Compartmentalization with nuclear landmarks yields random, yet precise, genome organization

染色质 基因组 核板 分区(防火) 基因组组织 生物 核仁 染色体 染色体构象捕获 计算生物学 遗传学 核心 DNA 细胞生物学 基因 核蛋白 增强子 转录因子 基因表达 生物化学
作者
Kartik Kamat,Zhuohan Lao,Yifeng Qi,Yuchuan Wang,Jian Ma,Bin Zhang
出处
期刊:Biophysical Journal [Elsevier BV]
卷期号:122 (7): 1376-1389 被引量:2
标识
DOI:10.1016/j.bpj.2023.03.003
摘要

The 3D organization of eukaryotic genomes plays an important role in genome function. While significant progress has been made in deciphering the folding mechanisms of individual chromosomes, the principles of the dynamic large-scale spatial arrangement of all chromosomes inside the nucleus are poorly understood. We use polymer simulations to model the diploid human genome compartmentalization relative to nuclear bodies such as nuclear lamina, nucleoli, and speckles. We show that a self-organization process based on a cophase separation between chromosomes and nuclear bodies can capture various features of genome organization, including the formation of chromosome territories, phase separation of A/B compartments, and the liquid property of nuclear bodies. The simulated 3D structures quantitatively reproduce both sequencing-based genomic mapping and imaging assays that probe chromatin interaction with nuclear bodies. Importantly, our model captures the heterogeneous distribution of chromosome positioning across cells while simultaneously producing well-defined distances between active chromatin and nuclear speckles. Such heterogeneity and preciseness of genome organization can coexist due to the nonspecificity of phase separation and the slow chromosome dynamics. Together, our work reveals that the cophase separation provides a robust mechanism for us to produce functionally important 3D contacts without requiring thermodynamic equilibration that can be difficult to achieve.

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