Characterization of IgA and IgM binding and internalization by surface-expressed human Fcα/μ receptor

► Recombinant human Fcα/μreceptor expressed on surface of human cell line. ► Dissociation constants for binding of human IgA and IgM to Fcα/μR are reported. ► IgM polymers do not require J chain for binding to Fcα/μR. ► IgA lacking N-linked glycans can associate with Fcα/μR. ► IgA can be internalized by Fcα/μR. The Fcα/μ receptor (Fcα/μR) is an unusual Fc receptor in that it binds to two different antibody isotypes, IgA and IgM. This receptor is of interest because it is thought to be involved in the capture of IgA- and IgM-immune complexes and antigen presentation. To further characterize this receptor, we were able to stably express human Fcα/μR on the surface of the 293T cell line. Using this system, we determined the affinity of the interactions of the receptor with IgA and IgM, which led to novel insights including the important finding that IgM polymers can bind to human Fcα/μR in the absence of J chain. This is in contrast to the polymeric immunoglobulin receptor (pIgR), which requires the presence of J chain to bind to polymeric IgA and IgM. The dissociation constants (Kd) of all of the different human IgA isotypes and allotypes for human Fcα/μR were determined, and we show that the N-linked glycans on IgA1 are not required for binding to the receptor. In addition, we demonstrate that IgA can be rapidly internalized by human Fcα/μR in the presence of cross-linking antibody.