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Functional Match between Influenza Virus Hemagglutinin and Neuraminidase Is Restored after Gene Reassortment

机译:基因重组后,流感病毒血凝素和神经氨酸酶之间的功能匹配得以恢复。

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摘要

Influenza virus A(FluA) reassortants with low-functional neuraminidase (NA) of subtype N1 and hemagglutinin (HA) of subtypes H2, H3, H4, and H13 display virion aggregation and accumulate to a lower titer because sialyl residues are not completely removed from virion components. Nonaggregating variants of FluA (H13N1) were shown to result from a mutation that reduces the HA affinity for sialyl substrates. Amino acid substitution K156E, which increases a negative charge at the edge of the receptor-binding pocket of HA large subunit (HA1), was revealed in two independent variants. This substitution was the only difference between HA1 of the original reassortant and one of its variants and, therefore, accounted for restoration of the functional match between HA and NA.
机译:具有亚型N1的低功能神经氨酸酶(NA)和亚型H2,H3,H4和H13的血凝素(HA)的甲型流感病毒(FluA)重排子显示病毒体聚集并且由于未从唾液酸残基中完全去除唾液酸残基而使其聚集度较低病毒体成分。 FluA(H13N1)的非聚集变体显示是由降低HA对唾液酸底物亲和力的突变产生的。在两个独立的变体中揭示了氨基酸取代K156E,它增加了HA大亚基(HA1)的受体结合袋边缘的负电荷。该取代是原始重配体的HA1与其变体之一之间的唯一区别,因此可解释为HA和NA之间功能匹配的恢复。

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