Marquez-Jurado Silvia, Nogales Aitor, Zuñiga Sonia, Enjuanes Luis, Almazán Fernando
Department of Molecular and Cell Biology, Centro Nacional de Biotecnología (CNB-CSIC), Campus Universidad Autónoma de Madrid, Madrid, Spain.
Department of Molecular and Cell Biology, Centro Nacional de Biotecnología (CNB-CSIC), Campus Universidad Autónoma de Madrid, Madrid, Spain
mBio. 2015 Mar 10;6(2):e00105. doi: 10.1128/mBio.00105-15.
A 32-nucleotide (nt) RNA motif located at the 3' end of the transmissible gastroenteritis coronavirus (TGEV) genome was found to specifically interact with the host proteins glutamyl-prolyl-tRNA synthetase (EPRS) and arginyl-tRNA synthetase (RRS). This RNA motif has high homology in sequence and secondary structure with the gamma interferon-activated inhibitor of translation (GAIT) element, which is located at the 3' end of several mRNAs encoding proinflammatory proteins. The GAIT element is involved in the translation silencing of these mRNAs through its interaction with the GAIT complex (EPRS, heterogeneous nuclear ribonucleoprotein Q, ribosomal protein L13a, and glyceraldehyde 3-phosphate dehydrogenase) to favor the resolution of inflammation. Interestingly, we showed that the viral RNA motif bound the GAIT complex and inhibited the in vitro translation of a chimeric mRNA containing this RNA motif. To our knowledge, this is the first GAIT-like motif described in a positive RNA virus. To test the functional role of the GAIT-like RNA motif during TGEV infection, a recombinant coronavirus harboring mutations in this motif was engineered and characterized. Mutations of the GAIT-like RNA motif did not affect virus growth in cell cultures. However, an exacerbated innate immune response, mediated by the melanoma differentiation-associated gene 5 (MDA5) pathway, was observed in cells infected with the mutant virus compared with the response observed in cells infected with the parental virus. Furthermore, the mutant virus was more sensitive to beta interferon than the parental virus. All together, these data strongly suggested that the viral GAIT-like RNA motif modulates the host innate immune response.
The innate immune response is the first line of antiviral defense that culminates with the synthesis of interferon and proinflammatory cytokines to limit virus replication. Coronaviruses encode several proteins that interfere with the innate immune response at different levels, but to date, no viral RNA counteracting antiviral response has been described. In this work, we have characterized a 32-nt RNA motif located at the 3' end of the TGEV genome that specifically interacted with EPRS and RRS. This RNA motif presented high homology with the GAIT element, involved in the modulation of the inflammatory response. Moreover, the disruption of the viral GAIT-like RNA motif led to an exacerbated innate immune response triggered by MDA5, indicating that the GAIT-like RNA motif counteracts the host innate immune response. These novel findings may be of relevance for other coronaviruses and could serve as the basis for the development of novel antiviral strategies.
在传染性胃肠炎冠状病毒(TGEV)基因组3'端发现一个32个核苷酸(nt)的RNA基序,它能特异性地与宿主蛋白谷氨酰胺 - 脯氨酰 - tRNA合成酶(EPRS)和精氨酰 - tRNA合成酶(RRS)相互作用。该RNA基序在序列和二级结构上与γ干扰素激活的翻译抑制因子(GAIT)元件具有高度同源性,GAIT元件位于几种编码促炎蛋白的mRNA的3'端。GAIT元件通过与GAIT复合物(EPRS、不均一核核糖核蛋白Q、核糖体蛋白L13a和甘油醛 - 3 - 磷酸脱氢酶)相互作用参与这些mRNA的翻译沉默,以促进炎症的消退。有趣的是,我们发现病毒RNA基序能结合GAIT复合物并抑制含有该RNA基序的嵌合mRNA的体外翻译。据我们所知,这是在正链RNA病毒中描述的首个类似GAIT的基序。为了测试类似GAIT的RNA基序在TGEV感染过程中的功能作用,构建并鉴定了在该基序中含有突变的重组冠状病毒。类似GAIT的RNA基序的突变并不影响病毒在细胞培养物中的生长。然而,与感染亲本病毒的细胞中观察到的反应相比,在感染突变病毒的细胞中观察到由黑色素瘤分化相关基因5(MDA5)途径介导的先天性免疫反应加剧。此外,突变病毒比亲本病毒对β干扰素更敏感。总之,这些数据强烈表明病毒类似GAIT的RNA基序调节宿主先天性免疫反应。
先天性免疫反应是抗病毒防御的第一道防线,最终通过干扰素和促炎细胞因子的合成来限制病毒复制。冠状病毒编码几种在不同水平干扰先天性免疫反应的蛋白质,但迄今为止,尚未描述过对抗抗病毒反应的病毒RNA。在这项研究中,我们鉴定了位于TGEV基因组3'端的一个32 - nt的RNA基序,它能特异性地与EPRS和RRS相互作用。该RNA基序与参与炎症反应调节的GAIT元件具有高度同源性。此外,病毒类似GAIT的RNA基序的破坏导致由MDA5触发的先天性免疫反应加剧,表明类似GAIT的RNA基序对抗宿主先天性免疫反应。这些新发现可能与其他冠状病毒相关,并可为开发新型抗病毒策略提供基础。
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