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Small molecule inhibitors of ER α-glucosidases are active against multiple hemorrhagic fever viruses

机译:ERα-葡萄糖苷酶的小分子抑制剂可对抗多种出血热病毒

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Host cellular endoplasmic reticulum α-glucosidases I and II are essential for the maturation of viral glycosylated envelope proteins that use the calnexin mediated folding pathway. Inhibition of these glycan processing enzymes leads to the misfolding and degradation of these viral glycoproteins and subsequent reduction in virion secretion. We previously reported that, CM-10-18, an imino sugar α-glucosidase inhibitor, efficiently protected the lethality of dengue virus infection of mice. In the current study, through an extensive structure-activity relationship study, we have identified three CM-10-18 derivatives that demonstrated superior in vitro antiviral activity against representative viruses from four viral families causing hemorrhagic fever. Moreover, the three novel imino sugars significantly reduced the mortality of two of the most pathogenic hemorrhagic fever viruses, Marburg virus and Ebola virus, in mice. Our study thus proves the concept that imino sugars are promising drug candidates for the management of viral hemorrhagic fever caused by variety of viruses.
机译:宿主细胞内质网α-葡萄糖苷酶I和II对于使用钙调蛋白介导的折叠途径的病毒糖基化包膜蛋白的成熟至关重要。这些聚糖加工酶的抑制导致这些病毒糖蛋白的错误折叠和降解以及随后病毒体分泌的减少。我们以前曾报道过,亚氨基糖α-葡萄糖苷酶抑制剂CM-10-18有效地保护了小鼠感染登革热病毒的致死性。在当前的研究中,通过广泛的构效关系研究,我们确定了三种CM-10-18衍生物,它们对来自引起出血热的四个病毒家族的代表性病毒表现出优异的体外抗病毒活性。此外,三种新型亚氨基糖显着降低了小鼠中两种最具致病性的出血热病毒马尔堡病毒和埃博拉病毒的死亡率。因此,我们的研究证明了亚氨基糖是用于管理由多种病毒引起的病毒性出血热的有前途的候选药物的概念。

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