Influence of Bee Venom Immunotherapy on Degranulation and Leukotriene Generation in Human Blood Basophils

Overview

Journal Clin Exp Allergy

Specialty Allergy & Immunology

Date 1996 Oct 1

PMID 8911695

Citations 16

Authors

M Jutel

U R Muller

M Fricker

S Rihs

W J Pichler

C Dahinden

Affiliations

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Abstract

Background: Rapid clinical tolerance can be induced over several hours by very fast bee venom immunotherapy (VIT) protocols.

Objective: To investigate the mechanisms underlying VIT we examined the changes of blood basophil responsiveness during VIT.

Methods: Seven bee venom allergic patients with a history of severe systemic reactions after a bee sting were investigated. A cumulative dose of 111.1 micrograms bee venom (BV) was administered sc over 3.5 h under intensive care conditions according to an ultra-rush protocol. The release of histamine and the formation of leukotrienes in response to BV, major BV allergen Phospholipase A2 (PLA), IgE receptor cross-linking with the use of monoclonal antibodies against IgE and IgE receptor, as well as IgE independent activation in response to C5a were determined in vitro before and after ultra-rush VIT.

Results: We demonstrated a decrease of total histamine in peripheral blood leucocytes just after VIT. Histamine release in response to all the stimuli used is not affected by ultra-rush VIT, if expressed as per cent release of total histamine. However, the absolute amount product released in response to stimulation was decreased, particularly with allergen (BV, PLA). We also found a significant reduction of LTC4 formation after VIT in samples stimulated with specific allergen (BV, PLA).

Conclusion: Blood basophils are a target for VIT, which induces impaired release of both preformed and newly generated mediators. However, we believe the basic mechanisms of rapid clinical tolerance induced by ultra-rush VIT remain to be investigated.

Citing Articles

Venom Immunotherapy: Immune Mechanisms of Induced Protection and Tolerance.

Luzar A, Korosec P, Kosnik M, Zidarn M, Rijavec M Cells. 2021; 10(7).

PMID: 34206562 PMC: 8306808. DOI: 10.3390/cells10071575.

Clinical Utility of Rush Venom Immunotherapy: Current Status.

Gruzelle V, Mailhol C, Waters D, Guilleminault L J Asthma Allergy. 2020; 13:1-10.

PMID: 32021308 PMC: 6954838. DOI: 10.2147/JAA.S200917.

Hymenoptera Venom Allergy: How Does Venom Immunotherapy Prevent Anaphylaxis From Bee and Wasp Stings?.

Sahiner U, Durham S Front Immunol. 2019; 10:1959.

PMID: 31497015 PMC: 6712168. DOI: 10.3389/fimmu.2019.01959.

The efficacy of oral and subcutaneous antigen-specific immunotherapy in murine cow's milk- and peanut allergy models.

Vonk M, Wagenaar L, Pieters R, Knippels L, Willemsen L, Smit J Clin Transl Allergy. 2017; 7:35.

PMID: 29021893 PMC: 5622477. DOI: 10.1186/s13601-017-0170-y.

Short-, Intermediate-, and Long-Term Changes in Basophil Reactivity Induced by Venom Immunotherapy.

Trabado A, Camara Hijon C, Ramos Cantarino A, Romero-Chala S, Garcia-Trujillo J, Pereira L Allergy Asthma Immunol Res. 2016; 8(5):412-20.

PMID: 27334779 PMC: 4921695. DOI: 10.4168/aair.2016.8.5.412.