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首页> 外文期刊>Journal of cellular biochemistry. >NF-Y-mediated trans-activation of the human thymidine kinase promoter is closely linked to activation of cyclin-dependent kinase.
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NF-Y-mediated trans-activation of the human thymidine kinase promoter is closely linked to activation of cyclin-dependent kinase.

机译:人胸苷激酶启动子的NF-Y介导的反式激活与细胞周期蛋白依赖性激酶的激活紧密相关。

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摘要

Transcriptional activation is important for the elevated expression of human thymidine kinase (hTK) in tumor cells. Here, we used TK(-133/+33)-luciferase reporter gene construct and bandshift assay to study the cis-elements involved in transcriptional activation of the hTK promoter. We found that two CCAAT boxes at -71/-67 and -40/-36 and Sp1 binding site located at -118/-113 were critical for maximal expression of the hTK promoter activity. As Sp1-mediated activation of the hTK promoter was not detectable for the promoter construct with double mutations at two CCAAT boxes, we proposed that NF-Y binding to the hTK promoter sequence is a requisite step for the functional interaction with Sp1. Here, we further showed that the hTK promoter activity was reduced in HeLa cells transfected with p16 or p21, both of which are inhibitors of cyclin-dependent kinases (CDKs). Inhibition of the hTK promoter activity by p16 could be abrogated by overexpression of cyclin A, indicating that the cyclin A activating event is more directly involved in transcriptional activation of the hTK promoter. We thus proposed that NF-Y-mediated activation of the hTK promoter is closely linked to the activation of CDK2/cyclin A pathway.
机译:转录激活对于肿瘤细胞中人胸苷激酶(hTK)的高表达很重要。在这里,我们使用TK(-133 / + 33)-萤光素酶报告基因构建和带移分析来研究参与hTK启动子转录激活的顺式元件。我们发现位于-71 / -67和-40 / -36的两个CCAAT框以及位于-118 / -113的Sp1结合位点对于hTK启动子活性的最大表达至关重要。由于在两个CCAAT盒中具有双突变的启动子构建体无法检测到Sp1介导的hTK启动子激活,因此我们提出与hTK启动子序列结合的NF-Y是与Sp1功能相互作用的必要步骤。在这里,我们进一步表明,在转染了p16或p21的HeLa细胞中,hTK启动子活性均降低,p16或p21都是细胞周期蛋白依赖性激酶(CDKs)的抑制剂。 p16对hTK启动子活性的抑制可以通过细胞周期蛋白A的过表达来消除,这表明细胞周期蛋白A的激活事件更直接地参与了hTK启动子的转录激活。因此,我们提出了hTK启动子的NF-Y介导的激活与CDK2 / cyclin A途径的激活紧密相关。

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