Reovirus σ1 Conformational Flexibility Modulates the Efficiency of Host Cell Attachment

Julia R. Diller (First Author), Sean R. Halloran (Co-Author), Melanie Koehler (Co-Author), Rita dos Santos Natividade (Co-Author), David Alsteens (Co-Author), Thilo Stehle (Co-Author), Terence S. Dermody* (Co-Author), Kristen M. Ogden* (Last Author)

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

11 Scopus citations

Abstract

Reovirus attachment protein σ1 is a trimeric molecule containing tail, body, and head domains. During infection, σ1 engages sialylated glycans and junctional adhesion molecule-A (JAM-A), triggering uptake into the endocytic compartment, where virions are proteolytically converted to infectious subvirion particles (ISVPs). Further disassembly allows σ1 release and escape of transcriptionally active reovirus cores into the cytosol. Electron microscopy has revealed a distinct conformational change in σ1 from a compact form on virions to an extended form on ISVPs. To determine the importance of σ1 conformational mobility, we used reverse genetics to introduce cysteine mutations that can cross-link σ1 by establishing disulfide bonds between structurally adjacent sites in the tail, body, and head domains. We detected phenotypic differences among the engineered viruses. A mutant with a cysteine pair in the head domain replicates with enhanced kinetics, forms large plaques, and displays increased avidity for JAM-A relative to the parental virus, mimicking properties of ISVPs. However, unlike ISVPs, particles containing cysteine mutations that cross-link the head domain uncoat and transcribe viral positive-sense RNA with kinetics similar to the parental virus and are sensitive to ammonium chloride, which blocks virion-to-ISVP conversion. Together, these data suggest that σ1 conformational flexibility modulates the efficiency of reovirus host cell attachment.

Original languageEnglish
Article numbere01163
JournalJournal of virology
Volume92
Issue number13
DOIs
StatePublished - Jul 2018
Externally publishedYes

Keywords

  • Crosslink
  • Disulfide
  • Glycan
  • Junctional adhesion molecule-A
  • Receptor
  • Reovirus
  • Sialic acid

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