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细胞重编程过程中的转录激活与三维开放染色质枢纽的形成相关。

Transcriptional activation during cell reprogramming correlates with the formation of 3D open chromatin hubs.

机构信息

CNAG-CRG, Centre for Genomic Regulation (CRG), Barcelona Institute of Science and Technology (BIST), Baldiri i Reixac 4, 08028, Barcelona, Spain.

Centre for Genomic Regulation (CRG), Barcelona Institute of Science and Technology (BIST), Dr. Aiguader 88, 08003, Barcelona, Spain.

出版信息

Nat Commun. 2020 May 22;11(1):2564. doi: 10.1038/s41467-020-16396-1.

Abstract

Chromosome structure is a crucial regulatory factor for a wide range of nuclear processes. Chromosome conformation capture (3C)-based experiments combined with computational modelling are pivotal for unveiling 3D chromosome structure. Here, we introduce TADdyn, a tool that integrates time-course 3C data, restraint-based modelling, and molecular dynamics to simulate the structural rearrangements of genomic loci in a completely data-driven way. We apply TADdyn on in situ Hi-C time-course experiments studying the reprogramming of murine B cells to pluripotent cells, and characterize the structural rearrangements that take place upon changes in the transcriptional state of 21 genomic loci of diverse expression dynamics. By measuring various structural and dynamical properties, we find that during gene activation, the transcription starting site contacts with open and active regions in 3D chromatin domains. We propose that these 3D hubs of open and active chromatin may constitute a general feature to trigger and maintain gene transcription.

摘要

染色体结构是广泛的核过程的关键调节因子。基于染色体构象捕获(3C)的实验与计算建模相结合对于揭示 3D 染色体结构至关重要。在这里,我们引入了 TADdyn,这是一种工具,它可以整合时程 3C 数据、基于约束的建模和分子动力学,以完全数据驱动的方式模拟基因组位点的结构重排。我们将 TADdyn 应用于原位 Hi-C 时程实验,该实验研究了小鼠 B 细胞向多能细胞的重编程,并表征了在转录状态变化时发生的 21 个基因组位点的结构重排,这些基因组位点具有不同的表达动力学。通过测量各种结构和动态特性,我们发现,在基因激活过程中,转录起始位点与 3D 染色质域中的开放和活跃区域接触。我们提出,这些开放和活跃染色质的 3D 中心可能构成触发和维持基因转录的一般特征。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e6c4/7244774/84ee57f43afe/41467_2020_16396_Fig1_HTML.jpg

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