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FOXA and master transcription factors recruit Mediator and Cohesin to the core transcriptional regulatory circuitry of cancer cells

机译:FOXA和Master转录因子招募介质和幼耳肝素转录调控性癌细胞

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摘要

Controlling the transcriptional program is essential to maintain the identity and the biological functions of a cell. The Mediator and Cohesin complexes have been established as central cofactors controlling the transcriptional program in normal cells. However, the distribution, recruitment and importance of these complexes in cancer cells have not been fully investigated. Here we show that FOXA and master transcription factors are part of the core transcriptional regulatory circuitry of cancer cells and are essential to recruit M ediator and Cohesin. Indeed, Mediator and Cohesin occupied the enhancer and promoter regions of actively transcribed genes and maintained the proliferation and colony forming potential. Through integration of publically available ChIP-Seq datasets, we predicted the core transcriptional regulatory circuitry of each cancer cell. Unexpectedly, for all cells investigated, the pioneer transcription factors FOXA1 and/or FOXA2 were identified in addition to cell-specific master transcription factors. Loss of both types of transcription factors phenocopied the loss of Mediator and Cohesin. Lastly, the master and pioneer transcription factors were essential to recruit Mediator and Cohesin to regulatory regions of actively transcribed genes. Our study proposes that maintenance of the cancer cell state is dependent on recruitment of Mediator and Cohesin through FOXA and master transcription factors.
机译:控制转录程序对于维持细胞的身份和生物学功能至关重要。已经建立了介体和休肽复合物作为控制正常细胞中转录程序的中央辅因子。然而,癌细胞中这些复合物的分布,招募和重要性尚未得到充分调查。在这里,我们表明FOXA和母程转录因子是癌细胞核心转录调节电路的一部分,对招募M Sepians和Cohesin至关重要。实际上,介质和凝聚蛋白占据了激发转录基因的增强剂和启动子区域,并保持了增殖和菌落形成潜力。通过集成公开的芯片-SEQ数据集,我们预测了每个癌细胞的核心转录调节电路。出乎意料地,对于所有研究的细胞,除细胞特异性母转录因子外,还鉴定了先驱转录因子FOXA1和/或FOXA2。两种类型的转录因子丧失衰弱的介质和幼蛋白的丧失。最后,掌握和先锋转录因子对于招募调解员和幼耳至积极转录基因的监管区域至关重要。我们的研究提出,癌细胞状态的维持取决于通过FOXA和母源型转录因子募集介质和幼耳。

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