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首页> 外文期刊>BMC Bioinformatics >Mammalian transcriptional hotspots are enriched for tissue specific enhancers near cell type specific highly expressed genes and are predicted to act as transcriptional activator hubs
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Mammalian transcriptional hotspots are enriched for tissue specific enhancers near cell type specific highly expressed genes and are predicted to act as transcriptional activator hubs

机译:哺乳动物转录热点在细胞类型特异性高表达基因附近富含组织特异性增强子,并有望充当转录激活中心

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Background Transcriptional hotspots are defined as genomic regions bound by multiple factors. They have been identified recently as cell type specific enhancers regulating developmentally essential genes in many species such as worm, fly and humans. The in-depth analysis of hotspots across multiple cell types in same species still remains to be explored and can bring new biological insights. Results We therefore collected 108 transcription-related factor (TF) ChIP sequencing data sets in ten murine cell types and classified the peaks in each cell type in three groups according to binding occupancy as singletons (low-occupancy), combinatorials (mid-occupancy) and hotspots (high-occupancy). The peaks in the three groups clustered largely according to the occupancy, suggesting priming of genomic loci for mid occupancy irrespective of cell type. We then characterized hotspots for diverse structural functional properties. The genes neighbouring hotspots had a small overlap with hotspot genes in other cell types and were highly enriched for cell type specific function. Hotspots were enriched for sequence motifs of key TFs in that cell type and more than 90% of hotspots were occupied by pioneering factors. Though we did not find any sequence signature in the three groups, the H3K4me1 binding profile had bimodal peaks at hotspots, distinguishing hotspots from mono-modal H3K4me1 singletons. In ES cells, differentially expressed genes after perturbation of activators were enriched for hotspot genes suggesting hotspots primarily act as transcriptional activator hubs. Finally, we proposed that ES hotspots might be under control of SetDB1 and not DNMT for silencing. Conclusion Transcriptional hotspots are enriched for tissue specific enhancers near cell type specific highly expressed genes. In ES cells, they are predicted to act as transcriptional activator hubs and might be under SetDB1 control for silencing.
机译:背景转录热点定义为受多种因素约束的基因组区域。最近,它们被鉴定为细胞类型特异性增强子,可调控蠕虫,苍蝇和人类等许多物种的发育必需基因。对同一物种中多种细胞类型的热点进行的深入分析仍有待探索,并且可以带来新的生物学见解。结果因此,我们收集了十种鼠类细胞类型的108个转录相关因子(TF)ChIP测序数据集,并根据结合占有率将其分为单组(低占有率),组合(中等占有率)三类。和热点(高占用率)。三组中的峰主要根据占用率聚集,这表明基因组位点对于中等占用率是引发的,而与细胞类型无关。然后,我们针对各种结构功能特性对热点进行了表征。热点附近的基因与其他细胞类型中的热点基因有很小的重叠,并且高度丰富了细胞类型的特定功能。在该细胞类型中,热点丰富了关键TF的序列基序,并且超过90%的热点被先驱因子占据。尽管我们在三组中均未发现任何序列签名,但H3K4me1结合谱在热点处具有双峰,从而将热点与单峰H3K4me1单例区分开。在ES细胞中,激活子扰动后差异表达的基因富集了热点基因,表明热点主要充当转录激活子中心。最后,我们建议ES热点可能在SetDB1的控制下,而不是在DNMT的控制下进行沉默。结论转录热点在细胞类型特异性高表达基因附近富含组织特异性增强子。在ES细胞中,预计它们将充当转录激活剂中枢,并可能在SetDB1控制下沉默。

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