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Network clustering along diabetes progression in three tissues of Goto-Kakizaki rats

机译:五岛崎崎大鼠三种组织中沿糖尿病进展的网络聚类

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We investigated the macroscopic changes in the regulatory coordination of diabetes progression during three periods in three tissues, adipose, liver and muscle, of Goto-Kakizaki (GK) rats. For this purpose, we performed network clustering by the Newman algorithm for the regulatory networks inferred by a modified path consistency algorithm, and investigated the biological functions of each cluster by an enrichment analysis of the constituent genes. We then compared the network clusters characterized by biological functions with the diabetes progression of GK rats in each of the three tissues. The network structure, the number of clusters, and the number of clusters characterized by biological functions during the three periods showed similar patterns in the three tissues. In contrast, further scrutiny of the biological functions at coordinated clusters revealed characteristic differences between the three tissues along the diabetes progression. In particular, the hypothetical roles of each tissue emerged: adipose and liver function at the cellular and molecular levels at the early stage, respectively, and all three tissues are responsible for diabetes progression, under the control of various transcriptional regulators.
机译:我们调查了五岛崎崎(GK)大鼠三个组织(脂肪,肝和肌肉)在三个时期内糖尿病进展的调控协调作用的宏观变化。为此,我们使用Newman算法对修改后的路径一致性算法推断出的调控网络进行了网络聚类,并通过对组成基因的富集分析研究了每个聚类的生物学功能。然后,我们将以生物学功能为特征的网络簇与GK大鼠在三种组织中的糖尿病进展进行了比较。在三个时期内,网络结构,簇数以及以生物学功能为特征的簇数在三种组织中显示出相似的模式。相反,对协调簇的生物学功能的进一步检查揭示了沿糖尿病进展的三个组织之间的特征差异。特别是出现了每种组织的假设性作用:分别在早期处于细胞和分子水平的脂肪和肝功能,并且在各种转录调节剂的控制下,所有三个组织都负责糖尿病的发展。

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