A Multi-Cohort and Multi-Omics Meta-Analysis Framework to Identify Network-Based Gene Signatures

被引:19
|
作者
Shafi, Adib [1 ]
Nguyen, Tin [2 ]
Peyvandipour, Azam [1 ]
Nguyen, Hung [2 ]
Draghici, Sorin [1 ,3 ]
机构
[1] Wayne State Univ, Dept Comp Sci, Detroit, MI 48202 USA
[2] Univ Nevada, Dept Comp Sci & Engn, Reno, NV 89557 USA
[3] Wayne State Univ, Dept Obstet & Gynecol, Detroit, MI 48202 USA
基金
美国国家卫生研究院; 美国国家科学基金会;
关键词
multi-cohort; multi-omics; meta-analysis; subnetwork identification; GBM; LGG; DNA METHYLATION; INTEGRATED ANALYSIS; TEMOZOLOMIDE RESISTANCE; EXPRESSION PROFILES; GENOMIC ANALYSIS; SYSTEMS BIOLOGY; DATABASE; PATHWAYS; SURVIVAL; CANCER;
D O I
10.3389/fgene.2019.00159
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Although massive amounts of condition-specific molecular profiles are being accumulated in public repositories every day, meaningful interpretation of these data remains a major challenge. In an effort to identify the biomarkers that describe the key biological phenomena for a given condition, several approaches have been developed over the past few years. However, the majority of these approaches either (i) do not consider the known intermolecular interactions, or (ii) do not integrate molecular data of multiple types (e.g., genomics, transcriptomics, proteomics, epigenomics, etc.), and thus potentially fail to capture the true biological changes responsible for complex diseases (e.g., cancer). In addition, these approaches often ignore the heterogeneity and study bias present in independent molecular cohorts. In this manuscript, we propose a novel multi-cohort and multi-omics meta-analysis framework that overcomes all three limitations mentioned above in order to identify robust molecular subnetworks that capture the key dynamic nature of a given biological condition. Our framework integrates multiple independent gene expression studies, unmatched DNA methylation studies, and protein-protein interactions to identify methylation-driven subnetworks. We demonstrate the proposed framework by constructing subnetworks related to two complex diseases: glioblastoma and low-grade gliomas. We validate the identified subnetworks by showing their ability to predict patients' clinical outcome on multiple independent validation cohorts.
引用
收藏
页数:16
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