Your search keyword '"factor H-related protein"' showing total 26 results

1. Variation in CFHR3 determines susceptibility to meningococcal disease by controlling factor H concentrations.

Author

Kumar, Vikrant, Pouw, Richard B., Autio, Matias I., Sagmeister, Manfred G., Phua, Zai Yang, Borghini, Lisa, Wright, Victoria J., Hoggart, Clive, Pan, Bangfen, Tan, Antson Kiat Yee, Binder, Alexander, Brouwer, Mieke C., Pinnock, Ellie, De Groot, Ronald, Hazelzet, Jan, Emonts, Marieke, Van Der Flier, Michiel, Reiter, Karl, Nöthen, Markus M., and Hoffmann, Per

Subjects

*DISEASE susceptibility, *COMPLEMENT factor H, *MENINGOCOCCAL infections, *NEISSERIA meningitidis, *PREVENTIVE medicine, *GENETIC variation

Abstract

Neisseria meningitidis protects itself from complement-mediated killing by binding complement factor H (FH). Previous studies associated susceptibility to meningococcal disease (MD) with variation in CFH , but the causal variants and underlying mechanism remained unknown. Here we attempted to define the association more accurately by sequencing the CFH - CFHR locus and imputing missing genotypes in previously obtained GWAS datasets of MD-affected individuals of European ancestry and matched controls. We identified a CFHR3 SNP that provides protection from MD (rs75703017, p value = 1.1 × 10−16) by decreasing the concentration of FH in the blood (p value = 1.4 × 10−11). We subsequently used dual-luciferase studies and CRISPR gene editing to establish that deletion of rs75703017 increased FH expression in hepatocyte by preventing promotor inhibition. Our data suggest that reduced concentrations of FH in the blood confer protection from MD; with reduced access to FH, N. meningitidis is less able to shield itself from complement-mediated killing. Neisseria meningitidis evades complement-mediated clearance by hijacking host complement regulator factor H (FH). Kumar et al. investigate the genetic variations in the CFH locus associating with meningococcal disease. A regulatory region in the adjacent CFHR3 gene controls CFH expression, thereby determining FH plasma amounts and susceptibility towards meningococcal disease. [ABSTRACT FROM AUTHOR]

Published

2022

2. Corrigendum: A Family Affair: Addressing the Challenges of Factor H and the Related Proteins

Author

Felix Poppelaars, Elena Goicoechea de Jorge, Ilse Jongerius, Antje J. Baeumner, Mark-Steven Steiner, Mihály Józsi, Erik J. M. Toonen, Diana Pauly, and the SciFiMed consortium

Subjects

complement system, factor H (FH), factor H-related protein, factor H-like protein 1, challenges - development directions, Immunologic diseases. Allergy, RC581-607

Published

2022

3. Selective Binding of Heparin/Heparan Sulfate Oligosaccharides to Factor H and Factor H-Related Proteins: Therapeutic Potential for C3 Glomerulopathies

Author

Markus A. Loeven, Marissa L. Maciej-Hulme, Cansu Yanginlar, Melanie C. Hubers, Edwin Kellenbach, Mark de Graaf, Toin H. van Kuppevelt, Jack Wetzels, Ton J. Rabelink, Richard J. H. Smith, and Johan van der Vlag

Subjects

complement, factor H (FH), factor H-related protein, heparan sulfate (HS), heparin, complement 3 glomerulopathy, Immunologic diseases. Allergy, RC581-607

Abstract

Complement dysregulation is characteristic of the renal diseases atypical hemolytic uremic syndrome (aHUS) and complement component 3 glomerulopathy (C3G). Complement regulatory protein Factor H (FH) inhibits complement activity, whereas FH-related proteins (FHRs) lack a complement regulatory domain. FH and FHRs compete for binding to host cell glycans, in particular heparan sulfates (HS). HS is a glycosaminoglycan with an immense structural variability, where distinct sulfation patterns mediate specific binding of proteins. Mutations in FH, FHRs, or an altered glomerular HS structure may disturb the FH : FHRs balance on glomerular endothelial cells, thereby leading to complement activation and the subsequent development of aHUS/C3G. In this study, we aimed to identify specific HS structures that could specifically compete off FHRs from HS glycocalyx (HSGlx), without interfering with FH binding. FH/FHR binding to human conditionally immortalized glomerular endothelial cells (ciGEnCs) and HSGlx purified from ciGEnC glycocalyx was assessed. HS modifications important for FH/FHR binding to HSGlx were analyzed using selectively desulfated heparins in competition with purified HSGlx. We further assessed effects of heparinoids on FHR1- and FHR5-mediated C3b deposition on ciGEnCs. In the presence of C3b, binding of FH, FHR1 and FHR5 to ciGEnCs was significantly increased, whereas binding of FHR2 was minimal. FHR1 and 5 competitively inhibited FH binding to HSGlx, leading to alternative pathway dysregulation. FHR1 and FHR5 binding was primarily mediated by N-sulfation while FH binding depended on N-, 2-O- and 6-O-sulfation. Addition of 2-O-desulfated heparin significantly reduced FHR1- and FHR5-mediated C3b deposition on ciGEnCs. We identify 2-O-desulfated heparin derivatives as potential therapeutics for C3G and other diseases with dysregulated complement.

Published

2021

4. Selective Binding of Heparin/Heparan Sulfate Oligosaccharides to Factor H and Factor H-Related Proteins: Therapeutic Potential for C3 Glomerulopathies.

