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首页> 外文期刊>Pattern Recognition: The Journal of the Pattern Recognition Society >Scoring disease-microRNA associations by integrating disease hierarchy into graph convolutional networks
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Scoring disease-microRNA associations by integrating disease hierarchy into graph convolutional networks

机译:通过将疾病层次分析纳入图形卷积网络,评分疾病 - MicroRNA关联

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摘要

In this study, we present an updated predictor DimiG 2.0, which uses a semi-supervised multi-label graph convolutional network (GCN) to infer disease-associated microRNAs (miRNAs) on an interaction network between protein coding genes (PCGs) and miRNAs using disease-PCG associations. DimiG 2.0 benefits from integrating the hierarchy of diseases into the GCN. DimiG 2.0 has the following updates: 1) It incorporates the hierarchy of diseases to regularize the GCN, encouraging diseases in the hierarchy to share similar miRNAs. 2) It integrates the PCGs with interacting partners but without associated diseases into model training, these unlabeled PCGs increase the size of the constructed interaction network. 3) It is able to predict associated miRNAs for 1017 diseases (updated from 248). 4) It updates expression data across tissues from the latest GTEx v7, and the expression values are quantified in Transcripts Per Million (TPM). Our results show that DimiG 2.0 outperforms state-of-the-art semi-supervised and supervised methods on the constructed benchmarked sets. (C) 2020 Elsevier Ltd. All rights reserved.
机译:在本研究中,我们提出了更新的预测器DIMIG 2.0,其使用半监督的多标记图卷积网络(GCN)来推断出蛋白质编码基因(PCG)和MiRNA之间的相互作用网络上的疾病相关的微大罗氏(miRNA)疾病 - PCG协会。 DIMIG 2.0将疾病层次集成到GCN中的优势。 DIMIG 2.0具有以下更新:1)它包含了疾病的层次结构,以规范GCN,鼓励层次结构中的疾病共享类似的miRNA。 2)将PCG与互动伴侣集成,但没有相关的疾病进入模型训练,这些未标记的PCG增加了构造的交互网络的大小。 3)它能够预测1017个疾病的相关miRNA(从248更新)。 4)它从最新的GTEX V7跨组织更新表达数据,并且表达值在每百万(TPM)中量化。我们的结果表明,DIMIG 2.0在构造的基准集上占据了最先进的半监督和监督方法。 (c)2020 elestvier有限公司保留所有权利。

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