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ZFP226 is a novel artificial transcription factor for selective activation of tumor suppressor KIBRA

机译:ZFP226是一种新的人工转录因子,用于肿瘤抑制kibra的选择性激活

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KIBRA has been suggested as a key regulator of the hippo pathway, regulating organ size, cell contact inhibition as well as tissue regeneration and tumorigenesis. Recently, alterations of KIBRA expression caused by promotor methylation have been reported for several types of cancer. Our current study aimed to design an artificial transcription factor capable of re-activating expression of the tumor suppressor KIBRA and the hippo pathway. We engineered a new gene named ‘ZFP226′ encoding for a ~23?kDa fusion protein. ZFP226 belongs to the Cys2-His2 zinc finger type and recognizes a nine base-pair DNA sequence 5′-GGC-GGC-GGC-3′ in the KIBRA core promoter P1a. ZFP226 showed nuclear localization in human immortalized kidney epithelial cells and activated the KIBRA core promoter (p??0.001) resulting in significantly increased KIBRA mRNA and protein levels (p??0.001). Furthermore, ZFP226 led to activation of hippo signaling marked by elevated YAP and LATS phosphorylation. In Annexin V flow cytometry assays ZFP226 overexpression showed strong pro-apoptotic capacity on MCF-7 breast cancer cells (p??0.01 early-, p??0.001 late-apoptotic cells). We conclude that the artificial transcription factor ZFP226 can be used for target KIBRA and hippo pathway activation. This novel molecule may represent a molecular tool for the development of future applications in cancer treatment.
机译:Kibra已被建议作为河马途径的关键调节器,调节器官尺寸,细胞接触抑制以及组织再生和肿瘤鉴定。最近,据报道,若干类型的癌症据报道了由促进剂甲基化引起的kibra表达的改变。我们目前的研究旨在设计一种能够重新激活肿瘤抑制kibra和河马途径的人工转录因子。我们设计了一个名为“ZFP226”编码的新基因,用于〜23?KDA融合蛋白。 ZFP226属于Cys2-His2锌指型,并在Kibra核心启动子P1A中识别九个碱基对DNA序列5'-GGC-GGC-GGC-3'。 ZFP226在人类永生化的肾上皮细胞中显示了核定位,并激活了Kibra核心启动子(P?<0.001),导致kibra mRNA和蛋白质水平显着增加(p?<0.001)。此外,ZFP226导致激活标有升高的YAP和LAT磷酸化的河马信号传导。在膜蛋白v流式细胞术中测定ZFP226过表达在MCF-7乳腺癌细胞上显示出强烈的促凋亡能力(P?<β01,P≤0.01晚期凋亡细胞)。我们得出结论,人工转录因子ZFP226可用于靶kibra和河马途径激活。该新型分子可以代表癌症治疗中未来应用的分子工具。

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