Grand challenge in chromatin epigenomics: everything, everywhere, all at once

Sharon Y. R. Dent
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Abstract

Our understanding of the regulation and functions of histone modifications has come a long way since they were first reported in the mid-1960s. So too has our understanding of the importance of DNA methylation, histone variants, nucleosome locations and arrangements, and progressively higher order structures that impact when and where DNA-templated processes take place. Recent advances have even allowed the first ever complete sequencing and epigenomic profiles of individual chromosomes from telomere to telomere, including highly repetitive regions that were previously refractory to analysis. The regulatory power of chromatin organization for gene transcription, DNA replication, recombination and repair is undisputable. Still, an ongoing challenge is to understand the full spectrum of changes (everything) that impact processes in cells and tissues (everywhere) and how each change impacts others (all at once).
染色质表观基因组学面临的巨大挑战:所有的东西,所有的地方,同时发生
自20世纪60年代中期首次报道组蛋白修饰以来,我们对组蛋白修饰的调控和功能的理解已经走过了很长的路。我们对DNA甲基化、组蛋白变异、核小体位置和排列以及影响DNA模板化过程发生的时间和地点的逐步高阶结构的重要性的理解也是如此。最近的进展甚至允许首次完成从端粒到端粒的单个染色体的测序和表观基因组图谱,包括以前难以分析的高度重复区域。染色质组织对基因转录、DNA复制、重组和修复的调控能力是无可争议的。然而,一个持续的挑战是了解影响细胞和组织(任何地方)过程的所有变化(一切),以及每个变化如何影响其他变化(同时发生)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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