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在基础和应激条件下,基因组关联分析 3D 染色质组织与基因表达程序之间的相互作用。

Genomic meta-analysis of the interplay between 3D chromatin organization and gene expression programs under basal and stress conditions.

机构信息

The Blavatnik School of Computer Science, Tel Aviv University, 69978, Tel Aviv, Israel.

Department of Human Molecular Genetics and Biochemistry, Sackler School of Medicine, Tel Aviv University, 69978, Tel Aviv, Israel.

出版信息

Epigenetics Chromatin. 2018 Aug 29;11(1):49. doi: 10.1186/s13072-018-0220-2.

Abstract

BACKGROUND

Our appreciation of the critical role of the genome's 3D organization in gene regulation is steadily increasing. Recent 3C-based deep sequencing techniques elucidated a hierarchy of structures that underlie the spatial organization of the genome in the nucleus. At the top of this hierarchical organization are chromosomal territories and the megabase-scale A/B compartments that correlate with transcriptional activity within cells. Below them are the relatively cell-type-invariant topologically associated domains (TADs), characterized by high frequency of physical contacts between loci within the same TAD, and are assumed to function as regulatory units. Within TADs, chromatin loops bring enhancers and target promoters to close spatial proximity. Yet, we still have only rudimentary understanding how differences in chromatin organization between different cell types affect cell-type-specific gene expression programs that are executed under basal and challenged conditions.

RESULTS

Here, we carried out a large-scale meta-analysis that integrated Hi-C data from thirteen different cell lines and dozens of ChIP-seq and RNA-seq datasets measured on these cells, either under basal conditions or after treatment. Pairwise comparisons between cell lines demonstrate a strong association between modulation of A/B compartmentalization, differential gene expression and transcription factor (TF) binding events. Furthermore, integrating the analysis of transcriptomes of different cell lines in response to various challenges, we show that A/B compartmentalization of cells under basal conditions significantly correlates not only with gene expression programs and TF binding profiles that are active under the basal condition but also with those induced in response to treatment. Yet, in pairwise comparisons between different cell lines, we find that a large portion of differential TF binding and gene induction events occur in genomic loci assigned to A compartment in both cell types, underscoring the role of additional critical factors in determining cell-type-specific transcriptional programs.

CONCLUSIONS

Our results further indicate the role of dynamic genome organization in regulation of differential gene expression between different cell types and the impact of intra-TAD enhancer-promoter interactions that are established under basal conditions on both the basal and treatment-induced gene expression programs.

摘要

背景

我们对基因组 3D 结构在基因调控中的关键作用的认识正在不断加深。最近基于 3C 的深度测序技术揭示了核基因组空间组织的结构层次。在这个层次结构的顶端是染色体区域和兆碱基尺度的 A/B 区室,它们与细胞内的转录活性相关。在它们之下是相对细胞类型不变的拓扑关联域(TAD),其特征是同一 TAD 内的基因座之间物理接触的高频,并且假定作为调控单元发挥作用。在 TAD 内,染色质环使增强子和靶启动子接近空间接近。然而,我们仍然只是初步了解不同细胞类型之间的染色质组织差异如何影响在基础和挑战条件下执行的细胞类型特异性基因表达程序。

结果

在这里,我们进行了大规模的元分析,该分析整合了来自 13 种不同细胞系的 Hi-C 数据以及在这些细胞上测量的数十个 ChIP-seq 和 RNA-seq 数据集,无论是在基础条件下还是在处理后。细胞系之间的两两比较表明,A/B 区室化的调节、差异基因表达和转录因子(TF)结合事件之间存在很强的关联。此外,整合不同细胞系在各种挑战下的转录组分析,我们表明细胞在基础条件下的 A/B 区室化不仅与基础条件下活性的基因表达程序和 TF 结合谱显著相关,而且与对治疗的反应诱导的基因表达谱显著相关。然而,在不同细胞系之间的两两比较中,我们发现大部分差异 TF 结合和基因诱导事件发生在两个细胞类型中都分配到 A 区室的基因组区域,这突出了在确定细胞类型特异性转录程序时其他关键因素的作用。

结论

我们的结果进一步表明,动态基因组组织在不同细胞类型之间差异基因表达的调节中的作用,以及在基础条件下建立的 TAD 内增强子-启动子相互作用对基础和治疗诱导的基因表达程序的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/25c0/6114837/ca48baece269/13072_2018_220_Fig1_HTML.jpg

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