Author

Loeven, Markus A., Maciej-Hulme, Marissa L., Yanginlar, Cansu, Hubers, Melanie C., Kellenbach, Edwin, de Graaf, Mark, van Kuppevelt, Toin H., Wetzels, Jack, Rabelink, Ton J., Smith, Richard J. H., and van der Vlag, Johan

Subjects

HEPARAN sulfate, GLYCOSAMINOGLYCANS, OLIGOSACCHARIDES, HEPARIN, HEMOLYTIC-uremic syndrome, PROTEINS, CARRIER proteins

Abstract

Complement dysregulation is characteristic of the renal diseases atypical hemolytic uremic syndrome (aHUS) and complement component 3 glomerulopathy (C3G). Complement regulatory protein Factor H (FH) inhibits complement activity, whereas FH-related proteins (FHRs) lack a complement regulatory domain. FH and FHRs compete for binding to host cell glycans, in particular heparan sulfates (HS). HS is a glycosaminoglycan with an immense structural variability, where distinct sulfation patterns mediate specific binding of proteins. Mutations in FH, FHRs, or an altered glomerular HS structure may disturb the FH : FHRs balance on glomerular endothelial cells, thereby leading to complement activation and the subsequent development of aHUS/C3G. In this study, we aimed to identify specific HS structures that could specifically compete off FHRs from HS glycocalyx (HSGlx), without interfering with FH binding. FH/FHR binding to human conditionally immortalized glomerular endothelial cells (ciGEnCs) and HSGlx purified from ciGEnC glycocalyx was assessed. HS modifications important for FH/FHR binding to HSGlx were analyzed using selectively desulfated heparins in competition with purified HSGlx. We further assessed effects of heparinoids on FHR1- and FHR5-mediated C3b deposition on ciGEnCs. In the presence of C3b, binding of FH, FHR1 and FHR5 to ciGEnCs was significantly increased, whereas binding of FHR2 was minimal. FHR1 and 5 competitively inhibited FH binding to HSGlx, leading to alternative pathway dysregulation. FHR1 and FHR5 binding was primarily mediated by N-sulfation while FH binding depended on N-, 2-O- and 6-O-sulfation. Addition of 2-O-desulfated heparin significantly reduced FHR1- and FHR5-mediated C3b deposition on ciGEnCs. We identify 2-O-desulfated heparin derivatives as potential therapeutics for C3G and other diseases with dysregulated complement. [ABSTRACT FROM AUTHOR]

Published

2021

5. A Family Affair: Addressing the Challenges of Factor H and the Related Proteins

Author

Felix Poppelaars, Elena Goicoechea de Jorge, Ilse Jongerius, Antje J. Baeumner, Mark-Steven Steiner, Mihály Józsi, Erik J. M. Toonen, Diana Pauly, and the SciFiMed consortium

Subjects

complement system, factor H (FH), factor H-related protein, factor H-like protein 1, challenges - development directions, Immunologic diseases. Allergy, RC581-607

Abstract

Inflammation is a common denominator of diseases. The complement system, an intrinsic part of the innate immune system, is a key driver of inflammation in numerous disorders. Recently, a family of proteins has been suggested to be of vital importance in conditions characterized by complement dysregulation: the human Factor H (FH) family. This group of proteins consists of FH, Factor H-like protein 1 and five Factor H-related proteins. The FH family has been linked to infectious, vascular, eye, kidney and autoimmune diseases. In contrast to FH, the functions of the other highly homologous proteins are largely unknown and, hence, their role in the different disease-specific pathogenic mechanisms remains elusive. In this perspective review, we address the major challenges ahead in this emerging area, including 1) the controversies about the functional roles of the FH protein family, 2) the discrepancies in quantification of the FH protein family, 3) the unmet needs for validated tools and 4) limitations of animal models. Next, we also discuss the opportunities that exist for the immunology community. A strong multidisciplinary approach is required to solve these obstacles and is only possible through interdisciplinary collaboration between biologists, chemists, geneticists and physicians. We position this review in light of our own perspective, as principal investigators of the SciFiMed Consortium, a consortium aiming to create a comprehensive analytical system for the quantitative and functional assessment of the entire FH protein family.

Published

2021

6. A Family Affair: Addressing the Challenges of Factor H and the Related Proteins.

Author

Poppelaars, Felix, Goicoechea de Jorge, Elena, Jongerius, Ilse, Baeumner, Antje J., Steiner, Mark-Steven, Józsi, Mihály, Toonen, Erik J. M., and Pauly, Diana

Subjects

PROTEINS, FUNCTIONAL assessment, AUTOIMMUNE diseases, KIDNEY diseases

Abstract

Inflammation is a common denominator of diseases. The complement system, an intrinsic part of the innate immune system, is a key driver of inflammation in numerous disorders. Recently, a family of proteins has been suggested to be of vital importance in conditions characterized by complement dysregulation: the human Factor H (FH) family. This group of proteins consists of FH, Factor H-like protein 1 and five Factor H-related proteins. The FH family has been linked to infectious, vascular, eye, kidney and autoimmune diseases. In contrast to FH, the functions of the other highly homologous proteins are largely unknown and, hence, their role in the different disease-specific pathogenic mechanisms remains elusive. In this perspective review, we address the major challenges ahead in this emerging area, including 1) the controversies about the functional roles of the FH protein family, 2) the discrepancies in quantification of the FH protein family, 3) the unmet needs for validated tools and 4) limitations of animal models. Next, we also discuss the opportunities that exist for the immunology community. A strong multidisciplinary approach is required to solve these obstacles and is only possible through interdisciplinary collaboration between biologists, chemists, geneticists and physicians. We position this review in light of our own perspective, as principal investigators of the SciFiMed Consortium, a consortium aiming to create a comprehensive analytical system for the quantitative and functional assessment of the entire FH protein family. [ABSTRACT FROM AUTHOR]

Published

2021

7. Regulation of the Complement System by Pentraxins

Author

Karita Haapasalo and Seppo Meri

Subjects

CRP–C-reactive protein, complement factor H, PTX3, innate, age-related macular degeneration (AMD), factor H-related protein, Immunologic diseases. Allergy, RC581-607

