首页> 外文期刊>Gene expression >SpSoxB1 serves an essential architectural function in the promoter SpAN, a tolloid/BMP1-related gene.
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SpSoxB1 serves an essential architectural function in the promoter SpAN, a tolloid/BMP1-related gene.

机译:SpSoxB1在启动子SpAN(类固醇/ BMP1相关基因)中起着至关重要的建筑功能。

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摘要

Transcription of SpAN, which encodes a secreted protease related to tolloid and BMP 1, is differentially regulated along the animal-vegetal axis of the sea urchin embryo by a maternally initiated mechanism. Regulatory sites that bind SpSoxB1 and CBF (CCAAT binding factor) are essential for strong transcriptional activity because mutations of these elements reduce promoter activity in vivo 20- and 10-fold, respectively. Here we show that multimerized SpSoxB1 elements cannot activate transcription from the SpAN basal promoter in vivo. However, like other factors containing HMG-class DNA binding domains, SpSoxB1 does induce strong bending of DNA. The CBF binding site lies abnormally far from the transcriptional start site at -200 bp. We show that the SpSoxB1 site is not required if the CCAAT element is moved 100 bp closer to the transcriptional start site, replacing the SpSoxB1 site. This supports a model in which the bending of SpAN promoter DNA by SpSoxB1 facilitates interactions between factors binding to upstream and downstream regulatory elements.
机译:SpAN的转录编码是由母本启动的机制沿海胆胚胎的动物-植物轴进行差异调节的,该转录编码与tolloid和BMP 1有关的一种分泌性蛋白酶。结合SpSoxB1和CBF(CCAAT结合因子)的调控位点对于强大的转录活性是必不可少的,因为这些元素的突变分别降低了20倍和10倍的体内启动子活性。在这里,我们显示多聚的SpSoxB1元素不能激活体内SpAN基础启动子的转录。但是,像其他包含HMG类DNA结合域的因子一样,SpSoxB1确实会诱导DNA强烈弯曲。 CBF结合位点异常远离转录起始位点-200 bp。我们显示,如果将CCAAT元素移至转录起始位点100 bp左右,以取代SpSoxB1位点,则不需要SpSoxB1位点。这支持了一个模型,其中通过SpSoxB1弯曲SpAN启动子DNA有助于与上游和下游调控元件结合的因子之间的相互作用。

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