首页> 美国卫生研究院文献>Molecular and Cellular Biology >Different cis-Acting Elements Are Involved in the Regulation of TRP1 and TRP2 Promoter Activities by Cyclic AMP: Pivotal Role of M Boxes (GTCATGTGCT) and of Microphthalmia
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Different cis-Acting Elements Are Involved in the Regulation of TRP1 and TRP2 Promoter Activities by Cyclic AMP: Pivotal Role of M Boxes (GTCATGTGCT) and of Microphthalmia

机译:不同的顺式作用元件参与循环AMP对TRP1和TRP2启动子活性的调节:M盒(GTCATGTGCT)和小眼科的关键作用

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摘要

In melanocytes and in melanoma cells, cyclic AMP (cAMP)-elevating agents stimulate melanogenesis and increase the transcription of tyrosinase, the rate-limiting enzyme in melanin synthesis. However, two other enzymes, tyrosinase-related protein 1 (TRP1) and TRP2, are required for a normal melanization process leading to eumelanin synthesis. In B16 melanoma cells, we demonstrated that stimulation of melanogenesis by cAMP-elevating agents results in an increase in tyrosinase, TRP1, and TRP2 expression. cAMP, through a cAMP-dependent protein kinase pathway, stimulates TRP1 and TRP2 promoter activities in both B16 mouse melanoma cells and normal human melanocytes. Regulation of the TRP1 and TRP2 promoters by cAMP involves a M box and an E box. Further, a classical cAMP response element-like motif participates in the cAMP responsiveness of the TRP2 promoter, demonstrating that the TRP2 gene is subjected to different regulatory processes, which could account for its different expression patterns during embryonic development or under specific physiological and pathological conditions. We also found that microphthalmia, a basic helix-loop-helix transcription factor, strongly stimulates the transcriptional activities of the TRP1 and TRP2 promoters, mainly through binding to the M boxes. Additionally, we demonstrated that cAMP increases microphthalmia expression and thereby its binding to TRP1 and TRP2 M boxes. These convergent and compelling results disclose at least a part of the molecular mechanism involved in the regulation of melanogenic gene expression by cAMP and emphasize the pivotal role of microphthalmia in this process.
机译:在黑色素细胞和黑色素瘤细胞中,环状AMP(cAMP)增强剂刺激黑色素生成并增加酪氨酸酶的转录,酪氨酸酶是黑色素合成中的限速酶。但是,其他两种酶,酪氨酸酶相关蛋白1(TRP1)和TRP2,是导致黑色素合成的正常黑化过程所必需的。在B16黑色素瘤细胞中,我们证明了cAMP升高剂对黑色素生成的刺激导致酪氨酸酶,TRP1和TRP2表达的增加。 cAMP通过cAMP依赖性蛋白激酶途径刺激B16小鼠黑素瘤细胞和正常人黑素细胞中的TRP1和TRP2启动子活性。 cAMP对TRP1和TRP2启动子的调控涉及M框和E框。此外,经典的cAMP反应元件样基序参与了TRP2启动子的cAMP反应,表明TRP2基因受到不同的调节过程,这可能解释了它在胚胎发育过程中或在特定生理和病理条件下的不同表达方式。 。我们还发现,小眼症是一种基本的螺旋-环-螺旋转录因子,主要通过与M盒结合,强烈刺激了TRP1和TRP2启动子的转录活性。此外,我们证明了cAMP可增加小眼症的表达,从而增加其与TRP1和TRP2 M盒的结合。这些趋同和令人信服的结果揭示了至少一部分分子机制涉及cAMP调节黑色素基因表达,并强调了小眼症在此过程中的关键作用。

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