作用。我们在分析214淋巴瘤病例中应用了融合方法。结果表明,融合方法鉴定的相互作用与淋巴瘤的相互作用比仅由MDR鉴定而不纳入CNV信息,更明显。因此,我们得出结论,CNVS和SNP的信息融合提供了检测疾病协会研究中基因基因相互作用的适当策略。

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