Your search keyword '"Complement C3b metabolism"' showing total 170 results

1. Alternative pathway amplification and infections.

Author

Shaughnessy J, Chabeda A, Lewis LA, and Ram S

Subjects

Humans, Properdin metabolism, Complement C3b metabolism, Complement Activation physiology, Complement Pathway, Alternative, Bacterial Infections metabolism

Abstract

The alternative pathway (AP) is the phylogenetically oldest arm of the complement system and may have evolved to mark pathogens for elimination by phagocytes. Studies using purified AP proteins or AP-specific serum showed that C3b amplification on bacteria commenced following a lag phase of about 5 min and was highly dependent on the concentration of complement. Most pathogens have evolved several elegant mechanisms to evade complement, including expressing proteases that degrade AP proteins and secreting proteins that block function of C3 convertases. In an example of convergent evolution, many microbes recruit the AP inhibitor factor H (FH) using molecular mechanisms that mimic FH interactions with host cells. In most instances, the AP serves to amplify C3b deposited on microbes by the classical pathway (CP). The role of properdin on microbes appears to be restricted to stabilization of C3 convertases; scant evidence exists for its role as an initiator of the AP on pathogens in the context of serum. Therapeutic complement inhibition carries with it an increased risk of infection. Antibody (Ab)-dependent AP activation may be critical for complement activation by vaccine-elicited Ab when the CP is blocked, and its molecular mechanism is discussed., (© 2022 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2023

2. Atypical Hemolytic Uremic Syndrome-Associated FHR1 Isoform FHR1*B Enhances Complement Activation and Inflammation.

Author

Xu B, Kang Y, Du Y, Guo W, Zhu L, and Zhang H

Subjects

Atypical Hemolytic Uremic Syndrome diagnosis, Binding, Competitive immunology, Biomarkers, Blood Proteins chemistry, Complement C3b immunology, Complement C3b metabolism, Disease Susceptibility, Endothelial Cells metabolism, Humans, Inflammation complications, Models, Molecular, Necrosis immunology, Necrosis metabolism, Protein Binding, Protein Conformation, Protein Isoforms, Structure-Activity Relationship, Atypical Hemolytic Uremic Syndrome etiology, Atypical Hemolytic Uremic Syndrome metabolism, Blood Proteins metabolism, Complement Activation immunology, Inflammation immunology, Inflammation metabolism

Abstract

Atypical hemolytic uremic syndrome (aHUS) is a rare but severe type of thrombotic microangiopathy that is triggered by the abnormal activation of the alternative complement pathway. Previous studies have reported that three completely linked coding variants of CFHR1 form two haplotypes, namely, CFHR1 *A (c.469C, c.475C, c.523G) and CFHR1 *B (c.469T, c.475G, c.523C). CFHR1 *B is associated with susceptibility to aHUS. To explore the genetic mechanism by which CFHR1 isoforms contribute to aHUS, we compared the structures of FHR1*A and FHR1*B by homology modeling and found differences in the angles between SCR3 and SCR4-SCR5, as FHR1*B had a larger angle than FHR1*A. Then, we expressed FHR1*A and FHR1*B recombinant proteins and compared their functions in complement system regulation and inflammation. We found that FHR1*B presented a significantly higher capacity for binding C3b and necrotic cells than FHR1*A. In a cofactor assay, the FHR-1*B showed stronger influence on FH mediated cofactor function than the FHR-1*A, resulted in fewer C3b cleavage products. In the C3 convertase assays, FHR1*B showed more powerful effect compared with FHR1*A regarding to de-regulate FH function of inhibition the assembling of C3bBb. Additionally, we also found that FHR1*B triggered monocytes to secrete higher levels of IL-1β and IL-6 than FHR1*A. In the present study, we showed that variants of CFHR1 might differently affect complement activation and sterile inflammation. Our findings provide a possible mechanism underlying the predisposition to aHUS caused by CFHR1 isoform CFHR1 *B., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Xu, Kang, Du, Guo, Zhu and Zhang.)

Published

2022

3. Erythrocytes identify complement activation in patients with COVID-19.

Author

Lam LKM, Reilly JP, Rux AH, Murphy SJ, Kuri-Cervantes L, Weisman AR, Ittner CAG, Pampena MB, Betts MR, Wherry EJ, Song WC, Lambris JD, Meyer NJ, Cines DB, and Mangalmurti NS

Subjects

COVID-19 immunology, COVID-19 virology, Complement C3b metabolism, Complement C4b metabolism, Erythrocytes metabolism, Erythrocytes virology, Female, Humans, Male, Middle Aged, Peptide Fragments metabolism, Respiratory Insufficiency immunology, Respiratory Insufficiency metabolism, Respiratory Insufficiency virology, SARS-CoV-2 isolation & purification, Sepsis immunology, Sepsis metabolism, Sepsis virology, COVID-19 complications, Complement Activation immunology, Complement C3b immunology, Complement C4b immunology, Erythrocytes immunology, Peptide Fragments immunology, Respiratory Insufficiency diagnosis, Sepsis diagnosis

Abstract

COVID-19, the disease caused by the SARS-CoV-2 virus, can progress to multisystem organ failure and viral sepsis characterized by respiratory failure, arrhythmias, thromboembolic complications, and shock with high mortality. Autopsy and preclinical evidence implicate aberrant complement activation in endothelial injury and organ failure. Erythrocytes express complement receptors and are capable of binding immune complexes; therefore, we investigated complement activation in patients with COVID-19 using erythrocytes as a tool to diagnose complement activation. We discovered enhanced C3b and C4d deposition on erythrocytes in COVID-19 sepsis patients and non-COVID sepsis patients compared with healthy controls, supporting the role of complement in sepsis-associated organ injury. Our data suggest that erythrocytes may contribute to a precision medicine approach to sepsis and have diagnostic value in monitoring complement dysregulation in COVID-19-sepsis and non-COVID sepsis and identifying patients who may benefit from complement targeted therapies.

Published

2021

4. Complement-Dependent Activity of CD20-Specific IgG Correlates With Bivalent Antigen Binding and C1q Binding Strength.

Author

Bondza S, Marosan A, Kara S, Lösing J, Peipp M, Nimmerjahn F, Buijs J, and Lux A

Subjects

Antibodies, Monoclonal, Humanized metabolism, Antibody Affinity, Antibody Specificity, Antigens, CD20 immunology, Antineoplastic Agents, Immunological metabolism, B-Lymphocytes immunology, B-Lymphocytes metabolism, B-Lymphocytes pathology, Binding Sites, Antibody, Complement C3b metabolism, Cytotoxicity, Immunologic drug effects, Humans, K562 Cells, Kinetics, Lymphoma, B-Cell immunology, Lymphoma, B-Cell metabolism, Lymphoma, B-Cell pathology, Phagocytosis drug effects, Protein Binding, Rituximab metabolism, Antibodies, Monoclonal, Humanized pharmacology, Antigens, CD20 metabolism, Antineoplastic Agents, Immunological pharmacology, B-Lymphocytes drug effects, Complement Activation drug effects, Complement C1q metabolism, Lymphoma, B-Cell drug therapy, Rituximab pharmacology

Abstract

Monoclonal antibodies directed against the CD20 surface antigen on B cells are widely used in the therapy of B cell malignancies. Upon administration, the antibodies bind to CD20 expressing B cells and induce their depletion via cell- and complement-dependent cytotoxicity or by induction of direct cell killing. The three antibodies currently most often used in the clinic are Rituximab (RTX), Ofatumumab (OFA) and Obinutuzumab (OBI). Even though these antibodies are all of the human IgG1 subclass, they have previously been described to vary considerably in the effector functions involved in therapeutic B cell depletion, especially in regards to complement activation. Whereas OFA is known to strongly induce complement-dependent cytotoxicity, OBI is described to be far less efficient. In contrast, the role of complement in RTX-induced B cell depletion is still under debate. Some of this dissent might come from the use of different in vitro systems for characterization of antibody effector functions. We therefore set out to systematically compare antibody as well as C1q binding and complement-activation by RTX, OFA and OBI on human B cell lines that differ in expression levels of CD20 and complement-regulatory proteins as well as human primary B cells. Applying real-time interaction analysis, we show that the overall strength of C1q binding to live target cells coated with antibodies positively correlated with the degree of bivalent binding for the antibodies to CD20. Kinetic analysis revealed that C1q exhibits two binding modes with distinct affinities and binding stabilities, with exact numbers varying both between antibodies and cell lines. Furthermore, complement-dependent cell killing by RTX and OBI was highly cell-line dependent, whereas the superior complement-dependent cytotoxicity by OFA was independent of the target B cells. All three antibodies were able to initiate deposition of C3b on the B cell surface, although to varying extent. This suggests that complement activation occurs but might not necessarily lead to induction of complement-dependent cytotoxicity. This activation could, however, initiate complement-dependent phagocytosis as an alternative mechanism of therapeutic B cell depletion., Competing Interests: SB is an employee and JB is an employee and shareholder of Ridgeview Instruments AB. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Bondza, Marosan, Kara, Lösing, Peipp, Nimmerjahn, Buijs and Lux.)

Published

2021

5. Quantification of Factor H Mediated Self vs. Non-self Discrimination by Mathematical Modeling.

Author

Tille A, Lehnert T, Zipfel PF, and Figge MT

Subjects

Communicable Diseases metabolism, Complement C3b immunology, Complement C3b metabolism, Complement Factor H immunology, Complement Factor H metabolism, Humans, Phagocytosis, Protein Binding, Signal Transduction, Communicable Diseases immunology, Complement Activation, Immune Evasion, Immunity, Innate, Models, Immunological, Self Tolerance

Abstract

The complement system is part of the innate immune system and plays an important role in the host defense against infectious pathogens. One of the main effects is the opsonization of foreign invaders and subsequent uptake by phagocytosis. Due to the continuous default basal level of active complement molecules, a tight regulation is required to protect the body's own cells (self cells) from opsonization and from complement damage. A major complement regulator is Factor H, which is recruited from the fluid phase and attaches to cell surfaces where it effectively controls complement activation. Besides self cells, pathogens also have the ability to bind Factor H; they can thus escape opsonization and phagocytosis causing severe infections. In order to advance our understanding of the opsonization process at a quantitative level, we developed a mathematical model for the dynamics of the complement system-termed DynaCoSys model -that is based on ordinary differential equations for cell surface-bound molecules and on partial differential equations for concentration profiles of the fluid phase molecules in the environment of cells. This hybrid differential equation approach allows to model the complement cascade focusing on the role of active C3b in the fluid phase and on the cell surface as well as on its inactivation on the cell surface. The DynaCoSys model enables us to quantitatively predict the conditions under which Factor H mediated complement evasion occurs. Furthermore, investigating the quantitative impact of model parameters by a sensitivity analysis, we identify the driving processes of complement activation and regulation in both the self and non-self regime. The two regimes are defined by a critical Factor H concentration on the cell surface and we use the model to investigate the differential impact of complement model parameters on this threshold value. The dynamic modeling on the surface of pathogens are further relevant to understand pathophysiological situations where Factor H mutants and defective Factor H binding to target surfaces results in pathophysiology such as renal and retinal disease. In the future, this DynaCoSys model will be extended to also enable evaluating treatment strategies of complement-related diseases., (Copyright © 2020 Tille, Lehnert, Zipfel and Figge.)

Published

2020

6. Complement-Mediated Neutralization of a Potent Neurotropic Human Pathogen, Chandipura Virus, Is Dependent on C1q.

Author

Kunnakkadan U, Nag J, Kumar NA, Mukesh RK, Suma SM, and Johnson JB

Subjects

Complement C3b metabolism, Complement C4b metabolism, Complement Pathway, Classical, Humans, Neutralization Tests, Serum immunology, Serum virology, Complement Activation, Complement C1q metabolism, Immunologic Factors metabolism, Vesiculovirus immunology

Abstract

Among the innate immune sentinels, the complement system is a formidable first line of defense against pathogens, including viruses. Chandipura virus (CHPV), a neurotropic vesiculovirus of the family Rhabdoviridae , is a deadly human pathogen known to cause fatal encephalitis, especially among children. The nature of interaction and the effect of human complement on CHPV are unknown. Here, we report that CHPV is a potent activator of complement and, thus, is highly sensitive to complement proteins in normal human serum (NHS). Utilizing a panel of specific complement component depleted/reconstituted human serum, we have demonstrated that CHPV neutralization is C3, C4, and C1q dependent and independent of factor B, suggesting the importance of the classical pathway in limiting CHPV. Employing a range of biochemical approaches, we showed (i) a direct association of C1q to CHPV, (ii) deposition of complement proteins C3b, C4b, and C1q on CHPV, and (iii) virus aggregation. Depletion of C8, an important component of the pore-forming complex of complement, had no effect on CHPV, further supporting the finding that aggregation and not virolysis is the mechanism of virus neutralization. With no approved vaccines or treatment modalities in place against CHPV, insights into such interactions can be exploited to develop potent vaccines or therapeutics targeting CHPV. IMPORTANCE Chandipura virus is a clinically important human pathogen of the Indian subcontinent. The rapidity of death associated with CHPV infection in addition to the absence of an effective vaccine or therapeutics results in poor clinical prognosis. The biology of the virus and its interaction with the host immune system, including the complement system, are understudied. Our investigation reveals the susceptibility of CHPV to fluid phase complement and also dissects the pathway involved and the mechanism of virus neutralization. Direct binding of C1q, an important upstream component of the classical pathway of complement to CHPV, and the strong dependency on C1q for virus neutralization highlight the significance of identifying such interactions to better understand CHPV pathogenesis and devise strategies to target this deadly pathogen., (Copyright © 2019 American Society for Microbiology.)

