AI Article Synopsis

  • Ticks need blood from vertebrates for survival, which increases hydrogen peroxide levels that can be damaging, so they use antioxidant enzymes like peroxiredoxins to manage this.
  • This study evaluated the potential of a tick peroxiredoxin (HlPrx2) as a vaccine candidate by expressing it in E. coli, confirming its purity and safety, and testing its ability to stimulate an immune response in mice.
  • The results showed that rHlPrx2 could provoke an immune response in mice, though it did not significantly impact the nymphal ticks, suggesting that it still holds potential as a vaccine candidate against ticks due to its immunogenic properties.

Article Abstract

Ticks require blood feeding on vertebrate animals throughout their life cycle, and also concentrate the iron-containing blood, resulting in a high concentration of hydrogen peroxide (HO). High concentrations of HO are harmful to organisms, due to their serious damage of macromolecules. Ticks have antioxidant enzymes, such as peroxiredoxins (Prxs), that scavenge HO. Prxs may have important roles in regulating the HO concentration in ticks during blood feeding and oviposition. Moreover, Prxs are considered potential vaccine candidates in other parasites, such as Leishmania and Fasciola. In the present study, the efficacy of a tick Prx (HlPrx2) as a vaccine candidate antigen was evaluated. First, recombinant HlPrx2 (rHlPrx2) was expressed in Escherichia coli, and then, its purity and endotoxin levels were confirmed prior to administration. The rHlPrx2 proteins were of high purity with acceptably low endotoxin levels. Second, the ability of rHlPrx2 administration to stimulate mouse immunity was evaluated. The rHlPrx2 protein, with or without an adjuvant, could stimulate immunity in mice, especially the IgG1 of Th2 immune response. Using Western blot analysis, we also observed whether rHlPrx2-immunized mice sera could recognize native HlPrx2 protein in crude tick midgut proteins. Western blot analysis demonstrated that rHlPrx2-administrated mouse sera could detect the native HlPrx2. Finally, the effects of rHlPrx2 immunization in mice were studied using nymphal ticks. Although the challenged ticks were not affected by rHlPrx2 immunization, rHlPrx2 still might be considered as a vaccine candidate against ticks because of its high immunogenicity.

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http://dx.doi.org/10.1007/s10493-018-0209-3DOI Listing

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