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宿主介导的流感病毒受体变体选择。A/鸭/乌克兰/1/63的唾液酸-α2,6半乳糖特异性克隆在鸡胚中回复为唾液酸-α2,3半乳糖特异性野生型。

Host-mediated selection of influenza virus receptor variants. Sialic acid-alpha 2,6Gal-specific clones of A/duck/Ukraine/1/63 revert to sialic acid-alpha 2,3Gal-specific wild type in ovo.

作者信息

Rogers G N, Daniels R S, Skehel J J, Wiley D C, Wang X F, Higa H H, Paulson J C

出版信息

J Biol Chem. 1985 Jun 25;260(12):7362-7.

PMID:3997874
Abstract

Human and animal influenza A isolates of the H3 serotype preferentially bind SA alpha 2,6Gal or SA alpha 2,3Gal linkages (where SA represents sialic acid), respectively, on cell-surface sialyloligosaccharides. Previously, we have demonstrated selection of SA alpha 2,3Gal-specific receptor variants of several human viruses which differed from the parent viruses by a single amino acid at residue 226 of the hemagglutinin which is located in the receptor binding pocket (Rogers, G. N., Paulson, J.C., Daniels, R.S., Skehel, J.J., Wilson, I.A., and Wiley, D.C. (1983) Nature 304, 76-78). In this report, the selection in the reverse direction was accomplished starting with a SA alpha 2,3Gal-specific avian virus, A/duck/Ukraine/1/63 (H3N7), yielding SA alpha 2,6Gal-specific variants that exhibit the receptor binding properties characteristic of the human isolates. Selection was again mediated at residue 226 of the hemagglutinin, in this case changing from Gln in the parent virus to Leu in the variants. Although the SA alpha 2,6Gal-specific avian virus variants were stable to passage in MDCK cells, they exhibited dramatic reversion to the SA alpha 2,3Gal-specific phenotype of the parent virus during a single passage in chicken embryos. This was in contrast to the SA alpha 2,6Gal-specific human virus isolates which were stable to passage in both hosts. The reversion of the avian virus variants in eggs provides compelling evidence for host-mediated selection of influenza virus receptor variants.

摘要

H3血清型的人类和动物甲型流感病毒分离株分别优先结合细胞表面唾液酸寡糖上的SAα2,6Gal或SAα2,3Gal连接(其中SA代表唾液酸)。此前,我们已证明几种人类病毒的SAα2,3Gal特异性受体变体的选择,这些变体与亲本病毒在血凝素位于受体结合口袋的第226位残基处仅有一个氨基酸不同(罗杰斯,G.N.,保尔森,J.C.,丹尼尔斯,R.S.,斯凯尔,J.J.,威尔逊,I.A.,和威利,D.C.(1983年)《自然》304,76 - 78)。在本报告中,反向选择是从一种SAα2,3Gal特异性禽病毒A/鸭/乌克兰/1/63(H3N7)开始实现的,产生了具有人类分离株特征性受体结合特性的SAα2,6Gal特异性变体。选择同样在血凝素的第226位残基处介导,在这种情况下,从亲本病毒中的谷氨酰胺变为变体中的亮氨酸。尽管SAα2,6Gal特异性禽病毒变体在MDCK细胞传代时稳定,但它们在鸡胚单次传代期间显著回复为亲本病毒的SAα2,3Gal特异性表型。这与在两种宿主中传代均稳定的SAα2,6Gal特异性人类病毒分离株形成对比。禽病毒变体在鸡蛋中的回复为宿主介导的流感病毒受体变体选择提供了有力证据。

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