Development, Characterization, and in vivo Validation of a Humanized C6 Monoclonal Antibody that Inhibits the Membrane Attack Complex

Heidi Gytz Olesen; Iliana Michailidou; Wioleta M Zelek; Jeroen Vreijling; Patrick Ruizendaal; Ferry de Klein; J Arnoud Marquart; Thomas B Kuipers; Hailiang Mei; Yuchun Zhang; Muhammad Ahasan; Krista K Johnson; Yi Wang; B Paul Morgan; Marcus van Dijk; Kees Fluiter; Gregers Rom Andersen; Frank Baas

doi:10.1159/000524587

Development, Characterization, and in vivo Validation of a Humanized C6 Monoclonal Antibody that Inhibits the Membrane Attack Complex

J Innate Immun. 2023;15(1):16-36. doi: 10.1159/000524587. Epub 2022 May 12.

Authors

Heidi Gytz Olesen¹, Iliana Michailidou², Wioleta M Zelek³, Jeroen Vreijling², Patrick Ruizendaal⁴, Ferry de Klein⁴, J Arnoud Marquart⁵, Thomas B Kuipers⁶, Hailiang Mei⁶, Yuchun Zhang⁷, Muhammad Ahasan⁷, Krista K Johnson⁷, Yi Wang⁷, B Paul Morgan³, Marcus van Dijk⁸, Kees Fluiter⁹, Gregers Rom Andersen¹, Frank Baas^{2

8}

Affiliations

¹ Department of Molecular Biology and Genetics - Protein Science, Aarhus University, Aarhus, Denmark.
² Department of Clinical Genetics, LUMC, Leiden, The Netherlands.
³ Division of Infection and Immunity and Dementia Research Institute, Systems Immunity Research Institute, School of Medicine, Cardiff University, Cardiff, UK.
⁴ Core Facility Genomics, Amsterdam UMC, Amsterdam, The Netherlands.
⁵ Molecular Hematology, Amsterdam, The Netherlands.
⁶ Sequencing Analysis Support Core, Department of Biomedical Data Sciences, LUMC, Leiden, The Netherlands.
⁷ Alexion, AstraZeneca Rare Disease, New Haven, Connecticut, USA.
⁸ Complement Pharma BV, Amsterdam, The Netherlands.
⁹ Department of Clinical Genetics, LUMC, Leiden, The Netherlands, k.fluiter@lumc.nl.

Abstract

Damage and disease of nerves activates the complement system. We demonstrated that activation of the terminal pathway of the complement system leads to the formation of the membrane attack complex (MAC) and delays regeneration in the peripheral nervous system. Animals deficient in the complement component C6 showed improved recovery after neuronal trauma. Thus, inhibitors of the MAC might be of therapeutic use in neurological disease. Here, we describe the development, structure, mode of action, and properties of a novel therapeutic monoclonal antibody, CP010, against C6 that prevents formation of the MAC in vivo. The monoclonal antibody is humanized and specific for C6 and binds to an epitope in the FIM1-2 domain of human and primate C6 with sub-nanomolar affinity. Using biophysical and structural studies, we show that the anti-C6 antibody prevents the interaction between C6 and C5/C5b by blocking the C6 FIM1-2:C5 C345c axis. Systemic administration of the anti-C6 mAb caused complete depletion of free C6 in circulation in transgenic rats expressing human C6 and thereby inhibited MAC formation. The antibody prevented disease in experimental autoimmune myasthenia gravis and ameliorated relapse in chronic relapsing experimental autoimmune encephalomyelitis in human C6 transgenic rats. CP010 is a promising complement C6 inhibitor that prevents MAC formation. Systemic administration of this C6 monoclonal antibody has therapeutic potential in the treatment of neuronal disease.

Keywords: Complement component 6; Complement system; Membrane attack complex; Monoclonal antibody.

MeSH terms

Animals
Antibodies, Monoclonal / therapeutic use
Complement C6
Complement Membrane Attack Complex* / chemistry
Complement Membrane Attack Complex* / metabolism
Complement System Proteins*
Humans
Rats
Rats, Transgenic

Substances

Complement Membrane Attack Complex
Complement System Proteins
Complement C6
Antibodies, Monoclonal

Grants and funding

B. Paul Morgan is funded by the UK Dementia Research Institute; Wioleta M. Zelek is funded by a Health and Care Research Wales Fellowship. This work was funded by Regenesance BV, her successor Complement Pharma BV and Alexion, AstraZeneca Rare Disease.