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通过系统发育地理学模型追踪环北极地区乙型肝炎病毒(HBV)基因型B5(原B6)的进化史。

Tracing hepatitis B virus (HBV) genotype B5 (formerly B6) evolutionary history in the circumpolar Arctic through phylogeographic modelling.

作者信息

Bouckaert Remco, Simons Brenna C, Krarup Henrik, Friesen T Max, Osiowy Carla

机构信息

Department of Computer Science, University of Auckland, Auckland, New Zealand.

Alaska Native Tribal Health Consortium, Anchorage, AK, United States of America.

出版信息

PeerJ. 2017 Aug 31;5:e3757. doi: 10.7717/peerj.3757. eCollection 2017.

Abstract

BACKGROUND

Indigenous populations of the circumpolar Arctic are considered to be endemically infected (>2% prevalence) with hepatitis B virus (HBV), with subgenotype B5 (formerly B6) unique to these populations. The distinctive properties of HBV/B5, including high nucleotide diversity yet no significant liver disease, suggest virus adaptation through long-term host-pathogen association.

METHODS

To investigate the origin and evolutionary spread of HBV/B5 into the circumpolar Arctic, fifty-seven partial and full genome sequences from Alaska, Canada and Greenland, having known location and sampling dates spanning 40 years, were phylogeographically investigated by Bayesian analysis (BEAST 2) using a reversible-jump-based substitution model and a clock rate estimated at 4.1 × 10 substitutions/site/year.

RESULTS

Following an initial divergence from an Asian viral ancestor approximately 1954 years before present (YBP; 95% highest probability density interval [1188, 2901]), HBV/B5 coalescence occurred almost 1000 years later. Surprisingly, the HBV/B5 ancestor appears to locate first to Greenland in a rapid coastal route progression based on the landscape aware geographic model, with subsequent B5 evolution and spread westward. Bayesian skyline plot analysis demonstrated an HBV/B5 population expansion occurring approximately 400 YBP, coinciding with the disruption of the Neo-Eskimo Thule culture into more heterogeneous and regionally distinct Inuit populations throughout the North American Arctic.

DISCUSSION

HBV/B5 origin and spread appears to occur coincident with the movement of Neo-Eskimo (Inuit) populations within the past 1000 years, further supporting the hypothesis of HBV/host co-expansion, and illustrating the concept of host-pathogen adaptation and balance.

摘要

背景

环北极地区的原住民被认为是乙肝病毒(HBV)的地方性感染人群(患病率>2%),这些人群中存在独特的B5亚基因型(原B6亚基因型)。HBV/B5的独特特性,包括高核苷酸多样性但无明显肝脏疾病,表明病毒通过长期的宿主-病原体关联实现了适应性进化。

方法

为了研究HBV/B5在环北极地区的起源和进化传播,对来自阿拉斯加、加拿大和格陵兰的57个部分和完整基因组序列进行了系统发育地理学研究,这些序列已知位置和采样日期,时间跨度为40年。采用基于可逆跳跃的替代模型和估计为4.1×10-6替代/位点/年的时钟速率,通过贝叶斯分析(BEAST 2)进行分析。

结果

在大约距今1954年(YBP;95%最高概率密度区间[1188, 2901])与亚洲病毒祖先首次分化后,HBV/B5的合并发生在近1000年后。令人惊讶的是,根据景观感知地理模型,HBV/B5的祖先似乎首先通过快速的沿海路线传播到格陵兰岛,随后B5在西部进化和传播。贝叶斯天际线图分析表明,HBV/B5种群扩张大约发生在距今400年,这与新爱斯基摩图勒文化在整个北美北极地区分裂为更多样化和地域上不同的因纽特人群相吻合。

讨论

HBV/B5的起源和传播似乎与过去1000年内新爱斯基摩人(因纽特人)的迁移同时发生,进一步支持了HBV/宿主共同扩张假说,并阐明了宿主-病原体适应和平衡的概念。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6ee1/5581946/915c2ee8b4a6/peerj-05-3757-g001.jpg

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