首页> 外文期刊>Nucleic Acids Research >Distinct promoter elements mediate the co-operative effect of Brn-3a and p53 on the p21 promoter and their antagonism on the Bax promoter
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Distinct promoter elements mediate the co-operative effect of Brn-3a and p53 on the p21 promoter and their antagonism on the Bax promoter

机译:不同的启动子元件介导Brn-3a和p53对p21启动子的协同作用以及它们对Bax启动子的拮抗作用

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摘要

Although the promoters of both the Bax and p21 genes are activated by p53, they differ in the effect on this activation of the POU family transcription factor Brn-3a. Thus, Brn-3a inhibits activation of the Bax promoter by P53 but enhances the ability of P53 to activate the p21 promoter. We demonstrate that repression of p53-mediated activation of the Bax promoter involves a complex upstream sequence in which two Brn-3a response elements flank the p53 response element. In contrast, a minimal P21 promoter is activated by Brn-3a and such activation cannot be abolished without abolishing basal promoter activity. Moreover, synergistic activation by Brn-3a and p53 continues to be observed when the p53-binding sites in the p21 promoter are substituted by the Bax p53 site or by the region of the Bax promoter essential for Brn-3a-mediated repression, indicating that the p21 core promoter plays a central role in this response. The significance of these effects is discussed in terms of the different responses of the Bax and p21 promoters and the overlapping but distinct roles of Brn-3a and p53 in neuronal growth arrest and apoptosis.
机译:尽管Bax和p21基因的启动子均被p53激活,但它们在POU家族转录因子Brn-3a的这种激活作用方面有所不同。因此,Brn-3a抑制了P53对Bax启动子的激活,但增强了P53激活p21启动子的能力。我们证明抑制p53介导的Bax启动子的激活涉及一个复杂的上游序列,其中两个Brn-3a反应元件位于p53反应元件的侧面。相反,最小的P21启动子被Brn-3a激活,并且在不消除基础启动子活性的情况下不能消除这种激活。此外,当p21启动子中的p53结合位点被Bax p53位点或Brn-3a介导的阻遏必不可少的Bax启动子区域取代时,继续观察到Brn-3a和p53的协同激活。 p21核心启动子在这一反应中起着核心作用。根据Bax和p21启动子的不同反应以及Brn-3a和p53在神经元生长停滞和凋亡中的重叠但不同的作用,讨论了这些作用的重要性。

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