Differential effects of FcRn antagonists on the subcellular trafficking of FcRn and albumin
Differential effects of FcRn antagonists on the subcellular trafficking of FcRn and albumin
The homeostasis of IgG is maintained by the neonatal Fc receptor, FcRn. Consequently, antagonism of FcRn to reduce endogenous IgG levels is an emerging strategy for treating antibody-mediated autoimmune disorders using either FcRn-specific antibodies or an engineered Fc fragment. For certain FcRn-specific antibodies, this approach has resulted in reductions in the levels of serum albumin, the other major ligand transported by FcRn. Cellular and molecular analyses of a panel of FcRn antagonists have been carried out to elucidate the mechanisms leading to their differential effects on albumin homeostasis. These analyses have identified 2 processes underlying decreases in albumin levels during FcRn blockade: increased degradation of FcRn and competition between antagonist and albumin for FcRn binding. These findings have potential implications for the design of drugs to modulate FcRn function.
Autoimmune diseases, Autoimmunity, Immunoglobulins, Immunology
Ma, Guanglong
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Crowley, Andrew R.
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Heyndrickx, Liesbeth
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Rogiers, Isle
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Parthoens, Eef
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Van Santbergen, Jolien
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Ober, Raimund J.
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Bobkov, Vladimir
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de Haard, Hans
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Ulrichts, Peter
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Hofman, Erik
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Louagie, Els
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Balbino, Bianca
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Ward, E. Sally
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7 May 2024
Ma, Guanglong
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Crowley, Andrew R.
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Heyndrickx, Liesbeth
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Rogiers, Isle
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Parthoens, Eef
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Van Santbergen, Jolien
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Ober, Raimund J.
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Bobkov, Vladimir
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de Haard, Hans
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Ulrichts, Peter
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Hofman, Erik
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Louagie, Els
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Balbino, Bianca
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Ward, E. Sally
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Ma, Guanglong, Crowley, Andrew R., Heyndrickx, Liesbeth, Rogiers, Isle, Parthoens, Eef, Van Santbergen, Jolien, Ober, Raimund J., Bobkov, Vladimir, de Haard, Hans, Ulrichts, Peter, Hofman, Erik, Louagie, Els, Balbino, Bianca and Ward, E. Sally
(2024)
Differential effects of FcRn antagonists on the subcellular trafficking of FcRn and albumin.
JCI Insight, 9 (10), [e176166].
(doi:10.1172/jci.insight.176166).
Abstract
The homeostasis of IgG is maintained by the neonatal Fc receptor, FcRn. Consequently, antagonism of FcRn to reduce endogenous IgG levels is an emerging strategy for treating antibody-mediated autoimmune disorders using either FcRn-specific antibodies or an engineered Fc fragment. For certain FcRn-specific antibodies, this approach has resulted in reductions in the levels of serum albumin, the other major ligand transported by FcRn. Cellular and molecular analyses of a panel of FcRn antagonists have been carried out to elucidate the mechanisms leading to their differential effects on albumin homeostasis. These analyses have identified 2 processes underlying decreases in albumin levels during FcRn blockade: increased degradation of FcRn and competition between antagonist and albumin for FcRn binding. These findings have potential implications for the design of drugs to modulate FcRn function.
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Differential effects of FcRn antagonists on the subcellular
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Accepted/In Press date: 10 April 2024
e-pub ahead of print date: 23 April 2024
Published date: 7 May 2024
Keywords:
Autoimmune diseases, Autoimmunity, Immunoglobulins, Immunology
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Local EPrints ID: 491029
URI: http://eprints.soton.ac.uk/id/eprint/491029
ISSN: 2379-3708
PURE UUID: f510f8de-4c6a-4256-95fe-b946533a032c
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Date deposited: 11 Jun 2024 16:40
Last modified: 12 Jun 2024 02:04
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Contributors
Author:
Guanglong Ma
Author:
Andrew R. Crowley
Author:
Liesbeth Heyndrickx
Author:
Isle Rogiers
Author:
Eef Parthoens
Author:
Jolien Van Santbergen
Author:
Vladimir Bobkov
Author:
Hans de Haard
Author:
Peter Ulrichts
Author:
Erik Hofman
Author:
Els Louagie
Author:
Bianca Balbino
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