Published

2019

7. Involvement of complement activation in the pulmonary vasoactivity of polystyrene nanoparticles in pigs: unique surface properties underlying alternative pathway activation and instant opsonization.

Author

Mészáros T, Kozma GT, Shimizu T, Miyahara K, Turjeman K, Ishida T, Barenholz Y, Urbanics R, and Szebeni J

Subjects

Animals, Complement Activation drug effects, Drug Hypersensitivity drug therapy, Humans, Liposomes chemistry, Male, Nanoparticles chemistry, Pulmonary Circulation drug effects, Surface Properties, Swine, Complement Activation immunology, Complement C3b metabolism, Drug Hypersensitivity immunology, Immunologic Factors metabolism, Nanoparticles administration & dosage, Polystyrenes chemistry, Pulmonary Circulation immunology

Abstract

Background: It has been proposed that many hypersensitivity reactions to nanopharmaceuticals represent complement (C)-activation-related pseudoallergy (CARPA), and that pigs provide a sensitive animal model to study the phenomenon. However, a recent study suggested that pulmonary hypertension, the pivotal symptom of porcine CARPA, is not mediated by C in cases of polystyrene nanoparticle (PS-NP)-induced reactions., Goals: To characterize PS-NPs and reexamine the contribution of CARPA to their pulmonary reactivity in pigs., Study Design: C activation by 200, 500, and 750 nm (diameter) PS-NPs and their opsonization were measured in human and pig sera, respectively, and correlated with hemodynamic effects of the same NPs in pigs in vivo., Methods: Physicochemical characterization of PS-NPs included size, ζ-potential, cryo-transmission electron microscopy, and hydrophobicity analyses. C activation in human serum was measured by ELISA and opsonization of PS-NPs in pig serum by Western blot and flow cytometry. Pulmonary vasoactivity of PS-NPs was quantified in the porcine CARPA model., Results: PS-NPs are monodisperse, highly hydrophobic spheres with strong negative surface charge. In human serum, they caused size-dependent, significant rises in C3a, Bb, and sC5b-9, but not C4d. Exposure to pig serum led within minutes to deposition of C5b-9 and opsonic iC3b on the NPs, and opsonic iC3b fragments (C3dg, C3d) also appeared in serum. PS-NPs caused major hemodynamic changes in pigs, primarily pulmonary hypertension, on the same time scale (minutes) as iC3b fragmentation and opsonization proceeded. There was significant correlation between C activation by different PS-NPs in human serum and pulmonary hypertension in pigs., Conclusion: PS-NPs have extreme surface properties with no relevance to clinically used nanomedicines. They can activate C via the alternative pathway, entailing instantaneous opsonization of NPs in pig serum. Therefore, rather than being solely C-independent reactivity, the mechanism of PS-NP-induced hypersensitivity in pigs may involve C activation. These data are consistent with the "double-hit" concept of nanoparticle-induced hypersensitivity reactions involving both CARPA and C-independent pseudoallergy., Competing Interests: Disclosure JS and RU are involved with SeroScience Ltd, an immunotoxicology contract-research organization. The authors report no other conflicts of interest in this work.

Published

2018

8. Aliskiren inhibits renin-mediated complement activation.

Author

Békássy ZD, Kristoffersson AC, Rebetz J, Tati R, Olin AI, and Karpman D

Subjects

Amides therapeutic use, Chemotaxis drug effects, Child, Complement C3 metabolism, Complement C3a chemistry, Complement C3a metabolism, Complement C3b chemistry, Complement C3b metabolism, Complement C4 chemistry, Complement C5a chemistry, Complement C5a metabolism, Complement C5b chemistry, Complement C5b metabolism, Complement Factor B chemistry, Complement Factor D chemistry, Female, Fumarates therapeutic use, Glomerular Basement Membrane pathology, Glomerulonephritis, Membranoproliferative pathology, Humans, Mast Cells physiology, Renin antagonists & inhibitors, Renin metabolism, Amides pharmacology, Complement Activation drug effects, Complement C3 chemistry, Fumarates pharmacology, Glomerulonephritis, Membranoproliferative metabolism, Glomerulonephritis, Membranoproliferative therapy, Renin chemistry

Abstract

Certain kidney diseases are associated with complement activation although a renal triggering factor has not been identified. Here we demonstrated that renin, a kidney-specific enzyme, cleaves C3 into C3b and C3a, in a manner identical to the C3 convertase. Cleavage was specifically blocked by the renin inhibitor aliskiren. Renin-mediated C3 cleavage and its inhibition by aliskiren also occurred in serum. Generation of C3 cleavage products was demonstrated by immunoblotting, detecting the cleavage product C3b, by N-terminal sequencing of the cleavage product, and by ELISA for C3a release. Functional assays showed mast cell chemotaxis towards the cleavage product C3a and release of factor Ba when the cleavage product C3b was combined with factor B and factor D. The renin-mediated C3 cleavage product bound to factor B. In the presence of aliskiren this did not occur, and less C3 deposited on renin-producing cells. The effect of aliskiren was studied in three patients with dense deposit disease and this demonstrated decreased systemic and renal complement activation (increased C3, decreased C3a and C5a, decreased renal C3 and C5b-9 deposition and/or decreased glomerular basement membrane thickness) over a follow-up period of four to seven years. Thus, renin can trigger complement activation, an effect inhibited by aliskiren. Since renin concentrations are higher in renal tissue than systemically, this may explain the renal propensity of complement-mediated disease in the presence of complement mutations or auto-antibodies., (Copyright © 2018 International Society of Nephrology. Published by Elsevier Inc. All rights reserved.)

Published

2018

9. Kallikrein Cleaves C3 and Activates Complement.

Author

Irmscher S, Döring N, Halder LD, Jo EAH, Kopka I, Dunker C, Jacobsen ID, Luo S, Slevogt H, Lorkowski S, Beyersdorf N, Zipfel PF, and Skerka C

Subjects

Amino Acid Sequence, Animals, Candida albicans immunology, Candidiasis immunology, Candidiasis microbiology, Cell Line, Transformed, Complement C3b chemistry, Complement C3b metabolism, Complement Factor B metabolism, Complement Factor D metabolism, Complement Factor H pharmacology, Complement Pathway, Alternative, Factor XII metabolism, Female, Humans, Immune Evasion, Mice, Inbred BALB C, Protein Binding drug effects, Complement Activation, Complement C3 metabolism, Complement C3-C5 Convertases metabolism, Kallikreins metabolism

Abstract

The human plasma contact system is an immune surveillance system activated by the negatively charged surfaces of bacteria and fungi and includes the kallikrein-kinin, the coagulation, and the fibrinolytic systems. Previous work shows that the contact system also activates complement, and that plasma enzymes like kallikrein, plasmin, thrombin, and FXII are involved in the activation process. Here, we show for the first time that kallikrein cleaves the central complement component C3 directly to yield active components C3b and C3a. The cleavage site within C3 is identical to that recognized by the C3 convertase. Also, kallikrein-generated C3b forms C3 convertases, which trigger the C3 amplification loop. Since kallikrein also cleaves factor B to yield Bb and Ba, kallikrein alone can trigger complement activation. Kallikrein-generated C3 convertases are inhibited by factor H; thus, the kallikrein activation pathway merges with the amplification loop of the alternative pathway. Taken together, these data suggest that activation of the contact system locally enhances complement activation on cell surfaces. The human pathogenic microbe Candida albicans activates the contact system in normal human serum. However, C. albicans immediately recruits factor H to the surface, thereby evading the alternative and likely kallikrein-mediated complement pathways., (© 2017 S. Karger AG, Basel.)

Published

2018

10. Plasma levels of complement activation fragments C3b and sC5b-9 significantly increased in patients with thrombotic microangiopathy after allogeneic stem cell transplantation.

Author

Qi J, Wang J, Chen J, Su J, Tang Y, Wu X, Ma X, Chen F, Ruan C, Zheng XL, Wu D, and Han Y

Subjects

Adolescent, Adult, Biomarkers blood, Female, Graft vs Host Disease blood, Graft vs Host Disease diagnosis, Graft vs Host Disease etiology, Hematopoietic Stem Cell Transplantation trends, Humans, Male, Thrombotic Microangiopathies diagnosis, Transplantation, Homologous adverse effects, Transplantation, Homologous trends, Young Adult, Complement Activation physiology, Complement C3b metabolism, Complement Membrane Attack Complex metabolism, Hematopoietic Stem Cell Transplantation adverse effects, Thrombotic Microangiopathies blood, Thrombotic Microangiopathies etiology

Abstract

Transplantation-associated thrombotic microangiopathy (TA-TMA) is an uncommon but severe complication in patients undergoing allogeneic stem cell transplantation (allo-SCT). However, the mechanism is unclear. From 2011 to 2014, 20 patients with TA-TMA, 20 patients without, and 54 patients with various other complications, including veno occlusive disease (VOD), graft-versus-host disease (GVHD), and infection, were recruited in the study. Plasma vWF antigen (vWFAg), vWF activity (vWFAc), and ADAMTS13 activity were determined in these patients by ELISAs and FRETS-vWF73 assay, respectively. Plasma C3b, sC5b-9, and CH50 were also determined by ELISAs. Plasma levels of C3b were significantly increased in patients with either TA-TMA (p < 0.0001) or GVHD (p < 0.01). Plasma sC5b-9 and CH50 levels in patients with TA-TMA were also significantly increased (p < 0.001). Plasma ADAMTS13 activity was lower in patients with VOD, but normal with other complications. Both plasma vWFAg and vWFAc levels were not elevated in patients with TA-TMA or VOD compared with those of other groups. Complement activation likely via an alternative pathway (increased C3b, sC5b-9, and CH50) may play a role in the pathogenesis of TA-TMA. ADAMTS13 activity is reduced in VOD, but the ADAMTS13/vWF axis appears to be unaffected in patients with TA-TMA.

Published

2017

11. Magnetic bead based assays for complement component C5.

Author

DiScipio RG and Schraufstatter IU

Subjects

Complement C3-C5 Convertases metabolism, Complement C3b metabolism, Complement C5 metabolism, Complement C7 metabolism, Complement Hemolytic Activity Assay, Complement Inactivating Agents pharmacology, Dextran Sulfate pharmacology, Hemolysis, Humans, Iron chemistry, Polysaccharides pharmacology, Protein Binding, Sepharose chemistry, beta-Glucans pharmacology, Complement Activation drug effects, Complement C3b immunology, Complement C5 immunology, Complement C7 immunology, Immunologic Techniques, Magnetics

Abstract

Two novel magnetic agarose bead based assays have been developed to measure complement component C5 interaction with C3b and the Factor I Modules (FIMs) of C7. One innovation was to couple C3b onto the magnetic agarose bead using the alternative pathway C3 convertase, which resulted in a linkage of the ligand by a covalent ester bond. A second innovation was to employ nickel ion charged N,N,N'-tris(carboxymethyl)ethylene-diamine-magnetic agarose to capture recombinantly prepared C7 FIMs that were expressed with an oligo-histidine linker followed by an acidic domain that provided a spacer enabling the C7 modules exposure to C5. Detection was brought about by peroxidase coupled to C5. Both assays exhibited adequate statistics suitable for screening. As examples of the utility of these new methods, we chose to examine influence of natural products on C5 interaction. Fucoidan and β-glucans were observed to inhibit C3b-C5 interaction, and dextran sulfate was similarly active; however, rosmarinic acid had no measurable effect. In contrast only β-glucans from two species of macrofungi were able to interfere with interaction of C5 with the FIMs of C7., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

12. Glomerular basement membrane heparan sulfate in health and disease: A regulator of local complement activation.

Author

Borza DB

Subjects

Agrin genetics, Agrin immunology, Animals, Collagen Type IV genetics, Collagen Type IV immunology, Complement C3b genetics, Complement C3b metabolism, Complement Factor H genetics, Complement Factor H metabolism, Glomerular Basement Membrane metabolism, Glomerulonephritis, Membranous genetics, Glomerulonephritis, Membranous pathology, Heparitin Sulfate metabolism, Humans, Laminin genetics, Laminin immunology, Lupus Nephritis genetics, Lupus Nephritis pathology, Membrane Glycoproteins genetics, Membrane Glycoproteins immunology, Signal Transduction, Static Electricity, Complement Activation, Gene Expression Regulation immunology, Glomerular Basement Membrane immunology, Glomerulonephritis, Membranous immunology, Heparitin Sulfate immunology, Lupus Nephritis immunology

Abstract

The glomerular basement membrane (GBM) is an essential component of the glomerular filtration barrier. Heparan sulfate proteoglycans such as agrin are major components of the GBM, along with α345(IV) collagen, laminin-521 and nidogen. A loss of GBM heparan sulfate chains is associated with proteinuria in several glomerular diseases and may contribute to the underlying pathology. As the major determinants of the anionic charge of the GBM, heparan sulfate chains have been thought to impart charge selectivity to the glomerular filtration, a view challenged by the negligible albuminuria in mice that lack heparan sulfate in the GBM. Recent studies provide increasing evidence that heparan sulfate chains modulate local complement activation by recruiting complement regulatory protein factor H, the major inhibitor of the alternative pathway in plasma. Factor H selectively inactivates C3b bound to surfaces bearing host-specific polyanions such as heparan sulfate, thus limiting complement activation on self surfaces such as the GBM, which are not protected by cell-bound complement regulators. We discuss mechanisms whereby the acquired loss of GBM heparan sulfate can impair the local regulation of the alternative pathway, exacerbating complement activation and glomerular injury in immune-mediated kidney diseases such as membranous nephropathy and lupus nephritis., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2017

13. Complement activation in leprosy: a retrospective study shows elevated circulating terminal complement complex in reactional leprosy.

