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Sortase-Mediated Ligation as a Modular Approach for the Covalent Attachment of Proteins to the Exterior of the Bacteriophage P22 Virus-like Particle
Bioconjugate Chemistry (2017)
  • Dustin P. Patterson
  • Benjamin Schwarz
  • John Avera
  • Brian Western
  • Matthew Hicks
  • Paul Krugler
  • Matthew Terra
  • Masaki Uchida
  • Kimberly McCoy
  • Trevor Douglas
Abstract
Virus-like particles are unique platforms well suited for the construction of nanomaterials with broad-range applications. The research presented here describes the development of a modular approach for the covalent attachment of protein domains to the exterior of the versatile bacteriophage P22 virus-like particle (VLP) via a sortase-mediated ligation strategy. The bacteriophage P22 coat protein was genetically engineered to incorporate an LPETG amino acid sequence on the C-terminus, providing the peptide recognition sequence utilized by the sortase enzyme to catalyze peptide bond formation between the LPETG-tagged protein and a protein containing a polyglycine sequence on the N-terminus. Here we evaluate attachment of green fluorescent protein (GFP) and the head domain of the influenza hemagglutinin (HA) protein by genetically producing polyglycine tagged proteins. Attachment of both proteins to the exterior of the P22 VLP was found to be highly efficient as judged by SDS-PAGE densitometry. These results enlarge the tool kit for modifying the P22 VLP system and provide new insights for other VLPs that have an externally displayed C-terminus that can use the described strategy for the modular modification of their external surface for various applications.
Keywords
  • Peptides and proteinsMonomersLigationImaging probesNucleic acid structur
Publication Date
August 16, 2017
DOI
10.1021/acs.bioconjchem.7b00296
Citation Information
Dustin P. Patterson, Benjamin Schwarz, John Avera, Brian Western, et al.. "Sortase-Mediated Ligation as a Modular Approach for the Covalent Attachment of Proteins to the Exterior of the Bacteriophage P22 Virus-like Particle" Bioconjugate Chemistry Vol. 28 Iss. 8 (2017) p. 2114 - 2124
Available at: http://works.bepress.com/dustin-patterson/23/