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首页> 外文期刊>Molecular and Cellular Biology >Analysis of the ERK-stimulated ETS transcription factor ER81.
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Analysis of the ERK-stimulated ETS transcription factor ER81.

机译:ERK刺激的ETS转录因子ER81的分析。

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A plethora of extracellular signals leads to the stimulation of Ras, which triggers intracellular protein kinase cascades, resulting in activation of transcription factors and thus in enhanced gene activity. In this report, it is demonstrated that the ETS transcription factor ER81, which appears to be localized within the cell nucleus by virtue of its DNA binding domain, is transcriptionally activated by oncogenic Ras. Since this activation was dependent on the presence of Raf-1 and ERK-1, ER81 is a target of the Ras/Raf/MEK/ERK signaling cascade. Consistently, activated ERK-1 is capable to phosphorylate ER81. However, the carboxy-terminal region of ER81, which contains no potential ERK phosphorylation sites, is also transcriptionally activated by ERK-1, suggesting that an ERK-stimulated protein kinase phosphorylates and thus stimulates ER81 activity. Two acidic stretches of amino acids, which are conserved in the related PEA3 and ERM proteins, are localized within the amino-and carboxy-terminal transactivation domains of ER81. In addition, an inhibitory domain may dampen the activation function of these two domains. In conclusion, ER81 is a target of Ras-dependent signaling cascades and may thus contribute to the nuclear response upon stimulation of cells and also to cellular transformation due to oncogenic Ras.
机译:大量的细胞外信号导致Ras的刺激,从而触发细胞内蛋白激酶级联反应,从而激活转录因子,从而增强基因活性。在该报告中,证明了由于其DNA结合域而似乎位于细胞核内的ETS转录因子ER81被致癌Ras转录激活。由于这种激活取决于Raf-1和ERK-1的存在,因此ER81是Ras / Raf / MEK / ERK信号级联反应的靶标。一致地,活化的ERK-1能够磷酸化ER81。但是,不包含潜在的ERK磷酸化位点的ER81的羧基末端区域也被ERK-1转录激活,这表明ERK刺激的蛋白激酶会磷酸化,从而刺激ER81的活性。在相关的PEA3和ERM蛋白中保守的两个酸性氨基酸段位于ER81的氨基和羧基末端反式激活域内。此外,抑制域可能会减弱这两个域的激活功能。总而言之,ER81是Ras依赖性信号传导级联的靶标,因此可能在刺激细胞后促进核反应,并由于致癌性Ras促进细胞转化。

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