C3d-Targeted factor H inhibits tissue complement in disease models and reduces glomerular injury without affecting circulating complement

Fei Liu; Sarah T. Ryan; Kelly C. Fahnoe; Jennifer G. Morgan; Anne E. Cheung; Michael J. Storek; Alejandro Best; Hui A. Chen; Monica Locatelli; Shuyun Xu; Enno Schmidt; Leon F. Schmidt-Jiménez; Katja Bieber; Joel M. Henderson; Christine G. Lian; Admar Verschoor; Ralf J. Ludwig; Ariela Benigni; Giuseppe Remuzzi; David J. Salant; Susan L. Kalled; Joshua M. Thurman; V. Michael Holers; Shelia M. Violette; Stefan Wawersik

doi:10.1016/j.ymthe.2024.02.001

C3d-Targeted factor H inhibits tissue complement in disease models and reduces glomerular injury without affecting circulating complement

Fei Liu, Sarah T. Ryan, Kelly C. Fahnoe, Jennifer G. Morgan, Anne E. Cheung, Michael J. Storek, Alejandro Best, Hui A. Chen, Monica Locatelli, Shuyun Xu, Enno Schmidt, Leon F. Schmidt-Jiménez, Katja Bieber, Joel M. Henderson, Christine G. Lian, Admar Verschoor, Ralf J. Ludwig, Ariela Benigni, Giuseppe Remuzzi, David J. SalantSusan L. Kalled, Joshua M. Thurman, V. Michael Holers, Shelia M. Violette, Stefan Wawersik^*

^*Korrespondierende/r Autor/-in für diese Arbeit

18 Zitate (Scopus)

Abstract

Complement-mediated diseases can be treated using systemic inhibitors. However, complement components are abundant in circulation, affecting systemic inhibitors’ exposure and efficacy. Furthermore, because of complement's essential role in immunity, systemic treatments raise infection risk in patients. To address these challenges, we developed antibody fusion proteins combining the alternative-pathway complement inhibitor factor H (fH_1–5) with an anti-C3d monoclonal antibody (C3d-mAb-2fH). Because C3d is deposited at sites of complement activity, this molecule localizes to tissue complement while minimizing circulating complement engagement. These fusion proteins bind to deposited complement in diseased human skin sections and localize to activated complement in a primate skin injury model. We further explored the pharmacology of C3d-mAb-2fH proteins in rodent models with robust tissue complement activation. Doses of C3d-mAb-2fH >1 mg/kg achieved >75% tissue complement inhibition in mouse and rat injury models while avoiding circulating complement blockade. Glomerular-specific complement inhibition reduced proteinuria and preserved podocyte foot-process architecture in rat membranous nephropathy, indicating disease-modifying efficacy. These data indicate that targeting local tissue complement results in durable and efficacious complement blockade in skin and kidney while avoiding systemic inhibition, suggesting broad applicability of this approach in treating a range of complement-mediated diseases.

Originalsprache	Englisch
Zeitschrift	Molecular Therapy
Jahrgang	32
Ausgabenummer	4
Seiten (von - bis)	1061-1079
Seitenumfang	19
ISSN	1525-0016
DOIs	https://doi.org/10.1016/j.ymthe.2024.02.001
Publikationsstatus	Veröffentlicht - 03.04.2024

UN SDGs

Dieser Output leistet einen Beitrag zu folgendem(n) Ziel(en) für nachhaltige Entwicklung

SDG 6 – Sauberes Wasser und sanitäre Einrichtungen

Strategische Forschungsbereiche und Zentren

Forschungsschwerpunkt: Infektion und Entzündung - Zentrum für Infektions- und Entzündungsforschung Lübeck (ZIEL)

