Shaping gene expression and its evolution by chromatin architecture and enhancer activity.

2区 生物学 Q1 Biochemistry, Genetics and Molecular Biology
Current Topics in Developmental Biology Pub Date : 2024-01-01 Epub Date: 2024-02-01 DOI:10.1016/bs.ctdb.2024.01.001
Jorge Mañes-García, Raquel Marco-Ferreres, Leonardo Beccari
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引用次数: 0

Abstract

Transcriptional regulation plays a pivotal role in orchestrating the intricate genetic programs governing embryonic development. The expression of developmental genes relies on the combined activity of several cis-regulatory elements (CREs), such as enhancers and silencers, which can be located at long linear distances from the genes that they regulate and that interact with them through establishment of chromatin loops. Mutations affecting their activity or interaction with their target genes can lead to developmental disorders and are thought to have importantly contributed to the evolution of the animal body plan. The income of next-generation-sequencing approaches has allowed identifying over a million of sequences with putative regulatory potential in the human genome. Characterizing their function and establishing gene-CREs maps is essential to decode the logic governing developmental gene expression and is one of the major challenges of the post-genomic era. Chromatin 3D organization plays an essential role in determining how CREs specifically contact their target genes while avoiding deleterious off-target interactions. Our understanding of these aspects has greatly advanced with the income of chromatin conformation capture techniques and fluorescence microscopy approaches to visualize the organization of DNA elements in the nucleus. Here we will summarize relevant aspects of how the interplay between CRE activity and chromatin 3D organization regulates developmental gene expression and how it relates to pathological conditions and the evolution of animal body plan.

通过染色质结构和增强子活性塑造基因表达及其进化。
转录调控在协调管理胚胎发育的复杂遗传程序中起着关键作用。发育基因的表达依赖于增强子和沉默子等几种顺式调控元件(CREs)的综合活性,这些元件与其调控的基因之间的线性距离很长,并通过建立染色质环路与之相互作用。影响这些基因活性或与其靶基因相互作用的突变可导致发育障碍,并被认为对动物体计划的进化做出了重要贡献。下一代测序方法的收入使得人类基因组中具有潜在调控能力的序列超过一百万个。鉴定它们的功能和建立基因-CREs图谱对于解码发育基因表达的逻辑至关重要,也是后基因组时代的主要挑战之一。染色质三维组织在决定 CREs 如何特异性地接触其靶基因,同时避免有害的脱靶相互作用方面起着至关重要的作用。随着染色质构象捕获技术和荧光显微镜方法的收入,我们对这些方面的理解有了很大的进步,可以直观地看到细胞核中 DNA 元素的组织。在此,我们将总结 CRE 活性与染色质三维组织之间的相互作用如何调控发育基因的表达,以及它与病理条件和动物体计划的进化之间的关系。
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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来源期刊
CiteScore
6.00
自引率
0.00%
发文量
91
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