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首页> 外文期刊>Oncology letters >MED28 increases the colony-forming ability of breast cancer cells by stabilizing the ZNF224 protein upon DNA damage
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MED28 increases the colony-forming ability of breast cancer cells by stabilizing the ZNF224 protein upon DNA damage

机译:通过在DNA损伤时通过稳定ZNF224蛋白来增加乳腺癌细胞的菌落形成能力

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摘要

The regulation of gene expression by transcription factors serves a critical function in cell proliferation. Zinc-finger protein 224 (ZNF224), a Kruppel-associated-box-containing zinc finger protein, is known to serve a crucial function in integrating the transcriptional co-factors that activate transcriptional regulation pathways in the cell. A previous study demonstrated that ZNF224 enhances cell proliferation by downregulating the expression of p21 and p53. The present study identified mediator complex subunit 28 (MED28) as a potential binding partner for ZNF224; this was confirmed by co-immunoprecipitation and a surface plasmon resonance assay. Additionally, the KRAB domain at the N-terminal of ZNF224 interacts with the MED domain of MED28. Bimolecular fluorescence complementation analysis revealed that ZNF224 associates with MED28 in the nucleus. In addition, ZNF224 was rapidly degraded upon treatment with the DNA-damaging agent camptothecin (CPT). Transient overexpression of MED28 inhibited the CPT-mediated degradation of ZNF224, resulting in increased colony formation by MCF-7 cells. The molecular mechanisms that underlie the biological outcomes of MED28 expression have not yet been fully elucidated. The present study provides molecular evidence for the function of ZNF224 and MED28 in the DNA-damage response.
机译:转录因子的基因表达的调节在细胞增殖中具有关键功能。已知锌 - 手指蛋白224(ZnF224),含kruppel相关盒的锌指蛋白质,用于积分激活细胞中的转录调节途径的转录共源的关键功能。先前的研究证明,通过下调P21和P53的表达来增强细胞增殖。本研究确定了介质复合亚基28(Med28)作为ZnF224的潜在结合配偶体;这通过共免疫沉淀和表面等离子体共振测定来证实。另外,ZnF224的N末端的Krab结构域与Med28的Med域相互作用。双分子荧光互补分析显示ZnF224与细胞核中的Med28相关联。此外,ZnF224在用DNA损伤剂CAMPTOTECIN(CPT)处理时迅速降解。 Med28的瞬时过表达抑制CPT介导的ZnF224的降解,导致MCF-7细胞增加菌落形成。提出了Med28表达的生物学结果的分子机制尚未完全阐明。本研究为DNA损伤反应中的ZnF224和Med28的功能提供了分子证据。

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