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Journal of Allergy and Clinical Immunology 2005-Oct

Antigen-specific targeting and elimination of EBV-transformed B cells by allergen toxins.

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Michael Stöcker
Torsten Klockenbring
Michael Huhn
Thomas Nachreiner
Daniel Wicklein
Arnd Petersen
Ralf Bauer
Roland Goerlich
Rainer Fischer
Stefan Barth

Keywords

Abstract

BACKGROUND

With the exception of antigen-specific immunotherapy, current treatments for atopic diseases provide only symptomatic relief. Because of the increasing incidence of such diseases, the development of novel strategies and concepts for the treatment of allergies is urgently needed.

OBJECTIVE

Here we present a new approach for the treatment of atopic diseases. The strategy is comparable to the application of immunotoxins in cancer therapy, in which a cytotoxic peptide is coupled to a cancer cell-specific antibody fragment or ligand. In the case of so-called allergen toxins (ATs), the target cell-specific moiety is an allergen or allergen-derived fragment, which should be bound only by allergen-reactive cells. After receptor-mediated internalization, allergen-specific cells are killed, and the allergic pathogenesis is interrupted.

METHODS

Proof of the AT principle was shown by using a human ex vivo system in which EBV was used to transform human B cells specific for the timothy grass pollen allergen Phl p 5b. The AT is composed of the major B-cell and T-cell epitopes of the Phl p 5b (P5) allergen fused to a truncated form of the highly toxic Pseudomonas aeruginosa exotoxin A (ETA').

RESULTS

Allergen-specific and nonspecific B cells were challenged with P5-ETA', but only the Phl p 5b-reactive B cells showed selective binding and cytotoxicity.

CONCLUSIONS

This approach represents an initial step toward a novel therapeutic strategy in the treatment of atopic diseases.

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