Targeting Ara h 2 with human‐derived monoclonal antibodies prevents peanut‐induced anaphylaxis in mice

Author:

Paolucci Marta1ORCID,Wuillemin Natascha2,Homère Valentine1,Bieli Dimitri2,Köhli Alice3,Ballmer‐Weber Barbara4,Waeckerle‐Men Ying1,Pengo Niccolò2ORCID,Kündig Thomas M.14,Sonati Tiziana2,Johansen Pål14ORCID

Affiliation:

1. Department of Dermatology University of Zurich Zurich Switzerland

2. Mabylon AG Schlieren Switzerland

3. Division of Allergology University Children's Hospital Zurich Zurich Switzerland

4. Department of Dermatology University Hospital Zurich Zurich Switzerland

Abstract

AbstractBackgroundPeanut allergy is a type‐I hypersensitivity immune reaction mediated by the binding of peanut allergens to IgE‐FcεRI complexes on mast cells and basophils and by their subsequent cellular degranulation. Of all major peanut allergens, Ara h 2 is considered the most anaphylactic. With few options but allergen avoidance, effective treatment of allergic patients is needed. Passive immunotherapy (herein called PIT) based on prophylactic administration of peanut‐specific monoclonal antibodies (mAbs) may present a promising treatment option for this under‐served disease.MethodFully human recombinant anti‐peanut IgG mAbs were tested in mice sensitized to peanut allergen extract. Allergic mice received intravenous immunotherapy with anti‐peanut Ara h 2‐specific IgG1 or IgG4 mAbs cocktails, and were then challenged by a systemic injection of high‐dose peanut allergen extract. The protection from allergic anaphylaxis was measured by monitoring the core body temperature.ResultsPIT with peanut‐specific mAbs was associated with a significant and dose‐dependent reduction of anaphylactic reactions in peanut‐sensitized mice challenged with peanut allergen extract. Complete protection was observed at doses approximately 0.3–0.6 mg mAbs. Mixtures of mAbs were more effective than single mAbs, and effective treatment could be obtained with mAbs of both IgG1 and IgG4 subclasses. The therapeutic effect of anti‐Ara h 2 mAbs was based on allergen neutralization and independent of the Fcγ receptor and mast‐cell inhibition.ConclusionThis is the first report that shows that human‐derived anti‐peanut mAbs can prevent allergic anaphylaxis in mice. The study demonstrates that neutralizing allergenic epitopes on Ara h 2 by mAbs may represent a promising treatment option in peanut‐allergy.

Funder

Universität Zürich

Publisher

Wiley

Subject

Immunology,Immunology and Allergy

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