首页> 外文期刊>Journal of biosciences >Analysis of phage Mu DNA transposition by whole-genome Escherichia coli tiling arrays reveals a complex relationship to distribution of target selection protein B, transcription and chromosome architectural elements
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Analysis of phage Mu DNA transposition by whole-genome Escherichia coli tiling arrays reveals a complex relationship to distribution of target selection protein B, transcription and chromosome architectural elements

机译:全基因组大肠杆菌平铺阵列对噬菌体Mu DNA转座的分析揭示了与靶选择蛋白B的分布,转录和染色体结构元件的复杂关系

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Of all known transposable elements, phage Mu exhibits the highest transposition efficiency and the lowest target specificity. In vitro, MuB protein is responsible for target choice. In this work, we provide a comprehensive assessment of the genome-wide distribution of MuB and its relationship to Mu target selection using high-resolution Escherichia coli tiling DNA arrays. We have also assessed how MuB binding and Mu transposition are influenced by chromosome-organizing elements such as AT-rich DNA signatures, or the binding of the nucleoid-associated protein Fis, or processes such as transcription. The results confirm and extend previous biochemical and lower resolution in vivo data. Despite the generally random nature of Mu transposition and MuB binding, there were hot and cold insertion sites and MuB binding sites in the genome, and differences between the hottest and coldest sites were large. The new data also suggest that MuB distribution and subsequent Mu integration is responsive to DNA sequences that contribute to the structural organization of the chromosome.
机译:在所有已知的转座因子中,噬菌体Mu表现出最高的转座效率和最低的靶标特异性。在体外,MuB蛋白负责靶标的选择。在这项工作中,我们使用高分辨率的大肠杆菌平铺DNA阵列对MuB的全基因组分布及其与Mu目标选择的关系提供了全面的评估。我们还评估了MuB结合和Mu转座是如何受染色体组织元素(例如富含AT的DNA签名)或与核苷酸相关的蛋白Fis的结合或诸如转录过程的影响的。结果证实并扩展了先前的生物化学和较低分辨率的体内数据。尽管Mu换位和MuB结合通常具有随机性,但基因组中存在热插入位点和冷插入位点以及MuB结合位点,最热和最冷位点之间的差异很大。新数据还表明,MuB分布和随后的Mu整合对有助于染色体结构组织的DNA序列有响应。

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