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A Polymorphism in the Hemagglutinin of the Human Isolate of a Highly Pathogenic H5N1 Influenza Virus Determines Organ Tropism in Mice

机译:高致病性H5N1流感病毒人类分离株的血凝素的多态性确定小鼠的器官趋向。

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摘要

We characterized a human H5N1 virus isolate (KAN-1) encoding a hemagglutinin (HA) with a K-to-E substitution at amino acid position 222 that was previously described to be selected in the lung of the infected patient. In mice, the growth of the HA222E-encoding virus was mainly confined to the lung, but reversion to 222K allowed virus to spread to the brain. The HA222E variant showed an overall reduced binding affinity compared to that of HA222K for synthetic Neu5Ac2-3Gal-terminated receptor analogues, except for one analogue [Neu5Acα2-3Galβ1-4(Fucα1-3)(6-HSO3)GlcNAcβ, Su-SLex]. Our results suggest that human-derived mutations in HA of H5N1 viruses can affect viral replication efficiency and organ tropism.
机译:我们表征了人类H5N1病毒分离株(KAN-1),其编码血凝素(HA)在氨基酸位置222处被K-E取代,该位置先前已描述为在感染患者的肺中被选择。在小鼠中,编码HA222E的病毒的生长主要限于肺部,但恢复到222K可使病毒传播到大脑。与HA222K相比,HA222E变异体对合成Neu5Ac2-3Gal终止的受体类似物的结合亲和力总体降低,除了一种类似物[Neu5Acα2-3Galβ1-4(Fucα1-3)(6-HSO3)GlcNAcβ,Su-SLe < sup> x ]。我们的结果表明,H5N1病毒的HA中人源性突变可影响病毒复制效率和器官嗜性。

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