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人H3N2流感病毒重配对于美国2017 - 18年流感季流感发病率和严重程度的影响:一项回顾性观察基因组分析。

Effect of human H3N2 influenza virus reassortment on influenza incidence and severity during the 2017-18 influenza season in the USA: a retrospective observational genomic analysis.

作者信息

Liu Hsuan, Shaw-Saliba Kathryn, Westerbeck Jason, Jacobs David, Fenstermacher Katherine, Chao Chia-Yu, Gong Yu-Nong, Powell Harrison, Ma Zexu, Mehoke Thomas, Ernlund Amanda W, Dziedzic Amanda, Vyas Siddhant, Evans Jared, Sauer Lauren M, Wu Chin-Chieh, Chen Shu-Hui, Rothman Richard E, Thielen Peter, Chen Kuan-Fu, Pekosz Andrew

机构信息

W Harry Feinstone Department of Molecular Microbiology and Immunology, Johns Hopkins Bloomberg School of Public Health, Baltimore, MD, USA.

Department of Emergency Medicine, Johns Hopkins University School of Medicine, Baltimore, MD, USA.

出版信息

Lancet Microbe. 2024 Aug;5(8):100852. doi: 10.1016/S2666-5247(24)00067-3. Epub 2024 May 8.

Abstract

BACKGROUND

During the 2017-18 influenza season in the USA, there was a high incidence of influenza illness and mortality. However, no apparent antigenic change was identified in the dominant H3N2 viruses, and the severity of the season could not be solely attributed to a vaccine mismatch. We aimed to investigate whether the altered virus properties resulting from gene reassortment were underlying causes of the increased case number and disease severity associated with the 2017-18 influenza season.

METHODS

Samples included were collected from patients with influenza who were prospectively recruited during the 2016-17 and 2017-18 influenza seasons at the Johns Hopkins Hospital Emergency Departments in Baltimore, MD, USA, as well as from archived samples from Johns Hopkins Health System sites. Among 647 recruited patients with influenza A virus infection, 411 patients with whole-genome sequences were available in the Johns Hopkins Center of Excellence for Influenza Research and Surveillance network during the 2016-17 and 2017-18 seasons. Phylogenetic trees were constructed based on viral whole-genome sequences. Representative viral isolates of the two seasons were characterised in immortalised cell lines and human nasal epithelial cell cultures, and patients' demographic data and clinical outcomes were analysed.

FINDINGS

Unique H3N2 reassortment events were observed, resulting in two predominant strains in the 2017-18 season: HA clade 3C.2a2 and clade 3C.3a, which had novel gene segment constellations containing gene segments from HA clade 3C.2a1 viruses. The reassortant re3C.2a2 viruses replicated with faster kinetics and to a higher peak titre compared with the parental 3C.2a2 and 3C.2a1 viruses (48 h vs 72 h). Furthermore, patients infected with reassortant 3C.2a2 viruses had higher Influenza Severity Scores than patients infected with the parental 3C.2a2 viruses (median 3·00 [IQR 1·00-4·00] vs 1·50 [1·00-2·00]; p=0·018).

INTERPRETATION

Our findings suggest that the increased severity of the 2017-18 influenza season was due in part to two intrasubtypes, cocirculating H3N2 reassortant viruses with fitness advantages over the parental viruses. This information could help inform future vaccine development and public health policies.

FUNDING

The Center of Excellence for Influenza Research and Response in the US, National Science and Technology Council, and Chang Gung Memorial Hospital in Taiwan.

摘要

背景

在美国2017 - 18年流感季节,流感疾病发病率和死亡率很高。然而,在占主导地位的H3N2病毒中未发现明显的抗原变化,且该季节的严重程度不能完全归因于疫苗不匹配。我们旨在调查基因重配导致的病毒特性改变是否是2017 - 18年流感季节病例数增加和疾病严重程度增加的根本原因。

方法

纳入的样本收集自2016 - 17年和2017 - 18年流感季节在美国马里兰州巴尔的摩市约翰霍普金斯医院急诊科前瞻性招募的流感患者,以及约翰霍普金斯健康系统各站点的存档样本。在647名招募的甲型流感病毒感染患者中,2016 - 17年和2017 - 18年期间约翰霍普金斯流感研究与监测卓越中心网络中有411名患者有全基因组序列。基于病毒全基因组序列构建系统发育树。对两个季节的代表性病毒分离株在永生化细胞系和人鼻上皮细胞培养物中进行特性分析,并分析患者的人口统计学数据和临床结局。

研究结果

观察到独特的H3N2重配事件,在2017 - 18年季节产生了两种主要毒株:HA进化枝3C.2a2和3C.3a,它们具有新的基因片段组合,包含来自HA进化枝3C.2a1病毒的基因片段。与亲本3C.2a2和3C.2a1病毒相比,重配的re3C.2a2病毒复制动力学更快,峰值滴度更高(48小时对72小时)。此外,感染重配3C.2a2病毒的患者的流感严重程度评分高于感染亲本3C.2a2病毒的患者(中位数3.00 [四分位间距1.00 - 4.00]对1.50 [1.00 - 2.00];p = 0.018)。

解读

我们的研究结果表明,2017 - 18年流感季节严重程度增加部分归因于两种亚型内共同流行的H3N2重配病毒,它们比亲本病毒具有适应性优势。这些信息有助于为未来的疫苗开发和公共卫生政策提供参考。

资金来源

美国流感研究与应对卓越中心、国家科学技术委员会以及台湾长庚纪念医院。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11b1/11338072/7a7f4437ecb2/nihms-2015082-f0001.jpg

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