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Correlation signature of the macroscopic states of the gene regulatory network in cancer

机译:癌症基因调控网络宏观状态的相关特征

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Although cancer types differ substantially, many cancers share common gene expression signatures. Consistent with this observation, we find convergent and representative distributions and correlation vectors that are distinct in cancer and noncancer ensembles. These differences originate in many genes, but comparatively few genes account for the major differences. We identify genes with different combinatorial regulation in cancer and non-cancer as indicated by significant differences in their correlation vectors. Among the identified genes are many established onco-genes and apoptotic genes (such as members of the Bcl-2, the MAPK, and the Ras families) and new candidate oncogenes. Our findings expand and complement the tumorigenic role of up and down regulation of these genes by emphasizing cancer-specific changes in their couplings and correlation patterns at genome-wide level that are independent from their mean levels of expression in cancer cells. Given the central role of these genes in defining the cancerous state it may be worth investigating them and the differences in their combinatorial regulation for developing wide-spectrum anticancer drugs.
机译:尽管癌症类型差异很大,但许多癌症具有共同的基因表达特征。与该观察结果一致,我们发现在癌症和非癌性集合体中不同的会聚和代表性分布以及相关向量。这些差异起源于许多基因,但相对较少的基因占主要差异。我们确定了在癌症和非癌症中具有不同组合调节作用的基因,如其相关载体的显着差异所表明。在已鉴定的基因中,有许多已建立的癌基因和凋亡基因(例如Bcl-2,MAPK和Ras家族的成员)和新的候选癌基因。我们的发现通过强调在全基因组水平上其偶联和相关模式的癌症特异性变化而独立于它们在癌细胞中的平均表达水平,从而扩展和补充了这些基因上调和下调的致癌作用。鉴于这些基因在定义癌性状态中的核心作用,可能值得研究它们,以及它们在开发广谱抗癌药物方面的组合调节方面的差异。

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