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禽流感 A(H5Nx)病毒中的功能性神经氨酸酶抑制剂耐药性基序。

Functional neuraminidase inhibitor resistance motifs in avian influenza A(H5Nx) viruses.

机构信息

The Pirbright Institute, Pirbright, United Kingdom.

The Pirbright Institute, Pirbright, United Kingdom.

出版信息

Antiviral Res. 2020 Oct;182:104886. doi: 10.1016/j.antiviral.2020.104886. Epub 2020 Aug 1.

Abstract

Neuraminidase inhibitors (NAIs) are antiviral agents recommended worldwide to treat or prevent influenza virus infections in humans. Past influenza virus pandemics seeded by zoonotic infection by avian influenza viruses (AIV) as well as the increasing number of human infections with AIV have shown the importance of having information about resistance to NAIs by avian NAs that could cross the species barrier. In this study we introduced four NAI resistance-associated mutations (N2 numbering) previously found in human infections into the NA of three current AIV subtypes of the H5Nx genotype that threaten the poultry industry and human health: highly pathogenic H5N8, H5N6 and H5N2. Using the established MUNANA assay we showed that a R292K substitution in H5N6 and H5N2 viruses significantly reduced susceptibility to three licenced NAIs: oseltamivir, zanamivir and peramivir. In contrast the mutations E119V, H274Y and N294S had more variable effects with NAI susceptibility being drug- and strain-specific. We measured the replicative fitness of NAI resistant H5N6 viruses and found that they replicated to comparable or significantly higher titres in primary chicken cells and in embryonated hens' eggs as compared to wild type - despite the NA activity of the viral neuraminidase proteins being reduced. The R292K and N294S drug resistant H5N6 viruses had single amino acid substitutions in their haemagglutinin (HA): Y98F and A189T, respectively (H3 numbering) which reduced receptor binding properties possibly balancing the reduced NA activity seen. Our results demonstrate that the H5Nx viruses can support drug resistance mutations that confer reduced susceptibility to licenced NAIs and that these H5N6 viruses did not show diminished replicative fitness in avian cell cultures. Our results support the requirement for on-going surveillance of these strains in bird populations to include motifs associated with human drug resistance.

摘要

神经氨酸酶抑制剂(NAIs)是一种被全球推荐用于治疗或预防人类流感病毒感染的抗病毒药物。过去由禽流感病毒(AIV)的动物源性感染引发的流感病毒大流行,以及越来越多的人感染 AIV,都表明了解禽类 NA 对 NAI 的耐药性信息的重要性,这些信息可能会跨越物种屏障。在这项研究中,我们将之前在人类感染中发现的四个与 NAI 耐药相关的突变(N2 编号)引入到三种目前对家禽业和人类健康构成威胁的 H5Nx 基因型的 AIV 亚型的 NA 中:高致病性 H5N8、H5N6 和 H5N2。使用已建立的 MUNANA 测定法,我们表明 H5N6 和 H5N2 病毒中的 R292K 取代显著降低了对三种许可的 NAIs 的敏感性:奥司他韦、扎那米韦和帕拉米韦。相比之下,E119V、H274Y 和 N294S 的突变具有更可变的影响,NAI 敏感性因药物和菌株而异。我们测量了 NAI 耐药性 H5N6 病毒的复制适应性,发现与野生型相比,它们在原代鸡细胞和鸡胚卵中复制到相当或显著更高的滴度-尽管病毒神经氨酸酶蛋白的 NA 活性降低。具有 R292K 和 N294S 耐药性的 H5N6 病毒在其血凝素(HA)中具有单个氨基酸取代:Y98F 和 A189T,分别为(H3 编号),这降低了受体结合特性,可能平衡了所观察到的 NA 活性降低。我们的研究结果表明,H5Nx 病毒可以支持赋予对许可的 NAI 敏感性降低的耐药性突变,并且这些 H5N6 病毒在禽细胞培养物中没有显示出复制适应性降低。我们的研究结果支持需要对鸟类种群中这些菌株进行持续监测,包括与人类耐药性相关的基序。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/09ca/7534037/a1a6bc9231ca/gr1.jpg

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