Dependence of antibody-mediated presentation of antigen on FcRn

Qiao, Shuo‐Wang; Kobayashi, Katsuaki; Johansen, Finn–Eirik; Sollid, Ludvig M.; Andersen, Jan Terje; Milford, Edgar L.; Roopenian, Derry C.; Lencer, Wayne I.; Blumberg, Richard S.

doi:10.1073/pnas.0801717105

Cited by 231 publications

(318 citation statements)

References 32 publications

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“…Kinetic rate values were calculated using predefined models (Langmuir 1:1 ligand model, heterogeneous ligand model, and steady-state affinity model) provided by using BIAevaluation 4.1 software. The closeness of the fit, described by the statistical value 2 , which represents the mean square, was lower than 2.0 in all affinity estimations.…”

Section: Construction Of Mutant Fcrn Variants-mentioning

confidence: 67%

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Cross-species Binding Analyses of Mouse and Human Neonatal Fc Receptor Show Dramatic Differences in Immunoglobulin G and Albumin Binding

Andersen

Daba

Berntzen

et al. 2010

Journal of Biological Chemistry

171

172

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The neonatal Fc receptor (FcRn) regulates the serum half-life of both IgG and albumin through a pH-dependent mechanism that involves salvage from intracellular degradation. WT bound strongly to human IgG1. The latter pair also interacted at physiological pH with calculated affinity in the micromolar range. In all cases, binding of albumin and IgG from either species to both receptors were additive. Cross-species albumin binding differences could partly be explained by nonconserved amino acids found within the ␣2-domain of the receptor. Such distinct cross-species FcRn binding differences must be taken into consideration when IgG-and albumin-based therapeutics and diagnostics are evaluated in rodents for their pharmacokinetics.

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Section: Construction Of Mutant Fcrn Variants-mentioning

confidence: 67%

“…Moreover, the receptor plays a role in antibody-mediated antigen presentation by dendritic cells (2). FcRn has also been found to salvage albumin from intracellular degradation (3), in a fashion similar to that described for IgG, which involves receptor ligand interactions in acidified endosomal compartments (1).…”

mentioning

confidence: 99%

Cross-species Binding Analyses of Mouse and Human Neonatal Fc Receptor Show Dramatic Differences in Immunoglobulin G and Albumin Binding

Andersen

Daba

Berntzen

et al. 2010

Journal of Biological Chemistry

171

172

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“…3,4 FcRn-IgG interaction also functions in antigen presentation and cross-presentation in macrophage and dendritic cells. 5,6 Each of these functions has important implications in therapeutic antibody development. Detailed review of the biology of FcRn function has also been covered elsewhere.…”

Section: Fundamental Biology Of Fcrnmentioning

confidence: 99%

“…35 In dendritic cells, FcRn can mediate antigen presentation and cross-presentation, functions that are critical for adaptive immunity and potential therapeutic immunization process. 5,6 Vascular endothelium. By conditional deletion of FcRn in mice using Cre recombinase under the control of the Tie2 promoter, it was demonstrated that FcRn in the vascular endothelium and hematopoietic cells are the major sites for maintaining IgG homeostasis.…”

Section: Fcrn Functions In Organsmentioning

confidence: 99%

Neonatal Fc receptor and IgG-based therapeutics

Kuo

Aveson²

2011

mAbs

200

191

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“…FcRn has been detected in numerous types of polarized epithelia, including those from the intestines, lung, breast, and kidney, as well as other parenchymal cells, including hepatocytes, endothelial cells, and hematopoietic cells, where it is expressed in dendritic cells, monocytes, macrophages, polymorphonuclear leukocytes, and, perhaps, B cells (7,8). FcRn protects monomeric IgG and albumin from degradation in both parenchymal and hematopoietic cells, is responsible for the bidirectional transcytosis of IgG and IgG antigen/antibody complexes across polarized epithelia, and, finally, directs immune complexes to lysosomes in dendritic cells for facilitation of antigen presentation (9,10).…”

mentioning

confidence: 99%

N-Glycan Moieties in Neonatal Fc Receptor Determine Steady-state Membrane Distribution and Directional Transport of IgG

Kuo

Muinck

Claypool

et al. 2009

Journal of Biological Chemistry

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The neonatal Fc receptor (FcRn) is a major histocompatibility complex class I-related molecule known to protect IgG and albumin from catabolism and transport IgG across polarized epithelial cells in a bidirectional manner. Previous studies have shown species-specific differences in ligand binding, IgG transport direction, and steady-state membrane distribution when expressed in polarized epithelial cells. We hypothesized that these differences may be due to the additional N-glycans expressed on the rat Mutant human FcRn clones that contained additional N-glycan side-chain modifications, including that which was fully rodentized, still exhibited specificity for human IgG and failed to bind to mouse IgG. At steady state, the mutant human FcRn with additional N-glycans redistributed to the apical cell surface similar to that of rat FcRn. Furthermore, the rodentized human FcRn exhibited a reversal of IgG transport with predominant transcytosis from an apical-to-basolateral direction, which resembled that of the rat FcRn isoform. These studies show that the N-glycans in FcRn contribute significantly to the steady-state membrane distribution and direction of IgG transport in polarized epithelia. The neonatal Fc receptor (FcRn)2 was originally proposed by Brambell and colleagues to be the Fc receptor responsible for transfer of IgG through neonatal rodent intestinal epithelium and yolk sac of pregnant rabbits more than three decades ago (1). These functional properties were confirmed to be mediated by FcRn with the subsequent isolation from neonatal rat intestinal brush borders followed by the cloning of the rat homologue identified as a 50-kDa major histocompatibility complex class I-related heavy chain in non-covalent association with a 12-kDa subunit consistent with

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Dependence of antibody-mediated presentation of antigen on FcRn

Cited by 231 publications

References 32 publications

Cross-species Binding Analyses of Mouse and Human Neonatal Fc Receptor Show Dramatic Differences in Immunoglobulin G and Albumin Binding

Cross-species Binding Analyses of Mouse and Human Neonatal Fc Receptor Show Dramatic Differences in Immunoglobulin G and Albumin Binding

Neonatal Fc receptor and IgG-based therapeutics

N-Glycan Moieties in Neonatal Fc Receptor Determine Steady-state Membrane Distribution and Directional Transport of IgG

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