Abstract

The functions of pentraxins, like C-reactive protein (CRP), serum amyloid protein P (SAP) and pentraxin-3 (PTX3), are to coordinate spatially and temporally targeted clearance of injured tissue components, to protect against infections and to regulate related inflammation together with the complement system. For this, pentraxins have a dual relationship with the complement system. Initially, after a focused binding to their targets, e.g., exposed phospholipids or cholesterol in the injured tissue area, or microbial components, the pentraxins activate complement by binding its first component C1q. However, the emerging inflammation needs to be limited to the target area. Therefore, pentraxins inhibit complement at the C3b stage to prevent excessive damage. The complement inhibitory functions of pentraxins are based on their ability to interact with complement inhibitors C4bp or factor H (FH). C4bp binds to SAP, while FH binds to both CRP and PTX3. FH promotes opsonophagocytosis through inactivation of C3b to iC3b, and inhibits AP activity thus preventing formation of the C5a anaphylatoxin and the complement membrane attack complex (MAC). Monitoring CRP levels gives important clinical information about the extent of tissue damage and severity of infections. CRP is a valuable marker for distinguishing bacterial infections from viral infections. Disturbances in the functions and interactions of pentraxins and complement are also involved in a number of human diseases. This review will summarize what is currently known about the FH family proteins and pentraxins that interact with FH. Furthermore, we will discuss diseases, where interactions between these molecules may play a role.

Published

2019

8. Regulation of the Complement System by Pentraxins.

Author

Haapasalo, Karita and Meri, Seppo

Subjects

PENTRAXINS, ECULIZUMAB, BLOOD proteins, COMPLEMENT inhibition, COMPLEMENT factor H, BACTERIAL diseases, C-reactive protein

Abstract

The functions of pentraxins, like C-reactive protein (CRP), serum amyloid protein P (SAP) and pentraxin-3 (PTX3), are to coordinate spatially and temporally targeted clearance of injured tissue components, to protect against infections and to regulate related inflammation together with the complement system. For this, pentraxins have a dual relationship with the complement system. Initially, after a focused binding to their targets, e.g., exposed phospholipids or cholesterol in the injured tissue area, or microbial components, the pentraxins activate complement by binding its first component C1q. However, the emerging inflammation needs to be limited to the target area. Therefore, pentraxins inhibit complement at the C3b stage to prevent excessive damage. The complement inhibitory functions of pentraxins are based on their ability to interact with complement inhibitors C4bp or factor H (FH). C4bp binds to SAP, while FH binds to both CRP and PTX3. FH promotes opsonophagocytosis through inactivation of C3b to iC3b, and inhibits AP activity thus preventing formation of the C5a anaphylatoxin and the complement membrane attack complex (MAC). Monitoring CRP levels gives important clinical information about the extent of tissue damage and severity of infections. CRP is a valuable marker for distinguishing bacterial infections from viral infections. Disturbances in the functions and interactions of pentraxins and complement are also involved in a number of human diseases. This review will summarize what is currently known about the FH family proteins and pentraxins that interact with FH. Furthermore, we will discuss diseases, where interactions between these molecules may play a role. [ABSTRACT FROM AUTHOR]

Published

2019

9. Complement factor H family proteins in their non-canonical role as modulators of cellular functions.

Author

Józsi, Mihály, Schneider, Andrea E., Kárpáti, Éva, and Sándor, Noémi

Subjects

*COMPLEMENT (Immunology), *CELL physiology, *LIGANDS (Biochemistry), *AMINO acid sequence, *COMPLEMENT factor H

Abstract

Abstract Complement factor H is a major regulator of the alternative pathway of the complement system. The factor H-related proteins are less characterized, but recent data indicate that they rather promote complement activation. These proteins have some common ligands with factor H and have both overlapping and distinct functions depending on domain composition and the degree of conservation of amino acid sequence. Factor H and some of the factor H-related proteins also appear in a non-canonical function that is beyond their role in the modulation of complement activation. This review covers our current understanding on this emerging role of factor H family proteins in modulating the activation and function of various cells by binding to receptors or receptor ligands. [ABSTRACT FROM AUTHOR]

Published

2019

10. Factor H related proteins modulate complement activation on kidney cells

Author

Brandon Renner, Jennifer Laskowski, Felix Poppelaars, Viviana P. Ferreira, Judith Blaine, Alexandra H. Antonioli, Jonathan P. Hannan, James M. Kovacs, Cees van Kooten, Zhiying You, Matthew C. Pickering, V. Michael Holers, and Joshua M. Thurman

Subjects

Mice, factor H-related protein, Nephrology, Complement Factor H, Humans, Animals, Kidney Diseases, complement, glomerulus, Complement System Proteins, Kidney, factor H, Complement Activation

Abstract

Complement activation at a particular location is determined by the balance of activating and inhibitory proteins. Factor H is a key regulator of the alternative pathway of complement, and genetic or acquired impairments in Factor H are associated with glomerular injury. The human Factor H-related proteins (FHRs) comprise a family of five proteins that are structurally related to Factor H. Variations in the genes or expression levels of the FHRs are also associated with glomerular disease, although the mechanisms of glomerular protection/injury are incompletely understood. To explore the role of the FHRs on complement regulation/ dysregulation in the kidney, we expressed and purified recombinant murine FHRs (FHRs A, B, C and E). These four distinct FHRs contain binding regions with high amino acid sequence homology to binding regions within Factor H, but we observed different interactions of the FHRs with Factor H binding ligands, including heparin and C3d. There was differential binding of the FHRs to the resident kidney cell types (mesangial, glomerular endothelial, podocytes, and tubular epithelial). All four FHRs caused complement dysregulation on kidney cell surfaces in vitro, although the magnitude of the effect differed among the FHRs and also varied among the different kidney cells. However, only FHR E caused glomerular complement dysregulation when injected in vivo but did not exacerbate injury when injected into mice with ischemic acute kidney injury, an alternative pathway-mediated model. Thus, our experiments demonstrate that the FHRs have unique, and likely context-dependent, effects on the different cell types within the kidney.

