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High-Throughput MicroRNA Profiles of Permissive Madin-Darby Canine Kidney Cell Line Infected with Influenza B Viruses

机译:允许的Madin-Darby犬肾脏细胞系感染B型流感病毒的高通量MicroRNA谱

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摘要

Victoria and Yamagata lineages of influenza B viruses are globally circulating in seasonal epidemics. Madin–Darby canine kidney (MDCK) cells are permissive for viral isolation and vaccine manufacture. Nevertheless, the interplay between influenza B viruses and host microRNAs has not been investigated in this cell line. Therefore, the present study aims at high-throughput analysis of canine microRNA profile upon infection of influenza B viruses. Briefly, MDCK cells were infected with Victoria or Yamagata lineage at MOI of 0.01. After being harvested at 6, 12 and 24 h post infection, microRNAs were subjected to high-throughput sequencing based on MiSeq platform (Illumina). The results demonstrated that five microRNAs including cfa-miR-197, cfa-miR-215, cfa-miR361, cfa-miR-1841, and cfa-miR-1842 were overexpressed in both Victoria and Yamagata lineage infections. Interestingly, computational prediction showed that karyopherin alpha 6 (KPNA6) was targeted by cfa-miR-197 and cfa-miR-215. Moreover, the binding sites of both microRNAs were assessed by 3′-UTR reporter assay. The results showed that only cfa-miR-197 could bind to the target sites of KPNA6, leading to suppressing luciferase activity. Additionally, silencing of KPNA6 was confirmed by overexpression of cfa-miR-197. This study provides canine microRNA responses to seasonal influenza B viruses, suggesting that virus-mediated microRNAs might play crucial roles in host gene regulation.
机译:乙型流感病毒的维多利亚和山形血统在全球季节性流行。 Madin–Darby犬肾(MDCK)细胞可用于病毒分离和疫苗生产。然而,尚未在该细胞系中研究B型流感病毒与宿主microRNA之间的相互作用。因此,本研究旨在针对乙型流感病毒感染后的犬microRNA谱进行高通量分析。简而言之,MDCK细胞以MOI为0.01感染了Victoria或Yamagata谱系。在感染后6、12和24 h收获microRNA后,对它们进行基于MiSeq平台(Illumina)的高通量测序。结果表明,五个小RNA,包括cfa-miR-197,cfa-miR-215,cfa-miR361,cfa-miR-1841和cfa-miR-1842在维多利亚和山形世系感染中均过表达。有趣的是,计算预测表明,核转运蛋白α6(KPNA6)被cfa-miR-197和cfa-miR-215靶向。此外,通过3'-UTR报告基因分析评估了两个microRNA的结合位点。结果表明,仅cfa-miR-197可以与KPNA6的靶位点结合,从而抑制萤光素酶活性。另外,通过过度表达cfa-miR-197证实了KPNA6的沉默。这项研究提供了犬对季节性B型流感病毒的microRNA反应,表明病毒介导的microRNA可能在宿主基因调控中起关键作用。

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