首页> 美国卫生研究院文献>Nucleic Acids Research >Conserved elements containing NF-E2 and tandem GATA binding sites are required for erythroid-specific chromatin structure reorganization within the human beta-globin locus control region.
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Conserved elements containing NF-E2 and tandem GATA binding sites are required for erythroid-specific chromatin structure reorganization within the human beta-globin locus control region.

机译:在人β-珠蛋白基因座控制区域内类胡萝卜素特异性染色质结构重组需要含有NF-E2和串联GATA结合位点的保守元件。

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摘要

Proper expression of the genes of the human beta-globin gene locus requires the associated locus control region (LCR). Structurally, the LCR is defined by the presence of four domains of erythroid-specific chromatin structure. These domains, which have been characterized as DNase I hypersensitive sites (HSs), comprise the active elements of the LCR. The major focus of this research is to define the cis -acting elements which are required for the formation of these domains of unique chromatin structure. Our previous investigations on the formation of LCR HS4 demonstrated that NF-E2 and tandem, inverted GATA binding sites are required for the formation of the native HS. Similarly arranged NF-E2 and tandem GATA sites are present within the core regions of the other human LCR HSs and are evolutionarily conserved. Using site-directed mutagenesis of human HSs 2 and 3 we have tested the hypothesis that these NF-E2 and GATA sites are common requirements for the formation of all LCR HSs. We find that mutation of these elements, and particularly the GATA elements, results in a decrease or complete loss of DNase I hypersensitivity. These data imply the presence of common structural elements within the core of each LCR HS which are required for erythroid-specific chromatin structure reorganization.
机译:人β-珠蛋白基因基因座基因的正确表达需要相关的基因座控制区(LCR)。在结构上,LCR是由存在类红细胞特异性染色质结构的四个结构域定义的。这些结构域已被表征为DNase I超敏位点(HSs),包含LCR的活性元件。这项研究的主要重点是定义形成独特染色质结构这些域所需的顺式作用元件。我们之前对LCR HS4形成的研究表明,天然HS的形成需要NF-E2和串联的反向GATA结合位点。排列相似的NF-E2和串联GATA位点存在于其他人LCR HS的核心区域内,并且在进化上是保守的。使用人类HS 2和3的定点诱变,我们测试了以下假设:这些NF-E2和GATA位点是形成所有LCR HS的共同要求。我们发现这些元素,特别是GATA元素的突变导致DNase I超敏性降低或完全丧失。这些数据表明,每个LCR HS核心中都存在共同的结构元素,这是类红细胞特异性染色质结构重组所必需的。

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