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真核生物复制起点的全基因组分析揭示了它们在特定但灵活的位点的组织,这些位点由保守特征定义。

Genome-scale analysis of metazoan replication origins reveals their organization in specific but flexible sites defined by conserved features.

机构信息

Institute of Human Genetics, CNRS, Montpellier, France.

出版信息

Genome Res. 2011 Sep;21(9):1438-49. doi: 10.1101/gr.121830.111. Epub 2011 Jul 12.

Abstract

In metazoans, thousands of DNA replication origins (Oris) are activated at each cell cycle. Their genomic organization and their genetic nature remain elusive. Here, we characterized Oris by nascent strand (NS) purification and a genome-wide analysis in Drosophila and mouse cells. We show that in both species most CpG islands (CGI) contain Oris, although methylation is nearly absent in Drosophila, indicating that this epigenetic mark is not crucial for defining the activated origin. Initiation of DNA synthesis starts at the borders of CGI, resulting in a striking bimodal distribution of NS, suggestive of a dual initiation event. Oris contain a unique nucleotide skew around NS peaks, characterized by G/T and C/A overrepresentation at the 5' and 3' of Ori sites, respectively. Repeated GC-rich elements were detected, which are good predictors of Oris, suggesting that common sequence features are part of metazoan Oris. In the heterochromatic chromosome 4 of Drosophila, Oris correlated with HP1 binding sites. At the chromosome level, regions rich in Oris are early replicating, whereas Ori-poor regions are late replicating. The genome-wide analysis was coupled with a DNA combing analysis to unravel the organization of Oris. The results indicate that Oris are in a large excess, but their activation does not occur at random. They are organized in groups of site-specific but flexible origins that define replicons, where a single origin is activated in each replicon. This organization provides both site specificity and Ori firing flexibility in each replicon, allowing possible adaptation to environmental cues and cell fates.

摘要

在后生动物中,每个细胞周期都会激活数千个 DNA 复制起点 (Ori)。它们的基因组组织和遗传性质仍然难以捉摸。在这里,我们通过新生链 (NS) 纯化和在果蝇和小鼠细胞中的全基因组分析来表征 Ori。我们表明,在这两种物种中,大多数 CpG 岛 (CGI) 都包含 Ori,尽管果蝇中的甲基化几乎不存在,这表明这种表观遗传标记对于定义激活的 ori 并不重要。DNA 合成的起始始于 CGI 的边界,导致 NS 呈现出明显的双峰分布,提示存在双重起始事件。 Ori 包含 NS 峰周围独特的核苷酸倾斜,特征是 Ori 位点的 5' 和 3' 处分别存在 G/T 和 C/A 的过度表达。检测到重复的 GC 丰富元件,它们是 Ori 的良好预测因子,表明常见的序列特征是后生动物 Ori 的一部分。在果蝇的异染色质染色体 4 中,Ori 与 HP1 结合位点相关。在染色体水平上,富含 Ori 的区域复制较早,而 Ori 较少的区域复制较晚。全基因组分析与 DNA 梳理分析相结合,以揭示 Ori 的组织。结果表明, Ori 数量过多,但它们的激活并非随机发生。它们以特定于位点但灵活的 ori 分组组织,其中每个复制子中仅激活一个 ori。这种组织在每个复制子中提供了位点特异性和 Ori 点火灵活性,允许可能适应环境线索和细胞命运。

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