A Cysteine Zipper Stabilizes a Pre-Fusion F Glycoprotein Vaccine for Respiratory Syncytial Virus

نویسندگان

  • Guillaume B. E. Stewart-Jones
  • Paul V. Thomas
  • Man Chen
  • Aliaksandr Druz
  • M. Gordon Joyce
  • Wing-Pui Kong
  • Mallika Sastry
  • Cinque Soto
  • Yongping Yang
  • Baoshan Zhang
  • Lei Chen
  • Gwo-Yu Chuang
  • Ivelin S. Georgiev
  • Jason S. McLellan
  • Sanjay Srivatsan
  • Tongqing Zhou
  • Ulrich Baxa
  • John R. Mascola
  • Barney S. Graham
  • Peter D. Kwong
  • Steven M. Varga
چکیده

Recombinant subunit vaccines should contain minimal non-pathogen motifs to reduce potential off-target reactivity. We recently developed a vaccine antigen against respiratory syncytial virus (RSV), which comprised the fusion (F) glycoprotein stabilized in its pre-fusion trimeric conformation by "DS-Cav1" mutations and by an appended C-terminal trimerization motif or "foldon" from T4-bacteriophage fibritin. Here we investigate the creation of a cysteine zipper to allow for the removal of the phage foldon, while maintaining the immunogenicity of the parent DS-Cav1+foldon antigen. Constructs without foldon yielded RSV F monomers, and enzymatic removal of the phage foldon from pre-fusion F trimers resulted in their dissociation into monomers. Because the native C terminus of the pre-fusion RSV F ectodomain encompasses a viral trimeric coiled-coil, we explored whether introduction of cysteine residues capable of forming inter-protomer disulfides might allow for stable trimers. Structural modeling indicated the introduced cysteines to form disulfide "rings", with each ring comprising a different set of inward facing residues of the coiled-coil. Three sets of rings could be placed within the native RSV F coiled-coil, and additional rings could be added by duplicating portions of the coiled-coil. High levels of neutralizing activity in mice, equivalent to that of the parent DS-Cav1+foldon antigen, were elicited by a 4-ring stabilized RSV F trimer with no foldon. Structure-based alteration of a viral coiled-coil to create a cysteine zipper thus allows a phage trimerization motif to be removed from a candidate vaccine antigen.

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عنوان ژورنال:

دوره 10  شماره 

صفحات  -

تاریخ انتشار 2015