Author

Bahia El Idrissi N, Hakobyan S, Ramaglia V, Geluk A, Morgan BP, Das PK, and Baas F

Subjects

Adolescent, Adult, Bangladesh, Biomarkers blood, Ethiopia, Female, Host-Pathogen Interactions, Humans, Leprosy blood, Leprosy diagnosis, Leprosy microbiology, Male, Middle Aged, Mycobacterium leprae immunology, Mycobacterium leprae pathogenicity, Retrospective Studies, Clusterin blood, Complement Activation, Complement C3b metabolism, Complement Membrane Attack Complex metabolism, Immunity, Innate, Leprosy immunology

Abstract

Mycobacterium leprae infection gives rise to the immunologically and histopathologically classified spectrum of leprosy. At present, several tools for the stratification of patients are based on acquired immunity markers. However, the role of innate immunity, particularly the complement system, is largely unexplored. The present retrospective study was undertaken to explore whether the systemic levels of complement activation components and regulators can stratify leprosy patients, particularly in reference to the reactional state of the disease. Serum samples from two cohorts were analysed. The cohort from Bangladesh included multi-bacillary (MB) patients with (n = 12) or without (n = 46) reaction (R) at intake and endemic controls (n = 20). The cohort from Ethiopia included pauci-bacillary (PB) (n = 7) and MB (n = 23) patients without reaction and MB (n = 15) patients with reaction. The results showed that the activation products terminal complement complex (TCC) (P ≤ 0·01), C4d (P ≤ 0·05) and iC3b (P ≤ 0·05) were specifically elevated in Bangladeshi patients with reaction at intake compared to endemic controls. In addition, levels of the regulator clusterin (P ≤ 0·001 without R; P < 0·05 with R) were also elevated in MB patients, irrespective of a reaction. Similar analysis of the Ethiopian cohort confirmed that, irrespective of a reaction, serum TCC levels were increased significantly in patients with reactions compared to patients without reactions (P ≤ 0·05). Our findings suggests that serum TCC levels may prove to be a valuable tool in diagnosing patients at risk of developing reactions., (© 2016 British Society for Immunology.)

Published

2016

14. Uncoupling complement C1s activation from C1q binding in apoptotic cell phagocytosis and immunosuppressive capacity.

Author

Colonna L, Parry GC, Panicker S, and Elkon KB

Subjects

Apoptosis immunology, Complement Activation immunology, Complement C1q immunology, Complement C1q metabolism, Complement C1s metabolism, Complement C3b drug effects, Complement C3b immunology, Complement C3b metabolism, Cytokines immunology, Cytophagocytosis immunology, Humans, In Vitro Techniques, Interleukin-1beta drug effects, Interleukin-1beta immunology, Interleukin-6 immunology, Jurkat Cells, Macrophages immunology, Phagocytosis drug effects, Phagocytosis immunology, Tumor Necrosis Factor-alpha drug effects, Tumor Necrosis Factor-alpha immunology, Antibodies, Monoclonal pharmacology, Apoptosis drug effects, Complement Activation drug effects, Complement C1q drug effects, Complement C1s antagonists & inhibitors, Cytokines drug effects, Cytophagocytosis drug effects, Immune Tolerance drug effects, Macrophages drug effects

Abstract

Complement activation contributes to inflammation in many diseases, yet it also supports physiologic apoptotic cells (AC) clearance and its downstream immunosuppressive effects. The roles of individual complement components in AC phagocytosis have been difficult to dissect with artificially depleted sera. Using human in vitro systems and the novel antibody complement C1s inhibitor TNT003, we uncoupled the role of the enzymatic activation of the classical pathway from the opsonizing role of C1q in mediating a) the phagocytosis of early and late AC, and b) the immunosuppressive capacity of early AC. We found that C1s inhibition had a small impact on the physiologic clearance of early AC, leaving their immunosuppressive properties entirely unaffected, while mainly inhibiting the phagocytosis of late apoptotic/secondary necrotic cells. Our data suggest that C1s inhibition may represent a valuable therapeutic strategy to control classical pathway activation without causing significant AC accumulation in diseases without defects in AC phagocytosis., (Copyright © 2016 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2016

15. Structural insights on complement activation.

Author

Alcorlo M, López-Perrote A, Delgado S, Yébenes H, Subías M, Rodríguez-Gallego C, Rodríguez de Córdoba S, and Llorca O

Subjects

Complement C3 chemistry, Complement C3b chemistry, Humans, Protein Conformation, Protein Interaction Domains and Motifs, Protein Stability, Proteolysis, Complement Activation, Complement C3 metabolism, Complement C3b metabolism, Models, Molecular

Abstract

The proteolytic cleavage of C3 to generate C3b is the central and most important step in the activation of complement, a major component of innate immunity. The comparison of the crystal structures of C3 and C3b illustrates large conformational changes during the transition from C3 to C3b. Exposure of a reactive thio-ester group allows C3b to bind covalently to surfaces such as pathogens or apoptotic cellular debris. The displacement of the thio-ester-containing domain (TED) exposes hidden surfaces that mediate the interaction with complement factor B to assemble the C3-convertase of the alternative pathway (AP). In addition, the displacement of the TED and its interaction with the macroglobulin 1 (MG1) domain generates an extended surface in C3b where the complement regulators factor H (FH), decay accelerating factor (DAF), membrane cofactor protein (MCP) and complement receptor 1 (CR1) can bind, mediating accelerated decay of the AP C3-convertase and proteolytic inactivation of C3b. In the last few years, evidence has accumulated revealing that the structure of C3b in solution is significantly more flexible than anticipated. We review our current knowledge on C3b structural flexibility to propose a general model where the TED can display a collection of conformations around the MG ring, as well as a few specialized positions where the TED is held in one of several fixed locations. Importantly, this conformational heterogeneity in C3b impacts complement regulation by affecting the interaction with regulators., (© 2015 FEBS.)

Published

2015

16. H-ficolin binds Aspergillus fumigatus leading to activation of the lectin complement pathway and modulation of lung epithelial immune responses.

Author

Bidula S, Sexton DW, Yates M, Abdolrasouli A, Shah A, Wallis R, Reed A, Armstrong-James D, and Schelenz S

Subjects

Alveolar Epithelial Cells immunology, Alveolar Epithelial Cells microbiology, Area Under Curve, Aspergillus fumigatus immunology, Aspergillus fumigatus pathogenicity, Biomarkers metabolism, Bronchoalveolar Lavage Fluid chemistry, Case-Control Studies, Cell Line, Tumor, Complement C3b immunology, Complement C3b metabolism, Glycoproteins immunology, Host-Pathogen Interactions, Humans, Interleukin-8 immunology, Interleukin-8 metabolism, Lectins immunology, Lung immunology, Lung microbiology, MAP Kinase Signaling System, Pneumonia immunology, Pneumonia microbiology, Predictive Value of Tests, Pulmonary Aspergillosis immunology, Pulmonary Aspergillosis microbiology, ROC Curve, Up-Regulation, Alveolar Epithelial Cells metabolism, Aspergillus fumigatus metabolism, Complement Activation, Complement Pathway, Mannose-Binding Lectin, Glycoproteins metabolism, Immunity, Innate, Lectins metabolism, Lung metabolism, Pneumonia metabolism, Pulmonary Aspergillosis metabolism

Abstract

Aspergillus fumigatus is an opportunistic fungal pathogen that typically infects the lungs of immunocompromised patients leading to a high mortality. H-Ficolin, an innate immune opsonin, is produced by type II alveolar epithelial cells and could participate in lung defences against infections. Here, we used the human type II alveolar epithelial cell line, A549, to determine the involvement of H-ficolin in fungal defence. Additionally, we investigated the presence of H-ficolin in bronchoalveolar lavage fluid from transplant patients during pneumonia. H-Ficolin exhibited demonstrable binding to A. fumigatus conidia via l-fucose, d-mannose and N-acetylglucosamine residues in a calcium- and pH-dependent manner. Moreover, recognition led to lectin complement pathway activation and enhanced fungal association with A549 cells. Following recognition, H-ficolin opsonization manifested an increase in interleukin-8 production from A549 cells, which involved activation of the intracellular signalling pathways mitogen-activated protein kinase MAPK kinase 1/2, p38 MAPK and c-Jun N-terminal kinase. Finally, H-ficolin concentrations were significantly higher in bronchoalveolar lavage fluid of patients with lung infections compared with control subjects (n = 16; P = 0·00726). Receiver operating characteristics curve analysis further highlighted the potential of H-ficolin as a diagnostic marker for lung infection (area under the curve = 0·77; P < 0·0001). Hence, H-ficolin participates in A. fumigatus defence through the activation of the lectin complement pathway, enhanced fungus-host interactions and modulated immune responses., (© 2015 John Wiley & Sons Ltd.)

Published

2015

17. Complement activation patterns in atypical haemolytic uraemic syndrome during acute phase and in remission.

Author

Volokhina EB, Westra D, van der Velden TJ, van de Kar NC, Mollnes TE, and van den Heuvel LP

Subjects

Acute Disease, Adolescent, Adult, Atypical Hemolytic Uremic Syndrome blood, Atypical Hemolytic Uremic Syndrome pathology, Atypical Hemolytic Uremic Syndrome therapy, Case-Control Studies, Child, Child, Preschool, Complement Factor B metabolism, Complement Factor H metabolism, Complement Pathway, Alternative drug effects, Female, Humans, Infant, Male, Middle Aged, Platelet-Rich Plasma, Protein Isoforms blood, Remission Induction, Renal Dialysis, Zymosan pharmacology, Atypical Hemolytic Uremic Syndrome immunology, Complement Activation drug effects, Complement C3b metabolism, Complement Membrane Attack Complex metabolism

Abstract

Atypical haemolytic uraemic syndrome (aHUS) is associated with (genetic) alterations in alternative complement pathway. Nevertheless, comprehensive evidence that the complement system in aHUS patients is more prone to activation is still lacking. Therefore, we performed a thorough analysis of complement activation in acute phase and in remission of this disease. Complement activation patterns of the aHUS patients in acute phase and in remission were compared to those of healthy controls. Background levels of complement activation products C3b/c, C3bBbP and terminal complement complex (TCC) were measured using enzyme-linked immunosorbent assay (ELISA) in ethylenediamine tetraacetic acid (EDTA) plasma. In vitro-triggered complement activation in serum samples was studied using zymosan-coating and pathway-specific assay. Furthermore, efficiencies of the C3b/c, C3bBbP and TCC generation in fluid phase during spontaneous activation were analysed. Patients with acute aHUS showed elevated levels of C3b/c (P < 0·01), C3bBbP (P < 0·0001) and TCC (P < 0·0001) in EDTA plasma, while values of patients in remission were normal, compared to those of healthy controls. Using data from a single aHUS patient with complement factor B mutation we illustrated normalization of complement activation during aHUS recovery. Serum samples from patients in remission showed normal in vitro patterns of complement activation and demonstrated normal kinetics of complement activation in the fluid phase. Our data indicate that while aHUS patients have clearly activated complement in acute phase of the disease, this is not the case in remission of aHUS. This knowledge provides important insight into complement regulation in aHUS and may have an impact on monitoring of these patients, particularly when using complement inhibition therapy., (© 2014 British Society for Immunology.)

Published

2015

18. Functional assessment of mouse complement pathway activities and quantification of C3b/C3c/iC3b in an experimental model of mouse renal ischaemia/reperfusion injury.

