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A deep sequencing reveals significant diversity among dominant variants and evolutionary dynamics of avian leukosis viruses in two infectious ecosystems

机译:深度测序揭示了两个传染性生态系统中禽白血病病毒的主要变异体和进化动力学之间的显着多样性

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Background As a typical retrovirus, the evolution of Avian leukosis virus subgroup J (ALV-J) in different infectious ecosystems is not characterized, what we know is there are a cloud of diverse variants, namely quasispecies with considerable genetic diversity. This study is to explore the selection of infectious ecosystems on dominant variants and their evolutionary dynamics of ALV-J between DF1 cells and specific-pathogen-free (SPF) chickens. High-throughput sequencing platforms provide an approach for detecting quasispecies diversity more fully. Results An average of about 20,000 valid reads were obtained from two variable regions of gp85 gene and LTR-U3 region from each sample in different infectious ecosystems. The top 10 dominant variants among ALV-J from chicken plasmas, DF1 cells and liver tumor were completely different from each other. Also there was a difference of shannon entropy and global selection pressure values (ω) in different infectious ecosystems. In the plasmas of two chickens, a large portion of quasispecies contained a 3-peptides “LSD” repeat insertion that was only less than 0.01% in DF1 cell culture supernatants. In parallel studies, the LTR-U3 region of ALV-J from the chicken plasmas demonstrated more variants with mutations in their transcription regulatory elements than those from DF1 cells. Conclusions Our data taken together suggest that the molecular epidemiology based on isolated ALV-J in cell culture may not represent the true evolution of virus in chicken flocks in the field. The biological significance of the “LSD” insert and mutations in LTR-U3 needs to be further studied.
机译:背景技术作为典型的逆转录病毒,禽白血病病毒J亚组(ALV-J)在不同传染性生态系统中的进化没有特征,我们知道有各种各样的变异云,即具有相当遗传多样性的准种。这项研究旨在探索主要变异体上传染性生态系统的选择及其在DF1细胞和无特定病原体(SPF)鸡之间的ALV-J进化动力学。高通量测序平台为更全面地检测准物种多样性提供了一种方法。结果从不同感染生态系统的每个样本中,从gp85基因的两个可变区和LTR-U3区平均获得约20,000个有效读数。来自鸡血浆,DF1细胞和肝肿瘤的ALV-J中最重要的10个显性变异彼此完全不同。在不同的传染性生态系统中,香农熵和总体选择压力值(ω)也存在差异。在两只鸡的血浆中,大部分准种包含3肽“ LSD”重复插入,在DF1细胞培养上清液中仅少于0.01%。在平行研究中,来自鸡血浆的ALV-J的LTR-U3区显示出比DF1细胞中的转录调控元件具有更多突变的变体。结论我们的数据加在一起表明,在细胞培养中基于分离的ALV-J的分子流行病学可能并不代表野外鸡群中病毒的真实进化。 LTR-U3中“ LSD”插入物和突变的生物学意义需要进一步研究。

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