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Adaptive evolution influences the infectious dose of MERS-CoV necessary to achieve severe respiratory disease

机译:自适应进化影响了实现严重呼吸道疾病所必需的MERS-COV的传染性剂量

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We recently established a mouse model (288-330(+/+)) that developed acute respiratory disease resembling human pathology following infection with a high dose (5 x 10(6) PFU) of mouse-adapted MERS-CoV (icMERSmal). Although this high dose conferred fatal respiratory disease in mice, achieving similar pathology at lower viral doses may more closely reflect naturally acquired infections. Through continued adaptive evolution of icMERSmal we generated a novel mouse-adapted MERS-CoV (maM35c4) capable of achieving severe respiratory disease at doses between 10(3) and 10(5) PFU. Novel mutations were identified in the maM35c4 genome that may be responsible for eliciting etiologies of acute respiratory distress syndrome at 10-1000 fold lower viral doses. Importantly, comparative genetics of the two mouse-adapted MERS strains allowed us to identify specific mutations that remained fixed through an additional 20 cycles of adaptive evolution. Our data indicate that the extent of MERS-CoV adaptation determines the minimal infectious dose required to achieve severe respiratory disease.
机译:我们最近建立了一种小鼠模型(288-330(+ / +)),其发育了在用高剂量(5×10(6)PFU)的小鼠适应的MERS-COV(Icmersmal)感染后类似人体病理学的急性呼吸系统疾病。虽然这种高剂量赋予小鼠的致命呼吸道疾病,但在较低的病毒剂量下实现了类似的病理可能更紧密地反映自然所获得的感染。通过Icmersmal的持续适应性演进,我们产生了一种新的小鼠适应的MERS-COV(MAM35C4),其能够在10(3)和10(5)个PFU之间的剂量以含量为严重的呼吸道疾病。在MAM35C4基因组中鉴定了新的突变,其负责以10-1000倍的病毒剂量引起急性呼吸窘迫综合征的引发病因。重要的是,两种小鼠适应的MERS菌株的比较遗传措施使我们能够鉴定通过另外20个适应性进化循环固定的特定突变。我们的数据表明MERS-COV适应的程度决定了实现严重呼吸道疾病所需的最小传染剂。

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