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Genome-wide Identification and Characterization of Enhancers Across 10 Human Tissues

机译:全基因组鉴定和表征跨10个人类组织的增强子

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Background: Enhancers can act as cis-regulatory elements (CREs) to control development and cellular function by regulating gene expression in a tissue-specific and ubiquitous manner. However, the regulatory network and characteristic of different types of enhancers (e.g., transcribedon-transcribed enhancers, tissue-specific/ubiquitous enhancers) across multiple tissues are still unclear. Results: Here, a total of 53,924 active enhancers and 10,307 enhancer-associated RNAs (eRNAs) in 10 tissues (adrenal, brain, breast, heart, liver, lung, ovary, placenta, skeletal muscle and kidney) were identified through the integration of histone modifications (H3K4me1, H3K27ac and H3K4me3) and DNase I hypersensitive sites (DHSs) data. Moreover, 40,101 tissue-specific enhancers (TS-Enh), 1,241 ubiquitously expressed enhancers (UE-Enh) as well as transcribed enhancers (T-Enh), including 7,727 unidirectionally transcribed enhancers (1D-Enh) and 1,215 bidirectionally transcribed enhancers (2D-Enh) were defined in 10 tissues. The results show that enhancers exhibited high GC content, genomic variants and transcription factor binding sites (TFBS) enrichment in all tissues. These characteristics were significantly different between TS-Enh and UE-Enh, T-Enh and NT-Enh, 2D-Enh and 1D-Enh. Furt hermore, the results showed that enhancers obviously upregulate the expression of adjacent target genes which were remarkably correlated with the functions of corresponding tissues. Finally, a free user-friendly tissue-specific enhancer database, TiED , has been built to store, visualize, and confer these results. Conclusion: Genome-wide analysis of the regulatory network and characteristic of various types of enhancers showed that enhancers associated with TFs, eRNAs and target genes appeared in tissue specificity and function across different tissues.
机译:背景:增强子可以通过以组织特异性和普遍存在的方式调节基因表达来充当顺式调控元件(CRE),以控制发育和细胞功能。但是,尚不清楚跨多个组织的不同类型的增强子(例如,转录的/非转录的增强子,组织特异性/遍在增强子)的调节网络和特性。结果:通过整合,共鉴定出10个组织(肾上腺,脑,乳腺,心脏,肝,肺,卵巢,胎盘,骨骼肌和肾脏)中的53,924个活性增强子和10,307个与增强子相关的RNA(eRNA)。组蛋白修饰(H3K4me1,H3K27ac和H3K4me3)和DNase I超敏位点(DHS)数据。此外,有40,101个组织特异性增强子(TS-Enh),1,241个普遍表达的增强子(UE-Enh)和转录增强子(T-Enh),包括7,727个单向转录增强子(1D-Enh)和1,215个双向转录增强子(2D -Enh)被定义在10个组织中。结果表明,增强子在所有组织中均表现出较高的GC含量,基因组变异和转录因子结合位点(TFBS)富集。这些特征在TS-Enh和UE-Enh,T-Enh和NT-Enh,2D-Enh和1D-Enh之间有显着差异。结果表明,增强子明显上调了邻近靶基因的表达,这些靶基因与相应组织的功能显着相关。最后,已经建立了一个免费的用户友好型组织特异性增强剂数据库TiED,用于存储,可视化和提供这些结果。结论:全基因组对调节网络和各种类型增强子特性的分析表明,与TF,eRNA和靶基因相关的增强子在不同组织中的组织特异性和功能均出现。

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