In these studies, we characterize an Fc receptor (FcR) for IgA that is present on human granulocytes, monocyte/macrophages, and their corresponding cell lines. Receptor expression appears to be constitutive but can be selectively upregulated on monocyte cell lines by stimulation with a phorbol ester and polymeric IgA. Both the induction requirements and ligand specificity of the IgA receptor differ from the IgG receptors, Fc gamma R I, II, and III, that are also expressed on monocytes and granulocytes. IgA binding to the cell surface receptor is mediated via the Fc alpha region. The Fc alpha R is a heterogenously charged, approximately 60-kD molecule with an isoelectric point of 4.5-5.6 that binds monomeric or polymeric IgA1 and IgA2 molecules. This transmembrane glycoprotein appears to be composed of 32- and 36-kD protein cores with multiple N-linked carbohydrate moieties. We conclude that this Fc alpha R represents a novel member of the FcR family that may have a distinctive role in host defense.
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1 March 1990
Article|
March 01 1990
Cellular distribution, regulation, and biochemical nature of an Fc alpha receptor in humans.
In Special Collection:
2019 Lasker Prize Collection
R C Monteiro,
R C Monteiro
Department of Medicine, University of Alabama, Birmingham 35294.
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H Kubagawa,
H Kubagawa
Department of Medicine, University of Alabama, Birmingham 35294.
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M D Cooper
M D Cooper
Department of Medicine, University of Alabama, Birmingham 35294.
Search for other works by this author on:
R C Monteiro
Department of Medicine, University of Alabama, Birmingham 35294.
H Kubagawa
Department of Medicine, University of Alabama, Birmingham 35294.
M D Cooper
Department of Medicine, University of Alabama, Birmingham 35294.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1990) 171 (3): 597–613.
Citation
R C Monteiro, H Kubagawa, M D Cooper; Cellular distribution, regulation, and biochemical nature of an Fc alpha receptor in humans.. J Exp Med 1 March 1990; 171 (3): 597–613. doi: https://doi.org/10.1084/jem.171.3.597
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