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Merkel 细胞多瘤病毒和人类多瘤病毒 6 的系统发生学:与人类的长期历史。

Phylodynamics of Merkel-cell polyomavirus and human polyomavirus 6: A long-term history with humans.

机构信息

Universidad de Buenos Aires, Facultad de Farmacia y Bioquímica, Departamento de Microbiología, Inmunología y Biotecnología, Cátedra de Virología, Buenos Aires, Argentina; CONICET, Buenos Aires, Argentina.

Universidad de Buenos Aires, Facultad de Farmacia y Bioquímica, Departamento de Microbiología, Inmunología y Biotecnología, Cátedra de Virología, Buenos Aires, Argentina; CONICET, Buenos Aires, Argentina.

出版信息

Mol Phylogenet Evol. 2018 Sep;126:210-220. doi: 10.1016/j.ympev.2018.04.025. Epub 2018 Apr 20.

DOI:10.1016/j.ympev.2018.04.025
PMID:29680507
Abstract

New human polyomaviruses have been described in the last years, including the Merkel-cell polyomavirus (MCPyV; Human polyomavirus 5) and the Human polyomavirus 6 (HPyV6). Although their infection is usually asymptomatic, in immunocompromised host can cause life-threatening pathologies, such as the Merkel cell carcinoma, an aggressive skin neoplasia associated to the MCPyV. Despite being prevalent viruses in population, epidemiological data from South America are scarce, as well as the characterization of the viral types circulating and their origin. The aims of this work were to describe MCPyV and HPyV6 from environmental samples with different geographical origin and to analyze their phylogenetic and evolutionary histories, particularly for MCPyV. Partial and complete genome sequences were obtained from sewage samples from Argentina, Uruguay and Spain. A total number of 87 sequences were obtained for MCPyV and 33 for HPyV6. Phylogenetic analysis showed that MCPyV sequences distributed according to their geographic origin in Europe/North America, Africa, Asia, South America and Oceania groups, suggesting that viral diversification might have followed human migrations across the globe. In particular, viruses from Argentina associated with Europe/North America and South America genotypes, whereas those from Uruguay and Spain also grouped with Africa genotype, reflecting the origin of the current population in each country, which could arrive not only during ancient human migration but also during recent migratory events. In addition, the South American group presented a high level of clusterization, showing internal clusters that could be related to specific locations, such as French Guiana and Brazil or the Southern region into South America, such as Argentina and Uruguay, suggesting a long term evolutionary process in the region. Additionally, in this work, we carried out the first analysis about the evolutionary history of MCPyV trough the integration of phylogenetic, epidemiological and historical data. Since a strong association is observed between the phylogenetic relationships and the origin of the sampled population, this analysis was based on the hypothesis of co-divergence between the virus and human populations. This analysis resulted in a substitution rate of 5.1 × 10 s/s/y (∼5.1% of divergence per million years) for the complete genome of MCPyV, which is in the range of those estimated for other double-stranded DNA viruses. Regarding HPyV6, a South American group with clusterization was observed (sequences from Uruguay). Meanwhile, sequences from Argentina grouped with European ones (France and Spain) and remained separated from those isolated in China, USA or Australia. The analysis of viruses from the environment allowed us to deep characterize prevalent infections in different geographic regions, reveling that viruses circulating in each population reflected its origin and that there are specific lineages associated with South America.

摘要

新的人类多瘤病毒在过去几年中被描述,包括 Merkel 细胞多瘤病毒(MCPyV;人类多瘤病毒 5)和人类多瘤病毒 6(HPyV6)。尽管它们的感染通常是无症状的,但在免疫功能低下的宿主中,可能会导致危及生命的病理,例如 Merkel 细胞癌,这是一种与 MCPyV 相关的侵袭性皮肤肿瘤。尽管这些病毒在人群中普遍存在,但来自南美的流行病学数据很少,包括循环病毒类型及其来源的特征。这项工作的目的是描述来自不同地理来源的环境样本中的 MCPyV 和 HPyV6,并分析它们的系统发育和进化历史,特别是对于 MCPyV。从阿根廷、乌拉圭和西班牙的污水样本中获得了部分和完整的基因组序列。获得了 87 个 MCPyV 序列和 33 个 HPyV6 序列。系统发育分析表明,MCPyV 序列根据其在欧洲/北美、非洲、亚洲、南美和大洋洲组的地理起源分布,表明病毒多样化可能遵循人类在全球范围内的迁移。特别是,来自阿根廷的病毒与欧洲/北美和南美的基因型相关,而来自乌拉圭和西班牙的病毒也与非洲的基因型相关,反映了每个国家当前人口的起源,这些人口不仅可能在古代人类迁移时到达,也可能在最近的迁徙事件中到达。此外,南美组表现出高水平的聚类,显示出可能与特定地点相关的内部聚类,例如法属圭亚那和巴西或南美洲的南部地区,例如阿根廷和乌拉圭,这表明该地区存在长期的进化过程。此外,在这项工作中,我们通过整合系统发育、流行病学和历史数据,首次对 MCPyV 的进化历史进行了分析。由于观察到系统发育关系与采样人群的起源之间存在很强的相关性,因此该分析基于病毒和人群共同进化的假设。这项分析导致 MCPyV 完整基因组的替换率为 5.1×10 s/s/y(每百万年约 5.1%的分歧),这在其他双链 DNA 病毒的估计范围内。关于 HPyV6,观察到一个具有聚类的南美组(来自乌拉圭的序列)。同时,来自阿根廷的序列与欧洲的序列(法国和西班牙)聚集在一起,与在中国、美国或澳大利亚分离的序列分开。对环境病毒的分析使我们能够深入描述不同地理区域的流行感染情况,揭示出在每个人群中循环的病毒反映了其起源,并且存在与南美洲相关的特定谱系。

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