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The 125th Lys and 145th Thr Amino Acids in the GTPase Domain of Goose Mx Confer Its Antiviral Activity against the Tembusu Virus

机译:GEOSE MX的GTPA酶结构域中的第125次LYS和145th THR氨基酸赋予Tembusu病毒的抗病毒活性

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摘要

The Tembusu virus (TMUV) is an avian pathogenic flavivirus that causes a highly contagious disease and catastrophic losses to the poultry industry. The myxovirus resistance protein (Mx) of innate immune effectors is a key antiviral “workhorse” of the interferon (IFN) system. Although mammalian Mx resistance against myxovirus and retrovirus was witnessed for decades, whether or not bird Mx has anti-flavivirus activity remains unknown. In this study, we found that the transcription of goose Mx (goMx) was obviously driven by TMUV infection, both in vivo and in vitro, and that the titers and copies of TMUV were significantly reduced by goMx overexpression. In both primary (goose embryo fibroblasts, GEFs) and passaged cells (baby hamster kidney cells, BHK21, and human fetal kidney cells, HEK 293T), it was shown that goMx was mainly located in the cytoplasm, and sporadically distributed in the nucleus. The intracellular localization of this protein is attributed to the predicted bipartite nuclear localization signal (NLS; 30 residues: the 441st–471st amino acids of goMx). Intuitively, it seems that the cells with a higher level of goMx expression tend to have lower TMUV loads in the cytoplasm, as determined by an immunofluorescence assay. To further explore the antiviral determinants, a panel of variants was constructed. Two amino acids at the 125th (Lys) and 145th (Thr) positions in GTP-binding elements, not in the L4 loop (40 residues: the 532nd–572nd amino acids of goMx), were vital for the antiviral function of goMx against TMUV in vitro. These findings will contribute to our understanding of the functional significance of the antiviral system in aquatic birds, and the development of goMx could be a valuable therapeutic agent against TMUV.
机译:Tembusu病毒(TMUV)是一种禽病原性黄病毒,导致对家禽行业的高度传染性疾病和灾难性损失。先天免疫效应器的肌瘤病毒抗性蛋白(MX)是干扰素(IFN)系统的关键抗病患者“摩托车”。尽管哺乳动物MX抗鼠尾病毒和逆转录病毒的抗性几十年来,但是否禽类MX具有抗黄病毒活性仍然未知。在这项研究中,我们发现鹅MX(GOMX)的转录显然是由体内和体内的TMUV感染的驱动,并且TMUV的滴度和拷贝通过GOMx过度表达显着降低。在主要(鹅胚胎成纤维细胞,GEF)和传代细胞(婴儿仓鼠肾细胞,BHK21和人胎儿肾细胞,HEK 293T)中,显示GOMX主要位于细胞质中,并在细胞核中分布在细胞核中。该蛋白质的细胞内定位归因于预测的二分核定位信号(NLS; 30个残基:441st-471st的GOMX)。直观地,似乎具有较高水平的GOMx表达水平的细胞倾向于细胞质中的TMUV载荷较低,如通过免疫荧光测定法测定。为了进一步探索抗病毒决定因素,构建了一种变体面板。在GTP结合元素的第125℃(Lys)和145(Thr)位置的两个氨基酸,不在L4环中(40个残基:GOMX的532nd-572nd氨基酸)对GOMX的抗病毒功能至关重要体外。这些发现将有助于了解抗病毒系统在水生鸟类的功能意义,并且GOMX的发展可能是针对TMUV的有价值的治疗剂。

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