Donald Danforth Plant Science Center, 975 North Warson Road, Saint Louis, MO 63132, USA.
J Virol. 2010 Jun;84(11):5836-41. doi: 10.1128/JVI.00314-10. Epub 2010 Mar 24.
Our previous structural studies on intact, infectious murine norovirus 1 (MNV-1) virions demonstrated that the receptor binding protruding (P) domains are lifted off the inner shell of the virus. Here, the three-dimensional (3D) reconstructions of recombinant rabbit hemorrhagic disease virus (rRHDV) virus-like particles (VLPs) and intact MNV-1 were determined to approximately 8-A resolution. rRHDV also has a raised P domain, and therefore, this conformation is independent of infectivity and genus. The atomic structure of the MNV-1 P domain was used to interpret the MNV-1 reconstruction. Connections between the P and shell domains and between the floating P domains were modeled. This observed P-domain flexibility likely facilitates virus-host receptor interactions.
我们之前对完整的、有感染性的鼠诺如病毒 1(MNV-1)病毒粒子的结构研究表明,受体结合突出(P)结构域从病毒的内壳中抬起。在此,通过冷冻电镜三维重构技术,我们将重组兔出血症病毒(rRHDV)病毒样颗粒(VLPs)和完整的 MNV-1 分别解析至约 8-A 的分辨率。rRHDV 也有一个凸起的 P 结构域,因此这种构象独立于感染力和属。我们使用 MNV-1 P 结构域的原子结构来解释 MNV-1 的重构。我们对 P 结构域和外壳结构域之间的连接,以及浮动的 P 结构域之间的连接进行了建模。这种观察到的 P 结构域的灵活性可能促进了病毒与宿主受体的相互作用。
