Immune Responses in Healthy and Allergic Individuals Are Characterized by a Fine Balance between Allergen-specific T Regulatory 1 and T Helper 2 Cells

Author:

Akdis Mübeccel1,Verhagen Johan1,Taylor Alison1,Karamloo Fariba1,Karagiannidis Christian1,Crameri Reto1,Thunberg Sarah12,Deniz Günnur13,Valenta Rudolf4,Fiebig Helmut5,Kegel Christian6,Disch Rainer6,Schmidt-Weber Carsten B.1,Blaser Kurt1,Akdis Cezmi A.1

Affiliation:

1. Swiss Institute of Allergy and Asthma Research, CH-7270 Davos, Switzerland

2. Clinical Immunology and Allergy, Karolinska Hospital, 171 76, Stockholm, Sweden

3. Institute for Experimental Medical Research, Istanbul University, 34280 Istanbul, Turkey

4. Department of Pathophysiology, University of Vienna, Medical School, A-1090 Vienna, Austria

5. Allergopharma Joachim Ganzer KG, D-21462 Reinbek, Germany

6. Clinic for Dermatology and Allergy, CH-7270 Davos, Switzerland

Abstract

The mechanisms by which immune responses to nonpathogenic environmental antigens lead to either allergy or nonharmful immunity are unknown. Single allergen-specific T cells constitute a very small fraction of the whole CD4+ T cell repertoire and can be isolated from the peripheral blood of humans according to their cytokine profile. Freshly purified interferon-γ–, interleukin (IL)-4–, and IL-10–producing allergen-specific CD4+ T cells display characteristics of T helper cell (Th)1-, Th2-, and T regulatory (Tr)1–like cells, respectively. Tr1 cells consistently represent the dominant subset specific for common environmental allergens in healthy individuals; in contrast, there is a high frequency of allergen-specific IL-4–secreting T cells in allergic individuals. Tr1 cells use multiple suppressive mechanisms, IL-10 and TGF-β as secreted cytokines, and cytotoxic T lymphocyte antigen 4 and programmed death 1 as surface molecules. Healthy and allergic individuals exhibit all three allergen-specific subsets in different proportions, indicating that a change in the dominant subset may lead to allergy development or recovery. Accordingly, blocking the suppressor activity of Tr1 cells or increasing Th2 cell frequency enhances allergen-specific Th2 cell activation ex vivo. These results indicate that the balance between allergen-specific Tr1 cells and Th2 cells may be decisive in the development of allergy.

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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