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首页> 外文期刊>Nucleic Acids Research >Systems biology of Ewing sarcoma: a network model of EWS-FLI1 effect on proliferation and apoptosis
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Systems biology of Ewing sarcoma: a network model of EWS-FLI1 effect on proliferation and apoptosis

机译:尤文氏肉瘤的系统生物学:EWS-FLI1对增殖和凋亡影响的网络模型

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摘要

Ewing sarcoma is the second most frequent pediatric bone tumor. In most of the patients, a chromosomal translocation leads to the expression of the EWS-FLI1 chimeric transcription factor that is the major oncogene in this pathology. Relative genetic simplicity of Ewing sarcoma makes it particularly attractive for studying cancer in a systemic manner. Silencing EWS-FLI1 induces cell cycle alteration and ultimately leads to apoptosis, but the exact molecular mechanisms underlying this phenotype are unclear. In this study, a network linking EWS-FLI1 to cell cycle and apoptosis phenotypes was constructed through an original method of network reconstruction. Transcriptome time-series after EWS-FLI1 silencing were used to identify core modulated genes by an original scoring method based on fitting expression profile dynamics curves. Literature data mining was then used to connect these modulated genes into a network. The validity of a subpart of this network was assessed by siRNA/RT-QPCR experiments on four additional Ewing cell lines and confirmed most of the links. Based on the network and the transcriptome data, CUL1 was identified as a new potential target of EWS-FLI1. Altogether, using an original methodology of data integration, we provide the first version of EWS-FLI1 network model of cell cycle and apoptosis regulation.
机译:尤因肉瘤是第二常见的小儿骨肿瘤。在大多数患者中,染色体易位导致EWS-FLI1嵌合转录因子的表达,而EWS-FLI1嵌合转录因子是该病理学中的主要致癌基因。尤因肉瘤的相对遗传简单性使其对于以系统方式研究癌症特别有吸引力。沉默EWS-FLI1诱导细胞周期改变并最终导致细胞凋亡,但尚不清楚该表型的确切分子机制。在这项研究中,通过原始的网络重建方法构建了一个将EWS-FLI1与细胞周期和凋亡表型联系起来的网络。使用EWS-FLI1沉默后的转录组时间序列,通过基于拟合表达谱动力学曲线的原始评分方法,鉴定核心调控基因。然后使用文献数据挖掘将这些调制基因连接到网络中。通过在另外四个尤因细胞系上的siRNA / RT-QPCR实验评估了该网络一个子部分的有效性,并证实了大多数联系。根据网络和转录组数据,CUL1被确定为EWS-FLI1的新潜在靶标。总之,使用原始的数据集成方法,我们提供了细胞周期和细胞凋亡调控的EWS-FLI1网络模型的第一版。

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