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比利时近期和古代猪A组轮状病毒的全基因组特征分析及其与人类轮状病毒进化关系的评估

Complete genome characterization of recent and ancient Belgian pig group A rotaviruses and assessment of their evolutionary relationship with human rotaviruses.

作者信息

Theuns Sebastiaan, Heylen Elisabeth, Zeller Mark, Roukaerts Inge D M, Desmarets Lowiese M B, Van Ranst Marc, Nauwynck Hans J, Matthijnssens Jelle

机构信息

Ghent University, Faculty of Veterinary Medicine, Department of Virology, Parasitology and Immunology, Laboratory of Virology, Merelbeke, Belgium

KU Leuven-University of Leuven, Department of Microbiology and Immunology, Laboratory for Clinical and Epidemiological Virology, Rega Institute for Medical Research, Leuven, Belgium.

出版信息

J Virol. 2015 Jan 15;89(2):1043-57. doi: 10.1128/JVI.02513-14. Epub 2014 Nov 5.

Abstract

UNLABELLED

Group A rotaviruses (RVAs) are an important cause of diarrhea in young pigs and children. An evolutionary relationship has been suggested to exist between pig and human RVAs. This hypothesis was further investigated by phylogenetic analysis of the complete genomes of six recent (G2P[27], G3P[6], G4P[7], G5P[7], G9P[13], and G9P[23]) and one historic (G1P[7]) Belgian pig RVA strains and of all completely characterized pig RVAs from around the globe. In contrast to the large diversity of genotypes found for the outer capsid proteins VP4 and VP7, a relatively conserved genotype constellation (I5-R1-C1-M1-A8-N1-T7-E1-H1) was found for the other 9 genes in most pig RVA strains. VP1, VP2, VP3, NSP2, NSP4, and NSP5 genes of porcine RVAs belonged to genotype 1, which is shared with human Wa-like RVAs. However, for most of these gene segments, pig strains clustered distantly from human Wa-like RVAs, indicating that viruses from both species have entered different evolutionary paths. However, VP1, VP2, and NSP3 genes of some archival human strains were moderately related to pig strains. Phylogenetic analysis of the VP6, NSP1, and NSP3 genes, as well as amino acid analysis of the antigenic regions of VP7, further confirmed this evolutionary segregation. The present results also indicate that the species barrier is less strict for pig P[6] strains but that chances for successful spread of these strains in the human population are hampered by the better adaptation of pig RVAs to pig enterocytes. However, future surveillance of pig and human RVA strains is warranted.

IMPORTANCE

Rotaviruses are an important cause of diarrhea in many species, including pigs and humans. Our understanding of the evolutionary relationship between rotaviruses from both species is limited by the lack of genomic data on pig strains. In this study, recent and ancient Belgian pig rotavirus isolates were sequenced, and their evolutionary relationship with human Wa-like strains was investigated. Our data show that Wa-like human and pig strains have entered different evolutionary paths. Our data indicate that pig P[6] strains form the most considerable risk for interspecies transmission to humans. However, efficient spread of pig strains in the human population is most likely hampered by the adaptation of some crucial viral proteins to the cellular machinery of pig enterocytes. These data allow a better understanding of the risk for direct interspecies transmission events and the emergence of pig rotaviruses or pig-human reassortants in the human population.

摘要

未标记

A 组轮状病毒(RVAs)是仔猪和儿童腹泻的重要病因。有人提出猪和人 RVAs 之间存在进化关系。通过对 6 株近期(G2P[27]、G3P[6]、G4P[7]、G5P[7]、G9P[13]和 G9P[23])和 1 株历史悠久(G1P[7])的比利时猪 RVA 毒株以及全球所有已完全鉴定的猪 RVA 的全基因组进行系统发育分析,进一步研究了这一假说。与在外衣壳蛋白 VP4 和 VP7 中发现的大量基因型多样性不同,在大多数猪 RVA 毒株中,其他 9 个基因发现了相对保守的基因型组合(I5-R1-C1-M1-A8-N1-T7-E1-H1)。猪 RVAs 的 VP1、VP2、VP3、NSP2、NSP4 和 NSP5 基因属于 1 型基因型,与人类 Wa 样 RVAs 共享。然而,对于这些基因片段中的大多数,猪毒株与人类 Wa 样 RVAs 的聚类距离较远,表明这两个物种的病毒已进入不同的进化路径。然而,一些存档人类毒株的 VP1、VP2 和 NSP3 基因与猪毒株有中度相关性。VP6、NSP1 和 NSP3 基因的系统发育分析以及 VP7 抗原区域的氨基酸分析进一步证实了这种进化分离。目前结果还表明,猪 P[6]毒株的种间屏障不太严格,但这些毒株在人群中成功传播的机会因猪 RVAs 对猪肠上皮细胞的更好适应性而受到阻碍。然而,未来仍有必要对猪和人 RVA 毒株进行监测。

重要性

轮状病毒是包括猪和人在内的许多物种腹泻的重要病因。我们对这两个物种的轮状病毒之间进化关系的理解因缺乏猪毒株的基因组数据而受到限制。在本研究中,对近期和古代的比利时猪轮状病毒分离株进行了测序,并研究了它们与人类 Wa 样毒株的进化关系。我们的数据表明,Wa 样人类和猪毒株已进入不同的进化路径。我们的数据表明,猪 P[6]毒株构成了跨物种传播给人类的最大风险。然而,猪毒株在人群中的有效传播很可能因一些关键病毒蛋白对猪肠上皮细胞的细胞机制的适应性而受到阻碍。这些数据有助于更好地理解直接跨物种传播事件的风险以及猪轮状病毒或猪 - 人重组体在人群中的出现。

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