首页> 美国卫生研究院文献>Nucleic Acids Research >SynLeGG: analysis and visualization of multiomics data for discovery of cancer ‘Achilles Heels’ and gene function relationships
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SynLeGG: analysis and visualization of multiomics data for discovery of cancer ‘Achilles Heels’ and gene function relationships

机译:Synlegg:发现癌症阿基尔脚跟和基因功能关系的分析与可视化

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摘要

Achilles’ heel relationships arise when the status of one gene exposes a cell's vulnerability to perturbation of a second gene, such as chemical inhibition, providing therapeutic opportunities for precision oncology. SynLeGG (www.overton-lab.uk/synlegg) identifies and visualizes mutually exclusive loss signatures in ‘omics data to enable discovery of genetic dependency relationships (GDRs) across 783 cancer cell lines and 30 tissues. While there is significant focus on genetic approaches, transcriptome data has advantages for investigation of GDRs and remains relatively underexplored. SynLeGG depends upon the MultiSEp algorithm for unsupervised assignment of cell lines into gene expression clusters, which provide the basis for analysis of CRISPR scores and mutational status in order to propose candidate GDRs. Benchmarking against SynLethDB demonstrates favourable performance for MultiSEp against competing approaches, finding significantly higher area under the Receiver Operator Characteristic curve and between 2.8-fold to 8.5-fold greater coverage. In addition to pan-cancer analysis, SynLeGG offers investigation of tissue-specific GDRs and recovers established relationships, including synthetic lethality for SMARCA2 with SMARCA4. Proteomics, Gene Ontology, protein-protein interactions and paralogue information are provided to assist interpretation and candidate drug target prioritization. SynLeGG predictions are significantly enriched in dependencies validated by a recently published CRISPR screen.
机译:当一个基因的地位暴露细胞脆性对第二基因的扰动等化学抑制的扰动,提供治疗机会的精密肿瘤的治疗机会时,会出现阿基拉斯的脚跟关系。 synlegg(www.overton-lab.uk/synlegg)识别和可视化“OMIC数据”中的互斥损失签名,以便在783个癌细胞系和30个组织中发现遗传依赖关系(GDR)。虽然有重点关注遗传方法,但转录组数据具有调查GDR的优势,并且仍然相对望远镜。 Synlegg取决于用于对基因表达群体的无监督分配的多学分配给基因表达集群,为分析CRISPR评分和突变状况提供了基础,以提出候选GDR。反对Synlethdb的基准展示了对竞争方法的多项企业的良好性能,在接收器操作员特征曲线下发现明显高的区域,并且覆盖范围内的2.8倍至8.5倍。除了泛癌分析外,SynleGG还提供了对组织特异性GDR的调查,并恢复了建立的关系,包括Smarca2的Smarca2的合成致死性。提供蛋白质组学,基因本体,蛋白质 - 蛋白质相互作用和亲蛋白酶信息,以协助解释和候选药物目标优先级排序。 Synlegg预测在最近发表的CRISPR屏幕验证的依赖关系中被显着丰富。

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