Transgenic papaya: a useful platform for oral vaccines Article

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Overview

abstract

• Main conclusion: Transgenic papaya callus lines expressing the components of the S3Pvac vaccine constitute a stable platform to produce an oral vaccine against cysticercosis caused byTaenia soliumorT. crassiceps. The development of effective delivery systems to cope with the reduced immunogenicity of new subunit vaccines is a priority in vaccinology. Herein, experimental evidence supporting a papaya-based platform to produce needle-free, recombinant, highly immunogenic vaccines is shown. Papaya (Carica papaya) callus lines were previously engineered by particle bombardment to express the three protective peptides of the S3Pvac anti-cysticercosis vaccine (KETc7, KETc12, KETc1). Calli were propagated in vitro, and a stable integration and expression of the target genes has been maintained, as confirmed by PCR, qRT-PCR, and HPLC. These results point papaya calli as a suitable platform for long-term transgenic expression of the vaccine peptides. The previously demonstrated protective immunogenic efficacy of S3Pvac-papaya orally administered to mice is herein confirmed in a wider dose-range and formulated with different delivery vehicles, adequate for oral vaccination. This protection is accompanied by an increase in anti-S3Pvac antibody titers and a delayed hypersensitivity response against the vaccine. A significant increase in CD4%2b and CD8%2b lymphocyte proliferation was induced in vitro by each vaccine peptide in mice immunized with the lowest dose of S3Pvac papaya (0.56 ng of the three peptides in 0.1 µg of papaya callus total protein per mouse). In pigs, the obliged intermediate host for Taenia solium, S3Pvac papaya was also immunogenic when orally administered in a two-log dose range. Vaccinated pigs significantly increased anti-vaccine antibodies and mononuclear cell proliferation. Overall, the oral immunogenicity of this stable S3Pvac-papaya vaccine in mice and pigs, not requiring additional adjuvants, supports the interest in papaya callus as a useful platform for plant-based vaccines. © 2017, Springer-Verlag Berlin Heidelberg.

authors

• Adalid L.
• Cervantes-Torres J.
• Chapula H.
• Figueroa A.
• Flores I.
• Fragoso G.
• Galvez L.
• Hernández M.
• Jiménez H.
• Monreal-Escalante E.
• Pezzat E.
• Ramírez-Aquino R.
• Rosales Mendoza Sergio
• Rosas G.
• Sciutto E.
• Segura-Velázquez R.
• Vazquez L.G.
• Villalobos N.

publication date

• 2017-01-01

published in

• Planta  Journal

Research

keywords

• Cysticercosis; Embryogenic callus; Oral vaccine; Taenia crassiceps; Taenia solium parasite antigen; recombinant vaccine; animal; Bagg albino mouse; Carica; cysticercosis; female; genetics; immunization; immunology; male; metabolism; mouse; oral drug administration; parasitology; pig; Swine Diseases; Taenia solium; transgenic plant; veterinary; Administration, Oral; Animals; Antigens, Helminth; Carica; Cysticercosis; Female; Immunization; Male; Mice; Mice, Inbred BALB C; Plants, Genetically Modified; Swine; Swine Diseases; Taenia solium; Vaccines, Synthetic

Identity

Digital Object Identifier (DOI)

• 10.1007/s00425-017-2658-z

PubMed ID

• 28194565

Additional Document Info

start page

• 1037

end page

• 1048

volume

• 245

issue

• 5