Author

Kotimaa JP, van Werkhoven MB, O'Flynn J, Klar-Mohamad N, van Groningen J, Schilders G, Rutjes H, Daha MR, Seelen MA, and van Kooten C

Subjects

Animals, Complement Activation genetics, Complement C3b genetics, Complement C3b metabolism, Complement C3c genetics, Complement C3c metabolism, Complement C9 immunology, Complement C9 metabolism, Disease Models, Animal, Enzyme-Linked Immunosorbent Assay methods, Feasibility Studies, Kidney blood supply, Kidney metabolism, Mice, Inbred C57BL, Mice, Knockout, Reproducibility of Results, Time Factors, Complement Activation immunology, Complement C3b immunology, Complement C3c immunology, Kidney immunology, Reperfusion Injury immunology

Abstract

The complement system is an essential component of our innate immunity, both for the protection against infections and for proper handling of dying cells. However, the complement system can also contribute to tissue injury and inflammatory responses. In view of novel therapeutic possibilities, there is an increasing interest in measurement of the complement system activation in the systemic compartment, both in the clinical setting as well as in experimental models. Here we describe in parallel a sensitive and specific sandwich ELISA detecting mouse C3 activation fragments C3b/C3c/iC3b, as well as functional complement ELISAs detecting specific activities of the three complement pathways at the level of C3 and at the level of C9 activation. In a murine model of renal ischaemia/reperfusion injury (IRI) we found transient complement activation as shown by generation of C3b/C3c/iC3b fragments at 24 h following reperfusion, which returned to base-line at 3 and 7 days post reperfusion. When the pathway specific complement activities were measured at the level of C3 activation, we found no significant reduction in any of the pathways. However, the functional complement activity of all three pathways was significantly reduced when measured at the level of C9, with the strongest reduction being observed in the alternative pathway. For all three pathways there was a strong correlation between the amount of C3 fragments and the reduction in functional complement activity. Moreover, at 24 h both C3 fragments and the functional complement activities showed a correlation with the rise in serum creatinine. Together our results show that determination of the systemic pathway specific complement activity is feasible in experimental mouse models and that they are useful in understanding complement activation and inhibition in vivo., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2015

19. Interplay between fibrinolysis and complement: plasmin cleavage of iC3b modulates immune responses.

Author

Foley JH, Peterson EA, Lei V, Wan LW, Krisinger MJ, and Conway EM

Subjects

Animals, Cell Line, Complement C3b immunology, Fibrinolysin immunology, Fibrinolysin pharmacology, Humans, Inflammation Mediators immunology, Inflammation Mediators metabolism, Interleukin-12 immunology, Interleukin-12 metabolism, Macrophages immunology, Peptide Fragments immunology, Peptide Fragments metabolism, Proteolysis, Rabbits, Signal Transduction, Time Factors, Complement Activation drug effects, Complement C3 Convertase, Alternative Pathway drug effects, Complement C3b metabolism, Fibrinolysin metabolism, Fibrinolysis drug effects, Immunity, Innate drug effects, Macrophages enzymology, Phagocytosis drug effects

Abstract

Background: The plasmin(ogen) and complement systems are simultaneously activated at sites of tissue injury, participating in hemostasis, wound healing, inflammation and immune surveillance. In particular, the C3 proteolytic fragment, iC3b, and its degradation product C3dg, which is generated by cleavage by factor I (FI) and the cofactor complement receptor CR1, are important in bridging innate and adaptive immunity. Via a thioester (TE) bond, iC3b and C3dg covalently tag pathogens, modulating phagocytosis and adaptive immune responses., Objective: To examine plasmin-mediated proteolysis of iC3b, and to evaluate the functional consequences, comparing the effects with products generated by FI/CR1 cleavage of iC3b., Methods: Dose-dependent and time-dependent plasmin-mediated cleavage of iC3b were characterized by analytical gel electrophoresis. The properties of the resultant TE bond-containing fragments on phagocytosis and induction of pro-inflammatory cytokines were measured in cell culture systems., Results: At low concentrations, plasmin effectively cleaves iC3b, but at numerous previously undescribed sites, giving rise to novel C3c-like and C3dg-like moieties, the latter of which retain the TE bond. When attached to zymosan or erythrocytes and exposed to THP-1 macrophages, the C3dg-like proteins behave almost identically to the bona fide C3dg, yielding less phagocytosis as compared with the opsonin iC3b, and more macrophage secretion of the pro-inflammatory cytokine, IL-12., Conclusion: Plasmin cleavage of iC3b provides a complement regulatory pathway that is as efficient as FI/CR1 but does not require a cellular cofactor., (© 2014 International Society on Thrombosis and Haemostasis.)

Published

2015

20. A revised mechanism for the activation of complement C3 to C3b: a molecular explanation of a disease-associated polymorphism.

Author

Rodriguez E, Nan R, Li K, Gor J, and Perkins SJ

Subjects

Arginine chemistry, Crystallography, X-Ray, Humans, Macroglobulins metabolism, Mutagenesis, Mutation, Protein Conformation, Protein Multimerization, Scattering, Radiation, Surface Plasmon Resonance, Ultracentrifugation, Complement Activation, Complement C3 metabolism, Complement C3b metabolism, Complement C3c metabolism, Complement C3d metabolism

Abstract

The solution structure of complement C3b is crucial for the understanding of complement activation and regulation. C3b is generated by the removal of C3a from C3. Hydrolysis of the C3 thioester produces C3u, an analog of C3b. C3b cleavage results in C3c and C3d (thioester-containing domain; TED). To resolve functional questions in relation to C3b and C3u, analytical ultracentrifugation and x-ray and neutron scattering studies were used with C3, C3b, C3u, C3c, and C3d, using the wild-type allotype with Arg(102). In 50 mm NaCl buffer, atomistic scattering modeling showed that both C3b and C3u adopted a compact structure, similar to the C3b crystal structure in which its TED and macroglobulin 1 (MG1) domains were connected through the Arg(102)-Glu(1032) salt bridge. In physiological 137 mm NaCl, scattering modeling showed that C3b and C3u were both extended in structure, with the TED and MG1 domains now separated by up to 6 nm. The importance of the Arg(102)-Glu(1032) salt bridge was determined using surface plasmon resonance to monitor the binding of wild-type C3d(E1032) and mutant C3d(A1032) to immobilized C3c. The mutant did not bind, whereas the wild-type form did. The high conformational variability of TED in C3b in physiological buffer showed that C3b is more reactive than previously thought. Because the Arg(102)-Glu(1032) salt bridge is essential for the C3b-Factor H complex during the regulatory control of C3b, the known clinical associations of the major C3S (Arg(102)) and disease-linked C3F (Gly(102)) allotypes of C3b were experimentally explained for the first time., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

21. Differential complement activation pathways promote C3b deposition on native and acetylated LDL thereby inducing lipoprotein binding to the complement receptor 1.

Author

Klop B, van der Pol P, van Bruggen R, Wang Y, de Vries MA, van Santen S, O'Flynn J, van de Geijn GJ, Njo TL, Janssen HW, de Man P, Jukema JW, Rabelink TJ, Rensen PC, van Kooten C, and Cabezas MC

Subjects

Animals, Apolipoproteins B metabolism, CHO Cells, Cells, Cultured, Complement C1q metabolism, Complement Pathway, Alternative, Complement Pathway, Classical, Cricetinae, Cricetulus, Edetic Acid pharmacology, Flow Cytometry, Humans, Immunoglobulin M metabolism, Leukocytes cytology, Leukocytes drug effects, Leukocytes metabolism, Lipopolysaccharides pharmacology, Opsonin Proteins metabolism, Properdin metabolism, Protein Binding drug effects, Receptors, Complement 3b genetics, Complement Activation, Complement C3b metabolism, Lipoproteins, LDL metabolism, Receptors, Complement 3b metabolism

Abstract

Lipoproteins can induce complement activation resulting in opsonization and binding of these complexes to complement receptors. We investigated the binding of opsonized native LDL and acetylated LDL (acLDL) to the complement receptor 1 (CR1). Binding of complement factors C3b, IgM, C1q, mannose-binding lectin (MBL), and properdin to LDL and acLDL were investigated by ELISA. Subsequent binding of opsonized LDL and acLDL to CR1 on CR1-transfected Chinese Hamster Ovarian cells (CHO-CR1) was tested by flow cytometry. Both native LDL and acLDL induced complement activation with subsequent C3b opsonization upon incubation with normal human serum. Opsonized LDL and acLDL bound to CR1. Binding to CHO-CR1 was reduced by EDTA, whereas MgEGTA only reduced the binding of opsonized LDL, but not of acLDL suggesting involvement of the alternative pathway in the binding of acLDL to CR1. In vitro incubations showed that LDL bound C1q, whereas acLDL bound to C1q, IgM, and properdin. MBL did neither bind to LDL nor to acLDL. The relevance of these findings was demonstrated by the fact that ex vivo up-regulation of CR1 on leukocytes was accompanied by a concomitant increased binding of apolipoprotein B-containing lipoproteins to leukocytes without changes in LDL-receptor expression. In conclusion, CR1 is able to bind opsonized native LDL and acLDL. Binding of LDL to CR1 is mediated via the classical pathway, whereas binding of acLDL is mediated via both the classical and alternative pathways. Binding of lipoproteins to CR1 may be of clinical relevance due to the ubiquitous cellular distribution of CR1., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

22. Intracellular complement activation sustains T cell homeostasis and mediates effector differentiation.

Author

Liszewski MK, Kolev M, Le Friec G, Leung M, Bertram PG, Fara AF, Subias M, Pickering MC, Drouet C, Meri S, Arstila TP, Pekkarinen PT, Ma M, Cope A, Reinheckel T, Rodriguez de Cordoba S, Afzali B, Atkinson JP, and Kemper C

Subjects

Adult, Arthritis, Rheumatoid immunology, CD4-Positive T-Lymphocytes metabolism, Cell Line, Cell Survival immunology, Child, Complement C3 immunology, Complement C3a metabolism, Complement C3b metabolism, Gene Expression Regulation immunology, Humans, B-Lymphocyte Subsets cytology, CD4-Positive T-Lymphocytes immunology, Cathepsin L metabolism, Cell Differentiation, Complement Activation physiology, Complement C3 metabolism, Homeostasis physiology

Abstract

Complement is viewed as a critical serum-operative component of innate immunity, with processing of its key component, C3, into activation fragments C3a and C3b confined to the extracellular space. We report here that C3 activation also occurred intracellularly. We found that the T cell-expressed protease cathepsin L (CTSL) processed C3 into biologically active C3a and C3b. Resting T cells contained stores of endosomal and lysosomal C3 and CTSL and substantial amounts of CTSL-generated C3a. While "tonic" intracellular C3a generation was required for homeostatic T cell survival, shuttling of this intracellular C3-activation-system to the cell surface upon T cell stimulation induced autocrine proinflammatory cytokine production. Furthermore, T cells from patients with autoimmune arthritis demonstrated hyperactive intracellular complement activation and interferon-γ production and CTSL inhibition corrected this deregulated phenotype. Importantly, intracellular C3a was observed in all examined cell populations, suggesting that intracellular complement activation might be of broad physiological significance., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

23. Activation of complement by monoclonal antibodies that target cell-associated β₂-microglobulin: implications for cancer immunotherapy.

Author

Pokrass MJ, Liu MF, Lindorfer MA, and Taylor RP

Subjects

Animals, Antibodies, Monoclonal metabolism, Cell Line, Tumor, Cells, Cultured, Complement C3b immunology, Complement C3b metabolism, Enzyme-Linked Immunosorbent Assay, Flow Cytometry, Humans, Immunoglobulin G immunology, Immunoglobulin G metabolism, Immunotherapy, Jurkat Cells, Leukocytes, Mononuclear immunology, Mice, Microscopy, Fluorescence, Neoplasms immunology, Neoplasms pathology, Neoplasms therapy, Neutrophils immunology, Protein Binding immunology, beta 2-Microglobulin metabolism, Antibodies, Monoclonal immunology, Antibody-Dependent Cell Cytotoxicity immunology, Complement Activation immunology, beta 2-Microglobulin immunology

Abstract

β₂-Microglobulin (β2M), the light chain of the class I major histocompatibilty complex (MHC-I), is a promising tumor target for monoclonal antibodies (mAbs) in cancer immunotherapy. Several reports indicate that chelation of cell-associated β2M by specific mouse mAbs promotes tumor cell destruction by inducing apoptosis or other cytotoxic signaling pathways. Human mAbs employed in cancer therapy are usually IgG1, which mediates cell-killing by effector mechanisms including complement dependent cytotoxicity (CDC). The analogous mouse IgG2a and IgG2b isotypes are similarly effective in activating complement. Therefore, we examined the complement-activating properties of anti-β2M mouse mAbs 1B749 (IgG2a) and HB28 (IgG2b) when either mAb was bound to tumor cell lines or normal cells; we compared these β2M-specific mAbs with mouse mAb W6/32 (IgG2a), specific for human leukocyte antigens in the MHC-I heavy chain. All three mAbs bind to most human cell lines and normal cells in approximately equal amounts, consistent with a 1:1 stoichiometry for the HLA heavy chain in association with β2M. The three mAbs promote rapid C3b deposition and substantial CDC of human cell lines, and mAbs 1B749 and W6/32 have robust cytotoxic activity on reaction with normal mononuclear cells and platelets. Curiously, mAb HB28 induces modest C3b deposition and little CDC of normal cells, and its weaker complement-fixing activity was confirmed by ELISA. Based on these findings, we suggest that human IgG mAbs that target β2M for cancer immunotherapy be selected or engineered so as not to activate complement, thus eliminating the potential adverse effects of complement-mediated lysis of normal cells., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

24. Complement activation by heme as a secondary hit for atypical hemolytic uremic syndrome.

Author

Frimat M, Tabarin F, Dimitrov JD, Poitou C, Halbwachs-Mecarelli L, Fremeaux-Bacchi V, and Roumenina LT

Subjects

Atypical Hemolytic Uremic Syndrome, Cell Line, Cell Membrane immunology, Cell Membrane metabolism, Complement C3 chemistry, Complement C3 genetics, Complement C3 immunology, Complement C3 metabolism, Complement C3-C5 Convertases metabolism, Complement C3b immunology, Complement C3b metabolism, Complement Pathway, Alternative immunology, Endothelial Cells immunology, Endothelial Cells metabolism, Heme chemistry, Heme metabolism, Hemolytic-Uremic Syndrome metabolism, Humans, Mutation, P-Selectin metabolism, Protein Binding immunology, Complement Activation immunology, Heme immunology, Hemolytic-Uremic Syndrome immunology

Abstract

Atypical hemolytic uremic syndrome (aHUS) is characterized by genetic and acquired abnormalities of the complement system leading to alternative pathway (AP) overactivation and by glomerular endothelial damage, thrombosis, and mechanical hemolysis. Mutations per se are not sufficient to induce aHUS, and nonspecific primary triggers are required for disease manifestation. We investigated whether hemolysis-derived heme contributes to aHUS pathogenesis. We confirmed that heme activates complement AP in normal human serum, releasing C3a, C5a, and sC5b9. We demonstrated that heme-exposed endothelial cells also activate the AP, resulting in cell-bound C3 and C5b9. This was exacerbated in aHUS by genetic abnormalities associated with AP overactivation. Heme interacted with C3 close to the thioester bond, induced homophilic C3 complexes, and promoted formation of an overactive C3/C5 convertase. Heme induced decreased membrane cofactor protein (MCP) and decay-accelerating factor (DAF) expression on endothelial cells, giving Factor H (FH) a major role in complement regulation. Finally, heme promoted a rapid exocytosis of Weibel-Palade bodies, with membrane expression of P-selectin known to bind C3b and trigger the AP, and the release of the prothrombotic von Willebrand factor. These results strongly suggest that hemolysis-derived heme represents a common secondary hit amplifying endothelial damage and thrombosis in aHUS.

