A synthetic protein as efficient multitarget regulator against complement over-activation

Author:

Ruiz-Molina NataliaORCID,Parsons JulianaORCID,Müller Madeleine,Hoernstein Sebastian N. W.ORCID,Bohlender Lennard L.ORCID,Pumple SteffenORCID,Zipfel Peter F.ORCID,Häffner KarstenORCID,Reski RalfORCID,Decker Eva L.ORCID

Abstract

AbstractThe complement system constitutes the innate defense against pathogens. Its dysregulation leads to diseases and is a critical determinant in many viral infections, e.g., COVID-19. Factor H (FH) is the main regulator of the alternative pathway of complement activation and could be a therapy to restore homeostasis. However, recombinant FH is not available. Engineered FH versions may be alternative therapeutics. Here, we designed a synthetic protein, MFHR13, as a multitarget complement regulator. It combines the dimerization and C5-regulatory domains of human FH-related protein 1 (FHR1) with the C3-regulatory and cell surface recognition domains of human FH, including SCR 13. In summary, the fusion protein MFHR13 comprises SCRs FHR11-2:FH1-4:FH13:FH19-20. It protects sheep erythrocytes from complement attack exhibiting 26 and 4-fold the regulatory activity of eculizumab and human FH, respectively. Furthermore, we demonstrate that MFHR13 and FHR1 bind to all proteins forming the membrane attack complex, which contributes to the mechanistic understanding of FHR1. We consider MFHR13 a promising candidate as therapeutic for complement-associated diseases.

Funder

Deutscher Akademischer Austauschdienst

Wissenschaftliche Gesellschaft Freiburg im Breisgau

Deutsche Forschungsgemeinschaft

KIdnees Iowa City USA

Publisher

Springer Science and Business Media LLC

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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