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EAGLE: An algorithm that utilizes a small number of genomic features to predict tissue/cell type-specific enhancer-gene interactions

机译:EAGLE:一种利用少量基因组特征预测组织/细胞类型特异性增强子-基因相互作用的算法

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摘要

Long-range regulation by distal enhancers is crucial for many biological processes. The existing methods for enhancer-target gene prediction often require many genomic features. This makes them difficult to be applied to many cell types, in which the relevant datasets are not always available. Here, we design a tool EAGLE, an enhancer and gene learning ensemble method for identification of Enhancer-Gene (EG) interactions. Unlike existing tools, EAGLE used only six features derived from the genomic features of enhancers and gene expression datasets. Cross-validation revealed that EAGLE outperformed other existing methods. Enrichment analyses on special transcriptional factors, epigenetic modifications, and eQTLs demonstrated that EAGLE could distinguish the interacting pairs from non- interacting ones. Finally, EAGLE was applied to mouse and human genomes and identified 7,680,203 and 7,437,255 EG interactions involving 31,375 and 43,724 genes, 138,547 and 177,062 enhancers across 89 and 110 tissue/cell types in mouse and human, respectively. The obtained interactions are accessible through an interactive database . The EAGLE method is available at and the predicted datasets are available in .
机译:远端增强剂的远程调节对于许多生物学过程至关重要。用于增强子-靶基因预测的现有方法经常需要许多基因组特征。这使得它们难以应用于许多单元格类型,在这些类型中,相关数据集并不总是可用。在这里,我们设计了一种工具EAGLE,一种用于识别增强子与基因(EG)相互作用的增强子和基因学习集成方法。与现有工具不同,EAGLE仅使用了六个来自增强子和基因表达数据集的基因组特征的特征。交叉验证显示,EAGLE优于其他现有方法。对特殊转录因子,表观遗传修饰和eQTL的富集分析表明,EAGLE可以区分相互作用的对和非相互作用的对。最后,将EAGLE应用于小鼠和人类基因组,确定了涉及小鼠和人类89种和110种组织/细胞类型的涉及31,375和43,724个基因,138,547和177,062个增强子的7,680,203和7,437,255个EG相互作用。可以通过交互式数据库访问获得的交互。的EAGLE方法可用,而的预测数据集可用。

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