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首页> 外文期刊>Briefings in functional genomics >Exploring the mechanisms of genome-wide long-range interactions: interpreting chromosome organization
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Exploring the mechanisms of genome-wide long-range interactions: interpreting chromosome organization

机译:探索全基因组远程相互作用的机制:解释染色体组织

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摘要

Developments in chromosome conformation capture (3C) technologies have revealed that the three-dimensional organization of a genome leads widely separated functional elements to reside in close proximity. However, the mechanisms responsible for mediating long-range interactions are still not completely known. In this review, we firstly evaluate and compare the current seven 3C-based methods, summarize their advantages and discuss their limitations to our current understanding of genome structure. Then, software packages available to perform the analysis of 3C-based data are described. Moreover, we review the insights into the two main mechanisms of long-range interactions, which regulate gene expression by bringing together promoters and distal regulatory elements and by creating structural domains that contain functionally related genes with similar expression landscape. At last, we summarize what is known about the mediating factors involved in stimulation/repression of long-range interactions, such as transcription factors and noncoding RNAs.
机译:染色体构象捕获(3C)技术的发展表明,基因组的三维组织导致广泛分离的功能元件紧密相邻。但是,负责调解远距离相互作用的机制仍不完全清楚。在本文中,我们首先评估和比较了目前基于7C的七个方法,总结了它们的优点,并讨论了它们对我们目前对基因组结构的了解的局限性。然后,描述了可用于执行基于3C数据分析的软件包。此外,我们回顾了对长距​​离相互作用的两种主要机制的见解,它们通过将启动子和远端调控元件聚集在一起并通过创建包含功能相似基因且功能相似的基因的结构域来调控基因表达。最后,我们总结了有关刺激/抑制远程相互作用的中介因子的知识,例如转录因子和非编码RNA。

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