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采用系统生物学方法研究矽肺相关的 microRNA 和转录因子调控网络。

Investigation of MicroRNA and transcription factor mediated regulatory network for silicosis using systems biology approach.

机构信息

Chhattisgarh Swami Vivekanand Technical University, Bhilai, C.G, 491107, India.

Raipur Institute of Technology, Raipur, C.G, 492001, India.

出版信息

Sci Rep. 2021 Jan 14;11(1):1265. doi: 10.1038/s41598-020-77636-4.

Abstract

Silicosis is a major health issue among workers exposed to crystalline silica. Genetic susceptibility has been implicated in silicosis. The present research demonstrates key regulatory targets and propagated network of gene/miRNA/transcription factor (TF) with interactions responsible for silicosis by integrating publicly available microarray data using a systems biology approach. Array quality is assessed with the Quality Metrics package of Bioconductor, limma package, and the network is constructed using Cytoscape. We observed and enlist 235 differentially expressed genes (DEGs) having up-regulation expression (85 nos) and down-regulation expression (150 nos.) in silicosis; and 24 TFs for the regulation of these DEGs entangled with thousands of miRNAs. Functional enrichment analysis of the DEGs enlighten that, the maximum number of DEGs are responsible for biological process viz, Rab proteins signal transduction (11 nos.) and Cellular Senescence (20 nos.), whereas IL-17 signaling pathway (16 nos.) and Signalling by Nuclear Receptors (14 nos.) etc. are Biological Pathway involving more DEGs. From the identified 1100 high target microRNA (miRNA)s involved in silicosis, 1055 miRNAs are found to relate with down-regulated genes and 847 miRNAs with up-regulated genes. The CDK19 gene (Up-regulated) is associated with 617 miRNAs whereas down-regulated gene ARID5B is regulated by as high as 747 high target miRNAs. In Prediction of Small-molecule signatures, maximum scoring small-molecule combinations for the DEGs have shown that CGP-60774 (with 20 combinations), alvocidib (with 15 combinations) and with AZD-7762 (24 combinations) with few other drugs having the high probability of success.

摘要

矽肺是接触结晶二氧化硅的工人面临的主要健康问题。遗传易感性与矽肺有关。本研究通过系统生物学方法,整合公开的微阵列数据,证明了关键的调控靶点和传播的基因/miRNA/转录因子(TF)网络,这些靶点和网络与矽肺的相互作用有关。使用 Bioconductor 的 Quality Metrics 包、limma 包评估阵列质量,并使用 Cytoscape 构建网络。我们观察到并列出了 235 个差异表达基因(DEG),其中 85 个基因上调表达,150 个基因下调表达;24 个 TF 参与这些 DEG 的调控,与数千个 miRNA 交织在一起。DEG 的功能富集分析表明,最大数量的 DEG 负责生物过程,如 Rab 蛋白信号转导(11 个)和细胞衰老(20 个),而 IL-17 信号通路(16 个)和核受体信号(14 个)等涉及更多 DEG 的生物途径。在鉴定的与矽肺相关的 1100 个高靶标 miRNA 中,发现 1055 个 miRNA 与下调基因相关,847 个 miRNA 与上调基因相关。CDK19 基因(上调)与 617 个 miRNA 相关,而下调基因 ARID5B 则由高达 747 个高靶标 miRNA 调控。在小分子特征预测中,DEG 的最大得分小分子组合表明,CGP-60774(20 种组合)、alvocidib(15 种组合)和 AZD-7762(24 种组合)以及其他一些具有高成功概率的药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f640/7809153/bbf763b8d218/41598_2020_77636_Fig1_HTML.jpg

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