Published

2022

11. Self-Damage Caused by Dysregulation of the Complement Alternative Pathway: Relevance of the Factor H Protein Family.

Author

Sánchez-Corral, Pilar, Pouw, Richard B., López-Trascasa, Margarita, and Józsi, Mihály

Subjects

GLYCOPROTEINS, RETINAL degeneration, PROTEIN analysis

Abstract

The alternative pathway is a continuously active surveillance arm of the complement system, and it can also enhance complement activation initiated by the classical and the lectin pathways. Various membrane-bound and plasma regulatory proteins control the activation of the potentially deleterious complement system. Among the regulators, the plasma glycoprotein factor H (FH) is the main inhibitor of the alternative pathway and its powerful amplification loop. FH belongs to a protein family that also includes FH-like protein 1 and five factor H-related (FHR-1 to FHR-5) proteins. Genetic variants and abnormal rearrangements involving the FH protein family have been linked to numerous systemic and organ-specific diseases, including age-related macular degeneration, and the renal pathologies atypical hemolytic uremic syndrome, C3 glomerulopathies, and IgA nephropathy. This review covers the known and recently emerged ligands and interactions of the human FH family proteins associated with disease and discuss the very recent experimental data that suggest FH-antagonistic and complement-activating functions for the FHR proteins. [ABSTRACT FROM AUTHOR]

Published

2018

12. The Murine Factor H-Related Protein FHR-B Promotes Complement Activation

Author

Marcell Cserhalmi, Ádám I. Csincsi, Zoltán Mezei, Anne Kopp, Mario Hebecker, Barbara Uzonyi, and Mihály Józsi

Subjects

complement deregulation, C-reactive protein, factor H, factor H-related protein, endothelial cell, extracellular matrix, Immunologic diseases. Allergy, RC581-607

Abstract

Factor H-related (FHR) proteins consist of varying number of complement control protein domains that display various degrees of sequence identity to respective domains of the alternative pathway complement inhibitor factor H (FH). While such FHR proteins are described in several species, only human FHRs were functionally investigated. Their biological role is still poorly understood and in part controversial. Recent studies on some of the human FHRs strongly suggest a role for FHRs in enhancing complement activation via competing with FH for binding to certain ligands and surfaces. The aim of the current study was the functional characterization of a murine FHR, FHR-B. To this end, FHR-B was expressed in recombinant form. Recombinant FHR-B bound to human C3b and was able to compete with human FH for C3b binding. FHR-B supported the assembly of functionally active C3bBb alternative pathway C3 convertase via its interaction with C3b. This activity was confirmed by demonstrating C3 activation in murine serum. In addition, FHR-B bound to murine pentraxin 3 (PTX3), and this interaction resulted in murine C3 fragment deposition due to enhanced complement activation in mouse serum. FHR-B also induced C3 deposition on C-reactive protein, the extracellular matrix (ECM) extract Matrigel, and endothelial cell-derived ECM when exposed to mouse serum. Moreover, mouse C3 deposition was strongly enhanced on necrotic Jurkat T cells and the mouse B cell line A20 by FHR-B. FHR-B also induced lysis of sheep erythrocytes when incubated in mouse serum with FHR-B added in excess. Altogether, these data demonstrate that, similar to human FHR-1 and FHR-5, mouse FHR-B modulates complement activity by promoting complement activation via interaction with C3b and via competition with murine FH.

Published

2017

13. Corrigendum

Subjects

factor H-related protein, challenges - development directions, factor H-like protein 1, factor H (FH), complement system

Abstract

There is an error in the Funding statement as published. The correct name for the Funder is “the European Union’s Horizon 2020 research and innovation programme”. The correct Funding statement is “This project has received funding from the European Union’s Horizon 2020 research and innovation programme under grant agreement No 899163”. The authors apologize for this error and state that this does not change the scientific conclusions of the article in any way. The original article has been updated.

Published

2022

14. Corrigendum: A Family Affair: Addressing the Challenges of Factor H and the Related Proteins (Front. Immunol., (2021), 12, (660194), 10.3389/fimmu.2021.660194)

Author

Landsteiner Laboratory and AII - Inflammatory diseases

Subjects

factor H-related protein, challenges - development directions, factor H-like protein 1, factor H (FH), complement system

Abstract

There is an error in the Funding statement as published. The correct name for the Funder is “the European Union’s Horizon 2020 research and innovation programme”. The correct Funding statement is “This project has received funding from the European Union’s Horizon 2020 research and innovation programme under grant agreement No 899163”. The authors apologize for this error and state that this does not change the scientific conclusions of the article in any way. The original article has been updated.

Published

2022

15. The Murine Factor H-Related Protein FHR-B Promotes Complement Activation.

Author

Cserhalmi, Marcell, Csincsi, Ádám I., Mezei, Zoltán, Kopp, Anne, Hebecker, Mario, Uzonyi, Barbara, and Józsi, Mihály

