Fully human monoclonal antibody inhibitors of the neonatal Fc receptor (FcRn) reduce circulating IgG in nonhuman primates

Andrew E Nixon; Jie eChen; Daniel J Sexton; Arumugam eMuruganandam; Alan J Bitonti; Jennifer eDumont; Malini eViswanathan; Diana eMartik; Dina eWassaf; Adam eMezo; Clive R Wood; Joseph C Biedenkapp; Christopher eTenHoor

doi:10.3389/fimmu.2015.00176

Frontiers in Immunology (Apr 2015)

Fully human monoclonal antibody inhibitors of the neonatal Fc receptor (FcRn) reduce circulating IgG in nonhuman primates

Andrew E Nixon,
Jie eChen,
Daniel J Sexton,
Arumugam eMuruganandam,
Alan J Bitonti,
Jennifer eDumont,
Malini eViswanathan,
Diana eMartik,
Dina eWassaf,
Adam eMezo,
Clive R Wood,
Joseph C Biedenkapp,
Christopher eTenHoor

Affiliations

Andrew E Nixon: Dyax Corp.
Jie eChen: Dyax Corp.
Daniel J Sexton: Dyax Corp.
Arumugam eMuruganandam: Dyax Corp.
Alan J Bitonti: Syntonix Pharmaceuticals, a wholly-owned subsidiary of Biogen Idec
Jennifer eDumont: Syntonix Pharmaceuticals, a wholly-owned subsidiary of Biogen Idec
Malini eViswanathan: Dyax Corp.
Diana eMartik: Dyax Corp.
Dina eWassaf: Dyax Corp.
Adam eMezo: Syntonix Pharmaceuticals, a wholly-owned subsidiary of Biogen Idec
Clive R Wood: Dyax Corp.
Joseph C Biedenkapp: Dyax Corp.
Christopher eTenHoor: Dyax Corp.

DOI: https://doi.org/10.3389/fimmu.2015.00176
Journal volume & issue: Vol. 6

Abstract

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The therapeutic management of antibody mediated autoimmune disease typically involves immunosuppressant and immunomodulatory strategies. However, perturbing the fundamental role of the neonatal Fc receptor (FcRn) in salvaging IgG from lysosomal degradation provides a novel approach – depleting the body of pathogenic immunoglobulin by preventing IgG binding to FcRn and thereby increasing the rate of IgG catabolism. Herein, we describe the discovery and preclinical evaluation of fully human monoclonal IgG antibody inhibitors of FcRn. Using phage display, we identified several potent inhibitors of human FcRn in which binding to FcRn is pH independent, with over 1000-fold higher affinity for human FcRn than human IgG-Fc at pH 7.4. FcRn antagonism in vivo using a human-FcRn knock-in transgenic mouse model caused enhanced catabolism of exogenously administered human IgG. In non-human primates we observed reductions in endogenous circulating IgG of > 60% with no changes in albumin, IgM, or IgA. FcRn antagonism did not disrupt the ability of non-human primates to mount IgM/IgG primary and secondary immune responses. Interestingly, the therapeutic anti-FcRn antibodies had a short serum half-life but caused a prolonged reduction in IgG levels. This may be explained by the high affinity of the antibodies to FcRn at both acidic and neutral pH. These results provide important preclinical proof of concept data in support of FcRn antagonism as a novel approach to the treatment of antibody mediated autoimmune diseases.

Published in Frontiers in Immunology

ISSN: 1664-3224 (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: http://journal.frontiersin.org/journal/immunology

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