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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >The mitotic checkpoint gene, SIL is regulated by E2F1.
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The mitotic checkpoint gene, SIL is regulated by E2F1.

机译:有丝分裂检查点基因SIL受E2F1调控。

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摘要

The SIL gene expression is increased in multiple cancers and correlates with the expression of mitotic spindle checkpoint genes and with increased metastatic potential. SIL regulates mitotic entry, organization of the mitotic spindle and cell survival. The E2F transcription factors regulate cell cycle progression by controlling the expression of genes mediating the G1/S transition. More recently, E2F has been shown to regulate mitotic spindle checkpoint genes as well. As SIL expression correlates with mitotic checkpoint genes, we hypothesized that SIL is regulated by E2F. We mined raw data of published experiments and performed new experiments by modification of E2F expression in cell lines, reporter assays and chromatin immunoprecipitation. Ectopic expression or endogenous activation of E2F induced the expression of SIL, while knockdown of E2F by shRNA, downregulated SIL expression. E2F activated SIL promoter by reporter assay and bound to SIL promoter in vivo. Taken together these data demonstrate that SIL is regulated by E2F. As SIL is essential for mitotic entry, E2F may regulate G2/M transition through the induction of SIL. Furthermore, as silencing of SIL cause apoptosis in cancer cells, these finding may have therapeutic relevance in tumors with constitutive activation of E2F.
机译:SIL基因表达在多种癌症中增加,并且与有丝分裂纺锤体检查点基因的表达和转移潜力增加相关。 SIL调节有丝分裂进入,有丝分裂纺锤体的组织和细胞存活。 E2F转录因子通过控制介导G1 / S过渡的基因的表达来调节细胞周期进程。最近,E2F也显示出调节有丝分裂纺锤体检查点基因。由于SIL表达与有丝分裂检查点基因相关,我们假设SIL受E2F调控。我们挖掘了已发表实验的原始数据,并通过修饰细胞系中的E2F表达,报道分子测定和染色质免疫沉淀来进行新实验。 E2F的异位表达或内源性激活诱导了SIL的表达,而shRNA抑制E2F的表达则下调了SIL的表达。 E2F通过报告基因检测激活了SIL启动子,并在体内与SIL启动子结合。这些数据加在一起表明SIL受E2F调节。由于SIL对于有丝分裂进入至关重要,因此E2F可能通过诱导SIL来调节G2 / M过渡。此外,由于SIL沉默导致癌细胞凋亡,因此这些发现在具有E2F组成型激活作用的肿瘤中可能具有治疗意义。

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