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全基因组范围内高度转录区域的复制起始事件耗竭。

Genome-wide depletion of replication initiation events in highly transcribed regions.

机构信息

Laboratory of Molecular Pharmacology, CCR, NCI, Bethesda, Maryland 20892, USA.

出版信息

Genome Res. 2011 Nov;21(11):1822-32. doi: 10.1101/gr.124644.111. Epub 2011 Aug 3.

Abstract

This report investigates the mechanisms by which mammalian cells coordinate DNA replication with transcription and chromatin assembly. In yeast, DNA replication initiates within nucleosome-free regions, but studies in mammalian cells have not revealed a similar relationship. Here, we have used genome-wide massively parallel sequencing to map replication initiation events, thereby creating a database of all replication initiation sites within nonrepetitive DNA in two human cell lines. Mining this database revealed that genomic regions transcribed at moderate levels were generally associated with high replication initiation frequency. In genomic regions with high rates of transcription, very few replication initiation events were detected. High-resolution mapping of replication initiation sites showed that replication initiation events were absent from transcription start sites but were highly enriched in adjacent, downstream sequences. Methylation of CpG sequences strongly affected the location of replication initiation events, whereas histone modifications had minimal effects. These observations suggest that high levels of transcription interfere with formation of pre-replication protein complexes. Data presented here identify replication initiation sites throughout the genome, providing a foundation for further analyses of DNA-replication dynamics and cell-cycle progression.

摘要

本报告研究了哺乳动物细胞如何协调 DNA 复制与转录和染色质组装。在酵母中,DNA 复制起始于无核小体区域,但在哺乳动物细胞中的研究并未揭示出类似的关系。在这里,我们使用全基因组大规模平行测序来绘制复制起始事件,从而在两个人类细胞系的非重复 DNA 中创建了所有复制起始位点的数据库。挖掘这个数据库显示,转录水平适中的基因组区域通常与高复制起始频率相关。在转录速率较高的基因组区域中,很少检测到复制起始事件。复制起始位点的高分辨率作图显示,复制起始事件不存在于转录起始位点,但在相邻的下游序列中高度富集。CpG 序列的甲基化强烈影响复制起始事件的位置,而组蛋白修饰的影响则很小。这些观察结果表明,高水平的转录会干扰前复制蛋白复合物的形成。本文提供的基因组范围内的复制起始位点数据,为进一步分析 DNA 复制动力学和细胞周期进程奠定了基础。

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