Decay-Accelerating Factor Restrains Complement Activation and Delays Progression of Murine cBSA-Induced Membranous Nephropathy

KEY POINTS: In a murine model of cationic bovine serum albumin (cBSA)–induced membranous nephropathy (MN), complement regulator decay-accelerating factor is upregulated and restrains complement activation. Studies using genetic deletion or pharmacological antagonism of C3aR indicate that the main ef...

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Autores principales: Budge, Kelly L, Verlato, Alberto, Bin, Sofia, Salem, Fadi E., Perin, Laura, La Manna, Gaetano, Zaza, Gianluigi, Fiaccadori, Enrico, Cantarelli, Chiara, Cravedi, Paolo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society of Nephrology 2023
Materias:
Original Investigation
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10371372/
https://www.ncbi.nlm.nih.gov/pubmed/37036696
http://dx.doi.org/10.34067/KID.0000000000000122
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author Budge, Kelly L
Verlato, Alberto
Bin, Sofia
Salem, Fadi E.
Perin, Laura
La Manna, Gaetano
Zaza, Gianluigi
Fiaccadori, Enrico
Cantarelli, Chiara
Cravedi, Paolo
author_facet Budge, Kelly L
Verlato, Alberto
Bin, Sofia
Salem, Fadi E.
Perin, Laura
La Manna, Gaetano
Zaza, Gianluigi
Fiaccadori, Enrico
Cantarelli, Chiara
Cravedi, Paolo
author_sort Budge, Kelly L
collection PubMed
description KEY POINTS: In a murine model of cationic bovine serum albumin (cBSA)–induced membranous nephropathy (MN), complement regulator decay-accelerating factor is upregulated and restrains complement activation. Studies using genetic deletion or pharmacological antagonism of C3aR indicate that the main effector mechanism of complement activation in cBSA-induced MN is C3a/C3aR signaling. C3a formation and/or C3aR-mediated signaling represent promising targets for hypothesis-driven therapies for MN. BACKGROUND: Complement activation is believed to play a major pathogenic role in membranous nephropathy (MN), but its effector mechanisms are still unclear. Even less investigated is the role of podocyte-expressed complement regulators, including decay-accelerating factor (DAF) in disease pathophysiology. METHODS: We induced MN by serial injections of cationic bovine serum albumin (cBSA) in WT, DAF(−/−), and C3aR(−/−) BALB/c mice and measured disease severity (by albuminuria, BUN, serum albumin, and glomerular histologic changes) and signs of complement activation in the glomeruli (immunofluorescence for C1q, C3b, and membrane attack complex). We also treated DAF(−/−) mice with cBSA-induced MN with a selective C3aR antagonist and measured the same readouts. RESULTS: cBSA-induced MN was associated with increased glomerular expression of DAF. Genetic deletion of DAF resulted in increased complement activation and higher disease severity than in WT animals. Treating cBSA-injected DAF(−/−) mice with a C3aR antagonist reduced disease severity. Similarly, C3aR(−/−) animals were protected from cBSA-induced MN, despite IgG deposition in the glomeruli and complement activation. Evidence of C1q and C3b deposition in the glomeruli of these mice suggest that IgG-cBSA immune complex formation in the glomeruli activates complement through the classical pathway. CONCLUSIONS: On cBSA-induced injury, podocytes upregulate DAF expression, which restrains complement activation. However, after prolonged injury, complement activation overcomes DAF regulatory effects leading to the formation of soluble anaphylatoxin C3a that, by signaling through C3aR, promotes glomerular injury and cBSA-induced MN disease progression. Considering the growing number of complement targeting therapies, our findings may have major translational effect on the treatment of patients with MN.
