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首页> 外文期刊>Nucleic Acids Research >Cell-type-specific long-range looping interactions identify distant regulatory elements of the CFTR gene
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Cell-type-specific long-range looping interactions identify distant regulatory elements of the CFTR gene

机译:细胞类型特异性的远程循环相互作用确定了CFTR基因的远距离调控元件

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摘要

Identification of regulatory elements and their target genes is complicated by the fact that regulatory elements can act over large genomic distances. Identification of long-range acting elements is particularly important in the case of disease genes as mutations in these elements can result in human disease. It is becoming increasingly clear that long-range control of gene expression is facilitated by chromatin looping interactions. These interactions can be detected by chromosome conformation capture (3C). Here, we employed 3C as a discovery tool for identification of long-range regulatory elements that control the cystic fibrosis transmembrane conductance regulator gene, CFTR. We identified four elements in a 460-kb region around the locus that loop specifically to the CFTR promoter exclusively in CFTR expressing cells. The elements are located 20 and 80 kb upstream; and 109 and 203 kb downstream of the CFTR promoter. These elements contain DNase I hypersensitive sites and histone modification patterns characteristic of enhancers. The elements also interact with each other and the latter two activate the CFTR promoter synergistically in reporter assays. Our results reveal novel long-range acting elements that control expression of CFTR and suggest that 3C-based approaches can be used for discovery of novel regulatory elements.
机译:调控元件可以在较大的基因组距离上起作用,这一事实使调控​​元件及其靶基因的鉴定变得复杂。在疾病基因的情况下,长距离作用元件的鉴定尤为重要,因为这些元件的突变会导致人类疾病。越来越清楚的是,染色质环相互作用促进了基因表达的远程控制。这些相互作用可以通过染色体构象捕获(3C)检测到。在这里,我们采用3C作为发现工具,用于识别控制囊性纤维化跨膜电导调节基因CFTR的远程调节元件。我们在基因座周围的460-kb区域中发现了四个元素,这些元素专门在CFTR表达细胞中专门循环到CFTR启动子。这些元素位于上游20 kb和80 kb; CFTR启动子下游的109和203 kb。这些元素包含DNase I超敏位点和增强子特有的组蛋白修饰模式。这些元素也彼此相互作用,后两个在报告基因分析中协同激活CFTR启动子。我们的结果揭示了控制CFTR表达的新型远程作用元件,并表明基于3C的方法可用于发现新型调控元件。

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