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首页> 外文期刊>Thorax: The Journal of the British Thoracic Society >A genome-wide analysis of open chromatin in human tracheal epithelial cells reveals novel candidate regulatory elements for lung function
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A genome-wide analysis of open chromatin in human tracheal epithelial cells reveals novel candidate regulatory elements for lung function

机译:全基因组分析人类气管上皮细胞中的开放染色质揭示了肺功能的新型候选调控元件

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Background: Distal cell-type-specific regulatory elements may be located at very large distances from the genes that they control and are often hidden within intergenic regions or in introns of other genes. The development of methods that enable mapping of regions of open chromatin genome wide has greatly advanced the identification and characterisation of these elements. Methods: Here we use DNase I hypersensitivity mapping followed by deep sequencing (DNase-seq) to generate a map of open chromatin in primary human tracheal epithelial (HTE) cells and use bioinformatic approaches to characterise the distribution of these sites within the genome and with respect to gene promoters, intronic and intergenic regions. Results: Genes with HTE-selective open chromatin at their promoters were associated with multiple pathways of epithelial function and differentiation. The data predict novel cell-type-specific regulatory elements for genes involved in HTE cell function, such as structural proteins and ion channels, and the transcription factors that may interact with them to control gene expression. Moreover, the map of open chromatin can identify the location of potentially critical regulatory elements in genome-wide association studies (GWAS) in which the strongest association is with single nucleotide polymorphisms in non-coding regions of the genome. We demonstrate its relevance to a recent GWAS that identifies modifiers of cystic fibrosis lung disease severity. Conclusion: Since HTE cells have many functional similarities with bronchial epithelial cells and other differentiated cells in the respiratory epithelium, these data are of direct relevance to elucidating the molecular basis of normal lung function and lung disease.
机译:背景:远距离细胞类型特异性调控元件可能位于与它们控制的基因相距非常远的位置,并且通常隐藏在基因间区域内或其他基因的内含子中。能够绘制全开放染色质基因组区域的图谱的方法的发展极大地促进了这些元素的鉴定和表征。方法:在这里,我们使用DNase I超敏感性作图,然后进行深度测序(DNase-seq),以在原代人气管上皮(HTE)细胞中生成开放染色质图,并使用生物信息学方法来表征这些位点在基因组中的分布以及关于基因启动子,内含子和基因间区域。结果:启动子上具有HTE选择性开放染色质的基因与上皮功能和分化的多种途径相关。数据预测了涉及HTE细胞功能的基因的新型细胞类型特异性调控元件,例如结构蛋白和离子通道,以及可能与它们相互作用以控制基因表达的转录因子。此外,开放染色质图谱可以确定全基因组关联研究(GWAS)中潜在关键调控元件的位置,其中最强的关联与基因组非编码区中的单核苷酸多态性相关。我们证明了其与最近的GWAS的相关性,后者确定了囊性纤维化肺病严重程度的改变因素。结论:由于HTE细胞与呼吸道上皮中的支气管上皮细胞和其他分化细胞具有许多功能相似性,因此这些数据与阐明正常肺功能和肺部疾病的分子基础直接相关。

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