Phase 2 study of efgartigimod, a novel FcRn antagonist, in adult patients with primary immune thrombocytopenia
Phase 2 study of efgartigimod, a novel FcRn antagonist, in adult patients with primary immune thrombocytopenia
Primary immune thrombocytopenia (ITP) is an acquired autoimmune bleeding disorder, characterized by a low platelet count (<100 × 10
9/L) in the absence of other causes associated with thrombocytopenia. In most patients, IgG autoantibodies directed against platelet receptors can be detected. They accelerate platelet clearance and destruction, inhibit platelet production, and impair platelet function, resulting in increased risk of bleeding and impaired quality of life. Efgartigimod is a human IgG1 antibody Fc-fragment, a natural ligand of the neonatal Fc receptor (FcRn), engineered for increased affinity to FcRn, while preserving its characteristic pH-dependent binding. Efgartigimod blocks FcRn, preventing IgG recycling, and causing targeted IgG degradation. In this Phase 2 study, 38 patients were randomized 1:1:1 to receive four weekly intravenous infusions of either placebo (N = 12) or efgartigimod at a dose of 5 mg/kg (N = 13) or 10 mg/kg (N = 13). This short treatment cycle of efgartigimod in patients with ITP, predominantly refractory to previous lines of therapy, was shown to be well tolerated, and demonstrated a favorable safety profile consistent with Phase 1 data. Efgartigimod induced a rapid reduction of total IgG levels (up to 63.7% mean change from baseline), which was associated with clinically relevant increases in platelet counts (46% patients on efgartigimod vs 25% on placebo achieved a platelet count of ≥50 × 10
9/L on at least two occasions, and 38% vs 0% achieved ≥50 × 10
9/L for at least 10 cumulative days), and a reduced proportion of patients with bleeding. Taken together, these data warrant further evaluation of FcRn antagonism as a novel therapeutic approach in ITP.
178-187
Newland, Adrian C.
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Sánchez‐González, Blanca
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Rejtő, László
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Egyed, Miklos
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Romanyuk, Nataliya
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Godar, Marie
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Verschueren, Katrien
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Gandini, Domenica
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Ulrichts, Peter
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Beauchamp, Jon
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Dreier, Torsten
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Ward, E. Sally
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Michel, Marc
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Liebman, Howard A.
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Haard, Hans
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Leupin, Nicolas
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Kuter, David J.
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1 February 2020
Newland, Adrian C.
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Sánchez‐González, Blanca
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Rejtő, László
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Egyed, Miklos
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Romanyuk, Nataliya
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Godar, Marie
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Verschueren, Katrien
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Gandini, Domenica
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Ulrichts, Peter
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Beauchamp, Jon
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Dreier, Torsten
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Ward, E. Sally
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Michel, Marc
aa79a2d1-b2fa-414f-bea6-ce74f71c9919
Liebman, Howard A.
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Haard, Hans
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Leupin, Nicolas
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Kuter, David J.
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Newland, Adrian C., Sánchez‐González, Blanca, Rejtő, László, Egyed, Miklos, Romanyuk, Nataliya, Godar, Marie, Verschueren, Katrien, Gandini, Domenica, Ulrichts, Peter, Beauchamp, Jon, Dreier, Torsten, Ward, E. Sally, Michel, Marc, Liebman, Howard A., Haard, Hans, Leupin, Nicolas and Kuter, David J.
(2020)
Phase 2 study of efgartigimod, a novel FcRn antagonist, in adult patients with primary immune thrombocytopenia.
American Journal of Hematology, 95 (2), .
(doi:10.1002/ajh.25680).