Published

2013

25. Complement C3f serum levels may predict breast cancer risk in women with gross cystic disease of the breast.

Author

Profumo A, Mangerini R, Rubagotti A, Romano P, Damonte G, Guglielmini P, Facchiano A, Ferri F, Ricci F, Rocco M, and Boccardo F

Subjects

Adult, Female, Fibrocystic Breast Disease complications, Humans, Middle Aged, Predictive Value of Tests, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Biomarkers, Tumor blood, Breast Neoplasms blood, Complement Activation, Complement C3b metabolism, Fibrocystic Breast Disease blood

Abstract

Gross cystic disease (GCDB) is a breast benign condition predisposing to breast cancer. Cryopreserved sera from GCDB patients, some of whom later developed a cancer (cases), were studied to identify potential risk markers. A MALDI-TOF mass spectrometry analysis found several complement C3f fragments having a significant increased abundance in cases compared to controls. After multivariate analysis, the full-length form of C3f maintained a predictive value of breast cancer risk. Higher levels of C3f in the serum of women affected by a benign condition like GCDB thus appears to be correlated to the development of breast cancer even 20 years later., Biological Significance: Increased complement system activation has been found in the sera of women affected by GCDB who developed a breast cancer, even twenty or more years later. C3f may predict an increased breast cancer risk in the healthy population and in women affected by predisposing conditions., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2013

26. Cartilage oligomeric matrix protein-induced complement activation in systemic sclerosis.

Author

Otteby KE, Holmquist E, Saxne T, Heinegård D, Hesselstrand R, and Blom AM

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Cartilage Oligomeric Matrix Protein analysis, Complement C3b analysis, Enzyme-Linked Immunosorbent Assay, Female, Humans, Male, Microscopy, Fluorescence, Middle Aged, Skin metabolism, Young Adult, Cartilage Oligomeric Matrix Protein blood, Complement Activation physiology, Complement C3b metabolism, Scleroderma, Systemic blood

Abstract

Introduction: Complexes between cartilage oligomeric matrix protein (COMP) and the complement activation product C3b have been found in the circulation of patients with rheumatoid arthritis and systemic lupus erythematosus. In systemic sclerosis (SSc) COMP expression in the skin is upregulated both in lesional and non-lesional skin, which is also reflected in an increased amount of circulating COMP. We investigated the presence of COMP-C3b complexes in serum and skin biopsies of patients with SSc., Methods: The presence of COMP and COMP-C3b complexes in the serum of 80 patients with limited cutaneous SSc (lcSSc, n = 40) and diffuse cutaneous SSc (dcSSc, n = 40) and 97 healthy controls was measured by ELISA and correlated to different clinical parameters. Samples were collected both at baseline and after three to five years to assess longitudinal changes in COMP-C3b complex levels. Furthermore, skin biopsies from seven patients with dcSSc and three healthy controls were analyzed for expression of COMP and deposition of C3b and IgG., Results: Serum levels of COMP-C3b were found to be elevated in both dcSSc and lcSSc compared to healthy controls and decreased at the second measurement in patients on immunosuppressive therapy. No co-localization of COMP and C3b was found in the skin biopsies, indicating that the COMP-C3b complexes are formed upon release of COMP into the circulation., Conclusion: COMP-C3b complexes are found in the serum of patients with SSc. The lack of co-localization between COMP and C3b in the skin suggests that COMP does not drive complement activation in the skin in SSc.

Published

2013

27. Complement dependent cytotoxicity in chronic lymphocytic leukemia: ofatumumab enhances alemtuzumab complement dependent cytotoxicity and reveals cells resistant to activated complement.

Author

Baig NA, Taylor RP, Lindorfer MA, Church AK, Laplant BR, Pavey ES, Nowakowski GS, and Zent CS

Subjects

Aged, Aged, 80 and over, Alemtuzumab, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal, Humanized therapeutic use, Complement C3b metabolism, Complement Membrane Attack Complex metabolism, Female, Humans, Leukemia, Lymphocytic, Chronic, B-Cell immunology, Male, Middle Aged, Antibodies, Monoclonal pharmacology, Antibodies, Monoclonal, Humanized pharmacology, Antineoplastic Agents therapeutic use, Complement Activation, Complement System Proteins immunology, Cytotoxicity, Immunologic drug effects, Leukemia, Lymphocytic, Chronic, B-Cell drug therapy

Abstract

Complement dependent cytotoxicity (CDC) is an important mechanism of action for monoclonal antibodies (mAbs) used in the treatment of chronic lymphocytic leukemia (CLL). We hypothesized that alemtuzumab (ALM) mediated CDC would be increased by the addition of ofatumumab (OFA). CLL cells from 21 previously untreated patients with progressive disease were tested in vitro for mAb binding, complement activation and CDC. The subpopulation of CDC resistant CLL cells was examined for levels of C3b and C5b-9 binding, and expression of complement regulatory proteins. OFA significantly increased complement activation and CDC in ALM-treated CLL cells, suggesting that combining ALM and OFA could improve clinical outcome in patients with CLL. Approximately 10% of CLL cells were resistant to CDC because of lower levels of complement activation or decreased cytotoxicity of activated complement. Improvement of clinical responses will require determining the mechanisms of CDC resistance and developing methods to overcome this problem.

Published

2012

28. The tick-over theory revisited: is C3 a contact-activated protein?

Author

Nilsson B and Nilsson Ekdahl K

Subjects

Adsorption, Animals, Blood Platelets immunology, Blood Platelets metabolism, Complement C3 chemistry, Complement C3 immunology, Complement C3b immunology, Complement C3b metabolism, Gases, Humans, Hydrolysis, Liver Cirrhosis, Biliary immunology, Platelet Activation, Protein Conformation, Complement Activation, Complement C3 metabolism, Complement C3-C5 Convertases metabolism, Complement Pathway, Alternative

Abstract

The tick-over theory was first introduced in the 1970s to explain the presence of the initial C3b molecules, which are able to trigger complement activation by the alternative pathway in human plasma under physiological conditions. After the identification of the thioester, the predominant hypothesis has been that this bond is hydrolyzed at a slow but constant rate by nucleophilic attack by H(2)O, leading to the generation of C3(H(2)O). Here we put forward the hypothesis that the rate of hydrolysis of C3 to C3(H(2)O) may be greatly accelerated by the interaction between C3 and a number of biological and artificial interfaces, including gas bubbles, biomaterial surfaces and different lipid surfaces and complexes. We therefore propose that C3 should preferentially be regarded as a contact activated protein rather than a target for passive, random hydrolysis in the fluid phase., (Copyright © 2012 Elsevier GmbH. All rights reserved.)

Published

2012

29. Complement activation in acetaminophen-induced liver injury in mice.

Author

Singhal R, Ganey PE, and Roth RA

Subjects

Alanine Transaminase blood, Alanine Transaminase metabolism, Animals, Chemical and Drug Induced Liver Injury metabolism, Chemical and Drug Induced Liver Injury pathology, Complement C3b genetics, Complement C3b metabolism, Drug Overdose, Glutathione metabolism, Interleukin-10 genetics, Interleukin-10 immunology, Interleukin-10 metabolism, Interleukin-6 genetics, Interleukin-6 immunology, Interleukin-6 metabolism, Liver drug effects, Liver immunology, Liver metabolism, Liver pathology, Male, Mice, Mice, Inbred C57BL, Necrosis, Neutrophils metabolism, Plasminogen Activator Inhibitor 1 genetics, Plasminogen Activator Inhibitor 1 metabolism, Acetaminophen toxicity, Chemical and Drug Induced Liver Injury genetics, Chemical and Drug Induced Liver Injury immunology, Complement Activation drug effects, Complement C3b immunology

Abstract

Overdose with acetaminophen (APAP) results in acute liver failure in humans and experimental animals. Complement comprises more than 30 proteins that can participate in tissue injury and/or repair, but the role of complement activation in APAP-induced hepatotoxicity has not been evaluated. Treatment of male, C57BL6J mice with APAP (200-400 mg/kg) resulted in liver injury as evidenced by increased activity of alanine aminotransferase (ALT) in plasma and hepatocellular necrosis. Plasma concentration of the complement component C3 was significantly reduced 6 h after treatment with APAP, indicating complement activation, and C3b (detected by immunostaining) accumulated in the centrilobular areas of liver lobules. Pretreatment with cobra venom factor (CVF; 15 U/mouse) to deplete complement components abolished APAP-mediated C3b accumulation, and this was accompanied by reductions in plasma ALT activity, hepatocellular necrosis, hepatic neutrophil accumulation, and expression of inflammatory genes (interleukin-6, interleukin-10, and plasminogen activation inhibitor-1) at 24 h after APAP treatment. Loss of hepatocellular GSH was similar in APAP-treated mice pretreated with either saline or CVF, suggesting that CVF pretreatment did not affect APAP bioactivation. Mice with a genetic deficiency in C3 had reduced ALT activity 6 and 12 h after APAP administration compared with wild-type animals. These results reveal a key role for complement activation in hepatic inflammation and progression of injury during the pathogenesis of APAP-induced hepatotoxicity.

Published

2012

30. The protective effect of SCR(15-18) on cerebral ischemia-reperfusion injury.

Author

Li S, Xian J, He L, Luo X, Tan B, Yang Y, Liu G, and Wang Z

Subjects

Animals, Brain drug effects, Brain metabolism, Brain pathology, Cerebral Infarction pathology, Complement C3b metabolism, Disease Models, Animal, Humans, Infarction, Middle Cerebral Artery metabolism, Male, Neuroprotective Agents pharmacology, Neutrophils, Peptide Fragments pharmacology, Rats, Recombinant Proteins pharmacology, Recombinant Proteins therapeutic use, Reperfusion Injury metabolism, Cerebral Infarction drug therapy, Complement Activation drug effects, DNA-(Apurinic or Apyrimidinic Site) Lyase therapeutic use, Infarction, Middle Cerebral Artery drug therapy, Neuroprotective Agents therapeutic use, Peptide Fragments therapeutic use, Receptors, Complement therapeutic use, Reperfusion Injury drug therapy

Abstract

Objectives: Soluble complement receptor type 1 (sCR1), a potent inhibitor of complement activation, has been shown to protect brain cells against cerebral ischemic/reperfusion (CI/R) injury due to its decay-accelerating activity for C3/C5 convertase and co-factor activity for C3b/C4b degradation. However, the effect of short consensus repeats (SCRs) 15-18, one of active domains of sCR1 with high C3b/C4b degradability, has not been demonstrated. Here, we investigated the protective effect of recombinant SCR(15-18) protein in middle cerebral artery occlusion (MCAO)-induced focal CI/R injury., Methods: Recombinant SCR(15-18) protein was successfully expressed in Escherichia coli and refolded to its optimal bioactivity. Seventy-five Sprague-Dawley rats were randomly assigned into three groups: sham-operated group, CI/R group, and SCR(15-18)+CI/R group pretreated with 20 mg/kg SCR(15-18) protein. After 2 hours of MCAO and subsequent 24 hours of reperfusion, rats were evaluated for neurological deficits and cerebral infarction. Polymorphonuclear leukocyte accumulation, C3b deposition, and morphological changes in cerebral tissue were also estimated., Results: SCR(15-18) pretreatment induced a 20% reduction of infarct size and an improvement of neurological function with 22·2% decrease of neurological deficit scores. Inhibition of cerebral neutrophils infiltration by SCR(15-18) was indicated from the reduction of myeloperoxidase activity in SCR(15-18)+CI/R rats. Decreased C3b deposition and improved morphological changes were also found in cerebral tissue of SCR(15-18)-treated rats., Discussion: Our studies suggest a definitive moderately protective effect of SCR(15-18) against CI/R damage and provide preclinical experimental evidence supporting the possibility of using it as a small anti-complement therapeutic agent for CI/R injury therapy.