DFG-Fachsystematik

2.21-05 Immunologie

Dokumente

10.1016/j.ymthe.2024.02.001

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Liu, F., Ryan, S. T., Fahnoe, K. C., Morgan, J. G., Cheung, A. E., Storek, M. J., Best, A., Chen, H. A., Locatelli, M., Xu, S., Schmidt, E., Schmidt-Jiménez, L. F., Bieber, K., Henderson, J. M., Lian, C. G., Verschoor, A., Ludwig, R. J., Benigni, A., Remuzzi, G., ... Wawersik, S. (2024). C3d-Targeted factor H inhibits tissue complement in disease models and reduces glomerular injury without affecting circulating complement. Molecular Therapy, 32(4), 1061-1079. https://doi.org/10.1016/j.ymthe.2024.02.001

@article{532cde484dcd449a8c9a20b6ea8a703b,

title = "C3d-Targeted factor H inhibits tissue complement in disease models and reduces glomerular injury without affecting circulating complement",

abstract = "Complement-mediated diseases can be treated using systemic inhibitors. However, complement components are abundant in circulation, affecting systemic inhibitors{\textquoteright} exposure and efficacy. Furthermore, because of complement's essential role in immunity, systemic treatments raise infection risk in patients. To address these challenges, we developed antibody fusion proteins combining the alternative-pathway complement inhibitor factor H (fH1–5) with an anti-C3d monoclonal antibody (C3d-mAb-2fH). Because C3d is deposited at sites of complement activity, this molecule localizes to tissue complement while minimizing circulating complement engagement. These fusion proteins bind to deposited complement in diseased human skin sections and localize to activated complement in a primate skin injury model. We further explored the pharmacology of C3d-mAb-2fH proteins in rodent models with robust tissue complement activation. Doses of C3d-mAb-2fH >1 mg/kg achieved >75\% tissue complement inhibition in mouse and rat injury models while avoiding circulating complement blockade. Glomerular-specific complement inhibition reduced proteinuria and preserved podocyte foot-process architecture in rat membranous nephropathy, indicating disease-modifying efficacy. These data indicate that targeting local tissue complement results in durable and efficacious complement blockade in skin and kidney while avoiding systemic inhibition, suggesting broad applicability of this approach in treating a range of complement-mediated diseases.",

author = "Fei Liu and Ryan, \{Sarah T.\} and Fahnoe, \{Kelly C.\} and Morgan, \{Jennifer G.\} and Cheung, \{Anne E.\} and Storek, \{Michael J.\} and Alejandro Best and Chen, \{Hui A.\} and Monica Locatelli and Shuyun Xu and Enno Schmidt and Schmidt-Jim{\'e}nez, \{Leon F.\} and Katja Bieber and Henderson, \{Joel M.\} and Lian, \{Christine G.\} and Admar Verschoor and Ludwig, \{Ralf J.\} and Ariela Benigni and Giuseppe Remuzzi and Salant, \{David J.\} and Kalled, \{Susan L.\} and Thurman, \{Joshua M.\} and Holers, \{V. Michael\} and Violette, \{Shelia M.\} and Stefan Wawersik",

note = "Publisher Copyright: {\textcopyright} 2024 Q32 Bio",

year = "2024",

month = apr,

day = "3",

doi = "10.1016/j.ymthe.2024.02.001",

language = "English",

volume = "32",

pages = "1061--1079",

journal = "Molecular Therapy",

issn = "1525-0016",

publisher = "Cell Press",

number = "4",

}

Liu, F, Ryan, ST, Fahnoe, KC, Morgan, JG, Cheung, AE, Storek, MJ, Best, A, Chen, HA, Locatelli, M, Xu, S, Schmidt, E , Schmidt-Jiménez, LF , Bieber, K, Henderson, JM, Lian, CG, Verschoor, A , Ludwig, RJ, Benigni, A, Remuzzi, G, Salant, DJ, Kalled, SL, Thurman, JM, Holers, VM, Violette, SM & Wawersik, S 2024, 'C3d-Targeted factor H inhibits tissue complement in disease models and reduces glomerular injury without affecting circulating complement', Molecular Therapy, Jg. 32, Nr. 4, S. 1061-1079. https://doi.org/10.1016/j.ymthe.2024.02.001

TY - JOUR

T1 - C3d-Targeted factor H inhibits tissue complement in disease models and reduces glomerular injury without affecting circulating complement

AU - Liu, Fei

AU - Ryan, Sarah T.

