Renate W. Hakze-van der Honing , Eelco Franz , Wim H.M. van der Poel , Claudia E. Coipan
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However, the dominant HEV subtypes circulating in Europe were relatively well classified even by the 493 nt fragment, with false negative rates as low as 8 in 1000 typed sequences. Most fragments also give comparable results in analyses of population size, albeit with shorter fragments showing a broader 95 % highest posterior density interval and less obvious increase of the viral effective population size. The reconstructed phylogenies of a heterochronous subset indicated a good concordance between all the fragments, with the major clades following similar branching patterns. Furthermore, we have used the HEV sequence data from the Netherlands available in the HEVnet database as a case study for reconstruction of population size changes in the past decades. This data showed that molecular and epidemiological results are concordant and point to an increase in the viral effective population size underlying the observed increase in incidence of acute HEV infection cases. 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引用次数: 0
摘要
本研究旨在探讨 HEV 基因组片段在多大程度上可用于准确诊断和推断病毒种群规模过程。为此,我们从 NCBI GenBank 中选取了所有已发表的全基因组序列,并将其修剪为不同长度的片段(ORF1、2、3、ORF1、ORF2、ORF3、ORF2 中的 493 nt 和 ORF2 中的 148 nt)。每个片段长度都用于推断病毒序列类型的丰富性和多样性、分型准确性以及在系统动力学中的潜在用途。我们对不同片段得出的结果进行了比较。我们发现,一般来说,用于分型的核酸片段越长,预测病毒亚型的准确性就越高。然而,即使使用 493nt 片段,欧洲流行的主要 HEV 亚型的分类也相对较好,假阴性率低至 1000 个分型序列中的 8 个。在种群规模分析中,大多数片段也给出了相似的结果,尽管较短的片段显示出更宽的 95% 最高后验密度区间,病毒有效种群规模的增加也不太明显。异源子集的系统发育重建结果表明,所有片段之间的一致性很好,主要支系的分支模式相似。此外,我们还利用 HEVnet 数据库中的荷兰 HEV 序列数据作为案例研究,重建了过去几十年中病毒种群规模的变化。这些数据表明,分子和流行病学结果是一致的,都表明病毒有效种群规模的增加是观察到的急性 HEV 感染病例发病率增加的基础。在缺乏全基因组测序数据的情况下,493bp 片段可用于分析目前在欧洲流行的 HEV 株系,因为它对描述短期种群规模过程具有参考价值。
Utility of various genome lengths in diversity and evolution analyses of Hepatitis E virus
The aim of this study was to investigate to what extent fragments of the HEV genome could be used for accurate diagnostics and inference of viral population-scale processes. For this, we selected all the published whole genome sequences from the NCBI GenBank and trimmed them to various fragment lengths (ORF1,2,3, ORF1, ORF2, ORF3, 493 nt in ORF2 and 148 nt in ORF2). Each of the fragment lengths was used to infer the richness and diversity of the viral sequence types, typing accuracy, and potential use in phylodynamics. The results obtained from the different fragments were compared. We observed that, generally, the longer the nucleic acid fragment used in typing, the better the accuracy in predicting the viral subtype. However, the dominant HEV subtypes circulating in Europe were relatively well classified even by the 493 nt fragment, with false negative rates as low as 8 in 1000 typed sequences. Most fragments also give comparable results in analyses of population size, albeit with shorter fragments showing a broader 95 % highest posterior density interval and less obvious increase of the viral effective population size. The reconstructed phylogenies of a heterochronous subset indicated a good concordance between all the fragments, with the major clades following similar branching patterns. Furthermore, we have used the HEV sequence data from the Netherlands available in the HEVnet database as a case study for reconstruction of population size changes in the past decades. This data showed that molecular and epidemiological results are concordant and point to an increase in the viral effective population size underlying the observed increase in incidence of acute HEV infection cases. In the absence of whole genome sequencing data, the 493 bp fragment can be used for analyzing HEV strains currently circulating in Europe, as it is informative for describing short term population-scale processes.
期刊介绍:
Virus Research provides a means of fast publication for original papers on fundamental research in virology. Contributions on new developments concerning virus structure, replication, pathogenesis and evolution are encouraged. These include reports describing virus morphology, the function and antigenic analysis of virus structural components, virus genome structure and expression, analysis on virus replication processes, virus evolution in connection with antiviral interventions, effects of viruses on their host cells, particularly on the immune system, and the pathogenesis of virus infections, including oncogene activation and transduction.