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Inaugural Article: DNA transposon Hermes inserts into DNA in nucleosome-free regions in vivo

机译:就职文章:DNA转座子爱马仕在体内插入无核小体区域的DNA

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摘要

Transposons are mobile genetic elements that are an important source of genetic variation and are useful tools for genome engineering, mutagenesis screens, and vectors for transgenesis including gene therapy. We have used second-generation sequencing to analyze ≈2 × 105 unique de novo transposon insertion sites of the transposon Hermes in the Saccharomyces cerevisiae genome from both in vitro transposition reactions by using purified yeast genomic DNA, to better characterize intrinsic sequence specificity, and sites recovered from in vivo transposition events, to characterize the effect of intracellular factors such as chromatin on target site selection. We find that Hermes transposon targeting in vivo is profoundly affected by chromatin structure: The subset of genome-wide target sites used in vivo is strongly associated (P < 2e-16 by Fisher's exact test) with nucleosome-free chromatin. Our characterization of the insertion site preferences of Hermes not only assists in the future use of this transposon as a molecular biology tool but also establishes methods to more fully determine targeting mechanisms of other transposons. We have also discovered a long-range sequence motif that defines S. cerevisiae nucleosome-free regions.
机译:转座子是可移动的遗传元件,是遗传变异的重要来源,是用于基因组工程,诱变筛选和用于包括基因治疗在内的转基因载体的有用工具。我们已使用第二代测序技术,通过使用纯化的酵母基因组DNA从两个体外转座反应中,分析了酿酒酵母基因组中转座子爱马仕的≈2×10 5 独特的从头转座子插入位点,更好地表征内在序列特异性,并从体内转座事件中恢复位点,以表征细胞内因子(例如染色质)对靶位点选择的影响。我们发现,在体内靶向Hermes的转座子受到染色质结构的深刻影响:体内使用的全基因组靶位点的子集与无核小体的染色质紧密相关(根据Fisher的精确检验,P <2e-16)。我们对爱马仕(Hermes)插入位点偏好的表征不仅有助于将来将该转座子用作分子生物学工具,而且还建立了可以更充分地确定其他转座子靶向机制的方法。我们还发现了一个远程序列基序,该基序定义了酿酒酵母无核小体区域。

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