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首页> 外文期刊>Virology >Binding of influenza viruses to sialic acids: reassortant viruses with A/NWS/33 hemagglutinin bind to alpha2,8-linked sialic acid.
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Binding of influenza viruses to sialic acids: reassortant viruses with A/NWS/33 hemagglutinin bind to alpha2,8-linked sialic acid.

机译:流感病毒与唾液酸的结合:具有A / NWS / 33血凝素的重组病毒与α2,8连接的唾液酸结合。

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摘要

We have examined the specificity of binding of A/NWS/33 hemagglutinin (HA), exploring the effects of fucosylation, changing the Gal-GlcNAc linkage between the second and third sugars, and binding affinity for alpha2,8-linked sialic acid. The HA of A/NWS/33(HA)-Tokyo/67(NA) (NWS-Tok, H1N2) virus binds to 3'-linked sialyllactose with 10-fold higher affinity than 3' sialyllactosamine and 3-fold higher affinity than 6' sialyllactosamine. The P227H mutation in A/NWS/33(P227H)(HA)-A/Memphis/31/98(NA) (NWS-Mem/98, H1N2) results in sevenfold lower affinity for 3' sialyllactose, but binding to 6' sialyllactosamine is unchanged. The apparent switch from 3' to 6' specificity is solely due to a loss of Siaalpha2,3 binding. Fucosylation of the third sugar and changing the linkage between second and third sugars had little effect on binding by NWS-Tok, but marked effects on A/NWS/33(P227H)(HA)-tern/Australia/G70c/75(NA) (NWS-G70c, H1N9) and NWS-Mem/98. NWS-Tok, NWS-G70c, and NWS-Mem/98 bind to alpha2,8-bisialic acidwith high affinity. NWS-Mem/98 can also bind to alpha2,8-trisialic acid, but with lower affinity. Together, these data show that alpha2,8-linked sialic acid, fucosylation of the third sugar, and linkage between the second and third sugars could play important roles in allowing efficient virus binding to its host cell. The finding that influenza viruses have the potential to bind to alpha2,8-linked sialic acid is a new influenza virus-receptor interaction pathway.
机译:我们已经检查了结合A / NWS / 33血凝素(HA)的特异性,探索岩藻糖基化的影响,改变了第二个和第三个糖之间的Gal-GlcNAc键,以及对α2,8-连接的唾液酸的结合亲和力。 A / NWS / 33(HA)-Tokyo / 67(NA)(NWS-Tok,H1N2)病毒的HA结合3'-连接的唾液乳糖的亲和力比3'唾液酸乳糖胺高10倍,亲和力比3' 6'唾液酸乳糖胺。 A / NWS / 33(P227H)(HA)-A / Memphis / 31/98(NA)(NWS-Mem / 98,H1N2)中的P227H突变导致对3'唾液乳糖的亲和力降低了七倍,但与6'结合唾液酸乳糖胺未改变。从3'到6'特异性的明显转变完全是由于Siaalpha2,3结合的丧失。第三糖的岩藻糖基化和改变第二糖和第三糖之间的键合对NWS-Tok的结合影响很小,但对A / NWS / 33(P227H)(HA)-tern / Australia / G70c / 75(NA)的影响明显(NWS-G70c,H1N9)和NWS-Mem / 98。 NWS-Tok,NWS-G70c和NWS-Mem / 98以高亲和力与alpha2,8-bisialic acid结合。 NWS-Mem / 98也可以与α2,8-三唾液酸结合,但亲和力较低。这些数据加在一起表明,α2,8连接的唾液酸,第三个糖的岩藻糖基化以及第二个和第三个糖之间的连接在允许病毒有效结合其宿主细胞方面可能起重要作用。流感病毒可能与α2,8连接的唾液酸结合的发现是一种新型的流感病毒-受体相互作用途径。

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