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首页> 外文期刊>International Journal of Genomics >Nonredundant, Highly Connected MicroRNAs Control Functionality in Breast Cancer Networks
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Nonredundant, Highly Connected MicroRNAs Control Functionality in Breast Cancer Networks

机译:非冗余,高度连接的MicroRNAS控制乳腺癌网络中的功能

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摘要

Alterations to transcriptional regulation are an important factor in breast cancer. Noncoding RNA, such as microRNA (miR), have very influential roles in the transcriptional regulation of genes. Transcriptional regulation can be successfully modeled and analyzed using complex network theory. Particularly, interactions between two distinct classes of biological elements, such as miR and genes, can be approached through the bipartite network formalism. Based on bipartite network properties, it is possible to identify highly influential miRs in the network, such as those that have a large number of connections indicating regulation of a large set of genes. Some miRs in a network are nonredundant, which indicates that they are solely responsible of theregulation of a particular set of genes, which in turn may be associated to a particular biological process. We hypothesize that highly influential, nonredundant miRs, which we call Commodore miRs (Cdre-miRs), have an important role on the control of biological functions through transcriptional networks. In this work, we analyze the regulation of gene expression by miRs in healthy and cancerous breast tissue using bipartite miR-gene networks inferred from the Cancer Genome Atlas (TCGA) expression data.We observe differences in the degree, clustering coefficient and redundancy distributions for miRs and genes in the network, indicating differences in the way that these elements interact with each other. Furthermore, we identify a small set of five Cdre-miRs in the breast cancer network: miR-190b, miR-let7i, miR-292-b, miR-511, and miR-141. The neighborhood of genes controlled by each of these miRs is involved in particular biological functions such as dynein structure-associated processes, immune response, angiogenesis, cytokine activity, and cell motility. We propose that these Cdre-miRs are important control elements of biological functions deregulated in breast cancer.
机译:转录调节的改变是乳腺癌的重要因素。非沉积RNA,例如microRNA(miR),在基因的转录调节中具有非常有影响力的作用。可以使用复杂的网络理论成功建模和分析转录调节。特别地,可以通过双链网络形式主义来接近两个不同类别的生物元素(例如miR和基因)之间的相互作用。基于二分网络属性,可以在网络中识别高度影响力的MIR,例如那些具有大量连接的那些指示大量基因的调节。网络中的一些MIR是非还原的,这表明它们仅负责在那种特定的基因集合中负责,这又可以与特定的生物过程相关联。我们假设我们呼叫Commodore MiR(CDRE-MIRS)的高度影响力,非冗余的MIR,对通过转录网络控制生物功能的重要作用。在这项工作中,我们使用从癌症基因组Atlas(TCGA)表达数据(TCGA)表达数据推断的二分miR-Gene网络来分析MIR在健康和癌乳腺组织中的基因表达调节。我们观察程度,聚类系数和冗余分布的差异网络中的MIR和基因,表明这些元件彼此相互作用的方式的差异。此外,我们在乳腺癌网络中识别一小组五种CDRE-MIR:MIR-190B,MIR-Let7i,MiR-292-B,MiR-511和MiR-141。由这些miR中的每一个控制的基因邻域涉及特定的生物学功能,例如Dynein结构相关的方法,免疫应答,血管生成,细胞因子活性和细胞运动。我们建议这些CDRE-MIRS是乳腺癌中消化生物功能的重要控制要素。

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