单纯疱疹病毒的病毒体宿主关闭核酸内切酶(UL41)与细胞帽结合复合物eIF4F相互作用。
The virion host shutoff endonuclease (UL41) of herpes simplex virus interacts with the cellular cap-binding complex eIF4F.
作者信息
Page Heidi G, Read G Sullivan
机构信息
Division of Cell Biology and Biophysics, School of Biological Sciences, University of Missouri-Kansas City, 5007 Rockhill Road, Kansas City, MO 64110, USA.
出版信息
J Virol. 2010 Jul;84(13):6886-90. doi: 10.1128/JVI.00166-10. Epub 2010 Apr 28.
Abstract
The herpes simplex virus Vhs endonuclease degrades host and viral mRNAs. Isolated Vhs cuts any RNA at many sites. Yet, within cells, it targets mRNAs and cuts at preferred sites, including regions of translation initiation. Previous studies have shown that Vhs binds the translation factors eIF4A and eIF4H. Here, we show that Vhs binds the cap-binding complex eIF4F. Association with eIF4F correlated with the ability of Vhs to bind eIF4A but not eIF4H. All Vhs proteins that degrade mRNAs associated with eIF4F. However, simply tethering an active endonuclease to eIF4F is not sufficient to degrade mRNAs. Binding to eIF4H may also be required.
摘要
单纯疱疹病毒Vhs核酸内切酶可降解宿主和病毒的mRNA。分离出的Vhs可在多个位点切割任何RNA。然而,在细胞内,它靶向mRNA并在偏好的位点进行切割,包括翻译起始区域。先前的研究表明,Vhs可结合翻译因子eIF4A和eIF4H。在此,我们表明Vhs可结合帽结合复合物eIF4F。与eIF4F的结合与Vhs结合eIF4A的能力相关,但与eIF4H无关。所有可降解mRNA的Vhs蛋白均与eIF4F相关。然而,仅仅将一种活性核酸内切酶与eIF4F拴系在一起并不足以降解mRNA。可能还需要与eIF4H结合。
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