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Neonatal Fc receptor antagonist efgartigimod safely and sustainably reduces IgGs in humans

Neonatal Fc receptor antagonist efgartigimod safely and sustainably reduces IgGs in humans
Neonatal Fc receptor antagonist efgartigimod safely and sustainably reduces IgGs in humans

BACKGROUND: Intravenous Ig (IVIg), plasma exchange, and immunoadsorption are frequently used in the management of severe autoimmune diseases mediated by pathogenic IgG autoantibodies. These approaches modulating IgG levels can, however, be associated with some severe adverse reactions and a substantial burden to patients. Targeting the neonatal Fc receptor (FcRn) presents an innovative and potentially more effective, safer, and more convenient alternative for clearing pathogenic IgGs.

METHODS: A randomized, double-blind, placebo-controlled first-in-human study was conducted in 62 healthy volunteers to explore single and multiple ascending intravenous doses of the FcRn antagonist efgartigimod. The study objectives were to assess safety, tolerability, pharmacokinetics, pharmacodynamics, and immunogenicity. The findings of this study were compared with the pharmacodynamics profile elicited by efgartigimod in cynomolgus monkeys.

RESULTS: Efgartigimod treatment resulted in a rapid and specific clearance of serum IgG levels in both cynomolgus monkeys and healthy volunteers. In humans, single administration of efgartigimod reduced IgG levels up to 50%, while multiple dosing further lowered IgGs on average by 75% of baseline levels. Approximately 8 weeks following the last administration, IgG levels returned to baseline. Efgartigimod did not alter the homeostasis of albumin or Igs other than IgG, and no serious adverse events related to efgartigimod infusion were observed.

CONCLUSION: Antagonizing FcRn using efgartigimod is safe and results in a specific, profound, and sustained reduction of serum IgG levels. These results warrant further evaluation of this therapeutic approach in IgG-driven autoimmune diseases.

TRIAL REGISTRATION: Clinicaltrials.gov NCT03457649.

FUNDING: argenx BVBA.

Journal Article
0021-9738
4372-4386
Ulrichts, Peter
c255fbf5-bc5c-439a-b95c-096310cb3f14
Guglietta, Antonio
01d44162-bdde-4c4c-ab95-066cf724d590
Dreier, Torsten
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van Bragt, Tonke
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Hanssens, Valérie
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Hofman, Erik
cd3363da-1a9e-4f84-bfcd-35c4563ba51d
Vankerckhoven, Bernhardt
430b3758-f400-4ad2-86de-95e213c40889
Verheesen, Peter
7c5b43bb-487d-435b-9002-31857e0e6cf8
Ongenae, Nicolas
5b2220a0-c737-4ea4-8f3e-c41c0e5009e8
Lykhopiy, Valentina
b826bd4a-a32a-4cb1-9176-75e53ce572c3
Enriquez, F Javier
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Cho, JunHaeng
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Ober, Raimund J
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Ward, E. Sally
b31c0877-8abe-485f-b800-244a9d3cd6cc
de Haard, Hans
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Leupin, Nicolas
69af1e1d-247b-4d1c-80c5-929c8f5cfb3c
Ulrichts, Peter
c255fbf5-bc5c-439a-b95c-096310cb3f14
Guglietta, Antonio
01d44162-bdde-4c4c-ab95-066cf724d590
Dreier, Torsten
2fcf8470-91e6-48c7-975c-2142980fb3ff
van Bragt, Tonke
1c5ac0ae-d34b-443f-9363-5d98f35c514c
Hanssens, Valérie
b5ca92da-b3b0-4b8a-812c-1a40d2653820
Hofman, Erik
cd3363da-1a9e-4f84-bfcd-35c4563ba51d
Vankerckhoven, Bernhardt
430b3758-f400-4ad2-86de-95e213c40889
Verheesen, Peter
7c5b43bb-487d-435b-9002-31857e0e6cf8
Ongenae, Nicolas
5b2220a0-c737-4ea4-8f3e-c41c0e5009e8
Lykhopiy, Valentina
b826bd4a-a32a-4cb1-9176-75e53ce572c3
Enriquez, F Javier
63ceb4bb-07f2-4f87-ae91-76454d48613e
Cho, JunHaeng
10b6b1e9-88ab-4a46-8c81-5e4a594416c3
Ober, Raimund J
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Ward, E. Sally
b31c0877-8abe-485f-b800-244a9d3cd6cc
de Haard, Hans
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Leupin, Nicolas
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Ulrichts, Peter, Guglietta, Antonio, Dreier, Torsten, van Bragt, Tonke, Hanssens, Valérie, Hofman, Erik, Vankerckhoven, Bernhardt, Verheesen, Peter, Ongenae, Nicolas, Lykhopiy, Valentina, Enriquez, F Javier, Cho, JunHaeng, Ober, Raimund J, Ward, E. Sally, de Haard, Hans and Leupin, Nicolas (2018) Neonatal Fc receptor antagonist efgartigimod safely and sustainably reduces IgGs in humans. Journal of Clinical Investigation, 128 (10), 4372-4386. (doi:10.1172/JCI97911).

