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可渗透的 TAD 边界及其对与基因组相关功能的影响。

Permeable TAD boundaries and their impact on genome-associated functions.

机构信息

MRC Molecular Haematology Unit, MRC Weatherall Institute of Molecular Medicine, Radcliffe Department of Medicine, University of Oxford, Oxford, UK.

Blood and Transplant Research Unit in Precision Cellular Therapeutics, National Institute of Health Research, Oxford, UK.

出版信息

Bioessays. 2024 Oct;46(10):e2400137. doi: 10.1002/bies.202400137. Epub 2024 Aug 2.

Abstract

TAD boundaries are genomic elements that separate biological processes in neighboring domains by blocking DNA loops that are formed through Cohesin-mediated loop extrusion. Most TAD boundaries consist of arrays of binding sites for the CTCF protein, whose interaction with the Cohesin complex blocks loop extrusion. TAD boundaries are not fully impermeable though and allow a limited amount of inter-TAD loop formation. Based on the reanalysis of Nano-C data, a multicontact Chromosome Conformation Capture assay, we propose a model whereby clustered CTCF binding sites promote the successive stalling of Cohesin and subsequent dissociation from the chromatin. A fraction of Cohesin nonetheless achieves boundary read-through. Due to a constant rate of Cohesin dissociation elsewhere in the genome, the maximum length of inter-TAD loops is restricted though. We speculate that the DNA-encoded organization of stalling sites regulates TAD boundary permeability and discuss implications for enhancer-promoter loop formation and other genomic processes.

摘要

TAD 边界是基因组元件,通过阻止通过 Cohesin 介导的环挤出形成的 DNA 环,将相邻结构域中的生物过程分隔开来。大多数 TAD 边界由 CTCF 蛋白结合位点的阵列组成,其与 Cohesin 复合物的相互作用阻止了环挤出。然而,TAD 边界并非完全不可渗透,而是允许有限量的跨 TAD 环形成。基于对 Nano-C 数据的重新分析,一种多接触染色体构象捕获测定法,我们提出了一个模型,其中簇集的 CTCF 结合位点促进 Cohesin 的连续停顿,并随后从染色质中解离。然而,一部分 Cohesin 仍然实现了边界通读。由于基因组其他部位的 Cohesin 解离率保持不变,因此跨 TAD 环的最大长度受到限制。我们推测,停顿位点的 DNA 编码组织调节 TAD 边界的通透性,并讨论了对增强子-启动子环形成和其他基因组过程的影响。

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