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Cul o 2 specific IgG3/5 antibodies predicted Culicoides hypersensitivity in a group imported Icelandic horses

Cul o 2 specific IgG3/5 antibodies predicted Culicoides hypersensitivity in a group imported Icelandic horses


Titill: Cul o 2 specific IgG3/5 antibodies predicted Culicoides hypersensitivity in a group imported Icelandic horses
Höfundur: Raza, Fahad
Ivanek, Renata
Freer, Heather
Reiche, Dania
Rose, Horst
Torsteinsdóttir, Sigurbjörg   orcid.org/0000-0002-3195-4937
Svansson, Vilhjálmur   orcid.org/0000-0002-3984-4441
Björnsdóttir, Sigríður
Wagner, Bettina   orcid.org/0000-0003-2370-6324
Útgáfa: 2020-08-10
Tungumál: Enska
Umfang: 283
Háskóli/Stofnun: Háskóli Íslands
University of Iceland
Deild: Tilraunastöð í meinafræði að Keldum (HÍ)
Institute for Experimental Pathology, Keldur (UI)
Birtist í: BMC Veterinary Research;16(1)
ISSN: 1746-6148
DOI: 10.1186/s12917-020-02499-w
Efnisorð: Allergy; Biomarkers; Clinical score; Culicoides hypersensitivity; Horse; IgE; IgG; Immunologically naïve; Major allergens; Ofnæmi; Lúsmý; Hestar
URI: https://hdl.handle.net/20.500.11815/2237

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Tilvitnun:

Raza, F., Ivanek, R., Freer, H. et al. Cul o 2 specific IgG3/5 antibodies predicted Culicoides hypersensitivity in a group imported Icelandic horses. BMC Veterinary Research 16, 283 (2020). https://doi.org/10.1186/s12917-020-02499-w

Útdráttur:

Background: Culicoides hypersensitivity (CH) is induced in horses by salivary allergens of Culicoides midges. In Iceland, the causal Culicoides species for CH are not present. Previous epidemiological data indicated that Icelandic horses are more susceptible to CH when they are exported from Iceland and first exposed to Culicoides at adult age. Horses born in countries where Culicoides is endemic, develop the disease less frequently. Here, we established a longitudinal allergy model to identify predictive and diagnostic serological biomarkers of CH. Results: Sixteen adult Icelandic horses from Iceland were imported to the Northeastern United States (US) during the winter and were kept in the same environment with natural Culicoides exposure for the next two years. None of the horses showed clinical allergy during the first summer of Culicoides exposure. In the second summer, 9/16 horses (56%) developed CH. Allergen specific IgE and IgG isotype responses in serum samples were analysed using nine potential Culicoides allergens in a fluorescent bead-based multiplex assay. During the first summer of Culicoides exposure, while all horses were still clinically healthy, Cul o 2 specific IgG3/5 antibodies were higher in horses that developed the allergic disease in the second summer compared to those that did not become allergic (p = 0.043). The difference in Cul o 2 specific IgG3/5 antibodies between the two groups continued to be detectable through fall (p = 0.035) and winter of the first year. During the second summer, clinical signs first appeared and Cul o 3 specific IgG3/5 isotypes were elevated in allergic horses (p = 0.041). Cul o 2 specific IgG5 (p = 0.035), and Cul o 3 specific IgG3/5 (p = 0.043) were increased in late fall of year two when clinical signs started to improve again. Conclusions: Our results identified IgG5 and IgG3/5 antibodies against Cul o 2 and Cul o 3, respectively, as markers for CH during and shortly after the allergy season in the Northeastern US. In addition, Cul o 2 specific IgG3/5 antibodies may be valuable as a predictive biomarker of CH in horses that have been exposed to Culicoides but did not yet develop clinical signs.

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