AU - Fahnoe, Kelly C.

AU - Morgan, Jennifer G.

AU - Cheung, Anne E.

AU - Storek, Michael J.

AU - Best, Alejandro

AU - Chen, Hui A.

AU - Locatelli, Monica

AU - Xu, Shuyun

AU - Schmidt, Enno

AU - Schmidt-Jiménez, Leon F.

AU - Bieber, Katja

AU - Henderson, Joel M.

AU - Lian, Christine G.

AU - Verschoor, Admar

AU - Ludwig, Ralf J.

AU - Benigni, Ariela

AU - Remuzzi, Giuseppe

AU - Salant, David J.

AU - Kalled, Susan L.

AU - Thurman, Joshua M.

AU - Holers, V. Michael

AU - Violette, Shelia M.

AU - Wawersik, Stefan

PY - 2024/4/3

Y1 - 2024/4/3

N2 - Complement-mediated diseases can be treated using systemic inhibitors. However, complement components are abundant in circulation, affecting systemic inhibitors’ exposure and efficacy. Furthermore, because of complement's essential role in immunity, systemic treatments raise infection risk in patients. To address these challenges, we developed antibody fusion proteins combining the alternative-pathway complement inhibitor factor H (fH1–5) with an anti-C3d monoclonal antibody (C3d-mAb-2fH). Because C3d is deposited at sites of complement activity, this molecule localizes to tissue complement while minimizing circulating complement engagement. These fusion proteins bind to deposited complement in diseased human skin sections and localize to activated complement in a primate skin injury model. We further explored the pharmacology of C3d-mAb-2fH proteins in rodent models with robust tissue complement activation. Doses of C3d-mAb-2fH >1 mg/kg achieved >75% tissue complement inhibition in mouse and rat injury models while avoiding circulating complement blockade. Glomerular-specific complement inhibition reduced proteinuria and preserved podocyte foot-process architecture in rat membranous nephropathy, indicating disease-modifying efficacy. These data indicate that targeting local tissue complement results in durable and efficacious complement blockade in skin and kidney while avoiding systemic inhibition, suggesting broad applicability of this approach in treating a range of complement-mediated diseases.

AB - Complement-mediated diseases can be treated using systemic inhibitors. However, complement components are abundant in circulation, affecting systemic inhibitors’ exposure and efficacy. Furthermore, because of complement's essential role in immunity, systemic treatments raise infection risk in patients. To address these challenges, we developed antibody fusion proteins combining the alternative-pathway complement inhibitor factor H (fH1–5) with an anti-C3d monoclonal antibody (C3d-mAb-2fH). Because C3d is deposited at sites of complement activity, this molecule localizes to tissue complement while minimizing circulating complement engagement. These fusion proteins bind to deposited complement in diseased human skin sections and localize to activated complement in a primate skin injury model. We further explored the pharmacology of C3d-mAb-2fH proteins in rodent models with robust tissue complement activation. Doses of C3d-mAb-2fH >1 mg/kg achieved >75% tissue complement inhibition in mouse and rat injury models while avoiding circulating complement blockade. Glomerular-specific complement inhibition reduced proteinuria and preserved podocyte foot-process architecture in rat membranous nephropathy, indicating disease-modifying efficacy. These data indicate that targeting local tissue complement results in durable and efficacious complement blockade in skin and kidney while avoiding systemic inhibition, suggesting broad applicability of this approach in treating a range of complement-mediated diseases.

UR - https://www.scopus.com/pages/publications/85185569938

U2 - 10.1016/j.ymthe.2024.02.001

DO - 10.1016/j.ymthe.2024.02.001

M3 - Journal articles

C2 - 38382529

AN - SCOPUS:85185569938

SN - 1525-0016

VL - 32

SP - 1061

EP - 1079

JO - Molecular Therapy

JF - Molecular Therapy

IS - 4

ER -

C3d-Targeted factor H inhibits tissue complement in disease models and reduces glomerular injury without affecting circulating complement

Abstract

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