Literature DB >> 20600517

Protection against pneumonic plague following oral immunization with a non-replicating vaccine.

Abby Jones1, Catharine Bosio, Angela Duffy, Andrew Goodyear, Martin Schriefer, Steven Dow.   

Abstract

Yersinia pestis is a dangerous bacterial pathogen that when inhaled can rapidly induce fatal pneumonic plague. Thus, there is a need for stable, safe, and easily administered mucosal vaccines capable of eliciting effective protection against pulmonary Y. pestis infections. Cationic liposome-nucleic acid complexes (CLDC) have been shown previously to be effective vaccine adjuvants for parenteral immunization, but have not been previously evaluated for use in oral immunization. Therefore, we investigated the ability of an orally administered CLDC adjuvanted vaccine to elicit protective immunity against lethal pneumonic plague. C57Bl/6 mice were vaccinated orally or subcutaneously using 10mug Y. pestis F1 antigen combined with CLDC and immune responses and protection from challenge was assessed. We found that oral immunization elicited high titers of anti-F1 antibodies, equivalent to those generated by parenteral immunization. Importantly, orally immunized mice were protected from lethal pulmonary challenge with virulent Y. pestis for up to 18 weeks following vaccination. Vaccine-induced protection following oral immunization was found to be dependent primarily on CD4+ T cells, with a partial contribution from CD8+ T cells. Thus, CLDC adjuvanted vaccines represent a new type of orally administered, non-replicating vaccine capable of generating effective protection against pulmonary infection with virulent Y. pestis.

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Year:  2010        PMID: 20600517      PMCID: PMC3398427          DOI: 10.1016/j.vaccine.2010.06.020

Source DB:  PubMed          Journal:  Vaccine        ISSN: 0264-410X            Impact factor:   3.641


  50 in total

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  10 in total

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Review 7.  Plague Vaccine Development: Current Research and Future Trends.

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8.  Non-specific protection from respiratory tract infections in cattle generated by intranasal administration of an innate immune stimulant.

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9.  Local immune and microbiological responses to mucosal administration of a Liposome-TLR agonist immunotherapeutic in dogs.

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Review 10.  Vaccine Potentiation by Combination Adjuvants.

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