Subjects

COMPLEMENT factor H, PENTRAXINS, T cells

Abstract

Factor H-related (FHR) proteins consist of varying number of complement control protein domains that display various degrees of sequence identity to respective domains of the alternative pathway complement inhibitor factor H (FH). While such FHR proteins are described in several species, only human FHRs were functionally investigated. Their biological role is still poorly understood and in part controversial. Recent studies on some of the human FHRs strongly suggest a role for FHRs in enhancing complement activation via competing with FH for binding to certain ligands and surfaces. The aim of the current study was the functional characterization of a murine FHR, FHR-B. To this end, FHR-B was expressed in recombinant form. Recombinant FHR-B bound to human C3b and was able to compete with human FH for C3b binding. FHR-B supported the assembly of functionally active C3bBb alternative pathway C3 convertase via its interaction with C3b. This activity was confirmed by demonstrating C3 activation in murine serum. In addition, FHR-B bound to murine pentraxin 3 (PTX3), and this interaction resulted in murine C3 fragment deposition due to enhanced complement activation in mouse serum. FHR-B also induced C3 deposition on C-reactive protein, the extracellular matrix (ECM) extract Matrigel, and endothelial cell-derived ECM when exposed to mouse serum. Moreover, mouse C3 deposition was strongly enhanced on necrotic Jurkat T cells and the mouse B cell line A20 by FHR-B. FHR-B also induced lysis of sheep erythrocytes when incubated in mouse serum with FHR-B added in excess. Altogether, these data demonstrate that, similar to human FHR-1 and FHR-5, mouse FHR-B modulates complement activity by promoting complement activation via interaction with C3b and via competition with murine FH. [ABSTRACT FROM AUTHOR]

Published

2017

16. Selective Binding of Heparin/Heparan Sulfate Oligosaccharides to Factor H and Factor H-Related Proteins: Therapeutic Potential for C3 Glomerulopathies

Author

Cansu Yanginlar, Mark de Graaf, Melanie C Hubers, Ton J. Rabelink, Richard J.H. Smith, Markus A. Loeven, Edwin Kellenbach, Johan van der Vlag, Toin H. van Kuppevelt, Marissa L. Maciej-Hulme, and Jack F.M. Wetzels

Subjects

factor H-related protein, complement 3 glomerulopathy, Immunology, Kidney Glomerulus, heparin, Glycocalyx, Glycosaminoglycan, chemistry.chemical_compound, All institutes and research themes of the Radboud University Medical Center, Sulfation, Atypical hemolytic uremic syndrome, medicine, Immunology and Allergy, Humans, complement, Complement Activation, Cells, Cultured, Original Research, Atypical Hemolytic Uremic Syndrome, Endothelial Cells, heparan sulfate (HS), Heparan sulfate, Heparin, Complement System Proteins, RC581-607, medicine.disease, Complement system, Cell biology, Reconstructive and regenerative medicine Radboud Institute for Molecular Life Sciences [Radboudumc 10], Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], chemistry, Complement Factor H, Complement C3b, Alternative complement pathway, factor H (FH), Heparitin Sulfate, Immunologic diseases. Allergy, Renal disorders Radboud Institute for Health Sciences [Radboudumc 11], medicine.drug, Protein Binding, Signal Transduction

Abstract

Complement dysregulation is characteristic of the renal diseases atypical hemolytic uremic syndrome (aHUS) and complement component 3 glomerulopathy (C3G). Complement regulatory protein Factor H (FH) inhibits complement activity, whereas FH-related proteins (FHRs) lack a complement regulatory domain. FH and FHRs compete for binding to host cell glycans, in particular heparan sulfates (HS). HS is a glycosaminoglycan with an immense structural variability, where distinct sulfation patterns mediate specific binding of proteins. Mutations in FH, FHRs, or an altered glomerular HS structure may disturb the FH : FHRs balance on glomerular endothelial cells, thereby leading to complement activation and the subsequent development of aHUS/C3G. In this study, we aimed to identify specific HS structures that could specifically compete off FHRs from HS glycocalyx (HSGlx), without interfering with FH binding. FH/FHR binding to human conditionally immortalized glomerular endothelial cells (ciGEnCs) and HSGlxpurified from ciGEnC glycocalyx was assessed. HS modifications important for FH/FHR binding to HSGlxwere analyzed using selectively desulfated heparins in competition with purified HSGlx. We further assessed effects of heparinoids on FHR1- and FHR5-mediated C3b deposition on ciGEnCs. In the presence of C3b, binding of FH, FHR1 and FHR5 to ciGEnCs was significantly increased, whereas binding of FHR2 was minimal. FHR1 and 5 competitively inhibited FH binding to HSGlx, leading to alternative pathway dysregulation. FHR1 and FHR5 binding was primarily mediated by N-sulfation while FH binding depended on N-, 2-O- and 6-O-sulfation. Addition of 2-O-desulfated heparin significantly reduced FHR1- and FHR5-mediated C3b deposition on ciGEnCs. We identify 2-O-desulfated heparin derivatives as potential therapeutics for C3G and other diseases with dysregulated complement.

Published

2021

17. A Family Affair

Subjects

factor H-related protein, development directions, factor H-like protein 1, factor H (FH), challenges, complement system

Abstract

Inflammation is a common denominator of diseases. The complement system, an intrinsic part of the innate immune system, is a key driver of inflammation in numerous disorders. Recently, a family of proteins has been suggested to be of vital importance in conditions characterized by complement dysregulation: the human Factor H (FH) family. This group of proteins consists of FH, Factor H-like protein 1 and five Factor H-related proteins. The FH family has been linked to infectious, vascular, eye, kidney and autoimmune diseases. In contrast to FH, the functions of the other highly homologous proteins are largely unknown and, hence, their role in the different disease-specific pathogenic mechanisms remains elusive. In this perspective review, we address the major challenges ahead in this emerging area, including 1) the controversies about the functional roles of the FH protein family, 2) the discrepancies in quantification of the FH protein family, 3) the unmet needs for validated tools and 4) limitations of animal models. Next, we also discuss the opportunities that exist for the immunology community. A strong multidisciplinary approach is required to solve these obstacles and is only possible through interdisciplinary collaboration between biologists, chemists, geneticists and physicians. We position this review in light of our own perspective, as principal investigators of the SciFiMed Consortium, a consortium aiming to create a comprehensive analytical system for the quantitative and functional assessment of the entire FH protein family.

