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A recombinant iron transport protein from Bordetella pertussis confers protection against Bordetella parapertussis
Author(s) -
Alvarez Hayes Jimena,
Oviedo Juan Marcos,
Valdez Hugo,
Laborde Juan Martín,
Maschi Fabricio,
Ayala Miguel,
Shah Rohan,
Fernandez Lahore Marcelo,
Rodriguez Maria Eugenia
Publication year - 2017
Publication title -
microbiology and immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.664
H-Index - 70
eISSN - 1348-0421
pISSN - 0385-5600
DOI - 10.1111/1348-0421.12532
Subject(s) - bordetella pertussis , biology , whooping cough , microbiology and biotechnology , recombinant dna , antigen , antibody , virology , immunization , pertussis vaccine , bacteria , immunology , vaccination , gene , genetics
Whooping cough, which is caused by Bordetella pertussis and B. parapertussis, is a reemerging disease. New protective antigens are needed to improve the efficacy of current vaccines against both species. Using proteomic tools, it was here found that B. parapertussis expresses a homolog of AfuA, a previously reported new vaccine candidate against B. pertussis . It was found that this homolog, named AfuA Bpp , is expressed during B. parapertussis infection, exposed on the surface of the bacteria and recognized by specific antibodies induced by the recombinant AfuA cloned from B. pertussis (rAfuA). Importantly, the presence of the O‐antigen, a molecule that has been found to shield surface antigens on B. parapertussis , showed no influence on antibody recognition of AfuA Bpp on the bacterial surface. The present study further showed that antibodies induced by immunization with the recombinant protein were able to opsonize B. parapertussis and promote bacterial uptake by neutrophils. Finally, it was shown that this antigen confers protection against B. parapertussis infection in a mouse model. Altogether, these results indicate that AfuA is a good vaccine candidate for acellular vaccines protective against both causative agents of whooping cough.

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