Cantini F, Banci L, Altincekic N, Bains J K, Dhamotharan K, Fuks C, Fürtig B, Gande S L, Hargittay B, Hengesbach M, Hutchison M T, Korn S M, Kubatova N, Kutz F, Linhard V, Löhr F, Meiser N, Pyper D J, Qureshi N S, Richter C, Saxena K, Schlundt A, Schwalbe H, Sreeramulu S, Tants J-N, Wacker A, Weigand J E, Wöhnert J, Tsika A C, Fourkiotis N K, Spyroulias G A
Magnetic Resonance Center - CERM, University of Florence, Via Luigi Sacconi 6, Sesto Fiorentino, 50019, Florence, Italy.
Department of Chemistry, University of Florence, Via della Lastruccia 3, Sesto Fiorentino, 50019, Florence, Italy.
Biomol NMR Assign. 2020 Oct;14(2):339-346. doi: 10.1007/s12104-020-09973-4. Epub 2020 Aug 14.
The SARS-CoV-2 genome encodes for approximately 30 proteins. Within the international project COVID19-NMR, we distribute the spectroscopic analysis of the viral proteins and RNA. Here, we report NMR chemical shift assignments for the protein Nsp3b, a domain of Nsp3. The 217-kDa large Nsp3 protein contains multiple structurally independent, yet functionally related domains including the viral papain-like protease and Nsp3b, a macrodomain (MD). In general, the MDs of SARS-CoV and MERS-CoV were suggested to play a key role in viral replication by modulating the immune response of the host. The MDs are structurally conserved. They most likely remove ADP-ribose, a common posttranslational modification, from protein side chains. This de-ADP ribosylating function has potentially evolved to protect the virus from the anti-viral ADP-ribosylation catalyzed by poly-ADP-ribose polymerases (PARPs), which in turn are triggered by pathogen-associated sensing of the host immune system. This renders the SARS-CoV-2 Nsp3b a highly relevant drug target in the viral replication process. We here report the near-complete NMR backbone resonance assignment (H, C, N) of the putative Nsp3b MD in its apo form and in complex with ADP-ribose. Furthermore, we derive the secondary structure of Nsp3b in solution. In addition, N-relaxation data suggest an ordered, rigid core of the MD structure. These data will provide a basis for NMR investigations targeted at obtaining small-molecule inhibitors interfering with the catalytic activity of Nsp3b.
严重急性呼吸综合征冠状病毒2(SARS-CoV-2)基因组编码约30种蛋白质。在国际项目COVID19-NMR中,我们对病毒蛋白和RNA进行光谱分析。在此,我们报告了Nsp3的一个结构域Nsp3b的核磁共振(NMR)化学位移归属。217 kDa的大Nsp3蛋白包含多个结构上独立但功能相关的结构域,包括病毒木瓜样蛋白酶和一个大结构域(MD)Nsp3b。一般来说,SARS-CoV和中东呼吸综合征冠状病毒(MERS-CoV)的MDs被认为通过调节宿主的免疫反应在病毒复制中起关键作用。这些MDs在结构上是保守的。它们很可能从蛋白质侧链上去除一种常见的翻译后修饰——ADP核糖。这种去ADP核糖基化功能可能已经进化,以保护病毒免受由聚ADP核糖聚合酶(PARP)催化的抗病毒ADP核糖基化作用,而PARP又是由宿主免疫系统对病原体相关的感知所触发的。这使得SARS-CoV-2 Nsp3b成为病毒复制过程中一个高度相关的药物靶点。我们在此报告了假定的Nsp3b MD在其无配体形式以及与ADP核糖结合时的近乎完整的NMR主链共振归属(H、C、N)。此外,我们推导了溶液中Nsp3b的二级结构。另外,N弛豫数据表明MD结构存在一个有序、刚性的核心。这些数据将为旨在获得干扰Nsp3b催化活性的小分子抑制剂的NMR研究提供基础。