Published

2011

31. The role of poly(ethylene glycol) brush architecture in complement activation on targeted microbubble surfaces.

Author

Chen CC and Borden MA

Subjects

Complement C3 metabolism, Complement C3b metabolism, Complement Fixation Tests, Enzyme-Linked Immunosorbent Assay, Flow Cytometry, Humans, Ligands, Oligopeptides metabolism, Peptides chemistry, Peptides metabolism, Protein Binding drug effects, Serum metabolism, Surface Properties drug effects, Complement Activation drug effects, Microbubbles, Polyethylene Glycols chemistry, Polyethylene Glycols pharmacology

Abstract

Complement fixation to surface-conjugated ligands plays a critical role in determining the fate of targeted colloidal particles after intravenous injection. In the present study, we examined the immunogenicity of targeted microbubbles with various surface architectures and ligand surface densities using a flow cytometry technique. Targeted microbubbles were generated using a post-labeling technique with a physiological targeting ligand, cyclic arginine-glycine-asparagine (RGD), attached to the distal end of the poly(ethylene glycol) (PEG) moieties on the microbubble surface. Microbubbles were incubated in human serum, washed and then mixed with fluorescent antibodies specific for various serum components. We found that complement C3/C3b was the main human serum factor to bind in vitro to the microbubble surface, compared to IgG or albumin. We also investigated the effect of PEG brush architecture on C3/C3b fixation to the microbubble surface. RGD peptide was able to trigger a complement immune response, and complement C3/C3b fixation depended on microbubble size and RGD peptide surface density. When the targeting ligand was attached to shorter PEG chains that were shielded by a PEG overbrush layer (buried-ligand architecture), significantly less complement activation was observed when compared to the more traditional exposed-ligand motif. The extent of this protective role by the PEG chains depended on the overbrush length. Taken together, our results confirm that the buried-ligand architecture may significantly reduce ligand-mediated immunogenicity. More generally, this study illustrates the use of flow cytometry and microbubbles to analyze the surface interactions between complex biological media and surface-engineered biomaterials., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

32. Increased complement consumption in MuSK-antibody-positive myasthenia gravis patients.

Author

Tüzün E, Yılmaz V, Parman Y, Oflazer P, Deymeer F, and Saruhan-Direskeneli G

Subjects

Adolescent, Adult, Aged, Analysis of Variance, Antigen-Antibody Reactions, Autoantibodies biosynthesis, Autoantibodies immunology, Autoantibodies metabolism, Case-Control Studies, Child, Complement C3b biosynthesis, Complement C3b immunology, Complement C3b metabolism, Complement C4a immunology, Complement C4a metabolism, Complement Factor B biosynthesis, Complement Factor B metabolism, Complement System Proteins immunology, Complement System Proteins metabolism, Enzyme-Linked Immunosorbent Assay, Female, Humans, Male, Middle Aged, Muscle, Skeletal immunology, Muscle, Skeletal metabolism, Myasthenia Gravis immunology, Receptor Protein-Tyrosine Kinases, Young Adult, Complement Activation, Complement System Proteins biosynthesis, Myasthenia Gravis pathology, Receptors, Cholinergic

Abstract

Objective: To investigate the activation of different complement pathways in myasthenia gravis (MG) subtypes., Subjects and Methods: Levels of complement breakdown products for different complement pathways were measured using ELISA in sera of acetylcholine receptor antibody (AChR-Ab)-positive (n = 21), muscle-specific receptor tyrosine kinase (MuSK)-Ab-positive (n = 23) and seronegative generalized MG patients (n = 21) and healthy controls (n = 22). Levels of factor Bb (FBb), the breakdown product of factor B, and C4d, the breakdown product of C4, were measured to evaluate the activity of the alternative and classical complement pathways, respectively. Serum iC3b levels were analyzed to assess total complement activity. The results were expressed as OD values., Results: MuSK-Ab-positive MG patients had a significantly higher mean concentration of serum FBb (0.638) than other MG subtypes (0.446 for AChR-Ab-positive, 0.537 for seronegative MG patients) and healthy controls (0.434) (p = 0.045). Mean serum iC3b (1.549-1.780) and C4d (0.364-0.395) levels were comparable among the groups., Conclusion: Our results suggest that MuSK-Ab-positive MG patients might have a complement-activating serum factor and the alternative complement pathway might be involved in the pathogenesis of the disease., (Copyright © 2011 S. Karger AG, Basel.)

Published

2011

33. EspP, a serine protease of enterohemorrhagic Escherichia coli, impairs complement activation by cleaving complement factors C3/C3b and C5.

Author

Orth D, Ehrlenbach S, Brockmeyer J, Khan AB, Huber G, Karch H, Sarg B, Lindner H, and Würzner R

Subjects

Complement C3 chemistry, Complement C3b chemistry, Complement C5 chemistry, Escherichia coli Proteins genetics, Gene Expression Regulation, Enzymologic, Hemolytic-Uremic Syndrome microbiology, Humans, Serine Endopeptidases genetics, Complement Activation drug effects, Complement C3 metabolism, Complement C3b metabolism, Complement C5 metabolism, Enterohemorrhagic Escherichia coli enzymology, Escherichia coli Proteins metabolism, Serine Endopeptidases metabolism

Abstract

Hemolytic-uremic syndrome (HUS) is a life-threatening disorder characterized by hemolytic anemia, thrombocytopenia, and renal insufficiency. It is caused mainly by infections with enterohemorrhagic Escherichia coli (EHEC). Recently, Shiga toxin 2, the best-studied virulence factor of EHEC, was reported to interact with complement, implying that complement may be involved in the pathogenesis of EHEC-induced HUS. The aim of the present study was to investigate whether or not the serine protease EspP, an important virulence factor of EHEC, interacts with complement proteins. EspP did not have any effect on the integrity of factor H or factor I. However, EspP was shown to cleave purified C3/C3b and C5. Cleavage of the respective complement proteins also occurred in normal human serum (NHS) as a source of C3/C3b or C5 or when purified complement proteins were added to the supernatant of an EspP-producing wild-type strain. Edman degradation allowed unequivocal mapping of all three main C3b fragments but not of the three main C5 fragments. Complement activation was significantly downregulated in all three pathways for C5-depleted serum to which C5, preincubated with EspP, was added (whereas C5 preincubated with an EspP mutant was able to fully reconstitute complement activation). This indicates that EspP markedly destroyed the functional activity, as measured by a commercial total complement enzyme-linked immunosorbent assay (Wieslab). Downregulation of complement by EspP in vivo may influence the colonization of EHEC bacteria in the gut or the disease severity of HUS.

Published

2010

34. Human C3 mutation reveals a mechanism of dense deposit disease pathogenesis and provides insights into complement activation and regulation.

Author

Martínez-Barricarte R, Heurich M, Valdes-Cañedo F, Vazquez-Martul E, Torreira E, Montes T, Tortajada A, Pinto S, Lopez-Trascasa M, Morgan BP, Llorca O, Harris CL, and Rodríguez de Córdoba S

Subjects

Adult, Complement C3 analysis, Complement C3-C5 Convertases physiology, Complement C3b metabolism, Complement Factor H metabolism, Female, Glomerulonephritis, Membranoproliferative etiology, Glomerulonephritis, Membranoproliferative immunology, Humans, Male, Middle Aged, Complement Activation, Complement C3 genetics, Glomerulonephritis, Membranoproliferative genetics, Mutation

Abstract

Dense deposit disease (DDD) is a severe renal disease characterized by accumulation of electron-dense material in the mesangium and glomerular basement membrane. Previously, DDD has been associated with deficiency of factor H (fH), a plasma regulator of the alternative pathway (AP) of complement activation, and studies in animal models have linked pathogenesis to the massive complement factor 3 (C3) activation caused by this deficiency. Here, we identified a unique DDD pedigree that associates disease with a mutation in the C3 gene. Mutant C(3923ΔDG), which lacks 2 amino acids, could not be cleaved to C3b by the AP C3-convertase and was therefore the predominant circulating C3 protein in the patients. However, upon activation to C3b by proteases, or to C3(H₂O) by spontaneous thioester hydrolysis, C(3923ΔDG) generated an active AP C3-convertase that was regulated normally by decay accelerating factor (DAF) but was resistant to decay by fH. Moreover, activated C(3b923ΔDG) and C3(H₂O)(923ΔDG) were resistant to proteolysis by factor I (fI) in the presence of fH, but were efficiently inactivated in the presence of membrane cofactor protein (MCP). These characteristics cause a fluid phase-restricted AP dysregulation in the patients that continuously activated and consumed C3 produced by the normal C3 allele. These findings expose structural requirements in C3 that are critical for recognition of the substrate C3 by the AP C3-convertase and for the regulatory activities of fH, DAF, and MCP, all of which have implications for therapeutic developments.

Published

2010

35. Differential activation of complement by apoptotic cells opsonized with anti-Ro60 and anti-La autoantibodies.

Author

Reed JH, Thurgood L, Gordon DL, and Gordon TP

Subjects

Complement C1q metabolism, Complement C3b metabolism, Complement Pathway, Classical immunology, Humans, Immunoglobulin G immunology, Jurkat Cells, T-Lymphocytes cytology, T-Lymphocytes metabolism, SS-B Antigen, Apoptosis immunology, Autoantibodies immunology, Autoantigens immunology, Complement Activation immunology, RNA, Small Cytoplasmic immunology, Ribonucleoproteins immunology, T-Lymphocytes immunology

Published

2010

36. Complement and alcoholic liver disease: role of C1q in the pathogenesis of ethanol-induced liver injury in mice.

Author

Cohen JI, Roychowdhury S, McMullen MR, Stavitsky AB, and Nagy LE

Subjects

Alanine Transaminase blood, Animals, Apoptosis drug effects, Aspartate Aminotransferases blood, Complement C1q deficiency, Complement C1q genetics, Complement C3b metabolism, Cytochrome P-450 CYP2E1 biosynthesis, Cytokines metabolism, Disease Models, Animal, Enzyme Induction, Fatty Liver chemically induced, Fatty Liver immunology, Female, Inflammation Mediators metabolism, Kupffer Cells immunology, Kupffer Cells pathology, Liver immunology, Liver pathology, Liver Diseases, Alcoholic genetics, Liver Diseases, Alcoholic pathology, Liver Diseases, Alcoholic prevention & control, Mice, Mice, Inbred C57BL, Mice, Knockout, Time Factors, Alcohol Drinking adverse effects, Complement Activation drug effects, Complement C1q metabolism, Ethanol toxicity, Kupffer Cells drug effects, Liver drug effects, Liver Diseases, Alcoholic immunology

Abstract

Background & Aims: Complement is involved in the development of alcoholic liver disease in mice; however, the mechanisms for complement activation during ethanol exposure have not been identified. C1q, the recognition subunit of the first complement component, binds to apoptotic cells, thereby activating the classical complement pathway. Because ethanol exposure increases hepatocellular apoptosis, we hypothesized that ethanol-induced apoptosis would lead to activation of complement via the classical pathway., Methods: Wild-type and C1qa-/- mice were allowed free access to ethanol-containing diets or pair-fed control diets for 4 or 25 days., Results: Ethanol feeding for 4 days increased apoptosis of Kupffer cells in both wild-type and C1qa-/- mice. Ethanol-induced deposition of C1q and C3b/iC3b/C3c was colocalized with apoptotic Kupffer cells in wild-type, but not C1qa-/-, mice. Furthermore, ethanol-induced increases in tumor necrosis factor-alpha and interleukin-6 expression at this early time point were suppressed in C1q-deficient mice. Chronic ethanol feeding (25 days) increased steatosis, hepatocyte apoptosis, and activity of serum alanine and aspartate aminotransferases in wild-type mice. These markers of hepatocyte injury were attenuated in C1qa-/- mice. In contrast, chronic ethanol (25 days)-induced increases in cytochrome P450 2E1 expression and oxidative stress did not differ between wild-type and C1qa-/- mice., Conclusions: For the first time, these data indicate that ethanol activates the classical complement pathway via C1q binding to apoptotic cells in the liver and that C1q contributes to the pathogenesis of ethanol-induced liver injury., (Copyright (c) 2010 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published

2010

37. An early complement-dependent and TLR-4-independent phase in the pathogenesis of ethanol-induced liver injury in mice.

Author

Roychowdhury S, McMullen MR, Pritchard MT, Hise AG, van Rooijen N, Medof ME, Stavitsky AB, and Nagy LE

Subjects

Alanine Transaminase metabolism, Animals, Complement C3b metabolism, Female, Immunity, Innate, Interferon-gamma metabolism, Interleukin-6 metabolism, Liver metabolism, Liver pathology, Mice, Mice, Inbred C57BL, Mice, Knockout, Receptor, Anaphylatoxin C5a metabolism, Receptors, Complement metabolism, Toll-Like Receptor 4 metabolism, Triglycerides metabolism, Complement Activation drug effects, Ethanol toxicity, Hepatitis, Alcoholic immunology, Kupffer Cells metabolism, Tumor Necrosis Factor-alpha metabolism

Abstract

Unlabelled: The innate immune system has been implicated in the pathogenesis of alcoholic liver disease. Although innate immunity is usually considered an early response to injury, previous work implicating innate immunity in ethanol-induced liver injury focuses primarily on long-term ethanol exposure. We investigated the early period of ethanol exposure to determine whether there were temporal associations between activation of innate immune responses and known correlates of liver injury. Female C57BL/6 mice were allowed free access to an ethanol-containing Lieber-DeCarli diet or were pair-fed a control diet. Within 4 days of ethanol exposure, we observed a striking spike in expression of hepatic proinflammatory cytokines-including tumor necrosis factor alpha (TNF-alpha), interleukin-6, and interferon-gamma-prior to hepatic triglyceride accumulation or increased plasma alanine aminotransferase activities, as well as before the induction of cytochrome P450 2E1 or oxidative stress. This early spike in inflammatory cytokines coincided with deposition of C3b-iC3b/C3c (C3b) in the liver. This deposition, resulting from the cleavage of the third component of the complement system (C3), is evidence for activation of complement in response to ethanol. C3(-/-) mice were protected from the early, ethanol-induced increase in hepatic TNF-alpha expression. Ethanol increased C3b deposition in mice deficient in C3a receptor or C5a receptor, as well as in wild-type mice depleted of hepatic macrophages; however, there was no increase in hepatic TNF-alpha in the absence of C3a receptor, C5a receptor, or hepatic macrophages. In contrast, the absence of Toll-like receptor 4 (TLR-4) had no effect on the early, ethanol-induced increase in either C3b or TNF-alpha., Conclusion: We have identified a complement- and macrophage-dependent, but TLR-4 independent, phase in the pathogenesis of ethanol-induced liver injury.