Published

2021

18. A Family Affair: Addressing the Challenges of Factor H and the Related Proteins

Subjects

factor H-related protein, challenges - development directions, factor H-like protein 1, factor H (FH), complement system

Abstract

Inflammation is a common denominator of diseases. The complement system, an intrinsic part of the innate immune system, is a key driver of inflammation in numerous disorders. Recently, a family of proteins has been suggested to be of vital importance in conditions characterized by complement dysregulation: the human Factor H (FH) family. This group of proteins consists of FH, Factor H-like protein 1 and five Factor H-related proteins. The FH family has been linked to infectious, vascular, eye, kidney and autoimmune diseases. In contrast to FH, the functions of the other highly homologous proteins are largely unknown and, hence, their role in the different disease-specific pathogenic mechanisms remains elusive. In this perspective review, we address the major challenges ahead in this emerging area, including 1) the controversies about the functional roles of the FH protein family, 2) the discrepancies in quantification of the FH protein family, 3) the unmet needs for validated tools and 4) limitations of animal models. Next, we also discuss the opportunities that exist for the immunology community. A strong multidisciplinary approach is required to solve these obstacles and is only possible through interdisciplinary collaboration between biologists, chemists, geneticists and physicians. We position this review in light of our own perspective, as principal investigators of the SciFiMed Consortium, a consortium aiming to create a comprehensive analytical system for the quantitative and functional assessment of the entire FH protein family.

Published

2021

19. Factor H related proteins modulate complement activation on kidney cells.

Author

Renner B, Laskowski J, Poppelaars F, Ferreira VP, Blaine J, Antonioli AH, Hannan JP, Kovacs JM, van Kooten C, You Z, Pickering MC, Holers VM, and Thurman JM

Subjects

Humans, Mice, Animals, Complement Activation, Complement System Proteins metabolism, Kidney metabolism, Complement Factor H genetics, Complement Factor H metabolism, Kidney Diseases

Abstract

Complement activation at a particular location is determined by the balance of activating and inhibitory proteins. Factor H is a key regulator of the alternative pathway of complement, and genetic or acquired impairments in Factor H are associated with glomerular injury. The human Factor H-related proteins (FHRs) comprise a family of five proteins that are structurally related to Factor H. Variations in the genes or expression levels of the FHRs are also associated with glomerular disease, although the mechanisms of glomerular protection/injury are incompletely understood. To explore the role of the FHRs on complement regulation/dysregulation in the kidney, we expressed and purified recombinant murine FHRs (FHRs A, B, C and E). These four distinct FHRs contain binding regions with high amino acid sequence homology to binding regions within Factor H, but we observed different interactions of the FHRs with Factor H binding ligands, including heparin and C3d. There was differential binding of the FHRs to the resident kidney cell types (mesangial, glomerular endothelial, podocytes, and tubular epithelial). All four FHRs caused complement dysregulation on kidney cell surfaces in vitro, although the magnitude of the effect differed among the FHRs and also varied among the different kidney cells. However, only FHR E caused glomerular complement dysregulation when injected in vivo but did not exacerbate injury when injected into mice with ischemic acute kidney injury, an alternative pathway-mediated model. Thus, our experiments demonstrate that the FHRs have unique, and likely context-dependent, effects on the different cell types within the kidney., (Copyright © 2022 International Society of Nephrology. Published by Elsevier Inc. All rights reserved.)

Published

2022

20. Corrigendum: A Family Affair: Addressing the Challenges of Factor H and the Related Proteins.

Author

Poppelaars, Felix, Goicoechea de Jorge, Elena, Jongerius, Ilse, Baeumner, Antje J., Steiner, Mark-Steven, Józsi, Mihály, Toonen, Erik J. M., and Pauly, Diana

Subjects

PROTEINS, COMPLEMENT activation

Published

2022

21. Complement dysregulation in glomerulonephritis

Author

Kaartinen, Kati, Safa, Adrian, Kotha, Soumya, Ratti, Giorgio, Meri, Seppo, Nefrologian yksikkö, HUS Abdominal Center, Department of Bacteriology and Immunology, TRIMM - Translational Immunology Research Program, Research Programs Unit, University of Helsinki, HUSLAB, and Seppo Meri / Principal Investigator

Subjects

IGA NEPHROPATHY, IgA glomerulonephritis, Complement, ALTERNATIVE PATHWAY, aHUS, C3 glomerulonephritis, FACTOR-H-AUTOANTIBODIES, Hemolytic uremic syndrome, C3 glomerulopathy, C3 nephritic factor, Membranoproliferative glomerulonephritis, DENSE DEPOSIT DISEASE, SERUM IGA/C3, Factor H, Streptococcus, Plasmapheresis, Eculizumab, Sialic acid, POSTINFECTIOUS GLOMERULONEPHRITIS, Factor H-related protein, Proteinuria, C3GN, FHB, HEMOLYTIC-UREMIC SYNDROME, MONOCLONAL GAMMOPATHY, 3111 Biomedicine, C3bBb

Abstract

Glomerulonephritis (GN) refers to a group of renal diseases affecting the glomeruli due to the damage mediated by immunological mechanisms. A large proportion of the disease manifestations are caused by disturbances in the complement system. They can be due to genetic errors, autoimmunity, microbes or abnormal immunoglobulins, like modified IgA or paraproteins. The common denominator in most of the problems is an overactive or misdirected alternative pathway complement activation. An assessment of kidney function, amount of proteinuria and hematuria are crucial elements to evaluate, when glomerulonephritis is suspected. However, the cornerstones of the diagnoses are renal biopsy and careful examination of the complement abnormality. Differential diagnostics between the various forms of GN is not possible based on clinical features, as they may vary greatly. This review describes the known mechanisms of complement dysfunction leading to different forms of primary GN (like IgA glomerulonephritis, dense deposit disease, C3 glomerulonephritis, post-infectious GN, membranous GN) and differences to atypical hemolytic uremic syndrome. It also covers the basic elements of etiology-directed therapy and prognosis of the most common forms of GN. Common principles in the management of GN include treatment of hypertension and reduction of proteinuria, some require immunomodulating treatment. Complement inhibition is an emerging treatment option. A thorough understanding of the basic disease mechanism and a careful follow-up are needed for optimal therapy.

