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首页> 外文期刊>Virus Research: An International Journal of Molecular and Cellular Virology >Strand-specific compositional asymmetries in double-stranded DNA viruses.
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Strand-specific compositional asymmetries in double-stranded DNA viruses.

机译:Strand-specific成分的不对称双链DNA病毒。

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摘要

Analysis of 22 complete sequences of double-stranded DNA viruses reveals striking compositional asymmetries between leading and lagging, and between transcribed and non-transcribed strands. In all bi-directionally replicated genomes analyzed, the observed leading strand GC skew (measuring relative excess of guanines versus cytosines) is different from that in the lagging strand. In most of these genomes GC skew switches polarity close to replication origins. GC skew changes linearly across adenovirus linear genomes, which replicate from one end. In papillomavirus, GC skew is positive in one half of the genome where transcription and replication proceed in the same direction, and is close to zero in the other half with divergent transcription and replication. Possible contributions of these two processes (and associated repair mechanisms) as well as other potential sources of strand bias in the observed asymmetries are discussed. Use of cumulative skew plots for genome comparisons is demonstrated on the example of herpes simplex virus.
机译:22的完整序列的分析双链DNA病毒显示出惊人的的领导和之间的不对称滞后,转录和non-transcribed链。复制的基因组分析,观察到的领导链(GC倾斜测量的相对过剩鸟嘌呤与胞核嘧啶)是不同的后随链。GC倾斜开关极性接近复制的起源。腺病毒基因组线性,复制一个结束。在一个基因组,转录和的一半复制在同一个方向,和接近于零的另一半发散转录和复制。的贡献(以及这两个过程修复机制)以及其他有关观察到的潜在来源链的偏见讨论了不对称。情节展现出对基因组的比较单纯疱疹病毒的例子。

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