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Uncoupling ribosome biogenesis regulation from RNA polymerase I activity during herpes simplex virus type 1 infection.

机译:在单纯疱疹病毒1型感染期间,RNA聚合酶I活性与核糖体生物发生调控脱钩。

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摘要

The ribosome is the central effector of protein synthesis, and its synthesis is intimately coordinated with that of proteins. At present, the most documented way to modulate ribosome biogenesis involves control of rDNA transcription by RNA polymerase I (RNA Pol I). Here we show that after infection of human cells with herpes simplex virus type 1 (HSV-1) the rate of ribosome biogenesis is modulated independently of RNA Pol I activity by a dramatic change in the rRNA maturation pathway. This process permits control of the ribosome biogenesis rate, giving the possibility of escaping ribosomal stress and eventually allowing assembly of specialized kinds of ribosomes.
机译:核糖体是蛋白质合成的主要效应物,其合成与蛋白质密切相关。目前,最有据可查的调节核糖体生物发生的方法涉及通过RNA聚合酶I(RNA Pol I)控制rDNA转录。在这里,我们显示在人类细胞感染单纯疱疹病毒1型(HSV-1)后,核糖体生物发生的速率通过rRNA成熟途径的显着变化独立于RNA Pol I活性进行调节。该过程可以控制核糖体的生物发生速率,从而有可能逃避核糖体的压力,并最终允许组装特殊种类的核糖体。

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