近期出现的3C.3a和3C.2a亚分支甲型H3N2人流感病毒在MDCK细胞中传代后的特征及抗原特性

The characteristics and antigenic properties of recently emerged subclade 3C.3a and 3C.2a human influenza A(H3N2) viruses passaged in MDCK cells.

作者信息

Lin Yipu, Wharton Stephen A, Whittaker Lynne, Dai Mian, Ermetal Burcu, Lo Janice, Pontoriero Andrea, Baumeister Elsa, Daniels Rodney S, McCauley John W

机构信息

The Francis Crick Institute, London, UK.

Centre for Health Protection, Department of Health, Hong Kong Special Administrative Region, China.

出版信息

Influenza Other Respir Viruses. 2017 May;11(3):263-274. doi: 10.1111/irv.12447. Epub 2017 Feb 28.

DOI:10.1111/irv.12447

PMID:28164446

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5410720/

Abstract

BACKGROUND

Two new subclades of influenza A(H3N2) viruses became prominent during the 2014-2015 Northern Hemisphere influenza season. The HA glycoproteins of these viruses showed sequence changes previously associated with alterations in receptor-binding properties. To address how these changes influence virus propagation, viruses were isolated and propagated in conventional MDCK cells and MDCK-SIAT1 cells, cells with enhanced expression of the human receptor for the virus, and analysed at each passage.

METHODS

Gene sequence analysis was undertaken as virus was passaged in conventional MDCK cells and MDCK-SIAT1 cells. Alterations in receptor recognition associated with passage of virus were examined by haemagglutination assays using red blood cells from guinea pigs, turkeys and humans. Microneutralisation assays were performed to determine how passage-acquired amino acid substitutions and polymorphisms affected virus antigenicity.

RESULTS

Viruses were able to infect MDCK-SIAT1 cells more efficiently than conventional MDCK cells. Viruses of both the 3C.2a and 3C.3a subclades showed greater sequence change on passage in conventional MDCK cells than in MDCK-SIAT1 cells, with amino acid substitutions being seen in both HA and NA glycoproteins. However, virus passage in MDCK-SIAT1 cells at low inoculum dilutions showed reducing infectivity on continued passage.

CONCLUSIONS

Current H3N2 viruses should be cultured in the MDCK-SIAT1 cell line to maintain faithful replication of the virus, and at an appropriate multiplicity of infection to retain infectivity.

摘要

背景

在2014 - 2015年北半球流感季节期间，甲型（H3N2）流感病毒的两个新亚分支变得显著。这些病毒的血凝素（HA）糖蛋白显示出先前与受体结合特性改变相关的序列变化。为了研究这些变化如何影响病毒传播，病毒在传统的犬肾传代细胞（MDCK细胞）和犬肾传代 - 唾液酸α - 2,6 - 岩藻糖基转移酶1细胞（MDCK - SIAT1细胞，该细胞增强表达该病毒的人类受体）中分离和传代，并在每一代进行分析。

方法

当病毒在传统MDCK细胞和MDCK - SIAT1细胞中传代时进行基因序列分析。使用豚鼠、火鸡和人类的红细胞通过血凝试验检查与病毒传代相关的受体识别变化。进行微量中和试验以确定传代获得的氨基酸取代和多态性如何影响病毒抗原性。

结果

病毒感染MDCK - SIAT1细胞比感染传统MDCK细胞更有效。3C.2a和3C.3a亚分支的病毒在传统MDCK细胞中传代时比在MDCK - SIAT1细胞中显示出更大的序列变化，在HA和NA糖蛋白中均可见氨基酸取代。然而，在低接种物稀释度下于MDCK - SIAT1细胞中传代的病毒在连续传代时显示出感染性降低。

结论

当前的H3N2病毒应在MDCK - SIAT1细胞系中培养以维持病毒的忠实复制，并在适当的感染复数下以保持感染性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b45b/5410720/082869a14be5/IRV-11-263-g001.jpg

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