Peripheral blood dendritic cells express Fc ε RI as a complex composed of Fc ε RI α- and Fc ε RI γ-chains and can use this receptor for IgE-mediated allergen presentation

Dieter Maurer(Medical University of Vienna), S Fiebiger(Medical University of Vienna), C. Ebner(Medical University of Vienna), Bärbel Reininger(Medical University of Vienna), G. Fischer(Medical University of Vienna), Sibylle Wichlas(Medical University of Vienna), M H Jouvin(Medical University of Vienna), Marcus Schmitt‐Egenolf(Medical University of Vienna), Dietrich Kraft(Medical University of Vienna), J.-P. Kinet(Medical University of Vienna), G Stingl(Medical University of Vienna)
The Journal of Immunology
July 1, 1996
Cited by 334

Abstract

Originally limited to basophils and mast cells, the spectrum of high affinity IgE receptor (Fc epsilon RI-bearing cells has expanded recently to include Langerhans cells, dermal dendritic cells (DC), monocytes, and eosinophils. As a result of studies on the distribution, structure, and function of Fc epsilon RI on APCs, we discovered a minor nonbasophil, nonmonocyte PBMC population that can bind IgE via Fc epsilon RI. This receptor occurs on the surface of these cells as a multimeric structure containing Fc epsilon RI alpha- and Fc epsilon RI gamma-chains but, unlike its counterpart on basophils, lacking Fc epsilon RI beta. Further experiments revealed that these Fc epsilon RI alpha gamma-expressing cells closely resemble peripheral blood DC by immunophenotype (HLA-DRhigh, HLA-DQhhigh; CD4+, CD11a+, CD32+, CD33+, B7/2 (CD86)+; CD11blow, CD14low, CD40low, CD54low, CD64low) and cell morphology. These features allowed us to isolate Fc epsilon RI-expressing DC from the peripheral blood and to investigate their immunostimulatory properties. We found Fc epsilon RI-positive DC to be efficient stimulators of both primary (allogeneic MLR) and Fc epsilon RI/IgE-dependent, secondary T cell responses at low cell numbers. Thus, Fc epsilon RI-expressing DC may not only amplify established type I allergic immune reactions but, unlike Fc epsilon RI-positive semiprofessional APCs, may be able to prime naive T cells to common and/or cryptic epitopes of IgE-reactive Ags.


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