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spelling pubmed-103713722023-08-03 Decay-Accelerating Factor Restrains Complement Activation and Delays Progression of Murine cBSA-Induced Membranous Nephropathy Budge, Kelly L Verlato, Alberto Bin, Sofia Salem, Fadi E. Perin, Laura La Manna, Gaetano Zaza, Gianluigi Fiaccadori, Enrico Cantarelli, Chiara Cravedi, Paolo Kidney360 Original Investigation KEY POINTS: In a murine model of cationic bovine serum albumin (cBSA)–induced membranous nephropathy (MN), complement regulator decay-accelerating factor is upregulated and restrains complement activation. Studies using genetic deletion or pharmacological antagonism of C3aR indicate that the main effector mechanism of complement activation in cBSA-induced MN is C3a/C3aR signaling. C3a formation and/or C3aR-mediated signaling represent promising targets for hypothesis-driven therapies for MN. BACKGROUND: Complement activation is believed to play a major pathogenic role in membranous nephropathy (MN), but its effector mechanisms are still unclear. Even less investigated is the role of podocyte-expressed complement regulators, including decay-accelerating factor (DAF) in disease pathophysiology. METHODS: We induced MN by serial injections of cationic bovine serum albumin (cBSA) in WT, DAF(−/−), and C3aR(−/−) BALB/c mice and measured disease severity (by albuminuria, BUN, serum albumin, and glomerular histologic changes) and signs of complement activation in the glomeruli (immunofluorescence for C1q, C3b, and membrane attack complex). We also treated DAF(−/−) mice with cBSA-induced MN with a selective C3aR antagonist and measured the same readouts. RESULTS: cBSA-induced MN was associated with increased glomerular expression of DAF. Genetic deletion of DAF resulted in increased complement activation and higher disease severity than in WT animals. Treating cBSA-injected DAF(−/−) mice with a C3aR antagonist reduced disease severity. Similarly, C3aR(−/−) animals were protected from cBSA-induced MN, despite IgG deposition in the glomeruli and complement activation. Evidence of C1q and C3b deposition in the glomeruli of these mice suggest that IgG-cBSA immune complex formation in the glomeruli activates complement through the classical pathway. CONCLUSIONS: On cBSA-induced injury, podocytes upregulate DAF expression, which restrains complement activation. However, after prolonged injury, complement activation overcomes DAF regulatory effects leading to the formation of soluble anaphylatoxin C3a that, by signaling through C3aR, promotes glomerular injury and cBSA-induced MN disease progression. Considering the growing number of complement targeting therapies, our findings may have major translational effect on the treatment of patients with MN. American Society of Nephrology 2023-04-08 /pmc/articles/PMC10371372/ /pubmed/37036696 http://dx.doi.org/10.34067/KID.0000000000000122 Text en Copyright © 2023 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Society of Nephrology https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the Creative Commons Attribution License 4.0 (CCBY) (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Investigation
Budge, Kelly L
Verlato, Alberto
Bin, Sofia
Salem, Fadi E.
Perin, Laura
La Manna, Gaetano
Zaza, Gianluigi
Fiaccadori, Enrico
Cantarelli, Chiara
Cravedi, Paolo
Decay-Accelerating Factor Restrains Complement Activation and Delays Progression of Murine cBSA-Induced Membranous Nephropathy
title Decay-Accelerating Factor Restrains Complement Activation and Delays Progression of Murine cBSA-Induced Membranous Nephropathy
title_full Decay-Accelerating Factor Restrains Complement Activation and Delays Progression of Murine cBSA-Induced Membranous Nephropathy
title_fullStr Decay-Accelerating Factor Restrains Complement Activation and Delays Progression of Murine cBSA-Induced Membranous Nephropathy
title_full_unstemmed Decay-Accelerating Factor Restrains Complement Activation and Delays Progression of Murine cBSA-Induced Membranous Nephropathy
title_short Decay-Accelerating Factor Restrains Complement Activation and Delays Progression of Murine cBSA-Induced Membranous Nephropathy
title_sort decay-accelerating factor restrains complement activation and delays progression of murine cbsa-induced membranous nephropathy
topic Original Investigation
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10371372/
https://www.ncbi.nlm.nih.gov/pubmed/37036696
http://dx.doi.org/10.34067/KID.0000000000000122
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