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Initiation of Vaccinia Virus Infection in Actinomycin D-pretreated Cells

机译:放线菌素D预处理细胞中牛痘病毒感染的起始

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摘要

The early steps in vaccinia virus infection were studied in HeLa cells which had been treated with actinomycin D (1 μg/ml) and then incubated for several hours in fresh medium prior to infection. Initiation of infection occurred in such cells even though the synthesis of cellular ribonucleic acid and deoxyribonucleic acid (DNA) was severely depressed. Thymidine kinase was synthesized in amounts that exceeded those found in untreated, infected cells. The breakdown of viral “cores” to liberate viral DNA and the synthesis of viral specific DNA-polymerase also occurred but were somewhat delayed. A deoxyribonuclease resembling an exonuclease was made by the infected, pretreated cells. The time course for these events suggested that the genetic code for synthesis of thymidine kinase can be expressed before “cores” are broken down, but the DNA-polymerase can be synthesized only after liberation of the viral DNA. The amount of viral specific DNA-polymerase which was made after infection was proportional to the total number of virus synthesizing sites even beyond the point where all the cells were infected with one infectious particle. A similar relationship was observed for the amount of thymidine kinase formed and for the rate of viral DNA synthesis from 3H-thymidine.
机译:在用放线菌素D(1μ​​g/ ml)处理过的HeLa细胞中研究了牛痘病毒感染的早期步骤,然后在感染前在新鲜培养基中孵育了几个小时。即使严重抑制了细胞核糖核酸和脱氧核糖核酸(DNA)的合成,感染仍会在此类细胞中发生。合成的胸苷激酶的量超过未处理的感染细胞中发现的量。释放病毒DNA的病毒“核心”的分解和病毒特异性DNA聚合酶的合成也发生了,但有所延迟。被感染的预处理细胞产生类似于核酸外切酶的脱氧核糖核酸酶。这些事件的时间进程表明,可以在“核心”被分解之前表达合成胸苷激酶的遗传密码,但是只有在释放病毒DNA后才能合成DNA聚合酶。感染后产生的病毒特异性DNA聚合酶的量与病毒合成位点的总数成比例,甚至超过所有细胞都被一个感染性颗粒感染的程度。从 3 H-胸腺嘧啶核苷形成的胸苷激酶的量和病毒DNA的合成速率也观察到类似的关系。

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