Published

2009

38. Acute antibody-mediated complement activation mediates lysis of pancreatic islets cells and may cause tissue loss in clinical islet transplantation.

Author

Tjernberg J, Ekdahl KN, Lambris JD, Korsgren O, and Nilsson B

Subjects

C-Peptide metabolism, Complement C3b metabolism, Cytotoxicity, Immunologic, Humans, Peptides, Cyclic pharmacology, Antibodies immunology, Complement Activation, Islets of Langerhans immunology, Islets of Langerhans Transplantation pathology

Abstract

Background: Clinical islet transplantation is associated with loss of transplanted islets necessitating tissue from more than one donor to obtain insulin independence. The instant blood-mediated inflammatory reaction (IBMIR) is one explanation to the tissue loss. Complement activation is an important cytotoxic component of the IBMIR, and in the present study, we have investigated this component in detail., Methods: Isolated human islets were analyzed by large particle flow cytometry and confocal microscopy after incubation in human ABO-compatible hirudin-plasma., Results: After incubation in plasma, the islets bound IgG and IgM, CIq, C4, C3 and C9. The binding of C3b/iC3b was evident already after 5 min. The binding of C3b/iC3b and the generation of C3a and sC5b-9 were inhibited by the complement inhibitor Compstatin. Lysis as reflected by propidium iodide (PI) staining and release of C-peptide was also inhibited by Compstatin. There were significant correlations between IgM/IgG versus C3b/iC3b and between sC5b-9 and C-peptide., Conclusion: The conclusion is that complement is activated by natural IgG and IgM antibodies already after 5 min. The complement activation leads to lysis of cells of the pancreatic islets. This very rapid reaction may be an essential entity of the damage induced by the IBMIR in clinical islet transplantation.

Published

2008

39. Human astrovirus coat protein inhibits serum complement activation via C1, the first component of the classical pathway.

Author

Bonaparte RS, Hair PS, Banthia D, Marshall DM, Cunnion KM, and Krishna NK

Subjects

Complement C3b metabolism, Complement C4b metabolism, Complement Membrane Attack Complex metabolism, Humans, Protein Binding, Capsid Proteins immunology, Complement Activation immunology, Complement C1q antagonists & inhibitors, Mamastrovirus immunology

Abstract

Human astroviruses (HAstVs) belong to a family of nonenveloped, icosahedral RNA viruses that cause noninflammatory gastroenteritis, predominantly in infants. Eight HAstV serotypes have been identified, with a worldwide distribution. While the HAstVs represent a significant public health concern, very little is known about the pathogenesis of and host immune response to these viruses. Here we demonstrate that HAstV type 1 (HAstV-1) virions, specifically the viral coat protein (CP), suppress the complement system, a fundamental component of the innate immune response in vertebrates. HAstV-1 virions and purified CP both suppress hemolytic complement activity. Hemolytic assays utilizing sera depleted of individual complement factors as well as adding back purified factors demonstrated that HAstV CP suppresses classical pathway activation at the first component, C1. HAstV-1 CP bound the A chain of C1q and inhibited serum complement activation, resulting in decreased C4b, iC3b, and terminal C5b-9 formation. Inhibition of complement activation was also demonstrated for HAstV serotypes 2 to 4, suggesting that this phenomenon is a general feature of these human pathogens. Since complement is a major contributor to the initiation and amplification of inflammation, the observed CP-mediated inhibition of complement activity may contribute to the lack of inflammation associated with astrovirus-induced gastroenteritis. Although diverse mechanisms of inhibition of complement activation have been described for many enveloped animal viruses, this is the first report of a nonenveloped icosahedral virus CP inhibiting classical pathway activation at C1.

Published

2008

40. Complement activation in Ghanaian children with severe Plasmodium falciparum malaria.

Author

Helegbe GK, Goka BQ, Kurtzhals JA, Addae MM, Ollaga E, Tetteh JK, Dodoo D, Ofori MF, Obeng-Adjei G, Hirayama K, Awandare GA, and Akanmori BD

Subjects

Age Factors, Anemia immunology, CD55 Antigens analysis, CD55 Antigens immunology, CD55 Antigens metabolism, Child, Child, Preschool, Complement Activation immunology, Complement C3b analysis, Complement C3b immunology, Complement C3b metabolism, Complement C3d analysis, Complement C3d immunology, Complement C3d metabolism, Coombs Test, Erythrocytes immunology, Flow Cytometry, Ghana, Hemoglobins analysis, Humans, Infant, Malaria, Cerebral immunology, Predictive Value of Tests, Receptors, Complement 3b analysis, Receptors, Complement 3b immunology, Receptors, Complement 3b metabolism, Respiratory Tract Diseases immunology, Statistics as Topic, Anemia etiology, Complement Activation physiology, Malaria, Cerebral etiology, Malaria, Falciparum immunology, Respiratory Tract Diseases etiology

Abstract

Background: Severe anaemia (SA), intravascular haemolysis (IVH) and respiratory distress (RD) are severe forms of Plasmodium falciparum malaria, with RD reported to be of prognostic importance in African children with malarial anaemia. Complement factors have been implicated in the mechanism leading to excess anaemia in acute P. falciparum infection., Methods: The direct Coombs test (DCT) and flow cytometry were used to investigate the mean levels of RBC-bound complement fragments (C3d and C3balphabeta) and the regulatory proteins [complement receptor 1 (CD35) and decay accelerating factor (CD55)] in children with discrete clinical forms of P. falciparum malaria. The relationship between the findings and clinical parameters including coma, haemoglobin (Hb) levels and RD were investigated., Results: Of the 484 samples tested, 131(27%) were positive in DCT, out of which 115/131 (87.8%) were positive for C3d alone while 16/131 (12.2%) were positive for either IgG alone or both. 67.4% of the study population were below 5 years of age and DCT positivity was more common in this age group relative to children who were 5 years or older (Odds ratio, OR = 3.8; 95%CI, 2.2-6.7, p < 0.001). DCT correlated significantly with RD (beta = -304, p = 0.006), but multiple regression analysis revealed that, Hb (beta = -0.341, p = 0.012) and coma (beta = -0.256, p = 0.034) were stronger predictors of RD than DCT (beta = 0.228, p = 0.061). DCT was also not associated with IVH, p = 0.19, while spleen size was inversely correlated with Hb (r = -402, p = 0.001). Flow cytometry showed similar mean fluorescent intensity (MFI) values of CD35, CD55 and C3balphabeta levels on the surfaces of RBC in patients and asymptomatic controls (AC). However, binding of C3balphabeta correlated significantly with CD35 or CD55 (p < 0.001)., Conclusion: These results suggest that complement activation contributed to anaemia in acute childhood P. falciparum malaria, possibly through induction of erythrophagocytosis and haemolysis. In contrast to other studies, this study did not find association between levels of the complement regulatory proteins, CD35 and CD55 and malarial anaemia. These findings suggest that complement activation could also be involved in the pathogenesis of RD but larger studies are needed to confirm this finding.

Published

2007

41. A mutation in factor I that is associated with atypical hemolytic uremic syndrome does not affect the function of factor I in complement regulation.

Author

Nilsson SC, Karpman D, Vaziri-Sani F, Kristoffersson AC, Salomon R, Provot F, Fremeaux-Bacchi V, Trouw LA, and Blom AM

Subjects

Adult, Child, Child, Preschool, Complement C3b genetics, Complement C3b metabolism, Complement C4b metabolism, DNA Mutational Analysis, Exons genetics, Female, Humans, Infant, Male, Recombinant Proteins genetics, Recombinant Proteins metabolism, Complement Activation genetics, Complement Factor I genetics, Complement Factor I metabolism, Hemolytic-Uremic Syndrome genetics, Hemolytic-Uremic Syndrome metabolism, Mutation, Missense

Abstract

Factor I (FI) is the major complement inhibitor that degrades C3b and C4b in the presence of cofactors such as factor H (FH) and membrane cofactor protein (MCP). Recently, mutations and polymorphisms in complement regulator molecules FH and MCP but also in FI have been associated with atypical hemolytic uremic syndrome (aHUS). HUS is a disorder characterized by hemolytic anemia, thrombocytopenia and acute renal failure. In this study, we report three unrelated patients with an identical heterozygous mutation, G261D, in the FI heavy chain who developed severe aHUS at different time points in their lives. Two of the patients also have polymorphisms in FH previously associated with risk of developing aHUS. Testing in particular one patient and control serum samples we did not observe major differences in complement hemolytic activity, FI plasma levels or the capability to degrade C4b or C3b. A recombinant protein was produced in order to analyze the functional consequences of the mutation. Mutant FI had a slightly different migration pattern during electrophoresis under reducing conditions. An alteration due to alternative splicing or glycosylation was ruled out, thus the altered migration may be due to proximity of the mutation to a cysteine residue. The recombinant mutant FI degraded C3b and C4b in a manner comparable to wild-type protein. In conclusion, despite the association between the heterozygous mutation in FI and aHUS we did not observe any abnormalities in the function of FI regarding complement regulation.

Published

2007

42. A simple, yet highly accurate, QSAR model captures the complement inhibitory activity of compstatin.

Author

Mulakala C, Lambris JD, and Kaznessis Y

Subjects

Complement C3b metabolism, Hydrophobic and Hydrophilic Interactions, Peptides, Cyclic antagonists & inhibitors, Peptides, Cyclic chemistry, Solvents, Complement Activation drug effects, Peptides, Cyclic pharmacology, Quantitative Structure-Activity Relationship

Abstract

Compstatin is a 13-residue cyclic peptide inhibitor of complement activation that was originally identified through phage-mediated presentation of a peptide library to C3b. Recent efforts to improve its activity have led to a rich dataset of complement analogs, with the most active analog being approximately 260 times more active than the parent compstatin. In the present work, a highly transparent quantitative structure-activity relationship model (Radj2=0.89) with four parameters is presented that captures important physico-chemical and geometrical properties of the analog molecules with regard to activity. The number of aromatic bonds and hydrophobicity of the fourth residue of compstatin correlated strongly with activity. Also important were the hydrophobic patch size near the disulfide bond and the solvent-accessible surface area occupied by nitrogen atoms of basic amino acid residues.

Published

2007

43. Cooperation between MASP-1 and MASP-2 in the generation of C3 convertase through the MBL pathway.

Author

Møller-Kristensen M, Thiel S, Sjöholm A, Matsushita M, and Jensenius JC

Subjects

Animals, Complement C3b metabolism, Humans, Mannose-Binding Lectins metabolism, Mice, Mice, Knockout, Complement Activation physiology, Complement C3-C5 Convertases biosynthesis, Mannose-Binding Lectin metabolism, Mannose-Binding Protein-Associated Serine Proteases metabolism

Abstract

The complement system is an important part of the innate immune system. Three pathways, the classical, the alternative and the lectin pathway, lead to the cleavage of complement factor C3, a central event in the activation of the complement system. We investigated the deposition of C3b (solid-phase C3 activation product) on a mannan-coated surface at high concentration of human serum (17%). At these conditions, mannan-binding lectin (MBL) promoted the activation of C3 through the combined action of MBL-associated serine protease (MASP)-1 and MASP-2 without appreciable involvement of the alternative pathway. In serum depleted of MASP-1, MASP-2 and MASP-3, we observed synergetic effect of reconstitution with MASP-1 and MASP-2. This was inhibited by MASP-3. No C3b deposition was observed with C2- or C4-depleted serum. Depletion of factor B had no effect on the MBL-MASP-promoted C3b deposition. Our results demonstrate a function of the orphan protease MASP-1 by providing evidence that this enzyme collaborates with MASP-2 in the generation of C3 convertase, a process observable at high serum concentration, but not at low serum concentration.

Published

2007

44. The structure of complement C3b provides insights into complement activation and regulation.

Author

Abdul Ajees A, Gunasekaran K, Volanakis JE, Narayana SV, Kotwal GJ, and Murthy HM

Subjects

Animals, Binding Sites, Crystallography, X-Ray, Humans, Models, Molecular, Protein Conformation, Rats, Structure-Activity Relationship, Complement Activation, Complement C3b chemistry, Complement C3b metabolism

Abstract

The human complement system is an important component of innate immunity. Complement-derived products mediate functions contributing to pathogen killing and elimination. However, inappropriate activation of the system contributes to the pathogenesis of immunological and inflammatory diseases. Complement component 3 (C3) occupies a central position because of the manifold biological activities of its activation fragments, including the major fragment, C3b, which anchors the assembly of convertases effecting C3 and C5 activation. C3 is converted to C3b by proteolysis of its anaphylatoxin domain, by either of two C3 convertases. This activates a stable thioester bond, leading to the covalent attachment of C3b to cell-surface or protein-surface hydroxyl groups through transesterification. The cleavage and activation of C3 exposes binding sites for factors B, H and I, properdin, decay accelerating factor (DAF, CD55), membrane cofactor protein (MCP, CD46), complement receptor 1 (CR1, CD35) and viral molecules such as vaccinia virus complement-control protein. C3b associates with these molecules in different configurations and forms complexes mediating the activation, amplification and regulation of the complement response. Structures of C3 and C3c, a fragment derived from the proteolysis of C3b, have revealed a domain configuration, including six macroglobulin domains (MG1-MG6; nomenclature follows ref. 5) arranged in a ring, termed the beta-ring. However, because neither C3 nor C3c is active in complement activation and regulation, questions about function can be answered only through direct observations on C3b. Here we present a structure of C3b that reveals a marked loss of secondary structure in the CUB (for 'complement C1r/C1s, Uegf, Bmp1') domain, which together with the resulting translocation of the thioester domain provides a molecular basis for conformational changes accompanying the conversion of C3 to C3b. The total conformational changes make many proposed ligand-binding sites more accessible and create a cavity that shields target peptide bonds from access by factor I. A covalently bound N-acetyl-l-threonine residue demonstrates the geometry of C3b attachment to surface hydroxyl groups.

