Cotranslational endoplasmic reticulum assembly of FcεRI controls the formation of functional IgE-binding receptors

Abstract

The human high affinity receptor for IgE (FcεRI) is a cell surface structure critical for the pathology of allergic reactions. Human FcεRI is expressed as a tetramer (αβγ₂) on basophils or mast cells and as trimeric (αγ₂) complex on antigen-presenting cells. Expression of the human α subunit can be down-regulated by a splice variant of FcεRIβ (β_var). We demonstrate that FcεRIα is the core subunit with which the other subunits assemble strictly cotranslationally. In addition to αβγ₂ and αγ₂, we demonstrate the presence of αβ and αβ_varγ₂ complexes that are stable in the detergent Brij 96. The role of individual FcεRI subunits for the formation of functional, immunoglobulin E–binding FcεRI complexes during endoplasmic reticulum (ER) assembly can be defined as follows: β and γ support ER insertion, signal peptide cleavage and proper N-glycosylation of α, whereas β_var allows accumulation of α protein backbone. We show that assembly of FcεRI in the ER is a key step for the regulation of surface expression of FcεRI. The ER quality control system thus regulates the quantity of functional FcεRI, which in turn controls onset and persistence of allergic reactions.