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体内远距离染色质调控相互作用。

Long-range chromatin regulatory interactions in vivo.

作者信息

Carter David, Chakalova Lyubomira, Osborne Cameron S, Dai Yan-feng, Fraser Peter

机构信息

Laboratory of Chromatin and Gene Expression, Developmental Genetics Programme, The Babraham Institute, Cambridge CB2 4AT, UK.

出版信息

Nat Genet. 2002 Dec;32(4):623-6. doi: 10.1038/ng1051. Epub 2002 Nov 11.

DOI:10.1038/ng1051
PMID:12426570
Abstract

Communication between distal chromosomal elements is essential for control of many nuclear processes. For example, genes in higher eukaryotes often require distant enhancer sequences for high-level expression. The mechanisms proposed for long-range enhancer action fall into two basic categories. Non-contact models propose that enhancers act at a distance to create a favorable environment for gene transcription, or act as entry sites or nucleation points for factors that ultimately communicate with the gene. Contact models propose that communication occurs through direct interaction between the distant enhancer and the gene by various mechanisms that 'loop out' the intervening sequences. Although much attention has focused on contact models, the existence and nature of long-range interactions is still controversial and speculative, as there is no direct evidence that distant sequences physically interact in vivo. Here, we report the development of a widely applicable in situ technique to tag and recover chromatin in the immediate vicinity of an actively transcribed gene. We show that the classical enhancer element, HS2 of the prototypical locus control region (LCR) of the beta-globin gene cluster, is in close physical proximity to an actively transcribed HBB (beta-globin) gene located over 50 kb away in vivo, suggesting a direct regulatory interaction. The results give unprecedented insight into the in vivo structure of the LCR-gene interface and provide the first direct evidence of long-range enhancer communication.

摘要

远端染色体元件之间的通讯对于许多核过程的调控至关重要。例如,高等真核生物中的基因通常需要远距离的增强子序列才能实现高水平表达。提出的远距离增强子作用机制可分为两大类。非接触模型提出,增强子在远距离发挥作用以创造有利于基因转录的环境,或作为最终与基因通讯的因子的进入位点或成核点。接触模型提出,通讯是通过远距离增强子与基因之间的直接相互作用,通过各种使中间序列“环出”的机制实现的。尽管很多注意力都集中在接触模型上,但远距离相互作用的存在和性质仍然存在争议且具有推测性,因为没有直接证据表明远距离序列在体内发生物理相互作用。在此,我们报告了一种广泛适用的原位技术的开发,用于标记和回收活跃转录基因紧邻区域的染色质。我们表明,经典的增强子元件,即β-珠蛋白基因簇典型基因座控制区(LCR)的HS2,在体内与位于50多kb外的活跃转录的HBB(β-珠蛋白)基因在物理上紧密相邻,提示存在直接的调控相互作用。这些结果为LCR-基因界面的体内结构提供了前所未有的见解,并为远距离增强子通讯提供了首个直接证据。

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