Published

2019

22. Self-Damage Caused by Dysregulation of the Complement Alternative Pathway: Relevance of the Factor H Protein Family

Author

Pilar Sánchez-Corral, Richard B. Pouw, Margarita López-Trascasa, Mihály Józsi, UAM. Departamento de Medicina, and Instituto de Investigación Sanitaria Hospital Universitario de La Paz (IdiPAZ)

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, opsonization, factor H-related protein, Atypical hemolytic uremic syndrome, Protein family, complement de-regulation, Medicina, Immunology, Review, Disease, Biology, Nephropathy, 03 medical and health sciences, 0302 clinical medicine, Opsonization, medicine, Immunology and Allergy, C3 glomerulopathy, age-related macular degeneration, chemistry.chemical_classification, complement activation, atypical hemolytic uremic syndrome, Age-related macular degeneration, Factor H, medicine.disease, factor H, Complement activation, Complement system, Factor H-related protein, Antibody opsonization, Complement de-regulation, 030104 developmental biology, chemistry, Alternative complement pathway, Cancer research, Glycoprotein, lcsh:RC581-607, 030215 immunology

Abstract

The alternative pathway is a continuously active surveillance arm of the complement system, and it can also enhance complement activation initiated by the classical and the lectin pathways. Various membrane-bound and plasma regulatory proteins control the activation of the potentially deleterious complement system. Among the regulators, the plasma glycoprotein factor H (FH) is the main inhibitor of the alternative pathway and its powerful amplification loop. FH belongs to a protein family that also includes FH-like protein 1 and five factor H-related (FHR-1 to FHR-5) proteins. Genetic variants and abnormal rearrangements involving the FH protein family have been linked to numerous systemic and organ-specific diseases, including age-related macular degeneration, and the renal pathologies atypical hemolytic uremic syndrome, C3 glomerulopathies, and IgA nephropathy. This review covers the known and recently emerged ligands and interactions of the human FH family proteins associated with disease and discuss the very recent experimental data that suggest FH-antagonistic and complement-activating functions for the FHR proteins, PS-C and ML-T are funded by grants PI16/00723 and PI15/00255 (Spanish Ministerio de Economía y Competitividad/ISCIII, and European Program FEDER) and B2017/BMD3673 (Complement II-CM network from the Comunidad de Madrid). MJ is supported by the National Research, Development and Innovation Fund of Hungary (NKFIA grants K 109055 and K 125219), the Kidneeds Foundation, Iowa, US, and by the Institutional Excellence Program of the Ministry of Human Capacities of Hungary

Published

2018

23. The Murine Factor H-Related Protein FHR-B Promotes Complement Activation

Author

Anne Kopp, Marcell Cserhalmi, Mihály Józsi, Mario Hebecker, Barbara Uzonyi, Zoltán Mezei, and Ádám I. Csincsi

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, factor H-related protein, extracellular matrix, Immunology, Complement factor I, Complement factor B, complement deregulation, C-reactive protein, 03 medical and health sciences, 0302 clinical medicine, Immunology and Allergy, pentraxin 3, Decay-accelerating factor, Original Research, necrotic cell, Complement component 2, biology, factor H, Molecular biology, Complement system, 030104 developmental biology, Factor H, embryonic structures, endothelial cell, Alternative complement pathway, biology.protein, lcsh:RC581-607, 030215 immunology, Complement control protein

Abstract

Factor H-related (FHR) proteins consist of varying number of complement control protein domains that display various degrees of sequence identity to respective domains of the alternative pathway complement inhibitor factor H. While such FHR proteins are described in several species, only human FHRs were functionally investigated. Their biological role is still poorly understood and in part controversial. Recent studies on some of the human FHRs strongly suggest a role for FHRs in enhancing complement activation via competing with factor H for binding to certain ligands and surfaces. The aim of the current study was the functional characterization of a murine FHR, FHR-B. To this end, FHR-B was expressed in recombinant form. Recombinant FHR-B bound to human C3b and was able to compete with human factor H for C3b binding. FHR-B supported the assembly of functionally active C3bBb alternative pathway C3 convertase via its interaction with C3b. This activity was confirmed by demonstrating C3 activation in murine serum. In addition, FHR-B bound to murine pentraxin 3 (PTX3), and this interaction resulted in murine C3 fragment deposition due to enhanced complement activation in mouse serum. FHR-B also induced C3 deposition on C-reactive protein (CRP), the extracellular matrix extract Matrigel, and endothelial cell-derived extracellular matrix when exposed to mouse serum. Moreover, mouse C3 deposition was strongly enhanced on necrotic Jurkat T cells and the mouse B cell line A20 by FHR-B. FHR-B also induced lysis of sheep erythrocytes when incubated in mouse serum with FHR-B added in excess. Altogether, these data demonstrate that, similar to human FHR-1 and FHR-5, mouse FHR-B modulates complement activity by promoting complement activation via interaction with C3b and via competition with murine factor H.

