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DNA复制与人类基因组组织之间的关系。

The relationship between DNA replication and human genome organization.

作者信息

Necsulea Anamaria, Guillet Claire, Cadoret Jean-Charles, Prioleau Marie-Noëlle, Duret Laurent

机构信息

Université de Lyon, Lyon, France.

出版信息

Mol Biol Evol. 2009 Apr;26(4):729-41. doi: 10.1093/molbev/msn303. Epub 2009 Jan 6.

Abstract

Assessment of the impact of DNA replication on genome architecture in Eukaryotes has long been hampered by the scarcity of experimental data. Recent work, relying on computational predictions of origins of replication, suggested that replication might be a major determinant of gene organization in human (Huvet et al. 2007. Human gene organization driven by the coordination of replication and transcription. Genome Res. 17:1278-1285). Here, we address this question by analyzing the first large-scale data set of experimentally determined origins of replication in human: 283 origins identified in HeLa cells, in 1% of the genome covered by ENCODE regions (Cadoret et al. 2008. Genome-wide studies highlight indirect links between human replication origins and gene regulation. Proc Natl Acad Sci USA. 105:15837-15842). We show that origins of replication are not randomly distributed as they display significant overlap with promoter regions and CpG islands. The hypothesis of a selective pressure to avoid frontal collisions between replication and transcription polymerases is not supported by experimental data as we find no evidence for gene orientation bias in the proximity of origins of replication. The lack of a significant orientation bias remains manifest even when considering only genes expressed at a high rate, or in a wide number of tissues, and is not affected by the regional replication timing. Gene expression breadth does not appear to be correlated with the distance from the origins of replication. We conclude that the impact of DNA replication on human genome organization is considerably weaker than previously proposed.

摘要

长期以来,实验数据的匮乏一直阻碍着对真核生物中DNA复制对基因组结构影响的评估。最近的研究工作依赖于对复制起点的计算预测,表明复制可能是人类基因组织的主要决定因素(Huvet等人,2007年。由复制和转录的协调驱动的人类基因组织。《基因组研究》17:1278 - 1285)。在这里,我们通过分析人类中第一个大规模的实验确定的复制起点数据集来解决这个问题:在HeLa细胞中鉴定出283个起点,位于ENCODE区域覆盖的1%的基因组中(Cadoret等人,2008年。全基因组研究突出了人类复制起点与基因调控之间的间接联系。《美国国家科学院院刊》105:15837 - 15842)。我们表明,复制起点并非随机分布,因为它们与启动子区域和CpG岛显示出显著重叠。复制和转录聚合酶之间避免正面碰撞的选择压力假说未得到实验数据的支持,因为我们在复制起点附近未发现基因方向偏差的证据。即使仅考虑高表达或在多种组织中表达的基因,缺乏显著的方向偏差仍然很明显,并且不受区域复制时间的影响。基因表达广度似乎与距复制起点的距离无关。我们得出结论,DNA复制对人类基因组组织的影响比先前提出的要弱得多。

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