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近期人类H3N2流感病毒的受体结合特异性

Receptor binding specificity of recent human H3N2 influenza viruses.

作者信息

Kumari Kshama, Gulati Shelly, Smith David F, Gulati Upma, Cummings Richard D, Air Gillian M

机构信息

Department of Biochemistry & Molecular Biology, University of Oklahoma Health Sciences Center, Oklahoma City, OK, USA.

出版信息

Virol J. 2007 May 9;4:42. doi: 10.1186/1743-422X-4-42.

Abstract

BACKGROUND

Human influenza viruses are known to bind to sialic acid linked alpha2-6 to galactose, but the binding specificity beyond that linkage has not been systematically examined. H3N2 human influenza isolates lost binding to chicken red cells in the 1990s but viruses isolated since 2003 have re-acquired the ability to agglutinate chicken erythrocytes. We have investigated specificity of binding, changes in hemagglutinin sequence of the recent viruses and the role of sialic acid in productive infection.

RESULTS

Viruses that agglutinate, or do not agglutinate, chicken red cells show identical binding to a Glycan Array of 264 oligosaccharides, binding exclusively to a subset of alpha2-6-sialylsaccharides. We identified an amino acid change in hemagglutinin that seemed to correlate with chicken red cell binding but when tested by mutagenesis there was no effect. Recombinant hemagglutinins expressed on Sf-9 cells bound chicken red cells but the released recombinant baculoviruses agglutinated only human red cells. Similarly, an isolate that does not agglutinate chicken red cells show hemadsorption of chicken red cells to infected MDCK cells. We suggest that binding of chicken red cells to cell surface hemagglutinin but not to virions is due to a more favorable hemagglutinin density on the cell surface. We investigated whether a virus specific for alpha2-6 sialyloligosaccharides shows differential entry into cells that have varying proportions of alpha2-6 and alpha2-3 sialic acids, including human A549 and HeLa cells with high levels of alpha2-6 sialic acid, and CHO cells that have only alpha2-3 sialic acid. We found that the virus enters all cell types tested and synthesizes viral nucleoprotein, localized in the nucleus, and hemagglutinin, transported to the cell surface, but infectious progeny viruses were released only from MDCK cells.

CONCLUSION

Agglutination of chicken red cells does not correlate with altered binding to any oligosaccharide on the Glycan Array, and may result from increased avidity due to density of hemagglutinin and not increased affinity. Absence of alpha2-6 sialic acid does not protect a cell from influenza infection and the presence of high levels of alpha2-6-sialic acids on a cell surface does not guarantee productive replication of a virus with alpha2-6 receptor specificity.

摘要

背景

已知人类流感病毒可与连接有α2-6连接的半乳糖的唾液酸结合,但超出该连接的结合特异性尚未得到系统研究。H3N2人类流感分离株在20世纪90年代失去了与鸡红细胞的结合能力,但自2003年以来分离出的病毒重新获得了凝集鸡红细胞的能力。我们研究了结合特异性、近期病毒血凝素序列的变化以及唾液酸在有效感染中的作用。

结果

凝集或不凝集鸡红细胞的病毒对包含264种寡糖的糖阵列显示出相同的结合,仅与α2-6-唾液酸糖的一个子集结合。我们在血凝素中鉴定出一个氨基酸变化,似乎与鸡红细胞结合相关,但经诱变测试后并无影响。在Sf-9细胞上表达的重组血凝素可结合鸡红细胞,但释放的重组杆状病毒仅凝集人类红细胞。同样,一株不凝集鸡红细胞的分离株在感染的MDCK细胞上显示出鸡红细胞的血细胞吸附现象。我们认为鸡红细胞与细胞表面血凝素而非病毒粒子的结合是由于细胞表面血凝素密度更有利。我们研究了对α2-6唾液酸寡糖具有特异性的病毒是否在具有不同比例α2-6和α2-3唾液酸的细胞中表现出不同的进入情况,包括具有高水平α2-6唾液酸的人类A549和HeLa细胞,以及仅具有α2-3唾液酸的CHO细胞。我们发现该病毒可进入所有测试的细胞类型,并合成位于细胞核中的病毒核蛋白以及转运至细胞表面的血凝素,但仅从MDCK细胞释放出有感染性的子代病毒。

结论

鸡红细胞的凝集与糖阵列上任何寡糖结合的改变无关,可能是由于血凝素密度导致的亲和力增加而非亲和力增强所致。缺乏α2-6唾液酸并不能保护细胞免受流感感染,细胞表面高水平的α2-6唾液酸的存在也不能保证具有α2-6受体特异性的病毒进行有效复制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/03f9/1876801/c772af3b5845/1743-422X-4-42-1.jpg

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