Published

2006

45. Structure of C3b in complex with CRIg gives insights into regulation of complement activation.

Author

Wiesmann C, Katschke KJ, Yin J, Helmy KY, Steffek M, Fairbrother WJ, McCallum SA, Embuscado L, DeForge L, Hass PE, and van Lookeren Campagne M

Subjects

Complement C3-C5 Convertases antagonists & inhibitors, Complement C3-C5 Convertases metabolism, Complement C3c chemistry, Complement C3c metabolism, Complement C5 antagonists & inhibitors, Complement C5 metabolism, Crystallography, X-Ray, Humans, Models, Molecular, Mutation genetics, Protein Binding, Protein Conformation, Receptors, Complement genetics, Receptors, Complement 3b, Structure-Activity Relationship, Complement Activation, Complement C3b chemistry, Complement C3b metabolism, Receptors, Complement chemistry, Receptors, Complement metabolism

Abstract

The complement system is a key part of the innate immune system, and is required for clearance of pathogens from the bloodstream. After exposure to pathogens, the third component of the complement system, C3, is cleaved to C3b which, after recruitment of factor B, initiates formation of the alternative pathway convertases. CRIg, a complement receptor expressed on macrophages, binds to C3b and iC3b mediating phagocytosis of the particles, but it is unknown how CRIg selectively recognizes proteolytic C3-fragments and whether binding of CRIg to C3b inhibits convertase activation. Here we present the crystal structure of C3b in complex with CRIg and, using CRIg mutants, provide evidence that CRIg acts as an inhibitor of the alternative pathway of complement. The structure shows that activation of C3 induces major structural rearrangements, including a dramatic movement (>80 A) of the thioester-bond-containing domain through which C3b attaches to pathogen surfaces. We show that CRIg is not only a phagocytic receptor, but also a potent inhibitor of the alternative pathway convertases. The structure provides insights into the complex macromolecular structural rearrangements that occur during complement activation and inhibition. Moreover, our structure-function studies relating the structural basis of complement activation and the means by which CRIg inhibits the convertases provide important clues to the development of therapeutics that target complement.

Published

2006

46. Critical role of the C-terminal domains of factor H in regulating complement activation at cell surfaces.

Author

Ferreira VP, Herbert AP, Hocking HG, Barlow PN, and Pangburn MK

Subjects

Animals, Binding Sites, Binding, Competitive, Complement Factor H genetics, Erythrocytes immunology, Hemolysis immunology, Humans, Protein Structure, Tertiary genetics, Protein Structure, Tertiary physiology, Recombinant Proteins genetics, Recombinant Proteins metabolism, Complement Activation, Complement C3b metabolism, Complement Factor H metabolism, Erythrocyte Membrane immunology

Abstract

The plasma protein factor H primarily controls the activation of the alternative pathway of complement. The C-terminal of factor H is known to be involved in protection of host cells from complement attack. In the present study, we show that domains 19-20 alone are capable of discriminating between host-like and complement-activating cells. Furthermore, although factor H possesses three binding sites for C3b, binding to cell-bound C3b can be almost completely inhibited by the single site located in domains 19-20. All of the regulatory activities of factor H are expressed by the N-terminal four domains, but these activities toward cell-bound C3b are inhibited by isolated recombinant domains 19-20 (rH 19-20). Direct competition with the N-terminal site is unlikely to explain this because regulation of fluid phase C3b is unaffected by domains 19-20. Finally, we show that addition of isolated rH 19-20 to normal human serum leads to aggressive complement-mediated lysis of normally nonactivating sheep erythrocytes and moderate lysis of human erythrocytes, which possess membrane-bound regulators of complement. Taken together, the results highlight the importance of the cell surface protective functions exhibited by factor H compared with other complement regulatory proteins. The results may also explain why atypical hemolytic uremic syndrome patients with mutations affecting domains 19-20 can maintain complement homeostasis in plasma while their complement system attacks erythrocytes, platelets, endothelial cells, and kidney tissue.

Published

2006

47. The complement system plays a critical role in the development of experimental autoimmune anterior uveitis.

Author

Jha P, Sohn JH, Xu Q, Nishihori H, Wang Y, Nishihori S, Manickam B, Kaplan HJ, Bora PS, and Bora NS

Subjects

Adoptive Transfer, Animals, Blotting, Western, Cell Adhesion Molecules metabolism, Chemokines genetics, Complement C3b metabolism, Cytokines genetics, Disease Progression, Enzyme-Linked Immunosorbent Assay, Fluorescent Antibody Technique, Indirect, Macrophage-1 Antigen metabolism, Male, RNA, Messenger metabolism, Rats, Rats, Inbred Lew, Reverse Transcriptase Polymerase Chain Reaction, Autoimmune Diseases immunology, Complement Activation immunology, Complement System Proteins physiology, Disease Models, Animal, Uveitis, Anterior immunology

Abstract

Purpose: The role of complement in ocular autoimmunity was explored in a experimental autoimmune anterior uveitis (EAAU) animal model., Methods: EAAU was induced in Lewis rats by immunization with bovine melanin-associated antigen. Complement activation in the eye was monitored by Western blot for iC3b. The importance of complement to the development of EAAU was studied by comparing the course of intraocular inflammation in normal Lewis rats (complement-sufficient) with cobra venom factor-treated rats (complement-depleted). Eyes were harvested from both complement-sufficient and complement-depleted rats for mRNA and protein analysis for IFN-gamma, IL-10, and interferon-inducible protein (IP)-10. Intracellular adhesion molecule (ICAM)-1 and leukocyte-endothelial cell adhesion molecule (LECAM)-1 were detected by immunofluorescent staining. OX-42 was used to investigate the importance of iC3b and CR3 interaction in EAAU., Results: There was a correlation between ocular complement activation and disease progression in EAAU. The incidence, duration, and severity of disease were dramatically reduced after active immunization in complement-depleted rats. Complement depletion also completely suppressed adoptive transfer EAAU. The presence of complement was critical for local production of cytokines (IFN-gamma and IL-10), chemokines (IP-10), and adhesion molecules (ICAM-1 and LECAM-1) during EAAU. Furthermore, intraocular complement activation, specifically iC3b production and engagement of complement receptor 3 (CR3), had a significant impact on disease activity in EAAU., Conclusions: The study provided the novel finding that complement activation plays a central role in the pathogenesis of ocular autoimmunity and may serve as a potential target for therapeutic intervention.

Published

2006

48. Investigation of the mechanisms of anti-complement activity in Ixodes ricinus ticks.

Author

Lawrie CH, Sim RB, and Nuttall PA

Subjects

Animals, Complement C3 Convertase, Alternative Pathway, Complement C3a antagonists & inhibitors, Complement C3a metabolism, Complement C3b drug effects, Complement C3b metabolism, Complement Factor B antagonists & inhibitors, Complement Factor B metabolism, Erythrocytes immunology, Erythrocytes parasitology, Humans, Ixodes pathogenicity, Peptide Fragments drug effects, Peptide Fragments metabolism, Rabbits, Cell Extracts pharmacology, Complement Activation drug effects, Ixodes immunology, Salivary Glands chemistry

Abstract

The feeding success of a tick upon a host depends on its ability to suppress host anti-tick responses which include activation of the complement system. We investigated the mechanism of inhibition of the alternative pathway of complement by salivary gland extract (SGE) of the ixodid tick species, Ixodes ricinus. SGE treatment strongly inhibited C3a generation and factor B cleavage in serum when rabbit erythrocytes were used as complement activator, but not when cobra venom factor (CVF) was used as an activator. SGE treatment strongly inhibited C3b deposition on rabbit erythrocytes, and the turnover of C3 (to C3b/iC3b) in serum. However, there was no significant effect upon the formation, stability or activity of C3 convertase (C3bBb) when formed from purified C3b, factor B and factor D. SGE treatment of isolated C3 resulted in a shift in mobility of the alpha-chain (by about 5 kDa). N-terminal sequencing of this species suggests that cleavage occurs at the C-terminus of the alpha-chain of C3. Consistent with this hypothesis, the modified alpha-chain was still a substrate for pre-formed convertase. The activity was specific for the alpha-chain of C3 but not of C3(H2O) nor the alpha'-chain of C3b. It is proposed that SGE-modified C3 does not participate in convertase formation, probably having a reduced affinity for factor B.

Published

2005

49. Human leukocyte antigen antibodies and human complement activation: role of IgG subclass, specificity, and cytotoxic potential.

Author

Kushihata F, Watanabe J, Mulder A, Claas F, and Scornik JC

Subjects

Antibodies, Monoclonal immunology, Complement C3 metabolism, Complement C3b metabolism, Humans, Immunoglobulin G classification, Antibody Specificity, Complement Activation, Cytotoxicity, Immunologic, HLA Antigens immunology, Immunoglobulin G physiology, Isoantibodies physiology

Abstract

Background: Human leukocyte antigen (HLA) antibodies are defined as complement (C) fixing and clinically relevant based upon the complement-dependent cytotoxicity (CDC) test. However, the sub-lytic activation of individual C components is of critical biologic significance. The requirements of HLA antibodies to activate human C are not known., Methods: IgG, IgM, IgG subclasses, and human C3b deposition upon T cells were evaluated by flow cytometry with sera from HLA-sensitized patients and human monoclonal HLA antibodies., Results: Comparative studies showed that there was poor correlation between the amount of IgG on target cells and their ability to produce CDC. Human C3b deposition was influenced more by the particular serum/cell combination under study than by the amount of IgG, with some combinations showing high IgG and low C3b and others showing low IgG and high C3b. IgG1 was the predominant IgG subclass in all patients. The other subclasses were low or undetectable and did not correlate with C3b deposition. Human monoclonal HLA antibodies, mostly IgG1, did not activate human C efficiently despite high IgG binding. However, combinations of two monoclonal antibodies to different epitopes of the same antigen did produce significant C3b deposition., Conclusions: Contrary to common assumptions, CDC, IgG binding, and IgG subclass are poor predictors of human C activation by HLA antibodies. The mix of specificities in a given serum and the antigens of a particular target cell appear to determine the efficiency of C activation. Measuring both antibody and C3b deposition (or other C component) may improve the assessment of donor-recipient compatibility.

Published

2004

50. C3b2-IgG complexes retain dimeric C3 fragments at all levels of inactivation.

Author

Jelezarova E, Luginbuehl A, and Lutz HU

Subjects

Blood immunology, Dimerization, Esters, Humans, Hydrolysis, Immunoglobulin G metabolism, Protein Binding, Receptors, Complement metabolism, Complement Activation, Complement C3b chemistry, Complement C3b metabolism, Immunoglobulin G chemistry, Peptide Fragments metabolism

Abstract

C3b2-IgG complexes are formed during complement activation in serum by attachment of two C3b molecules (the proteolytically activated form of C3) to one IgG heavy chain (IgG HC) via ester bonds. Because of the presence of two C3b molecules, these complexes are very efficient activators of the alternative complement pathway. Likewise, dimeric C3b is known to enhance complement receptor 1-dependent phagocytosis, and dimeric C3d (the smallest thioester-containing fragment of C3) linked to a protein antigen facilitates CR2-dependent B-cell proliferation. Because the efficiency of all these interactions depends on the number of C3 fragments, we investigated whether C3b2-IgG complexes retained dimeric structure upon physiological inactivation. We used two-dimensional SDS-PAGE and Western blot to study the arrangement of the C3b molecules by analyzing the fragmentation pattern after cleavage of the ester bonds. Upon inactivation with factors H and I, a 185-kDa band was generated under reducing conditions. It released IgG HC and the 65-kDa fragment of C3b alpha' chain after hydrolysis of the ester bonds with hydroxylamine. The two C3b molecules were not 65-kDa-to-40-kDa linked, because neither ester-bonded 65 kDa HC nor 65 kDa-40 kDa fragments were observed, nor was a 40-kDa peptide released after hydroxylamine cleavage. Factor I and CR1 cleaved the C3b2-IgG molecule to its final physiological product, C3dg2-IgG, which migrated as a 133-kDa fragment in reduced form. This fragment released exclusively C3dg (the final physiological product of C3b inactivation by factor I) and IgG HC. C3dg2-HC appeared as a double band on SDS-PAGE only at low gel porosity, suggesting the presence of two conformers of the same composition. Our results suggest that, upon physiological inactivation, C3b2-IgG complexes retain dimeric inactivated C3b and C3dg, which allows bivalent binding to the corresponding complement receptors.

Published

2003