Tristetraprolin招募单纯疱疹病毒体宿主关闭核糖核酸酶至应激反应mRNA中的富含AU元件,以实现其切割。
Tristetraprolin Recruits the Herpes Simplex Virion Host Shutoff RNase to AU-Rich Elements in Stress Response mRNAs To Enable Their Cleavage.
作者信息
Shu Minfeng, Taddeo Brunella, Roizman Bernard
机构信息
Marjorie B. Kovler Viral Oncology Laboratories, The University of Chicago, Chicago, Illinois, USA.
Marjorie B. Kovler Viral Oncology Laboratories, The University of Chicago, Chicago, Illinois, USA
出版信息
J Virol. 2015 May;89(10):5643-50. doi: 10.1128/JVI.00091-15. Epub 2015 Mar 11.
UNLABELLED
Herpes simplex viruses (HSV) package and bring into cells an RNase designated virion host shutoff (VHS) RNase. In infected cells, the VHS RNase targets primarily stress response mRNAs characterized by the presence of AU-rich elements in their 3' untranslated regions (UTRs). In uninfected cells, these RNAs are sequestered in exosomes or P bodies by host proteins that bind to the AU-rich elements. In infected cells, the AU-rich RNAs are deadenylated and cleaved close to the AU-rich elements, leading to long-term persistence of nontranslatable RNAs consisting of the 5' portions of the cleavage products. The host proteins that bind to the AU-rich elements are either resident in cells (e.g., TIA-1) or induced (e.g., tristetraprolin). Earlier, this laboratory reported that tristetraprolin binds VHS RNase. To test the hypothesis that tristetraprolin directs VHS RNase to the AU-rich elements, we mapped the domains of VHS and tristetraprolin required for their interactions. We report that VHS binds to the domain of tristetraprolin that enables its interaction with RNA. A single amino acid substitution in that domain abolished the interaction with RNA but did not block the binding to VHS RNase. In transfected cells, the mutant but not the wild-type tristetraprolin precluded the degradation of the AU-rich RNAs by VHS RNase. We conclude that TTP mediates the cleavage of the 3' UTRs of stress response mRNAs by recruiting the VHS RNase to the AU-rich elements.
IMPORTANCE
The primary host response to HSV infection is the synthesis of stress response mRNAs characterized by the presence of AU-rich elements in their 3' UTRs. These mRNAs are the targets of the virion host shutoff (VHS) RNase. The VHS RNase binds both to mRNA cap structure and to tristetraprolin, an inducible host protein that sequesters AU-rich mRNAs in exosomes or P bodies. Here we show that tristetraprolin recruits VHS RNase to the AU-rich elements and enables the degradation of the stress response mRNAs.
未标记
单纯疱疹病毒(HSV)包装并将一种名为病毒体宿主关闭(VHS)核糖核酸酶的核糖核酸酶带入细胞。在受感染的细胞中,VHS核糖核酸酶主要靶向应激反应信使核糖核酸,其特征是在其3'非翻译区(UTR)中存在富含AU的元件。在未感染的细胞中,这些核糖核酸被与富含AU的元件结合的宿主蛋白隔离在外泌体或P小体中。在受感染的细胞中,富含AU的核糖核酸会被去腺苷酸化,并在靠近富含AU的元件处被切割,导致由切割产物的5'部分组成的不可翻译核糖核酸长期存在。与富含AU的元件结合的宿主蛋白要么存在于细胞中(如TIA-1),要么是被诱导产生的(如锌指蛋白)。此前,本实验室报道锌指蛋白与VHS核糖核酸酶结合。为了验证锌指蛋白将VHS核糖核酸酶导向富含AU的元件这一假说,我们绘制了VHS和锌指蛋白相互作用所需的结构域图谱。我们报告称,VHS与锌指蛋白中使其能够与核糖核酸相互作用的结构域结合。该结构域中的单个氨基酸取代消除了与核糖核酸的相互作用,但并未阻断与VHS核糖核酸酶的结合。在转染的细胞中,突变型而非野生型锌指蛋白阻止了VHS核糖核酸酶对富含AU的核糖核酸的降解。我们得出结论,锌指蛋白通过将VHS核糖核酸酶招募到富含AU的元件来介导应激反应信使核糖核酸3'UTR的切割。
重要性
宿主对HSV感染的主要反应是合成应激反应信使核糖核酸,其特征是在其3'UTR中存在富含AU的元件。这些信使核糖核酸是病毒体宿主关闭(VHS)核糖核酸酶的靶标。VHS核糖核酸酶既与信使核糖核酸的帽结构结合,也与锌指蛋白结合,锌指蛋白是一种可诱导的宿主蛋白,可将富含AU的信使核糖核酸隔离在外泌体或P小体中。在这里,我们表明锌指蛋白将VHS核糖核酸酶招募到富含AU的元件,并使应激反应信使核糖核酸能够被降解。
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