蛋白质合成抑制剂对脑心肌炎病毒复制抑制作用的特异性
Specificity of protein synthesis inhibitors in the inhibition of encephalomyocarditis virus replication.
作者信息
Ramabhadran T V, Thach R E
出版信息
J Virol. 1980 Apr;34(1):293-6. doi: 10.1128/JVI.34.1.293-296.1980.
Abstract
Effect of protein synthesis inhibitors on encephalomyocarditis virus production in L-cells was studied. Inhibition of initiation by hypertonicity, harringtonine, or pactamycin decreased viral protein synthesis to a lesser extent than that of host. Virus yield was unaffected or actually enhanced by low concentrations of these inhibitors. On the contrary, the elongation inhibitors cycloheximide, anisomycin, and emetine, shown previously to inhibit viral protein synthesis preferentially, had a greater effect on virus yield than on overall protein synthesis. These results support our earlier proposal that the antiviral activity of cycloheximide derives from its specific effect on the rate of elongation of protein synthesis, and that elongation inhibitors in general may show varying degrees of specific antiviral activity.
摘要
研究了蛋白质合成抑制剂对L细胞中脑心肌炎病毒产生的影响。高渗、三尖杉酯碱或放线菌酮对起始的抑制作用,相比于宿主蛋白合成,对病毒蛋白合成的降低程度较小。低浓度的这些抑制剂对病毒产量没有影响,甚至实际上会使其增加。相反,先前显示能优先抑制病毒蛋白合成的延伸抑制剂环己酰亚胺、茴香霉素和吐根碱,对病毒产量的影响比对总蛋白合成的影响更大。这些结果支持了我们之前的观点,即环己酰亚胺的抗病毒活性源于其对蛋白质合成延伸速率的特定作用,并且一般来说延伸抑制剂可能会表现出不同程度的特定抗病毒活性。
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