Nanopore sequencing provides snapshots of the genetic variation within salmonid alphavirus-3 (SAV3) during an ongoing infection in Atlantic salmon (Salmo salar) and brown trout (Salmo trutta).

IF 3.7 1区 农林科学 Q1 VETERINARY SCIENCES
HyeongJin Roh, Kai Ove Skaftnesmo, Dhamotharan Kannimuthu, Abdullah Madhun, Sonal Patel, Bjørn Olav Kvamme, H Craig Morton, Søren Grove
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引用次数: 0

Abstract

Frequent RNA virus mutations raise concerns about evolving virulent variants. The purpose of this study was to investigate genetic variation in salmonid alphavirus-3 (SAV3) over the course of an experimental infection in Atlantic salmon and brown trout. Atlantic salmon and brown trout parr were infected using a cohabitation challenge, and heart samples were collected for analysis of the SAV3 genome at 2-, 4- and 8-weeks post-challenge. PCR was used to amplify eight overlapping amplicons covering 98.8% of the SAV3 genome. The amplicons were subsequently sequenced using the Nanopore platform. Nanopore sequencing identified a multitude of single nucleotide variants (SNVs) and deletions. The variation was widespread across the SAV3 genome in samples from both species. Mostly, specific SNVs were observed in single fish at some sampling time points, but two relatively frequent (i.e., major) SNVs were observed in two out of four fish within the same experimental group. Two other, less frequent (i.e., minor) SNVs only showed an increase in frequency in brown trout. Nanopore reads were de novo clustered using a 99% sequence identity threshold. For each amplicon, a number of variant clusters were observed that were defined by relatively large deletions. Nonmetric multidimensional scaling analysis integrating the cluster data for eight amplicons indicated that late in infection, SAV3 genomes isolated from brown trout had greater variation than those from Atlantic salmon. The sequencing methods and bioinformatics pipeline presented in this study provide an approach to investigate the composition of genetic diversity during viral infections.

在大西洋鲑鱼(Salmo salar)和褐鳟鱼(Salmo trutta)的持续感染过程中,纳米孔测序提供了鲑鱼α-病毒-3(SAV3)内部遗传变异的快照。
RNA 病毒的频繁变异引发了人们对毒性变种进化的担忧。本研究旨在调查大西洋鲑鱼和褐鳟鱼在实验感染过程中鲑鱼α-病毒-3(SAV3)的遗传变异。采用同居挑战法感染大西洋鲑和褐鳟鱼稚鱼,在挑战后2周、4周和8周采集心脏样本分析SAV3基因组。利用 PCR 扩增出八个重叠的扩增子,覆盖了 SAV3 基因组的 98.8%。随后使用 Nanopore 平台对这些扩增子进行测序。纳米孔测序发现了大量单核苷酸变异(SNV)和缺失。在两个物种的样本中,SAV3 基因组的变异都很普遍。大多数情况下,在某些采样时间点的单条鱼身上观察到了特定的 SNV,但在同一实验组的四条鱼中,有两条鱼身上观察到了两个相对频繁(即主要)的 SNV。另外两个频率较低(即次要)的 SNV 仅在褐鳟鱼中出现频率增加。使用 99% 的序列同一性阈值对 Nanopore 读数进行从头聚类。对于每个扩增片段,都观察到了一些由相对较大的缺失所定义的变异群。对八个扩增子的聚类数据进行的非度量多维缩放分析表明,在感染后期,从褐鳟鱼体内分离出来的 SAV3 基因组比从大西洋鲑鱼体内分离出来的基因组有更大的变异。本研究中介绍的测序方法和生物信息学管道为研究病毒感染过程中遗传多样性的组成提供了一种方法。
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来源期刊
Veterinary Research
Veterinary Research 农林科学-兽医学
CiteScore
7.00
自引率
4.50%
发文量
92
审稿时长
3 months
期刊介绍: Veterinary Research is an open access journal that publishes high quality and novel research and review articles focusing on all aspects of infectious diseases and host-pathogen interaction in animals.
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