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首页> 外文期刊>Virulence >The non-structural (NS) gene segment of H9N2 influenza virus isolated from backyard poultry in Pakistan reveals strong genetic and functional similarities to the NS gene of highly pathogenic H5N1
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The non-structural (NS) gene segment of H9N2 influenza virus isolated from backyard poultry in Pakistan reveals strong genetic and functional similarities to the NS gene of highly pathogenic H5N1

机译:从巴基斯坦后院家禽中分​​离出的H9N2流感病毒的非结构(NS)基因片段显示出与高致病性H5N1的NS基因的强烈遗传和功能相似性

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摘要

Apart from natural reassortment, co-circulation of different avian influenza virus strains in poultry populations can lead to generation of novel variants and reassortant viruses. In this report, we studied the genetics and functions of a reassorted non-structural gene (NS) of H9N2 influenza virus collected from back yard poultry (BYP) flock. Phylogenetic reconstruction based on hemagglutinin and neuraminidase genes indicates that an isolate from BYP belongs to H9N2. However, the NS gene-segment of this isolate cluster into genotype Z, clade 2.2 of the highly pathogenic H5N1. The NS gene plays essential roles in the host-adaptation, cell-tropism, and virulence of influenza viruses. However, such interpretations have not been investigated in naturally recombinant H9N2 viruses. Therefore, we compared the NS1 protein of H9N2 (H9N2/NS1) and highly pathogenic H5N1 (H5N1/NS1) in parallel for their abilities to regulate different signaling pathways, and investigated the molecular mechanisms of IFN-β production in human, avian, and mink lung cells. We found that H9N2/NS1 and H5N1/NS1 are comparably similar in inhibiting TNF-α induced nuclear factor kB and double stranded RNA induced activator protein 1 and interferon regulatory factor 3 transcription factors. Thus, the production of IFN-β was inhibited equally by both NS1s as demonstrated by IFN stimulatory response element and IFN-β promoter activation. Moreover, both NS1s predominantly localized in the nucleus when transfected to human A549 cells. This study therefore suggests the possible increased virulence of natural reassortant viruses for their efficient invasion of host immune responses, and proposes that these should not be overlooked for their epizootic and zoonotic potential.
机译:除了自然重组外,家禽种群中不同禽流感病毒株的共同流通还可以导致产生新的变异和重组病毒。在本报告中,我们研究了从后院家禽(BYP)群收集的H9N2流感病毒的重组非结构基因(NS)的遗传学和功能。基于血凝素和神经氨酸酶基因的系统发育重建表明,来自BYP的分离物属于H9N2。但是,此分离株的NS基因片段聚集成基因型Z,即高致病性H5N1的进化枝2.2。 NS基因在流感病毒的宿主适应性,细胞嗜性和毒力中起重要作用。但是,尚未在天然重组H9N2病毒中研究此类解释。因此,我们并行比较了H9N2(H9N2 / NS1)和高致病性H5N1(H5N1 / NS1)的NS1蛋白调节不同信号通路的能力,并研究了人,禽和人体内IFN-β产生的分子机制。水貂肺细胞。我们发现H9N2 / NS1和H5N1 / NS1在抑制TNF-α诱导的核因子kB和双链RNA诱导的激活蛋白1和干扰素调节因子3转录因子方面具有相似的相似性。因此,如IFN刺激反应元件和IFN-β启动子激活所证明的,NS1均对IFN-β的产生同样地抑制。此外,两个NS1s在转染到人A549细胞后都主要位于细胞核中。因此,这项研究表明,自然重配病毒可能会增加其有效入侵宿主免疫反应的毒力,并建议不应因其流行和人畜共患病潜力而忽视这些病毒。

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