Immunological evaluation in nonhuman primates of formulations based on the chimeric protein P64k-domain III of dengue 2 and two components of Neisseria meningitidis
Autor: | Jorge Sánchez, Rafael Martínez, María G. Guzmán, Gerardo Guillén, Tamara Menéndez, Lázaro Gil, Jorge Martín, Laura Lazo, Yaremis Romero, Olivia Niebla, Iris Valdés, Lisset Hermida, Lidice Bernardo, Jorge Fernandez de Castro, Carlos López |
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Rok vydání: | 2009 |
Předmět: |
Recombinant Fusion Proteins
medicine.medical_treatment Aluminum Hydroxide Dengue Vaccines Neisseria meningitidis Dengue virus Biology Antibodies Viral medicine.disease_cause Virus law.invention Microbiology Dengue Adjuvants Immunologic Viral Envelope Proteins law Chlorocebus aethiops medicine Animals Dengue vaccine Vaccines Synthetic General Veterinary General Immunology and Microbiology Secretory Vesicles Polysaccharides Bacterial Public Health Environmental and Occupational Health Dengue Virus biology.organism_classification Survival Analysis Virology Fusion protein Flavivirus Infectious Diseases Recombinant DNA Molecular Medicine Adjuvant |
Zdroj: | Vaccine. 27:995-1001 |
ISSN: | 0264-410X |
DOI: | 10.1016/j.vaccine.2008.11.106 |
Popis: | The main problem in the development of successful vaccines against dengue based on recombinant proteins is the necessity to use potent adjuvants to reach a proper functional immune response. Our group reported the expression, characterization and immunological evaluation of the recombinant protein PD5, which contains the domain III of the Envelope protein from dengue 2 virus fused to the carrier protein P64k. This construct completely protected monkeys against viral challenge when the Freund's adjuvant was employed. Therefore, to define suitable formulations for human use, the present work relies on the evaluation of PD5, produced with a high purity and under GMP conditions, when formulated either with outer membrane vesicles (OMV) or the serogroup A capsular polysaccharide (CPS-A) from Neisseria meningitidis, both adsorbed on aluminium hydroxide. The antibody response to the formulation containing the CPS-A was clearly superior to that of the formulation with OMV. The experiment of in vivo protection supported this evidence, since only the group immunized with PD5 and CPS-A was partially protected upon viral challenge. This is the first study in which the polysaccharide A of N. meningitidis is successfully employed as adjuvant for viral antigens. |
Databáze: | OpenAIRE |
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