Mould allergen Alt a 1 spiked with the micronutrient retinoic acid reduces Th2 response and ameliorates Alternaria allergy in BALB/c mice

Author:

Fakhimahmadi Aila12ORCID,Roth‐Walter Franziska12ORCID,Hofstetter Gerlinde1ORCID,Wiederstein Markus3ORCID,Jensen Sebastian A.14ORCID,Berger Markus1,Szepannek Nathalie1,Bianchini Rodolfo1ORCID,Pali‐Schöll Isabella12ORCID,Jensen‐Jarolim Erika1245ORCID,Hufnagl Karin124ORCID

Affiliation:

1. Messerli Research Institute, Department of Interdisciplinary Life Sciences University of Veterinary Medicine Vienna Austria

2. Institute of Pathophysiology and Allergy Research, Center of Pathophysiology, Infectiology and Immunology Medical University of Vienna Vienna Austria

3. Department of Biosciences and Medical Biology University of Salzburg Salzburg Austria

4. AllergyCare Allergy Diagnosis Center Private Clinic Döbling Vienna Austria

5. Biomedical International R+D GmbH Vienna Austria

Abstract

AbstractBackgroundWe investigated the biological function of the mould allergen Alt a 1 as a carrier of micronutrients, such as the vitamin A metabolite retinoic acid (RA) and the influence of RA binding on its allergenicity in vitro and in vivo.MethodsAlt a 1‐RA complex formation was analyzed in silico and in vitro. PBMCs from Alternaria‐allergic donors were stimulated with Alt a 1 complexed with RA (holo‐Alt a 1) or empty apo‐Alt a 1 and analyzed for cytokine production and CD marker expression. Serum IgE‐binding and crosslinking assays to apo‐ and holo‐protein were correlated to B‐cell epitope analysis. Female BALB/c mice already sensitized to Alt a 1 were intranasally treated with apo‐Alt a 1, holo‐Alt a 1 or RA alone before measuring anaphylactic response, serum antibody levels, splenic cytokines and CD marker expression.ResultsIn silico docking calculations and in vitro assays showed that the extent of RA binding depended on the higher quaternary state of Alt a 1. Holo‐Alt a 1 loaded with RA reduced IL‐13 released from PBMCs and CD3+CD4+CRTh2 cells. Complexing Alt a 1 to RA masked its IgE B‐cell epitopes and reduced its IgE‐binding capacity. In a therapeutic mouse model of Alternaria allergy nasal application of holo‐Alt a 1, but not of apo‐Alt a 1, significantly impeded the anaphylactic response, impaired splenic antigen‐presenting cells and induced IL‐10 production.ConclusionHolo‐Alt a 1 binding to RA was able to alleviate Th2 immunity in vitro, modulate an ongoing Th2 response and prevent anaphylactic symptoms in vivo, presenting a novel option for improving allergen‐specific immunotherapy in Alternaria allergy.

Publisher

Wiley

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