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果蝇基因组中开放和封闭染色质结构域图谱。

Map of open and closed chromatin domains in Drosophila genome.

作者信息

Milon Beatrice, Sun Yezhou, Chang Weizhong, Creasy Todd, Mahurkar Anup, Shetty Amol, Nurminsky Dmitry, Nurminskaya Maria

机构信息

Department of Biochemistry and Molecular Biology, School of Medicine, University of Maryland, 108 N, Greene St,, Baltimore, MD 21201, USA.

出版信息

BMC Genomics. 2014 Nov 18;15(1):988. doi: 10.1186/1471-2164-15-988.

Abstract

BACKGROUND

Chromatin compactness has been considered a major determinant of gene activity and has been associated with specific chromatin modifications in studies on a few individual genetic loci. At the same time, genome-wide patterns of open and closed chromatin have been understudied, and are at present largely predicted from chromatin modification and gene expression data. However the universal applicability of such predictions is not self-evident, and requires experimental verification.

RESULTS

We developed and implemented a high-throughput analysis for general chromatin sensitivity to DNase I which provides a comprehensive epigenomic assessment in a single assay. Contiguous domains of open and closed chromatin were identified by computational analysis of the data, and correlated to other genome annotations including predicted chromatin "states", individual chromatin modifications, nuclear lamina interactions, and gene expression. While showing that the widely trusted predictions of chromatin structure are correct in the majority of cases, we detected diverse "exceptions" from the conventional rules. We found a profound paucity of chromatin modifications in a major fraction of closed chromatin, and identified a number of loci where chromatin configuration is opposite to that expected from modification and gene expression patterns. Further, we observed that chromatin of large introns tends to be closed even when the genes are expressed, and that a significant proportion of active genes including their promoters are located in closed chromatin.

CONCLUSIONS

These findings reveal limitations of the existing predictive models, indicate novel mechanisms of epigenetic regulation, and provide important insights into genome organization and function.

摘要

背景

染色质紧密程度被认为是基因活性的主要决定因素,并且在少数个别基因位点的研究中已与特定的染色质修饰相关联。与此同时,全基因组范围内开放和封闭染色质的模式尚未得到充分研究,目前很大程度上是根据染色质修饰和基因表达数据来预测的。然而,这种预测的普遍适用性并非不言而喻,需要实验验证。

结果

我们开发并实施了一种针对DNase I对一般染色质敏感性的高通量分析方法,该方法可在单一检测中提供全面的表观基因组评估。通过对数据的计算分析确定了开放和封闭染色质的连续结构域,并将其与其他基因组注释相关联,包括预测的染色质“状态”、个体染色质修饰、核纤层相互作用和基因表达。虽然表明在大多数情况下对染色质结构的广泛信任的预测是正确的,但我们检测到了与传统规则不同的各种“例外”情况。我们发现大部分封闭染色质中染色质修饰严重缺乏,并确定了一些染色质构型与修饰和基因表达模式预期相反的位点。此外,我们观察到即使基因表达,大内含子的染色质也倾向于封闭,并且相当一部分包括其启动子的活性基因位于封闭染色质中。

结论

这些发现揭示了现有预测模型的局限性,表明了表观遗传调控的新机制,并为基因组组织和功能提供了重要见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c6ee/4289254/6630f221470e/12864_2014_6860_Fig1_HTML.jpg

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