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鼠肝炎病毒(MHV)核衣壳(N)蛋白的功能转录调控序列(TRS)RNA 结合和螺旋去稳定决定因素。

Functional transcriptional regulatory sequence (TRS) RNA binding and helix destabilizing determinants of murine hepatitis virus (MHV) nucleocapsid (N) protein.

机构信息

Department of Chemistry, Indiana University, Bloomington, Indiana 47405-7102, USA.

出版信息

J Biol Chem. 2012 Mar 2;287(10):7063-73. doi: 10.1074/jbc.M111.287763. Epub 2012 Jan 12.

Abstract

Coronavirus (CoV) nucleocapsid (N) protein contains two structurally independent RNA binding domains. These are denoted N-terminal domain (NTD) and C-terminal domain and are joined by a charged linker region rich in serine and arginine residues (SR linker). In mouse hepatitis virus (MHV), the NTD binds the transcriptional regulatory sequence (TRS) RNA, a conserved hexanucleotide sequence required for subgenomic RNA synthesis. The NTD is also capable of disrupting a short RNA duplex. We show here that three residues on the β3 (Arg-125 and Tyr-127) and β5 (Tyr-190) strands play key roles in TRS RNA binding and helix destabilization with Ala substitutions of these residues lethal to the virus. NMR studies of the MHV NTD·TRS complex revealed that this region defines a major RNA binding interface in MHV with site-directed spin labeling studies consistent with a model in which the adenosine-rich 3'-region of TRS is anchored by Arg-125, Tyr-127, and Tyr-190 in a way that is critical for efficient subgenomic RNA synthesis in MHV. Characterization of CoV N NTDs from infectious bronchitis virus and from severe acute respiratory syndrome CoV revealed that, although detailed NTD-TRS determinants are distinct from those of MHV NTD, rapid helix destabilization activity of CoV N NTDs is most strongly correlated with CoV function and virus viability.

摘要

冠状病毒(CoV)核衣壳(N)蛋白包含两个结构上独立的 RNA 结合结构域。这些结构域分别表示为 N 端结构域(NTD)和 C 端结构域,通过富含丝氨酸和精氨酸残基的带电连接区(SR 连接区)连接。在鼠肝炎病毒(MHV)中,NTD 结合转录调控序列(TRS)RNA,这是亚基因组 RNA 合成所必需的保守六核苷酸序列。NTD 还能够破坏短 RNA 双链。我们在这里表明,β3(Arg-125 和 Tyr-127)和β5(Tyr-190)链上的三个残基在 TRS RNA 结合和螺旋不稳定中起关键作用,这些残基的 Ala 取代对病毒是致命的。对 MHV NTD·TRS 复合物的 NMR 研究表明,该区域在 MHV 中定义了一个主要的 RNA 结合界面,定点旋转标记研究与一个模型一致,该模型表明,TRS 的富含腺苷的 3'-区通过 Arg-125、Tyr-127 和 Tyr-190 锚定,这对 MHV 中的有效亚基因组 RNA 合成至关重要。对传染性支气管炎病毒和严重急性呼吸系统综合征 CoV 的 CoV N NTD 的表征表明,尽管详细的 NTD-TRS 决定因素与 MHV NTD 的不同,但 CoV N NTD 的快速螺旋不稳定活性与 CoV 功能和病毒活力密切相关。

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