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Antiviral Activity of Binase against the Pandemic Influenza A (H1N1) Virus

机译:Binase对大流行性流感A(H1N1)病毒的抗病毒活性

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摘要

The lack of effective antiviral drugs restricts the control of the dangerous RNA-containing influenza A (H1N1) virus. Extracellular ribonuclease of Bacilli (binase) was shown to manifest antiviral activity during single- and multi-cycle viral replication in the range of concentrations non-toxic to epithelial cells and 0.01-0.1 multiplicity of infection. During antiviral treatment for 15-30 min, the concentration of 1 μg/ml binase reduced the amount of focus-forming units of viruses by a factor of 3-10 and suppressed the virus-induced cytopathic effect in A549 human lung cells. The possible mechanisms of interaction between the virus and enzyme are discussed. Positive charges in both binase and viral hemagglutinin cause electrostatic interaction with negatively charged sialic acid on the host cell’s surface followed by its penetration into the cell. Capsid elimination and release of viral RNA from endosome to the cytoplasm allows catalytic RNA cleavage by internalized binase. The data obtained confirm that binase is an effective antiviral agent against the pandemic influenza A (H1N1) virus. Certain progress in this field is associated with clarifying the detailed mechanism underlying the antiviralaction of binase and development of the most effective way for its practicaluse.
机译:缺乏有效的抗病毒药物限制了对危险的含RNA的甲型H1N1流感病毒的控制。芽孢杆菌的胞外核糖核酸酶(binase)在单周期和多周期病毒复制过程中表现出抗病毒活性,在对上皮细胞无毒的浓度范围和0.01-0.1的感染复数范围内。在15到30分钟的抗病毒治疗期间,浓度为1μg/ ml的Binase将病毒的焦点形成单位数量减少了3-10倍,并抑制了病毒诱导的A549人肺细胞的细胞病变作用。讨论了病毒和酶之间相互作用的可能机制。 Binase和病毒血凝素中的正电荷会导致与宿主细胞表面带负电荷的唾液酸发生静电相互作用,然后渗透到细胞中。衣壳的消除和病毒核糖体从内体到细胞质的释放,可通过内部化的二合酶催化RNA裂解。获得的数据证实binase是一种有效的抗大流行性流感A(H1N1)病毒的抗病毒剂。该领域的某些进展与阐明抗病毒药物的详细机制有关Binase的作用及其发展的最有效方法采用。

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