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系统发生基因组分析揭示了世卫组织推荐疫苗株和其他非洲株中 9 年来乌干达甲型流感病毒株的变异情况。

Phylogenomic analysis uncovers a 9-year variation of Uganda influenza type-A strains from the WHO-recommended vaccines and other Africa strains.

机构信息

Department of Immunology and Molecular Biology, Makerere University, Kampala, Uganda.

Makerere University/UVRI Centre of Excellence in Infection and Immunity Research and Training (MUII-Plus), Uganda Virus Research Institute (UVRI), Entebbe, Uganda.

出版信息

Sci Rep. 2023 Apr 4;13(1):5516. doi: 10.1038/s41598-023-30667-z.

Abstract

Genetic characterisation of circulating influenza viruses directs annual vaccine strain selection and mitigation of infection spread. We used next-generation sequencing to locally generate whole genomes from 116 A(H1N1)pdm09 and 118 A(H3N2) positive patient swabs collected across Uganda between 2010 and 2018. We recovered sequences from 92% (215/234) of the swabs, 90% (193/215) of which were whole genomes. The newly-generated sequences were genetically and phylogenetically compared to the WHO-recommended vaccines and other Africa strains sampled since 1994. Uganda strain hemagglutinin (n = 206), neuraminidase (n = 207), and matrix protein (MP, n = 213) sequences had 95.23-99.65%, 95.31-99.79%, and 95.46-100% amino acid similarity to the 2010-2020 season vaccines, respectively, with several mutated hemagglutinin antigenic, receptor binding, and N-linked glycosylation sites. Uganda influenza type-A virus strains sequenced before 2016 clustered uniquely while later strains mixed with other Africa and global strains. We are the first to report novel A(H1N1)pdm09 subclades 6B.1A.3, 6B.1A.5(a,b), and 6B.1A.6 (± T120A) that circulated in Eastern, Western, and Southern Africa in 2017-2019. Africa forms part of the global influenza ecology with high viral genetic diversity, progressive antigenic drift, and local transmissions. For a continent with inadequate health resources and where social distancing is unsustainable, vaccination is the best option. Hence, African stakeholders should prioritise routine genome sequencing and analysis to direct vaccine selection and virus control.

摘要

对循环流感病毒的遗传特征分析指导了每年的疫苗株选择和感染传播的缓解。我们使用下一代测序技术,从 2010 年至 2018 年期间在乌干达各地采集的 116 份 A(H1N1)pdm09 和 118 份 A(H3N2)阳性患者拭子中,局部生成了全基因组。我们从 92%(215/234)的拭子中恢复了序列,其中 90%(193/215)为全基因组序列。新生成的序列与世界卫生组织推荐的疫苗以及自 1994 年以来在非洲采集的其他毒株进行了遗传和系统发育比较。乌干达毒株血凝素(n=206)、神经氨酸酶(n=207)和基质蛋白(MP,n=213)序列与 2010-2020 季节疫苗的氨基酸相似性分别为 95.23-99.65%、95.31-99.79%和 95.46-100%,具有几个突变的血凝素抗原、受体结合和 N-糖基化位点。2016 年之前测序的乌干达甲型流感病毒株独特聚集,而后来的病毒株与其他非洲和全球毒株混合。我们首次报告了新型 A(H1N1)pdm09 亚系 6B.1A.3、6B.1A.5(a,b)和 6B.1A.6(±T120A),这些亚系于 2017-2019 年在东非、西非和南非流行。非洲是全球流感生态系统的一部分,具有高度的病毒遗传多样性、渐进性抗原漂移和本地传播。对于一个卫生资源不足且无法实施社交距离的大陆来说,接种疫苗是最佳选择。因此,非洲利益相关者应优先进行常规基因组测序和分析,以指导疫苗选择和病毒控制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fcd4/10073182/ed45f8374672/41598_2023_30667_Fig1_HTML.jpg

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