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Time-series analyses of directional sequence changes in SARS-CoV-2 genomes and an efficient search method for candidates for advantageous mutations for growth in human cells

机译:SARS-COV-2基因组的定向序列变化的时间序列分析以及用于人细胞生长的有利突变的候选者的有效搜索方法

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摘要

We first conducted time-series analysis of mono- and dinucleotide composition for over 10,000 SARS-CoV-2 genomes, as well as over 1500 Zaire ebolavirus genomes, and found clear time-series changes in the compositions on a monthly basis, which should reflect viral adaptations for efficient growth in human cells. We next developed a sequence alignment free method that extensively searches for advantageous mutations and rank them in an increase level for their intrapopulation frequency. Time-series analysis of occurrences of oligonucleotides of diverse lengths for SARS-CoV-2 genomes revealed seven distinctive mutations that rapidly expanded their intrapopulation frequency and are thought to be candidates of advantageous mutations for the efficient growth in human cells.
机译:我们首先对单核苷酸组合物进行多次和二核苷酸组合物的时间序列分析,以超过10,000个SARS-COV-2基因组,以及超过1500埃博尔·埃博拉病毒基因组,并每月挑选组合物的清晰时间序列变化,这应该反映病毒适应,用于人体细胞有效生长。接下来,我们开发了一种序列对准方法,其广泛地搜索有利的突变,并在增加频率的增加水平中排列它们。 SARS-COV-2基因组不同长度的寡核苷酸发生的时间序列分析揭示了七种独特的突变,迅速扩大其跨扫描频率,并且被认为是人体细胞有效生长的有利突变的候选者。

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