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与鸡蛋适应相关的唾液酸结合的变化可降低人鼻腔上皮细胞培养物中活减毒流感病毒的复制。

Changes in sialic acid binding associated with egg adaptation decrease live attenuated influenza virus replication in human nasal epithelial cell cultures.

机构信息

W. Harry Feinstone Department of Molecular Microbiology and Immunology, Johns Hopkins University Bloomberg School of Public Health, United States.

W. Harry Feinstone Department of Molecular Microbiology and Immunology, Johns Hopkins University Bloomberg School of Public Health, United States.

出版信息

Vaccine. 2021 Jun 2;39(24):3225-3235. doi: 10.1016/j.vaccine.2021.04.057. Epub 2021 May 11.

Abstract

Live Attenuated Influenza Virus (LAIV) is administered to and replicates in the sinonasal epithelium. Candidate LAIV vaccine strains are selected based on their ability to replicate to a high titer in embryonated hen's eggs, a process that can lead to mutations which alter the receptor binding and antigenic structure of the hemagglutinin (HA) protein. In the 2012-2013 northern hemisphere vaccine, the H3N2 HA vaccine strain contained three amino acid changes - H156Q, G186V and S219Y - which altered HA antigenic structure and thus presumably decreased vaccine efficacy. To determine if these mutations also altered LAIV replication, reabcombinant viruses were created that encoded the wild-type (WT) parental HA of A/Victoria/361/2011 (WT HA LAIV), the egg adapted HA (EA HA LAIV) from the A/Victoria/361/2011 vaccine strain and an HA protein with additional amino acid changes to promote α2,3 sialic acid binding (2,3 EA HA LAIV). The WT HA LAIV bound α2,6 sialic compared to the EA HA LAIV and 2,3 EA HA LAIV which both demonstrated an increased preference for α2,3 sialic acid. On MDCKs, the WT HA and EA HA LAIVs showed similar replication at 32 °C but at 37 °C the EA HA LAIV replicated to lower infectious virus titers. The 2,3 EA HA LAIV replicated poorly at both temperatures. This replication phenotype was similar on human nasal epithelial cell (hNEC) cultures, however the WT HA LAIV induced the highest amount of IFN-λ and infected more nasal epithelial cells compared to the other viruses. Together, these data indicate that egg adaption mutations in the HA protein that confer preferential α2,3 sialic acid binding may adversely affect LAIV replication and contribute to reduced vaccine efficacy.

摘要

减毒活流感病毒(LAIV)在鼻黏膜上皮细胞中进行复制。候选 LAIV 疫苗株是根据其在鸡胚中高滴度复制的能力来选择的,这一过程可能导致改变血凝素(HA)蛋白的受体结合和抗原结构的突变。在 2012-2013 年北半球疫苗中,H3N2 HA 疫苗株包含三个氨基酸变化 - H156Q、G186V 和 S219Y - 改变了 HA 抗原结构,因此推测降低了疫苗效力。为了确定这些突变是否也改变了 LAIV 的复制,创建了重新重组的病毒,这些病毒编码了 A/Victoria/361/2011 的野生型(WT)亲本 HA(WT HA LAIV)、来自 A/Victoria/361/2011 疫苗株的鸡蛋适应的 HA(EA HA LAIV)和具有促进α2,3 唾液酸结合的额外氨基酸变化的 HA 蛋白(2,3 EA HA LAIV)。WT HA LAIV 与 EA HA LAIV 和 2,3 EA HA LAIV 相比,结合了α2,6 唾液酸,而 EA HA LAIV 和 2,3 EA HA LAIV 都表现出对α2,3 唾液酸的偏好增加。在 MDCKs 上,WT HA 和 EA HA LAIV 在 32°C 时表现出相似的复制,但在 37°C 时,EA HA LAIV 复制到较低的感染性病毒滴度。2,3 EA HA LAIV 在两种温度下复制都很差。在人鼻上皮细胞(hNEC)培养物上,这种复制表型也相似,但与其他病毒相比,WT HA LAIV 诱导了最高量的 IFN-λ 和感染了更多的鼻上皮细胞。总的来说,这些数据表明,HA 蛋白中的鸡蛋适应突变赋予了对α2,3 唾液酸的优先结合,可能会对 LAIV 的复制产生不利影响,并导致疫苗效力降低。

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