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c-Myc靶基因网络。

The c-Myc target gene network.

作者信息

Dang Chi V, O'Donnell Kathryn A, Zeller Karen I, Nguyen Tam, Osthus Rebecca C, Li Feng

机构信息

Division of Hematology, Department of Medicine, Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.

出版信息

Semin Cancer Biol. 2006 Aug;16(4):253-64. doi: 10.1016/j.semcancer.2006.07.014. Epub 2006 Jul 25.

Abstract

For more than a decade, numerous studies have suggested that the c-Myc oncogenic protein is likely to broadly influence the composition of the transcriptome. However, the evidence required to support this notion was made available only recently, much to the anticipation of an eagerly awaiting field. In the past 5 years, many high-throughput screens based on microarray gene expression profiling, serial analysis of gene expression (SAGE), chromatin immunoprecipitation (ChIP) followed by genomic array analysis, and Myc-methylase chimeric proteins have generated a wealth of information regarding Myc responsive and target genes. From these studies, the c-Myc target gene network is estimated to comprise about 15% of all genes from flies to humans. Both genomic and functional analyses of c-Myc targets suggest that while c-Myc behaves as a global regulator of transcription, groups of genes involved in cell cycle regulation, metabolism, ribosome biogenesis, protein synthesis, and mitochondrial function are over-represented in the c-Myc target gene network. c-Myc also consistently represses genes involved in cell growth arrest and cell adhesion. The overexpression of c-Myc predisposes cells to apoptosis under nutrient or growth factor deprivation conditions, although the critical sets of genes involved remain elusive. Despite tremendous advances, the downstream target genes that distinguish between physiologic and tumorigenic functions of c-Myc remain to be delineated.

摘要

十多年来,众多研究表明,致癌蛋白c-Myc可能会广泛影响转录组的组成。然而,支持这一观点所需的证据直到最近才得以获得,这让翘首以盼的该领域研究人员倍感期待。在过去5年里,许多基于微阵列基因表达谱分析、基因表达序列分析(SAGE)、染色质免疫沉淀(ChIP)后进行基因组阵列分析以及Myc-甲基化酶嵌合蛋白的高通量筛选,已经产生了大量关于Myc反应性基因和靶基因的信息。从这些研究中估计,c-Myc靶基因网络包含从果蝇到人类所有基因的约15%。对c-Myc靶标的基因组和功能分析均表明,虽然c-Myc作为一种全局转录调节因子发挥作用,但参与细胞周期调控、代谢、核糖体生物合成、蛋白质合成和线粒体功能的基因群在c-Myc靶基因网络中占比过高。c-Myc也始终抑制参与细胞生长停滞和细胞黏附的基因。在营养或生长因子缺乏的条件下,c-Myc的过表达会使细胞易于发生凋亡,尽管其中涉及的关键基因集仍不清楚。尽管取得了巨大进展,但区分c-Myc生理功能和致瘤功能的下游靶基因仍有待确定。

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