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Overexpression of Sp1 transcription factor induces apoptosis

机译:Sp1转录因子的过表达诱导细胞凋亡

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摘要

Transcription factor Sp1 has recently been shown to be overexpressed in a number of human cancers and its overexpression contributes to malignant transformation. Sp1 regulates the expression of a number of genes participating in multiple aspects of tumorigenesis such as angiogenesis, cell growth and apoptosis resistance. To better understand the role of increased Sp1 levels on apoptosis regulation we have used retroviruses to overexpress this protein in haematopoietic Baf-3 cells and in 3T3 fibroblasts. We have also used inducible expression systems to control ectopic Sp1 levels in different cell types. Surprisingly, Sp1 overexpression on its own induces apoptosis in all the cellular models tested. The apoptotic pathways induced by Sp1 overexpression are cell type specific. Finally, using a truncated form of Sp1, we show that Sp1-induced apoptosis requires its DNA-binding domain. Our results highlight that Sp1 levels in untransformed cells must be tightly regulated as Sp1 overexpression leads to the induction of apoptosis. Our results also suggest that cancer cells overexpressing Sp1 can avoid Sp1-induced apoptosis.
机译:最近发现转录因子Sp1在许多人类癌症中均过表达,其过表达有助于恶性转化。 Sp1调节参与肿瘤发生的多个方面的许多基因的表达,例如血管生成,细胞生长和凋亡抗性。为了更好地了解Sp1水平升高对凋亡调控的作用,我们使用了逆转录病毒在造血Baf-3细胞和3T3成纤维细胞中过表达该蛋白。我们还使用了诱导型表达系统来控制不同细胞类型中异位Sp1的水平。出人意料的是,Sp1自身表达过高会在所有测试的细胞模型中诱导凋亡。 Sp1过表达诱导的凋亡途径是细胞类型特异性的。最后,使用Sp1的截短形式,我们显示Sp1诱导的细胞凋亡需要其DNA结合域。我们的结果表明,未转化细胞中Sp1的水平必须受到严格调节,因为Sp1的过表达会导致细胞凋亡。我们的结果还表明,过量表达Sp1的癌细胞可以避免Sp1诱导的细胞凋亡。

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