Abstract
Primary immune thrombocytopenia (ITP) is an acquired autoimmune bleeding disorder, characterized by a low platelet count (<100 × 10
9/L) in the absence of other causes associated with thrombocytopenia. In most patients, IgG autoantibodies directed against platelet receptors can be detected. They accelerate platelet clearance and destruction, inhibit platelet production, and impair platelet function, resulting in increased risk of bleeding and impaired quality of life. Efgartigimod is a human IgG1 antibody Fc-fragment, a natural ligand of the neonatal Fc receptor (FcRn), engineered for increased affinity to FcRn, while preserving its characteristic pH-dependent binding. Efgartigimod blocks FcRn, preventing IgG recycling, and causing targeted IgG degradation. In this Phase 2 study, 38 patients were randomized 1:1:1 to receive four weekly intravenous infusions of either placebo (N = 12) or efgartigimod at a dose of 5 mg/kg (N = 13) or 10 mg/kg (N = 13). This short treatment cycle of efgartigimod in patients with ITP, predominantly refractory to previous lines of therapy, was shown to be well tolerated, and demonstrated a favorable safety profile consistent with Phase 1 data. Efgartigimod induced a rapid reduction of total IgG levels (up to 63.7% mean change from baseline), which was associated with clinically relevant increases in platelet counts (46% patients on efgartigimod vs 25% on placebo achieved a platelet count of ≥50 × 10
9/L on at least two occasions, and 38% vs 0% achieved ≥50 × 10
9/L for at least 10 cumulative days), and a reduced proportion of patients with bleeding. Taken together, these data warrant further evaluation of FcRn antagonism as a novel therapeutic approach in ITP.
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Newland_et_al-2020-American_Journal_of_Hematology
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Accepted/In Press date: 11 November 2019
e-pub ahead of print date: 10 December 2019
Published date: 1 February 2020
Additional Information:
Funding Information:
Adrian C. Newland: consultant for Amgen, Angle, argenx, Dova, Novartis, Ono, Rigel, and Shionogi; received funding from Amgen, Novartis, and Rigel; received honoraria directly from Amgen, Angle, argenx, Dova, Novartis, Ono, Rigel, and Shionogi; and paid expert testimony from argenx and Rigel. Blanca Sánchez‐González: received honoraria directly and paid expert testimony from Novartis, Takeda, Amgen, Alexion, Gilead and Shire; and Board of Directors or its advisory committees at Novartis, Takeda, Amgen. László Rejtő, Miklos Egyed, and Nataliya Romanyuk: none. E. Sally Ward: receives funding and royalty payments from argenx, and has equity ownership in argenx. Marc Michel: consultant for Novartis, Amgen, and Rigel. Howard A. Liebman: consultant for argenx, Novartis, Rigel, Pfizer, Dova, and received funding from Janssen and Bristol‐Myers. David J. Kuter: consultant for Actelion (Syntimmune), Agios, Alnylam, Amgen, argenx, Bristol Myers Squibb (BMS), Caremark, Daiichi Sankyo, Dova, Kyowa‐Kirin, Merck Sharp Dohme, Momenta, Novartis, Pfizer, Platelet Disorder Support Association, Principia, Protalex, Protalix, Rigel, Sanofi, Genzyme, Shionogi, Shire, Takeda (Bioverativ), UCB, Up‐To‐Date, Zafgen; and received funding from Actelion (Syntimmune), Agios, Alnylam, Amgen, argenx, Bristol Myers Squibb (BMS), Kezar, Principia, Protalex, Rigel, and Takeda (Bioverativ). Katrien Verschueren: consultant for argenx. Marie Godar, Domenica Gandini, Peter Ulrichts, Jon Beauchamp, Torsten Dreier, Hans de Haard, and Nicolas Leupin: employees and equity ownership in argenx.
Publisher Copyright:
© 2019 The Authors. American Journal of Hematology published by Wiley Periodicals, Inc.
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Local EPrints ID: 437640
URI: http://eprints.soton.ac.uk/id/eprint/437640
ISSN: 0361-8609
PURE UUID: 5f281384-cf41-4860-a579-3e1324ecb0ba
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Date deposited: 07 Feb 2020 17:32
Last modified: 17 Mar 2024 03:53
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Contributors
Author:
Adrian C. Newland
Author:
Blanca Sánchez‐González
Author:
László Rejtő
Author:
Miklos Egyed
Author:
Nataliya Romanyuk
Author:
Marie Godar
Author:
Katrien Verschueren
Author:
Domenica Gandini
Author:
Peter Ulrichts
Author:
Jon Beauchamp
Author:
Torsten Dreier
Author:
Marc Michel
Author:
Howard A. Liebman
Author:
Hans Haard
Author:
Nicolas Leupin
Author:
David J. Kuter
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