Record type: Article

Abstract

BACKGROUND: Intravenous Ig (IVIg), plasma exchange, and immunoadsorption are frequently used in the management of severe autoimmune diseases mediated by pathogenic IgG autoantibodies. These approaches modulating IgG levels can, however, be associated with some severe adverse reactions and a substantial burden to patients. Targeting the neonatal Fc receptor (FcRn) presents an innovative and potentially more effective, safer, and more convenient alternative for clearing pathogenic IgGs.

METHODS: A randomized, double-blind, placebo-controlled first-in-human study was conducted in 62 healthy volunteers to explore single and multiple ascending intravenous doses of the FcRn antagonist efgartigimod. The study objectives were to assess safety, tolerability, pharmacokinetics, pharmacodynamics, and immunogenicity. The findings of this study were compared with the pharmacodynamics profile elicited by efgartigimod in cynomolgus monkeys.

RESULTS: Efgartigimod treatment resulted in a rapid and specific clearance of serum IgG levels in both cynomolgus monkeys and healthy volunteers. In humans, single administration of efgartigimod reduced IgG levels up to 50%, while multiple dosing further lowered IgGs on average by 75% of baseline levels. Approximately 8 weeks following the last administration, IgG levels returned to baseline. Efgartigimod did not alter the homeostasis of albumin or Igs other than IgG, and no serious adverse events related to efgartigimod infusion were observed.

CONCLUSION: Antagonizing FcRn using efgartigimod is safe and results in a specific, profound, and sustained reduction of serum IgG levels. These results warrant further evaluation of this therapeutic approach in IgG-driven autoimmune diseases.

TRIAL REGISTRATION: Clinicaltrials.gov NCT03457649.

FUNDING: argenx BVBA.

This record has no associated files available for download.

More information

Accepted/In Press date: 3 July 2018
e-pub ahead of print date: 24 July 2018
Published date: October 2018
Keywords: Journal Article

Identifiers

Local EPrints ID: 424173
URI: http://eprints.soton.ac.uk/id/eprint/424173
DOI: doi:10.1172/JCI97911
ISSN: 0021-9738
PURE UUID: 204b46fc-8ce0-440e-98d7-4fedb1fa2275
ORCID for Raimund J Ober: ORCID iD orcid.org/0000-0002-1290-7430
ORCID for E. Sally Ward: ORCID iD orcid.org/0000-0003-3232-7238

Catalogue record

Date deposited: 05 Oct 2018 11:31
Last modified: 16 Mar 2024 04:37

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Contributors

Author: Peter Ulrichts
Author: Antonio Guglietta
Author: Torsten Dreier
Author: Tonke van Bragt
Author: Valérie Hanssens
Author: Erik Hofman
Author: Bernhardt Vankerckhoven
Author: Peter Verheesen
Author: Nicolas Ongenae
Author: Valentina Lykhopiy
Author: F Javier Enriquez
Author: JunHaeng Cho
Author: Raimund J Ober ORCID iD
Author: E. Sally Ward ORCID iD
Author: Hans de Haard
Author: Nicolas Leupin

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