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Intranasal delivery of a formulation containing stage-specific recombinant proteins of Fasciola hepatica cathepsin L5 and cathepsin B2 triggers an anti-fecundity effect and an adjuvant-mediated reduction in fluke burden in sheep

journal contribution
posted on 2024-11-02, 08:08 authored by Luke Norbury, Katarzyna Basałaj, Anna Zawistowska-Deniziak, Alicja Sielicka, Przemysław Wilkowski, Agnieszka Wesołowska, Peter SmookerPeter Smooker, Halina Wędrychowicz
Fasciola hepatica infection continues to be a major problem in the agriculture sector, particularly in sheep and cattle. Cathepsin L and B proteases are major components of the excretory/secretory material of the parasite, and their roles in several important aspects of parasite invasion and survival has led to their use as targets in rational vaccine design. Previous studies in rats demonstrated that the use of stage-specific antigens, cathepsin B2 and cathepsin L5, as part of a multivalent vaccine, was able to confer significant protection against challenge. In the present study, recombinant versions of cathepsin L5 and cathepsin B2 produced in yeast were used in combination to vaccinate sheep. Intramuscular and intranasal forms of administration were applied, and sheep were subsequently challenged with 150 F. hepatica metacercariae. Intramuscular vaccination was able to induce a strong systemic antibody response against both antigens, but failed to confer significant protection. Conversely, no elevated antibody response was detected against the vaccine antigens following nasal vaccination; however, a reduction in parasite egg viability (>92%) and a statistically significant (p = 0.006), predominantly adjuvant-mediated reduction in worm burdens was observed.

History

Journal

Veterinary Parasitology

Volume

258

Start page

14

End page

23

Total pages

10

Publisher

Elsevier

Place published

Netherlands

Language

English

Copyright

© 2018 Elsevier B.V. All rights reserved.

Former Identifier

2006084456

Esploro creation date

2020-06-22

Fedora creation date

2018-09-20

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