Published

2017

24. Regulation of regulators: Role of the complement factor H-related proteins.

Author

Cserhalmi, Marcell, Papp, Alexandra, Brandus, Bianca, Uzonyi, Barbara, and Józsi, Mihály

Subjects

*COMPLEMENT activation, *PROTEINS, *NATURAL immunity, *AUTOIMMUNE diseases, *FAMILY health

Abstract

The complement system, while being an essential and very efficient effector component of innate immunity, may cause damage to the host and result in various inflammatory, autoimmune and infectious diseases or cancer, when it is improperly activated or regulated. Factor H is a serum glycoprotein and the main regulator of the activity of the alternative complement pathway. Factor H, together with its splice variant factor H-like protein 1 (FHL-1), inhibits complement activation at the level of the central complement component C3 and beyond. In humans, there are also five factor H-related (FHR) proteins, whose function is poorly characterized. While data indicate complement inhibiting activity for some of the FHRs, there is increasing evidence that FHRs have an opposite role compared with factor H and FHL-1, namely, they enhance complement activation directly and also by competing with the regulators FH and FHL-1. This review summarizes the current stand and recent data on the roles of factor H family proteins in health and disease, with focus on the function of FHR proteins. [ABSTRACT FROM AUTHOR]

Published

2019

25. Complement dysregulation in glomerulonephritis.

Author

Kaartinen K, Safa A, Kotha S, Ratti G, and Meri S

Subjects

Animals, Bacterial Infections complications, Biomarkers, Complement Activation genetics, Complement System Proteins metabolism, Glomerulonephritis diagnosis, Glomerulonephritis, IGA etiology, Glomerulonephritis, IGA metabolism, Glomerulonephritis, IGA pathology, Glomerulonephritis, Membranoproliferative etiology, Glomerulonephritis, Membranoproliferative metabolism, Glomerulonephritis, Membranoproliferative pathology, Hemolytic-Uremic Syndrome etiology, Hemolytic-Uremic Syndrome metabolism, Hemolytic-Uremic Syndrome pathology, Humans, Complement Activation immunology, Complement System Proteins immunology, Disease Susceptibility immunology, Glomerulonephritis etiology, Glomerulonephritis metabolism

Abstract

Glomerulonephritis (GN) refers to a group of renal diseases affecting the glomeruli due to the damage mediated by immunological mechanisms. A large proportion of the disease manifestations are caused by disturbances in the complement system. They can be due to genetic errors, autoimmunity, microbes or abnormal immunoglobulins, like modified IgA or paraproteins. The common denominator in most of the problems is an overactive or misdirected alternative pathway complement activation. An assessment of kidney function, amount of proteinuria and hematuria are crucial elements to evaluate, when glomerulonephritis is suspected. However, the cornerstones of the diagnoses are renal biopsy and careful examination of the complement abnormality. Differential diagnostics between the various forms of GN is not possible based on clinical features, as they may vary greatly. This review describes the known mechanisms of complement dysfunction leading to different forms of primary GN (like IgA glomerulonephritis, dense deposit disease, C3 glomerulonephritis, post-infectious GN, membranous GN) and differences to atypical hemolytic uremic syndrome. It also covers the basic elements of etiology-directed therapy and prognosis of the most common forms of GN. Common principles in the management of GN include treatment of hypertension and reduction of proteinuria, some require immunomodulating treatment. Complement inhibition is an emerging treatment option. A thorough understanding of the basic disease mechanism and a careful follow-up are needed for optimal therapy., (Copyright © 2019 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2019

26. The MFHR1 Fusion Protein Is a Novel Synthetic Multitarget Complement Inhibitor with Therapeutic Potential.

Author

Michelfelder S, Fischer F, Wäldin A, Hörle KV, Pohl M, Parsons J, Reski R, Decker EL, Zipfel PF, Skerka C, and Häffner K

Subjects

Animals, Atypical Hemolytic Uremic Syndrome genetics, Atypical Hemolytic Uremic Syndrome immunology, Complement C3 metabolism, Complement C3-C5 Convertases antagonists & inhibitors, Complement C3-C5 Convertases metabolism, Complement C3b antagonists & inhibitors, Complement C3b Inactivator Proteins deficiency, Complement C5 metabolism, Complement Factor H genetics, Complement Inactivating Agents isolation & purification, Complement Inactivating Agents therapeutic use, Complement Membrane Attack Complex biosynthesis, Complement Pathway, Alternative, Drug Design, Drug Evaluation, Preclinical, Kidney Glomerulus chemistry, Kidney Glomerulus pathology, Mice, Mice, Knockout, Protein Domains, Recombinant Fusion Proteins isolation & purification, Recombinant Fusion Proteins therapeutic use, Atypical Hemolytic Uremic Syndrome blood, Blood Proteins deficiency, Complement C3b Inactivator Proteins genetics, Complement Inactivating Agents pharmacology, Molecular Targeted Therapy, Recombinant Fusion Proteins pharmacology

Abstract

The complement system is essential for host defense, but uncontrolled complement system activation leads to severe, mostly renal pathologies, such as atypical hemolytic uremic syndrome or C3 glomerulopathy. Here, we investigated a novel combinational approach to modulate complement activation by targeting C3 and the terminal pathway simultaneously. The synthetic fusion protein MFHR1 links the regulatory domains of complement factor H (FH) with the C5 convertase/C5b-9 inhibitory fragment of the FH-related protein 1. In vitro , MFHR1 showed cofactor and decay acceleration activity and inhibited C5 convertase activation and C5b-9 assembly, which prevented C3b deposition and reduced C3a/C5a and C5b-9 generation. Furthermore, this fusion protein showed the ability to escape deregulation by FH-related proteins and form multimeric complexes with increased inhibitory activity. In addition to substantially inhibiting alternative and classic pathway activation, MFHR1 blocked hemolysis mediated by serum from a patient with aHUS expressing truncated FH. In FH-/- mice, MFHR1 administration augmented serum C3 levels, reduced abnormal glomerular C3 deposition, and ameliorated C3 glomerulopathy. Taking the unique design of MFHR1 into account, we suggest that the combination of proximal and terminal cascade inhibition together with the ability to form multimeric complexes explain the strong inhibitory capacity of MFHR1, which offers a novel basis for complement therapeutics., (Copyright © 2018 by the American Society of Nephrology.)

Published

2018