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多时间尺度上乙型肝炎病毒前基因组 RNA 的构象动力学:对病毒复制的影响。

Conformational Dynamics of the Hepatitis B Virus Pre-genomic RNA on Multiple Time Scales: Implications for Viral Replication.

机构信息

Center for Biomolecular Structure and Organization, Department of Chemistry and Biochemistry, University of Maryland, College Park, MD 20742, USA.

Basic Science Program, Frederick National Laboratory for Cancer Research, Frederick, MD 21702, USA.

出版信息

J Mol Biol. 2022 Sep 30;434(18):167633. doi: 10.1016/j.jmb.2022.167633. Epub 2022 May 17.

DOI:10.1016/j.jmb.2022.167633
PMID:35595167
Abstract

Human hepatitis B virus (HBV) replication is initiated by the binding of the viral polymerase (P) to epsilon (ε), an ≈85-nucleotide (nt) cis-acting regulatory stem-loop RNA located at the 5'-end of the pre-genomic RNA (pgRNA). This interaction triggers P and pgRNA packaging and protein-primed reverse transcription and is therefore an attractive therapeutic target. Our recent nuclear magnetic resonance (NMR) structure of ε provides a useful starting point toward a detailed understanding of HBV replication, and hints at the functional importance of ε dynamics. Here, we present a detailed description of ε motions on the ps to ns and μs to ms time scales by NMR spin relaxation and relaxation dispersion, respectively. We also carried out molecular dynamics simulations to provide additional insight into ε conformational dynamics. These data outline a series of complex motions on multiple time scales within ε. Moreover, these motions occur in mostly conserved nucleotides from structural regions (i.e., priming loop, pseudo-triloop, and U43 bulge) that biochemical and mutational studies have shown to be essential for P binding, P-pgRNA packaging, protein-priming, and DNA synthesis. Taken together, our work implicates RNA dynamics as an integral feature that governs HBV replication.

摘要

人类乙型肝炎病毒 (HBV) 的复制是由病毒聚合酶 (P) 与 ε 结合启动的,ε 是一种约 85 个核苷酸 (nt) 的顺式作用调节茎环 RNA,位于前基因组 RNA (pgRNA) 的 5' 端。这种相互作用触发了 P 和 pgRNA 的包装以及蛋白引发的逆转录,因此是一个有吸引力的治疗靶点。我们最近对 ε 的核磁共振 (NMR) 结构为深入了解 HBV 复制提供了一个有用的起点,并暗示了 ε 动力学的功能重要性。在这里,我们通过 NMR 自旋弛豫和弛豫分散分别详细描述了 ε 在 ps 到 ns 和 μs 到 ms 时间尺度上的运动。我们还进行了分子动力学模拟,以提供对 ε 构象动力学的更多见解。这些数据概述了 ε 内多个时间尺度上的一系列复杂运动。此外,这些运动发生在结构区域(即引发环、伪三叶草环和 U43 凸起)的大多数保守核苷酸上,生化和突变研究表明这些区域对于 P 结合、P-pgRNA 包装、蛋白引发和 DNA 合成至关重要。总之,我们的工作表明 RNA 动力学是控制 HBV 复制的一个整体特征。

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