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甲型流感病毒核蛋白的寡聚化途径。

Oligomerization paths of the nucleoprotein of influenza A virus.

机构信息

Virologie et Immunologie Moléculaires, UR 892, INRA, Centre de Jouy en Josas, Domaine de Vilvert, Jouy en Josas 78350, France.

出版信息

Biochimie. 2012 Mar;94(3):776-85. doi: 10.1016/j.biochi.2011.11.009. Epub 2011 Nov 29.

DOI:10.1016/j.biochi.2011.11.009
PMID:22155087
Abstract

The influenza viruses contain a segmented, negative strand RNA genome. Each RNA segment is covered by multiple copies of the nucleoprotein (NP) and is associated with the polymerase complex into ribonucleoprotein (RNP) particles. Despite its importance in the virus life cycle, the interactions between the NP and the genome are not well understood. Here, we studied the assembly process of NP-RNA oligomers and analyzed how the oligomeric/monomeric status of RNA-free NP affects RNA binding and oligomerization. Recombinant wild-type NP purified in low salt concentrations and a derived mutant engineered for oligomerization deficiency (R416A) were mainly monomeric in RNA-free solutions as shown by biochemical and electron microscopy techniques. NP monomer formed with RNA a fast 1/1 complex characterized by surface plasmon resonance. In a subsequent and slow process that depended on the RNA length, oligomerization of NP was mediated by RNA binding. In contrast, preparations of wild-type NP purified in high salt concentrations as well as mutant Y148A engineered for deficiency in nucleic acid binding were partly or totally oligomeric in RNA-free solutions. These trimer/tetramer NP oligomers bind directly as oligomers to RNA with a higher affinity than that of the monomers. Both oligomerization routes we characterized could be exploited by cellular or viral factors to modulate or control viral RNA encapsidation by NP.

摘要

流感病毒含有分段的负链 RNA 基因组。每个 RNA 片段都被多个核蛋白 (NP) 覆盖,并与聚合酶复合物一起形成核糖核蛋白 (RNP) 颗粒。尽管 NP 在病毒生命周期中具有重要作用,但 NP 与基因组之间的相互作用仍未得到很好的理解。在这里,我们研究了 NP-RNA 低聚物的组装过程,并分析了无 RNA 的 NP 的寡聚体/单体状态如何影响 RNA 结合和寡聚化。重组野生型 NP 在低盐浓度下纯化,并对寡聚化缺陷的突变体(R416A)进行工程改造,如生化和电子显微镜技术所示,在无 RNA 的溶液中主要以单体形式存在。NP 单体与 RNA 形成快速的 1/1 复合物,其特征是表面等离子体共振。在随后的缓慢过程中,NP 的寡聚化取决于 RNA 的长度,由 RNA 结合介导。相比之下,在高盐浓度下纯化的野生型 NP 制剂以及核酸结合缺陷的突变体 Y148A 主要以单体形式存在。这些三聚体/四聚体 NP 寡聚体以寡聚体形式直接与 RNA 结合,亲和力高于单体。我们表征的这两种寡聚化途径都可以被细胞或病毒因子利用,以调节或控制 NP 对病毒 RNA 的包裹。

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