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在人类细胞中携带复制起始区域的发夹帽DNA的游离型高拷贝数维持。

Episomal high copy number maintenance of hairpin-capped DNA bearing a replication initiation region in human cells.

作者信息

Harada Seiyu, Uchida Masafumi, Shimizu Noriaki

机构信息

Graduate School of Biosphere Science, Hiroshima University, Higashi-hiroshima 739-8521, Japan.

出版信息

J Biol Chem. 2009 Sep 4;284(36):24320-7. doi: 10.1074/jbc.M109.008128. Epub 2009 Jul 18.

Abstract

We previously found that a plasmid bearing a replication initiation region efficiently initiates gene amplification in mammalian cells and that it generates extrachromosomal double minutes and/or chromosomal homogeneously staining regions. During analysis of the underlying mechanism, we serendipitously found that hairpin-capped linear DNA was stably maintained as numerous extrachromosomal tiny episomes for more than a few months in a human cancer cell line. Generation of such episomes depended on the presence of the replication initiation region in the original plasmid. Despite extrachromosomal maintenance, episomal gene expression was epigenetically suppressed. The Southern blot analysis of the DNA of cloned cells revealed that the region around the hairpin end was diversified between the clones. Furthermore, the bisulfite-modified PCR and the sequencing analyses revealed that the palindrome sequence that derived from the original hairpin end or its end-resected structure were well preserved during clonal long term growth. From these data, we propose a model that explains the formation and maintenance of these episomes, in which replication of the hairpin-capped DNA and cruciform formation and its resolution play central roles. Our findings may be relevant for the dissection of mammalian replicator sequences.

摘要

我们先前发现,携带复制起始区域的质粒可在哺乳动物细胞中高效启动基因扩增,并产生染色体外双微体和/或染色体均匀染色区。在对其潜在机制进行分析的过程中,我们意外发现,在一种人类癌细胞系中,发夹帽状线性DNA可作为众多染色体外微小附加体稳定存在数月之久。此类附加体的产生依赖于原始质粒中复制起始区域的存在。尽管是染色体外维持状态,但附加体基因表达受到表观遗传抑制。对克隆细胞DNA的Southern印迹分析表明,各克隆之间发夹末端周围区域存在差异。此外,亚硫酸氢盐修饰的PCR和测序分析表明,源自原始发夹末端的回文序列或其末端切除结构在克隆的长期生长过程中得到了很好的保留。基于这些数据,我们提出了一个解释这些附加体形成和维持的模型,其中发夹帽状DNA的复制、十字形结构的形成及其解析起着核心作用。我们的发现可能与哺乳动物复制子序列的剖析有关。

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