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TitleCryo-electron Microscopy Structures of Expanded Poliovirus with VHHs Sample the Conformational Repertoire of the Expanded State.
Journal, issue, pagesJ Virol, Vol. 91, Issue 3, Year 2017
Publish dateFeb 1, 2017
AuthorsMike Strauss / Lise Schotte / Krishanthi S Karunatilaka / David J Filman / James M Hogle /
PubMed AbstractBy using cryo-electron microscopy, expanded 80S-like poliovirus virions (poliovirions) were visualized in complexes with four 80S-specific camelid VHHs (Nanobodies). In all four complexes, the VHHs ...By using cryo-electron microscopy, expanded 80S-like poliovirus virions (poliovirions) were visualized in complexes with four 80S-specific camelid VHHs (Nanobodies). In all four complexes, the VHHs bind to a site on the top surface of the capsid protein VP3, which is hidden in the native virus. Interestingly, although the four VHHs bind to the same site, the structures of the expanded virus differ in detail in each complex, suggesting that each of the Nanobodies has sampled a range of low-energy structures available to the expanded virion. By stabilizing unique structures of expanded virions, VHH binding permitted a more detailed view of the virus structure than was previously possible, leading to a better understanding of the expansion process that is a critical step in infection. It is now clear which polypeptide chains become disordered and which become rearranged. The higher resolution of these structures also revealed well-ordered conformations for the EF loop of VP2, the GH loop of VP3, and the N-terminal extensions of VP1 and VP2, which, in retrospect, were present in lower-resolution structures but not recognized. These structural observations help to explain preexisting mutational data and provide insights into several other stages of the poliovirus life cycle, including the mechanism of receptor-triggered virus expansion.
IMPORTANCE: When poliovirus infects a cell, it undergoes a change in its structure in order to pass RNA through its protein coat, but this altered state is short-lived and thus poorly understood. The structures of poliovirus bound to single-domain antibodies presented here capture the altered virus in what appear to be intermediate states. A careful analysis of these structures lets us better understand the molecular mechanism of infection and how these changes in the virus lead to productive-infection events.
External linksJ Virol / PubMed:27852863 / PubMed Central
MethodsEM (single particle)
Resolution4.3 - 6.9 Å
Structure data

EMDB-8277: expanded poliovirus bound to VHH 10E
PDB-5kwl: expanded poliovirus in complex with VHH 10E
Method: EM (single particle) / Resolution: 4.8 Å

EMDB-8284, PDB-5ktz:
expanded poliovirus in complex with VHH 12B
Method: EM (single particle) / Resolution: 4.3 Å

EMDB-8285, PDB-5ku0:
expanded poliovirus in complex with VHH 17B
Method: EM (single particle) / Resolution: 5.3 Å

EMDB-8286, PDB-5ku2:
expanded poliovirus in complex with VHH 7A
Method: EM (single particle) / Resolution: 5.3 Å

EMDB-8292:
expanded poliovirus in complex with VHH 12B
Method: EM (single particle) / Resolution: 6.9 Å

Source
  • Human poliovirus 1
  • poliovirus type 1 (strain mahoney)
  • poliovirus type 1
  • camelus dromedarius (Arabian camel)
KeywordsVIRUS/immune system / poliovirus / VHH / nanobody / 80S / expanded / single domain antibody / VIRUS-immune system complex

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