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Patterns of Evolution and Host Gene Mimicry in Influenza and Other RNA Viruses

机译:流行性感冒和其他RNA病毒的进化和宿主基因拟态模式

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摘要

It is well known that the dinucleotide CpG is under-represented in the genomic DNA of many vertebrates. This is commonly thought to be due to the methylation of cytosine residues in this dinucleotide and the corresponding high rate of deamination of 5-methycytosine, which lowers the frequency of this dinucleotide in DNA. Surprisingly, many single-stranded RNA viruses that replicate in these vertebrate hosts also have a very low presence of CpG dinucleotides in their genomes. Viruses are obligate intracellular parasites and the evolution of a virus is inexorably linked to the nature and fate of its host. One therefore expects that virus and host genomes should have common features. In this work, we compare evolutionary patterns in the genomes of ssRNA viruses and their hosts. In particular, we have analyzed dinucleotide patterns and found that the same patterns are pervasively over- or under-represented in many RNA viruses and their hosts suggesting that many RNA viruses evolve by mimicking some of the features of their host's genes (DNA) and likely also their corresponding mRNAs. When a virus crosses a species barrier into a different host, the pressure to replicate, survive and adapt, leaves a footprint in dinucleotide frequencies. For instance, since human genes seem to be under higher pressure to eliminate CpG dinucleotide motifs than avian genes, this pressure might be reflected in the genomes of human viruses (DNA and RNA viruses) when compared to those of the same viruses replicating in avian hosts. To test this idea we have analyzed the evolution of the influenza virus since 1918. We find that the influenza A virus, which originated from an avian reservoir and has been replicating in humans over many generations, evolves in a direction strongly selected to reduce the frequency of CpG dinucleotides in its genome. Consistent with this observation, we find that the influenza B virus, which has spent much more time in the human population, has adapted to its human host and exhibits an extremely low CpG dinucleotide content. We believe that these observations directly show that the evolution of RNA viral genomes can be shaped by pressures observed in the host genome. As a possible explanation, we suggest that the strong selection pressures acting on these RNA viruses are most likely related to the innate immune response and to nucleotide motifs in the host DNA and RNAs.
机译:众所周知,在许多脊椎动物的基因组DNA中,二核苷酸CpG的表达不足。通常认为这是由于该二核苷酸中胞嘧啶残基的甲基化和相应的5-甲基胞嘧啶脱氨基率高,这降低了该二核苷酸在DNA中的频率。令人惊讶的是,在这些脊椎动物宿主中复制的许多单链RNA病毒在其基因组中也存在非常低的CpG二核苷酸。病毒是专性的细胞内寄生虫,病毒的进化与宿主的性质和命运紧密相关。因此,人们期望病毒和宿主基因组应该具有共同的特征。在这项工作中,我们比较了ssRNA病毒及其宿主基因组中的进化模式。特别是,我们分析了二核苷酸模式,发现在许多RNA病毒及其宿主中普遍存在相同或过量的相同模式,这表明许多RNA病毒通过模仿其宿主基因(DNA)的某些特征而进化,并且很可能以及它们相应的mRNA。当病毒越过物种壁垒进入另一个宿主时,复制,生存和适应的压力使二核苷酸频率上的足迹减小。例如,由于人类基因似乎比禽类基因承受更大的压力来消除CpG二核苷酸基序,因此与在禽类宿主中复制相同病毒的基因组相比,这种压力可能反映在人类病毒(DNA和RNA病毒)的基因组中。 。为了验证这一观点,我们分析了自1918年以来流感病毒的进化过程。我们发现,源自禽类水库并已在人类中世代复制的甲型流感病毒朝着强烈选择的方向发展,从而降低了发病率。基因组中的CpG二核苷酸序列。与该观察结果一致,我们发现在人群中花费了更多时间的乙型流感病毒已经适应了其人类宿主,并且显示出极低的CpG二核苷酸含量。我们相信这些观察结果直接表明,RNA病毒基因组的进化可以通过宿主基因组中观察到的压力来决定。作为一种可能的解释,我们认为,作用于这些RNA病毒的强大选择压力最有可能与先天免疫应答以及宿主DNA和RNA中的核苷酸基序有关。

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