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Herpes Simplex Virus Virion Host Shutoff Protein Is Stimulated by Translation Initiation Factors eIF4B and eIF4H

机译:翻译起始因子eIF4B和eIF4H刺激单纯疱疹病毒病毒粒子宿主关闭蛋白

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摘要

The virion host shutoff protein (vhs) of herpes simplex virus triggers accelerated degradation of cellular and viral mRNAs while sparing other cytoplasmic RNA species. Previous work has shown that vhs forms a complex with translation initiation factor eIF4H, which displays detectable RNase activity in the absence of other viral or host proteins. However, the contributions of eIF4H and other host factors to the activity and mRNA targeting properties of vhs have not yet been directly examined. An earlier report from our laboratory demonstrated that rabbit reticulocyte lysate (RRL) contains one or more factors that strongly stimulate the RNase activity of vhs produced in Saccharomyces cerevisiae. We report here that such yeast extracts display significant vhs-dependent RNase activity in the absence of mammalian factors. This activity differs from that displayed by vhs generated in RRL in that it is not targeted to the encephalomyocarditis virus (EMCV) internal ribosome entry site (IRES). Activity was strongly enhanced by the addition of RRL, eIF4H, or the related translation factor eIF4B. RRL also reconstituted strong targeting to the EMCV IRES, resulting in a major change in the RNA cleavage pattern. In contrast, eIF4H and eIF4B did not reconstitute IRES-directed targeting. These data indicate that eIF4B and 4H stimulate the nuclease activity of vhs, and they provide evidence that additional mammalian factors are required for targeting to the EMCV IRES.
机译:单纯疱疹病毒的病毒体宿主封闭蛋白(vhs)触发细胞和病毒mRNA的加速降解,同时保留其他胞质RNA种类。先前的工作表明,vhs与翻译起始因子eIF4H形成复合物,在没有其他病毒或宿主蛋白的情况下,它显示出可检测的RNase活性。但是,尚未直接检查eIF4H和其他宿主因子对vhs的活性和mRNA靶向特性的贡献。我们实验室的较早报告表明,兔网织红细胞裂解液(RRL)包含一种或多种能强烈刺激酿酒酵母中产生的vhs的RNase活性的因子。我们在这里报告说,在没有哺乳动物因素的情况下,这种酵母提取物显示出重要的依赖vhs的RNase活性。此活动与RRL中生成的vhs所显示的活动不同,因为它不针对脑心肌炎病毒(EMCV)内部核糖体进入位点(IRES)。通过添加RRL,eIF4H或相关的翻译因子eIF4B,可大大增强活性。 RRL还重组了对EMCV IRES的强靶向性,导致RNA裂解模式发生了重大变化。相比之下,eIF4H和eIF4B不能重构IRES导向的靶向。这些数据表明eIF4B和4H刺激vhs的核酸酶活性,并且它们提供证据表明靶向EMCV IRES需要其他哺乳动物因子。

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