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An integrated network platform for contextual prioritization of drugs and pathways

机译:一个综合的网络平台可根据上下文确定药物和途径的优先级

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摘要

Repurposing of drugs to novel disease indications has a promise of faster clinical translation. However, identifying best drugs for a given pathological context is not trivial. We developed an integrated random walk-based network framework that combines functional biomolecular relationships and known drug-target interactions as a platform for contextual prioritization of drugs, genes and pathways. We show that the use of gene-centric or drug-centric data, such as gene expression data or a phenotypic drug screen, respectively, within this network platform can effectively prioritize drugs and pathways, respectively, to the studied biological context. We demonstrate that various genomic data can be used as contextual cues to effectively prioritize drugs to the studied context, while similarly, phenotypic drug screen data can be used to effectively prioritize genes and pathways to the studied phenotypic context. As a proof-of-principle, we showcase the use of our platform to identify known and novel drug indications against different subsets of breast cancers through contextual prioritization based on genome-wide gene expression, shRNA and drug screen and clinical survival data. The integrated network and associated methods are incorporated into the NetWalker suite for functional genomics analysis ().
机译:将药物用于新的疾病适应症有望实现更快的临床翻译。但是,在给定的病理背景下确定最佳药物并非易事。我们开发了一个集成的,基于随机行走的网络框架,该框架结合了功能性生物分子关系和已知的药物-靶标相互作用,将其作为对药物,基因和途径进行上下文优先排序的平台。我们表明,在此网络平台内分别使用以基因为中心或以药物为中心的数据(例如基因表达数据或表型药物筛选)可以分别有效地区分所研究的生物学背景中的药物和途径。我们证明了各种基因组数据可以用作上下文线索,以有效地将药物优先于研究的上下文,而类似地,表型药物筛选数据可以用于有效地对基因和进入研究的表型上下文的途径进行优先排序。作为原理的证明,我们展示了使用我们的平台通过基于全基因组基因表达,shRNA和药物筛选以及临床生存数据的上下文优先级确定针对乳腺癌不同子集的已知和新药适应症。集成的网络和相关方法已合并到NetWalker套件中,以进行功能基因组分析。

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