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首页> 外文期刊>Viruses >The PB2 Polymerase Host Adaptation Substitutions Prime Avian Indonesia Sub Clade 2.1 H5N1 Viruses for Infecting Humans
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The PB2 Polymerase Host Adaptation Substitutions Prime Avian Indonesia Sub Clade 2.1 H5N1 Viruses for Infecting Humans

机译:PB2聚合酶宿主适应性替代原代禽鸟亚进化枝2.1 H5N1病毒感染人类。

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Significantly higher numbers of human infections with H5N1 virus have occurred in Indonesia and Egypt, compared with other affected areas, and it is speculated that there are specific viral factors for human infection with avian H5N1 viruses in these locations. We previously showed PB2-K526R is present in 80% of Indonesian H5N1 human isolates, which lack the more common PB2-E627K substitution. Testing the hypothesis that this mutation may prime avian H5N1 virus for human infection, we showed that: (1) K526R is rarely found in avian influenza viruses but was identified in H5N1 viruses 2–3 years after the virus emerged in Indonesia, coincident with the emergence of H5N1 human infections in Indonesia; (2) K526R is required for efficient replication of Indonesia H5N1 virus in mammalian cells in vitro and in vivo and reverse substitution to 526K in human isolates abolishes this ability; (3) Indonesian H5N1 virus, which contains K526R-PB2, is stable and does not further acquire E627K following replication in infected mice; and (4) virus containing K526R-PB2 shows no fitness deficit in avian species. These findings illustrate an important mechanism in which a host adaptive mutation that predisposes avian H5N1 virus towards infecting humans has arisen with the virus becoming prevalent in avian species prior to human infections occurring. A similar mechanism is observed in the Qinghai-lineage H5N1 viruses that have caused many human cases in Egypt; here, E627K predisposes towards human infections. Surveillance should focus on the detection of adaptation markers in avian strains that prime for human infection.
机译:与其他受影响地区相比,印度尼西亚和埃及的人类感染H5N1病毒的人数明显增加,据推测在这些地区存在人类感染禽类H5N1病毒的特定病毒因素。我们先前显示,PB2-K526R存在于80%的印度尼西亚H5N1人类分离株中,它们缺乏更常见的PB2-E627K取代。通过检验该突变可能引发禽H5N1病毒引起人类感染的假说,我们发现:(1)K526R在禽流感病毒中很少发现,但在印尼出现这种病毒后2-3年在H5N1病毒中被发现,与印度尼西亚出现H5N1型人类感染; (2)K526R是印度尼西亚H5N1病毒在哺乳动物细胞内和体外有效复制所必需的,而在人类分离株中反向替换为526K消除了这种能力; (3)含有K526R-PB2的印度尼西亚H5N1病毒稳定,在感染小鼠中复制后不再获得E627K; (4)含K526R-PB2的病毒在禽类中无适应能力缺陷。这些发现说明了一种重要的机制,其中出现了使禽类H5N1病毒易于感染人类的​​宿主适应性突变,该病毒在人类感染发生前已在禽类中流行。在青海谱系的H5N1病毒中观察到了类似的机制,该病毒在埃及引起了许多人类病例。在这里,E627K容易感染人类。监测应集中在检测主要感染人类的​​禽流感病毒株中的适应性标志物上。

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