Immunological and clinical factors associated with adverse systemic reactions during the build-up phase of honeybee venom immunotherapy

P Korošec; K Žiberna; M Šilar; M Dežman; N Čelesnik Smodiš; M Rijavec; P Kopač; R Eržen; N Lalek; N Bajrović; M Košnik; M Zidarn

doi:10.1111/cea.12582

Immunological and clinical factors associated with adverse systemic reactions during the build-up phase of honeybee venom immunotherapy

Clin Exp Allergy. 2015 Oct;45(10):1579-89. doi: 10.1111/cea.12582.

Authors

P Korošec¹, K Žiberna¹, M Šilar¹, M Dežman¹, N Čelesnik Smodiš¹, M Rijavec¹, P Kopač¹, R Eržen¹, N Lalek¹, N Bajrović¹, M Košnik¹, M Zidarn¹

Affiliation

¹ University Clinic of Respiratory and Allergic Diseases, Golnik, Slovenia.

PMID: 26046807
DOI: 10.1111/cea.12582

Abstract

Background: Adverse systemic reactions (SRs) are more common in honeybee venom immunotherapy (VIT) than in wasp VIT. Factors that might be associated with SRs during the honeybee VIT are poorly understood.

Objective: Our aim was to evaluate risk factors for SRs during the build-up phase of honeybee venom immunotherapy.

Methods: We included 93 patients who underwent ultra-rush honeybee VIT. The adverse SRs and their severity was compared to various immunological (sIgE, tIgE, basophil CD63 response, baseline tryptase, and skin tests), patient-specific (age, sex, cardiovascular conditions and medications, and other allergic diseases), and sting-specific factors (anaphylaxis severity, time interval to onset of symptoms, and absence of cutaneous symptoms).

Results: Twenty-three patients (24.7%) experienced mild SRs and 13 patients (14%) severe SRs. In five patients with severe SRs, the build-up was stopped. High basophil allergen sensitivity, evaluated as dose-response curve metrics of EC15, EC50, CD-sens, AUC, or the response to submaximal 0.01 μg/mL of venom concentration, was the most significant risk factor and only independent predictor of severe SRs and/or build-up stop. Time interval of <5 min after sting to onset of symptoms and lower specific IgEs to rApi m1 was also associated with severe SRs. There was no difference in other immunological, patient-specific, or sting-specific factors, including the baseline tryptase. None of the studied factors was associated with mild SRs.

Conclusion and clinical relevance: High basophil allergen CD63 sensitivity phenotype was a major indicator of severe adverse SRs during the build-up phase of honeybee VIT. Possibly role was also showed for short latency to filed sting reaction and low sIgE to rApi m1. Before honeybee VIT, measurement of basophil allergen sensitivity should be used to identify patients with a high risk for severe side-effects.

Keywords: CD63; IgE; adverse systemic reactions; basophils; honeybee venom allergy; immunotherapy; risk factors.

Publication types

Clinical Trial
Comparative Study

MeSH terms

Adolescent
Adult
Aged
Basophils / immunology*
Basophils / metabolism
Bee Venoms / administration & dosage
Bee Venoms / adverse effects*
Dose-Response Relationship, Drug
Female
Humans
Hypersensitivity / blood
Hypersensitivity / immunology*
Immunotherapy / adverse effects*
Male
Middle Aged
Tetraspanin 30 / blood
Tetraspanin 30 / immunology*

Substances

Bee Venoms
Tetraspanin 30