Development and Optimization of Bifunctional Fusion Proteins to Locally Modulate Complement Activation in Diseased Tissue

Sustained complement activation is an underlying pathologic driver in many inflammatory and autoimmune diseases. Currently approved anti-complement therapies are directed at the systemic blockade of complement. Consequently, these therapies provide widespread inhibition of complement pathway activit...

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Autores principales: Fahnoe, Kelly C., Liu, Fei, Morgan, Jennifer G., Ryan, Sarah T., Storek, Michael, Stark, Ellen Garber, Taylor, Fred R., Holers, V. Michael, Thurman, Joshua M., Wawersik, Stefan, Kalled, Susan L., Violette, Shelia M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9244803/
https://www.ncbi.nlm.nih.gov/pubmed/35784298
http://dx.doi.org/10.3389/fimmu.2022.869725
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author Fahnoe, Kelly C.
Liu, Fei
Morgan, Jennifer G.
Ryan, Sarah T.
Storek, Michael
Stark, Ellen Garber
Taylor, Fred R.
Holers, V. Michael
Thurman, Joshua M.
Wawersik, Stefan
Kalled, Susan L.
Violette, Shelia M.
author_facet Fahnoe, Kelly C.
Liu, Fei
Morgan, Jennifer G.
Ryan, Sarah T.
Storek, Michael
Stark, Ellen Garber
Taylor, Fred R.
Holers, V. Michael
Thurman, Joshua M.
Wawersik, Stefan
Kalled, Susan L.
Violette, Shelia M.
author_sort Fahnoe, Kelly C.
collection PubMed
description Sustained complement activation is an underlying pathologic driver in many inflammatory and autoimmune diseases. Currently approved anti-complement therapies are directed at the systemic blockade of complement. Consequently, these therapies provide widespread inhibition of complement pathway activity, beyond the site of ongoing activation and the intended pharmacodynamic (PD) effects. Given the essential role for complement in both innate and adaptive immunity, there is a need for therapies that inhibit complement in diseased tissue while limiting systemic blockade. One potential approach focuses on the development of novel fusion proteins that enable tissue-targeted delivery of complement negative regulatory proteins. These therapies are expected to provide increased potency and prolonged tissue PD, decreased dosing frequency, and the potential for improved safety profiles. We created a library of bifunctional fusion proteins that direct a fragment of the complement negative regulator, complement receptor type 1 (CR1) to sites of tissue injury. Tissue targeting is accomplished through the binding of the fusion protein to complement C3 fragments that contain a surface-exposed C3d domain and which are covalently deposited on tissues where complement is being activated. To that end, we generated a fusion protein that contains an anti-C3d monoclonal antibody recombinantly linked to the first 10 consensus repeats of CR1 (CR1(1-10)) with the intention of delivering high local concentrations of this complement negative regulatory domain to tissue-bound complement C3 fragments iC3b, C3dg and C3d. Biochemical and in vitro characterization identified several fusion proteins that inhibit complement while maintaining the C3d domain binding properties of the parent monoclonal antibody. Preclinical in vivo studies further demonstrate that anti-C3d fusion proteins effectively distribute to injured tissue and reduce C3 fragment deposition for periods beyond 14 days. The in vitro and in vivo profiles support the further evaluation of C3d mAb-CR1(1-10) as a novel approach to restore proper complement activation in diseased tissue in the absence of continuous systemic complement blockade.
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spelling pubmed-92448032022-07-01 Development and Optimization of Bifunctional Fusion Proteins to Locally Modulate Complement Activation in Diseased Tissue Fahnoe, Kelly C. Liu, Fei Morgan, Jennifer G. Ryan, Sarah T. Storek, Michael Stark, Ellen Garber Taylor, Fred R. Holers, V. Michael Thurman, Joshua M. Wawersik, Stefan Kalled, Susan L. Violette, Shelia M. Front Immunol Immunology Sustained complement activation is an underlying pathologic driver in many inflammatory and autoimmune diseases. Currently approved anti-complement therapies are directed at the systemic blockade of complement. Consequently, these therapies provide widespread inhibition of complement pathway activity, beyond the site of ongoing activation and the intended pharmacodynamic (PD) effects. Given the essential role for complement in both innate and adaptive immunity, there is a need for therapies that inhibit complement in diseased tissue while limiting systemic blockade. One potential approach focuses on the development of novel fusion proteins that enable tissue-targeted delivery of complement negative regulatory proteins. These therapies are expected to provide increased potency and prolonged tissue PD, decreased dosing frequency, and the potential for improved safety profiles. We created a library of bifunctional fusion proteins that direct a fragment of the complement negative regulator, complement receptor type 1 (CR1) to sites of tissue injury. Tissue targeting is accomplished through the binding of the fusion protein to complement C3 fragments that contain a surface-exposed C3d domain and which are covalently deposited on tissues where complement is being activated. To that end, we generated a fusion protein that contains an anti-C3d monoclonal antibody recombinantly linked to the first 10 consensus repeats of CR1 (CR1(1-10)) with the intention of delivering high local concentrations of this complement negative regulatory domain to tissue-bound complement C3 fragments iC3b, C3dg and C3d. Biochemical and in vitro characterization identified several fusion proteins that inhibit complement while maintaining the C3d domain binding properties of the parent monoclonal antibody. Preclinical in vivo studies further demonstrate that anti-C3d fusion proteins effectively distribute to injured tissue and reduce C3 fragment deposition for periods beyond 14 days. The in vitro and in vivo profiles support the further evaluation of C3d mAb-CR1(1-10) as a novel approach to restore proper complement activation in diseased tissue in the absence of continuous systemic complement blockade. Frontiers Media S.A. 2022-06-16 /pmc/articles/PMC9244803/ /pubmed/35784298 http://dx.doi.org/10.3389/fimmu.2022.869725 Text en Copyright © 2022 Fahnoe, Liu, Morgan, Ryan, Storek, Stark, Taylor, Holers, Thurman, Wawersik, Kalled and Violette https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Fahnoe, Kelly C.
Liu, Fei
Morgan, Jennifer G.
Ryan, Sarah T.
Storek, Michael
Stark, Ellen Garber
Taylor, Fred R.
Holers, V. Michael
Thurman, Joshua M.
Wawersik, Stefan
Kalled, Susan L.
Violette, Shelia M.
Development and Optimization of Bifunctional Fusion Proteins to Locally Modulate Complement Activation in Diseased Tissue
title Development and Optimization of Bifunctional Fusion Proteins to Locally Modulate Complement Activation in Diseased Tissue
title_full Development and Optimization of Bifunctional Fusion Proteins to Locally Modulate Complement Activation in Diseased Tissue
title_fullStr Development and Optimization of Bifunctional Fusion Proteins to Locally Modulate Complement Activation in Diseased Tissue
title_full_unstemmed Development and Optimization of Bifunctional Fusion Proteins to Locally Modulate Complement Activation in Diseased Tissue
title_short Development and Optimization of Bifunctional Fusion Proteins to Locally Modulate Complement Activation in Diseased Tissue
title_sort development and optimization of bifunctional fusion proteins to locally modulate complement activation in diseased tissue
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9244803/
https://www.ncbi.nlm.nih.gov/pubmed/35784298
http://dx.doi.org/10.3389/fimmu.2022.869725
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