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Nonspaced inverted DNA repeats are preferential targets for homology-directed gene repair in mammalian cells

机译:非间隔反向DNA重复序列是哺乳动物细胞中同源基因修复的优先靶标

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摘要

DNA repeats constitute potential sites for the nucleation of secondary structures such as hairpins and cruciforms. Studies performed mostly in bacteria and yeast showed that these noncanonical DNA structures are breakage-prone, making them candidate targets for cellular DNA repair pathways. Possible culprits for fragility at repetitive DNA sequences include replication and transcription as well as the action of structure–specific nucleases. Despite their patent biological relevance, the parameters governing DNA repeat-associated chromosomal transactions remain ill-defined. Here, we established an episomal recombination system based on donor and acceptor complementary DNA templates to investigate the role of direct and inverted DNA repeats in homologous recombination (HR) in mammalian cells. This system allowed us also to ascertain in a stringent manner the impact of repetitive sequence replication on homology-directed gene repair. We found that nonspaced DNA repeats can, per se, engage the HR pathway of the cell and that this process is primarily dependent on their spacing and relative arrangement (i.e. parallel or antiparallel) rather than on their sequence. Indeed, our data demonstrate that contrary to direct and spaced inverted repeats, nonspaced inverted repeats are intrinsically recombinogenic motifs in mammalian cells lending experimental support to their role in genome dynamics in higher eukaryotes.
机译:DNA重复序列构成了发夹和十字形等二级结构成核的潜在位点。大多数在细菌和酵母菌中进行的研究表明,这些非规范的DNA结构易于断裂,使其成为细胞DNA修复途径的候选靶标。重复DNA序列易碎的可能原因包括复制和转录以及结构特异性核酸酶的作用。尽管它们具有专利生物学相关性,但是控制DNA重复相关染色体交易的参数仍然不确定。在这里,我们建立了一个基于供体和受体互补DNA模板的附加型重组系统,以研究直接和反向DNA重复序列在哺乳动物细胞中同源重组(HR)中的作用。该系统还允许我们以严格的方式确定重复序列复制对同源性指导的基因修复的影响。我们发现无间隔的DNA重复序列本身可以参与细胞的HR途径,并且这个过程主要取决于它们的间隔和相对排列(即平行或反平行)而不是它们的序列。确实,我们的数据表明,与直接和间隔的反向重复序列相反,非间隔的反向重复序列是哺乳动物细胞中固有的重组原基,这为它们在高等真核生物基因组动力学中的作用提供了实验性支持。

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