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We described the rapid production of the domain III (DIII) of the envelope (E) protein in plants as a vaccine candidate for West Nile Virus (WNV). Using various combinations of vector modules of a deconstructed viral vector expression system, DIII

We described the rapid production of the domain III (DIII) of the envelope (E) protein in plants as a vaccine candidate for West Nile Virus (WNV). Using various combinations of vector modules of a deconstructed viral vector expression system, DIII was produced in three subcellular compartments in leaves of Nicotiana benthamiana by transient expression. DIII expressed at much higher levels when targeted to the endoplasmic reticulum (ER) than that targeted to the chloroplast or the cytosol, with accumulation level up to 73 μg DIII per gram of leaf fresh weight within 4 days after infiltration. Plant ER-derived DIII was soluble and readily purified to > 95% homogeneity without the time-consuming process of denaturing and refolding. Further analysis revealed that plant-produced DIII was processed properly and demonstrated specific binding to an anti-DIII monoclonal antibody that recognizes a conformational epitope. Furthermore, subcutaneous immunization of mice with 5 and 25 μg of purified DIII elicited a potent systemic response. This study provided the proof of principle for rapidly producing immunogenic vaccine candidates against WNV in plants with low cost and scalability.

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    Title
    • A Plant-Produced Antigen Elicits Potent Immune Responses Against West Nile Virus in Mice
    Contributors
    Date Created
    2014-04-03
    Resource Type
  • Text
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    Identifier
    • Digital object identifier: 10.1155/2014/952865
    • Identifier Type
      International standard serial number
      Identifier Value
      2314-6133
    • Identifier Type
      International standard serial number
      Identifier Value
      2314-6141

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    He, J., Peng, L., Lai, H., Hurtado, J., Stahnke, J., & Chen, Q. (2014). A Plant-Produced Antigen Elicits Potent Immune Responses against West Nile Virus in Mice. BioMed Research International, 2014, 1-10. doi:10.1155/2014/952865

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