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首页> 外文期刊>Cell cycle >Kinetic profiling of the c-Myc transcriptome and bioinformatic analysis of repressed gene promoters.
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Kinetic profiling of the c-Myc transcriptome and bioinformatic analysis of repressed gene promoters.

机译:c-Myc转录组的动力学分析和抑制的基因启动子的生物信息学分析。

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摘要

Mammalian c-Myc is a member of a small family of three related proto-oncogenic transcription factors. c-Myc has an unusually broad array of regulatory functions, which include roles in cell cycle and apoptosis, a variety of metabolic functions, cell differentiation, senescence, and stem cell maintenance. c-Myc modulates the expression of a very large number of genes, but the magnitude of the majority of the regulatory effects is only 2-fold or less. c-Myc can both activate and repress the promoters of its target genes. Identification of genes directly regulated by c-Myc has been an enduring question in the field. We report here microarray expression profiling of a high resolution time course of c-Myc induction, using fibroblast cells in which c-Myc activity can be modulated from null to physiological. The c-Myc transcriptome dataset presented is the largest reported to date with 4,186 differentially regulated genes (1,826 upregulated, 2,360 downregulated, 1% FDR). The gene expression patterns fit well with the known biological functions of c-Myc. We describe several novel findings and present tools for further data mining. Although the mechanisms of transcriptional activation by c-Myc are well understood, how c-Myc represses an even greater number of genes remains incompletely described. One mechanism involves the binding of c-Myc to other, positively acting transcription factors, and interfering with their activities. We identified rapid-response genes likely to be direct c-Myc targets, and analyzed the promoters of the repressed genes to identify transcription factors that could be targets of c-Myc repression.
机译:哺乳动物c-Myc是三个相关的原癌基因转录因子的小家族的成员。 c-Myc具有异常广泛的调节功能,包括在细胞周期和凋亡,各种代谢功能,细胞分化,衰老和干细胞维持中的作用。 c-Myc调节大量基因的表达,但大多数调节作用的幅度仅为2倍或更小。 c-Myc可以激活和抑制其靶基因的启动子。鉴定由c-Myc直接调控的基因一直是该领域中一个长期存在的问题。我们在这里报告了使用成纤维细胞将c-Myc活性从零调节为生理的成纤维细胞对c-Myc诱导的高分辨率时间进程的微阵列表达谱。呈现的c-Myc转录组数据集是迄今为止报告的最大数据,包含4,186个差异调节基因(1,826个上调,2,360个下调,1%FDR)。基因表达模式与c-Myc的已知生物学功能非常吻合。我们描述了一些新颖的发现,并介绍了用于进一步数据挖掘的工具。尽管众所周知c-Myc激活转录的机制,但c-Myc如何抑制更多基因的方法仍未完全描述。一种机制涉及c-Myc与其他正性转录因子的结合,并干扰其活性。我们鉴定了可能是直接c-Myc靶标的快速反应基因,并分析了被抑制基因的启动子,以鉴定可能是c-Myc抑制靶标的转录因子。

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