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Topology of Mammalian Transcription Networks

机译:哺乳动物转录网络的拓扑

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We present a first attempt to evaluate the generic topological principles underlying the mammalian transcriptional regulatory networks. Transcription networks, TN, studied here are represented as graphs where vertices are genes coding for transcription factors and edges are causal links between the genes, each edge combining both-gene expression and irans-regulation events. Two transcription networks were retrieved from the TRANSPATH?database: The first one, TN.RN, is a 'complete' transcription network referred to as a reference network. The second one, TN.p53, displays a particular transcriptional sub-network centered at p53 gene. We found these networks to be fundamentally non-random and inhomogeneous. Their topology follows a power-law degree distribution and is best described by the scale-free model. Shortest-path-length distribution and the average clustering coefficient indicate a small-world feature of these networks. The networks show the dependence of the clustering coefficient on the degree of a vertex, thereby indicating the presence of hierarchical modularity. Clear positive correlation between the values of betweenness and the degree of vertices has been observed in both networks. The top list of genes displaying high degree and high betweennes, such as p53, c-fos, c-jun and c-myc, is enriched with genes that are known as having tumor-suppressor or proto-oncogene properties, which supports the biological significance of the identified key topological elements.
机译:我们展示了第一次尝试评估哺乳动物转录监管网络底层的通用拓扑原则。这里研究的转录网络TN表示为曲线图,其中顶点是编码转录因子的基因,并且边缘是基因之间的因果关系,每个边缘组合既有基因表达和伊朗调节事件。从Transpath检索两个转录网络?数据库:第一个,TN.rn是作为参考网络称为参考网络的“完整”转录网络。第二个,TN.P53显示以P53基因为中心的特定转录子网。我们发现这些网络基本上是非随机的和不均匀的。他们的拓扑遵循幂律程度分布,最好是由无尺度模型描述的。最短路径长度分布和平均聚类系数表示这些网络的小世界特征。网络示出了聚类系数对顶点的程度的依赖性,从而指示了分层模块化的存在。在两个网络中观察到,在两个网络中观察到间度和顶点之间的值之间的阳性相关性。显示出高度和高度的基因的顶部列表,例如p53,c-fos,c-jun和c-myc,富含了称为具有肿瘤抑制剂或原癌基因特性的基因,其支持生物学所识别的关键拓扑元素的意义。

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