首页> 美国卫生研究院文献>Nucleic Acids Research >Concordance of experimentally mapped or predicted Z-DNA sites with positions of selected alternating purine-pyrimidine tracts.
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Concordance of experimentally mapped or predicted Z-DNA sites with positions of selected alternating purine-pyrimidine tracts.

机译:实验定位或预测的Z-DNA位点与选定的嘌呤-嘧啶交替片段位置的一致性。

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摘要

The recent electronmicroscopic and biochemical mapping of Z-DNA sites in phi X174, SV40, pBR322 and PM2 DNAs has been used to determine two sets of criteria for identification of potential Z-DNA sequences in natural DNA genomes. The prediction of potential Z-DNA tracts and corresponding statistical analysis of their occurrence have been made on a sample of 14 DNA genomes. Alternating purine and pyrimidine tracts longer than 5 base pairs in length and their clusters (quasi alternating fragments) in the 14 genomes studied are under-represented compared to the expectation from corresponding random sequences. The fragments [d(G X C)]n and [d(C X G)]n (n greater than or equal to 3) in general do not occur in circular DNA genomes and are under-represented in the linear DNAs of phages lambda and T7, whereas in linear genomes of adenoviruses they are strongly over-represented. With minor exceptions, potential Z-DNA sites are also under-represented compared to random sequences. In the 14 genomes studied, predicted Z-DNA tracts occur in non-coding as well as in protein coding regions. The predicted Z-DNA sites in phi X174, SV40, pBR322 and PM2 correspond well with those mapped experimentally. A complete listing together with a compact graphical representation of alternating purine-pyrimidine fragments and their Z-forming potential are presented.
机译:phi X174,SV40,pBR322和PM2 DNA中Z-DNA位点的最新电子显微镜和生化图谱已用于确定两组标准,用于鉴定天然DNA基因组中潜在的Z-DNA序列。对14个DNA基因组样本进行了潜在Z-DNA片段的预测和相应的统计分析。与来自相应随机序列的预期相比,交替的嘌呤和嘧啶片段的长度超过5个碱基对,并且它们在研究的14个基因组中的簇(准交替片段)的表达不足。片段[d(GXC)] n和[d(CXG)] n(n大于或等于3)通常不会出现在环状DNA基因组中,而在噬菌体λ和T7的线性DNA中代表性不足,而在腺病毒的线性基因组中,它们的表达量过高。除少数例外,与随机序列相比,潜在的Z-DNA位点也不足。在研究的14个基因组中,预测的Z-DNA片段出现在非编码区和蛋白质编码区。 phi X174,SV40,pBR322和PM2中的预测Z-DNA位点与实验定位的位点非常吻合。介绍了完整的清单以及交替的嘌呤-嘧啶片段及其Z形成潜力的紧凑图形表示。

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