Molecular diagnostics and inhibition of cross‐reactive carbohydrate determinants in Hymenoptera venom allergy

Dragana Jovanovic; Aleksandra Peric‐Popadic; Vojislav Djuric; Maja Stojanovic; Branislav Lekic; Ognjen Milicevic; Branka Bonaci‐Nikolic

doi:10.1002/clt2.12230

Clinical and Translational Allergy (Mar 2023)

Molecular diagnostics and inhibition of cross‐reactive carbohydrate determinants in Hymenoptera venom allergy

Dragana Jovanovic,
Aleksandra Peric‐Popadic,
Vojislav Djuric,
Maja Stojanovic,
Branislav Lekic,
Ognjen Milicevic,
Branka Bonaci‐Nikolic

Affiliations

Dragana Jovanovic: Clinic of Allergy and Immunology University Clinical Center of Serbia Belgrade Serbia
Aleksandra Peric‐Popadic: Clinic of Allergy and Immunology University Clinical Center of Serbia Belgrade Serbia
Vojislav Djuric: Clinic of Allergy and Immunology University Clinical Center of Serbia Belgrade Serbia
Maja Stojanovic: Clinic of Allergy and Immunology University Clinical Center of Serbia Belgrade Serbia
Branislav Lekic: University of Belgrade Faculty of Medicine Belgrade Serbia
Ognjen Milicevic: University of Belgrade Faculty of Medicine Belgrade Serbia
Branka Bonaci‐Nikolic: Clinic of Allergy and Immunology University Clinical Center of Serbia Belgrade Serbia

DOI: https://doi.org/10.1002/clt2.12230
Journal volume & issue: Vol. 13, no. 3
pp. n/a – n/a

Abstract

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Abstract Background The composition of venom extracts, cross‐reactive carbohydrate determinants (CCD) and the component‐resolved diagnostics (CRD) are important fields of investigation. IgE‐reactivity to CCD complicates the interpretation of IgE to Hymenoptera venoms, especially in patients with multiple‐positivity. We analyzed the clinical importance of CRD and CCD‐inhibition for selection of allergens for venom immunotherapy (VIT). Methods In 71 patients, we measured specific IgE (sIgE) to honeybee venom (HBV), wasp venom (WV), hornet venom (HV), CCD, and recombinant allergens: phospholipase A2 (rApi m 1), hyaluronidase (rApi m 2), icarapin (rApi m 10), antigen 5 (rVes v 5), and phospholipase A1 (Immunoblot). In 29/71 HBV/WV/HV/CCD‐positive patients CCD‐inhibition was performed. According to CRD and CCD‐inhibition, we identified true sensitization and defined groups of multiple‐positive patients who needed CCD‐inhibition before starting VIT. Results sIgE‐rApi m 1, sIgE‐rApi m 2, and sIgE‐rApi m 10 were detected in 65.7%, 68.4%, and 58%, respectively. In HBV allergic patients, CRD sensitivity was 86.8%. In WV allergic patients, sensitivity of sIgE‐rVes v 5 was 94%. True multiple‐sensitization was found in 44.8% of HBV/WV/HV/CCD‐positive patients after CCD‐inhibition. Patients with multiple venom‐ and CCD‐positivity had more frequent severe allergic reactions (p < 0.001). CCD‐inhibition was helpful in HBV/WV/HV/CCD‐positive patients who were negative to all tested recombinant honeybee allergens. Persistence of HBV‐positivity after CCD‐inhibition requires CRD to other honeybee recombinant allergens. Conclusion CRD, using a profile of five most important recombinant allergens and CCD, has a high sensitivity for the diagnosis of venom allergy, especially in patients positive to several venom extracts. CRD and CCD‐inhibition are helpful to reveal the clinically relevant, true sensitization and improve the selection of venoms for long‐lasting VIT.

Published in Clinical and Translational Allergy

ISSN: 2045-7022 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: https://onlinelibrary.wiley.com/journal/20457022

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