Hurst-Hess Kelley R, Kuo Lili, Masters Paul S
Wadsworth Center, New York State Department of Health, Albany, New York, USA.
Wadsworth Center, New York State Department of Health, Albany, New York, USA
J Virol. 2015 Jun;89(11):6033-47. doi: 10.1128/JVI.00197-15. Epub 2015 Mar 25.
Coronaviruses, the largest RNA viruses, have a complex program of RNA synthesis that entails genome replication and transcription of subgenomic mRNAs. RNA synthesis by the prototype coronavirus mouse hepatitis virus (MHV) is carried out by a replicase-transcriptase composed of 16 nonstructural protein (nsp) subunits. Among these, nsp3 is the largest and the first to be inserted into the endoplasmic reticulum. nsp3 comprises multiple structural domains, including two papain-like proteases (PLPs) and a highly conserved ADP-ribose-1″-phosphatase (ADRP) macrodomain. We have previously shown that the ubiquitin-like domain at the amino terminus of nsp3 is essential and participates in a critical interaction with the viral nucleocapsid protein early in infection. In the current study, we exploited atypical expression schemes to uncouple PLP1 from the processing of nsp1 and nsp2 in order to investigate the requirements of nsp3 domains for viral RNA synthesis. In the first strategy, a mutant was created in which replicase polyprotein translation initiated with nsp3, thereby establishing that complete elimination of nsp1 and nsp2 does not abolish MHV viability. In the second strategy, a picornavirus autoprocessing element was used to separate a truncated nsp1 from nsp3. This provided a platform for further dissection of amino-terminal domains of nsp3. From this, we found that catalytic mutation of PLP1 or complete deletion of PLP1 and the adjacent ADRP domain was tolerated by the virus. These results showed that neither the PLP1 domain nor the ADRP domain of nsp3 provides integral activities essential for coronavirus genomic or subgenomic RNA synthesis.
The largest component of the coronavirus replicase-transcriptase complex, nsp3, contains multiple modules, many of which do not have clearly defined functions in genome replication or transcription. These domains may play direct roles in RNA synthesis, or they may have evolved for other purposes, such as to combat host innate immunity. We initiated a dissection of MHV nsp3 aimed at identifying those activities or structures in this huge molecule that are essential to replicase activity. We found that both PLP1 and ADRP could be entirely deleted, provided that the requirement for proteolytic processing by PLP1 was offset by an alternative mechanism. This demonstrated that neither PLP1 nor ADRP plays an essential role in coronavirus RNA synthesis.
冠状病毒是最大的RNA病毒,具有复杂的RNA合成程序,包括基因组复制和亚基因组mRNA的转录。原型冠状病毒小鼠肝炎病毒(MHV)的RNA合成由一个由16个非结构蛋白(nsp)亚基组成的复制酶-转录酶进行。其中,nsp3是最大的,也是第一个插入内质网的。nsp3包含多个结构域,包括两个木瓜样蛋白酶(PLP)和一个高度保守的ADP-核糖-1″-磷酸酶(ADRP)大结构域。我们之前已经表明,nsp3氨基末端的泛素样结构域是必不可少的,并且在感染早期参与与病毒核衣壳蛋白的关键相互作用。在当前的研究中,我们利用非典型表达方案将PLP1与nsp1和nsp2的加工过程解偶联,以研究nsp3结构域对病毒RNA合成的需求。在第一种策略中,创建了一个突变体,其中复制酶多聚蛋白翻译从nsp3开始,从而确定完全消除nsp1和nsp2不会消除MHV的生存能力。在第二种策略中,使用微小RNA病毒自加工元件将截短的nsp1与nsp3分离。这为进一步剖析nsp3的氨基末端结构域提供了一个平台。由此,我们发现病毒可以耐受PLP1的催化突变或PLP1和相邻ADRP结构域的完全缺失。这些结果表明,nsp3的PLP1结构域和ADRP结构域都不提供冠状病毒基因组或亚基因组RNA合成所必需的完整活性。
冠状病毒复制酶-转录酶复合物的最大组成部分nsp3包含多个模块,其中许多在基因组复制或转录中没有明确的功能。这些结构域可能在RNA合成中起直接作用,或者它们可能是为其他目的而进化的,例如对抗宿主先天免疫。我们开始对MHV nsp3进行剖析,旨在确定这个巨大分子中那些对复制酶活性至关重要的活性或结构。我们发现,只要PLP1蛋白水解加工的需求被另一种机制抵消,PLP1和ADRP都可以完全缺失。这表明PLP1和ADRP在冠状病毒RNA合成中都不发挥重要作用。
